As filed with the Securities and Exchange Commission on June 27, 2019
UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
___________________________________________________________
FORM 20-F
___________________________________________________________
☐ REGISTRATION STATEMENT PURSUANT TO SECTION 12(b) OR 12(g) OF THE SECURITIES EXCHANGE ACT OF 1934
OR
ý ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
For the fiscal year ended March 31, 2019
OR
☐ TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
For the transition period from to
OR
☐ 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
Commission file number: 001-38757
___________________________________________________________
Takeda Yakuhin Kogyo Kabushiki Kaisha
(Exact name of registrant as specified in its charter)
___________________________________________________________
Takeda Pharmaceutical Company Limited
(Translation of registrant’s name into English)
___________________________________________________________
Japan
(Jurisdiction of incorporation or organization)
1-1, Nihonbashi-Honcho 2-Chome
Chuo-ku, Tokyo 103-8668, Japan
(Address of principal executive offices)
Costa Saroukos
1-1, Nihonbashi-Honcho 2-Chome
Chuo-ku, Tokyo 103-8668, Japan
Tel: +81 3 3278-2306
Fax: +81 3 3278-2268
(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
American Depositary Shares Representing Common Stock
Common Stock, no par value*
Trading Symbols
TAK
Name of Each Exchange On Which Registered
New York Stock Exchange
* Listed not for trading, but only in connection with the registration of the American Depositary Shares, pursuant to the requirements of the Securities and Exchange Commission.
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.
118,250,000 ADSs outstanding as of March 31, 2019
1,565,005,908 shares of common stock as of March 31, 2019
Indicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act. Yes ☐ No ý
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. Yes ☐ No ý
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. Yes ý 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). Yes ý No ☐
Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, 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
☐
Accelerated filer
☐
Non-accelerated filer ý
Emerging growth company
☐
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. ☐
† The term “new or revised financial accounting standard” refers to any update issued by the Financial Accounting Standards Board to its Accounting Standards Codification after April 5,
2012.
Indicate by check mark which basis of accounting the registrant has used to prepare the financial statements included in this filing:
U.S. GAAP ☐
International Financial Reporting Standards as issued
by the International Accounting Standards Board ý
Other ☐
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 ☐ Item 18
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). Yes ☐ No ý
(APPLICABLE ONLY TO ISSUERS INVOLVED IN BANKRUPTCY PROCEEDINGS DURING THE PAST FIVE YEARS)
1
Indicate by check mark whether the registrant has filed all documents and reports required to be filed by Sections 12, 13 or 15(d) of the Securities Exchange Act of 1934 subsequent to
the distribution of securities under a plan confirmed by a court. Yes ☐ No ☐
2
TABLE OF CONTENTS
Special Note Regarding Forward-Looking Statements
PART I
Item 1. Identity of Directors, Senior Management and Advisers
Item 2. Offer Statistics and Expected Timetable
Item 3. Key Information
3.A Selected financial data
3.B Capitalization and indebtedness
3.C Reason for the offer and proceeds
3.D Risk factors
Item 4. Information on the Company
4.A History and development of the company
4.B Business overview
4.C Organizational structure
4.D Property, plant and equipment
Item 4A. Unresolved Staff Comments
Item 5. Operating and Financial Review and Prospects
5.A Operating results
5.B Liquidity and capital resources
5.C Research and development, patents and licenses
5.D Trend information
5.E Off-balance sheet arrangements
5.F Tabular disclosure of contractual obligations
5.G Safe harbor
Item 6. Directors, Senior Management and Employees
6.A Directors and senior management
6.B Compensation
6.C Board practices
6.D Employees
6.E Share ownership
Item 7. Major Shareholders and Related Party Transactions
7.A Major shareholders
7.B Related party transactions
7.C Interest of experts and counsel
Item 8. Financial Information
8.A Consolidated statements and other financial information
8.B Significant changes
Item 9. The Offer and Listing
9.A Offer and listing details
9.B Plan of distribution
9.C Markets
9.D Selling shareholders
9.E Dilution
9.F Expenses of the issue
Item 10. Additional Information
10.A Share capital
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6
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7
7
7
7
23
23
24
50
50
51
51
51
63
66
66
66
67
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10.B Memorandum and articles of association
10.C Material contracts
10.D Exchange controls
10.E Taxation
10.F Dividends and paying agents
10.G Statement by experts
10.H Documents on display
10.I Subsidiary information
Item 11. Quantitative and Qualitative Disclosures about Market Risk
Item 12. Description of Securities Other Than Equity Securities
12.A Debt securities
12.B Warrants and rights
12.C Other securities
12.D American Depositary Shares
PART II
Item 13. Defaults, Dividend Arrearages and Delinquencies
Item 14. Material Modifications to the Rights of Security Holders and Use of Proceeds
Item 15. Controls and Procedures
Item 16A. Audit Committee Financial Expert
Item 16B. Code of Ethics
Item 16C. Principal Accountant Fees and Services
Item 16D. Exemptions from the Listing Standards for Audit Committees
Item 16E. Purchases of Equity Securities by the Issuer and Affiliated Purchasers
Item 16F. Change in Registrant’s Certifying Accountant
Item 16G. Corporate Governance
Item 16H. Mine Safety Disclosure
PART III
Item 17. Financial Statements
Item 18. Financial Statements
Item 19. Exhibits
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As used in this annual report, references to the “Company,” “Takeda,” “we,” “us” and “our” are to Takeda Pharmaceutical Company Limited and,
except as the context otherwise requires, its consolidated subsidiaries.
In this annual report, we present our audited consolidated financial statements as of March 31, 2018 and 2019 and for the fiscal years ended
March 31, 2017, 2018 and 2019. Our consolidated financial statements are prepared in accordance with International Financial Reporting Standards
as issued by the International Accounting Standards Board (“IFRS”). The term IFRS also includes International Accounting Standards (“IAS”) and
the related interpretations of the committees (Standard Interpretations Committee and International Financial Reporting Interpretations Committee).
As used in this annual report, “yen,” “¥” or "JPY" means the lawful currency of Japan, “U.S. dollar,” “$” or "USD" means the lawful
currency of the United States of America (“U.S.”), “pound sterling” or “£” means the lawful currency of the United Kingdom and “euro,” “€” or
“EUR” means the lawful currency of the member states of the European Monetary Union.
As used in this annual report, “ADS” means an American Depositary Share, representing 0.5 shares of the Company’s common stock, and
“ADR” means an American Depositary Receipt evidencing one or more ADSs. See “Item 12. Description of Securities Other Than Equity Securities—
D. American Depositary Shares.”
As used in this annual report, except as the context otherwise requires, the “Companies Act” means the Companies Act of Japan.
Amounts shown in this annual report have been rounded to the nearest indicated digit unless otherwise specified. In tables and graphs with
rounded figures, sums may not add up due to rounding.
5
Special Note Regarding Forward-Looking Statements
This annual report contains forward-looking statements. These statements appear in a number of places in this annual report and include
statements regarding the intent, belief, or current and future expectations of our management with respect to our business, financial condition and results
of operations. In some cases, you can identify forward-looking statements by terms such as “may,” “will,” “should,” “would,” “expect,” “intend,”
“project,” “plan,” “aim,” “seek,” “target,” “anticipate,” “believe,” “estimate,” “predict,” “potential” or the negative of these terms or other similar
terminology. These statements are not guarantees of future performance and are subject to various risks and uncertainties. Actual results, performance
or achievements, or those of our industry, may differ materially from any future results, performance or achievements expressed or implied by these
forward-looking statements. In addition, these forward-looking statements are necessarily dependent upon assumptions, estimates and data that may be
incorrect or imprecise and involve known and unknown risks and uncertainties. These forward-looking statements involve statements regarding:
•
•
•
•
•
•
•
•
our ability to achieve the expected benefits of our acquisition of Shire plc (including, except as the context otherwise requires, its
consolidated subsidiaries "Shire");
our goals and strategies;
our ability to develop and bring to market new products;
expected changes in our revenue, costs, expenditures, operating income or other components of our results;
expected changes in the pharmaceutical industry or in government policies and regulations relating to it;
developments regarding or the outcome of any litigation or other legal, administrative, regulatory or governmental proceedings;
information regarding competition within our industry; or
the effect of economic, political, legislative or other developments on our business or results of operations.
Forward-looking statements regarding operating income and operating results are particularly subject to a variety of assumptions, some or
all of which may not be realized. Accordingly, the forward-looking statements included in this annual report should not be interpreted as predictions or
representations of future events or circumstances.
Potential risks and uncertainties include those identified and discussed in “Item 3. Key Information—D. Risk Factors,” “Item 5. Operating
and Financial Review and Prospects,” “Item 4. Information on the Company” and elsewhere in this annual report. Given these risks and uncertainties,
undue reliance should not be placed on any forward-looking statements, which speak only as of the date of this annual report. Except as required by
law, we disclaim any obligation to update or review any forward-looking statements contained in this annual report, whether as a result of new information,
future events or otherwise.
Item 1. Identity of Directors, Senior Management and Advisers
A.
Directors and Senior Management.
Not applicable.
B.
Advisers.
Not applicable.
C.
Auditors.
Not applicable.
Item 2. Offer Statistics and Expected Timetable
A.
Offer Statistics.
Not applicable.
B.
Method and Expected Timetable.
Not applicable.
6
Item 3. Key Information
A.
Selected Financial Data.
The following table presents selected financial information as of and for the years ended March 31, 2015, 2016, 2017, 2018 and 2019,
derived from our consolidated financial statements. These financial statements are prepared in accordance with IFRS.
The selected consolidated financial information set forth below should be read in conjunction with Item 5. “Operating and Financial Review
and Prospects” and our consolidated financial statements and notes thereto included in this annual report.
Selected Statements of Operations Data:
Revenue
Operating (loss) profit
Share of profit (loss) of investments accounted for using the equity method
(Loss) profit before tax
Net (loss) profit for the year
Net (loss) profit attributable to owners of the Company
Per share amounts
Basic (losses) earnings
Diluted (losses) earnings
Annual cash dividends
Cash dividends in U.S. dollars(1)
Selected Statements of Financial Position Data:
Cash and cash equivalents
Total assets
Total bonds and loans
Total liabilities
Total equity
Other Data:
For the fiscal year ended March 31,
2015
2016
2017
2018
2019
(billions of yen, except share and per share data and where
designated as U.S. dollar)
¥ 1,777.8
¥ 1,807.4
¥ 1,732.1
¥ 1,770.5
¥ 2,097.2
(129.3)
1.3
(145.4)
(143.0)
(145.8)
130.8
(0.0)
120.5
83.5
80.2
155.9
(1.5)
143.3
115.5
114.9
241.8
(32.2)
217.2
186.7
186.9
205.0
(43.6)
94.9
109.0
109.1
¥ (185.37) ¥ 102.26
¥ 147.15
¥ 239.35
¥ 113.50
(185.37)
180.00
101.71
180.00
146.26
180.00
237.56
180.00
112.86
180.00
$
1.50
$
1.60
$
1.62
$
1.69
$
1.63
¥
652.1
¥
451.4
¥
319.5
¥
294.5
¥
702.1
4,296.2
3,824.1
729.4
2,090.0
2,206.2
768.2
1,812.9
2,011.2
4,346.8
1,144.9
2,397.8
1,949.0
4,106.5
13,872.3
985.7
2,089.1
2,017.4
5,751.0
8,708.7
5,163.6
Number of shares outstanding at end of period (in thousands)
789,924
790,284
790,521
794,688
1,565,006
____________
Note:
(1)
Calculated using the Japanese yen—U.S. dollar exchange rate as of March 31 of each respective year, based on the noon buying rate in New
York City for cable transfers in foreign currencies as certified for customs purposes by the Federal Reserve Bank of New York.
B.
Capitalization and Indebtedness.
Not applicable.
C.
Reasons for the Offer and Use of Proceeds.
Not applicable.
D.
Risk Factors.
Any investment in our common stock or ADSs involves risk. Investors should carefully consider, in light of their own financial circumstances
and investment objectives, the following risks before making an investment decision with respect to our common stock or ADSs. If any of the following
risks actually occurs, it could have a material adverse effect on our business, financial condition, results of operations and future prospects, and the
market value of our common stock or ADSs may be adversely affected.
7
The risks discussed below are those that we believe are material, but these risks and uncertainties may not be the only risks that we face. Additional
risks that are not known to us at this time, or that are currently believed to be not material, could also have a material adverse effect on our business,
financial condition, results of operations, future prospects and the market value of our common stock or ADSs.
Risks Relating to the Shire Acquisition
We may fail to realize the anticipated benefits of the Shire Acquisition and expect to continue to record significant expenses related to it.
On January 8, 2019, we acquired the entire issued and to-be-issued share capital of Shire pursuant to a Scheme of Arrangement under the
laws of Jersey (the “Shire Acquisition”). The success of the Shire Acquisition depends on our ability to realize the anticipated growth opportunities and
synergies leading to cost savings we expect from combining the companies' businesses. We will need to continue to devote significant time and resources
to the reorganization of our personnel structure, enhancement of cost-efficiency and the strengthening of management and operational functions in order
to realize the anticipated synergies of the Shire Acquisition. We expect to incur non-recurring cash costs totaling approximately $3.0 billion in connection
with the integration of Shire in the first three fiscal years following the completion of the Shire Acquisition.
Furthermore, in connection with the Shire Acquisition and the application of our inventory policies to the acquired businesses, we recognized
significant non-cash expenses relating to the unwinding of fair value adjustments to inventory as a component of cost of sales in the fiscal year ended
March 31, 2019 and expect that such expenses will increase in future fiscal years. We also recorded significant intangible assets in connection with the
Shire Acquisition and, as a result, amortization and impairment losses increased significantly in the fiscal year ended March 31, 2019, and are expected
to continue to increase in the fiscal year ending March 31, 2020.
As a result of the non-recurring cash costs in connection with the integration of Shire, the continued expenses relating to the unwinding of
fair value adjustments to inventory, the increase in amortization and impairment losses on certain intangible assets and ongoing financial expenses (such
as interest expenses) related to the Shire Acquisition, we expect to record a net loss in the fiscal year ending March 31, 2020. We expect certain of these
expenses to continue into the fiscal year ending March 31, 2021.
We recorded significant amounts of goodwill in connection with the Shire Acquisition, and, if we are unable to achieve the anticipated
benefits of this acquisition, we could be required to recognize significant impairment losses related to such goodwill and to intangible assets recorded
in connection with the acquisition, potentially up to their full value.
The expected synergies of the Shire Acquisition and the projected cash costs necessary to achieve the synergies may be affected by changes
in the overall economic, political and regulatory environment, including applicable tax regimes and fluctuations in foreign exchange rates, and the
realization of the other risks relating to our business described herein. Furthermore, the integration process may divert management’s attention from
other strategic opportunities and the day-to-day operation of our business. If we are not able to successfully manage the integration process and create
a unified business culture, the anticipated benefits of the acquisition and subsequent integration may not be realized fully or at all or may take longer or
prove more costly to realize than expected.
Although integration activities are underway, we may face significant challenges in integrating the organizations, business cultures, procedures
and operations of Takeda and Shire, including:
•
•
•
•
•
•
•
•
•
integrating personnel, operations and systems, such as research and development, manufacturing, distribution, marketing and
promotional activities and information technology systems, while maintaining focus on selling and promoting existing and newly
acquired or produced products;
inability to realize expected benefits from newly acquired or produced products, including pipeline products under development;
coordinating and integrating geographically dispersed organizations;
changes or conflicts in the standards, controls, procedures and accounting and other policies, as well as business cultures and
compensation structures;
the need to manage, train and integrate Shire’s personnel, who may have limited experience with the respective companies’ business
lines and products, and to retain existing employees, particularly high-skilled or other key employees and senior members of the
management team;
maintaining and growing Shire’s customer base;
incremental tax exposure based on the differences in our corporate structure and Shire’s, including the exposure of each of the legacy
Takeda businesses and the legacy Shire businesses to new tax regimes, particularly, in the case of Shire, to Japanese tax rules;
maintaining business relationships with suppliers, third-party alliance partners and other key counterparties; and
inefficiencies associated with the integration of the operations of the two companies.
Additionally, because we issued a significant number of additional shares of our common stock as part of the consideration for the Shire
Acquisition, a failure to achieve the anticipated benefits of the Shire Acquisition could negatively affect our earnings per share.
8
We are subject to additional risks arising from the acquired businesses of Shire, particularly its plasma-derived and rare disease therapies, and from
the legal, regulatory and tax regimes that Shire operated under.
We have assumed the risks related to Shire’s businesses, which differ from, or will amplify, certain risks we faced prior to the Shire Acquisition.
For example, markets outside Japan, particularly the United States, represent a larger portion of the legacy Shire business than ours, and our overall
exposure to these markets has increased following the completion of the Shire Acquisition. Additionally, the acquired Shire businesses include new
areas for us, such as rare diseases and plasma-derived therapies. Plasma-derived therapies, in particular, present significant challenges relating to the
sourcing and transportation of plasma, and production and distribution of plasma-derived products, all of which are complex and subject to extensive
regulation, in addition to being capital intensive. If we are unable to manage this new business effectively, we may lose market share or customer
confidence, be required to record charges related to idle capacity or impairment on facilities or take other actions which could materially and adversely
affect the plasma-derived therapies business. Moreover, sales for the rare disease portfolio we acquired as part of the Shire Acquisition are particularly
concentrated among small groups of customers, and we may be disproportionately affected by changes in their purchasing patterns, including if we are
unable to appropriately manage this business.
Furthermore, we have become subject to additional legal, regulatory and tax regimes applicable to the acquired businesses of Shire, many
of which are complex and could subject us to additional risks or liabilities. For example, the legacy Shire business is subject to evolving and complex
tax laws in various jurisdictions and Shire routinely obtained advice on tax matters, including the tax treatment of the break fee of $1.635 billion it
received in connection with the terminated offer to acquire Shire made by AbbVie, Inc. in 2014. In this respect, the Irish Revenue issued an assessment
received by Shire on November 28, 2018 for €398 million on the basis that the break fee was a taxable capital gain. Based on continued advice that no
tax liability should arise from the break fee, Shire has appealed this assessment and the appeals process is continuing. However, the appeal may not be
successful and at this time the outcome is unknown. In addition, in connection with its acquisition of Baxalta Incorporated (“Baxalta”) in 2016, Shire
agreed to indemnify Baxter International Inc., its affiliates and each of their respective officers, directors and employees against certain tax-related losses
if the merger of Baxalta and Shire causes the prior spin-off of Baxalta by Baxter and related transactions to fail to qualify as tax-free. Although Shire
received an opinion of tax counsel that the merger will not cause such prior transactions to fail to qualify as tax-free, such opinion is not binding on the
tax authorities and the potential tax indemnification obligations are not limited in amount.
If we are unable to effectively manage these additional risks, our business, results of operations or financial conditions could be materially
and adversely affected.
We have substantial debt, including a significant amount incurred in connection with the Shire Acquisition, which may limit our ability to execute
our business strategy, refinance existing debt or incur new debt, and if we are unable to meet our goals for deleveraging, we could be at a greater
risk of a downgrade of our credit ratings.
Our consolidated bonds and loans were ¥5,751.0 billion as of March 31, 2019, the majority of which was incurred in connection with the
Shire Acquisition or represents indebtedness of Shire now included on our consolidated balance sheet. This significant amount of aggregate debt and
the substantial amount of cash required for payments of interest and principal could adversely affect our liquidity. In particular, if we are unable to realize
the anticipated benefits of the Shire Acquisition, we may not be able to service our indebtedness. We are also required to comply with certain covenants
within various financing arrangements and violations of such covenants may require the acceleration and immediate repayment of the indebtedness,
which may in turn have a material adverse effect on our financial condition. In particular, under the Loan Agreement with Japan Bank for International
Cooperation (“JBIC”) that we entered into in December 2018 (the "JBIC Loan") for an aggregate principal amount of $3.7 billion, our profit before tax
must not be negative for two consecutive years. As discussed above, we expect to continue to record significant expenses related to the Shire Acquisition
and we expect certain of these costs to continue in the fiscal years ending March 31, 2020 and 2021. We may fail to realize the anticipated benefits of
the Shire Acquisition, and expect to continue to record significant expenses related to it. If we record a net loss before tax in both of the fiscal years
ending March 31, 2020 and 2021, and are unable to negotiate a waiver or otherwise prevent the acceleration of amounts due under the JBIC Loan, the
amounts due thereunder and under our other financing arrangements containing cross-default provisions may become immediately due and payable,
thus requiring us to refinance such debt which may result in increased interest costs. Furthermore, we may desire to or be required from time to time to
incur additional borrowings, including in relation to the repayment or refinancing any of the Term Loan Credit Agreement that we entered into on June
8, 2018 (the “Term Loan Credit Agreement”) for an aggregate principal amount of $7.5 billion, the JBIC Loan, or any other indebtedness incurred in
connection with the Shire Acquisition, such as the U.S. dollar and Euro-denominated bonds issued in November 2018 or the subordinated hybrid bonds
issued in June 2019, or Shire’s previously existing indebtedness. Our ability to arrange a re-financing will depend on our financial position and performance,
prevailing market conditions and other factors beyond our control. Moreover, if we decide to refinance indebtedness as it comes due, our overall leverage
may not necessarily decrease.
We aim to decrease our leverage, with a target ratio of net debt to Adjusted EBITDA(1) of 2x or less within three to five years following the
January 2019 completion of the Shire Acquisition and we have begun the process of disposal of certain non-core assets to generate cash in order to
increase the pace of deleveraging. However, we may not be able to meet these goals if we are unable to sufficiently decrease our overall indebtedness,
or if we are unable to achieve sufficient increases in earnings to offset our increased levels of debt. We may also not be successful in selecting non-core
assets for disposal, and disposals may affect our business, financial condition or results of operations adversely, leading to larger-than-expected decreases
in earnings. We may also not be able to dispose of such assets successfully in a manner that allows us to meet our goals or at all.
______________
(1) We define EBITDA as net profit before income tax expenses, depreciation and amortization and net interest expense. We define Adjusted EBITDA as EBITDA further
adjusted to exclude impairment losses, other operating expenses and income (excluding depreciation and amortization), finance expenses and income (excluding net interest
expense), our share of loss from investments accounted for under the equity method and other items that management believes are unrelated to our core operations such
as purchase accounting effects and transaction related costs.
9
If we are unable to decrease our leverage, we may be unable to improve our credit ratings or be subject to ratings downgrades or other
adverse actions by third-party ratings agencies. In May 2018, Moody’s (Japan) K.K. lowered our credit rating to A2 from A1, reflecting its expectations
for our overall levels of leverage in the future, even in the absence of the Shire Acquisition, and in December 2018 Moody’s (Japan) K.K. further lowered
our credit rating to Baa2, reflecting the increase in our ratio of net debt to Adjusted EBITDA after giving effect to the Shire Acquisition. In February
2019, S&P Global Ratings downgraded our ratings to BBB+, also in light of our aggregate debt and earnings profile following the Shire Acquisition. If
we are unable to improve our credit ratings or if our credit ratings are further downgraded, it may negatively influence the terms for the refinancing of
our existing debt or new borrowings on terms that we would consider to be commercially reasonable.
Risks Relating to Our Business
Research and development of pharmaceutical products are expensive and subject to significant uncertainties, and we may be unsuccessful in bringing
commercially successful products to market or recouping development costs.
Our ability to continue to grow our business depends significantly on the success of our research and development activities in identifying,
developing and successfully commercializing new products in a timely and cost-effective manner. To accomplish this, we commit substantial efforts,
funds and other resources to research and development, both in-house and through collaborations with third parties. However, these research and
development programs are expensive and involve intensive preclinical evaluation and clinical trials in connection with a highly complex and lengthy
regulatory approval process. See “—If we fail to comply with government regulations over product development, regulatory approvals and reimbursement
requirements, our business could be adversely affected.” The research and development process for a new pharmaceutical product also requires us to
attract and retain sufficient numbers of highly-skilled employees and can take up to 10 years to 15 years or longer from discovery to commercial launch.
Moreover, even if we successfully develop and bring to market new products, there is only a limited available patent life in which to recoup these
development costs.
During each stage of the approval process and post-approval life cycle of our products, there is a substantial risk that we will encounter
serious obstacles, including the following:
•
•
•
•
•
•
•
•
•
•
•
•
unfavorable results from preclinical testing of a new compound;
difficulty in enrolling patients in clinical trials, or delays or clinical trial holds at clinical trial sites;
delays in completing formulation and other testing and work necessary to support an application for regulatory approval;
adverse reactions to the product candidate or indications of other safety concerns;
insufficient clinical trial data to support the safety or efficacy of the product candidate;
difficulty or delays in obtaining all necessary regulatory approvals in each jurisdiction where we propose to market such products;
failure to bring a product to market prior to a competitor, or to develop a product sufficiently differentiated from a competing product
to achieve significant market share;
difficulty in obtaining reimbursement at satisfactory rates for our approved products from governments and insurers;
difficulty in obtaining regulatory approval for additional indications;
failure to enter into or implement successful alliances for the development and/or commercialization of products;
inability to manufacture sufficient quantities of a product candidate for development or commercialization activities in a timely or
cost-efficient manner; and
the degree of market acceptance of any approved product candidate by the medical community, including physicians, healthcare
professionals and patients, will depend on a number of factors, including relative convenience and ease of administration, the prevalence
and severity of any adverse reactions, availability of alternative treatments, pricing and our sales and marketing strategy.
In addition, to the extent that new regulations raise the costs of obtaining and maintaining product authorizations or limit the economic value
of a new product to its originator, our profitability and growth prospects could be diminished. Development of new and innovative products can also
require the use of emerging platforms and technologies for which regulations either do not yet exist or are under development or modification. This may
lead to greater uncertainty and risk in establishing the necessary data for approvals to conduct clinical trials and/or receiving marketing approvals.
