ANNUAL REPORT
2024
GLOBAL LEADER IN ALLOGENEIC
CELLULAR MEDICINES FOR
INFLAMMATORY DISEASES
CORPORATE GOVERNANCE
Mesoblast Limited and its Board of Directors are committed to implementing and achieving an effective corporate
governance framework to ensure that the Company is managed effectively and in an honest and ethical way.
The Company’s Corporate Governance Statement for the financial year ending 30 June 2024 has been approved
by the Board and is available on our website at www.mesoblast.com/company/corporate-governance
CONTENTS
MESSAGE FROM THE CHAIR
1
CHIEF EXECUTIVE’S REPORT
2
FORM 20-F
5
SHAREHOLDER INFORMATION
247
CORPORATE DIRECTORY
249
MESOBLAST LIMITED 2024 ANNUAL REPORT 1
MESSAGE FROM THE CHAIR
Dear fellow shareholders,
I am pleased to deliver my first report to you as Chair for
the financial year ended 30 June 2024, marking another
year of significant milestones and progress for Mesoblast.
This year has seen our Company go from strength to
strength as a leading developer of innovative allogeneic
cellular medicines with an extensive clinical-stage pipeline
of therapeutic assets validated by clinical data that address
serious and life-threatening inflammatory illnesses.
We are making great progress in advancing the pipeline of
late-stage product candidates targeting key areas such as
cardiovascular disease, chronic low back pain, and acute life-
threatening inflammatory conditions including graft versus
host disease (GvHD). Through the leadership of our Chief
Executive Officer and Managing Director (CEO and MD),
Dr Silviu Itescu and his team we have made tremendous
strides in the past year in our engagement with regulators,
in clinical development of our lead products, and in
preparedness for product commercialization.
2024 has been pivotal in our journey toward
commercializing our therapies. Our positive interactions
with the United States Food and Drug Administration (FDA)
allowed us to resubmit the Biologics License Application
(BLA) for approval of Ryoncil® (remestemcel-L) for steroid-
refractory acute GvHD in children, and work towards filing
for accelerated approval of Revascor® (rexlemestrocel-L) in
end-stage heart failure patients. In addition, we commenced
a pivotal Phase 3 trial of rexlemestrocel-L for chronic low
back pain and expect to accelerate patient enrollment
across multiple centers in the U.S. over the coming year.
Our focus has turned to implementing the
commercialization strategies that will allow us to
successfully launch RYONCIL, a much-needed treatment
for desperately ill children, early in 2025 upon FDA
approval.
Our balance sheet has been well-managed, including
recently securing access to US$50 million to fund our
planned commercial launch and ongoing operational
activities, while at the same time maintaining financial
discipline through the implementation of cost reduction
strategies to maximize our financial runway. Prudent
financial management combined with strategic
partnerships and non-dilutive financing opportunities
will continue to facilitate the Company’s pursuit of our
ambitious objectives while enhancing shareholder value.
As we plan for 2025 and beyond, I am very optimistic
about Mesoblast’s future. The strength of our science,
the dedication of our impressive team, and the support
of our shareholders position us to achieve our goal of
delivering transformative therapies to patients in need.
I would like to express my sincere gratitude to our
shareholders for your continued trust and support. Your
belief in our vision drives us forward and strengthens our
resolve to bring our breakthrough therapies to market.
Furthermore, I wish to thank my fellow Directors, our
CEO and MD, Dr Silviu Itescu for his strong commitment
to and leadership of Mesoblast, our executive team, and
employees whose unwavering commitment to innovation
and excellence makes everything we accomplish possible.
Lastly, I would like to acknowledge the significant
contribution from my predecessor and retiring board
member Mr Joseph Swedish who admirably chaired the
Company from 2019 to April 2024.
Together, we are on the cusp of realizing the full potential
of Mesoblast’s transformative allogeneic cellular medicines,
and I look forward to sharing our success with you in the
year ahead.
Yours sincerely,
Jane C. Bell AM
Chair of the Board
Jane C. Bell AM
Chair of the Board
CHIEF EXECUTIVE’S REPORT
Dr Silviu Itescu
Chief Executive Officer and Managing Director
2 MESOBLAST LIMITED 2024 ANNUAL REPORT
Dear shareholders,
It is with a great sense of purpose that I present to you
the 2024 Chief Executive’s Report. This has been a
defining year for Mesoblast as we prepare for launch and
commercialization of what we anticipate will be our first
approved product in the United States.
Tremendous progress has been made in the past year in
advancing our late-stage pipeline of innovative cellular
medicines for patients suffering from some of the most
serious or life-threatening inflammatory diseases such as
acute graft versus host disease (GvHD), ischemic heart
failure, and discogenic back pain.
We are now implementing our go-to-market
commercialization plan that will allow us to successfully
bring Ryoncil® (remestemcel-L), a much-needed treatment
for desperately ill children with acute steroid-refractory
GvHD following allogeneic bone marrow transplantation,
to market early in 2025 upon United States Food and Drug
Administration (FDA) approval.
Our balance sheet has been well-managed, having recently
secured access to US$50 million to fund our planned
commercial launch and ongoing operational activities,
while at the same time maintaining financial discipline
to implement cost reduction strategies and maximize
operational runway.
Operational Highlights: Bringing Our Innovative
Therapies to Patients with Serious or Life-Threatening
Inflammatory Diseases
Over the past year, we have achieved critical milestones
that position us for success. Our focus remains on
commercializing our products that are in Phase 3 or beyond,
with a particular emphasis on the following key areas:
1. Remestemcel-L (RYONCIL) for steroid-refractory
acute GvHD in children
2. Remestemcel-L (RYONCIL) for steroid-refractory
acute GvHD in adults
3. Rexlemestrocel-L (Revascor®) for children with
hypoplastic left heart syndrome
4. Rexlemestrocel-L (REVASCOR) for adults with
advanced inflammatory heart failure with low
ejection fraction
5. Rexlemestrocel-L (MPC-06-ID) for chronic low
back pain due to inflammatory disc disease
RYONCIL (remestemcel-L) for Acute GvHD in
Children and Adults
Survival outcomes have not improved over the past two
decades for children or adults with steroid-refractory acute
GvHD despite a first FDA approval in adults more than
three years ago, meaning there remains a major need for a
safe and effective therapy in children and adults with the
most severe forms of this disease. There are no approved
treatments for children under 12 with steroid-refractory
acute GvHD, making approval in this vulnerable population
the most urgent need.
Earlier this year the FDA informed Mesoblast that the
available clinical data from its Phase 3 study in children with
steroid-refractory acute GvHD appears sufficient to support
resubmission of the RYONCIL Biologics License Application
(BLA). FDA accepted the BLA resubmission within two
weeks, considering it to be a complete response, and is
currently in an active review process involving ongoing
interactions with Mesoblast. FDA has already conducted the
Pre-License Inspection (PLI) of the manufacturing process
for RYONCIL in May 2023 and this did not result in the
issuance of any Form 483. We anticipate a decision prior to
or on the FDA’s Prescription Drug User Fee Act (PDUFA)
goal date of January 7, 2025.
Our label extension strategy for RYONCIL in adults is to
target the 40-45% of patients with steroid-refractory acute
GvHD who fail second-line therapy, including the only
approved agent in these patients, ruxolitinib. While survival
in these patients is a dismal 20-30% by 100 days, use of
RYONCIL under expanded access has resulted in >70%
survival rates.
Mesoblast is collaborating with the Blood and Marrow
Transplant Clinical Trials Network (BMT CTN) in the United
States, a body that is funded by the National Institutes
of Health (NIH) and is responsible for approximately 80%
of all US allogeneic bone marrow transplants, to conduct a
pivotal trial in this adult population.
Commercial Pathway: Preparing for Successful Launch
and Beyond
We have been working diligently to lay the groundwork for
a successful launch of RYONCIL to treat steroid-refractory
acute GvHD in children. This includes hiring select senior
positions to implement a targeted commercial strategy. Key
pre-launch activities focusing on non-promotional activities
include market access initiatives, payer engagement,
MESOBLAST LIMITED 2024 ANNUAL REPORT 3
identification, profiling, and targeting plans for center
roll-out, and maintaining key opinion leader (KOL)
relationships with experience using RYONCIL.
Post-launch implementation of a staged approach will
initially be based on centers with highest volume and
experience using the RYONCIL product. This will be
implemented using a targeted sales force focussing initially
on the 15 highest volume centers which account for
approximately 50% of pediatric transplant patients, with
staged rollout beyond. We have built our inventory and
have an established supply chain to ensure cryopreserved
product is available for delivery to meet the needs of each
site immediately post approval, with ability to scale up as
necessary going forward.
REVASCOR (rexlemestrocel-L) for Pediatric Congenital
Heart Disease
During the year FDA granted REVASCOR both Rare
Pediatric Disease Designation and Orphan-Drug Designation
for the treatment of hypoplastic left heart syndrome
(HLHS), a condition responsible for up to 40% of all
neonatal cardiac mortality.
Results from a randomized, placebo-controlled prospective
trial of REVASCOR conducted in the United States in
children with HLHS were published in the December
2023 issue of the peer reviewed The Journal of Thoracic
and Cardiovascular Surgery Open (JTCVS Open). A single
intramyocardial administration of REVASCOR at the
time of staged surgery resulted in the desired outcome
of significantly larger increases in left ventricular
(LV) end-systolic and end-diastolic volumes over 12
months compared with controls as measured by 3D
echocardiography (p=0.009 & p=0.020 respectively). These
changes are indicative of clinically important growth of
the small left ventricle, facilitating the ability to have a
successful surgical correction, known as full biventricular
(BiV) conversion, which allows for a normal two ventricle
circulation. Without full BiV conversion the right heart
chamber is under excessive strain with increased risk of
heart failure and death.
On potential FDA approval of a BLA for REVASCOR for the
treatment of HLHS, Mesoblast may be eligible to receive
a Priority Review Voucher that can be redeemed for any
subsequent marketing application or may be sold or
transferred to a third party.
REVASCOR (rexlemestrocel-L) for Chronic Heart
Failure with Reduced Ejection Fraction and Persistent
Inflammation
Chronic heart failure remains one of society’s greatest
unmet medical needs affecting approximately 6.5 million
people in the U.S. and 26 million people globally with
increasing prevalence and incidence. Heart failure with low
ejection fraction (HFrEF) occurs in approximately 50% of all
heart failure patients and is associated with high mortality.
Over 60% of HFrEF patients have underlying ischemia and
these are at highest risk of major adverse cardiac events
(MACE, cardiovascular death, heart attacks or strokes).
Earlier this year, FDA informed Mesoblast that it supports
an accelerated approval pathway for its second generation
allogeneic, STRO3-immunoselected, and industrially
manufactured stromal cell product REVASCOR for
patients with end-stage ischemic HFrEF kept alive by a left
ventricular assist device (LVAD). This followed presentation
to FDA of the results of two complementary randomized
controlled trials of REVASCOR, one in patients with end-
stage HFrEF and LVADs and a second in advanced NYHA
class II/III HFrEF patients.
In results of the trial in NYHA class II/III HFrEF patients
published last year in the premier peer-reviewed journal for
cardiovascular medicine, the Journal of the American College
of Cardiology (JACC), REVASCOR significantly reduced
MACE in patients with inflammation.
Mesoblast has received Regenerative Medicine
Advanced Therapy (RMAT) designation for REVASCOR
(rexlemestrocel-L) in the treatment of end-stage heart
failure in patients kept alive with an LVAD. Mesoblast
intends to meet with FDA to discuss timing and FDA
expectations for an accelerated approval filing in these
patients.
Rexlemestrocel-L for Chronic Low Back Pain (CLBP)
Associated with Inflammatory Disc Disease
The confirmatory Phase 3 trial of Mesoblast’s second
generation allogeneic, STRO3-immunoselected,
and industrially manufactured stromal cell product
rexlemestrocel-L in patients with CLBP due to inflammatory
degenerative disc disease of less than five years duration
has commenced enrollment at multiple sites across the
United States.
4 MESOBLAST LIMITED 2024 ANNUAL REPORT
The FDA has previously agreed on the design of this
300-patient randomized, placebo-controlled confirmatory
Phase 3 trial, and the 12-month primary endpoint of pain
reduction as an approvable indication. This endpoint was
successfully met in Mesoblast’s first Phase 3 trial. Key
secondary measures include improvement in quality of
life and function.
A particular focus is on treatment of patients on opioids,
since discogenic back pain accounts for approximately
50% of prescription opioid usage in the US. Significant
pain reduction and opioid cessation were observed in
Mesoblast’s first Phase 3 trial.
Last year rexlemestrocel-L received RMAT designation
from FDA for the treatment of chronic low back pain.
RMAT designation provides all the benefits of Breakthrough
and Fast Track designations, including rolling review and
eligibility for priority review on filing of a BLA.
Strategic Partnerships and Collaborations
Strategic partnerships have been pivotal to our progress.
Our collaborations with pharmaceutical companies,
academic institutions, and research networks have helped
accelerate development timelines and will potentially
expand our market reach. We continue to explore
opportunities for co-development and licensing agreements
that broaden market reach for our products, enhance
development of our pipeline, and create long-term value
for shareholders.
Financial Management: A Disciplined Approach
This year, we have continued to adopt a disciplined approach
to our financial management. Our capital strategy has been
focused on ensuring that we are well-positioned to execute
our clinical, manufacturing, and commercialization plans.
Through targeted fundraising initiatives and successful
implementation of our strategic cost management plan,
we strengthened our balance sheet in 2024, extending our
operational runway. We will continue to explore a variety
of funding avenues, including non-dilutive capital and
strategic partnerships, to support the launch and global
expansion of our lead assets.
To ensure that the Company is well capitalized for a
commercial launch of RYONCIL, we recently entered into
a convertible note subscription agreement with our largest
shareholder for issue, at Mesoblast’s sole discretion, up
to US$50.0 million (A$72.7 million) convertible notes on
approval of RYONCIL by FDA.
Building a Sustainable Future
Sustainability and responsible corporate stewardship
remain core to our ethos. As we move forward, we are
committed to ensuring that our therapies not only
transform patient lives but also contribute to the broader
health and well-being of society. This includes ongoing work
in responsible manufacturing practices, access to medicines,
environmental sustainability, and our dedication to ethical
standards in all facets of our operations.
Looking Ahead: A Transformative Year Awaits
As we approach 2025, I believe Mesoblast is on the
verge of gaining a first approval in the U.S. which will
be transformative for our company. With an approval
from FDA potentially just months away, and our plans
for commercialization in train, we are closer than ever to
achieving our goal of making a meaningful difference in
the lives of children suffering from acute steroid-refractory
GvHD.
Our vision is ambitious, but it is also within reach, thanks
to the unwavering dedication of our talented team, the
strategic partnerships we have cultivated, and the support
of our investors and shareholders. I am confident that the
steps we have taken in 2024 have laid a solid foundation for
sustained growth and long-term success.
I would like to extend my sincere gratitude to our
employees for their hard work and passion, to my fellow
directors for their oversight and invaluable input, and to
you, our shareholders, for your continued trust and support.
Together, we are building a company that not only leads in
allogeneic cellular medicine but also improves the lives of
countless patients worldwide.
Thank you for being part of our journey.
Yours sincerely,
Dr Silviu Itescu
Chief Executive Officer and Managing Director
UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
WASHINGTON, D.C. 20549
______________________________
FORM 20-F
______________________________
o
REGISTRATION STATEMENT PURSUANT TO SECTION 12(b) OR (g) OF THE SECURITIES EXCHANGE ACT OF 1934
OR
x
ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
For the fiscal year ended June 30, 2024
OR
o
TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
OR
o
SHELL COMPANY REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
Date of event requiring this shell company report
For the transition period from ______ to ______
Commission file number 001-37626
______________________________
MESOBLAST LIMITED
(Exact name of Registrant as specified in its charter)
______________________________
N/A
(Translation of Registrant’s name into English)
AUSTRALIA
(Jurisdiction of incorporation or organization)
Level 38, 55 Collins Street
Melbourne, VIC, 3000, Australia
Telephone: +61 (3) 9639 6036
(Address of principal executive offices)
Silviu Itescu
Chief Executive Officer
Telephone: +61 (3) 9639 6036; Fax: +61 (3) 9639 6030
Level 38, 55 Collins Street
Melbourne, VIC, 3000, Australia
(Name, Telephone, E-mail and/or Facsimile number and Address of Company Contact Person)
Securities registered or to be registered pursuant to Section 12(b) of the Act.
Title of each class
Trading Symbol(s)
Name of each exchange on which registered
American Depositary Shares, each representing ten Ordinary
Shares*
MESO
The NASDAQ Global Select Market
Securities registered or to be registered pursuant to Section 12(g) of the Act.
None
Securities for which there is a reporting obligation pursuant to Section 15(d) of the Act.
None
______________________________
Indicate the number of outstanding shares of each of the issuer’s classes of capital or common stock as of the close of the period covered by the annual report.
1,141,784,114 Ordinary Shares
Indicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act.
o Yes x No
If this report is an annual or transition report, indicate by check mark if the registrant is not required to file reports pursuant to Section 13 or 15(d) of the Securities
Exchange Act of 1934.
o Yes x No
Indicate by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during the
preceding 12 months (or for such shorter period that the registrant was required to file such reports), and (2) has been subject to such filing requirements for the past 90 days.
x Yes o No
Indicate by check mark whether the registrant has submitted electronically every Interactive Data File required to be submitted pursuant to Rule 405 of Regulation S-T
(§232.405 of this chapter) during the preceding 12 months (or for such shorter period that the registrant was required to submit such files).
x Yes o No
Table of Contents
Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, or a non-accelerated filer, or an emerging growth company. See
definition of “large accelerated filer,” “accelerated filer,” and “emerging growth company” in Rule 12b-2 of the Exchange Act. (Check one):
Large accelerated filer
o
Accelerated filer
x
Non-accelerated filer
o
Emerging growth company
o
If an emerging growth company that prepares its financial statements in accordance with U.S. GAAP, indicate by check mark if the registrant has elected not to use the
extended transition period for complying with any new or revised financial accounting standards† provided pursuant to Section 13(a) of the Exchange Act. o
Indicate by check mark whether the registrant has filed a report on and attestation to its management’s assessment of the effectiveness of its internal control over
financial reporting under Section 404(b) of the Sarbanes-Oxley Act (15 U.S.C. 7262(b)) by the registered public accounting firm that prepared or issued its audit report.x
If securities are registered pursuant to Section 12(b) of the Act, indicate by check mark whether the financial statements of the registrant included in the filing reflect
the correction of an error to previously issued financial statements. o
Indicate by check mark whether any of those error corrections are restatements that required a recovery analysis of incentive based compensation received by any of
the registrant’s executive officers during the relevant recovery period pursuant to §240.10D-1(b). o
Indicate by check mark which basis of accounting the registrant has used to prepare the financial statements included in this filing:
U.S. GAAP
o
International Financial Reporting Standards as issued by the International
Accounting Standards Board
x
Other
o
If “Other” has been checked in response to the previous question, indicate by check mark which financial statement item the registrant has elected to follow.
Item 17 o Item 18 o
If this is an annual report, indicate by check mark whether the registrant is a shell company (as defined in Rule 12b-2 of the Exchange Act).
o Yes x No
Table of Contents
Table of Contents
INTRODUCTION AND USE OF CERTAIN TERMS
3
FORWARD-LOOKING STATEMENTS
4
PART I
6
Item 1.
Identity of Directors, Senior Management and Advisers
6
Item 2.
Offer Statistics and Expected Timetable
6
Item 3.
Key Information
6
3.A
[Reserved]
6
3.B
Capitalization and Indebtedness
6
3.C
Reasons for the offer and use of proceeds
6
3.D
Risk Factors
6
Item 4.
Information on the Company
44
4.A
History and Development of Mesoblast
44
4.B
Business Overview
54
4.C
Organizational Structure
79
4.D
Property, Plants and Equipment
79
Item 4A.
Unresolved Staff Comments
79
Item 5.
Operating and Financial Review and Prospects
79
5.A
Operating Results
79
5.B
Liquidity and Capital Resources
89
5.C
Research and Development, Patents and Licenses
91
5.D
Trend Information
91
5.E
Critical Accounting Estimates
91
Item 6.
Directors, Senior Management and Employees
91
6.A
Directors and Senior Management
91
6.B
Compensation
100
6.C
Board Practices
127
6.D
Employees
130
6.E
Share Ownership
131
6.F
Disclosure of a Registrant’s Action to Recover Erroneously Awarded Compensation
132
Item 7.
Major Shareholders and Related Party Transactions
132
7.A
Major Shareholders
132
7.B
Related Party Transactions
133
7.C
Interests of Experts and Counsel
133
Item 8.
Financial Information
133
8.A
Consolidated Statements and Other Financial Information
133
8.B
Significant Changes
134
Item 9.
The Offer and Listing
134
9.A
Offer and Listing Details
134
9.B
Plan of Distribution
134
9.C
Markets
134
9.D
Selling Shareholders
135
9.E
Dilution
135
9.F
Expenses of the Issue
135
Item 10.
Additional Information
135
10.A
Share Capital
135
Table of Contents
10.B
Memorandum and Articles of Association
135
10.C
Material Contracts
140
10.D
Exchange Controls
144
10.E
Taxation
146
10.F
Dividends and Paying Agents
153
10.G
Statement by Experts
153
10.H
Documents on Display
153
10.I
Subsidiary Information
154
10.J
Annual Report to Security Holders
154
Item 11.
Quantitative and Qualitative Disclosures about Market Risk
154
Item 12.
Description of Securities Other than Equity Securities
154
12.A
Debt Securities
154
12.B
Warrants and Rights
154
12.C
Other Securities
154
12.D
American Depositary Shares
154
PART II
155
Item 13.
Defaults, Dividend Arrearages and Delinquencies
155
Item 14.
Material Modifications to the Rights of Security Holders and Use of Proceeds
155
Item 15.
Controls and Procedures
155
Item 16.
[Reserved]
155
Item 16A.
Audit Committee Financial Expert
155
Item 16B.
Code of Ethics
156
Item 16C.
Principal Accountant Fees and Services
156
Item 16D.
Exemptions from the Listing Standards for Audit Committees
156
Item 16E.
Purchases of Equity Securities by the Issuer and Affiliated Purchasers
156
Item 16F.
Change in Registrant’s Certifying Accountant
156
Item 16G.
Corporate Governance
156
Item 16H.
Mine Safety Disclosure
157
Item 16I.
Disclosure Regarding Foreign Jurisdiction that Prevent Inspections
157
Item 16J.
Insider Trading Policies
157
Item 16K.
Cybersecurity
157
PART III
158
Item 17.
Financial Statements
158
Item 18.
Financial Statements
158
Item 19.
Exhibits
243
SIGNATURES
246
Table of Contents
INTRODUCTION AND USE OF CERTAIN TERMS
Mesoblast Limited and its consolidated subsidiaries publish consolidated financial statements expressed in U.S.
dollars, unless otherwise indicated. This Annual Report on Form 20-F is presented in U.S. dollars, unless otherwise
indicated. Our consolidated financial statements found in Item 18 of this Annual Report on Form 20-F are prepared in
accordance with International Financial Reporting Standards as issued by the International Accounting Standards Board
and Australian equivalents to International Financial Reporting Standards as issued by the Australian Accounting
Standards Board.
Except where the context requires otherwise and for purposes of this Form 20-F only:
•
“ADSs” refers to our American depositary shares, each of which represents ordinary shares, and “ADRs”
refers to the American depositary receipts that evidence our ADSs.
•
“Mesoblast,” “we,” “us” or “our” refer to Mesoblast Limited and its subsidiaries.
•
“A$” or “Australian dollar” refers to the legal currency of Australia.
•
“AIFRS” refers to the Australian equivalents to International Financial Reporting Standards as issued by
the Australian Accounting Standards Board, or AASB.
•
“CHF” refers to the legal currency of Switzerland.
•
“FDA” refers to the United States Food and Drug Administration.
•
“GBP” refers to the legal currency of the United Kingdom.
•
“IFRS” refers to the International Financial Reporting Standards as issued by the International
Accounting Standards Board, or IASB.
•
“S$” or “SGD” or “Singapore dollar” refers to the legal currency of Singapore.
•
“U.S. GAAP” refers to the Generally Accepted Accounting Principles in the United States.
•
“US$” or “U.S. dollars” refers to the legal currency of the United States.
•
“U.S.” or “United States” refers to the United States of America.
•
“€” or “Euro” refers to the legal currency of the European Union.
Australian Disclosure Requirements
Our ordinary shares are primarily quoted on the Australian Securities Exchange (“ASX”) in addition to our listing
of our ADSs on The Nasdaq Global Select Market. As part of our ASX listing, we are required to comply with various
disclosure requirements as set out under the Australian Corporations Act 2001 and the ASX Listing Rules. Information
furnished under the sub-heading “Australian Disclosure Requirements” is intended to comply with ASX listing and
Corporations Act 2001 disclosure requirements and is not intended to fulfill information required by this Annual Report on
Form 20-F.
Table of Contents
3
FORWARD-LOOKING STATEMENTS
This Form 20-F includes forward-looking statements within the meaning of Section 27A of the Securities Act of
1933, as amended, and Section 21E of the Securities Exchange Act of 1934, as amended, that are based on our current
expectations, assumptions, estimates and projections about the Company, our industry, economic conditions in the markets
in which we operate, and certain other matters. These statements include, among other things, the discussions of our
business strategy and expectations concerning our market position, future operations, margins, profitability, liquidity and
capital resources. These statements are subject to known and unknown risks, uncertainties and other factors that may cause
our actual results, levels of activity, performance or achievements to differ materially from any future results, levels of
activity, performance or achievements expressed or implied by these forward-looking statements. Words such as, but not
limited to, “believe,” “expect,” “anticipate,” “estimate,” “intend,” “plan,” “target,” “likely,” “will,” “would,” “could,”
“should”, “may”, “goal,” “objective” and similar expressions or phrases identify forward-looking statements. We have
based these forward-looking statements largely on our current expectations and future events and financial trends that we
believe may affect our financial condition, results of operation, business strategy and financial needs. Forward- looking
statements include, but are not limited to, statements about:
•
the initiation, timing, progress and results of our preclinical and clinical studies, and our research and
development programs;
•
our ability to advance product candidates into, enroll and successfully complete, clinical studies,
including multi-national clinical trials;
•
our ability to advance our manufacturing capabilities;
•
the timing or likelihood of regulatory filings and approvals, manufacturing activities and product
marketing activities, if any;
•
our ability to take advantage of the potential benefits of the 21st Century Cures Act;
•
the impact that any future pandemic could have on business operations;
•
the commercialization of our product candidates, if approved;
•
regulatory or public perceptions and market acceptance surrounding the use of cell based therapies;
•
the potential for our product candidates, if any are approved, to be withdrawn from the market due to
patient adverse events or deaths;
•
the potential benefits of strategic collaboration agreements and our ability to enter into and maintain
established strategic collaborations;
•
our ability to establish and maintain intellectual property on our product candidates and our ability to
successfully defend these in cases of alleged infringement;
•
the scope of protection we are able to establish and maintain for intellectual property rights covering our
product candidates and technology;
•
our ability to obtain additional financing;
•
estimates of our expenses, future revenues, capital requirements and our needs for additional financing;
•
our financial performance;
•
developments relating to our competitors and our industry;
•
the pricing and reimbursement of our product candidates, if approved; and
•
other risks and uncertainties, including those listed under the caption “Risk Factors”.
You should read this Form 20-F and the documents that we refer to herein thoroughly with the understanding that
our actual future results may be materially different from and/or worse than what we expect. We qualify all of our forward-
looking statements by these cautionary statements. Other sections of this Form 20-F include additional factors which could
adversely impact our business and financial performance. Moreover, we operate in an evolving environment. New risk
factors emerge from time to time and it is not possible for our management to predict all risk factors, nor can we assess the
impact of all factors on our business or the extent to which any factor, or combination of factors, may cause actual results
to differ materially from those contained in any forward-looking statements.
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This Form 20-F also contains third-party data relating to the biopharmaceutical market that includes projections
based on a number of assumptions. The biopharmaceutical market may not grow at the rates projected by market data, or at
all. The failure of this market to grow at the projected rates may have a material adverse effect on our business and the
market price of our ordinary shares and ADSs. Furthermore, if any one or more of the assumptions underlying the market
data turns out to be incorrect, actual results may differ from the projections based on these assumptions. You should not
place undue reliance on these forward-looking statements.
You should not rely upon forward-looking statements as predictions of future events. The forward-looking
statements made in this Form 20-F relate only to events or information as of the date on which the statements are made in
this Form 20-F. We undertake no obligation to update or revise any forward-looking statements, whether as a result of new
information, future events or otherwise.
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PART I
Item 1. Identity of Directors, Senior Management and Advisers
Not applicable.
Item 2. Offer Statistics and Expected Timetable
Not applicable.
Item 3. Key Information
3.A
[Reserved]
3.B
Capitalization and Indebtedness
Not applicable.
3.C
Reasons for the offer and use of proceeds
Not applicable.
3.D
Risk Factors
You should carefully consider the risks described below and all other information contained in this Annual Report
on Form 20-F before making an investment decision. If any of the following risks actually occur, our business, financial
condition and results of operations could be materially and adversely affected. In that event, the trading price of our
ordinary shares and ADSs could decline, and you may lose part or all of your investment. This Annual Report on Form 20-
F also contains forward-looking information that involves risks and uncertainties. Our actual results could differ materially
from those anticipated in these forward-looking statements as a result of many factors, including the risks described below
and elsewhere in this Annual Report on Form 20-F.
Risks Related to Our Financial Position and Capital Requirements
We have incurred operating losses since our inception and anticipate that we will continue to incur substantial
operating losses for the foreseeable future. We may never achieve or sustain profitability.
We are a clinical-stage biotechnology company and we have not yet generated significant revenues. We have
incurred net losses during most of our fiscal periods since our inception. Our net loss for the year ended June 30, 2024 was
$88.0 million. As of June 30, 2024, we have an accumulated deficit of $908.8 million since our inception. We do not know
whether or when we will become profitable. Our losses have resulted principally from costs incurred in clinical
development and manufacturing activities.
We anticipate that our expenses will increase as we move toward commercialization, including the scaling up of our
manufacturing activities and our establishment of infrastructure and logistics necessary to support potential product
launches. Biopharmaceutical product development is a highly speculative undertaking and involves a substantial degree of
risk. To achieve and maintain profitability, we must successfully develop our product candidates, obtain regulatory
approval, and manufacture, market and sell those products for which we obtain regulatory approval. If we obtain regulatory
approval to market a product candidate, our future revenue will depend upon the size of any markets in which our product
candidates may receive approval, and our ability to achieve and maintain sufficient market acceptance, pricing,
reimbursement from third-party payors, and adequate market share for our product candidates in those markets. We may
not succeed in these activities, and we may never generate revenue from product sales that is significant enough to achieve
profitability. Our failure to become or remain profitable would depress our market value and could impair our ability to
raise capital, expand our business, discover or develop other product candidates or continue our operations. A decline in the
value of our company could cause you to lose part or all of your investment.
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We have never generated revenue from product sales and may never be profitable.
Our ability to generate revenue and achieve profitability depends on our ability, either alone or with strategic
collaboration partners, to successfully complete the development of, and obtain the regulatory approvals necessary to
commercialize, our product candidates. We do not currently generate revenues from product sales (other than licensing
revenue from sales of TEMCELL® HS. Inj. (“TEMCELL”), a registered trademark of JCR Pharmaceuticals Co., Ltd.
(“JCR”), by JCR in Japan, and royalty revenue from net sales of Alofisel® a registered trademark of TiGenix NV
(“TiGenix”), previously known as Cx601, an adipose-derived mesenchymal stromal cell product developed by TiGenix,
now a wholly owned subsidiary of Takeda Pharmaceutical Company Limited (“Takeda”) and approved for marketing in
the EU and Japan), and we may never generate product sales. Our ability to generate future revenues from product sales
depends heavily on our success in a number of areas, including:
•
completing research, preclinical and clinical development of our product candidates;
•
seeking and obtaining regulatory and marketing approvals for product candidates for which we complete
clinical studies;
•
establishing and maintaining supply and manufacturing relationships with third parties that can provide
adequate (in amount and quality) products and services to support clinical development and the market
demand for our product candidates, if approved;
•
launching and commercializing product candidates for which we obtain regulatory and marketing approval,
either by collaborating with a partner or, if launched independently, by establishing commercial and
distribution capabilities necessary to effectively seek and maintain market access and ensure compliance with
legal and regulatory requirements relating to interactions with healthcare providers, healthcare organizations
and government agencies;
•
obtaining market acceptance of our product candidates as viable treatment options;
•
addressing competing technological and market developments;
•
obtaining and sustaining an adequate level of reimbursement from payors;
•
identifying and validating new cell therapy product candidates;
•
negotiating favorable terms in any collaboration, licensing or other arrangements into which we may enter;
•
maintaining, protecting and expanding our portfolio of intellectual property rights, including patents, trade
secrets, know-how and trademarks;
•
attracting, hiring and retaining qualified personnel; and
•
implementing additional internal systems and infrastructure, as needed.
Even if one or more of the product candidates that we develop is approved for commercial sale, we anticipate
incurring significant costs associated with commercializing and distributing any approved product candidate. Our expenses
could increase beyond expectations if we are required by the United States Food and Drug Administration (“FDA”), the
European Medicines Agency (“EMA”), or other regulatory agencies, to perform clinical and other studies in addition to
those that we currently anticipate. We may not become profitable and may need to obtain additional funding to continue
operations.
We require substantial additional financing to achieve our goals, and our failure to obtain this necessary capital or
establish and maintain strategic partnerships to provide funding support for our development programs could force us
to delay, limit, reduce or terminate our product development or commercialization efforts.
Our operations have consumed substantial amounts of cash since inception. As of June 30, 2024, our cash and cash
equivalents were $63.0 million. Subject to us achieving successful regulatory approval, we expect an increase in our total
expenses and an increase our cumulative operating losses for the foreseeable future in connection with our planned
research and development, manufacturing commercialization and selling, general and administrative expenses as we move
towards commercialization. In addition, we will require additional financing to achieve our goals and our failure to do so
could adversely affect our commercialization efforts. We anticipate that our expenses will increase if and as we:
•
continue the research and clinical development of our product candidates, including MPC-150-IM (Class II-
IV Chronic Heart Failure (“CHF”)), MPC-06-ID (Chronic Low Back Pain (“CLBP”)), remestemcel-L and
MPC-300-IV (inflammatory conditions) product candidates;
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•
seek to commercialize remestemcel-L for pediatric SR-aGVHD in the United States in the event that we
receive marketing authorization by the FDA;
•
seek to identify, assess, acquire, and/or develop other and combination product candidates and technologies;
•
seek regulatory and marketing approvals in multiple jurisdictions for our product candidates that successfully
complete clinical studies and identify and apply for regulatory designations to facilitate development and
ultimate commercialization of our products;
•
establish and maintain collaborations and strategic partnerships with third parties for the development and
commercialization of our product candidates, or otherwise build and maintain a sales, marketing and
distribution infrastructure and/or external logistics to commercialize any products for which we may obtain
marketing approval;
•
further develop and implement our proprietary manufacturing processes in both planar technology and our
bioreactor programs and expand our manufacturing capabilities and resources for commercial production;
•
seek coverage and reimbursement from third-party payors, including government and private payors for
future products;
•
make milestone or other payments under our agreements pursuant to which we have licensed or acquired
rights to intellectual property and technology;
•
seek to maintain, protect and expand our intellectual property portfolio;
•
seek to attract and retain skilled personnel; and
•
develop the compliance and other infrastructure necessary to support product commercialization and
distribution.
If we were to experience any delays or encounter issues with any of the above, including clinical holds, failed
studies, inconclusive or complex results, safety or efficacy issues, or other regulatory challenges that require longer follow-
up of existing studies, additional studies, or additional supportive studies in order to pursue marketing approval, it could
further increase the costs associated with the above. Further, the net operating losses we incur may fluctuate significantly
from quarter to quarter and year to year, such that a period-to-period comparison of our results of operations may not be a
good indication of our future performance.
To the extent that we raise additional capital through the sale of equity or convertible debt securities, your ownership
interest may be diluted, and the terms of these securities may include liquidation or other preferences that adversely affect
your rights as a shareholder or as a holder of the ADSs. Debt financing, if available, may involve agreements that include
covenants limiting or restricting our ability to take certain actions, such as incurring additional debt, making capital
expenditures or declaring dividends. If we raise additional funds through strategic collaborations or partnerships, or
marketing, distribution or licensing arrangements with third parties, we may be required to do so at an earlier stage than
would otherwise be ideal and/or may have to limit valuable rights to our intellectual property, technologies, product
candidates or future revenue streams, or grant licenses or other rights on terms that are not favorable to us. Furthermore,
any additional fundraising efforts may divert our management from their day-to-day activities, which may adversely affect
our ability to develop and commercialize our product candidates.
As of June 30, 2024, we held total cash reserves of $63.0 million. During the year ended June 30, 2024, we
executed on reprioritization of projects and operational streamlining activities and as a result have reduced net cash usage
for operating activities, which were $48.5 million for the year ended June 30, 2024, a reduction of 23% compared to the
prior period. As we prepare for a potential first product approval by the FDA, and in line with our commercial launch
plans, additional inflows from capital markets, strategic partnerships, product specific financing or royalty monetization
will be required to meet our projected expenditure consistent with our business strategy over at least the next 12 months.
As a result of these matters, there is material uncertainty related to events or conditions that may cast significant doubt (or
raise substantial doubt as contemplated by Public Company Accounting Oversight Board (“PCAOB”) standards) on our
ability to continue as a going concern and, therefore, that we may be unable to realize our assets and discharge our
liabilities in the normal course of business. Our consolidated financial statements do not include any adjustments that may
result from the outcome of this uncertainty. If we are unable to obtain adequate funding or partnerships beyond the 12-
month period we may not be able to continue as a going concern, and our shareholders and holders of the ADSs may lose
some or all of their investment in Mesoblast. See Note 1(i) of our accompanying financial statements.
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8
The terms of our loan facilities with funds associated with Oaktree Capital Management, L.P. (“Oaktree”) and
NovaQuest Capital Management, L.L.C. (“NovaQuest”) could restrict our operations, particularly our ability to respond
to changes in our business or to take specified actions.
On November 19, 2021, we entered into a loan agreement and guaranty with Oaktree, with a secured five-year
senior debt facility. The balance of funds drawn down is $50.0 million as of June 30, 2024. On June 29, 2018, we entered
into a loan and security agreement with NovaQuest for a $40.0 million non-dilutive, eight-year term credit facility,
repayable from net sales of our allogeneic product candidate remestemcel-L in pediatric patients with steroid-refractory
acute graft versus host disease (“SR-aGVHD”), in the United States and other geographies excluding Asia. We drew the
first tranche of $30.0 million on closing. Our loan facilities with Oaktree and NovaQuest contain a number of covenants
that impose operating restrictions on us, which may restrict our ability to respond to changes in our business or take
specified actions. Under the terms of our Oaktree agreement the minimum unrestricted cash balance we need to maintain is
$25.0 million. Our ability to comply with the various covenants under the agreements may be affected by events beyond
our control, and we may not be able to continue to meet the covenants. Upon the occurrence of an event of default, Oaktree
or NovaQuest could elect to declare all amounts outstanding under the loan facility to be immediately due and payable and
terminate all commitments to extend further credit. If Oaktree or NovaQuest accelerates the repayment, we may not have
sufficient funds to repay our existing debt. If we were unable to repay the owed amounts, Oaktree or NovaQuest could
proceed against the collateral granted to it to secure such indebtedness. We have pledged substantially all of our assets as
collateral under the loan facility with Oaktree, and a portion of our assets relating to the SR-aGVHD product candidate as
collateral under the loan facility with NovaQuest.
We are subject to risks associated with currency fluctuations, and changes in foreign currency exchange rates could
impact our results of operations.
Historically, a substantial portion of our operating expenses has been denominated in U.S. dollars and our main
currency requirements are U.S. dollars, Australian dollars and Singapore dollars. Approximately 76% of our cash and cash
equivalents as of June 30, 2024 were denominated in U.S. dollars, 23% were denominated in Australian dollars and 1%
were denominated in other currencies. Because we have multiple functional currencies across different jurisdictions,
changes in the exchange rate between these currencies and the foreign currencies of the transactions recorded in our
accounts could materially impact our reported results of operations and distort period-to-period comparisons. For example,
where a portion of our research and clinical trials are undertaken in Australia, payment will be made in Australian dollar
currency, and may exceed the budgeted expenditure if there are adverse currency fluctuations against the U.S. dollar.
More specifically, if we decide to convert our Australian dollars into U.S. dollars for any business purpose,
appreciation of the U.S. dollar against the Australian dollar would have a negative effect on the U.S. dollar amount
available to us. Appreciation or depreciation in the value of the Australian dollar relative to the U.S. dollar would affect our
financial results reported in U.S. dollar terms without giving effect to any underlying change in our business or results of
operations. As a result of such foreign currency fluctuations, it could be more difficult to detect underlying trends in our
business and results of operations.
Unfavorable global economic or political conditions could adversely affect our business, financial condition or results
of operations.
Our results of operations could be adversely affected by general conditions in the global economy and in the global
financial markets. A global financial crisis or a global or regional political disruption could cause extreme volatility in the
capital and credit markets. A severe or prolonged economic downturn or political disruption could result in a variety of
risks to our business, including weakened demand for our product candidates, if approved, and our ability to raise
additional capital when needed on acceptable terms, if at all. A weak or declining economy or political disruption could
also strain our manufacturers or suppliers, possibly resulting in supply disruption. Any of the foregoing could harm our
business and we cannot anticipate all of the ways in which the political or economic climate and financial market
conditions could adversely impact our business.
Risks Related to Clinical Development and Regulatory Review and Approval of Our Product Candidates
Our product candidates are based on our novel mesenchymal lineage cell technology, which makes it difficult to
accurately and reliably predict the time and cost of product development and subsequently obtaining regulatory
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9
approval. At the moment, no industrially manufactured, non-hematopoietic, allogeneic cell products have been
approved in the United States.
Other than with respect to sales of products by our licensees, we have not commercially marketed, distributed or
sold any products. The success of our business depends on our ability to develop and commercialize our lead product
candidates. We have concentrated our product research and development efforts on our mesenchymal lineage cell platform,
a novel type of cell therapy. Our future success depends on the successful development of this therapeutic approach. There
can be no assurance that any development problems we experience in the future related to our mesenchymal lineage cell
platform will not cause significant delays or unanticipated costs, or that such development problems can be solved. We
may also experience delays in developing sustainable, reproducible and scalable manufacturing processes or transferring
these processes to collaborators, which may prevent us from completing our clinical studies or commercializing our
products on a timely or profitable basis, if at all.
In addition, the clinical study requirements of the FDA, the EMA and other regulatory agencies and the criteria these
regulators use to determine the safety and efficacy of a product candidate vary substantially according to the type,
complexity, novelty and intended use and market of the potential product candidates. The regulatory approval process for
novel product candidates such as ours can be more expensive and take longer to develop than for other, better known or
extensively studied pharmaceutical or other product candidates. In addition, adverse developments in clinical trials of cell
therapy products conducted by others may cause the FDA or other regulatory bodies to change the requirements for
approval of any of our product candidates.
We may fail to demonstrate safety and efficacy to the satisfaction of applicable regulatory agencies.
We must conduct extensive testing of our product candidates to demonstrate their safety and efficacy, including both
preclinical animal testing and evaluation in human clinical trials, before we can obtain regulatory approval to market and
sell them. Conducting such testing is a lengthy, time-consuming, and expensive process and there is a high rate of failure.
Our current and completed preclinical and clinical results for our product candidates are not necessarily predictive of
the results of our ongoing or future clinical trials. Promising results in preclinical studies of a product candidate may not be
predictive of similar results in humans during clinical trials, and successful results from early human clinical trials of a
product candidate may not be replicated in later and larger human clinical trials or in clinical trials for different indications.
If the results of our or our collaborators’ ongoing or future clinical trials are negative or inconclusive with respect to the
efficacy of our product candidates, or if these trials do not meet the clinical endpoints with statistical significance, or if
there are safety concerns or adverse events associated with our product candidates, we or our collaborators may be
prevented or delayed in obtaining marketing approval for our product candidates.
Even if ongoing or future clinical studies meet the clinical endpoints with statistical significance, the FDA or other
regulatory agencies may still find the data insufficient to support marketing approval based on other factors.
We may encounter substantial delays in our clinical studies, including as a result of disruptive events beyond our
control, including pandemics.
We cannot guarantee that any preclinical testing or clinical trials will be conducted as planned or completed on
schedule, if at all. As a result, we may not achieve our expected clinical milestones. A failure can occur at any stage of
testing. Events that may prevent successful or timely commencement, enrollment or completion of clinical development
include:
•
problems which may arise as a result of our transition of research and development programs from licensors
or previous sponsors;
•
delays in raising, or inability to raise, sufficient capital to fund the planned trials;
•
delays by us or our collaborators in reaching a consensus with regulatory agencies on trial design;
•
changes in trial design;
•
inability to identify, recruit and train suitable clinical investigators;
•
inability to add new clinical trial sites;
•
delays in reaching agreement on acceptable terms for the performance of the trials with contract research
organizations (“CROs”), and clinical trial sites;
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•
delays in obtaining required Institutional Review Board (“IRB”), approval at each clinical trial site;
•
delays in recruiting suitable clinical sites and patients (i.e., subjects) to participate in clinical trials and delays
in accruing medical events necessary to complete any events-driven trial;
•
imposition of a clinical hold by regulatory agencies for any reason, including negative clinical results, safety
concerns or as a result of an inspection of manufacturing or clinical operations or trial sites;
•
failure by CROs, other third parties or us or our collaborators to adhere to clinical trial requirements;
•
failure to perform in accordance with the FDA’s current Good Clinical Practices (“cGCP”), or applicable
regulatory guidelines in other countries;
•
delays in testing, validation, manufacturing and delivery of a product candidate to clinical trial sites;
•
delays caused by patients not completing participation in a trial or not returning for post-treatment follow-up;
•
delays caused by clinical trial sites not completing a trial;
•
failure to demonstrate adequate efficacy;
•
occurrence of serious adverse events in clinical trials that are associated with a product candidates and that are
viewed to outweigh its potential benefits;
•
changes in regulatory requirements and guidance that require amending or submitting new clinical protocols;
or
•
disagreements between us and the FDA or other regulatory agencies regarding a clinical trial design, protocol
amendments, or interpreting the data from our clinical trials.
In addition, our ongoing clinical trials may be affected by delays caused by disruptive events outside our control,
such as delays in monitoring and data collection as a result of geopolitical instability, significant climate events and
pandemics, including due to prioritization of hospital resources, travel restrictions, and the inability to access sites for
patient monitoring. In addition, some patients may be unable to comply with clinical trial protocols if quarantines or stay at
home orders impede patient movement or interrupt health services.
Delays, including delays caused by the above factors, can be costly and could negatively affect our or our
collaborators’ ability to complete clinical trials for our product candidates. If we or our collaborators are not able to
successfully complete clinical trials or are not able to do so in a timely and cost-effective manner, we will not be able to
obtain regulatory approval and/or will not be able to commercialize our product candidates and our commercial partnering
opportunities will be harmed.
We may find it difficult to enroll patients in our clinical trials, which could delay or prevent development of our product
candidates.
Identifying and qualifying patients to participate in clinical trials of our product candidates is critical to our success.
The timing of our clinical trials depends on the speed at which we can recruit patients to participate in testing our product
candidates as well as completion of required follow-up periods. In general, if patients are unwilling to participate in our cell
therapy trials because of negative publicity from adverse events in the biotechnology or cell therapy industries or for other
reasons, including competitive clinical trials for similar patient populations, the timeline for recruiting patients, conducting
trials and obtaining regulatory approval for our product candidates may be delayed. Additionally, we or our collaborators
generally will have to run multi-site and potentially multi-national trials, which can be time consuming, expensive and
require close coordination and supervision. If we have difficulty enrolling a sufficient number of patients or otherwise
conducting clinical trials as planned, we or our collaborators may need to delay, limit or terminate ongoing or planned
clinical trials, any of which would have an adverse effect on our business.
If there are delays in accumulating the required number of trial subjects or, in trials where clinical events are a
primary endpoint, if the events needed to assess performance of our clinical candidates do not accrue at the anticipated rate,
there may be delays in completing the trial. These delays could result in increased costs, delays in advancing development
of our product candidates, including delays in testing the effectiveness, or even termination of the clinical trials altogether.
Patient enrollment and completion of clinical trials are affected by factors including:
•
size of the patient population, particularly in orphan diseases;
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•
severity of the disease under investigation;
•
design of the trial protocol;
•
eligibility criteria for the particular trial;
•
perceived risks and benefits of the product candidate being tested;
•
proximity and availability of clinical trial sites for prospective patients;
•
availability of competing therapies and clinical trials;
•
efforts to facilitate timely enrollment in clinical trials;
•
patient referral practices of physicians and level and effectiveness of study site recruitment efforts; and
•
ability to monitor patients adequately during and after treatment.
Once enrolled, patients may choose to discontinue their participation at any time during the trial, for any reason.
Participants also may be terminated from the study at the initiative of the investigator, for example if they experience
serious adverse clinical events or do not follow the study directions. If we are unable to maintain an adequate number of
patients in our clinical trials, we may be required to delay or terminate an ongoing clinical trial, which would have an
adverse effect on our business.
We may conduct multinational clinical trials, which present additional and unique risks.
We plan to seek initial marketing approval for our product candidates in the United States and in select non-U.S.
jurisdictions such as Europe, Japan and Canada. Conducting trials on a multinational basis requires collaboration with
foreign medical institutions and healthcare providers. Our ability to successfully initiate, enroll and complete a clinical trial
in multiple countries is subject to numerous risks unique to conducting business internationally, including:
•
difficulty in establishing or managing relationships with physicians, sites and CROs;
•
standards within different jurisdictions for conducting clinical trials and recruiting patients;
•
our ability to effectively interface with non-US regulatory authorities;
•
our inability to identify or reach acceptable agreements with qualified local consultants, physicians and
partners;
•
the potential burden of complying with a variety of foreign laws, medical standards and regulatory
requirements, including the regulation of pharmaceutical and biotechnology products and treatments, and
anti-corruption/anti-bribery laws;
•
differing genotypes, average body weights and other patient profiles within and across countries from our
donor profile may impact the optimal dosing or may otherwise impact the results of our clinical trials; and
•
global events like geopolitical instability, climate events and pandemics limiting our ability to commence and
conduct studies, including recruiting patients.
The complexity of conducting multinational clinical trials could negatively affect our or our collaborators’ ability to
complete trials as intended which could have an adverse effect on our business.
Serious adverse events or other safety risks could require us to abandon development and preclude, delay or limit
approval of our product candidates, or limit the scope of any approved indication or market acceptance.
Participants in clinical trials of our investigational cell therapy products may experience adverse reactions or other
undesirable side effects. While some of these can be anticipated, others may be unexpected. We cannot predict the
frequency, duration, or severity of adverse reactions or undesirable side effects that may occur during clinical investigation
of our product candidates. If any of our product candidates, prior to or after any approval for commercial sale, cause
serious adverse events or are associated with other safety risks, a number of potentially significant negative consequences
could result, including:
•
regulatory authorities may suspend (e.g., through a clinical hold) or terminate clinical trials;
•
regulatory authorities may deny regulatory approval of our product candidates;
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•
regulators may restrict the indications or patient populations for which a product candidate is approved;
•
regulatory authorities may require certain labeling statements, such as warnings or contraindications or
limitations on the indications for use, and/or impose restrictions on distribution in the form of a risk
evaluation and mitigation strategy (“REMS”), in connection with approval, if any;
•
regulatory authorities may withdraw their approval, require more onerous labeling statements or impose a
more restrictive REMS than any product that is approved;
•
we may be required to change the way the product is administered or conduct additional clinical trials;
•
patient recruitment into our clinical trials may suffer;
•
our relationships with our collaborators may suffer;
•
we could be required to provide compensation to subjects for their injuries, e.g., if we are sued and found to
be liable or if required by the laws of the relevant jurisdiction or by the policies of the clinical site; or
•
our reputation may suffer.
There can be no assurance that adverse events associated with our product candidates will not be observed, in such
settings where no prior adverse events have occurred. As is typical in clinical development, we have a program of ongoing
toxicology studies in animals for our clinical-stage product candidates and cannot provide assurance that the findings from
such studies or any ongoing or future clinical trials will not adversely affect our clinical development activities.
We may voluntarily suspend or terminate our clinical trials if at any time we believe that they present an
unacceptable risk to participants or if preliminary data demonstrate that our product candidates are unlikely to receive
regulatory approval or unlikely to be successfully commercialized. In addition, regulatory agencies, IRBs or data safety
monitoring boards may at any time recommend the temporary or permanent discontinuation of our clinical trials or request
that we cease using investigators in the clinical trials if they believe that the clinical trials are not being conducted in
accordance with applicable regulatory requirements, or that they present an unacceptable safety risk to participants. If we
elect or are forced to suspend or terminate a clinical trial for any of our product candidates, the commercial prospects for
that product as well as our other product candidates may be harmed and our ability to generate product revenue from these
product candidates may be delayed or eliminated. Furthermore, any of these events could prevent us or our collaborators
from achieving or maintaining market acceptance of the affected product and could substantially increase the costs of
commercializing our product candidates and impair our ability to generate revenue from the commercialization of these
product candidates either by us or by our collaborators.
Several of our product candidates are being evaluated for the treatment of patients who are extremely ill, and patient
deaths that occur in our clinical trials could negatively impact our business even if they are not shown to be related to
our product candidates.
We are developing MPC-150-IM, which will focus on patients with heart failure with reduced ejection fraction
associated with ischemic and/or diabetic etiology, and remestemcel-L, which will focus on SR-aGVHD. The patients who
receive our product candidates are very ill due to their underlying diseases.
Generally, patients remain at high risk following their treatment with our product candidates and may more easily
acquire infections or other common complications during the treatment period, which can be serious and life threatening.
As a result, it is likely that we will observe severe adverse outcomes in patients during our Phase 3 and other trials for these
product candidates, including patient death. If a significant number of study subject deaths were to occur, regardless of
whether such deaths are attributable to our product candidates, our ability to obtain regulatory approval for the applicable
product candidate may be adversely impacted and our business could be materially harmed. Should studies of a candidate
product result in regulatory approval, any association with a significant number of study subject deaths could limit the
commercial potential of an approved product candidate, or negatively impact the medical community’s willingness to use
our product with patients.
The requirements to obtain regulatory approval of the FDA and regulators in other jurisdictions can be costly, time-
consuming, and unpredictable. If we or our collaborators are unable to obtain timely regulatory approval for our
product candidates, our business may be substantially harmed.
The regulatory approval process is expensive and the time and resources required to obtain approval from the FDA
or other regulatory authorities in other jurisdictions to sell any product candidate is uncertain and approval may take years.
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Whether regulatory approval will be granted is unpredictable and depends upon numerous factors, including the discretion
of the regulatory authorities. For example, governing legislation, approval policies, regulations, regulatory policies, or the
type and amount of preclinical and clinical data necessary to gain approval may change during the course of a product
candidate’s clinical development and may vary among jurisdictions. It is possible that none of our existing or future
product candidates will ever obtain regulatory approval, even if we expend substantial time and resources seeking such
approval.
Further, regulatory requirements governing cell therapy products in particular have changed and may continue to
change in the future. For example, in December 2016, the 21st Century Cures Act (“Cures Act”) was signed into law in the
United States. This law is designed to advance medical innovation, and includes a number of provisions that may impact
our product development programs. For example, the Cures Act establishes a new “regenerative medicine advanced
therapy” designation (“RMAT”), and creates a pathway for increased interaction with FDA for the development of
products which obtain designations. Although the FDA issued guidance documents in 2019, it remains unclear how and
when the FDA will fully implement all deliverables under the Cures Act.
Any regulatory review committees and advisory groups and any contemplated new guidelines may lengthen the
regulatory review process, require us to perform additional studies, increase our development costs, lead to changes in
regulatory positions and interpretations, delay or prevent approval and commercialization of our product candidates or lead
to significant post-approval limitations or restrictions. As we advance our product candidates, we will be required to
consult with these regulatory and advisory groups, and comply with applicable guidelines. If we fail to do so, we may be
required to delay or discontinue development of our product candidates. Delay or failure to obtain, or unexpected costs in
obtaining, the regulatory approval necessary to bring a product candidate to market could decrease our ability to generate
sufficient revenue to maintain our business.
Our product candidates could fail to receive regulatory approval for many reasons, including the following:
•
we may be unable to successfully complete our ongoing and future clinical trials of product candidates;
•
we may be unable to demonstrate to the satisfaction of the FDA or other regulatory authorities that a product
candidate is safe, pure, and potent for any or all of a product candidate’s proposed indications;
•
we may be unable to demonstrate that a product candidate’s benefits outweigh the risk associated with the
product candidate;
•
the FDA or other regulatory authorities may disagree with the design or implementation of our clinical trials;
•
the results of clinical trials may not meet the level of statistical significance required by the FDA or other
regulatory authorities for approval;
•
the FDA or other regulatory authorities may disagree with our interpretation of data from preclinical studies
or clinical trials;
•
a decision by the FDA, other regulatory authorities or us to suspend or terminate a clinical trial at any time;
•
the data collected from clinical trials of our product candidates may be inconclusive or may not be sufficient
to support the submission of a Biologics License Application (“BLA”), or other submission or to obtain
regulatory approval in the United States or elsewhere;
•
our third party manufacturers of supplies needed for manufacturing product candidates may fail to satisfy
FDA or other regulatory requirements and may not pass inspections that may be required by FDA or other
regulatory authorities;
•
the failure to comply with applicable regulatory requirements following approval of any of our product
candidates may result in the refusal by the FDA or similar foreign regulatory agency to approve a pending
BLA or supplement to a BLA submitted by us for other indications or new product candidates; and
•
the approval policies or regulations of the FDA or other regulatory authorities outside of the United States
may significantly change in a manner rendering our clinical data insufficient for approval.
We or our collaborators may gain regulatory approval for any of our product candidates in some but not all of the
territories available and any future approvals may be for some but not all of the target indications, limiting their
commercial potential. Regulatory requirements and timing of product approvals vary from country to country and some
jurisdictions may require additional testing beyond what is required to obtain FDA approval. Approval by the FDA does
not ensure approval by regulatory authorities in other countries or jurisdictions, and approval by one foreign regulatory
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authority does not ensure approval by regulatory authorities in other countries or by the FDA. The foreign regulatory
approval process may include all of the risks associated with obtaining FDA approval.
Our drug candidates may not benefit from an expedited approval path for cellular medicines designated as Regenerative
Medicine Advanced Therapies (RMATs) under the 21st Century Cures Act.
In 2017, the FDA granted RMAT designation for our novel mesenchymal precursor cell ("MPC") therapy in the
treatment of heart failure patients with left ventricular systolic dysfunction and left ventricular assist devices. The FDA
granted RMAT designation for our novel MPC therapy in the treatment of chronic lower back pain due to degenerative disc
disease. While the Cures Act offers several potential benefits to drugs designated as RMATs, including eligibility for
increased agency support and advice during development, priority review on filing, a potential pathway for accelerated or
full approval based on surrogate or intermediate endpoints, and the potential to use patient registry data and other sources
of real world evidence for post approval confirmatory studies, there is no assurance that any of these potential benefits will
either apply to any or all of our drug candidates or, if applicable, accelerate marketing approval. RMAT designation does
not change the evidentiary standards of safety and effectiveness needed for marketing approval.
Furthermore, there is no certainty as to whether any of our product candidates that have not yet received RMAT
designation under the Cures Act will receive such designation under the Cures Act. Designation as an RMAT is within the
discretion of the FDA. Accordingly, even if we believe one of our products or product candidates meets the criteria for
RMAT designation, the FDA may disagree. Additionally, for any product candidate that receives RMAT designation, we
may not experience a faster development, review or approval process compared to conventional FDA procedures. The
FDA may withdraw RMAT designation if it believes that the product no longer meets the qualifying criteria for
designation.
Even if we obtain regulatory approval for our product candidates, our products will be subject to ongoing regulatory
scrutiny.
Any of our product candidates that are approved in the United States or in other jurisdictions will continue to be
subject to ongoing regulatory requirements relating to the quality, identity, strength, purity, safety, efficacy, testing,
manufacturing, marketing, advertising, promotion, distribution, sale, storage, packaging, pricing, import or export, record-
keeping and submission of safety and other post-market information for all approved product candidates. In the United
States, this includes both federal and state requirements. In particular, as a condition of approval of a BLA, the FDA may
require a REMS, to ensure that the benefits of the drug outweigh the potential risks. REMS can include medication guides,
communication plans for healthcare professionals and elements to assure safe use (“ETASU”). ETASU can include, but are
not limited to, special training or certification for prescribing or dispensing, dispensing only under certain circumstances,
special monitoring, and the use of patient registries. Moreover, regulatory approval may require substantial post-approval
(Phase 4) testing and surveillance to monitor the drug’s safety or efficacy. Delays in the REMS approval process could
result in delays in the BLA approval process. In addition, as part of the REMS, the FDA could require significant
restrictions, such as restrictions on the prescription, distribution and patient use of the product, which could significantly
impact our ability to effectively commercialize our product candidates, and dramatically reduce their market potential
thereby adversely impacting our business, results of operations and financial condition. Post-approval study requirements
could add additional burdens, and failure to timely complete such studies, or adverse findings from those studies, could
adversely affect our ability to continue marketing the product.
Any failure to comply with ongoing regulatory requirements, as well as post-approval discovery of previously
unknown problems, including adverse events of unanticipated severity or frequency, or with manufacturing operations or
processes, may significantly and adversely affect our ability to generate revenue from our product candidates, and may
result in, among other things:
•
restrictions on the marketing or manufacturing of the product candidates, withdrawal of the product
candidates from the market, or voluntary or mandatory product recalls;
•
suspension or withdrawal of regulatory approval;
•
costly regulatory inspections;
•
fines, warning letters, or holds on clinical trials;
•
refusal by the FDA to approve pending applications or supplements to approved applications filed by us or
our collaborators, or suspension or revocation of BLAs;
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•
restrictions on our operations;
•
product seizure or detention, or refusal to permit the import or export of products; or
•
injunctions or the imposition of civil or criminal penalties by FDA or other regulatory bodies.
If regulatory sanctions are applied or if regulatory approval is withdrawn, the value of our business and our
operating results will be adversely affected.
The FDA’s policies, or that of the applicable regulatory bodies in other jurisdictions, may change, and additional
government regulations may be enacted that could prevent, limit or delay regulatory approval of our product candidates.
We cannot predict the likelihood, nature or extent of government regulation that may arise from future legislation or
administrative action, either in the United States or abroad. If we or our collaborators are not able to maintain regulatory
compliance, are slow or unable to adopt new requirements or policies, or effect changes to existing requirements, we or our
collaborators may no longer be able to lawfully market our product, and we may not achieve or sustain profitability, which
would adversely affect our business.
Ethical and other concerns surrounding the use of embryonic stem cell-based therapy may negatively affect regulatory
approval or public perception of our non-embryonic stem cell product candidates, which could reduce demand for our
products or depress our share price.
The use of embryonic stem cells (“ESCs”), for research and therapy has been the subject of considerable public
debate, with many people voicing ethical, legal and social concerns related to their collection and use. Our cells are not
ESCs, which have been the predominant focus of this public debate and concern in the United States and elsewhere.
However, the distinction between ESCs and non-ESCs, such as our mesenchymal lineage cells, may be misunderstood by
the public. Negative public attitudes toward cell therapy and publicity and harm from cell therapy usage clinically by others
could also result in greater governmental regulation of cell therapies, which could harm our business. The improper use of
cells could give rise to ethical and social commentary adverse to us, which could harm the market demand for new
products and depress the price of our ordinary shares and ADSs. Ongoing lack of understanding of the difference between
ESCs and non-ESCs could negatively impact the public’s perception of our company and product candidates and could
negatively impact us.
Additional government-imposed restrictions on, or concerns regarding possible government regulation of, the use of
cell therapies in research, development and commercialization could also cause an adverse effect on us by harming our
ability to establish important partnerships or collaborations, delaying or preventing the development of certain product
candidates, and causing a decrease in the price of our ordinary shares and ADSs, or by otherwise making it more difficult
for us to raise additional capital. For example, concerns regarding such possible regulation could impact our ability to
attract collaborators and investors. Also, existing and potential government regulation of cell therapies may lead
researchers to leave the field of cell therapy research altogether in order to assure that their careers will not be impeded by
restrictions on their work. This may make it difficult for us to find and retain qualified scientific personnel.
Orphan drug designation may not ensure that we will benefit from market exclusivity in a particular market, and if we
fail to obtain or maintain orphan drug designation or other regulatory exclusivity for some of our product candidates,
our competitive position would be harmed.
A product candidate that receives orphan drug designation can benefit from potential commercial benefits following
approval. Under the Orphan Drug Act, the FDA may designate a product candidate as an orphan drug if it is intended to
treat a rare disease or condition, defined as affecting (1) a patient population of fewer than 200,000 in the United States, (2)
a patient population greater than 200,000 in the United States where there is no reasonable expectation that the cost of
developing the drug will be recovered from sales in the United States, or (3) an “orphan subset” of a patient population
greater than 200,000 in the United States. In the European Union (“EU”), the EMA’s Committee for Orphan Medicinal
Products grants orphan drug designation to promote the development of products that are intended for the diagnosis,
prevention or treatment of a life-threatening or chronically debilitating condition affecting not more than 10,000 persons in
the EU. Currently, this designation provides market exclusivity in the United States and the EU for seven years and ten
years, respectively, if a product is the first such product approved for such orphan indication. This market exclusivity does
not, however, pertain to indications other than those for which the drug was specifically designated in the approval, nor
does it prevent other types of drugs from receiving orphan designations or approvals in these same indications. Further,
even after an orphan drug is approved, the FDA can subsequently approve a drug with similar chemical structure for the
same condition if the FDA concludes that the new drug is clinically superior to the orphan product or a market shortage
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occurs. In the EU, orphan exclusivity may be reduced to six years if the drug no longer satisfies the original designation
criteria or can be lost altogether if the marketing authorization holder consents to a second orphan drug application or
cannot supply enough drug, or when a second applicant demonstrates its drug is “clinically superior” to the original orphan
drug.
Our remestemcel-L product candidate has received orphan drug designation for the treatment of aGVHD by the
FDA and EMA, and our CHF product candidate, rexlemestrocel-L has received orphan drug designation from the FDA for
both the prevention of post-implantation mucosal bleeding in end-stage CHF patients who require a left ventricular assist
device (“LVAD”) and children with hypoplastic left heart syndrome ("HLHS"). If we seek orphan drug designations for
other product candidates in other indications, we may fail to receive such orphan drug designations and, even if we
succeed, such orphan drug designations may fail to result in or maintain orphan drug exclusivity upon approval, which
would harm our competitive position.
We may face competition from biosimilars due to changes in the regulatory environment.
In the United States, the Biologics Price Competition and Innovation Act of 2009 created an abbreviated approval
pathway for biological products that are demonstrated to be “highly similar”, or biosimilar, to or “interchangeable” with an
FDA-approved innovator (original) biological product. This pathway could allow competitors to reference data from
innovator biological products already approved after 12 years from the time of approval. For several years the annual
budget requests of President Obama’s administration included proposals to cut this 12-year period of exclusivity down to
seven years. Those proposals were not adopted by Congress. Under President Biden’s administration, it is unclear if a
similar change will be pursued in the future. In Europe, the European Commission has granted marketing authorizations for
several biosimilars pursuant to a set of general and product class-specific guidelines for biosimilar approvals issued over
the past few years. In Europe, a competitor may reference data from biological products already approved, but will not be
able to get on the market until ten years after the time of approval. This 10-year period will be extended to 11 years if,
during the first eight of those 10 years, the marketing authorization holder obtains an approval for one or more new
therapeutic indications that bring significant clinical benefits compared with existing therapies. In addition, companies may
be developing biosimilars in other countries that could compete with our products. If competitors are able to obtain
marketing approval for biosimilars referencing our products, our products may become subject to competition from such
biosimilars causing the price for our products and our potential market share to suffer, resulting in lower product sales.
Our BLA submission for pediatric SR-aGVHD may not be approved and even if it is approved, we will continue to be
closely regulated by FDA.
As a biological product, our allogeneic cellular medicine, remestemcel-L, for the treatment of children with SR-
aGVHD, requires regulatory approval from the FDA before it may legally be distributed in U.S. commerce. In particular,
remestemcel-L will require FDA approval of a BLA under Section 351 of the Public Health Service Act to be
commercialized.
We have received Fast Track designation from the FDA for remestemcel-L in pediatrics with SR-aGVHD. Fast
Track designation may provide for a more streamlined development or approval process but it does not change the
standards for approval and may be rescinded by the FDA if the product no longer meets the qualifying criteria. A biologic
product that receives Fast Track designation can be eligible for regulatory benefits, including rolling BLA review. Rolling
review of a BLA enables individual modules of the application to be submitted to and reviewed by the FDA on an ongoing
basis, rather than waiting for all sections of a BLA to be completed before submission. Note that there is no benefit of Fast
Track in relation to the review time for the resubmitted BLA.
Remestemcel-L was accepted for Priority Review by the FDA with an action date of September 30, 2020, under the
Prescription Drug User Fee Act (“PDUFA”). In August 2020, the Oncologic Drugs Advisory Committee (“ODAC”) of the
FDA voted in favor that available data from a single-arm Phase 3 trial and evidence from additional studies support the
efficacy of remestemcel-L in pediatric patients with SR-aGVHD. Although the FDA considers the recommendation of the
panel, the final decision regarding the approval of the product is made solely by the FDA, and the recommendations by the
panel are non-binding. On September 30, 2020, the FDA issued a Complete Response Letter to our BLA for remestemcel-
L for the treatment of pediatric SR-aGVHD. Despite the overwhelming ODAC vote, the FDA recommended that we
conduct at least one additional randomized, controlled study in adults and/or children to provide further evidence of the
effectiveness of remestemcel-L for SR-aGVHD.
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On January 31, 2023, we resubmitted the BLA and, on August 1, 2023, the FDA issued a Complete Response Letter
in relation to the resubmitted BLA requiring more data to support marketing approval, including potency assay or clinical
data. The FDA acknowledged in the resubmission review that changes implemented appeared to improve assay
performance relative to the original version of the assay used in the pediatric Phase 3 trial.
On July 8, 2024, we resubmitted the BLA for approval of Ryoncil® (remestemcel-L) in the treatment of children
with SR-aGVHD and on July 22, 2024, the FDA accepted the BLA and provided a PDUFA goal date of January 7, 2025.
The BLA resubmission was made after being informed by FDA at the end of March 2024 that, following additional
consideration, the available clinical data from the Phase 3 study MSB-GVHD001 appears sufficient to support submission
of the proposed BLA for remestemcel-L for treatment of pediatric patients with SR-aGVHD.
In line with our overall commercial strategy to progress to adult populations, we intend to conduct a targeted,
controlled study in the highest-risk adults with the greatest mortality. In connection with its review of the BLA, the FDA
conducted a pre-license inspection of the manufacturing process of remestemcel-L which did not result in the issuance of a
Form 483 and there were no observed concerns.
The FDA reviews a BLA to determine, among other things, whether a product is safe, pure and potent and the
facility in which it is manufactured, processed, packed, or held meets standards designed to assure the product’s continued
safety, purity and potency. During the course of review of our BLA, the FDA may request or require additional preclinical,
clinical, chemistry and manufacturing, controls (or CMC), or other data and information. The development and provision
of these data and information may be time consuming and expensive. Our failure to comply, or the failure of our contract
manufacturers to satisfy, applicable FDA CMC requirements could result in a delay or failure to obtain approval of our
BLA. If the FDA determines that the application, manufacturing process or manufacturing facilities are not acceptable, it
will outline the deficiencies in our submission and may request additional testing or information. The testing and approval
process requires substantial time, effort and financial resources, and may take several years to complete. In addition, the
FDA or other regulatory agencies may find the data from our clinical studies insufficient to support marketing approval.
For example, our Phase 3 study for remestemcel-L for the treatment of pediatric SR-aGVHD, which met the primary
clinical endpoint with statistical significance, was conducted as a single-arm study due to the seriousness of the condition,
the rapid clinical deterioration of affected patients, the mounting literature suggesting a meaningful treatment effect, and
the position in the medical community that a randomized controlled trial was neither feasible nor ethical in this patient
population. In addition, new government requirements, including those resulting from new legislation, may be established,
or the FDA’s policies may change, which could delay or prevent regulatory approval of our products under development.
It is possible that we will have to participate in other Advisory Committee proceedings for other of our product
candidates. FDA Advisory Committees are convened to conduct public hearings on matters of importance that come before
the FDA, to review the issues involved, and to provide advice and recommendations to the FDA. New product candidates
may be referred for review by Advisory Committees whether the FDA has identified issues or concerns in respect of such
candidates or not. Advisory Committee input and recommendations may be used at the discretion of the FDA. Advisory
Committee proceedings are in part conducted publicly. While the recommendations made by Advisory Committees in
respect of marketing applications for any product are not dispositive, such determinations and recommendations are often
influential, and may be made available publicly and to the advantage of our competitors. In addition, it is possible that
safety findings and recommendations as well as other concerns and considerations raised by Advisory Committee
members, who constitute a multi-disciplinary group of experts (including representatives and/or advocates from the
consumer sector), may impact the FDA’s review of our product candidate submissions or labeling unfavorably.
Furthermore, commentary from Advisory Committee proceedings can figure into future product and other litigation.
Even if we receive regulatory approval for a product, such approval may entail limitations on the indicated uses for
which such product may be marketed and/or require post-marketing testing and surveillance to monitor safety or efficacy
of our product. The FDA may limit further marketing of our product based on the results of post-marketing studies, if
compliance with pre- and post-marketing regulatory standards is not maintained, or if problems occur after our product
reaches the marketplace such as later discovery of previously unknown problems or concerns with our product, including
adverse events of unanticipated severity or frequency, or with our manufacturing processes.
Risks Related to Collaborators
We rely on third parties to conduct our nonclinical and clinical studies and perform other tasks for us. If these third
parties do not successfully carry out their contractual duties, meet expected deadlines, or comply with regulatory
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requirements, we may not be able to obtain regulatory approval for or commercialize our product candidates in a timely
and cost-effective manner or at all, and our business could be substantially harmed.
We have relied upon and plan to continue to rely upon third-party entities, including CROs, academic institutions,
hospitals and other third-party collaborators, to monitor, support, conduct and/or oversee preclinical and clinical studies of
our current and future product candidates. We rely on these parties for execution of our nonclinical and clinical studies, and
control only certain aspects of their activities. Nevertheless, we are responsible for ensuring that each of our studies is
conducted in accordance with the applicable protocol, legal, regulatory, and scientific standards and our reliance on the
CROs does not relieve us of our regulatory responsibilities. If we or any of these third-parties fail to comply with the
applicable protocol, legal, regulatory, and scientific standards, the clinical data generated in our clinical studies may be
deemed unreliable and the FDA, EMA or comparable foreign regulatory authorities may require us to perform additional
clinical studies before approving our marketing applications.
If any of our relationships with these third parties terminate, we may not be able to enter into arrangements with
alternative parties or do so on commercially reasonable terms. In addition, these parties are not our employees, and except
for remedies available to us under our agreements with such third parties, we cannot control whether or not they devote
sufficient time and resources to our on-going nonclinical and clinical programs. If third parties do not successfully carry
out their contractual duties or obligations or meet expected deadlines, if they need to be replaced or if the quality or
accuracy of the data they obtain is compromised due to the failure to adhere to our protocols, regulatory requirements, or
for other reasons, our clinical studies may be extended, delayed, or terminated and we may not be able to obtain regulatory
approval for or successfully commercialize our product candidates. Third parties may also generate higher costs than
anticipated. As a result, our results of operations and the commercial prospects for our product candidates would be
harmed, our costs could increase, and our ability to generate revenue could be delayed.
Switching or adding additional third parties involves additional cost and requires management time and focus. In
addition, there is a natural transition period when a new third party commences work. As a result, delays occur, which can
materially impact our ability to meet our desired clinical development timelines. Though we carefully manage our
relationships with these third parties, there can be no assurance that we will not encounter similar challenges or delays in
the future or that these delays or challenges will not have a material adverse impact on our business, financial condition,
and prospects.
Our existing product development and/or commercialization arrangements, and any that we may enter into in the
future, may not be successful, which could adversely affect our ability to develop and commercialize our product
candidates.
We are a party to, and continue to seek additional, collaboration arrangements with biopharmaceutical companies for
the development and/or commercialization of our current and future product candidates. We may enter into new
arrangements on a selective basis depending on the merits of retaining certain development and commercialization rights
for ourselves as compared to entering into selective collaboration arrangements with leading pharmaceutical or
biotechnology companies for each product candidate, both in the United States and internationally. To the extent that we
decide to enter into collaboration agreements, we will face significant competition in seeking appropriate collaborators.
Any failure to meet our clinical milestones with respect to an unpartnered product candidate would make finding a
collaborator more difficult. Moreover, collaboration arrangements are complex, costly and time consuming to negotiate,
document and implement, and we cannot guarantee that we can successfully maintain such relationships or that the terms
of such arrangements will be favorable to us. If we fail to establish and implement collaboration or other alternative
arrangements, the value of our business and operating results will be adversely affected.
We may not be successful in our efforts to establish, implement and maintain collaborations or other alternative
arrangements if we choose to enter into such arrangements. The terms of any collaboration or other arrangements that we
may establish may not be favorable to us. The management of collaborations may take significant time and resources that
distract our management from other matters.
Our ability to successfully collaborate with any existing or future collaborators may be impaired by multiple factors
including:
•
a collaborator may shift its priorities and resources away from our programs due to a change in business
strategies, or a merger, acquisition, sale or downsizing of its company or business unit;
•
a collaborator may cease development in therapeutic areas which are the subject of our strategic alliances;
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•
a collaborator may change the success criteria for a particular program or product candidate thereby delaying
or ceasing development of such program or candidate;
•
a significant delay in initiation of certain development activities by a collaborator will also delay payments
tied to such activities, thereby impacting our ability to fund our own activities;
•
a collaborator could develop a product that competes, either directly or indirectly, with our current or future
products, if any;
•
a collaborator with commercialization obligations may not commit sufficient financial or human resources to
the marketing, distribution or sale of a product;
•
a collaborator with manufacturing responsibilities may encounter regulatory, resource or quality issues and be
unable to meet demand requirements;
•
a collaborator may exercise its rights under the agreement to terminate our collaboration;
•
a dispute may arise between us and a collaborator concerning the research or development of a product
candidate or commercialization of a product resulting in a delay in milestones, royalty payments or
termination of a program and possibly resulting in costly litigation or arbitration which may divert
management attention and resources;
•
the results of our clinical trials may not match our collaborators’ expectations, even if statistically significant;
•
a collaborator may not adequately protect or enforce the intellectual property rights associated with a product
or product candidate; and
•
a collaborator may use our proprietary information or intellectual property in such a way as to invite litigation
from a third party.
Any such activities by our current or future collaborators could adversely affect us financially and could harm our
business reputation.
Risks Related to Our Manufacturing and Supply Chain
We have no experience manufacturing our product candidates at a commercial scale. We may not be able to
manufacture our product candidates in quantities sufficient for development and commercialization if our product
candidates are approved, or for any future commercial demand for our product candidates.
We have manufactured clinical and commercial quantities of our mesenchymal lineage cell product candidates in
manufacturing facilities owned by Lonza Walkersville, Inc. and Lonza Bioscience Singapore Pte. Ltd. (collectively referred
to as “Lonza”). In 2023, FDA conducted a pre-license inspection of the manufacturing process of remestemcel-L which did
not result in the issuance of a Form 483 and there were no observed concerns. On approval, the process will be subject to
continued surveillance inspections, typically on a 3 year cycle, to ensure ongoing compliance with Good Manufacturing
Practices.
The production of any biopharmaceutical, particularly cell-based therapies, involves complex processes and
protocols. We cannot provide assurance that such production efforts will enable us to manufacture our product candidates
in the quantities and with the quality needed and in a timely manner for clinical trials, regulatory approval(s), and/or any
resulting commercialization.
If we are unable to do so, our clinical trials and commercialization efforts, if any, may not proceed in a timely
fashion and our business will be adversely affected. If any of our product candidates are approved for commercialization
and marketing, we may be required to manufacture the product in large quantities to meet demand. Producing product in
commercial quantities requires developing and adhering to complex manufacturing processes that are different from the
manufacture of a product in smaller quantities for clinical trials, including adherence to additional and more demanding
regulatory standards. Although we believe that we have developed processes and protocols that will enable us to
consistently manufacture commercial-scale quantities of product, we cannot provide assurance that such processes and
protocols will enable us to manufacture our product candidates in quantities that may be required for commercialization of
the product with yields and at costs that will be commercially attractive. If we are unable to establish or maintain
commercial manufacture of the product or are unable to do so at costs that we currently anticipate, our business will be
adversely affected.
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We are focusing on the introduction of novel manufacturing approaches with the potential to result in efficiency and
yield improvements to our current process. Certain of these novel approaches include modifying the media used in cell
production. Another approach includes the development of 3-dimensional (“3D”) bioreactor-based production for
mesenchymal lineage cells. There is no guarantee that we will successfully complete either of these processes or meet all
applicable regulatory requirements. This may be due to multiple factors, including the failure to produce sufficient
quantities and the inability to produce cells that are equivalent in physical and therapeutic properties as compared to the
products produced using our current manufacturing processes. In the event our transition to these improved manufacturing
processes is unsuccessful, we may not be able to produce certain of our products in a cost-efficient manner and our
business may be adversely affected.
Global events may adversely impact the manufacturing and commercialization of remestemcel-L, and other product
candidates.
On October 17, 2019, we announced that we had entered into a manufacturing service agreement with Lonza
Bioscience Singapore Pte. Ltd. for the supply of commercial product for the potential approval and launch of remestemcel-
L. We currently also manufacture our other product candidates with Lonza Singapore.
Due to the after-effects of the COVID-19 pandemic, and recent geopolitical instability, countries in which we have
operations, including Singapore, have experienced some challenges in the ability of our suppliers and contractors to source,
supply or acquire raw materials or components needed for our manufacturing process and supply chain. As a result, the
manufacturing and commercialization of remestemcel-L and other product candidates could be adversely affected if those
impacts and impacts from other disruptive events such as significant climate and geopolitical events are experienced, with
potential for increased costs.
We rely on contract manufacturers to supply and manufacture our product candidates. Our business could be harmed if
Lonza fails to provide us with sufficient quantities of these product candidates or fails to do so at acceptable quality
levels or prices.
We do not currently have, nor do we plan to acquire, the infrastructure or capability internally to manufacture our
mesenchymal lineage cell product candidates for use in the conduct of our clinical trials, and we currently lack the internal
resources and the capability to manufacture any of our product candidates on a clinical or commercial scale. As a result, we
currently depend on Lonza to manufacture our mesenchymal lineage cell product candidates. Relying on Lonza to
manufacture our mesenchymal lineage cell product candidates entails risks, and Lonza may:
•
cease or reduce production or deliveries, raise prices or renegotiate terms;
•
be unable to meet any product specifications and quality requirements consistently;
•
delay or be unable to procure or expand sufficient manufacturing capacity, which may harm our reputation or
frustrate our customers;
•
not have the capacity sufficient to support the scale-up of manufacturing for our product candidates;
•
have manufacturing and product quality issues related to scale-up of manufacturing;
•
experience costs and validation of new equipment facilities requirement for scale-up that it will pass on to us;
•
fail to comply with cGMP and similar international standards;
•
lose its manufacturing facility in Singapore, stored inventory or laboratory facilities through fire or other
causes, or other loss of materials necessary to manufacture our product candidates;
•
experience disruptions to its operations by conditions unrelated to our business or operations, including the
bankruptcy or interruptions of its suppliers;
•
experience carrier disruptions or increased costs that it will pass on to us;
•
fail to secure adequate supplies of essential ingredients in our manufacturing process;
•
experience failure of third parties involved in the transportation, storage or distribution of our products,
including the failure to deliver supplies it uses for the manufacture of our product candidates under specified
storage conditions and in a timely manner;
•
terminate agreements with us; and
•
appropriate or misuse our trade secrets and other proprietary information.
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Any of these events could lead to delays in the development of our product candidates, including delays in our
clinical trials, or failure to obtain regulatory approval for our product candidates, or it could impact our ability to
successfully commercialize our current product candidates or any future products. Some of these events could be the basis
for FDA or other regulatory action, including injunction, recall, seizure or total or partial suspension of production.
In addition, the lead time needed to establish a relationship with a new manufacturer can be lengthy and expensive,
and we may experience delays in meeting demand in the event we must switch to a new manufacturer. We are expanding
our manufacturing collaborations in order to meet future demand and to provide back-up manufacturing options, which
also involves risk and requires significant time and resources. Our future collaborators may need to expand their facilities
or alter the facilities to meet future demand and changes in regulations. These activities may lead to delays, interruptions to
supply, or may prove to be more costly than anticipated. Any problems in our manufacturing process could have a material
adverse effect on our business, results of operations and financial condition.
We may not be able to manufacture or commercialize our product candidates in a profitable manner.
We intend to implement a business model under which we control the manufacture and supply of our product
candidates, including but not exclusively, through our product suppliers, including Lonza. We and the suppliers of our
product candidates, including Lonza, have no experience manufacturing our product candidates at commercial scale.
Accordingly, there can be no assurance as to whether we and our suppliers will be able to scale-up the manufacturing
processes and implement technological improvements in a manner that will allow the manufacture of our product
candidates in a cost effective manner. Our or our collaborators’ inability to sell our product candidates at a price that
exceeds our cost of manufacture by an amount that is profitable for us will have a material adverse result on the results of
our operations and our financial condition.
Collaborators’ ability to identify, test and verify new donor tissue in order to create new master cell banks involves many
risks.
The initial stage of manufacturing involves obtaining mesenchymal lineage cell-containing bone marrow from
donors, for which we currently rely on our suppliers. Mesenchymal lineage cells are isolated from each donor’s bone
marrow and expanded to create a master cell bank. Each individual master cell bank comes from a single donor. A single
master cell bank can source many production runs, which in turn can produce up to thousands of doses of a given product,
depending on the dose level. The process of identifying new donor tissue, testing and verifying its validity in order to
create new master cell banks and validating such cell bank with the FDA and other regulatory agencies is time consuming,
costly and prone to the many risks involved with creating living cell products. There could be consistency or quality
control issues with any new master cell bank. Although we believe we and our collaborators have the necessary know-how
and processes to enable us to create master cell banks with consistent quality and within the timeframe necessary to meet
projected demand and we have begun doing so, we cannot be certain that we or our collaborators will be able to
successfully do so, and any failure or delays in creating new master cell banks may have a material adverse impact on our
business, results of operations, financial conditions and growth prospects and could result in our inability to continue
operations.
We and our collaborators depend on a limited number of suppliers for our product candidates’ materials, equipment or
supplies and components required to manufacture our product candidates. The loss of these suppliers, or their failure to
provide quality supplies on a timely basis, could cause delays in our current and future capacity and adversely affect our
business.
We and our collaborators depend on a limited number of suppliers for the materials, equipment and components
required to manufacture our product candidates, as well as various “devices” or “carriers” for some of our programs (e.g.,
the catheter for use with MPC-150-IM, and the hyaluronic acid used for chronic lower back pain). The main consumable
used in our manufacturing process is our media, which currently is sourced from fetal bovine serum (“FBS”). This material
comes from limited sources, and as a result is expensive. Consequently, we or our collaborators may not be able to obtain
sufficient quantities of our product candidates or other critical materials equipment and components in the future, at
affordable prices or at all. A delay or interruption by our suppliers may also harm our business, and operating results. In
addition, the lead time needed to establish a relationship with a new supplier can be lengthy, and we or our collaborators
may experience delays in meeting demand in the event we must switch to a new supplier. The time and effort to qualify for
and, in some cases, obtain regulatory approval for a new supplier could result in additional costs, diversion of resources or
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reduced manufacturing yields, any of which would negatively impact our operating results. Our and our collaborators’
dependence on single-source suppliers exposes us to numerous risks, including the following:
•
our or our collaborators’ suppliers may cease or reduce production or deliveries, raise prices or renegotiate
terms;
•
our or our collaborators’ suppliers may not be able to source materials, equipment or supplies and
components required to manufacture our product candidates as a result of the after-effects of the COVID-19
pandemic or geopolitical and/or economic instability adversely or the impact of climate events affecting the
supply chain;
•
we or our collaborators may be unable to locate suitable replacement suppliers on acceptable terms or on a
timely basis, or at all; and
•
delays caused by supply issues may harm our reputation, frustrate our customers and cause them to turn to our
competitors for future needs.
We and our collaborators and Lonza are subject to significant regulation with respect to manufacturing our product
candidates. The Lonza manufacturing facilities on which we rely may not continue to meet regulatory requirements or
may not be able to meet supply demands.
All entities involved in the preparation of therapeutics for clinical studies or commercial sale, including our existing
manufacturers, including Lonza, are subject to extensive regulation. Components of a finished therapeutic product
approved for commercial sale or used in late-stage clinical studies must be manufactured in accordance with current
international Good Manufacturing Practice and other international regulatory requirements. These regulations govern
manufacturing processes and procedures (including record keeping) and the implementation and operation of quality
systems to control and assure the quality of investigational products and products approved for sale. Poor control of
production processes can lead to the introduction of contaminants or to inadvertent changes in the properties or stability of
our product candidates. We, our collaborators, or suppliers must supply all necessary documentation in support of a BLA
on a timely basis and must adhere to current Good Laboratory Practice and current Good Manufacturing Practice
regulations enforced by the FDA and other regulatory agencies through their facilities inspection program. Lonza and other
suppliers have never produced a commercially approved cellular therapeutic product and therefore have not yet obtained
the requisite regulatory authority approvals to do so.
Before we can begin commercial manufacture of our products for sale in the United States, we must obtain FDA
regulatory approval for the product, in addition to the approval of the processes and quality systems associated with the
manufacturing of such product, which requires a successful FDA inspection of the facility handling the manufacturing of
our product, including Lonza’s manufacturing facilities. The novel nature of our product candidates creates significant
challenges in regards to manufacturing. For example, the U.S. federal and state governments and other jurisdictions impose
restrictions on the acquisition and use of tissue, including those incorporated in federal Good Tissue Practice regulations.
We may not be able to identify or develop sources for the cells necessary for our product candidates that comply with these
laws and regulations.
In addition, the regulatory authorities may, at any time before or after product approval, audit or inspect a
manufacturing facility involved with the preparation of our product candidates or raw materials or the associated quality
systems for compliance with the regulations applicable to the activities being conducted. In 2023, FDA conducted a pre-
license inspection of the manufacturing process of remestemcel-L which did not result in the issuance of a Form 483 and
there were no observed concerns. Although we oversee each contract manufacturer involved in the production of our
product candidates, we cannot control the manufacturing process of, and are dependent on, the contract manufacturer for
compliance with the regulatory requirements. If the contract manufacturer is unable to comply with manufacturing
regulations, we may be subject to fines, unanticipated compliance expenses, recall or seizure of any approved products,
total or partial suspension of production and/or enforcement actions, including injunctions, and criminal or civil
prosecution. These possible sanctions would adversely affect our business, results of operations and financial condition. If
the manufacturer fails to maintain regulatory compliance, the FDA or other applicable regulatory authority can impose
regulatory sanctions including, among other things, refusal to approve a pending application for a new drug product or
biologic product, withdrawal of an approval, or suspension of production. As a result, our business, financial condition, and
results of operations may be materially harmed.
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We will rely on third parties to perform many necessary services for the commercialization of our product candidates,
including services related to the distribution, storage and transportation of our products.
We will rely upon third parties for certain storage, distribution and other logistical services. In accordance with
certain laws, regulations and specifications, our product candidates must be stored and transported at extremely low
temperatures within a certain range. If these environmental conditions deviate, our product candidates’ remaining shelf-
lives could be impaired or their efficacy and safety could become adversely affected, making them no longer suitable for
use. If any of the third parties that we intend to rely upon in our storage, distribution and other logistical services process
fail to comply with applicable laws and regulations, fail to meet expected deadlines, or otherwise do not carry out their
contractual duties to us, or encounter physical damage or natural disaster at their facilities, our ability to deliver product to
meet commercial demand may be significantly impaired. In addition, as our cellular therapies will constitute a new form of
product, experience in commercial distribution of such therapies in the United States is extremely limited, and as such is
subject to execution risk. While we intend to work closely with our selected distribution logistics providers to define
appropriate parameters for their activities to ensure product remains intact throughout the process, there is no assurance that
such logistics providers will be able to maintain all requirements and handle and distribute our products in a manner that
does not significantly impair them, which may impact our ability to satisfy commercial demand. Likewise, the after-effects
from the COVID-19 pandemic, geopolitical and economic instability, and climate events may adversely impact access to
raw materials and distribution, storage and transportation of our products, and the cost of those activities.