As a result of the foregoing or other factors, we may decide to abandon the development of potential pipeline products in which we have
invested significant resources, even where the product is in the late stages of development. Moreover, there can also be no assurance that we will be
successful in bringing new products to market, marketing them, achieving sufficient acceptance thereof and recouping our investments in their
development. For example, our pipeline compounds may not receive regulatory approval, become commercially successful or achieve satisfactory rates
of reimbursement. Additionally, products approved for use and successfully marketed in one market may be unable to obtain regulatory approval, become
commercially successful or achieve satisfactory rates of reimbursement in other markets. As a result, we may be unable to earn returns on investments
that we originally anticipated or at all, or may be forced to revise our research and development strategy, and our business, financial condition and results
of operations could be materially and adversely affected.
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If we fail to comply with government regulations over product development, regulatory approvals and reimbursement requirements, our business
could be adversely affected.
Obtaining marketing approval for pharmaceutical products is a lengthy, complex and highly regulated process that requires intensive
preclinical and clinical data, and the approval process can vary significantly depending on the regulatory authority. Relevant health authorities may, at
the time of the filing of the application for a marketing authorization, or later during their review, impose requirements that can evolve over time,
including requiring additional clinical trials, and such authorities may delay or refuse to grant approval. Even where we have obtained marketing approval
for a product in one or more major markets, we may need to invest significant time and resources in applying for approval in other markets, and there
is no assurance that we will be able to obtain such approval. In recent years, health authorities have become increasingly focused on product safety and
on the risk/benefit profile of pharmaceutical products, which could lead to more burdensome and costly approval processes and negatively affect our
ability to obtain regulatory approval for products under development. For example, the U.S. Food and Drug Administration (the “FDA”), the European
Medicines Agency (the “EMA”), and the Pharmaceuticals and Medical Devices Agency (the “PMDA”) in Japan have been implementing strict
requirements for approval, particularly in terms of the volume of data needed to demonstrate a product’s efficacy and safety.
Even after regulatory approval is obtained, marketed products are subject to various post-approval requirements, including continual review,
risk evaluations, comparative effectiveness studies and, in some cases, requirements to conduct post-approval clinical trials to gather additional safety
and other data. Regulatory authorities in many countries have worked to enhance post-approval monitoring in recent years, which has increased post-
approval regulatory burdens. Post-regulatory approval reviews and data analyses can lead to the issuance of recommendations by government agencies,
health professional and patients or other specialized organizations regarding the use of products; for example, a recommendation to limit the patient
population of a drug’s indication, the imposition of marketing restrictions, including changes in product labeling, or the suspension or withdrawal of
the product. Any such action can result in reductions in sales volume and/or new or increased concerns about the adverse reactions or efficacy of a
product. These substantial regulatory requirements have, over time, increased the costs associated with maintaining regulatory approvals and achieving
reimbursement for our products.
If the regulatory approval process or post-approval, reimbursement, monitoring or other requirements become significantly more burdensome
in any of our major markets, we could become subject to increased costs and may be unable to obtain or maintain approval to market our products. Any
such adverse changes could materially and adversely affect our business, results of operations or financial condition.
If we fail to comply with laws and regulations governing the sales and marketing of our products, our business could be adversely affected.
We engage in various marketing, promotional and educational activities pertaining to, as well as the sale of, pharmaceutical products in a
number of jurisdictions around the world. The promotion, marketing and sale of pharmaceutical products and medical devices is highly regulated and
the sales and marketing practices of market participants such as us have been subject to increasing supervision by governmental authorities, and we
believe that this trend will continue.
For example, in the United States, our sales and marketing activities are monitored by a number of regulatory authorities and law enforcement
agencies, including the U.S. Department of Health and Human Services (the “HHS”), the FDA, the U.S. Department of Justice, the U.S. Securities and
Exchange Commission (the "SEC") and the Drug Enforcement Administration (the “DEA”). These authorities and agencies and their equivalents in
other countries have broad authority to investigate market participants for potential violations of laws relating to the sale, marketing and promotion of
pharmaceutical products and medical devices, including the False Claims Act, the Anti-Kickback Statute, the United Kingdom (the “UK”) Bribery Act
of 2010 and the Foreign Corrupt Practices Act, among others, for alleged improper conduct, including corrupt payments to government officials, improper
payments to medical professionals, off-label marketing of pharmaceutical products and medical devices, and the submission of false claims for
reimbursement by the federal government. Healthcare companies may also be subject to enforcement actions or prosecution for such improper conduct.
Any inquiries or investigations into the operations of, or enforcement or other regulatory action against, us by such authorities could result in significant
defense costs, fines, penalties and injunctive or administrative remedies, distract management to the detriment of the business, result in the exclusion
of certain products, or us as a whole, from government reimbursement programs or subject us to regulatory controls or government monitoring of its
activities in the future. We are also subject to certain ongoing investigations by governmental agencies.
Government policies and other pressures to reduce medical costs could have an adverse effect on sales of our pharmaceutical products.
We are subject to governmental regulations mandating price controls in various countries in which we operate. The growth of overall
healthcare costs as a percentage of gross domestic product in many countries means that governments and payers are under intense pressure to control
spending even more tightly. See “Item 4. Information on the Company—B. Business Overview—Third Party Reimbursement and Pricing.”
In the United States, there has been increasing pricing pressure from managed care groups and institutional and governmental purchasers.
In particular, as managed care groups have grown in size due to market consolidation, pharmaceutical companies have faced increased pressure in pricing
and usage negotiations, and there is fierce competition among pharmaceutical companies to have their products included in the care providers’ formularies.
Moreover, as a result of the changing legislative and regulatory environment in the United States we have experienced heightened pricing pressure on,
and limitations on access to, our branded pharmaceutical products sold in the United States. There has been increasing attention paid to the level of
pricing of pharmaceutical products by policymakers and stakeholders, which could lead to political pressure or legislative, regulatory or other efforts
to introduce lower prices, and change how the pharmaceutical supply chain could operate. In addition, there are efforts by the federal government to
reduce spending on the Medicare and Medicaid programs, including proposals by the Congressional Budget Office to require pharmaceutical companies
to pay a minimum rebate on drug products covered under Medicare Part D for low-income beneficiaries and to cap federal Medicaid payments to the
states. Congressional proposals to convert the Medicare fee-for-service program into a premium support program could also lead to significant reductions
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in Medicare spending. The future of the U.S. healthcare legislation, as well as the potential impact of any new legislation, is uncertain, but we expect
the health care industry in the United States will continue to be subject to increasing pricing and spending pressure, including from regulation and
political and legal action.
In Japan, manufacturers of pharmaceutical products must have new products listed on the National Health Insurance (the “NHI”) price list
published by the Ministry of Health, Labour and Welfare of Japan (the “MHLW”) for the coverage under the public medical care insurance systems.
The NHI price list provides rates for calculating the price of pharmaceutical products used in medical services provided under various public medical
care insurance systems. Prices on the NHI price list have been subject to revision generally once every two years on the basis of the actual prices at
which the pharmaceutical products are purchased by medical institutions in Japan after discounts and rebates are deducted from listed price. The average
price of previously listed products generally decreases as a result of these price revisions. The Japanese government is currently undertaking healthcare
reform initiatives with a goal of sustaining the universal coverage of the NHI program, and is addressing the efficient use of drugs, including promotion
of generic use with a target of 80% penetration by volume by September 2020 with respect to products for which market exclusivity has expired. As
part of these initiatives, the NHI price list is expected to be revised annually from April 1, 2021, which could lead to more frequent downward price
revisions. In addition, cost-effectiveness analysis was officially introduced by the MHLW in April 2019. Products on the NHI price list nominated based
on pre-defined criteria, such as the innovativeness and the financial impact, will be subject to review, and subject to price adjustments depending on
outcome of this review.
In Europe, as in the United States, drug prices have been subject to downward pressure due to measures implemented in each country to
control drug costs, and prices continue to come under pressure due to parallel imports, generic competition, increasing use of health technology assessment
based upon cost-effectiveness and other factors. European pricing and reimbursement authorities have also intensified efforts to increase transparency
of prices as well as exchange of information among the various European pricing authorities in order to raise pressure towards the industry. This pricing
debate has impacted the overall political climate in Europe and has triggered a European policy initiative to review the pharmaceutical industry’s
intellectual property incentives with a particular emphasis on orphan drugs. Any new legislation in this area would take at least two to three years to be
adopted but could have significant impact on our business model. We are also facing similar pricing pressures in other regions, such as various emerging
countries.
We expect these efforts to control costs to continue as healthcare payers around the globe, in particular government-controlled health
authorities, publicly funded or subsidized health programs, insurance companies and managed care organizations (the “MCOs”), increasingly pursue
initiatives to reduce the overall cost of healthcare, restrict access to higher-priced new medicines, increase the use of generics and impose overall price
revisions. Such further implementation of these policies could have a material adverse effect on our business, financial condition and results of operations.
The expiration or loss of patent or regulatory data protection over our products or patent infringement by generic manufacturers could lead to
significant competition from generic versions of the relevant product and lead to declines in market share and price levels of our products.
Our pharmaceutical products are generally protected for a defined period by various patents (including those covering drug substance, drug
product, approved indications, methods of administration, methods of manufacturing, formulations and dosages) and/or regulatory exclusivity, which
are intended to provide us with exclusive rights to market the products for the life of the patent or duration of the regulatory data protection period. The
loss of market exclusivity for pharmaceutical products opens such products to competition from generic substitutes that are typically priced significantly
lower than the original products, which typically adversely affects the market share and prices of the original products.
Generic substitutes have high market shares in a number of key markets, including the United States, Europe and many emerging countries,
and the adverse effects of the launch of generic products are particularly significant in such markets. The introduction of generic versions of a
pharmaceutical product typically leads to a swift and substantial decline in the sales of the original product. Our active life cycle management efforts
cannot fully mitigate the impact of competition from generics. In the United States and the European Union (“EU”), for example, political pressure to
reduce spending on prescription drugs has led to legislation and other measures that encourage the use of generic products. In Japan, the government is
implementing various measures to control drug costs, including by encouraging medical practitioners to use and prescribe generic drugs, and in June
2017 announced its intention to raise generic drug penetration with respect to products for which market exclusivity has expired to 80% by volume by
September 2020. Legislation has also been passed in the United States and Europe encouraging the use of biosimilar products. Similar to generics,
biosimilars aim to provide less expensive versions of innovative biologic products. New legislation has provided abbreviated pathways for the approval
and marketing of biosimilar products, which may affect the profitability and commercial viability of our biologic products.
Certain of our products have begun to, or are expected over the next several years to, face declining sales due to the loss of market exclusivity.
For example, following the expiration of patent protection over bortezomib, the active ingredient in VELCADE, one of our largest selling products in
the United States, a competing bortezomib-containing product has been introduced. This has led to a decrease in sales of VELCADE, and further entry
of competing products could result in substantial additional declines. Such decreases may accelerate following the scheduled expiration of patent
protection over the formulation of VELCADE in 2022, or earlier if a competitor is able to develop a way to formulate VELCADE in a manner that does
not infringe the relevant patent or succeed in getting the formulation patent invalidated. Patent protections over VYVANSE, which we acquired as part
of the Shire Acquisition and which was Shire’s largest selling product, are scheduled to expire in 2023, which we anticipate will lead to declines in sales.
In addition, as patent protection has expired for PANTOPRAZOLE in many major markets including the United States and the EU, sales of
PANTOPRAZOLE have continued to decline in those markets.
We may also be subject to competition from generic drug manufacturers prior to the expiration of patents if a manufacturer successfully
challenges the validity of our patents, or if the manufacturer believes that the benefits of launching the generic drug “at risk” (prior to the expiration of
our patent) outweigh the costs of defending infringement litigation. If such a competitor launches a generic product “at risk” before the initiation or
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completion of court proceedings, a court may decline to grant us a preliminary injunction to halt further “at risk” sales and remove the infringing product
from the market. While we may be entitled to obtain damages subsequently, the amount we may ultimately be awarded and able to collect may be
insufficient to compensate for the loss of sales and other harm caused to us. Furthermore, if we lose patent protection as a result of an adverse court
decision or a settlement, in certain jurisdictions, we may face the risk that government and private third-party payers and purchasers of pharmaceutical
products may claim damages alleging they have over-reimbursed or overpaid for a drug.
If our patent and other intellectual property rights are infringed by generic drug manufacturers or other third parties, we may not be able to
take full advantage of the potential or existing demand for our products. The protection that we are able to obtain for our prescription drugs varies from
product to product and country to country and may not always be sufficient because of local variations in issued patents, or differences in national law
or legal systems, including inconsistency in the enforcement or application of law and limitations on the availability of meaningful legal remedies. In
particular, patent protection in emerging markets is often less certain than in developed markets. Certain countries may also engage in compulsory
licensing of pharmaceutical intellectual property to other manufacturers as a result of local political pressure. Furthermore, the attention of our management
and other personnel could be diverted from their normal business activities if we decide to litigate against such infringement. The realization of any
such risks could adversely and materially affect our business, financial condition and results of operations.
We are subject to the risk of intellectual property infringement claims directed at us by third parties.
We are subject to the risk of infringement claims directed at us by third parties, even if we do not knowingly infringe on any valid third-
party intellectual property rights. Although we monitor our operations to prevent infringement on the intellectual property rights of third parties, if we
are found to have infringed the intellectual property rights of others or if we agree to settle infringement claims, we may be required to recall the relevant
products, terminate manufacturing and sales of such products, pay significant damages or pay significant royalties.
We evaluate any such infringement claims to assess the likelihood of unfavorable outcomes and to estimate, if possible, the amount of
potential losses. Based on these assessments and estimates, and in keeping with applicable accounting and disclosure standards, we establish reserves
and/or disclose the relevant litigation claims or decide not to establish reserves or disclose litigation claims. These assessments and estimates are based
on the information available to our management at such time and involve a significant amount of management judgment. Actual outcomes or losses
may differ materially from those envisioned by our current assessments and estimates. Although the parties to such patent and intellectual property
disputes in the pharmaceutical industry have often settled through licensing or similar arrangements, the costs associated with these arrangements may
be substantial and could include the payment of ongoing royalties. Furthermore, the necessary licenses may not be available on acceptable terms or at
all. Therefore, if we are unable to successfully defend against infringement claims by third parties, our financial results could be materially and adversely
affected.
The illegal distribution and sale by third parties of counterfeit versions of our products or products stolen from us could have an adverse effect on
our reputation and business.
Third parties may illegally distribute and sell counterfeit versions of our products, which do not meet the rigorous manufacturing and testing
standards to which our products are subject. A patient who receives a counterfeit drug may be at risk for a number of dangerous health consequences.
Reports of adverse reactions to counterfeit drugs or increased levels of counterfeiting could materially affect patient confidence in our products, which
could have a material adverse effect on our reputation and financial results. In addition, thefts at warehouses, at plants, or in transit of inventory that is
not properly stored or that is sold through unauthorized channels could materially and adversely affect patient safety, our reputation and our results of
operations.
We may not be able to adequately expand our product portfolio through third-party alliance arrangements.
We expect that we will continue to rely on third parties for key aspects of our business, including the discovery and development of new
products, in-licensing products, and the marketing and distribution of approved products. A major part of our research and development strategy is to
initiate alliances with third parties in the biotechnology industry, academia and the public sector, and we believe that the overall strength of our research
and development program and product pipeline depends on our ability to identify and initiate partnerships, in-licensing arrangements and other
collaborations with third parties. However, there can be no assurance that any of our third-party alliances will lead to the successful development and
marketing of new products. Moreover, reliance on third-party alliances subjects us to a number of risks, including:
• We may be unable to identify suitable opportunities at a reasonable cost and on terms that are acceptable to us due to active and intense
competition among pharmaceutical groups for alliance opportunities or other factors;
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Entering into in-licensing or partnership agreements may require the payment of significant “milestones” well before the relevant
products are placed in the market, without any assurance that such investments will ultimately become profitable in the long term. To
the extent such milestone payments are recorded as assets on our balance sheet, any termination of the relevant partnership could
require us to recognize an impairment loss up to the full value of such asset;
• When we research and market our products through collaboration arrangements, the performance of certain key tasks or functions are
the responsibility of our collaboration partners, who may not perform effectively or otherwise meet our expectations; and
•
Decisions may be under the control of or subject to the approval of our collaboration partners, and we may have differing views or be
unable to agree upon an appropriate course of action. Any conflicts or difficulties that we may have with our partners during the course
of these agreements or at the time of their renewal or renegotiation or any disruption in the relationships with our partners may affect
the development, launch and/or marketing of certain of our products or product candidates.
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In addition, a licensor may attempt to terminate its license agreement with us or elect not to renew it to pursue other marketing opportunities.
Our licensors could also merge with or be acquired by another company or experience financial or other setbacks unrelated to our licensing arrangements.
Any of these events may force us to abandon a development project and adversely affect our ability to adequately expand or maintain our product
portfolio.
Our operating results and financial condition may fluctuate due to a number of factors and may not be comparable across periods.
Our operating results and financial condition may fluctuate from quarter to quarter and year to year for a number of reasons, including
acquisitions, divestitures, major product launches, patent expiration or expiration of regulatory data protection for key products and other reasons. In
particular, as part of our efforts to refocus our business portfolio, we have recently entered into a number of significant transactions that are expected
to affect our results of operations, including:
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the Shire Acquisition;
the acquisition of TiGenix NV in July 2018;
the divestment of Wako Pure Chemical Industries, Ltd. (“Wako Pure Chemical”), one of our consolidated subsidiaries, to FUJIFILM
Corporation in April 2017;
the acquisition of ARIAD Pharmaceuticals, Inc. (“ARIAD”) in February 2017; and
the transfer of certain long-listed products, consisting of products for which patent protection and regulatory data protection have
expired, to Teva Takeda Yakuhin Ltd., a wholly-owned subsidiary of Teva Takeda Pharma Ltd., a joint venture we formed with Teva
Pharmaceutical Industries Ltd., in April 2016, and the subsequent sale of seven additional long-listed products in May 2017.
We intend to continue to pursue both acquisitions of new businesses and dispositions of existing businesses in the future. As a result, period-
to-period comparisons of our results of operations may not always be directly comparable, and these comparisons should not be relied upon as an
indication of future performance. Our operating results and financial condition are also subject to fluctuations from the risks described throughout this
section.
We have significant global operations, which expose us to additional risks.
Our global operations, which encompass approximately 80 countries and regions across the world, are subject to a number of risks, including
the following:
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difficulties in monitoring and coordinating research and development, marketing, supply-chain and other operations in a large number
of jurisdictions;
risks related to various laws, regulations and policies, including those implemented following changes in political leadership and trade,
capital and exchange controls;
changes with respect to taxation, including impositions or increases of withholding and other taxes on remittances and other payments
by our overseas subsidiaries;
varying standards and practices in the legal, regulatory and business cultures in which we operate, including potential inability to
enforce contracts or intellectual property rights;
trade restrictions and changes in tariffs;
complex sanctions regimes in various countries such as the United States, the EU and other jurisdictions, violations of which could
lead to fines or other penalties;
risks related to political instability and uncertain business environments;
changes in the political, economic or social climate, including inter-country relationships;
acts of terrorism, war, epidemics and other sources of social disruption; and
difficulties associated with managing local personnel and preventing misconduct by local third-party alliance partners.
Any one or more of these or other factors could increase our costs, reduce our revenues, or disrupt our operations, with possible material
adverse effects on our business, financial condition and results of operations. Further expansion overseas has been one of our key strategies, and, in the
fiscal year ended March 31, 2019, regions outside of Japan accounted for 72.8% of our consolidated revenue, with the United States in particular
contributing 39.5% of consolidated revenue, and we anticipate that these proportions will further increase once Shire’s businesses have been included
in our consolidated results of operations for a full fiscal year. We expect that markets outside Japan, particularly the United States and also Europe,
Canada and emerging markets, will continue to be increasingly important to our business and results of operations, increasing the likelihood that any
of these risks is realized.
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We may not be able to realize the expected benefits of our investments in emerging markets.
We have been taking steps to grow our business in emerging markets, which we define to include Russia/Commonwealth of Independent
States (“CIS”), Latin America, Asia (excluding Japan) and Other (including the Middle East, Oceania and Africa). Our revenue from emerging markets
was ¥291.6 billion (or 13.9% of our total revenue) for the fiscal year ended March 31, 2019, and we intend to pursue further growth in such emerging
markets.
However, there is no guarantee that our efforts to expand sales in emerging markets will succeed. Some countries may be especially vulnerable
to periods of global financial instability or may have very limited resources to spend on healthcare. Emerging markets present particular challenges in
obtaining funding, achieving market access for our products and successfully ensuring that we receive appropriate levels of reimbursement. Emerging
markets also tend to require substantial efforts in patient support and other programs. All of these factors may adversely affect the profitability of our
businesses in these emerging markets.
In order to successfully implement our emerging markets strategy, we must also attract and retain qualified personnel, despite the possibility
that some emerging markets may have a relatively limited number of persons with the required skills and training. We may also be required to increase
our reliance on third-party agents within less-developed markets, which may put us at increased risk of liability. In addition, many emerging markets
have currencies that fluctuate substantially, and if such currencies are devalued and we cannot offset the devaluations, our financial performance in such
countries may be adversely affected. Further, many emerging markets have relatively weak intellectual property protection and inadequate protection
against crime, including counterfeiting, corruption and fraud. Operations in certain emerging countries, where corruption may be more prevalent than
in more developed countries and where internal compliance practices may not be well established, may also pose challenges from a legal and regulatory
compliance perspective.
For reasons including but not limited to the above, sales within emerging markets carry significant risks, and the realization of such risks
could have a material adverse effect on our business, financial condition and results of operations.
We face risks relating to the expected exit of the United Kingdom from the European Union.
On June 23, 2016, the United Kingdom held a remain-or-leave referendum on the United Kingdom’s membership within the European
Union, the result of which favored the exit of the United Kingdom from the EU (commonly known as “Brexit”). A process of negotiation will likely
determine the future terms of the United Kingdom’s relationship with the EU, as well as whether the United Kingdom will be able to continue to benefit
from the EU’s free trade and similar agreements. Additionally, Brexit has impacted the EMA, which is the primary regulator of the pharmaceutical
industry in the EU and which has stated that it expects to lose about 25% of its 900 staff members due to the EMA’s relocation from London to Amsterdam
as a result of Brexit. The EMA has developed a business continuity plan that allows EMA to temporarily scale back or temporarily suspend lower priority
activities during the relocation and as it prepares for Brexit. For example, the EMA noted in its annual report for 2018 that, in order to be able to
concentrate on Brexit and the EMA’s relocation to Amsterdam, it had to delay updating its guidelines on the development of new medicines to treat
hemophilia A and B. Delays in EMA processes such as this caused by Brexit may adversely affect or delay our business, including our ability to develop
and market new or existing products in the EU.
The timing of Brexit and potential impact of Brexit on our market share, sales, profitability and results of operations is unclear. Depending
on the terms of Brexit and any continuing impact on the EMA, economic conditions in the United Kingdom, the European Union and global markets
may be adversely affected by reduced growth and volatility. The uncertainty before, during and after the period of negotiation is also expected to have
a negative economic impact and increase volatility in the markets, particularly in the Eurozone. Such volatility and negative economic impact could, in
turn, adversely affect our revenues, financial condition or results of operations.
Our results of operations and financial condition may be adversely affected by foreign currency exchange rate fluctuations.
We manufacture and sell products to customers in numerous countries, and we have entered and will enter into acquisition, licensing,
borrowings or other financial transactions that give rise to translation and transaction risks related to foreign currency exposure. Fluctuations in currency
exchange rates in the markets where we are active could negatively affect our results of operations, financial position and cash flows. For the fiscal year
ended March 31, 2019, 72.8% of our sales were in markets outside Japan, and we expect this proportion to be even higher for subsequent fiscal periods,
due to anticipated increases in overseas sales of growth driver products and the contribution of Shire’s results to our results of operations, particularly
in the U.S. market. Our consolidated financial statements are presented in Japanese yen, and by translating the foreign currency financial statements of
our foreign subsidiaries into yen, the amounts of our revenue, operating profit, assets and equity, on a consolidated basis, are affected by prevailing rates
of exchange.
We utilize certain hedging measures with respect to some of our foreign currency transactions. However, such hedging measures do not
cover all of our exposures and, even to the extent they do, they may only delay, or may otherwise be unable to completely eliminate, the impact of
fluctuations in foreign currency exchange rates.
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Our reliance on third parties for the performance of certain key business functions, particularly product manufacture and commercialization,
heightens the risks faced by our business.
We rely on suppliers, vendors and partners, including alliances with other pharmaceutical companies, for certain key aspects of our business,
including manufacture and commercialization of products, support for information technology systems and certain human resource functions. We do
not control these partners, but we depend on them in ways that may be significant to us. If these parties fail to meet our expectations or fulfill their
obligations to us, we may fail to receive the expected benefits. In addition, if any of these third parties fails to comply with applicable laws and regulations
in the course of its performance of services for us, there is a risk that we may be held responsible for such violations as well. This risk is particularly
serious in emerging markets, where corruption is often prevalent and where many of the third parties on which we rely do not have internal compliance
resources comparable to our own. Any such failures by third parties, in emerging markets or elsewhere, could adversely affect our business, reputation,
financial condition or results of operations.
Our dependence on third parties for the inputs for our products subjects us to various risks, and changes in the costs of materials may adversely
affect our profitability.
Although we develop and manufacture the active ingredients used in some of our products at our own facilities, we are dependent on third-
party suppliers for a substantial portion of the raw materials and compounds used in the products we produce. The price and availability of the raw
materials for our products, including chemical compounds and biologics, are subject to the effects of weather, natural disasters, market forces, the
economic environment, fuel costs and foreign exchange rates. If our cost for such materials increases, we may not be able to make corresponding
increases in the prices of our products due to market conditions or our relationships with our customers, and as a result, our profitability could be
materially and adversely affected.
In particular, we rely on third-party suppliers of key manufacturing inputs of certain drug products, including, but not limited to, ADCETRIS,
ADVATE, ADYNOVATE, ALUNBRIG, CINRYZE, CUVITRU, ENTYVIO, FEIBA, FIRAZYR, GATTEX/REVESTIVE, HYQVIA, LEUPRON, MEPACT,
NINLARO, TAKHZYRO, and VELCADE. Furthermore, certain active ingredients for these products are sourced from a single supplier. We also rely in
part on third-party sources to provide the donated plasma necessary for our plasma-derived therapies. In addition, although we dual-source certain key
products and/or active ingredients, we currently rely on a single source for production of the final drug product for certain of our products, including,
but not limited to, ADDERALL XR, ADYNOVATE, ALOFISEL, ALUNBRIG, CINRYZE, CUVITRU, FIRAZYR, HYQVIA, LIALDA, MEPACT, NINLARO,
PENTASA and TAKHZYRO. Sources of some materials may be limited to a single supplier, and if such supplier faces any difficulty in supplying the
materials, we may not be able to find an alternative supplier in a timely manner or at all. If materials become unavailable or if quality problems related
to the materials arise, we may be forced to halt production and sales of products that use them. In the event that any of our third-party suppliers is delayed
in its delivery of such raw materials or compounds, is unable to deliver the full quantity ordered by us at the appropriate level of quality, or is unable to
deliver any raw materials or compounds at all, our ability to sell our products in the quantities demanded by the market may be impaired, which could
damage our reputation and relationships with customers and patients. In such a case, our business and results of operations could be adversely affected.
The manufacture of our products is technically complex and highly regulated, and supply interruptions, product recalls or other production problems
caused by unforeseen events may reduce sales, adversely affect our operating results and financial condition and delay the launch of new products.
The manufacture of our products is technically complex and highly regulated, and as a result we may experience difficulties or delays
including but not limited to the following:
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seizure or recalls of products or shut-downs of manufacturing plants;
problems with business continuity, including as a result of a natural or man-made disaster, at one of our facilities or at a critical supplier
or vendor;
failure by us or by any of our vendors or suppliers to comply with Good Manufacturing Practice and other applicable regulations and
quality assurance guidelines, which could lead to manufacturing shutdowns, product shortages and delays in product manufacturing;
problems with manufacturing, quality assurance/quality control or supply, or governmental approval delays, due to our consolidation
and rationalization of manufacturing facilities and the sale or closure of certain sites;
failure of a sole source or single source supplier to provide us with necessary raw materials, supplies or finished goods for an extended
period of time, which could impact continuous supply;
failure of a third-party manufacturer to supply us with semi-finished or finished products on time;
construction or regulatory approval delays related to new facilities or the expansion of existing facilities;
additional costs related to deficiencies identified by regulatory agencies in connection with inspections of our facilities, and enforcement,
remedial or punitive actions by regulatory authorities if we fail to remedy any deficiencies; and
other manufacturing or distribution problems including limits to manufacturing capacity due to regulatory requirements (e.g.
Registration, Evaluation, Authorisation and Restriction of Chemicals (“REACH”) regulation in the EU), changes in the types of products
produced, physical limitations or other business interruptions that could impact continuous supply.
The development and manufacture of biologics including products added to our portfolio following the completion of the Shire Acquisition
and stem cell therapies resulting from our acquisition of Tigenix NV in July 2018, present heightened or additional risks. The manufacture of biologics,
including stem cell products, is highly complex and is characterized by inherent risks and challenges, such as raw material inconsistencies, logistical
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and sourcing challenges, significant quality control and assurance requirements, manufacturing complexity (including heightened regulatory
requirements) and significant manual processing. Unlike products that rely on chemicals for efficacy, such as most pharmaceuticals, biologics are difficult
to characterize due to the inherent variability of biological input materials. As a result, assays of the finished product may not be sufficient to ensure
that the product will perform in the intended manner. Problems with the manufacturing process, even minor deviations from the normal process, could
result in product defects or manufacturing failures that result in, among other things, lot failures, product recalls, product liability claims or insufficient
inventory, which could be costly to us or result in reputational damage.
Any of the above may reduce sales, delay the launch of new products, and adversely affect our business, financial condition and results of
operations.
We are involved in litigation relating to our operations on an ongoing basis, and such litigation could result in financial losses or harm our business.
We are involved in various litigation relating to our operations on an ongoing basis, including claims related to product liability and intellectual
property as well as to antitrust, sales and marketing and other regulatory regimes. Given the inherent unpredictability of litigation, it is possible that an
adverse outcome in one or more pending or future litigation matters could have a material adverse effect on our operating results or cash flows. For a
description of certain ongoing litigation, see Note 32 to our audited consolidated financial statements included in this annual report.
Economic and financial conditions may have a material adverse effect on our business, financial condition and results of operations.
Growth of the global pharmaceutical market has become increasingly tied to global economic growth. In this context, a substantial and
lasting slowdown of the global economy or major national economies could negatively affect growth in the global pharmaceutical market and, as a
result, adversely affect our business. In particular, weak economic conditions can have a particularly adverse impact on pharmaceutical demand in
markets having significant co-pays or lacking a developed third-party payer system, as individual patients may delay or decrease out-of-pocket healthcare
expenditures. Negative economic developments could also reduce the sources of funding for national social security systems, leading to heightened
pressure on drug prices, increased substitution of generic drugs, and the exclusion of certain products from formularies.
Following the global financial crisis in 2008, economic growth continues to be stagnant in major developed countries while the pace of
growth in many emerging economies has declined. The Brexit referendum in the U.K, political volatility in the United States following recent mid-term
elections, continued instability in the Middle East and North Korea and global developments in trade and security policy have increased political and
economic uncertainty. To the extent that economic or financial conditions weaken in any of our major operating markets, demand for our products or
product pricing could be negatively affected. In addition, to the extent that economic and financial conditions negatively affect the global business
environment, we could experience a disruption or delay in the performance of third parties on which we rely for parts of our business, including
collaboration partners and suppliers. Such disruptions or delays could have a material and adverse effect on our business, financial condition and results
of operations.
We may have difficulty maintaining the competitiveness of our products.
The pharmaceutical industry is highly competitive, and in order to maintain the competitiveness of our product portfolio, we are required
to maintain ongoing, extensive research for technological innovations, including new compounds, to develop and commercialize existing pipeline
products, to expand our product portfolio through acquisitions and in-licensing, and to market our products effectively, including by communicating the
efficacy, safety and value of our products to healthcare professionals. However, healthcare professionals and consumers may choose competitors’ products
over ours nonetheless, if they perceive these products to be safer, more reliable, more effective, easier to administer or less expensive. The success of
any product depends on our ability to effectively communicate with and educate the healthcare professionals and patients and convince them of the
advantage of our products over those of our competitors. We often carry out costly clinical trials even after our products have been launched to produce
data to be utilized for these purposes, but such trials do not always produce the desired outcomes. Furthermore, many of our competitors have greater
financial and other resources to conduct such trials in more detail and with larger patient populations, which may ultimately enable them to promote
their products more effectively than we do. Moreover, if relevant regulators increase their approvals of new therapies developed by competitors for the
conditions treated by our products, such as in order to increase the number of treatment options available for rare or orphan diseases, our business and
results of operations could be materially and adversely affected.
For example, in recent years, competitors have introduced additional plasma-based hemophilia products, or such products have been approved
for additional uses, which may affect (and in certain cases has affected) sales of our plasma-based hemophilia products, such as FEIBA. Moreover,
certain competitors are developing other hemophilia therapies, including gene-based therapies, which, if successfully introduced, could also harm sales
of our plasma-based therapies. Increased competition from new products or therapies could similarly affect our other products.
In Japan, reduced approval times for drugs already marketed outside Japan have led to increased competition through the introduction of
such drugs into the Japanese market by foreign competitors. In addition, new competing products or the development of superior medical technologies
and other treatment options could make our products or technologies lose their competitiveness or become obsolete. As discussed above, our products
are also subject to competition from inexpensive generic versions of our products, as well as generic versions of our competitors’ products, upon the
expiration or loss of related patent protection and regulatory data protection, which may result in loss of market share. If we are unable to maintain the
competitiveness of our products, our business, financial position and results of operations could be materially and adversely affected.
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Our products may have unanticipated adverse effects or possible adverse effects, which may restrict use of the product or give rise to product liability
claims.
As a pharmaceutical company, we are subject to significant risks related to product liability. Unanticipated adverse reactions or unfavorable
publicity from complaints concerning any of our products, or those of our competitors, could have an adverse effect on our ability to obtain or maintain
regulatory approvals or successfully market our products, and may even result in recalls, withdrawal of regulatory approval or adverse labeling of the
product.
While our products are subject to comprehensive clinical trials and rigorous statistical analysis during the development process prior to
approval, there are inherent limitations with regard to the design of such trials, including the limited number of patients enrolled in such trials, the limited
time used to measure the efficacy of the product and the limited ability to perform long-term monitoring. In the event that such unanticipated adverse
reactions are discovered, we may be required to add descriptions of the adverse reactions as “precautions” to the packaging of our products, recall and
terminate sales of products or conduct costly post-launch clinical trials. Furthermore, concerns relating to potential adverse reactions could arise among
consumers or medical professionals, and such concerns, whether justified or not, could have an adverse effect on sales of our products and our reputation.
We could also be subject to product liability litigation by patients who have suffered or claim to have suffered such adverse reactions resulting in harm
to their health.
Although we maintain product liability insurance at coverage levels that we believe are appropriate, we could be subject to product liability
that significantly exceeds such levels. Product liability coverage is also increasingly difficult and costly to obtain, and may not be available in the future
on acceptable terms. Therefore, in the future, it is possible that we may need to rely increasingly on self-insurance for the management of product liability
risk. In cases where we self-insure, the legal costs that we would bear for handling such claims and potential indemnifications to be paid to claimants
could materially and adversely affect our financial condition. In addition, the negative publicity from product liability claims, whether or not justified,
may damage our reputation and may negatively impact the number of prescriptions of the product in question or our other products. As a result, our
business, financial condition and results of operations could be materially and adversely affected.
We may not be able to attract and retain key management and other personnel.
In order to produce, develop, support and market our products, we depend on the expertise and leadership of our senior management team
and other key members of our organization. The loss of key members of our organization, including senior members of our scientific and management
teams, high-quality researchers and development specialists, could delay or prevent the achievement of major business objectives. The market for such
talents has become increasingly competitive, including in specific geographic regions and in specialized fields such as clinical development and
biosciences, and we are required to invest heavily in the recruitment, training and retention of qualified individuals, including salary and other
compensation to reward performance and incentivize employees. Despite our efforts to retain them, key employees could terminate their employment
with us for any reason or for no reason, and there is no assurance that we will be able to attract or retain key employees and successfully manage them.
Our inability to attract, integrate and retain highly skilled personnel, particularly those in leadership positions, may weaken our succession plans and
may materially adversely affect our ability to implement our strategy and meet our strategic objectives, which could ultimately adversely affect our
business and results of operations.
We are increasingly dependent on information technology systems and our systems and infrastructure face the risk of theft, exposure, tampering or
other intrusions.
A variety of important processes relating to the research and development, production and sale of our products depend heavily on our
information systems, including cloud-based computing, or those of third party providers to whom we outsource certain business functions, including
the storage and transfer of critical, confidential, sensitive or personal information regarding our patients, clinical trial subjects, vendors, customers,
employees and others. The size and complexity of these computer systems make them potentially vulnerable to service interruptions, malicious intrusions
and random attacks. Cyber-attacks are increasing in frequency, sophistication and intensity. Such attacks are made by groups and individuals with a
wide range of motives (including, but not limited to, industrial espionage) and expertise, including organized criminal groups, “hacktivists,” nation-
states and others. Cyber-attacks could include the deployment of harmful malware, denial of service attacks, worms, social engineering and other means
to affect service reliability and threaten data confidentiality, integrity and availability. The development and maintenance of systems to safeguard against
such attacks is costly and requires ongoing monitoring and updating as technologies change and efforts to overcome security measures become increasingly
more sophisticated. Moreover, the costs related to these security measures are expected to continue to increase. Despite our efforts, the possibility of a
future data compromise cannot be eliminated entirely, and risks associated with intrusion, exposure, tampering, and theft remain. For “zero-day threats,”
or new vectors of attack which are currently unknown, the risk that our defenses will be inadequate are particularly pronounced.
If our data systems are compromised, our business operations may be impaired, we may lose profitable opportunities, or the value of those
opportunities may be diminished, and we may lose revenue because of unlicensed use of our intellectual property or confidential or proprietary information.
Cyber-attacks could significantly impact the availability of data systems that are essential to conducting routine business operations across the company,
including product manufacturing or clinical development, and the recovery efforts could be both time consuming and costly. If personal information
of our customers or employees is misappropriated, our reputation with our customers and employees may be injured resulting in loss of business and/
or morale, and we may incur costs to remediate possible injury to our customers and employees or be required to pay fines or take other action with
respect to judicial or regulatory actions arising out of such incidents. Data privacy or security breaches by employees and others with permitted access
to our systems, including in some cases third-party service providers to which we may outsource certain business functions, may also pose a risk that
sensitive data, including intellectual property or personal information, will be exposed to unauthorized persons or to the public.
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Changes in data privacy and protection laws and regulations, particularly in Europe, or any failure to comply with such laws and regulations, could
adversely affect our business and financial results.
We are subject to laws and regulations globally regarding privacy, data protection, and data security, including those related to the collection,
storage, handling, use, disclosure, transfer, and security of personal data. Significant uncertainty exists as privacy and data protection laws may be
interpreted and applied differently from country to country and may create inconsistent or conflicting requirements. For example, the EU’s General Data
Protection Regulation (the “GDPR”), which imposes additional obligations on companies regarding the handling of personal data and provides certain
individual privacy rights to persons whose data is processed, became effective on May 25, 2018. Moreover, significant regulatory fines may be imposed
on us for violation of these requirements, particularly in the case of the GDPR, which are set at a maximum of the higher of €20 million or 4% of annual
global turnover for the most serious breaches, or the higher of €10 million or 2% of annual global turnover for certain others. There is also significant
uncertainty as to how the various EU member states or individual regulators will implement and interpret the GDPR, and we are still in the process of
identifying and unifying differences between our and Shire’s historical GPDR compliance practices. Furthermore, legislators and regulators in the United
States are proposing new and more robust cybersecurity rules in light of the recent broad-based cyberattacks at a number of companies. Compliance
with existing, proposed and recently enacted laws (including implementation of the privacy and process enhancements called for under GDPR) and
regulations can be costly; any failure to comply with these regulatory standards could subject us to legal and reputational risks. Misuse of or failure to
secure personal information could also result in violation of data privacy laws and regulations, proceedings against us by governmental entities or others
or damage to our reputation and credibility and could also have a negative impact on revenues and profits.
Social media platforms and new technologies present risks and challenges for our reputation and business.
Consumers, the media, pharmaceutical companies and other parties increasingly use social media and other new technologies to communicate
about pharmaceutical products and the diseases they are intended to treat. For pharmaceutical companies, the use of these technologies requires specific
attention, monitoring programs and moderation of comments. For example, negative or inaccurate posts or comments about us or our products on any
social media networking platforms could damage our reputation and business. Social media could also be used to bring negative attention to us or to
the pharmaceutical industry as a whole, which could in turn cause reputational harm to us and negatively impact our business. The nature of evidence-
based health care, however, may prevent us from rapidly and adequately defending our interests against such comments. In addition, our employees and
partners may use social media and mobile technologies inappropriately, which may expose us to liability, or which could lead to breaches of data security,
loss of trade secrets or other intellectual property or public disclosure of sensitive information, including information about our employees, clinical trial
subjects or customers.
Sales to wholesalers are concentrated, which exposes us to credit risks and pricing pressures.
A significant portion of our global sales are made to a relatively small number of wholesale distributors, retail chains and other purchasing
groups. In the fiscal year ended March 31, 2019, our largest wholesale distributor accounted for 10.8% of our total revenue. If one of our significant
wholesale distributors encounters financial or other difficulties, such distributor may decrease the amount of business that it does with us, and we may
be unable to collect the amounts that the distributor owes us on a timely basis or at all. Furthermore, the concentration of wholesale distributors has been
increasing through mergers and acquisitions. In addition to increased credit risks, this has resulted in such distributors gaining additional purchasing
leverage, which may increase pricing pressure on our products. Such credit concentration risks and pricing pressure could adversely affect our business,
financial condition and results of operations.
We face risks from the pursuit of acquisitions, and the anticipated benefits and synergies resulting from acquisitions may not be realized.
We regularly pursue acquisitions for a number of reasons, including strengthening our pipeline, complementing existing lines of business,
adding research and development capabilities or pursuing other synergies. The pursuit of these acquisitions requires the commitment of significant
management and capital resources in various stages, from the exploration of potential acquisition targets to the negotiation and execution of an acquisition
to the integration of an acquired business into our own. The required commitment of time and resources may divert the attention of management or
capital or other resources away from our day-to-day business. Moreover, we may not be able to recoup the investment of capital or other resources
through the successful integration of acquired businesses, including the realization of any expected cost or other synergies. Specifically, we may encounter
the following difficulties:
• We may face significant challenges in combining the infrastructure, management and information systems of acquired companies with
ours, including integrating research and development, manufacturing, distribution, marketing and promotion activities and information
technology systems;
•
There may be difficulties in conforming standards, controls, procedures and accounting and other policies, as well as business cultures
and compensation structures;
• We may not be able to retain key personnel at acquired companies, or our own employees may be motivated to leave due to acquisitions;
• We may not be successful in identifying and eliminating redundancies and achieving other cost savings as expected; and
• We may not be able to successfully realize benefits from acquired products, including pipeline products under development.
Integrating the operations of multiple new businesses with that of our own is a complex process that requires significant management attention
and resources. The integration process may disrupt our existing and other newly acquired businesses and, if implemented ineffectively, could have an
adverse impact not only on our ability to realize the benefits of a given acquisition but also on the results of our existing operations. Integration-related
risks may be heightened in cases where acquired businesses’ operations, employees or customers are located outside our major markets and we incur
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higher costs than anticipated due to regulatory changes, environmental factors or foreign exchange fluctuations. We continue to pursue strategic business
acquisitions globally as a key part of our continuous growth strategy. If we are not able to achieve the anticipated benefits of any future acquisitions in
full or in a timely manner, we could be required to recognize impairment losses, we may not be able to recoup our investment, and our business, financial
position and results of operations could be materially and adversely affected. Particularly, we may be unable to achieve the expected revenues pursuant
to licensing, co-promotion or co-development agreements or collaborations. We may also assume unexpected contingent or other liabilities, or be required
to mark up the fair value of liabilities (or mark down the fair value of assets) acquired upon the close of an acquisition.
We may incur substantial costs due to our environmental compliance efforts or claims relating to our use, manufacture, handling, storage or disposal
of hazardous materials.
Our research and development and manufacturing processes use hazardous materials, including chemicals and radioactive and biological
materials, and produce hazardous waste. National and local laws and regulations in many of the jurisdictions in which we operate impose substantial
potential liability for the improper use, manufacture, handling, storage and disposal of hazardous materials as well as for land contamination, and, in
some cases, this liability may continue over long periods of time. Despite our compliance efforts, we cannot completely eliminate the risk of accidental
contamination and any resultant injury from these materials. For example, real properties that we owned or used in the past or that we own or use now
or in the future may contain detected or undetected contamination resulting from our manufacturing operations at those sites or the activities of prior
owners or occupants. We may suffer from expenses, claims or liability which may fall outside of or exceed our insurance coverage. Furthermore, changes
to current environmental laws and regulations may impose further compliance requirements on us that may impair our research, development and
production efforts as well as our other business activities.
We may suffer large losses in the event of a natural or other disaster, such as an earthquake, terrorist attack or other catastrophic event, in any of
the markets in which we operate.
Japan and other regions in the world in which we operate are subject to the risk of earthquakes and other natural disasters, including volcanic
eruptions, tidal waves, typhoons, floods and hurricanes. For example, the Great East Japan Earthquake and subsequent tsunami that occurred in March
2011 caused unprecedented property and other damage, although we did not incur any significant damage to our facilities. In addition, other events
outside our control, such as war, civil or political unrest, deliberate acts of sabotage, or industrial accidents such as fire and explosion, whether due to
human or equipment error, could damage, cause operational interruptions, or otherwise adversely affect certain of our manufacturing or other facilities
as well as potentially cause injury or death to our personnel. In the event of a major natural disaster or other uncontrollable event or accident, our facilities,
particularly our production plants, may experience catastrophic loss, operations at such facilities may be halted, shipments of products may be suspended
or delayed and large losses and expenses to repair or replace facilities may be incurred. Such negative consequences could cause product shortages,
significant losses of sales or require significant unexpected expenditures, and materially adversely affect our business, financial condition and results
of operations. In addition, our business may also be adversely affected if our suppliers or business partners were to experience a catastrophic loss due
to natural disasters, accidents or other uncontrollable events.
Although we purchase comprehensive global insurance to cover property damage and consequent business interruption for certain potential
losses at sites owned by us and at certain critical supplier sites, we do not maintain earthquake insurance in Japan, and our insurance policies may not
be adequate to cover all possible losses and expenses.
We may have to recognize additional charges on our statements of income due to impairment of goodwill, other intangible assets and equity method
investments.
We carry significant amounts of goodwill and intangible assets on our balance sheet as a result of past acquisitions, including the Shire
Acquisition. As of March 31, 2019, we had goodwill of ¥4,161.4 billion and intangible assets of ¥4,860.4 billion. Goodwill and intangible assets recorded
in relation to acquisitions are recognized on our balance sheet on the acquisition date. Under IFRS, we are required to examine such assets for impairment
whenever events or changes in circumstances indicate that the carrying amount of an asset may not be recoverable. See “Item 5. Operating and Financial
Review and Prospects—A. Operating Results—Critical Accounting Policies—Impairment of Goodwill and Intangible Assets.”
We occasionally enter into business ventures with third-party entities where we have significant influence over the decisions on financial and
operating policies, but do not have control or joint control (referred to as “investments in associates”). We also enter into joint arrangements whereby
we and the other parties that have joint control of the arrangement have rights to the net assets of the arrangement (referred to as “joint venture”). We
account for these investments using the equity method of accounting. As of March 31, 2019, the carrying amount of investments accounted for using
the equity method was ¥114.7 billion. Under IFRS, at each reporting period, we are required to determine whether there is objective evidence that the
investment in each associate or joint venture is impaired.
The recognition of such impairment charges may adversely affect our business, financial condition and results of operations.
If we fail to maintain effective internal control over financial reporting, the accuracy and timeliness of our financial reporting may be adversely
affected, which could cause investors to lose confidence in our reported financial information and may lead to a decline in the trading price of our
ADSs.
Our common stock is currently listed on the Tokyo Stock Exchange and other local Japanese stock exchanges, and we have established
internal control over financial reporting pursuant to the requirements applicable to companies listed only in Japan. In addition, our ADSs are listed on
the New York Stock Exchange (the “NYSE”), making us subject to, among other things, the requirements under the Sarbanes-Oxley Act of 2002 (the
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“Sarbanes-Oxley Act”). The standards for internal control over financial reporting under the Sarbanes-Oxley Act are significantly more extensive than
those applicable to companies listed only in Japan. For example, we will be required, pursuant to Section 404 of the Sarbanes-Oxley Act (“Section 404”),
to furnish a report by management on, among other things, the effectiveness of our internal control over financial reporting. This assessment will need
to include disclosure of any material weaknesses identified by our management in our internal control over financial reporting, as well as a statement
that our independent registered public accounting firm has issued an opinion on our internal control over financial reporting. Pursuant to the instructions
to Form 20-F, we expect to include this report in our next annual report filed with the SEC, which we currently expect will be filed by no later than
July 31, 2020. We are still in the costly and challenging process of compiling the system and processing documentation necessary to perform the evaluation
needed to comply with Section 404.
Neither our management nor independent registered public accounting firm has ever performed a comprehensive evaluation of our internal
control over financial reporting in accordance with the provisions of the Sarbanes-Oxley Act because no such evaluation has been required, and we
cannot be certain that material weaknesses in our internal control over financial reporting will not develop or be identified. Any failure to achieve and
maintain adequate internal control over financial reporting or to implement required, new or improved controls, or difficulties encountered in their
implementation could cause material weaknesses or other deficiencies in our internal control over financial reporting in the future. If we are unable to
successfully remediate any material weaknesses or other deficiencies in our internal control over financial reporting, the accuracy and timing of our
financial reporting may be adversely affected, and investors may lose confidence in our financial reporting, and the price of our ADSs may decline as
a result. In addition, if we are unable to continue to meet these requirements, we may not be able to remain listed on the NYSE.
We are subject to additional risk due to uncertainty relating to the calculation of LIBOR, EURIBOR and other reference rates and their potential
discontinuance.
The JBIC Loan and the Term Loan Credit Agreement are subject to a floating interest rate calculated in reference to LIBOR, while the
floating rate Euro-denominated senior notes we issued in connection with the Shire Acquisition are subject to floating rate interest calculated in reference
to EURIBOR. LIBOR, EURIBOR and other interest rate, equity, commodity, foreign exchange rate and other types of indices which are deemed to be
“benchmarks” are the subject of ongoing national, international and other regulatory guidance and proposals for reform. Some of these reforms are
already effective while others are still to be implemented. These reforms may cause such “benchmarks” to perform differently than they have performed
in the past or to be discontinued entirely or may have other consequences that cannot be predicted, which could have a material adverse effect on our
financial condition or results of operations or require us to seek to amend the terms of the relevant indebtedness, which may require significant additional
time, effort or money in the form of consent payments or otherwise, and may not be possible on cost-efficient terms or at all.
In particular, regulators and law enforcement agencies in the United Kingdom and elsewhere are conducting criminal and civil investigations
into whether the banks that contribute information to the British Banker Association (the “BBA”) in connection with the daily calculation of LIBOR
may have been under-reporting or otherwise manipulating or attempting to manipulate LIBOR. A number of BBA members banks have entered into
settlements with their regulators and law enforcement agencies, as well as the ICE Benchmark Administration (the current administrator of LIBOR),
which may result in changes to the manner in which LIBOR is determined or the establishment of alternative reference rates. On July 27, 2017, the
Chief Executive of the U.K. Financial Conduct Authority (the “FCA”), which regulates LIBOR, announced that the FCA will no longer persuade or
compel banks to submit rates for the calculation of LIBOR after 2021. Such announcement indicates that the continuation of LIBOR on the current basis
cannot and will not be guaranteed after 2021. Notwithstanding the foregoing, it appears highly likely that LIBOR will be discontinued or modified by
2021. A number of alternatives to LIBOR have been proposed or are being developed, but it is not clear which, if any, will be adopted. Any of these
alternative methods may result in interest payments that are higher than expected or that do not otherwise correlate over time with the payments that
would have been made on such indebtedness for the interest periods if the applicable LIBOR rate was available in its current form. More generally, any
of the foregoing changes, any other changes to LIBOR as a result of national, international and other regulatory guidance and proposals for reform or
other initiatives or investigations, or any further uncertainty surrounding the implementation of such changes, could have a material adverse effect on
affected indebtedness.