Product recalls or inventory losses caused by unforeseen events may adversely affect our operating results and financial
condition.
Our product candidates are manufactured, stored and distributed using technically complex processes requiring
specialized facilities, highly specific raw materials and other production constraints. The complexity of these processes, as
well as strict company and government standards for the manufacture, storage and distribution of our product candidates,
subjects us to risks. For example, during the manufacturing process we have from time to time experienced several
different types of issues that have led to a rejection of various batches. Historically, the most common reasons for batch
rejections include major process deviations during the production of a specific batch and failure of manufactured product to
meet one or more specifications. While product candidate batches released for the use in clinical trials or for
commercialization undergo sample testing, some latent defects may only be identified following product release. In
addition, process deviations or unanticipated effects of approved process changes may result in these product candidates
not complying with stability requirements or specifications. The occurrence or suspected occurrence of production and
distribution difficulties can lead to lost inventories, and in some cases product recalls, with consequential reputational
damage and the risk of product liability. The investigation and remediation of any identified problems can cause production
delays, substantial expense, lost sales and delays of new product launches. In the event our production efforts require a
recall or result in an inventory loss, our operating results and financial condition may be adversely affected.
Risks Related to Commercialization of Our Product Candidates
Our future commercial success depends upon attaining significant market acceptance of our product candidates, if
approved, among physicians, patients and healthcare payors.
Even when product development is successful and regulatory approval has been obtained, our ability to generate
significant revenue depends on the acceptance of our products by physicians, payors and patients. Many potential market
participants have limited knowledge of, or experience with, cell therapy-based products, so gaining market acceptance and
overcoming any safety or efficacy concerns may be more challenging than for more traditional therapies. Our efforts to
educate the medical community and third-party payors on the benefits of our product candidates may require significant
resources and may never be successful. Such efforts to educate the marketplace may require more or different resources
than are required by the conventional therapies marketed by our competitors. We cannot assure you that our products will
achieve the expected market acceptance and revenue if and when they obtain the requisite regulatory approvals.
Alternatively, even if we obtain regulatory approval, that approval may be for indications or patient populations that are not
as broad as intended or desired or may require labeling that includes significant use or distribution restrictions or safety
warnings. The market acceptance of each of our product candidates will depend on a number of factors, including:
•
the efficacy and safety of the product candidate, as demonstrated in clinical trials;
•
the clinical indications for which the product is approved, and the label approved by regulatory authorities for
use with the product, including any warnings or contraindications that may be required on the label;
•
acceptance by physicians, patients, and with pediatric indications by parents/caregivers of the product as a
safe and effective treatment;
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•
the cost, safety and efficacy of treatment in relation to alternative treatments;
•
the continued projected growth of markets for our various indications;
•
relative convenience and ease of administration;
•
the prevalence and severity of adverse side effects;
•
the effectiveness of our, and our collaborators’ sales and marketing efforts; and
•
sufficient third-party insurance and other payor (e.g., governmental) coverage and reimbursement.
Market acceptance is critical to our ability to generate significant revenue. Any product candidate, if approved and
commercialized, may be accepted in only limited capacities or not at all. If any approved products are not accepted by the
market to the extent that we expect, we may not be able to generate significant revenue and our business would suffer.
If, in the future, we are unable to establish our own commercial capabilities across sales, marketing and distribution, or
enter into licensing or collaboration agreements for these purposes, we may not be successful in independently
commercializing any future products.
We have limited sales, marketing or distribution infrastructure and experience. Commercializing our product
candidates, if such product candidates obtain regulatory approval, would require significant sales, distribution and
marketing capabilities. Where and when appropriate, we may elect to utilize contract sales forces or distribution
collaborators to assist in the commercialization of our product candidates. If we enter into arrangements with third parties
to perform sales, marketing and distribution/price reporting services for our product candidates, the resulting revenue or the
profitability from this revenue to us may be lower than if we had sold, marketed and distributed that product ourselves. In
addition, we may not be successful in entering into arrangements with third parties to sell, market and distribute any future
products or may be unable to do so on terms that are favorable to us. We may have little control over such third parties, and
any of these third parties may fail to devote the necessary resources and attention to sell, market and distribute our current
or any future products effectively.
To the extent we are unable to engage third parties to assist us with these functions, we will have to invest
significant amounts of financial and management resources, some of which will need to be committed prior to any
confirmation that any of our proprietary product candidates will be approved. For any future products for which we decide
to perform sales, marketing and distribution functions ourselves, we could face a number of additional risks, including:
•
our inability to recruit and retain adequate numbers of effective sales and marketing personnel or to develop
alternative sales channels;
•
the inability of sales personnel to obtain access to physicians or persuade adequate numbers of physicians to
prescribe any future products;
•
the inability of account teams to obtain formulary acceptance for our products, allowing for reimbursement
and hence patient access;
•
the lack of complementary products to be offered by sales personnel, which may put us at a competitive
disadvantage relative to companies with multiple products; and
•
unforeseen costs and expenses associated with creating and maintaining an independent sales and marketing
organization.
We face substantial competition, which may result in others discovering, developing or commercializing products
before, or more successfully, than we do.
The biopharmaceutical industry is highly competitive and subject to rapid change. The industry continues to expand
and evolve as an increasing number of competitors and potential competitors enter the market. Many of our potential
competitors have significantly greater development, financial, manufacturing, marketing, technical and human resources
than we do. Large pharmaceutical companies, in particular, have extensive experience in conducting clinical trials,
obtaining regulatory approvals, manufacturing pharmaceutical and biologic products and commercializing such therapies.
Recent and potential future merger and acquisition activity in the biotechnology and pharmaceutical industries may result
in even more resources being concentrated among a smaller number of our competitors. Established pharmaceutical
companies may also invest heavily to accelerate discovery and development of novel compounds that could make our
product candidates obsolete. As a result of all of these factors, our competitors may succeed in obtaining patent protection
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and/or FDA approval or discovering, developing and commercializing our product candidates or competitors to our product
candidates before we do. Specialized, smaller or early-stage companies may also prove to be significant competitors,
particularly those with a focus and expertise in cell therapies. In addition, any new product that competes with an approved
product must demonstrate compelling advantages in efficacy, convenience, tolerability and safety in order to overcome
price competition and to be commercially successful. If we are not able to compete effectively against potential
competitors, our business will not grow and our financial condition and results of operations will suffer.
Our marketed products may be used by physicians for indications that are not approved by the FDA. If the FDA finds
that we marketed our products in a manner that promoted off-label use, we may be subject to civil or criminal penalties.
Under the Federal Food, Drug and Cosmetic Act (“FDCA”), and other laws and regulations, if any of our product
candidates are approved by the FDA, we would be prohibited from promoting our products for off-label uses. This means,
for example, that we would not be able to make claims about the use of our marketed products outside of their approved
indications, and we would not be able to proactively discuss or provide information on off-label uses of such products, with
very specific and limited exceptions. The FDA does not, however, prohibit physicians from prescribing products for off-
label uses in the practice of medicine. Should the FDA determine that our activities constituted the promotion of off-label
use, the FDA could issue a warning or untitled letter or, through the Department of Justice, bring an action for seizure or
injunction, and could seek to impose fines and penalties on us and our executives. In addition, failure to follow FDA rules
and guidelines relating to promotion and advertising can result in, among other things, the FDA’s refusal to approve a
product, the suspension or withdrawal of an approved product from the market, product recalls, fines, disgorgement of
money, operating restrictions, injunctions or criminal prosecutions, and also may figure into civil litigation against us.
Healthcare legislative reform measures may have a material adverse effect on our business and results of operations.
In the United States, there have been and continue to be a number of legislative initiatives to contain healthcare
costs. For example, in 2010, the Patient Protection and Affordable Care Act, as amended by the Health Care and Education
Reconciliation Act, or collectively, the Affordable Care Act, was passed. The Affordable Care Act is a sweeping law
intended to broaden access to health insurance, reduce or constrain the growth of healthcare spending, enhance remedies
against fraud and abuse, add new transparency requirements for healthcare and the health insurance industry, impose new
taxes and fees on the healthcare industry and impose additional health policy reforms. In addition, on August 16, 2022, the
U.S. government enacted the Inflation Reduction Act of 2022, which, among other things, includes policies that are
designed to have a direct impact on drug prices and reduce drug spending by the federal government. There have been a
number of judicial challenges to certain aspects of each law. We can provide no assurance that laws such as the Affordable
Care Act or the Inflation Reduction Act, as currently enacted or as amended in the future, will not adversely affect our
business and financial results, and we cannot predict how future federal or state legislative or administrative changes
relating to healthcare reform will affect our business.
Currently, the outcome of potential reforms and changes to government negotiation/regulation to healthcare costs
are unknown. If changes in policy limit reimbursements that we are able to receive through federal programs, it could
negatively impact reimbursement levels from those payors and private payors, and our business, revenues or profitability
could be adversely affected.
If we or our collaborators fail to obtain and sustain an adequate level of reimbursement for our products by third-party
payors, sales and profitability would be adversely affected.
Our and our collaborators’ ability to commercialize any products successfully will depend, in part, on the extent to
which coverage and reimbursement for our products and related treatments will be available from government healthcare
programs, private health insurers, managed care plans, and other organizations. Additionally, even if there is a
commercially viable market, if the level of third-party reimbursement is below our expectations, our revenue and
profitability could be materially and adversely affected.
Third-party payors, such as government programs, including Medicare or Medicaid in the United States, or private
healthcare insurers, carefully review and increasingly question the coverage of, and challenge the prices charged for
medical products and services, and many third-party payors limit or delay coverage of or reimbursement for newly
approved healthcare products. Reimbursement rates from private health insurance companies vary depending on the
company, the insurance plan and other factors, including the third-party payor’s determination that use of a product is:
•
a covered benefit under its health plan;
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•
safe, effective and medically necessary;
•
appropriate for the specific patient;
•
cost-effective; and
•
neither experimental nor investigational.
A current trend in the U.S. healthcare industry as well as in other countries around the world is toward cost
containment. Large public and private payors, managed care organizations, group purchasing organizations and similar
organizations are exerting increasing influence on decisions regarding the use of, and reimbursement levels for, particular
treatments. In particular, third-party payors may limit the covered indications. Cost-control initiatives could decrease the
price we might establish for any product, which could result in product revenue and profitability being lower than
anticipated.
There may be significant delays in obtaining coverage and reimbursement for newly approved drugs, and coverage
may be more limited than the purposes for which the drug is approved by the FDA or other regulatory authorities.
Moreover, eligibility for coverage and reimbursement does not imply that a drug will be paid for in all cases or at a rate that
covers our costs, including research, development, manufacture, sale and distribution expenses. Interim reimbursement
levels for new drugs, if applicable, may also be insufficient to cover our and any collaborator’s costs and may not be made
permanent. Reimbursement rates may vary according to the use of the drug and the clinical setting in which it is used, may
be based on reimbursement levels already set for lower cost drugs and may be incorporated into existing payments and
treatment codes for other services. Our inability to promptly obtain coverage and profitable payment rates from both
government-funded and private payors for any approved products that we develop could have a material adverse effect on
our operating results, our ability to raise capital needed to commercialize products and our overall financial condition.
Furthermore, reimbursement systems in international markets vary significantly by country and by region, and
reimbursement approvals must be obtained on a country-by-country basis. Our existing or future collaborators, if any, may
elect to reduce the price of our products in order to increase the likelihood of obtaining reimbursement approvals which
could adversely affect our revenues and profits. In many countries, including for example in Japan, products cannot be
commercially launched until reimbursement is approved. Further, the post-approval price negotiation process in some
countries can exceed 12 months. In addition, pricing and reimbursement decisions in certain countries can be affected by
decisions taken in other countries, which can lead to mandatory price reductions and/or additional reimbursement
restrictions across a number of other countries, which may thereby adversely affect our sales and profitability. In the event
that countries impose prices which are not sufficient to allow us or our collaborators to generate a profit, our collaborators
may refuse to launch the product in such countries or withdraw the product from the market, which would adversely affect
sales and profitability.
Due to the novel nature of our cell therapy and the potential for our product candidates to offer therapeutic benefit in a
single administration, we face uncertainty related to pricing and reimbursement for these product candidates.
Our target patient populations for some of our product candidates may be relatively small, and as a result, the pricing
and reimbursement of our product candidates, if approved, must be adequate to support commercial infrastructure. If we
are unable to obtain adequate levels of reimbursement, our ability to successfully market and sell our product candidates
will be adversely affected. Due to the novel nature of our cell therapy technology, the manner and level at which
reimbursement is provided for services related to our product candidates (e.g., for administration of our product to patients)
is uncertain. Inadequate reimbursement for such services may lead to physician resistance and adversely affect our ability
to market or sell our products. Further, if the results of our clinical trials and related cost benefit analyses do not clearly
demonstrate the efficacy or overall value of our product candidates in a manner that is meaningful to prescribers and
payors, our pricing and reimbursement may be adversely affected.
Price controls may be imposed in foreign markets, which may adversely affect our future profitability.
In some countries, particularly EU member states, Japan, Australia and Canada, the pricing of prescription drugs is
subject to governmental control. In these countries, pricing negotiations with governmental authorities can take
considerable time after receipt of marketing approval for a product. In addition, there can be considerable pressure by
governments and other stakeholders on prices and reimbursement levels, including as part of cost containment measures.
Political, economic and regulatory developments may further complicate pricing negotiations, and pricing negotiations may
continue after reimbursement has been obtained. Reference pricing used by various EU member states and parallel
distribution, or arbitrage between low-priced and high-priced member states, can further reduce prices. In some countries,
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we or our collaborators may be required to conduct a clinical trial or other studies that compare the cost-effectiveness of
our product candidates to other available therapies in order to obtain or maintain reimbursement or pricing approval.
Publication of discounts by third-party payors or authorities may lead to further pressure on the prices or reimbursement
levels within the country of publication and other countries. If reimbursement of our products is unavailable or limited in
scope or amount, or if pricing is set at unsatisfactory levels, our business, revenues or profitability could be adversely
affected.
If the market opportunities for our product candidates are smaller than we believe they are, our revenues may be
adversely affected and our business may suffer. Because the target patient populations of certain of our product
candidates are small, we must be able to successfully identify physicians with access to appropriate patients and achieve
a significant market share to maintain profitability and growth.
Our projections of the number of people with diseases targeted by our product candidates are based on estimates.
These estimates may prove to be incorrect and new studies may change the estimated incidence or prevalence of these
diseases. In addition, physicians who we believe have access to patients in need of our products may in fact not often treat
the diseases targeted by our product candidates, and may not be amenable to use of our product. Further, the number of
patients in the United States, Europe and elsewhere may turn out to be lower than expected, may not be otherwise
amenable to treatment with our products, or new patients may become increasingly difficult to identify or gain access to, all
of which would adversely affect our results of operations and our business.
We are exposed to risks related to our licensees and our international operations, and failure to manage these risks may
adversely affect our operating results and financial condition.
We and our subsidiaries operate out of Australia, the United States, Singapore, the United Kingdom and
Switzerland. We have licensees, with rights to commercialize products based on our MSC technology, including JCR in
Japan. Our primary manufacturing collaborator, Lonza, serves us primarily out of their facilities in Singapore, and through
contractual relationships with third parties, has access to storage facilities in the U.S., Europe, Australia and Singapore. As
a result, a significant portion of our operations are conducted by and/or rely on entities outside the markets in which certain
of our trials take place, our suppliers are sourced, our product candidates are developed, and, if any such product candidates
obtain regulatory approval, our products may be sold. Accordingly, we import a substantial number of products and/or
materials into such markets. We may be denied access to our customers, suppliers or other collaborators or denied the
ability to ship products from any of these sites as a result of a closing of the borders of the countries in which we operate,
or in which these operations are located, due to economic, legislative, political, health or military conditions in such
countries. If any of our product candidates are approved for commercialization, we may enter into agreements with third
parties to market them on a worldwide basis or in more limited geographical regions. We expect that we will be subject to
additional risks related to entering into international business relationships, including:
•
unexpected changes in tariffs, trade barriers and regulatory requirements;
•
economic weakness, including inflation, or political instability in particular foreign economies and markets;
•
logistics and regulations associated with shipping cell samples and other perishable items, including
infrastructure conditions and transportation delays;
•
potential import and export issues and other trade barriers and restrictions with the U.S. Customs and Border
Protection and similar bodies in other jurisdictions;
•
compliance with tax, employment, immigration and labor laws for employees living or traveling abroad;
•
workforce uncertainty in countries where labor unrest is more common than in the United States;
•
reduced protection for intellectual property rights in some countries and practical difficulties of enforcing
intellectual property and contract rights abroad;
•
changes in diplomatic and trade relationships, including new tariffs, trade protection measures, import or
export licensing requirements, trade embargoes and other trade barriers;
•
tariffs imposed by the U.S. on goods from other countries, including the recently implemented tariffs and
additional tariff that have been proposed by the U.S. government on various imports from China and the EU
and by the governments of these jurisdictions on certain U.S. goods, and any other possible tariffs that may be
imposed on products such as ours, the scope and duration of which, if implemented, remains uncertain;
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•
deterioration of political relations, for example between Russia and other nations, and between the U.K. and
members of the EU, which could have a material adverse effect on our supply chains, and sales and
operations in these countries;
•
changes in social, political and economic conditions or in laws, regulations and policies governing foreign
trade, manufacturing, development and investment both domestically as well as in the other countries and
jurisdictions into which we sell our products;
•
fluctuations in currency exchange rates and the related effect on our results of operations;
•
increased financial accounting and reporting burdens and complexities;
•
potential increases on tariffs or restrictions on trade generally;
•
production shortages resulting from any events affecting raw material supply or manufacturing capabilities
abroad; and
•
business interruptions resulting from geopolitical actions, including war (such as Russia’s invasion of
Ukraine) and terrorism, or climate related events and natural disasters including earthquakes, typhoons, floods
and fires.
Use of animal-derived materials could harm our product development and commercialization efforts.
Some of the manufacturing materials and/or components that we use in, and which are critical to, implementation of
our technology involve the use of animal-derived products, including FBS. Suppliers or regulatory changes may limit or
restrict the availability of such materials for clinical and commercial use. While FBS is commonly used in the production
of various marketed biopharmaceuticals, the suppliers of FBS that meet our strict quality standards are limited in number
and region. As such, to the extent that any such suppliers or regions face an interruption in supply (for example, if there is a
new occurrence of so-called “mad cow disease”), it may lead to a restricted supply of the serum currently required for our
product manufacturing processes. Any restrictions on these materials would impose a potential competitive disadvantage
for our products or prevent our ability to manufacture our cell products. The FDA has issued regulations for controls over
bovine material in animal feed. These regulations do not appear to affect our ability to purchase the manufacturing
materials we currently use. However, the FDA may propose new regulations that could affect our operations. Our inability
to develop or obtain alternative compounds would harm our product development and commercialization efforts. There are
certain limitations in the supply of certain animal-derived materials, which may lead to delays in our ability to complete
clinical trials or eventually to meet the anticipated market demand for our cell products.
If product liability lawsuits are brought against us, we may incur substantial liabilities and may be required to limit
commercialization of our product candidates.
We face an inherent risk of product liability as a result of the human clinical use of our product candidates and will
face an even greater risk if we commercialize any products. For example, we may be sued if any product we develop
allegedly causes injury or is found to be otherwise unsuitable during product design, testing, manufacturing, marketing or
sale. Any such product liability claims may include allegations of defects in manufacturing, defects in design, a failure to
warn of dangers inherent in the product, negligence, strict liability, and a breach of warranties. Claims could also be
asserted under state consumer protection and other acts. If we cannot successfully defend ourselves against product liability
claims, we may incur substantial liabilities or be required to limit commercialization of our product candidates. Even a
successful defense would require significant financial and management resources. Regardless of the merits or eventual
outcome, liability claims may result in:
•
decreased demand for our products, even if such products are approved;
•
injury to our reputation;
•
withdrawal of clinical trial participants;
•
costs to defend the related litigations;
•
a diversion of management’s time and our resources;
•
substantial monetary awards to trial participants or patients;
•
product recalls, withdrawals, or labeling, marketing or promotional restrictions;
•
increased cost of liability insurance;
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•
loss of revenue;
•
the inability to commercialize our product candidates; and
•
a decline in our ordinary share price.
Failure to obtain and retain sufficient product liability insurance at an acceptable cost to protect against potential
product liability claims could prevent or inhibit the commercialization of products we develop. Additionally, our insurance
policies have various exclusions, and we may be subject to a product liability claim for which we have no coverage or
reduced coverage. Any claim that may be brought against us could result in a court judgment or settlement in an amount
that is not covered, in whole or in part, by our insurance or that is in excess of the limits of our insurance coverage. We will
have to pay any amounts awarded by a court or negotiated in a settlement that exceed our coverage limitations or that are
not covered by our insurance, and we may not have, or be able to obtain, sufficient capital to pay such amounts.
Risks Related to Our Intellectual Property
We may not be able to protect our proprietary technology in the marketplace.
Our success will depend, in part, on our ability to obtain patents, protect our trade secrets and operate without
infringing on the proprietary rights of others. We rely upon a combination of patents, trade secret protection, and
confidentiality agreements to protect the intellectual property of our product candidates. Patents might not be issued or
granted with respect to our patent applications that are currently pending, and issued or granted patents might later be found
to be invalid or unenforceable, be interpreted in a manner that does not adequately protect our current product or any future
products, or fail to otherwise provide us with any competitive advantage. As such, we do not know the degree of future
protection that we will have on our proprietary products and technology, if any, and a failure to obtain adequate intellectual
property protection with respect to our product candidates and proprietary technology could have a material adverse impact
on our business.
Filing, prosecuting and defending patents throughout the world would be prohibitively expensive, so our policy is to
patent technology in jurisdictions with significant or otherwise relevant commercial opportunities or activities. However,
patent protection may not be available for some of the products or technology we are developing. If we must spend
significant time and money protecting or enforcing our patents, designing around patents held by others or licensing,
potentially for large fees, patents or other proprietary rights held by others, our business, results of operations and financial
condition may be harmed.
The patent positions of biopharmaceutical products are complex and uncertain.
The scope and extent of patent protection for our product candidates are particularly uncertain. To date, our principal
product candidates have been based on specific subpopulations of known and naturally occurring adult stem cells. We
anticipate that the products we develop in the future will continue to include or be based on the same or other naturally
occurring stem cells or derivatives or products thereof. Although we have sought and expect to continue to seek patent
protection for our product candidates, their methods of use and methods of manufacture, any or all of them may not be
subject to effective patent protection. Publication of information related to our product candidates by us or others may
prevent us from obtaining or enforcing patents relating to these products and product candidates. Furthermore, others may
independently develop similar products, may duplicate our products, or may design around our patent rights. In addition,
any of our issued patents may be declared invalid. If we fail to adequately protect our intellectual property, we may face
competition from companies who attempt to create a generic product to compete with our product candidates. We may also
face competition from companies who develop a substantially similar product to our other product candidates that may not
be covered by any of our patents.
Filing, prosecuting and defending patents on product candidates in all countries throughout the world would be
prohibitively expensive, and our intellectual property rights in some countries outside the U.S. can be less extensive than
those in the U.S. In addition, the laws of some foreign countries do not protect intellectual property rights to the same
extent as federal and state laws in the U.S. Consequently, we may not be able to prevent third parties from practicing our
inventions in all countries outside the U.S., or from selling or importing products made using our inventions in and into the
U.S. or other jurisdictions. Competitors may use our technologies in jurisdictions where we have not obtained patent
protection to develop their own products and further, may export otherwise infringing products to territories where we have
patent protection, but enforcement is not as strong as that in the U.S. These products may compete with our current or
future products, if any, and our patents or other intellectual property rights may not be effective or sufficient to prevent
them from competing.
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Many companies have encountered significant problems in protecting and defending intellectual property rights in
foreign jurisdictions. The legal systems of certain countries do not favor the enforcement of patents, trade secrets and other
intellectual property protection, particularly those relating to biotechnology products, which could make it difficult for us to
stop the infringement of our patents or marketing of competing products in violation of our proprietary rights generally.
Proceedings to enforce our patent rights in foreign jurisdictions could result in substantial costs and divert our efforts and
attention from other aspects of our business, could put our patents at risk of being invalidated or interpreted narrowly and
our patent applications at risk of not issuing and could provoke third parties to assert claims against us. We may not prevail
in any lawsuits that we initiate and the damages or other remedies awarded, if any, may not be commercially meaningful.
Accordingly, our efforts to enforce our intellectual property rights around the world may be inadequate to obtain a
significant commercial advantage from the intellectual property that we develop or license.
We may be unable to adequately prevent disclosure of trade secrets and other proprietary information.
We maintain certain of our proprietary know-how and technological advances as trade secrets, especially where we
do not believe patent protection is appropriate or obtainable, including, but not exclusively, with respect to certain aspects
of the manufacturing of our products. However, trade secrets are difficult to protect. We take a number of measures to
protect our trade secrets including, limiting disclosure, physical security and confidentiality and non-disclosure agreements.
We enter into confidentiality agreements with our employees, consultants, outside scientific collaborators, contract
manufacturing partners, sponsored researchers and other advisors and third parties to protect our trade secrets and other
proprietary information. These agreements may not effectively prevent disclosure of confidential information and may not
provide an adequate remedy in the event of unauthorized disclosure of confidential information. In addition, others may
independently discover our trade secrets and proprietary information. Costly and time-consuming litigation could be
necessary to enforce and determine the scope of our proprietary rights. Failure to obtain or maintain trade secret protection,
or failure to adequately protect our intellectual property could enable competitors to develop generic products or use our
proprietary information to develop other products that compete with our products or cause additional, material adverse
effects upon our business, results of operations and financial condition.
We may be forced to litigate to enforce or defend our intellectual property rights, and/or the intellectual property rights
of our licensors.
We may be forced to litigate to enforce or defend our intellectual property rights against infringement by
competitors, and to protect our trade secrets against unauthorized use. In so doing, we may place our intellectual property at
risk of being invalidated, unenforceable, or limited or narrowed in scope and may no longer be used to prevent the
manufacture and sale of competitive product. Further, an adverse result in any litigation or other proceedings before
government agencies such as the United States Patent and Trademark Office (“USPTO”), may place pending applications
at risk of non-issuance. Further, interference proceedings, derivation proceedings, entitlement proceedings, ex parte
reexamination, inter partes reexamination, inter partes review, post-grant review, and opposition proceedings provoked by
third parties or brought by the USPTO or any foreign patent authority may be used to challenge inventorship, ownership,
claim scope, or validity of our patent applications. Furthermore, because of the substantial amount of discovery required in
connection with intellectual property litigation, there is a risk that some of our confidential and proprietary information
could be compromised by disclosure during this type of litigation.
Intellectual property disputes could cause us to spend substantial resources and distract our personnel from their
normal responsibilities.
Even if resolved in our favor, litigation or other legal proceedings relating to intellectual property claims may cause
us to incur significant expenses, and could distract our technical and/or management personnel from their normal
responsibilities. In addition, there could be public announcements of the results of hearings, motions or other interim
proceedings or developments and if securities analysts or investors perceive these results to be negative, it could have a
substantial adverse effect on the market price of our ADSs and ordinary shares. Such litigation or proceedings could
substantially increase our operating losses and reduce the resources available for development activities or any future sales,
marketing or distribution activities. We may not have sufficient financial or other resources to adequately conduct such
litigation or proceedings. Some of our competitors may be able to sustain the costs of litigation proceedings more
effectively than we can because of their greater financial resources and personnel. In addition, the uncertainties associated
with litigation could have a material adverse effect on our ability to raise the funds necessary to conduct our clinical trials,
continue our internal research programs, in-license needed technology or enter into strategic collaborations that would help
us bring our product candidates to market. As a result, uncertainties resulting from the initiation and continuation of patent
litigation or other proceedings could have a material adverse effect on our ability to compete in the marketplace.
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U.S. patent reform legislation and court decisions could increase the uncertainties and costs surrounding the
prosecution of our patent applications and the enforcement or defense of our issued U.S. patents.
Changes in either the patent laws or interpretation of the patent laws in the United States could increase the
uncertainties and costs surrounding the prosecution of patent applications and the enforcement or defense of issued patents.
Under the current patent laws, a third party that files a patent application in the USPTO before us for a particular invention
could therefore be awarded a patent covering such invention even if we had made that invention before it was made by
such third party. This requires us to be cognizant of the time from invention to filing of a patent application.
The current US legislation allows third party submissions of prior art to the USPTO during patent prosecution and
additional procedures for attacking the validity of a patent through USPTO administered post-grant proceedings, including
post-grant review, inter partes review, and derivation proceedings. Because a lower evidentiary standard applies in USPTO
proceedings compared to the evidentiary standards applied in United States federal courts in actions seeking to invalidate a
patent claim, a third party could potentially provide evidence in a USPTO proceeding sufficient for the USPTO to hold a
claim invalid even though the same evidence would be insufficient to invalidate the claim if challenged in a district court
action. Accordingly, a third party may attempt to use available USPTO procedures to invalidate our patent claims that
would not otherwise have been invalidated if first challenged by the third party in a district court action. These post-grant
review (PGR) proceedings, which are similar to European “opposition” proceedings and provide third-party petitioners
with the ability to challenge the validity of a patent on more expansive grounds than those permitted in other USTPO
proceedings, allow for validity to be examined by the USPTO based not only on prior art patents and publications, but also
on prior invalidating public use and sales, the presence of non-statutory subject matter in the patent claims and inadequate
written description or lack of enablement. Discovery for PGR proceedings is accordingly likely to be expansive given that
the issues addressed in PGR are more comprehensive than those addressed in other USPTO proceedings.
As compared to intellectual property-reliant companies generally, the patent positions of companies in the
development and commercialization of biologics and pharmaceuticals are particularly uncertain. Recent U.S. Supreme
Court rulings have narrowed the scope of patent protection available in certain circumstances and weakened the rights of
patent owners in certain situations. These rulings have created uncertainty with respect to the validity and enforceability of
patents, even once obtained. Depending on future actions by the U.S. Congress, the federal courts, and the USPTO, the
laws and regulations governing patents could change in unpredictable ways that could have a material adverse effect on our
existing patent portfolio and our ability to protect and enforce our intellectual property in the future.
If third parties claim that intellectual property used by us infringes upon their intellectual property, commercialization
of our product candidates and our operating profits could be adversely affected.
There is a substantial amount of litigation, both within and outside the United States, involving patent and other
intellectual property rights in the biopharmaceutical industry. We may, from time to time, be notified of claims that we are
infringing upon patents, trademarks, copyrights, or other intellectual property rights owned by third parties, and we cannot
provide assurances that other companies will not, in the future, pursue such infringement claims against us or any third-
party proprietary technologies we have licensed. Any such claims could also be expensive and time consuming to defend
and divert management’s attention and resources, and could delay or prevent us from commercializing our product
candidates. Our competitive position could suffer as a result. Although we have reviewed certain third-party patents and
patent filings that we believe may be relevant to our product candidates, we have not conducted a freedom-to-operate
search or analysis for our product candidates, and we may not be aware of patents or pending or future patent applications
that, if issued, would block us from commercializing our product candidates. Thus, we cannot guarantee that our product
candidates, or our commercialization thereof, do not and will not infringe any third party’s intellectual property.
If we do not obtain patent term extension in the United States under the Hatch-Waxman Act and in foreign countries
under similar legislation, thereby potentially extending the term of our marketing exclusivity of our product candidates,
our business may be materially harmed.
Depending on the timing, duration and specifics of FDA marketing approval of our product candidates, if any, one
of the U.S. patents covering each of such approved product(s) or the use thereof may be eligible for up to five years of
patent term restoration under the Hatch-Waxman Act. The Hatch-Waxman Act allows a maximum of one patent to be
extended per FDA approved product. Patent term extension also may be available in certain foreign countries upon
regulatory approval of our product candidates, including by the EMA in the EU or the PMDA in Japan. Nevertheless, we
may not be granted patent term extension either in the United States or in any foreign country because of, for example,
failing to apply within applicable deadlines, failing to apply prior to expiration of relevant patents or otherwise failing to
satisfy applicable requirements. Moreover, the term of extension, as well as the scope of patent protection during any such
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extension, afforded by the governmental authority could be less than we request. In addition, if a patent we wish to extend
is owned by another party and licensed to us, we may need to obtain approval and cooperation from our licensor to request
the extension.
If we are unable to obtain patent term extension or restoration, or the term of any such extension is less than we
request, the period before we might face generic or follow-on competition could be shortened and we may not be able to
stop our competitors from launching competing products following our patent expiration, and our revenue could be
reduced, possibly materially.
Risks Related to Our Business and Industry
If we fail to attract and keep senior management and key scientific, commercial, regulatory affairs and other personnel,
we may be unable to successfully develop our product candidates, conduct our clinical trials and commercialize our
product candidates.
We are highly dependent on members of our executive management, particularly Dr. Silviu Itescu, our Chief
Executive Officer. Dr. Itescu was an early pioneer in the study and clinical development of cell therapeutics and is globally
recognized in the field of regenerative medicine. The loss of the services of Dr. Itescu or any other member of the
executive management team could impede the achievement of our research, development and commercialization
objectives.
Recruiting and retaining qualified scientific, clinical, manufacturing, regulatory affairs, sales and marketing
personnel will also be critical to our success. We may not be able to attract and retain these personnel on acceptable terms
given the competition among numerous pharmaceutical and biotechnology companies for similar personnel. We also
experience competition for the hiring of scientific and clinical personnel from universities and research institutions.
Our employees, principal investigators, consultants and collaboration partners may engage in misconduct or other
improper activities, including noncompliance with laws and regulatory standards and requirements and insider trading.
We are exposed to the risk of employee fraud or other misconduct. Misconduct by employees could include failures
to comply with FDA regulations, to provide accurate information to the FDA, to comply with manufacturing standards we
have established, to comply with federal and state healthcare fraud and abuse laws and regulations, to report financial
information or data accurately or to disclose unauthorized activities to us. In particular, sales, marketing and business
arrangements (including arrangements with healthcare providers, opinion leaders, research institutions, distributors and
payors) in the healthcare industry are subject to extensive laws and regulations intended to prevent fraud, kickbacks, self-
dealing and other abusive practices. These laws and regulations restrict or prohibit a wide range of activity relating to
pricing, discounting, marketing and promotion, sales commissions, customer incentive programs and other business
arrangements. Employee misconduct could also involve the improper use of information obtained in the course of clinical
trials, which could result in regulatory sanctions and serious harm to our reputation, or, given we are a listed company in
Australia and the United States, breach of insider trading or other securities laws and regulations. It is not always possible
to identify and deter employee misconduct, and the precautions we take to detect and prevent this activity may not be
effective in controlling unknown or unmanaged risks or losses or in protecting us from governmental investigations or
other actions or lawsuits stemming from a failure to be in compliance with such laws or regulations. If any such actions are
instituted against us, and we are not successful in defending ourselves or asserting our rights, those actions could have a
significant impact on our business, including the imposition of significant fines or other sanctions.
We may acquire other companies or assets which could divert our management’s attention, result in additional dilution
to our shareholders and otherwise disrupt our operations and harm our operating results.
We have in the past and may in the future seek to acquire businesses, products or technologies that we believe could
complement or expand our product offerings, enhance our technical capabilities or otherwise offer growth opportunities.
For example, we acquired MSC assets in 2013. The pursuit of potential acquisitions may divert the attention of
management and cause us to incur various expenses in identifying, investigating and pursuing suitable acquisitions,
whether or not they are consummated. If we acquire additional businesses, we may not be able to integrate the acquired
personnel, operations and technologies successfully, or effectively manage the combined business following the
acquisition. We also may not achieve the anticipated benefits from the acquired business due to a number of factors,
including:
•
incurrence of acquisition-related costs;
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•
diversion of management’s attention from other business concerns;
•
unanticipated costs or liabilities associated with the acquisition;
•
harm to our existing business relationships with collaborators as a result of the acquisition;
•
harm to our brand and reputation;
•
the potential loss of key employees;
•
use of resources that are needed in other parts of our business; and
•
use of substantial portions of our available cash to consummate the acquisition.
In the future, if our acquisitions do not yield expected returns, we may be required to take charges to our operating
results arising from the impairment assessment process. Acquisitions may also result in dilutive issuances of equity
securities or the incurrence of debt, which could adversely affect our operating results. In addition, if an acquired business
fails to meet our expectations, our business, results of operations and financial condition may be adversely affected.
We and our collaborators must comply with environmental laws and regulations, and failure to comply with these laws
and regulations could expose us to significant liabilities.
We and our collaborators are subject to various federal, state and local environmental laws, rules and regulations,
including those relating to the discharge of materials into the air, water and ground, the manufacture, storage, handling, use,
transportation and disposal of hazardous and biological materials, and the health and safety of employees with respect to
laboratory activities required for the development of products and technologies. In the event of contamination or injury, or
failure to comply with environmental, occupational health and safety and export control laws and regulations, it could
cause an interruption of our commercialization efforts, research and development efforts, or business operations, and we
could be held liable for any resulting damages and any such liability could exceed our assets and resources.
We work with outside scientists and their institutions in developing product candidates. These scientists may have other
commitments or conflicts of interest, which could limit our access to their expertise and harm our ability to leverage our
discovery platform.
We work with scientific advisors and collaborators at academic research institutions in connection with our product
development. These scientific advisors serve as our link to the specific pools of trial participants we are targeting in that
these advisors may:
•
identify individuals as potential candidates for study;
•
obtain their consent to participate in our research;
•
perform medical examinations and gather medical histories;
•
conduct the initial analysis of suitability of the individuals to participate in our research based on the
foregoing; and
•
collect data and biological samples from trial participants periodically in accordance with our study protocols.
These scientists and collaborators are not our employees, rather they serve as either independent contractors or the
primary investigators under research collaboration agreements that we have with their sponsoring academic or research
institution. Such scientists and collaborators may have other commitments that would limit their availability to us.
Although our scientific advisors generally agree not to do competing work, if an actual or potential conflict of interest
between their work for us and their work for another entity arises, we may lose their services. It is also possible that some
of our valuable proprietary knowledge may become publicly known through these scientific advisors if they breach their
confidentiality agreements with us, which would cause competitive harm to our business.
If our ability to use cumulative carry forward net operating losses is or becomes subject to certain limitations or if
certain tax incentive credits from which we may benefit expire or no longer apply to us, our business, results of
operations and financial condition may be adversely affected.
We are an Australian company subject to taxation in Australia and other jurisdictions. As of June 30, 2024, our
cumulative operating losses have a total potential tax benefit of $214.7 million at local tax rates (excluding other temporary
differences). These losses may be available for use once we are in a tax profitable position. These losses were incurred in
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different jurisdictions and can only be offset against profits earned in the relevant jurisdictions. Tax losses are able to be
carried forward at their nominal amount indefinitely in Australia and in Singapore, and for up to 20 years in the U.S. as
long as certain conditions are met; however, new tax reform legislation in the United States allows for indefinite
carryforward of any net operating loss arising in a tax year ending after December 31, 2018, subject to certain conditions.
In order to use these tax losses, it is necessary to satisfy certain tests and, as a result, we cannot assure you that the tax
losses will be available to offset profits if and when we earn them. Utilization of our net operating loss and research and
development credit carryforwards in the U.S. may be subject to substantial annual limitation due to ownership change
limitations that could occur in the future generally provided by Section 382 of the Internal Revenue Code of 1986, as
amended. In addition, U.S. tax reform introduced a limitation on the amount of net operating losses arising in taxable years
beginning after December 31, 2017, that a corporation may deduct in a single tax year equal to the lesser of the available
net operating loss carryover or 80 percent of a taxpayer’s pre-net operating loss deduction taxable income. With respect to
carryforward net operating losses in the U.S. that are subject to the 20-year carry-forward limit, our carry forward net
operating losses first start to expire in 2032.
In addition, we may be eligible for certain research and development tax incentive refundable credits in Australia
that may increase our available cash flow. The Australian federal government's Research and Development Tax Incentive
grant is available for eligible research and development purposes based on the filing of an annual application. The
Australian government may in the future decide to modify the requirements of, reduce the amounts of the research and
development tax incentive credits available under, or discontinue its research and development tax incentive program. For
instance, the Australian government undertook a review of its Research and Development Tax Incentive program in the
May 2020 Federal budget and in October 2020 introduced new legislation for the tax offset applicable to eligible
companies for income tax years commencing from July 1, 2021. One of the legislation changes made was to allow a tax
offset for companies with an aggregated turnover of A$20.0 million or more. For companies with an aggregated turnover
of A$20.0 million or more, the rate of tax offset is the company’s corporate tax rate plus a rate between 8.5% and 16.5%
depending on the proportion of research and development expenditures in relation to total expenditures. For companies
with an aggregated turnover below A$20.0 million, the rate of the refundable research and development tax offset was set
as at 18.5% above the company’s tax rate. If the Research and Development Tax program incentives are revoked or
modified, or if we are no longer eligible for such incentives due to other circumstances, our business, results of operations
and financial condition may be adversely affected.
We assess, on an annual basis, the quantum of previous research and development tax claims and on-going
eligibility to claim this tax incentive in Australia. For the years ended June 30, 2024 and 2023, we recognized $0.9 million
and $3.5 million in research and development tax incentive income, respectively. During the year ended June 30, 2023,
management concluded its assessment of qualifying activities and recognized the relevant income for the years ended June
30, 2023, 2022 and 2021. No income was recognized in the years ended June 30, 2022 and 2021 as management were yet
to confirm if our research and development activities were eligible under the incentive scheme and therefore had not
applied for a tax offset. There can be no assurances that we will benefit from these incentives in the future if our activities
are not eligible under the incentive scheme or that the tax incentive credit programs will not be revoked or modified in any
way in the future.
Taxing authorities could reallocate our taxable income within our subsidiaries, which could increase our consolidated
tax liability.
We conduct operations in multiple tax jurisdictions and the tax laws of those jurisdictions generally require that the
transfer pricing between affiliated companies in different jurisdictions be the same as those between unrelated companies
dealing at arms’ length, and that such prices are supported by contemporaneous documentation. While we believe that we
operate in compliance with applicable transfer pricing laws and intend to continue to do so, our transfer pricing procedures
are not binding on applicable tax authorities. If tax authorities in any of these countries were to successfully challenge our
transfer pricing as not reflecting arms’ length transactions, they could require us to adjust our transfer pricing and thereby
reallocate our income to reflect these revised transfer pricing, which could result in a higher tax liability to us, and possibly
interest and penalties, and could adversely affect our business, results of operations and financial condition.
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The pharmaceutical industry is highly regulated and pharmaceutical companies are subject to various federal and state
fraud and abuse laws, including, without limitation, the federal Anti-Kickback Statute and the federal False Claims Act.
Healthcare fraud and abuse regulations are complex and can be subject to varying interpretations as to whether or
not a statute has been violated. The laws that may affect our ability to operate include:
•
the federal Anti-Kickback Statute which prohibits, among other things, the knowing and willful payment of
remuneration to induce or reward patient referrals, prescribing or recommendation of products, or the
generation of business involving any item or service which may be payable by the federal health care
programs (e.g., drugs, supplies, or health care services for Medicare or Medicaid patients);
•
the federal False Claims Act which prohibits, among other things, individuals or entities from knowingly
presenting, or causing to be presented, claims for payment for government funds (e.g., payment from
Medicare or Medicaid) or knowingly making, using, or causing to be made or used a false record or
statement, material to a false or fraudulent claim for government funds;
•
the federal Health Insurance Portability and Accountability Act of 1996 (“HIPAA”), as amended by the
Health Information Technology for Economic and Clinical Health Act, and its implementing regulations,
imposes certain requirements relating to the privacy, security and transmission of individually identifiable
health information. Among other things, HIPAA imposes civil and criminal liability for the wrongful access
or disclosure of protected health information;
•
the federal Physician Payments Sunshine Act, created under Section 6002 of the Patient Protection and
Affordable Care Act (“ACA”), as amended, requires certain manufacturers of drugs, devices, biologics and
medical supplies for which payment is available under Medicare, Medicaid or the Children’s Health
Insurance Program (with certain exceptions) to report information related to certain payments or other
transfers of value made or distributed to physicians and teaching hospitals, or to entities or individuals at the
request of, or designated on behalf of, those physicians and teaching hospitals and to report annually certain
ownership and investment interests held by physicians and their immediate family members;
•
the FDCA, which, among other things, regulates the testing, development, approval, manufacture, promotion
and distribution of drugs, devices and biologics. The FDCA prohibits manufacturers from selling or
distributing “adulterated” or “misbranded” products. A drug product may be deemed misbranded if, among
other things, (i) the product labeling is false or misleading, fails to contain requisite information or does not
bear adequate directions for use; (ii) the product is manufactured at an unregistered facility; or (iii) the
product lacks the requisite FDA clearance or approval;
•
the U.S. Foreign Corrupt Practices Act (“FCPA”), which prohibits corrupt payments, gifts or transfers of
value to non-U.S. officials; and
•
non-U.S. and U.S. state law equivalents of each of the above federal laws, such as anti-kickback and false
claims laws which may apply to items or services reimbursed by any third-party payor, including commercial
insurers.
Any failure to comply with these laws, or the regulations adopted thereunder, could result in administrative, civil,
and/or criminal penalties, and could result in a material adverse effect on our reputation, business, results of operations and
financial condition.
The federal fraud and abuse laws have been interpreted to apply to arrangements between pharmaceutical
manufacturers and a variety of health care professionals and healthcare organizations. Although the federal Anti-Kickback
Statute has several statutory exemptions and regulatory safe harbors protecting certain common activities from prosecution,
all elements of the potentially applicable exemption or safe harbor must be met in order for the arrangement to be
protected, and prosecutors have interpreted the federal healthcare fraud statutes to attack a wide range of conduct by
pharmaceutical companies. In addition, most states have statutes or regulations similar to the federal anti-kickback and
federal false claims laws, which apply to items and services covered by Medicaid and other state programs, or, in several
states, apply regardless of the payor. Administrative, civil and criminal sanctions may be imposed under these federal and
state laws.
Further, the ACA, among other things, amended the intent standard under the Anti-Kickback Statute such that a
person or entity no longer needs to have actual knowledge of the statute or specific intent to violate it in order to have
committed a violation. In addition, the ACA makes clear that a claim including items or services resulting from a violation
of the federal Anti-Kickback Statute constitutes a false or fraudulent claim under the federal False Claims Act. Any
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violations of these laws, or any action against us for violation of these laws, even if we successfully defend against it, could
result in a material adverse effect on our reputation, business, results of operations and financial condition.
A failure to adequately protect private health information could result in severe harm to our reputation and subject us to
significant liabilities, each of which could have a material adverse effect on our business.
Throughout the clinical trial process, we may obtain the private health information of our trial subjects. There are a
number of state, federal and international laws protecting the privacy and security of health information and personal data.
As part of the American Recovery and Reinvestment Act 2009 (“ARRA”), Congress amended the privacy and security
provisions of HIPAA. HIPAA imposes limitations on the use and disclosure of an individual’s healthcare information by
healthcare providers conducting certain electronic transactions, healthcare clearinghouses, and health insurance plans,
collectively referred to as covered entities. The HIPAA amendments also impose compliance obligations and
corresponding penalties for non-compliance on certain individuals and entities that provide services to or perform certain
functions on behalf of healthcare providers and other covered entities involving the use or disclosure of individually
identifiable health information, collectively referred to as business associates. ARRA also made significant increases in the
penalties for improper use or disclosure of an individual’s health information under HIPAA and extended enforcement
authority to state attorneys general. The amendments also create notification requirements to federal regulators, and in
some cases local and national media, for individuals whose health information has been inappropriately accessed or
disclosed. Notification is not required under HIPAA if the health information that is improperly used or disclosed is
deemed secured in accordance with certain encryption or other standards developed by the U.S. Department of Health and
Human Services, or HHS. Most states have laws requiring notification of affected individuals and state regulators in the
event of a breach of personal information, which is a broader class of information than the health information protected by
HIPAA. Many state laws impose significant data security requirements, such as encryption or mandatory contractual terms
to ensure ongoing protection of personal information. Activities outside of the U.S. implicate local and national data
protection standards, impose additional compliance requirements and generate additional risks of enforcement for non-
compliance. The EU’s General Data Protection Regulation, Canada’s Personal Information Protection and Electronic
Documents Act and other data protection, privacy and similar national, state/provincial and local laws and regulations may
also restrict the access, use and disclosure of patient health information abroad. We may be required to expend significant
capital and other resources to ensure ongoing compliance with applicable privacy and data security laws, to protect against
security breaches and hackers or to alleviate problems caused by such breaches, and the failure to so comply may lead to
fines or penalties.
Our operations are subject to anti-corruption laws, including Australian bribery laws, the United Kingdom Bribery Act,
and the FCPA and other anti-corruption laws that apply in countries where we do business.
Anti-corruption laws generally prohibit us and our employees and intermediaries from bribing, being bribed or
making other prohibited payments to government officials or other persons to obtain or retain business or gain some other
business advantage. Although we believe that we have adequate policies and enforcement mechanisms to ensure legal and
regulatory compliance with the FCPA, the U.K. Bribery Act 2010 and other similar regulations, we participate in
collaborations and relationships with third parties, and it is possible that any of our employees, subcontractors, agents or
partners may violate any such legal and regulatory requirements, which may expose us to criminal or civil enforcement
actions, including penalties and suspension or disqualification from U.S. federal procurement contracting. In addition, we
cannot predict the nature, scope or effect of future regulatory requirements to which our international operations might be
subject or the manner in which existing laws might be administered or interpreted.
There is no assurance that we will be completely effective in ensuring our compliance with all applicable anti-
corruption laws or other laws including trade related laws. If we are not in compliance with these laws, we may be subject
to criminal and civil penalties, disgorgement and other sanctions and remedial measures, and legal expenses, which could
have an adverse impact on our business, financial condition, results of operations and liquidity. Likewise, any investigation
of any potential violations of these laws by respective government bodies could also have an adverse impact on our
reputation, our business, results of operations and financial condition.
We may lose our foreign private issuer status, which would then require us to comply with the Exchange Act’s domestic
reporting regime and cause us to incur additional legal, accounting and other expenses.
In order to maintain our current status as a foreign private issuer, either (1) a majority of our ordinary shares must be
either directly or indirectly owned of record by non-residents of the United States or (2) (a) a majority of our executive
officers or directors must not be U.S. citizens or residents, (b) more than 50 percent of our assets cannot be located in the
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U.S. and (c) our business must be administered principally outside the U.S. If we lost this status, we would be required to
comply with the Exchange Act reporting and other requirements applicable to U.S. domestic issuers, which are more
detailed and extensive than the requirements for foreign private issuers. We may also be required to make changes in our
corporate governance practices in accordance with various SEC rules and Nasdaq listing standards. Further, we would be
required to comply with U.S. GAAP, as opposed to IFRS, in the preparation and issuance of our financial statements for
historical and current periods. The regulatory and compliance costs to us under U.S. securities laws if we are required to
comply with the reporting requirements applicable to a U.S. domestic issuer may be higher than the cost we would incur as
a foreign private issuer. As a result, we expect that a loss of foreign private issuer status would increase our legal and
financial compliance costs.
If we fail to maintain proper internal controls, our ability to produce accurate financial statements or comply with
applicable regulations could be impaired.
Section 404(a) of the Sarbanes-Oxley Act of 2002 (the “Sarbanes-Oxley Act”) requires that our management assess
and report annually on the effectiveness of our internal controls over financial reporting and identify any material
weaknesses in our internal controls over financial reporting. In order to maintain and improve the effectiveness of our
disclosure controls and procedures and internal control over financial reporting, we have expended, and anticipate that we
will continue to expend, significant resources, including accounting-related costs and significant management oversight.
If either we are unable to conclude that we have effective internal controls over financial reporting or our
independent auditors are unwilling or unable to provide us with an unqualified report on the effectiveness of our internal
controls over financial reporting as required by Section 404(b) of the Sarbanes-Oxley Act, investors may lose confidence in
our operating results, the price of the ADSs could decline and we may be subject to litigation or regulatory enforcement
actions. In addition, if we are unable to meet the requirements of Section 404 of the Sarbanes-Oxley Act, we may not be
able to remain listed on Nasdaq Global Select Market (“Nasdaq”).
We have incurred and will continue to incur significant increased costs as a result of operating as a company whose
ADSs are publicly traded in the United States, and our management will continue to be required to devote substantial
time to compliance initiatives.
As a company whose ADSs are publicly traded in the United States, we have incurred and will continue to incur
significant legal, accounting, insurance and other expenses. The Sarbanes-Oxley Act, Dodd-Frank Wall Street Reform and
Consumer Protection Act and related rules implemented by the SEC and Nasdaq, have imposed various requirements on
public companies including requiring establishment and maintenance of effective disclosure and financial controls. Our
management and other personnel will need to continue to devote a substantial amount of time to these compliance
initiatives, and we will need to add additional personnel and build our internal compliance infrastructure. Moreover, these
rules and regulations have increased and will continue to increase our legal and financial compliance costs and will make
some activities more time-consuming and costly. These laws and regulations could also make it more difficult and
expensive for us to attract and retain qualified persons to serve on our board of directors, our board committees or as our
senior management. Furthermore, if we are unable to satisfy our obligations as a public company, we could be subject to
delisting of the ADSs, fines, sanctions and other regulatory action and potentially regulatory investigations and
enforcement and/or civil litigation.
We have never declared or paid dividends on our ordinary shares, and we do not anticipate paying dividends in the
foreseeable future. Therefore, you must rely on price-appreciation of our ordinary shares or ADSs for a return on your
investment.
We have never declared or paid cash dividends on our ordinary shares. For the foreseeable future, we currently
intend to retain all available funds and any future earnings to support our operations and to finance the growth and
development of our business. Any future determination to declare cash dividends will be made at the discretion of our
board of directors, subject to compliance with applicable laws and covenants under the loan facilities with Oaktree and
NovaQuest or other current or future credit facilities, which may restrict or limit our ability to pay dividends, and will
depend on our financial condition, operating results, capital requirements, general business conditions and other factors that
our board of directors may deem relevant. We do not anticipate paying any cash dividends on our ordinary shares in the
foreseeable future. As a result, a return on your investment in our ordinary shares or ADSs will likely only occur if our
ordinary share or ADS price appreciates. There is no guarantee that our ordinary shares or ADSs will appreciate in value in
the future.
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Australian takeover laws may discourage takeover offers being made for us or may discourage the acquisition of a
significant position in our ordinary shares or ADSs.
We are incorporated in Australia and are subject to the takeover laws of Australia. Among other things, we are
subject to the Australian Corporations Act 2001 (the “Corporations Act”). Subject to a range of exceptions, the
Corporations Act prohibits the acquisition of a direct or indirect interest in our issued voting shares if the acquisition of that
interest will lead to a person’s voting power in us increasing to more than 20%, or increasing from a starting point that is
above 20% and below 90%. Australian takeover laws may discourage takeover offers being made for us or may discourage
the acquisition of a significant position in our ordinary shares. This may have the ancillary effect of entrenching our board
of directors and may deprive or limit our shareholders’ opportunity to sell their ordinary shares or ADSs and may further
restrict the ability of our shareholders to obtain a premium from such transactions.
Significant disruptions of information technology systems, data security breaches or unauthorized disclosure of
sensitive data could adversely affect our business by exposing us to liability and affect our business and reputation.
The Company is increasingly dependent on critical, complex, and interdependent information technology systems
(IT systems), including cloud-based software and external servers, some of which are managed or hosted by third parties,
to support business processes as well as internal and external communications. The information and data processed and
stored in our IT systems, and those of our research collaborators, CROs, contract manufacturers, suppliers, distributors, or
other third parties for which we depend to operate our business, may be vulnerable to cybersecurity breaches from
unauthorized activity by our employees, contractors or malware, hacking, business email compromise, phishing or other
cyberattacks directed by other parties. Such breaches can result in loss, damage, denial-of-service, unauthorized access or
misappropriation and may pose a risk that sensitive data, including our intellectual property, trade secrets or personal
information of our employees, patients, customers or other business partners may be exposed to unauthorized persons or to
the public. In addition, our increased reliance on personnel working from home may negatively impact productivity, or
disrupt, delay, or otherwise adversely impact our business. The increase in working remotely could increase our
cybersecurity risk, create data accessibility concerns, and make us more susceptible to communication disruptions, any of
which could adversely impact our business operations or delay necessary interactions with local and federal regulators,
manufacturing sites, clinical trial sites, and other third parties.
The rapidly moving nature of technology and the increasing sophistication of cybersecurity threats, may mean our
measures to prevent, respond to and minimize such risks may be ineffective. If a material incident or interruption were to
occur, it could result in a disruption of our development programs and future commercial operations, including due to a
loss, corruption or unauthorized disclosure of our proprietary or sensitive information. Additionally, the costs to the
company to investigate and mitigate cybersecurity incidents could be significant. Any disruption, security breach, or action
by the company, its employees, or contractors that might be inconsistent with the rapidly evolving data privacy and security
laws and regulations applicable within Australia and the United States and elsewhere where we conduct business, could
result in; enforcement actions by both countries state and federal governments or foreign governments, liability or
sanctions under data privacy laws including healthcare laws such as the Privacy Act or HIPAA that protect certain types of
sensitive information, regulatory penalties, other legal proceedings such as but not limited to private litigation, the
incurrence of significant remediation costs, disruptions to our development programs, business operations and
collaborations, diversion of management efforts and damage to our reputation which could harm our business and
operations.
Risks Related to Our Trading Markets
The market price and trading volume of our ordinary shares and ADSs may be volatile and may be affected by
economic conditions beyond our control. Such volatility may lead to securities litigation.
The market price of our ordinary shares and ADSs may be highly volatile and subject to wide fluctuations. In
addition, the trading volume of our ordinary shares and ADSs may fluctuate and cause significant price variations to occur.
We cannot assure you that the market price of our ordinary shares and ADSs will not fluctuate or significantly decline in
the future.
Some specific factors that could negatively affect the price of our ordinary shares and ADSs or result in fluctuations
in their price and trading volume include:
•
results of clinical trials of our product candidates;
•
results of clinical trials of our competitors’ products;
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•
regulatory actions with respect to our products or our competitors’ products;
•
actual or anticipated fluctuations in our quarterly operating results or those of our competitors;
•
publication of research reports by securities analysts about us or our competitors in the industry;
•
our failure or the failure of our competitors to meet analysts’ projections or guidance that we or our
competitors may give to the market;
•
fluctuations of exchange rates between the U.S. dollar and the Australian dollar;
•
additions to or departures of our key management personnel;
•
issuances by us of debt or equity securities;
•
litigation or investigations involving our company, including: shareholder litigation; investigations or audits
by regulators into the operations of our company; or proceedings initiated by our competitors or clients;
•
strategic decisions by us or our competitors, such as acquisitions, divestitures, spin-offs, joint ventures,
strategic investments or changes in business strategy;
•
the passage of legislation or other regulatory developments affecting us or our industry;
•
fluctuations in the valuation of companies perceived by investors to be comparable to us;
•
changes in trading volume of ADSs on the Nasdaq and of our ordinary shares on the ASX;
•
sales or perceived potential sales of the ADSs or ordinary shares by us, our directors, senior management or
our shareholders in the future;
•
short selling or other market manipulation activities;
•
announcement or expectation of additional financing efforts;
•
terrorist acts, acts of war or periods of widespread civil unrest (such as Russia’s invasion of Ukraine);
•
natural disasters, the impact of climate change and other calamities;
•
changes in market conditions for biopharmaceutical companies; and
•
conditions in the U.S. or Australian financial markets or changes in general economic conditions.
In the past, following periods of volatility in the market price of a company’s securities, shareholders often instituted
securities class action litigation against that company. If we were involved in a class action suit, it could divert the attention
of senior management, require significant expenditure for defense costs, and, if adversely determined, could have a
material adverse effect on our results of operations and financial condition.
A class action proceeding in the Federal Court of Australia was served on the Company in May 2022 by the law
firm William Roberts Lawyers on behalf of persons who, between February 22, 2018, and December 17, 2020, acquired an
interest in Mesoblast shares, American Depository Receipts, and/or related equity swap arrangements. In June 2022, the
firm Phi Finney McDonald commenced a second shareholder class action against the Company in the Federal Court of
Australia asserting similar claims arising during the same period. The Australian class actions relate to the Complete
Response Letter released by the FDA in relation to our GvHD product candidate; they also relate to certain representations
made by the Company in relation to our COVID-19 product candidate and the decline in the market price of our ordinary
shares in December 2020. The Australian class actions have been consolidated into one lawsuit. On August 21, 2024, the
Company announced that the class action had been resolved subject to Federal Court approval. The settlement (inclusive of
interest and costs) will be funded entirely by Mesoblast's insurers and includes no admission of liability. The settlement
will have no impact on Mesoblast's cashflow or financial results.
The dual listing of our ordinary shares and the ADSs may adversely affect the liquidity and value of these securities.
Our ADSs are listed on the Nasdaq and our ordinary shares are listed on the ASX. We cannot predict the effect of
this dual listing on the value of our ordinary shares and ADSs. However, the dual listing of our ordinary shares and ADSs
may dilute the liquidity of these securities in one or both markets and may adversely affect the development of an active
trading market for the ADSs in the United States. The price of the ADSs could also be adversely affected by trading in our
ordinary shares on the ASX, and vice versa.
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If securities or industry analysts do not publish research reports about our business, or if they issue an adverse opinion
about our business, the market price and trading volume of our ordinary shares and/or ADSs could decline.
The trading market for our ordinary shares and ADSs could be influenced by the research and reports that securities
or industry analysts publish about us or our business. Securities and industry analysts may discontinue research on our
company, to the extent such coverage currently exists, or in other cases, may never publish research on our company. If too
few securities or industry analysts commence coverage of our company, the trading price for our ordinary shares and ADSs
would likely be negatively impacted. If one or more of the analysts who cover us downgrade our ordinary shares or ADSs
or publish inaccurate or unfavorable research about our business, the market price of our ADSs would likely decline. If one
or more of these analysts cease coverage of our company or fail to publish reports on us regularly, demand for our ordinary
shares and/or ADSs could decrease, which might cause our price and trading volume to decline.
Risks Related to Ownership of Our ADSs
An active trading market for the ADSs may not develop in the United States.
Our ADSs are listed in the United States on the Nasdaq under the symbol “MESO.” However, we cannot assure you
that an active public market in the United States for the ADSs will develop on that exchange, or if developed, that this
market will be sustained.
We currently report our financial results under IFRS, which differs in certain significant respect from U.S. GAAP.
Currently we report our financial statements under IFRS. There have been and there may in the future be certain
significant differences between IFRS and U.S. GAAP, including differences related to revenue recognition, intangible
assets, share-based compensation expense, income tax and earnings per share. As a result, our financial information and
reported earnings for historical or future periods could be significantly different if they were prepared in accordance with
U.S. GAAP. In addition, we do not intend to provide a reconciliation between IFRS and U.S. GAAP unless it is required
under applicable law. As a result, you may not be able to meaningfully compare our financial statements under IFRS with
those companies that prepare financial statements under U.S. GAAP.
As a foreign private issuer, we are permitted and expect to follow certain home country corporate governance practices
in lieu of certain Nasdaq requirements applicable to domestic issuers and we are permitted to file less information with
the Securities and Exchange Commission than a company that is not a foreign private issuer. This may afford less
protection to holders of our ADSs.
As a “foreign private issuer”, as defined in Rule 405 under the Securities Exchange Act of 1933, as amended (the
“Securities Act”), whose ADSs will be listed on the Nasdaq, we will be permitted to, and plan to, follow certain home
country corporate governance practices in lieu of certain Nasdaq requirements. For example, we may follow home country
practice with regard to certain corporate governance requirements, such as the composition of the board of directors and
quorum requirements applicable to shareholders’ meetings. This difference may result in a board that is more difficult to
remove and less shareholder approvals required generally. In addition, we may follow home country practice instead of the
Nasdaq Global Select Market requirement to hold executive sessions and to obtain shareholder approval prior to the
issuance of securities in connection with certain acquisitions or private placements of securities. The above differences may
result in less shareholder oversight and requisite approvals for certain acquisition or financing related decisions. Further,
we may follow home country practice instead of the Nasdaq Global Select Market requirement to obtain shareholder
approval prior to the establishment or amendment of certain share option, purchase or other compensation plans. This
difference may result in less shareholder oversight and requisite approvals for certain company compensation related
decisions. A foreign private issuer must disclose in its annual reports filed with the Securities and Exchange Commission,
or SEC, and the Nasdaq Global Select Market, the requirements with which it does not comply followed by a description of
its applicable home country practice. The Australian home country practices described above may afford less protection to
holders of the ADSs than that provided under the Nasdaq Global Select Market rules.
Further, as a foreign private issuer, we are exempt from certain rules under the “Exchange Act”, that impose
disclosure requirements as well as procedural requirements for proxy solicitations under Section 14 of the Exchange Act.
In addition, our officers, directors and principal shareholders are exempt from the reporting and “short-swing” profit
recovery provisions of Section 16 of the Exchange Act. Moreover, we are not required to file periodic reports and financial
statements with the SEC as frequently or as promptly as a company that files as a domestic issuer whose securities are
registered under the Exchange Act, nor are we generally required to comply with the SEC’s Regulation FD, which restricts
the selective disclosure of material non-public information. Accordingly, the information may not be disseminated in as
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timely a manner, or there may be less information publicly available concerning us generally than there is for a company
that files as a domestic issuer.
ADS holders may be subject to additional risks related to holding ADSs rather than ordinary shares.
ADS holders do not hold ordinary shares directly and, as such, are subject to, among others, the following additional
risks.
•
As an ADS holder (and not the holder of ordinary shares underlying your ADSs), we will not treat you as one
of our shareholders and you will not be able to exercise shareholder rights, except through the American
depositary receipt, or ADR, depositary as permitted by the deposit agreement.
•
Distributions on the ordinary shares represented by your ADSs will be paid to the ADR depositary, and
before the ADR depositary makes a distribution to you on behalf of your ADSs, any withholding taxes that
must be paid will be deducted. Additionally, if the exchange rate fluctuates during a time when the ADR
depositary cannot convert the foreign currency, you may lose some or all of the value of the distribution.
•
We and the ADR depositary may amend or terminate the deposit agreement without the ADS holders’
consent in a manner that could prejudice ADS holders.
ADS holders must act through the ADR depositary to exercise your voting rights and, as a result, you may be unable
to exercise your voting rights on a timely basis.
As a holder of ADSs (and not the ordinary shares underlying your ADSs), we will not treat you as one of our
shareholders, and you will not be able to exercise shareholder rights. The ADR depositary will be the holder of the ordinary
shares underlying your ADSs, and ADS holders will be able to exercise voting rights with respect to the ordinary shares
represented by the ADSs only in accordance with the deposit agreement relating to the ADSs. There are practical
limitations on the ability of ADS holders to exercise their voting rights due to the additional procedural steps involved in
communicating with these holders. For example, holders of our ordinary shares will receive notice of shareholders’
meetings by mail or email and will be able to exercise their voting rights by either attending the shareholders meeting in
person or voting by proxy. ADS holders, by comparison, will not receive notice directly from us. Instead, in accordance
with the deposit agreement, we will provide notice to the ADR depositary of any such shareholders meeting and details
concerning the matters to be voted upon. As soon as practicable after receiving notice from us of any such meeting, the
ADR depositary will mail to holders of ADSs the notice of the meeting and a statement as to the manner in which voting
instructions may be given by ADS holders. To exercise their voting rights, ADS holders must then instruct the ADR
depositary as to voting the ordinary shares represented by their ADSs. Due to these procedural steps involving the ADR
depositary, the process for exercising voting rights may take longer for ADS holders than for holders of ordinary shares.
The ordinary shares represented by ADSs for which the ADR depositary fails to receive timely voting instructions will not
be voted. Under Australian law and our Constitution, any resolution to be considered at a meeting of the shareholders shall
be decided on a show of hands unless a poll is demanded by the shareholders at or before the declaration of the result of the
show of hands. Under voting by a show of hands, multiple “yes” votes by ADS holders will only count as one “yes” vote
and will be negated by a single “no” vote, unless a poll is demanded.
If we are or become classified as a passive foreign investment company, our U.S. securityholders may suffer adverse tax
consequences.
Based upon an analysis of our income and assets for the taxable year ended June 30, 2024, we do not believe we
were a passive foreign investment company (a "PFIC") for our most recent tax year. In general, if at least 75% of our gross
income for any taxable year consists of passive income or at least 50% of the average quarterly value of assets is
attributable to assets that produce passive income or are held for the production of passive income, including cash, then we
will be classified as a PFIC for U.S. federal income tax purposes. Passive income for this purpose generally includes
dividends, interest, certain royalties and rents, and gains from commodities and securities transactions. Passive assets for
this purpose generally includes assets held for the production of passive income. Accordingly, passive assets generally
include any cash, cash equivalents and cash invested in short-term, interest bearing, debt instruments or bank deposits that
are readily convertible into cash. Since PFIC status depends upon the composition of our income and assets and the market
value of our assets from time to time, and since the determination of PFIC status must be made annually at the end of each
taxable year, there can be no assurance that we will not be considered a PFIC for any future taxable year. Investors should
be aware that our gross income for purposes of the PFIC income test depends on the receipt of active revenue, and there
can be no assurances that such active revenue will continue, or that we will receive other gross income that is not
considered passive for purposes of the PFIC income test. If we were a PFIC for any taxable year during a U.S. investor’s
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holding period for the ordinary shares or ADSs, we would ordinarily continue to be treated as a PFIC for each subsequent
year during which the U.S. investor owned the ordinary shares or ADSs. If we were treated as a PFIC, U.S. investors would
be subject to special punitive tax rules with respect to any "excess distribution" received from us and any gain realized
from a sale or other disposition (including a pledge) of the ordinary shares or ADSs unless a U.S. investor made a timely
"qualified electing fund" or "mark-to-market" election. For a more detailed discussion of the U.S. tax consequences to U.S.
investors if we were classified as a PFIC, see Item 10.E - "Taxation — Certain Material U.S. Federal Income Tax
Considerations to U.S. Holders — Passive Foreign Investment Company".
Changes in foreign currency exchange rates could impact amounts you receive as a result of any dividend or
distribution we declare on our ordinary shares.
Any significant change in the value of the Australian dollar may impact amounts you receive in U.S. dollars as a
result of any dividend or distribution we declare on our ordinary shares as a holder of our ADSs. More specifically, any
dividends that we pay on our ordinary shares will be in Australian dollars. The depositary for the ADSs has agreed to pay
to you the cash dividends or other distributions it or the custodian receives on our ordinary shares or other deposited
securities after deducting its fees and expenses, including any such fees or expenses incurred to convert any such
Australian dollars into U.S. dollars. You will receive these distributions in U.S. dollars in proportion to the number of our
ordinary shares your ADSs represent. Depreciation of the U.S. dollar against the Australian dollar would have a negative
effect on any such distribution payable to you.
You may not receive distributions on our ordinary shares represented by the ADSs or any value for such distribution if
it is illegal or impractical to make them available to holders of ADSs.
While we do not anticipate paying any dividends on our ordinary shares in the foreseeable future, if such a dividend
is declared, the depositary for the ADSs has agreed to pay to you the cash dividends or other distributions it or the
custodian receives on our ordinary shares or other deposited securities after deducting its fees and expenses. You will
receive these distributions in proportion to the number of our ordinary shares your ADSs represent. However, in
accordance with the limitations set forth in the deposit agreement, it may be unlawful or impractical to make a distribution
available to holders of ADSs. We have no obligation to take any other action to permit the distribution of the ADSs,
ordinary shares, rights or anything else to holders of the ADSs. This means that you may not receive the distributions we
make on our ordinary shares or any value from them if it is unlawful or impractical to make them available to you. These
restrictions may have a material adverse effect on the value of your ADSs.
You may be subject to limitations on transfers of your ADSs.
ADSs are transferable on the books of the depositary. However, the depositary may close its transfer books at any
time or from time to time when it deems expedient in connection with the performance of its duties. In addition, the
depositary may refuse to deliver, transfer or register transfers of ADSs generally when our books or the books of the
depositary are closed, or at any time if we or the depositary deems it advisable to do so because of any requirement of law
or of any government or governmental body, or under any provision of the deposit agreement, or for any other reason.
U.S. investors may have difficulty enforcing civil liabilities against our company, our directors or members of our senior
management.
Several of our officers and directors are non-residents of the United States, and a substantial portion of the assets of
such persons are located outside the U.S. As a result, it may be impossible to serve process on such persons in the United
States or to enforce judgments obtained in U.S. courts against them based on civil liability provisions of the securities laws
of the U.S. Even if you are successful in bringing such an action, there is doubt as to whether Australian courts would
enforce certain civil liabilities under U.S. securities laws in original actions or judgments of U.S. courts based upon these
civil liability provisions. In addition, awards of punitive damages in actions brought in the U.S. or elsewhere may be
unenforceable in Australia or elsewhere outside the U.S. An award for monetary damages under the U.S. securities laws
would be considered punitive if it does not seek to compensate the claimant for loss or damage suffered and is intended to
punish the defendant. The enforceability of any judgment in Australia will depend on the particular facts of the case as well
as the laws and treaties in effect at the time. The U.S. and Australia do not currently have a treaty or statute providing for
recognition and enforcement of the judgments of the other country (other than arbitration awards) in civil and commercial
matters. As a result, our public shareholders and holders of the ADSs may have more difficulty in protecting their interests
through actions against us, our management, our directors than would shareholders of a corporation incorporated in a
jurisdiction in the United States.
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Item 4. Information on the Company
4.A
History and Development of Mesoblast
Mesoblast Limited
Mesoblast Limited was incorporated on June 8, 2004 as a public company in Australia under the Corporations Act
2001 with an indefinite duration. On December 16, 2004 we became listed on the Australian Securities Exchange (the
“ASX”). On November 13, 2015, we became listed on the Nasdaq Global Select Market (“Nasdaq”) and from this date we
have been dual-listed in Australia and the United States. Our registered office is located at the following address:
Mesoblast Ltd
Level 38
55 Collins Street
Melbourne VIC 3000
Australia
Telephone: +61 3 9639 6036
Web: www.mesoblast.com
Our agent for service of process in the United States is Mesoblast Inc., 505 Fifth Avenue, Level 3, New York, NY
10017. All information we file with the SEC is available through the SEC's Electronic Data Gathering, Analysis and
Retrieval system, which may be accessed through the SEC's website at www.sec.gov.
For a list of our significant subsidiaries, see Exhibit 8.1 to this Annual Report.
Important Corporate Developments
Fiscal year 2024 to date of annual report
August 2024
Announced that the consolidated shareholder class action, filed in the Federal Court of Australia
in 2022, has been resolved subject to Federal Court approval. The settlement (inclusive of
interests and costs) will be funded entirely by Mesoblast's insurers and includes no admission of
liability.
July 2024
Announced the United States Food and Drug Administration ("FDA") has accepted our
Biologics License Application ("BLA") resubmission for Ryoncil® (remestemcel-L) in the
treatment of children with steroid-refractory acute graft versus host disease ("SR-aGVHD").
FDA considered the resubmission to be a complete response and set a Prescription Drug User
Fee Act ("PDUFA") goal date of January 7, 2025.
The confirmatory Phase 3 trial of rexlemestrocel-L in patients with chronic low back pain
("CLBP") due to inflammatory degenerative disc disease of less than five years duration has
commenced enrollment at multiple sites across the United States.
Mesoblast resubmitted its BLA for approval of RYONCIL in the treatment of children with SR-
aGVHD.
April 2024
Jane Bell AM appointed to the role of non-executive Chair of Mesoblast's Board of Directors.
March 2024
Announced that FDA has informed the company that following additional consideration the
available clinical data from its Phase 3 study MSB-GVHD001 appears sufficient to support
submission of the proposed BLA for remestemcel-L for treatment of pediatric patients with SR-
aGVHD.
Announced that US FDA supports an accelerated approval pathway for rexlemestrocel-L in
patients with end-stage ischemic heart failure with reduced ejection fraction ("HFrEF") and a left
ventricular assist device ("LVAD"). FDA provided this feedback in formal minutes to the
company following the Type B meeting held with FDA on February 21, 2024 for rexlemestrocel-
L (Revascor®) under the existing Regenerative Medicine Advanced Therapy ("RMAT")
designation.
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February 2024
Announced that the FDA granted Mesoblast’s allogeneic cell therapy Revascor® (rexlemestrocel-
L) an Orphan Drug Designation (“ODD”) following submission of results from the randomized
controlled trial in children with hypoplastic left heart syndrome (“HLHS”), a potentially life
threatening congenital heart condition.
January 2024
Announced that the FDA granted Mesoblast’s cell therapy Revascor® (rexlemestrocel-L) a Rare
Pediatric Disease ("RPD") designation following submission of results from the randomized
controlled trial in children with HLHS.
December 2023
Completed a private placement to institutional and sophisticated investors and 1 for 4 pro-rata
accelerated non-renounceable entitlement offer to shareholders in Australia and certain other
countries that raised A$60.3 million at an issue price of A$0.30 per ordinary share.
November 2023
Announced filing for RPD designation with the FDA for REVASCOR in the treatment of the
congenital heart disease HLHS. The filings were based on results from a blinded, randomized,
controlled prospective trial of REVASCOR conducted at a single center in the US in 19 children
with HLHS and accepted for publication in peer reviewed The Journal of Thoracic and
Cardiovascular Surgery Open (JTCVS Open).
Announced that the Blood and Marrow Transplant Clinical Trials Network (BMT CTN), a body
including centers responsible for approximately 80% of all US allogeneic BMTs, has entered
into an agreement to develop a pivotal trial of Mesoblast’s lead product candidate Ryoncil®
(remestemcel-L) in the treatment of adults with SR-aGvHD.
September 2023
Announced the appointment of independent director Ms. Jane Bell as Chair of the Mesoblast
Board Audit and Risk Committee.
August 2023
The FDA provided a complete response to the BLA resubmission for remestemcel-L for the
treatment of pediatric SR-aGVHD and requires more data to support marketing approval,
including potency assay or clinical data. Mesoblast intends to conduct a targeted, controlled
study in the highest-risk adults with the greatest mortality. This adult study is in line with our
overall commercial strategy, which envisioned a sequenced progression from pediatric to adult
SR-aGVHD indications. As part of its review FDA completed the Pre-License Inspection ("PLI")
of the manufacturing facility, did not issue any Form 483, and found no objectionable conditions.
In addition, FDA acknowledged in the resubmission review that changes implemented appear to
improve assay performance relative to the original version of the assay used in the pediatric
Phase 3 trial.
Environmental, Social and Governance (“ESG”) Statement
Introduction: Our Approach to Sustainability
We consider the greatest contribution Mesoblast makes to sustainability is its purpose in seeking to provide access
to treatment for patients suffering a range of hitherto unmet medical needs including cardiac diseases, immune-mediated
and inflammatory conditions, oncology and haematology diseases, and spine orthopaedic disorders, subject to regulatory
approval. This has not only a potentially high social and financial value, but in terms of adding value in the way it operates,
the Company prizes and develops its people as key assets, while its environmental footprint is light. Together with a strong
ethical and governance framework, this puts the Company on a sound footing for delivering on its purpose in the medium
to long term.
Our commitment to sustainability is instilled through Mesoblast’s five key corporate values which articulate who we
are and what we stand for. Mesoblast values reflect our commitment to our customers, our colleagues, and the patients we
serve. Integrity is at our core, while accountability to our commitments, collective teamwork, a pursuit of excellence, and
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outside the-box thinking and innovation surround our every business decision. Mesoblast personnel are expected to
practice these values each and every day.
Integrity - We act with integrity in all of our dealings, with the
best interest of patients, care givers and our people as our guide.
What we do we do with conviction.
Accountability - We hold ourselves and each other responsible
and ensure that our words and actions support Mesoblast’s vision
and values
Teamwork - We believe in what we can achieve collectively and
have an appreciation of our shared and unique ability to collaborate
with our people and our partners, while focused on our patients and
their families.
Excellence - We engage in continual learning so that we, as
individuals and as an organization, can reach our highest potential.
Innovation - We are focused on the bold pursuit of developing and
delivering novel treatments to improve patient outcomes through
cutting edge science.
Acknowledging that sustainability is an overarching concept that can be applied to all areas of business finance, operations
and impact, for the purposes of this Statement, we specifically focus on key environmental, social and governance (“ESG”)
matters. When assessing and reporting our ESG initiatives and performance, we take into account:
•
Mesoblast’s size and stage in its growth cycle: it is a small development-stage biotechnology company
with fewer than 100 employees, limited manufacturing and currently no commercialized product. This
means that some reporting topics will be less relevant for us and our stakeholders until we grow our
product portfolio and operations; and
•
Appropriate sustainability standards: for example, the Sustainability Accounting Standards Board’s
(“SASB”) Biotechnology & Pharmaceuticals Sustainability Accounting Standard, the Global Reporting
Initiative’s (“GRI”) Universal Standards, and the Biopharma Investor ESG Communications Guidance
4.0 are relevant.
We identified the following material ESG topics based on an assessment of their impact on the business and our
understanding of their importance to stakeholders:
1.
Corporate Governance
2.
Business Ethics, Integrity, and Compliance
3.
Risk Management
4.
Human Capital Management
5.
Product Quality and Patient Safety
6.
Supply Chain Management
7.
Access to Healthcare
8.
Environmental Impacts
These are dealt with in turn below.
1.
Corporate Governance
Mesoblast is committed to implementing and achieving an effective corporate governance framework to ensure
that the Company is managed effectively, honestly and ethically. More information on our corporate governance practices
is set out in Mesoblast’s Corporate Governance Statement, available at www.mesoblast.com. The Company references and
reports against ASX Corporate Governance Council’s (Council) Corporate Governance Principles and Recommendations.
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Mesoblast’s Board of Directors (the “Board”) provides oversight of the Company’s ESG-related risks and
opportunities on a regular basis at Board meetings, and in particular focus through its two committees:
•
Nomination and Remuneration Committee (“NRC”)
•
Audit and Risk Committee (“ARC”)
The NRC assists the Board in the discharge of its responsibilities, and in particular to ensure that there is an
environment where the Board can carry out effective and responsible decision making and oversight, including on ESG
matters such as fair remuneration and health & safety. Since June 2022, all independent, Non-Executive Directors of the
Board are members of the NRC reflecting the importance the Board places on ESG.
In addition to its main financial reporting responsibilities, the ARC is tasked with overseeing the effective
operation of Mesoblast’s risk management framework, in which certain ESG matters are considered.
Management is responsible for assessing and managing ESG-related risks and opportunities within the board
approved control framework, and for reporting progress against goals and targets to the Board.
2.
Business Ethics, Integrity, and Compliance
We are committed to the highest standards of ethical conduct and transparency in the way we deal with our
patients, employees, strategic partners, and other important stakeholders. We comply with all national and local laws and
regulations applying to our Company. Zero cases of material non-compliance occurred in FY24.
Mesoblast has established a Code of Business Conduct & Ethics (“Code”) to promote honest and ethical conduct,
comprehensive disclosures of business dealings, compliance with government laws and regulations, and a positive work
environment. All Mesoblast personnel, including Directors, officers, employees, contractors, and consultants, are expected
to comply with the principles set out in the Code. The Code covers the following topics:
•
Our Values
•
Ethical business practices
•
Safe workplace and respectful workplace conduct
•
Fair competition
•
Conflicts of interest
•
Social media use
•
Confidentiality and protection of assets
•
Quality assurance
•
Price reporting
•
Financial reporting
•
Securities trading
•
Ethical research
•
Interactions with the patient community
•
Ensuring product quality and patient safety
•
Interactions with healthcare professionals
•
Ethical marketing and advertising
•
Compliance with laws and regulations
The Code also states that it is against Mesoblast policy for personnel to use illegal drugs or be under the influence
of or impaired by alcohol or drugs while on company property or performing company work.
No issues of Code non-compliance have been brought forward to the Board in FY24.
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Mesoblast has an Anti-Bribery and Anti-Corruption Policy and complies with global and regional laws preventing
corrupt business practices and bribery, including the U.S. Foreign Corrupt Practices Act and the United Kingdom Bribery
Act.
We have a Disclosure of Complaints and Concerns Policy which addresses, among other things, breaches under
the Company’s Code, Anti-Bribery and Anti-Corruption Policy, or other Company policies. Under the Disclosure of
Complaints and Concerns Policy, Mesoblast personnel are entitled to robust employment protections if they report
concerns and suspected violations covered under the policy. Personnel can report to Legal, the Audit and Risk Committee,
or other officers or senior managers, and may do so anonymously. Further, Mesoblast’s Fair Treatment Policy requires
personnel to report workplace harassment and prohibits retaliation of any kind against anyone who does so in good faith.
During FY24, Mesoblast was in compliance with the Fair Treatment Policy. The Company is satisfied that it adhered to its
policies.
In addition, Mesoblast has an ‘Ethics Hotline’ that is managed by a third-party, where our personnel and other
stakeholders may make a report anonymously, 24 hours a day, seven days a week. There have been no whistle-blower
reports to this hotline in the reporting period.
All Mesoblast personnel are required to acknowledge the Code and other key policies and are required to
participate in annual compliance training.
The Company has a process in place to inform the Board or a committee of the Board of any material breaches of
the Code, the Anti-Bribery and Anti-Corruption Policy, and material incidents reported under the Disclosure of Complaints
and Concerns Policy.
A copy of the Code and other key policies can be found at www.mesoblast.com.
3.
Risk Management
The Board is responsible for satisfying itself annually, or more frequently as required, that management has
developed and implemented an effective system of risk management and internal control. Management is responsible for
ensuring there are adequate policies in relation to risk management, compliance, and internal control systems. The ARC
monitors Mesoblast’s risk management by overseeing management’s actions in the evaluation, management, monitoring,
and reporting of material operational, financial, compliance, strategic, and certain ESG risks.
Mesoblast’s risk management group is part of the Operating Committee comprising of executive management.
This group is responsible for designing, implementing, monitoring, and reporting on Mesoblast’s management of material
business risks and the effectiveness of Mesoblast’s risk management and internal control system. ESG risks have been
incorporated into and are considered as part of Mesoblast’s risk management system. The Operating Committee regularly
reviews Mesoblast’s risks across its business and operations, and Mesoblast’s material business risks and risk management
framework are reviewed at least annually by the ARC.
As part of the process of continual improvement, we introduced a standardized tool to assess our portfolio and
corporate risk.
For cybersecurity management, see Section 16K of this Annual Report.
4.
Human Capital Management
4.1 Diversity and Inclusion
Mesoblast has a Diversity Policy which encompasses differences in ethnicity, gender, language, age, sexual
orientation, religion, socioeconomic status, physical and mental ability, thinking styles, experience, and education. We
believe that the wide array of perspectives that results from such diversity promotes innovation and business success. Being
diverse makes us more creative, flexible, and productive. Mesoblast’s policy is to engage the most appropriate and relevant
partner organizations, consultants, experts, and personnel. This includes recruiting people who are well-qualified for their
position and those who as aligned to Mesoblast’s five values and will embrace the Mesoblast culture and work ethic.
In order to meet and comply with our Diversity Policy, Mesoblast employs the following principles:
•
Mesoblast seeks and encourages diversity in current and potential employees;
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•
Mesoblast promotes equal employment opportunities based on capability, performance and potential for
growth and progression;
•
Recruitment, professional development, succession management, promotion, and remuneration decisions
are all based on performance and capability aligned to the specific job role, salary ranges, and a pre-set
criteria prior to the activities to ensure any biases are reduced;
•
Mesoblast seeks to build a safe working environment by recognizing and taking action against
inappropriate workplace behavior, including bullying, discrimination, harassment, victimization, and
vilification;
•
Mesoblast promotes flexible work practices where possible and reasonable in the circumstances, to meet
the differing needs of our employees; and
•
Mesoblast ensures appropriate policies and procedures exist that encourage diversity and meet legislative
requirements.
Line management is supported to manage diversity to ensure that employees are treated fairly and objectively. We
have clear reporting procedures for any type of discrimination or harassment, combined with follow-up procedures to
prevent future incidents.
The Board, through the NRC, is responsible for overseeing our Diversity Policy. Mesoblast’s Head of Human
Resources, with the support of the Chief Executive Officer and the executive team, is responsible for implementing the
Diversity Policy.
The Board, through the NRC, is responsible for approving and reviewing measurable objectives for achieving
gender diversity in the workplace. Mesoblast has set the following measurable objectives:
i)
Increase the number of women on the Board as vacancies arise and circumstances permit;
ii)
Increase the number of women who hold senior executive positions as vacancies arise and circumstances
permit; and
iii)
Ensure the opportunity exists for equal gender participation in all levels of professional development
programs.
All Mesoblast employees were provided access to the same development programs. A copy of Mesoblast’s
Diversity Policy can be found at www.mesoblast.com.
Table – Gender diversity statistics*
Gender
FY24 Senior Executives**
FY24 Total Workforce
FY23 Senior Executives**
FY23 Total Workforce
Male
7
35
6
39
Female
3
38
3
44
Other
—
—
—
—
% Female
30%
52%
33%
53%
*Based on number of employees as at June 30. Excludes contractors and consultants.
**A senior executive position is one held by an executive who reports directly to the Chief Executive.
Every employee, consultant and service provider has the right to work with Mesoblast in an environment that is
safe, and free from intimidation, harassment, and abuse. Mesoblast prohibits harassment for any reason, including veteran
status, uniform service member status, or any other protected class under federal, state, or local law. Inappropriate
behavior, including verbal or physical conduct by any individual that harasses another, disrupts another’s work
performance, or creates an intimidating, offensive, abusive, or hostile workplace, is not tolerated. In addition, we will not
tolerate comments, jokes, or materials, including emails, which others might consider offensive. All Mesoblast personnel
are required to complete mandatory training on an annual basis to recognize and deal with inappropriate behavior in our
workplaces, including the New York City Commission on Human Rights – Accredited Program: Confronting Sexual
Harassment; Tools & Strategies to Create a Harassment Free Workplace and Mesoblast’s Fair Treatment policy. No cases
of harassment reported in FY24, FY23 or in FY22.
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4.2 Health and Safety
Mesoblast provides a workplace that is clean and safe for all associates and one that complies with health and
safety laws. As an organization whose activities are predominantly office and laboratory based, Mesoblast chooses to track
its safety record using total recordable incident frequency rate (“TRIFR”) i.e., number of recorded injuries for each one
million hours worked. No incidents were recorded for FY24. An Environment Health and Safety Management System and
supporting policies have been developed and aligned for each jurisdiction in preparation for company wide training.
Mesoblast continued to implement hybrid/flexible working arrangements and the employee assistance program was made
available across all sites.
4.3 Recruitment, Development and Retention
Mesoblast operates at the forefront of a highly specialized industry and we recognize that our talented people are
key to developing our cell therapy technology.
Our policies and procedures follow equal employment opportunities principles for fair treatment, including
diversity and compensation. Our employees are given equal access to job opportunities and promotions based on
capability, performance and potential for growth and progression as part of our retention program.
Mesoblast’s recruitment process enables our line managers to prepare a job description that outlines
accountabilities and selection criteria that emphasize the skills, knowledge and experience. Job criteria and interview
guides are prepared for each role advertised to ensure consistency across all the interviews. Jobs are advertised through
multiple channels based on the specialization of the job role. All job roles are published on the Mesoblast intranet site
providing transparency to all employees within the company and an equal opportunity to apply. Job descriptions are
prepared in a way that enables employees to consider lateral moves based on competence rather than expertise in years of
service.
In FY24, the voluntary turnover rate was approximately 5% with 60% male and 40% females departing the
Company. Exit interviews are conducted with all departing employees and trends are monitored so that actions to minimize
the turnover can be taken. Mesoblast employed one female and one male for two approved replacement roles. While acting
and higher duty opportunities were minimal during this period, job profiles were prepared to enable existing employees to
consider lateral moves based on competence rather than years of service, where appropriately credentialed.
We provide opportunities for all colleagues to participate in professional training and education so they can
enhance their skill sets and career. During FY24, employees were given the opportunity to participate in a development
program that is linked to the annual Performance Management System.
During the reporting period, Mesoblast continued with an online performance and merit management program and
integrated an online professional development program that links the recording of participation in professional
development aligned to job role. The online performance management program enables employees to track their
performance and receive regular feedback from their manager. The formal annual review process assesses the individual
employee’s performance against objectives and quantifiable criteria that are aligned to the Mesoblast business plan,
reducing the risk of bias. All employees below the executive level participated in this program during the period.
5.
Product Quality and Safety
5.1 Scientific Research and Innovation
Over the past decade there has been a surge of interest internationally in the cutting-edge science of cellular
medicines and their use in treating a wide range of diseases.
Mesoblast is a clinical stage biotechnology company and works in close collaborative associations with leading
cell therapy research centers, as well as having our own in-house R&D laboratories and specialists. We ensure rigorous
scientific investigations are performed with well characterized cell populations in order to understand mechanisms of
action for each potential medical application. We undertake extensive pre-clinical translational studies to guide subsequent
clinical trials.