At this time, it is not possible to predict the effect that these developments, any discontinuance, modification or other reforms to LIBOR,
EURIBOR or any other reference rate, or the establishment of alternative reference rates may have on LIBOR, EURIBOR, other benchmarks or floating
rate indebtedness.
Risks Relating to the ADSs
A holder of ADSs has fewer rights than a holder of our common stock has, and a holder of ADSs has to act through the depositary to exercise those
rights.
The rights of shareholders under Japanese law to take various actions, including voting their shares, receiving dividends and distributions,
bringing derivative actions, examining a company’s accounting books and records and exercising appraisal rights, are available only to holders of record.
Because the depositary, through its custodian agents, is the record holder of the shares underlying the ADSs, only the depositary can exercise those rights
in connection with the deposited shares. Pursuant to the deposit agreement, the depositary will endeavor, to the extent practicable, to make efforts to
vote or cause to be voted the shares underlying the ADSs as instructed by the holders and will pay to the holders the dividends and distributions collected
from the Company. The depositary and its agents may not be able to send voting instructions to holders of ADSs or carry out their voting instructions
in a timely manner. Furthermore, the depositary and its agents will not be responsible for any failure to carry out any instructions to vote, for the manner
in which any vote is cast or for the effect of any such vote. As a result, holders of ADSs may not be able to exercise their right to vote. Moreover, in the
capacity as an ADS holder, such holder will not be able to bring a derivative action, examine the Company’s accounting books or records or exercise
appraisal rights except through the depositary.
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Rights of shareholders under Japanese law may be more limited than under the laws of other jurisdictions.
Our Articles of Incorporation, Regulations of the Board of Directors, Regulations of the Audit and Supervisory Committee and the Companies
Act govern our corporate affairs. Legal principles relating to such matters as the validity of corporate procedures, directors’ and officers’ fiduciary duties,
and shareholders’ rights may be different from those that would apply to a non-Japanese company. Shareholders’ rights under Japanese law may not be
as extensive as shareholders’ rights under the laws of other jurisdictions. ADS holders may have more difficulty in asserting their rights as a shareholder
than such holders would as shareholders of a corporation organized in another jurisdiction. In addition, Japanese courts may not be willing to enforce
liabilities against the Company in actions brought in Japan that are based upon the securities laws of other jurisdictions.
Because of daily price range limitations under Japanese stock exchange rules, a holder of ADSs who has surrendered his or her ADSs in favor of
shares of our common stock may not be able to sell his/her shares of our common stock at a particular price on any particular trading day, or at all.
Stock prices on Japanese stock exchanges are determined on a real-time basis by the equilibrium between bids and offers. These exchanges
are order-driven markets without specialists or market makers to guide price formation. To prevent excessive volatility, these exchanges set daily upward
and downward price fluctuation limits for each stock, based on the previous day’s closing price. Although transactions may continue at the upward or
downward limit price if the limit price is reached on a particular trading day, no transactions may take place outside these limits. Consequently, a holder
of ADSs who has surrendered his or her ADSs in favor of shares of our common stock wishing to sell on a Japanese stock exchange at a price above or
below the relevant daily limit may not be able to sell his or her shares at such price on a particular trading day, or at all.
U.S. investors may have difficulty in serving process or enforcing a judgment against us or our directors or executive officers.
We are a limited liability, joint stock corporation incorporated under the laws of Japan. Many of our directors and executive officers reside
in Japan, Europe or elsewhere outside of the United States, and a large portion of our assets and the assets of these persons are located in Japan and
elsewhere outside the United States. It may not be possible, therefore, for U.S. investors to effect service of process within the United States upon us or
these persons or to enforce against us or these persons judgments obtained in U.S. courts predicated upon the civil liability provisions of the federal
securities laws of the United States. There is doubt as to the enforceability in Japan, in original actions or in actions for enforcement of judgment of U.S.
courts, of liabilities predicated solely upon the federal securities laws of the United States.
Investors holding less than a full unit of shares will have limited rights as shareholders.
Our Articles of Incorporation provide that 100 shares of our common stock constitute one unit. Although holders of ADSs may withdraw
shares of our common stock constituting less than one unit, in connection with the direct holding of the shares of our common stock, the Companies
Act imposes significant restrictions and limitations on holders of shares of our common stock that do not constitute a full unit. In general, holders of
shares of our common stock constituting less than one unit do not have the right to vote with respect to those shares.
Dividend payments and the amount you may realize upon a sale of our ADSs will be affected by fluctuations in the exchange rate between the U.S.
dollar and the Japanese yen.
Cash dividends, if any, in respect of the shares of our common stock represented by our ADSs will be paid to the depositary in Japanese yen
and then converted by the depositary into U.S. dollars, subject to certain conditions. Accordingly, fluctuations in the exchange rate between the Japanese
yen and the U.S. dollar will affect, among other things, the U.S. dollar amounts a holder of ADSs will receive from the depositary in respect of dividends,
the U.S. dollar value of the proceeds that a holder of ADSs would receive upon sale in Japan of the shares of our common stock obtained upon surrender
of ADSs and the secondary market price of ADSs.
Our shareholders of record on a given record date may not receive the dividend they anticipate.
The customary dividend payout practice of publicly listed companies in Japan may significantly differ from the practices widely followed
or otherwise deemed necessary or fair in foreign markets. We ultimately have a discretion to determine any dividend payment amount to our shareholders
of record as of a record date, including whether we will make any dividend payment to such shareholders at all, only after such record date. For that
reason, our shareholders of record on a given record date may not receive the dividends they anticipate.
ADS holders may not be entitled to a jury trial with respect to claims arising under the deposit agreement, which could result in less favorable
outcomes to the plaintiff(s) in any such action.
The deposit agreement governing the ADSs provides that, to the fullest extent permitted by law, ADS holders waive the right to a jury trial
for any claim they may have against us or the depositary arising out of or relating to our shares, the ADSs or the deposit agreement, which may include
any claim under the U.S. federal securities laws.
If we or the depositary were to oppose a jury trial based on this waiver, the court would have to determine whether the waiver was enforceable
based on the facts and circumstances of the case in accordance with applicable state and federal law. To our knowledge, the enforceability of a contractual
pre-dispute jury trial waiver in connection with claims arising under the federal securities laws has not been finally adjudicated by the United States
Supreme Court. However, we believe that a contractual pre-dispute jury trial waiver provision is generally enforceable, including under the laws of the
State of New York, which govern the deposit agreement, or by a federal or state court in the City of New York, which has jurisdiction over matters
arising under the deposit agreement. In determining whether to enforce a contractual pre-dispute jury trial waiver, courts will generally consider whether
22
a party knowingly, intelligently and voluntarily waived the right to a jury trial. We believe that this would be the case with respect to the deposit agreement
and the ADSs. It is advisable that prospective investors consult legal counsel regarding the jury waiver provision before investing in the ADSs.
As a result, if a holder or beneficial owner of ADSs brings a claim against us or the depositary in connection with matters arising under the
deposit agreement or the ADSs, including claims under federal securities laws, such holder or beneficial owner may not be entitled to a jury trial with
respect to such claims, which may have the effect of limiting and discouraging lawsuits against us or the depositary. If a lawsuit is brought against us
or the depositary under the deposit agreement, it may be heard only by a judge or justice of the applicable trial court, which would be conducted according
to different civil procedures and may result in different outcomes than a trial by jury would have, including outcomes that could be less favorable to the
plaintiff(s) in any such action.
Nevertheless, if this jury trial waiver is not enforced under applicable law, an action could proceed under the terms of the deposit agreement
with a jury trial. No condition, stipulation or provision of the deposit agreement or the ADSs serves as a waiver by any holder or beneficial owner of
ADSs or by us or the depositary of compliance with any substantive provision of the U.S. federal securities laws and the rules and regulations promulgated
thereunder.
Item 4. Information on the Company
A.
History and Development of the Company.
We are a global, values-based, research and development driven biopharmaceutical company with operations in approximately 80 countries.
We bring highly innovative, life changing medicines to patients across the globe, with prescription drugs marketed directly or through our partners in
approximately 100 countries worldwide. Our global workforce is committed to bringing better health and a brighter future to patients. We develop and
market pharmaceutical products to treat a broad range of medical conditions including GI diseases, cancer, neurological and psychiatric diseases, and
rare diseases including immunology and hematology, as well as plasma-derived therapies and vaccines. We are also committed to our corporate social
responsibility program, which is dedicated to global health, and our access to medicine strategy, which aims to increase access to innovative and potentially
lifesaving medicines for patients with some of the highest unmet medical needs across the world.
Our 238-year history started in 1781, when Chobei Takeda began selling traditional Japanese and Chinese medicines in Doshomachi, Osaka.
After Japan’s Meiji Restoration opened the country to increase overseas trade in the late 1860s, we were one of the first companies to begin importing
western medicines into Japan. In 1895, we began our pharmaceutical manufacturing business, and our research division was formed in 1914, allowing
us to begin to introduce our own pharmaceutical products. In 1925, we were incorporated as Chobei Takeda & Co., Ltd. and our name was later changed
to Takeda Pharmaceutical Company Limited. In 1949, our shares were listed on the Tokyo and Osaka stock exchanges. We began expanding into overseas
markets in the 1960s, first in Asia and, subsequently, other markets around the world. We began enhancing our overseas business infrastructure in the
late 1990s, with the formation of new subsidiaries in the United States and Europe.
Since 2014, our efforts have been focused on enhancements to our research and development capabilities and successful cross-border merger
and acquisition activities and post-acquisition integration. For example, in February 2017, we acquired ARIAD, a commercial-stage biotechnology
company and in July 2018, we acquired TiGenix NV, an advanced biopharmaceutical company developing novel stem cell therapies for serious medical
conditions, with the aim to bring new treatment options to patients with gastrointestinal disorders.
Most recently, in January 2019, we completed our acquisition of Shire. With the Shire Acquisition, we have taken the next major step in
our development into a global pharmaceutical company. The Shire Acquisition allows us to create a global, values-based, research and development-
driven biopharmaceutical company with an attractive geographic footprint with a significantly increased presence in the United States, an important and
innovation-driven market. Specifically, the Shire Acquisition strengthens our core therapeutic areas, bringing together Takeda and Shire’s complementary
positions in GI and neuroscience and providing leading positions in rare diseases and plasma-derived therapies to complement our existing strength in
oncology and focused efforts in vaccines. It also creates a highly complementary, robust, modality-diverse pipeline and a strengthened research and
development engine focused on innovation.
During the three fiscal years ended March 31, 2019, we have also divested a number of businesses and assets in non-core areas. For example,
in April 2017, we completed the sale of our shares in Wako Pure Chemical to FUIJIFILM Corporation and in December 2017, we entered into an
agreement with Takashimaya Company Limited to sell our Tokyo Takeda building and the Takeda Shin-Edobashi building. Further, in July 2018, we
sold and divested all our shares and assets in Multilab Indústria e Comércio de Produtos Farmacêuticos Ltda. to Novamed Fabricação de Produtos
Farmacêuticos Ltda and in August 2018, we sold and divested all our shares and assets in Guangdong Techpool Bio-Pharma Co., Ltd. to Shanghai
Pharmaceutical Holding Co. Ltd. We will continue to divest certain businesses and assets as we integrate Shire and focus on our core business. For
example, on May 9, 2019, we announced the sales of two of our non-core businesses, Xiidra® (lifitegrast ophthalmic solution) and TachoSil™ (Fibrin
Sealant Patch). For additional details on these transactions, see Note 33 to our audited consolidated financial statements included in this annual report.
Our principal capital expenditures during the three fiscal years ended March 31, 2019 consisted of additions to property, plant and equipment
and additions to intangible assets. In the fiscal years ended March 31, 2017, 2018 and 2019, excluding acquisitions, we made capital expenditures
(consisting of the additions to property, plant and equipment and intangible assets recorded on our consolidated balance sheet) of ¥148.1 billion,
¥124.1 billion and ¥244.6 billion, respectively, including the following highlights:
•
In the fiscal year ended March 31, 2017, we invested ¥8.3 billion to prepare the manufacturing facility in Brooklyn Park, Minnesota
acquired from Baxalta US. Inc. for the production of ENTYVIO;
23
•
•
In the fiscal year ended March 31, 2018, we invested ¥17.9 billion to construct our new global headquarters in Tokyo. We also invested
¥11.4 billion to purchase manufacturing equipment at our German subsidiary, Takeda GmbH, including ¥4.9 billion in equipment for
manufacturing of vaccines for dengue fever; and
In the fiscal year ended March 31, 2019, we received an additional 20-year extension agreement (from 2030 to 2050) for our two leased
properties in Cambridge, Massachusetts. The total lease liability for these properties including this renewal option that we are reasonably
certain to exercise is ¥88.8 billion as of March 31, 2019.
We currently have various capital expenditures projects in process, the most significant of which includes the construction of a biologics
facility in Dunboyne, Ireland, which will be funded through internally generated cash flows.
The address of our global head office is 1-1, Nihonbashi-Honcho 2-Chome, Chuo-ku, Tokyo, 103-8668, Japan; telephone number:
81-3-3278-2306. Takeda’s agent in the United States in connection with this annual report is Shire HGT, Inc., 300 Shire Way, Lexington, MA 02421
U.S.A., telephone number: 1-617-349-0200.
The SEC maintains an Internet site that contains reports, proxy and information statements, and other information regarding issuers that file
electronically with the SEC at www.sec.gov. As a foreign private issuer, we are exempt from the rules under the Securities Exchange Act of 1934 (the
"Exchange Act") prescribing the furnishing and content of proxy statements to shareholders. Our corporate website is www.takeda.com.
B.
Business Overview.
We are a global, values-based, research and development-driven biopharmaceutical company with an innovative portfolio, engaged primarily
in the research, development, production and marketing of pharmaceutical products. Our mission is to strive towards a better health and a brighter future
for people worldwide through leading innovation in medicine. Our culture is based on the achievement of this mission by acting with integrity, fairness,
honesty and perseverance and prioritizing the patient, trust, reputation and the business.
Our three strategic priorities to drive sustainable mid to long-term growth are business area focus, our research and development engine and
financial strength.
We are focused on five key business areas of GI, rare diseases, plasma-derived therapies, oncology, and neuroscience. We believe these five
business areas will drive our future growth. We have been making targeted acquisitions and divestitures to further increase our level of focus on these
areas and plan to continue to refine our business portfolio going forward.
Our research and development engine is based on a therapeutic area focus, a leading partnership model and patient-centric, science-driven
culture of innovation. Our strengthened and revitalized research and development engine is focused on the therapeutic areas of oncology, GI, rare diseases
and neuroscience with targeted investments in plasma-derived therapies and vaccines. In order to deliver value in areas of high unmet medical needs,
we strive to progress our pipelines by focusing on innovative medicines.
Our financial strength involves driving margin expansion and generating cash flows to invest in the business, to deleverage and to return
cash to shareholders. We also are prioritizing selected disposal of non-core assets to generate cash in order to accelerate the pace of deleveraging.
We are also focused on successfully executing the integration of Shire while sustaining business momentum. The execution of our integration
plan is underway and we believe that the integration will have relatively minimal disruption on the business and pipeline due to the strong strategic and
geographic fit of the two companies. We also believe that we will experience minimal disruption to our research and development efforts as we are
adding rare diseases to our already defined research and development model. We believe a smooth integration will result in a stronger and more innovative
portfolio supported by a lean and focused organization.
Our key growth driver products will be derived from 14 global brands in five business areas and include: ENTYVIO, GATTEX/REVESTIVE,
ALOFISEL, NATPARA, ADYNOVATE/ADYNOVI, TAKHZYRO, ELAPRASE, VPRIV, GAMMAGARD LIQUID, HYQVIA, CUVITRU, ALBUMIN/
FLEXBUMIN, NINLARO, and ALUNBRIG.
The following is a summary of our principal products by key business area. Revenues attributable to products acquired as part of the Shire
Acquisition for the year ended March 31, 2019 given in this section refer to revenues recorded on our consolidated statement of income following the
completion of the Shire Acquisition on January 8, 2019.
In GI, our principal products include:
•
ENTYVIO (vedolizumab), a treatment for moderate to severe ulcerative colitis and Crohn’s disease. Sales of ENTYVIO have grown
strongly since its launch in 2014 to become our top selling product in the fiscal year ended March 31, 2019. ENTYVIO is now approved
in more than 50 countries worldwide, and we continue to seek approval for ENTYVIO in additional countries. In the fiscal year ended
March 31, 2019, our revenue from ENTYVIO was ¥269.2 billion.
24
•
•
•
TAKECAB (vonoprazan fumurate), a treatment for acid-related diseases. TAKECAB was launched in Japan in 2015 and has achieved
significant growth following the expiration of the prescription limitation period in March 2016. In the fiscal year ended March 31,
2019, our revenue from TAKECAB was ¥58.2 billion.
GATTEX/REVESTIVE (teduglutide [rDNA origin]) for injection is the first prescription medicine for the long-term treatment of adults
with short bowel syndrome (“SBS”) who are dependent on parenteral support. We added GATTEX/REVESTIVE to our GI portfolio
with the acquisition of Shire, which was completed in January 2019. In May 2019, the FDA approved extending the indication of
GATTEX for children 1 year of age and older with SBS. In the fiscal year ended March 31, 2019, our revenue from GATTEX/REVESTIVE
was ¥12.8 billion.
ALOFISEL (darvadstrocel), previously Cx601, a treatment for complex perianal fistulas in adult patients with nonactive/mildly active
luminal Crohn’s disease, when fistulas have shown an inadequate response to at least one conventional or biologic therapy. ALOFISEL
was approved in the EU in 2018 which marked the first allogenic stem cell therapy to receive central marketing authorization (“MA”)
approval in Europe. In the fiscal year ended March 31, 2019, our revenue from ALOFISEL was ¥0.05 billion.
In rare diseases, our principal products are:
•
•
•
•
•
•
NATPARA/NATPAR (parathyroid hormone) for injection is indicated as an adjunct to calcium and vitamin D to control hypocalcemia
in patients with hypoparathyroidism (“HPT”). HPT is a rare condition in which the parathyroid glands fail to produce sufficient amounts
of parathyroid hormone (“PTH”) or where the PTH lacks biologic activity. We added NATPARA/NATPAR to our rare diseases portfolio
with the acquisition of Shire, which was completed in January 2019. In the fiscal year ended March 31, 2019, our revenue from
NATPARA/NATPAR was ¥7.1 billion.
ADYNOVATE/ADYNOVI (antihemophilic factor (recombinant) [PEGylated]) is an extended half-life recombinant factor VIII treatment
for hemophilia A based on ADVATE. ADYNOVATE/ADYNOVI uses the same manufacturing process as ADVATE and adds a proven
technology, PEGylation (a chemical process that prolongs the amount of time a compound remains in circulation, potentially allowing
for fewer injections), which we exclusively licensed from Nektar Therapeutics. We added ADYNOVATE/ADYNOVI to our rare diseases
portfolio with the acquisition of Shire, which was completed in January 2019. In the fiscal year ended March 31, 2019, our revenue
from ADYNOVATE/ADYNOVI was ¥10.7 billion.
TAKHZYRO (lanadelumab-flyo) injection, a fully human monoclonal antibody that specifically binds and decreases plasma kallikrein.
TAKHZYRO is the only monoclonal antibody (mAb) that provides targeted inhibition of plasma kallikrein, an enzyme which is
chronically uncontrolled in people with hereditary angioedema (“HAE”), to help prevent attacks. We added TAKHZYRO to our rare
diseases portfolio with the acquisition of Shire, which was completed in January 2019. In the fiscal year ended March 31, 2019, our
revenue from TAKHZYRO was ¥9.7 billion.
ELAPRASE (idursulfase), an enzyme replacement treatment for Hunter syndrome (also known as Mucopolysaccharidosis Type II or
MPS II). We added ELAPRASE to our rare diseases portfolio with the acquisition of Shire, which was completed in January 2019. In
the fiscal year ended March 31, 2019, our revenue from ELAPRASE was ¥15.1 billion.
REPLAGAL (agalsidase alfa for infusion), an enzyme replacement marketed for the treatment of Fabry disease outside of the U.S.
Fabry disease is a rare, inherited genetic disorder resulting from a deficiency in the activity of the lysosomal enzyme alpha-galactosidase
A, which is involved in the breakdown of fats. We added REPLAGAL to our rare diseases portfolio with the acquisition of Shire, which
was completed in January 2019. In the fiscal year ended March 31, 2019, our revenue from REPLAGAL was ¥11.4 billion.
VPRIV (velaglucerase alfa for injection), an enzyme replacement treatment for type 1 Gaucher disease. We added VPRIV to our rare
diseases portfolio with the acquisition of Shire, which was completed in January 2019. In the fiscal year ended March 31, 2019, our
revenue from VPRIV was ¥8.7 billion.
In the fiscal year ended March 31, 2019, our revenue from plasma-derived therapy products was ¥111.7 billion. In plasma-derived
therapies, our principal products are:
•
•
•
GAMMAGARD LIQUID (Immune Globulin Intravenous (Human) 10%), a liquid formulation of the antibody replacement therapy
immunoglobulin ("IG") product. GAMMAGARD LIQUID is used to treat adult and pediatric patients two years of age or older with
primary immunodeficiencies (“PID”) and can be administered either intravenously or subcutaneously. GAMMAGARD LIQUID is also
used to treat adult patients with multifocal motor neuropathy (“MMN”) administered intravenously. KIOVIG is the brand name used
for GAMMAGARD LIQUID in many countries outside of the U.S. KIOVIG is approved in Europe for use by patients with PID and
certain secondary immunodeficiencies, and for adults with MMN. We added GAMMAGARD LIQUID to our plasma-derived therapies
portfolio with the acquisition of Shire, which was completed in January 2019.
GAMMAGARD S/D [Immune Globulin Intravenous (Human)] IgA less than 1 μg/mL in a 5% solution is indicated for the treatment
of PID in patients two years old and older. GAMMAGARD S/D is also indicated for prevention of bacterial infections in
hypogammaglobulinemia and/or recurrent bacterial infections associated with Bcell chronic lymphocytic leukemia (“CLL”), treatment
of adult patients with chronic idiopathic thrombocytopenic purpura (“ITP”) to increase platelet count and to prevent and/or control
bleeding, and prevention of coronary artery aneurysms associated with Kawasaki Syndrome in pediatric patients. GAMMAGARD S/
D is provided for patients who require a low IgA content in their IV treatment (IgA less than 1 μg/mL in a 5% solution). We added
GAMMAGARD S/D to our plasma-derived therapies portfolio with the acquisition of Shire, which was completed in January 2019.
HYQVIA [Immune Globulin Infusion 10% (Human) with Recombinant Human Hyaluronidase] is a product consisting of human normal
IG and recombinant human hyaluronidase (licensed from Halozyme). HYQVIA is the only subcutaneous IG treatment for PID patients
25
with a dosing regimen requiring only one infusion up to once per month and one injection site per infusion to deliver a full therapeutic
dose of IG. We added HYQVIA to our plasma-derived therapies portfolio with the acquisition of Shire, which was completed in January
2019. HYQVIA is approved in Europe for use by patients with PID syndromes and myeloma or CLL with severe secondary
hypogammaglobulinemia and recurrent infections, and in the United States for adults with PID.
•
•
CUVITRU is an Immune Globulin Subcutaneous (Human) (“IGSC”), 20% Solution indicated as replacement therapy for primary
humoral immunodeficiency in adult and pediatric patients two years of age and older. CUVITRU is also indicated in the EU for the
treatment of certain secondary immunodeficiencies. CUVITRU is the only 20% subcutaneous IG treatment option without proline and
with the ability to infuse up to 60 mL (12 grams) per site and 60 mL per hour, per site as tolerated, resulting in fewer infusion sites and
shorter infusion durations compared to other conventional subcutaneous IG treatments. We added CUVITRU to our plasma-derived
therapies portfolio with the acquisition of Shire, which was completed in January 2019.
FLEXBUMIN (Human Albumin in a bag) and Human Albumin (glass) are available as 5% and 25% solutions. Both products are
indicated for hypovolemia, hypoalbuminemia due to general causes and burns, and for use during cardiopulmonary bypass surgery as
a component of the pump prime. FLEXBUMIN 25% is also indicated for hypoalbuminemia associated with adult respiratory distress
syndrome (“ARDS”) and nephrosis, and hemolytic disease of the newborn (“HDN”). We added FLEXBUMIN to our plasma-derived
therapies portfolio with the acquisition of Shire, which was completed in January 2019.
In oncology, our principal products include:
•
•
•
NINLARO (ixazomib), the first oral proteasome inhibitor for the treatment of multiple myeloma (“MM”). NINLARO has experienced
a strong uptake in sales since launching in the United States in 2015. NINLARO was approved in the EU in 2016 and in Japan in 2017,
and we are seeking marketing authorization in a number of additional countries. In the fiscal year ended March 31, 2019, revenue from
NINLARO was ¥62.2 billion.
ADCETRIS (brentuximab vedotin), an anti-cancer agent used to treat Hodgkin lymphoma (“HL”) and systemic anaplastic large cell
lymphoma (“sALCL”). ADCETRIS was launched in the United States, the EU and Japan in 2011, 2012 and 2014, respectively.
ADCETRIS has received marketing authorization by regulatory authorities in more than 60 countries worldwide. We jointly develop
ADCETRIS with Seattle Genetics, Inc. and have commercialization rights in countries outside the United States and Canada. In the
fiscal year ended March 31, 2019, our revenue from ADCETRIS was ¥42.9 billion.
ALUNBRIG (brigatinib), an orally administered small molecule anaplastic lymphoma kinase (“ALK”) inhibitor used to treat non-small
cell lung cancer (“NSCLC”). ALUNBRIG was developed by ARIAD Pharmaceuticals. ALUNBRIG was granted accelerated approval
in the United States in April 2017, and the European Commission granted the product marketing authorization in November 2018. In
the fiscal year ended March 31, 2019, our revenue from ALUNBRIG was ¥5.2 billion.
In neuroscience, our principal products are:
•
•
VYVANSE (lisdexamfetamine dimesylate) is a stimulant medication indicated for the treatment of attention deficit hyperactivity disorder
(“ADHD”) in patients ages six and above and for the treatment of moderate to severe binge eating disorder in adults. We added
VYVANSE to our neuroscience portfolio with the acquisition of Shire, which was completed in January 2019. In the fiscal year ended
March 31, 2019, our revenue from VYVANSE was ¥49.4 billion.
TRINTELLIX (vortioxetine), an antidepressant indicated for the treatment of major depressive disorder in adults. TRINTELLIX was
co-developed with H. Lundbeck A/S, and was launched in 2014 in the United States. We have commercialization rights in the United
States and Japan. In the fiscal year ended March 31, 2019, our revenue from TRINTELLIX was ¥57.6 billion in the United States.
For a breakdown of revenues by geographic region, see Note 4 to our audited consolidated financial statements included in this annual report.
Research and Development
Research and development of pharmaceutical products is a lengthy and expensive process that can span more than 10 years. The process
includes evaluations of the product’s efficacy and safety, application for approval and investigation and approval by regulatory authorities. Only a small
number of compounds pass such detailed investigation and are used in clinical treatments. Once approved, there is ongoing research and development
support for marketed products, including medical affairs and other investments.
Clinical trials, which comply with regional and international regulatory guidelines, generally take five to seven years or longer and require
substantial expenditures. As a result, only a small fraction of compounds that enter the clinical trials results in commercially viable products. In general,
clinical trials are performed in accordance with the guidelines set by the International Conference on Harmonisation of Technical Requirements for
Registration of Pharmaceuticals for Human Use. The relevant regulatory authorities are the MHLW for Japan, the FDA for the United States and the
EMA for the EU.
26
The three phases of human clinical trials, which may overlap with each other, are as follows:
Phase I (“P-I”) clinical trials
Conducted using a small group of healthy adult volunteers in order to evaluate safety and absorption, distribution,
metabolism and excretion of the drug.
Phase II (“P-II”) clinical trials
Conducted using a small group of patient volunteers in order to evaluate safety, efficacy, dosage and administration
methods. P-II clinical trials may be divided into two sub-categories, P-IIa and P-IIb. P-IIa are usually pilot studies
designed to demonstrate clinical efficacy or biological activity. P-IIb studies look to find the optimum dose at
which the drug shows biological activity with minimal side-effects.
Phase III (“P-III”) clinical trials
Conducted using a large number of patient volunteers in order to evaluate safety and efficacy in comparison to
other medications already available or placebo.
Of these three phases, Phase III requires the largest expenditures and thus the decision to proceed with Phase III testing is a critical business
decision in the drug development process. For those drug candidates that pass Phase III clinical trials, a New Drug Application ("NDA") or a Marketing
Authorization Application (“MAA”) is submitted to the relevant governmental authorities for approval and subsequent launch of the drug. The preparation
of an NDA or MAA involves considerable data collection, verification, analysis and expense. Even after the launch of the product, health authorities
require post-marketing surveillance of adverse events, and they may request a post-marketing study to provide additional information regarding the risks
and benefits of the product.
In July 2016, we initiated a five-year research and development transformation program to re-invigorate the pipeline and build an agile,
global research and development organization driven by innovative science. A significant component of the program has been an intensive focus in the
following three key areas:
•
•
•
Therapeutic area focus: Leveraging therapeutic area expertise to progress innovative assets.
Partnerships and capabilities: Enhancing capabilities internally and through external collaborations.
Innovative research engine: Developing new technologies and new modalities to treat disease.
Our research and development efforts are focused in four key therapeutic areas of oncology, GI, rare diseases and neuroscience, plus the
plasma-derived therapies and vaccines business areas.
We have also concentrated our in-house research and development operations in Japan and the United States. We intend to integrate the
legacy Shire research and development operations into ours.
Our key in-house research and development facilities include:
•
•
•
Shonan Heath Innovation Park: Located in Fujisawa and Kamakura in Kanagawa Prefecture in Japan, the Shonan Health Innovation
Park ("Shonan iPark") was established in 2011 as the Shonan Research Center, and is our primary location for neuroscience research.
In April 2018, we launched Shonan iPark by transforming the Shonan Research Center to enhance scientific innovation. Shonan iPark
aims to gather 3,000 researchers by the year 2020 and become a place where experts from the pharmaceutical industry, including
venture start-ups, government and academia, can gather and incubate and accelerate research initiatives to create health solutions.
Boston Research and Development Site: Our Boston research and development hub is located in Cambridge, Massachusetts in the
United States. Our Boston site is the center of our global oncology and GI research and development and also supports research and
development in other therapeutic areas including plasma-derived therapies and vaccines, and research in immunomodulation and
biologics.
San Diego Research and Development Site: Our research and development site located in San Diego, California in the United States
supports research and development of specialized technologies in the GI and neuroscience areas.
In addition to our concentrated efforts to increase our in-house research and development capabilities, external partnerships with third-party
partners are a key component of our strategy for enhancing our research and development pipeline. In the fiscal year ended March 31, 2019, we entered
into more than 40 such new partnerships. Our strategy to expand and diversify our external partnerships allows us to take part in research of a wide
variety of new products and increases the chances that we will be able to take part in a major research-related breakthrough. See “–Licensing and
Collaboration” for further information on our research and development collaborations.
The following summarizes our research and development activities within each of our therapeutic and business areas. The compounds in
our pipeline disclosed within the key therapeutic and business areas below are in various stages of development, and the contents of the pipeline may
change as compounds currently under development are removed and new compounds are introduced. Whether the compounds listed below are ever
successfully released as products depends on various factors, including the results of pre-clinical and clinical trials, market conditions for various drugs
and regulatory approvals. The listings in the tables below are limited to the U.S., EU, Japan, and China, but we are also conducting development activities
in other regions. "Global" refers to U.S., EU, Japan, and China.
Oncology
In oncology, we endeavor to deliver novel medicines to patients with cancer worldwide through the commitment to breakthrough innovation
and a passion for improving the lives of patients. This therapeutic area focuses on three key areas (1) building on our foundational expertise in hematologic
27
malignancies through continued investment in lifecycle management programs for marketed products NINLARO, ADCETRIS and ICLUSIG, as well as
in pipeline assets in multiple myeloma, acute myeloid leukemia and myelodysplastic syndromes and other blood cancers, (2) further developing our
portfolio in lung cancer and (3) pursuing novel immuno-oncology targets and next-generation platforms with external partners, as well as exploring
innovative cell therapies.
Our oncology pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent
developments, is as follows:
Development code
Brand name
(country/region)(1)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
SGN-35
ADCETRIS (EU,
Japan)
CD30 monoclonal
antibody-drug
Conjugate
(injection)
ALUNBRIG (U.S.,
EU)
ALK inhibitor
(oral)
Front line Peripheral
T-cell Lymphoma
(“PTCL”)
Relapsed/ refractory
Hodgkin lymphoma
Relapsed/ refractory
systemic anaplastic
large-cell
lymphoma (“sALCL”)
1L ALK-positive non-
small cell lung cancer
2L ALK-positive non-
small cell lung cancer
in patients previously
treated with ALK
inhibitors
2L ALK-positive non-
small cell lung cancer
in patients progress on
2nd generation TKI
(tyrosine kinase
inhibitors)
2L ALK-positive non-
small cell lung cancer
(head to head with
alectinib)
In-license
(Seattle
Genetics, Inc.)
EU
Japan
China
P-III
Filed (March 2019)
Filed (March 2019)
China
Filed (March 2019)
U.S.
EU
China
Japan
China
P-III
P-III
P-I
P-II(a)
P-II(a)
Global
P-II
In-house
Global
P-III
28
Development code
Brand name
(country/region)(1)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
Newly diagnosed
multiple myeloma
Maintenance therapy
in patients with newly
diagnosed multiple
myeloma following
autologous stem cell
transplant
Maintenance therapy
in patients with newly
diagnosed multiple
myeloma not treated
with stem cell
transplant
Relapsed/refractory
primary amyloidosis
Relapsed/refractory
multiple myeloma
(doublet regimen with
dexamethasone)
Relapsed/refractory
multiple myeloma
(triplet regimen with
daratumumab and
dexamethasone)
Front line Philadelphia
chromosome-positive
acute lymphoblastic
leukemia
Dose ranging study for
TKI resistant patients
with
chronic-phase chronic
myeloid leukemia
High-risk
myelodysplastic
syndromes,
chronic
myelomonocytic
leukemia,
low-blast acute
myelogenous leukemia
Prostate cancer
1L renal cell
carcinoma in
combination with
nivolumab
2L renal cell
carcinoma
2L hepatocellular
carcinoma
MLN9708
NINLARO
Proteasome inhibitor
(oral)
ICLUSIG
BCR-ABL inhibitor
(oral)
TAK-924
NEDD 8 activating
enzyme inhibitor
(injection)
TAK-385
LH-RH antagonist
(oral)
Multi-targeted kinase
inhibitor (oral)
Global
P-III
Japan
U.S.
EU
China
Filed (April 2019)
P-III
P-III
P-III
Global
P-III
In-house
Global
U.S.
EU
Japan
P-III(3)
P-III
P-III
P-III
Global
P-II
U.S.
P-III
U.S.
P-II(b)
In-house
In-house
In-house
P-III
P-III
P-III
P-III
P-I
P-III
U.S.
EU
Japan
Japan
China
Japan
Japan
Japan
29
In-license
(Exelixis, Inc.)
Filed (April 2019)
P-II(a)
TAK-659
<->
TAK-931
< ->
TAK-788
<->
TAK-079
<->
TAK-164
<->
TAK-573
<- >
TAK-981
<- >
TAK-252/SL-279252
Development code
Brand name
(country/region)(1)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
PARPl/2 inhibitor
(oral)
TAK-228
mTORCl/2 inhibitor
(oral)
SYK/FLT3 kinase
inhibitor
(oral)
CDC7 inhibitor
(oral)
Ovarian cancer -
maintenance
Ovarian cancer –
salvage
Endometrial cancer
Diffuse large 8-cell
lymphoma
Hematologic
malignancies
Squamous esophageal
cancer, squamous non-
small cell lung cancer
Japan
Japan
U.S.
-
-
-
P-II
P-II
P-II(b)
P-II(a)
P-I
In-license
(GlaxoSmithKline plc)
In-house
In-house
P-II(a)
In-house
EGFR/ HER2 exon 20
inhibitor
(oral)
Non-small cell lung
cancer with Exon-20
insertion
Anti-CD38
monoclonal antibody
(injection)
Anti-guanylyl cyclase
C antibody
drug conjugate
(injection)
CD38-targeted lgG4
genetically
fused with an
attenuated IFNa
(injection)
SUMO inhibitor
(injection)
PD-1-Fc-OX40L
(injection)
Relapsed/refractory
multiple myeloma
Systemic lupus
erythematosus
GI malignancies
Relapsed/refractory
Multiple myeloma
Multiple cancers
Solid tumors
Global
P-II
In-house
-
-
-
-
-
-
P-I
P-I
P-I
P-I
P-I
P-I
In-house
In-house
In-license
(Teva
Pharmaceutical
Industries Ltd.)
In-house
In-license
(Shattuck Labs, Inc.)
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
On June 6, 2019, Takeda announced that this P-III trial did not meet the first of two primary endpoints and Takeda decided to discontinue this
trial.
(2)
(3)
30
GI
In GI, we focus on delivering innovative, life-changing therapeutics for patients with GI and liver diseases. We are expanding our position
in specialty GI with ENTYVIO and progressing a pipeline built through partnerships exploring opportunities in motility disorders, celiac disease, liver
disease and the microbiome.
Our GI pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent developments, is as
follows:
Development Code
Brand name
(country/region)(1)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
MLN0002
ENTYVIO
Humanized
monoclonal antibody
against a47 integrin
(injection)
Crohn's disease
Ulcerative colitis
Subcutaneous
formulation for
ulcerative colitis
Subcutaneous
formulation for
Crohn's disease
Adalimumab head-to-
head in patients with
ulcerative colitis
Graft-versus-host
disease prophylaxis in
patients undergoing
allogeneic
hematopoietic stem
cell transplantation
Japan
China
China
U.S.
EU
Japan
U.S.
EU
Japan
Filed (July 2018)(3)
P-III
P-III
Filed (March 2019)
Filed (March 2019)
P-III
P-III
Filed (March 2019)
P-III
Global
P-III
In-house
Europe
P-III
Cx601
ALOFISEL (EU)
A suspension of
allogeneic expanded
adipose-derived stem
cell (injection)
Refractory complex
perianal fistulas in
patients with Crohn’s
disease
U.S.
Japan
P-III
P-III
In-house
Acid-related diseases
China
Filed (February 2018)
TAK-438
TAKECAB
Potassium-competitive
acid
blocker
(oral)
TAK-633/SHP633
GATTEX (U.S.)/
REVESTIVE (EU)
GLP-2 analogue
(injection)
Gastro-esophageal
reflux disease in
patients who have a
partial response
following treatment
with a proton pump
inhibitor
Short bowel syndrome,
pediatric indication
Short bowel syndrome,
adult
TAK-721/SHP621
Glucocorti costeroid
(oral)
Eosinophilic
esophagitis
EU
P-II(b)
U.S.
Japan
Japan
U.S.
Filed (September
2018)(4)
P-III
P-III
P-III
In-house
In-house
In-house (Partnership
with UCSD and Fortis
Advisors)
TAK-906(5)
< ->
Dopamine D2/D3
receptor antagonist
(oral)
Gastroparesis
-
P-II(b)
In-house
31
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
Development Code
Brand name
(country/region)(1)
TAK-954
<->
TIMP-GLIA
<->
TAK-951
<->
TAK-671
<->
5-HT4-
hydroxytryptamine
receptor agonist
(injection)
Tolerizing Immune
Modifying
nanoParticle (TIMP)
(injection)
Post-operative
gastrointestinal
dysfunction
Celiac disease
Peptide agent
Nausea and vomiting
Protease inhibitor
(injection)
Acute pancreatitis
TAK-018/EB8018
<->
FimH antagonist (oral) Crohn's disease
TAK-681
<->
Kuma062
<->
GLP-2 long-acting
analogue (injection)
Short bowel syndrome
Glutenase
(oral)
Celiac disease
-
-
-
-
-
-
-
P-II(b)
In-license (Theravance
Biopharma, Inc.)
P-II(a)
P-I
P-I
P-I
P-I
P-I
In-license (Cour
Pharmaceutical
Development
Company, Inc.)
In-house
In-house (Co-
development with
Samsung Bioepis Co,
Ltd)
In-license (Enterome
Bioscience SA)
In-house
In-license (PvP
Biologics, Inc.)
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
On May 22, 2019, Takeda announced that the MHLW approved an additional indication for the treatment of moderately to severely active Crohn's
disease in Japan.
On May 17, 2019, Takeda announced that the FDA approved extending this indication to pediatric patients 1 year of age and older with short
bowel syndrome who need additional nutrition or fluids from intravenous feeding (parenteral support).
TAK-906 was previously known as ATC 1906. In March 2017, Takeda executed its option right to acquire Altos Therapeutics, LLC.
(2)
(3)
(4)
(5)
Rare diseases
We acquired our rare disease business and pipeline through our acquisition of Shire. We focus on (1) rare immunology (e.g., Hereditary
angioedema) including through recently launched TAKHZYRO to transform the treatment paradigm, (2) rare hematology with the broadest portfolio
across our competitors in hematology and (3) rare metabolic diseases, focused on addressing with approved treatments for Fabry disease, Hunter syndrome
and Gaucher disease.
Our rare disease pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent developments,
is as follows:
Development Code
Brand name
(country/region)(1)
TAK-743/SHP643
TAKHZYRO (U.S.,
EU)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
Plasma kallikrein
inhibitor (injection)
Hereditary
angioedema
China
Filed (December 2018)
In-house
TAK-672/SHP672
<->
OBIZUR (U.S., EU)
Antihemophilic factor
[recombinant], porcine
sequence (injection)
Congenital hemophilia
A with inhibitors
U.S.
EU
P-III
P-III
Purchased (IPSEN)
32
Development Code
Brand name
(country/region)(1)
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
TAK-577/SHP677
<->
VONVENDI U.S.),
VEYVONDI (EU)
von Willebrand factor
[recombinant]
(injection)
TAK-660/SHP660
<->
ADYNOVATE (U.S.),
ADYNOVI (EU)
Antihemophilic Factor
(recombinant),
PEGylated
(injection)
Prophylactic treatment
of von Willebrand
disease
Pediatric on-demand
treatment of von
Willebrand disease
Global
Global
Pediatric hemophilia A
EU
TAK-755/SHP655
<->
Replacement of the
deficient-ADAMTS13
enzyme (injection)
Congenital thrombotic
thrombocytopenic
purpura
TAK-620/SHP620
Benzimidazole
riboside inhibitor
(oral)
Cytomegalovirus
infection in transplant
patients
U.S.
EU
U.S.
EU
TAK-607 /SHP607
<->
TAK-609/SHP609
<->
Insulin- like Growth
Factor / IGF
Binding Protein
(injection)
Recombinant human
iduronate-2 -sulfatase
for intrathecal
administration
(injection)
Chronic lung disease
-
Hunter syndrome
central nervous system
(“CNS”)
U.S.
EU
cTAK-611/SHP611
<->
Recombinant human
arylsulfatase A
(injection)
Metachromatic
leukodystrophy
Gene therapy to
restore
endogenous FVIII
expression
Fusion protein of
iduronate-2-sulfatase
+antibody (injection)
Hemophilia A
Hunter syndrome CNS
-
-
-
TAK-754/SHP654
<->
TAK-531/SHP631
<->
TAK-834/SHP634
<->
NATPARA (U.S.),
NATPAR (EU)
Parathyroid hormone
(injection)
Hypoparathyroidism
Japan
P-III
P-III
P-III
P-III
P-III
P-III
P-III
P-II
P-II
P-II
In-house
In-house
In-house
In-license (KM
Biologics, Co, Ltd.)
In-license
(GlaxoSmithKline plc)
In-house
In-house
P-I/II
In-house
P-I/II
P-I
P-I
In-license
(Askepios
Biopharmaceutical,
Inc.)
In-license
(ArmaGen, Inc.)
In-house
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
(2)
33
Neuroscience
In neuroscience, we aim to bring innovative medicines to patients suffering from neurologic and psychiatric diseases for whom there are
no treatments available. We are expanding our presence in psychiatric diseases through continued investment in TRINTELLIX for major depressive
disorder and the ADHD portfolio acquired from Shire. We are also building our pipeline in neurology (e.g., Alzheimer's disease, Parkinson's disease)
and selected rare CNS diseases through a combination of in-house expertise and collaboration with partners.
Our neuroscience pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent developments,
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
is as follows:
Development Code
Brand name
(country/region)(1)
Lu AA21004
TRINTELLIX
TAK-815/SHP615
BUCCOLAM (EU)
TAK-831
<->
TAK-935
<->
WVE-120101
<->
WVE-120102
<->
Multimodal anti-
depressant
(oral)
GABA Allosteric
Modulator
(oral)
Major depressive
disorder
Status epilepticus
(seizures)
D-amino acid oxidase
(“DAAO”)
inhibitor (oral)
Negative symptoms
and/or cognitive
impairment associated
with schizophrenia
CH24H inhibitor
(oral)
Rare pediatric
epilepsies
mHTT SNP1 antisense
oligonucleotide
(injection)
mHTT SNP2 antisense
oligonucleotide
(injection)
Huntington's disease
Huntington's disease
Negative symptoms
and/or cognitive
impairment associated
with schizophrenia
Parkinson's disease
Kabuki syndrome
Treatment resistant
depression
TAK-041
<->
GPR139 agonist
(oral)
MEDI1341
<->
TAK-418
<->
TAK-653
<->
TAK-925
<->
Alpha-synuclein
antibody
(injection)
LSDl1 inhibitor
(oral)
AMPA receptor
potentiator
(oral)
Orexin 2R agonist
(injection)
Narcolepsy
Japan
Japan
Filed (September
2018)
In-license
(H. Lundbeck
A/S)
P-III
In-house
-
-
-
-
-
-
-
-
-
P-II(a)
In-house
P-II(a)
P-I/II
P-I/II
P-I
P-I
P-I
P-I
P-I
In-house (Co-
development with
Ovid Therapeutics)
In-license
(Wave Life
Sciences Ltd.)
In-license
(Wave Life
Sciences Ltd.)
In-house
In-license
(AstraZeneca plc)
In-house
In-house
In-house
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
(2)
Plasma-derived therapies
We acquired our plasma derived therapies business and pipeline through our acquisition of Shire. In plasma-derived therapies, we focus on
developing products which are essential for effectively treating patients with a variety of rare, life-threatening, chronic and genetic diseases across the
world.
34
Our plasma-derived therapies pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent
developments, is as follows:
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
Development Code
Brand name
(country/region)(1)
TAK-616/SHP616
<->
CINRYZE
Cl INH inhibits the
complement system
(injection)
Hereditary angioedema
Japan
TAK-771/SHP671
<->
HYQVIA (U.S., EU)
Immunoglobulin
(lgG) +
recombinant
hyaluronidase
replacement therapy
(injection)
Pediatric indication for
primary
immunodeficiency
Chronic inflammatory
demyelinating
polyradiculoneuropathy
U.S.
U.S.
EU
P-III
P-III
P-III
P-III
In-house
In-house (Partnership
with Halozyme
Therapeutics, Inc.)
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
(2)
Vaccines
In vaccines, we apply innovation to develop solutions to treat infectious diseases such as dengue, zika, norovirus, and polio. To support the
expansion of our pipeline and the development of our programs, we entered in partnerships with government organizations (in Japan, the U.S., and
Singapore) and leading global institutions. Such partnerships are essential to helping us build critical capabilities necessary to deliver on our programs
and realize their full potential.
Our vaccines pipeline as of May 14, 2019 (the date of our annual earnings release), along with notes for major subsequent developments, is
Drug class
(administration route)
Indications/additional
formulations
Stage by country/region(2)
In-house/In-license
as follows:
Development Code
Brand name
(country/region)(1)
TAK-003
<->
TAK-214
<->
TAK-021
<->
Tetravalent dengue
vaccine (injection)
Norovirus vaccine
(injection)
EV71 vaccine
(injection)
Prevention of the
dengue fever caused
by dengue virus
Prevention of the acute
gastroenteritis caused
by norovirus
Prevention of hand,
food, and mouth
disease caused by
enterovirus 71
TAK-426
<->
Zika vaccine
(injection)
Prevention of zika
virus infection
-
-
-
-
P-III
In-house
P-II(b)
In-house
P-I
P-I
In-house
In-house (Partnership
with the Biomedical
Advanced Research
and Development
Authority – U.S.
Government)
_____________
Notes:
(1)
Brand name and country/region indicate the brand name and country in which the specific asset has already been approved for any indication
in any of the U.S., EU, Japan or China and Takeda has commercialization rights for such asset.
Country/region in this column denote where a clinical study is ongoing or a filing has been made with our specific intention to pursue approval
in any of the U.S., EU, Japan or China.
(2)
35
Availability of Raw Materials
In the ordinary course of business, we purchase raw materials and supplies essential to our operations from suppliers around the world.
While we develop and manufacture the active ingredients used in some of our products at our own facilities, we are dependent on third-party suppliers
for a portion of the raw materials and compounds used in some of the other products we produce. We believe that, in the event we are unable to source
any products or ingredients from any of our major suppliers, we could replace those products or substitute ingredients from other suppliers, although
we may not be able to do so without significant difficulty or significant increases in our cost of goods sold. While efforts are made to diversify our
sources of components and materials, in certain instances we acquire components and materials from a sole supplier.
We are dependent on human donors for the supply of human plasma. Human plasma is a critical active ingredient in our plasma derived
therapies. We source human plasma internally and externally through a distinctive and flexible infrastructure, which provides us an enhanced capability
with respect to the consistent delivery of high-quality plasma-based products. We own and operate plasma collection facilities, principally the U.S.,
Austria, Hungary and Czech Republic, and we also maintain relationships with other plasma suppliers to ensure that we retain the flexibility to meet
market demand for our plasma-based therapies.
We closely monitor, continuously review and revise the supply sourcing strategy for our products to identify in a timely manner any risks in
our supply chain, including risks arising from our dependency on outsourced manufacturing relationships with third party suppliers. Where necessary,
inventory levels of either key materials and finished products are managed strategically to address potential risks relating to operational and quality
issues, production capacity and single sourcing among others. For critical and new technology products, we have decided to make significant long-term
capital investments to build internal manufacturing capacity and secure dual sources to reduce the current dependency on outsourced manufacturing
relationship with third-party suppliers.
Manufacturing
Following the acquisition of Shire in January 2019, we will continue to operate locally with the ability to access global manufacturing and
distribution networks as required.
The manufacture of our products is highly regulated by governmental health authorities around the world, including the FDA, EMA and
PMDA. Furthermore, many of our products involve technically complex manufacturing processes or may require a supply of highly specialized raw
materials.
We manufacture certain of our products in our own facilities worldwide. In addition, we source certain other of our products from third-party
contract manufacturers. We have a network for over 300 contract manufacturers which support approximately 30% of our products in different capacities
such as active pharmaceutical ingredients production and sourcing, bulk drug product, aseptic fill finish and final packaging. We manage the risks
associated with reliance on single sources of production by carrying additional inventories.
Sales and Marketing
Our primary sales and marketing activities are organized around United States, Japan Pharma, Europe-Canada (“EUCAN”) and Emerging
Markets. These business units make focused investments that support growth potential in the market and enhance efficiency.
The United States is the largest pharmaceutical market in the world. The United States business unit focuses on recently approved products
such as ENTYVIO, TRINTELLIX, ADYNOVATE, and TAKHZYRO as well as continuing to grow more established products such as VYVANSE, ADVATE
and GAMMAGARD LIQUID. These and other principal products are supported by significant marketing and sales force promotion.