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5.2 Use of Stem Cells
Mesoblast’s novel allogeneic product candidates are based on rare (approximately 1:100,000 in bone marrow)
mesenchymal lineage cells that respond to tissue damage, secreting mediators that promote tissue repair and modulate
immune responses.
Mesenchymal lineage cells are collected from the bone marrow of healthy adult donors, and proprietary processes
are utilized to expand them to a uniform, well characterized, and highly reproducible cell population. This enables
manufacturing at industrial scale for commercial purposes. Mesoblast’s cells can be administered to patients without the
need for donor-recipient matching or recipient immune suppression.
The distinction between embryonic stem cells (“ESCs”) and non-ESCs, such as our mesenchymal lineage cells,
can be easily misunderstood by the public and has the potential to create negative public attitudes toward cell therapy. As
Mesoblast’s cells are not ESCs, we minimize the risk of being exposed to ethical, legal, or social concerns that have arisen
in relation to the collection and use of ESCs.
5.3 Use of Animal in Research
Mesoblast is committed to the welfare and humane treatment of animals and only undertakes development studies
in animal models where required by applicable regulatory bodies. These studies are undertaken by expert third-party
providers who are specialists in the management of animals and their welfare.
Mesoblast’s approach to product development is to ensure rigorous scientific investigations are performed with
well-characterized cell populations in order to understand mechanisms of action for each potential indication. Extensive
preclinical translational studies guide clinical trials that are structured to meet stringent safety and efficacy criteria set by
international regulatory agencies.
In the United States where the majority of our clinical development takes place, all of our product candidates are
regulated as biological products by the Center for Biologics Evaluation and Research (“CBER”) in the FDA. Biological
products are subject to federal regulation under the Federal Food, Drug, and Cosmetic Act (“FDCA”), the Public Health
Service (“PHS”) Act, and other federal, state, local and foreign statutes and regulations. Both the FDCA and the PHS Act,
as applicable, and their corresponding regulations govern, among other things, the testing, manufacturing, safety, efficacy,
labeling, packaging, storage, record keeping, distribution, import, export, reporting, advertising and other promotional
practices involving drugs and biological products.
The process required by the FDA before a biological product may be marketed in the U.S. generally involves
years of studies and many complex steps. The first of these is completion of nonclinical laboratory studies, meaning in vivo
and in vitro experiments in which an investigational product is studied prospectively in a test system under laboratory
conditions to determine its safety, must be conducted according to Good Laboratory Practice (“GL”) regulations, as well
as, in the case of nonclinical laboratory studies involving animal test systems, in accordance with applicable requirements
for the humane use of laboratory animals and other applicable regulations.
Some of the manufacturing materials and/or components that we use in, and which are critical to, implementation
of our technology involve the use of animal-derived products. Our media is sourced from fetal bovine serum (“FBS”), and
is the main consumable used in our manufacturing process.
While FBS is commonly used in the production of various marketed biopharmaceuticals, our suppliers of FBS
must meet our strict quality standards are thus limited in number and region.
5.4 Product Quality
The Company has a Quality Management Department with appropriate controls in place for monitoring and
compliance of clinical and non-clinical studies as well as manufacturing operations. Our quality assurance processes align
with the widely accepted quality standards from the ICH Guidelines created by The International Conference on
Harmonization of Technical Requirements for Pharmaceuticals for Human Use (“ICH”) as well as FDA Regulations. All
Mesoblast personnel are responsible for the identification and prompt reporting of all actual or potential adverse events or
product quality complaints. This may include any reported problem with a finished product, its packaging, inappropriate
healthcare professional use, or unintended patient reaction. We have a regulatory obligation to report all adverse events and
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product complaints, with serious adverse events requiring reporting within 24 hours of receiving notification. The
Company provides personnel with regular training in relation to our obligations and responsibilities.
5.5 Clinical Trials and Patient Safety
Mesoblast works with healthcare professionals, academic organizations, and contract research organizations
(“CRO”) to perform company-sponsored pre-clinical and clinical research. The Company also provides financial support or
drug product for independent third-party studies such as Investigator Initiated Trials (IITs) via grant requests. All studies
must be scientifically valid and likely to generate data that will be relevant to a defined product development or other
clinical and/or business need. These research initiatives are never used as a way to induce a healthcare professional or
healthcare organization to use, recommend, or purchase Mesoblast products, or to encourage off-label use of marketed
products.
Each potential study subject/study subject legal guardian is provided with an Informed Consent Form (“ICF”) by
the clinical trial site study team. The ICF contains information that must be provided to each possible study candidate, such
as an explanation of the purpose of the research, possible risks/benefits as well as statements describing the confidentiality
of information collected, how the information may be used and who may view this information. Each potential study
subject/legal guardian is given time to read the ICF and to ask questions about anything they don’t understand. In addition,
the ICF provides the Primary Investigator’s (“PI”) and Independent Review Board’s (“IRB”) contact information to the
subject to ask questions and/or report any study related concerns. Once all questions are answered, signatures are obtained
to record consent. Mesoblast, as the Sponsor, together with the CRO, monitors the sites for any protocol deviations
throughout the course of the study. If and when protocol deviations are identified, we will work with the CRO and site(s) to
address them as quickly as possible. Study subject safety is front and foremost in our conduct of all our clinical studies.
Between our Therapeutic Area Heads, Quality Assurance (“QA”), and Safety and Clinical Operations, we monitor the
conduct of our clinical trials extremely thoroughly and work to protect the well-being of the study subjects as well as the
integrity of the trial.
Company exploration of innovative therapies, including research projects, database reviews, and pre-clinical and
clinical trials, are designed to first and foremost protect the rights and safety of study subjects and to maintain the integrity
of research data. We do this by complying with all regulatory standards regarding research programs and encouraging all
involved persons to report any deviations, including inaccurate reporting of study data, inappropriate use of study funds or
pharmaceutical product, falsification of study reports, or failure to obtain Independent Review Board or other required
approval prior to conducting a study. This process includes all clinical trial investigators attesting that they’ve read and
understood the contents of the clinical trial protocol and agree to conduct the trial in compliance with the protocol, good
clinical practice and applicable regulatory requirements.
6.
Supply Chain Management
Mesoblast has an established vendor assurance program through which suppliers are audited for purposes of being
qualified and added to an approved suppliers list. All approved suppliers are audited on a routine basis. Our Supplier
Management procedure describes the detailed process for qualifying and managing suppliers which includes quality
agreements, supply agreements, due diligence activities, and audits.
6.1 Manufacturing Safe Products
Given the current scale of our operations, elements of our business including manufacturing are outsourced to
third-party providers. Mesoblast has established a strategic alliance with Lonza, a global leader in biopharmaceutical
manufacturing. We monitor Lonza and other third-party providers through our vendor assurance program. In addition, all
entities involved in the preparation of therapeutics for clinical studies or commercial sale, including Lonza, are subject to
extensive external regulation. Components of a finished therapeutic product approved for commercial sale or used in late-
stage clinical studies must be manufactured in accordance with current international Good Manufacturing Practice
(“GMP”) and other international regulatory requirements. These regulations govern manufacturing processes and
procedures (including record keeping) and the implementation and operation of quality systems to control and assure the
quality of investigational products and products approved for sale.
Mesoblast, our collaborators, and our suppliers as appropriate must supply all necessary documentation in support
of any application for product approval and must adhere to current GLP and current GMP regulations enforced by the FDA
and other regulators through their facilities inspection program. Before we can begin commercial manufacture of our
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products for sale in the United States, we must obtain FDA regulatory approval for the product. In addition, the processes
and quality systems associated with the manufacturing of such product must also be approved, which requires a successful
FDA inspection of the manufacturing facilities, including Lonza’s manufacturing facilities.
In addition, regulators may at any time audit or inspect a manufacturing facility involved with the preparation of
our product candidates, raw materials, or the associated quality systems. Although we cannot control the manufacturing
process of, and are dependent on, the contract manufacturer for compliance with the regulatory requirements, through our
vendor assurance program, we monitor the performance and undertake an annual audit of each contract manufacturer
involved in the production of our product candidates. In addition, Lonza is monitored through an established governance
structure with multiple feedback loops to ensure compliance to established contracts, specifications, and policies. In
addition to having staff onsite and personnel in the plant to oversee ongoing activities, the organizations review numerous
manufacturing and quality metrics to ensure consistent product manufacture.
6.2 Bone Marrow
The initial stage of manufacturing involves obtaining mesenchymal lineage cell-containing bone marrow from
healthy consenting donors. The process of identifying new donor tissue, testing and verifying its validity in order to create
new cell banks is tightly regulated and validated with the FDA and other regulators. For example, U.S. federal and state
governments and other jurisdictions impose restrictions on the acquisition and use of tissue, including those incorporated in
federal Good Tissue Practice regulations. Our manufacturing partner Lonza also has a dedicated U.S. facility for bone
marrow acquisition. Lonza maintains all documents and records generated during the lifecycle of donor screening and bone
marrow aspiration in a donor-specific file under its site quality system.
6.3 Storage and Distribution
Storage and distribution of our product candidates are contracted to CSM on Demand, ICS AmerisourceBergen,
CryoSite, and CryoPort Solutions who are experts in innovative storage and/or distribution solutions for pharmaceutical
manufacturers. Performance is monitored through established contractual agreements, and the interactions of our joint
project teams, as well as through regular supplier audits and qualifications.
7.
Access to Healthcare
Mesoblast does not currently have a product approved and commercialized. In July 2024, we resubmitted a BLA
to the FDA for approval of Ryoncil (remestemcel-L) in the treatment of children with SR-aGVHD. FDA considered the
resubmission to be a complete response and set a PDUFA goal date of January 7, 2025. If approved by FDA, this product
would constitute the Company’s first commercialized product. We acknowledge and support the social importance of
providing access to healthcare across all geographic regions regardless of socio-economic status and recognize this is
frequently regarded as one of the top ESG topics for the Biopharma sector. Despite our current size, financial status, and
stage of clinical development, we have in place elements that reflect this important social topic.
7.1 Expanded Access Programs
Under a compassionate use protocol in the US, Mesoblast has continued to make remestemcel-L available to
children as ‘salvage therapy’ where all other treatment avenues have been exhausted and the risk of mortality is high. More
than 250 children have had access to remestemcel-L under these circumstances, provided by us at no cost.
In 2020, an Expanded Access Protocol (“EAP”) was initiated in the US for compassionate use of remestemcel-L
in the treatment of COVID-19 infected children with cardiovascular and other complications of MIS-C (multisystem
inflammatory syndrome in children). MIS-C is a life-threatening complication of COVID-19 in otherwise healthy children
and adolescents that includes massive simultaneous inflammation of multiple critical organs and their vasculature.
Mesoblast has provided treatment at no charge to three children under this EAP.
7.2 Product Pricing
In the United States, Federal and state government agencies may purchase Mesoblast products and provide
reimbursement on those products via the state and federal healthcare programs, such as Medicare and Medicaid, once
Mesoblast’s product receives regulatory approval and is able to be commercialized. Various federal laws and/or
government contracting requirements give some of these purchasers and reimbursors the right to discounted prices and/or
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rebates on Company products. Depending on the requirements that apply to the pricing terms the Company is reporting,
our prices should reflect any reductions, rebates, up-front payments, coupons, goods in kind, free or reduced-price services,
grants, price concessions, or other benefits offered to induce a sale may be considered pricing terms. Mesoblast is
committed to accurately taking these items into account.
8.
Environment
Mesoblast is committed to protecting the world in which we live and work, and we aim to minimize our impact on
the wider environment and its component parts. Currently, Mesoblast’s direct physical footprint is limited to office and
laboratory space for our employee base of less than 100, so our direct, physical environmental impact is currently limited.
Nonetheless, Mesoblast has begun initiatives to improve our impact such as sourcing our electricity from green energy
providers and introducing office waste recycling programs. In addition, as noted above, many of our employees and
consultants are dispersed and are infrequently in our office spaces.
We are also driving initiatives to minimize the inputs and outputs to our manufacturing processes through our
investment in research and development that focuses on the scaling of technologies and minimizing waste. We are
developing a 3D bioreactor process to expand our cell product which will replace our current 2D process involving plates.
This will reduce the amount of plastic and biohazardous waste that will be generated by our manufacturing processes.
As mentioned above, we rely on third-party providers for important elements of our business. We and our partners
must comply with environmental laws and regulations, including those relating to the discharge of materials into the air,
water and ground, the manufacture, storage, handling, use, transportation and disposal of hazardous and biological
materials, and the health, wellbeing and safety of employees with respect to laboratory activities required for the
development of products and technologies.
4.B
Business Overview
Mesoblast has developed a range of late-stage product candidates derived from our first and second generation
proprietary mesenchymal lineage cell therapy technology platforms.
Remestemcel-L is our first-generation mesenchymal lineage stromal cell (“MSC”) product platform and is in late
stage development for treatment of systemic inflammatory diseases including:
•
Steroid refractory acute graft versus host disease (SR-aGVHD); and
•
Biologic refractory inflammatory bowel disease, including Crohn's disease.
Rexlemestrocel-L is our second generation mesenchymal lineage precursor cell product platform and is in late
stage development for treatment of:
•
Chronic heart failure (CHF); and
•
Chronic low back pain (CLBP) due to degenerative disc disease.
Both platforms have life cycle management strategies with promising emerging pipelines.
The Company’s proprietary manufacturing processes yield industrial-scale, cryopreserved, off-the-shelf, cellular
medicines. These cell therapies, with defined pharmaceutical release criteria, are planned to be readily available to patients
worldwide upon receiving marketing authorizations.
Mesoblast’s immuno-selected, culture expanded cellular medicines are based on mesenchymal precursor cells
(“MPCs”) and their progeny, MSCs. These are rare cells (approximately 1:100,000 in bone marrow) found around blood
vessels that are central to blood vessel maintenance, repair and regeneration. These cells have a unique immunological
profile with immunomodulatory effects that reduce inflammation allowing healing and repair. This mechanism of action
enables the targeting of multiple disease pathways across a wide spectrum of complex diseases with significant unmet
medical needs.
Mesenchymal lineage cells are collected from the bone marrow of healthy adult donors and proprietary processes
are utilized to expand them to a uniform, well characterized, and highly reproducible cell population. This enables
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manufacturing at industrial scale for commercial purposes. Another key feature of Mesoblast’s cells is they can be
administered to patients without the need for donor–recipient matching or recipient immune suppression.
Mesoblast’s approach to product development is to ensure rigorous scientific investigations are performed with
well-characterized cell populations in order to understand mechanisms of action for each potential indication. Extensive
preclinical translational studies guide clinical trials that are structured to meet stringent safety and efficacy criteria set by
international regulatory agencies. All trials are conducted under the continuing review of independent Data Safety
Monitoring Boards comprised of independent medical experts and statisticians. These safeguards are intended to ensure the
integrity and reproducibility of results, and to ensure that outcomes observed are scientifically reliable.
Allogeneic, Off-the-Shelf, Commercially Scalable Products
Our technology platform enables development of a diverse range of products derived from the mesenchymal cell
lineage in adult tissues. MPCs constitute the earliest known cell type in the mesenchymal lineage in-vivo.
MPCs can be isolated using monoclonal antibodies and culture-expanded using methods that enable efficient
expansion without differentiation. MSCs are defined biologically in culture following density gradient separation from
other tissue cell types and following culture by plastic adherence. MSCs presumably represent culture-expanded in-vitro
progeny of the undifferentiated MPCs present in-vivo. The functional characteristics of each cell type enable product
development for specific indications.
Our proprietary mesenchymal lineage cell-based products have distinct biological characteristics enabling their
use for allogeneic purposes.
Immune Privilege: Mesenchymal lineage cells are immune privileged, in that they do not express specific cell
surface co-stimulatory molecules that initiate immune allogeneic responses.
Expansion: We have developed proprietary methods that enable the large-scale expansion of our cells while
maintaining their ability to produce the key biomolecules associated with tissue health and repair. This allows us to
produce a cellular product intended to demonstrate consistent and well-defined characterization and activity.
Products Commercialized by Licensees
Two allogeneic mesenchymal stromal cell (MSC) products developed and commercialized by Mesoblast licensees
have been approved in Japan and Europe, with both licensees the first to receive full regulatory approval for an allogeneic
cellular medicine in these major markets.
Mesoblast’s licensee in Japan, JCR Pharmaceuticals Co. Ltd. (“JCR”), is marketing its MSC-based product in
Japan for the treatment of aGVHD in children and adults. TEMCELL® HS Inj. (“TEMCELL”) was the first allogeneic
cellular medicine to receive full regulatory approval in Japan. Mesoblast receives royalty income on sales of TEMCELL®
in Japan.
In 2017, Mesoblast granted TiGenix S.A.U (“TiGenix”), now a wholly owned subsidiary of Takeda
Pharmaceutical Co. Ltd. (“Takeda”), exclusive access to certain of its patents to support global commercialization of
Alofisel®, the first allogeneic MSC therapy to receive central marketing authorization approval from the European
Commission. Mesoblast receives royalty income on Takeda’s worldwide sales of Alofisel® in the local treatment of
perianal fistulae.
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Mesoblast Product Candidates
Ryoncil® (remestemcel-L) for the Treatment of Steroid Refractory Acute Graft Versus Host Disease
Overview
Ryoncil® (remestemcel-L) is an intravenously delivered product candidate for the treatment of steroid-refractory
acute graft versus host disease, or SR-aGVHD, following an allogeneic bone marrow transplant (“BMT”).
In a bone marrow transplant, donor cells can attack the recipient, causing a-GVHD. The donor T-cell mediated
inflammatory response involves secretion of TNF-alpha and IFN-gamma, resulting in activation of pro-inflammatory T-
cells and tissue damage in the skin, gut and liver, which can be fatal.
Remestemcel-L is suggested to have immunomodulatory properties to counteract the cytokine storm that is
implicated in various inflammatory conditions. The mechanism of action is thought to involve down-regulating the
production of pro-inflammatory cytokines, increasing production of anti-inflammatory cytokines, and enabling recruitment
of naturally occurring anti-inflammatory cells to involved tissues.
This life-threatening disease occurs in approximately 50% of patients who receive an allogeneic BMT. Over
30,000 patients worldwide undergo an allogeneic BMT annually, primarily during treatment for blood cancers, and these
numbers are increasing. In patients with the most severe form of SR-aGVHD (Grade C/D or III/IV) mortality can be as
high as 90% despite optimal best available therapy. There are currently no FDA-approved treatments in the United States
for children under 12 with SR-aGVHD.
Current Status and Anticipated Milestones
Mesoblast submitted its completed BLA to the FDA for RYONCIL in January 2020. The BLA was subsequently
accepted for priority review by the FDA on March 30, 2020, with a Prescription Drug User Fee Act (“PDUFA”) action
date set for September 30, 2020. In August 2020, the FDA’s Oncologic Drugs Advisory Committee (“ODAC”) voted
overwhelmingly in favor (nine to one(1)) that the available data support the efficacy of RYONCIL in pediatric patients with
SR-aGVHD. FDA issued a CRL on September 30, 2020, noting deficiencies related to clinical and Chemistry,
Manufacturing and Controls (“CMC”) data.
Mesoblast has worked to address the issues noted in the Complete Response Letter, through multiple interactions
with FDA for guidance. Mesoblast provided these new data to FDA to address all CMC outstanding items as required in
January 2023. In March, 2023, the FDA accepted the BLA resubmission considering the resubmission to be a complete
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response and set a PDUFA goal date of August 2, 2023. In August 2023, the FDA provided a CRL to the BLA
resubmission for RYONCIL for the treatment of pediatric SR-aGVHD requiring more data to support marketing approval,
including potency assay or clinical data. As part of the BLA review, FDA completed the PLI of the manufacturing facility,
did not issue any Form 483, and found no objectionable conditions.
In February 2024, ahead of a scheduled meeting with FDA, Mesoblast provided new data from a second potency
assay for RYONCIL that provided additional product characterization as requested by FDA. In March 2024, FDA
informed Mesoblast that following additional consideration the available clinical data from its Phase 3 study MSB-
GVHD001 appears sufficient to support submission of the proposed BLA for remestemcel-L for treatment of pediatric
patients with SR-aGVHD. In July 2024, Mesoblast resubmitted the BLA for approval. FDA considered the resubmission to
be a complete response and provided a Prescription Drug User Fee Act ("PDUFA") goal date of January 7, 2025.
There are currently no FDA-approved treatments in the US for children under 12 with SR-aGVHD and only one
FDA-approved treatment in the US for other SR-aGVHD patients.
Mesoblast intends to conduct a targeted, controlled study in the highest-risk adults with the greatest mortality.
This adult study is in line with our overall commercial strategy, which envisioned a sequenced progression from pediatric
to adult SR-aGVHD indications. Adults comprise 80% of the SR-aGVHD market. Mesoblast is collaborating with Blood
and Marrow Transplant Clinical Trials Network (BMT CTN) in the United States, a body that is funded by the National
Institutes of Health (NIH) and is responsible for approximately 80% of all US allogeneic BMTs, to conduct a pivotal trial
in adults with SR-aGVHD.
We believe the U.S. adult and pediatric SR-aGVHD market requires a small, targeted commercial footprint. The
target call point for SR-aGVHD will primarily be physicians in hematology/oncology who perform hematopoietic stem cell
transplants. In the U.S., there are approximately 80 centers that perform pediatric transplants, with 50% of all transplants
occurring at approximately 15 centers. Similarly, there are approximately 110 centers that perform adult transplants with
half of those transplants occurring at approximately 20 centers.
The Company has put in place a lifecycle extension strategy to generate evidence-based clinical outcomes to
maximize the value of remestemcel-L in other pediatric and adult rare diseases that do not require large distribution
channels. In addition, we plan to expand investigator-initiated clinical trials for chronic GVHD and other indications that
are currently underway or planned for the near future.
(1)
This vote included a change to the original vote by one of the ODAC panel members after electronic voting
closed.
Remestemcel-L for Inflammatory Bowel Disease (IBD) – Ulcerative Colitis (UC) and Crohn’s Colitis
Overview
According to recent estimates, more than three million people (1.3%) in the United States alone have
inflammatory bowel disease, with more than 33,000 new cases of Crohn’s disease and 38,000 new cases of ulcerative
colitis diagnosed every year. Despite recent advances, approximately 30% of patients are primarily unresponsive to anti-
TNFα agents and even among responders, up to 10% will lose their response to the drug every year. Up to 80% of patients
with medically refractory Crohn’s disease eventually require surgical treatment of their disease, which can have a
devastating impact on quality of life.
Current Status
A small investigator-initiated randomized, controlled study of remestemcel-L delivered by an endoscope directly
to the areas of inflammation and tissue injury with medically refractory Crohn’s disease and ulcerative colitis was
undertaken at Cleveland Clinic. The study is the first in humans using local cell delivery in the gut and will enable
Mesoblast to compare clinical outcomes using this delivery method with results from an ongoing randomized, placebo-
controlled trial in patients with biologic-refractory Crohn’s disease where remestemcel-L was administered intravenously.
Results from the randomized, controlled study of remestemcel-L by direct endoscopic delivery to areas of inflammation in
patients with medically refractory Crohn’s colitis were published in the peer-reviewed journal British Journal of Surgery.
Strategically, Mesoblast views UC and Crohn’s colitis as a potentially important label extension for remestemcel-
L given the gastrointestinal involvement common to acute graft versus host disease and inflammatory bowel disease.
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Gastrointestinal damage is the major driver of aGVHD mortality and is linked to systemic inflammation in aGVHD.
Biomarkers that predict high mortality in aGVHD, such as blood levels of soluble suppression of tumorigenicity 2 (ST2)
have shown to be significantly reduced in patients treated with remestemcel-L. ST2 has also been shown to be associated
with active IBD (UC & Crohn’s).
Rexlemestrocel-L for Chronic Low Back Pain (CLBP) associated with Degenerative Disc Disease (DDD)
Overview
Rexlemestrocel-L (MPC-06-ID) for CLBP consists of a unit dose of 6 million MPCs administered by syringe
directly into a damaged disc.
In CLBP, damage to the disc is the result of a combination of factors related to aging, genetics, and micro-injuries,
which compromises the disc’s capacity to act as a fluid-filled cushion between vertebrae and to provide anatomical
stability. Damage to the disc also results in an inflammatory response with ingrowth of nerves which results in chronic
pain. This combination of anatomic instability and nerve ingrowth results in CLBP and functional disability.
With respect to mechanisms of action in CLBP, extensive pre-clinical studies have established that MLCs have
anti-inflammatory effects and secrete multiple paracrine factors that stimulate new proteoglycan and collagen synthesis by
chondrocytes in vitro and by resident cells in the nucleus and annulus in vivo.
It is estimated that over 7 million people in the U.S. alone suffer from CLBP associated with DDD, of which 3.2
million patients have moderate disease. This market is projected to have annual growth rate similar to that of the US
population annual growth rate. After failure of conservative measures (medication, injections, physical therapy etc.), there
is a need for non-opioid treatments that are effective over a sustained period of time. When disc degeneration has
progressed to a point that pain and loss of function can no longer be managed by conservative means, major invasive
surgery such as spinal fusion is the most commonly offered option.
All non-surgical therapies for progressive, severe and debilitating pain due to degenerating intervertebral discs
treat the symptoms of the disease. However, they do not address the underlying cause of the disease. Surgical intervention
is not always successful in addressing the patient’s pain and functional deficit. It has been estimated that the incidence of
failed back surgery is as high as 50% for standard procedures and may increase for more complex surgeries. Total costs of
low back pain are estimated to be between $100.0 billion and $200.0 billion annually with two thirds attributed to patients’
decreased wages and productivity.
As a result, we believe that the most significant unmet need and commercial opportunity in the treatment of CLBP
is a therapy that has the ability to impact the chronic pain and disability associated with the condition.
Current Status and Anticipated Milestones
The Phase 3 clinical trial for CLBP completed enrollment in March 2018 with 404 patients enrolled across 48
centers in the United States and Australia randomized 1:1:1 to receive either 6 million MPCs with hyaluronic acid
(MPC+HA), 6 million MPCs without hyaluronic acid (MPC) or saline control. Although the trial's composite outcomes of
pain reduction together with functional responses to treatment were not met by either MPC group; the MPC+HA treatment
group achieved substantial and durable reductions in pain compared to control through 24 months across the entire
evaluable study population (n=391) compared with saline controls. Greatest pain reduction was observed in the pre-
specified population with CLBP of shorter duration than the study median of 68 months (n=194) and subjects using opioids
at baseline (n=168) with the MPC+HA group having substantially greater reduction at all time points (1, 3, 6, 12, 18 and 24
months) compared with saline controls. There was no appreciable difference in the safety of MPC groups compared to
saline control over the 24-month period of follow-up in the entire study population. In subjects using opioids at baseline,
the MPC+HA demonstrated a reduction in the average opioid dose over 24 months, while saline control subjects had
essentially no change.
In July 2024, enrollment commenced at multiple sites across the United States in a confirmatory Phase 3 trial of
rexlemestrocel-L in patients with CLBP due to inflammatory degenerative disc disease of less than five years duration. The
FDA has previously confirmed alignment with Mesoblast on the design of the 300-patient randomized, placebo-controlled
trial and the 12-month primary endpoint of pain reduction as an approvable indication. Key secondary measures include
improvement in quality of life, function, and reduced opioid usage.
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In February 2023, FDA granted Regenerative Medicine Advanced Therapy ("RMAT") designation for
rexlemestrocel-L in the treatment of CLBP associated with disc degeneration, in combination with HA as delivery agent for
injection into the lumbar disc. RMAT designations aim to expedite the development of regenerative medicine therapies
intended to treat, modify, reverse, or cure a serious or life-threatening disease or condition where preliminary clinical
evidence indicates that the drug has the potential to address unmet medical needs for the disease or condition. An RMAT
designation for rexlemestrocel-L provides all the benefits of Breakthrough and Fast Track designations, including rolling
review and eligibility for priority review on filing of a BLA.
Revascor® (rexlemestrocel-L) for Chronic Heart Failure with Reduced Ejection Fraction (HFrEF)
Overview
Mesoblast is developing rexlemestrocel-L to fill the treatment gap for chronic heart failure (CHF). Patients with
CHF continue to represent high unmet medical need despite recent advances in new therapeutic agents for chronic heart
failure. The American Heart Association (AHA) estimated in 2017 that prevalence is expected to grow 46% by 2030 in the
U.S., affecting more than 8 million Americans. CHF causes severe economic, social, and personal costs. In the U.S., it is
estimated that CHF results in direct costs of $60.2 billion annually when identified as a primary diagnosis and $115.0
billion as part of a disease milieu. Mesoblast believes that targeting high-risk chronic patients with the highest unmet
clinical needs provides the company with the most efficient path to market.
Revascor® (rexlemestrocel-L) for HFrEF consists of 150 million mesenchymal precursor cells (MPCs)
administered by direct cardiac injection. MPCs release a range of factors when triggered by specific receptor-ligand
interactions within damaged tissue. Based on preclinical data, we believe that the factors released from the MPCs induce
functional cardiac recovery by simultaneous activation of multiple pathways, including induction of endogenous vascular
network formation, reduction in harmful inflammation, reduction in cardiac fibrosis, and reversal of endothelial
dysfunction through activation of intrinsic tissue precursors.
CHF is classified in relation to the severity of the symptoms experienced by the patient. The most commonly used
classification system for functional severity of heart failure, established by the NYHA, is:
•
Class I (mild): patients experience none or very mild symptoms with ordinary physical activity
•
Class II (mild/moderate): patients experience fatigue and shortness of breath during moderate physical
activity
•
Class III (moderate/severe): patients experience shortness of breath during even light physical activity
•
Class IV or end-stage (severe): patients are exhausted even at rest
Risk for recurrent heart failure-related hospitalizations, occurrence of non-fatal myocardial infarction (MI, heart
attack) or non-fatal stroke, or death increases progressively with increases in left ventricular volumes, reduction in left
ventricular ejection fraction (LVEF), and progression in NYHA functional class. Approximately 50% of all CHF patients
have heart failure with reduced ejection fraction (HFrEF) defined as LVEF <40%, and are at considerable risk of repeated
hospitalizations and death despite maximal drug therapy.
Program in End Stage Heart Failure Patients Requiring Mechanical Support
REVASCOR is being evaluated in patients with end-stage HFrEF implanted with a left ventricular assist device
(“LVAD”).
Every year in the United States over 100,000 patients progress to end-stage HFrEF. In these patients, more than
2,500 life prolonging LVADs are implanted in the U.S. annually, of whom approximately 80% undergo the procedure as
destination or permanent therapy. Most patients receiving LVADs as destination therapy have an ischemic HFrEF etiology.
Compared to patients with non-ischemic HFrEF, patients with ischemic HFrEF have a 76% lower likelihood of LV
functional recovery following LVAD implantation, and increased mortality over the initial 1-2 years. Resistance to
functional recovery in ischemic HFrEF patients is thought to be due to excessive inflammation and microvascular
insufficiency in the ischemic myocardium.
A Phase 2 trial was conducted by a multi-center team of researchers within the United States National Institutes of
Health (“NIH”)-funded Cardiothoracic Surgical Trials Network (“CTSN”), led by Icahn School of Medicine at Mount
Sinai, New York. The National Institute of Neurological Disorders and Stroke, and the Canadian Institutes for Health
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Research also supported this trial. Results of this Phase 2 trial were released in November 2018. The trial was a
prospective, multi-center, double-blind, placebo controlled, 2:1 randomized (MPC to placebo), single-dose cohort trial to
evaluate the safety and efficacy of injecting a dose of 150 million MPCs into the native myocardium of LVAD recipients.
Patients with advanced CHF, implanted with an FDA-approved LVAD as bridge-to-transplant or destination therapy, were
eligible to participate in the trial. All patients were followed until 12 months post randomization.
Across the 159 patients in this Phase 2 trial, the trial did not show a significant difference in the ability for patients
to tolerate a wean for a period of 60 minutes. In the, 70 patients with end-stage ischemic HFrEF the key findings were:
•
Ischemic controls were characterized by persistently elevated levels of the inflammatory cytokine IL-6,
by reduced ability to be weaned from LVAD support, and by high mortality.
•
In contrast, in ischemic patients treated with rexlemestrocel-L, IL-6 levels returned to normal by 2
months and remained low through 12 months.
•
63% of ischemic patients who received a single administration of rexlemestrocel-L successfully
underwent temporary weaning from full LVAD support as early as month 2 as compared with 36% of
controls (p = 0.008).
•
The cumulative incidence of successful temporary weans off the LVAD device over 6 months was also
increased by 1.55-fold over control in ischemic patients who received rexlemestrocel-L ([95% CI 1.01,
2.36]; p=0.02).
•
Only 4.9% of ischemic patients treated with a single administration of rexlemestrocel-L died from month
2 through month 12, as compared with 26.9% of ischemic controls, an 82% reduction (p = 0.02).
Current Status and Anticipated Milestones
In March 2024, FDA provided this feedback in formal minutes to the company following the Type B meeting held
with FDA in February, 2024 for rexlemestrocel-L (Revascor®) under the existing Regenerative Medicine Advanced
Therapy (RMAT) designation. The FDA supported an accelerated approval pathway for rexlemestrocel-L in patients with
end-stage ischemic HFrEF and a left ventricular assist device (LVAD).
In feedback provided to Mesoblast regarding potential pathways to licensure for rexlemestrocel-L, FDA’s
comments indicated that the presented results may support a reasonable likelihood of clinical benefit of MPCs against
mortality in LVAD patients, consistent with the criteria for accelerated approval.
Mesoblast intends to request a pre-BLA meeting with FDA to discuss data presentation, timing and FDA
expectations for an accelerated approval filing in end-stage ischemic HFrEF patients with LVAD implantation.
Rexlemestrocel-L has regenerative medicine advanced therapy (RMAT) designation from the FDA for treatment
of chronic heart failure with left ventricular systolic dysfunction in patients with an LVAD.
Program for Class II/III CHF patients
A multicenter, double-blinded, 1:1 randomized, sham-procedure-controlled Phase 3 study of remestemcel-L was
completed across North America with 565 NYHA Class II/III patients at high risk of repeated heart failure hospitalizations
or a terminal cardiac event (cardiac death, LVAD placement, heart transplant or insertion of an artificial heart). The
enrollment criteria for this trial included a prior decompensated heart failure event (e.g. hospitalization) within the previous
nine months and/or very high level of NT-proBNP, a protein used in diagnosis and screening of CHF. These inclusion
criteria were designed for enrichment in patients with substantial left ventricular contractile abnormality, advanced CHF
due to left ventricular systolic dysfunction and higher risk of recurrent decompensated heart failure hospitalizations and
TCEs. This target patient population was shown to respond effectively to treatment with rexlemestrocel-L in our previous
Phase 2 trial.
Topline results from the 537 patients who met the criteria which allowed for treatment to occur on a 1:1
randomization basis between rexlemestrocel-L and sham control were announced in December 2021. Over a mean 30
months of follow-up, patients with advanced chronic heart failure who received a single endomyocardial treatment with
rexlemestrocel-L on top of maximal therapies had 60% reduction in incidence of heart attacks or strokes and 60% reduction
in death from cardiac causes when treated at an earlier stage in the progressive disease process. Despite significant
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reduction in the pre-specified endpoint of cardiac death, there was no reduction in study primary end point of recurrent
non-fatal decompensated heart failure events, which was the trial’s primary endpoint.
The combination of the three pre-specified outcomes of cardiac death, heart attack or stroke into a single
composite outcome - called the three-point major adverse cardiovascular event (MACE) is a well-established endpoint used
by the FDA to determine cardiovascular risk. Rexlemestrocel-L reduced this three-point MACE by 30% compared to
controls across the population of 537 patients. In the NYHA class II subgroup of 206 patients, rexlemestrocel-L reduced
the three-point MACE by 55% compared to controls.
DREAM-HF Phase 3 trial results were published in the premier peer-reviewed journal for cardiovascular
medicine, the Journal of the American College of Cardiology (JACC) in February 2023.
Complementary Technologies
In addition to having the most mature and diverse allogeneic cell therapy product pipeline and technology
platform in the field of cellular medicines, we have strategically targeted the acquisition of rights to technologies that are
complementary to and synergistic with our mesenchymal lineage cell technology platform. The aim of this activity is to
maintain our technology leadership position in the regenerative medicine space, while simultaneously expanding our
targeted disease applications and managing the life-cycle of our current lead programs.
Our complementary technologies and additional product candidates include other types of mesenchymal lineage
cells, cell surface modification technologies, pay-loading technology and protein and gene technologies.
Manufacturing and Supply Chain
Our manufacturing strategy for our cellular product candidates focuses on the following important factors:
(i)
ability for product delineation to protect pricing and partner markets by creating distinct products using
discrete manufacturing processes, culture conditions, formulations, routes of administration, and/or dose
regimens;
(ii)
establishing proprietary commercial scale-up and supply to meet increasing demand;
(iii)
implementing efficiencies and yield improvement measures to reduce cost-of-goods;
(iv)
maintaining regulatory compliance with best practices; and
(v)
establishing and maintaining multiple manufacturing sites for product supply risk mitigation.
The cell therapy manufacturing and distribution process generally involves five major steps.
•
Procure bone marrow—acquire bone marrow from healthy adults with specific FDA-defined criteria,
which is accompanied by significant laboratory testing to establish the usability of the donated tissues.
•
Create master cell banks—isolate MLCs from the donated bone marrow and perform a preliminary
expansion to create master cell banks. Each individual master cell bank comes from a single donor.
•
Expand to therapeutic quantities—expand master cell banks to produce therapeutic quantities, a process
that can yield thousands of doses per master cell bank, with the ultimate number depending on the dose
for the respective product candidate being produced.
•
Formulate, package and cryopreserve.
•
Distribute—our cellular products are cryopreserved at the manufacturer and shipped to storage sites in
the U.S. and other jurisdictions via cryoshippers. Those distribution centers then re-package and send the
products on to treatment centers in cryoshippers. Treatment centers will either move the products into
their own freezers or receive the cryoshipper in “real time” and the product stays in the cryoshipper until
thawed for patient use within a well-defined window. We intend to continue utilizing this approach in the
future.
To date our product candidates have been manufactured in two-dimensional, or 2D, planar, 10-layer cell factories,
using media containing fetal bovine serum, or FBS.
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The relatively small patient numbers and orphan drug designation for remestemcel-L lead us to believe that 2D
manufacturing will be adequate to meet demand for this product candidate if fully approved. We also believe that 2D
manufacturing process and facilities are commercially feasible for Phase 3 trial supply and the initial launch of MPC-06-ID
for CLBP.
However, to build up commercial supply for certain of our product candidates long-term, we are developing novel
manufacturing processes using three-dimensional, or 3D, bioreactors with greater capacity to improve efficiency and
yields, with resulting lower-cost of goods. We intend to evaluate products produced in 3D bioreactors in pre-clinical and
potentially clinical studies, which may serve as FDA required comparability studies to 2D if successful.
We are also focusing on the introduction of FBS-free media which has the potential to result in efficiency and
yield improvements to the current 2D process. We intend to conduct comparability studies to illustrate that products
produced with this media are equivalent to those produced using FBS based media. While we remain confident in our
ability to deliver successful outcomes from each of these activities, any unexpected issues or challenges faced in doing so
could delay our programs or prevent us from continuing our programs.
Our manufacturing activities to date have met stringent criteria set by international regulatory agencies, including
the FDA. By using well-characterized cell populations, our manufacturing processes promote reproducibility and batch-to-
batch consistency for our allogeneic cell product candidates. We have developed robust quality assurance procedures and
lot release assays to support this reproducibility and consistency.
Intellectual Property
We have a large patent portfolio of issued and pending claims covering compositions of matter, uses for our
mesenchymal lineage cell-based technologies and other proprietary regenerative product candidates and technologies, as
well as for elements of our manufacturing processes. As of July 2024, the patent portfolio comprises approximately 1,085
patents and patent applications across 66 patent families, with protection extending through to at least 2045 in all major
markets.
One of our major objectives is to continue to protect and expand our extensive estate of patent rights and trade
secrets, which we believe enables us to deliver commercial advantages and long-term protection for our product candidates
based on our proprietary technologies, and support our corporate strategy to target large, mature and emerging healthcare
markets for our exploratory therapeutic product candidates.
More specifically, our patent estate includes issued patent and patent applications in major markets, including, but
not limited to, the United States, Europe, Japan and China. The patents that we have obtained, and continue to apply for,
cover mesenchymal lineage cell technologies and product candidates derived from these technologies, irrespective of the
tissue source, including bone marrow, adipose, placenta, umbilical cord and dental pulp.
These patents cover, among other technology areas, a variety of MLCs (including MPCs and MSCs), and the use
of MLC for expansion of hematopoietic stem cells, or HSCs. Among the indication-specific issued or pending patents
covering product candidates derived from our mesenchymal lineage cells are those which are directed to our lead product
candidates: aGVHD, ARDS, CLBP, CHF and chronic inflammatory conditions such as RA. We also have issued and
pending patents covering other pipeline indications, including diabetic kidney disease, inflammatory bowel disease (e.g.,
Crohn’s disease), neurologic diseases, eye diseases and additional orthopedic diseases. In addition, we have in-licensed
patents covering complementary technologies, such as other types of mesenchymal lineage cells, cell surface modification
technologies, pay-loading technology and protein and gene technologies, as part of our strategy to expand our targeted
disease applications and manage the life-cycle of our current lead programs.
Our patent portfolio also includes issued and pending coverage of proprietary manufacturing processes that are
being used with our current two-dimensional manufacturing platform as well as the 3D bioreactor manufacturing processes
currently under development. These cell manufacturing patents cover isolation, expansion, purification, scale up, culture
conditions, aggregates minimization, cryopreservation, release testing and potency assays. In addition, we maintain as a
trade secret, among other things, our proprietary FBS-free media used in our 3D bioreactor manufacturing processes.
We maintain trade secrets covering a significant body of know-how and proprietary information relating to our
core product candidates and technologies. We protect our confidential know-how and trade secrets in a number of ways,
including requiring all employees and third parties that have access to our confidential information to sign non-disclosure
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agreements, limiting access to confidential information on a need-to-know basis, maintaining our confidential information
on secure computers, and providing our contract manufacturers with certain key ingredients for our manufacturing process.
In addition, in many major jurisdictions there are other means that may be available to us by which we would be
able to extend the period during which we have commercial exclusivity for our product candidates, which include, but are
not limited to the exclusive right to reference our data, orphan drug exclusivity and patent term extensions.
As part of our strategy, we seek patent protection for our product candidates and technologies in major
jurisdictions including the United States, Europe, Japan, China, and Australia and file independent and/or counterpart
patents and patent applications in other jurisdictions globally that we deem appropriate under the circumstances, including
India, Canada, Hong Kong, Israel, Korea and Singapore. As of July 2024, our patent portfolio includes the following
patents and patent applications in the following major jurisdictions: 67 granted U.S. patents and 51 pending U.S. patent
applications; 64 granted Japanese patents and 35 pending Japanese patent applications; 31 granted Chinese patents and 32
pending Chinese patent applications; 50 granted European patents and 37 pending European patent applications; and 51
granted Australian patents and 32 pending Australian patent applications.
Our policy is to patent the technology, inventions and improvements that we consider important to the
development of our business, only in those cases in which we believe that the costs of obtaining patent protection is
justified by the commercial potential of the technology and associated product candidates, and typically only in those
jurisdictions that we believe present significant commercial opportunities to us. In those cases where we choose neither to
seek patent protection nor protect the inventions as trade secrets, we may publish the inventions so that it defensively
becomes prior art in order for us to secure a freedom to operate position and to prevent third parties from patenting the
invention.
We also seek to protect as trade secrets our proprietary and confidential know-how and technologies that are either
not patentable or where we deem it inadvisable to seek patent protection. To this end, we generally require all third parties
with whom we share confidential information and our employees, consultants and advisors to enter into confidentiality
agreements prohibiting the disclosure of confidential information. These agreements with our employees and consultants
engaged in the development of our technologies require disclosure and assignment to us of the ideas, developments,
discoveries and inventions, and associated intellectual property rights, important to our business. Additionally, these
confidentiality agreements, among others, require that our employees, consultants and advisors do not bring to us, or use
without proper authorization, any third party’s proprietary technology.
License and Collaboration Agreements
All of our revenue relates to upfront, royalty and milestone payments recognized under the license and
collaboration agreements below. For further information on the categorical revenue breakdown during the last three fiscal
years, see “Item 18. Financial Statements – Note 3”.
Grünenthal arrangement
In September 2019, Mesoblast entered into a strategic partnership with Grünenthal GmbH (Grünenthal) to develop
and commercialize MPC-06-ID, the Company’s Phase 3 allogeneic cell therapy candidate for the treatment of chronic low
back pain due to degenerative disc disease in patients who have exhausted conservative treatment options. The agreement
was amended by the parties in June 2021. Under the partnership, Grünenthal will have exclusive commercialization rights
to MPC-06-ID for Europe and Latin America. Mesoblast may receive up to $112.5 million in upfront and milestone
payments prior to product launch, inclusive of $17.5 million already received, if certain clinical and regulatory milestones
are satisfied and reimbursement targets are achieved. Cumulative milestone payments could exceed $1.0 billion depending
on the final outcome of Phase 3 studies and patient adoption. Mesoblast will also receive tiered double-digit royalties on
product sales. There cannot be any assurance as to the total amount of future milestone and royalty payments that
Mesoblast will receive nor when they will be received.
JCR Pharmaceuticals Co., Ltd.—Hematological Malignancies and Hepatocytes Collaboration in Japan
In October 2013, we acquired all of Osiris Therapeutics, Inc.’s business and assets related to culture expanded
MSCs. These assets included assumption of a collaboration agreement with JCR (“JCR Agreement”), which will continue
in existence until the later of 15 years from the first commercial sale of any product covered by the agreement and
expiration of the last Osiris patent covering any such product. JCR is a research and development oriented pharmaceutical
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company in Japan. Under the JCR Agreement we assumed from Osiris, JCR has the right to develop our MSCs in two
fields for the Japanese market: exclusive in conjunction with the treatment of hematological malignancies by the use of
HSCs derived from peripheral blood, cord blood or bone marrow, or the First JCR Field; and non-exclusive for developing
assays that use liver cells for non-clinical drug screening and evaluation, or the Second JCR Field. Under the JCR
Agreement, JCR obtained rights in Japan to our MSCs, for the treatment of aGVHD. JCR also has a right of first
negotiation to obtain rights to commercialize MSC-based products for additional orphan designations in Japan. We retain
all rights to those products outside of Japan.
JCR received full approval in September 2015 for its MSC-based product for the treatment of children and adults
with aGVHD, TEMCELL. TEMCELL is the first culture-expanded allogeneic cell therapy product to be approved in
Japan. It was launched in Japan in February 2016.
Under the JCR Agreement, JCR is responsible for all development and manufacturing costs including sales and
marketing expenses. With respect to the First JCR Field, we have received all sales milestone payments, a total of $3.0
million. Ongoing we are entitled to escalating double-digit royalties in the twenties. These royalties are subject to possible
renegotiation downward in the event of competition from non-infringing products in Japan. With respect to the Second
JCR Field, we are entitled to an approximately 50% profit share.
Intellectual property is licensed both ways under the JCR Agreement, with JCR receiving exclusive and non-
exclusive rights as described above from us and granting us non-exclusive, royalty-free rights (excluding in the First JCR
Field and Second JCR Field in Japan) under the intellectual property arising out of JCR’s development or
commercialization of MSC-based products licensed in Japan.
JCR has the right to terminate the JCR Agreement for any reason, and we have a limited right to terminate the
JCR Agreement, including a right to terminate in the event of an uncured material breach by JCR. In the event of a
termination of the JCR Agreement other than for our breach, JCR must provide us with its owned product registrations and
technical data related to MSC-based products licensed in Japan and all licenses of our intellectual property rights will revert
to us.
We expanded our partnership with JCR in Japan for two new indications: for wound healing in patients with EB in
October 2018, and for neonatal hypoxic ischemic encephalopathy ("HIE"), a condition suffered by newborns who lack
sufficient blood supply and oxygen to the brain, in June 2019.
We will receive royalties on TEMCELL product sales for licensed indications, if and when such indications
receive marketing approval in Japan.
We have the right to use all safety and efficacy data generated by JCR in Japan to support our development and
commercialization plans for our MSC product candidate remestemcel-L in the United States and other major healthcare
markets, including for GVHD, EB and HIE.
Lonza—Manufacturing Collaboration
In September 2011, we entered into a manufacturing services agreement, or MSA, with Lonza Walkersville, Inc.
and Lonza Bioscience Singapore Pte. Ltd., collectively referred to as Lonza, a global leader in biopharmaceutical
manufacturing. Under the MSA, we pay Lonza on a fee for service basis to provide us with manufacturing process
development capabilities for our product candidates, including formulation development, establishment and maintenance of
master cell banks, records preparation, process validation, manufacturing and other services.
We have agreed to order a certain percentage of our clinical requirements and commercial requirements for MPC
products from Lonza. Lonza has agreed not to manufacture or supply commercially biosimilar versions of any of our
product candidates to any third party, during the term of the MSA, subject to our meeting certain thresholds for sales of our
products.
We can trigger a process requiring Lonza to construct a purpose-built manufacturing facility exclusively for our
product candidates. In return if we exercise this option, we will purchase agreed quantities of our product candidates from
this facility. We also have a right to buy out this manufacturing facility at a pre-agreed price two years after the facility
receives regulatory approval.
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The MSA will expire on the three-year anniversary of the date of the first commercial sale of product supplied
under the MSA, unless it is terminated earlier. We have the option of extending the MSA for an additional 10 years,
followed by the option to extend for successive three-year periods subject to Lonza’s reasonable consent. We may
terminate the MSA with two years prior written notice, and Lonza may terminate with five years prior written notice. The
MSA may also terminate for other reasons, including if the manufacture or development of a product is suspended or
abandoned due to the results of clinical trials or guidance from a regulatory authority. In the event we request that Lonza
construct the manufacturing facility described above, neither we nor Lonza may terminate before the third anniversary of
the date the facility receives regulatory approval to manufacture our product candidates, except in certain limited
circumstances. Upon expiration or termination of the MSA, we have the right to require Lonza to transfer certain
technologies and lease the Singapore facility or the portion of such facility where our product candidates are manufactured,
subject to good faith negotiations.
We currently rely, and expect to continue to rely, on Lonza for the manufacture of our product candidates for
preclinical and clinical testing, as well as for commercial manufacture of our product candidates if marketing approval is
obtained.
In October 2019, we entered into an agreement with Lonza for commercial manufacture of remestemcel-L for
pediatric SR-aGVHD. This agreement has facilitated inventory build ahead of the planned US market launch of
remestemcel-L and commercial supply to meet Mesoblast’s long-term market projections. The agreement provides for
Lonza to expand its Singapore cGMP facilities if required to meet long-term growth and capacity needs for the product.
Additionally, it anticipates introduction of new technologies and process improvements which are expected to result in
significant increases in yields and efficiencies.
Singapore Economic Development Board (EDB)—Singapore Operations
In 2014, the Economic Development Board of Singapore, or EDB, granted us certain financial incentives tied to
revenues generated by our Singapore operations, among other things. The incentive for manufacturing activities is for a 15-
year period (broken into five-year increments). We will be eligible for this incentive if we meet certain investment or
activity thresholds in Singapore, including employment levels, amounts of business or manufacturing related expenses.
For example, in order to obtain full financial benefits from the EDB for our manufacturing-related incentives, we
must manufacture at least 50% of the global volume of our first three commercial products in Singapore (subject to certain
exceptions), and we would be required to construct and operate a manufacturing facility in Singapore, and hire and
maintain a specified number of professionals (including supply chain personnel) in connection with the operation of that
facility. The activities under our MSA with Lonza could be used to fulfill all or part of the requirements to obtain the EDB
financial incentives.
Central Adelaide Local Health Network Incorporated—Mesenchymal Precursor Cell Intellectual Property
In October 2004, we, through our wholly-owned subsidiary, Angioblast Systems Inc., now Mesoblast, Inc.,
acquired certain intellectual property relating to our MPCs, or Medvet IP, pursuant to an Intellectual Property Assignment
Deed, or IP Deed, with Medvet Science Pty Ltd, or Medvet. Medvet’s rights under the IP Deed were transferred to Central
Adelaide Local Health Network Incorporated, or CALHNI, in November 2011. In connection with our use of the Medvet
IP, we are obligated to pay CALHNI, as successor in interest to Medvet, (i) certain aggregated milestone payments of up to
$2.2 million and single-digit royalties on net sales of products covered by the Medvet IP, for cardiac muscle and blood
vessel applications and bone and cartilage regeneration and repair applications, subject to minimum annual royalties
beginning in the first year of commercial sale of those products and (ii) and single-digit royalties on net sales of the
specified products for applications outside the specified fields. Additionally, we are obligated to pay CALHNI a double-
digit percentage in the teens of any revenue that we receive in exchange for a grant of a sublicense to the Medvet IP in the
specified fields. Under the IP Deed, we also granted to Medvet a non-exclusive, royalty-free license to the Medvet IP for
non-commercial, internal research and academic research.
Pursuant to the IP Deed, we were assigned the rights in three U.S. patents or patent applications (including all
substitutions, continuations, continuations-in-part, divisional, supplementary protection certificates, renewals, all letters
patent granted thereon, and all reissues, reexaminations, extensions, confirmations, revalidations, registrations and patents
of addition and foreign equivalents thereof) and all future intellectual property rights, including improvements, that might
arise from research conducted at CALHNI related to MPCs and methods of isolating, culturing and expanding MPCs and
their use in any therapeutic area. We also acquired all related materials, information and know-how.
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Osiris Acquisition—Continuing Obligations
In October 2013, we and Osiris entered into a purchase agreement, as amended, or the Osiris Purchase Agreement,
under which we acquired all of Osiris’ business and assets related to culture expanded MSCs. Pursuant to the Osiris
Purchase Agreement, we also agreed to make certain milestone and royalty payments to Osiris pertaining to remestemcel-L
for the treatment of aGVHD and Crohn’s disease. Each milestone payment is for a fixed dollar amount and may be paid in
cash or our ordinary shares or ADSs, at our option. The maximum amount of future milestone payments we may be
required to make to Osiris is $40.0 million. Any ordinary shares or ADSs we issue as consideration for a milestone
payment will be subject to a contractual one year holding period, which may be waived in our discretion. In the event that
the price of our ordinary shares or ADSs decreases between the issue date and the expiration of any applicable holding
period, we will be required to make an additional payment to Osiris equal to the reduction in the share price multiplied by
the amount of issued shares under that milestone payment. This additional payment can be made either wholly in cash or
50% in cash and 50% in our ordinary shares, in our discretion. We have also agreed to pay varying earnout amounts as a
percentage of annual net sales of acquired products, ranging from low single-digit to 10% of annual sales in excess of
$750.0 million. These royalty payments will cease after the earlier of a ten year commercial sales period and the first sale
of a relevant competing product. The first royalty payments were made in 2016.
Tasly Pharmaceutical Group — Cardiovascular Alliance for China
In July 2018, we entered into a Development and Commercialization Agreement with Tasly.
The Development and Commercialization Agreement provides Tasly with exclusive rights to develop,
manufacture and commercialize REVASCOR in China for the treatment or prevention of CHF and MPC-25-IC for the
treatment or prevention of AMI. Tasly will fund all development, manufacturing and commercialization activities in China
for REVASCOR and MPC-25-IC. On closing, we received a $20.0 million upfront technology access fee. Further, we will
receive $25.0 million upon product regulatory approvals in China. Mesoblast will receive double-digit escalating royalties
on net product sales. Mesoblast is eligible to receive six escalating milestone payments upon the product candidates
reaching certain sales thresholds in China.
Tasly can terminate the Development and Commercialization Agreement with a specified amount of notice, on the
later of (a) third anniversary of the agreement coming into effect and (b) receipt of marketing approval in China for each of
REVASCOR or MPC-25-IC. Mesoblast has termination rights with respect to certain patent challenges by Tasly and if
certain competing activities are undertaken by Tasly. Either party may terminate the agreement on material breach of the
agreement if such breach is not cured within the specified cure period or if certain events related to bankruptcy of the other
party occur.
TiGenix NV – patent license for treatment of fistulae
In December 2017, we entered into a Patent License Agreement with TiGenix, now a wholly owned subsidiary of
Takeda, which granted Takeda exclusive access to certain of our patents to support global commercialization of the
adipose-derived MSC product Alofisel®, previously known as Cx601, a product candidate of Takeda, for the local
treatment of fistulae. The agreement includes the right for Takeda to grant sub-licenses to affiliates and third parties.
As part of the agreement, we received $5.9 million (€5.0 million) before withholding tax as a non-refundable
upfront payment, a further payment of $5.9 million (€5.0 million) before withholding tax 12 months after the patent license
agreement date, and a further $1.2 million (€1.0 million) product regulatory milestone payment in the year ended June 30,
2022. We are entitled to further payments of up to €9.0 million when Takeda reaches certain product regulatory milestones.
Additionally, we receive single digit royalties on net sales of Alofisel®.
The agreement will continue in full force in each country (other than the United States) until the date upon which
the last issued claim of any licensed patent covering Alofisel® expires in such country (currently expected to be 2029) or,
with respect to the United States, until the later of (i) the date upon which the last issued claim of any licensed patent
covering Alofisel® in the United States expires (currently expected to be around 2031) or (ii) the expiration of the
regulatory exclusivity period in the United States with an agreed maximum term.
Either we or Takeda may terminate the agreement for any material breach that is not cured within 90 days after
notice thereof. We also have the right to terminate the agreement, with a written notice in the event that Takeda file a
petition in bankruptcy or insolvency or Takeda makes an assignment of substantially all of its assets for the benefit of its
creditors.
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Takeda have the right to terminate their obligation to pay royalties for net sales in a specific country if it is of the
opinion that there is no issued claim of any licensed patent covering Alofisel® in such country, subject to referral of the
matter to the joint oversight/cooperation committee established under the agreement if we disagree.
Competition
The biotechnology and pharmaceutical industries are highly competitive and are characterized by rapidly
advancing technologies and a strong emphasis on proprietary products. Any product candidates that we and our
collaborators successfully develop and commercialize will compete with existing products and new products that may
become available in the future.
A number of our potential competitors, particularly large biopharmaceutical companies, have significantly greater
financial resources and general expertise in research and development, manufacturing, preclinical testing, conducting
clinical trials, obtaining regulatory approvals and marketing approved products than we do. Our market has been
characterized by significant consolidation by pharmaceutical and biotechnology companies, which is likely to result in even
more resources being concentrated among a smaller number of our potential competitors.
Government Regulation
We are developing cellular therapy product candidates. These products are subject to extensive legislation.
Governmental authorities around the world, including the FDA, are charged with the administration and enforcement of
numerous laws and regulations that impact all aspects of the development, production, importing, testing, approval,
labeling, promotion, advertising, and sale of products such as ours. Such governmental authorities are also charged with
administering what is often a lengthy and technical review and approval process before candidate therapies such as ours
may be marketed for any use. Authorization or approval for marketing must generally be obtained from the local health
authorities in each country in which the product is to be sold. Approval and authorization procedures may differ from
country to country, as may the requirements for maintaining approvals. It is typical however for these procedures to require
evidence of rigorous testing and documentation regarding the candidate therapy, which may include significant non-clinical
and clinical evaluations. Extensive controls and requirements apply to the non-clinical and clinical development of our
therapeutic candidates. Those requirements and their enforcement and implementation by local regulatory authorities
around the world significantly impact whether a product candidate can be developed into a marketable product, and notably
impact the cost, resources and timing for any such development. Changes in regulatory requirements and differences in
requirements from country to country may also increase the costs of bringing new technologies such as ours to market and
maintaining approvals, if obtained.
To obtain marketing approval of a new product, an extensive dossier of evidence establishing the safety, efficacy
and quality of the product must be submitted for review by regulatory authorities. Dossier form and substance, while often
similar may have notable differences in different countries. Submission of an application to regulators does not guarantee
approval to market that product, despite the fact that criteria for approval in many countries may be quite similar. Some
regulatory authorities may require additional data and analyses, and may have standards that apply that are more stringent
than others for review of the submitted dossier and content. Additionally, the review process, risk tolerance, and openness
to new technologies may vary from country to country.
Obtaining marketing approval can take several months to several years, depending on the country, the quality of
the data, the efficiencies and procedures of the reviewing regulatory authority and their familiarity with the product
technology. Some countries, like the US, may have accelerated approval processes for certain categories of products, for
example products which represent a breakthrough in the field, or which meet certain thresholds and have obtained certain
designations of particular interest. Nevertheless, ultimate availability to patients may be affected, even post approval, by
requirements in some countries to negotiate selling prices and reimbursement terms with government regulators or other
payors.
Maintaining marketing approval may require the conduct of additional post-approval studies in some situations,
and the continued capture, monitoring and assessment of safety and other information about the product, as well as
adherence to requirements to ensure the purity and integrity of manufactured product. The process for obtaining and
maintaining regulatory authorizations and approvals to market our products and the subsequent compliance with
appropriate federal, state, local and foreign laws and regulations require the expenditure of substantial time and the
commitment of significant financial and other resources, and we may not be able to obtain the required regulatory
approvals.
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Product Development Process
All of our product candidates are regulated as biological products by the Center for Biologics Evaluation and
Research in the FDA. In the United States, biological products are subject to federal regulation under the Federal Food,
Drug, and Cosmetic Act (“FDCA”), the Public Health Service (“PHS”) Act, and other federal, state, local and foreign
statutes and regulations. Both the FDCA and the PHS Act, as applicable, and their corresponding regulations govern,
among other things, the testing, manufacturing, safety, efficacy, labeling, packaging, storage, record keeping, distribution,
import, export, reporting, advertising and other promotional practices involving drugs and biological products. Before
clinical testing of a new drug or biological product may commence, the sponsor of the clinical study must submit an
application for investigational new drug (“IND”) application to FDA, which must include, among other information, the
proposed clinical study protocol(s). To obtain marketing authorization once clinical testing has concluded, a BLA must be
submitted for FDA approval.
The process required by the FDA before a biological product may be marketed in the U.S. generally involves the
following:
•
completion of nonclinical laboratory studies, meaning in vivo and in vitro experiments in which an
investigational product is studied prospectively in a test system under laboratory conditions to determine
its safety, must be conducted according to cGLP (good laboratory practice) regulations, as well as, in the
case of nonclinical laboratory studies involving animal test systems, in accordance with applicable
requirements for the humane use of laboratory animals and other applicable regulations;
•
submission to the FDA of an application for an IND, which must become effective before human clinical
studies may begin;
•
performance of adequate and well-controlled human clinical studies according to the FDA’s cGCPs
(good clinical practices) and all other applicable regulatory requirements for the protection of human
research subjects and their health information, to establish the safety, purity and potency of the proposed
product for its intended use and to ensure the product has an appropriate risk-benefit profile;
•
development and demonstration of a manufacturing process that can produce product of consistent and
adequate quality;
•
submission to the FDA of a BLA for marketing approval demonstrating the quality, safety, and efficacy
of the product which must be supported by substantial evidence from adequate and well-controlled
clinical investigations as well as demonstration of mode of action through non-clinical studies, evidence
to support appropriate manufacturing capabilities and controls, and evidence of the stability of the
product in the form it is intended to be provided;
•
negotiation with FDA of proposed product labeling (and determination of appropriate risk mitigation
strategies and programs, if any required), as well as participation in any required advisory committee
proceedings;
•
satisfactory completion of an FDA inspection of all manufacturing, testing and distribution facilities
where the product is produced, tested or stored and distributed, to assess compliance with cGMP (good
manufacturing practices) to assure that the facilities, methods and controls for production are adequate to
preserve the product’s identity, strength, purity and potency;
•
potential FDA inspection of nonclinical facilities and likely inspection of select clinical study sites that
generated the data in support of the BLA; and
•
FDA review and approval of the BLA.
Human testing of a biological product candidate is preceded by preclinical testing, including nonclinical
laboratory studies in which the product candidate is studied prospectively in a test system under laboratory conditions to
determine its safety. A test system may include any animal, plant, microorganism, or subparts thereof to which the test or
control article is administered or added for study.
The clinical study sponsor must submit the results of the preclinical tests, together with manufacturing
information, analytical data, any available clinical data or literature and a proposed clinical protocol, to the FDA as part of
the IND. Some preclinical testing may continue even after the IND is submitted. The IND automatically becomes effective
30 days after receipt by the FDA, unless the FDA places the clinical study covered by the IND on a clinical hold within that
30-day time period. In such a case, the IND sponsor and the FDA must resolve any outstanding concerns before the clinical
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study can begin. The FDA may also impose clinical holds on a product candidate at any time during clinical studies due to
safety concerns or non-compliance. If the FDA imposes a clinical hold, studies may not recommence unless FDA removes
the clinical hold and then only under terms authorized by the FDA. Accordingly, we cannot be sure that submission of an
IND will result in the FDA allowing clinical studies to begin, or that, once begun, issues will not arise that suspend or
terminate such studies.
Clinical studies involve the administration of the product candidate to subjects under the supervision of qualified
independent investigators, generally physicians or other qualified scientists and medical personnel who are not employed
by or under the study sponsor’s control. Clinical studies are conducted under protocols detailing, among other things, the
objectives of the clinical study, dosing procedures, subject selection and exclusion criteria, and the parameters to be used to
monitor subject safety, including stopping rules that assure a clinical study will be stopped if certain adverse events, or
AEs, should occur. Each new protocol and certain amendments to the protocol must be submitted to the FDA. Clinical
studies must be conducted in accordance with the FDA’s cGCP regulations and guidance, and monitored to ensure
compliance with applicable regulatory requirements. These include the requirement that written informed consent is
obtained from all subjects who participate in the study. Further, each clinical study must be reviewed and approved by an
independent Institutional Review Board, or IRB, at or servicing each institution at which the clinical study will be
conducted. An IRB is charged with protecting the welfare and rights of study participants and considers such items as
whether the risks to individuals participating in the clinical studies are minimized and are reasonable in relation to
anticipated benefits. The IRB also approves the form and content of the informed consent document that must be signed by
each clinical study subject or his or her legal representative and must monitor the clinical study until completed.
Throughout the study, certain information about certain serious adverse events must be reported to the IRB, in some cases
on an expedited basis, and to FDA (as well as to regulators in other countries in which studies of the product are also being
conducted).
Human clinical studies are typically conducted in three sequential phases that may in some cases overlap or be
combined:
•
Phase 1. The product candidate is initially introduced into a small number of human subjects. In the case
of cellular therapy products, the initial human testing is conducted in patients with the disease or
condition targeted by the biological product candidate. Phase 1 studies are intended to determine the
metabolism and pharmacologic actions (including adverse reactions), the side effects associated with
increasing doses, immunogenicity, and, if possible, to gain early evidence of effectiveness. The
information obtained in Phase 1 should be sufficient to permit the design of well-controlled, scientifically
valid Phase 2 studies.
•
Phase 2. Controlled clinical studies are conducted in a larger number of human subjects to evaluate the
effectiveness of the drug for a particular indication or indications in patients with the disease or condition
under study. Phase 2 studies are intended to assess side effects and risks, and to examine exposure–
response relationships, and to further explore pharmacologic actions and immunogenicity associated with
the drug. These studies also provide helpful information for the design of phase 3 studies.
•
Phase 3. Assuming preliminary evidence suggesting effectiveness has been obtained in phase 2
(generally considered to be “proof of concept”), controlled studies are conducted in a larger group of
subjects to gather additional information about effectiveness and safety in order to evaluate the overall
benefit-risk relationship of the drug and to provide an adequate basis for physician labeling.
Post-approval clinical studies, sometimes referred to as Phase 4 clinical studies, may be conducted after initial
marketing approval. In some cases, FDA may require a Phase 4 study to be performed as a condition of product approval.
Sponsors also can voluntarily conduct Phase 4 studies to gain additional experience from the treatment of patients in the
intended therapeutic indication, particularly for long-term safety follow-up or in select populations. FDA regulations
extend to all phases of clinical development and apply to sponsors and investigators of clinical studies. FDA oversight
includes inspection of the sites and investigators involved in conducting the studies.
Concurrent with clinical studies, companies usually complete additional animal studies, and must also develop
additional information about the physical characteristics of the biological product as well as finalize a process for
manufacturing the product in commercial quantities in accordance with cGMP requirements.
To help reduce the risk of the introduction of adventitious agents with use of biological products, the PHS Act
emphasizes the importance of manufacturing control for products whose attributes cannot be precisely defined. The
manufacturing process must be capable of consistently producing quality batches of the product candidate and, among
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other things; the sponsor must develop methods for testing the identity, purity and potency of the final biological product.
All such testing and controls requires the application of significant human and financial resources.
Additionally, appropriate packaging must be selected and tested and stability studies must be conducted to
demonstrate that the biological product candidate does not undergo unacceptable deterioration over its shelf life.
U.S. Review and Approval Processes
After the completion of clinical studies of a product candidate, FDA approval of a BLA must be obtained before
commercial marketing of the biological product. The BLA must include results of product development, laboratory and
animal studies, human studies, information on the manufacture and composition of the product, proposed labeling and
other relevant information. In addition, under the Pediatric Research Equity Act (“PREA”), a BLA or supplement to a BLA
must contain data to assess the safety and effectiveness of the product for the claimed indications in all relevant pediatric
subpopulations and to support dosing and administration for each pediatric subpopulation for which the product is safe and
effective. The FDA may grant deferrals for submission of data or full or partial waivers. Unless otherwise required by
regulation, PREA does not apply to any biological product for an indication for which orphan designation has been
granted. The testing and approval processes require substantial time and effort and there can be no assurance that the FDA
will accept the BLA for filing and, even if filed, that any approval will be granted on a timely basis, if at all.
Under the Prescription Drug User Fee Act (“PDUFA”), as amended, each BLA must be accompanied by a
substantial user fee. PDUFA also imposes an annual product fee for biologics and an annual establishment fee on facilities
used to manufacture prescription biologics. Fee waivers or reductions are available in certain circumstances, including a
waiver of the application fee for the first application filed by a small business.
Additionally, an application fee is not assessed on BLAs for products designated as orphan drugs, unless the
product also includes a non-orphan indication.
Within 60 days following submission of the application, the FDA reviews the BLA submitted to determine if it is
substantially complete before the agency accepts it for filing. The FDA may refuse to file any marketing application that it
deems incomplete or not properly reviewable at the time of submission and may request additional information. In this
event, the BLA must be resubmitted with the additional information. The resubmitted application also is subject to review
before the FDA accepts it for filing. Once the submission is accepted for filing, the FDA begins an in-depth substantive
review of the BLA. The FDA reviews the application to determine, among other things, whether the proposed product is
safe and effective, for its intended use, and has an acceptable purity profile, and whether the product is being manufactured
in accordance with cGMP to assure and preserve the product’s identity, safety, potency and purity. The FDA may refer
applications for novel products or products that present difficult questions of safety or efficacy to an advisory committee,
typically a panel that includes clinicians and other experts, for review, evaluation and a recommendation as to whether the
application should be approved and under what conditions. The FDA is not bound by the recommendations of an advisory
committee, but it considers such recommendations carefully when making decisions. During the product approval process,
the FDA also will determine whether a Risk Evaluation and Mitigation Strategy, or REMS, is necessary to assure the safe
use of the product. If the FDA concludes a REMS is needed, the sponsor of the BLA must submit a proposed REMS; the
FDA will not approve the application without a REMS, if required.
Before approving a BLA, the FDA will typically inspect the facilities at which the product is manufactured. The
FDA will not approve the product unless it determines that the manufacturing processes and facilities are in compliance
with cGMP requirements and adequate to assure consistent production of the product within required specifications.
Additionally, before approving a BLA, the FDA will typically inspect one or more clinical sites to assure that the clinical
studies were conducted in compliance with IND study and cGCP requirements. To assure cGMP and cGCP compliance, an
applicant must incur significant expenditure of time, money and effort in the areas of training, record keeping, production,
and quality control.
Notwithstanding the submission of relevant data and information, the FDA may ultimately decide that the BLA
does not satisfy its regulatory criteria for approval and deny approval. Data obtained from clinical studies are not always
conclusive and the FDA may interpret data differently than we interpret the same data. If the agency decides not to approve
the marketing application, it will issue a complete response letter describing specific deficiencies in the application
identified by the FDA. Additionally, the complete response letter may recommend actions that the applicant might take to
place the application in a condition for approval. Such recommended actions could include the conduct of additional
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studies. If a complete response letter is issued, the applicant may either resubmit the BLA, addressing all of the deficiencies
identified in the letter, or withdraw the application.
If a product receives regulatory approval, the approval may be significantly limited to specific diseases and
dosages or the indications for use may otherwise be limited, which could restrict the commercial value of the product.
Further, the FDA may require that certain contraindications, warnings or precautions be included in the product labeling.
The FDA may impose restrictions and conditions on product distribution, prescribing, or dispensing in the form of a risk
management plan, or otherwise limit the scope of any approval. In addition, the FDA may require post-approval clinical
studies, to further assess a product’s safety and effectiveness, and testing and surveillance programs to monitor the safety
of approved products that have been commercialized.
One of the performance goals agreed to by the FDA under the PDUFA is to complete its review of 90% of
standard BLAs within 10 months from filing and 90% of priority BLAs within six months from filing, whereupon a review
decision is to be made. The FDA does not always meet its PDUFA goal dates and its review goals are subject to change
from time to time. The review process and the PDUFA goal date may be extended by three months if the FDA requests or
the application sponsor otherwise provides additional information or clarification regarding information already provided
in the submission within the last three months before the PDUFA goal date.
Post-Approval Requirements
Maintaining substantial compliance with applicable federal, state, and local statutes and regulations requires the
expenditure of substantial time and the commitment of substantial human and financial resources. Rigorous and extensive
FDA regulation of biological products continues after approval, particularly with respect to cGMP. We will rely, and
expect to continue to rely, on third parties for the production of clinical and commercial quantities of any products that we
may commercialize. Manufacturers of our products are required to comply with applicable requirements in the cGMP
regulations, including quality control and quality assurance and maintenance of records and documentation.
Other post-approval requirements applicable to drug and biological products include reporting post marketing
surveillance to continuously monitor the safety of the approved product. This is done through the collection of spontaneous
reports of adverse events and side effects, the assessment of safety signals, if any, and prescription event monitoring,
among other methods. FDA maintains a system of postmarketing surveillance because all possible side effects of a new
drug may not be evident in preapproval studies, which involve only several hundred to several thousand patients. Through
postmarketing surveillance and risk assessment programs, FDA and sponsors seek to identify adverse events that did not
appear during the drug approval process. In addition, FDA monitors adverse events such as adverse reactions and
poisonings. FDA may use this information for a variety of purposes to identify safety signals not previously identified with
the product, to update drug labeling, and, on rare occasions, to reevaluate the approval or marketing decision with respect
to a product.
In addition, post-approval regulatory requirements include reporting of cGMP deviations that may affect the
identity, potency, purity and overall safety of a distributed product, record-keeping requirements, and complying with
electronic record and signature requirements. After a BLA is approved, the product also may be subject to official lot
release. As part of the manufacturing process, the manufacturer is required to perform certain tests on each lot of the
product before it is released for distribution. If the product is subject to official release by the FDA, the manufacturer
submits samples of each lot of product to the FDA together with a release protocol showing a summary of the history of
manufacture of the lot and the results of all of the manufacturer’s tests performed on the lot. The FDA also may perform
certain confirmatory tests on lots of some products before releasing the lots for distribution by the manufacturer. In
addition, the FDA conducts laboratory research related to the regulatory standards on the safety, purity, potency, and
effectiveness of drug and biological products. The FDA will also conduct routine scheduled and unannounced inspections
of drug production and control facilities and processes, using field investigators and analysts, to assure ongoing safety and
effectiveness of approved marketed products. Inspections may be made in conjunction with regulators from other
jurisdictions and in certain cases, inspection findings and observations may be made public or may impair our ability to use
the inspected facility, or to continue to produce and market a product.
We also must comply with the FDA’s advertising and promotion requirements, such as those related to direct- to-
consumer advertising, the prohibition on promoting products for uses or in patient populations that are not described in the
product’s approved labeling (known as “off-label use”), industry-sponsored scientific and educational activities, and
promotional activities involving the internet and notably, social media. In addition, discovery of previously unknown
problems or the failure to comply with the applicable regulatory requirements may result in restrictions on the marketing of
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a product or withdrawal of the product from the market as well as possible civil or criminal sanctions. Failure to comply
with the applicable U.S. requirements at any time during the product development process, approval process or after
approval, may subject an applicant or manufacturer to administrative or judicial civil or criminal sanctions and adverse
publicity. Sanctions authorized under FDA’s legal authorities could include refusal to approve pending applications,
withdrawal of an approval, clinical hold, warning or untitled letters, product recalls, product seizures, total or partial
suspension of production or distribution, injunctions, fines, mandated corrective advertising or communications with
doctors, debarment, restitution, disgorgement of profits, or civil or criminal penalties.
Violations of the FDCA may serve as a basis for the refusal of, or exclusion from, government contracts,
including federal reimbursement programs, as well as other adverse consequences including lawsuits and actions by state
attorneys general. Any agency or judicial enforcement action could have a material adverse effect on us. Drug and
biological product manufacturers and other entities involved in the manufacture and distribution of approved drug or
biological products are required to register their establishments with the FDA and certain state agencies, and are subject to
periodic unannounced inspections by the FDA and certain state agencies for compliance with cGMPs and other laws.
Accordingly, manufacturers must continue to expend time, money, and effort in the area of production and quality control
to maintain cGMP compliance. Discovery of problems with a product after approval may result in restrictions on a product,
manufacturer, or holder of an approved BLA, including withdrawal of the product from the market. In addition, changes to
a manufacturing process or facility generally require prior FDA approval before being implemented and other types of
changes to the approved product, such as adding new indications and additional labeling claims, are also subject to further
FDA review and approval.
U.S. Patent Term Restoration and Marketing Exclusivity
Depending upon the timing, duration and specifics of the FDA approval of the use of our product candidates,
some of our U.S. patents may be eligible for limited patent term extension under the Drug Price Competition and Patent
Term Restoration Act of 1984, commonly referred to as the Hatch-Waxman Amendments. The Hatch-Waxman
Amendments permit a patent restoration term of up to five years as compensation for patent term lost during product
development and the FDA regulatory review process. However, patent term restoration cannot extend the remaining term
of a patent beyond a total of 14 years from the product’s approval date. The patent term restoration period is generally one-
half the time between the effective date of an IND and the submission date of a new drug application, or NDA, or BLA
plus the time between the submission date of an NDA or BLA and the approval of that application. Only one patent
applicable to an approved product can be extended and the application for the extension must be submitted prior to the
expiration of the patent. The U.S. Patent and Trademark Office, in consultation with the FDA, reviews and approves the
application for any patent term extension or restoration.
A drug or biological product can obtain pediatric market exclusivity in the U.S. Pediatric exclusivity, if granted,
adds six months to existing exclusivity periods and patent terms. This six-month exclusivity, which runs from the end of
other exclusivity protection or patent term, may be granted based on the voluntary completion of a pediatric study in
accordance with an FDA-issued “Written Request” for such a study.
The Biologics Price Competition and Innovation Act of 2009 created an abbreviated approval pathway for
biological products shown to be similar to, or interchangeable with, an FDA-licensed reference biological product.
Biosimilarity, which requires that there be no clinically meaningful differences between the biological product and the
reference product in terms of safety, purity, and potency, can be shown through analytical studies, animal studies, and a
clinical study or studies. Interchangeability requires that a product is biosimilar to the reference product and the product
must demonstrate that it can be expected to produce the same clinical results as the reference product and, for products
administered multiple times, the biologic and the reference biologic may be switched after one has been previously
administered without increasing safety risks or risks of diminished efficacy relative to exclusive use of the reference
biologic.
A new biologic is granted 12 years of exclusivity from the time of first licensure during which a biosimilar may
not be launched.
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Government Regulation Outside of the U.S.
European Union Regulation
In addition to regulations in the U.S., we will be subject to a variety of regulations in other jurisdictions
governing, among other things, clinical studies and any commercial sales and distribution of our products. In particular, we
view the EU and Japan as important jurisdictions for our business.
For purposes of developing our products, we must obtain the requisite approvals from regulatory authorities in
each country prior to the commencement of clinical studies or marketing of the product in those countries. Certain
countries outside of the U.S. have a similar process that requires the submission of a clinical study application much like
the IND prior to the commencement of human clinical studies. In the EU, for example, a clinical trial application (“CTA”),
must be submitted to each country’s national health authority and an independent ethics committee, much like the FDA and
the IRB, respectively. Once the CTA is approved in accordance with a country’s requirements, clinical study development
may proceed.
The EU has two main procedures for obtaining marketing authorizations in the EU Member States: a centralized
procedure or national authorization procedure, under the latter of which one can seek to go through the mutual recognition
procedure or the decentralized procedure. All biotechnology products are assessed through the centralized procedure.
Under the centralized authorization procedure, sponsors submit a single marketing-authorization application to the
EMA. This allows the marketing-authorization holder to market the product and make it available to patients and
healthcare professionals throughout the EU on the basis of a single marketing authorization. EMA's Committee for
Medicinal products for Human Use (“CHMP”) carries out a scientific assessment of the application and give a
recommendation on whether the medicine should be marketed or not. Once granted by the EMA, the centralized marketing
authorization is valid in all EU Member States as well as in the European Economic Area countries Iceland, Liechtenstein
and Norway. The centralized procedure is mandatory for biotechnology products.
Any product candidates we seek to commercialize in the EU are subject to review and approval by the European
Medicines Authority (“EMA”). Submissions for marketing authorization to the EMA must be received and validated by
that body which appoints a Rapporteur and Co-Rapporteur to review it. The entire review process must be completed
within 210 days, with a “clock-stop” at day 120 to allow the submitting company to respond to questions set forth in the
Rapporteur and Co-Rapporteur’s assessment report. Once the company responds in full, the clock for review re-starts on
day 121. If further clarification is needed, the EMA may request an Oral Explanation on day 180, and the company
submitting the application must appear before the CHMP to provide the requested information. On day 210, the CHMP
will vote to recommend for or against the approval of the application. The final decision of EMA for marketing
authorization following a positive CHMP recommendation is typically made within 60 days, with a draft decision within
15 days of the CHMP recommendation.
After Marketing Authorizations have been granted, the company must submit periodic safety reports to the EMA
(if approval was granted under the Centralized Procedure) or to the National Health Authorities (if approval was granted
under the DCP or the MRP). In addition, pharmacovigilance measures must be implemented and monitored to ensure
appropriate adverse event collection, evaluation and expedited reporting, as well as timely updates to any applicable risk
management plans. For some medications, post approval studies may be required to complement available data with
additional data to evaluate long term effects or to gather additional efficacy data.
European marketing authorizations have an initial duration of five years. After this time, the marketing
authorization may be renewed by the competent authority on the basis of re-evaluation of the risk/benefit balance. Any
marketing authorization which is not followed within three years of its granting by the actual placing on the market of the
corresponding medicinal product ceases to be valid.
United Kingdom (post BREXIT)
Marketing Authorization in the United Kingdom no longer falls under the EMA centralized process, and requires
compliance to local laws and regulations, with a separate application required either concurrently or sequentially with the
centralized procedure.
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EU Exclusivity Periods
To obtain regulatory approval of an investigational biological product under EU regulatory systems, we must
submit a marketing authorization application. The application used to file the BLA in the U.S. is similar to that required in
the EU, with the exception of, among other things, country-specific document requirements. The EU also provides
opportunities for market exclusivity. For example, in the EU, upon receiving marketing authorization, new chemical
entities generally receive eight years of data exclusivity and an additional two years of market exclusivity. If granted, data
exclusivity prevents regulatory authorities in the EU from referencing the innovator’s data to assess a generic application.
During the additional two-year period of market exclusivity, a generic marketing authorization can be submitted, and the
innovator’s data may be referenced, but no generic product can be marketed until the expiration of the market exclusivity.
However, there is no guarantee that a product will be considered by the EU’s regulatory authorities to be a new chemical
entity, and products may not qualify for data exclusivity. Products receiving orphan designation in the EU can receive 10
years of market exclusivity, during which time no similar medicinal product for the same indication may be placed on the
market. An orphan product can also obtain an additional two years of market exclusivity in the EU for pediatric studies. No
extension to any supplementary protection certificate can be granted on the basis of pediatric studies for orphan indications.
The criteria for designating an “orphan medicinal product” in the EU are similar in principle to those in the U.S.
Under Article 3 of Regulation (EC) 141/2000, a medicinal product may be designated as orphan if (1) it is intended for the
diagnosis, prevention or treatment of a life-threatening or chronically debilitating condition; (2) either (a) such condition
affects no more than five in 10,000 persons in the EU when the application is made, or (b) the product, without the benefits
derived from orphan status, would not generate sufficient return in the EU to justify investment; and (3) there exists no
satisfactory method of diagnosis, prevention or treatment of such condition authorized for marketing in the EU, or if such a
method exists, the product will be of significant benefit to those affected by the condition, as defined in Regulation (EC)
847/2000. Orphan medicinal products are eligible for financial incentives such as reduction of fees or fee waivers and are,
upon grant of a marketing authorization, entitled to 10 years of market exclusivity for the approved therapeutic indication.
The application for orphan drug designation must be submitted before the application for marketing authorization. The
applicant will receive a fee reduction for the marketing authorization application if the orphan drug designation has been
granted, but not if the designation is still pending at the time the marketing authorization is submitted. Orphan drug
designation does not convey any advantage in, or shorten the duration of, the regulatory review and approval process.
The 10-year market exclusivity may be reduced to six years if, at the end of the fifth year, it is established that the
product no longer meets the criteria for orphan designation, for example, if the product is sufficiently profitable not to
justify maintenance of market exclusivity. Additionally, marketing authorization may be granted to a similar product for
the same indication at any time if:
•
the second applicant can establish that its product, although similar, is safer, more effective or otherwise
clinically superior;
•
the applicant consents to a second orphan medicinal product application; or
•
the applicant cannot supply enough orphan medicinal product.
In addition to law and regulation specific to drug development, we note that new data protection regulations that
have gone into effect in Europe are likely to have a significant impact on our activities, personnel, and may have an impact
on our ability to timely complete clinical trials and effectively develop and commercialize our product candidates. The
General Data Protection Regulation (the “GDPR”) was approved and adopted by the EU Parliament in April 2016 and
went into effect on May 25, 2018. Unlike a Directive, the GDPR does not require any enabling legislation to be passed by
any government. The GDPR not only applies to organizations located within the EU but may also apply to organizations
located outside of the EU if they offer goods or services to, or monitor the behavior of, EU data subjects or if they process
the personal data of subjects residing in the European Union. The implications of this regulation are therefore far reaching
and may impose significant burdens on the Company and its processes and systems. Additionally, the UK government has
implemented data protection legislation, which also went into effect on May 25, 2018, that substantially implements the
GDPR. For other countries outside of the EU, such as countries in Eastern Europe, Latin America or Asia, the requirements
governing the conduct of clinical studies, product licensing, coverage, pricing and reimbursement vary from country to
country. In all cases, again, the clinical studies are conducted in accordance with cGCP and the applicable regulatory
requirements and the ethical principles that have their origin in the Declaration of Helsinki.
If we fail to comply with applicable foreign regulatory requirements, we may be subject to, among other things,
fines, suspension or withdrawal of regulatory approvals, product recalls, seizure of products, operating restrictions and
criminal prosecution.
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Pharmaceutical Coverage, Pricing and Reimbursement
Significant uncertainty exists as to the coverage and reimbursement status of any product candidates for which we
obtain regulatory approval. In the U.S. and markets in other countries, sales of any products for which we receive
regulatory approval for commercial sale will depend, in part, on the availability of coverage and adequate reimbursement
from third-party payors. Third-party payors include government programs such as Medicare or Medicaid, managed care
plans, private health insurers, and other organizations. These third-party payors may deny coverage or reimbursement for a
product or therapy in whole or in part if they determine that the product or therapy was not medically appropriate or
necessary or if another less expensive potential alternative exists. Third-party payors may attempt to control costs by
limiting coverage to specific drug products on an approved list, or formulary, which might not include all of the FDA-
approved drug products for a particular indication, and by limiting the amount of reimbursement for particular procedures
or drug treatments. In addition, in the United States, participation in government health programs such as Medicare and
Medicaid are subject to complex rules and controls relating to price reporting and calculation of prices to ensure that
pricing provided to government entities for periodic reporting purposes is aligned and compliant with numerous complex
statutory requirements and the lowest possible price is the one used by government programs. The infrastructure and/or
external resources necessary to ensure continued compliance with these requirements is extensive and manufacturers are
subject to audit both by the Centers for Medicare and Medicaid Services and by State Medicaid authorities.
The cost of pharmaceuticals and devices continues to generate substantial governmental and third-party payor
interest. We expect that the pharmaceutical industry will experience pricing pressures due to the trend toward managed
healthcare, the increasing influence of managed care organizations and additional legislative proposals. Third-party payors
are increasingly challenging the price and examining the medical necessity and cost-effectiveness of medical products and
services, in addition to their safety and efficacy. We may need to conduct expensive pharmacoeconomic studies in order to
demonstrate the medical necessity and cost-effectiveness of our products, in addition to the costs required to obtain the
FDA approvals. More recently in the US and for certain high-cost rare disease drugs, payors have negotiated a provision
that requires manufactures to refund the cost of the treatment if patients discontinue the drug for clinical reasons. Our
product candidates may not be considered medically necessary or cost-effective. A payor’s decision to provide coverage
for a drug product does not imply that an adequate reimbursement rate will be approved. Adequate third-party
reimbursement may not be available to enable us to maintain price levels sufficient to realize an appropriate return on our
investment in product development.
Some third-party payors also require pre-approval of coverage for new or innovative devices or drug therapies
before they will reimburse healthcare providers who use such therapies. While we cannot predict whether any proposed
cost-containment measures will be adopted or otherwise implemented in the future, these requirements or any
announcement or adoption of such proposals could have a material adverse effect on our ability to obtain adequate prices
for our product candidates and to operate profitably.
In international markets, reimbursement and healthcare payment systems vary significantly by country, and many
countries have instituted price ceilings (or mandatory price decreases) on specific products and therapies. There can be no
assurance that our products will be considered medically reasonable and necessary for a specific indication, that our
products will be considered cost-effective by third-party payors, that coverage or an adequate level of reimbursement will
be available or that the third-party payors reimbursement policies will not adversely affect our ability to sell our product
profitably.
Healthcare Reform
In the U.S. and foreign jurisdictions, there have been a number of legislative and regulatory changes to the
healthcare system that could affect our future results of operations. In particular, there have been and continue to be a
number of initiatives at the U.S. federal and state levels that seek to reduce healthcare costs. In the U.S., the Medicare
Prescription Drug, Improvement, and Modernization Act of 2003, or the Medicare Modernization Act, changed the way
Medicare covers and pays for pharmaceutical products. The Medicare Modernization Act expanded Medicare coverage for
drug purchases by the elderly by establishing Medicare Part D and introduced a new reimbursement methodology based on
average sales prices for physician administered drugs under Medicare Part B. In addition, this legislation provided authority
for limiting the number of drugs that will be covered in any therapeutic class under the new Medicare Part D program. Cost
reduction initiatives and other provisions of this legislation could decrease the coverage and reimbursement rate that we
receive for any of our approved products. While the Medicare Modernization Act applies only to drug benefits for
Medicare beneficiaries, private payors often follow Medicare coverage policy and payment limitations in setting their own
reimbursement rates.
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Therefore, any reduction in reimbursement that results from the Medicare Modernization Act may result in a
similar reduction in payments from private payors.
In March 2010, the Affordable Care Act (“ACA”) came into effect, a sweeping law intended to broaden access to
health insurance, reduce or constrain the growth of healthcare spending, enhance remedies against healthcare fraud and
abuse, add new transparency requirements for healthcare and health insurance industries, impose new taxes and fees on
pharmaceutical and medical device manufacturers and impose additional health policy reforms. We expect that the rebates,
discounts, taxes and other costs resulting from the ACA over time will have a negative effect on our expenses and
profitability in the future. Furthermore, expanded government investigative authority and increased disclosure obligations
may increase the cost of compliance with new regulations and programs.
The current presidential administration and Congress are also expected to continue recent attempts to make
changes to the current health care laws and regulations. The impact of those changes on us and potential effect on the
pharmaceutical industry as a whole is currently unknown. But, any changes to the health care laws or regulations,
especially to Medicare drug reimbursement, are likely to have an impact on our results of operations and may have a
material adverse effect on our results of operations. We cannot predict what other health care programs and regulations will
ultimately be implemented at the federal or state level or the effect of any future legislation or regulation in the United
States may have on our business.
It is possible that healthcare reform measures that have been and may be adopted in the future, may result in more
rigorous coverage criteria and in additional downward pressure on the price that we receive for any approved product, and
could seriously harm our future revenue. Any reduction in reimbursement from Medicare or other government programs
may result in a similar reduction in payments from private payors, and formulary restrictions among private payors
including the largest pharmacy benefit managers have increased over recent months, especially as regards to new and high
cost market entrants. The implementation of cost containment measures or other healthcare reforms may prevent us from
being able to generate revenue, attain profitability, or commercialize our products.
In addition, different pricing and reimbursement schemes exist in other countries. In the European Community,
governments influence the price of pharmaceutical products through their pricing and reimbursement rules and control of
national healthcare systems that fund a large part of the cost of those products to consumers. Some jurisdictions operate
positive and negative list systems under which products may be marketed only once a reimbursement price has been agreed
upon. Some of these countries may require, as condition of obtaining reimbursement or pricing approval, the completion of
clinical trials that compare the cost- effectiveness of a particular product candidate to currently available therapies. Other
member states allow companies to fix their own prices for medicines but monitor and control company profits. The
downward pressure on healthcare costs in general, particularly prescription drugs, has become very intense. As a result,
increasingly high barriers are being erected to the entry of new products. In addition, in some countries, cross- border
imports from low-priced markets exert a commercial pressure on pricing within a country.
Other Healthcare Laws and Compliance Requirements
In the U.S., the research, manufacturing, distribution, sale and promotion of drug products, including biologics,
and medical devices are potentially subject to regulation by various federal, state and local authorities in addition to the
FDA, divisions of the U.S. Department of Health and Human Services, including the Office of Inspector General and the
Centers for Medicare and Medicaid Services, the U.S. Department of Justice, state Attorneys General, and other state and
local government agencies. For example, sales, marketing and scientific/educational grant programs must comply with
fraud and abuse laws such as the federal Anti-Kickback Statute, as amended, the federal False Claims Act, as amended, and
similar state laws. Pricing and rebate programs must comply with the Medicaid Drug Rebate Program requirements of the
Omnibus Budget Reconciliation Act of 1990, as amended, and the Veterans Health Care Act of 1992, as amended. If
products are made available to authorized users of the Federal Supply Schedule of the General Services Administration,
additional laws and requirements apply. All of these activities are also potentially subject to federal and state consumer
protection and unfair competition laws.
The federal Anti-Kickback Statute prohibits any person, including a prescription drug manufacturer (or a party
acting on its behalf), from knowingly and willfully soliciting, receiving, offering or providing remuneration, directly or
indirectly, to induce or reward either the referral of an individual, or the furnishing, recommending, or arranging for a good
or service, for which payment may be made under a federal healthcare program such as the Medicare and Medicaid
programs. This statute has been interpreted to apply to arrangements between pharmaceutical manufacturers on one hand
and prescribers, purchasers, and formulary managers on the other. The term “remuneration” has been broadly interpreted to
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include anything of value, including for example, gifts, discounts, the furnishing of supplies or equipment, credit
arrangements, payments of cash, waivers of payments, ownership interests and providing anything at less than its fair
market value. Even the award of grant moneys, or the provision of in kind support, publicity and even authorship, in certain
cases, may be deemed to be “remuneration.” Although there are a number of statutory exceptions and regulatory safe
harbors protecting certain business arrangements from prosecution, the exception and safe harbors are drawn narrowly, and
practices that involve remuneration intended to induce prescribing, purchasing or recommending may be subject to scrutiny
if they do not qualify for an exception or safe harbor. Our practices may not in all cases meet all of the criteria for safe
harbor protection from federal Anti-Kickback Statute liability. The reach of the Anti-Kickback Statute was broadened by
the ACA, so that the government need no longer prove, for purposes of establishing intent under the federal Anti-Kickback
Statute, that a person or entity had actual knowledge of the statute or specific intent to violate it. In addition, the ACA
provides that a violation of the federal Anti-Kickback Statute constitutes a false or fraudulent claim for purposes of the
federal False Claims Act (discussed below). Additionally, many states have adopted laws similar to the federal Anti-
Kickback Statute, and some of these state prohibitions apply to the referral of patients for healthcare items or services
reimbursed by any third-party payor, including private payors. In at least some cases, these state laws do not contain safe
harbors.
The federal False Claims Act imposes liability on any person or entity that, among other things, knowingly
presents, or causes to be presented, a false or fraudulent claim for payment by a federal healthcare program. The qui tam
provisions of the False Claims Act allow a private individual to bring civil actions on behalf of the federal government and
share in any recovery. In recent years, the number of suits brought by private individuals has increased dramatically. In
addition, various states have enacted false claims laws analogous to the False Claims Act. Many of these state laws apply
where a claim is submitted to any third-party payor and not merely a federal healthcare program. There are many potential
bases for liability under the False Claims Act. Liability arises, primarily, when an entity knowingly submits, or causes
another to submit, a false claim for reimbursement to the federal government. The False Claims Act has been used to assert
liability on the basis of inadequate care, kickbacks and other improper referrals, improperly reported government pricing
metrics such as Best Price or Average Manufacturer Price, improper use of Medicare numbers when detailing the provider
of services, improper promotion of off-label uses (i.e., uses not expressly approved by FDA in a drug’s label), and
allegations as to misrepresentations with respect to the services rendered.
Substantial resources have been allocated by both the Department of Justice and the Federal Bureau of
Investigation, among other branches of the US government to identify and investigate possible health care fraud activities.
Recent investigations include those relating to allegedly egregious price increases by manufacturers and alleged fraud
involving co-pay arrangements supported by sponsors. As new theories of liability arise, there is a corresponding cost of
doing business in order to maintain compliance.
Our future activities relating to the reporting of discount and rebate information and other information affecting
federal, provincial, state and third party reimbursement of our products, and the sale and marketing of our products and our
service arrangements or data purchases, among other activities, may be subject to scrutiny under these laws. We are unable
to predict whether we would be subject to actions under the False Claims Act or a similar state law, or the impact of such
actions. However, the cost of defending such claims, as well as any sanctions imposed, could adversely affect our financial
performance. Also, the Health Insurance Portability and Accountability Act of 1996 (“HIPAA”), created several new
federal crimes including healthcare fraud and false statements relating to healthcare matters. The healthcare fraud provision
of HIPAA prohibits knowingly and willfully executing a scheme to defraud any healthcare benefit program, including
private third-party payors. The false statements provision prohibits knowingly and willfully falsifying, concealing or
covering up a material fact or making any materially false, fictitious or fraudulent statement in connection with the delivery
of or payment for healthcare benefits, items or services.
In addition, we may be subject to, or our marketing activities may be limited by, data privacy and security
regulation by both the federal government and the states in which we conduct our business. For example, HIPAA and its
implementing regulations established uniform federal standards for certain “covered entities” (healthcare providers, health
plans and healthcare clearinghouses) governing the conduct of certain electronic healthcare transactions and protecting the
security and privacy of protected health information. The American Recovery and Reinvestment Act of 2009, commonly
referred to as the economic stimulus package, included expansion of HIPAA’s privacy and security standards called the
Health Information Technology for Economic and Clinical Health Act (“HITECH”), which became effective on February
17, 2010. Among other things, HITECH makes HIPAA’s privacy and security standards directly applicable to “business
associates”—independent contractors or agents of covered entities that create, receive, maintain, or transmit protected
health information in connection with providing a service for or on behalf of a covered entity. HITECH also increased the
civil and criminal penalties that may be imposed against covered entities, business associates and possibly other persons,
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and gave state attorneys general new authority to file civil actions for damages or injunctions in federal courts to enforce
the federal HIPAA laws and seek attorney’s fees and costs associated with pursuing federal civil actions.
There are also an increasing number of state “sunshine” laws that require manufacturers to make reports to states
on pricing and marketing information, as well as regarding payments to healthcare professionals. Several states have
enacted legislation requiring pharmaceutical companies to, among other things, establish marketing compliance programs,
file periodic reports with the state, make periodic public disclosures on sales, marketing, pricing, clinical trials and other
activities, and/or register their sales representatives, as well as to prohibit certain other sales and marketing practices. State
laws are not harmonized and contain different reporting requirements and restrictions which must be noted and adhered to.
We currently do not report under these state laws, but will be required to do if we are successful in obtaining marketing
authorization for our products. We will need to develop the infrastructure or rely on third party contractors to assist us in
our compliance with these laws, and failure to comply may result in financial and other penalties and consequences. In
addition, beginning in 2013, a similar “sunshine” federal requirement began requiring manufacturers to track and report to
the federal government certain payments and other transfers of value made to certain covered recipients, including
physicians and other healthcare professionals, and teaching hospitals. In addition to payments, reporting may encompass
requirements to report on ownership or investment interests held by physicians and their immediate family members. The
efforts and resources needed to track and report payments go well beyond our affiliates operating in the United States, as
reporting is required also for payments made by affiliated entities in many cases to US covered recipients. In other
jurisdictions (eg, Australia, Japan and Europe) similar “sunshine-like” laws have also been adopted, which may require
disclosure of certain payment and other information to covered recipients. Extensive administration and systems, including
to aggregate and categorize spend, are necessary in order to enable compliant and timely reporting under these
requirements. The US federal government began disclosing the reported information on a publicly available website in
2014. These laws may affect our development, sales, marketing, and other promotional activities by imposing
administrative and compliance burdens on us. If we fail to track and report as required by these laws or otherwise fail to
comply with these laws, we could be subject to the penalty and sanctions of the pertinent state and federal authorities.
Because of the breadth of these laws and the narrowness of available statutory and regulatory exemptions, it is
possible that some of our business activities could be subject to challenge under one or more of such laws. If our operations
are found to be in violation of any of the federal and state laws described above or any other governmental regulations that
apply to us, we may be subject to penalties, including criminal and significant civil monetary penalties, damages, fines,
imprisonment, exclusion from participation in government healthcare programs, injunctions, recall or seizure of products,
total or partial suspension of production, denial or withdrawal of premarketing product approvals, private qui tam actions
brought by individual whistleblowers in the name of the government or refusal to allow us to enter into supply contracts,
including government contracts, and the curtailment or restructuring of our operations, any of which could adversely affect
our ability to operate our business and our results of operations. To the extent that any of our products are sold in a foreign
country, we may be subject to similar foreign laws and regulations, which may include, for instance, applicable post-
approval requirements, including safety surveillance, anti-fraud and abuse laws, implementation of corporate compliance
programs and reporting of payments or transfers of value to healthcare professionals.
Australian Disclosure Requirements
Business Strategies and Prospects for Future Years
We are focused on the following core strategic imperatives:
•
continue to innovate and optimize our disruptive technology platform for cell-based therapeutics;
•
develop a portfolio of clinically distinct products;
•
focus on bringing late-stage products to market and portfolio prioritization;
•
enabling manufacturing scale-up to meet demands of the portfolio;
•
leverage talent base to continue to establish a culture of shared leadership and accountability;
•
focus on strategic partnerships;
•
focus on prudent cash management; and
•
continue to strengthen our substantial and robust intellectual property estate.
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Dividends
No dividends were paid during the course of the fiscal year ended June 30, 2024. There are no dividends or
distributions recommended or declared for payment to members, but not yet paid, during the year.
4.C
Organizational Structure
See “Item 4. Information on the Company – 4.B Business Overview – Overview”, “Item 18. Financial Statements
– Note 12” and Exhibit 8.1 to this Annual Report.
4.D
Property, Plants and Equipment
We lease approximately 11,150 square feet of office space in Melbourne, Australia, where our headquarters are
located. We pay approximately A$1,100,000 per year for this lease, which expires in April 2026. We have sub-leased
approximately 5,400 square feet of this space and we receive approximately A$360,000 per year for this sub-lease, which
expires in April 2026. We also lease approximately 15,600 square feet in New York City, where significant development
and pre-commercial activities are conducted. We pay approximately $1,000,000 per year for this lease, which expires in
September 2024. We also lease laboratory and office space in Singapore. We pay approximately S$270,000 per year for
this lease, which expires in September 2025. We also lease laboratory space in Texas and pay approximately $320,000 per
year for this lease, which expires in December 2026. Our manufacturing operations are primarily located at Lonza’s
manufacturing facilities. See “Item 4.B Business Overview – Manufacturing and Supply Chain.”
Item 4A.
Unresolved Staff Comments
Not applicable.
Item 5. Operating and Financial Review and Prospects
5.A
Operating Results
This operating and financial review should be read together with our consolidated financial statements in this
Annual Report, which have been prepared in accordance with IFRS as published by the IASB.
Financial Overview
We have incurred significant losses since our inception. We have incurred net losses during most of our fiscal
periods since our inception. As at June 30, 2024, we had an accumulated deficit of $908.8 million. Our net loss for the year
ended June 30, 2024 was $88.0 million.
We anticipate that we may continue to incur significant losses for the foreseeable future. There can be no assurance
that we will ever achieve or maintain profitability.
We expect our future capital requirements will continue as we:
•
continue the research and clinical development of our product candidates;
•
initiate and advance our product candidates into larger clinical studies;
•
seek to commercialize remestemcel-L for pediatric steroid refractory acute graft versus host disease ("SR-
aGVHD") in the United States in the event that we receive marketing authorization by the United States Food
and Drug Administration ("FDA");
•
seek to identify, assess, acquire, and/or develop other product candidates and technologies;
•
seek regulatory and marketing approvals in multiple jurisdictions for our product candidates that successfully
complete clinical studies;
•
establish collaborations with third parties for the development and commercialization of our product
candidates, or otherwise build and maintain a sales, marketing, and distribution infrastructure to
commercialize any products for which we may obtain marketing approval;
•
further develop and implement our proprietary manufacturing processes and expand our manufacturing
capabilities and resources for commercial production;
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•
seek coverage and reimbursement from third-party payors, including government and private payors for
future products;
•
make interest payments, principal repayments and other charges on our debt financing arrangements;
•
make milestone or other payments under our agreements pursuant to which we have licensed or acquired
rights to intellectual property and technology;
•
seek to maintain, protect, and expand our intellectual property portfolio; and
•
seek to attract and retain skilled personnel.
Subject to us achieving successful regulatory approval, we expect an increase in our total expenses driven by an
increase in our planned research and development, manufacturing commercialization and selling, general and
administrative expenses as we move towards commercialization. Therefore, we will need additional capital to fund our
operations, which we may raise through equity offerings, debt financings, other third-party funding, marketing and
distribution arrangements and other collaborations, strategic alliances and licensing arrangements. We do not know when,
or if, we will generate revenues from our product sales significant enough to generate profits. We do not expect to generate
significant revenue from product sales unless and until we obtain regulatory approval of and commercialize one or more of
our cell-based product candidates. For further discussion on our ability to continue as a going concern, see Note 1(i) in our
accompanying financial statements.
Commercialization and Milestone Revenue. Commercialization and milestone revenue relates to upfront, royalty and
milestone payments recognized under development and commercialization agreements; milestone payments, the receipt of
which is dependent on certain clinical, regulatory or commercial milestones; as well as royalties on product sales of
licensed products, if and when such product sales occur; and revenue from the supply of products. Payment is generally
due on standard terms of 30 to 60 days.
Amounts received prior to satisfying the revenue recognition criteria are recorded as deferred consideration in our
consolidated balance sheet, depending on the nature of the arrangement. Amounts expected to be recognized as revenue
within the 12 months following the consolidated balance sheet date are classified within current liabilities. Amounts not
expected to be recognized as revenue within the 12 months following the consolidated balance sheet date are classified
within non-current liabilities.
Research and Development. Research and development expenditure is recognized as an expense as incurred.
Our research and development expenses consist primarily of:
•
third party costs comprising all external expenditure on our research and development programs such as fees
paid to Contract Research Organizations (“CROs”) and on our pre-commercial activities, such as research
pertaining to market access and pricing, brand marketing and initiation of trade and distribution contracts.
Third party costs also comprise fees paid to consultants who perform research on our behalf and under our
direction, rent and utility costs for our research and development facilities, and database analysis fees;
•
third party costs under license and/or sub-license arrangements for the research and development, license,
manufacture and/or commercialization of products and/or product candidates, such as payments for options to
acquire rights to products and product candidates as well as contingent obligations under the agreements;
•
product support costs consisting primarily of salaries and related overhead expenses for personnel in research
and development and pre-commercial functions (for example wages, salaries and associated on costs such as
superannuation, share-based incentives and payroll taxes, plus travel costs and recruitment fees for new
hires);
•
intellectual property support costs comprising payments to our patent attorneys to progress patent applications
and all costs of renewing our granted patents; and
•
amortization of currently marketed products on a straight-line basis over the life of the asset.
Our research and development expenses are not charged to specific products or programs, since the number of
clinical and preclinical product candidates or development projects tends to vary from period to period and since internal
resources are utilized across multiple products and programs over any given period of time. As a result, our management
does not maintain and evaluate research and development costs by product or program. Acquired in-process research and
development is capitalized as an asset and is not amortized but is subject to annual impairment review during the
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development phase. Upon completion of its development, the acquired in-process research and development amortization
will commence.
Manufacturing Commercialization. Manufacturing commercialization expenditure is recognized as an expense as
incurred. Our manufacturing commercialization expenses consist primarily of:
•
salaries and related overhead expenses including share-based incentives for personnel in manufacturing
functions;
•
fees paid to our contract manufacturing organizations, which perform process development on our behalf and
under our direction;
•
costs related to laboratory supplies used in our manufacturing development efforts; and
•
provision for the carrying value of pre-launch inventory costs on the balance sheet.
Management and Administration. Management and administration expenses consist primarily of salaries and related
costs including share-based incentives for directors and employees in corporate and administrative functions, including the
executives of those areas. Other significant management and administration expenses include legal and professional
services, rent and depreciation of leasehold improvements, insurance and information technology services.
Fair Value Remeasurement of Contingent Consideration. Remeasurement of contingent consideration pertains to the
acquisition of the MSC assets from Osiris Therapeutics, Inc. (“Osiris”). The fair value remeasurement of contingent
consideration is recognized as a net result of changes to the key assumptions of the contingent consideration valuation such
as developmental timelines, market growth, probability of success and payment, market penetration, product pricing and
the increase in valuation as the time period shortens between the valuation date and the potential settlement dates of
contingent consideration.
Fair Value Movement of Warrants. Remeasurement of warrants pertain to the warrants granted to Oaktree Capital
Management, L.P ("Oaktree") in relation to the refinancing and amendment of our senior debt facility. The fair value
movement of warrants is recognized when there is a change in the valuation assumptions such as share price, risk-free
interest rates and volatility.
Other Operating Income and Expenses. Other operating income and expenses primarily comprise foreign exchange
gains and losses.
Tax incentives comprise payments from the Australian government’s Innovation Australia Research and
Development Tax Incentive program for research and development activities conducted in relation to our qualifying
research that meets the regulatory criteria. The research and development tax incentive credit is available for our research
and development activities in Australia. Eligible companies can receive a refundable tax offset for a percentage of their
research and development spending.
Foreign exchange gains and losses relate to unrealized foreign exchange gains and losses on our foreign currency
amounts in our Australian based entity, whose functional currency is the A$, and foreign currency amounts in our
Switzerland and Singapore based entities, whose functional currencies are the US$, plus realized gains and losses on any
foreign currency payments to our suppliers due to movements in exchange rates.
Interest Revenue. Interest revenue is accrued on a time basis by reference to the principal outstanding and at the
effective interest rate applicable.
Finance Costs. Finance costs primarily consists of remeasurement of borrowing arrangements, interest expense in
relation to finance lease charges, accrued interest expense and interest expense in relation to the amortization of transaction
costs and other charges associated with the borrowings as represented in our consolidated balance sheet using the effective
interest rate method over the period of initial recognition through maturity.
Remeasurement of borrowing arrangements recognized pertain to our loan and security agreements with NovaQuest
Capital Management, L.L.C. (“NovaQuest”) and Oaktree. Remeasurement of borrowing arrangements is recognized when
there is a modification of the borrowing arrangement with no significant change to the contractual cash flows of the
borrowings at the remeasurement date or when there is a revision in the estimated future cash flows which is recorded as an
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adjustment of the carrying amount of the financial liability. The carrying amount is recalculated by computing the present
value of the revised estimated future cash flows at the financial instrument’s original effective interest rate.
Income Tax Benefit/Expense. Income tax benefit/expense consists of net changes in deferred tax assets and liabilities
recognized on the balance sheet during the period.
Results of Operations
Comparison of Our Results for the Year ended June 30, 2024 with the Year ended June 30, 2023
The following table summarizes our results of operations for the years ended June 30, 2024 and 2023, together with
the changes in those items in dollars and as a percentage.
Year ended
June 30,
(in U.S. dollars, in thousands except per share information)
2024
2023
$ Change
% Change
Consolidated Income Statement Data:
Revenue:
Commercialization revenue
$
5,902 $
7,501
(1,599)
(21%)
Total revenue
5,902
7,501
(1,599)
(21%)
Research & development
(25,353)
(27,189)
1,836
(7%)
Manufacturing commercialization
(15,717)
(27,733)
12,016
(43%)
Management and administration
(23,626)
(25,374)
1,748
(7%)
Fair value remeasurement of contingent consideration
(9,693)
8,771
(18,464)
NM
Fair value movement of warrants
779
(2,205)
2,984
(135%)
Other operating income and expenses
2,570
4,250
(1,680)
(40%)
Finance costs
(23,009)
(20,122)
(2,887)
14%
Loss before income tax
(88,147)
(82,101)
(6,046)
7%
Income tax benefit
191
212
(21)
(10%)
Loss attributable to the owners of Mesoblast Limited
$
(87,956) $
(81,889)
(6,067)
7%
Losses per share from continuing operations attributable to
the ordinary equity holders:
Cents
Cents
Cents
% Change
Basic - losses per share
(8.91)
(10.53)
1.62
(15%)
Diluted - losses per share
(8.91)
(10.53)
1.62
(15%)
* NM = not meaningful.
Revenue
Revenues were $5.9 million for the year ended June 30, 2024, compared with $7.5 million for the year ended
June 30, 2023, a decrease of $1.6 million. The following table shows the movement within revenue for the years ended
June 30, 2024 and 2023, together with the changes in those items.
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Revenue:
Commercialization revenue
5,902
7,501
(1,599)
(21%)
Revenue
$
5,902 $
7,501
(1,599)
(21%)
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Commercialization revenue from royalty income earned on sales of TEMCELL in Japan and Alofisel® decreased by
$1.6 million for the year ended June 30, 2024. Royalty income on sales of TEMCELL in Japan by our licensee JCR were
$5.5 million in the year ended June 30, 2024 compared to $7.1 million in the year ended June 30, 2023, a decrease of $1.6
million. Of this $1.6 million decrease, $0.4 million was due to foreign exchange rate changes as the Japanese Yen
depreciated against the U.S. dollar. Royalty income on sales of Alofisel® by our licensee Takeda were consistent at $0.4
million in the years ended June 30, 2024 and 2023.
Research and development
Research and development expenses were $25.4 million for the year ended June 30, 2024, compared with $27.2
million for the year ended June 30, 2023, a decrease of $1.8 million. The $1.8 million decrease in research and
development expenses is primarily due to the movements in third party costs and product support costs.
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Research and development:
Third party costs
3,776
8,398
(4,622)
(55%)
Product support costs
17,338
14,107
3,231
23%
Intellectual property support costs
2,784
3,222
(438)
(14%)
Amortization of current marketed products
1,455
1,462
(7)
0%
Research and development
$
25,353 $
27,189
(1,836)
(7%)
Third party costs, which consist of all external expenditure on our research and development programs and pre-
commercial activities, decreased by $4.6 million in the year ended June 30, 2024 compared with the year ended June 30,
2023.
This $4.6 million decrease was due to a reduction in our third party costs for our Phase 3 clinical trials for the
treatment of MPC-150-IM (CHF) and ARDS in COVID-19 patients. The decrease of these costs were primarily due to
higher activities in relation to patient monitoring during follow up visits and higher data analysis being performed in the
year ended June 30, 2023 compared with the year ended June 30, 2024. In the year ended June 30, 2024, we incurred costs
associated with start-up activities for our confirmatory Phase 3 clinical trial for MPC-06-ID (CLBP). In the year ended
June 30, 2024, we also incurred costs of $0.6 million associated with our pre-commercial activities as we prepared for the
potential launch of remestemcel-L in the United States.
Product support costs, which consist primarily of salaries and related overhead expenses for personnel in research
and development and pre-commercial functions, have increased by $3.2 million, for the year ended June 30, 2024
compared with the year ended June 30, 2023 due to an increase of $3.2 million in product support costs for research and
development functions. The product support costs for pre-commercial functions remained relatively consistent for the year
ended June 30, 2024 compared with the year ended June 30, 2023.
The $3.2 million increase in product support costs for personnel in research and development functions is primarily
due to an increase of $2.7 million in short-term incentives. In the year ended June 30, 2024, we recognized short-term
incentives of $1.8 million related to the year ended June 30, 2023 given that subsequent to June 30, 2023 the conditions of
achievement of the short-term incentive for year ended June 30, 2023 were modified to make it dependent on Mesoblast
achieving FDA marketing authorization. There was also an increase of $1.2 million in share-based payment expenses for
the year ended June 30, 2024 compared with the year ended June 30, 2023. These increases were offset by a decrease of
$0.2 million in consulting expenses for the year ended June 30, 2024 compared with the year ended June 30, 2023. There
was also a decrease of $0.5 million across salaries and associated costs as full time equivalents decreased by 1.7 (4%) from
43.7 for the year ended June 30, 2023 to 42.0 for the year ended June 30, 2024.
Also included in research and development expenses are intellectual property support costs, which consist of
payments to our patent attorneys to progress patent applications and costs of renewing our granted patents. These costs
have decreased by $0.4 million in the year ended June 30, 2024 compared with the year ended June 30, 2023 due to
decreased activities across our entire patent portfolio.
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Manufacturing commercialization
Manufacturing commercialization expenses were $15.7 million for the year ended June 30, 2024, compared with
$27.7 million for the year ended June 30, 2023, a decrease of $12.0 million. This decrease is due to a decrease in platform
technology costs.
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Manufacturing commercialization:
Platform technology
13,472
25,964
(12,492)
(48%)
Manufacturing support costs
2,245
1,769
476
27%
Manufacturing commercialization
$
15,717 $
27,733
(12,016)
(43%)
Platform technology costs decreased by $12.5 million for the year ended June 30, 2024 compared with year ended
June 30, 2023. These costs consist of fees paid to our contract manufacturing organizations, potency assay work that
supported the aGVHD Biologics License Application ("BLA") resubmission, process development of our proprietary
technology that facilitates the increase in yields necessary for the long-term commercial supply of our product candidates
and next generation manufacturing processes to reduce labor, drive down cost of goods and improve manufacturing
efficiencies in our MPC and MSC based products. The decrease of these costs was primarily due to lower MSC
development activities during the year ended June 30, 2024 compared with the year ended June 30, 2023.
Manufacturing support costs, which consist primarily of salaries and related overhead expenses for personnel in
manufacturing commercialization functions increased by $0.5 million for the year ended June 30, 2024 compared with the
year ended June 30, 2023 primarily due to an increase in short-term incentives for the year ended June 30, 2024 compared
with the year ended June 30, 2023. In the year ended June 30, 2024, we recognized short-term incentives of $0.2 million
related to the year ended June 30, 2023 given that subsequent to June 30, 2023 the conditions of achievement of the short-
term incentive for year ended June 30, 2023 were modified to make it dependent on Mesoblast achieving FDA marketing
authorization.
Management and administration
Management and administration expenses were $23.6 million for the year ended June 30, 2024, compared with
$25.3 million for the year ended June 30, 2023, a decrease of $1.7 million. This decrease was primarily due to a decrease in
corporate overheads.
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Management and administration:
Labor and associated expenses
10,059
9,854
205
2%
Corporate overheads
11,129
12,501
(1,372)
(11%)
Legal and professional fees
2,438
3,019
(581)
(19%)
Management and administration
$
23,626 $
25,374
(1,748)
(7%)
Labor and associated expenses increased by $0.2 million from $9.9 million for the year ended June 30, 2023 to
$10.1 million for the year ended June 30, 2024. This $0.2 million increase is primarily due to an increase of $1.0 million in
share-based payment expenses and $1.3 million in short-term incentives. In the year ended June 30, 2024, we recognized
short-term incentives of $0.9 million related to the year ended June 30, 2023 given that subsequent to June 30, 2023 the
conditions of achievement of the short-term incentive for year ended June 30, 2023 were modified to make it dependent on
Mesoblast achieving FDA marketing authorization. As a result of managements cost containment strategy, these increases
were offset by a decrease of $0.8 million in consulting expenses and $0.3 million in recruitment. There was also a decrease
in overall cost of salaries and associated expenses by $0.8 million in the year ended June 30, 2024, compared with the year
ended June 30, 2023 due to full time equivalents decreasing by 2.6 (11%) from 24.5 for the year ended June 30, 2023 to
21.9 for the year ended June 30, 2024. Labor and associated expenses also experienced favorable exchange rate
fluctuations of $0.2 million in the year ended June 30, 2024 compared with the year ended June 30, 2023, as the A$
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weakened against the US$ given the majority of management and administration expenses are incurred in A$ by our
headquarter office located in Australia.
Corporate overhead expenses decreased by $1.4 million from $12.5 million for the year ended June 30, 2023 to
$11.1 million for the year ended June 30, 2024 primarily due to a decrease of insurance premiums.
Legal and professional fees decreased by $0.6 million from $3.0 million for the year ended June 30, 2023 to $2.4
million for the year ended June 30, 2024 as legal activities decreased in the period.
Fair value remeasurement of contingent consideration
Fair value remeasurement of contingent consideration was a $9.7 million loss for the year ended June 30, 2024
compared with a $8.8 million gain for the year ended June 30, 2023. The $9.7 million loss for the year ended June 30, 2024
was due to the remeasurement of contingent consideration pertaining to the acquisition of assets from Osiris. This loss was
a net result of changing the key assumptions of the contingent consideration valuation such as probability of success,
development timelines and the increase in valuation as the time period shortens between the valuation date and the
potential settlement dates of contingent consideration.
The $8.8 million gain for the year ended June 30, 2023 was due to the remeasurement of contingent consideration
pertaining to the acquisition of assets from Osiris. This gain was a net result of changing the key assumptions of the
contingent consideration valuation such as probability of payment, development timelines and the increase in valuation as
the time period shortens between the valuation date and the potential settlement dates of contingent consideration,
including the impact from the complete response from the FDA on our BLA for remestemcel-L for the treatment of
pediatric SR-aGVHD in August 2023. The assumptions relating to development timelines were updated to reflect
expectations as a result of the complete response.
With respect to future milestone payments, contingent consideration will be payable in cash or shares at our
discretion. With respect to commercialization, product royalties will be payable in cash which will be funded from royalties
received from net sales.
Fair value movement of warrants
Fair value movement of warrants was a $0.8 million gain for the year ended June 30, 2024 compared with a $2.2
million loss for the year ended June 30, 2023. This $0.8 million gain for the year ended June 30, 2024 is a net result of
changes to the key valuation inputs of the warrants such as the share price, risk-free interest rates and volatility.
Other operating income and expenses
In relation to other operating income and expenses, we recognized an income of $2.6 million for the year ended
June 30, 2024, compared with an income of $4.3 million for the year ended June 30, 2023, a decrease in income of $1.7
million. The following table shows movements within other operating income and expenses for the year ended June 30,
2024 and 2023, together with the changes in those items:
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Other operating income and expenses:
Research and development tax incentive income
(859)
(3,506)
2,647
(75%)
Interest income
(1,824)
(831)
(993)
119%
Foreign exchange losses (net)
76
163
(87)
(53%)
Derecognition of right of use asset
—
(76)
76
(100%)
Foreign withholding tax
37
—
37
NM
Other operating (income) and expenses
$
(2,570) $
(4,250)
1,680
(40%)
* NM = not meaningful.
Research and development tax incentive income decreased by $2.6 million from $3.5 million for the year ended
June 30, 2023 to $0.9 million for the year ended June 30, 2024. We have recognized incentive income pertaining to the
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85
eligible expenditure undertaken in each of these periods. At each period end, management estimates the refundable tax
incentive available to us based on available information at the time. We employ independent tax specialist to review, on an
annual basis, the quantum of our previous research and development tax claims and our on-going eligibility to claim the
research and development tax incentive in Australia.
Within the $3.5 million recognized for the year ended June 30, 2023, $1.2 million pertains to the year ended June
30, 2023, $1.1 million pertains to the year ended June 30, 2022 and $1.2 million pertains to the year ended June 30, 2021,
whereas in the year ended June 30, 2024 we recognized $0.9 million which pertains to income for the year ended June 30,
2024. Therefore the decrease in income is due to the impact of management concluding its assessment of qualifying
activities of prior periods in the year ended June 30, 2023.
The $1.0 million increase in interest income for the year ended June 30, 2024 compared with the year ended
June 30, 2023 was primarily driven by higher interest rates on A$ and US$ cash deposits in the year ended June 30, 2024,
when compared to the year ended June 30, 2023.
We are subject to foreign exchange gains and losses on foreign currency cash balances, creditors and debtors. In the
year ended June 30, 2024, we recognized a foreign exchange loss of $0.1 million, primarily due to movements in exchange
rates on US$ liabilities held in Mesoblast Limited, whose functional currency is the A$, as the A$ depreciated against the
US$. In the year ended June 30, 2023, we recognized a foreign exchange loss of $0.2 million.
In the year ended June 30, 2023, we recognized an income of $0.1 million for the derecognition of right of use asset.
There was no derecognition of right of use asset in the year ended June 30, 2024.
Finance costs
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Finance costs:
Remeasurement of borrowing arrangements
2,351
678
1,673
NM
Interest expense
20,658
19,444
1,214
6%
Finance costs
$
23,009 $
20,122
2,887
14%
* NM = not meaningful.
In the year ended June 30, 2024, we recognized an overall loss of $2.4 million for remeasurement of borrowing
arrangements in relation to the adjustment of the carrying amount of our financial liability to reflect the revised estimated
future cash flows from our credit facilities with NovaQuest and Oaktree, an increase in losses of $1.7 million as compared
with a $0.7 million loss for the year ended June 30, 2023.
Within the $2.4 million loss in the year ended June 30, 2024, in relation to our existing credit facility with
NovaQuest, we recognized a $0.1 million loss for remeasurement of borrowing arrangements in relation to the adjustment
of the carrying amount of our financial liability to reflect the revised estimated future cash flows as a net result of changes
to the key assumption in development timelines, a decrease in gains of $1.0 million as compared with a $0.9 million gain
recognized for the year ended June 30, 2023.
Also within the $2.4 million loss in the year ended June 30, 2024, in relation to our existing credit facility with
Oaktree, we recognized a $2.3 million loss for remeasurement of borrowing arrangements in relation to the adjustment of
the carrying amount of our financial liability to reflect the revised estimated future cash flows, an increase in losses of $0.7
million as compared with a $1.6 million loss for the year ended June 30, 2023. Within the $1.6 million loss recognized in
the year ended June 30, 2023, $1.0 million related to the remeasurement due to additional warrants being issued to Oaktree
as a result of the first amendment to the loan agreement and $0.6 million related to the adjustment of the carrying amount
of our financial liability to reflect the revised estimated future cash flows.
Interest expense increased by $1.2 million from $19.4 million for the year ended June 30, 2023 to $20.6 million for
the year ended June 30, 2024.
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In the year ended June 30, 2024, in relation to our loan and security agreement with Oaktree, we recognized $9.4
million of interest expense, compared with $9.2 million for the year ended June 30, 2023. Within the $9.4 million
recognized in the year ended June 30, 2024, $5.6 million was recognized with regards to interest expense payable on the
loan balance within the year of which $5.2 million was paid and $0.4 million was added to the outstanding loan balance
and shall accrue further interest. A further $3.8 million of interest expense was recognized with regard to the amortization
of transaction costs incurred on the outstanding loan principal for the year ended June 30, 2024 using the effective interest
rate method over the period of initial recognition through maturity.
In the year ended June 30, 2024, in relation to our loan and security agreement with NovaQuest, we recognized
$10.6 million of interest expense, an increase of $1.5 million as compared with $9.1 million for the year ended June 30,
2023. Interest expense relating to the NovaQuest loan is accrued on the loan principal balance and all interest payments are
deferred until the earlier of loan maturity or from after the first commercial sale of our allogeneic product candidate
remestemcel-L for the treatment of pediatric patients with SR-aGVHD in the United States and other geographies
excluding Asia.
In line with IFRS 16 Leases, we also recognized interest expenses of $0.4 million and $0.5 million in relation to
lease charges for the year ended June 30, 2024 and 2023, respectively.
In the year ended June 30, 2024 and 2023, we recognized $0.2 million and $0.6 million of interest charges in
relation to manufacturing payments, respectively.
Loss after income tax
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Loss before income tax
(88,147)
(82,101)
(6,046)
7%
Income tax benefit
191
212
(21)
(10%)
Loss after income tax
$
(87,956) $
(81,889)
(6,067)
7%
Loss before income tax was $88.1 million for the year ended June 30, 2024 compared with $82.1 million for the
year ended June 30, 2023, an increase in the loss by $6.0 million. This increase is the net effect of the changes in revenues
and expenses that have been discussed above.
A non-cash income tax benefit of $0.2 million was recognized in the year ended June 30, 2024, in relation to the net
change in deferred tax assets and liabilities recognized on the consolidated balance sheet during the period.
A non-cash income tax benefit of $0.2 million was recognized in the year ended June 30, 2023 in relation to the net
change in deferred tax assets and liabilities recognized on the consolidated balance sheet during the period.
Comparison of Our Results for the Year ended June 30, 2023 with the Year ended June 30, 2022
For results of operations for the years ended June 30, 2023 and 2022, together with the changes in those items in
dollars and as a percentage and the related discussions on these results, refer to Results of Operations within “Item 5.A
Operating Results” in our Annual Report on Form 20-F for the year ended June 30, 2023, filed with the SEC on August 31,
2023.
Certain Differences Between IFRS and U.S. GAAP
IFRS differs from U.S. GAAP in certain respects. Management has not assessed the materiality of differences
between IFRS and U.S. GAAP. Our significant accounting policies are described in “Item 18 Financial Statements – Note
23”.
Quantitative and Qualitative Disclosure about Market Risk
We are exposed to interest rate risk, share price risk, price risk and foreign currency exchange risk. We make use
of sensitivity analyses which are inherently limited in estimating actual losses in fair value that can occur from changes in
market conditions. For further assessment on our market risks, see “Item 18. Financial Statements – Note 10(a).”
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87
Off-Balance Sheet Arrangements
We did not have during the periods presented, and we do not currently have, any off-balance sheet arrangements,
other than the purchase commitments and contingent liabilities as mentioned below.
Contractual Obligations and Commitments
Contractual commitments:
Purchase commitments means an agreement to purchase goods or services that is enforceable and legally binding
that specifies all significant terms, including: fixed or minimum quantities to be purchased; fixed, minimum or variable
price provisions; and the approximate timing of the transaction. Purchase obligations are not recognized as liabilities at
June 30, 2024. For a description of our contractual commitment, refer to "Item 18. Financial Statements - Note 14(b)."
Lease commitment – as lessee:
We lease various offices under non-cancellable leases expiring within 1 to 3 years. The leases have varying terms,
escalation clauses and renewal rights. On renewal, the terms of the leases are renegotiated. We subleased a portion of our
office in Melbourne Australia under a non-cancellable lease expiring within 2 years. We also lease a manufacturing suite
under a manufacturing services agreement with Lonza for the supply of commercial product for the potential approval and
launch of remestemcel-L for the treatment of pediatric SR-aGVHD in the US market expiring within 2 years from June 30,
2024, which is cancellable in limited circumstances.
Contingent liabilities
We acquired certain intellectual property relating to our MPCs, or Medvet IP, pursuant to an Intellectual Property
Assignment Deed, or IP Deed, with Medvet Science Pty Ltd, or Medvet. Medvet’s rights under the IP Deed were
transferred to Central Adelaide Local Health Network Incorporated, or CALHNI, in November 2011. In connection with
our use of the Medvet IP, on completion of certain milestones we will be obligated to pay CALHNI, as successor in interest
to Medvet, (i) certain aggregated milestone payments of up to $2.2 million, and single-digit royalties on net sales of
products covered by the Medvet IP, for cardiac muscle and blood vessel applications and bone and cartilage regeneration
and repair applications, subject to minimum annual royalties beginning in the first year of commercial sale of those
products and (ii) single-digit royalties on net sales of the specified products for applications outside the specified fields.
We have entered into a number of agreements with other third parties pertaining to intellectual property. Contingent
liabilities may arise in the future if certain events or developments occur in relation to these agreements and as of June 30,
2024 we have assessed that the probability of outflows is remote.
Capital commitments
We did not have any commitments for future capital expenditure outstanding as of June 30, 2024.
Australian Disclosure Requirements
Significant Changes in the State of Affairs
There have been no significant changes within the state of our affairs during the year ended June 30, 2024 except
as noted in the “Important Corporate Developments” section included in Item 4.A.
Likely Developments and Expected Results of Operations
In March 2024, the FDA informed us that following additional consideration, the available clinical data from our
Phase 3 study MSB-GVHD001 appears sufficient to support submission of the proposed BLA for remestemcel-L for the
treatment of pediatric patients with SR-aGVHD. The BLA was resubmitted to FDA in July 2024 and was accepted within
two weeks. FDA considered the resubmission to be a complete response and set a Prescription Drug User Fee Act
("PDUFA") goal date of January 7, 2025.
Other significant milestones are expected in the upcoming financial year in relation to our other lead product
candidates, as detailed elsewhere in this report.
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88
Environmental Regulations
Our operations are not subject to any significant environmental regulations under either Commonwealth of
Australia or State/Territory legislation. We consider that adequate systems are in place to manage our obligations and are
not aware of any breach of environmental requirements pertaining to us.
5.B
Liquidity and Capital Resources
Sources of Liquidity
As of June 30, 2024, we held total cash reserves of $63.0 million. During the year ended June 30, 2024, we
executed on reprioritization of projects and operational streamlining activities and as a result has reduced net cash usage for
operating activities, which was $48.5 million for the year ended June 30, 2024, a reduction of 23% compared to the prior
period.
As we prepare for a potential first product approval by the FDA, and in line with our commercial launch plans,
additional inflows from capital markets, strategic partnerships, product specific financing or royalty monetization will be
required to meet our projected expenditure consistent with our business strategy over at least the next 12 months. As a
result of these matters, there is material uncertainty related to events or conditions that may cast significant doubt (or raise
substantial doubt as contemplated by Public Company Accounting Oversight Board (“PCAOB”) standards) on our ability
to continue as a going concern and, therefore, that we may be unable to realize our assets and discharge our liabilities in the
normal course of business. The consolidated financial statements do not include any adjustments that might result from the
outcome of this uncertainty.
Our primary sources of liquidity have historically been equity raisings, upfront and milestone payments from
strategic license agreements, and borrowings under our loan agreements. We also expect net sales to become a source of
liquidity. While in the long-term we expect to be able to complete transactions, draw upon these facilities and achieve
approval of our product candidates to provide liquidity as needed, there can be no assurance as to whether we will be
successful or, if successful, what the terms or proceeds may be.
Cash flows
Year ended
June 30,
(in U.S. dollars, in thousands)
2024
2023
$ Change
% Change
Cash Flow Data:
Net cash (outflows) in operating activities
(48,458)
(63,269)
14,811
(23%)
Net cash (outflows) in investing activities
(97)
(194)
97
(50%)
Net cash inflows by financing activities
40,252
74,502
(34,250)
(46%)
Net (decrease)/increase in cash and cash equivalents
(8,303)
11,039
(19,342)
(175%)
Comparison of cash flows for the Year ended June 30, 2024 with the Year ended June 30, 2023
Net cash outflows in operating activities
Net cash outflows for operating activities were $48.5 million for the year ended June 30, 2024, compared with $63.3
million for the year ended June 30, 2023, a decrease of $14.8 million. The decrease of $14.8 million is due to a decrease in
cash outflows of $11.8 million and an increase in cash inflows of $3.0 million in the year ended June 30, 2024, compared
with the year ended June 30, 2023.
The $3.0 million increase of inflows comprised: inflows from royalty income earned on sales of TEMCELL in Japan
and Alofisel® decreased by $0.7 million during the year ended June 30, 2024, compared with the year ended June 30, 2023;
received $3.8 million of receipts for research and development tax incentive during the year ended June 30, 2024,
compared to $1.1 million for the year ended June 30, 2023; and inflows from interest receipts increased by $1.0 million in
the year ended June 30, 2024, compared with the year ended June 30, 2023.
Outflows for payments to suppliers and employees decreased by $11.8 million from $72.7 million for the year ended
June 30, 2023 to $60.8 million for the year ended June 30, 2024. The decrease in payments was primarily due to the cost
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containment strategy introduced in August 2024, which reduced payroll payments and director fees, insurance,
manufacturing and clinical trials given clinical trial activities were reduced in the period.
Net cash outflows in investing activities
Net cash outflows for investing activities decreased by $0.1 million in the year ended June 30, 2024, compared with
the year ended June 30, 2023.
Net cash inflows in financing activities
Net cash inflows for financing activities decreased by $34.2 million for the year ended June 30, 2024, compared
with the year ended June 30, 2023. The decrease of $34.2 million is due to a decrease in cash inflows of $23.2 million and
an increase in cash outflows of $11.0 million in the year ended June 30, 2024 compared with the year ended June 30, 2023.
The $23.2 million decrease in inflows comprised: $45.1 million of proceeds received in August 2022 and $43.5
million of proceeds received in April 2023 on completion of private placements during the year ended June 30, 2023,
compared with $65.4 million of proceeds received from an institutional placement and entitlement offer during the year
ended June 30, 2024;
The $11.0 million increase in outflows comprised: payments of $3.5 million and $2.6 million for lease liabilities
during the years ended June 30, 2024 and 2023, respectively; payments of $5.7 million and $6.0 million for interest and
other costs of finance during the years ended June 30, 2024 and 2023, respectively; payments of $4.3 million and $4.9
million for capital raising costs in the years ended June 30, 2024 and 2023, respectively; payments of $1.5 million and $0.5
million for borrowings costs in the years ended June 30, 2024 and 2023, respectively; principal repayment of $10.0 million
to reduce debt under our five-year facility with Oaktree during the year ended June 30, 2024, compared to $Nil for the year
ended June 30, 2023.
Operating Capital Requirements
We do not know when, or if, we will generate revenues from our product sales significant enough to generate
profits. We do not expect to generate significant revenue from product sales unless and until we obtain regulatory approval
of and commercialize more of our cell-based product candidates. We anticipate that we will continue to incur losses for the
foreseeable future, and we expect the losses to increase as we continue the development of, and seek regulatory approvals
for, our cell-based product candidates, and begin to commercialize any approved products either directly ourselves or
through a collaborator or partner. We are subject to all of the risks inherent in the development of new cell-based products,
and we may encounter unforeseen expenses, difficulties, complications, delays and other unknown factors that may
adversely affect our business. We anticipate that we will need substantial additional funding in connection with our
continuing operations.
Subject to us achieving successful regulatory approval we expect an increase in our total expenses driven by an
increase in our planned research and development, manufacturing commercialization and selling, general and
administrative expenses as we move towards commercialization. Therefore, we will need additional capital to fund our
operations, which we may raise through a combination of equity offerings, debt financings, other third-party funding,
marketing and distribution arrangements and other collaborations, strategic alliances and licensing arrangements.
Additional capital may not be available on reasonable terms, if at all. If we are unable to raise additional capital in
sufficient amounts or on terms acceptable to us, we may have to significantly delay, scale back or discontinue the
development or commercialization of one or more of our product candidates. If we raise additional funds through the
issuance of additional debt or equity securities, it could result in dilution to our existing shareholders, increased fixed
payment obligations and the existence of securities with rights that may be senior to those of our ordinary shares. If we
incur further indebtedness, we could become subject to covenants that would restrict our operations and potentially impair
our competitiveness, such as limitations on our ability to incur additional debt, limitations on our ability to acquire, sell or
license intellectual property rights and other operating restrictions that could adversely impact our ability to conduct our
business. Any of these events could significantly harm our business, financial condition and prospects.
Borrowings
For a description of our borrowing arrangements, refer to "Item 18. Financial Statements - Note 5(f)."
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5.C
Research and Development, Patents and Licenses
For a description of the amount spent during each of the last three fiscal years on company-sponsored research and
development activities, as well as the components of research and development expenses, see “Item 5.A Operating Results
– Results of Operations.”
For a description of our research and development process, see “Item 4.B Business Overview.”
5.D
Trend Information
As a biotechnology company which primarily is still in the development stage, we are subject to costs of our
clinical trials and other work necessary to support applications for regulatory approval of our product candidates. Health
regulators have increased their focus on product safety. In addition, regulators have also increased their attention on
whether or not a new product offers evidence of substantial treatment effect. These developments have led to requests for
more clinical trial data, for the inclusion of a higher number of patients in clinical trials, and for more detailed analyses of
the trials. In light of these developments, we expect these aspects of our research and development expenses may need to
increase as we continue to fund our programs to the market. Notwithstanding this upward trend, our research and
development expenses may still fluctuate from period to period due to varied rates of patient enrollment and the timing of
our clinical trials as our existing trials are completed and new trials commence. We cannot predict with any degree of
accuracy the outcome of our research or commercialization efforts.
5.E
Critical Accounting Estimates
Not applicable. See “Item 18. Financial Statements.”
Item 6. Directors, Senior Management and Employees
6.A
Directors and Senior Management Personnel
Details of Directors and Senior Management
Board of Directors
Jane Bell – B.Ec, LLB, LLM (London)
Non-Executive Member of the Board of Directors
Commenced as Board Chair April 30, 2024
Experience and expertise
Ms. Bell AM has 30 years experience as a banking and finance lawyer with leading law firms, financial services
and corporate treasury operations in the United States, Canada, Australia and the United Kingdom. She is an experienced
Chair and non-executive Director in highly regulated sectors including delivery of healthcare, life sciences, medical
research, and funds management. Ms. Bell currently serves as Deputy Chair of Monash Health, Australia’s largest and
most diverse public health service delivering more than 3.46 million episodes of care, and Chair of its Audit Committee.
She is also a director of publicly-listed biotechnology company Amplia Therapeutics and Chair of its Audit Committee and
of Jessie McPherson Private Hospital. She is a former Chair of Royal Melbourne Hospital and former Chair of Biomedical
Research Victoria as well as of Advisory Groups for the Royal Australian and New Zealand College of Obstetricians and
Melbourne Genomics Health Alliance, a former director of Hudson Institute of Medical Research and Chair of its
Intellectual Property and Commercialization Committee and director of U Ethical, Australia’s first ethical funds manager.
Ms Bell holds a Master of Laws from King’s College (London), Bachelor of Laws University of Melbourne, and Bachelor
of Economics Monash University. In 2023 Ms Bell was appointed a Member of the Order of Australia (AM) for her
significant service to governance in the medical research, healthcare and not-for-profit sectors.
Other current directorships of listed public companies
Non-Executive Director, Amplia Therapeutics Limited (since 2021)
Former directorships of listed public companies within the last 3 years
None
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Joseph Swedish, MHA
Non-Executive Member of the Board of Directors
Board Chair until April 30, 2024
Experience and expertise
Joseph R. Swedish is the former Chairman, President and CEO of Anthem, Inc, (currently Elevance Health) a
Fortune 22 company and the nation’s leading health benefits provider. This became the foundation for Elevance Health
today serving nearly 47.3 million members – or one in seven Americans – through its affiliated health plans, and over 117
million individuals across 33 states through its broad portfolio of health insurance and service subsidiaries. He served as
the Chairman, President and CEO from 2013 to 2018. Subsequently he served as a Strategic Advisor from 2018 to 2020.
During his tenure Anthem’s membership grew by four million, or 11 percent, the average share price nearly quadrupled,
and operating revenue increased 39 percent to over $89 billion. Core strategic imperatives included improving medical
costs, working with physicians and health care organizations to improve quality and access, and improving the consumer
experience. As a business executive, conservationist, and philanthropist, Joe serves on the board of directors for CDW,
Centrexion Therapeutics, Accelus and Navitus Health Solutions. Most recently, he served on the board of directors for
IBM, as chairman of America’s Health Insurance Plans (AHIP), and chairman of the Catholic Health Association. He
currently serves as a board member for The Nature Conservancy (Colorado). He has also held board and advisory positions
with American Hospital Association, Coventry Health Care, Inc., RehabCare Group, Inc., Cross Country, National Quality
Forum, the National Center for Healthcare Leadership, and Loyola University Chicago. He is also a member and past
chairman of Duke University’s Fuqua School of Business Board of Visitors. Prior to joining Anthem, Joe served as CEO
for several major integrated health care delivery systems, including president and CEO of Trinity Health, an 18-state
integrated health care delivery system. He also held CEO and senior leadership positions with the Hospital Corporation of
America, Colorado’s Centura Health, and integrated health systems in Florida, Virginia, and the Carolinas. In 2018, he
continued to apply his expertise leveraging his extensive health care experience as co-founder of Concord Health Partners,
a private equity firm investing in data analytics, provider enablement services and consumer engagement enterprises. He is
now Partner Emeritus having recently departed active status. More broadly, he has built a reputation as a trend-setter by
leveraging value-creating assets through high-performing governance, creative strategies, consumer marketing, clinical
innovations, and mergers/acquisitions – all efforts focused on organization renewal and growth. For 12 years in a row,
Modern Healthcare named him one of the 100 Most Influential People in Healthcare, ranking in the top 20 of the health
sector’s most senior-level executives, high-level government administrators, elected officials, academics, and thought-
leaders for five consecutive years. He received his bachelor’s degree from the University of North Carolina at Charlotte
and his master’s degree in health administration from Duke University.
Other current directorships of listed public companies
Non-Executive Director, IBM Corporation (since 2017)
Non-Executive Director, CDW Corporation (since 2015)
Former directorships of listed public companies within the last 3 years
None
William Burns, BA
Non-Executive Member of the Board of Directors
Experience and expertise
Mr. Burns has served on the Board of Directors since 2014 and was appointed Vice Chairman in 2016. He spent
his entire management career at the Beecham Group and F. Hoffmann-La Roche Ltd. Mr Burns was Chief Executive
Officer of Roche Pharmaceuticals from 2001 to 2009, when he joined the Board of Directors of F. Hoffmann-La Roche
Ltd. until he retired in 2014. He is the Chair of Molecular Partners, and has been a Non-Executive Director of Shire PLC,
Chugai Pharmaceutical Co., Genentech, Crucell, and Chairman of Biotie Therapies Corp. from 2014 until its sale to Acorda
Therapeutics Inc. in 2016. Mr Burns is also a member of the Oncology Advisory Board of the Universities of Cologne/
Bonn in Germany. In 2014, he was appointed a trustee of the Institute of Cancer Research(ICR), London, and in 2016 a
Governor of The Wellcome Trust in London, UK. Mr Burns completed his terms of office at both ICR and Wellcome Trust
and has retired from both positions.
Other current directorships of listed public companies
Chair of Molecular Partners (since 2018)
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Former directorships of listed public companies within the last 3 years
None
Philip Facchina
Non-Executive Member of the Board of Directors
Experience and expertise
Mr. Facchina brings more than 35 years of experience in corporate strategy, finance, and business development
across several industries, including healthcare. Since 2018, Mr. Facchina has been Chief Strategy Officer at SurgCenter,
overseeing the company’s strategic relationships, including its relationships with the broad US ambulatory surgical center
(ASC) market and its constituents. Prior to SurgCenter, Mr. Facchina spent two decades in the public and private capital
markets, where he directly managed public and private capital transactions of equity and debt, led M&A and special
advisory processes including take-privates. From 2008 to 2017, Mr. Facchina served as a Partner, Co-Portfolio Manager
and the Chief Operating Officer of Ramsey Asset Management, an institutional investment management firm, and from
1998 to 2008 Mr. Facchina led the technology, media, and communications and healthcare investment banking groups of
FBR Capital Markets. Mr. Facchina currently serves as an independent director for ViON Corporation and MilltechFX, and
is Advisor to the CEO of Johanna Foods Inc, where he chairs the Audit Committee. Previously, among other directorships
and committee posts, Mr. Facchina served on the Board of Web.com (Nasdaq: WEB), where he led Corporate Governance.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
None
Philip Krause, MD
Non-Executive Member of the Board of Directors
Experience and expertise
With over 30 years of experience at the Food and Drug Administration, Dr. Krause has a unique combination of
scientific, regulatory, clinical, and public health experience. He is a physician with board certification in internal medicine
and infectious diseases and a researcher with over 100 publications on topics spanning clinical evaluation of vaccines, viral
pathogenesis and immunology, and biological product development. He is currently an independent consultant, providing
strategic and regulatory advice related to biological product development. He recently served as deputy director of FDA’s
Office of Vaccines Research and Review, where he led assessments of biological products for evaluation and licensure and
helped to oversee the development and evaluation of all vaccines authorized and licensed in the US from 2011-2021. He
graduated from Yale Medical School (MD), Florida State University (MBA) and the University of Illinois (BS and MS in
Computer Science). Dr Krause has a strategic advisory consulting role with Mesoblast, providing advice on regulatory
strategies.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
None
Michael Spooner, BCom
Non-Executive Member of the Board of Directors - resigned effective September 26, 2023
Experience and expertise
Mr. Spooner served on the Board of Directors from 2004 to September 2023. During this period he has filled
various roles including as Chairman from the date of the ASX public listing in 2004 until 2007, Chair of the Audit and Risk
Committee as well as a member of the Remuneration Committee . Over the past several years Mr. Spooner has served on
the board of directors in various capacities at several Australian and international biotechnology companies, including
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BiVacor Pty Ltd (2009-2013), Advanced Surgical Design & Manufacture Limited (2010-2011), Peplin, Inc. (2004-2009),
Hawaii Biotech, Inc. (2010-2012), Hunter Immunology Limited (2007-2008), and Ventracor Limited (2001-2003). He has
been the Chairman of Simavita Ltd since May 2016 and Chairman of MicrofluidX since February 2018. Prior to returning
to Australia in 2001, he spent much of his career internationally where he served in various roles including as a partner to
PA Consulting Group, a UK-based management consultancy, and a Principal Partner and Director of Consulting Services
with PricewaterhouseCoopers (Coopers & Lybrand) in Hong Kong. In addition Mr Spooner has owned and operated
several international companies providing services and has consulted to a number of American and Asian public
companies.
Other current directorships of listed public companies
Former directorships of listed public companies within the last 3 years
Chairman, Simavita Ltd (2016 - 2021)
Company Secretary
Niva Sivakumar – BCom, LLB
Joint Company Secretary
Experience and expertise
Ms. Sivakumar joined Mesoblast’s legal team in 2014 and is a member of the Company’s Intellectual Property
Committee. Previously, she was a senior associate in the corporate and commercial teams at major law firm, Dentons, and
a senior lawyer at K&L Gates. Ms. Sivakumar has a Commerce/Law degree from the University of Melbourne.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
None
Paul Hughes – BPharm, BBus (Banking & Finance)
Joint Company Secretary
Experience and expertise
Mr. Hughes began working with Mesoblast in February 2019 and has served as the Company’s Global Head of
Corporate Communications since December 2020. He has an extensive background as an investment banker and corporate
advisor for firms including Macquarie Bank and Commonwealth Bank of Australia. Mr. Hughes has a Bachelor of
Pharmacy and Bachelor of Business (Banking & Finance) from Monash University, Melbourne.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
None
Senior Management – Key Management Personnel
Silviu Itescu, MBBS (Hons), FRACP, FACP, FACRA
Chief Executive Officer (CEO)
Executive Member of the Board of Directors
Experience and expertise
Dr. Itescu has served on the Board of Directors since the Company's founding in 2004, was Executive Director
from 2007, and became Chief Executive Officer and Managing Director in 2011. Prior to founding Mesoblast in 2004, Dr.
Itescu established an international reputation as a physician scientist in the fields of stem cell biology, autoimmune
diseases, organ transplantation, and heart failure. Dr Itescu has been a faculty member of Columbia University in New
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94
York, and the University of Melbourne and Monash University in Australia. In 2013, Dr Itescu received the inaugural Key
Innovator Award from the Vatican’s Pontifical Council for Culture for his leadership in translational science and clinical
medicine in relation to adult stem cell therapy. In 2011, Dr. Itescu was named BioSpectrum Asia Person of the Year. Dr.
Itescu has consulted for various international pharmaceutical companies, has been an adviser to biotechnology and health
care investor groups, and has served on the board of directors of several publicly listed life sciences companies.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
None
Eric Rose, MD
Chief Medical Officer (CMO)
Executive Member of the Board of Directors
Experience and expertise
Dr. Rose is a highly respected physician scientist with focus on clinical investigation, drug discovery, biodefense,
and health policy. As a world-renowned heart surgeon and scientist, Dr. Rose led the Columbia Presbyterian heart
transplantation program from 1982 through 1992 and made history in 1984 when he performed the first successful pediatric
heart transplant. From 1994 through 2007, he served as Chairman of Columbia University’s Department of Surgery and
Surgeon-in-Chief of Columbia Presbyterian Medical Center in New York. During this time his leadership of the NIH
supported program Randomized Evaluation of Mechanical Circulatory Support in Heart Failure (REMATCH) resulted in
the first FDA approval of an implantable left ventricular assist device for long term circulatory support, spawning an entire
new industry. From 2007-2011, Dr. Rose served on the National Biodefense Scientific Board which advises the United
States Health and Human Services Secretary on biodefense, influenza, and emerging diseases. In 2007 he was appointed
Chairman and CEO of SIGA Technologies where he oversaw development of the first antipoxviral drug approved in the
United States, TPOXX for the treatment of smallpox. Dr. Rose played a key role in obtaining FDA approval of the drug in
2019, and he was responsible for securing contracts with BARDA under which the US Government has procured 1.7
million courses of TPOXX for more than US$1billion into the Strategic National Stockpile (SNS). Dr. Rose’s tenure on the
ABIOMED board ended in December 2022 with the sale of the company to Johnson & Johnson for $17.7 billion.
Other current directorships of listed public companies
None
Former directorships of listed public companies within the last 3 years
Chairman, SIGA Technologies, Inc. (2017 - 2021)
Non-executive Director, ABIOMED, Inc. which was acquired by Johnson & Johnson. (2007 - 2012, 2014 - 2022)
Other Senior Management
Andrew Chaponnel, BCom, CAANZ
Chief Financial Officer (interim)
Mr. Chaponnel has around 25 years of experience in finance roles including 13 years with Mesoblast, initially as
the Group Financial Controller (6 years), then as Head of Finance (3 years) and now as interim Chief Financial Officer for
the past three years. As part of Mesoblast Group finance leadership he has been integral to the implementation and
maintenance of our borrowing arrangements, various strategic partnerships, equity placements, the NASDAQ IPO and
leads both ASX and NASDAQ financial reporting. Previously Mr. Chaponnel has held several roles including management
roles in chartered accountancy, logistics, retail and a CFO role within construction before moving into Healthcare. He is a
member of the Chartered Accountants of Australia & New Zealand.
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Peter Howard, BSc, LLB (Hons)
Group General Counsel and Corporate Executive, Chair of the Patent Committee
Mr. Howard has served as our Group General Counsel and Corporate Executive, and Chair of the Patent
Committee, since July 2011. As external counsel and partner at Australian law firm, Middletons (now, K&L Gates), Mr.
Howard has been integrally involved with Mesoblast since its inception and public listing on the ASX in 2004. More
generally, Mr. Howard has extensive experience with many biopharmaceutical firms and major research institutions,
covering public listings, private financings, strategic, licensing, intellectual property and mergers and acquisition activities.
He has done so in several roles, including as a partner at a major law firm, entrepreneur, director and senior executive.
Justin Horst, BS
Head of Manufacturing
Justin Horst has 18 years of experience in clinical cell therapy manufacturing and industry development. During
the past eight years, he has been Mesoblast’s Deputy Head of Manufacturing, with accountability for chemistry,
manufacturing and control of the manufacturing processes. Before joining Mesoblast, Mr. Horst was at Lonza Walkersville
Inc. for 10 years, holding numerous senior level positions within the manufacturing, project management, and business
development groups. At Lonza, he was instrumental in the establishment of the contract manufacturing business, and
managed multiple manufacturing teams supporting numerous custom supply processes. Mr. Horst obtained his B.S. in
Biology from Towson University in Maryland.
Dagmar Rosa-Bjorkeson, MS, MBA
Chief Operating Officer until November 1, 2023 from which time has been a part-time consultant.
Dagmar Rosa-Bjorkeson has more than 25 years of global experience in the pharmaceutical industry, including
executive leadership in corporate and product strategy, market development and operational execution. She has led
multiple successful product launches, including Gilenya® for multiple sclerosis and Elidel® for atopic eczema. During her
17 years at Novartis, Ms. Rosa-Bjorkeson was Vice President and Head of its Multiple Sclerosis Business Unit; Vice
President, Business Development and Licensing in the United States; and Country Head and President for Novartis
Sweden. More recently, she served as Executive Vice President and President, Biosimilars, at Baxalta, now a wholly
owned subsidiary of Takeda Pharmaceutical Company. Ms. Rosa-Bjorkeson was also Executive Vice President and Chief
Strategy and Development Officer at Mallinckrodt Pharmaceuticals. She holds an MBA in Marketing, an MS in Chemistry
and a BS, Chemistry from the University of Texas.
Michael Schuster, MBA
Pharma Partnering
Mr. Schuster, who joined Mesoblast in 2004, leads the Group's partnering discussions. Previously he was the head
of the Group's investor relations outreach program and was part of the founding executive team at both Mesoblast Limited
and Angioblast Systems, Inc. Mr. Schuster was Executive Vice President of Global Therapeutic Programs from 2010 to
2013 and was the Director of Business Development and Vice President of Operations from 2004 to 2010. He holds an
undergraduate degree in science from Tufts University, a Master’s degree in Immunology & Microbiology from New York
Medical College, and an MBA from Fordham University in New York.
Paul Simmons, PhD
Scientific Advisor to the Chief Executive Officer
Dr. Simmons served as our Head of Research and New Product Development since 2011 and transitioned to
Scientific Advisor to the Chief Executive Officer in the current year. He has nearly 30 years of experience in stem cell
research, especially research in basic hematopoiesis and in precursor cells for the stromal system of the bone marrow, and
served as President of the International Society of Stem Cell Research, or ISSCR, from 2006 to 2007. Prior to joining
Mesoblast, Dr. Simmons held the C. Harold and Lorine G. Wallace Distinguished University Chair at the University of
Texas Health from 2008 to 2011 and served as the inaugural Professor and Director of the Centre for Stem Cell Research at
the Brown Foundation Institute of Molecular Medicine from 2006 to 2011. Dr. Simmons is, or has served as, an associate
editor, a member of the editorial board, or a reviewer on multiple scientific and medical journals including Experimental
Hematology, Cytotherapy and Stem Cell Research, Cell Stem Cell, Stem Reports, Science and Nature.
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Geraldine Storton, BSc, MMS, MBA
Head of Regulatory Affairs and Quality Management
Ms. Storton is a seasoned pharmaceutical executive with more than 30 years’ experience across the full value
chain of Pharmaceutical and Medical Device Research and Development, production and commercialization worldwide.
She has an extensive background in regulatory affairs and quality, most recently as a consultant to cell therapy companies.
Prior to this, Ms. Storton held executive roles at Hospira, and its predecessor companies in both regulatory affairs and
quality, with a focus on major program management. As Vice President, Program Management, Quality, at Hospira
headquarters in Chicago, she led a company-wide quality remediation program to improve compliance in manufacturing
across 15 facilities worldwide. As Regional Director, Commercial Quality ANZ, Asia and Japan, Ms. Storton was
responsible for quality oversight and management of all products sold in Asia Pacific countries. Her responsibilities
included regulatory compliance, batch release, field actions, complaints management, change control, due diligence and
new product launch. As director of global regulatory operations, Ms. Storton managed development and registration of new
products and on-market management of the existing product portfolio for all Hospira’s products developed or
manufactured within Asia Pacific for global distribution. She joined Mesoblast in December 2015.
Fiona See, PhD
SVP and Head, Translational Research
Dr. Fiona See is an experienced scientist and leader in translational research and development within the
biotechnology sector. Currently serving as the Senior Vice President and Head of Translational Research at Mesoblast in
New York, she provides strategic scientific leadership across the lifecycle of mesenchymal lineage stromal cell (MLC)
therapy products, focusing on cardiovascular, musculoskeletal, and immunological diseases. Dr. See has successfully led
teams in developing nonclinical pharmacology/toxicology packages and product characterization. Previously, Dr. See
served as Vice President and Senior Director of Translational Development at Mesoblast, developing and overseeing
nonclinical and translational strategies. Dr. See holds a PhD and a Bachelor of Laws/Bachelor of Science (Honors) from
Monash University. She has conducted NIH-funded research at NYU Langone School of Medicine, Columbia University,
and NHMRC-funded research at The University of Melbourne, focusing on stem cell-based platforms and therapies for
heart disease. She has published numerous peer-reviewed articles in respected journals, reflecting her contributions to
translational research and therapeutic innovation.
There are no family relationships among any of our directors and senior management. The business address of
each of our directors and senior management is Mesoblast Limited, Level 38, 55 Collins Street, Melbourne, VIC 3000,
Australia.
The Mesoblast board of directors (the "Board”) presents the 2023/2024 Remuneration Report, which has been
prepared in accordance with the relevant Corporations Act 2001 (Cth) (“Corporations Act”) and accounting standards
requirements.
The remuneration report sets out remuneration information for our company’s key management personnel
(“KMP”) as defined in the International Accounting Standards 24 ‘Related Party Disclosures’ and the Australian
Corporations Act 2001 for the financial year ended June 30, 2024.
(Start of the Remuneration Report for Australian Disclosure Requirements)
Introductory Comments from Bill Burns, Nomination and Remuneration Committee Chairman
Throughout the year there was a concerted focus on advancing the Biologics License Application (BLA)
submission for paediatric Graft versus Host Disease and continued dialogue with the United Sates Food and Drug
Administration (FDA) involving all programs in our late-stage clinical pipeline. On March 26, 2024, the FDA informed
Mesoblast that following additional consideration the available clinical data from the Phase 3 study MSB-GVHD001
appeared sufficient to support submission of the proposed BLA for remestemcel-L for the treatment of pediatric patients
with steroid-refractory acute graft versus host disease (SR-aGVHD). In July 2024, Mesoblast resubmitted our BLA for
remestemcel-L for the treatment of pediatric SR-aGVHD.
During the year, Mesoblast progressed our Chronic Low Back (CLBP) and Chronic Heart Failure (CHF)
programs. The FDA informed the Group that it supports an accelerated approval pathway for rexlemestrocel-L in patients
with end-stage ischemic heart failure with reduced ejection fraction (HFrEF) and a left ventricular assist device (LVAD).
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The confirmatory Phase 3 trial of rexlemestrocel-L in patients with CLBP due to inflammatory degenerative disc disease of
less than five years duration has commenced enrollment at multiple sites across the United States.
Joe Swedish, who served as chair since March 2019, stepped down from the Board chair role during the year.
Jane Bell took over as Chair of Board from April 2024. Joe remains with us as a Board director until completion of his
term at the Annual General Meeting later this year.
The Group raised proceeds of US$40 million and US$25 million in December 2023 and March 2024 respectively,
strengthening our balance sheet and providing the funds necessary to enable all existing product development and research
programs to continue and our next major technical and clinical development milestones to readout.
Cash burn was reduced during the year through the successful executing of the cost containment plan announced
in August 2023. Overall, net operating cash usage was reduced by 23% for FY24 as compared to FY23.
The cost containment plan included the following remuneration related initiatives which were successfully
introduced and executed during FY24:
•
The CEO and CMO volunteered base salary reductions of 30% for a 12-month period to August 2024. In
compensation for the reduction in cash pay, an option grant was approved by shareholders with an approval vote
of 95% at the 2023 AGM, increasing their long-term equity-based at risk pay for further alignment of their
interests with shareholders;
•
Other members of our management team also volunteered to reduce cash pay and receive long-term equity based
at-risk pay in compensation;
•
Cash payment of the STI relating to the fiscal year ended June 30, 2023 has been deferred until an FDA approval
for SR-aGVHD; and
•
Non-executive directors voluntarily deferred 50% of their director fees until an FDA decision and agreed to
receive the remaining 50% of their fees in equity, approved by shareholders at the 2023 AGM. No cash payment
will be made until a decision is made on FDA approval.
Despite the significant strides made during FY24, our immediate goal of obtaining FDA marketing authorization
for remestemcel-L for the treatment of pediatric SR-aGVHD has not yet been achieved and therefore the cost containment
plan will continue in FY25 for the following remuneration related initiatives continuing:
•
The CEO and CMO voluntary base salary reductions of 30% will continue through until August 2025. In
compensation for the reduction in cash pay, an option grant will be proposed which will increase their long-term
equity-based at-risk pay, further aligning their interests to those of shareholders, subject to shareholder approval.
•
Other management team members will continue to be able to sacrifice cash pay for options in FY25.
•
The Board has decided against awarding any increases to fixed remuneration prior to the FDA decision on
pediatric SR-aGVHD.
•
Cash payment of the STI relating to the financial year ended June 30, 2024 has been deferred and is dependent on
an FDA approval (further detail on this below). Subsequent to FY24, there has been a modification to the STI
plan providing all employees with the choice to elect into receiving an option grant in lieu of cash payment of
their STI entitlements for the years ended FY23 and FY24; and
•
Non-executive directors are continuing to voluntarily defer 50% of their director fees until an FDA decision and
have agreed to receive 50% of their fees in equity, subject to shareholder approval. Aside from retiring directors,
no cash payments will be made until a decision is made on FDA approval.
Our responsible management of remuneration was positively received by investors with a vote approval of 94%
for the remuneration report resolution at the 2023 AGM.
FY24 Remunerations Outcomes
Mesoblast's remuneration mix remains weighted towards long term performance, aligning executive outcomes to
long term sustainability and success. Milestone LTI awards in the biotechnology sector have a higher risk profile than those
in the broader market and may not materialize to levels anticipated at grant or in the general market. Our decision to
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98
maintain this framework is consistent with the preference of our investors for long term at risk pay that is aligned to
shareholder experience and returns.
Within our LTI incentives, executives must meet both milestone and service requirements before vesting can
occur. 88% of the CEO's Nov 2023 grant and 66% of his total outstanding milestone-based LTI incentives have not yet
met milestone achievement requirements to be eligible for vesting. The remaining portion of the LTI's met milestone
requirements and these options become eligible to vest once time-based service requirements are met (see table 6a). After
application of both milestone and service requirements, 7% of the CEO’s total milestone-based options vested in FY24. At
June 30, 2024, 100% of these vested LTI options were underwater and had zero intrinsic value.
The Board assessed our Group’s short-term incentive (STI) key performance indicator (KPI) performance for the
financial year ended June 30, 2024, as achieving 100% of maximum after significantly exceeding KPIs related to our
financing clinical and regulatory strategy. Nevertheless, given the criticality of the BLA resubmission in July, Board
discretion has been exercised not to pay the STI unless and until the FDA provides marketing authorization for SR-
aGVHD. On achievement, Mesoblast will pay the CEO the maximum STI outcome plus 20%.
Subsequent to FY24 and prior to payment being due, the Board approved a modification to the STI plan providing
all employees with the choice to elect into receiving an option grant in lieu of cash payment of their STI entitlements for
the years ended FY23 and FY24. The level of participation and the terms of the modification are yet to be determined at
the date of this report.
On balance, we believe the remuneration framework, including several years’ absence of fixed remuneration
increases for executives, the Board’s decision to defer cash payment of the FY23 and FY24 STI until FDA approval for
SR-aGVHD has been achieved, and the continuation of cost containment remuneration initiatives in FY24 ensure our
remuneration strategy is appropriate for this stage of our Group’s growth and is strongly aligned to our key milestones and
shareholder value.
I invite you to read the remainder of the remuneration report and welcome your feedback.
Bill Burns
Nomination and Remuneration Committee Chairman
Key Management Personnel (KMP)
Key management personnel (KMP), defined as individuals who have authority and responsibility for planning,
directing and controlling the activities of the company, directly or indirectly, and including all directors, are listed in Table
1.
Table 1 – Mesoblast KMP during FY2024, including to the Date of this Report
Name
Position
Country
Portion of FY2024 year
served as KMP
Non-executive directors
Jane Bell
Independent Chair of Board (from
April 30, 2024)
Member, Nomination and
Remuneration Committee
Member, Audit and Risk Committee
Australia
Full Year
Joseph Swedish
Independent Chair (until April 30,
2024), Board of Directors
Member, Audit and Risk Committee
Member, Nomination and
Remuneration Committee
US
Full Year
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William Burns
Independent Vice Chair, Board of
Directors
Chair, Nomination and
Remuneration Committee
Switzerland
Full Year
Philip Facchina
Independent Non-executive Director
Member, Audit and Risk Committee
Member, Nomination and
Remuneration Committee
US
Full Year
Philip Krause
Independent Non-Executive
Director to August 28, 2023
Non-independent Non-executive
Director from August 29, 2023
Member, Nomination and
Remuneration Committee until
August 28, 2024
US
Full Year.
Michael Spooner
Independent Non-executive Director
Chair, Audit and Risk Committee
Member, Nomination and
Remuneration Committee
Singapore
Resigned effective
September 26, 2023
Executive directors
Silviu Itescu
Chief Executive Officer
Executive Director
Australia
Full Year
Eric Rose
Chief Medical Officer
Executive Director
US
Full Year
6.B
Compensation
KMP Remuneration Governance
The Board is responsible for Mesoblast’s remuneration strategy and approach. The Nomination and Remuneration
Committee advises the Board on remuneration and incentive policies and practices generally, and makes specific
recommendations on remuneration packages and other terms of employment for executive Directors, other senior
executives and non-executive Directors.
The Nomination and Remuneration Committee is wholly comprised of independent members. The board is
satisfied that all members of the Nomination and Remuneration Committee during the reporting period are independent.
The Nomination and Remuneration Committee is primarily responsible for making recommendations to the Board
on:
•
Board appointments
•
Non-executive director fees
•
Executive remuneration framework
•
Remuneration for executive directors, namely the CEO, CMO and other key executives
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100
•
Short-term and long-term incentive awards
•
Share ownership plans
The Nomination and Remuneration Committee’s objective is to ensure remuneration policies are fair and
competitive having regard for industry benchmarks whilst being aligned with the objectives of our company.
The Committee receives proposals from the executive team, which it critically reviews. When appropriate the
Nomination and Remuneration Committee will seek advice or recommendations from independent expert consultants,
including benchmarking studies. Advice provided by consultants during the year did not constitute a ‘remuneration
recommendation’ as defined in section 9B of the Corporations Act and was received free from any undue influence by Key
Management Personnel to whom the advice related.
Executive Remuneration Strategy
The remuneration strategy is designed to ensure Mesoblast can:
•
Attract and retain experienced leaders and emerging experts in an innovative field and on a global basis
•
Reward performance that will lead in the long term to improved patient outcomes and increased
shareholder wealth.
Our team is small. Mesoblast has only 73 employees, 57% of whom are in the US, with the remainder in
Australia, Singapore and Switzerland. Retaining these employees, who often are at the top of their respective fields, is
imperative in ensuring Mesoblast can continue to work towards what are difficult, complex and long-term goals.
Biopharmaceutical product development is a highly specialized and speculative undertaking and it involves a
substantial degree of risk. To achieve and maintain long term profitability, companies must successfully develop product
candidates, obtain regulatory approval, and manufacture, market and sell those products for which regulatory approval is
obtained. If this occurs, revenues depend on the size of markets in which product candidates receive approval, the ability to
achieve and maintain sufficient market acceptance, pricing, reimbursement from third-party payors, and adequate market
share for our product candidates in those markets. Not all companies succeed in these activities, and not all companies
generate revenue from product sales that is significant enough to achieve profitability.
To have a chance of success, it is imperative that executives
a)
possess the specialized skills to understand the complex products being developed and the various
regulatory requirements imposed across the globe
b)
apply high degrees of discipline to ensure research and trials are undertaken safely and effectively, to a
rigorous standard and schedule, within tight budget constraints
c)
seek to deliver earlier, with lower costs, key, well-defined milestones critical to progressing Mesoblast
technology
d)
stay focused on the end goal of commercialization.
While it may be many years from initial research until milestones lead to profitable outcomes, this does not reduce
the importance of the milestones themselves. Without the interim milestone steps on the way to therapy commercialization,
the extensive safety and efficacy data required would not be sufficient and approval by global regulatory authorities would
not be achievable. Time and costs are an important component in this process of research, testing and milestone
achievement, as both have compounding effects on shareholder value.
To address the above, Mesoblast’s remuneration framework comprises:
-
competitive fixed remuneration
-
annual incentive payments contingent on intensive research, approvals and trials being undertaken on
time and budget
-
longer term milestone-based incentive payments
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101
-
payment delivered, in part, as options, which conserves cash, aligns with shareholder interests, and
focuses executives on strategy, risk management, and execution that optimizes shareholder value.
Mesoblast generally sets cash-based STIs at a lower quantum than option-based LTIs to conserve cash flow, focus
executives on value creation, and align executives with shareholders.
The current average tenure of our executive team of 10 years suggests that the framework works well to attract
and retain appropriate executive leadership.
Executive Remuneration Framework
Further details on the Mesoblast Executive Remuneration Framework is provided in Table 2 – Executive
Remuneration Framework.
Table 2 – Executive Remuneration Framework
Strategic Rationale
Attract
and
retain
key
personnel on a global basis via
competitive remuneration.
Comply with regional statutory
and customary benefits (e.g.,
superannuation in Australia;
medical insurance in the US.)
Focuses attention on key KPIs
(in areas such as clinical,
financial
and
partnering
strategy,
manufacturing,
commercial, or organizational
structure and development)
under
cost
and
time
constraints that will lead to
long-term
improvement
in
patient
outcomes
and
shareholder wealth.
Serves multi-pronged purpose:
- Aligns remuneration outcomes
with
shareholder
wealth
creation.
- Provides a framework for
wealth creation by prioritizing
key objectives that are critical
for long-term profitability.
- Rewards
speed
of
achievement, that can have
long
term
compounding
effects
- Retains employees via deferral
- Provides
value
only
if
milestones lead to increases in
share price, aligning with the
shareholder experience.
- Conserves cash.
- Enables risk management via
malus.
Process
Assessed annually on market
relativities
in
employee's
domicile based on position
accountabilities.
The
Nomination and Remuneration
Committee
makes
specific
recommendations to the board
on remuneration packages for
senior executives for approval.
Paid annually for performance
against annual corporate and
individual
KPIs.
The
Nomination
and
Remuneration Committee sets
the CEO’s KPIs. These are
used to measure company
performance,
which
determines the pool available
for
other
employees.
Allocations from that pool for
senior
management
are
determined with reference to
individual KPIs set by the
CEO. Resulting outcomes are
approved by the Nomination
and Remuneration Committee.
The
Nomination
and
Remuneration
Committee
assesses
LTI
milestone
achievement
for
vesting
eligibility.
Fixed Pay
Performance-based Remuneration
Short-term Incentives
Long-term Incentives
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102
Eligibility
All employees
All employees hired on or
before March 31, 2024 are
eligible
for
consideration.
Employees hired during the
year are recognized on a pro-
rata basis.
All eligible participants who are
in
positions
to
influence
achievement of our long- term
outcomes and, where required,
for attraction and retention.
Quantum of
opportunity
Set
according
to
each
position’s accountabilities, the
incumbent’s experience and
qualifications,
and
regional
market relativities.
Set as a percentage of fixed
pay. Quantum generally lower
than LTI to conserve cash.
Current CEO maximum STI:
50% of Fixed Remuneration.
Current CMO maximum STI:
50% of Fixed Remuneration.
Set using a percentage of fixed
pay as a guideline.
Current CEO maximum LTI:
approximately 200% of fixed
remuneration.
Current CMO maximum LTI:
100% of fixed remuneration.
The actual grant value for the
CEO and CMO LTI may vary
year
on
year
from
this
proportion based on various
factors being taken account
including:
- shareholder dilution
- internal relativities
- share price volatility
Delivered as
Cash.
Cash.
Subsequent to FY24, our STI
plan was modified and will
provide all employees with
the choice to receive an option
grant in lieu of cash payment
of their STI entitlements for
the years ended FY23 and
FY24.
Options over ordinary shares in
Mesoblast Limited with a 7-year
expiry date. Option exercise
price will be based on the higher
of the VWAP of the 5 ASX
trading
days
up
to
board
approval of the grant, and the
last closing price of an ordinary
share on the ASX at board
approval.
Performance and
service period
N/A
1 year
Three years, with provision for
earlier vesting limited to one
third per year to (a) encourage
speed of achievement, (b) defer
material
amounts
for
better
governance and (c) encourage
executive focus on achievements
that have a longer term impact
on shareholder value.
Fixed Pay
Performance-based Remuneration
Short-term Incentives
Long-term Incentives
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103
Discretion, malus
and clawback
N/A
The board has the authority to
use its discretion to amend
individual outcomes “in year”,
including down to zero, prior
to any payment. Additionally,
effective FY24 we adopted a
policy for the recovery of
erroneously awarded incentive
compensation.
The
board
has
ultimate
discretion in determining vesting
outcomes. Until options are
exercised, the board may also
apply discretion in situations
where executives have behaved
dishonestly or fraudulently to
lapse options (unvested and
vested). Additionally, effective
FY24 we adopted a policy for
the recovery of erroneously
awarded
incentive
compensation.
Cessation of
employment
N/A
No award will be made to
employees who have ceased
employment unless the Board
exercises it's discretion.
Unvested options are forfeited
unless
Board
exercises
discretion. Vested options can be
retained
subject
to
being
exercised within a certain period
specified in our Employee Share
Option Rules (usually 60 days of
cessation).
Hedging
The Company’s share trading policy prohibits hedging via the Company’s derivatives.
Oversight
Individual outcomes are reviewed and approved first by the Nomination & Remuneration
Committee and then the Board.
Fixed Pay
Performance-based Remuneration
Short-term Incentives
Long-term Incentives
Remuneration Mix
FY24 target remuneration mix at maximum for the CEO and the CMO is described in Figure 1.
Figure 1 – Executive KMP Remuneration Mix.
28.6%
40.0%
14.3%
20.0%
57.1%
40.0%
TFR
STI
LTI
0%
10%
20%
30%
40%
50%
60%
70%
80%
90%
100%
CEO
CMO
The actual grant value year-on-year may vary from the target remuneration mix depending on factors such as:
•
Dilution considerations
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104
•
Internal relativities
•
Date of grant
Responses to frequent questions on the Mesoblast framework
The following table presents responses to common queries on the Mesoblast remuneration framework.
Table 3 – Executive Remuneration Framework
Why do you use milestone performance
measures for the STI and LTI?
Traditional financial metrics are not meaningful, nor can they be effectively
used to accurately reflect the performance of our company. What creates
lasting shareholder value are successful outcomes from research and
development, entry into new collaborations and achievement of other planned
and well considered corporate objectives. Success will only result in
significant reward under the LTI if the market values our achievements. If it
does, our share price increases. The LTI options become valuable. If not, the
options have no intrinsic value. This combination of milestones and payment
in options work in tandem for fair payment for performance aligned with
shareholder returns. This is a standard biotechnology company practice.
Why does some of the long term incentive
award vest earlier than a three year
period?
Within biotechnology, basing long term incentives on achievement of
performance milestones is an established method for aligning pay with
performance. The other factor that is critical is time. While we allow three
years for milestones, earlier achievement is better, because if milestones are
achieved earlier then less cash will have been used by the Group to support
the program and associated overheads than if achieved at the end of 3 years.
Therefore, we have configured the plan to allow for early vesting for early
achievement, but only to a point. We still insist that even if all milestones are
achieved early, some options remain unvested for 3 years, to ensure that, if
given a choice with a limited budget, employees focus on those milestones
most likely to deliver the most value over the longer term, as well as
encouraging employee retention. We believe that this framework is
innovative, and a great fit for the nature of our business. We acknowledge it
does not look and feel like a typical ASX-listed company LTI, and therefore
may not meet the standard guidelines applied by many, but we are not typical.
We are open to considering alternatively designed incentives that address the
value drivers of milestone achievement, time to achieve them, prioritization of
milestones given limited resourcing, and impact on longer term share price,
but so far we have not found any quite as effective.
What
is
Mesoblast’s
position
on
diversity?
The Group values diversity and recognizes the benefits it can bring to the
organization’s ability to achieve its goals. Diversity can lead to a competitive
advantage through broadening the talent pool for recruitment of high quality
employees, by encouraging innovation and improving a corporation’s
professionalism and reputation. Accordingly, the Group is committed to
promoting diversity within the organization and has adopted a formal policy
outlining the Group’s diversity objectives.
With respect to gender diversity, as at June 30, 2024, 52% of the Company’s
employee base were female and 30% of the Company’s senior executives
were female. In April 2024, a female Board Chair was appointed. The Board
is conscious of the gender imbalance at board level (with only one of the four
non-executive directors being female). The Board has an objective to increase
the number of female board members as vacancies arise and circumstances
permit.
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105
What is Mesoblast's position on STI
deferral?
STI deferral is applied as and when considered appropriate. Payment of both
the FY23 and FY24 STI has been deferred and is dependent on FDA
marketing authorization for SR-aGVHD being achieved.
Why is there no consideration of ENS
(Environment and Sustainability) issues in
the STI or LTI vesting considerations?
Mesoblast’s mission to bring to market innovative medicines comprised of
naturally-occurring cellular materials to treat serious and life-threatening
illnesses is fundamentally consistent with ENS principles, although there are
relevant supply chain and carbon footprint considerations. At this stage,
Mesoblast’s physical footprint is limited to office and laboratory space for its
employee base of less than 100, so while management is actively engaged in
reducing the Company’s carbon footprint, its ability to materially improve its
ENS impact is currently limited. We will continue to consider having ENS-
related remuneration milestones in the future, in particular if and when
Mesoblast has its own manufacturing facilities and approved products.
Mesoblast performance during FY2024
Table 4 provides share price performance data and selected financial results.
Table 4 – Company share price performance and selected financial results over the last five years
Currency
2024
2023
2022
2021
2020
Share price (ASX:MSB)
– closing at June 30
A$
0.99
1.14
0.61
1.98
3.25
– high for the year
A$
1.39
1.28
2.10
5.5
4.45
– low for the year
A$
0.26
0.68
0.61
1.72
1.02
Market capitalization at June 30
(millions)
A$
1,130
924
397
1,285
1898
– increase/(decrease) – (millions)
A$
206
527
(888)
-613
1160
– increase/(decrease) – as %
22%
133%
(69%)
(32)%
157%
Revenue (millions)
US$
5.9
7.5
10.2
7.5
32.2
– increase/(decrease) – as %
(21%)
(27%)
37%
(77)%
92%
Loss before income tax (millions)
US$
88.1
82.1
91.6
99.6
87.4
Net Assets (millions)
US$
480.4
501.8
497.0
581.4
549.3
Dividends paid
—
—
—
—
—
Return of Capital to Shareholders
—
—
—
—
—
During the year we advanced BLA submission for pediatric Graft versus Host Disease and had continued dialogue
with the FDA involving all programs in our late-stage clinical pipeline. On March 26, 2024, the FDA informed Mesoblast
that following additional consideration the available clinical data from the Phase 3 study MSB-GVHD001 appeared
sufficient to support submission of the proposed BLA for remestemcel-L for the treatment of pediatric patients with SR-
aGVHD. In July 2024, Mesoblast resubmitted our BLA for remestemcel-L for the treatment of pediatric SR-aGVHD.
During the year, Mesoblast progressed our Chronic Low Back (CLBP) and Chronic Heart Failure (CHF)
programs. The FDA informed the Company that it supports an accelerated approval pathway for rexlemestrocel-L in
patients with end-stage ischemic heart failure with reduced ejection fraction (HFrEF) and a left ventricular assist device
(LVAD). The confirmatory Phase 3 trial of rexlemestrocel-L in patients with CLBP due to inflammatory degenerative disc
disease of less than five years duration has commenced enrollment at multiple sites across the United States.
Mesoblast successfully executed on its cost containment plan announced in August 2023, reducing net operating
cash usage by 23% in FY24 as compared to FY23.
In relation to funding, with support from its shareholders the Company raised US$40 million and US$25 million
in December 2023 and March 2024, respectively. These raises strengthen our consolidated balance sheet as we undertake
activities for the potential launch and commercialization of remestemcel-L.
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106
In summary management executed on the following corporate achievements:
-
Completed US$40 million rights issue in December 2023.
-
Completed US$25 million capital raise in March 2024.
-
During the year we appointed Jane Bell as Board Chair.
In relation to our product candidates, management executed on the following achievements:
-
After our interactions with the FDA during the year, the FDA informed Mesoblast that following
additional consideration the available clinical data from its Phase 3 study MSB-GVHD001 appears
sufficient to support submission of the proposed BLA for remestemcel-L for treatment of pediatric
patients with SR-aGVHD.
-
During the year we advanced our resubmission of the BLA for approval of remestemcel-L in the
treatment of children with SR-aGVHD which ultimately resulted in the formal resubmission and
acceptance by the FDA of the filing in July 2024.
-
In March 2024 Mesoblast announced that the FDA supports an accelerated approval pathway for
rexlemestrocel-L, Mesoblast’s allogeneic mesenchymal precursor cell (MPC) product, in patients with
end-stage ischemic HFrEF and an LVAD. FDA provided this feedback in formal minutes to the company
following the Type B meeting held with FDA on February 21, 2024 for rexlemestrocel-L (Revascor®)
under the existing Regenerative Medicine Advanced Therapy (RMAT) designation.