The Japan Pharma business unit focuses on retaining our position as one of the leading pharmaceutical companies in our home market of
Japan, where the government is driving stricter control of drug prices and promoting the penetration of generics.
The EUCAN business unit focuses on a specialized approach in the European and Canadian markets, where public insurance has set a higher
bar for the reimbursement of medicines, requiring innovation and differentiation for the products to be reimbursed. As Canada’s health insurance system
is very similar to that of Europe, the Canadian market is managed by the EUCAN business unit.
The Emerging Markets business unit focuses on maximizing growth potential in areas across Asia Pacific, Greater China, Latin America,
Near East, Middle East and Africa and Russia/ CIS.
Intellectual Property
An important part of our business strategy is to protect our products and technologies using patents and trademarks, to the extent available.
We rely on trade secrets, proprietary know-how, technological innovations and contractual arrangements with third parties to maintain and enhance our
competitive position. Our commercial success depends, in part, upon our ability to obtain and enforce strong patents, to maintain trade secret protection,
to operate without infringing the proprietary rights of others and to comply with the terms of licenses granted to it. Due to the lengthy development
periods for new drugs, the high costs of research and development and the small percentage of researched compounds that reach the market, the protection
of intellectual property plays an important role in the return of investments for research and development of a new drug.
36
We seek patent protection for proprietary technology whenever possible in the U.S., Japan and major European countries. Where practicable,
we seek patent protection in other countries on a selective basis. In all cases, we endeavor to either obtain patent protection itself or support patent
applications through licensors. Patents are our primary means of protecting the technologies we use. Patents provide the holder with the right to exclude
others from using an invention related to a pharmaceutical product. We use various types of patents to protect our pharmaceutical products, including
substance patents, which cover active ingredients, as well as patents covering usage, manufacturing processes and formulation of drugs.
Our low molecule products (small molecules) are mainly protected by substance patents. While the expiration of a substance patent usually
results in a loss of market exclusivity for the protected pharmaceutical products, commercial benefits may continue to be protected by non-substance
patents such as patents relating to the use of such substance, patents relating to the method of use of such substance, patents relating the manufacturing
method of such substance, and patents relating to the new composition or formulation of such substance. The products can be also protected by regulatory
data protection under relevant law in each country even if the substance patent expired. While our biologics products can and may be protected by one
or more substance patents, certain products may be protected by non-substance patents and/or regulatory data protection. However, for biologics, patent
protection may be less important than for traditional pharmaceutical products, as similar products for the same indication and/or biosimilars may be
developed and marketed by competitors without infringing on our patents.
In the United States, patents generally expire twenty years after the filing date of the application, subject to potential patent term adjustments
for delays in patent issuance based upon certain delays in prosecution by the United States Patent and Trademark Office. A U.S. pharmaceutical patent
that claims a product, method of treatment using a product or method of manufacturing a product may also be eligible for a patent term extension based
on the time the FDA took to approve the product. This type of extension may only extend the patent term for a maximum of five years and may not
extend the patent term beyond fourteen years from regulatory approval. Only one patent may be extended for any product based on FDA delay. In
addition to patent exclusivities, the FDA may provide data or market exclusivity for a new chemical entity or an “orphan drug,” each of which run in
parallel to any patent protection. Regulatory data protection or exclusivity prevents a potential generic competitor from relying on clinical trial data that
were generated by the sponsor when establishing the safety and efficacy of its competing product for a period of five years for a new chemical entity,
or seven years for an orphan drug. Market exclusivity prohibits any marketing of the same drug for the same indication.
In Japan, a patent can be issued for active pharmaceutical ingredients by the Japan Patent Office (“JPO”). Although methods of treatment,
such as dosage and administration, are not patentable in Japan, pharmaceutical compositions for a specific dosage or administration method as well as
processes to make a pharmaceutical composition are patentable. Patents in Japan generally expire 20 years after the filing date of the patent application.
Patents for pharmaceuticals may be extended for up to five years, depending on the amount of time spent for the drug approval process. Japan also has
a regulatory data protection system called a “re-examination period” of eight years for pharmaceuticals that contain new active pharmaceutical ingredients
and four years to six years for new indications and formulations and a ten-year orphan drug exclusivity system.
In the EU, patent applications may be filed in the European Patent Office (“EPO”) or in a country in Europe. The EPO system permits a single
application to be granted for the EU, plus certain other non-EU countries, such as Switzerland and Turkey. When the EPO grants a patent, it is then
validated in the countries that the patent owner designates. The term of a patent granted by the EPO or a European country office is generally 20 years
from the filing date of the patent application. Pharmaceutical patents covering an approved medicinal product can be granted a further period of exclusivity
under the Supplementary Protection Certificate (“SPC”) system. SPCs are designed to compensate the owner of the patent for the time it took to receive
marketing authorization by the European Medicines Agency or the National Health Authorities. An SPC may be granted to provide, in combination with
the patent, up to 15 years of exclusivity from the date of the first European marketing authorization. However, an SPC cannot last longer than five years.
The SPC duration can additionally be extended by a further Pediatric Extension of six months if the SPC relates to a medicinal product for children for
which data has been submitted according to a Pediatric Investigation Plan ("PIP"). The post-grant phase of patents, including the SPC system, is currently
administered on a country-by-country basis under national laws. Therefore, although regulations concerning patents and SPCs have been created at EPO
and EU level, respectively, due to different national implementation they may not always lead to the same result, for example, if challenged at National
Courts in the various EU countries. The EU also provides a system of regulatory data exclusivity for authorized human medicines, which runs in parallel
to any patent protection. The system for drugs being approved today is usually referred to as “8+2+1” rule because it provides an initial period of eight
years of data exclusivity, during which a competitor cannot rely on the relevant data, a further period of two years of market exclusivity, during which
the data can be used to support applications for marketing authorization but the competitive product cannot be launched and a possible one-year extension
of the market exclusivity period if, during the initial eight-year data exclusivity period, the sponsor registered a new therapeutic indication for the
concerned drug. However, the additional one-year extension is only available if either no therapy exists for the new indication or if the concerned product
provides for the new indication a "significant clinical benefit over existing therapies". This system applies both to national and centralized authorizations.
The EU also has an orphan drug exclusivity system for medicines similar to the U.S system. If a medicine is designated as an orphan drug, it benefits
from ten years of market exclusivity, during which time a similar medicine for the same indication will not receive marketing authorization. Under
certain circumstances, this exclusivity can be extended with a two-year Pediatric Extension for completion of a PIP.
Worldwide, we experience challenges in the area of intellectual property from factors such as the penetration of generic versions of our products
following the expiry of the relevant patents and the launch by competitors of over-the-counter versions of our products. Our Global General Counsel is
responsible for the oversight of our Intellectual Property operations, as well as our legal operations. Our Intellectual Property Department supports our
overall corporate strategy by focusing efforts on three main themes:
•
•
•
maximization of the value of our products and research pipeline and protection of related rights aligned to the strategies of our therapeutic
area units;
facilitation of more dynamic harnessing of external innovation through partner alliance support; and
securing and protection of intellectual property rights around the world, including in emerging markets.
37
As infringement of our intellectual property rights poses a risk of loss of expected earnings derived from those rights, we have internal processes
in place to manage patents and other intellectual property. This program includes both remaining vigilant against patent infringement by others as well
as exercising caution, starting at the research and development stage, to ensure that our products and activities do not violate intellectual property rights
held by others.
In the regular course of business, our patents may be challenged by third parties. We are party to litigation or other proceedings relating to
intellectual property rights. Details of material ongoing litigation are provided in Note 32 to our audited consolidated financial statements included in
this annual report.
The following table describes our outstanding substance patents and the regulatory data protection (“RDP”) (US and EU) or re-examination period
(“RP”) (Japan) for the indicated product by territory and expiry date. The table includes RDP or RP information only if the protection provided by
regulatory exclusivity exceeds the patent expiry. Patent term extensions (“PTE”), supplemental protection certificates (“SPC”), and pediatric exclusivity
periods (“PEP”) are reflected in the expiry dates to the extent they have been granted by the issuing authority. For PTE’s, SPC’s, and PEP’s in which
the application is in process but not yet granted, the extended expiry is separately provided.
Our biologic products may face or already face competition from companies who produce similar products for the same indications, and/or
biosimilars, regardless of expiry dates below. Certain of the European patents are the subject of supplemental protection certificates that provide additional
protection for the product in certain countries beyond the dates listed in the table.
Our product
Japan expiry dates(1)(2)
U.S. expiry dates(1)
EU expiry dates(1)
GI:
ENTYVIO
PANTOPRAZOLE
DEXILANT
TAKECAB(3)
AMITIZA(4)
GATTEX/REVESTIVE
Patent: —
Patent: September 2021
RP: July 2026(2)
Patent: —
Not commercialized
Patent: August 2031
Patent: —(4)
Patent: —
RDP: May 2026
Patent: —
Patent: —
Patent: —(3)
Patent: May 2021(5)
Patent: October 2020(6)
LIALDA/MEZAVANT(3)
Patent: — (3)
Patent: —
Patent: August 2017 (Extended
expiry of August 2022 in certain
countries)
RDP: May 2024
Patent: —
Patent: —
Patent: —(3)
Not commercialized
Patent: —
RDP: September 2024
Patent: —
Rare Diseases
VPRIV
ELAPRASE
REPLAGAL
NATPARA
RP: September 2022(2)
Patent: —
RP: July 2024(2)
Patent: —
Patent: —
Patent: —
FIRAZYR
Patent: —
ADVATE
ADYNOVATE
FEIBA(7)
HEMOFIL(7)
IMMUNATE(7)
IMMUNINE(7)
TAKHZYRO
RP: September 2028(2)
Patent: —
Patent: January 2026
Patent: —
Not commercialized
Patent: —
Not commercialized
January 2031
Patent: —
Patent: —
Patent: September 2019
Not commercialized
Patent: —
RDP: January 2027
Patent: July 2019
Patent: —
RDP: August 2022
Patent: —
Patent: —
Patent: —
RDP: April 2029
Patent: —
RDP: July 2020
Patent: —
Patent: February 2026
Patent: January 2028 if granted
RDP: November 2027
RDP: January 2028
Patent: —
Patent: —
Not commercialized
Not commercialized
December 2031, February 2032,
March 2032
Patent: —
Not commercialized
Patent: —
Patent: —
January 2031
Extended expiry of November
2034 if PTE granted
Extended expiry of August 2032 if
PTE granted
Extended expiry of January 2036 if
SPC granted
38
Our product
Japan expiry dates(1)(2)
U.S. expiry dates(1)
EU expiry dates(1)
KALBITOR
CINRYZE(7)
Not commercialized
Patent: —
GAMMAGARD LIQUID(7)
ALBUMIN IN GLASS(7)
HYQVIA(7)
Not commercialized
Not commercialized
Not commercialized
December 2023
Patent: —
RDP: October 2020
Patent: —
Patent: —
Patent: —
Not commercialized
Patent: —
Patent: —
Patent: —
Patent: —
CUVITRU(7)
Not commercialized
Patent: —
FLEXBUMIN(7)
Oncology:
Not commercialized
RDP: September 2028
Patent: —
Patent: —
RDP: July 2027
Patent: —
LEUPLIN/ENANTONE
Patent: —
Patent: —
Patent: —
RDP: September 2026
RDP: May 2024
VELCADE(3)
NINLARO
ADCETRIS(4)
ALUNBRIG
ICLUSIG(3)
VECTIBIX(4)
Neuroscience:
TRINTELLIX (4)
RP: September 2019(2)(8)
Patent: —(3)
Patent: July 2031
Patent: April 2022, April 2026 (9)
Patent: —
Patent: August 2027
Patent: —(3)
Patent: November 2031
Extended expiry of November
2029 if PTE granted
Patent: —(4)
Patent: October 2027
Patent: May 2029
Patent: July 2030
Patent: May 2029
Extended expiry of February 2033
if PTE granted
Patent: —(3)
Patent: August 2022
Extended expiry of April 2031 if
PTE granted
Patent: January 2027
Patent: —(4)
Extended expiry of November
2033 if SPC granted
Patent: —(3)
Patent: —(4)
Patent: October 2022
Patent: June 2026
Patent: —(4)
Extended expiry of October 2027 if
PTE granted
Extended expiry of December 2026
if PTE granted
VYVANSE
Patent: June 2024
Patent: February 2023
Extended expiry of June 2029 if
PTE granted
Patent: June 2024 (Extended expiry
of February 2028 or March 2029 in
certain countries)
ADDERALL XR
ROZEREM
REMINYL
INTUNIV
Other:
NESINA
ULORIC(4)
COLCRYS
LOTRIGA(4)
AZILVA
_____________
Notes:
RP: March 2027(2)
Not commercialized
Patent: March 2022
Patent: —
Patent: —
RP: March 2025(2)
Patent: April 2028
Patent: —(4)
Not commercialized
Patent: —
RP: September 2020(2)
Patent: —
RP: October 2021(2)
Patent: —
Patent: July 2019
Patent: —
Patent: —
Patent: June 2028
Patent: —
Patent: —
Patent: — (4)
Not commercialized
Not commercialized
Patent: —
Patent: —
RDP: September 2025
Patent: September 2028
Patent: —(4)
Not commercialized
Patent: — (4)
Not commercialized
Not commercialized
39
(1) A “-” within the table indicates the substance patent is expired or not applicable.
(2)
In Japan, an application for a generic product is filed after the re-examination period ends, and the product is listed in the approval and drug price
listing after a regulatory review. Therefore, the generic product would enter the market after a certain period of time from the expiry of the re-
examination period.
(3) This product is not sold by Takeda in all regions because of out-licensing agreements to third parties.
(4) This product is not sold by Takeda in all regions because of in-licensing agreements from third parties exclusive to certain regions. See “-Business
Overview” principal products descriptions and “-Licensing and Collaboration” for further information on the licensing agreements.
(5) Generic may be introduced after January 2021 (or earlier under certain circumstances) based on a settlement with an ANDA filer.
(6) Generic may be introduced after March 2023 based on a settlement with an ANDA filer.
(7) Relates to plasma-derived therapies products.
(8) LEUPLIN/ENANTONE has a re-examination period in Japan for formulation(6M) through September 2019.
(9) Generic/biosimilar may be introduced after July 2026 dependent on when access to the U.S. or European market is available.
Licensing and Collaboration
In the ordinary course of business, we enter into arrangements for licensing and collaboration for the development and commercialization
of products with third parties. Our business does not materially depend on any one of these arrangements. Instead they form a portion of our strategy
and give us the ability to leverage a mix of internal and external resources to develop and commercialize new products. Certain of the agreements which
that have led to successful commercialization to date are summarized below:
•
•
•
ADCETRIS: We entered into a Collaboration Agreement with Seattle Genetics in 2009 for the global co-development of ADCETRIS
and its commercialization around the world (other than the U.S. and Canada, where ADCETRIS is commercialized by Seattle Genetics).
We may be required to pay milestone payments related to regulatory and commercial progress by us under the collaboration. We also
pay tiered royalties with percentages ranging from the mid-teens and to the mid-twenties based on net sales of ADCETRIS within our
licensed territories. We and Seattle Genetics equally co-fund the cost of selected development activities conducted under the
collaboration. Either party may terminate the collaboration for cause, or by mutual consent. We may terminate the collaboration at
will, and Seattle Genetics may terminate the collaboration in certain circumstances. If neither party terminates the collaboration
agreement, then the agreement automatically terminates on the expiration of all payment obligations. As of March 31, 2019, our
aggregate potential development and commercial milestone payments under the ADCETRIS collaboration were $47.5 million.
TRINTELLIX: We entered into a License, Development, Supply and Commercialization Agreement with H. Lundbeck A/S in September
2007 for the exclusive co-development and co-commercialization in the United States and Japan of several compounds in Lundbeck’s
pipeline for the treatment of mood and anxiety disorders, under which agreement we commercialize TRINTELLIX in the U.S.
TRINTELLIX has not yet been launched in Japan. Under the agreement, we and Lundbeck have agreed to jointly develop the relevant
compounds, with most of development funding from us. Revenues for TRINTELLIX are booked by us, and we pay to Lundbeck a
portion of our sales, as well as tiered royalties ranging from the mid-teens to twenties on the portion of sales retained by us. We have
also agreed to pay to Lundbeck certain development and commercialization milestone payments relating to regulatory and commercial
progress under the collaboration. The term of the agreement is indefinite, but the agreement may be terminated by mutual decision of
the parties or for cause. As of March 31, 2019, our aggregate potential development and commercial milestone payments under the
TRINTELLIX collaboration were $130.0 million.
AMITIZA: In October 2004, we entered into an agreement with Sucampo Pharmaceuticals (subsequently acquired by Mallinckrodt) to
purchase, develop and commercialize AMITIZA for gastrointestinal indications in the U.S. and Canada. The initial term of the agreement
is through December 31, 2020, after which the agreement continues automatically until terminated by us. We purchase AMITIZA from
Mallinckrodt under the agreement at an agreed upon price and pay tiered royalties on sales in North America ranging from the high
teens to mid-twenties, resetting each year. Beginning on January 1, 2021, we will share equally with Mallinckrodt in the net annual
sales revenue from branded AMITIZA sales. We have agreed to fund development costs, including regulatory-required studies, subject
to agreed-upon caps, with excess costs being shared equally, with certain exceptions. We have a similar agreement with Mallinckrodt
covering the rest of the world, except for Japan and the People’s Republic of China. We have agreed to additional commercial milestone
payments contingent on the achievement of certain net sales revenue targets, and to provide a minimum annual commercial investment
during the term of the agreement, which we may reduce when a generic equivalent enters the market. As of March 31, 2019, our
aggregate potential commercial milestone payments under the AMITIZA collaboration were $50.0 million.
Our other research and development licensing and collaboration arrangements include, but are not limited to, the following:
Partner
Oncology:
Adimab LLC
Centre d’Immunologie de
Marseille-Luminy
ASKA Pharmaceutical Co.
Country
Description of collaboration
U.S.
France
Japan
Agreement for the discovery, development and commercialization of three monoclonal antibodies
and three CD3 Bi-Specific antibodies for oncology indications.
Collaboration agreement to bring together expertise of Bernard Malissen group in innate biology
with our BacTrap capabilities to identify novel targets and pathways in myeloid cells.
Licensing agreement to grant exclusive commercialization rights for uterine fibroids and
exclusive development and commercialization rights for endometriosis for Japan to maximize
the product value of relugolix (TAK-385).
40
Partner
Country
Description of collaboration
Crescendo Biologics Ltd.
Exelixis, Inc.
GammaDelta Therapeutics Ltd.
("GammaDelta Therapeutics")
UK
U.S.
UK
Collaboration and licensing agreement for the discovery, development and commercialization of
Humabody®-based therapeutics for cancer indications.
Exclusive licensing agreement to commercialize and further clinical development of cabozantinib
in Japan. We receive exclusive commercial rights for all potential future cabozantinib indications
in Japan, including advanced renal cell carcinoma, for which cabozantinib is marketed in the
U.S. and EU as CABOMETYX™ tablets.
Collaboration agreement to develop GammaDelta Therapeutics' novel T cell platform based on
the unique properties of gamma delta T cells derived from human tissues. The companies intend
to use this novel platform to discover and develop new immunotherapies in oncology.
HaemaLogiX Pty. Ltd.
Australia
Research collaboration and licensing agreement for the development of new therapeutics to novel
antigens in multiple myeloma.
Heidelberg Pharma GmbH
Germany
Antibody-drug-conjugate ("ADC") research collaboration on two targets and licensing agreement
(α-amanitin payload and proprietary linker).
ImmunoGen, Inc. ("ImmunoGen")
U.S.
Licensing agreement for exclusive rights to use ImmunoGen's ADC technology to develop and
commercialize targeted anticancer therapeutics for up to two undisclosed targets.
Maverick Therapeutics Inc.
(“Maverick”)
U.S.
Collaboration agreement for the development of Maverick’s T cell engagement platform created
specifically to improve the utility of T cell redirection therapy for the treatment of cancer. Under
the agreement, we have the exclusive right to purchase Maverick after five years.
Myovant Sciences Ltd.
(“Myovant”)
Switzerland We granted Myovant an exclusive, worldwide license (excluding Japan and certain other Asian
countries) to relugolix (TAK-385) and an exclusive, worldwide license to MVT-602 (TAK-448).
Memorial Sloan Kettering Cancer
Center
Molecular Templates, Inc.
(“MTEM”)
U.S.
U.S.
Alliance to discover and develop novel chimeric antigen receptor T (“CAR-T”) cell products for
the potential treatment of hematological malignancies and solid tumors. This partnership pursues
the development of therapies that redirect T cell immunity against liquid or solid tumors.
Collaboration agreement related to oncology drug discovery programs. The collaboration will
apply MTEM’s engineered toxin bodies technology platform to potential therapeutic targets. In
September 2018,
joint development and
commercialization of CD38-targeted engineered toxin bodies for the treatment of patients with
diseases such as multiple myeloma.
this collaboration was expanded for
the
National Cancer Center of Japan
Japan
Nektar Therapeutics (“Nektar”)
U.S.
Partnership agreement with the National Cancer Center of Japan to develop basic research to
clinical development by promoting exchanges among researchers, physicians, and others engaged
in anti-cancer drug discovery and cancer biology research.
Collaboration agreement to explore the combination of Nektar’s lead immuno-oncology
candidate, the CD122-biased agonist NKTR-214, with five oncology compounds from our cancer
portfolio.
Noile-Immune Biotech Inc.
("Noile-Immune")
Japan
Collaboration agreement to develop next generation CAR-T cell therapy. We have exclusive
options to obtain licensing rights for the development and commercialization of Noile-Immune’s
pipeline and products resulting from this partnership.
Shattuck Labs Inc. ("Shattuck")
U.S.
GlaxoSmithKline plc
Teva Pharmaceutical Industries
Ltd. ("Teva")
GI:
Ambys Medicines (“Ambys”)
Arcturus Therapeutics, Inc.
("Arcturus")
UK
Israel
U.S.
U.S.
Beacon Discovery (“Beacon”)
U.S.
Collaboration agreement to explore and develop checkpoint fusion proteins using Shattuck’s
Agonist Redirected Checkpoint platform that have the potential to become highly differentiated,
next-generation immunotherapies. We will hold options for exclusive global development and
commercialization rights for up to four molecules resulting from the collaboration.
Exclusive licensing agreement to develop and commercialize novel cancer therapy niraparib for
the treatment of all tumor types in Japan, and all tumor types excluding prostate cancer in South
Korea, Taiwan, Russia and Australia.
Multi-target discovery collaboration agreement for access to Teva’s attenukine platform including
a license to TEV-48573, a CD38 targeted antibody fused with attenuated interferon alpha for the
treatment of multiple myeloma.
Partnership to collaborate on transformative therapies for the treatment of serious liver diseases.
Ambys is applying novel modalities, cell and gene therapy to restore liver function and prevent
the progression to liver failure for diseases that are untreatable or poorly treated today. Under the
terms of the agreement, we receive an option to ex-U.S. commercialization rights for the first
four products that reach an investigational NDA.
Agreement to develop RNA-based therapeutics for the treatment of non-alcoholic steatohepatitis
and other gastrointestinal related disorders using Arcturus' wholly-owned LUNA™ lipid-
meditated delivery systems and UNA Oligomer chemistry.
Multi-year drug discovery collaboration on a few G-protein coupled receptors ("GPCRs") that
play an important role in the pathology of gastrointestinal disorders. The agreement grants us
worldwide rights to develop, manufacture and commercialize products resulting from the
collaboration.
41
Partner
Country
Description of collaboration
Cour Pharmaceutical
Development Company, Inc.
(“Cour”)
U.S.
Agreement to research and develop novel immune modulating therapies for the potential treatment
of celiac disease and other gastrointestinal disease using Cour's Tolerizing Immune Modifying
nano Particle ("TIMP") platform to co-develop TIMP-Gliadin.
Enterome Bioscience SA
France
Agreement for a strategic drug discovery collaboration to research and develop potential new
therapeutics directed at microbiome targets thought to play crucial roles in gastrointestinal
disorders, including IBDs such as ulcerative colitis and motility disorders such as irritable bowel
syndrome. The agreement includes a global license and co-development of EB8018/TAK-018
in Crohn's disease.
Finch Therapeutics Group, Inc.
(“Finch”)
Hemoshear Therapeutics, LLC
("Hemoshear")
U.S.
U.S.
Global collaboration agreement to jointly develop FIN-524, a live biotherapeutic product
composed of cultured bacterial strains linked to favorable clinical outcomes in studies of
microbiota transplantations in IBD. We obtain the exclusive worldwide rights to develop and
commercialize FIN-524 and rights to follow-on products in IBD. We and Finch may elect to
extend this collaboration to additional and related indications on similar terms.
Collaboration agreement for novel target and therapeutic development for liver diseases,
including nonalcoholic steatohepatitis. We will receive exclusive access to Hemoshear’s
proprietary disease modeling platform to discover and develop best-in-class therapeutics for
specific liver diseases.
Janssen Pharmaceuticals, Inc.
Belgium
Exclusive license agreement to develop and market prucalopride as a treatment for chronic
constipation in the U.S. Motegrity, approved in December 2018.
NuBiyota LLC (“NuBiyota”)
Canada
PvP Biologics, Inc. (“PvP”)
U.S.
Agreement for the development of Microbial Ecosystem Therapeutic products for GI indications
with a high unmet medical need. We will collaborate with NuBiyota to advance oral microbial
consortia products developed by using NuBiyota’s microbiome platform for GI indications.
Global agreement for the development of KumaMax, a novel enzyme designed to break down
the immune-reactive parts of gluten in the stomach. We will provide financing for PvP to conduct
research and development through Phase I proof-of-principle studies and obtain an exclusive
option to acquire PvP following receipt of a pre-defined data package.
Samsung Bioepis Co, Ltd
South
Korea
Strategic collaboration agreement to jointly fund and co-develop multiple novel biologic therapies
in unmet disease areas. The program’s first therapeutic candidate is TAK-671, which is intended
to treat severe acute pancreatitis.
Theravance Biopharma Inc
Ireland
UCSD/Fortis Advisors LLC
Rare diseases:
AB Biosciences, Inc.