-
The confirmatory Phase 3 trial of rexlemestrocel-L in patients with CLBP due to inflammatory
degenerative disc disease of less than five years duration has commenced enrollment at multiple sites
across the United States.
-
Entered into an agreement to develop a pivotal trial of Mesoblast’s lead product candidate Ryoncil®
(remestemcel-L) in the treatment of adults with SR-aGvHD with the Blood and Marrow Transplant
Clinical Trials Network (BMT CTN), a body including centers responsible for approximately 80% of all
US allogeneic BMTs. The BMT CTN is funded by the United States National Institutes of Health (NIH).
-
Following submission of results from the randomized controlled trial in children with hypoplastic left
heart syndrome (HLHS), a potentially life threatening congenital heart condition, Mesoblast was granted
orphan drug designation (ODD) and rare pediatric disease designation (RPDD) with the United States
Food and Drug Administration (FDA) for its allogeneic cell therapy Revascor® (rexlemestrocel-L) in the
treatment of the congenital heart disease HLHS.
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107
Remuneration outcomes for the year ended June 30, 2024
STI
The Corporate STI objectives and outcomes for FY24 are described in Table 5.
Table 5 - Group Performance against FY24 STI KPIs
Objectives/Performance Assessment
Maximum
as % of
total STI
Rating
Outcome
as
% of total
STI
Execute on clinical and regulatory strategy of our key product candidates (50%)
During the year we advanced our resubmission of the BLA SR-aGVHD which
ultimately resulted in the formal resubmission and acceptance by the FDA of the
filing in July 2024.
Entered into an agreement to develop a pivotal trial of remestemcel-L in the
treatment of adults SR-aGvHD with the Blood and Marrow Transplant Clinical
Trials Network (BMT CTN), a body including centers responsible for
approximately 80% of all US allogeneic BMTs,. The BMT CTN is funded by the
NIH.
Mesoblast progressed our CLBP and CHF programs with positive results. The
FDA’s OTAT granted RMAT designation for rexlemestrocel-L in the treatment of
CLBP associated with disc degeneration and supported an accelerated approval for
rexlemestrocel-L in patients with end-stage ischemic HFrEF and an LVAD.
Following submission of results from the randomized controlled trial in children
with HLHS, a potentially life threatening congenital heart condition, Mesoblast
was granted ODD and RPDD with the FDA for its allogeneic cell therapy
Revascor® (rexlemestrocel-L) in the treatment of the congenital heart disease
HLHS.
The Board has decided this objective has been met.
50%
100%
50%
Execute on Financing Strategy (20%)
In relation to Finance, there have been substantial achievements during the year.
We completed a capital raise of $40 million in December 2023 and $25 million in
March 2024. The Board has decided this objective has been met.
20%
100%
20%
Execute on Manufacturing Process Development & Cost Containment (30%)
During the year we enhanced our manufacturing processes. Separately, we reduced
our cash burn through the successful execution of the cost containment plan
announced in August 2023. Overall, net operating cash usage was reduced by 23%
for FY24 as compared to FY23, a target flagged in the 2023 annual report. The
Board has decided this objective has been met.
30%
100%
30%
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108
The Board assessed our Group’s performance on these KPIs for the financial year ended June 30, 2024 as
achieving 100% of targets, reflecting significant out performance in the face of changing priorities in reaction to the FDA's
communications in March that lead to Mesoblast's BLA resubmission.
Nevertheless, given the central nature of the BLA resubmission and our current cash position, the Board has
exercised negative discretion not to pay the FY24 STI unless and until Mesoblast receives FDA marketing authorization for
SR-aGVHD.
Considering the negative discretion to pay a zero STI if FDA marketing authorization is not achieved, the Board
has also increased the potential of the CEO’s payment by 20% if authorization is achieved.
Subsequent to FY24, there has been a modification to the STI plan providing all employees with the choice to
elect into receiving an option grant in lieu of cash payment of their STI entitlements for the years ended FY23 and FY24.
The level of participation and the terms of the modification are yet to be determined at the date of this report.
LTI
Two conditions must be met for milestone options to vest.
•
The milestone for that option must be met
•
Achievement must be within the performance period
•
The executive must be employed at the time of vesting
When LTI milestones are set it is not expected that all or any milestones will be achieved within the next 12
months. The LTI plan is designed to align the CEO objectives with creating long term shareholder value.
The vesting of the CEO’s LTI is based on meeting clinical and commercialization milestones, as well as
completion of licensing or collaboration agreements to build shareholder value.
The LTI vesting for our executive and non-executive KMPs, based on FY24 and prior year performance, along
with the financial year in which those options will vest once milestones have been met, are summarized in Tables 6a, 6b
and 6c.
Where an LTI milestone remains commercial in confidence it has been described in general terms. Many
milestones also have an associated delivery window and/or budget which are taken into account when determining if it was
achieved. Some clinical outcomes can be partially met depending on the quality and/or cost of results or extent of patient
participation.
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109
Table 6a – LTI Outcomes of CEO's milestone-based grants
Nov
2023(1)
Regulatory milestone
related to gain
alignment with FDA
on certain aspects of
the development
program for CHF.
242,000
FY24
—
— 242,000
—
—
100%
—
Financial & Business
Development related
milestone to
completion of a
strategic capital raise
to fund development
programs through to
key milestones.
726,000
FY24
—
—
564,667
161,333
—
100%
—
Regulatory and clinical
milestones in relation
to the remestemcel-L
and rexlemestrocel-L
platforms.
1,452,000
Pending
—
—
—
—
—
—
1,452,000
Total for Nov 2023
Grant
2,420,000
—
—
806,667
161,333
—
40%
1,452,000
Nov
2022(2)
Commercial and
clinical milestones in
relation to the potential
launch of remestemcel-
L.
1,395,000
Pending
—
—
—
—
—
—
1,395,000
Financial and business
development
milestones in relation
to remestemcel-L and
rexlemestrocel-L
platforms
930,000
Pending
—
—
—
—
—
—
930,000
Total for Nov 2022
Grant
2,325,000
—
—
—
—
—
—
2,325,000
Nov
2021(3)
Regulatory/
Commercialization
progress with respect
to our aGVHD
program and clinical
progress across the
Company’s lead
programs with specific
allocation for each
program milestone
based on priority.
510,000
FY23
— 510,000(7)
—
—
—
100%
—
110,000
FY24
— 110,000
—
—
—
100%
—
Completion of a
significant licensing/
collaboration
agreement to build
shareholder value and
other confidential
financing objectives.
620,000
Pending
—
—
—
—
—
—
620,000
Manufacturing
milestones related to
process development.
310,000
Pending
—
—
—
—
—
—
310,000
Total for Nov 2021
Grant
1,550,000
— 620,000
—
—
—
40%
930,000
Date
Granted
Milestone
No. of
Options
Year
Milestone
Achieved
FY in which the tranche has/will vest after factoring in
time- based vesting conditions
%
Vested
Pending
Pre FY24
FY24
FY25
FY26
FY27
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110
Nov
2020(4)
Clinical/
Commercialization
milestones related to
clinical and
commercialization
progress across the
Company’s lead
programs.
480,000
FY22
480,000
—
—
—
—
100%
—
Completion of a
significant licensing/
collaboration
agreement to build
shareholder value and
other confidential
financing objectives.
480,000
Pending
—
—
—
—
—
—
480,000
Manufacturing
milestones related to
process development.
240,000
FY22
240,000
—
—
—
—
100%
—
Total for Nov 2020
Grant
1,200,000
720,000
—
—
—
—
60%
480,000
Nov
2019(5)
Granting of a PDUFA
date for remestemcel-
L(6).
673,334
FY20
673,334
—
—
—
—
100%
—
US FDA approval of
remestemcel-L(6).
673,333
Pending
—
—
—
—
—
—
673,333
Total for Nov 2019
Grant
1,346,667
673,334
—
—
—
—
50%
673,333
Date
Granted
Milestone
No. of
Options
Year
Milestone
Achieved
FY in which the tranche has/will vest after factoring in
time- based vesting conditions
%
Vested
Pending
Pre FY24
FY24
FY25
FY26
FY27
(1)
This grant was approved by the Board on October 16, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
This grant was approved by the Board on October 17, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(3)
This grant was approved by the Board on September 8, 2021 and granted on November 29, 2021 after shareholder
approval for the grant was received at the AGM.
(4)
This grant was approved by the Board on July 16, 2020 and granted on November 24, 2020 after shareholder
approval for the grant was received at the AGM.
(5)
This grant was approved by the Board on July 20, 2019 and granted on November 27, 2019 after shareholder
approval for the grant was received at the AGM. 538,667 of the options granted were not milestone based and
have not been included in the above table. The 538,667 options were granted as a substitute for a reduction made
to the FY19 short-term cash bonus to conserve cash.
(6)
For the treatment of pediatric SR acute GVHD.
(7)
Regardless of when the milestone was achieved, the milestone vesting date is determined as the date of Board
approval. In this case Board approval was in July 2023.
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111
Table 6b – LTI Outcomes of CMO's milestone-based grants
Nov
2023(1)
Regulatory milestone
related to gain alignment
with FDA on certain
aspects of the
development program for
CHF.
148,000
FY24
—
— 148,000
—
—
100%
—
Regulatory and clinical
milestones in relation to
the remestemcel-L and
rexlemestrocel-L
platforms.
444,000
Pending
—
—
—
—
—
—
444,000
Strategic corporate
partnership milestones in
relation to the
remestemcel-L and
rexlemestrocel-L
platforms.
148,000
Pending
—
—
—
—
—
—
148,000
Total for Nov 2023
Grant
740,000
—
— 148,000
—
—
20%
592,000
Nov
2022(2)
Milestones related to the
regulatory progress of
remestemcel-L(3)
600,000
FY24
— 300,000
—
—
—
50%
300,000
Milestone related to the
clinical progress of the
Company’s lead products.
300,000
Pending
—
—
—
—
—
—
300,000
Total for Nov 2022
Grant
900,000
— 300,000
—
—
—
33%
600,000
Date
Granted
Milestone
No. of
Options
Year
Milestone
Achieved
FY in which the tranche has/will vest after factoring in
time- based vesting conditions
%
Vested
Pending
Pre FY24
FY24
FY25
FY26
FY27
(1)
This grant was approved by the Board on October 16, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
This grant was approved by the Board on October 17, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(3)
For pediatric patients with SR-aGVHD with the FDA, including the resubmission of its BLA and its potential
approval by the FDA.
Table 6c – LTI Outcomes of milestone-based grants to Phil Krause
Nov
2023(1)
Milestones related to the
regulatory progress of
remestemcel-L(3)
325,050
FY24
—
— 325,050(2)
—
—
100%
—
Regulatory milestones in
relation to the
remestemcel-L and
rexlemestrocel-L
platforms
659,950
Pending
—
—
—
—
—
—
659,950
Total for Nov 2023
Grant
985,000
—
— 325,050
—
—
33%
659,950
Date
Granted
Milestone
No. of
Options
Year
Milestone
Achieved
FY in which the tranche has/will vest after factoring in
time- based vesting conditions
%
Vested
Pending
Pre FY24
FY24
FY25
FY26
FY27
(1)
This grant was approved by the Board on October 24, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
The milestone was achieved in July 2024.
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112
(3)
For pediatric patients with SR-aGVHD with the FDA, including the resubmission of its BLA and its potential
approval by the FDA.
Table 7 represents remuneration paid to each executive KMP during the year as required by Section 300A of the
Corporations Act 2001.
Table 7 – Statutory remuneration paid to executive KMP
Short-term benefits
Base
salary
Short-
term
cash
bonus(1)
Annual
Leave/
Holiday
Pay(2)
Non-
monetary
benefits
Health and
Other
Benefits(3)
Post-
employm
ent
benefits
Super-
annuatio
n
Long-
term
benefits
Long
service
leave(2)
Share-
based
payments
Options
Other
Termi-
nation
benefits
Total
Statutory
Remuneration
% of
performance-
based
remuneration
Name
Year
Currency
$
$
$
$
$
$
$
$
$
$
%
Silviu Itescu
2024
A$
757,500
1,007,187
77,904
—
—
27,399
16,926
1,137,219
—
3,024,136
71%
Silviu Itescu
2023
A$
1,010,000
—
77,694
—
—
25,292
16,880
536,138
—
1,666,004
32%
Eric Rose
2024
A$
701,841
848,348
(5,984)
—
28,561
—
—
714,708
—
2,287,474
68%
Eric Rose
2023
A$
916,542
—
5,878
—
34,194
—
—
578,236
—
1,534,850
38%
Total Executive Directors
2024
A$
1,459,341
1,855,535
71,920
—
28,561
27,399
16,926
1,851,927
—
5,311,610
70%
Total Executive Directors
2023
A$
1,926,542
—
83,572
—
34,194
25,292
16,880
1,114,374
—
3,200,854
35%
Total Executive Directors
2024
US$(4)
959,079
1,219,458
47,266
—
18,770
18,006
11,124
1,217,086
—
3,490,790
70%
Total Executive Directors
2023
US$(4)
1,292,710
—
56,077
—
22,944
16,971
11,326
747,745
—
2,147,773
35%
(1)
Includes $457,812 related to the FY23 period but not yet paid and $549,375 related to the FY24 period but not yet
paid. Subsequent to FY23, the conditions of achievement of the FY23 STI was modified to make it dependent on
Mesoblast achieved FDA marketing authorization. Payment of the FY23 and FY24 bonus is dependent on
Mesoblast achieving FDA marketing authorization. Furthermore, subsequent to FY24, there has been a
modification to the STI plan providing all employees with the choice to elect into receiving an option grant in lieu
of cash payment of their STI entitlements for the years ended FY23 and FY24. The level of participation and the
terms of the modification are yet to be determined at the date of this report.
(2)
Annual leave and Long service leave reflect the movement in provision balances at June 30, 2024 compared with
June 30, 2023.
(3)
Includes health, dental, vision, life, long and short-term disability insurances.
(4)
The A$ results have been determined by calculating the average rate of the exchange rates on the last trading day
of each month during the period. A US$:A$ exchange rate of 1:0.6572 has been used for the year ended June 30,
2024 and 1:0.6710 for the year ended June 30, 2023.
Fixed remuneration
The CEO's fixed remuneration has not changed since 2015. Eric Rose was appointed as our CMO in FY22, his
monthly fixed remuneration has not changed since his appointment. Both our CEO and CMO volunteered base salary
reductions of 30% for a 12-month period to 30 June 2024. In compensation for the reduction in cash pay, an option grant
was approved by shareholders with an approval vote of 95% at the 2023 AGM, increasing the CEO and CMO's long-term
equity-based at risk pay for further alignment of their interests with shareholders.
Non-Executive Director (“NED”) Remuneration
As at June 30, 2024 the Board comprised of four NEDs; one based in Australia, two in the United States, and one
in Switzerland. These directors are global experts in the biopharmaceutical industry and capital markets, each with relevant
experience in biotechnology and/or healthcare industries.
The NED fees (in Table 8) reflect responsibilities and work involved with directing a company of Mesoblast’s
technological and geographical complexity, our financial position, regulatory and compliance context, and market practice
in each director’s domicile. The fee levels and structures reflect what is necessary to recruit and retain directors with global
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113
experience in this industry. There have been no changes to NED fees from last year. No NED fees were paid during the
year – 50% are deferred until an FDA approval decision and 50% were paid as options (more detail below).
Table 8 – Annual NED fees
(exclusive of superannuation where applicable for Australian directors)
As at June 30, 2024
Position
Currency
Board of
Directors
Audit and
Risk
Committee
Nomination
and
Remuneration
Committee
Chair(1)
A$
250,000
20,000
20,000
Vice Chair
A$
175,000
—
—
Member
A$
128,250
10,000
10,000
(1) Joe Swedish NED fees for his position as Chair of the Board were US$250,000 per annum.
The NEDs' fixed fees for their services are not to exceed a maximum fee pool of A$1,500,000, as approved by
shareholders at the 2018 Annual General Meeting.
NEDs do not receive performance-related remuneration and are not provided with retirement benefits other than
statutory superannuation. An exception is a performance based LTI grant to our non-independent NED, Philip Krause, in
relation to his role as a strategic regulatory advisor.
NEDs are reimbursed for costs directly related to conducting Mesoblast business. The key terms of NED service
are documented in a letter of appointment to the Board.
Mesoblast grants options to NEDs, usually at the start of their tenure. Additionally in FY24 options were granted
to replace NED cash fees which were reduced by 50%. Options in lieu of cash are typical in the biotechnology industry.
These options vest one third each after one, two and three years. For our NEDs, options are only forfeited if the director
engages in conduct that is adverse to the company or breach the terms of their engagement.
The grants enable Mesoblast to secure NEDs with global pharmaceutical experience cash-effectively. Governance
is not compromised because no performance or service conditions apply. The majority of shareholders voted in favor of our
NED LTI grants at the November 2023, 2022 and 2021 AGMs.
Philip Krause has been a non-executive director of Mesoblast since March 2022. Philip Krause was appointed to a
formal strategic advisory role on June 4, 2023 where he was remunerated at an hourly rate and the agreement was able to
be terminated on 15 written days notice. The consulting agreement was in addition to Philip Krause's existing role as non-
executive director. Philip Krause was determined not to be independent on August 28, 2023 and his director fees ceased
from August 1, 2023. On October 1, 2023, Philip Krause's consulting agreement was amended, where he is now
remunerated via a monthly retainer of US$20,000 for strategic advisory services and his role as non-executive director. In
addition to the monthly retainer, Philip Krause will receive 540,000 time-based options issued in three equal tranches
vesting at 12, 24 and 26 months from grant date, which are subject to shareholder approval, and 985,000 milestone-based
options which will vest subject to achieving the performance milestones and time-based vesting conditions. All options will
have a 7 year term. The agreement is ongoing, with either party able to terminate on 90 written days notice. The total
aggregate fees paid to Philip Krause through the original consulting agreement for the year ended June 30, 2023 and 2024
was US$110,383 and US$220,900 respectively. As the fees relating to the amended consulting agreement are in relation to
both his advisory and director roles, they are disclosed in Table 9.
Further details on the number of options and exercise price can be found in section “Terms and conditions of
share-based payment arrangements”.
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114
Remuneration Details - NEDs
Details of the remuneration of our NEDs for the years ended June 30, 2024 and June 30, 2023 are in Table 9.
Table 9 – Director Fees
Year
Currency
Base Salary(2)
Super-
annuation
Share-based
payments
Options
Total Statutory
Remuneration
Jane Bell
2024
A$
91,851
1,359
137,214
230,424
Jane Bell
2023
A$
128,798
13,524
66,804
209,126
William Burns
2024
A$
105,625
—
95,349
200,974
William Burns
2023
A$
195,247
—
3,989
199,236
Philip Facchina
2024
A$
81,135
—
87,475
168,611
Philip Facchina
2023
A$
148,497
—
55,120
203,617
Philip Krause(3)
2024
A$
285,410
—
229,861
515,271
Philip Krause(3)
2023
A$
138,497
—
69,199
207,696
Eric Rose(4)
2023
A$
—
—
3,989
3,989
Michael Spooner
2024
A$
38,153
—
—
38,153
Michael Spooner
2023
A$
158,250
—
—
158,250
Joseph Swedish
2024
A$
186,266
—
192,507
378,773
Joseph Swedish
2023
A$
372,276
—
—
372,276
Shawn Tomasello
2023
A$
23,042
—
—
23,042
Total Non-Executive Directors
2024
A$
788,441
1,359
742,406
1,532,205
Total Non-Executive Directors
2023
A$
1,164,607
13,524
199,101
1,377,232
Total Non-Executive Directors (1)
2024
US$
518,163
893
487,909
1,006,965
Total Non-Executive Directors (1)
2023
US$
781,451
9,075
133,597
924,123
(1)
The A$ results have been determined by calculating the average rate of the exchange rates on the last trading day
of each month during the period. A US$:A$ exchange rate of 1:0.6572 has been used for the year ended June 30,
2024 and 1:0.6710 for the year ended June 30, 2023.
(2)
Other than fees for the month of July 2024 and all fees owed to Michael Spooner on his retirement, no payments
of monthly fees have been made in 2024 given the decision to defer NED fee payments until a decision is made by
the FDA on the BLA resubmission.
(3)
Philip Krause has been a non-executive director of Mesoblast since March 2022. FY2023 relates to Director Fees
earned in his role as an independent non-executive director. Within FY2024, A$11,521 relates to Director Fees
earned in his role as an independent non-executive director and A$273,889 relates to his amended consulting
agreement through which he was paid a monthly retainer of US$20,000 as compensation for strategic advisory
services and his role as non executive director from October 1, 2023 to June 30, 2024.
(4)
Eric Rose has been a non-executive director of Mesoblast since 2013. On February 1, 2022, he was appointed as
an executive director of Mesoblast and payments of director fees ceased at that time. Share-based payments
reported as part of Eric’s director fees above relate to options granted during his appointment as a non-executive
director.
Table of Contents
115
Terms and conditions of option grants and equity holdings
Details of options over ordinary shares provided as remuneration to each director and member of key management
personnel for the years ended June 30, 2024 and June 30, 2023 are provided in the tables below.
Table 10 – The value of options granted, exercised and lapsed.
Number of
options granted
Remuneration
consisting of
options (1)
Values of options
granted (2)
A$
Value of options
exercised (3)
A$
Value of options
lapsed (4)
A$
For the year ended June 30, 2024
Silviu Itescu(5)
3,693,070
38%
767,005
—
—
Eric Rose(5)
1,960,765
31%
451,305
—
—
Jane Bell(6)
326,729
60%
85,178
—
—
William Burns(6)
409,651
47%
106,796
—
—
Philip Facchina(6)
290,432
52%
75,716
—
—
Philip Krause(7)(8)
985,000
45%
256,790
—
—
Michael Spooner
—
—
—
—
—
Joseph Swedish(6)
827,077
51%
215,619
—
—
For the year ended June 30, 2023
Silviu Itescu(9)
2,325,000
32%
1,422,203
—
—
Eric Rose(9)
2,150,000
38%
1,315,155
—
—
Jane Bell(10)
200,000
32%
128,780
—
—
William Burns
—
2%
—
—
—
Philip Facchina
—
—
—
—
—
Philip Krause(11)
200,000
33%
120,120
—
—
Michael Spooner
—
—
—
—
—
Joseph Swedish
—
—
—
—
—
Shawn Tomasello
—
—
—
—
—
(1)
The percentage of the value of remuneration consisting of options, based on the value of options expensed during
the year presented in accordance with IFRS 2 Share-based Payment. For details on the assumptions made for each
grant, see information in note 17 Share-based payments within Item 18 Financial Statements of this report.
(2)
The fair value at grant date of options that were granted during the year presented as part of remuneration,
determined using Black-Scholes valuation model and in accordance with IFRS 2 Share-based Payment. The grant
date is the date at which the entity and the employee agree to a share-based payment arrangement, being when the
entity and the employee have a shared understanding of the terms and conditions of the arrangement.
(3)
The intrinsic value at exercise date of options that were exercised during the year presented, having been granted
as part of remuneration previously.
(4)
The intrinsic value at lapse date of options that lapsed during the year.
(5)
These grants were approved by the Board on October 12, 2023 and October 16, 2023, respectively, and granted on
November 28, 2023 after shareholder approval for the grant was received at the AGM.
(6)
This grant was approved by the Board on October 12, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(7)
This grant was approved by the Board on October 24, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(8)
The board approved a grant of 540,000 options for Philip Krause on March 11, 2024, this grant is subject to
shareholder approval at the upcoming AGM.
(9)
This grant was approved by the Board on October 17, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
Table of Contents
116
(10)
This grant was approved by the Board on August 24, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(11)
This grant was approved by the Board on May 23, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
There have been no modifications to any terms and conditions of share-based payment transactions during the
years ended June 30, 2024 and 2023.
Reconciliation of Options held by KMP
The table below shows a reconciliation of options over ordinary shares of Mesoblast Limited held by each KMP
from the beginning to the end of FY24.
Table 11 – Reconciliation of options held by each KMP during FY24.
Balance at July 1, 2023
Granted as
compensat
ion during
FY24
Vested during
FY24
Exercised
during FY24
Forfeited /
Lapsed during
FY24
Balance at June 30, 2024
Name
Grant Date
Vested
Unvested
Number
Number
%
Number
%
Number
%
Vested and
exercisable
Unvested
Silviu Itescu
28-Nov-23(1)
—
—
2,420,000
—
—
—
—
—
—
—
2,420,000
Silviu Itescu
28-Nov-23(2)
—
—
1,273,070
424,357
33
—
—
—
—
424,357
848,713
Silviu Itescu
23-Nov-22(3)
—
2,325,000
—
—
—
—
—
—
—
—
2,325,000
Silviu Itescu
29-Nov-21(4)
—
1,550,000
—
620,000
40
—
—
—
—
620,000
930,000
Silviu Itescu
24-Nov-20(5)
720,000
480,000
—
—
—
—
—
—
—
720,000
480,000
Silviu Itescu
27-Nov-19(6)
1,212,001
673,333
—
—
—
—
—
—
—
1,212,001
673,333
Eric Rose
28-Nov-23(1)
—
—
740,000
—
—
—
—
—
—
—
740,000
Eric Rose
28-Nov-23(2)
—
—
1,220,765
406,922
33
—
—
—
—
406,922
813,843
Eric Rose
23-Nov-22(3)
—
1,250,000
—
416,667
33
—
—
—
—
416,667
833,333
Eric Rose
23-Nov-22(3)
—
900,000
—
—
—
—
—
—
—
—
900,000
Eric Rose
30-Nov-18
120,000
—
—
—
—
—
—
—
—
120,000
—
Eric Rose
27-Nov-19
100,000
—
—
—
—
—
—
—
—
100,000
—
Jane Bell
28-Nov-23(2)
—
—
326,729
108,910
33
—
—
—
—
108,910
217,819
Jane Bell
23-Nov-22(7)
—
200,000
—
66,667
33
—
—
—
—
66,667
133,333
William Burns
28-Nov-23(2)
—
—
409,651
136,551
33
—
—
—
—
136,551
273,100
William Burns
30-Nov-18
120,000
—
—
—
—
—
—
—
—
120,000
—
William Burns
27-Nov-19
100,000
—
—
—
—
—
—
—
—
100,000
—
Philip Facchina
28-Nov-23(2)
—
—
290,432
96,811
33
—
—
—
—
96,811
193,621
Philip Facchina
29-Nov-21(8)
133,334
66,666
—
66,666
33
—
—
—
—
200,000
—
Philip Krause(11)
28-Nov-23(9)
—
—
985,000
—
—
—
—
—
—
—
985,000
Philip Krause
23-Nov-22(10)
66,667
133,333
—
66,667
33
—
—
—
—
133,334
66,666
Michael
Spooner(12)
30-Nov-18
100,000
—
—
—
—
—
—
—
—
100,000
—
Joseph Swedish
28-Nov-23(2)
—
—
827,077
275,693
33
—
—
—
—
275,693
551,384
Joseph Swedish
27-Nov-19
300,000
—
—
—
—
—
—
—
—
300,000
—
Joseph Swedish
30-Nov-18
200,000
—
—
—
—
—
—
—
—
200,000
—
(1)
This grant was approved by the Board on October 16, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
This grant was approved by the Board on October 12, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(3)
This grant was approved by the Board on October 17, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(4)
This grant was approved by the Board on September 8, 2021 and granted on November 29, 2021 after shareholder
approval for the grant was received at the AGM.
Table of Contents
117
(5)
This grant was approved by the Board on July 16, 2020 and granted on November 24, 2020 after shareholder
approval for the grant was received at the AGM.
(6)
This grant was approved by the Board on July 20, 2019 and granted on November 27, 2019 after shareholder
approval for the grant was received at the AGM.
(7)
This grant was approved by the Board on August 24, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(8)
This grant was approved by the Board on April 15, 2021 and granted on November 29, 2021 after shareholder
approval for the grant was received at the AGM.
(9)
This grant was approved by the Board on October 24, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(10)
This grant was approved by the Board on May 23, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(11)
The board approved a grant of 540,000 options for Philip Krause on March 11, 2024, this grant is subject to
shareholder approval at the upcoming AGM.
(12)
On September 26, 2023, Mr. Spooner resigned as director of the Company.
Terms and conditions of share-based payment arrangements
The terms and conditions of each grant of options affecting remuneration in the current or a future reporting
period are as follows:
Table 12 – Terms and conditions of share-based payment arrangements
28-Nov-23(1)
Philip Krause
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 24-Oct-2024
one third - 24-Oct-2025
one third - 24-Oct-2026
23-Oct-30
0.37
0.26
28-Nov-23(2)
Silviu Itescu
Eric Rose
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 16-Oct-2024
one third - 16-Oct-2025
one third - 16-Oct-2026
15-Oct-30
0.35
0.18
28-Nov-23(3)
Silviu Itescu
Eric Rose
Jane Bell
William Burns
Philip Facchina
Joseph Swedish
one third - 12-Apr-2024
one third - 12-July-2024
one third - 12-Oct-2024
11-Oct-30
0.36
0.26
23-Nov-22(4)
Philip Krause
one third - 23-May-2023
one third - 23-May-2024
one third - 23-May-2025
22-May-29
1.01
0.60
23-Nov-22(5)
Jane Bell
one third - 24-Aug-2023
one third - 24-Aug-2024
one third - 24-Aug-2025
23-Aug-29
0.85
0.64
23-Nov-22(6)
Eric Rose
one third - 17-Oct-2023
one third - 17-Oct-2024
one third - 17-Oct-2025
16-Oct-29
1.03
0.61
23-Nov-22(6)
Silviu Itescu
Eric Rose
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 17-Oct-2023
one third - 17-Oct-2024
one third - 17-Oct-2025
16-Oct-29
1.03
0.61
Grant date
Recipients of Grants
Vesting date
Expiry date
Exercise
price A$
Value per
option at grant
date A$
Table of Contents
118
29-Nov-21(7)
Silviu Itescu
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 8-Sep-2022
one third - 8-Sep-2023
one third - 8-Sep-2024
7-Sep-28
1.77
0.42
29-Nov-21(8)
Philip Facchina
one third - 15 Apr 2022
one third - 15 Apr 2023
one third - 15 Apr 2024
14-Apr-28
2.28
1.11
24-Nov-20(9)
Silviu Itescu
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 16-Jul-2021
one third - 16-Jul-2022
one third - 16-Jul-2023
15-Jul-27
3.41
0.92
27-Nov-19(10)
Silviu Itescu
Vesting in accordance with the following
schedule, but only after achievement of
performance milestones:
one third - 19-Jul-2020
one third - 19-Jul-2021
one third - 19-Jul-2022
19-Jul-26
1.47
1.03
27-Nov-19(10)
Silviu Itescu
one third - 19-Jul-2020
one third - 19-Jul-2021
one third - 19-Jul-2022
19-Jul-26
1.47
1.03
27-Nov-19
William Burns
Eric Rose
one third - 17 Nov 2020
one third - 17 Nov 2021
one third - 17 Nov 2022
17-Nov-26
1.83
0.94
27-Nov-19
Joseph Swedish
one third - 4 Apr 2020
one third - 4 Apr 2021
one third - 4 Apr 2022
3-Apr-26
1.48
0.78
30-Nov-18
William Burns
Eric Rose
Michael Spooner
one third - 30 Nov 2019
one third - 30 Nov 2020
one third - 30 Nov 2021
29-Nov-25
1.33
0.54
30-Nov-18
Joseph Swedish
one third - 18 Jun 2019
one third - 18 Jun 2020
one third - 18 Jun 2021
17-Jun-25
1.52
0.85
Grant date
Recipients of Grants
Vesting date
Expiry date
Exercise
price A$
Value per
option at grant
date A$
(1)
This grant was approved by the Board on October 24, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
This grant was approved by the Board on October 16, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(3)
This grant was approved by the Board on October 12, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(4)
This grant was approved by the Board on May 23, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(5)
This grant was approved by the Board on August 24, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(6)
This grant was approved by the Board on October 17, 2022 and granted on November 23, 2022 after shareholder
approval for the grant was received at the AGM.
(7)
This grant was approved by the Board on September 8, 2021 and granted on November 29, 2021 after shareholder
approval for the grant was received at the AGM.
(8)
This grant was approved by the Board on April 15, 2021 and granted on November 29, 2021 after shareholder
approval for the grant was received at the AGM.
(9)
This grant was approved by the Board on July 16, 2020 and granted on November 24, 2020 after shareholder
approval for the grant was received at the AGM.
Table of Contents
119
(10)
This grant was approved by the Board on July 20, 2019 and granted on November 27, 2019 after shareholder
approval for the grant was received at the AGM.
Table 13 - Shares provided to KMPs on the exercise of remuneration options
No. of
options
exercised
during the
period
No. of
ordinary
shares in
Mesoblast
Limited
issued
Exercise Date
Value per
share at
exercise date
A$
Exercise
price per
option
A$
For the year ended June 30, 2024
Nil
—
—
—
—
—
For the year ended June 30, 2023
Nil
—
—
—
—
—
KMP Shareholdings
The table below shows a reconciliation of ordinary shares held by each KMP from the beginning to the end of the
2024 financial year.
Table 14 – KMP Shareholdings
Name
Balance at the
start of the year
Received during
the year upon
exercise of
options
Acquisitions/
(Disposals)
during the year
Balance at the
end of the year
Silviu Itescu
68,958,928
—
10,000,000
78,958,928
Eric Rose
—
—
411,620
411,620
Jane Bell
247,618
—
295,823
543,441
William Burns
85,000
—
21,250
106,250
Philip Facchina
273,225
—
(150,005)(2)
123,220
Philip Krause
100,000
—
187,500
287,500
Michael Spooner(1)
1,091,335
—
—
1,091,335
Joseph Swedish
—
—
459,420
459,420
(1)
This total includes shareholdings of related parties, of this balance, Mr. Spooner has a relevant interest, as defined
under the Corporations Act, of 1,069,000 ordinary shares. On September 26, 2023, Mr. Spooner resigned as
director of the Company.
(2)
Philip Facchina disposed 150,000 ordinary shares during FY24. An adjustment down of 5 ordinary shares was
made on January 10, 2024 following the ratio change to Mesoblast's ADR program from 5 ordinary shares
representing 1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio).
Employment Agreements
The employment of our CEO and CMO are formalized in agreements, the key terms of which are as follows:
Table 15 – KMP Employment Agreements
Name
Term
Agreement Type
Notice period
Termination benefit
Silviu Itescu (CEO)
Initial term of 3 years commencing April 1, 2014, and
continuing subject to a 12 months’ notice period.
Employment
12 months
12 months base salary
Eric Rose (CMO)
An ongoing employment agreement until notice is given by
either party.
Employment
3 months
3 months base salary
Table of Contents
120
On termination of employment our CEO, who is based in Australia, is entitled to receive his statutory entitlements
of accrued annual and long service leave, together with any superannuation benefits.
On termination of employment our CMO, who is based in the United States, is entitled to participate in the
Company’s healthcare plan during the severance period.
There is no entitlement to a termination payment in the event of resignation (except, in the case of the CMO, if the
Company has materially reduced his role or benefits or materially moved office location) or removal for misconduct.
KMP Loans or other related transactions
There were no loans or other related transactions with KMP during the financial year other than that described
above.
(End of Remuneration Report)
Table of Contents
121
Employee Profile
As of June 30, 2024, we had 73 (2023:83) employees globally:
Employees by Education
5
36
18
12
2
Diploma/Certificates
Bachelor
Masters
PhD
MD
Employees by Region
41
9
22
1
USA
Singapore
Australia
Switzerland
Employees by Gender
38
35
Female
Male
57% of our employees and a majority of our executives are based in the United States where Mesoblast
operational activities are concentrated.
Australia is the corporate headquarters where 30% of the employees work. This includes the CEO and a portion of
the executive team. The remaining 12% of employees are located in Singapore and 1% in Switzerland where research and
development activities are primarily conducted.
Table of Contents
122
Australian Disclosure Requirements
Options Granted as Remuneration
The following table presents options that have been granted over unissued shares during or since the end of the
year ended June 30, 2024, to our Directors and our next 5 most highly remunerated officers.
Table 16 – Options Granted as Remuneration
Name
Issue Date
Exercise
Price
A$
Number of
shares, under
option
Directors
Silviu Itescu
28-Nov-23(1)
0.35
2,420,000
Silviu Itescu
28-Nov-23(2)
0.36
1,273,070
Eric Rose
28-Nov-23(1)
0.35
740,000
Eric Rose
28-Nov-23(2)
0.36
1,220,765
Non-Directors
Geraldine Storton
16-Oct-23
0.35
480,000
Kenneth Borow
16-Oct-23
0.35
1,398,393
Michael Schuster
16-Oct-23
0.35
590,000
Peter Howard
16-Oct-23
0.35
660,000
Roger Brown
16-Oct-23
0.35
490,000
(1)
This grant was approved by the Board on October 16, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
(2)
This grant was approved by the Board on October 12, 2023 and granted on November 28, 2023 after shareholder
approval for the grant was received at the AGM.
KMP Interests
The relevant interest of each KMP, as defined by section 608 of the Corporations Act, in the share capital of
Mesoblast, as notified by the directors to the ASX in accordance with section 205G(1) of the Corporations Act, at the date
of this report is as follows:
Table 17 – KMP Interests
Director
Mesoblast
Limited ordinary
shares
Options over
Mesoblast
Limited ordinary
shares
Silviu Itescu
78,958,928
10,653,404
Eric Rose
411,620
4,330,765
Jane Bell
543,441
526,729
William Burns
106,250
629,651
Philip Facchina(1)
123,220
490,432
Philip Krause(2)
287,500
1,185,000
Michael Spooner(3)
1,069,000
100,000
Joseph Swedish
459,420
1,327,077
(1)
Mr Facchina also has a relevant interest in 68,306 warrants over ordinary shares.
(2)
The board approved a grant of 540,000 options for Philip Krause on March 11, 2024, this grant is subject to
shareholder approval at the upcoming AGM.
(3)
On September 26, 2023, Mr. Spooner resigned as director of the Company.
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123
Meeting of Directors
The number of meetings our board of directors (including committee meetings of directors) held during the year
ended June 30, 2024 and the number of meetings attended by each director were:
Table 18 – Meeting of Directors
Board of Directors
Audit and Risk Committee
Nomination and Remuneration
Committee
Director
A*
B*
A
B
A
B
Silviu Itescu
19
19
—
—
—
—
Eric Rose
19
19
—
—
—
—
Jane Bell
19
19
2
2
4
4
William Burns
19
19
—
—
4
4
Philip Facchina
19
17
2
2
4
4
Philip Krause
19
19
—
—
2
2
Michael Spooner
8
8
2
1
2
1
Joseph Swedish
19
18
2
1
4
4
A = Number of meetings held during the time the director held office or was a member of the committee.
B = Number of meetings attended by board/committee members
* = This includes both meetings scheduled in the board calendar as well as teleconference meetings organized on an ad-hoc
basis. For the most part, each director attended every scheduled meeting in the board calendar.
Shares under option
Unissued ordinary shares of Mesoblast Limited under option at the date of this Directors’ report are as follows:
16-Sep-17
1.52
15-Sep-24
50,000
13-Oct-17
1.92
12-Oct-24
815,000
13-Oct-17
1.74
12-Oct-24
902,425
24-Nov-17
1.39
23-Nov-24
750,000
24-Nov-17
1.26
23-Nov-24
750,000
18-Jun-18
1.50
17-Jun-25
200,000
11-Jul-18
1.54
10-Jul-25
200,000
18-Jul-18
1.85
17-Jul-25
2,998,332
18-Jul-18
1.85
17-Jul-25
350,000
30-Nov-18
1.31
29-Nov-25
590,000
19-Jan-19
1.43
18-Jan-26
3,333
19-Jan-19
1.43
18-Jan-26
150,000
4-Apr-19
1.46
3-Apr-26
300,000
20-Jul-19
1.60
19-Jul-26
2,708,669
20-Jul-19
1.45
19-Jul-26
2,833,332
20-Jul-19
1.45
19-Jul-26
1,346,667
20-Jul-19
1.45
19-Jul-26
538,667
20-Jul-19
1.45
19-Jul-26
700,000
25-Nov-19
1.96
24-Nov-26
20,000
29-May-19
1.46
28-May-26
350,000
18-Nov-19
1.81
17-Nov-26
200,000
25-Nov-19
1.78
24-Nov-26
100,000
Grant date
Exercise price of
options
A$
Expiry date of
options
Number of
shares under
option
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124
25-Nov-19
1.96
24-Nov-26
150,000
24-Jan-20
3.36
23-Jan-27
10,000
18-May-20
4.00
17-May-27
1,200,000
18-May-20
3.63
17-May-27
1,200,000
16-Jul-20
3.73
15-Jul-27
3,040,000
16-Jul-20
3.39
15-Jul-27
1,735,000
16-Jul-20
3.39
15-Jul-27
350,000
16-Jul-20
3.39
15-Jul-27
300,000
16-Jul-20
3.39
15-Jul-27
1,200,000
11-Sep-20
4.76
10-Sep-27
200,000
20-Nov-20
3.58
19-Nov-27
200,000
20-Nov-20
3.58
19-Nov-27
100,000
17-Feb-21
2.65
16-Feb-28
250,000
15-Apr-21
2.26
14-Apr-28
200,000
8-Sep-21
1.93
7-Sep-28
2,929,666
8-Sep-21
1.75
7-Sep-28
3,850,000
8-Sep-21
1.75
7-Sep-28
1,550,000
23-Dec-21
1.40
22-Dec-28
200,000
17-Oct-22
1.01
16-Oct-29
1,250,000
23-May-22
0.99
22-May-29
200,000
24-Aug-22
0.83
23-Aug-29
200,000
17-Oct-22
1.11
16-Oct-29
5,054,500
17-Oct-22
1.01
16-Oct-29
4,350,000
17-Oct-22
1.11
16-Oct-29
225,000
17-Oct-22
1.01
16-Oct-29
3,225,000
17-Oct-22
1.01
16-Oct-29
1,200,000
8-Aug-22
0.91
7-Aug-29
100,000
11-Dec-20
4.58
10-Dec-27
100,000
21-Nov-22
1.10
20-Nov-29
100,000
30-Mar-23
1.01
29-Mar-30
45,000
30-Mar-23
0.92
29-Mar-30
600,000
12-Oct-23
0.36
11-Oct-30
2,493,835
12-Oct-23
0.36
11-Oct-30
1,853,889
16-Oct-23
0.39
15-Oct-30
5,434,500
16-Oct-23
0.35
15-Oct-30
1,995,000
16-Oct-23
0.35
15-Oct-30
3,160,000
16-Oct-23
0.35
15-Oct-30
2,730,000
16-Oct-23
0.35
15-Oct-30
873,393
24-Oct-23
0.37
23-Oct-30
985,000
16-Oct-23
0.35
15-Oct-30
300,000
30-May-24
1.23
29-May-31
220,000
30-May-24
1.23
29-May-31
200,000
30-May-24
1.35
29-May-31
210,000
Grand Total
72,626,208
Grant date
Exercise price of
options
A$
Expiry date of
options
Number of
shares under
option
No option holder has any right under the options plan to participate in any other of our share issues.
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125
Shares issued on exercise of options during the year
There were no exercise of options during or since the end of the financial year.
Indemnification of Officers
During the financial year, we paid premiums in respect of a contract insuring our directors and company
secretaries, and all of our executive officers. The liabilities insured are to the extent permitted by the Corporations Act
2001. Further disclosure required under section 300(9) of the Corporations Act 2001 is prohibited under the terms of the
insurance contract.
Proceedings on Our Behalf
The Corporations Act 2001 allows specified persons to bring, or intervene in, proceedings on our behalf. No
proceedings have been brought or intervened in on our behalf with leave of the Court under section 237 of the
Corporations Act 2001.
Non-Audit Services
We may decide to employ the auditor on assignments additional to their statutory audit duties where the auditor’s
expertise and experience are relevant and considered to be important.
The board of directors considers the position and in accordance with advice received from the audit committee,
only permits the provision of the non-audit services compatible with the general standard of independence for auditors
imposed by the Corporations Act 2001.
During both the current and prior financial years, no fees were paid or payable for non-audit services provided by
the auditor of the parent entity, its related practices and non-related audit firms.
Auditor’s Independence Declaration
A copy of the auditor’s independence declaration under Section 307C of the Corporations Act in relation to the
audit for the year ended June 30, 2024 is included in Exhibit 99.2 of this annual report on Form 20-F.
Rounding of Amounts
Our company is of a kind referred to in ASIC Corporations (Rounding in Financial/Directors’ Reports)
Instrument 2016/191, issued by the Australian Securities and Investments Commission, relating to the ‘rounding off’ of
amounts in the directors’ report. Unless mentioned otherwise, amounts within this report have been rounded off in
accordance with that Legislative Instrument to the nearest thousand dollars, or in certain cases, to the nearest dollar.
The components of our directors’ report are incorporated in various places within this annual report on the Form
20-F. A table charting these components is included within ‘Exhibit 99.1 Appendix 4E’.
Directors’ Resolution
This report is made in accordance with a resolution of the directors.
/s/ Jane Bell
/s/ Silviu Itescu
Jane Bell
Silviu Itescu
Chair of Board
Chief Executive Officer
Dated: August 29, 2024
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126
6.C
Board Practices
Our board of directors currently consists of seven members: five non-executive directors and two executive
directors, being Dr, Silviu Itescu, our Chief Executive Officer and Dr. Eric Rose, our Chief Medical Officer.
Our directors are generally elected to serve three-year terms in a manner similar to a “staggered” board of
directors under Delaware law. No director, except the Managing Director (currently designated as our Chief Executive
Officer, Silviu Itescu), may hold office for a period in excess of three years, or beyond the third annual general meeting
following the director’s last election, whichever is the longer, without submitting himself or herself for re-election. As a
result of the staggered terms, not all of our directors will be elected in any given year.
Name
First election at
AGM
Last election at
AGM
End of current
term
William Burns
2014
2023
2026
Eric Rose
2013
2022
2025
Michael Spooner(1)
2004
2021
N/A
Joseph Swedish
2018
2021
2024
Philip Facchina
2021
2023
2026
Philip Krause
2022
2022
2025
Jane Bell
2022
2022
2025
(1)
Mr. Spooner resigned from the board on September 26, 2023.
We believe that each of our directors has relevant industry experience. The membership of our board of directors
is directed by the following requirements:
•
our Constitution specifies that there must be a minimum of 3 directors and a maximum of 10, and our
board of directors may determine the number of directors within those limits;
•
we may appoint or remove any director by resolution passed in the general meeting of shareholders;
•
our directors may appoint any person to be a director, and that person only holds office until the next
general meeting at which time the director may stand for election by shareholders at that meeting;
•
it is the intention of our board of directors that its membership consists of a majority of independent
directors who satisfy the criteria for independence recommended by the ASX’s Corporate Governance
Principles and Recommendations and the Rulebook of the Nasdaq Stock Market;
•
the chairperson of our board of directors should be an independent director who satisfies the criteria for
independence recommended by the ASX’s Corporate Governance Principles and Recommendations;
•
Australia's Corporations Act requires that at least two of our directors must be resident Australians; and
•
our board of directors should, collectively, have the appropriate level of personal qualities, skills,
experience, and time commitment to properly fulfill its responsibilities or have ready access to such skills
where they are not available.
Our board of directors is responsible for, and has the authority to determine, all matters relating to our corporate
governance, including the policies, practices, management and operation. The principal roles and responsibilities of our
board of directors are to:
•
facilitate board of directors and management accountability to our company and its shareholders;
•
ensure timely reporting to shareholders;
•
provide strategic guidance to us, including contributing to the development of, and approving, the
corporate strategy;
•
oversee management and ensure there are effective management processes in place;
•
monitor:
◦
organizational performance and the achievement of our strategic goals and objectives;
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127
◦
financial performance including approval of the annual and half-year financial reports and
liaison with our auditors;
◦
progress of major capital expenditures and other significant corporate projects including any
acquisitions or divestments;
◦
compliance with our code of conduct;
◦
progress in relation to our diversity objectives and compliance with its diversity policy;
•
review and approve business plans, the annual budget and financial plans including available resources
and major capital expenditure initiatives;
•
approve major corporate initiatives;
•
enhance and protect the reputation of the organization;
•
oversee the operation of our system for compliance and risk management reporting to shareholders; and
•
ensure appropriate resources are available to senior management.
Our non-executive directors do not have any service contracts with Mesoblast that provide for benefits upon
termination of those services.
Committees
To assist our board of directors with the effective discharge of its duties, it has established a Nomination and
Remuneration Committee and an Audit and Risk Committee. Each committee operates under a specific charter approved
by our board of directors.
Nomination and Remuneration Committee. The members of our Nomination and Remuneration Committee for the
full year ended June 30, 2024 to the date of this report unless otherwise noted are Messrs. Burns (Chair), Swedish, Spooner
(resignation effective September 26, 2023), Facchina, Krause (resignation from the committee effective August 28, 2023)
and Ms. Bell. The remuneration committee is a committee of our board of directors, and is primarily responsible for
making recommendations to our board of directors on:
•
board appointments;
•
non-executive director fees;
•
the executive remuneration framework;
•
remuneration of executive directors, including the CEO and other key executives;
•
short-term and long-term incentive awards; and
•
share ownership plans.
The committee’s objective is to ensure remuneration policies are fair and competitive and in line with similar
industry benchmarks while aligned with our objectives. The remuneration committee seeks independent advice from
remuneration consultants as and when it deems necessary. See “Management—Remuneration.”
Audit and Risk Committee. The members of our Audit and Risk Committee for the full year ended June 30, 2024
to the date of this report unless otherwise noted are Messrs. Spooner (Chair until his resignation from this committee
effective September 20, 2023), Facchina (Chair from April 30, 2024), Swedish and Ms. Bell (Chair between September 20,
2023 to April 30, 2024), all of whom are independent, non-executive directors. This committee oversees, reviews, acts on
and reports on various auditing and accounting matters to our board of directors, including the selection of our independent
accountants, the scope of our annual audits, fees to be paid to the independent accountants, the performance of our
independent accountants and our accounting practices. In addition, the committee oversees, reviews, acts on and reports on
various risk management matters to our board of directors.
The effective management of risk is central to our ongoing success. We have adopted a risk management policy to
ensure that:
•
appropriate systems are in place to identify, to the extent that is reasonably practical, all material risks
that we face in conducting our business;
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128
•
the financial impact of those risks is understood and appropriate controls are in place to limit exposures
to them;
•
appropriate responsibilities are delegated to control the risks; and
•
any material changes to our risk profile are disclosed in accordance with our continuous disclosure
reporting requirements in Australia.
It is our objective to appropriately balance, protect and enhance the interests of all of our shareholders. Proper
behavior by our directors, officers, employees and those organizations that we contract to carry out work is essential in
achieving this objective.
We have established a code of conduct, which sets out the standards of behavior that apply to every aspect of our
dealings and relationships, both within and outside Mesoblast. The following standards of behavior apply:
•
patient well-being;
•
comply with all laws that govern us and our operations;
•
act honestly and with integrity and fairness in all dealings with others and each other;
•
avoid or manage conflicts of interest;
•
use our assets properly and efficiently for the benefit of all of our shareholders; and
•
seek to be an exemplary corporate citizen.
Board Diversity
The following matrix sets forth Board diversity information required by the Nasdaq’s rules for Mesoblast as a
foreign private issuer.
Board Diversity Matrix as at June 30, 2024
Country of Principal Executive Offices
Australia
Foreign Private Issuer
Yes
Disclosure Prohibited under Home Country Law
No
Total Number of Directors
7
Female
Male
Non-Binary
Did Not Disclose Gender
Part I: Gender Identity
Directors
1
4
—
2
Part II: Demographic Background
Underrepresented Individual in Home Country Jurisdiction
—
LGBTQ+
—
Did not Disclose Demographic Background
2
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129
Board Diversity Matrix as at June 30, 2023
Country of Principal Executive Offices
Australia
Foreign Private Issuer
Yes
Disclosure Prohibited under Home Country Law
No
Total Number of Directors
8
Female
Male
Non-Binary
Did Not Disclose Gender
Part I: Gender Identity
Directors
1
3
—
4
Part II: Demographic Background
Underrepresented Individual in Home Country Jurisdiction
1
LGBTQ+
—
Did not Disclose Demographic Background
7
6.D
Employees
As of June 30, 2024, we had 73 employees, 42 of whom are based in the United States, 21 of whom are based in
Australia, including our CEO and certain executive team members, 9 of whom are based in Singapore, and 1 of whom is
based in Switzerland. We had 83 and 77 employees as of June 30, 2023 and 2022, respectively.
The table below sets forth the breakdown of the total year-end number of our employees by main category of
activity and geographic area for the past three years:
As of June 30, 2024
Research &
Development
Commercial
Manufacturing
Corporate
Total
USA
30
—
4
7
41
Australia
7
—
1
14
22
Singapore
1
—
7
1
9
Switzerland
1
—
—
—
1
Total
39
—
12
22
73
As of June 30, 2023
Research &
Development
Commercial
Manufacturing
Corporate
Total
USA
35
—
5
9
49
Australia
8
—
1
15
24
Singapore
4
—
4
1
9
Switzerland
1
—
—
—
1
Total
48
—
10
25
83
As of June 30, 2022
Research &
Development
Commercial
Manufacturing
Corporate
Total
USA
32
—
4
8
44
Australia
8
—
1
15
24
Singapore
1
—
6
1
8
Switzerland
1
—
—
—
1
Total
42
—
11
24
77
We have no collective bargaining agreement with our employees. We have not experienced any work stoppages to
date and consider our relations with our employees to be good.
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130
See “Item 6.A Directors and Senior Management – Employee Profile”.
6.E
Share Ownership
The table below sets forth information regarding the beneficial ownership of our ordinary shares based on
1,141,784,114 ordinary shares outstanding at August 29, 2024 by each of our directors and key management personnel.
We have determined beneficial ownership in accordance with the rules of the SEC. A person has a beneficial
ownership of a security if he, she or it possesses sole or shared voting or investment power of that security, including
options that are exercisable within 60 days of August 29, 2024. Ordinary shares subject to options currently exercisable or
exercisable within 60 days of August 29, 2024 are deemed to be outstanding for computing the percentage ownership of
the person holding these options and the percentage ownership of any group of which the holder is a member, however are
not deemed outstanding for computing the percentage of any other person.
Unless otherwise indicated, to our knowledge each shareholder possesses sole voting and investment power over
the ordinary shares listed. None of our shareholders has different voting rights from other shareholders. Unless otherwise
indicated, the principal address of each of the shareholders below is c/o Mesoblast Limited, Level 38, 55 Collins Street,
Melbourne 3000, Australia.
Ordinary Shares
beneficially owned
Name
Number
%
Directors and key management personnel:
Silviu Itescu(1)
83,590,666
7.3%
Eric Rose(2)
3,433,719
*
Jane Bell(3)
1,003,504
*
William Burns(4)
735,901
*
Philip Facchina(5)
681,958
*
Philip Krause(6)
745,884
*
Michael Spooner(7)
1,169,000
*
Joseph Swedish(8)
1,786,497
*
All directors and key management personnel as a group
(8 persons)
93,147,129
8.1%
_______________
*
Less than 1% of the outstanding ordinary shares.
(1)
Includes (a) 67,756,838 ordinary shares owned by Dr. Itescu, (b) 8,821,137 ordinary shares owned by Josaka
Investments Pty Ltd, the trustee of Dr. Itescu’s self-managed superannuation fund, (c) 2,380,953 ordinary shares
owned by Tamit Nominees Pty Ltd, an Australian corporation owned by Dr. Itescu and (d) 4,631,738 ordinary
shares subject to options of which; 1,212,001 exercisable at a price of A$1.45 per share until July 19, 2026,
720,000 exercisable at a price of A$3.39 per share until July 15, 2027, 620,000 exercisable at a price of A$1.75
per share until September 7, 2028, 1,273,070 exercisable at a price of A$0.36 per share until October 11, 2030 and
806,667 exercisable at a price of A$0.35 per share until October 15, 2030.
(2)
Includes (a) 411,620 ordinary shares owned by Dr. Rose (held as American Depository Shares) and (b) 3,022,099
ordinary shares subject to options of which; 120,000 exercisable at a price of A$1.31 per share until November 29,
2025, 100,000 exercisable at a price of A$1.81 per share until November 17, 2026, 1,433,334 exercisable at a
price of A$1.01 per share until October 16, 2029, 1,220,765 exercisable at a price of A$0.36 per share until
October 11, 2030 and 148,000 exercisable at a price of A$0.35 per share until October 15, 2030.
(3)
Includes (a) 543,441 ordinary shares owned by Ms. Bell and Mr. Geoffrey Arthur Bell as trustees for Ms. Bell's
family trust, (b) 460,063 ordinary shares subject to options of which: 133,334 exercisable at a price of A$0.83 per
share until August 23, 2029 and 326,729 exercisable at a price of A$0.36 per share until October 11, 2030.
(4)
Includes (a) 106,250 ordinary shares owned by Mr. Burns (through a custodian) and (b) 629,651 ordinary shares
subject to options of which; 120,000 exercisable at a price of A$1.31 per share until November 29, 2025, 100,000
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131
exercisable at a price of A$1.81 per share until November 17, 2026 and 409,651 exercisable at a price of A$0.36
per share until October 11, 2030.
(5)
Includes (a) 123,220 ordinary shares owned by HNP, LLC (held as American Depository Shares), (b) 68,306
warrants over ordinary shares owned by HNP, LLC and (c) 490,432 ordinary shares subject to options of which:
200,000 exercisable at a price of A$2.26 per share until April 14, 2028 and 290,432 exercisable at a price of
A$0.36 per share until October 11, 2030.
(6)
Includes (a) 287,500 ordinary shares owned by Mr. Krause (held as American Depository Shares) and (b) 458,384
ordinary shares subject to options of which: 133,334 exercisable at a price of A$0.99 per share until May 22, 2029
and 325,050 exercisable at a price of A$0.37 per share until October 23, 2030.
(7)
Includes (a) 356,533 ordinary shares owned by Mr. Spooner, (b) 712,467 ordinary shares owned by Mr. Spooner's
family trusts and (c) 100,000 ordinary shares subject to options exercisable at a price of A$1.31 per share until
November 29, 2025. On September 26, 2023, Mr. Spooner resigned as director of the Company.
(8)
Includes (a) 459,420 ordinary shares owned by Mr. Swedish (held as American Depository Shares) and (b)
1,327,077 ordinary shares subject to options of which; 200,000 are exercisable at a price of A$1.50 per share until
June 17, 2025, 300,000 are exercisable at a price of A$1.46 per share until April 3, 2026 and 827,077 exercisable
at a price of A$0.36 per share until October 11, 2030.
6.F Disclosure of a Registrant’s Action to Recover Erroneously Awarded Compensation
Not applicable.
Item 7. Major Shareholders and Related Party Transactions
7.A
Major Shareholders
The following table and accompanying footnotes present certain information regarding the beneficial ownership
of our ordinary shares based on 1,141,784,114 ordinary shares outstanding at August 29, 2024 by each person known by us
to be the beneficial owner of more than 5% of our ordinary shares. Based upon information known to us, as of August 16,
2024 we had approximately 38 registered shareholders (ordinary shares) with addresses in the United States. These
shareholders held an aggregate of 327,584,347 of our ordinary shares, or approximately 37.43% of our outstanding
ordinary shares. None of our shareholders has different voting rights from other shareholders.
Ordinary Shares
beneficially owned
Name
Number
%
5% or Greater Shareholders:
Silviu Itescu(1)
83,590,666
7.3%
G to the Fourth Investments, LLC(2)
186,678,344
16.3%
(1)
Includes (a) 67,756,838 ordinary shares owned by Dr. Itescu, (b) 8,821,137 ordinary shares owned by Josaka
Investments Pty Ltd, the trustee of Dr. Itescu’s self-managed superannuation fund and (c) 2,380,953 ordinary
shares owned by Tamit Nominees Pty Ltd, an Australian corporation owned by Dr. Itescu, (d) 1,212,001 ordinary
shares subject to options exercisable at a price of A$1.45 per share until July 19, 2026, (e) 720,000 ordinary shares
subject to options exercisable at a price of A$3.39 per share until July 15, 2027, and (f) 620,000 ordinary shares
subject to options exercisable at a price of A$1.75 per share until September 7, 2028, (g) 806,667 ordinary shares
subject to options exercisable at a price of A$0.35 per share until October 15, 2030; and (h) 1,273,070 ordinary
shares subject to options exercisable at a price of A$0.36 per share until October 11, 2030.
(2)
Includes (a) 61,347,527 ordinary shares owned by G to the Fourth Investments, LLC and Gregory George, (b)
5,538,970 ordinary shares owned by James George (held as American Depository Shares), (c) 6,000,000 ordinary
shares owned by Grant George (held as American Depository Shares) (d) 106,961,245 ordinary shares owned by
Gregory George and (e) 6,830,602 ordinary shares subject to warrants.
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To our knowledge, there have not been any significant changes in the ownership of our ordinary shares by major
shareholders over the past three years, except as follows (which is based on notices filed with the ASX and SEC).
•
M&G Investment Group reported that as of August 12, 2022 in total it held 93,150,226 ordinary shares
(including 1,320,000 ADSs, each representing 5 ordinary shares), or 12.64% of the total voting power as
of that date. It reported that as of May 1, 2023 it held 86,251,092 ordinary shares (including 532,981
ADSs, each representing 5 ordinary shares), or 10.60% of the total voting power as of that date. It
reported that as of July 27, 2023 in total it held 76,996,783 ordinary shares, or 9.46% of the total voting
power as of that date. It reported that as of August 4, 2023 in total it held 58,312,858 ordinary shares, or
7.16% of the total voting power as of that date. It reported that as of August 8, 2023 in total it held
48,079,421 ordinary shares, or 5.91% of the total voting power as of that date. It reported that as of
August 9, 2023 that it had ceased to be a substantial shareholder.
•
G to the Fourth Investments, LLC reported that as of May 1, 2023 it held 53,920,195 ordinary shares, or
6.62% of the total voting power as of that date. It reported that as of August 24, 2023 in total it held
66,366,800 ordinary shares, or 8.15% of the total voting power as of that date. It reported that as of
March 18, 2024, it held 116,316,795 ordinary shares, or 10.23% of the total voting power as of that date.
It reported that as of March 28, 2024 it held 136,435,560 ordinary shares, or 11.99% of the total voting
power as of that date. It reported that as of April 5, 2024 it held 150,183,635 ordinary shares, or 13.20%
of the total voting power as of that date. It reported that as of April 30, 2024 it held 166,849,364 ordinary
shares, or 14.67% of the total voting power as of that date. It reported that as of July 9, 2024 it held
179,847,742 ordinary shares, or 15.81% of the total voting power as of that date.
•
Dr.Itescu reported that as of December 12, 2023 he held 78,958,928 ordinary shares, or 7.8% of the total
voting power as of that date.
7.B
Related Party Transactions
The Company has not entered into any related party transactions during the years ended June 30, 2024 or 2023
other than compensation and other services provided by Directors and other members of key management personnel, see
“Item 6.B Compensation”.
7.C
Interests of Experts and Counsel
Not applicable.
Item 8. Financial Information
8.A
Consolidated Statements and Other Financial Information
See “Item 18. Financial Statements.”
Legal Proceedings
A class action proceeding in the Federal Court of Australia was served on the Company in May 2022 by the law
firm William Roberts Lawyers on behalf of persons who, between February 22, 2018, and December 17, 2020, acquired an
interest in Mesoblast shares, American Depository Receipts, and/or related equity swap arrangements. In June 2022, the
firm Phi Finney McDonald commenced a second shareholder class action against the Company in the Federal Court of
Australia asserting similar claims arising during the same period. The Australian class actions relate to the Complete
Response Letter released by the FDA in September 2020 in relation to the Company's GvHD product candidate; they also
relate to certain representations made by the Company in relation to our COVID-19 product candidate and the decline in
the market price of the Company's ordinary shares in December 2020. The Australian class actions have been consolidated
into one lawsuit. On August 21, 2024, the Company announced that the class action had been resolved subject to Federal
Court approval. The settlement (inclusive of interest and costs) will be funded entirely by Mesoblast's insurers and includes
no admission of liability.
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Dividend policy
Since our inception, we have not declared or paid any dividends on our shares. We intend to retain any earnings
for use in our business and do not currently intend to pay cash dividends on our ordinary shares. Dividends, if any, on our
outstanding ordinary shares will be declared by and subject to the discretion of our board of directors, and subject to
Australian law.
Any dividend we declare will be paid to the holders of ADSs, subject to the terms of the deposit agreement, to the
same extent as holders of our ordinary shares, to the extent permitted by applicable law and regulations, less the fees and
expenses payable under the deposit agreement. Any dividend we declare will be distributed by the depositary bank to the
holders of our ADSs, subject to the terms of the deposit agreement. See “Item 12.D. Description of American Depositary
Shares.”
8.B
Significant Changes
In July 2024, we resubmitted our Biologic License Application ("BLA") with United States Food & Drug
Administration ("FDA") for approval of remestemcel-L in the treatment of children with steroid-refractory acute graft
versus host disease ("SR-aGVHD") and the FDA accepted our resubmission and set a Prescription Drug User Fee Act goal
date of January 7, 2025.
In August 2024, we modified the short term incentive plan providing employees with the choice to elect into
receiving an option grant in lieu of cash payment of their short term incentive entitlements for the years ended June 30,
2024 and 2023, which have been deferred to BLA approval. The level of participation and the terms of the modification are
yet to be determined at the date of this report.
In August 2024, we announced that the consolidated shareholder class action, filed in the Federal Court of
Australia in 2022, has been resolved subject to Federal Court approval. The settlement (inclusive of interest and costs) will
be funded entirely by Mesoblast's insurers and includes no admission of liability.
There were no other events that have arisen subsequent to June 30, 2024 and prior to the signing of this report that
would likely have a material impact on the financial results presented.
Item 9. The Offer and Listing
9.A
Offer and Listing Details
Our ordinary shares have been listed in Australia on the Australian Securities Exchange (ASX) since December
2004. Our ordinary shares have been trading under the symbol “MSB”.
American Depositary Shares (“ADSs”), each representing ten ordinary shares, are available in the US through an
American Depositary Receipts (“ADR”) program.
On January 10, 2024, the ratio under Mesoblast's ADR program was changed from 5 ordinary shares representing
1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio). This program was established under
the deposit agreement which we entered into with JP Morgan Chase Bank N.A. as depositary and our ADR holders. Our
ADRs have been listed on the Nasdaq Global Select Market since November 2015 and are traded under the symbol
“MESO”.
9.B
Plan of Distribution
Not applicable.
9.C
Markets
See “Item 9.A Offer and Listing Details.”
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9.D
Selling Shareholders
Not applicable.
9.E
Dilution
Not applicable.
9.F
Expenses of the Issue
Not applicable.
Item 10. Additional Information
10.A
Share Capital
Not applicable.
10.B
Memorandum and Articles of Association
Our Constitution is similar in nature to the bylaws of a U.S. corporation. It does not provide for or prescribe any
specific objectives or purposes of Mesoblast. Our Constitution is subject to the terms of the ASX Listing Rules and the
Australian Corporations Act. It may be modified or repealed and replaced by special resolution passed at a meeting of
shareholders, which a resolution is passed by at least 75% of the votes cast by shareholders (including proxies and
representatives of shareholders) entitled to vote on the resolution.
Under Australian law, a company has the legal capacity and powers of an individual both within and outside
Australia. The material provisions of our Constitution are summarized below. This summary is not intended to be complete
nor to constitute a definitive statement of the rights and liabilities of our shareholders, and is qualified in its entirety by
reference to the complete text of our Constitution, a copy of which is on file with the SEC.
Directors
Interested Directors
Except as permitted by the Corporations Act and the ASX Listing Rules, a director must not vote in respect of a
matter that is being considered at a directors' meeting in which the director has a material personal interest according to our
Constitution. Such director must not be counted in a quorum, must not vote on the matter and must not be present at the
meeting while the matter is being considered, unless the non-interested directors resolve otherwise.
Pursuant to our Constitution, the fact that a director holds office as a director, and has fiduciary obligations arising
out of that office will not require the director to account to us for any profit realized by or under any contract or
arrangement entered into by or on behalf of Mesoblast and in which the director may have an interest.
Unless a relevant exception applies, the Corporations Act requires our directors to provide disclosure of certain
interests and prohibits directors of companies listed on the ASX from voting on matters in which they have a material
personal interest and from being present at the meeting while the matter is being considered. In addition, unless a relevant
exception applies, the Corporations Act and the ASX Listing Rules require shareholder approval of any provision of
financial benefits (including the issue by us of ordinary shares and other securities) to our directors, including entities
controlled by them and certain members of their families.
Borrowing Powers Exercisable by Directors
Pursuant to our Constitution, our business is managed by our board of directors. Our board of directors has the
power to raise or borrow money, and charge any of our property or business or all or any of our uncalled capital, and may
issue debentures or give any other security for any of our debts, liabilities or obligations or of any other person, and may
guarantee or become liable for the payment of money or the performance of any obligation by or of any other person.
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Election, Removal and Retirement of Directors
We may appoint or remove any director by resolution passed in a general meeting of shareholders. Additionally,
our directors are elected to serve maximum three-year terms in a manner similar to a “staggered” board of directors under
Delaware law. No director except the Managing Director (currently designated as our chief executive officer, Silviu Itescu)
may hold office for a period in excess of three years, or beyond the third annual general meeting following the director’s
last election, whichever is the longer, without submitting himself or herself for re-election. If no such director would be
required to submit for re-election but the ASX Listing Rules require an election of directors to be held, the director to retire
will be as agreed by the directors among themselves or, failing agreement, determined by lot.
A director who is appointed during the year by the other directors only holds office until the next general meeting
at which time the director may stand for election by shareholders at that meeting.
In addition, provisions of the Corporations Act apply where at least 25% of the votes cast on a resolution to adopt
our remuneration report (which resolution must be proposed each year at our annual general meeting) are against the
adoption of the report at two successive annual general meetings. Where these provisions apply, a resolution must be put to
a vote at the second annual general meeting to the effect that a further meeting, or a spill meeting, take place within 90
days. At the spill meeting, the directors in office when the remuneration report was considered at the second annual general
meeting (other than the Managing Director) cease to hold office and resolutions to appoint directors (which may involve re-
appointing the former directors) are put to a vote.
Voting restrictions apply in relation to the resolutions to adopt our remuneration report and to propose a spill
meeting. These restrictions apply to our key management personnel and their closely related parties. See “Rights and
Restrictions on Classes of Shares—Voting Rights” below.
Pursuant to our Constitution, a person is eligible to be elected as a director at a general meeting only if:
•
the person is in office as a director immediately before the meeting, in respect of an election of directors
at a general meeting that is a spill meeting as defined in section 250V(1) of the Corporations Act;
•
the person has been nominated by the directors before the meeting;
•
where the person is a shareholder, the person has, at least 35 business days but no more than 90 business
days before the meeting, given to us a notice signed by the person stating the person's desire to be a
candidate for election at the meeting; or
•
where the person is not a shareholder, a shareholder intending to nominate the person for election at that
meeting has, at least 35 business days but no more than 90 business days before the meeting, given to us
a notice signed by the shareholder stating the shareholder's intention to nominate the person for election,
and a notice signed by the person stating the person's consent to the nomination.
Share Qualifications
There are currently no requirements for directors to own our ordinary shares in order to qualify as directors.
Rights and Restrictions on Classes of Shares
Subject to the Corporations Act and the ASX Listing Rules, the rights attaching to our ordinary shares are detailed
in our Constitution. Our Constitution provides that any of our ordinary shares may be issued with preferential, deferred or
special rights, privileges or conditions, with any restrictions in regard to dividends, voting, return of share capital or
otherwise as our board of directors may determine from time to time. Subject to the Corporations Act, the ASX Listing
Rules and any rights and restrictions attached to a class of shares, we may issue further ordinary shares on such terms and
conditions as our board of directors resolve. Currently, our outstanding ordinary share capital consists of only one class of
ordinary shares.
Dividend Rights
Our board of directors may from time to time determine to pay dividends to shareholders; however, no dividend is
payable except in accordance with the thresholds set out in the Corporations Act.
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Voting Rights
Under our Constitution, the general conduct and procedures of each general meeting of shareholders will be
determined by the chairperson, including any procedures for casting or recording votes at the meeting whether on a show
of hands or on a poll. A poll may be demanded by the chairman of the meeting; by at least five shareholders present and
having the right to vote on at the meeting; or any shareholder or shareholders representing at least 5% of the votes that may
be cast on the resolution on a poll. On a show of hands, each shareholder entitled to vote at the meeting has one vote
regardless of the number of ordinary shares held by such shareholder. If voting takes place on a poll, rather than a show of
hands, each shareholder entitled to vote has one vote for each ordinary share held and a fractional vote for each ordinary
share that is not fully paid, such fraction being equivalent to the proportion of the amount that has been paid (not credited)
of the total amounts paid and payable, whether or not called (excluding amounts credited), to such date on that ordinary
share.
Under Australian law, an ordinary resolution is passed on a show of hands if it is approved by a simple majority
(more than 50%) of the votes cast by shareholders present (in person or by proxy) and entitled to vote. If a poll is
demanded or required, an ordinary resolution is passed if it is approved by holders representing a simple majority of the
total voting rights of shareholders present (in person or by proxy) who (being entitled to vote) vote on the resolution.
Special resolutions require the affirmative vote of not less than 75% of the votes cast by shareholders present (in person or
by proxy) and entitled to vote at the meeting. Votes on resolutions set out in a notice of meeting must be voted on by poll.
Pursuant to our Constitution, each shareholder entitled to attend and vote at a meeting may attend and vote:
•
in person physically or by electronic means;
•
by proxy, attorney or by representative; or
•
other than in relation to any clause which specifies a quorum, a member who has duly lodged a valid vote
delivered to us by post, fax or other electronic means approved by the directors in accordance with the
Constitution.
Under Australian law, shareholders of a public listed company are generally not permitted to approve corporate
matters by written consent. Our Constitution does not specifically provide for cumulative voting.
Note that ADS holders may not directly vote at a meeting of the shareholders but may instruct the depositary to
vote the number of deposited ordinary shares their ADSs represent. Under voting by a show of hands, multiple “yes” votes
by ADS holders will only count as one “yes” vote and will be negated by a single “no” vote, unless a poll is demanded.
There are a number of circumstances where the Corporations Act or the ASX Listing Rules prohibit or restrict
certain shareholders or certain classes of shareholders from voting. For example, key management personnel whose
remuneration details are included elsewhere in this prospectus are prohibited from voting on the resolution that must be
proposed at each annual general meeting to adopt our remuneration report, as well as any resolution to propose a spill
meeting. An exception applies to exercising a directed proxy which indicates how the proxy is to vote on the proposed
resolution on behalf of someone other than the key management personnel or their closely related parties; or that person is
chair of the meeting and votes an undirected proxy where the shareholder expressly authorizes the chair to exercise that
power. Key management personnel and their closely related parties are also prohibited from voting undirected proxies on
remuneration related resolutions. A similar exception to that described above applies if the proxy is the chair of the
meeting.
Right to Share in Our Profits
Subject to the Corporations Act and pursuant to our Constitution, our shareholders are entitled to participate in our
profits by payment of dividends. The directors may by resolution declare a dividend or determine a dividend is payable,
and may fix the amount, the time for and method of payment.
Rights to Share in the Surplus in the Event of Winding Up
Our Constitution provides for the right of shareholders to participate in a surplus in the event of our winding up.
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Redemption Provisions
Under our Constitution and subject to the Corporations Act, the directors have power to issue and allot shares with
any preferential, deferred or special rights, privileges or conditions; with any restrictions in regard to the dividend, voting,
return of capital or otherwise; and preference shares which are liable to be redeemed or converted.
Sinking Fund Provisions
Our Constitution allows our directors to set aside any amount available for distribution as a dividend such
amounts by way of reserves as they think appropriate before declaring or determining to pay a dividend, and may apply the
reserves for any purpose for which an amount available for distribution as a dividend may be properly applied. Pending
application or appropriation of the reserves, the directors may invest or use the reserves in our business or in other
investments as they think fit.
Liability for Further Capital Calls
According to our Constitution, our board of directors may make any calls from time to time upon shareholders in
respect of all monies unpaid on partly paid shares respectively held by them, subject to the terms upon which any of the
partly paid shares have been issued. Each shareholder is liable to pay the amount of each call in the manner, at the time and
at the place specified by our board of directors. Calls may be made payable by instalment.
Provisions Discriminating Against Holders of a Substantial Number of Shares
There are no provisions under our Constitution discriminating against any existing or prospective holders of a
substantial number of our ordinary shares.
Variation or Cancellation of Share Rights
The rights attached to shares in a class of shares may only be varied or cancelled by a special resolution of
shareholders, together with either:
•
a special resolution passed at a separate meeting of members holding shares in the class; or
•
the written consent of members with at least 75% of the votes in the class.
General Meetings of Shareholders
General meetings of shareholders may be called by our board of directors or, under the Corporations Act, by a
single director. Except as permitted under the Corporations Act, shareholders may not convene a meeting. Under the
Corporations Act, shareholders with at least 5% of the votes that may be cast at a general meeting may call and arrange to
hold a general meeting. The Corporations Act requires the directors to call and arrange to hold a general meeting on the
request of shareholders with at least 5% of the votes that may be cast at a general meeting. Notice of the proposed meeting
of our shareholders is required at least 28 days prior to such meeting under the Corporations Act.
No business shall be transacted at any general meeting unless a quorum is present at the time when the meeting
proceeds to business. Under our Constitution, the presence, in person or by proxy, attorney or representative, of two
shareholders constitutes a quorum, or if we have less than two shareholders, then those shareholders constitute a quorum. If
a quorum is not present within 30 minutes after the time appointed for the meeting, the meeting must be either dissolved if
it was requested or called by shareholders or adjourned in any other case. A meeting adjourned for lack of a quorum is
adjourned to the same day in the following week at the same time and place, unless otherwise decided by our directors. The
reconvened meeting is dissolved if a quorum is not present within 30 minutes after the time appointed for the meeting.
Change of Control
Takeovers of listed Australian public companies, such as Mesoblast, are regulated by the Corporations Act, which
prohibits the acquisition of a “relevant interest” in issued voting shares in a listed company if the acquisition will lead to
that person’s or someone else’s voting power in Mesoblast increasing from 20% or below to more than 20% or increasing
from a starting point that is above 20% and below 90% (“Takeovers Prohibition”), subject to a range of exceptions.
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Generally, a person will have a relevant interest in securities if the person:
•
is the holder of the securities or the holder of an ADS over the shares;
•
has power to exercise, or control the exercise of, a right to vote attached to the securities; or
•
has the power to dispose of, or control the exercise of a power to dispose of, the securities (including any
indirect or direct power or control)
If, at a particular time:-
•
a person has a relevant interest in issued securities; and
•
the person has:
◦
entered or enters into an agreement with another person with respect to the securities;
◦
given or gives another person an enforceable right, or has been or is given an enforceable right
by another person, in relation to the securities; or
◦
granted or grants an option to, or has been or is granted an option by, another person with
respect to the securities; and
•
the other person would have a relevant interest in the securities if the agreement were performed, the
right enforced or the option exercised,
then, the other person is taken to already have a relevant interest in the securities.
There are a number of exceptions to the above Takeovers Prohibition on acquiring a relevant interest in issued
voting shares above 20%. In general terms, some of the more significant exceptions include:
•
when the acquisition results from the acceptance of an offer under a formal takeover bid;
•
when the acquisition is conducted on market by or on behalf of the bidder during the bid period for a full
takeover bid that is unconditional or only conditional on certain 'prescribed' matters set out in the
Corporations Act;
•
when the acquisition has been previously approved by resolution passed at general meeting by
shareholders of Mesoblast;
•
an acquisition by a person if, throughout the six months before the acquisition, that person or any other
person has had voting power in Mesoblast of at least 19% and, as a result of the acquisition, none of the
relevant persons would have voting power in Mesoblast more than three percentage points higher than
they had six months before the acquisition;
•
when the acquisition results from the issue of securities under a pro rata rights issue;
•
when the acquisition results from the issue of securities under a dividend reinvestment plan or bonus
share plan;
•
when the acquisition results from the issue of securities under certain underwriting arrangements;
•
when the acquisition results from the issue of securities through a will or through operation of law;
•
an acquisition that arises through the acquisition of a relevant interest in another company listed on the
ASX or other Australian financial market or a foreign stock exchange approved in writing by ASIC;
•
an acquisition arising from an auction of forfeited shares; or
•
an acquisition arising through a compromise, arrangement, liquidation or buy-back.
A formal takeover bid may either be a bid for all securities in the bid class or a fixed proportion of such securities,
with each holder of bid class securities receiving a bid for that proportion of their holding. Under our Constitution, a
proportionate takeover bid must first be approved by resolution of our shareholders in a general meeting before it may
proceed.
Breaches of the takeovers provisions of the Corporations Act are criminal offenses. In addition, ASIC and, on
application by ASIC or an interested party, such as a shareholder, the Australian Takeovers Panel have a wide range of
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powers relating to breaches of takeover provisions, including the ability to make orders cancelling contracts, freezing
transfers of, and rights (including voting rights) attached to, securities, and forcing a party to dispose of securities including
by vesting the securities in ASIC for sale. There are certain defenses to breaches of the takeover provisions provided in the
Corporations Act.
Ownership Threshold
There are no provisions in our Constitution that require a shareholder to disclose ownership above a certain
threshold. The Corporations Act, however, requires a substantial shareholder to notify us and the ASX once a 5% interest
in our ordinary shares is obtained. Further, once a shareholder has (alone or together with associates) a 5% or greater
interest in us, such shareholder must notify us and the ASX of any increase or decrease of 1% or more in its interest in our
ordinary shares. In addition, the Constitution requires a shareholder to provide information to the Company in relation to its
entry into any arrangement restricting the transfer or other disposal of shares, which are of the nature of arrangements that
Mesoblast is required to disclose under the ASX Listing Rules. Following our initial public offering in the United States,
our shareholders are also subject to disclosure requirements under U.S. securities laws.
Issues of Shares and Change in Capital
Subject to our Constitution, the Corporations Act, the ASX Listing Rules and any other applicable law, we may at
any time grant options over unissued shares and issue shares on any terms, with any preferential, deferred or special rights,
privileges or conditions; with any restrictions in regard to dividend, voting, return of capital or otherwise, and for the
consideration and other terms that the directors determine. Our power to issue shares includes the power to issue bonus
shares (for which no consideration is payable to Mesoblast), preference shares and partly paid shares.
Subject to the requirements of our Constitution, the Corporations Act, the ASX Listing Rules and any other
applicable law, including relevant shareholder approvals, we may reduce our share capital (provided that the reduction is
fair and reasonable to our shareholders as a whole, does not materially prejudice our ability to pay creditors and obtains the
necessary shareholder approval) or buy back our ordinary shares including under an equal access buy-back or on a
selective basis. Under the Constitution, the directors may do anything required to give effect to any resolution altering or
approving the reduction of our share capital.
Access to and Inspection of Documents
Inspection of our records is governed by the Corporations Act. Any member of the public has the right to inspect
or obtain copies of our share registers on the payment of a prescribed fee. Shareholders are not required to pay a fee for
inspection of our share registers or minute books of the meetings of shareholders. Other corporate records, including
minutes of directors’ meetings, financial records and other documents, are not open for inspection by shareholders. Where
a shareholder is acting in good faith and an inspection is deemed to be made for a proper purpose, a shareholder may apply
to the court to make an order for inspection of our books.
10.C
Material Contracts
Manufacturing Service Agreements with Lonza Bioscience Singapore Pte. Ltd.
In September 2011, we entered into a manufacturing services agreement, or MSA, with Lonza Walkersville, Inc.
and Lonza Bioscience Singapore Pte. Ltd., collectively referred to as Lonza, a global leader in biopharmaceutical
manufacturing. Under the MSA, we pay Lonza on a fee for service basis to provide us with manufacturing process
development capabilities for our product candidates, including formulation development, establishment and maintenance of
master cell banks, records preparation, process validation, manufacturing and other services.
We have agreed to order a certain percentage of our clinical requirements and commercial requirements for MPC
products from Lonza. Lonza has agreed not to manufacture or supply commercially biosimilar versions of any of our
product candidates to any third party, during the term of the MSA, subject to our meeting certain thresholds for sales of our
products.
We can trigger a process requiring Lonza to construct a purpose-built manufacturing facility exclusively for our
product candidates. In return if we exercise this option, we will purchase agreed quantities of our product candidates from
this facility. We also have a right to buy out this manufacturing facility at a pre-agreed price two years after the facility
receives regulatory approval.
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The MSA will expire on the three-year anniversary of the date of the first commercial sale of product supplied
under the MSA, unless it is sooner terminated. We have the option of extending the MSA for an additional 10 years,
followed by the option to extend for successive three-year periods subject to Lonza’s reasonable consent. We may
terminate the MSA with two years prior written notice, and Lonza may terminate with five years prior written notice. The
MSA may also terminate for other reasons, including if the manufacture or development of a product is suspended or
abandoned due to the results of clinical trials or guidance from a regulatory authority. In the event we request that Lonza
construct the manufacturing facility described above, neither we nor Lonza may terminate before the third anniversary of
the date the facility receives regulatory approval to manufacture our product candidates, except in certain limited
circumstances. Upon expiration or termination of the MSA, we have the right to require Lonza to transfer certain
technologies and lease the Singapore facility or the portion of such facility where our product candidates are manufactured,
subject to good faith negotiations.
We currently rely, and expect to continue to rely, on Lonza for the manufacture of our MPC product candidates
for preclinical and clinical testing, as well as for commercial manufacture of our MPC product candidates if marketing
approval is obtained.
In October 2019, we entered into an agreement with Lonza for commercial manufacture of remestemcel-L for
pediatric SR-aGVHD. This agreement has facilitated inventory build ahead of the planned US market launch of
remestemcel-L and commercial supply to meet Mesoblast’s long-term market projections. The agreement provides for
Lonza to expand its Singapore cGMP facilities if required to meet long-term growth and capacity needs for the product.
Additionally, it anticipates introduction of new technologies and process improvements which are expected to result in
significant increases in yields and efficiencies.
Under the agreement, we agree to order a certain percentage of our commercial requirements for remestemcel-L
from Lonza. The agreement is subject to standard provisions for termination and its effects, including termination by either
party for uncured, material breach of the other, by us in the event of FDA related rejection or delay of approval of
remestemcel-L and after a specified minimum period following the initiation date by either party, on advance notice to the
other, which in the case Lonza is the terminating party is intended to provide us sufficient time to transfer the manufacture
of the product to an alternative manufacturer.
License Agreement with Grünenthal GmbH
In September 2019, we entered into a strategic partnership with Grünenthal GmbH (Grünenthal) to develop and
commercialize MPC-06-ID, the Company’s Phase 3 allogeneic cell therapy candidate for the treatment of chronic low back
pain due to degenerative disc disease in patients who have exhausted conservative treatment options. The agreement was
amended by the parties in June 2021. Under the partnership, Grünenthal will have exclusive commercialization rights to
MPC-06-ID for Europe and Latin America. We may receive up to $112.5 million in upfront and milestone payments prior
to product launch, inclusive of $17.5 million already received, if certain clinical and regulatory milestones are satisfied and
reimbursement targets are achieved. Cumulative milestone payments could exceed $1.0 billion depending on the final
outcome of Phase 3 studies and patient adoption. We will also receive tiered double-digit royalties on product sales. There
cannot be any assurance as to the total amount of future milestone and royalty payments that Mesoblast will receive nor
when they will be received.
Grünenthal is able to terminate the agreement with a specified period of notice without cause, or on shorter notice
in the case of certain clinical, regulatory and commercial events. We have termination rights with respect to certain patent
challenges by Grünenthal. Either party may terminate the agreement on material breach of the agreement if such breach is
not cured within the specified cure period or if certain events related to bankruptcy of the other party occurs. For more
information, see “Item 18. Financial Statements - Note 23 – Revenue recognition.”
Agreements with JCR Pharmaceuticals Co., Ltd.
In October 2013, we acquired all of Osiris Therapeutics, Inc.’s business and assets related to culture expanded
MSCs. These assets included assumption of a collaboration agreement with JCR (“JCR Agreement”), which will continue
in existence until the later of 15 years from the first commercial sale of any product covered by the agreement and
expiration of the last Osiris patent covering any such product. JCR is a research and development oriented pharmaceutical
company in Japan. Under the JCR Agreement we assumed from Osiris, JCR has the right to develop our MSCs in two
fields for the Japanese market: exclusive in conjunction with the treatment of hematological malignancies by the use of
HSCs derived from peripheral blood, cord blood or bone marrow, or the First JCR Field; and non-exclusive for developing
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assays that use liver cells for non-clinical drug screening and evaluation, or the Second JCR Field. Under the JCR
Agreement, JCR obtained rights in Japan to our MSCs, for the treatment of aGVHD. JCR also has a right of first
negotiation to obtain rights to commercialize MSC-based products for additional orphan designations in Japan. We retain
all rights to those products outside of Japan.
JCR received full approval in September 2015 for its MSC-based product for the treatment of children and adults
with aGVHD, TEMCELL. TEMCELL is the first culture-expanded allogeneic cell therapy product to be approved in
Japan. It was launched in Japan in February 2016.
Under the JCR Agreement, JCR is responsible for all development and manufacturing costs including sales and
marketing expenses. With respect to the First JCR Field, we have received all sales milestone payments, a total of $3.0
million. Ongoing we are entitled to escalating double-digit royalties in the twenties. These royalties are subject to possible
renegotiation downward in the event of competition from non-infringing products in Japan. With respect to the Second
JCR Field, we are entitled to an approximately 50% profit share.
Intellectual property is licensed both ways under the JCR Agreement, with JCR receiving exclusive and non-
exclusive rights as described above from us and granting us non-exclusive, royalty-free rights (excluding in the First JCR
Field and Second JCR Field in Japan) under the intellectual property arising out of JCR’s development or
commercialization of MSC-based products licensed in Japan.
JCR has the right to terminate the JCR Agreement for any reason, and we have a limited right to terminate the
JCR Agreement, including a right to terminate in the event of an uncured material breach by JCR. In the event of a
termination of the JCR Agreement other than for our breach, JCR must provide us with its owned product registrations and
technical data related to MSC-based products licensed in Japan and all licenses of our intellectual property rights will revert
to us.
We expanded our partnership with JCR in Japan for two new indications: for wound healing in patients with EB in
October 2018, and for neonatal hypoxic ischemic encephalopathy ("HIE"), a condition suffered by newborns who lack
sufficient blood supply and oxygen to the brain, in June 2019.
We will receive royalties on TEMCELL product sales for licensed indications, if and when such indications
receive marketing approval in Japan.
We have the right to use all safety and efficacy data generated by JCR in Japan to support our development and
commercialization plans for our MSC product candidate remestemcel-L in the United States and other major healthcare
markets, including for GVHD, EB and HIE.
Loan Agreement with Oaktree
In November 2021, we entered into a five-year senior debt facility provided by funds associated with Oaktree. The
balance of funds drawn down is $50.0 million as of June 30, 2024. The facility has a three-year interest only period, at a
fixed rate of 9.75% per annum, after which the principal amortizes 5% per quarter beginning December 2024 and a final
payment is due no later than November 2026. The facility also allowed us to make quarterly payments of interest at a rate
of 8.0% per annum for the first two years, and the unpaid interest portion (1.75% per annum) has been added to the
outstanding loan balance and shall accrue further interest at a fixed rate of 9.75% per annum. The loan agreement contains
certain covenants, see “Item 18. Financial Statements - Note 5(f).”
In November 2021, Oaktree was granted warrants to purchase 1,769,669 American Depositary Shares (“ADSs”)
at $7.26 per ADS, a 15% premium to the 30-day VWAP. The warrants were legally issued in January 2022 and may be
exercised within 7 years of issuance.
In December 2022, we amended the terms of the loan agreement with Oaktree and in connection with the loan
amendment, Oaktree was granted warrants to purchase 455,000 ADSs at $3.70 per ADS, a 15% premium to the 30-day
VWAP. The warrants were legally issued in March 2023 and may be exercised within 7 years of issuance.
In January 2024, the ratio under Mesoblast's American Depository Receipt ("ADR") program was changed from 5
ordinary shares representing 1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio). As a
result of this ratio change and as a result of initiating the pro-rata accelerated non-renounceable rights issue in December
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2023, the number and exercise price for the warrants granted to Oaktree was adjusted in accordance with the terms of these
warrants. The warrants issued to Oaktree in November 2021 changed from 1,769,669 ADSs at $7.26 per ADS to 884,838
ADSs at $14.36 per ADS. The warrants issued to Oaktree in December 2022 changed from 455,000 ADSs at $3.70 per
ADS to 227,502 ADSs at $7.24 per ADS.