ArmaGen, Inc.
U.S.
U.S.
U.S.
Asklepios Biopharmaceutical, Inc.
U.S.
BioMarin Pharmaceutical Inc.
U.S.
Global license, development and commercialization agreement for TD-8954, a selective 5-HT4
receptor agonist being investigated for potential use in the treatment of GI motility disorders,
including enteral feeding intolerance (“EFI”). TD-8954 is being developed for the short-term use
with EFI to achieve early nutritional adequacy in critically ill patients at high nutritional risk, an
indication for which the compound received the FDA Fast Track Designation.
Technology license to develop oral budesonide formulation (TAK-721/SHP621) for treatment
of eosinophilic esophagitis.
Research collaboration agreement to potentially develop assets for rare disease with pan-receptor
interacting molecules targeted for specific immunological conditions with a focus on autoimmune
modulated inflammatory diseases.
Worldwide licensing and collaboration agreement to develop AGT-182 (TAK-531/SHP631), an
investigational enzyme replacement therapy for potential treatment of both the central nervous
system ("CNS") and somatic (body-related) manifestations of Hunter syndrome.
Agreement for multiple research and development collaborations using FVIII gene therapy for
the treatment of hemophilia A and B.
Agreement for the in-license of enabling technology for the exogenous replacement of
iduronate-2-sulfatase with Idursulfase-IT in patients via direct delivery to the CNS for the long-
term treatment of Hunter syndrome in patients with cognitive impairment in order to slow
progression of cognitive impairment (TAK-609/SHP609).
GlaxoSmithKline plc (“GSK”)
UK
In-license agreement between GSK and University of Michigan for TAK-620/SHP620
(marabivir) in the treatment of human cytomegalovirus.
Harrington Discovery Institute at
University Hospitals in Cleveland,
Ohio
IPSEN
KM Biologics Co., Ltd.
NanoMedSyn
U.S.
Collaboration agreement for the advancement of medicines for rare diseases.
France
Japan
France
Purchase agreement to develop Obizur for the treatment of Acquired Hemophilia A, including
for patients with Congenital Hemophilia A with inhibitors indication in elective or emergency
surgery.
Collaboration agreement to jointly development TAK-755/SHP655 to overcome the ADAMTS13
deficiency.
Pre-clinical research collaboration agreement to evaluate a potential enzyme replacement therapy
using NanoMedSyn's proprietary synthetic derivatives named AMFA.
42
Partner
Novimmune SA
Rani Therapeutics
Ultragenyx Pharmaceutical Inc.
Xenetic Biosciences, Inc.
Neuroscience:
AstraZeneca plc ("AstraZeneca")
Denali Therapeutics Inc.
("Denali")
Mindstrong Health
Ovid Therapeutics Inc. ("Ovid")
Country
Description of collaboration
Switzerland
Agreement for the exclusive worldwide rights to develop and commercialize an innovative, bi-
specific antibody in pre-clinical development for the treatment of hemophilia A.
U.S.
U.S.
U.S.
UK
U.S.
U.S.
U.S.
Research collaboration agreement to evaluate a micro tablet pill technology for oral delivery of
FVIII therapy in hemophilia.
Collaboration agreement to develop and commercialize therapies for rare genetic diseases.
Exclusive research and development license agreement for PolyXen delivery technology for
hemophilia factors VII, VIII, IX, X.
Collaboration agreement to jointly develop and commercialize MEDI1341, an alpha-synuclein
antibody currently in development as a potential treatment for Parkinson’s disease. AstraZeneca
will lead Phase I development while we will lead future clinical development activities. The
companies will share equally future development and commercialization costs as well as any
future revenues.
Strategic option and collaboration agreement to develop and commercialize up to three specified
therapeutic product candidates for neurodegenerative diseases incorporating Denali’s antibody
transport vehicle platform for increased exposure of biotherapeutic products in the brain.
Collaboration to explore development of digital biomarkers for selected mental health conditions,
in particular schizophrenia and treatment-resistant depression.
Agreement to clinically develop and commercialize a novel, potent and highly selective CH24H
inhibitor, in rare pediatric epilepsies (TAK-935). We received equity in Ovid and may be eligible
to receive certain milestone payments based on the advancement of TAK-935. We will lead
commercialization in Japan and have the option to lead commercialization in Asia and other
selected geographies. Ovid will lead clinical development activities and commercialization of
TAK-935 in the United States, Europe, Canada and Israel.
StrideBio Inc.
U.S.
Collaboration and license agreement to develop in vivo Adeno-Associated Virus (“AAV”) based
therapies for Friedreich’s Ataxia and two additional undisclosed targets.
Wave Life Sciences Ltd.
Singapore
Research, development and commercial collaboration and multi-program option agreement to
develop antisense oligonucleotides for genetically-defined neurological diseases. The first
component of the collaboration will focus on programs targeting Huntington’s disease,
amyotrophic lateral sclerosis, frontotemporal dementia and spinocerebellar ataxia type 3. The
second component of the collaboration provides us with the rights to exclusively license multiple
preclinical programs targeting other neurological disorders including Alzheimer’s disease and
Parkinson’s disease.
Plasma derived therapies:
Halozyme Therapeutics, Inc.
(“Halozyme”)
Kamada Ltd.
Vaccines:
Biological E. Limited
U.S. Government - The
Biomedical Advanced Research
and Development Authority
("BARDA")
Zydus Cadila
Other / Multiple Therapeutic
Areas:
U.S.
Israel
India
U.S.
In-license agreement for Halozyme’s proprietary ENHANZE™ platform technology to increase
dispersion and absorption of HyQvia. On-going development work for a US pediatric indication
to treat primary and secondary immunodeficiencies and a Phase 3 indication in Chronic
Inflammatory Demyelinating Polyradiculoneuropathy.
In-license agreement to develop and commercialize Alpha-1 proteinase inhibitor (Glassia);
Exclusive supply and distribution of Glassia in the US, Canada, Australia and New Zealand;
Development of protocol for post market commitment trial ongoing.
We agreed to transfer existing measles and acellular pertussis vaccine bulk production technology
to develop low-cost combination vaccines for India, China and low- and middle-income countries.
Partnership to develop a Zika vaccine (TAK-426, our Zika vaccination candidate) to support the
Zika response in the U.S. and affected regions around the world. Selected by BARDA, a division
of the Office of the Assistant Secretary for Preparedness and Response (“ASPR”), within the
U.S. Department of Health and Human Services.
India
Partnership agreement to address the global threat of chikungunya and develop a chikungunya
vaccine an emerging infectious disease in Africa, Asia and the Indian subcontinent.
Bridge Medicines
U.S.
Center for IPS Cell Research
Application, Kyoto University
Japan
Partnership with Tri-Institutional Therapeutics Discovery Institute, Bay City Capital and
Deerfield Management in the establishment of Bridge Medicines. Research projects accepted
into the Tri-Institutional Therapeutics Discovery Institute will be able to graduate to Bridge
Medicines, where they will be given financial, operational and managerial support to move
seamlessly from validating proof-of-concept studies to clinical trials.
Ten-year collaboration and establishment of a joint research program to develop clinical
applications of induced pluripotent stem cells in therapeutic areas including cancer, heart failure,
diabetes mellitus, neuro-degenerative disorders and intractable muscle diseases.
43
Partner
HiFiBiO Inc.
HitGen Ltd.
("HitGen")
lsogenica Ltd.
("Isogenica")
Numerate, Inc.
Portal Instruments, Inc.
("Portal")
Recursion Pharmaceuticals
Schrödinger, LLC ("Schrödinger")
Seattle Collaboration
Stanford University
Tri-Institutional Therapeutics
Discovery Institute ("Tri-I TDI")
Competition
Country
Description of collaboration
U.S.
China
UK
U.S.
U.S.
U.S.
U.S.
U.S.
U.S.
U.S.
Collaboration for functional therapeutics high-throughput antibody discovery platform that
enables identification of antibodies for rare events, for discovery of therapeutic antibodies for GI
and Oncology therapeutic areas.
Agreement that HitGen will apply its advanced technology platform, based on DNA-encoded
library design, synthesis and screening, to discover novel leads which will be licensed exclusively
to us.
Agreement with Isogenica for access to a sdAb (single-domain antibody) platform to generate a
toolbox of VHH (Variable domain of Heavy chain of Heavy chain antibody) for various immune
cells, and we are targeting pathway validation and pipeline development across our GI and
Oncology portfolio.
Agreement for joint-discovery programs aimed at identifying clinical candidates for use in our
core therapeutic areas, namely GI, oncology and neuroscience.
Collaboration with Portal to develop and commercialize Portal’s needle-free drug delivery device
for potential use with our investigational or approved biologic medicines.
Agreement to provide pre-clinical candidates for our TAK-celerator™ development pipeline.
Multi-target research collaboration combining Schrödinger's in silico platform-driven drug
discovery capabilities with our deep therapeutic area knowledge and expertise in structural
biology.
Research alliance, Seattle Partnership for Research on Innovative Therapies (“SPRInT”), aiming
to accelerate the translation of Fred Hutchinson Cancer Research Center’s and University of
Washington’s cutting-edge discoveries into treatments for human disease, with a focus on GI,
oncology and neuroscience.
Collaboration with Stanford University to form the Stanford Alliance for Innovative Medicines
(“Stanford AIM”) to develop innovative treatments and therapies in a more effective manner.
Partnered with the Tri-I TDI, a collaboration of academia institution and industry to more
effectively develop innovative treatments and therapies.
Competition in our market is based on, among other things, product safety, efficacy, convenience of dosing, reliability, availability and
prices. Competitors include large international companies whose capabilities cover the entire product creation process from research and development
to production and marketing as well as smaller companies that focus on selling generic versions of products for which patent protection and regulatory
data protection have lapsed.
We also face competition from generic drugs that enter the market when our patent protection or regulatory exclusivity expires. See “—
Intellectual Property” for additional description of our patents. Additionally, we may face competition from our own introduction of new products with
similar treatments as our older products.
The competition we face often differs by product and geographic market, and companies emerge and fall away as competitors over time
due to innovations, merger activity and other business and market changes.
The following table shows the principal sources of competition for our main products:
Our product
GI:
DEXILANT, PANTOPRAZOLE
(Protonix)
ENTYVIO
Principal competing product
Primary manufacturer or
distributor
generic lansoprazole,
esomeprazole
Remicade
Humira
Simponi
Stelara
Cimzia
generic infliximab
—
Janssen Biotech
Abbvie
Janssen Biotech
Janssen Biotech
UCB
—
TAKECAB
GATTEX/REVESTIVE
Nexium
generic lansoprazole, omeprazole
AstraZeneca
—
Zorbtive
Nutrestore
EMD/Serono
Emmaus LifeSciences
44
Our product
ALOFISEL
Rare Diseases:
ADVATE and ADYNOVATE
Principal competing product
Autologous tissue, chronic seton
usage
Remicade
Primary manufacturer or
distributor
Johnson & Johnson's
Xyntha/Refacto AF
Pfizer and Sobi
Kogenate
Helixate
Kovaltry
Iblias
Eloctate/Elocta
Novoeight
Nuwiq
Afstyla
Hemlibra
Haegarda
Berinert
Fabrazyme
Galafold
Fabagal
Cerezyme
Elelyso/uplyso
Zavesca
Cerdelga
Cerezyme
Privigen
Carimune
Gamunex-C
Flebogamma
Bivigam
Gammaked
Gammaplex
Octagam
Panzya
Hizentra
Gamunex-C
Gammanorm
TAKHZYRO
REPLAGAL
VPRIV
Plasma-derived therapies
GAMMAGARD LIQUID, KIOVIG
GAMMAGARD LIQUID,
GAMMAGARD SD, HYQVIA,
CUVITRU
FLEXBUMIN and Human Albumin
Alburex/Alburx
Oncology:
ADCETRIS
ALUNBRIG
Albumnar
Plasbumin
Albutein
Albunorm
Kedbumin
chemotherapy regimens
Xalkori
Zykadia
Alecensa
45
Bayer
CSL
Bayer
CSL
Sanofi and Sobi
Novo Nordisk
Octapharma
CSL
Roche
CSL
CSL
Genzyme
Amicus
Isu Abaxis
Genzyme
Pfizer/Protalix
Actelion
Genzyme
Isu Abxis
CSL
CSL
Grifols
Grifols
Biotest
Kendrion
BPL
Octapharma
Octapharma
CSL
Grifols
Octapharma
CSL
CSL
Grifols
Grifols
Octapharma
Kendrion
—
Pfizer
Novartis
Roche
Our product
ICLUSIG
LEUPRORELIN (LEUPLIN)
NINLARO, VELCADE
Principal competing product
Primary manufacturer or
distributor
Gleevec
Tasigna
Sprycel
Bosulif
Zoladex
generic leuprorelin
Revlimid
Pomalyst/Imnovid
Kyprolis
Darzalex
Empliciti
Novartis
Novartis
Bristol-Myers Squibb
Pfizer
AstraZeneca
—
Celgene
Celgene
Amgen
Janssen Biotech
Bristol-Myers Squibb
Neuroscience:
TRINTELLIX
VYVANSE
Other:
AZILVA
NESINA
Viibryd
Fetzima
generic duloxetine, escitalopram
Allergan
Allergan
—
generic mixed salts of a single-
entity amphetamine product
generic mixed salts of a single-
entity amphetamine product,
extended release
generic methylphenidate, extended
release
—
—
—
generic candesartan, olmesartan
—
Januvia
generic pioglitazone
Merck Co., Inc.
—
Regulation
The pharmaceutical industry is subject to extensive global regulation by regional, national, state and local agencies. The regulatory agencies
and their regulations govern the testing, approval, production, labeling, distribution, post-market surveillance, advertising, dissemination of information
and promotion of our products. The following is a description of the major regulations affecting our products in the United States, Japan and the EU,
our largest markets.
The introduction of new pharmaceutical products generally entails a lengthy approval process. Products must be authorized or registered
prior to marketing, and such authorization or registration must subsequently be maintained. In recent years, the registration process has required increased
testing and documentation for the approval of new drugs, with a corresponding increase in the expense of product introduction. To register a pharmaceutical
product, a registration dossier containing evidence establishing the safety, efficacy and quality of the product must be submitted to regulatory authorities.
Generally, a therapeutic product must be registered in each country in which it will be sold. It is possible that a drug can be registered and marketed in
one country while the registration authority in another country may, prior to registration, request additional information from the pharmaceutical company
or even reject the product. It is also possible that a drug may be approved for different indications in different countries. The registration process generally
takes between six months and several years, depending on the country, the quality of the data submitted, the efficiency of the registration authority’s
procedures and the nature of the product. Many countries provide for accelerated processing of registration applications for innovative products of
therapeutic interest. In recent years, efforts have been made among the U.S., Japan and the EU to harmonize registration requirements to achieve shorter
development and registration times for medical products.
United States
In the United States, applications for drug registration are submitted to and reviewed by the FDA, which regulates the testing, manufacturing,
labeling and approval for marketing of pharmaceutical products intended for commercialization. The FDA continues to monitor the safety of
pharmaceutical products after they have been approved for sale in the U.S. market. When a pharmaceutical company has gathered data to demonstrate
a drug’s safety, efficacy and quality, it may file for the drug an NDA or Biologics License Application (“BLA”), along with information regarding the
clinical experiences of patients tested in the drug’s clinical trials. A supplemental new drug application ("sNDA") or BLA amendment must be filed for
new indications for a previously approved drug.
Once an application is submitted, the FDA assigns reviewers from its staff, including experts in biopharmaceutics, chemistry, clinical
microbiology, pharmacology/toxicology, and statistics. After a complete review, these content experts then provide written evaluations of the NDA or
BLA. These evaluations are consolidated and are used by senior FDA staff in its final evaluation of the NDA or BLA. Based on that final evaluation,
the FDA then provides to the NDA or BLA’s sponsor an approval, or a “complete response” letter if the NDA or BLA application is not approved. If
not approved, the letter will state the specific deficiencies in the NDA or BLA which need to be addressed. The sponsor must then submit an adequate
46
response to the deficiencies to restart the review procedure. Once the FDA has approved an NDA, BLA, sNDA or BLA amendment, the company can
make the new drug available for physicians to prescribe. The drug owner must submit periodic reports to the FDA, including any cases of adverse
reactions. For some medications, the FDA requires additional post-approval studies (Phase IV) to evaluate long-term effects or to gather information
on the use of the product under specified conditions. Throughout the life cycle of a product, the FDA requires compliance with standards relating to
good laboratory, clinical and manufacturing practices. The FDA also requires compliance with rules pertaining to the manner in which we may promote
our products.
The Drug Price Competition and Patent Restoration Term Act of 1984, known as the Hatch-Waxman Act, established the application
procedures for obtaining FDA approval for generic forms of brand-name drugs. Under these procedures, instead of conducting full-scale pre-clinical
and clinical trials, the FDA can accept data establishing that the drug formulation, which is the subject of an abbreviated application, is bio-equivalent
and has the same therapeutic effect as the previously approved drug, among other requirements. This act also provides market exclusivity provisions
for brand-name drugs that can delay the submission and/or the approval of abbreviated new drug applications (the “ANDAs”), which are the applications
for generic drug registrations. The Orphan Drug Act of 1983 grants seven years of exclusive marketing rights to a specific drug for a specific orphan
indication. The term “orphan drug” refers, generally, to a drug that treats a rare disease affecting fewer than 200,000 persons in the U.S. Market exclusivity
provisions are distinct from patent protections and apply equally to patented and non-patented drug products.
While the Hatch-Waxman Act addresses the development and entrance of generic products, the Patent Protection and Affordable Care Act
(the "ACA") amended the Public Health Service Act to create an abbreviated licensure pathway for biological products that are demonstrated to be
“biosimilar” to or “interchangeable” with an FDA-licensed biological product. The Biologics Price Competition and Innovation Act of 2009 allows for
approval of a biosimilar if data substantiates that the product is “highly similar” to an approved and existing biological product. Furthermore, as codified
in the 2016 Physician Fee Schedule Final Rule, effective January 1, 2016, the physician reimbursement amount for a biosimilar is based on the average
sales price (the “ASP”) of all National Drug Codes (the “NDCs”) assigned to the biosimilars included within the same billing and payment code. Similar
to a non-biologic product, an interchangeable biological product may be substituted for the reference product by a pharmacist without the intervention
of the health care provider who prescribed the reference product. Generally, there will be a common physician reimbursement limit and Healthcare
Common Procedure Coding System (the “HCPCS”) code for those biosimilars referenced to the original product filed under the BLA.
Japan
Manufacturers and sellers of drugs, quasi-drugs, cosmetics, medical devices and regenerative medical products (collectively the “Designated
Products”) in Japan are subject to the supervision of the Minister of Health, Labour and Welfare (the “Minister”) primarily under the Act on Securing
Quality, Efficacy and Safety of Pharmaceuticals, Medical Devices, Regenerative and Cellular Therapy Products, Gene Therapy Products, and Cosmetics
of Japan (the “Pharmaceutical Act”).
Under the Pharmaceutical Act, a person is required to obtain from the Minister the relevant licenses in order to conduct the business of
manufacturing, marketing or selling Designated Products.
Applications for the approval of new products are made through the PMDA. The data of results of clinical trials and other pertinent data
must be attached for an application for approval. If the drugs, medical devices or regenerative medical products under application are of types designated
by ministerial ordinance of the MHLW, the attached data mentioned above must be obtained in compliance with the standards established by the Minister,
such as the Good Laboratory Practice (the “GLP”) and the Good Clinical Practice (the “GCP”). Once an application for approval is submitted, a review
team is formed, which consists of specialized officials of the PMDA, including chemistry/manufacturing, non-clinical, clinical, and biostatistics. Team
evaluation results are passed to the PMDA’s external experts, who then report back to the PMDA. After a further team evaluation, a report is provided
to the Minister; the Minister makes a final determination for approval and refers this to the Council on Drugs and Foods Sanitation, which then advises
the MHLW on final approvability. Marketing and distribution approvals require a review to determine whether or not the product in the application is
suitable as a drug to be manufactured and distributed by a person who has obtained a manufacturing and distribution business license for the type of
drug concerned, and to confirm that the product has been manufactured in a plant compliant with Good Manufacturing Practice.
Once the MHLW has approved the application, the company can make the new drug available for physicians to prescribe. After that, the
MHLW lists its NHI price within 60 days (or 90 days at the latest) from the approval, and physicians can obtain reimbursement. For some medications,
the MHLW requires additional post‑marketing studies (Phase IV) to further evaluate safety and/or to gather information concerning the quality, efficacy,
and safety of the product under specified conditions. The MHLW also requires the drug’s sponsor to submit periodic safety update reports. Within three
months from the specified re‑examination period, which is designated at the time of the approval of the application for the new product, the company
must submit a re‑examination application to enable the drug’s quality, efficacy, and safety to be reassessed against approved labeling by the PMDA.
The Pharmaceutical Act also provides for special regulations applicable to drugs, quasi-drugs, cosmetics and medical devices made of biological
raw materials. These regulations impose various obligations on manufacturers and other persons in relation to manufacturing facilities, explanation to
patients, labeling on products, record-keeping and reporting to the Minister.
Under the Pharmaceutical Act, the Minister may take various measures to supervise manufacturing and marketing license holders of
Designated Products. The Minister has authority to order manufacturing and marketing license holders to temporarily suspend the marketing, leasing
or providing of the Designated Products to prevent risks, or increases in risks, to the public health. Also, the Minister may revoke a license or approval
granted to a manufacturing and marketing license holders or order a temporary business suspension under certain limited circumstances such as violation
of laws relating to drugs.
47
European Union
In the EU, there are three main procedures for application for authorization to market pharmaceutical products in the EU Member States:
the Centralized Procedure, the Mutual Recognition Procedure (the “MRP”) and the Decentralized Procedure (“the DCP”). It is also possible to obtain
a pure national authorization for products intended for commercialization in a single EU Member State only, or for additional indications for licensed
products.
Under the Centralized Procedure, applications are made to the EMA for an authorization which is valid throughout the EU. The Centralized
Procedure is mandatory for all biotechnology products and for new chemical entities in cancer, neurodegenerative disorders, diabetes and AIDS,
autoimmune diseases or other immune dysfunctions and optional for other new chemical entities or innovative medicinal products or in the interest of
public health. When a pharmaceutical company has gathered data which it believes sufficiently demonstrates a drug’s safety, efficacy and quality, then
the company may submit an application to the EMA. The EMA then receives and validates the application and the Committee for Medicinal Products
for Human Use (the “CHMP”) appoints a Rapporteur and Co-Rapporteur to lead review of the dossier. The entire review cycle must be completed within
210 days, although there is a “clock stop” at day 120, which allows the company to respond to questions set forth in the Rapporteur and Co-Rapporteur’s
Assessment Report. After the company’s complete response is submitted to the EMA, the clock restarts on day 121. If there are further aspects of the
dossier requiring clarification, the EMA will then request an Oral Explanation on day 180, in which case the sponsor must appear before the CHMP to
provide the requested additional information. On day 210, the CHMP will then take a vote to recommend the approval or non-approval of the application.
The final decision under this Centralized Procedure is a European Community decision which is binding in its entirety on all EU Member States. This
decision occurs on average 60 days after a positive CHMP recommendation. In the case of a negative opinion, a written request for re-examination of
the opinion can be made by the applicant within a time limit of 15 days from the date of the opinion. The detailed grounds for re-examination must be
submitted to the EMA within 60 days from the date of the opinion. In the EU, biosimilars are approved under a specialized pathway of the centralized
procedure. Similar to the pathway in the U.S., applicants seek and obtain regulatory approval for a biosimilar once the data exclusivity period for the
original reference product has expired relying in part on the data submitted for the original reference product together with data evidencing that the
biosimilar is “highly similar” in terms of quality, safety and efficacy to the original reference product authorized in the European Economic Area.
Under both the MRP and DCP, the assessment is led by a single EU Member State, called the Reference Member State (the “RMS”), which
then liaises with other EU Member States, known as the concerned member states (the “CMSs”). In the MRP, the company first obtains a marketing
authorization in the RMS, which is then recognized by the CMSs in 90 days. In the DCP, the application is done simultaneously in the RMS and all
CMSs. During the DCP, the RMS drafts an assessment report within 120 days. Within an additional 90 days, the CMSs review the application and can
issue objections or requests for additional information. On day 90, each CMS must be assured that the product is safe and effective, and that it will cause
no risks to the public health. Once an agreement has been reached, each member state grants national marketing authorizations for the product.
After the 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, several
pharmacovigilance measures must be implemented and monitored including Adverse Event collection, evaluation and expedited reporting and
implementation, as well as update Risk Management Plans. For some medications, post approval studies (Phase IV) may be required to complement
available data with additional data to evaluate long term effects (called a Post Approval Safety Study) or to gather additional efficacy data (called a Post
Approval Efficacy Study).
European Marketing Authorizations have an initial duration of five years. After this first five-year period, the holder of the marketing
authorization must apply for its renewal, which may be granted based on the competent authority’s full benefit-risk review of the product. Once renewed,
the marketing authorization is generally valid for an unlimited period. Any Marketing Authorization which is not followed within three years of its
granting by the actual placing on the market in any EU member state of the corresponding medicinal product ceases to be valid.
Third Party Reimbursement and Pricing
We consider domestic and international competitive conditions, such as the price of competing products, in setting and revising the price of
our pharmaceutical products. Government regulation also has a significant effect in determining the price of pharmaceutical products in many of the
countries in which we operate due to the fact that government policy in many countries has emphasized and purchasers continue to seek large discounts
on pharmaceutical products.
United States
In the United States our sales are subject to various rebate programs and government programs, which vary depending on the type and can
have a significant impact on our results. The most significant of these include rebates associated with commercial managed care, Medicaid, Medicare
and government programs.
Commercial Managed Care
Payers negotiate rebates to reduce the pricing of products, and use formularies to encourage members to utilize preferred products to manage
their costs. Exclusion from a formulary, or a disfavored formulary position, can directly reduce product usage. Consolidation of payers, pharmacy benefit
managers and pharmacies may result in increasing rebates and other discounts due to the purchasing power of the consolidated entities. Copay assistance
to help patients afford their prescribed drugs may also affect product usage. In recent years, some states such as California and Massachusetts, have
48
passed legislation that limits the use of manufacturer sponsored copay assistance programs, and some payers have limited manufacturer copay assistance
benefits to patients.