Loan Agreement with NovaQuest
In June 2018, we entered into an eight-year non-dilutive secured loan with NovaQuest for $40.0 million. We drew
the first tranche of $30.0 million on closing. The loan term includes an interest only period of approximately four years
through until July 8, 2022, then a four-year amortization period through until maturity on July 8, 2026.
All interest and principal payments will be deferred until after the first commercial sale of our allogeneic product
candidate remestemcel-L for the treatment in pediatric patients with SR-aGVHD, in the United States and other
geographies excluding Asia (“pediatric aGVHD”). Principal is repayable in equal quarterly instalments over the
amortization period of the loan and is subject to the payment cap described below. Interest on the loan will accrue at a fixed
rate of 15% per annum. If there are no net sales of remestemcel-L for pediatric SR-aGVHD, the loan is only repayable at
maturity. We can elect to prepay all outstanding amounts owing at any time prior to maturity, subject to a prepayment
charge, and may decide to do so if net sales of pediatric aGVHD are significantly higher than current forecasts.
Following approval and first commercial sales, repayments commence based on a percentage of net sales and are
limited by a payment cap which is equal to the principal due for the next 12 months, plus accumulated unpaid principal and
accrued unpaid interest. During the four-year period commencing July 8, 2022, principal amortizes in equal quarterly
instalments payable only after approval and first commercial sales. If in any quarterly period, 25% of net sales of pediatric
SR-aGVHD exceed the annual payment cap, we will pay the payment cap and an additional portion of excess sales which
will be used towards the prepayment amount in the event there is an early prepayment of the loan. If in any quarterly period
25% of net sales of pediatric SR-aGVHD is less than the annual payment cap, then the payment is limited to 25% of net
sales of pediatric SR-aGVHD. Any unpaid interest will be added to the principal amounts owing and will accrue further
interest. At maturity date, any unpaid loan balances are repaid. The loan agreement contains certain covenants, see “Item
5.B Liquidity and Capital Resource – Borrowings.”
Osiris Acquisition—Continuing Obligations
In October 2013, we and Osiris entered into a purchase agreement, as amended, or the Osiris Purchase Agreement,
under which we acquired all of Osiris’ business and assets related to culture expanded MSCs. Pursuant to the Osiris
Purchase Agreement, we also agreed to make certain milestone and royalty payments to Osiris pertaining to remestemcel-L
for the treatment of aGVHD and Crohn’s disease. Each milestone payment is for a fixed dollar amount and may be paid in
cash or our ordinary shares or ADSs, at our option. The maximum amount of future milestone payments we may be
required to make to Osiris is $40.0 million. Any ordinary shares or ADSs we issue as consideration for a milestone
payment will be subject to a contractual one year holding period, which may be waived in our discretion. In the event that
the price of our ordinary shares or ADSs decreases between the issue date and the expiration of any applicable holding
period, we will be required to make an additional payment to Osiris equal to the reduction in the share price multiplied by
the amount of issued shares under that milestone payment. This additional payment can be made either wholly in cash or
50% in cash and 50% in our ordinary shares, in our discretion. We have also agreed to pay varying earnout amounts as a
percentage of annual net sales of acquired products, ranging from low single-digit to 10% of annual sales in excess of
$750.0 million. These royalty payments will cease after the earlier of a ten year commercial sales period and the first sale
of a relevant competing product. The first royalty payments were made in 2016.
Agreements with Tasly Pharmaceutical Group
In July 2018, we entered into a Development and Commercialization Agreement with Tasly.
The Development and Commercialization Agreement provides Tasly with exclusive rights to develop,
manufacture and commercialize in China MPC-150-IM for the treatment or prevention of chronic heart failure and
MPC-25-IC for the treatment or prevention of acute myocardial infarction. Tasly will fund all development, manufacturing
and commercialization activities in China for MPC-150-IM and MPC-25-IC. On closing, we received a $20.0 million
upfront technology access fee. Further, we will receive $25.0 million on product regulatory approvals in China. Mesoblast
will receive double-digit escalating royalties on net product sales. Mesoblast is eligible to receive six escalating milestone
payments upon the product candidates reaching certain sales thresholds in China.
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The Development and Commercialization Agreement provides that Tasly can terminate this agreement with a
specified amount of notice, on the later of (a) third anniversary of the agreement coming into effect and (b) receipt of
marketing approval in China for each of MPC-150-IM or MPC-25-IC. Mesoblast has termination rights with respect to
certain patent challenges by Tasly and if certain competing activities are undertaken by Tasly. Either party may terminate
the agreement on material breach of the agreement if such breach is not cured within the specified cure period or if certain
events related to bankruptcy of the other party occurs.
TiGenix NV – patent license for treatment of fistulae
In December 2017, we entered into a Patent License Agreement with TiGenix NV, now a wholly owned
subsidiary of Takeda, which granted Takeda exclusive access to certain of our patents to support global commercialization
of the adipose-derived mesenchymal stromal cell product Alofisel®, previously known as Cx601, a product candidate of
Takeda, for the local treatment of fistulae. The agreement includes the right for Takeda to grant sub-licenses to affiliates
and third parties.
As part of the agreement, we received $5.9 million (€5.0 million) before withholding tax as a non-refundable
upfront payment, a further payment of $5.9 million (€5.0 million) before withholding tax 12 months after the patent license
agreement date, and a further $1.2 million (€1.0 million) product regulatory milestone payment in the year ended June 30,
2022. We are entitled to further payments up to €9.0 million when Takeda reaches certain product regulatory milestones.
Additionally, we receive single digit royalties on net sales of Alofisel®.
The agreement will continue in full force in each country (other than the United States) until the date upon which
the last issued claim of any licensed patent covering Alofisel® expires in such country (currently expected to be 2029) or,
with respect to the United States, until the later of (i) the date upon which the last issued claim of any licensed patent
covering Alofisel® in the United States expires (currently expected to be around 2031) or (ii) the expiration of the
regulatory exclusivity period in the United States with an agreed maximum term.
Either we or Takeda may terminate the agreement for any material breach that is not cured within 90 days after
notice. We also have the right to terminate the agreement with a written notice in the event that Takeda file a petition in
bankruptcy or insolvency or Takeda makes an assignment of substantially all of its assets for the benefit of its creditors.
Takeda has the right to terminate its obligation to pay royalties for net sales in a specific country if it is of the
opinion that there is no issued claim of any licensed patent covering Alofisel® in such country, subject to referral of the
matter to the joint oversight/cooperation committee established under the agreement if we disagree.
10.D
Exchange Controls
The Australian dollar is freely convertible into U.S. dollars. In addition, there are currently no specific rules or
limitations regarding the export from Australia of profits, dividends, capital or similar funds belonging to foreign investors,
except that certain payments to non-residents must be reported to the Australian Transaction Reports and Analysis Centre
(“AUSTRAC”), which monitors such transaction, and amounts on account of potential Australian tax liabilities may be
required to be withheld unless a relevant taxation treaty can be shown to apply.
Regulation of acquisition by foreign entities
Under Australian law, in certain circumstances foreign persons are prohibited from acquiring more than a limited
percentage of the shares in an Australian company without approval from the Australian Treasurer (or their delegate).
These limitations are set forth in the Foreign Acquisitions and Takeovers Act 1975 (Cth) (FATA) and its associated
legislative instruments. These limitations are in addition to the more general overarching Takeovers Prohibition of an
acquisition of more than a 20% interest in a public company (in the absence of an applicable exception) under the takeovers
provisions of the Corporations Act 2001 (Cth) (Corporations Act) by any person whether foreign or otherwise.
Under the FATA, as currently in effect, any foreign person, together with associates (including parties acting in
concert) is prohibited from acquiring 20% or more of the shares in any company having consolidated total assets of or that
is valued at A$330.0 million or more (or A$1,427.0 million or more for investors from certain Foreign Trade Agreement
countries including the U.S.). A smaller interest threshold of 10% applies to foreign government investors, and no asset
threshold applies to this class of investors. Different rules apply to national security sectors (including critical
infrastructure, critical goods, services or technology for a military use, and businesses that have access to security classified
information and/or information that could compromise Australia's national security) sensitive industries (such as media,
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telecommunications, and encryption and security technologies), companies owning land or that are agribusinesses.
“Associates” is a broadly defined term under the FATA and includes in relation to any person:
•
any relative of the person;
•
any person with whom the person is acting or proposes to act in concert in relation to an action to which
the FATA applies;
•
any person with whom the person carries on a business in partnership;
•
any entity of which the person is a ‘senior officer’ (such as a director or executive);
•
if the person is an entity, any holding entity or any senior officer of the entity;
•
any entity whose senior officers are accustomed or obliged to act in accordance with the directions,
instructions or wishes of the person or if the person is an entity, its senior officers or vice versa;
•
any corporation in which the person holds a ‘substantial interest’ (generally, 20% or more) or any person
holding a substantial interest in the person if a corporation;
•
a trustee of a trust in which the person holds a substantial interest or if the person is the trustee of a trust,
a person who holds a substantial interest in the trust;
•
if the person is a foreign government, a separate government entity or a foreign government investor in
relation to a foreign country, any other person that is a foreign government, a separate government entity
or foreign government investor, in relation to that country.
The Australian Treasurer also has power in certain circumstances to make an order specifying that two or more
persons are associates.
Each foreign person seeking to acquire holdings in excess of the above caps (including their associates, as the case
may be) would need to complete an application form setting out the proposal and relevant particulars of the acquisition/
shareholding and pay the relevant application fees. The Australian Treasurer then has 30 days to consider the application
and make a decision. However, the Australian Treasurer may extend the period if more time is required to complete the
assessment, including by up to a further 90 days by publishing an interim order. The Australian Foreign Investment Review
Board (FIRB), an Australian advisory board to the Australian Treasurer, has provided a guideline titled Australia’s Foreign
Investment Policy which provides an outline of the policy. As for the risk associated with seeking approval, the policy
provides, among other things, that the Treasurer will prohibit a proposed transaction if it is contrary to Australia's national
interest (or national security).
If the necessary approvals are not obtained, the Australian Treasurer is empowered to make a number of adverse
orders, including an order requiring the acquirer to dispose of the shares it has acquired within a specified period of time.
Civil and criminal penalties also apply for breaches of the FATA including imprisonment for up to 10 years and fines of up
to 150,000 penalty units.
As a public company with its primary listing on the Australian Securities Exchange (ASX), Mesoblast will be
considered a foreign person under the FATA where:
•
a single foreign person (including an individual not ordinarily resident in Australia, a foreign corporation,
or a foreign government) holds a substantial interest; or
•
multiple foreign persons hold together, in aggregate, 40% or more of the total issued shares after
discounting any person holding an interest (alone or with its associates) that is not a 'substantial holding'
within the meaning of the Corporations Act.
In such event, we would be required to obtain the approval of the Australian Treasurer for our company, together
with our associates, to acquire (i) more than 20% of an Australian company or business having total assets of, or that is
valued at, A$330.0 million or more; or (ii) any interest in Australian land; or (iii) any ‘direct interest’ in any agribusiness or
national security business. Different thresholds will apply to the extent that we are considered to be a foreign government
investor due to our ownership.
The percentage of foreign ownership in our company may also be included in determining the foreign ownership
of any Australian company or business in which we may choose to invest. Since we have no current plans for any such
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acquisition and do not own any property, any such approvals required to be obtained by us as a foreign person under the
FATA will not affect our current or future ownership or lease of property in Australia.
Our Constitution does not contain any additional limitations on the right to hold or vote our securities by reason of
being a non-resident.
Australian law requires the transfer of shares in our company to be made in writing or electronically through the
Clearing House Electronic Sub-register System.
10.E
Taxation
The following summary of the material Australian and U.S. federal income tax consequences of an investment in
our ADSs or ordinary shares is based upon laws and relevant interpretations thereof in effect as of the date of this Form 20-
F, all of which are subject to change, possibly with retroactive effect. This summary does not deal with all possible tax
consequences relating to an investment in our ADSs or ordinary shares, such as the tax consequences under U.S. state,
local and other tax laws other than Australian and U.S. federal income tax laws.
Certain Material U.S. Federal Income Tax Considerations to U.S. Holders
The following summary describes certain material U.S. federal income tax consequences to U.S. holders (as
defined below) of the ownership and disposition of our ordinary shares and ADSs as of the date hereof. Except where
noted, this summary deals only with our ordinary shares or ADSs acquired and held as capital assets within the meaning of
Section 1221 of the Internal Revenue Code of 1986, as amended (the “Code”). This section does not discuss the tax
consequences to any particular holder, nor any tax considerations that may apply to holders subject to special tax rules,
such as:
•
banks, insurance companies, regulated investment companies and real estate investment trusts;
•
financial institutions;
•
individual retirement and other tax-deferred accounts;
•
certain former U.S. citizens or long-term residents;
•
brokers or dealers in securities or currencies;
•
traders that elect to use a mark-to-market method of accounting;
•
partnerships and other entities treated as partnership or pass through entities for U.S. federal income tax
purposes, and partners or investors in such entities;
•
tax-exempt organizations (organizations that would be exempt from tax under U.S. law, including public
charities and private foundations);
•
persons that may have been subject to the alternative minimum tax;
•
persons that hold or dispose of ordinary shares or ADSs as a position in a straddle or as part of a hedging,
constructive sale, conversion or other integrated transaction;
•
persons that have a functional currency other than the U.S. dollar;
•
persons that own (directly, indirectly or constructively) 10% or more of the vote or value of our equity;
•
persons subject to special tax accounting rules as a result of any item of gross income with respect to
ordinary shares or ADSs being taken into account in an applicable financial statement;
•
persons who acquire ordinary shares or ADSs pursuant to the exercise of any employee share option or
otherwise as compensation; or
•
persons that are not U.S. holders (as defined below).
In this section, a “U.S. holder” means a beneficial owner of ordinary shares or ADSs, other than a partnership or
other entity treated as a partnership for U.S. federal income tax purposes, that is, for U.S. federal income tax purposes:
•
an individual who is a citizen or resident of the United States (for U.S. federal income tax purposes);
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•
a corporation (or other entity classified for purposes of and pursuant to U.S. federal income tax laws as a
corporation) created or organized in or under the laws of the United States or any state thereof or the
District of Columbia;
•
an estate the income of which is includable in gross income for U.S. federal income tax purposes
regardless of its source; or
•
a trust (i) the administration of which is subject to the primary supervision of a court in the United States
and for which one or more U.S. persons have the authority to control all substantial decisions or (ii) that
has an election in effect under applicable U.S. income tax regulations to be treated as a U.S. person.
The discussion below is based upon the provisions of the Code, and the U.S. Treasury regulations, rulings and
judicial decisions thereunder as of the date hereof, and such authorities may be replaced, revoked or modified, possibly
with retroactive effect, so as to result in U.S. federal income tax consequences different from those discussed below. In
addition, this summary is based, in part, upon the terms of the deposit agreement and assumes that the deposit agreement,
and all other related agreements, will be performed in accordance with their terms.
If a partnership or an entity or arrangement treated as a partnership for U.S. federal income tax purposes acquires,
owns or disposes of ordinary shares or ADSs, the U.S. federal income tax treatment of a partner generally will depend on
the status of the partner and the activities of the partnership. Partners of partnerships that acquire, own or dispose of
ordinary shares or ADSs should consult their tax advisors.
You are urged to consult your own tax advisor with respect to the U.S. federal, as well as state, local and non-U.S., tax
consequences to you of acquiring, owning and disposing of ordinary shares or ADSs in light of your particular
circumstances, including the possible effects of changes in U.S. federal income and other tax laws and the effects of any
tax treaties.
ADSs
Assuming the deposit agreement and all other related agreements will be performed in accordance with their
terms, a U.S. holder of ADSs will be treated as the beneficial owner for U.S. federal income tax purposes of the underlying
shares represented by the ADSs. The U.S. Treasury has expressed concerns that parties to whom American depositary
shares are released before shares are delivered to the depositary, or intermediaries in the chain of ownership between
holders of American depositary shares and the issuer of the security underlying the American depositary shares, may be
taking actions that are inconsistent with claiming foreign tax credits by holders of American depositary shares. These
actions would also be inconsistent with claiming the reduced rate of tax, described below, applicable to dividends received
by certain non-corporate holders. Accordingly, the creditability of any foreign taxes and the availability of the reduced tax
rate for dividends received by certain non-corporate U.S. holders, each described below, could be affected by actions taken
by such parties or intermediaries.
Distributions
Subject to the passive foreign investment company, or PFIC, rules discussed below, U.S. holders generally will
include as gross dividend income the U.S. dollar value of the gross amount of any distributions of cash or property, other
than certain pro rata distributions of ordinary shares, with respect to ordinary shares or ADSs to the extent the distributions
are made from our current or accumulated earnings and profits, as determined for U.S. federal income tax purposes.
Subject to the PFIC rules, a U.S. holder may be permitted to credit the taxes withheld, subject to a limitation, or deduct the
taxes withheld. A U.S. holder will include the dividend income on the day actually or constructively received: (i) by the
holder, in the case of ordinary shares, or (ii) by the depositary, in the case of ADSs. To the extent, if any, that the amount of
any distribution by us exceeds our current and accumulated earnings and profits, as so determined, the excess with respect
to any share (ordinary share or ADS) will be treated first as a tax-free return of the U.S. holder’s tax basis in such ordinary
share or ADS and thereafter as capital gain on such share. Notwithstanding the foregoing, we do not intend to determine
our earnings and profits on the basis of U.S. federal income tax principles. Consequently, any distributions generally will
be reported as dividend income for U.S. information reporting purposes. See “—Backup Withholding Tax and Information
Reporting Requirements” below. Dividends paid by us will not be eligible for the dividends-received deduction generally
allowed to U.S. corporate shareholders.
The U.S. dollar amount of dividends received by an individual, trust or estate with respect to the ordinary shares
or ADSs will be subject to taxation at preferential rates if the dividends are “qualified dividends.” Dividends paid on
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ordinary shares or ADSs will be treated as qualified dividends if (i)(a) we are eligible for the benefits of a comprehensive
income tax treaty with the United States that the Secretary of the Treasury of the United States determines is satisfactory
for this purpose and includes an exchange of information program or (b) the dividends are with respect to ordinary shares
(or ADSs in respect of such shares) which are readily tradable on a U.S. securities market; (ii) certain holding period
requirements are met; and (iii) we are not classified as a PFIC for the taxable year in which the dividend is paid or for the
preceding taxable year. The Agreement between the Government of the United States of America and the Government of
Australia for the Avoidance of Double Taxation and the Prevention of Fiscal Evasion with Respect to Taxes on Income, or
the Treaty, has been approved for the purposes of the qualified dividend rules, and we expect to qualify for benefits under
the Treaty. In addition, our ADSs are listed on the Nasdaq Global Select Market, and as such U.S. Treasury Department
guidance indicates that our ADSs will be readily tradable on an established U.S. securities market. Thus, we believe that as
long as we are not a PFIC, dividends we pay generally should be eligible for the preferential tax rates on qualified
dividends. However, the determination of whether a dividend qualifies for the preferential tax rates must be made at the
time the dividend is paid. U.S. holders should consult their own tax advisors regarding the availability of the preferential
tax rates on dividends.
Includible distributions paid in Australian dollars, including any Australian withholding taxes, will be included in
the gross income of a U.S. holder in a U.S. dollar amount calculated by reference to the spot exchange rate in effect on the
date of actual or constructive receipt, regardless of whether the Australian dollars are converted into U.S. dollars at that
time. If Australian dollars are converted into U.S. dollars on the date of actual or constructive receipt, the tax basis of the
U.S. holder in those Australian dollars will be equal to their U.S. dollar value on that date and, as a result, a U.S. holder
generally should not be required to recognize any foreign currency exchange gain or loss. If Australian dollars so received
are not converted into U.S. dollars on the date of receipt, the U.S. holder will have a basis in the Australian dollars equal to
their U.S. dollar value on the date of receipt. Any foreign currency exchange gain or loss on a subsequent conversion or
other disposition of the Australian dollars generally will be treated as ordinary income or loss to such U.S. holder and
generally will be income or loss from sources within the United States for foreign tax credit limitation purposes.
Dividends received by a U.S. holder with respect to ordinary shares (or ADSs in respect of such shares) will be
treated as foreign source income, which may be relevant in calculating the holder’s foreign tax credit limitation. The
limitation on foreign taxes eligible for credit is calculated separately with respect to specific classes of income. For this
purpose, dividends distributed by us with respect to ADSs or ordinary shares will generally constitute “passive category
income” but could, in the case of certain U.S. holders, constitute “general category income.”
Subject to certain complex limitations, including the PFIC rules discussed below, a U.S. holder generally will be
entitled, at such holder’s option, to claim either a credit against such holder’s U.S. federal income tax liability or a
deduction in computing such holder’s U.S. federal taxable income in respect of any Australian taxes withheld. If a U.S.
holder elects to claim a deduction, rather than a foreign tax credit, for Australian taxes withheld for a particular taxable
year, the election will apply to all foreign taxes paid or accrued by or on behalf of the U.S. holder in the particular taxable
year.
The availability of the foreign tax credit and the application of the limitations on its availability are fact specific
and are subject to complex rules. You are urged to consult your own tax advisor as to the consequences of Australian
withholding taxes and the availability of a foreign tax credit or deduction. See “—Australian Tax Considerations Australian
—Income Tax—Taxation of Dividends” below.
Sale, Exchange or Other Disposition of Ordinary Shares or ADSs
Subject to the PFIC rules discussed below, a U.S. holder generally will, for U.S. federal income tax purposes,
recognize capital gain or loss, if any, on a sale, exchange or other disposition of ordinary shares or ADSs equal to the
difference between the amount realized on the disposition and the U.S. holder’s tax basis (in U.S. dollars) in the ordinary
shares or ADSs. This recognized gain or loss will generally be long-term capital gain or loss if the U.S. holder has held the
ordinary shares or ADSs for more than one year. Generally, for U.S. holders who are individuals (as well as certain trusts
and estates), long-term capital gains are subject to U.S. federal income tax at preferential rates. For foreign tax credit
limitation purposes, gain or loss recognized upon a disposition generally will be treated as from sources within the United
States. The deductibility of capital losses is subject to limitations for U.S. federal income tax purposes.
You should consult your own tax advisor regarding the tax consequences if a foreign tax is imposed on a
disposition of ADSs or ordinary shares, including availability of a foreign tax credit or deduction in respect of any
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Australian tax imposed on a sale or other disposition of ordinary shares or ADSs. See “—Australian Tax Considerations—
Australian Income Tax—Tax on Sales or Other Dispositions of Shares—Capital Gains Tax.”
Passive Foreign Investment Company
As a non-U.S. corporation, we will be a PFIC for any taxable year if either: (i) 75% or more of our gross income
for the taxable year is passive income (such as certain dividends, interest, rents or royalties and certain gains from the sale
of shares and securities or commodities transactions, including amounts derived by reason of the temporary investment of
funds raised in offerings of our ordinary shares or ADSs); or (ii) the average quarterly value of our gross assets during the
taxable year that produce passive income or are held for the production of passive income is at least 50% of the value of
our total assets. For purposes of the PFIC asset test, passive assets generally include any cash, cash equivalents and cash
invested in short-term, interest bearing debt instruments or bank deposits that are readily convertible into cash. If we own at
least 25% (by value) of the stock of another corporation, we will be treated, for purposes of the PFIC income and asset
tests, as owning our proportionate share of the other corporation’s assets and receiving our proportionate share of the other
corporation’s income.
We do not believe that we were a PFIC for the taxable year ending June 30, 2024. However, if there is a change in
the type or composition of our gross income, or our actual business results do not match our projections, it is possible that
we may become a PFIC in future taxable years. Investors should be aware that our gross income for purposes of the PFIC
income test depends on the receipt of Australian research and development tax incentive credits and other revenue, and
there can be no assurances that such tax incentive credit programs will not be revoked or modified, that we will continue to
conduct our operations in the manner necessary to be eligible for such incentives or that we will receive other gross income
that is not considered passive for purposes of the PFIC income test. The value of our assets for purposes of the PFIC asset
test will generally be determined by reference to our market capitalization, which may fluctuate. The composition of our
income and assets will also be affected by how, and how quickly, we spend the cash raised in offerings of our ordinary
shares or ADSs. Under circumstances where our gross income from activities that produce passive income significantly
increases relative to our gross income from activities that produce non-passive income or where we decide not to deploy
significant amounts of cash for active purposes, our risk of becoming classified as a PFIC may substantially increase. Since
a separate factual determination as to whether we are or have become a PFIC must be made each year (after the close of
such year), we cannot assure you that we will not be or become a PFIC in the current year or any future taxable year. There
can be no assurance that we will not be a PFIC for any taxable year, as PFIC status is determined each year and depends on
the composition of our income and assets and the value of our assets in such year. If we are a PFIC for any taxable year,
upon request, we intend to provide U.S. holders with the information necessary to make and maintain a “Qualified Electing
Fund” election, as described below.
Default PFIC Rules
If we are a PFIC for any taxable year during which you own our ordinary shares or ADSs, unless you make the
mark-to-market election or the Qualified Electing Fund election described below, you will generally be (and remain)
subject to additional taxes and interest charges, regardless of whether we remain a PFIC in any subsequent taxable year, (i)
on certain “excess distributions” we may make; and (ii) on any gain realized on the disposition or deemed disposition of
your ordinary shares or ADSs. Distributions in respect of your ordinary shares (or ADSs in respect of such shares) during
the taxable year will generally constitute “excess” distributions if, in the aggregate, they exceed 125% of the average
amount of distributions in respect of your ordinary shares (or ADSs) over the three preceding taxable years or, if shorter,
the portion of your holding period before such taxable year.
To compute the tax on “excess” distributions or any gain: (i) the “excess” distribution or the gain will be allocated
ratably to each day in your holding period for the ADSs or the ordinary shares; (ii) the amount allocated to the current
taxable year and any taxable year before we became a PFIC will be taxed as ordinary income in the current year; (iii) the
amount allocated to other taxable years will be taxable at the highest applicable marginal rate in effect for that year; and
(iv) an interest charge at the rate for underpayment of taxes will be imposed with respect to any portion of the “excess”
distribution or gain described under (iii) above that is allocated to such other taxable years. In addition, if we are a PFIC or,
with respect to a particular U.S. holder, we are treated as a PFIC for the taxable year in which the distribution was paid or
the prior taxable year, no distribution that you receive from us will qualify for taxation at the preferential rate for non-
corporate holders discussed in “—Distributions” above. You should consult with your own tax advisor regarding the
application of the default PFIC rules based on your particular circumstances.
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If we are a PFIC for any taxable year during which a U.S. holder holds our ADSs or ordinary shares and any of
our non-U.S. subsidiaries is also a PFIC (i.e., a lower-tier PFIC), such U.S. holder would be treated as owning a
proportionate amount (by value) of the shares of the lower-tier PFIC and would be subject to the rules described above on
certain distributions by the lower-tier PFIC and our disposition of shares of the lower-tier PFIC, even though such U.S.
holder may not receive the proceeds of those distributions or dispositions. You should consult with your own tax advisor
regarding the application to you of the PFIC rules to any of our subsidiaries if we are a PFIC.
Mark-to-Market Election
If we are a PFIC for any taxable year during which you own our ADSs or ordinary shares, you will be able to
avoid the rules applicable to “excess” distributions or gains described above if the ordinary shares or ADSs are
“marketable” and you make a timely “mark-to-market” election with respect to your ordinary shares or ADSs. The ordinary
shares or ADSs will be “marketable” stock as long as they remain regularly traded on a national securities exchange, such
as the Nasdaq Global Select Market, or a foreign securities exchange regulated by a governmental authority of the country
in which the market is located and which meets certain requirements, including that the rules of the exchange effectively
promote active trading of listed stocks. If such stock is traded on such a qualified exchange or other market, such stock
generally will be “regularly traded” for any calendar year during which such stock is traded, other than in de minimis
quantities, on at least 15 days during each calendar quarter, but no assurances can be given in this regard. Our ordinary
shares are traded on the ASX, which may qualify as an eligible foreign securities exchange for this purpose.
If you are eligible to make a “mark-to-market” election with respect to our ordinary shares or ADSs and you make
this election in a timely fashion, you will generally recognize as ordinary income or ordinary loss the difference between
the fair market value of your ordinary shares or ADSs on the last day of any taxable year and your adjusted tax basis in the
ordinary shares or ADSs. Any ordinary income resulting from this election will generally be taxed at ordinary income
rates. Any ordinary losses will be deductible only to the extent of the net amount of previously included income as a result
of the mark-to-market election, if any. Your adjusted tax basis in the ordinary shares or ADSs will be adjusted to reflect
any such income or loss. Any gain recognized on the sale or other disposition of your ordinary shares or ADSs in a year
when we are a PFIC will be treated as ordinary income, and any loss will be treated as an ordinary loss (but only to the
extent of the net amount previously included as ordinary income as a result of the mark-to-market election).
Because a mark-to-market election cannot be made for any lower-tier PFICs that we may own, a U.S. holder may
continue to be subject to the PFIC rules with respect to such holder’s indirect interest in any investments held by us that are
treated as an equity interest in a PFIC for U.S. federal income tax purposes, including shares in any of our subsidiaries that
are treated as PFICs.
You should consult with your own tax advisor regarding the applicability and potential advantages and
disadvantages to you of making a “mark-to-market” election with respect to your ordinary shares or ADSs if we are or
become a PFIC, including the tax issues raised by lower-tier PFICs that we may own and the procedures for making such
an election.
QEF Election
Alternative rules to those set forth under “Default PFIC Rules” above apply if an election is made to treat us as a
“Qualified Electing Fund,” or QEF, under Section 1295 of the Code. A QEF election is available only if a U.S. holder
receives an annual information statement from us setting forth such holder’s pro rata share of our ordinary earnings and net
capital gains, as calculated for U.S. federal income tax purposes.
Upon request from a U.S. holder, we will endeavor to provide to the U.S. holder within 90 days after the request
an annual information statement, in order to enable the U.S. holder to make and maintain a QEF election for us or for any
of our subsidiaries that is or becomes a PFIC. However, there is no assurance that we will have timely knowledge of our or
our subsidiaries’ status as a PFIC in the future or of the required information to be provided. You should consult your own
tax advisor regarding the availability and tax consequences of a QEF election with respect to the ordinary shares or ADSs
or with respect to any lower-tier PFIC that we may own under your particular circumstances.
Reporting
If we are a PFIC for any taxable year during which you own our ordinary shares or ADSs, as a U.S. holder, you
will generally be required to file IRS Form 8621 on an annual basis and other reporting requirements may apply. The PFIC
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rules are complex and you should consult with your own tax advisor regarding whether we or any of our subsidiaries are a
PFIC, the tax consequences of any elections that may be available to you, and how the PFIC rules may affect the U.S.
federal income tax consequences of the receipt, ownership, and disposition of our ordinary shares or ADSs.
Tax on Net Investment Income
Certain non-corporate U.S. holders will be subject to a 3.8% tax on the lesser of (i) the U.S. holder’s “net
investment income” for the relevant taxable year; and (ii) the excess of the U.S. holder’s modified adjusted gross income
for the taxable year over a certain threshold. A U.S. holder’s net investment income will generally include dividends
received on the ordinary shares or ADSs and net gains from the disposition of ordinary shares or ADSs, unless such
dividend income or net gains are derived in the ordinary course of the conduct of a trade or business (other than a trade or
business that consists of certain passive or trading activities). A U.S. holder that is an individual, estate or trust should
consult the holder’s tax advisor regarding the applicability of the tax on net investment income to the holder’s dividend
income and gains in respect of the holder’s investment in the ordinary shares or ADSs.
Backup Withholding Tax and Information Reporting Requirements
U.S. backup withholding tax and information reporting requirements generally apply to payments to non-
corporate holders of ordinary shares or ADSs. Information reporting will apply to payments of dividends on, and to
proceeds from the disposition of, ordinary shares or ADSs by a paying agent within the United States to a U.S. holder,
other than U.S. holders that are exempt from information reporting and properly certify their exemption. A paying agent
within the United States will be required to withhold at the applicable statutory rate, currently 24%, in respect of any
payments of dividends on, and the proceeds from the disposition of, ordinary shares or ADSs within the United States to a
U.S. holder (other than U.S. holders that are exempt from backup withholding and properly certify their exemption) if the
holder fails to furnish its correct taxpayer identification number or otherwise fails to comply with applicable backup
withholding requirements. U.S. holders who are required to establish their exempt status generally must provide a properly
completed IRS Form W-9.
Backup withholding is not an additional tax. Amounts withheld as backup withholding may be credited against a
U.S. holder’s U.S. federal income tax liability. A U.S. holder generally may obtain a refund of any amounts withheld under
the backup withholding rules in excess of such holder’s U.S. federal income tax liability by filing the appropriate claim for
refund with the IRS in a timely manner and furnishing any required information.
Certain U.S. holders may be required to report (on IRS Form 8938) information with respect to such holder’s
interest in “specified foreign financial assets” (as defined in Section 6038D of the Code), including stock of a non-U.S.
corporation that is not held in an account maintained by a U.S. “financial institution.” Persons who are required to report
specified foreign financial assets and fail to do so may be subject to substantial penalties. U.S. holders are urged to consult
their own tax advisors regarding foreign financial asset reporting obligations and their possible application to the holding of
ordinary shares or ADSs.
The discussion above is a general summary only. It is not intended to constitute a complete analysis of all tax
considerations applicable to an investment in our ADSs or ordinary shares. You should consult with your own tax
advisor concerning the tax consequences to you of an investment in our ADSs or ordinary shares in light of your
particular circumstances.
Australian Tax Considerations
In this section, we discuss the material Australian income tax, stamp duty and goods and services (“GST”) tax
considerations related to the acquisition, ownership and disposal by the absolute beneficial owners of the ordinary shares or
ADSs. It is based upon existing Australian tax law as of the date of this annual report, which is subject to change, possibly
retrospectively. This discussion does not address all aspects of Australian tax law which may be important to particular
investors in light of their individual investment circumstances, such as shares held by investors subject to special tax rules
(for example, financial institutions, insurance companies, tax exempt organizations or employee share scheme
participants). In addition, this summary does not discuss any non-Australian tax considerations. Prospective investors are
urged to consult their tax advisors regarding the Australian and foreign income and other tax considerations of the
acquisition, ownership and disposition of the shares. This summary is based upon the premise that the holder is not an
Australian tax resident and is not carrying on business in Australia through a permanent establishment (referred to as a
“Foreign Shareholder” in this summary).
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Australian Income Tax
Nature of ADSs for Australian Taxation Purposes
Ordinary shares represented by ADSs held by a U.S. holder will be treated for Australian income tax purposes as
held under a “bare trust” for such holder. Consequently, the underlying ordinary shares will be regarded as owned by the
ADS holder for Australian income tax (including capital gains tax (“CGT”)) purposes. Dividends paid on the underlying
ordinary shares will also be treated as dividends paid to the ADS holder, as the person beneficially entitled to those
dividends.
Taxation of Dividends
Australia operates a dividend imputation system under which dividends may be declared to be “franked” to the
extent of tax paid on company profits. Fully franked dividends paid to Foreign Shareholders are not subject to dividend
withholding tax. Dividends paid to Foreign Shareholders are generally subject to dividend withholding tax, to the extent
that the dividends are not foreign (i.e. non-Australian) sourced, are not declared to be “conduit foreign income” (“CFI”),
and are unfranked. Dividend withholding tax will be imposed at 30%, unless a Foreign Shareholder is a resident of a
country with which Australia has a double taxation agreement ("DTA") and qualifies for the benefits of the DTA. Under
the provisions of the current DTA between Australia and the United States (“Australia-U.S. DTA”), the rate of tax
Australian tax to be withheld on unfranked dividends paid by Mesoblast Limited (the “Company”) (which are not declared
to CFI) to which a resident of the United States is beneficially entitled, is generally limited to 15% if the U.S. resident
holds less than 10% of the voting power in the Company.
If a Foreign Shareholder that is a company and is a resident of the United States holds 10% or more of the voting
power in the Company and is beneficially entitled to dividends from the Company, the rate of Australian dividend
withholding tax is limited to 5%. In limited circumstances, the rate of withholding can be reduced to zero.
Tax on Sales or Other Dispositions of Shares – CGT
A Foreign Shareholder will not be subject to Australian CGT on any gain made on the sale or other disposal of
ordinary shares in the Company, unless broadly it, together with associates, holds 10% or more of the issued capital in the
Company, at the time of disposal or for 12 months of the last 2 years prior to disposal.
A Foreign Shareholder who, together with associates, owns a 10% or more interest would be subject to Australian
CGT on the sale of that interest if more than 50% of the Company’s assets by market value (held directly or indirectly and
determined by reference to market value), consists of interests in Australian real property, which includes land and leases
of land, as well as mining, quarrying or prospecting rights (this is referred to as “taxable Australian property” (“TAP”)).
The Australian Government has announced changes to the TAP rules which are expected to take effect from 1 July 2025
and expand the definition, but legislation has not yet been introduced in this regard.
Relief from Australian CGT is unlikely to be provided by the Australian-U.S. DTA. Australian CGT applies to net
capital gains of Foreign Shareholders at the Australian tax rates for non-Australian residents, which start at a marginal rate
of 30% for individuals effective from 1 July 2024 (previously this was 32.5%). Net capital gains are calculated after
reduction for capital losses (including carry forward net capital losses provided that the relevant loss utilization tests have
been satisfied), noting that capital losses may only be offset against capital gains.
The 50% CGT discount is not available to non-Australian residents on gains that accrued after May 8, 2012.
Companies, whether Australian resident or not, are not entitled to the CGT discount.
Broadly, where there is a disposal of TAP, the purchaser will be required to withhold and remit to the Australian
Taxation Office (“ATO”) 12.5% of the proceeds from the sale. A transaction is excluded from the withholding
requirements in certain circumstances, including where the value of the TAP is less than A$750,000, the transaction is an
on-market transaction conducted on an approved stock exchange, a securities lending arrangement, or the transaction is
conducted using a broker operated crossing system. The Foreign Shareholder may be entitled to receive a tax credit for the
tax withheld by the purchaser which they may claim in their Australian income tax return. The Government has announced
amendments with effect from 1 January 2025 which will increase the withholding rate from 12.5% to 15.0% and remove
the current A$750,000 threshold. The amendments will require non-Australian residents disposing of shares and other
interests exceeding A$20 million in value to notify the ATO prior to the transaction being executed.
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Tax on Sales or Other Dispositions of Shares – Shareholders Holding Shares on Revenue Account
Some Foreign Shareholders may hold ordinary shares on “revenue” account rather than on capital account – for
example, share traders. These shareholders may have the gains made on the sale or other disposal of the ordinary shares
included in their assessable income under the ordinary income or trading stock provisions of the income tax law, if the
gains are sourced in Australia.
Foreign Shareholders assessable under these ordinary income provisions in respect of gains made on ordinary
shares held on revenue account would be assessed for such gains at the Australian tax rates for non-Australian residents,
which start at a marginal rate of 30.0% for individuals effective from 1 July 2024 (previously 32.5%). Relief from
Australian income tax may be available to such Foreign Shareholders under the Australia-U.S. DTA.
The comments above in “Tax on Sales or Other Dispositions of Shares—Capital Gains Tax” regarding a purchaser
being required to withhold 12.5% tax on the acquisition of TAP (increasing to 15% from 1 January 2025) equally applies
where the disposal of the Australian real property asset by a foreign resident is likely to generate gains on revenue account,
rather than a capital gain.
Australian Death Duty
Australia does not have estate or death duties. As a general rule, no CGT liability is realized upon the inheritance
of a deceased person’s ordinary shares. The disposal of inherited ordinary shares by beneficiaries may, however, give rise
to a CGT liability if the gain falls within the scope of Australia’s jurisdiction to tax (as discussed above).
Stamp Duty
Generally, no Australian stamp duty is payable by Australian residents or non-Australian residents on the issue,
agreement to transfer, transfer, surrender of, or other dealing in, the ADSs or the ordinary shares in the Company, provided
that at the time of such dealing, all of the issued shares in the Company are quoted on the ASX and the dealing does not
result in a person or entity acquiring or commencing to hold or otherwise being beneficially entitled to (on an associate
inclusive basis) 90% or more of the total issued shares in the Company.
GST
The supply of ADSs and/or ordinary shares in the Company will not be subject to Australian GST. Similarly, any
distributions or dividends will not be subject to Australian GST.
10.F
Dividends and Paying Agents
Not applicable.
10.G
Statement by Experts
Not applicable.
10.H
Documents on Display
Any statement in this Form 20-F about any of our contracts or other documents is not necessarily complete. If the
contract or document is filed as an exhibit to the Form 20-F the contract or document is deemed to modify the description
contained in this Form 20-F. You must review the exhibits themselves for a complete description of the contract or
document.
In addition, the SEC maintains a website at http://www.sec.gov that contains reports and other information
regarding issuers that file electronically with the SEC. These SEC filings are also available to the public from commercial
document retrieval services.
We are required to file or furnish reports and other information with the SEC under the Securities Exchange Act
of 1934 and regulations under that act. As a foreign private issuer, we are exempt from the rules under the Exchange Act
prescribing the form and content of proxy statements and our officers, directors and principal shareholders are exempt from
the reporting and short swing profit recovery provisions contained in Section 16 of the Exchange Act.
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10.I
Subsidiary Information
For information about our subsidiaries, see “Item 18. Financial Statements – Note 12.”
10.J
Annual Report to Security Holders
Not applicable.
Item 11. Quantitative and Qualitative Disclosures about Market Risk
For information about our exposure to market risk and how we manage this risk, see “Item 18. Financial
Statements – Note 10.”
Item 12. Description of Securities Other than Equity Securities
12.A
Debt Securities
Not applicable.
12.B
Warrants and Rights
Not applicable.
12.C
Other Securities
Not applicable.
12.D
American Depositary Shares
Fees Payable by ADR Holders
Holders of our ADRs may have to pay our ADS depositary, JPMorgan Chase Bank N.A. (JPMorgan), fees or
charges up to the amounts described in the following table:
Persons depositing or withdrawing ordinary shares or
ADS holders must pay:
Description of service
$5.00 (or less) per 100 ADSs (or portion of 100 ADSs)
• Issuance of ADSs, including issuances pursuant to a
deposits of shares, share or rights distributions, stock
dividend, stock split, merger or any other transactions
affecting the issuance of ADSs
• Cancellation of ADSs for the purpose of withdrawal of
deposited securities
$0.05 (or less) per ADS
• Cash distribution to ADS holders
$0.005 per ADS per calendar year
• Administrative services performed by the depositary
Fees Payable by the Depositary to the Issuer
From time to time, the depositary may make payments to us to reimburse and/or share revenue from the fees
collected from ADS holders, or waive fees and expenses for services provided, generally relating to costs and expenses
arising out of establishment and maintenance of the ADS program. In performing its duties under the deposit agreement,
the depositary may use brokers, dealers or other service providers that are affiliates of the depositary and that may earn or
share fees or commissions.
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PART II
Item 13. Defaults, Dividend Arrearages and Delinquencies
Not applicable.
Item 14. Material Modifications to the Rights of Security Holders and Use of Proceeds
Not applicable.
Item 15. Controls and Procedures
Evaluation of Disclosure Controls and Procedures
Our management, with the participation of our Chief Executive Officer and our interim Chief Financial Officer,
evaluated the effectiveness of our disclosure controls and procedures as of June 30, 2024. “Disclosure controls and
procedures,” as defined in Rules 13a-15(e) under the Exchange Act, are designed to ensure that information required to be
disclosed by a company in the reports that it files or submits under the Exchange Act is (i) recorded, processed,
summarized and reported within the time periods specified in the Securities and Exchange Commission’s rules and forms
and (ii) accumulated and communicated to the company’s management, including its principal executive officer and
principal financial officer, as appropriate to allow timely decisions regarding required disclosure.
Based on the evaluation of our disclosure controls and procedures, our Chief Executive Officer and interim Chief
Financial Officer concluded that our disclosure controls and procedures were effective as of June 30, 2024.
Management’s Report on Internal Control over Financial Reporting
Our management is responsible for establishing and maintaining adequate internal control over financial reporting,
as defined in Rule 13a-15(f) and 15d-15(f) under the Exchange Act. Our management conducted an assessment of the
effectiveness of our internal control over financial reporting as of June 30, 2024 based on the criteria set forth in Internal
Control-Integrated Framework (2013) issued by the Committee of Sponsoring Organizations of the Treadway
Commission. Based on that assessment, our management has concluded that its internal control over financial
reporting was effective as of June 30, 2024.
Changes in Internal Control over Financial Reporting
There were no changes to our internal control over financial reporting that occurred during the period covered by
this Form 20-F that have materially affected, or are reasonably likely to materially affect, our internal control over financial
reporting.
Limitations on Internal Control
Because of its inherent limitations, internal control over financial reporting may not prevent or
detect misstatements. Also, projections of any evaluation of effectiveness to future periods are subject to the risk that
controls may become inadequate because of changes in conditions, or that the degree of compliance with the policies or
procedures may deteriorate.
Item 16. [Reserved]
Item 16A.
Audit Committee Financial Expert
The Board of Directors of Mesoblast Ltd has determined that the following directors each possess specific
accounting and financial management expertise and that each is an Audit Committee Financial Expert as defined by the
SEC.
•
Philip Facchina (Audit and Risk Committee Chair, from May 1, 2024);
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•
Jane Bell (Audit and Risk Committee Chair, from September 20, 2023 to April 30, 2024) and;
•
Michael Spooner (Audit and Risk Committee Chair until September 20, 2023, resigned from the Board
effective September 26, 2023)
The Board of Directors has also determined that Joseph Swedish, member of the Audit and Risk Committee, has
sufficient experience and ability in finance and compliance matters to enable them to adequately discharge their
responsibilities. All members of the Audit and Risk Committee are “independent” according to the listing standards of the
Nasdaq Global Select Market.
Item 16B.
Code of Ethics
Our Code of Business Conduct and Ethics covers conflicts of interest, confidentiality, fair dealing, protection of
assets, compliance with laws and regulations, whistle blowing, security trading and commitments to stakeholders. In
summary, the Code requires that at all times all Company personnel act with the utmost integrity, objectivity and in
compliance with the letter and the spirit of the law and Company policies. This document is accessible on our internet
website at: http://www.mesoblast.com/company/corporate-governance/code-of-conduct-and-values.
Item 16C.
Principal Accountant Fees and Services
Pre-Approval of Audit and Non-Audit Services
The Audit and Risk Committee’s pre-approval is required for all services provided by PwC. These services may
include audit services, audit-related services, tax services and permissible non-audit services, and are subject to a specific
budget. The Audit and Risk Committee uses a combination of two approaches – general pre-approval and specific pre-
approval – in considering whether particular services or categories of services are consistent with the SEC’s rules on
auditor independence. Under general pre-approval proposed services may be pre-approved without consideration of
specific case-by-case services.
Audit and Non-Audit Services Fees
See “Item 18. Financial Statements – Note 18”. For the purpose of SEC classification, there were no audit-related,
tax or other fees that were paid or payable to PwC that were not pre-approved by the Audit and Risk Committee during the
years ended June 30, 2024 and 2023.
Item 16D.
Exemptions from the Listing Standards for Audit Committees
Not applicable.
Item 16E.
Purchases of Equity Securities by the Issuer and Affiliated Purchasers
Not applicable.
Item 16F.
Change in Registrant’s Certifying Accountant
Not applicable.
Item 16G.
Corporate Governance
Under Nasdaq Stock Market Rule 5615(a)(3), foreign private issuers, such as our company, are permitted to follow
certain home country corporate governance practices instead of certain provisions of the Nasdaq Stock Market Rules. For
example, we may follow home country practice with regard to certain corporate governance requirements, such as the
composition of the board of directors and quorum requirements applicable to shareholders’ meetings. In addition, we may
follow home country practice instead of the Nasdaq Stock Market Rules requirement to hold executive sessions and to
obtain shareholder approval prior to the issuance of securities in connection with certain acquisitions or private placements
of securities. Further, we may follow home country practice instead of the Nasdaq Stock Market Rules requirement to
obtain shareholder approval prior to the establishment or amendment of certain share option, purchase or other
compensation plans. A foreign private issuer that elects to follow a home country practice instead of any Nasdaq rule must
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156
submit to Nasdaq, in advance, a written statement from an independent counsel in such issuer’s home country certifying
that the issuer’s practices are not prohibited by the home country’s laws. We submitted such a written statement to Nasdaq.
Other than as set forth below, we currently intend to comply with the corporate governance listing standards in the
Nasdaq Stock Market Rules to the extent possible under Australian law. However, we may choose to change such practices
to follow home country practice in the future.
The Nasdaq Stock Market Rules require that a listed company specify that the quorum for any meeting of the
holders of share capital be at least 33 1/3% of the outstanding shares of the company’s common voting stock. We follow
our home country practice, rather than complying with this rule. Consistent with Australian law, our constitution does not
require a quorum of at least 33 1/3% of the issued voting shares of Mesoblast for any general meeting of its shareholders.
Our constitution provides that a quorum for a general meeting of our shareholders constitutes two shareholders present in
person, by proxy, by attorney, or, where the shareholders is a body corporate, by representative. This provision and our
practice of holding meetings with this quorum are not prohibited by the ASX Listing Rules or any other Australian law.
In addition, we may follow home country practice instead of Nasdaq Rule 5635(d), which requires a company to
obtain shareholder approval for an issuance of securities (other than a public offering) that equals of 20% or more of the
outstanding voting power in the company before such issuance. This Nasdaq rule is inconsistent with an ASX Listing Rule
that provides a company cannot issue a number of securities over any rolling 12-month period exceeding 15% of the
outstanding capital of the company without approval of shareholders but subject to certain exceptions such as pro-rata
offers of securities to all shareholders.
Item 16H.
Mine Safety Disclosure
Not applicable.
Item 16I.
Disclosure Regarding Foreign Jurisdiction that Prevent Inspections
Not applicable.
Item 16J.
Insider Trading Policies
We have a Share Trading Policy (“Policy”) which sets out the policy and procedures governing the purchase, sale
and other dispositions of the Company’s securities and applies to directors, officers, employees, contractors and consultants
of the Company and its subsidiaries ("Mesoblast Personnel").
The Policy aims to (i) restrict Mesoblast Personnel in possession of "inside information" from trading in our
securities and (ii) ensure compliance with all applicable securities laws, rules and regulations, and listing standards.
We have filed the Policy as an exhibit to this Annual Report on Form 20-F.
Item 16K.
Cybersecurity
The Company’s cybersecurity strategy is designed to provide a comprehensive approach to securing cybersecurity
risks across our technology stack, governance framework, and human elements for our operations globally. Cybersecurity
risk management is a critical component of our broader risk management strategy. Our cybersecurity program is built on
industry best practices and is designed to proactively identify, assess, and mitigate cybersecurity risks, including threats
associated with the use of all third-party service providers. Our cybersecurity risk assessment framework categorizes risks
based on their potential impact and severity, and the Company implements targeted risk treatment plans to ensure robust
protection and resilience.
The interim Chief Financial Officer and Head of Regulatory Affairs & Quality Management are the members of our
executive management team who oversee the prevention, detection, mitigation, and remediation of cybersecurity incidents.
Both these executives have extensive experience in risk management and compliance generally, and have been overseeing
cybersecurity and IT management at the Company for over three years. They are supported by the Company’s IT systems
administrator and an external managed IT and cybersecurity service provider. The service provider has been engaged by
the Company for over ten years, to provide strategic IT advice and manage the Company's IT systems and infrastructure.
The service provider, who has over 20 years of experience in securing IT in health and life sciences organizations, manages
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157
cybersecurity risks through a number of measures including the development and implementation of cybersecurity policies
and procedures, training and penetration testing and systems monitoring. Our executive management team members
regularly collaborate and receive reports from our managed IT and cybersecurity service provider, enabling ongoing
assessment and monitoring of the Company’s cyber risk profile and initiatives.
Our Board of Directors entrusts its Audit & Risk Committee with overseeing Mesoblast’s cybersecurity risk
management, including ensuring that management has established processes to evaluate and manage cybersecurity risks.
Our executive management team members together with our managed IT and cybersecurity service provider update the
Audit and Risk Committee on the Company’s cybersecurity initiatives, significant risks and mitigation work being
undertaken.
In the fiscal year 2024, we did not identify any cybersecurity threats that have materially impacted or are likely to
materially impact our business strategy, operational results, or financial condition. However, despite our proactive
measures, we cannot entirely eliminate cybersecurity risks or guarantee that no undetected incidents have occurred.
PART III
Item 17. Financial Statements
See “Item 18. Financial Statements”.
Item 18. Financial Statements
The following financial statements are filed as part of this Annual Report on Form 20-F.
Australian Disclosure Requirements
All press releases, financial reports and other information are available on our website: www.mesoblast.com.
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158
Index to Financial Statements
Report Of Independent Registered Public Accounting Firm (PricewaterhouseCoopers, Melbourne, Australia,
Auditor Firm ID: 1379)
160
Consolidated Income Statement
164
Consolidated Statement of Comprehensive Income
165
Consolidated Statement of Changes in Equity
166
Consolidated Balance Sheet
167
Consolidated Statement of Cash Flows
168
Notes to Consolidated Financial Statements
169
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PricewaterhouseCoopers, ABN 52 780 433 757
2 Riverside Quay, SOUTHBANK VIC 3006, GPO Box 1331, MELBOURNE VIC 3001
T: 61 3 8603 1000, F: 61 3 8603 1999, www.pwc.com.au
Liability limited by a scheme approved under Professional Standards Legislation.
Auditor’s Independence Declaration
As lead auditor for the audit of Mesoblast Limited for the year ended 30 June 2024, I declare that to
the best of my knowledge and belief, there have been:
(a)
no contraventions of the auditor independence requirements of the Corporations Act 2001 in
relation to the audit; and
(b)
no contraventions of any applicable code of professional conduct in relation to the audit.
This declaration is in respect of Mesoblast Limited and the entities it controlled during the period.
Jon Roberts
Melbourne
Partner
PricewaterhouseCoopers
29 August 2024
161
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Mesoblast Limited
Consolidated Income Statement
Year Ended June 30,
(in U.S. dollars, in thousands, except per share amount)
Note
2024
2023
2022
Revenue
3
5,902
7,501
10,211
Research & development
(25,353)
(27,189)
(32,815)
Manufacturing commercialization
(15,717)
(27,733)
(30,757)
Management and administration
(23,626)
(25,374)
(27,210)
Fair value remeasurement of contingent consideration
3
(9,693)
8,771
913
Fair value remeasurement of warrant liability
3
779
(2,205)
5,896
Other operating income and expenses
3
2,570
4,250
(536)
Finance costs
3
(23,009)
(20,122)
(17,288)
Loss before income tax
3
(88,147)
(82,101)
(91,586)
Income tax benefit/(expense)
4
191
212
239
Loss attributable to the owners of Mesoblast Limited
(87,956)
(81,889)
(91,347)
Losses per share from continuing operations attributable to the ordinary
equity holders of the Group:
Cents
Cents
Cents
Basic - losses per share
19
(8.91)
(10.53)
(13.38)
Diluted - losses per share
19
(8.91)
(10.53)
(13.38)
The above consolidated income statement should be read in conjunction with the accompanying Notes.
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Mesoblast Limited
Consolidated Statement of Comprehensive Income
Year Ended June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
2022
Loss for the period
(87,956)
(81,889)
(91,347)
Other comprehensive (loss)/income
Items that may be reclassified to profit and loss
Exchange differences on translation of foreign operations
7(b)
51
(573)
91
Items that will not be reclassified to profit and loss
Financial assets at fair value through other comprehensive
income
7(b)
(743)
(1)
(322)
Other comprehensive (loss)/income for the period, net of tax
(692)
(574)
(231)
Total comprehensive losses attributable to the owners of
Mesoblast Limited
(88,648)
(82,463)
(91,578)
The above consolidated statement of comprehensive income should be read in conjunction with the accompanying Notes.
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165
Mesoblast Limited
Consolidated Statement of Changes in Equity
(in U.S. dollars, in thousands)
Note
Issued
Capital
Share
Option
Reserve
Investment
Revaluation
Reserve
Foreign
Currency
Translation
Reserve
Warrant
Reserve
Retained
Earnings/
(accumulated
losses)
Total
Balance as of July 1, 2021
1,163,153 92,855
(220)
(39,791) 12,969
(647,569) 581,397
Loss for the period
—
—
—
—
—
(91,347) (91,347)
Other comprehensive income/(loss)
—
—
(322)
91
—
—
(231)
Total comprehensive income/(loss) for
the period
—
—
(322)
91
—
(91,347) (91,578)
Transactions with owners in their
capacity as owners:
Contributions of equity net of transaction
costs
1,928
—
—
—
—
—
1,928
1,928
—
—
—
—
—
1,928
Tax credited / (debited) to equity
—
(239)
—
—
—
—
(239)
Transfer of exercised options
228
(228)
—
—
—
—
—
Fair value of share-based payments
17
—
5,536
—
—
—
—
5,536
228
5,069
—
—
—
—
5,297
Balance as of June 30, 2022
7(a)
1,165,309 97,924
(542)
(39,700) 12,969
(738,916) 497,044
Balance as of July 1, 2022
1,165,309 97,924
(542)
(39,700) 12,969
(738,916) 497,044
Loss for the period
—
—
—
—
—
(81,889) (81,889)
Other comprehensive (loss)/income
—
—
(1)
(573)
—
—
(574)
Total comprehensive (loss)/income for
the period
—
—
(1)
(573)
—
(81,889) (82,463)
Transactions with owners in their
capacity as owners:
Contributions of equity net of transaction
costs
83,814
—
—
—
—
— 83,814
83,814
—
—
—
—
— 83,814
Tax credited / (debited) to equity
—
(212)
—
—
—
—
(212)
Fair value of share-based payments
17
—
3,655
—
—
—
—
3,655
—
3,443
—
—
—
—
3,443
Balance as of June 30, 2023
7(a)
1,249,123 101,367
(543)
(40,273) 12,969
(820,805) 501,838
Balance as of July 1, 2023
1,249,123 101,367
(543)
(40,273) 12,969
(820,805) 501,838
Loss for the period
—
—
—
—
—
(87,956) (87,956)
Other comprehensive (loss)/income
—
—
(743)
51
—
—
(692)
Total comprehensive (loss)/income for
the period
—
—
(743)
51
—
(87,956) (88,648)
Transactions with owners in their
capacity as owners:
Contributions of equity net of transaction
costs
60,486
—
—
—
—
— 60,486
Contributions of equity for unissued
ordinary shares, net of transaction costs
1,000
—
—
—
—
—
1,000
61,486
—
—
—
—
— 61,486
Tax credited / (debited) to equity
—
(191)
—
—
—
—
(191)
Transfer of exercised options
204
(204)
—
—
—
—
—
Fair value of share-based payments
17
—
5,870
—
—
—
—
5,870
204
5,475
—
—
—
—
5,679
Balance as of June 30, 2024
7(a)
1,310,813 106,842
(1,286)
(40,222)
12,969
(908,761) 480,355
The above consolidated statement of changes in equity should be read in conjunction with the accompanying Notes.
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166
Mesoblast Limited
Consolidated Balance Sheet
As of June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
Assets
Current Assets
Cash & cash equivalents
5(a)
62,960
71,318
Trade & other receivables
5(b)
20,952
6,998
Prepayments
5(b)
2,551
3,342
Total Current Assets
86,463
81,658
Non-Current Assets
Property, plant and equipment
6(a)
1,106
1,357
Right-of-use assets
6(b)
2,732
5,134
Financial assets at fair value through other comprehensive income
5(c)
1,014
1,757
Other non-current assets
5(d)
2,102
2,326
Intangible assets
6(c)
575,736
577,183
Total Non-Current Assets
582,690
587,757
Total Assets
669,153
669,415
Liabilities
Current Liabilities
Trade and other payables
5(e)
7,070
20,145
Provisions
6(d)
45,038
6,399
Borrowings
5(f)
13,862
5,952
Lease liabilities
6(b)
2,626
4,060
Warrant liability
5(f)
4,647
5,426
Total Current Liabilities
73,243
41,982
Non-Current Liabilities
Provisions
6(d)
10,620
16,612
Borrowings
5(f)
100,483
102,811
Lease liabilities
6(b)
1,952
3,672
Deferred consideration
6(f)
2,500
2,500
Total Non-Current Liabilities
115,555
125,595
Total Liabilities
188,798
167,577
Net Assets
480,355
501,838
Equity
Issued Capital
7(a)
1,310,813
1,249,123
Reserves
7(b)
78,303
73,520
Accumulated losses
(908,761)
(820,805)
Total Equity
480,355
501,838
The above consolidated balance sheet should be read in conjunction with the accompanying Notes.
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167
Mesoblast Limited
Consolidated Statement of Cash Flows
Year Ended June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
2022
Cash flows from operating activities
Commercialization revenue received
6,776
7,480
9,980
Government grants and tax incentives and credits received
3,819
1,118
24
Payments to suppliers and employees (inclusive of goods and
services tax)
(60,835)
(72,683)
(75,769)
Interest received
1,778
796
7
Income taxes received /(paid)
4
20
(24)
Net cash (outflows) in operating activities
8(b)
(48,458)
(63,269)
(65,782)
Cash flows from investing activities
Investment in fixed assets
(271)
(264)
(157)
Receipts from investment in sublease
234
120
—
Payments for licenses
(60)
(50)
(75)
Net cash (outflows) in investing activities
(97)
(194)
(232)
Cash flows from financing activities
Proceeds from borrowings
—
—
51,919
Repayment of borrowings
(10,000)
—
(55,458)
Payment of transaction costs from borrowings
(1,559)
(574)
(5,527)
Interest and other costs of finance paid
(5,717)
(6,014)
(6,084)
Proceeds from issue of shares
65,406
88,635
209
Proceeds from issue of warrants
—
—
8,081
Payments for share issue costs
(4,356)
(4,889)
(222)
Payments for lease liabilities
(3,522)
(2,656)
(2,788)
Net cash inflows/(outflows) by financing activities
40,252
74,502
(9,870)
Net increase/(decrease) in cash and cash equivalents
(8,303)
11,039
(75,884)
Cash and cash equivalents at beginning of period
71,318
60,447
136,881
FX (loss)/gain on the translation of foreign bank accounts
(55)
(168)
(550)
Cash and cash equivalents at end of period
8(a)
62,960
71,318
60,447
The above consolidated statement of cash flows should be read in conjunction with the accompanying Notes.
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168
Mesoblast Limited
Notes to Consolidated Financial Statements
Mesoblast Limited (“the Company”) and its subsidiaries (“the Group”) are primarily engaged in the development
of regenerative medicine products. The Group’s primary proprietary regenerative medicine technology platform is based on
specialized cells known as mesenchymal lineage cells. The Company was formed in 2004 as an Australian company and
has been listed on the Australian Securities Exchange (the “ASX”) since 2004. In November 2015, the Company listed in
the United States of America (“U.S.”) on the Nasdaq Global Select Market (“Nasdaq”) and from this date has been dual-
listed in Australia and the U.S.
These financial statements and notes are presented in U.S. dollars (“$” or “USD” or “US$”), unless otherwise
noted, including certain amounts that are presented in Australian dollars (“AUD” or “A$”) and Singapore dollars (“SGD”
or “S$”).
1. Basis of preparation
The general purpose financial statements of Mesoblast Limited and its subsidiaries have been prepared in
accordance with International Financial Reporting Standards, as issued by the International Accounting Standards Board
and Australian equivalent International Financial Reporting Standards, as issued by the Australian Accounting Standards
Board. Mesoblast Limited is a for-profit entity for the purpose of preparing the financial statements.
The financial statements cover Mesoblast Limited and its subsidiaries. The financial statements were authorized
for issue by the board of directors on August 29, 2024. The directors have the power to amend and reissue the financial
statements.
(i)
Going concern
As of June 30, 2024, the Group held total cash reserves of $63.0 million. During the year ended June 30, 2024, the
Group executed on reprioritization of projects and operational streamlining activities and as a result has reduced net cash
usage for operating activities, which was $48.5 million for the year ended June 30, 2024, a reduction of 23% compared to
the prior period.
As the Group prepares for a potential first product approval by the United States Food and Drug Administration
("FDA"), and in line with its commercial launch plans, additional inflows from capital markets, strategic partnerships,
product specific financing or royalty monetization will be required to meet the Group's projected expenditure consistent
with the Group's business strategy over at least the next 12 months. As a result of these matters, there is material
uncertainty related to events or conditions that may cast significant doubt (or raise substantial doubt as contemplated by
Public Company Accounting Oversight Board (“PCAOB”) standards) on the Group’s ability to continue as a going concern
and, therefore, that the Group may be unable to realize its assets and discharge its liabilities in the normal course of
business. The consolidated financial statements do not include any adjustments that might result from the outcome of this
uncertainty.
(ii)
Historical cost convention
These financial statements have been prepared under the historical cost convention, as modified by the revaluation
of financial assets at fair value through other comprehensive income and financial assets and liabilities (including
derivative instruments) at fair value through profit or loss and investment property.
(iii)
New and amended standards adopted by the Group
There were no new or amended standards adopted by the Group in the year ended June 30, 2024 that materially
impacted the Group. These financial statements follow the same accounting policies as compared to the June 30, 2023
consolidated financial statements and related notes as filed with the Australian Securities Exchange and the Securities and
Exchange Commission.
(iv)
New accounting standards and interpretations not yet adopted by the Group
In April 2024, IFRS 18, “Presentation and Disclosure in Financial Statements” was issued to achieve
comparability of the financial performance of similar entities. The standard, which replaces IAS 1 “Presentation of
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169
Financial Statements”, impacts the presentation of primary financial statements and notes, including the statement of
earnings where companies will be required to present separate categories of income and expense for operating, investing,
and financing activities with prescribed subtotals for each new category. The standard will also require management-
defined performance measures to be explained and included in a separate note within the consolidated financial statements.
The standard is effective for annual reporting periods beginning on or after January 1, 2027, including interim financial
statements, and requires retrospective application. The Group is currently assessing the impact of the new standard.
There were no other new accounting standards and interpretations not yet adopted by the Group for the June 30,
2024 reporting period that are expected to materially impact the Group.
(v)
Use of estimates
The preparation of these consolidated financial statements requires the Group to make estimates and judgments
that affect the reported amounts of assets, liabilities, income and expenses and related disclosures. On an ongoing basis, the
Group evaluates its significant accounting policies and estimates. Estimates are based on historical experience and on
various market-specific and other relevant assumptions that the Group believes to be reasonable under the circumstances,
the results of which form the basis for making judgments about the carrying values of assets and liabilities.
(vi)
Impact of after effects of COVID-19, geopolitical or economic instability and climate events
Estimates are assessed each period and updated to reflect current information, such as the economic considerations
related to the after effects of the COVID-19 pandemic, geopolitical and/or economic instability or the impact of climate
events could have on the Group’s significant accounting estimates. The Group does not expect these areas to have a
material impact on the Group's significant accounting estimates.
2. Significant changes in the current reporting period
(i)
Significant events
The financial position and performance of the Group was affected by the following events during the year ended
June 30, 2024:
•
In August 2023, the FDA provided a complete response letter ("CRL") to the Group's Biologics License
Application ("BLA") resubmission for remestemcel-L for the treatment of pediatric steroid-refractory acute graft
versus host disease ("SR-aGVHD") and required more data to support marketing approval, including potency
assay or clinical data. In March 2024, the FDA informed the Group that, following additional consideration, the
available clinical data from the Phase 3 study MSB-GVHD001 appears sufficient to support submission of the
proposed BLA for remestemcel-L for the treatment of pediatric patients with SR-aGVHD. In July 2024, as
discussed in Note 15, the Group resubmitted its BLA for approval of remestemcel-L for the treatment of pediatric
patients with SR-aGVHD, addressing remaining items in the August 2023 CRL. In July 2024, the FDA accepted
the Group's BLA resubmission and set a Prescription Drug User Fee Act ("PDUFA") goal date of January 7, 2025.
Assumptions associated with SR-aGVHD are included within the impairment assessment of Osiris mesenchymal
stem cell ("MSC") products within in-process research and development, contingent consideration, pre-launch
inventory and the NovaQuest borrowings on the consolidated balance sheet and forecast net operating cash usage.
The outcome from the FDA decision on the Group's BLA resubmission could lead to a change in the assumptions
used within these areas.
•
In March 2024, the Group completed a pro-rata accelerated non-renounceable entitlement offer together with an
institutional placement of new fully paid ordinary shares in Mesoblast Limited to existing eligible shareholders
that was launched in December 2023, raising A$97.0 million at an issue price of A$0.30 per share. Proceeds of
$39.7 million (A$60.3 million) and $24.7 million (A$36.7 million) were received and recognized in cash and cash
equivalents in December 2023 and March 2024, respectively.
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170
3. Loss before income tax
Revenue
Commercialization revenue
5,902
7,501
9,039
Milestone revenue
—
—
1,172
Total Revenue
5,902
7,501
10,211
Clinical trial and research & development
(3,963)
(8,771)
(10,483)
Manufacturing production & development
(13,252)
(25,468)
(28,884)
Employee benefits
Salaries and employee benefits
(20,415)
(17,197)
(18,997)
Defined contribution superannuation expenses
(369)
(384)
(402)
Equity settled share-based payment transactions(1)
(5,870)
(3,655)
(5,536)
Total Employee benefits
(26,654)
(21,236)
(24,935)
Depreciation and amortization of non-current assets
Plant and equipment depreciation
(410)
(953)
(1,144)
Right of use asset depreciation
(2,771)
(1,661)
(1,717)
Intellectual property amortization
(1,485)
(1,493)
(1,519)
Total Depreciation and amortization of non-current assets
(4,666)
(4,107)
(4,380)
Other Management & administration expenses
Overheads & administration
(8,584)
(10,104)
(10,157)
Consultancy
(2,458)
(3,922)
(3,751)
Legal, patent and other professional fees
(2,342)
(3,695)
(5,571)
Intellectual property expenses (excluding the amount amortized
above)
(2,777)
(2,993)
(2,621)
Total Other Management & administration expenses
(16,161)
(20,714)
(22,100)
Fair value remeasurement of contingent consideration
Remeasurement of contingent consideration
5(g)(iii)
(9,693)
8,771
913
Total Fair value remeasurement of contingent consideration
(9,693)
8,771
913
Fair value remeasurement of warrant liability
Remeasurement of warrant liability
5(g)(vi)
779
(2,205)
5,896
Total Fair value remeasurement of warrant liability
779
(2,205)
5,896
Other operating income and expenses
Research and development tax incentive income(2)
859
3,506
—
Interest income
1,824
831
3
Foreign exchange (losses)/gains
(76)
(163)
(536)
Derecognition of right-of-use asset
—
76
—
Foreign withholding tax paid
(37)
—
(3)
Total Other operating income and expenses
2,570
4,250
(536)
Year Ended June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
2022
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171
Finance (costs)/gains
Remeasurement of borrowing arrangements
(2,351)
(678)
(382)
Interest expense
(20,658)
(19,444)
(16,906)
Total Finance costs
(23,009)
(20,122)
(17,288)
Total loss before income tax
(88,147)
(82,101)
(91,586)
Year Ended June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
2022
(1)
Share-based payment transactions
For the years ended June 30, 2024, 2023 and 2022, share-based payment transactions have been reflected in the
Consolidated Statement of Comprehensive Income functional expense categories as follows:
Year Ended June 30,
(in U.S. dollars)
2024
2023
2022
Research and development
2,797,830
1,669,514
3,547,182
Manufacturing and commercialization
176,907
(1,136)
378,096
Management and administration
2,895,431
1,986,968
1,610,567
Equity settled share-based payment transactions
5,870,168
3,655,346
5,535,845
(2)
Research and development tax incentive
The Group's research and development activities are eligible under the Australian government's Innovation
Australia Research and Development Tax Incentive program for research and development activities conducted in relation
to qualifying research that meets the regulatory criteria. Management has assessed these activities and expenditures to
determine which costs are likely to be eligible under the incentive scheme. The Group assesses, on an annual basis, the
quantum of previous research and development tax claims and on-going eligibility to claim this tax incentive in Australia.
The Group recorded $0.9 million, $3.5 million and $nil in research and development tax incentive income for the
years ended June 30, 2024, 2023 and 2022, respectively. Within the $3.5 million recognized in the year ended June 30,
2023, $1.2 million pertained to the year ended June 30, 2023, $1.1 million pertained to the year ended June 30, 2022 and
$1.2 million pertained to the year ended June 30, 2021. Management concluded it's assessment of qualifying activities
during the year ended June 30, 2023 and recognized the relevant income for the years ended June 30, 2023, 2022 and 2021.
No income was recognized in the years ended June 30, 2022 and 2021 as management were yet to confirm if the Group's
research and development activities were eligible under the incentive scheme.
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172
4. Income tax benefit/(expense)
Year Ended June 30,
(in U.S. dollars, in thousands)
2024
2023
2022
(a)
Reconciliation of income tax to prima facie tax payable
Loss from continuing operations before income tax
(88,147)
(82,101)
(91,586)
Tax benefit at the Australian tax rate of 30% (2023: 30%, 2022: 30%)
(26,444)
(24,630)
(27,476)
Tax effect of amounts which are not deductible/(exempt) in
calculating taxable income:
Share-based payments expense
1,752
1,089
1,588
Research and development tax concessions
324
(730)
(869)
Foreign exchange translation (losses)/gains
(103)
501
159
Contingent consideration
2,908
(2,631)
(274)
Other sundry items
(231)
695
(2,036)
Subtotal
(21,794)
(25,706)
(28,908)
Adjustments for current tax of prior periods
198
274
(923)
Differences in overseas tax rates
6,051
8,537
8,407
Tax benefit not recognized
15,354
16,683
21,185
Change in tax rate on Deferred tax assets(1)
—
—
(8,326)
Change in tax rate on Deferred tax liability(1)
—
—
8,326
Income tax benefit attributable to loss before income tax
(191)
(212)
(239)
(1) On June 30, 2022, there was a change in the expected tax rate applicable on future taxable profits in Singapore. The
Group was expecting to benefit from concessionary tax rates (tax holiday) in Singapore under the tax incentives
granted to the Group by the Singapore Economic Development Board, however at June 30, 2022 the Group had not
met the conditions under the agreement to access the concessionary tax rates and therefore have recognized a change
in the expected tax rate in Singapore to reflect the statutory tax rate of 17%. The Group is in current discussions with
the Singapore Economic Development Board to amend the conditions of the incentive agreement and access these
concessionary tax rates in the future.
Year Ended June 30,
(in U.S. dollars, in thousands)
2024
2023
2022
(b)
Income tax (benefit)/expense
Current tax
Current tax
—
—
—
Total current tax (benefit)/expense
—
—
—
Deferred tax
(Increase)/decrease in deferred tax assets
56
38
(8,317)
(Decrease)/increase in deferred tax liabilities
(247)
(250)
8,078
Total deferred tax (benefit)/expense
(191)
(212)
(239)
Income tax (benefit)/expense
(191)
(212)
(239)
Deferred tax assets have been brought to account only to the extent that it is foreseeable that they are recoverable
against future tax liabilities.
Deferred tax assets are recognized for unused tax losses to the extent that it is probable that future taxable profit
will be available against which the unused tax losses can be utilized. Deferred tax assets are offset against taxable
temporary differences (deferred tax liabilities) when the deferred tax balances relate to the same tax jurisdiction in
accordance with our accounting policy.
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173
Deferred taxes are measured at the rate in which they are expected to settle within the respective jurisdictions,
which can change based on factors such as new legislation or timing of utilization and reversal of associated assets and
liabilities.
Year Ended June 30,
(in U.S. dollars, in thousands)
2024
2023
2022
(c)
Amounts that would be recognized directly in equity if brought to
account
Aggregate current and deferred tax arising in the reporting period and
not recognized in net loss or other comprehensive income but which
would have been directly applied to equity had it been brought to
account:
Current tax recorded in equity (if brought to account)
(1,329)
(1,716)
(142)
Deferred tax recorded in equity (if brought to account)
1,029
839
715
(300)
(877)
573
Year Ended June 30,
(in U.S. dollars, in thousands)
2024
2023
2022
(d)
Amounts recognized directly in equity
Aggregate current and deferred tax arising in the reporting period and
not recognized in net loss or other comprehensive income but
debited/credited to equity
Current tax recorded in equity
—
—
—
Deferred tax recorded in equity
191
212
239
191
212
239
Year Ended June 30,
(in U.S. dollars, in thousands)
2024
2023
2022
(e)
Deferred tax assets not brought to account
Unused tax losses
Potential tax benefit at local tax rates
140,129
125,728
111,283
Other temporary differences
Potential tax benefit at local tax rates
14,204
12,318
11,046
Other tax credits
Potential tax benefit at local tax rates
3,220
3,220
3,220
157,553
141,266
125,549
The Group has not brought to account $620.6 million (2023: $553.0 million, 2022: $477.8 million) of gross tax
losses, which includes the benefit arising from tax losses in overseas countries. As of June 30, 2024 $620.6 million of tax
losses not brought to account have an indefinite life. Gross tax losses of $44.5 million recognized as deferred tax asset
expire within a range of 9 to 14 years. The benefits of unused tax losses will only be brought to account when it is probable
that they will be realized.
This benefit of tax losses will only be obtained if:
•
the Group derives future assessable income of a nature and an amount sufficient to enable the benefit
from the deductions for the losses to be realized;
•
the Group continues to comply with the conditions for deductibility imposed by tax legislation; and
•
no changes in tax legislation adversely affect the Group in realizing the benefit from the deductions for
the losses.
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174
5. Financial assets and liabilities
This note provides information about the Group's financial instruments, including:
•
an overview of all financial instruments held by the Group;
•
specific information about each type of financial instrument;
•
accounting policies; and
•
information used to determine the fair value of the instruments, including judgments and estimation
uncertainty involved.
The Group holds the following financial instruments:
Financial assets
(in U.S. dollars, in thousands)
Notes
Assets at
FVOCI(1)
Assets at
FVTPL(2)
Assets at
amortized
cost
Total
As of June 30, 2024
Cash & cash equivalents
5(a)
—
—
62,960
62,960
Trade & other receivables
5(b)
—
—
20,952
20,952
Financial assets at fair value through other
comprehensive income
5(c)
1,014
—
—
1,014
Other non-current assets
5(d)
—
—
2,102
2,102
1,014
—
86,014
87,028
As of June 30, 2023
Cash & cash equivalents
5(a)
—
—
71,318
71,318
Trade & other receivables
5(b)
—
—
6,998
6,998
Financial assets at fair value through other
comprehensive income
5(c)
1,757
—
—
1,757
Other non-current assets
5(d)
—
—
2,326
2,326
1,757
—
80,642
82,399
(1)
Fair value through other comprehensive income
(2)
Fair value through profit or loss
Financial liabilities
(in U.S. dollars, in thousands)
Notes
Liabilities at
FVOCI(1)
Liabilities at
FVTPL(2)
Liabilities at
amortized
cost
Total
As of June 30, 2024
Trade and other payables
5(e)
—
—
7,070
7,070
Borrowings
5(f)
—
—
114,345
114,345
Contingent consideration
5(g)(iii)
—
26,892
—
26,892
Warrant liability
5(g)(vi)
—
4,647
—
4,647
—
31,539
121,415
152,954
As of June 30, 2023
Trade and other payables
5(e)
—
—
20,145
20,145
Borrowings
5(f)
—
—
108,763
108,763
Contingent consideration
5(g)(iii)
—
17,199
—
17,199
Warrant liability
5(g)(vi)
—
5,426
—
5,426
—
22,625
128,908
151,533
(1)
Fair value through other comprehensive income
(2)
Fair value through profit or loss
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175
The Group’s exposure to various risks associated with the financial instruments is discussed in Note 10. The
maximum exposure to credit risk at the end of the reporting period is the carrying amount of each class of financial assets
mentioned above.
a.
Cash and cash equivalents
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Cash at bank
62,563
70,920
Deposits at call(1)
397
398
62,960
71,318
(1) As of June 30, 2024 and June 30, 2023, interest-bearing deposits at call include amounts of $0.4 million and $0.4
million, respectively, held as security and restricted for use.
(i)
Classification as cash equivalents
Term deposits are presented as cash equivalents if they have a maturity of three months or less from the date of
acquisition.
b.
Trade and other receivables and prepayments
(i)
Trade and other receivables
As of June 30,
(in U.S. dollars, in thousands)
Note
2024
2023
Trade receivables
1,403
2,276
Tax incentives recoverable
854
2,363
Foreign withholding tax recoverable
471
471
U.S. Tax credits
—
1,473
Net investment in sublease
224
195
Interest receivables
23
18
Other recoverable taxes (Goods and services tax and value-added tax)
423
202
Insurance Asset
22
17,554
—
Trade and other receivables
20,952
6,998
(ii)
Prepayments
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Clinical trial research and development expenditure
391
950
Prepaid insurance and subscriptions
1,775
2,025
Other
385
367
Prepayments
2,551
3,342
(iii)
Classification as trade and other receivables
Trade receivables and other receivables represent the principal amounts due at balance date less, where applicable,
any provision for expected credit losses. The Group uses the simplified approach to measuring expected credit losses,
which uses a lifetime expected credit loss allowance. Debts which are known to be uncollectible are written off in the
consolidated income statement. All trade receivables and other receivables, with the exception of the net investment in
sublease, are recognized at the value of the amounts receivable, as they are due for settlement within 60 days and therefore
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176
do not require remeasurement. The net investment in sublease is recognized at the present value of minimum lease
payments receivable over the remaining life of the lease.
(iv)
Fair values of trade and other receivables
Due to the short-term nature of the current receivables, their carrying amount is assumed to be the same as their
fair value.
(v)
Impairment and risk exposure
Information about the impairment of trade and other receivables, their credit quality and the Group’s exposure to
credit risk, foreign currency risk and interest rate risk can be found in Note 10(a) and (b).
c.
Financial assets at fair value through other comprehensive income
Financial assets at fair value through other comprehensive income include the following classes of financial
assets:
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Unlisted securities:
Equity securities
1,014
1,757
1,014
1,757
(i)
Classification of financial assets at fair value through other comprehensive income
Financial assets at fair value through other comprehensive income comprises equity securities which are not held
for trading, and which the Group has irrevocably elected at initial recognition to recognize in this category. These are
strategic investments and the Group considers this classification to be more relevant.
The financial assets are presented as non-current assets unless they mature, or management intends to dispose of
them within 12 months of the end of the reporting period.
(ii)
Impairment indicators for financial assets at fair value through other comprehensive income
Impairment losses (and reversal of impairment losses) on equity investments measured at FVOCI are not reported
separately from other changes in fair value. See Note 23(m)(iv) for further details about the Group’s impairment policies
for financial assets.
(iii)
Amounts recognized in other comprehensive income
For the years ended June 30, 2024, 2023 and 2022, the Group recognized in statement of comprehensive income a
loss of $0.7 million, a $Nil gain/loss and a loss of $0.3 million respectively, for change in fair value of the financial assets
through other comprehensive income.
(iv)
Fair value, impairment and risk exposure
Information about the methods and assumptions used in determining fair value is provided in Note 5(g). None of
the financial assets through other comprehensive income are either past due or impaired.
All financial assets at fair value through other comprehensive income are denominated in US$.
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177
d.
Other non-current assets
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Bank guarantee
481
481
Net investment in sublease
190
414
Letter of credit
1,179
1,179
Security deposit
252
252
2,102
2,326
(i)
Classification of financial assets as other non-current assets
Bank guarantee
These funds are held in an account named Mesoblast Limited at National Australia Bank according to the terms of
a Bank Guarantee which is security for the sublease agreement for our occupancy of Level 38, 55 Collins Street,
Melbourne, Victoria, Australia. The Bank Guarantee is security for the full and faithful performance and observance by the
subtenant of the terms, covenants and conditions of the sublease. The Bank Guarantee continues in force until it is released
by the lessor.
Letter of credit
These funds held in an account named Mesoblast, Inc. at the Bank of America according to the terms of an
irrevocable standby letter of credit which is security for the sublease agreement for our occupancy of 505 Fifth Avenue,
New York, New York, United States of America. The letter of credit is security for the full and faithful performance and
observance by the subtenant of the terms, covenants and conditions of the sublease. The letter of credit is deemed to
automatically extend without amendment for a period of one year at each anniversary.
(ii)
Impairment and risk exposure
Information about the impairment of other non-current assets and their credit quality and the Group’s exposure to
credit risk can be found in Note 10(b).
e.
Trade and other payables
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Trade payables and other payables
7,070
20,145
Trade and other payables
7,070
20,145
The carrying amounts of trade and other payables are assumed to be the same as their fair values, due to their
short-term nature.
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178
f.
Borrowings
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Borrowings
Secured liabilities:
Borrowing arrangements
81,919
81,919
Less: transaction costs
(9,833)
(8,740)
Amortization of carrying amount, net of payments made
42,259
35,584
114,345
108,763
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Borrowings
Current
Borrowings - NovaQuest
1,869
336
Borrowings - Oaktree
11,993
5,616
13,862
5,952
Non-current
Borrowings - NovaQuest
64,562
55,739
Borrowings - Oaktree
35,921
47,072
100,483
102,811
114,345
108,763
(i)
Borrowing arrangements
Funds associated with Oaktree Capital Management, L.P. (“Oaktree”)
In November 2021, the Group entered into a five-year senior debt facility provided by funds associated with
Oaktree. The balance of funds drawn down is $50.0 million as of June 30, 2024. The facility has a three-year interest only
period, at a fixed rate of 9.75% per annum, after which the principal amortizes 5% per quarter beginning December 2024
and a final payment is due no later than November 2026. The facility also allows the Group to make quarterly payments of
interest at a rate of 8.0% per annum for the first two years, and the unpaid interest portion (1.75% per annum) has been
added to the outstanding loan balance and currently accrues further interest at a fixed rate of 9.75% per annum.
On November 19, 2021, Oaktree were granted warrants to purchase 1,769,669 American Depositary Shares
(“ADSs”) at US$7.26 per ADS, a 15% premium to the 30-day VWAP. The Group determined that an obligation to issue
the warrants arose from the time the debt facility was signed; consequently, a liability for the warrants was recognized in
November 2021. The warrants were legally issued on January 11, 2022 and may be exercised within 7 years of issuance.
On the issuance date of the Oaktree facility and the warrants, the warrants were initially measured at fair value and the
Oaktree borrowing liability measured as the difference between the initial draw down of funds from the Oaktree facility
and the fair value of the warrants. In December 2022, the Group amended the terms of the loan agreement with Oaktree
and in connection with the loan amendment, Oaktree was granted warrants to purchase 455,000 ADSs at $3.70 per ADS, a
15% premium to the 30-day VWAP. The Group determined that an obligation to issue the warrants arose from the time the
first amendment to the loan agreement was signed; consequently, a liability for the warrants was recognized in December
2022. The warrants were legally issued on March 8, 2023 and may be exercised within 7 years of issuance. Refer to Note
5(g)(vi) for more details on warrants issued.
On January 10, 2024, the ratio under Mesoblast's American Depository Receipt ("ADR") program was changed
from 5 ordinary shares representing 1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio).
As a result of this ratio change and as a result of initiating the pro-rata accelerated non-renounceable rights issue in
December 2023, the number and exercise price for the warrants was adjusted in accordance with the terms of these
warrants. The warrants issued in November 2021 changed from 1,769,669 ADSs at $7.26 per ADS to 884,838 ADSs at
$14.36 per ADS. The warrants issued in December 2022 changed from 455,000 ADSs at $3.70 per ADS to 227,502 ADSs
at $7.24 per ADS.
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179
In the years ended June 30, 2024, 2023 and 2022, respectively, the Group recognized losses of $2.3 million, $1.6
million and a minimal gain in the Consolidated Income Statement as remeasurement of borrowing arrangements within
finance costs in relation to the adjustment of the carrying amount of our financial liability to reflect the revised estimated
future cash flows from our facility. Within the $1.6 million loss recognized in the year ended June 30, 2023, $1.0 million
related to the remeasurement due to additional warrants being issued to Oaktree as a result of the first amendment to the
loan agreement and $0.6 million related to the adjustment of the carrying amount of our financial liability to reflect the
revised estimated future cash flows from our credit facility.
The Group has pledged substantially all of its assets as collateral under the loan facility with Oaktree.
NovaQuest Capital Management, L.L.C.
On June 29, 2018, the Group entered into an eight-year, $40.0 million loan and security agreement with
NovaQuest before drawing the first tranche of $30.0 million of the principal in July 2018. The loan term includes an
interest only period of approximately four years through until July 8, 2022.
All interest and principal payments (i.e. the amortization period) are deferred until the earlier of loan maturity or
from after the first commercial sale of remestemcel-L for the treatment in pediatric patients with SR-aGVHD in the United
States and other geographies excluding Asia ("remestemcel-L for pediatric SR-aGVHD"). Principal is repayable in equal
quarterly instalments over the amortization period of the loan and is subject to the payment cap described below. The loan
has a fixed interest rate of 15% per annum. If there are no net sales of remestemcel-L for pediatric SR-aGVHD, the loan is
only repayable at maturity. The Group can elect to prepay all outstanding amounts owing at any time prior to maturity,
subject to a prepayment charge.
Following approval and first commercial sales, repayments commence based on a percentage of net sales and are
limited by a payment cap which is equal to the principal due for the next 12 months, plus accumulated unpaid principal and
accrued unpaid interest. During the four-year period commencing July 8, 2022, principal amortizes in equal quarterly
instalments payable only after approval and first commercial sales. If in any quarterly period, 25% of net sales of
remestemcel-L for pediatric SR-aGVHD exceed the annual payment cap, the Group will pay the payment cap and an
additional portion of excess sales which will be used towards the prepayment amount in the event there is an early
prepayment of the loan. If in any quarterly period 25% of net sales of remestemcel-L for pediatric SR-aGVHD is less than
the annual payment cap, then the payment is limited to 25% of net sales of remestemcel-L for pediatric SR-aGVHD. Any
unpaid interest will be added to the principal amounts owing and shall accrue further interest. At maturity date, any unpaid
loan balances are repaid.
Because of this relationship of net sales and repayments, changes in our estimated net sales may trigger an
adjustment of the carrying amount of the financial liability to reflect the revised estimated cash flows. The carrying amount
is recalculated by computing the present value of the revised estimated future cash flows at the financial instrument’s
original effective interest rate. The adjustment is recognized in the Income Statement as remeasurement of borrowing
arrangements within finance costs in the period the revision is made.
In the years ended June 30, 2024, 2023 and 2022, respectively, the Group recognized a loss of $0.1 million and
gains of $0.9 million and $0.5 million in the Consolidated Income Statement as remeasurement of borrowing arrangements
within finance costs in relation to the adjustment of the carrying amount of the Group's financial liability to reflect the
revised estimated future cash flows as a net result of changes to the key assumptions in development timelines.
The Group recognizes a liability as current based on repayments linked to estimates of sales of remestemcel-L.
However, if sales of remestemcel-L are higher than estimated, actual repayments will exceed this amount, subject to the
annual payment cap described above.
The carrying amount of the loan and security agreement with NovaQuest is subordinated to the Group’s fixed rate
loan with the senior creditor, Oaktree. The Group have pledged a portion of our assets relating to the SR-aGVHD product
candidate as collateral under the loan facility with NovaQuest.
(ii)
Compliance with loan covenants
Our loan facilities with Oaktree and NovaQuest contain a number of covenants that impose operating restrictions
on us, which may restrict our ability to respond to changes in our business or take specified actions. The Group has an
operating objective to at all times maintain unrestricted cash reserves in excess of six months liquidity. The objective aligns
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180
with our loan and security agreement with Oaktree where the Group is currently obliged to maintain a minimum
unrestricted cash balance of $25.0 million.
The Group has complied with the financial and other restrictive covenants of its borrowing facilities during the
year ended June 30, 2024 and during the year ended June 30, 2023.
(iii)
Net debt reconciliation
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Cash and cash equivalents
62,960
71,318
Borrowings
(114,345)
(108,763)
Lease liabilities
(4,578)
(7,732)
Warrant liability
(4,647)
(5,426)
Net Debt(1)
(60,610)
(50,603)
Cash and cash equivalents
62,960
71,318
Gross debt - fixed interest rates
(118,923)
(116,495)
Gross debt - variable interest rates
—
—
Warrant liability
(4,647)
(5,426)
Net Debt(1)
(60,610)
(50,603)
(1)
Net debt amount includes leases and borrowing arrangements
Liabilities from financing activities
Other assets
(in U.S. dollars, in thousands)
Borrowings
Leases
Warrant
liability
Sub-total
Cash and
cash
equivalents
Total
Net Debt as at June 30, 2023
(108,763)
(7,732)
(5,426) (121,921)
71,318
(50,603)
Cash Flows(1)
16,921
3,877
—
20,798
(8,303)
12,495
Remeasurement adjustments
(2,351)
—
779
(1,572)
—
(1,572)
Other Changes(2)
(20,152)
(724)
—
(20,876)
—
(20,876)
Foreign exchange adjustments
—
1
1
(55)
(54)
Net Debt as at June 30, 2024
(114,345)
(4,578)
(4,647) (123,570)
62,960
(60,610)
(1)
Cash flows for borrowings and leases include the payments of borrowings, lease liabilities, interest and debt
transaction costs which are presented as financing cash flows in the statement of cash flows.
(2)
Other changes include modification of leases and accrued interest expenses for borrowings and leases.
(i)
Fair values of borrowing arrangements
The carrying amount of the borrowings at amortized cost in accordance with our accounting policy is a reasonable
approximation of fair value.
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181
g.
Recognized fair value measurements
(i)
Fair value hierarchy
The following table presents the Group's financial assets and financial liabilities measured and recognized at fair
value as of June 30, 2024 and June 30, 2023 on a recurring basis, categorized by level according to the significance of the
inputs used in making the measurements:
As of June 30, 2024
(in U.S. dollars, in thousands)
Notes
Level 1
Level 2
Level 3
Total
Financial Assets
Financial assets at fair value through other comprehensive
income:
Equity securities - biotech sector
5(c)
—
—
1,014
1,014
Total Financial Assets
—
—
1,014
1,014
Financial Liabilities
Financial liabilities at fair value through profit or loss:
Contingent consideration
5(g)(iii)
—
—
26,892
26,892
Warrant liabilities
5(g)(vi)
—
—
4,647
4,647
Total Financial Liabilities
—
—
31,539
31,539
There were no transfers between any of the levels for recurring fair value measurements during the period.
As of June 30, 2023
(in U.S. dollars, in thousands)
Notes
Level 1
Level 2
Level 3
Total
Financial Assets
Financial assets at fair value through other comprehensive
income:
Equity securities - biotech sector
5(c)
—
—
1,757
1,757
Total Financial Assets
—
—
1,757
1,757
Financial Liabilities
Financial liabilities at fair value through profit or loss:
Contingent consideration
5(g)(iii)
—
—
17,199
17,199
Warrant liabilities
5(g)(vi)
—
—
5,426
5,426
Total Financial Liabilities
—
—
22,625
22,625
The Group’s policy is to recognize transfers into and transfers out of fair value hierarchy levels as at the end of the
reporting period.
Level 1: The fair value of financial instruments traded in active markets (such as publicly traded derivatives, and
trading and financial assets at fair value through other comprehensive income securities) is based on quoted market prices
at the end of the reporting period. The quoted market price used for financial assets held by the Group is the current bid
price. These instruments are included in level 1.
Level 2: The fair value of financial instruments that are not traded in an active market (for example, foreign
exchange contracts) is determined using valuation techniques which maximize the use of observable market data and rely
as little as possible on entity-specific estimates. If all significant inputs required to fair value an instrument are observable,
the instrument is included in level 2.
Level 3: If one or more of the significant inputs is not based on observable market data, the instrument is included
in level 3. This is the case for provisions (contingent consideration), equity securities (unlisted) and warrant liabilities.
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182
(ii)
Valuation techniques used.
The Group did not hold any level 1 or 2 financial instruments as at June 30, 2024 or June 30, 2023.
The Group’s level 3 assets consists of an investment in unlisted equity securities in the biotechnology sector.
Level 3 assets were 100% of total assets measured at fair value as at June 30, 2024 and June 30, 2023. The Group’s level 3
liabilities consist of a contingent consideration provision related to the acquisition of Osiris’ MSC business and warrant
liabilities related to the warrants granted to Oaktree as part of the debt facility. Level 3 liabilities were 100% of total
liabilities measured at fair value as at June 30, 2024 and June 30, 2023. The Group used discounted cash flow analysis to
determine the fair value measurements of Osiris’ MSC business and used the Black-Scholes valuation method to determine
the fair value of warrant liabilities. Refer to Note 5(g)(vi) for the fair value measurement and movements in warrant
liability for the period ended June 30, 2024 and June 30, 2023.
(iii)
Fair value measurements using significant unobservable inputs (level 3)
The following table presents the changes in the contingent consideration balances within the level 3 instruments
for the years ended June 30, 2024 and June 30, 2023:
(in U.S. dollars, in thousands)
Contingent
consideration
provision
Opening balance - July 1, 2022
23,284
Reclassification during the period
2,686
Charged/(credited) to consolidated income statement:
Remeasurement(1)
(8,771)
Closing balance - June 30, 2023
17,199
Opening balance - July 1, 2023
17,199
Charged/(credited) to consolidated income statement:
Remeasurement(2)
9,693
Closing balance - June 30, 2024
26,892
(1) In the year ended June 30, 2023, a gain of $8.8 million was recognized on the remeasurement of contingent
consideration pertaining to the acquisition of assets from Osiris. This remeasurement was a net result of changing the
key assumptions of the contingent consideration valuation such as probability of payment, development timelines and
the increase in valuation as the time period shortens between the valuation date and the potential settlement dates of
contingent consideration, including the impact from the CRL from the FDA on the Group's BLA for remestemcel-L
for the treatment of pediatric SR-aGVHD in August 2023. The assumptions relating to development timelines were
updated to reflect expectations as a result of the CRL.
(2) In the year ended June 30, 2024, a loss of $9.7 million was recognized on the remeasurement of contingent
consideration pertaining to the acquisition of assets from Osiris. This remeasurement was a net result of changing key
assumptions of the contingent consideration valuation, such as probability of success, development timelines and the
increase in valuation as the time period shortens between the valuation date and the potential settlement dates of
contingent consideration. The outcome from the FDA decision on the Group's BLA resubmission in July 2024, as
discussed in Note 15, could lead to a change in the assumptions used within the valuation of the contingent
consideration.
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183
(iv)
Valuation inputs and relationship to fair value
The following table summarizes the quantitative information about the significant unobservable inputs used in
level 3 fair value measurements:
Range of inputs
(weighted average)
(in U.S. dollars, in thousands,
except percent data)
Description
Fair value
as of
June 30,
2024)
Fair value
as of
June 30,
2023)
Valuation
technique
Unobservable
inputs(1)
Year Ended
June 30,
2024
Year Ended
June 30,
2023
Relationship of
unobservable inputs to
fair value
Contingent consideration provision
26,892
17,199
Discounted
cash flows
Risk adjusted
discount rate
11%-13%
(12.5%)
11%-13%
(12.5%)
Year ended June 30, 2024: A
change in the discount rate by
0.5% would have no impact to
the fair value.
Year ended June 30, 2023: A
change in the discount rate by
0.5% would increase/decrease
the fair value by 0.01%.
Expected unit
sales price
Various
Various
Year ended June 30, 2024: A
change in the price
assumptions by 10% would
increase/decrease the fair value
by 0.1%.
Year ended June 30, 2023: A
change in the price
assumptions by 10% would
increase/decrease the fair value
by 0.1%.
Expected sales
volumes
Various
Various
Year ended June 30, 2024: A
change in the volume
assumptions by 10% would
increase/decrease the fair value
by 0.1%.
Year ended June 30, 2023: A
change in the volume
assumptions by 10% would
increase/decrease the fair value
by 0.1%.
Probability of
success and
payment
Various
Various
Year ended June 30, 2024: A
change in the probability of
success and payment
assumptions by 10% and 20%
would increase/decrease the
fair value by 10% and 20.1%,
respectively.
Year ended June 30, 2023: A
change in the probability of
success and payment
assumptions by 10% and 20%
would increase/decrease the
fair value by 8% and 16%,
respectively.
(1)
There were no significant inter-relationships between unobservable inputs that materially affect fair values.
(v)
Valuation processes
In connection with the Osiris acquisition, on October 11, 2013 (the “acquisition date”), an independent valuation
of the contingent consideration was carried out by an independent valuer.
For the years ended June 30, 2024 and June 30, 2023, the Group has adopted a process to value contingent
consideration internally. This valuation has been completed by the Group’s internal valuation team and reviewed by the
interim Chief Financial Officer (the "CFO"). The valuation team is responsible for the valuation model. The valuation team
also manages a process to continually refine the key assumptions within the model. This is done with input from the
relevant business units. The key assumptions in the model have been clearly defined and the responsibility for refining
those assumptions has been assigned to the most relevant business units. For each indication we determine the probability
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of success based on the current development status within each jurisdiction and payment provisions within the agreement.
Cash flows relevant to each jurisdiction are discounted appropriately based on the discount rate assumed. The
remeasurement charged to the consolidated income statement in the year ended June 30, 2024 was a net result of changing
the key assumptions of the contingent consideration valuation such as probability of success, development timelines and
the increase in valuation as the time period shortens between the valuation date and the potential settlement dates of
contingent consideration. The outcome from the FDA decision on the Group's BLA resubmission in July 2024, with a
PDUFA goal date of January 7, 2025, as discussed in Note 15, could lead to a change in the assumptions associated with
SR-aGVHD and a remeasurement of contingent consideration, up or down, could occur.
As of June 30,
The fair value of contingent consideration (in U.S. dollars, in thousands)
2024
2023
Fair value of cash or stock payable, dependent on achievement of future late-stage clinical
or regulatory targets
26,236
16,606
Fair value of royalty payments from commercialization of the intellectual property
acquired
656
593
26,892
17,199
The main level 3 inputs used by the Group are evaluated as follows:
Risk adjusted discount rate:
The discount rate used in the valuation has been determined based on required rates of
returns of listed companies in the biotechnology industry (having regards to their stage of
development, their size and number of projects) and the indicative rates of return required
by suppliers of venture capital for investments with similar technical and commercial
risks. This assumption is reviewed as part of the valuation process outlined above.
Expected unit sales prices:
Expected market sale price giving consideration to comparable products available in the
market place and a value based pricing assessment. This assumption is reviewed as part
of the valuation process outlined above.
Expected sales volumes:
Expected sales volumes of the most comparable products currently available in the
market place. This assumption is reviewed as part of the valuation process outlined
above.
Probability of success and
payment:
Expected cash flows used to measure contingent consideration are risk adjusted for the
probability of successful development of products and payment provisions with the
agreement. These assumptions are reviewed as part of the valuation process outlined
above.
(vi)
Warrant liability
(in U.S. dollars, in thousands)
As of June 30,
Warrant liability
2024
2023
Opening balance
5,426
2,185
Warrants fair value at grant date - December 22, 2022
—
1,036
Remeasurement of warrant liability
(779)
2,205
Closing Balance
4,647
5,426
On November 19, 2021, in connection with the initial draw down of the Oaktree debt, Oaktree was granted the
right to warrants to purchase 1,769,669 ADSs at US$7.26 per ADS, a 15% premium to the 30-day VWAP. Given that
Oaktree received an unconditional right to the warrants on November 19, 2021, this date has been determined as the
measurement date. The warrant instruments were issued on January 11, 2022, following the required administrative
process, and these warrants may be exercised within 7 years of issuance of the warrant instruments. The warrants do not
confer any rights to dividends or a right to participate in a new issue without exercising the warrant.
On December 21, 2022, the Group amended the terms of the loan agreement with Oaktree and in connection with
the loan amendment, Oaktree was granted warrants to purchase 455,000 ADSs at $3.70 per ADS, a 15% premium to the
30-day VWAP. The Group determined that an obligation to issue the warrants arose from the time the first amendment to
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185
the loan agreement was signed; consequently, a liability for the warrants was recognized in December 2022. The warrants
were legally issued on March 8, 2023 and may be exercised within 7 years of issuance. The warrants do not confer any
rights to dividends or a right to participate in a new issue without exercising the warrant.
On January 10, 2024, the ratio under Mesoblast's American Depository Receipt ("ADR") program was changed
from 5 ordinary shares representing 1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio).
As a result of this ratio change and as a result of completing the pro-rata accelerated non-renounceable rights issue in
December 2023, the number and exercise price for the warrants was adjusted in accordance with the terms of these
warrants. The warrants issued in November 2021 changed from 1,769,669 ADSs at US$7.26 per ADS to 884,838 ADSs at
US$14.36 per ADS. The warrants issued in December 2022 changed from 455,000 ADSs at US$3.70 per ADS to 227,502
ADSs at US$7.24 per ADS.
The exercise price of the warrants will be received in US$, which is different to Mesoblast Limited’s functional
currency of A$ which gives rise to variability in the cash flow. As a result, the warrants are classified as a financial liability
in accordance with IAS32 Financial Instruments: Presentation. The financial liability is recorded in warrant liability at fair
value at grant date and subsequently remeasured at each reporting period with changes being recorded in the Consolidated
Income Statement as remeasurement of warrant liability. The warrant liabilities are considered level 3 liabilities as the
determination of fair value includes various assumptions about the share prices and historical volatility as inputs.
As of June 30, 2024 and 2023, the fair value of warrant liability was $4.6 million and $5.4 million, respectively.
During the year ended June 30, 2024, a remeasurement gain of $0.8 million was recognized on the remeasurement of
warrant liability. During the year ended June 30, 2023, a remeasurement loss of $2.2 million was recognized on the
remeasurement of warrant liability.
(vii)
Fair value of warrants
The warrants granted are not traded in an active market and therefore the fair value has been estimated by using
the Black-Scholes valuation method based on the following assumptions. Key terms of the warrants are included below.
The following assumptions were based on observable market conditions that existed as of June 30, 2024 and 2023.
(in U.S. dollars, except percent data and as
otherwise noted)
Assumption
As of June 30,
2024
As of June 30,
2023
Rationale
Share Price
$6.81
$3.91
Closing share price on valuation date from
external market source
Exercise Price(1)
$7.24 to
$14.36
$3.70 to $7.26
As per subscription agreement
Expected Term
5 to 6 years
6 to 7 years
As per subscription agreement
Dividend Yield
0%
0%
Based on Company’s nil dividend history
Expected Volatility
91.91%
81.26%
Based on historical volatility data for the
Company
Risk Free Interest Rate
4.38%
4.01%
Based on the closing U.S. treasury issued
7 year bonds on valuation date
Fair value per warrant
$3.9352 to
$5.1211
$2.3103 to
$2.9401
Determined using Black-Scholes valuation
model with the inputs above
Fair value
$4,647,075
$5,426,212
Fair value of 1,112,340(1)warrants of
$4,647,075 as of June 30, 2024 and fair
value of 2,224,669(1) warrants of
$5,426,212 as of June 30, 2023
(1) As a result of the ratio change under Mesoblast's ADR program on January 10, 2024 and as a result of completing the
pro-rata accelerated non-renounceable rights issue in December 2023, the warrants issued in November 2021 changed
from 1,769,669 ADSs at US$7.26 per ADS to 884,838 ADSs at US$14.36 per ADS. The warrants issued in
December 2022 changed from 455,000 ADSs at US$3.70 per ADS to 227,502 ADSs at US$7.24 per ADS.
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186
6. Non-financial assets and liabilities
a.
Property, plant and equipment
(in U.S. dollars, in thousands)
Plant and
Equipment
Office Furniture
and Equipment
Computer
Hardware
and Software
Total
Year Ended June 30, 2023
Opening net book amount
1,208
692
145
2,045
Additions
171
43
60
274
Exchange differences
(104)
113
(18)
(9)
Depreciation charge
(818)
(45)
(90)
(953)
Closing net book value
457
803
97
1,357
As of June 30, 2023
Cost
6,910
2,074
3,353
12,337
Accumulated depreciation
(6,453)
(1,271)
(3,256)
(10,980)
Net book value
457
803
97
1,357
Year Ended June 30, 2024
Opening net book amount
457
803
97
1,357
Additions
38
—
120
158
Disposals
—
(2)
(7)
(9)
Exchange differences
(6)
(8)
16
2
Depreciation charge
(281)
(41)
(80)
(402)
Closing net book value
208
752
146
1,106
As of June 30, 2024
Cost
6,067
2,044
644
8,755
Accumulated depreciation
(5,859)
(1,292)
(498)
(7,649)
Net book value
208
752
146
1,106
(i)
Depreciation methods and useful lives
Depreciation is calculated using the straight-line method to allocate their cost or revalued amounts, net of their
residual values, over the estimated useful lives. The estimated useful lives are:
•
Plant and equipment 3 – 15 years
•
Office furniture and equipment 5 – 20 years
•
Computer hardware and software 3 – 5 years
See Note 23(o) for other accounting policies relevant to property, plant and equipment.
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187
b.
Leases
(i)
Amounts recognized on the consolidated balance sheet
Right-of-use assets
(in U.S. dollars, in thousands)
Buildings
Manufacturing
Total
Year Ended June 30, 2023
Opening net book amount
5,096
2,824
7,920
Additions/(derecognition)
(649)
—
(649)
Remeasurement
526
(302)
224
Exchange differences
(15)
—
(15)
Depreciation charge
(1,661)
(685)
(2,346)
Closing net book value
3,297
1,837
5,134
As of June 30, 2023
Cost
9,957
6,178
16,135
Accumulated depreciation
(6,660)
(4,341)
(11,001)
Net book value
3,297
1,837
5,134
Year Ended June 30, 2024
Opening net book amount
3,297
1,837
5,134
Additions
—
—
—
Remeasurement
—
369
369
Exchange differences
—
—
—
Depreciation charge
(1,570)
(1,201)
(2,771)
Closing net book value
1,727
1,005
2,732
As of June 30, 2024
Cost
9,128
6,245
15,373
Accumulated depreciation
(7,401)
(5,240)
(12,641)
Net book value
1,727
1,005
2,732
Lease liabilities
As of June 30,
2024
2023
Current
2,626
4,060
Non-current
1,952
3,672
Lease liabilities included in the balance sheet
4,578
7,732
The lease liability is measured at the present value of the fixed and variable lease payments net of cash lease
incentives that are not paid at the balance date. Lease payments are apportioned between the finance charges and reduction
of the lease liability using the incremental borrowing rate to achieve a constant rate of interest on the remaining balance of
the liability. Lease payments for buildings exclude service fees for cleaning and other costs. The interest expense (included
in finance costs) for leases was $0.4 million, $0.5 million and $0.6 million for the years ended June 30, 2024, 2023 and
2022, respectively. In the years ended June 30, 2024 and 2023, total payments associated with lease liabilities were $3.9
million and $3.2 million, respectively.
Payments associated with short-term leases with a lease term of 12 months or less, contracts that contain lease and
non-lease components that are cancellable within 12 months and leases of low-value assets are recognized on a straight-line
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188
basis as an expense in profit or loss. The expense relating to short-term leases was $0.3 million for the year ended June 30,
2024 and $1.1 million for the year ended June 30, 2023.
(ii)
Depreciation methods and useful lives of right-of use assets
Depreciation is calculated using the straight-line method to allocate their cost or revalued amounts over the
estimated useful lives. Depreciation for leases relating to buildings for the years ended June 30, 2024, 2023 and 2022 was
$1.6 million, $1.7 million and $1.7 million, respectively.
Depreciation for the lease relating to manufacturing was $1.2 million, $0.7 million, and $1.4 million for the years
ended June 30, 2024, 2023 and 2022, respectively, of which the $1.2 million of depreciation in the year ended June 30,
2024 was recognized in the consolidated income statement. Prior to the year ended June 30, 2024, depreciation on the
manufacturing lease was capitalized within pre-launch inventory.
(iii)
Extension and termination options
Extension options and termination options may be included in the right-of-use asset leases across the Group.
These are used to maximize operational flexibility in terms of managing the assets used in the Group’s operations.
In determining the lease term, management considers all facts and circumstances that create an economic
incentive to exercise an extension option, or not exercise a termination option. Extension options and periods after
termination options are only included in the lease term if the lease is reasonably certain to be extended or not terminated.
A right-of-use asset and lease liability has been recognized in relation to the manufacturing service agreement
entered into with Lonza in October 2019 for the supply of commercial product for the potential approval and launch of
remestemcel-L for the treatment of SR-aGVHD in the US market. Management has determined that this agreement has a
non-cancellable lease term expiring within 2 years from June 30, 2024, which is cancellable in limited circumstances.
As of June 30, 2024, the anticipated future contractual cash flows relating to the lease component of the Lonza
agreement are $1.9 million on an undiscounted basis, as included within lease liabilities in Note 10(c). The anticipated
future contractual cash flows exclude cashflows beyond the non-cancellable lease term as it is not reasonably certain the
Group will extend the agreement. At the Group's discretion, the minimum financial commitment relating to the lease
component under this manufacturing services agreement can be reduced by $1.0 million under certain conditions.
See Note 23(v) for other accounting policies relevant to lease accounting.
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189
c.
Intangible assets
(in U.S. dollars, in thousands)
Goodwill
Acquired
licenses
to patents
In-process
research and
development
acquired
Current
marketed
products
Total
Year Ended June 30, 2023
Opening net book amount
134,453
1,632
427,779
14,788
578,652
Additions/reversals
—
23
—
—
23
Exchange differences
—
1
—
—
1
Amortization charge
—
(38)
—
(1,455)
(1,493)
Closing net book amount
134,453
1,618
427,779
13,333
577,183
As of June 30, 2023
Cost
134,453
2,993
489,698
23,999
651,143
Accumulated amortization
—
(1,375)
—
(10,666)
(12,041)
Accumulated impairment
—
—
(61,919)
—
(61,919)
Net book amount
134,453
1,618
427,779
13,333
577,183
Year Ended June 30, 2024
Opening net book amount
134,453
1,618
427,779
13,333
577,183
Additions
—
37
—
—
37
Exchange differences
—
1
—
—
1
Amortization charge
—
(30)
—
(1,455)
(1,485)
Closing net book amount
134,453
1,626
427,779
11,878
575,736
As of June 30, 2024
Cost
134,453
3,032
489,698
24,000
651,183
Accumulated amortization
—
(1,406)
—
(12,122)
(13,528)
Accumulated impairment
—
—
(61,919)
—
(61,919)
Net book amount
134,453
1,626
427,779
11,878
575,736
(i)
Carrying value of in-process research and development acquired by product
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Cardiovascular products(1)
254,351
254,351
Intravenous products for metabolic diseases and inflammatory/immunologic conditions(2)
70,730
70,730
MSC products(3)
102,698
102,698
427,779
427,779
(1)
Includes MPC-150-IM for the treatment or prevention of chronic heart failure and MPC-25-IC for the treatment or
prevention of acute myocardial infarction
(2)
Includes MPC-300-IV for the treatment of biologic-refractory rheumatoid arthritis and diabetic nephropathy
(3)
Includes remestemcel-L for the treatment of SR-aGVHD and remestemcel-L for the treatment of Crohn’s disease
For all products included within the above balances, the underlying currency of each item recorded is US$.
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(ii)
Amortization methods and useful lives
The Group amortizes intangible assets with a finite useful life using the straight-line method over the following
periods:
•
Acquired licenses to patents 7 – 16 years
•
Current marketed products 15 – 20 years
See Note 23(p) for the other accounting policies relevant to intangible assets and Note 23(j) for the Group’s policy
regarding impairments.
(iii)
Significant estimate: Impairment of goodwill and assets with an indefinite useful life
The Group tests annually, or more frequently if events or changes in circumstances indicate that they might be
impaired, whether goodwill and its assets with indefinite useful lives have suffered any impairment in accordance with its
accounting policy stated in Note 23(j). The recoverable amounts of these assets and cash-generating units have been
determined based on fair value less costs to dispose calculations, which require the use of market-participant assumptions
that are based on development strategies using external data sources as well as past experience. The full annual impairment
assessment was performed at March 31, 2024 and no impairment of the in-process research and development and goodwill
was identified.
In August 2023, the FDA issued a CRL to the Group's BLA for remestemcel-L for the treatment of pediatric SR-
aGVHD and the Group has considered this to be an impairment indicator that could cause the carrying amount of its
intangible assets to exceed its recoverable amounts. As a result, the Group completed an impairment assessment on its
MSC products intangible asset and goodwill, which considered the impact of the FDA's CRL. An external valuation was
also obtained for the MSC products for the impairment assessment performed as a result of the receipt of the CRL. No
impairment of the in-process research and development and goodwill was identified.
In July 2024, as discussed in Note 15, the Group resubmitted its BLA for approval of remestemcel-L for the
treatment of pediatric SR-aGVHD, and the FDA accepted the Group's BLA resubmission and set a PDUFA goal date of
January 7, 2025. The outcome from the FDA decision on the Group's BLA resubmission could lead to a change in the
assumptions used within the impairment assessment associated with SR-aGVHD that could cause the carrying amount of
our intangible asset to exceed its recoverable amount.
(iv)
Impairment tests for goodwill and intangible assets with an indefinite useful life
The Group has recognized goodwill as a result of two separate acquisitions. Goodwill of $118.4 million was
recognized on acquisition of Angioblast Systems Inc. in 2010, $13.9 million was recognized on the acquisition of the MSC
assets from Osiris (“MSC business combination”) in 2013 and $2.1 million was recognized on finalization of the MSC
business combination of Osiris in 2015. In all cases the goodwill recognized represented excess in the purchase price over
the net identifiable assets and in-process research and development acquired in the transaction.
On acquisition, goodwill was not able to be allocated to the cash generating unit (“CGU”) level or to a group of
CGU given the synergies of the underlying research and development. For the purpose of impairment testing, goodwill is
monitored by management at the operating segment level. The Group is managed as one operating segment, being the
development of cell technology platform for commercialization.
IFRS requires that acquired in-process research and development be measured at fair value upon acquisition and
carried as an indefinite life intangible asset subject to annual impairment reviews. The Group have recognized in-process
research and development as a result of two separate acquisitions. In-process research and development of $387.0 million
was recognized on the acquisition of Angioblast Systems Inc. in 2010 and $126.7 million was recognized on the
acquisition of assets from Osiris in 2013 and $24.0 million was reclassified to current marketed products upon the
TEMCELL asset becoming available for use in Japan. In 2016, the Group fully impaired $61.9 million of in-process
research and development relating to our product candidates, MPC-MICRO-IO for the treatment of age-related macular
degeneration and MPC-CBE for the expansion of hematopoietic stem cells within cord blood, as the Group suspended
further patient enrollment of the Phase IIa MPC-MICRO-IO clinical trial and the Phase III MPC-CBE clinical trial as the
Group prioritized the funding of its lead product candidates.
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The Group still believe these product candidates remain viable upon further funding, or partnership, and
accordingly these products should not be regarded as abandoned, where typically, abandoned programs would be closed
down and the related research and development efforts are considered impaired and the asset is fully expensed. The
remaining carrying amount of in-process research and development as at June 30, 2024 and June 30, 2023 was $427.8
million.
In-process research and development acquired is considered to be an indefinite life intangible asset on the basis
that it is incomplete and cannot be used in its current form (see Note 23(p)(iii)). The intangible asset’s life will remain
indefinite until such time it is completed and commercialized or impaired. The carrying value of in-process research and
development is a separate asset which has been subject to impairment testing at the cash generating unit level, which has
been determined to be at the product level.
The recoverable amount of both goodwill and in-process research and development was assessed as of March 31,
2024 based on the fair value less costs to dispose. No impairment was identified as a result of this impairment assessment.
Management assess for indicators of impairment as at June 30, 2024, including considering events up to the date
of the approval of the financial statements. In July 2024, as discussed in Note 15, the Group resubmitted its BLA for
approval of remestemcel-L for the treatment of pediatric SR-aGVHD, and the FDA accepted the Group's BLA
resubmission and set a PDUFA goal date of January 7, 2025. The outcome from the FDA decision on the Group's BLA
resubmission could lead to a change in the assumptions used within the impairment assessment associated with SR-
aGVHD that could cause the carrying amount of our intangible asset to exceed its recoverable amount.
(v)
Key assumptions used for fair value less costs to dispose calculations
In determining the fair value less costs to dispose the Group has given consideration to the following internal and
external indicators:
•
discounted expected future cash flows of programs valued by the Group’s internal valuation team and
reviewed by the interim CFO. The valuation team also manages a process to continually refine the key
assumptions within the model. This is done with input from the relevant business units. The key
assumptions in the model have been clearly defined and the responsibility for refining those assumptions
has been assigned to the most relevant business units. When determining key assumptions, the business
units refer to both external sources and past experience as appropriate. The valuation is considered to be
level 3 in the fair value hierarchy due to unobservable inputs used in the valuation;
•
the scientific results and progress of the trials since acquisition;
•
the market capitalization of the Group on the ASX (ASX:MSB); and
•
the valuation of the Group’s assets from an independent valuation. An independent valuation was
obtained for all assets at March 31, 2023 and for the MSC products for the impairment assessment
performed as a result of the receipt of the complete response in August 2023.
Costs of disposal were assumed to be immaterial.
Discounted cash-flows used a real post-tax discount rate range of 13.8% to 15.5%, and include estimated real cash
inflows and outflows for each program through to expected patent expiry which ranges from 8 to 24 years.
In relation to cash outflows consideration has been given to cost of goods sold, selling costs and clinical trial
schedules including estimates of numbers of patients and per patient costs. Associated expenses such as regulatory fees and
patent maintenance have been included as well as any further preclinical development if applicable.
In relation to cash inflows consideration has been given to product pricing, market population and penetration,
sales rebates and discounts, launch timings and probability of success in the relevant applicable markets.
There are no standard growth rates applied, other than our estimates of market penetration which increase initially,
plateau and then decline.
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192
The assessment of the recoverable amount of each product has been made in accordance with the discounted cash-
flow assumptions outlined above. The assessments showed that the recoverable amount of each product exceeds the
carrying amount and therefore there is no impairment.
The assessment of goodwill showed the recoverable amount of the Group's operating segment, including goodwill
and remaining in-process research and development, exceeds carrying amounts, and therefore there is no impairment.
(vi)
Impact of possible changes in key assumptions
The Group has considered and assessed reasonably possible changes in the key assumptions and has not identified
any instances that could cause the carrying amount of our intangible assets to exceed its recoverable amount.
Whilst there is no impairment, the key sensitivities in the valuation are dependent on the continued successful
development of our technology platforms. In July 2024, as discussed in Note 15, the Group resubmitted its BLA for
approval of remestemcel-L for the treatment of pediatric SR-aGVHD, and the FDA accepted the Group's BLA
resubmission and set a PDUFA goal date of January 7, 2025. The outcome from the FDA decision on the Group's BLA
resubmission could lead to a change in the assumptions used within the impairment assessment associated with SR-
aGVHD that could cause the carrying amount of our intangible asset to exceed its recoverable amount. If the Group is
unable to successfully develop our technology platforms, an impairment of the carrying amount of our intangible assets
may result.
d.
Provisions
As of June 30, 2024
As of June 30, 2023
(in U.S. dollars, in thousands)
Notes
Current
Non-
current
Total
Current
Non-
current
Total
Contingent consideration
16,298
10,594
26,892
636
16,563
17,199
Employee benefits
7,436
26
7,462
2,013
49
2,062
Provision for license agreements
3,750
—
3,750
3,750
—
3,750
Provision for litigation settlements
22
17,554
—
17,554
—
—
—
45,038
10,620
55,658
6,399
16,612
23,011
(i)
Information about individual provisions and significant estimates
Contingent consideration
The contingent consideration provision relates to the Group’s liability for certain milestones and royalty
achievements pertaining to the acquired MSC assets from Osiris. Further disclosures can be found in Note 5(g)(iii).
Employee benefits
The provision for employee benefits relates to the Group’s liability for annual leave, short term incentives, long
service leave and deferred director fees.
Employee benefits include accrued annual leave. As of June 30, 2024 and 2023, the entire amount of the annual
leave accrual was $1.2 million and $1.1 million respectively, and is presented as current, since the Group does not have an
unconditional right to defer settlement for any of these obligations.
Employee benefits include a provision for the Group's liability for short term incentives. As of June 30, 2024 and
2023, the provision for short term incentive incentives was $5.4 million and $0.4 million, respectively, and the provision as
of June 30, 2024 of $5.4 million includes $2.4 million and $3.0 million relating to the entitlements for the years ended
June 30, 2024 and 2023, respectively, given that subsequent to June 30, 2023 the conditions of achievement of the short-
term incentive for year ended June 30, 2023 were modified to make it dependent on Mesoblast achieving FDA marketing
authorization. In August 2024, as discussed in Note 15, the Group modified the short term incentive plan providing
employees with the choice to elect into receiving an option grant in lieu of cash payment of their short term incentive
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193
entitlements for the years ended June 30, 2024 and 2023, which have been deferred to BLA approval. The level of
participation and the terms of the modification are yet to be determined at the date of this report.
(ii)
Movements
The contingent consideration provision relates to the Group’s liability for certain milestones and royalty
achievements. Refer to Note 5(g)(iii) for movements in contingent consideration for the years ended June 30, 2024 and
2023.
e.
Deferred tax balances
(i)
Deferred tax balances
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Deferred tax assets
The balance comprises temporary differences attributable to:
Tax losses
74,602
76,020
Other temporary differences
13,143
11,972
Total deferred tax assets
87,745
87,992
Deferred tax liabilities
The balance comprises temporary differences attributable to:
Intangible assets
87,745
87,992
Total deferred tax liabilities
87,745
87,992
Net deferred tax liabilities
—
—
(ii)
Movements
(in U.S. dollars, in thousands)
Tax losses(1)
(DTA)
Other
temporary
differences(1)
(DTA)
Intangible
assets (DTL)
Total (DTL)
As of June 30, 2022
80,411
7,831
(88,242)
—
Credited/(charged) to:
- profit or loss
(4,179)
4,141
250
212
- directly to equity
(212)
—
—
(212)
As of June 30, 2023
76,020
11,972
(87,992)
—
Credited/(charged) to:
- profit or loss
(1,227)
1,171
247
191
- directly to equity
(191)
—
—
(191)
As of June 30, 2024
74,602
13,143
(87,745)
—
(1)
Deferred tax assets are netted against deferred tax liabilities.
f.
Deferred consideration
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Opening balance(1)
2,500
2,500
Amount recognized as revenue during the period
—
—
Balance as of the end of the period
2,500
2,500
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194
(1)
The $2.5 million milestone payment received in December 2019 from Grünenthal was considered constrained and
resulted in deferred consideration as of June 30, 2024.
7. Equity
a.
Contributed equity
(i)
Share capital
As of June 30,
2024
2023
2022
2024
2023
2022
Shares No.
(U.S. dollars, in thousands)
Contributed equity
(i) Share capital
Ordinary shares
1,141,784,114
814,204,825
650,454,551
1,310,813 1,249,123 1,165,309
Less: Treasury Shares
(542,903)
(542,903)
(542,903)
—
—
—
Total Contributed Equity
1,141,241,211
813,661,922
649,911,648
1,310,813 1,249,123 1,165,309
(ii)
Movements in ordinary share capital
As of June 30,
As of June 30,
2024
2023
2022
2024
2023
2022
Shares No.
(U.S. dollars, in thousands)
Opening balance
814,204,825
650,454,551
648,696,070
1,249,123 1,165,309 1,163,153
Issues of ordinary shares during
the period
Exercise of share options(1)
—
—
—
7
—
209
Transfer to employee share trust(1)
1,072,363
—
—
—
—
—
Share based compensation for
services rendered
—
—
1,758,481
—
—
1,698
Entitlement offer to existing
eligible shareholders and
institutional placement(2)
326,506,926
—
—
64,399
——
—
Placement of shares under a share
placement agreement(3)
—
163,750,274
—
—
89,141
—
Transaction costs arising on share
issue
—
—
—
(3,920)
(5,327)
21
327,579,289
163,750,274
1,758,481
60,486
83,814
1,928
Unissued ordinary shares
during the period
Placement of shares under a share
placement agreement(2)
—
—
—
1,000
—
—
—
—
—
1,000
—
—
Total contributions of equity
during the period
327,579,289
163,750,274
1,758,481
61,486
83,814
1,928
Share options reserve transferred
to equity on exercise of options
—
—
—
204
—
228
Ending balance
1,141,784,114
814,204,825
650,454,551
1,310,813 1,249,123 1,165,309
(1) Options are issued to employees, directors and consultants in accordance with the Mesoblast Employee Share Option
Plan. Unpaid shares are issued to the share trust to enable future option exercises to be settled. On exercise of options,
the proceeds of the exercise are recorded in ordinary share capital in Mesoblast Limited and the exercise is settled by
transfer of the shares from the share trust to the employee.
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195
(2) In December 2023 and March 2024, respectively, 201,137,412 and 125,369,514 shares were issued in a 1 for 4 pro-
rata accelerated non-renounceable entitlement offer of new fully paid ordinary shares in Mesoblast Limited to
existing shareholders in Australia and certain other countries together with an institutional placement of new fully
paid ordinary shares in Mesoblast Limited, at A$0.30 per share. As part of the placement in March 2024, Dr. Eric
Rose, the Company's Chief Medical Offer and a director of Mesoblast, subscribed for 5,039,814 shares in Mesoblast
Limited at A$0.30 per share, subject to shareholder approval, and therefore the shares remain in unissued capital until
the shares are issued.
(3) In August 2022, 86,666,667 shares were issued in an equity purchase of Mesoblast Limited at A$0.75 per share to
existing and new institutional investors, representing a 5.00% discount to the thirty trading-day volume weighted
average price. In April 2023, 77,083,607 shares were issued in an equity purchase of Mesoblast Limited at A$0.85
per share primarily to existing major shareholders, representing a 15.00% discount to the five trading-day volume
weighted average price.
(iii)
Movements of shares in share trust
As of June 30
As of June 30
2024
2023
2022
2024
2023
2022
Shares No.
(U.S. dollars, in thousands)
Opening balance
542,903
542,903
771,983
—
—
—
Movement of shares in
share trust
Transfer to employee share
trust(1)
1,072,363
—
—
—
—
—
Exercise of share options(1)
(1,072,363)
—
(229,080)
—
—
—
Ending balance
542,903
542,903
542,903
—
—
—
(1) Options are issued to employees, directors and consultants in accordance with the Mesoblast Employee Share Option
Plan. Unpaid shares are issued to the share trust to enable future option exercises to be settled. On exercise of options,
the proceeds of the exercise are recorded in ordinary share capital in Mesoblast Limited and the exercise is settled by
transfer of the shares from the share trust to the employee.
(iv)
Ordinary shares
Ordinary shares participate in dividends and the proceeds on winding up of the Group in equal proportion to the
number of shares held. At shareholders meetings each ordinary share is entitled to one vote when a poll is called, otherwise
each shareholder has one vote on a show of hands. Ordinary shares have no par value and the Company does not have a
limited amount of authorized capital.
(v)
Employee share options
Information relating to the Group’s employee share option plan, including details of shares issued under the
scheme, is set out in Note 17.
b.
Reserves
(i)
Reserves
As at June 30,
(in U.S. dollars, in thousands)
2024
2023
Share-based payments reserve
106,842
101,367
Investment revaluation reserve
(1,286)
(543)
Foreign currency translation reserve
(40,222)
(40,273)
Warrants reserve
12,969
12,969
78,303
73,520
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196
(ii)
Reconciliation of reserves
(in U.S. dollars, in thousands)
As at June 30,
Share-based payments reserve
2024
2023
Opening balance
101,367
97,924
Tax credited / (debited) to equity
(191)
(212)
Transfer to ordinary shares on exercise of options
(204)
—
Share-based payment expense for the year
5,870
3,655
Closing Balance
106,842
101,367
Investment revaluation reserve
Opening balance
(543)
(542)
Changes in the fair value of financial assets through other comprehensive income
(743)
(1)
Closing Balance
(1,286)
(543)
Foreign currency translation reserve
Opening balance
(40,273)
(39,700)
Currency gain/(loss) on translation of foreign operations net assets
51
(573)
Closing Balance
(40,222)
(40,273)
Warrant reserve
Opening balance
12,969
12,969
Movements during the period
—
—
Closing Balance
12,969
12,969
(iii)
Nature and purpose of reserves
Share-based payment reserve
The share-based payments reserve is used to recognize:
•
the fair value(1) of options issued but not exercised; and
•
the fair value(1) of deferred shares granted but not yet vested.
(1)
The fair value recognized is determined at the acceptance date, which is the date at which the entity and
the employee agree to a share-based payment arrangement, being when the entity and the employee have a shared
understanding of the terms and conditions of the arrangement or when they are approved by shareholders when this
is required.
Foreign currency translation reserve
Exchange differences arising on translation of a foreign controlled entity are recognized in other comprehensive
income and accumulated in a separate reserve within equity. The cumulative amount is reclassified to profit or loss when
the net investment is disposed of.
Warrants reserve
In March 2021, the Group completed a A$138.0 million (US$110.0 million) private placement of 60,109,290 new
fully-paid ordinary shares at a price of A$2.30. As part of this placement, the Group also issued one warrant for every four
ordinary shares issued in the placement, which resulted in a further 15,027,327 warrants issued. Each warrant has an
exercise price of A$2.88 per share and a 7 year term. The Group has a right to compel exercise of the warrants at any time,
subject to the price of the Group’s ordinary shares trading at least A$4.32 for 45 consecutive days on the ASX. The
warrants do not confer any rights to dividends or a right to participate in a new issue without exercising the warrant. As a
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197
result of completing the pro-rata accelerated non-renounceable rights issue in December 2023, the exercise price for the
warrants was adjusted from A$2.88 per share to A$2.86 per share with effect from January 5, 2024.
The terms of the warrants include certain anti-dilution clauses, which adjust the exercise price or conversion ratio
in the event of a rights issue or bonus issue. Management analyzed these clauses and determined the fixed-for-fixed
requirement was still satisfied because the relative rights of shareholders and warrant holders were maintained. Therefore
the warrants were classified as equity. The warrants were initially measured in equity at fair value, which was determined
using a Monte Carlo simulation (refer to Note 7(b)(iv)), with the residual consideration being attributed to the ordinary
shares issued in the same transaction. The warrants are not remeasured for subsequent changes in fair value.
(iv)
Fair value of warrants
The warrants granted are not traded in an active market and therefore the fair value has been estimated by using
the Monte Carlo pricing model based on the following assumptions. Key terms of the warrants are included above. The
following assumptions were based on observable market conditions that existed at the issue date.
(in U.S. dollars, except percent data and
as otherwise noted)
Assumption
At Issue date - March
18, 2021
Rationale
Share Price
A$2.41
Closing share price on valuation date from external
market source
Exercise Price(1)
A$2.88
As per subscription agreement
Expected Term
7 years
As per subscription agreement
Dividend Yield
0%
Based on Company’s nil dividend history
Expected Volatility
66.88%
Based on historical volatility data for the Company
A$-US$ FX Spot Rate
0.7827
Closing FX rate on valuation date from the Reserve
Bank of Australia historical foreign exchange rate
tables
Risk Free Interest Rate
1.24%
Based on the mid-point of the Australian
Government issued 5 year and 10 year bonds
Fair value per warrant
$0.863 (A$1.103)
Determined using Monte Carlo pricing models with
the inputs above
Fair value
$12,968,583
Fair value of 15,027,327 warrants as at issue date
(1) As a result of completing the pro-rata accelerated non-renounceable rights issue in December 2023, the exercise price
for the warrants was adjusted from A$2.88 per share to A$2.86 per share with effect from January 5, 2024.
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198
8. Cash flow information
(in U.S. dollars, in thousands)
As of June 30,
(a) Reconciliation of cash and cash equivalents
2024
2023
2022
Cash at bank
62,563
70,920
60,034
Deposits at call
397
398
413
62,960
71,318
60,447
(in U.S. dollars, in thousands)
As of June 30,
(b) Reconciliation of net cash flows used in operations with loss after income tax
2024
2023
2022
Loss for the period
(87,956)
(81,889)
(91,347)
Add/(deduct) net loss for non-cash items as follows:
Depreciation and amortization
4,666
4,107
4,380
Foreign exchange losses/(gains)
78
62
536
Finance costs
22,792
20,122
17,288
Remeasurement of contingent consideration
9,693
(8,771)
(913)
Remeasurement of warrant liabilities
(779)
2,205
(5,896)
Equity settled share-based payment
5,870
3,655
5,536
Deferred tax benefit
(191)
(212)
(235)
Gain on derecognition of right-of-use assets
—
(76)
—
Change in operating assets and liabilities:
Decrease/(increase) in trade and other receivables
(15,466)
(118)
140
Decrease/(increase) in prepayments
807
1,650
1,555
Increase/(decrease) in trade and other payables
(12,378)
(398)
4,777
Decrease/(increase) in tax incentive recoverable
1,490
(2,388)
—
Increase/(decrease) in provisions
22,916
(1,218)
(1,603)
Net cash outflows used in operations
(48,458)
(63,269)
(65,782)
9. Significant estimates, judgments and errors
The preparation of financial statements requires the use of accounting estimates which, by definition, will seldom
equal the actual results. Management also needs to exercise judgment in applying the Group’s accounting policies.
This note provides an overview of the areas that involved a higher degree of judgment or complexity, and of items
which are more likely to be materially adjusted due to estimates and assumptions turning out to be wrong. Detailed
information about each of these estimates and judgments is included in Notes 1 to 8 together with information about the
basis of calculation for each affected line item in the financial statements. In addition, this note also explains where there
have been actual adjustments this year as a result of an error and of changes to previous estimates.
Significant estimates and judgments
The areas involving significant estimates or judgments are:
•
recognition of revenue (Note 3 and Note 23(e));
•
fair value of contingent liabilities and contingent purchase consideration in a business combination (Note
5(g) and 13);
•
recoverable amount of goodwill and other intangible assets including in-process research and
development (Note 6(c));
•
useful life of intangible assets (Note 6(c));
•
recognition of deferred tax assets and deferred tax liabilities (Note 4);
•
fair value of share-based payments (Note 17);
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199
•
remeasurement of borrowings due to change in estimated cash flows (Note 5(f));
•
recognition of pre-launch inventory costs (Note 23(f)); and
•
fair value of warrant liability (Note 5(g)).
The preparation of these consolidated financial statements requires the Group to make estimates and judgments
that affect the reported amounts of assets, liabilities, income and expenses and related disclosures. On an ongoing basis, the
Group evaluates its significant accounting policies and estimates. Estimates are based on historical experience and on
various market-specific and other relevant assumptions that the Group believes to be reasonable under the circumstances,
the results of which form the basis for making judgments about the carrying values of assets and liabilities.
10. Financial risk management
This note explains the Group’s exposure to financial risks and how these risks could affect the Group’s future
financial performance. Current year profit and loss information has been included where relevant to add further context.
Risk
Exposure arising from
Measurement
Management
Market risk – currency
risk
Future commercial
transactions
Recognized financial assets
and liabilities not
denominated in the
functional currency of each
entity within the Group
Cash flow
forecasting
Sensitivity
analysis
The future cash flows of each currency are
forecast and the quantum of cash reserves
held for each currency are managed in line
with future forecasted requirements. Cross
currency swaps are undertaken as required.
Market risk – interest
rate risk
Term deposits at fixed rates
Cash deposits at variable
rates
Sensitivity
analysis
Vary length of term deposits, utilize interest
bearing accounts and periodically review
interest rates available to ensure we earn
interest at market rates.
Market risk – price
risk
Long-term borrowings
Sensitivity
analysis
Forecasts of net sales of the product
underlying the NovaQuest borrowing
arrangement are updated on a quarterly basis
to evaluate the impact on the carrying
amount of the financial liability.
Market risk - share
price risk
Warrant liability
Sensitivity
analysis
The future exercise of warrants will not
impact the Group's future cash flows
significantly given the warrants will be paid
in shares upon exercise. Therefore there are
no significant cashflow risks associated with
these warrants. The Group monitors the
profit or loss impact that share price
movements have on the valuation of the
warrant liability each period.
Credit risk
Cash and cash equivalents,
trade and other receivables
and other non-current assets
Aging analysis
Credit ratings
Transact primarily with the best risk rated
banks available in each region giving
consideration to the products required, the
quantum of cash reserves held and future
forecasted requirements
Liquidity risk
Cash and cash equivalents,
borrowings, trade payables,
lease liabilities and
contingent consideration
Rolling cash flow
forecasts
Future cash flows requirements are
forecasted and capital raising strategies are
planned to ensure sufficient cash balances
are maintained to meet the Group’s future
commitments.
a.
Market risk
(i)
Currency risk
The Group has foreign currency amounts owing relating to clinical, regulatory and overhead activities and foreign
currency deposits held primarily in the Group’s Australian based entity, whose functional currency is the A$. The Group
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200
also has foreign currency amounts owing in the Group’s Swiss and Singapore based entities, whose functional currencies
are the US$. The Group also has foreign currency amounts owing in various other non-US$ currencies in A$ and US$
functional currency entities in the Group relating to clinical, regulatory and overhead activities. These foreign currency
balances give rise to a currency risk, which is the risk of the exchange rate moving, in either direction, and the impact it
may have on the Group’s financial performance.
Currency risk is minimized by ensuring the proportion of cash reserves held in each currency matches the
expected rate of spend of each currency.
As of June 30, 2024, the Group held 76% of its cash in US$, 23% in A$ and 1% in other currencies. As of
June 30, 2023 the Group held 67% of its cash in US$, and 33% in A$.
The balances held at the end of the year that give rise to currency risk exposure are presented in US$ in the
following table, together with a sensitivity analysis which assesses the impact that a change of +/-20% in the exchange rate
as of June 30, 2024 and June 30, 2023 would have had on the Group’s reported net profits/(losses) and/or equity balance.
The bank balances held at the end of the year that are presented in the following table give rise to currency risk exposure as
they are not in the functional currency of the entity in which it is held.
+20%
-20%
(in U.S. dollars, in thousands, unless otherwise noted)
As of June 30, 2024
Foreign
currency
balance held
Profit/(Loss)
US$
Profit/(Loss)
US$
Bank accounts – USD
US$819 $
164 $
(164)
Bank accounts – CHF
CHF96 $
21 $
(21)
Bank accounts – SGD
S$62 $
9 $
(9)
Bank accounts – EUR
EUR151 $
32 $
(32)
Trade and other receivables - USD
US$400 $
80 $
(80)
Trade and other receivables - SGD
S$396 $
58 $
(58)
Trade and other receivables - CHF
CHF4 $
1 $
(1)
Trade and other receivables - EUR
EUR175 $
37 $
(37)
Trade payables and accruals - USD
(US$1,024) $
(204) $
204
Trade payables and accruals - AUD
(A$130) $
(17) $
17
Trade payables and accruals - SGD
(S$217) $
(32) $
32
Trade payables and accruals - GBP
(GBP60) $
(15) $
15
Trade payables and accruals - EUR
(EUR36) $
(8) $
8
Trade payables and accruals - CHF
(CHF19) $
(4) $
4
Provisions – USD
(US$1,750) $
(350) $
350
$
(228) $
228
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201
+20%
-20%
(in U.S. dollars, in thousands, unless otherwise noted)
As of June 30, 2023
Foreign
currency
balance held
Profit/(Loss)
US$
Profit/(Loss)
US$
Bank accounts – USD
US$60 $
12 $
(12)
Bank accounts – CHF
CHF79 $
18 $
(18)
Bank accounts – SGD
S$80 $
12 $
(12)
Bank accounts – EUR
EUR4 $
1 $
(1)
Trade and other receivables - USD
US$400 $
80 $
(80)
Trade and other receivables - SGD
S$106 $
16 $
(16)
Trade and other receivables - CHF
CHF3 $
1 $
(1)
Trade and other receivables - EUR
EUR292 $
63 $
(63)
Trade payables and accruals - USD
(US$1,361) $
(272) $
272
Trade payables and accruals - AUD
(A$1,064) $
(141) $
141
Trade payables and accruals - SGD
(S$422) $
(62) $
62
Trade payables and accruals - GBP
(GBP45) $
(11) $
11
Trade payables and accruals - EUR
(EUR26) $
(6) $
6
Trade payables and accruals - CHF
(CHF40) $
(9) $
9
Provisions – USD
(US$1,750) $
(350) $
350
$
(648) $
648
(ii)
Cash flow and interest rate risk
The Group is exposed to interest rate movements which impacts interest income earned on its deposits and at call
accounts. The interest rate risk is managed by spreading the maturity date of our deposits across various periods. The
Group ensures that sufficient funds are available, in at call accounts, to meet the working capital requirements of the
Group.
The deposits held which derive interest revenue are described in the table below, together with the maximum and
minimum interest rates being earned as of June 30, 2024 and June 30, 2023. The effect on profit is shown if interest rates
change by 10%, in either direction, is as follows:
As of
Jun 30, 2024
As of
June 30, 2023
(in U.S. dollars, in thousands, except percent data)
Low
High
US$
Low
High
US$
Funds invested – US$
1.84 %
1.84 %
25,123
1.79 %
1.79 %
40,569
Rate increase by 10%
2.02 %
2.02 %
46
1.97 %
1.97 %
73
Rate decrease by 10%
1.66 %
1.66 %
(46)
1.61 %
1.61 %
(73)
As of
Jun 30, 2024
As of
June 30, 2023 (1)
(in Australian dollars, in thousands, except percent
data)
Low
High
A$
Low
High
A$
Funds invested – A$
3.85 %
4.86 %
22,169
3.60 %
4.59 %
35,707
Rate increase by 10%
4.24 %
5.35 %
95
3.96 %
5.05 %
143
Rate decrease by 10%
3.47 %
4.37 %
(95)
3.24 %
4.13 %
(143)
(1) A$ deposits held as of June 30, 2023 have been updated to reflect the increasing impact of higher interest rates.
(iii)
Price risk
Price risk is the risk that future cash flows derived from financial instruments will be altered as a result of a
market price movement, which is defined as movements other than foreign currency rates and interest rates. The Group is
Table of Contents
202
exposed to price risk which arises from long-term borrowings under its facility with NovaQuest, where the timing and
amounts of principal and interest payments is dependent on net sales of remestemcel-L for the treatment of SR-aGVHD in
pediatric patients in the United States and other territories excluding Asia. As net sales of remestemcel-L for the treatment
of SR-aGVHD in pediatric patients in these territories increase/decrease, the timing and amount of principal and interest
payments relating to the financing arrangement will also fluctuate, resulting in an adjustment to the carrying amount of
financial liability. The adjustment is recognized in the Consolidated Income Statement as remeasurement of borrowing
arrangements within finance costs in the period the revision is made.
The exposure of the Group’s borrowing to price rate changes are as follows:
As of
Jun 30, 2024
As of
June 30, 2023
(in U.S. dollars, in thousands, except percent data)
Total
% of total
borrowings
Total
% of total
borrowings
Financial liabilities
Current borrowings
Borrowings – NovaQuest
1,869
2 %
336
0 %
Non-current borrowings
Borrowings – NovaQuest
64,562
56 %
55,739
51 %
66,431
58 %
56,075
51 %
As at June 30, 2024, all other factors held constant, a +/-20% change in the forecast net sales of remestemcel-L for
the treatment of SR-aGVHD in pediatric patients in the United States and other territories excluding Asia would not have a
significant impact on non-current borrowings and profit.
The Group is also exposed to price risk on contingent consideration provision balances, as expected unit revenues
are a significant unobservable input used in the level 3 fair value measurements. As at June 30, 2024, all other factors held
constant, the increase/decrease in price assumptions adopted in the fair value measurements of the contingent consideration
provision are discussed in Note 5(g)(iv).
The Group does not consider it has any exposure to price risk other than those already described above.
(iv)
Share price risk
The Group's exposure to share price risk arises from warrant liabilities held by the Group and classified in the
statement of financial position at fair value through profit or loss. The future exercise of these warrants will not impact the
Group's future cash flows significantly given the warrants will be paid in shares upon exercise, therefore there are no
significant cashflow risks associated with these warrants. The Group monitors the impact on profit or loss that share price
movements have on the valuation of the warrant liability each period.
The table below summarizes the impact of the increase/decrease of Mesoblast's share price on the Group's profit
or loss during the period, based on the assumption that the share price had increased/decreased by 10% and 10% with all
other variables held constant as of June 30, 2024 and June 30, 2023 respectively.
(in U.S. dollars, in thousands)
As of
June 30, 2024
As of
June 30, 2023
Financial liabilities
Warrant liability
4,647
5,426
Impact on profit or (loss)
Share price increase by 10% (2023: 10%)
(598)
(698)
Share price decrease by 10% (2023: 10%)
587
686
Table of Contents
203
b. Credit risk
Credit risk is the risk that one party to a financial instrument will fail to discharge its obligation and cause
financial loss to the other party. The maximum exposure to credit risk at the end of the reporting period is the carrying
amount of each class of financial assets. The Group’s receivables are tabled below.
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Cash and cash equivalents
Deposits at call (Note 5(a)) - minimum A rated
397
398
Cash at bank (Note 5(a)) - minimum A rated
62,563
70,920
Trade and other receivables
Receivable from other parties (non-rated)
1,403
2,276
Receivable from the Australian Government (Income Tax)
854
2,363
Receivable from the United States Government (U.S. tax credits)
—
1,473
Receivable from the Australian Government (Foreign Withholding Tax)
400
400
Receivable from the Australian Government (Goods and Services Tax)
126
121
Receivable from the Singapore Government (Goods and Services Tax)
292
78
Receivable from the United States Government (Foreign Withholding Tax)
71
71
Receivable from minimum A rated bank deposits (interest)
23
18
Receivable from the Swiss Government (Value-Added Tax)
5
3
Receivable from the United States Government (Income Tax)
—
—
Other non-current assets
Minimum A rated bank deposits (held as security)
1,912
1,912
c. Liquidity risk
Liquidity risk is the risk that the Group will not be able to pay its debts as and when they fall due. Liquidity risk
has been assessed in Note 1(i).
All financial liabilities, excluding contingent consideration, borrowings and lease liabilities held by the Group as
of June 30, 2024 and June 30, 2023 mature within 6 months. Trade payables and contingent consideration held by the
Group as of June 30, 2024 and June 30, 2023 are non-interest bearing. The total contractual cash flows associated with
trade payables equate to the carrying amount disclosed within the financial statements.
As of June 30, 2024, the maturity profile of the anticipated future contractual cash flows, on an undiscounted basis
and removing probability adjustments as applicable for contingent consideration, and which, therefore differs from the
carrying value, is as follows:
(in U.S. dollars, in thousands)
Within
1 year
Between
1-2 years
Between
2-5 years
Over
5 years
Total
contractual
cash flows
Carrying
amount
Borrowings(1)(2)
(15,763) (140,716)
—
— (156,479) (114,345)
Trade payables
(7,071)
—
—
—
(7,071)
(7,070)
Lease liabilities
(2,819)
(1,797)
(206)
—
(4,822)
(4,578)
Contingent consideration(3)
(5,500)
(1,604)
—
—
(7,104)
(656)
(31,153) (144,117)
(206)
— (175,476) (126,649)
(1)
Contractual cash flows include payments of principal, interest and other charges. Interest is calculated based on
debt held at June 30, 2024 without taking into account drawdowns of further tranches.
(2)
In relation to the contractual maturities of the NovaQuest borrowings, there is variability in the maturity profile of
the anticipated future contractual cash flows given the timing and amount of payments are calculated based on our
estimated net sales of remestemcel-L for the treatment of pediatric SR-aGVHD in the United States and other
territories excluding Asia.
Table of Contents
204
(3)
In relation to the contractual maturities of the royalty payments related to contingent consideration, there is
variability in the maturity profile of the anticipated future contractual cash flows given the timing and amount of
payments are calculated based on our estimated net sales of remestemcel-L for the treatment of children and adults
with aGVHD. Product royalties will be payable in cash which will be funded from royalties received from net
sales. With respect to future milestone payments, contingent consideration will be payable in cash or shares at our
discretion. The carrying amount reflects the discounted and probability adjusted contractual balance related to
royalty payments.
11. Capital management
The Group’s objective when managing capital is to safeguard its ability to continue as a going concern, so that it
can provide returns for shareholders and benefits for other stakeholders. See Note 5(a) for the cash reserves of the Group as
at the end of the financial reporting period.
12. Interests in other entities
The Group’s subsidiaries as of June 30, 2024 and 2023 are set out below. Unless otherwise stated, they have share
capital consisting solely of ordinary shares that are held directly by the Group, and the proportion of ownership interests
held equals the voting rights held by the Group. The country of incorporation or registration is also their principal place of
business, aside from BeiCell Ltd, which was incorporated in the Cayman Islands however operates in Hong Kong.
Country of
incorporation
Class of
shares
Equity holding
As of June 30,
2024
2023
%
%
Mesoblast, Inc.
USA
Ordinary
100
100
Mesoblast International Sàrl (includes Mesoblast
International Sàrl Singapore Branch)
Switzerland
Ordinary
100
100
Mesoblast Australia Pty Ltd
Australia
Ordinary
100
100
Mesoblast UK Ltd
United
Kingdom
Ordinary
100
100
BeiCell Ltd
Cayman
Islands
Ordinary
100
100
13. Contingent assets and liabilities
a.
Contingent assets
The Group did not have any contingent assets outstanding as of June 30, 2024 and June 30, 2023.
b.
Contingent liabilities
(i)
Central Adelaide Local Health Network Incorporated (“CALHNI”) (formerly Medvet)
The Group acquired certain intellectual property relating to our MPCs, or Medvet IP, pursuant to an Intellectual
Property Assignment Deed, or IP Deed, with Medvet Science Pty Ltd, or Medvet. Medvet’s rights under the IP Deed were
transferred to Central Adelaide Local Health Network Incorporated, or CALHNI, in November 2011. In connection with its
use of the Medvet IP, on completion of certain milestones the Group will be obligated to pay CALHNI, as successor in
interest to Medvet, (i) certain aggregated milestone payments of up to $2.2 million and single-digit royalties on net sales of
products covered by the Medvet IP, for cardiac muscle and blood vessel applications and bone and cartilage regeneration
and repair applications, subject to minimum annual royalties beginning in the first year of commercial sale of those
products and (ii) single-digit royalties on net sales of the specified products for applications outside the specified fields.
(ii)
Other contingent liabilities
The Group has entered into a number of other agreements with other third parties pertaining to intellectual
property. Contingent liabilities may arise in the future if certain events or developments occur in relation to these
Table of Contents
205
agreements. As of June 30, 2024, the Group has assessed these contingent liabilities to be remote and specific disclosure is
not required.
14. Commitments
a.
Capital commitments
The Group did not have any commitments for future capital expenditure outstanding as of June 30, 2024 and
June 30, 2023.
b.
Purchase commitments
In December 2019, the Group commenced production under its manufacturing service agreement with Lonza for
the supply of commercial product for the potential approval and launch of remestemcel-L for the treatment of pediatric SR-
aGVHD in the US market. This agreement contains lease and non-lease components. As of June 30, 2024, the agreement
contains a minimum remaining financial commitment of the non-lease component of $9.1 million, payable until December
2025, which is cancellable in limited circumstances. The Group has accounted for the lease component within the
agreement as a lease liability separately from the non-lease components. As of June 30, 2024, the lease component is $1.9
million on an undiscounted basis, as disclosed within the total contractual cash flows as lease liabilities in Note 10(c). At
the Group's discretion, the minimum financial commitment under this manufacturing services agreement can be reduced by
$4.9 million under certain conditions, with $1.0 million of this reduction relating to the lease component and $3.9 million
relating to the non-lease component of the agreement.
The group have agreements with third parties related to contract manufacturing and other goods and services. As
of June 30, 2024, the Group had $3.4 million of non-cancellable purchase commitments related to raw materials,
manufacturing agreements and other goods and services. This amount represents our minimum contractual obligations,
including termination fees. Certain agreements provide for termination rights subject to termination fees. Under such
agreement, the Group are contractually obligated to make certain payments, mainly, to reimburse them for their
unrecoverable outlays incurred prior to cancellation.
The Group did not have any other purchase commitments as of June 30, 2024.
15. Events occurring after the reporting period
In July 2024, the Group resubmitted it's BLA with the FDA for approval of remestemcel-L in the treatment of
children with SR-aGVHD and the FDA accepted the Group's BLA resubmission and set a PDUFA goal date of January 7,
2025. Assumptions associated with SR-aGVHD are included within the impairment assessment of Osiris MSC products
within in-process research and development, contingent consideration, pre-launch inventory and the NovaQuest
borrowings on the consolidated balance sheet and forecast net operating cash usage.
In August 2024, the Group modified the short term incentive plan providing employees with the choice to elect
into receiving an option grant in lieu of cash payment of their short term incentive entitlements for the years ended June 30,
2024 and 2023, which have been deferred to BLA approval. The level of participation and the terms of the modification are
yet to be determined at the date of this report.
In August 2024, the Group announced that the consolidated class action, filed in the Federal Court in Australia in
2022, has been resolved subject to Federal Court approval and includes no admission of liability. In relation to the
settlement of the class action, which was assessed as an adjusting subsequent event, the Group recognized a provision for
litigation settlement as of June 30, 2024 in the consolidated balance sheet (inclusive of interest and costs), refer to Note
6(d). Given the settlement will be funded entirely by Mesoblast's insurers, the Group has also recognized an insurance asset
within trade and other receivables in the consolidated balance sheet as of June 30, 2024, refer to Note 5(b).
There were no other events that have occurred after June 30, 2024 and prior to the signing of this financial report
that would likely have a material impact on the financial results presented.
Table of Contents
206
16. Related party transactions
a.
Parent entity
The parent entity within the Group is Mesoblast Limited.
b.
Subsidiaries
Details of interests in subsidiaries are disclosed in Note 12 to the financial statements.
c.
Key management personnel compensation
The aggregate compensation made to Directors and other members of key management personnel ("KMP") of the
Group is set out below:
Year Ended June 30,
(in U.S. dollars)
2024
2023
Short-term employee benefits
2,762,736
2,153,181
Long-term employee benefits
11,124
11,326
Post-employment benefits
18,900
23,935
Share based payments
1,704,995
881,342
4,497,755
3,069,784
The aggregate other service payments made to Directors and other members of key management personnel of the
Group is set out below:
Philip Krause has been a non-executive director of Mesoblast since March 2022. Philip Krause was appointed to a
formal strategic advisory role on June 4, 2023 where he was remunerated at an hourly rate and the agreement was able to
be terminated on 15 written days notice. The consulting agreement was in addition to Philip Krause's existing role as non-
executive director. Philip Krause was determined not to be independent on August 28, 2023 and his director fees ceased
from August 1, 2023. On October 1, 2023, Philip Krause's consulting agreement was amended, where he is now
remunerated via a monthly retainer of $20,000 for strategic advisory services and his role as non-executive director and
these fees are included in the table above. The agreement is ongoing, with either party able to terminate on 90 written days
notice. The total aggregate fees paid to Philip Krause through the original consulting agreement for the year ended June 30,
2024 and 2023 was $220,900 and $110,383, respectively.
There were no loans or other related transactions with KMP during the financial year.
d.
Transactions with other related parties
Accounts receivable from revenues, accounts payable to expenses and loans from subsidiaries as at the end of the
fiscal year have been eliminated on consolidation of the Group.
e.
Terms and conditions
All other transactions were made on normal commercial terms and conditions and at market rates, except that
there are no fixed terms for the repayment of loans between the parties.
Outstanding balances are unsecured and are repayable in cash.
17. Share-based payments
The Company has adopted an Employee Share Option Plan (“ESOP”) to foster an ownership culture within the
Company and to motivate senior management and consultants to achieve performance targets. Selected directors,
employees and consultants may be eligible to participate in ESOP at the absolute discretion of the board of directors, and in
the case of directors, upon approval by shareholders.
Table of Contents
207
Grant policy
In accordance with the Company’s policy, options are typically issued in three equal tranches. The length of time
from grant date to expiry date is typically 7 years.
Options issued to employees generally vest based on performance or time conditions, or both. In the year ended
June 30, 2024, senior executives were issued options that vest based on performance and time conditions. These options are
required to satisfy certain pre-specified performance conditions and time-based vesting conditions prior to vesting. Time-
based conditions restrict vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met. For time-based vesting options, the first
tranche typically vests 12 months after grant date, the second tranche 24 months after grant date, and the third tranche 36
months after grant date.
The exercise price is determined by reference to the Company policy. Generally the exercise price is the higher of
the volume weighted average share price of the five ASX trading days up to Board approval of the grant, and the last
closing price of an ordinary share on the ASX at Board approval. In the case of options that have time-based vesting
conditions only, the board of directors adds a 10% premium to the market price. Options with performance based vesting
conditions are issued with no premium. The board of directors’ policy is not to issue options at a discount to the market
price.
The aggregate number of options which may be issued pursuant to the ESOP must not exceed 10,000,000 with
respect to US incentive stock options, and with respect to Australian residents, the limit imposed under the Australian
Securities and Investments Commission Class Order 14/1000.
a.
Reconciliation of outstanding share based payments
35a
08-Jul-20
08-Jul-23
A$2.86
1,500,000
—
(1,500,000)
—
—
36
06-Dec-16
05-Dec-23
A$1.31
533,000
—
(533,000)
—
—
36a
06-Dec-16
05-Dec-23
A$1.19
1,950,730
—
(1,950,730)
—
—
38
16-Sep-17
15-Sep-24
A$1.52
50,000
—
—
50,000
50,000
39
13-Oct-17
12-Oct-24
A$1.92
975,000
—
(160,000)
815,000
815,000
39a
13-Oct-17
12-Oct-24
A$1.74
902,425
—
—
902,425
902,425
40
24-Nov-17
23-Nov-24
A$1.39
750,000
—
—
750,000
750,000
40a
24-Nov-17
23-Nov-24
A$1.26
750,000
—
—
750,000
—
41
18-Jun-18
17-Jun-25
A$1.50
200,000
—
—
200,000
200,000
42
11-Jul-18
10-Jul-25
A$1.54
200,000
—
—
200,000
200,000
43
18-Jul-18
17-Jul-25
A$1.85
3,133,332
—
(135,000)
2,998,332
2,998,332
43b
18-Jul-18
17-Jul-25
A$1.85
350,000
—
—
350,000
350,000
45
30-Nov-18
29-Nov-25
A$1.31
590,000
—
—
590,000
590,000
46
19-Jan-19
18-Jan-26
A$1.43
3,333
—
—
3,333
3,333
47
19-Jan-19
18-Jan-26
A$1.43
150,000
—
—
150,000
150,000
48
04-Apr-19
03-Apr-26
A$1.46
300,000
—
—
300,000
300,000
49
20-Jul-19
19-Jul-26
A$1.60
3,018,669
—
(310,000)
2,708,669
2,708,669
49a
20-Jul-19
19-Jul-26
A$1.45
2,833,332
—
—
2,833,332
1,883,332
49b
20-Jul-19
19-Jul-26
A$1.45
1,346,667
—
—
1,346,667
673,334
49c
20-Jul-19
19-Jul-26
A$1.45
538,667
—
—
538,667
538,667
50
20-Jul-19
19-Jul-26
A$1.45
700,000
—
—
700,000
175,000
54
25-Nov-19
24-Nov-26
A$1.96
20,000
—
—
20,000
20,000
55
29-May-19
28-May-26
A$1.46
350,000
—
—
350,000
300,000
56
18-Nov-19
17-Nov-26
A$1.81
200,000
—
—
200,000
200,000
57
25-Nov-19
24-Nov-26
A$1.78
100,000
—
—
100,000
100,000
58
25-Nov-19
24-Nov-26
A$1.96
150,000
—
—
150,000
150,000
59
24-Jan-20
23-Jan-27
A$3.36
10,000
—
—
10,000
10,000
63
18-May-20
17-May-27
A$4.00
1,200,000
—
—
1,200,000
1,200,000
Series
Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
Table of Contents
208
63a
18-May-20
17-May-27
A$3.63
1,200,000
—
—
1,200,000
500,000
64
16-Jul-20
15-Jul-27
A$3.73
3,253,333
—
(213,333)
3,040,000
3,040,000
64a
16-Jul-20
15-Jul-27
A$3.39
1,735,000
—
—
1,735,000
478,334
64c
16-Jul-20
15-Jul-27
A$3.39
350,000
—
—
350,000
116,666
64d
16-Jul-20
15-Jul-27
A$3.39
300,000
—
—
300,000
200,000
64e
16-Jul-20
15-Jul-27
A$3.39
1,200,000
—
—
1,200,000
720,000
66
11-Sep-20
10-Sep-27
A$4.76
200,000
—
—
200,000
100,000
68
20-Nov-20
19-Nov-27
A$3.58
200,000
—
—
200,000
200,000
69
20-Nov-20
19-Nov-27
A$3.58
100,000
—
—
100,000
100,000
71
17-Feb-21
16-Feb-28
A$2.65
250,000
—
—
250,000
250,000
72
15-Apr-21
14-Apr-28
A$2.26
200,000
—
—
200,000
200,000
74
08-Sep-21
07-Sep-28
A$1.93
3,186,333
—
(143,335)
2,929,666
1,942,003
74
08-Sep-21
07-Sep-28
A$1.93
(113,332) *
74a
08-Sep-21
07-Sep-28
A$1.75
3,850,000
—
—
3,850,000
1,653,334
74b
08-Sep-21
07-Sep-28
A$1.75
1,550,000
—
—
1,550,000
620,000
75
23-Dec-21
22-Dec-28
A$1.40
200,000
—
—
200,000
200,000
76
17-Oct-22
16-Oct-29
A$1.01
1,250,000
—
—
1,250,000
416,667
77
23-May-22
22-May-29
A$0.99
200,000
—
—
200,000
133,334
78
24-Aug-22
23-Aug-29
A$0.83
200,000
—
—
200,000
66,667
79
17-Oct-22
16-Oct-29
A$1.11
5,754,500
—
(30,000)
5,054,500
1,668,167
79
17-Oct-22
16-Oct-29
A$1.11
(670,000) *
79a
17-Oct-22
16-Oct-29
A$1.01
4,350,000
—
—
4,350,000
635,000
79b
17-Oct-22
16-Oct-29
A$1.11
225,000
—
—
225,000
75,000
79c
17-Oct-22
16-Oct-29
A$1.01
3,225,000
—
—
3,225,000
—
79d
17-Oct-22
16-Oct-29
A$1.01
1,200,000
—
—
1,200,000
390,000
80
08-Aug-22
07-Aug-29
A$0.91
100,000
—
—
100,000
100,000
81
11-Dec-20
10-Dec-27
A$4.58
100,000
—
—
100,000
100,000
82
21-Nov-22
20-Nov-29
A$1.10
100,000
—
—
100,000
33,334
83
30-Mar-23
29-Mar-30
A$1.01
150,000
—
(105,000) *
45,000
15,000
84
30-Mar-23
29-Mar-30
A$0.92
—
600,000
—
—
600,000
100,000
85
12-Oct-23
11-Oct-30
A$0.36
—
2,493,835
—
—
2,493,835
831,279
86
12-Oct-23
11-Oct-30
A$0.36
—
1,853,889
—
—
1,853,889
617,965
87
16-Oct-23
15-Oct-30
A$0.39
—
5,459,500
—
(25,000) *
5,434,500
—
87a
16-Oct-23
15-Oct-30
A$0.35
—
1,995,000
—
—
1,995,000
—
87b
16-Oct-23
15-Oct-30
A$0.35
—
3,160,000
—
—
3,160,000
—
87c
16-Oct-23
15-Oct-30
A$0.35
—
2,730,000
—
—
2,730,000
—
88
16-Oct-23
15-Oct-30
A$0.35
—
873,393
—
—
873,393
291,131
89
24-Oct-23
23-Oct-30
A$0.37
—
985,000
—
—
985,000
—
90
28-Feb-24
28-May-24
A$0.01
—
1,072,363
(1,072,363)
—
—
—
92
16-Oct-23
15-Oct-30
A$0.35
—
300,000
—
—
300,000
—
93
30-May-24
29-May-31
A$1.23
—
220,000
—
—
220,000
—
94
30-May-24
29-May-31
A$1.23
—
200,000
—
—
200,000
—
June 30, 2024
57,434,321
21,942,980
(1,072,363)
(5,888,730)
72,416,208
31,061,973
Weighted average share purchase price
A$1.85
A$0.38
A$0.01
A$1.79
A$1.43
A$1.98
Series
Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
(1)
The dates presented in the grant date column represent the date on which board approval was obtained. For
valuation dates per IFRS 2, refer to Note 17(c).
Table of Contents
209
34
27-Apr-16
06-Mar-23
A$2.80
1,678,979
—
—
(1,678,979)
—
—
34b
31-Oct-16
06-Mar-23
A$2.80
200,000
—
—
(200,000)
—
—
35a
08-Jul-20
08-Jul-23
A$2.86
1,500,000
—
—
—
1,500,000
1,500,000
36
06-Dec-16
05-Dec-23
A$1.31
533,000
—
—
—
533,000
533,000
36a
06-Dec-16
05-Dec-23
A$1.19
1,950,730
—
—
—
1,950,730
1,809,064
38
16-Sep-17
15-Sep-24
A$1.54
50,000
—
—
—
50,000
50,000
38a
16-Sep-17
15-Sep-24
A$1.40
150,000
—
—
(150,000)
—
—
39
13-Oct-17
12-Oct-24
A$1.94
975,000
—
—
—
975,000
975,000
39a
13-Oct-17
12-Oct-24
A$1.76
902,425
—
—
—
902,425
902,425
40
24-Nov-17
23-Nov-24
A$1.41
750,000
—
—
—
750,000
750,000
40a
24-Nov-17
23-Nov-24
A$1.28
750,000
—
—
—
750,000
—
41
18-Jun-18
17-Jun-25
A$1.52
200,000
—
—
—
200,000
200,000
42
11-Jul-18
10-Jul-25
A$1.56
200,000
—
—
—
200,000
200,000
43
18-Jul-18
17-Jul-25
A$1.87
3,793,332
—
—
(660,000)
3,133,332
3,133,332
43b
18-Jul-18
17-Jul-25
A$1.87
350,000
—
—
—
350,000
350,000
45
30-Nov-18
29-Nov-25
A$1.33
590,000
—
—
—
590,000
590,000
46
19-Jan-19
18-Jan-26
A$1.45
3,333
—
—
—
3,333
3,333
47
19-Jan-19
18-Jan-26
A$1.45
150,000
—
—
—
150,000
150,000
48
04-Apr-19
03-Apr-26
A$1.48
300,000
—
—
—
300,000
300,000
49
20-Jul-19
19-Jul-26
A$1.62
3,098,670
—
—
(66,667)
3,018,669
3,018,669
49
20-Jul-19
19-Jul-26
A$1.62
—
—
(13,334) *
49a
20-Jul-19
19-Jul-26
A$1.47
3,499,998
—
—
(466,666)
2,833,332
1,883,332
49a
20-Jul-19
19-Jul-26
A$1.47
—
—
(200,000) *
49b
20-Jul-19
19-Jul-26
A$1.47
1,346,667
—
—
—
1,346,667
673,334
49c
20-Jul-19
19-Jul-26
A$1.47
538,667
—
—
—
538,667
538,667
50
20-Jul-19
19-Jul-26
A$1.47
700,000
—
—
—
700,000
175,000
50a
20-Jul-19
19-Jul-26
A$1.47
400,000
—
—
(400,000) *
—
—
52
29-Aug-19
28-Aug-26
A$1.62
400,000
—
—
(400,000)
—
—
53
29-Aug-19
28-Aug-26
A$1.47
800,000
—
—
(800,000)
—
—
54
25-Nov-19
24-Nov-26
A$1.98
153,334
—
—
(133,334)
20,000
20,000
55
29-May-19
28-May-26
A$1.48
350,000
—
—
—
350,000
300,000
56
18-Nov-19
17-Nov-26
A$1.83
200,000
—
—
—
200,000
200,000
57
25-Nov-19
24-Nov-26
A$1.80
100,000
—
—
—
100,000
100,000
58
25-Nov-19
24-Nov-26
A$1.98
450,000
—
—
(200,000)
150,000
150,000
58
25-Nov-19
24-Nov-26
A$1.98
—
—
(100,000) *
59
24-Jan-20
23-Jan-27
A$3.38
10,000
—
—
—
10,000
10,000
63
18-May-20
17-May-27
A$4.02
1,200,000
—
—
—
1,200,000
1,200,000
63a
18-May-20
17-May-27
A$3.65
2,400,000
—
—
(800,000)
1,200,000
200,000
63a
18-May-20
17-May-27
A$3.65
—
—
(400,000) *
64
16-Jul-20
15-Jul-27
A$3.75
3,498,333
—
—
(176,668)
3,253,333
2,160,009
64
16-Jul-20
15-Jul-27
A$3.75
—
—
(68,332) *
64a
16-Jul-20
15-Jul-27
A$3.41
2,700,000
—
—
(965,000) *
1,735,000
478,334
64c
16-Jul-20
15-Jul-27
A$3.41
350,000
—
—
—
350,000
116,666
64d
16-Jul-20
15-Jul-27
A$3.41
300,000
—
—
—
300,000
100,000
64e
16-Jul-20
15-Jul-27
A$3.41
1,200,000
—
—
—
1,200,000
720,000
65
26-Aug-20
25-Aug-27
A$5.76
5,000
—
—
(3,334)
—
—
65
26-Aug-20
25-Aug-27
A$5.76
—
—
(1,666) *
66
11-Sep-20
10-Sep-27
A$4.78
200,000
—
—
—
200,000
100,000
68
20-Nov-20
19-Nov-27
A$3.60
200,000
—
—
—
200,000
133,333
69
20-Nov-20
19-Nov-27
A$3.60
100,000
—
—
—
100,000
100,000
71
17-Feb-21
16-Feb-28
A$2.67
250,000
—
—
—
250,000
166,667
72
15-Apr-21
14-Apr-28
A$2.28
200,000
—
—
—
200,000
133,334
Series Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
Table of Contents
210
74
08-Sep-21
07-Sep-28
A$1.77
3,423,000
—
—
(50,001)
3,186,333
1,051,007
74
08-Sep-21
07-Sep-28
A$1.77
—
—
(186,666) *
74a
08-Sep-21
07-Sep-28
A$1.77
4,150,000
—
—
(300,000) *
3,850,000
923,334
74b
08-Sep-21
07-Sep-28
A$1.77
1,550,000
—
—
—
1,550,000
—
74c
08-Sep-21
07-Sep-28
A$1.77
650,000
—
—
(650,000) *
—
—
75
23-Dec-21
22-Dec-28
A$1.42
200,000
—
—
—
200,000
100,000
76
17-Oct-22
16-Oct-29
A$1.03
—
1,250,000
—
—
1,250,000
—
77
23-May-22
22-May-29
A$1.01
—
200,000
—
—
200,000
66,667
78
24-Aug-22
23-Aug-29
A$0.85
—
200,000
—
—
200,000
—
79
17-Oct-22
16-Oct-29
A$1.13
—
5,844,500
—
(90,000) *
5,754,500
—
79a
17-Oct-22
16-Oct-29
A$1.03
—
4,350,000
—
—
4,350,000
—
79b
17-Oct-22
16-Oct-29
A$1.13
—
225,000
—
—
225,000
—
79c
17-Oct-22
16-Oct-29
A$1.03
—
3,225,000
—
—
3,225,000
—
79d
17-Oct-22
16-Oct-29
A$1.03
—
1,200,000
—
—
1,200,000
—
80
08-Aug-22
07-Aug-29
A$0.93
—
100,000
—
—
100,000
100,000
81
11-Dec-20
10-Dec-27
A$4.60
—
100,000
—
—
100,000
100,000
82
21-Nov-22
20-Nov-29
A$1.12
—
100,000
—
—
100,000
—
83
30-Mar-23
29-Mar-30
A$1.03
—
180,000
—
(30,000) *
150,000
—
June 30, 2023
49,650,468
16,974,500
—
(9,190,647)
57,434,321
26,464,507
Weighted average share purchase price
A$2.21
A$1.08
A$—
A$2.39
A$1.85
A$2.12
Series Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
(1)
The dates presented in the grant date column represent the date on which board approval was obtained. For
valuation dates per IFRS 2, refer to Note 17(c).
32
10-Jul-15
30-Jun-22
US$4.20
1,753,334
—
—
(1,753,334)
—
—
33
26-Aug-15
16-Aug-22
A$4.05
75,000
—
—
(75,000)
—
—
34
27-Apr-16
6-Mar-23
A$2.80
1,858,979
—
—
(180,000)
1,678,979
1,678,979
34b
31-Oct-16
6-Mar-23
A$2.80
200,000
—
—
—
200,000
200,000
35a
8-Jul-20
8-Jul-23
A$2.86
1,500,000
—
—
—
1,500,000
1,500,000
36
6-Dec-16
5-Dec-23
A$1.31
623,000
—
(50,000)
(40,000)
533,000
533,000
36a
6-Dec-16
5-Dec-23
A$1.19
1,950,730
—
—
—
1,950,730
1,809,064
38
16-Sep-17
15-Sep-24
A$1.54
50,000
—
—
—
50,000
50,000
38a
16-Sep-17
15-Sep-24
A$1.40
150,000
—
—
—
150,000
150,000
39
13-Oct-17
12-Oct-24
A$1.94
1,090,000
—
—
(115,000)
975,000
975,000
39a
13-Oct-17
12-Oct-24
A$1.76
902,425
—
—
—
902,425
902,425
40
24-Nov-17
23-Nov-24
A$1.41
750,000
—
—
—
750,000
750,000
40a
24-Nov-17
23-Nov-24
A$1.28
750,000
—
—
—
750,000
—
41
18-Jun-18
17-Jun-25
A$1.52
200,000
—
—
—
200,000
200,000
42
11-Jul-18
10-Jul-25
A$1.56
200,000
—
—
—
200,000
200,000
43
18-Jul-18
17-Jul-25
A$1.87
4,201,666
—
(20,000)
(388,334)
3,793,332
3,793,332
43b
18-Jul-18
17-Jul-25
A$1.87
350,000
—
—
—
350,000
350,000
44
15-Jul-18
14-Jul-25
A$1.72
150,000
—
—
(150,000)
—
—
45
30-Nov-18
29-Nov-25
A$1.33
590,000
—
—
—
590,000
590,000
46
19-Jan-19
18-Jan-26
A$1.45
3,333
—
—
—
3,333
3,333
47
19-Jan-19
18-Jan-26
A$1.45
150,000
—
—
—
150,000
150,000
48
4-Apr-19
3-Apr-26
A$1.48
300,000
—
—
—
300,000
300,000
49
20-Jul-19
19-Jul-26
A$1.62
3,638,671
—
(113,334)
(277,999)
3,098,670
1,940,654
Series
Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
Table of Contents
211
49
20-Jul-19
19-Jul-26
A$1.62
—
(148,668) *
49a
20-Jul-19
19-Jul-26
A$1.47
3,999,998
—
—
(333,334)
3,499,998
1,316,665
49a
20-Jul-19
19-Jul-26
A$1.47
—
(166,666) *
49b
20-Jul-19
19-Jul-26
A$1.47
1,346,667
—
—
—
1,346,667
673,334
49c
20-Jul-19
19-Jul-26
A$1.47
538,667
—
—
—
538,667
359,112
50
20-Jul-19
19-Jul-26
A$1.47
700,000
—
—
—
700,000
—
50a
20-Jul-19
19-Jul-26
A$1.47
400,000
—
—
—
400,000
—
51
29-Aug-19
28-Aug-26
A$1.47
150,000
—
—
(150,000) *
—
—
52
29-Aug-19
28-Aug-26
A$1.62
400,000
—
—
—
400,000
266,666
53
29-Aug-19
28-Aug-26
A$1.47
800,000
—
—
—
800,000
533,334
54
25-Nov-19
24-Nov-26
A$1.98
295,000
—
—
(25,000)
153,334
146,668
54
25-Nov-19
24-Nov-26
A$1.98
—
(116,666) *
55
29-May-19
28-May-26
A$1.48
350,000
—
—
—
350,000
300,000
56
18-Nov-19
17-Nov-26
A$1.83
200,000
—
—
—
200,000
133,332
57
25-Nov-19
24-Nov-26
A$1.80
100,000
—
—
—
100,000
100,000
58
25-Nov-19
24-Nov-26
A$1.98
450,000
—
—
—
450,000
300,000
59
24-Jan-20
23-Jan-27
A$3.38
10,000
—
—
—
10,000
10,000
61
17-Apr-20
16-Apr-27
A$2.51
50,000
—
—
(16,666)
—
—
61
17-Apr-20
16-Apr-27
A$2.51
—
(33,334) *
63
18-May-20
17-May-27
A$4.02
1,200,000
—
—
—
1,200,000
800,000
63a
18-May-20
17-May-27
A$3.65
2,400,000
—
—
—
2,400,000
400,000
64
16-Jul-20
15-Jul-27
A$3.75
4,280,000
—
—
(225,003)
3,498,333
1,201,676
64
16-Jul-20
15-Jul-27
A$3.75
(556,664) *
64a
16-Jul-20
15-Jul-27
A$3.41
3,050,000
—
—
(350,000) *
2,700,000
133,334
64b
16-Jul-20
15-Jul-27
A$3.41
325,000
—
—
(325,000) *
—
—
64c
16-Jul-20
15-Jul-27
A$3.41
350,000
—
—
—
350,000
—
64d
16-Jul-20
15-Jul-27
A$3.41
300,000
—
—
—
300,000
—
64e
16-Jul-20
15-Jul-27
A$3.41
1,200,000
—
—
—
1,200,000
—
65
26-Aug-20
25-Aug-27
A$5.76
5,000
—
—
—
5,000
1,667
66
11-Sep-20
10-Sep-27
A$4.78
200,000
—
—
—
200,000
100,000
67
8-Oct-20
7-Oct-27
A$3.84
200,000
—
—
(66,667)
—
—
67
8-Oct-20
7-Oct-27
A$3.84
—
(133,333) *
68
20-Nov-20
19-Nov-27
A$3.60
200,000
—
—
—
200,000
66,666
69
20-Nov-20
19-Nov-27
A$3.60
100,000
—
—
—
100,000
100,000
71
17-Feb-21
16-Feb-28
A$2.67
250,000
—
—
—
250,000
—
72
15-Apr-21
14-Apr-28
A$2.28
—
200,000
—
—
200,000
66,667
73
30-Jun-21
30-Aug-21
A$—
45,746
—
(45,746)
—
—
—
74
08-Sep-21
07-Sep-28
A$1.77
—
3,973,000
—
(550,000) *
3,423,000
—
74a
08-Sep-21
07-Sep-28
A$1.77
—
4,150,000
—
—
4,150,000
—
74b
08-Sep-21
07-Sep-28
A$1.77
—
1,550,000
—
—
1,550,000
—
74c
08-Sep-21
07-Sep-28
A$1.77
—
650,000
—
—
650,000
—
75
23-Dec-21
22-Dec-28
A$1.42
—
200,000
—
—
200,000
—
June 30, 2022
45,333,216
10,723,000
(229,080)
(6,176,668)
49,650,468
23,084,908
Weighted average share purchase price
A$2.42
A$1.77
A$1.25
A$2.99
A$2.21
A$2.06
Series
Grant Date(1)
Expiry Date
Exercise
Price
Opening
Balance
Granted No.
(during the
year)
Exercised
No. (during
the year)
Lapsed/
Forfeited*
No. (during
the year)
Closing
Balance
Vested and
exercisable
No (end of
year)
(1)
The dates presented in the grant date column represent the date on which board approval was obtained. For
valuation dates per IFRS 2, refer to Note 17(c).
The weighted average share price at the date of exercise of options exercised during the years ended June 30,
2024, 2023 and 2022 were A$0.93, N/A and A$1.82 respectively. The weighted average remaining contractual life of share
options outstanding as of June 30, 2024, 2023 and 2022 were 4.24 years, 4.13 years and 4.16 years, respectively.
Table of Contents
212
b.
Existing share-based payment arrangements
General terms and conditions attached to share based payments
Share options pursuant to the employee share option plan are generally granted in three equal tranches. The length
of time from grant date to expiry date is typically seven years. Vesting occurs based on achievement of performance
conditions and/or progressively over the life of the option with the first tranche vesting one year from grant date, the
second tranche two years from grant date, and the third tranche three years from grant date. On cessation of employment
the Company’s board of directors determines if a leaver is a bad leaver or not. If a participant is deemed a bad leaver, all
rights, entitlements and interests in any unexercised options held by the participant will be forfeited and will lapse
immediately. If a leaver is not a bad leaver they may retain vested options, however, they must be exercised within 60 days
of cessation of employment (or within a longer period if so determined by the Company’s board of directors), after which
time they will lapse. Unvested options will normally be forfeited and lapse.
This policy applies to all issues shown in the above table with the exception of the following:
35a
Additional incentive rights granted pursuant to the Amendment Deed of the Equity Facility
Agreement with Kentgrove Capital, dated July 30, 2019, had fully vested on the agreement date and
will expire thirty six months after the date of the issue of the incentive right.
36a
Options were granted in two or three equal tranches and will vest on the date that the option holder
has direct involvement (to the reasonable satisfaction of the Company’s board of directors) in the
Company achieving certain confidential commercial objectives.
49a, 49b, 50, 50a,
53, 64b, 64c, 64d,
64e, 71, 74a, 74b,
74c, 79c, 84, 87a,
89, 94
Options were granted in two or three equal tranches and are required to satisfy certain pre-specified
performance conditions and time-based vesting conditions prior to vesting. Time-based conditions
restrict vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met.
38a, 40a, 57 & 66
Options were granted in one tranche and will vest on the date that the option holder has direct
involvement (to the reasonable satisfaction of the Company’s board of directors) in the Company
achieving certain confidential commercial objectives.
39a
Options were granted in one or two equal tranches and will vest on the date that the option holder
has direct involvement (to the reasonable satisfaction of the Company’s board of directors) in the
Company achieving certain confidential commercial objectives.
51 & 75
Options were granted in two equal tranches and will vest on the date that the option holder has
direct involvement (to the reasonable satisfaction of the Company’s board of directors) in the
Company achieving certain confidential commercial objectives.
55
Options were granted in five tranches and will vest on the date that the option holder has direct
involvement (to the reasonable satisfaction of the Company’s board of directors) in the Company
achieving certain confidential commercial objectives.
63a
Options were granted in three or eight tranches and will vest on the date that the option holder has
direct involvement (to the reasonable satisfaction of the Company’s board of directors) in the
Company achieving certain confidential commercial objectives. Time-based conditions restrict
vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met.
64a
Options were granted in one, two, three or five tranches and will vest on the date that the option
holder has direct involvement (to the reasonable satisfaction of the Company’s board of directors)
in the Company achieving certain confidential commercial objectives. Time-based conditions
restrict vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met.
69, 73, 80, 81 & 90
Options were granted in one tranche and vested on the date on which board approval was obtained
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213
79a, 79d
Options were granted in two, three, four or five tranches and will vest on the date that the option
holder has direct involvement (to the reasonable satisfaction of the Company's board of directors) in
the Company achieving certain confidential commercial objectives. Time-based conditions restrict
vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met.
85, 86, 88, 93
Options were granted in three equal tranches and are required to satisfy time-based vesting
conditions. Time-based conditions restrict vesting to a maximum of one third at 6 months, two
thirds at 9 months and full grant at 12 months.
87c
Options were granted in three tranches and will vest on the date that the option holder has direct
involvement (to the reasonable satisfaction of the Company’s board of directors) in the Company
achieving certain confidential commercial objectives. Time-based conditions restrict vesting to a
maximum of one third at 12 months, two thirds at 24 months and full grant at 36 months, but only if
the pre-specified performance conditions have been met.
87b
Options were granted in four or five tranches and will vest on the date that the option holder has
direct involvement (to the reasonable satisfaction of the Company’s board of directors) in the
Company achieving certain confidential commercial objectives. Time-based conditions restrict
vesting to a maximum of one third at 12 months, two thirds at 24 months and full grant at 36
months, but only if the pre-specified performance conditions have been met.
92
Options were granted in four tranches and will vest on the date that the option holder has direct
involvement (to the reasonable satisfaction of the Company’s board of directors) in the Company
achieving certain confidential commercial objectives. Time-based conditions restrict vesting to a
maximum of one third at 12 months, two thirds at 24 months and full grant at 36 months, but only if
the pre-specified performance conditions have been met.
Modifications to share-based payment arrangements
During the year ended June 30, 2024, as a result of a 1 for 4 pro-rata accelerated non-renounceable entitlement
offer to existing eligible shareholders in December 2023, the exercise price of all outstanding options at the time was
reduced by A$0.02 per option subject to the ESOP plan under clause 8.3. There were no further modifications made to
share-based payment arrangements during the years ended June 30, 2024, June 30, 2023, and June 30, 2022.
c.
Fair values of share based payments
The weighted average fair value of share options granted during the years ended June 30, 2024, 2023 and 2022
were A$0.39, A$0.66 and A$0.56, respectively.
The fair value of all shared-based payments made has been calculated using the Black-Scholes model. This model
requires the following inputs:
Share price at acceptance date
The share price used in valuation is the share price at the date at which the entity and the employee agree to a
share-based payment arrangement, being when the entity and the employee have a shared understanding of the terms and
conditions of the arrangement or at shareholder approval date where this approval is required. This price is generally the
volume weighted average share price for the five trading days leading up to the date.
Exercise price
The exercise price is a known value that is contained in the agreements.
Share price volatility
The model requires the Company’s share price volatility to be measured. In estimating the expected volatility of
the underlying shares our objective is to approximate the expectations that would be reflected in a current market or
negotiated exchange price for the option. Historical volatility data is considered in determining expected future volatility.
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214
Life of the option
The life is generally the time period from grant date through to expiry. Certain assumptions have been made
regarding “early exercise” i.e. options exercised ahead of the expiry date. These assumptions have been based on historical
trends for option exercises within the Company and take into consideration exercise trends that are also evident as a result
of local taxation laws.
Dividend yield
The Company has yet to pay a dividend so it has been assumed the dividend yield on the shares underlying the
options will be 0%.
Risk free interest rate
This has been sourced from the Reserve Bank of Australia historical interest rate tables for government bonds.
Model inputs
The model inputs for the valuations of options approved and granted during the year ended June 30, 2024 are as
follows:
Series
Valuation
date(1)
Exercise
price per
share
A$
Share price
at
valuation
date
A$
Expected
share
price
volatility
Life(2)
Dividend
yield
Risk-free
interest
rate
84
31-Jul-23
0.92
1.18
64.95%
6.1 yrs
0%
3.84%
85
28-Nov-23
0.36
0.39
69.82%
6.3 yrs
0%
4.21%
86
28-Nov-23
0.36
0.39
69.82%
6.3 yrs
0%
4.21%
87
09-Jan-24
0.39
0.29
70.10%
6.2 yrs
0%
3.79%
87a
03-Jun-24
0.35
1.17
72.84%
5.8 yrs
0%
4.07%
87b
12-Jan-24
0.35
0.29
70.07%
6.1 yrs
0%
3.74%
87c(3)
30-Jun-24
0.35
0.99
72.72%
5.7 yrs
0%
4.08%
88
15-Nov-23
0.35
0.37
69.82%
6.3 yrs
0%
4.23%
89
28-Nov-23
0.37
0.39
69.82%
6.3 yrs
0%
4.21%
90
28-Feb-24
0.01
0.30
69.97%
0.2 yrs
0%
3.80%
92
11-Apr-24
0.35
0.89
72.66%
5.9 yrs
0%
3.90%
93
03-Jun-24
1.23
1.17
72.84%
6.4 yrs
0%
4.07%
94(3)
30-Jun-24
1.23
0.99
72.72%
6.3 yrs
0%
4.08%
(1)
Valuation date is the date at which the entity and the employee agree to a share-based payment arrangement, being
when the entity and the employee have a shared understanding of the terms and conditions of the arrangement.
(2)
Expected life after factoring likely early exercise.
(3)
Fair value estimated at June 30, 2024 as the valuation date under AASB2 has not been met as of June 30, 2024.
The closing share market price of an ordinary share of Mesoblast Limited on the ASX as of June 30, 2024 was
A$0.99.
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215
The model inputs for the valuations of options approved and granted during the year ended June 30, 2023 are as
follows:
Series
Valuation
date(1)
Exercise
price per
share
A$
Share price
at
valuation
date
A$
Expected
share
price
volatility
Life(2)
Dividend
yield
Risk-free
interest
rate
76
23-Nov-22
1.03
0.99
65.37%
6.3 yrs
0%
3.38%
77
23-Nov-22
1.01
0.99
65.37%
5.9 yrs
0%
3.38%
78
23-Nov-22
0.85
0.99
65.37%
6.1 yrs
0%
3.38%
79
09-Dec-22
1.13
1.04
65.43%
6.2 yrs
0%
3.11%
79a
21-Jun-23
1.03
1.18
65.04%
5.8 yrs
0%
3.88%
79b
16-Mar-23
1.13
0.97
65.29%
6.0 yrs
0%
2.99%
79c
23-Nov-22
1.03
0.99
65.37%
6.3 yrs
0%
3.38%
79d
07-Jul-23
1.01
1.15
64.98%
5.7 yrs
0%
4.19%
80
18-Nov-22
0.93
0.95
65.35%
6.1 yrs
0%
3.35%
81
18-Nov-22
4.60
0.95
65.35%
4.6 yrs
0%
3.35%
82
30-Dec-22
1.12
0.89
65.31%
6.3 yrs
0%
3.70%
83
06-Apr-23
1.03
0.97
65.17%
6.4 yrs
0%
2.90%
(1)
Valuation date is the date at which the entity and the employee agree to a share-based payment arrangement, being
when the entity and the employee have a shared understanding of the terms and conditions of the arrangement.
(2)
Expected life after factoring likely early exercise.
The closing share market price of an ordinary share of Mesoblast Limited on the ASX as of June 30, 2023 was
A$1.14.
The model inputs for the valuations of options approved and granted during the year ended June 30, 2022 are as
follows:
Series
Valuation
date(1)
Exercise
price per
share
A$
Share price
at
valuation
date
A$
Expected
share
price
volatility
Life(2)
Dividend
yield
Risk-free
interest
rate
72
05-May-21
2.28
1.94
66.62%
6.3 yrs
0%
0.69%
74
10-Nov-21
1.95
1.69
65.85%
6.2 yrs
0%
1.31%
74a
07-Nov-22
1.77
0.93
65.41%
5.3 yrs
0%
3.55%
74b
07-Nov-22
1.77
0.93
65.41%
5.3 yrs
0%
3.55%
74c
15-Feb-22
1.77
1.16
65.89%
5.9 yrs
0%
1.91%
75
17-Mar-22
1.42
1.21
65.98%
6.1 yrs
0%
2.18%
(1)
Valuation date is the date at which the entity and the employee agree to a share-based payment arrangement, being
when the entity and the employee have a shared understanding of the terms and conditions of the arrangement.
(2)
Expected life after factoring likely early exercise.
The closing share market price of an ordinary share of Mesoblast Limited on the ASX as of June 30, 2022 was
A$0.61.
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216
18. Remuneration of auditors
During the year the following fees were paid or payable for services provided by the auditor of the parent entity,
its related practices and non-related audit firms:
Year Ended June 30,
(in U.S. dollars)
2024
2023
2022
a. PricewaterhouseCoopers Australia
Audit and other assurance services
Audit and review of financial reports
623,605
669,603
745,021
Other audit services(1)
33,180
180,339
67,238
Total remuneration of PricewaterhouseCoopers Australia
656,785
849,942
812,259
b. Network firms of PricewaterhouseCoopers Australia
Audit and other assurance services
Audit and review of financial reports
65,722
144,864
133,309
Total remuneration of Network firms of PricewaterhouseCoopers
Australia
65,722
144,864
133,309
Total auditors' remuneration(2)
722,507
994,806
945,568
(1)
Other audit services relates to services performed in connection with the filing of registration statements on the
Form F-3.
(2)
All services provided are considered audit fees for the purpose of SEC classification.
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217
19. Losses per share
Years Ended June 30,
2024
2023
2022
(Losses) per share
(in cents)
(a) Basic (losses) per share
From continuing operations attributable to the ordinary equity holders of
the company
(8.91)
(10.53)
(13.38)
Total basic (losses) per share attributable to the ordinary equity holders of
the company
(8.91)
(10.53)
(13.38)
(b) Diluted (losses) per share
From continuing operations attributable to the ordinary equity holders of
the company
(8.91)
(10.53)
(13.38)
Total basic (losses) per share attributable to the ordinary equity holders of
the company
(8.91)
(10.53)
(13.38)
(c) Reconciliation of (losses) used in calculating (losses) per share
(in U.S. dollars, in thousands)
Basic (losses) per share
(Losses) attributable to the ordinary equity holders of the company used in
calculating basic (losses) per share:
From continuing operations
(87,956)
(81,889)
(91,347)
Diluted (losses) per share
(Losses) from continuing operations attributable to the ordinary equity
holders of the company:
Used in calculating basic (losses) per share
(87,956)
(81,889)
(91,347)
(Losses) attributable to the ordinary equity holders of the company used in
calculating diluted losses per share
(87,956)
(81,889)
(91,347)
2024
Number
2023
Number
2022
Number
Weighted average number of ordinary shares used as the denominator in
calculating basic losses per share
986,702,919
777,719,091
682,861,425
Weighted average number of ordinary shares and potential ordinary shares
used in calculating diluted losses per share
986,702,919
777,719,091
682,861,425
Options granted to employees and warrants (see Note 17) are considered to be potential ordinary shares. These
securities have been excluded from the determination of basic losses per shares in the years ended June 30, 2024, 2023 and
2022. Shares that may be paid as contingent consideration have also been excluded from basic losses per share. They have
also been excluded from the calculation of diluted losses per share because they are anti-dilutive for the years ended
June 30, 2024, 2023 and 2022.
The calculations for the years ended June 30, 2023 and 2022 have been adjusted to reflect the bonus element in the
entitlement offer to existing eligible shareholders which occurred during December 2023.
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218
20. Parent entity financial information
a.
Summary financial information
The parent entity financial information disclosure is an Australian Disclosure Requirement as required by
Corporations Regulations 2001. The individual financial statements for the parent entity show the following aggregate
amounts:
As of June 30,
(in U.S. dollars, in thousands)
2024
2023
Balance Sheet
Current Assets
37,166
28,850
Total Assets
958,323
890,120
Current Liabilities
30,709
11,941
Total Liabilities
33,358
15,282
Shareholders' Equity
Issued Capital
1,310,813
1,249,123
Reserves
Foreign Currency Translation Reserve
(261,745)
(261,377)
Share Options Reserve
91,940
86,274
Warrant Reserve
12,969
12,969
(Accumulated losses)/retained earnings
(229,012)
(212,165)
924,965
874,824
Loss for the period
(16,847)
(18,848)
Total comprehensive loss for the period
(16,847)
(18,848)
b.
Contingent liabilities of the parent entity
(i)
Central Adelaide Local Health Network Incorporated (“CALHNI”) (formerly Medvet)
Mesoblast Limited acquired certain intellectual property relating to our MPCs, or Medvet IP, pursuant to an
Intellectual Property Assignment Deed, or IP Deed, with Medvet Science Pty Ltd, or Medvet. Medvet’s rights under the IP
Deed were transferred to Central Adelaide Local Health Network Incorporated, or CALHNI, in November 2011. In
connection with its use of the Medvet IP, on completion of certain milestones Mesoblast Limited will be obligated to pay
CALHNI, as successor in interest to Medvet, (i) certain aggregated milestone payments of up to $2.2 million and single-
digit royalties on net sales of products covered by the Medvet IP, for cardiac muscle and blood vessel applications and
bone and cartilage regeneration and repair applications, subject to minimum annual royalties beginning in the first year of
commercial sale of those products and (ii) single-digit royalties on net sales of the specified products for applications
outside the specified fields.
21. Segment information
Operating segments are identified on the basis of whether the allocation of resources and/or the assessment of
performance of a particular component of the Company’s activities are regularly reviewed by the Company’s chief
operating decision maker as a separate operating segment. By these criteria, the activities of the Company are considered to
be one segment being the development of cell technology platform for commercialization, and the segmental analysis is the
same as the analysis for the Company as a whole. The chief operating decision maker (Chief Executive Officer) reviews
the consolidated income statement, consolidated balance sheet, and statement of cash flows regularly to make decisions
about the Company’s resources and to assess overall performance.
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219
22. Legal proceedings
A class action proceeding in the Federal Court of Australia was served on the Company in May 2022 by the law
firm William Roberts Lawyers on behalf of persons who, between February 22, 2018, and December 17, 2020, acquired an
interest in Mesoblast shares, American Depository Receipts, and/or related equity swap arrangements. In June 2022, the
firm Phi Finney McDonald commenced a second shareholder class action against the Company in the Federal Court of
Australia asserting similar claims arising during the same period. The Australian class actions relate to the Complete
Response Letter released by the FDA in September 2020 in relation to the Company's GvHD product candidate; they also
relate to certain representations made by the Company in relation to our COVID-19 product candidate and the decline in
the market price of the Company's ordinary shares in December 2020. The Australian class actions have been consolidated
into one lawsuit. On August 21, 2024, the Company announced that the class action had been resolved subject to Federal
Court approval and includes no admission of liability. In relation to the settlement of the class action, which was assessed
as an adjusting subsequent event, the Group recognized a provision for litigation settlement as of June 30, 2024 in the
consolidated balance sheet (inclusive of interest and costs), refer to Note 6(d). Given the settlement will be funded entirely
by Mesoblast's insurers, the Group has also recognized an insurance asset within trade and other receivables in the
consolidated balance sheet as of June 30, 2024, refer to Note 5(b)(i).
23. Summary of material accounting policies
This note provides the principal accounting policies adopted in the preparation of these consolidated financial
statements as set out below. These policies have been consistently applied to all the years presented, unless otherwise
stated. The financial statements are for the consolidated entity consisting of Mesoblast Limited and its subsidiaries.
a.
Change in accounting policies
There were no new accounting policies adopted by the Group that materially impacted the Group in the year
ended June 30, 2024.
b.
Principles of consolidation
i.
Subsidiaries
The consolidated financial statements incorporate the assets and liabilities of all subsidiaries of Mesoblast Limited
(“Company” or “Parent Entity”) as of June 30, 2024 and the results of all subsidiaries for the year then ended. Mesoblast
Limited and its subsidiaries together are referred to in this financial report as the Group or the consolidated entity.
Subsidiaries are all entities (including structured entities) over which the Group has control. The Group controls
an entity when the Group is exposed to, or has rights to, variable returns from its involvement with the entity and has the
ability to affect those returns through its power to direct the activities of the entity.
Subsidiaries are fully consolidated from the date on which control is transferred to the Group. They are
deconsolidated from the date that control ceases.
The acquisition method of accounting is used to account for business combinations by the Group.
Intercompany transactions, balances and unrealized gains on transactions between Group companies are
eliminated. Unrealized losses are also eliminated unless the transaction provides evidence of the impairment of the asset
transferred. Accounting policies of subsidiaries have been changed where necessary to ensure consistency with the policies
adopted by the Group.
ii.
Employee share trust
The Group has formed a trust to administer the Group’s employee share scheme. This trust is consolidated, as the
substance of the relationship is that the trust is controlled by the Group.
c.
Segment reporting
The Group operates in one segment as set out in Note 21.
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220
d.
Foreign currency translation
(i)
Functional and presentation currency
Items included in the financial statements of each of the Group’s entities are measured using the currency of the
primary economic environment in which the entity operates (the “functional currency”). The functional currency of
Mesoblast Limited is A$. The consolidated financial statements are presented in US$, which is the Group’s presentation
currency.
(ii)
Translations and balances
Foreign currency transactions are translated into the functional currency using the exchange rates prevailing at the
dates of the transactions. Foreign exchange gains and losses resulting from the settlement of such transactions and from the
transaction at period end exchange rates of monetary assets and liabilities denominated in foreign currencies are recognized
in net loss, except when they are deferred in equity as qualifying cash flow hedges and qualifying net investment hedges or
attributable to part of the net investment in a foreign operation.
Non-monetary items that are measured at fair value in a foreign currency are translated using the exchange rates at
the date when the fair value was determined. Translation differences on assets and liabilities carried at fair value are
reported as part of the fair value gain or loss. For example, translation differences on non-monetary assets and liabilities
such as equities held at fair value through profit or loss are recognized in net loss as part of the fair value gain or loss and
translation differences on non-monetary assets such as equities classified as financial assets at fair value are recognized in
other comprehensive income.
(iii)
Group companies
The results and financial position of all the Group entities (none of which has the currency of a hyperinflationary
economy) that have a functional currency different from the presentation currency are translated into the presentation
currency as follows:
•
assets and liabilities for the consolidated balance sheets presented are translated at the closing rate at the
date of that consolidated balance sheets;
•
income and expenses for the statements of comprehensive income are translated at average exchange
rates (unless this is not a reasonable approximation of the cumulative effect of the rates prevailing on the
transaction dates, in which case income and expenses are translated at the dates of the transactions); and
•
all resulting exchange differences are recognized in other comprehensive income.
(iv)
Other
On consolidation, exchange differences arising from the translation of any net investment in foreign entities, and
of borrowings and other financial instruments designated as hedges of such investments, are recognized in other
comprehensive income. When a foreign operation is sold or any borrowings forming part of the net investment are repaid,
the associated exchange differences are reclassified to net loss, as part of the gain or loss on sale.
Goodwill and fair value adjustments arising on the acquisition of a foreign entity are treated as assets and
liabilities of the foreign entities and translated at the closing rate.
e.
Revenue recognition
Revenue from contracts with customers is measured and recognized in accordance with the five step model
prescribed by IFRS 15 Revenue from Contracts with Customers.
First, contracts with customers within the scope of IFRS 15 are identified. Distinct promises within the contract
are identified as performance obligations. The transaction price of the contract is measured based on the amount of
consideration the Group expect to be entitled from the customer in exchange for goods or services. Factors such as
requirements around variable consideration, significant financing components, noncash consideration, or amounts payable
to customers also determine the transaction price. The transaction is then allocated to separate performance obligations in
the contract based on relative standalone selling prices. Revenue is recognized when, or as, performance obligations are
satisfied, which is when control of the promised good or service is transferred to the customer.
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221
Revenues from contracts with customers comprise commercialization and milestone revenue.
(i)
Commercialization and milestone revenue
Commercialization and milestone revenue generally includes non-refundable upfront license and collaboration
fees; milestone payments, the receipt of which is dependent upon the achievement of certain clinical, regulatory or
commercial milestones; as well as royalties on product sales of licensed products, if and when such product sales occur;
and revenue from the supply of products. Payment is generally due on standard terms of 30 to 60 days.
Amounts received prior to satisfying the revenue recognition criteria are recorded as deferred revenue or deferred
consideration in our consolidated balance sheets, depending on the nature of arrangement. Amounts expected to be
recognized as revenue within the 12 months following the consolidated balance sheet date are classified within current
liabilities. Amounts not expected to be recognized as revenue within the 12 months following the consolidated balance
sheet date are classified within non-current liabilities.
Milestone revenue
The Group applies the five-step method under the standard to measure and recognize milestone revenue.
The receipt of milestone payments is often contingent on meeting certain clinical, regulatory or commercial
targets, and is therefore considered variable consideration. The Group estimate the transaction price of the contingent
milestone using the most likely amount method. The Group include in the transaction price some or all of the amount of the
contingent milestone only to the extent that it is highly probable that a significant reversal in the amount of cumulative
revenue recognized will not occur when the uncertainty associated with the contingent milestone is subsequently resolved.
Milestone payments that are not within the control of the Company, such as regulatory approvals, are not considered highly
probable of being achieved until those approvals are received. Any changes in the transaction price are allocated to all
performance obligations in the contract unless the variable consideration relates only to one or more, but not all, of the
performance obligations.
When consideration for milestones is a sale-based or usage-based royalty that arises from licenses of IP (such as
cumulative net sales targets), revenue is recognized at the later of when (or as) the subsequent sale or usage occurs, or
when the performance obligation to which some or all of the royalty has been allocated has been satisfied (or partially
satisfied).
Licenses of intellectual property
When licenses of IP are distinct from other goods or services promised in the contract, the Group recognize the
transaction price allocated to the license as revenue upon transfer of control of the license to the customer. The Group
evaluate all other promised goods or services in the license agreement to determine if they are distinct. If they are not
distinct, they are combined with other promised goods or services to create a bundle of promised goods or services that is
distinct.
The transaction price allocated to the license performance obligation is recognized based on the nature of the
license arrangement. The transaction price is recognized over time if the nature of the license is a “right to access” license.
This is when the Group undertake activities that significantly affect the IP to which the customer has rights, the rights
granted by the license directly expose the customer to any positive or negative effects of our activities, and those activities
do not result in the transfer of a good or service to the customer as those activities occur. When licenses do not meet the
criteria to be a right to access license, the license is a “right to use” license, and the transaction price is recognized at the
point in time when the customer obtains control over the license.
Sales-based or usage-based royalties
Licenses of IP can include royalties that are based on the customer’s usage of the IP or sale of products that
contain the IP. The Group apply the specific exception to the general requirements of variable consideration and the
constraint on variable consideration for sales-based or usage-based royalties promised in a license of IP. The exception
requires such revenue to be recognized at the later of when (or as) the subsequent sale or usage occurs and the performance
obligation to which some or all of the sales-based or usage-based royalty has been allocated has been satisfied (or partially
satisfied).
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Grünenthal arrangement
In September 2019, the Group entered into a strategic partnership with Grünenthal for the development and
commercialization in Europe and Latin America of the Group’s allogeneic mesenchymal precursor cell (“MPC”) product,
MPC-06-ID, receiving exclusive rights to the Phase 3 allogeneic product candidate for the treatment of low back pain due
to degenerative disc disease.
The Group received a non-refundable upfront payment of $15.0 million in October 2019, on signing of the
contract with Grünenthal. The Group received a milestone payment in December 2019 of $2.5 million in relation to
meeting a milestone event as part of the strategic partnership with Grünenthal.
In June 2022, the Group amended the strategic partnership with Grünenthal and is eligible to receive payments up
to US$112.5 million prior to product launch, inclusive of US$17.5 million already received, if certain clinical and
regulatory milestones are satisfied and reimbursement targets are achieved. Cumulative milestone payments could reach
US$1 billion depending on the final outcome of Phase 3 studies and patient adoption. The Group will also receive tiered
double-digit royalties on product sales as per the original agreement.
The $2.5 million milestone payment received in December 2019 from Grünenthal was considered deferred
consideration as of June 30, 2024, as the performance obligation has not been met. There was no milestone revenue
recognized in relation to this strategic partnership with Grünenthal in the years ended June 30, 2024, 2023 and 2022.
Tasly arrangement
In July 2018, the Group entered into a strategic alliance with Tasly Pharmaceutical Group (“Tasly”) for the
development, manufacture and commercialization in China of the Group’s allogeneic MPC products, MPC-150-IM and
MPC-25-IC. Tasly received all exclusive rights for MPC-150-IM and MPC-25-IC in China and Tasly will fund all
development, manufacturing and commercialization activities in China.
The Group received a $20.0 million upfront technology access fee from Tasly upon closing of this strategic
alliance in October 2018. The Group recognized $10.0 million from this $20.0 million up-front technology access fee at
closing in October 2018 and the remaining $10.0 million was recognized in revenue in February 2020. The Group is also
entitled to receive $25.0 million on product regulatory approvals in China, double-digit escalating royalties on net product
sales and up to six escalating milestone payments when the product candidates reach certain sales thresholds in China.
For the years ended June 30, 2024, 2023 and 2022, no revenue was recognized in relation to this strategic alliance
with Tasly.
TiGenix arrangement
In December 2017, the Group entered into a patent license agreement with TiGenix NV (“TiGenix”), now a
wholly owned subsidiary of Takeda Pharmaceutical Company Limited (“Takeda”), which granted Takeda exclusive access
to certain of our patents to support global commercialization of the adipose-derived MSC product, Alofisel® a registered
trademark of TiGenix, previously known as Cx601, for the local treatment of fistulae. The agreement includes the right for
Takeda to grant sub-licenses to affiliates and third parties.
As part of the agreement, the Group received $5.9 million (€5.0 million) before withholding tax as a non-refundable
up-front payment, a further payment of $5.9 million (€5.0 million) before withholding tax 12 months after the patent
license agreement date, and a further $1.2 million (€1.0 million) product regulatory milestone payment in the year ended
June 30, 2022. The Group is entitled to further payments up to €9.0 million when Takeda reaches certain product
regulatory milestones. Additionally, the Group receive single digit royalties on net sales of Alofisel®.
In the years ended June 30, 2024, 2023 and 2022, the Group earned $0.4 million, $0.4 million and $0.3 million,
respectively, of royalty income on sales of Alofisel® by our licensee Takeda.
No milestone revenue was recognized in the years ended June 30, 2024 and 2023 in relation to the Group's patent
license agreement with Takeda entered into in December 2017. In the year ended June 30, 2022, $1.2 million milestone
revenue was recognized with regards to the €1.0 million regulatory milestone payment receivable from Takeda given
Takeda received approval to manufacture and market Alofisel® (darvadstrocel) in Japan for the treatment of complex
perianal fistulas in patients with non-active or mildly active luminal Crohn’s Disease.
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JCR arrangement
In October 2013, the Group acquired all of the culture-expanded, MSC-based assets from Osiris. These assets
included assumption of a collaboration agreement with JCR, a research and development oriented pharmaceutical company
in Japan. Revenue recognized under this agreement is limited to the amount of cash received or for which the Group is
entitled, as JCR has the right to terminate the agreement at any time.
Under the JCR Agreement, JCR is responsible for all development and manufacturing costs including sales and
marketing expenses. Under the JCR Agreement, JCR has the right to develop our MSCs in two fields for the Japanese
market: exclusive in conjunction with the treatment of hematological malignancies by the use of hematopoietic stem cells
derived from peripheral blood, cord blood or bone marrow, or the First JCR Field; and non-exclusive for developing assays
that use liver cells for non-clinical drug screening and evaluation, or the Second JCR Field. With respect to the First JCR
Field, the Group are entitled to payments when JCR reaches certain commercial milestones and to escalating double-digit
royalties in the twenties. These royalties are subject to possible renegotiation downward in the event of competition from
non-infringing products in Japan. With respect to the Second JCR Field, the Group are entitled to an approximately 50%
profit share. The Group expanded our partnership with JCR in Japan for two new indications: for wound healing in patients
with Epidermolysis Bullosa (“EB”) in October 2018, and for neonatal hypoxic ischemic encephalopathy (“HIE”), a
condition suffered by newborns who lack sufficient blood supply and oxygen to the brain, in June 2019. The Group will
receive royalties on TEMCELL product sales for licensed indications, if and when JCR begins selling TEMCELL for such
indications in Japan. The Group applies the sales-based and usage-based royalty exception for licenses of intellectual
property and therefore recognizes royalty revenue at the later of when the subsequent sale or usage occurs and the
associated performance obligation has been satisfied.
In the years ended June 30, 2024, 2023 and 2022, the Group recognized $5.5 million, $7.1 million, and
$8.7 million in commercialization revenue, respectively, relating to royalty income earned on sales of TEMCELL in Japan
by our licensee JCR. These amounts were recorded in revenue as there are no further performance obligations required in
regards to these items.
(ii)
Interest income
Interest income is accrued on a time basis by reference to the principal outstanding and at the effective interest
rate applicable, which is the rate that exactly discounts estimated future cash receipts through the expected life of the
financial asset to that asset’s net carrying amount.
(iii)
Research and development tax incentive
Tax incentives comprise payments from the Australian government’s Innovation Australia Research and
Development Tax Incentive program for research and development activities conducted in relation to our qualifying
research that meets the regulatory criteria. The research and development tax incentive credit is available for the Group's
research and development activities in Australia. Eligible companies can receive a refundable tax offset for a percentage of
their research and development spending.
The research and development tax incentive credit is available for the Group’s research and development activities
in Australia as well as research and development activities outside of Australia to the extent such non-Australian based
activities relate to intellectual property owned by our Australian resident entities do not exceed half the expenses for the
relevant activities and are approved by the Australian government. Eligible companies can receive a refundable tax offset
for a percentage of their research and development spending. In October 2020, the Australian Government introduced new
legislation for the tax offset applicable to eligible companies for income tax years commencing from July 1, 2021. Per the
new legislation, the tax offset for companies with an aggregated turnover of A$20.0 million or more is the Company’s
corporate tax rate plus a rate between 8.5% and 16.5% depending on the proportion of research and development
expenditures in relation to total expenditures. For companies with an aggregated turnover below A$20.0 million, the
refundable research and development tax offset is 18.5% above the Company's tax rate.
The Group recorded $0.9 million and $3.5 million and $nil in research and development tax incentive income for
the years ended June 30, 2024, 2023 and 2022, respectively. Within the $3.5 million recognized in the year ended June 30,
2023, $1.2 million pertained to the year ended June 30, 2023, $1.1 million pertained to the year ended June 30, 2022 and
$1.2 million pertained to the year ended June 30, 2021. Management concluded it's assessment of qualifying activities
during the year ended June 30, 2023 and recognized the relevant income for the years ended June 30, 2023, 2022 and 2021.
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No income was recognized in the years ended June 30, 2022 and 2021 as management were yet to confirm if the Group's
research and development activities were eligible under the incentive scheme.
f.
Inventories
Inventories are included in the financial statements at the lower of cost (including raw materials, direct labour,
other direct costs and related production overheads) and net realizable value. Pre-launch inventory is held as an asset when
there is a high probability of regulatory approval for the product in accordance with IAS 2 Inventories. Before that point, a
provision is made against the carrying value to its recoverable amount in accordance with IAS 2 Inventories; the provision
is then reversed at the point when a high probability of regulatory approval is determined.
The Group considers a number of factors in determining the probability of the product candidate realizing future
economic benefit, including the product candidate’s current status in the regulatory approval process, results from the
related pivotal clinical trial, results from meetings with relevant regulatory agencies prior to the filing of regulatory
applications, the market need, historical experience, as well as potential impediments to the approval process such as
product safety or efficacy, commercialization and market trends.
When a provision is made against the carrying value of pre-launch inventory the costs are recognized within
Manufacturing Commercialization expenses. When the high probability threshold is met, the provision will be reversed
through Manufacturing Commercialization expenses.
All inventory costs are currently fully provided for and are recognized within Manufacturing Commercialization
expenses. Where it is determined that the pre-launch inventory will be used within a clinical trial, that amount is removed
from the cost of pre-launch inventory. There is no impact on the consolidated income statement as the carrying value has
been previously fully provided for.
As of June 30, 2024 and June 30, 2023, there was $19.2 million and $22.4 million of pre-launch inventory
recognized on the consolidated balance sheet that was fully provided for, respectively. The future commercial use of the
remaining pre-launch inventory recognized on the consolidated balance sheet will be dependent on future discussions with
the FDA and remains fully provided for.
For the year ended June 30, 2024, $3.2 million of pre-launch inventory was used for chemistry and manufacturing
controls ("CMC") and research and development activities. For the years ended June 30, 2023 and 2022, $3.5 million and
$7.0 million of pre-launch inventory costs have been recognized within Manufacturing Commercialization expenses in
relation to the provision against the carrying value of pre-launch inventory, respectively.
g.
Research and development undertaken internally
The Group currently does not have any capitalized development costs. Research expenditure is recognized as an
expense as incurred. Costs incurred on development projects, which consist of preclinical and clinical trials, manufacturing
development, and general research, are recognized as intangible assets when it is probable that the project will, after
considering its commercial and technical feasibility, be completed and generate future economic benefits and its costs can
be measured reliably.
The expenditure capitalized comprises all directly attributable costs, including costs of materials, services, direct
labor and an appropriate proportion of overheads. Other development costs that do not meet these criteria are expensed as
incurred. Development costs previously recognized as expenses, are not recognized as an asset in a subsequent period and
will remain expensed. Capitalized development costs are recorded as intangible assets and amortized from the point at
which the asset is ready for use on a straight-line basis over its useful life.
h.
Income tax
The income tax expense or benefit for the period is the tax payable on the current period’s taxable income based
on the applicable income tax rate for each jurisdiction adjusted by changes in deferred tax assets and liabilities attributable
to temporary differences and to unused tax losses.
The current income tax charge is calculated on the basis of the tax laws enacted or substantively enacted at the end
of the reporting period in the countries where the Group’s subsidiaries and associates operate and generate taxable income.
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Management periodically evaluates positions taken in tax returns with respect to situations in which applicable tax
regulation is subject to interpretation. It establishes provisions where appropriate on the basis of amounts expected to be
paid to the tax authorities.
Deferred income tax is provided in full, using the liability method, on temporary differences arising between the
tax bases of assets and liabilities and their carrying amounts in the consolidated financial statements. However, the deferred
income tax is not accounted for if it arises from initial recognition of an asset or liability in a transaction other than a
business combination or lease transaction that at the time of the transaction affects neither accounting, nor taxable profit or
loss. Deferred income tax is determined using tax rates (and laws) that have been enacted or substantially enacted by the
end of the reporting period and are expected to apply when the related deferred income tax asset is realized or the deferred
income tax liability is settled.
Deferred tax assets are recognized for deductible temporary differences and unused tax losses only if it is probable
that future taxable amounts will be available to utilize those temporary differences and losses. Deferred tax assets are only
recognized to the extent that there are sufficient deferred tax liabilities unwinding.
Deferred tax liabilities and assets are not recognized for temporary differences between the carrying amount and
tax bases of investments in controlled entities where the parent entity is able to control the timing of the reversal of the
temporary differences and it is probable that the differences will not reverse in the foreseeable future.
Deferred tax assets and liabilities are offset when there is a legally enforceable right to offset current tax assets
and liabilities and when the deferred tax balances relate to the same taxation authority. Current tax assets and tax liabilities
are offset where the entity has a legally enforceable right to offset and intends either to settle on a net basis, or to realize the
asset and settle the liability simultaneously.
Current and deferred tax is recognized in net loss, except to the extent that it relates to items recognized in other
comprehensive income or directly in equity. In this case, the tax is also recognized in other comprehensive income or
directly in equity, respectively.
Pillar Two legislation has been enacted or substantially enacted in certain jurisdictions in which the Group
operates. However, this legislation does not apply to the Group as its consolidated revenue is less than the threshold of
€750 million.
i.
Business combinations
The acquisition method of accounting is used to account for all business combinations, regardless of whether
equity instruments or other assets are acquired. The consideration transferred for the acquisition of a subsidiary comprises
the fair values of the assets transferred, the liabilities incurred and the equity interests issued by the Group. The
consideration transferred also includes the fair value of any asset or liability resulting from a contingent consideration
arrangement and the fair value of any pre-existing equity interest in the subsidiary. Acquisition-related costs are expensed
as incurred. Identifiable assets acquired and liabilities and contingent liabilities assumed in a business combination are,
with limited exceptions, measured initially at their fair values at the acquisition date. On an acquisition-by-acquisition
basis, the Group recognizes any noncontrolling interest in the acquiree either at fair value or at the non-controlling
interest’s proportionate share of the acquiree’s net identifiable assets.
The excess of the consideration transferred and the amount of any non-controlling interest in the acquiree over the
fair value of the net identifiable assets acquired is recorded as goodwill. If those amounts are less than the fair value of the
net identifiable assets of the subsidiary acquired and the measurement of all amounts has been reviewed, the difference is
recognized directly in net loss as a bargain purchase.
Where settlement of any part of cash consideration is deferred, the amounts payable in the future are discounted to
their present value as at the date of exchange. The discount rate used is the entity’s incremental borrowing rate, being the
rate at which a similar borrowing could be obtained from an independent financier under comparable terms and conditions.
Contingent consideration is classified either as equity or a financial liability. Amounts classified as a financial
liability are subsequently remeasured to fair value with changes in fair value recognized in profit or loss.
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j.
Impairment of assets
Goodwill and intangible assets that have an indefinite useful life are not subject to amortization and are tested
annually for impairment or more frequently if events or changes in circumstances indicate that they might be impaired.
Other assets are tested for impairment whenever events or changes in circumstances indicate that the carrying amount may
not be recoverable.
An impairment loss is recognized for the amount by which the asset’s carrying amount exceeds its recoverable
amount. The recoverable amount is the higher of an asset’s fair value less costs to dispose and value in use. For the
purposes of assessing impairment, assets are grouped at the lowest levels for which there are separately identifiable cash
inflows which are largely independent of the cash inflows from other assets or groups of assets (cash-generating units).
Non-financial assets (other than goodwill) that have suffered impairment are reviewed for possible reversal of the
impairment at the end of each reporting period.
Management maintains internal valuations of each asset annually (or more frequently should indicators of
impairment be identified) and valuations from independent experts are requested periodically, within every three year
period. The internal valuations are continually reviewed by management and consideration is given as to whether there are
indicators of impairment which would warrant impairment testing. An external valuation of our assets was carried out by
an independent expert as at March 31, 2023 with the recoverable amount of each asset exceeding its carrying amount.
In August 2023,the FDA issued a CRL to the Group's BLA for remestemcel-L for the treatment of pediatric SR-
aGVHD and the Group considered this to be an impairment indicator that could cause the carrying amount of its intangible
assets to exceed its recoverable amounts. As a result, the Group completed an impairment assessment on its MSC products
and intangible asset and goodwill, which considered the impact of the FDA's CRL. An external valuation was also obtained
for the MSC products for the impairment assessment performed as a result of the receipt of the CRL. No impairment of the
in-process research and development and goodwill was identified.
In July 2024, as discussed in Note 15, the Group resubmitted its BLA for approval of remestemcel-L for the
treatment of pediatric SR-aGVHD, and the FDA accepted the Group's BLA resubmission and set a PDUFA goal date of
January 7, 2025. The outcome from the FDA decision on the Group's BLA resubmission could lead to a change in the
assumptions used within the impairment assessment associated with SR-aGVHD that could cause the carrying amount of
our intangible asset to exceed its recoverable amount.
k.
Cash and cash equivalents
For the purpose of presentation in the statement of cash flows, cash and cash equivalents includes cash on hand,
deposits held at call with financial institutions, other short-term and highly liquid investments with original maturities of
three months or less that are readily convertible to known amounts of cash and which are subject to an insignificant risk of
changes in value.
l.
Trade and other receivables
Trade receivables and other receivables represent the principal amounts due at balance date less, where applicable,
any provision for expected credit losses. The Group uses the simplified approach to measuring expected credit losses,
which uses a lifetime expected credit loss allowance. Debts which are known to be uncollectible are written off in the
consolidated income statement. All trade receivables and other receivables are recognized at the value of the amounts
receivable, as they are due for settlement within 60 days and therefore do not require remeasurement.
m.
Investments and other financial assets
(i)
Classification
The Group classifies its financial assets in the following measurement categories:
•
those to be measured subsequently at fair value (either through OCI or through profit or loss); and
•
those to be measured at amortized cost
The classification depends on the Group’s business model for managing the financial assets and the contractual
terms of the cash flow. For assets measured at fair value, gains and losses will either be recorded in profit or loss or OCI.
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For investments in equity instruments that are not held for trading, this will depend on whether the group has made an
irrevocable election at the time of initial recognition to account for the equity investment at fair value through other
comprehensive income (FVOCI). See Note 5 for details about each type of financial asset.
(ii)
Recognition and derecognition
Regular way purchases and sales of financial assets are recognized on trade-date, the date on which the Group
commits to purchase or sell the asset. Financial assets are derecognized when the rights to receive cash flows from the
financial assets have expired or have been transferred and the Group has transferred substantially all the risks and rewards
of ownership.
(iii)
Measurement
At initial recognition, the Group measures a financial asset at its fair value plus, in the case of a financial asset not
at fair value through profit or loss (FVPL), transaction costs that are directly attributable to the acquisition of the financial
asset. Transaction costs of financial assets carried at FVPL are expensed in profit or loss. Financial assets with embedded
derivatives are considered in their entirety when determining whether their cash flows are solely payment of principal and
interest.
Details on how the fair value of financial instruments is determined are disclosed in Note 5(g).
Equity instruments
The group subsequently measures all equity investments at fair value. Where the Group has elected to present fair
value gains and losses on equity investments in OCI, there is no subsequent reclassification of fair value gains and losses to
profit or loss following the derecognition of the investment. Dividends from such investments continue to be recognized in
profit or loss as other income when the group’s right to receive payments is established.
Changes in the fair value of financial assets at FVPL are recognized in other gains/(losses) in the statement of
profit or loss as applicable. Impairment losses (and reversal of impairment losses) on equity investments measured at
FVOCI are not reported separately from other changes in fair value.
(iv)
Impairment
For trade receivables, the group applies the simplified approach permitted by IFRS 9, which requires expected
lifetime losses to be recognized from initial recognition of the receivables, see Note 5(b) for further details.
n.
Derivatives
Derivatives are initially recognized at fair value on the date a derivative contract is entered into and are
subsequently remeasured to their fair value at the end of each reporting period. As at June 30, 2024 and 2023, the Group
did not have any derivative instruments that qualified for hedge accounting.
Derivatives that do not qualify for hedge accounting
Certain derivative instruments do not qualify for hedge accounting. Changes in the fair value of any derivative
instrument that does not qualify for hedge accounting are recognized immediately in profit or loss and are included in other
income or other expenses.
o.
Property, plant and equipment
Plant and equipment are stated at historical cost less accumulated depreciation and impairment. Cost includes
expenditure that is directly attributable to the acquisition of the item.
Subsequent cost are included in the asset’s carrying amount or recognized as a separate asset, as appropriate, only
when it is probable that future economic benefits associates with the item will flow to the Group and the cost of the item
can be measured reliably. All other repairs and maintenance are charged to profit and loss during the reporting period in
which they are incurred.
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Property, plant and equipment, other than freehold land, are depreciated over their estimated useful lives using the
straight line method (see Note 6(a)).
The assets’ residual values and useful lives are reviewed, and adjusted if appropriate, at the end of each reporting
period.
An asset’s carrying amount is written down immediately to its recoverable amount if the asset’s carrying amount
is greater than its estimated recoverable amount.
Gains and losses on disposal of plant and equipment are taken into account in determining the profit for the year.
p.
Intangible assets
(i)
Goodwill
Goodwill is measured as described in Note 23(i). Goodwill on acquisition of subsidiaries is included in intangible
assets (Note 6(c)). Goodwill is not amortized but it is tested for impairment annually or more frequently if events or
changes in circumstances indicate that it might be impaired, and is carried at cost less accumulated impairment losses.
Gains and losses on the disposal of an entity include the carrying amount of goodwill relating to the entity sold.
Goodwill is tested for impairment in accordance with IAS 36 Impairment of Assets which requires testing be
performed at any time during an annual period, provided the test is performed at the same time every year. The Group tests
for impairment annually in the third quarter of each year. Additionally, assets must be tested for impairment if there is an
indication that an asset may be impaired. The recoverable amounts of our assets and cash-generating units have been
determined based on fair value less costs to sell calculations, which require the use of certain assumptions.
Goodwill is allocated to cash generating units for the purpose of impairment testing. The allocation is made to
those cash generating units or groups of cash generating units that are expected to benefit from the business combination in
which the goodwill arose, identified according to operating segments (Note 21).
(ii)
Acquired licenses to patents
Acquired licenses have a finite useful life and are carried at cost less accumulated amortization and impairment
losses. Each asset is amortized through to the estimated patent expiry date which is reviewed and adjusted as patent
extensions are granted.
Payments made to third parties to acquire licenses to patents, including initial upfront and subsequent milestone
payments are capitalized. For subsequent payments under existing license agreements payments are capitalized if they meet
the definition of an intangible asset. Management reviews the substance of the payment to determine its classification.
Generally, payments made for a verifiable outcome, such as completion of a clinical trial, regulatory approvals and sales
target milestones would be accumulated into the cost of the intangible.
The Group periodically evaluates whether current facts or circumstances indicate that the carrying value of its
acquired intangibles may not be recoverable. If such circumstances are determined to exist, an estimate of the undiscounted
future cash flow of these assets, or appropriate assets grouping is compared to the carrying value to determine whether an
impairment exists. If the asset is determined to be impaired, the loss is measured based on the differences between the
carrying value of the intangible asset and its fair value, which is determined based on the net present value of estimated
future cash flows.
Royalty payments under license and sublicense agreements are expensed.
(iii)
In-process research and development acquired
In-process research and development that has been acquired as part of a business acquisition is considered to be an
indefinite life intangible asset on the basis that it is incomplete and cannot be used in its current form. Indefinite life
intangible assets are not amortized but rather are tested for impairment annually in the third quarter of each year, or
whenever events or circumstances present an indication of impairment.
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In-process research and development will continue to be tested for impairment until the related research and
development efforts are either completed or abandoned. Upon completion of the related research and development efforts,
management determines the remaining useful life of the intangible assets and amortizes them accordingly. In order for
management to determine the remaining useful life of the asset, management would consider the expected flow of future
economic benefits to the entity with reference to the product life cycle, competitive landscape, obsolescence, market
demand, any remaining patent useful life and various other relevant factors. At the time of completion, when the asset
becomes available for use, all costs recognized in in-process research and development that related to the completed asset
are transferred to the intangible asset category, current marketed products, at the asset’s historical cost.
In the case of abandonment, the related research and development efforts are considered impaired and the asset is
fully expensed.
(iv)
Current marketed products
Current marketed products contain products that are currently being marketed. The assets are recognized on our
consolidated balance sheet as a result of business acquisitions or reclassifications from In-process research and
development upon completion. Upon completion, when assets become available for use, assets are reclassified from in-
process research and development to current marketed products at the historical value that they were recognized at within
the in-process research and development category.
Upon reclassification to the current market products category management determines the remaining useful life of
the intangible assets and amortizes them from the date they become available for use. In order for management to
determine the remaining useful life of the asset, management would consider the expected flow of future economic benefits
to the entity with reference to the product life cycle, competitive landscape, obsolescence, market demand, any remaining
patent useful life and any other relevant factors.
Management have chosen to amortize all intangible assets with a finite useful life on a straight-line basis over the
useful life of the asset. Current marketed products are tested for impairment in accordance with IAS 36 Impairment of
Assets which requires testing whenever there is an indication that an asset may be impaired.
q.
Trade and other payables
Payables represent the principal amounts outstanding at balance date plus, where applicable, any accrued interest.
Liabilities for payables and other amounts are carried at cost which approximates fair value of the consideration to be paid
in the future for goods and services received, whether or not billed. The amounts are unsecured and are usually paid within
30 to 60 days of recognition.
r.
Borrowings
Borrowings are initially recognized at fair value, net of transaction costs incurred. Borrowings are subsequently
measured at amortized cost. Any difference between the proceeds (net of transaction costs) and the redemption amount is
recognized in profit or loss over the period of the borrowings using the effective interest method.
Borrowings are removed from the consolidated balance sheet when the obligation specified in the contract is
discharged, cancelled or expired. The difference between the carrying amount of a financial liability that has been
extinguished or transferred to another party and the consideration paid, including any non-cash assets transferred of
liabilities assumed, is recognized in profit or loss as other income or finance costs.
Borrowings are classified as current liabilities unless the Group has an unconditional right to defer settlement of
the liability for at least 12 months after the reporting period
Funds associated with Oaktree Capital Management, L.P. (“Oaktree”)
In November 2021, the Group entered into a five-year senior debt facility provided by funds associated with
Oaktree. The balance of funds drawn down is currently $50.0 million as of June 30, 2024. The facility has a three-year
interest only period, at a fixed rate of 9.75% per annum, after which the principal amortizes 5% per quarter beginning
December 2024 and a final payment is due no later than November 2026. The facility also allows the Group to make
quarterly payments of interest at a rate of 8.0% per annum for the first two years, and the unpaid interest portion (1.75%
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per annum) has been added to the outstanding loan balance and currently accrues further interest at a fixed rate of 9.75%
per annum.
On November 19, 2021, Oaktree were granted warrants to purchase 1,769,669 American Depositary Shares
(“ADSs”) at US$7.26 per ADS, a 15% premium to the 30-day VWAP. The Group determined that an obligation to issue
the warrants arose from the time the debt facility was signed; consequently, a liability for the warrants was recognized in
November 2021. The warrants were legally issued on January 11, 2022 and may be exercised within 7 years of issuance.
On the issuance date of the Oaktree facility and the warrants, the warrants were initially measured at fair value and the
Oaktree borrowing liability measured as the difference between the initial draw down of funds from the Oaktree facility
and the fair value of the warrants. In December 2022, the Group amended the terms of the loan agreement with Oaktree
and in connection with the loan amendment, Oaktree was granted warrants to purchase 455,000 ADSs at $3.70 per ADS, a
15% premium to the 30-day VWAP. The Group determined that an obligation to issue the warrants arose from the time the
first amendment to the loan agreement was signed; consequently, a liability for the warrants was recognized in December
2022. The warrants were legally issued on March 8, 2023 and may be exercised within 7 years of issuance. Refer to Note
5(g)(vi) for more details on warrants issued.
On January 10, 2024, the ratio under Mesoblast's American Depository Receipt ("ADR") program was changed
from 5 ordinary shares representing 1 ADS (5:1 ratio) to a new ratio of 10 ordinary shares representing 1 ADS (10:1 ratio).
As a result of this ratio change and as a result of initiating the pro-rata accelerated non-renounceable rights issue in
December 2023, the number and exercise price for the warrants was adjusted in accordance with the terms of these
warrants. The warrants issued in November 2021 changed from 1,769,669 ADSs at $7.26 per ADS to 884,838 ADSs at
$14.36 per ADS. The warrants issued in December 2022 changed from 455,000 ADSs at $3.70 per ADS to 227,502 ADSs
at $7.24 per ADS.
In the years ended June 30, 2024, 2023 and 2022, respectively, the Group recognized losses of $2.3 million, $1.6
million and a minimal gain in the Consolidated Income Statement as remeasurement of borrowing arrangements within
finance costs in relation to the adjustment of the carrying amount of our financial liability to reflect the revised estimated
future cash flows from our facility. Within the $1.6 million loss recognized in the year ended June 30, 2023, $1.0 million
related to the remeasurement due to additional warrants being issued to Oaktree as a result of the first amendment to the
loan agreement and $0.6 million related to the adjustment of the carrying amount of our financial liability to reflect the
revised estimated future cash flows from our credit facility.
The Group has pledged substantially all of its assets as collateral under the loan facility with Oaktree.
NovaQuest Capital Management, L.L.C.
On June 29, 2018, the Group entered into an eight-year, $40.0 million loan and security agreement with
NovaQuest before drawing the first tranche of $30.0 million of the principal in July 2018. The loan term includes an
interest only period of approximately four years through until July 8, 2022. All interest and principal payments (i.e. the
amortization period) are deferred until the earlier of loan maturity or from after the first commercial sale of remestemcel-L
for the treatment in pediatric patients with SR-aGVHD in the United States and other geographies excluding Asia
("remestemcel-L for pediatric SR-aGVHD"). Principal is repayable in equal quarterly instalments over the amortization
period of the loan and is subject to the payment cap described below. The loan has a fixed interest rate of 15% per annum.
If there are no net sales of remestemcel-L for pediatric SR-aGVHD, the loan is only repayable at maturity. The Group can
elect to prepay all outstanding amounts owing at any time prior to maturity, subject to a prepayment charge.
Following approval and first commercial sales, repayments commence based on a percentage of net sales and are
limited by a payment cap which is equal to the principal due for the next 12 months, plus accumulated unpaid principal and
accrued unpaid interest. During the four-year period commencing July 8, 2022, principal amortizes in equal quarterly
instalments payable only after approval and first commercial sales. If in any quarterly period, 25% of net sales of
remestemcel-L for pediatric SR-aGVHD exceed the annual payment cap, the Group will pay the payment cap and an
additional portion of excess sales which will be used towards the prepayment amount in the event there is an early
prepayment of the loan. If in any quarterly period 25% of net sales of remestemcel-L for pediatric SR-aGVHD is less than
the annual payment cap, then the payment is limited to 25% of net sales of remestemcel-L for pediatric SR-aGVHD. Any
unpaid interest will be added to the principal amounts owing and shall accrue further interest. At maturity date, any unpaid
loan balances are repaid.
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Because of this relationship of net sales and repayments, changes in our estimated net sales may trigger an
adjustment of the carrying amount of the financial liability to reflect the revised estimated cash flows. The carrying amount
is recalculated by computing the present value of the revised estimated future cash flows at the financial instrument’s
original effective interest rate. The adjustment is recognized in the Income Statement as remeasurement of borrowing
arrangements within finance costs in the period the revision is made.
In the years ended June 30, 2024, 2023 and 2022, respectively, the Group recognized a loss of $0.1 million and
gains of $0.9 million and $0.5 million in the Consolidated Income Statement as remeasurement of borrowing arrangements
within finance costs in relation to the adjustment of the carrying amount of the Group's financial liability to reflect the
revised estimated future cash flows as a net result of changes to the key assumptions in development timelines.
The Group recognizes a liability as current based on repayments linked to estimates of sales of remestemcel-L.
However, if sales of remestemcel-L are higher than estimated, actual repayments will exceed this amount, subject to the
annual payment cap described above.
The carrying amount of the loan and security agreement with NovaQuest is subordinated to the Group’s fixed rate
loan with the senior creditor, Oaktree. The Group have pledged a portion of our assets relating to the SR-aGVHD product
candidate as collateral under the loan facility with NovaQuest.
s.
Provisions
Provisions are recognized when the Group has a present legal obligation as a result of a past event, it is probable
that the Group will be required to settle the obligation, and a reliable estimate can be made of the amount of the obligation.
Provisions are measured at the present value of management’s best estimate of the expenditure required to settle
the present obligation at the end of the reporting period. The discount rate used to determine the present value is a pre-tax
rate that reflects current market assessments of the time value of money and the risks specific to the liability. The increase
in the provision due to the passage of time is recognized as interest expense.
Provisions are recorded on acquisition of a subsidiary, to the extent they relate to a subsidiary’s contingent
liabilities, if it relates to a past event, regardless of whether it is probable the amount will be paid.
t.
Employee benefits
A liability is recognized for benefits accruing to employees in respect of wages and salaries, bonuses, annual leave
and long service leave.
Liabilities recognized in respect of employee benefits which are expected to be settled within 12 months after the
end of the period in which the employees render the related services are measured at their nominal values using the
remuneration rates expected to apply at the time of settlement.
Liabilities recognized in respect of employee benefits which are not expected to be settled within 12 months after
the end of the period in which the employees render the related services are measured as the present value of the estimated
future cash outflows to be made by the Group in respect of services provided by employees up to reporting date.
The obligations are presented as current liabilities in the consolidated balance sheet if the entity does not have an
unconditional right to defer settlement for at least twelve months after the reporting period, regardless of when the actual
settlement is expected to occur.
Termination benefits are payable when employment is terminated by the Group before the normal retirement date,
or when an employee accepts voluntary redundancy in exchange for these benefits. The Group recognizes termination
benefits at the earlier of the following dates: when the Group can no longer withdraw the offer of those benefits and when
the entity recognizes costs for a restructuring that is within the scope of IAS 37 and involves the payment of termination
benefits.
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232
u.
Share-based payments
Share-based payments are provided to eligible employees, directors and consultants via the Employee Share
Option Plan (“ESOP”).
Equity-settled share-based payments with employees and others providing similar services are measured at the fair
value of the equity instrument at acceptance date. Fair value is measured using the Black-Scholes model. The expected life
used in the model has been adjusted, based on management’s best estimate, for the effects of non-transferability, exercise
restrictions, and behavioral considerations. It does not make any allowance for the impact of any service and non-market
performance vesting conditions. Further details on how the fair value of equity-settled share-based transactions has been
determined can be found in Note 17.
The fair value determined at the acceptance date of the equity-settled share-based payments is expensed on a
straight-line basis over the vesting period, based on management’s estimate of shares that will eventually vest, with a
corresponding increase in equity. At the end of each period, the entity revises its estimates of the number of shared-based
payments that are expected to vest based on the non-market vesting conditions. It recognizes the impact of the revision to
original estimates, if any, in profit or loss, with a corresponding adjustment to equity.
v.
Leases
Leases are recognized as a right-of-use asset and a corresponding liability at the date at which the leased asset is
available for use by the Group. Assets and liabilities arising from a lease are initially measured on a present value basis.
Lease liabilities include the net present value of the following lease payments:
•
fixed payments (including in-substance fixed payments), less any lease incentives receivable;
•
variable lease payment that are based on an index or a rate;
•
amounts expected to be payable by the lessee under residual value guarantees;
•
the exercise price of a purchase option if the lessee is reasonably certain to exercise that option; and
•
payments of penalties for terminating the lease, if the lease term reflects the lessee exercising that option.
Variable lease payments that are not based on an index or a rate are not included in the initial measurement of the
lease liability and are expensed in the Consolidated Income Statement when incurred. There were no variable lease
payments that were expensed in the Consolidated Income Statement for the years ended June 30, 2024, 2023 and 2022. The
Group remeasures the lease liability and makes a corresponding adjustment to the related right-of-use asset whenever there
is a change to the lease terms or expected payments under the lease, or a modification that is not accounted for as a separate
lease.
For certain contracts that contain lease and non-lease components, the Group accounts for each lease component
within the contract as a lease separately from non-lease components of the contract. The Group identifies a separate lease
component if there is an explicit or implicit identified asset in the contract and if the Group controls use of the identified
asset.
The lease payments are discounted using the interest rate implicit in the lease, if that rate can be determined, or the
Group’s incremental borrowing rate.
Right-of-use assets are measured at cost comprising the following:
•
the amount of the initial measurement of lease liability;
•
any lease payments made at or before the commencement date, less any lease incentives received;
•
any initial direct costs; and
•
restoration costs.
Payments associated with short-term leases with a lease term of 12 months or less, contracts that contain lease and
non-lease components that are cancellable within 12 months and leases of low-value assets are recognized on a straight-line
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233
basis as an expense in profit or loss. Low-value assets comprise IT-equipment, small items of office furniture or low-value
storage costs.
w.
Warrants
Warrants reserve is measured as described in Note 7(b). For details on warrant liability, see Note 5(g)(vi).
x.
Contributed equity
Ordinary shares are classified as equity.
Transaction costs arising on the issue of equity instruments are recognized separately in equity. Transaction costs
are the costs that are incurred directly in connection with the issue of those equity instruments and which would not have
been incurred had those instruments not been issued.
y.
Loss per share
(i)
Basic losses per share
Basic losses per share is calculated by dividing:
•
the loss attributable to equity holders of the Group, excluding any costs of servicing equity other than
ordinary shares;
•
by the weighted average number of ordinary shares outstanding during the fiscal year, adjusted for bonus
elements in ordinary shares issued during the year.
(ii)
Diluted losses per share
Diluted losses per share adjusts the figures used in the determination of basic earnings per share to take into
account
•
the after income tax effect of interest and other financing costs associated with dilutive potential ordinary
shares; and
•
the weighted average number of shares assumed to have been issued for no consideration in relation to
dilutive potential ordinary shares.
z.
Goods and services tax (“GST”)
Revenues, expenses and assets are recognized net of the amount of GST except where the GST incurred on a
purchase of goods and services is not recoverable from the taxation authority, in which case the GST is recognized as part
of the cost of acquisition of the asset or as part of the expense.
Receivables and payables are stated with the amount of GST included. The net amount of GST recoverable from,
or payable to, the taxation authority is included as part of receivables or payables in the Consolidated Balance Sheet.
Cash flows are included in the statement of cash flow on a gross basis. The GST component of cash flows arising
from investing and financing activities, which is recoverable from, or payable to, the taxation authority, are classified as
operating cash flows.
aa.
Rounding of amounts
Our company is of a kind referred to in ASIC Corporations (Rounding in Financial/Directors’ Reports) Instrument
2016/191, issued by the Australian Securities and Investments Commission, relating to the ‘rounding off’ of amounts in the
financial report. Unless mentioned otherwise, amounts within this report have been rounded off in accordance with that
Legislative Instrument to the nearest thousand dollars, or in certain cases, to the nearest dollar.
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234
Additional Australian Financial Reporting Requirements
Consolidated entity disclosure statement
As at June 30, 2024
Name of entity
Type of entity
Trustee,
partner or
participant
in JV
% of
share
capital
Place of
incorporation
Australian
resident or
foreign resident
Foreign
jurisdiction(s) of
foreign residents
Mesoblast Limited
Body corporate
—
—
Australia
Australian
N/A
Mesoblast, Inc.
Body corporate
—
100
United States of
America
Foreign
United States of
America
Mesoblast International
Sàrl (includes
Mesoblast
International Sàrl
Singapore Branch)
Body corporate
—
100
Switzerland
Foreign
Switzerland
Mesoblast Australia Pty
Ltd
Body corporate
Trustee(1)
100
Australia
Australian
N/A
Mesoblast UK Limited
Body corporate
—
100
United Kingdom
Foreign
United Kingdom
BeiCell Ltd
Body corporate
—
100
Cayman Islands
Australian
N/A
Mesoblast Employee
Share Trust(2)
Trust
—
—
N/A
Australian
N/A
Mesoblast Employee
Share Trust(3)
Trust
—
—
N/A
Australia
N/A
(1) Mesoblast Australia Pty Ltd is a trustee of Mesoblast Employee Share Trust established in 2011.
(2) Established in 2011
(3) Established in 2020
Basis of preparation
This consolidated entity disclosure statement ("CEDS") has been prepared in accordance with the Corporations
Act 2001 and includes information for each entity that was part of the consolidated entity as at the end of the financial year
in accordance with AASB 10 Consolidated Financial Statements.
Determination of tax residency
Section 295 (3A)(vi) of the Corporation Act 2001 defines tax residency as having the meaning in the Income Tax
Assessment Act 1997. The determination of tax residency involves judgement as there are different interpretations that
could be adopted, and which could give rise to a different conclusion on residency.
In determining tax residency, the consolidated entity has applied the following interpretations:
•
Australian tax residency
The consolidated entity has applied current legislation and judicial precedent, including having regard to
the Tax Commissioner's public guidance in Tax Ruling TR 2018/5.
•
Foreign tax residency
Where necessary, the consolidated entity has used independent tax advisers in foreign jurisdictions to
assist in its determination of tax residency to ensure applicable foreign tax legislation has been complied
with (see section 295(3A)(vii) of the Corporations Act 2001).
Trusts
Australian tax law generally does not contain corresponding residency tests for trusts and these entities are
typically taxed on a flow-through basis.
Additional disclosures on the tax status of trusts have been provided where relevant.
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235
Directors’ Declaration
In the directors’ opinion:
(a)
the financial statements and Notes set out on pages 164 to 234 are in accordance with the Corporations
Act 2001, including:
(i)
Complying with Accounting Standards, the Corporations Regulations 2001 and other
mandatory professional reporting requirements, and
(ii)
Giving a true and fair view of the consolidated entity’s financial position as at June 30, 2024 and
of its performance for the fiscal year ended on that date, and
(b)
There are reasonable grounds to believe that the Group will be able to pay its debts as and when they
become due and payable, and
(c)
the consolidated entity disclosure statement on page 235 is true and correct.
Note 1 ‘Basis of preparation’ confirms that the financial statements also comply with International Financial
Reporting Standards as issued by the International Accounting Standards Board.
The directors have been given the declarations by the chief executive officer and chief financial officer required
by section 295A of the Corporations Act 2001.
This declaration is made in accordance with a resolution of the directors.
/s/ Jane Bell
/s/ Silviu Itescu
Jane Bell
Silviu Itescu
Chair of Board
Chief Executive Officer
Melbourne, August 29, 2024
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236
PricewaterhouseCoopers, ABN 52 780 433 757
2 Riverside Quay, SOUTHBANK VIC 3006, GPO Box 1331, MELBOURNE VIC 3001
T: 61 3 8603 1000, F: 61 3 8603 1999
Liability limited by a scheme approved under Professional Standards Legislation.
Independent auditor’s report
To the members of Mesoblast Limited
Report on the audit of the financial report
Our opinion
In our opinion:
The accompanying financial report of Mesoblast Limited (the Company) and its controlled entities
(together the Group) is in accordance with the Corporations Act 2001, including:
(a)
giving a true and fair view of the Group's financial position as at 30 June 2024 and of its
financial performance for the year then ended
(b)
complying with Australian Accounting Standards and the Corporations Regulations 2001.
What we have audited
The financial report comprises:
x
the consolidated balance sheet as at 30 June 2024
x
the consolidated income statement for the year then ended.
x
the consolidated statement of comprehensive income for the year then ended.
x
the consolidated statement of changes in equity for the year then ended.
x
the consolidated statement of cash flows for the year then ended.
x
the notes to the consolidated financial statements, including material accounting policy
information and other explanatory information.
x
the consolidated entity disclosure statement as at 30 June 2024
x
the directors’ declaration.
Basis for opinion
We conducted our audit in accordance with Australian Auditing Standards. Our responsibilities under
those standards are further described in the Auditor’s responsibilities for the audit of the financial
report section of our report.
We believe that the audit evidence we have obtained is sufficient and appropriate to provide a basis
for our opinion.
Independence
We are independent of the Group in accordance with the auditor independence requirements of the
Corporations Act 2001 and the ethical requirements of the Accounting Professional & Ethical
Standards Board’s APES 110 Code of Ethics for Professional Accountants (including Independence
Standards) (the Code) that are relevant to our audit of the financial report in Australia. We have also
fulfilled our other ethical responsibilities in accordance with the Code.
237
Material uncertainty related to going concern
We draw attention to Note 1(i) in the financial report, which indicates that the Group had net cash
outflows from operating activities of $48.5 million and the ability of the Group to continue as a going
concern is dependent upon the Group obtaining additional funding from one or more sources to meet
the Group's projected expenditure consistent with its business strategy. These conditions, along with
other matters set forth in Note 1(i), indicate that material uncertainty exists that may cast significant
doubt on the Group's ability to continue as a going concern. Our opinion is not modified in respect to
this matter.
Our audit approach
An audit is designed to provide reasonable assurance about whether the financial report is free from
material misstatement. Misstatements may arise due to fraud or error. They are considered material if
individually or in aggregate, they could reasonably be expected to influence the economic decisions of
users taken on the basis of the financial report.
We tailored the scope of our audit to ensure that we performed enough work to be able to give an
opinion on the financial report as a whole, taking into account the geographic and management
structure of the Group, its accounting processes and controls and the industry in which it operates.
The Group is a biopharmaceutical entity headquartered in Melbourne, Australia. lt is in the process of
developing and commercialising innovative cell-based medicines for inflammatory diseases. The
Group has operations in Australia, the United States and Singapore.
Audit Scope
x
Our audit focused on where the Group made subjective judgements; for example, significant
accounting estimates involving assumptions and inherently uncertain future events.
x
Audit procedures were performed over Australian, United States and Singaporean operations
to enable us to give an opinion over the financial report as a whole.
Key audit matters
Key audit matters are those matters that, in our professional judgement, were of most significance in
our audit of the financial report for the current period. The key audit matters were addressed in the
context of our audit of the financial report as a whole, and in forming our opinion thereon, and we do
not provide a separate opinion on these matters. Further, any commentary on the outcomes of a
particular audit procedure is made in that context. We communicated the key audit matters to the
Audit and Risk Committee.
In addition to the matter described in the Material uncertainty related to going concern section, we
have determined the matters described below to be the key audit matters to be communicated in our
report.
238
Key audit matter
How our audit addressed the key audit matter
Impairment assessment of in-process research
and development intangible assets and goodwill
As described in Note 6(c) to the consolidated financial
statements, the Group’s consolidated in-process
research and development (“IPRD”) intangible assets
balance and consolidated goodwill balance were
$427.8 million and $134.5 million as at 30 June 2024,
respectively.
The Group tests the IPRD intangible assets and
goodwill balances for impairment on an annual basis
or more frequently if events or changes in
circumstances indicate that they might be impaired.
The recoverability of the carrying values of IPRD
intangible assets and goodwill are estimated by the
Group using future cash flow projections and
assumptions related to the outcome of research and
development activities. These significant judgements
and assumptions made by the Group are specific to
the nature of the Group’s activities including
estimates of market populations, product pricings,
launch timings, probabilities of success and discount
rates.
The principal considerations for our determination
that performing procedures relating to the impairment
assessment of IPRD intangible assets and goodwill is
a key audit matter are there were significant
judgements made by the Group in estimating the
recoverable amount of the Group’s IPRD intangible
assets and goodwill. This in turn led to a high degree
of auditor judgement, subjectivity and effort in
performing procedures to evaluate the Group’s cash
flow projections and significant assumptions,
including estimates of market populations, product
pricings, launch timings, probabilities of success and
discount rates applied. In addition, the audit effort
involved the use of professionals with specialised skill
and knowledge to assist in performing these
procedures and evaluating the audit evidence
obtained.
Our audit procedures included, amongst others,
testing the Group’s process used to develop the fair
value estimate, which included:
x
evaluating the appropriateness of the
valuation methodology and discounted cash
flow models used to estimate the
recoverable amount of the Group’s IPRD
intangible assets and goodwill;
x
testing the completeness, accuracy and
relevance of the underlying data used in the
models; and
x
evaluating the appropriateness of significant
assumptions used by the Group, including
estimates of market populations, product
pricings, launch timings, probabilities of
success and discount rates applied.
Evaluating the significant assumptions relating to the
estimates of the recoverable amount of IPRD
intangible assets and goodwill involved evaluating
whether the significant assumptions used by the
Group were appropriate considering consistency with:
x
external market and industry data;
x
the outcome of clinical trials;
x
formal communications from regulatory
authorities;
x
announcements made by the Group; and
x
other comparable estimates of the Group’s
valuation released by securities analysts.
Professionals with specialised skill and knowledge
were used to assist in the evaluation of the Group’s
discount rates assumptions.
239
Key audit matter
How our audit addressed the key audit matter
Fair value measurement of contingent
consideration
As described in Note 5(g) to the consolidated
financial statements, the Group had a balance of
$26.9 million as at 30 June 2024 for contingent
consideration, which the Group determined using an
internal valuation with a discounted cash flow model
requiring the use of inputs classified as level 3 in the
fair value hierarchy. Significant assumptions used by
the Group to value contingent consideration included
probabilities of success and probability of payment.
The principal considerations for our determination
that performing procedures relating to the fair value
measurement of contingent consideration is a key
audit matter are there were significant judgements
made by the Group in estimating the fair value of
contingent consideration. This in turn led to a high
degree of auditor judgement, subjectivity and effort in
performing procedures to evaluate the Group’s cash
flow projections and significant assumptions,
including probabilities of success and probability of
payment.
Our audit procedures included, amongst others,
testing the Group’s process used to develop the fair
value estimate, which included:
x
evaluating the appropriateness of the
valuation methodology and discounted cash
flow model used to estimate the value of
contingent consideration;
x
testing the completeness, accuracy and
relevance of the underlying data used in the
model; and
x
evaluating the appropriateness of significant
assumptions used by the Group, including
probabilities of success and probability of
payment.
Evaluating the significant assumptions relating to the
estimates of the fair value measurement of contingent
consideration involved evaluating whether the
significant assumptions used by the Group were
appropriate considering consistency with:
x
external market and industry data;
x
the outcome of clinical trials;
x
formal communications from regulatory
authorities;
x
announcements made by the Group; and
x
the impairment assessment of IPRD
intangible assets.
Other information
The directors are responsible for the other information. The other information comprises the
information included in the annual report for the year ended 30 June 2024, but does not include the
financial report and our auditor’s report thereon included in Item 18 of the Form 20-F. Prior to the date
of this auditor's report, the other information we obtained included all other sections of the Form 20-F.
We expect the remaining other information to be made available to us after the date of this auditor's
report.
Our opinion on the financial report does not cover the other information and we do not and will not
express an opinion or any form of assurance conclusion thereon through our opinion on the financial
report. We have issued a separate opinion on the remuneration report.
240
In connection with our audit of the financial report, our responsibility is to read the other information
and, in doing so, consider whether the other information is materially inconsistent with the financial
report or our knowledge obtained in the audit, or otherwise appears to be materially misstated.
If, based on the work we have performed on the other information that we obtained prior to the date of
this auditor’s report, we conclude that there is a material misstatement of this other information, we
are required to report that fact. We have nothing to report in this regard.
When we read the other information not yet received, if we conclude that there is a material
misstatement therein, we are required to communicate the matter to the directors and use our
professional judgement to determine the appropriate action to take.
Responsibilities of the directors for the financial report
The directors of the Company are responsible for the preparation of the financial report in accordance
with Australian Accounting Standards and the Corporations Act 2001, including giving a true and fair
view, and for such internal control as the directors determine is necessary to enable the preparation of
the financial report that is free from material misstatement, whether due to fraud or error.
In preparing the financial report, the directors are responsible for assessing the ability of the Group to
continue as a going concern, disclosing, as applicable, matters related to going concern and using the
going concern basis of accounting unless the directors either intend to liquidate the Group or to cease
operations, or have no realistic alternative but to do so.
Auditor’s responsibilities for the audit of the financial report
Our objectives are to obtain reasonable assurance about whether the financial report as a whole is
free from material misstatement, whether due to fraud or error, and to issue an auditor’s report that
includes our opinion. Reasonable assurance is a high level of assurance, but is not a guarantee that
an audit conducted in accordance with the Australian Auditing Standards will always detect a material
misstatement when it exists. Misstatements can arise from fraud or error and are considered material
if, individually or in the aggregate, they could reasonably be expected to influence the economic
decisions of users taken on the basis of the financial report.
A further description of our responsibilities for the audit of the financial report is located at the Auditing
and Assurance Standards Board website at:
https://www.auasb.gov.au/admin/file/content102/c3/ar1_2020.pdf. This description forms part of our
auditor's report.
Report on the remuneration report
Our opinion on the remuneration report
We have audited the remuneration report included in in Item 6 (Directors, Senior Management and
Employees) of the Form 20-F for the year ended 30 June 2024 identified by the title ‘Start of the
Remuneration Report for Australian Disclosure Requirements’ to ‘End of Remuneration Report’.
In our opinion, the remuneration report of Mesoblast Limited for the year ended 30 June 2024
complies with section 300A of the Corporations Act 2001.
241
Responsibilities
The directors of the Company are responsible for the preparation and presentation of the
remuneration report in accordance with section 300A of the Corporations Act 2001. Our responsibility
is to express an opinion on the remuneration report, based on our audit conducted in accordance with
Australian Auditing Standards.
PricewaterhouseCoopers
Jon Roberts
Melbourne
Partner
29 August 2024
242
Item 19. Exhibits
Item
1.1
Constitution of Mesoblast Limited adopted on November 28, 2023
1.2
Certificate of Registration of Mesoblast Limited (incorporated by reference to Exhibit 3.1 to the Company’s
Registration Statement on Form F-1 filed with the SEC on November 2, 2015).
2.1
Description of Securities (incorporated by reference to Exhibit 2.1 to the Company's Annual Report on Form
20-F filed with the SEC on August 31, 2023).
4.1
Form of Amended and Restated Deposit Agreement between Mesoblast Limited and JPMorgan Chase Bank,
N.A., as depositary, and Holders of the American Depositary Receipts (incorporated by reference to Exhibit
4.1 to the Company’s Registration Statement on Form F-1 filed with the SEC on November 2, 2015).
4.2
Form of Amendment No. 1 to the Amended and Restated Deposit Agreement among Mesoblast Limited, JP
Morgan Chase Bank, N. A., as depositary, and all Holders of the American Depositary Receipts.
4.3
Form of American Depositary Receipt evidencing American Depositary Shares (included in Exhibit 4.1).
4.4†
Manufacturing Services Agreement by and between Mesoblast Limited and Lonza Walkersville, Inc. and
Lonza Bioscience Singapore Pte. Ltd., dated September 20, 2011 (incorporated by reference to Exhibit 10.6 to
the Company’s Registration Statement on Form F-1 filed with the SEC on November 2, 2015).
4.5
Purchase Agreement by and between Mesoblast International Sàrl and Osiris Therapeutics, Inc., dated
October 10, 2013 (incorporated by reference to Exhibit 10.7 to the Company’s Registration Statement on
Form F-1 filed with the SEC on November 2, 2015).
4.6
Amendment #1 to Purchase Agreement by and between Mesoblast International Sàrl and Osiris Therapeutics,
Inc., dated December 17, 2014 (incorporated by reference to Exhibit 10.8 to the Company’s Registration
Statement on Form F-1 filed with the SEC on November 2, 2015).
4.7†
License Agreement by and between Osiris Acquisition II, Inc. and JCR Pharmaceuticals Co., Ltd., dated
August 26, 2003 (incorporated by reference to Exhibit 10.9 to the Company’s Registration Statement on Form
F-1 filed with the SEC on November 2, 2015).
4.8†
Amendment 1 to License Agreement by and between Osiris Acquisition II, Inc. and JCR Pharmaceuticals Co.,
Ltd., dated June 27, 2005 (incorporated by reference to Exhibit 10.10 to the Company’s Registration
Statement on Form F-1 filed with the SEC on November 2, 2015).
4.9#
Employment Agreement, dated August 8, 2014, by and between Mesoblast Limited and Silviu Itescu
(incorporated by reference to Exhibit 10.19 to the Company’s Registration Statement on Form F-1 filed with
the SEC on November 2, 2015).
4.10
Amendment to employment agreement, dated September 15, 2023, by and between Mesoblast Limited and
Silviu Itescu.
4.11#
Form of employment agreement between Mesoblast Limited and executive officers (incorporated by reference
to Exhibit 4.9 to the Company's Annual Report on Form 20-F filed with the SEC on August 31, 2023).
4.12
Form of 2012 Deed of Indemnity, Insurance and Access (incorporated by reference to Exhibit 10.23 to the
Company’s Registration Statement on Form F-1 filed with the SEC on November 2, 2015).
4.13
Form of 2014 Deed of Indemnity, Insurance and Access (incorporated by reference to Exhibit 10.24 to the
Company’s Registration Statement on Form F-1 filed with the SEC on November 2, 2015).
4.14†
Patent License and Settlement Agreement with TiGenix S.A.U., dated December 14, 2017 (incorporated by
reference to Exhibit 4.21 to the Company's Annual Report on Form 20-F filed with the SEC on August 31,
2018).
4.15†
Loan and Security Agreement by and between Mesoblast Limited, Mesoblast UK Limited, Mesoblast, Inc.,
Mesoblast International (UK) Limited, Mesoblast International Sàrl and NQP SPV II, L.P., dated June 29,
2018 (incorporated by reference to Exhibit 4.23 to the Company's Annual Report on Form 20-F filed with the
SEC on August 31, 2018).
4.16†
Development and Commercialization Agreement by and between Mesoblast Inc., Mesoblast International Sàrl
and Tasly Pharmaceutical Group Co., Ltd. dated July 17, 2018 (incorporated by reference to Exhibit 4.24 to
the Company's Annual Report on Form 20-F filed with the SEC on August 31, 2018).
4.17✓
Supplementary Agreement for Additional License by and between Mesoblast International Sarl and JCR
Pharmaceuticals Co., Ltd., dated October 12, 2018 (incorporated by reference to Exhibit 4.25 to the
Company’s Annual Report on Form 20-F filed with the SEC on September 9, 2019).
Table of Contents
243
4.18✓
Second Supplementary Agreement for Additional License by and between Mesoblast International Sarl and
JCR Pharmaceuticals Co., Ltd., dated June 5, 2019 (incorporated by reference to Exhibit 4.27 to the
Company’s Annual Report on Form 20-F filed with the SEC on September 9, 2019).
4.19
Employee Share Option Plan (incorporated by reference to Exhibit 99.1 to the Company’s Post-Effective
Amendment to the Registration Statement on Form S-8 (File No. 333- 267663) filed with the SEC on
December 20, 2022).
4.20✓
Development and Commercialization Agreement by and between Mesoblast Limited and Mesoblast
International Sàrl and Grünenthal GmbH, dated September 9, 2019 (incorporated by reference to Exhibit 4.22
to the Company’s Annual Report on Form 20-F filed with the SEC on September 3, 2020).
4.21✓
Manufacturing Services Agreement by and between Lonza Biosciences Singapore Pte. Ltd. and Mesoblast
International Sàrl, dated October 9, 2019 (incorporated by reference to Exhibit 4.23 to the Company’s Annual
Report on Form 20-F filed with the SEC on September 3, 2020).
4.22✓
Amendment to Development and Commercialization Agreement by and between Mesoblast Limited and
Mesoblast International Sàrl and Grünenthal GmbH dated June 30, 2021 (incorporated by reference to Exhibit
4.27 to the Company’s Annual Report on Form 20-F filed with the SEC on August 31, 2021).
4.23
Form of Warrant to purchase Ordinary Shares (incorporated by reference to Exhibit 4.31 to the Company’s
Annual Report on Form 20-F filed with the SEC on August 31, 2021).
4.24✓
Loan Agreement and Guaranty between Mesoblast Limited, Mesoblast UK Limited, Mesoblast, Inc.,
Mesoblast International Sàrl and Oaktree Fund Administration, LLC, dated November 19, 2021 (incorporated
by reference to Exhibit 4.32 to the Company's Annual Report on Form 20-F filed with the SEC on August 31,
2022).
4.25
Form of Warrant, dated January 11, 2022, to purchase American Depositary Shares (incorporated by
reference to Exhibit 4.23 to the Company's Annual Report on Form 20-F filed with the SEC on August 31,
2023).
4.26✓
First Amendment to Loan Agreement and Guaranty between Mesoblast Limited, Mesoblast UK Limited,
Mesoblast, Inc., Mesoblast International Sàrl and Oaktree Fund Administration, LLC, dated December 22,
2022 (incorporated by reference to Exhibit 4.24 to the Company's Annual Report on Form 20-F filed with the
SEC on August 31, 2023).
4.27
Form of Warrant, dated March 7, 2023, to purchase American Depositary Shares (incorporated by reference
to Exhibit 4.25 to the Company's Annual Report on Form 20-F filed with the SEC on August 31, 2023).
4.28✓
Third Amendment to Loan Agreement and Guaranty between Mesoblast Limited, Mesoblast UK Limited,
Mesoblast, Inc., Mesoblast International Sàrl and Oaktree Fund Administration, LLC, dated May 19, 2023
(incorporated by reference to Exhibit 4.26 to the Company's Annual Report on Form 20-F filed with the SEC
on August 31, 2023).
4.29✓
Fifth Amendment to Loan Agreement and Guaranty between Mesoblast Limited, Mesoblast UK Limited,
Mesoblast, Inc., Mesoblast International Sàrl and Oaktree Fund Administration, LLC, dated February 29,
2024.
8.1
List of Significant Subsidiaries of Mesoblast Limited. (incorporated by reference to Exhibit 8.1 to the
Company's Annual Report on Form 20-F filed with the SEC on August 31, 2023).
12.1
Certification of the Chief Executive Officer pursuant to rules 13a-14(a) and 15d-14(a) under the Securities
Exchange Act of 1934, as adopted pursuant to section 302 of the Sarbanes-Oxley Act of 2002.
12.2
Certification of the Chief Financial Officer pursuant to rules 13a-14(a) and 15d-14(a) under the Securities
Exchange Act of 1934, as adopted pursuant to section 302 of the Sarbanes-Oxley Act of 2002.
13.1
Certification of the Chief Executive Officer pursuant to 18 U.S.C. section 1350, as adopted pursuant to
section 906 of the Sarbanes-Oxley Act of 2002
13.2
Certification of the Chief Financial Officer pursuant to 18 U.S.C. section 1350, as adopted pursuant to section
906 of the Sarbanes-Oxley Act of 2002
15.1
Consent of independent registered public accounting firm.
15.2
Share Trading Policy of Mesoblast Limited (incorporated by reference to Exhibit 15.2 to the Company's
Annual Report on Form 20-F filed with the SEC on August 31, 2023).
97.1
Recovery of Erroneously Awarded Incentive Compensation Policy
99.1
Appendix 4E preliminary final report for the twelve months to June 30, 2024.
99.2*
Auditor’s independence declaration, dated August 29, 2024.
101.INS
Inline XBRL Instance Document
Table of Contents
244
101.SCH
Inline XBRL Taxonomy Extension Schema Document
101.CAL
Inline XBRL Taxonomy Extension Calculation Linkbase Document
101.DEF
Inline XBRL Taxonomy Extension Definition Linkbase Document
101.LAB
Inline XBRL Taxonomy Extension Label Linkbase Document
101.PRE
Inline XBRL Taxonomy Extension Presentation Linkbase Document
104
Cover Page Interactive Data File (formatted as inline XBRL and contained in Exhibit 101)
#
Indicates management contract or compensatory plan.
*
Filed herewith.
†
Confidential treatment has been requested for portions of this exhibit. These portions have been omitted and
have been filed separately with the Securities and Exchange Commission.
✓
Certain confidential portions of this exhibit were omitted by means of marking such portions with brackets
(“[***]”) because the identified confidential portions are not material and are the type that the registrant treats
as private or confidential.
Table of Contents
245
SIGNATURES
The registrant hereby certifies that it meets all of the requirements for filing on Form 20-F and that it has duly
caused and authorized the undersigned to sign this annual report on its behalf.
Mesoblast Limited
By:
/s/ Jane Bell
Name:
Jane Bell
Title:
Chair of Board
By:
/s/ Silviu Itescu
Name:
Silviu Itescu
Title:
Chief Executive Officer
Dated: August 29, 2024
Table of Contents
246
SHAREHOLDER INFORMATION
A. Substantial Shareholders
Holders of substantial holdings of ordinary shares in the Company and the numbers of shares in which they and their
associates have a relevant interest as of 27 September 2024 (as disclosed in notices announced on the Australian
Securities Exchange):
Shareholder
Number of ordinary shares held
Gregory George and G to the Fourth Investments, LLC
179,847,742
Professor Silviu Itescu
78,958,928
B. Distribution of Equity Securities and Voting Rights
Distribution of holders of equity securities as of 27 September 2024:
Range
Ordinary shares(1)
Options(2)
Warrants(3)
ADS Warrants(4)
ADS Warrants 2(5)
Number of
holders
% of
Ordinary
shares held
by holders
Number of
holders
% of
Options
held by
holders
Number of
holders
% of
Warrants
held by
holders
Number of
holders
% of ADS
Warrants
held by
holders
Number of
holders
% of ADS
Warrants
2 held by
holders
1 – 1,000
12,662
0.55%
0
0%
0
0%
0
0%
0
0%
1,001 – 5,000
10,943
2.51%
0
0%
0
0%
0
0%
0
0%
5,001 – 10,000
3,671
2.50%
0
0%
3
0.13%
0
0%
2
6.37%
10,001 – 100,000
4,866
12.76%
20
2%
10
2.08%
7
45.04%
7
93.63%
100,001 and over
724
81.68%
70
98%
16
97.79%
3
54.96%
0
0%
Total number of
holders of equity
securities
32,866
–
90
–
29
–
10
–
9
–
(1) There are 6,227 holders of less than a marketable parcel of 445 ordinary shares ($1.125 per share) as of 27 September 2024.
(2) There are 69,436,208 Options on issue as of 27 September 2024.
(3) 15,027,327 Warrants are on issue as of 27 September 2024, including 6,830,602 Warrants issued to G to the Fourth Investments, LLC.
(4) 884,838 ADS Warrants are on issue as of 27 September 2024, including 248,801 ADS Warrants issued to Oaktree LSL Fund Holdings
EURRC S.A.R.L.
(5) 227,502 ADS Warrants 2 are on issue as of 27 September 2024, including 63,970 ADS Warrants 2 issued to Oaktree LSL Fund Holdings
EURRC S.A.R.L.
The voting rights attaching to each class of equity securities are:
i. Ordinary shares
On a show of hands, every member present at a meeting, in person or by proxy, shall have one vote and upon a poll each
share shall have one vote.
ii. Other classes of equity securities
There are no voting rights attaching to Options, Warrants, ADS Warrants or ADS Warrants 2.
MESOBLAST LIMITED 2024 ANNUAL REPORT 247
C. Twenty Largest Holders of Quoted Securities
The names of the 20 largest shareholders in the Company’s one class of quoted equity security as of 27 September 2024
are listed below.
Rank Name
No. of shares held
% of total shares
1
J P Morgan Nominees Australia Pty Limited
372,563,409
32.63
2
HSBC Custody Nominees (Australia) Limited
127,511,937
11.17
3
Citicorp Nominees Pty Limited
73,041,006
6.40
4
Professor Silviu Itescu
67,751,838
5.93
5
UBS Nominees Pty Ltd
14,630,688
1.28
6
Tiga Trading Pty Ltd
10,000,000
0.88
6
Thorney Holdings Pty Ltd
10,000,000
0.88
7
BNP Paribas Noms Pty Ltd
9,515,494
0.83
8
Josaka Investments Pty Ltd
8,821,137
0.77
9
Independent Asset Management Pty Limited
6,715,891
0.59
10
Merrill Lynch (Australia) Nominees Pty Limited
5,684,853
0.50
11
HSBC Custody Nominees (Australia) Limited
5,301,000
0.46
12
BNP Paribas Nominees Pty Ltd
5,011,552
0.44
13
BNP Paribas Nominees Pty Ltd
4,086,170
0.36
14
Mr Gregory John Matthews & Mrs Janine Marie Matthews
3,141,063
0.28
15
National Nominees Limited
2,856,026
0.25
16
Finclear Services Pty Ltd
2,729,106
0.24
17
Citicorp Nominees Pty Limited
2,502,195
0.22
18
Tamit Nominees Pty Ltd
2,380,953
0.21
19
Mann Securities Pty Ltd
2,352,942
0.21
20
Lavya Pty Ltd
2,000,166
0.18
738,597,426
64.69
D. Securities under escrow
There are no current securities under escrow.
E. On-Market Buy-Back
There is no current on-market buy-back of the Company’s ordinary shares.
F. Stock Exchanges
The Company’s ordinary shares are listed on the Australian Securities Exchange and are traded under the symbol ‘MSB’.
The Company’s American Depositary Shares, each representing ten ordinary shares, are listed on the NASDAQ Global
Select Market and are traded under the symbol ‘MESO’.
248 MESOBLAST LIMITED 2024 ANNUAL REPORT
CORPORATE DIRECTORY
Directors
Jane Bell (Chair)
Silviu Itescu
William Burns
Joseph Swedish
Eric Rose
Philip Facchina
Philip Krause
Company Secretaries
Niva Sivakumar
Paul Hughes
Registered Office
Level 38, 55 Collins Street
Melbourne VIC 3000
Australia
Telephone +61 3 9639 6036
Facsimile +61 3 9639 6030
Country of Incorporation
Australia
Listing
Australian Securities Exchange
(ASX Code: MSB)
NASDAQ Global Select Market
(NASDAQ Code: MESO)
Website
www.mesoblast.com
Share Registry
Link Market Services Limited
Level 10, Tower 4
727 Collins Street
Melbourne
Victoria 3008
Australia
Telephone +61 1300 554 474
Facsimile +61 2 9287 0303
www.linkmarketservices.com.au
Auditors
PricewaterhouseCoopers
2 Riverside Quay
Southbank
Victoria 3006
Australia
Telephone +61 3 8603 1000
Facsimile +61 3 8603 1999
MESOBLAST LIMITED 2024 ANNUAL REPORT 249
www.mesoblast.com