Medicaid
Medicaid is a state administered program adhering to federal requirements that provides healthcare coverage to eligible low-income adults,
children, pregnant women, elderly adults and people with disabilities.
Takeda must pay rebates on purchases of our products under the Medicaid Drug Rebate Program. Takeda must also calculate and report to
government agencies the amount of the rebate. The required calculations are complex, and a misrepresentation in the reported information may expose
Takeda to penalties. We are required to report any revisions to prior calculations, which could affect the rebate liability for prior quarters.
Medicare
The Medicare Prescription Drug Program has two arms, Medicare Part D and Medicare Part B. Medicare Part D is a voluntary offering available
to Medicare beneficiaries through private health insurance plans that contract with the government to deliver this benefit. Medicare Part B covers some
drugs, under the medical benefit, that are among the most biologically complex; these medicines are generally administered in a doctor’s office or
hospital outpatient setting.
Takeda offers rebates on purchases of pharmaceutical products covered under Medicare Part D. In addition, Takeda and other pharmaceutical
manufacturers are required to provide a discount of 70% on drugs used in the Medicare Part D coverage gap. Takeda must also calculate and report
specific prices to government agencies, including Average Sales Price used by the Medicare Part B program. The required calculations are complex,
and a misrepresentation in the reported pricing may expose Takeda to penalties.
340B and Federal Agency Discounted Pricing
Takeda must offer discounted pricing for purchases by certain designated health care entities and federal agencies under certain federal
programs, including the Public Health Service (PHS) pharmaceutical pricing program (340B) and the Federal Supply Schedule (FSS.)
Health Care System Reform
Any sudden change to the current health care system runs the risk of restricting patient access and placing all parties at financial risk. Spurred
by the Administration’s priority to bring down the cost of drug prices, a number of changes to the Medicare Part D and Part B programs are being
proposed - these changes may impact patient access and affordability, and may adversely affect our business by impacting demand for, or pricing of,
our products. The Trump Administration’s Blueprint to Lower Drug Prices and Reduce Out of Pocket Costs and the resulting regulatory activity has
already changed the way companies behave with fewer and lower price increases in 2018 than 2017.
Japan
In Japan, manufacturers of pharmaceutical products must have new products listed on the National Health Insurance (the NHI), a price list
published by the Ministry of Health, Labour and Welfare of Japan (the MHLW). The NHI price list provides rates for calculating the price of pharmaceutical
products used in medical services provided under various public medical care insurance systems. Prices on the NHI price list have been subject to
revisions generally once every two years based on the actual prices at which the pharmaceutical products are purchased by medical institutions in Japan
after discounts and rebates from listed price. The average price of previously listed products generally decreases as a result of these price revisions. The
Japanese government is currently undertaking healthcare reform initiatives with the goal of sustaining the universal coverage of the NHI program, and
is addressing the efficient use of drugs, including promotion of generic use with a target of 80% penetration by volume by September 2020 with respect
to products for which market exclusivity has expired. As part of these initiatives, the NHI price list is expected to be revised annually from April 1, 2021,
which could lead to more frequent downward price revisions. In addition, cost-effectiveness analysis was officially introduced by the MHLW from April
2019. Products on the NHI price list nominated based on pre-defined criteria, such as the innovativeness and the financial impact, will be subject to
review, and subject to price adjustments depending on outcome of this review.
European Union
In the EU, our operations are subject to significant price and marketing regulations. Many governments in the EU are introducing healthcare
reforms to curb increasing healthcare costs. The governments in the EU influence the price of pharmaceutical products through their control of national
healthcare systems that fund a large part of the cost of such products to patients. The general downward pressure on healthcare costs, particularly regarding
prescription drugs, has been increasing. In addition, prices for marketed products are referenced within and amongst the EU Member States, which
further affects pricing in each EU Member State. As an additional control for healthcare budgets, some EU Member States have passed legislation to
impose further mandatory rebates for pharmaceutical products and financial claw-backs on the pharmaceutical industry. In this regard, many countries
have health technology assessment organizations that use formal economic metrics such as cost-effectiveness to determine prices, coverage and
reimbursement of new therapies, and these organizations are expanding in established and emerging markets. We expect that countries will continue to
take aggressive actions to seek to reduce expenditures on drugs and biologics. Similarly, fiscal constraints may also affect the extent to which countries
are willing to approve new and innovative therapies and/or allow access to new treatments.
49
Furthermore, the European Union is currently undergoing an analysis of the rewards extended for intellectual property of pharmaceutical
products as well as the overall regulatory framework for the approval and commercialization of all medicinal products. This may lead to significant
changes in the way drugs are approved and commercialized as well as the duration of exclusivity, in particular for orphan drugs. These changes are
likely to affect the market within a 3-5-year timeframe.
Other
Many other countries around the world are also taking steps to control prescription drug prices. For example, in 2017, China - one of our most
important Emerging Growth Markets - organized national price negotiations for certain products directly linked to national drug reimbursement, which
will apply nationwide both in public and military hospitals. Drug prices in China may further decline due to a stated national policy of reducing healthcare
costs, including continued strategic initiatives specifically designed to reduce drug prices. Canada has proposed amendments to its Patented Medicines
Regulations that could reduce prices for specialty medicines, such as biologics and medicines for rare diseases.
C.
Organizational Structure.
We are a holding company and administer our business through a number of subsidiaries worldwide. Information about Takeda’s organizational
structure, including a list of our subsidiaries, their country of incorporation and residence and our proportion of ownership interest, is included in Note
29 to the audited consolidated financial statements included in this annual report.
D.
Property, Plant and Equipment.
Our registered head office is located in Osaka, Japan and our global head office is located in Tokyo, Japan. We generally own our facilities
or have entered into long-term lease arrangements for them.
As of March 31, 2019, the net book values of the buildings and structures, land, machinery and vehicles and tools, furniture and fixtures we
owned were ¥692.5 billion, ¥101.4 billion, ¥335.8 billion and ¥47.1 billion, respectively. We own the substantial majority of our facilities, none of which
are subject to any material encumbrances. The following table describes our major facilities as of March 31, 2019:
Group company
Name of facility (location)
Type of facility
Takeda Pharmaceutical Company Limited
Head Office (Chuo-ku, Osaka and others)
Administrative and sales
Takeda Pharmaceutical Company Limited
Global Head Office (Chuo-ku, Tokyo)
Administrative and sales
Takeda Pharmaceutical Company Limited
Osaka Plant (Yodogawa-ku, Osaka)
Manufacturing, Research and development
Takeda Pharmaceutical Company Limited
Hikari Plant (Hikari, Yamaguchi)
Manufacturing, Research and development
Takeda Pharmaceutical Company Limited
Shonan Health Innovation Park (Fujisawa,
Kanagawa)
Research
Takeda Real Estate Co, Ltd.
Nihon Pharmaceutical Co. Ltd.
Takeda Healthcare Products Co., Ltd.
Millennium Pharmaceuticals, Inc.
Baxalta U.S. Inc
Takeda Midosuji Building and others
(Chuo-ku, Tokyo)
Osaka Plant and other
(Izumisano, Osaka)
Head Office, Plant
(Fukuchiyama, Kyoto)
Head Office, Plant and other properties
(Cambridge, Massachusetts, U.S.)
Head Office (Covington, Georgia, U.S.)
Administrative and sales
Manufacturing, Research and development
Manufacturing
Research and development
Manufacturing, Warehouse, Administrative and
sales
Shire Human Genetic Therapies, Inc
Head Office (Lexington, Massachusetts, U.S.) Manufacturing, Warehouse, Administrative and
sales
Baxter AG
Baxalta Bioscience Manufacturing S.a.r.l.
Production facility and other (Orth an der
Donau, Austria and Vienna, Austria)
Head Office (Neuchatel, Switzerland)
Manufacturing, Distribution, Warehouse,
Plasma centers and Administrative and sales
Manufacturing, Administrative and sales
Shire Pharmaceuticals Ireland Ltd.
Production facility (Dunboyne, Ireland)
Manufacturing
Baxalta Belgium Manufacturing SA
Production facility (Lessines, Belgium)
Manufacturing
50
Environmental Matters
We are subject to laws and regulations concerning the environment, safety matters, regulation of chemicals and product safety in the countries
where we manufacture and sell our products or otherwise operate our business. These requirements include regulation of the handling, manufacture,
transportation, use and disposal of materials, including the discharge of pollutants into the environment. In the normal course of our business, we are
exposed to risks relating to possible releases of hazardous substances into the environment, which could cause environmental or property damage or
personal injuries, and which could require remediation of contaminated soil and groundwater, in some cases over many years, regardless of whether the
contamination was caused by us, or by previous occupants of the property. See “Item 3. Key Information—D. Risk Factors—We may incur substantial
costs due to our environmental compliance efforts or claims relating to our use, manufacture, handling, storage or disposal of hazardous materials.
Item 4A. Unresolved Staff Comments
Not applicable.
ltem 5. Operating and Financial Review and Prospects
You should read the following discussion of our operating and financial review and prospects together with our consolidated financial
statements included in Item 18 in this annual report. Our consolidated financial statements are prepared in accordance with IFRS, as issued by the
International Accounting Standard Boards (“IASB”). IFRS includes International Accounting Standard (“IAS”) and related interpretations of the
committees (SIC and IFRIC).
The following discussion and analysis contains forward-looking statements that involve risks, uncertainties and assumptions. Our actual
results may differ materially from those anticipated in these forward-looking statements as a result of factors, including, but not limited to, those under
Item 3. D “Risk Factors” and elsewhere in this annual report.
A.
Operating Results.
Overview
We have grown both organically and through acquisitions, completing a series of major transactions that have resulted in growth in our areas
of therapeutic, geographic and pipeline focus. In particular, our acquisition of Shire in January 2019 strengthened our presence in GI and neuroscience,
while providing us with a leading position in rare disease and plasma driven therapies. It also enhanced our research and development pipeline and
created a highly complementary, robust, modality-diverse pipeline. Commercially, the Shire Acquisition significantly strengthened our presence in the
United States. As a result of the acquisition of Shire, we incurred significant indebtedness to finance the cash portion of the consideration. We plan to
de-lever following the Shire Acquisition using cash flows from operations and we are initiating disposals of non-core assets to accelerate the pace of
deleveraging and to refocus our business on our key business areas of GI, rare diseases, plasma-derived therapies, oncology, and neuroscience.
We organize our business as a single operating segment, reflecting the presentation of information to our management for the purposes of
allocating resources, measuring performance and forecasting future periods. In the fiscal year ended March 31, 2019, our revenue was ¥2,097.2 billion,
our operating profit was ¥205.0 billion.
Factors Affecting Our Results of Operations
Our results are affected by the global industry trends and operating environment as described in Item 4 of this annual report and other factors
described below.
Acquisitions
We may acquire new businesses to expand our research and development capabilities (including expanding into new methodologies) and to
acquire new products (whether in the development pipeline or at the marketing stage) or other strategic regions. Similarly, we regularly divest businesses
and product lines to maintain our focus on our key growth drivers and to manage our portfolio.
We account for these acquisitions as business combinations and record the assets and liabilities acquired at fair value. Our results are impacted
due to the impacts of purchase accounting, which typically includes fair value step-ups of inventory and property, plant and equipment and recognized
material intangible assets which result in costs related to unwind of the step up and amortization expense, respectively, in future periods. Our results are
also impacted due to additional interest expenses when an acquisition is financed with incremental borrowings.
On January 8, 2019, we acquired Shire for an aggregate consideration of ¥6.21 trillion, of which ¥3,029.4 billion was paid in cash and the
remainder mainly in shares of our common stock. We incurred ¥3,295.9 billion in indebtedness in order to finance the cash portion of the consideration,
and as a result of the Shire Acquisition assumed ¥1,603.2 billion of indebtedness of Shire which is included in our consolidated statement of financial
position. We recorded goodwill of ¥3,087.4 billion and intangible assets of ¥3,899.3 billion in relation to the Shire Acquisition. The acquisition of Shire
has significantly changed our business through, among other things, the significant expansion of our product portfolio and geographic presence. Our
results will be significantly impacted by the Shire Acquisition with an increase to our revenues, and associated costs, and the impact of the acquisition
including incremental amortization expenses related to the acquired intangible assets, incremental cost of sales resulting from the unwinding of the
inventory fair value step up, the interest expense associated with the borrowings used to fund the acquisition, and the costs incurred to integrate the
51
business. We are actively engaged in integrating Shire and expect to be able to achieve significant, recurring pre-tax synergies of approximately $2.0
billion annually by the end of the third fiscal year after the completion of the Shire Acquisition, originating from efficiencies in the combined company’s
sales, marketing and administrative functions, research and development rationalization efforts and product manufacturing and supply. We estimate that
the realization of these synergies will require non-recurring costs of approximately $3.0 billion in the first three fiscal years following the completion
of the Shire Acquisition. We believe that the substantial cash flow generation expected to result from the Shire Acquisition will enable us to maintain
our well-established dividend policy, and de-lever following completion. We have begun initiating the disposal of certain non-core assets and businesses
to increase the pace of de-leveraging our debt.
On February 16, 2017, we acquired ARIAD Pharmaceuticals, Inc. for a net consideration of ¥583.1 billion. Headquartered in Cambridge,
Massachusetts in the United States, ARIAD was a commercial-stage biotechnology company focusing on discovering, developing and commercializing
precision therapies for patients with rare forms of chronic and acute leukemia, lung cancer and other rare cancers.
As a result of our acquisitions, and the impacts described above, our results year over year may not be comparable.
Divestitures
In addition to acquisitions, we divest businesses and product lines to maintain our focus on our key growth drivers and to manage our
portfolio and to provide additional cash flow to accelerate the repayment of long-term borrowings.
In April 2017, we completed the sale of our shares in Wako Pure Chemical to FUJIFILM Corporation for a sale price of ¥198.5 billion, for
which we recognized a gain of ¥106.3 billion in the fiscal year ended March 31, 2018. Wako Pure Chemical generated revenue of ¥76.6 billion and
¥79.1 billion for the fiscal years ended March 31, 2016 and 2017, respectively. There was no revenue recognized related to Wako Pure Chemical for the
fiscal year ended March 31, 2018.
In April 2016, we transferred certain long-listed products in Japan to Teva Takeda Yakuhin Ltd., a wholly-owned subsidiary of Teva Takeda
Pharma Ltd., a joint venture we formed with Teva Pharmaceutical Industries Ltd. in which we hold a 49% interest, representing shares of Teva Takeda
Pharma Ltd. received as consideration for the transfer. At the time of the transfer, we recognized a gain for the difference between the fair value
consideration received (shares of Teva Takeda Pharma Ltd.) and the carrying value of the business to the extent we disposed of the business. The
remainder of the gain was deferred and will be amortized over a period of 15 years from the date of the transfer, representing the estimated useful life
of the intangible assets associated with the products transferred. In the fiscal year ended March 31, 2017, we recognized a gain related to this transfer
of ¥115.4 billion. ¥102.9 billion of such amount was the amount of the gain recognized at the time of disposal. The remainder represents the amount of
the deferred gain amortized during such fiscal year. We receive income from the joint venture in the form of a supply and distribution fee, in addition
to a 49% share of the joint venture’s income or losses.
We have communicated our intention to continue to divest businesses that are not core to our operations and to reduce our borrowings with
the proceeds. In May 2019, we announced the sale of Xiidra® (lifitegrast ophthalmic solution), which we obtained as part of the Shire Acquisition and
the sale of Tachosil™, as described further in Note 33 to our audited consolidated financial statements included in this annual report.
Patent Protection and Generic Competition
For pharmaceutical products in particular, patent protection and/or regulatory exclusivity benefit our results of operations by restricting
competition. Newly introduced products, particularly those which treat conditions for which alternative treatments may not be readily available, in
particular may significantly contribute to sales. However, even protected products must compete with products of other manufacturers based on efficacy,
lack of adverse reactions and price. On the other hand, the loss or expiration of patent protection or regulatory exclusivity with respect to any of our
principal products could have a material adverse effect on our results of operations, as generic products, which tend to be quickly adopted once introduced,
may enter the market. Some of our principal products face, or are expected to face, considerable competition due to the expiration of patent or other
intellectual property protection. For example, following the expiration of patent protection over bortezomib, the active ingredient in VELCADE, one of
our largest selling products in the United States, a competing bortezomib-containing product has been introduced. This has led to a decrease in sales of
VELCADE, and further entry of competing products could result in substantial additional declines. In certain cases, generic competitors may successfully
challenge the validity of patents, or the manufacturer may decide that the benefits of prematurely launching “at risk” the generic drug outweigh the costs
of defending infringement litigation. In situations where the validity of patents or the value of the protection is challenged, we may record impairment
losses with respect to the relevant intangible property.
Impact of the Availability of Raw Materials
Our results of operations may be impacted if we are not able to internally or externally source critical raw materials. For example, human
plasma is a critical raw material in our plasma derived therapies. Efforts to increase the collection of plasma may include the contracting and regulatory
approval of additional plasma collection facilities and plasma fractionation facilitates. During the year ended March 31, 2019, our results of operations
were impacted by the fact that the demand to produce plasma derived therapies was greater than the supply of critical raw material needed.
Foreign Exchange Fluctuations
In the fiscal year ended March 31, 2019, 72.8% of our revenue was from outside of Japan, and we expect this ratio to further increase when
we consolidate a full year of Shire results. Changes in foreign exchange rates, particularly for the U.S. dollar and the euro, relative to the yen, which is
our reporting currency, will impact our revenues and expenses. When the yen weakens against other currencies, our revenues attributable to such other
currencies increase, having a positive impact on our results of operations, which may be offset by increased expenses denominated in such currencies.
52
Conversely, when the yen strengthens against other currencies, our revenues attributable to such currencies decrease, having a negative impact on our
results of operations, which may be offset by decreased expenses denominated in such currencies. To mitigate the risk exposed by foreign exchange
fluctuations, we utilize certain hedging measures with respect to some of our significant foreign currency transactions, primarily forward exchange
contracts, currency swaps and currency options for individually significant foreign currency transactions.
Periodic Trends
Our revenues, operating profit and net income were lower in the fourth quarter of each of the fiscal years ended March 31, 2017, 2018 and
2019, due mainly to fluctuations in sales in Japan. Japanese pharmaceutical product wholesalers generally control their inventory more tightly towards
their fiscal year ends, typically March 31, which causes decreased revenue in the fourth fiscal quarter. Japanese pharmaceutical product wholesalers
also tend to increase purchases ahead of the New Year holidays, causing a concentration of sales in our third fiscal quarter, from October 1 to December
31.
Critical Accounting Policies
Our consolidated financial statements have been prepared in accordance with IFRS. The preparation of our consolidated financial statements
requires management to make estimates and assumptions that affect the reported amount of assets and liabilities, the disclosure of contingent assets and
liabilities at the date of the financial statements and the reported amounts of revenues and expenses during the reported period. On an ongoing basis,
management evaluates its estimates and assumptions. Management bases its estimates and assumptions on historical experience and on various other
factors that it believes to be reasonable at the time the estimates and assumptions are made. Actual outcomes may differ from those estimates and
assumptions.
We believe the following critical accounting policies are affected by management’s estimates and assumptions, changes to which could have
a significant impact on our consolidated financial statements.
Revenue Recognition
Our revenue is primarily related to the sale of pharmaceutical products and is generally recognized when control of the products is passed to
the customer in an amount that reflects the consideration to which we expect to be entitled in exchange for those products. Our gross sales are subject
to various deductions, which are primarily composed of rebates and discounts to retail customers, government agencies, wholesalers, health insurance
companies and managed healthcare organizations. These deductions represent estimates of the related obligations, requiring the use of judgement when
estimating the effect of these sales deductions on gross sales for a reporting period. These adjustments are deducted from gross sales to arrive at net
sales. The U.S. market has the most complex arrangements related to revenue deductions.
The following summarizes the nature of the most significant adjustments to revenue:
•
•
U.S. Medicaid and Medicare: The U.S. Medicaid Drug Rebate Program is administered by state governments using state and federal
funds to provide assistance to certain vulnerable and needy individuals and families. Calculating the rebates to be paid related to this
program involves interpreting relevant regulations, which are subject to challenge or change in interpretative guidance by government
authorities. Provisions for Medicaid rebates are calculated using a combination of historical experience, product and population growth,
product pricing and the mix of contracts and specific terms in the individual state agreements. The U.S. Federal Medicare Program,
which funds healthcare benefits to individuals age 65 or older and certain disabilities, provides prescription drug benefits under Part
D section of the program. This benefit is provided and administrated through private prescription drug plans. Provisions for Medicare
Part D rebates are calculated based on the terms of individual plan agreements, product sales and population growth, product pricing
and the mix of contracts. There is often a time lag of several months between us recording the revenue deductions and our final
accounting for Medicare and Medicaid rebates.
Customer rebates: Customer rebates are offered to purchasing organizations, health insurance companies, managed healthcare
organizations, and other direct and indirect customers to sustain and increase market share, and to ensure patient access to our products.
Since rebates are contractually agreed upon, the related provisions are estimated based on the terms of the individual agreements,
historical experience, and projected product growth rates.
• Wholesaler chargebacks: We have arrangements with certain indirect customers whereby the customer is able to buy products from
wholesalers at reduced prices. A chargeback represents the difference between the invoice price to the wholesaler and the indirect
customer’s contractual discounted price. Provisions for estimating chargebacks are calculated based on the terms of each agreement,
historical experience and product growth rates.
•
Return reserves: When we sell a product providing a customer the right to return it, we record a provision for estimated sales returns
based on our sales return policy and historical return rates. We estimate the proportion of recorded revenue that will result in a return
by considering relevant factors, including past product returns activity, the estimated level of inventory in the distribution channel and
the shelf life of products.
Because the amounts are estimated, they may not fully reflect the final outcome, and the amounts are subject to change dependent upon,
amongst other things, the type of purchasing organization, end consumer, and product sales mix.
Historically, our adjustments of estimates, to reflect actual results or updated expectations, have not been material to our overall business.
Product-specific rebates, however, can have a significant impact on year- over-year individual product growth trends. If any of our ratios, factors,
53
assessments, experiences or judgments are not indicative or accurate predictors of our future experience, our results could be materially affected. The
sensitivity of our estimates can vary by program, type of customer and geographic location.
Impairment of Goodwill and Intangible Assets
We review long-lived intangible assets for impairment whenever events or changes in circumstance indicate that the asset’s balance sheet
carrying amount may not be recoverable. Goodwill and other currently not amortized intangible assets are reviewed for impairment at least annually.
As of March 31, 2019, we have ¥4,161.4 billion of goodwill and ¥4,860.4 billion of intangible assets which in aggregate represent 65.0% of our total
assets.
Intangible assets related to commercially marketed products are amortized using the straight-line method over the estimated useful life, which
is based on expected exclusivity period, ranging from three to 20 years. Intangible assets related to in-process research and development (“IPR&D”)
product rights are not amortized until the product is approved for sale by regulatory authorities in specified markets. At that time, we will determine the
useful life of the asset and begin amortization.
Assets are generally considered impaired when their balance sheet carrying amount exceeds their estimated recoverable amount. The recoverable
amount is estimated for each individual asset or at the larger cash generating unit level when cash is generated in combination with other assets. Goodwill
is allocated to cash generating units, or groups of cash generating units based on expected synergies as determined and the recoverable amount is estimated
at the cash generating unit level. Our cash generating units are identified base on the smallest identifiable group of assets that generate independent cash
inflows and are represented by the countries where we sell our products. The estimation of recoverable value requires us to make a number of assumptions
including:
•
•
•
•
•
•
amount and timing of projected future cash flows;
behavior of competitors (launch of competing products, marketing initiatives, etc.);
probability of obtaining regulatory approvals;
future tax rates;
terminal growth rate; and
discount rate.
Events that may result in the change in cash flows include IPR&D projects which are not successfully developed, and/or commercially marketed
products whose value becomes impaired, fail during development, are abandoned or subject to significant delay or do not receive the relevant regulatory
approvals. If these events were to occur, we may not realize the future cash flows that we have estimated nor recover the value of the initial or subsequent
R&D investments made subsequent to acquisition of the asset project.
Due to changes in these assumptions in subsequent periods, we have recognized impairments and reversal of impairments related to intangible
assets during the periods presented. See Notes 11 and 12 to our audited consolidated financial statements.
Retirement and Other Post-Employment Benefit Plans
We sponsor pension and other post-employment benefit plans that cover a significant portion of our employees. We are required to make
significant assumptions and estimates about future events in calculating the expense and the present value of the liability related to these plans. These
include assumptions about the interest rates we apply to estimate future defined benefit obligations and net periodic pension expense, as well as rates
of future pension increases. In addition, our actuarial consultants provide our management with historical statistical information such as withdrawal and
mortality rates in connection with these estimates. Assumptions and estimates used by us may differ materially from the actual results we experience
due to changing market and economic conditions, higher or lower withdrawal rates, and longer or shorter life spans of participants among other factors.
See Note 22 to our audited consolidated financial statements for sensitivity information related to the most significant assumptions. A significant change
in the assumptions in future periods could have a material impact on our consolidated financial statements. As of March 31, 2019, we have net defined
benefit liabilities of ¥156.5 billion.
Business Combination – Fair value
Accounting for a business combination requires us to estimate the fair value of the assets acquired and liabilities assumed and the value of
any contingent consideration. The estimate of fair value requires us to make a number of assumptions including estimated future cash flows, discount
rates, development and approval milestones, expected market performance and for contingent consideration the likelihood of payment.
Contingent consideration is recorded at fair value at the end of each period. The changes in the fair value based on time value of money are
recognized in Finance expenses while other changes are recognized in Other operating income or Other operating expenses on the consolidated statement
of income. During the year ended March 31, 2019, the change in fair value of contingent consideration reduced the amount to be paid to us by ¥2.2
billion.
Our estimates are based on our prior experiences and industry knowledge. We believe that our estimates are reasonable, but actual outcomes
could differ significantly from our estimates. A significant change in our estimates used to value acquired asset groups or business combinations could
result in future write-downs of tangible or intangible assets acquired by us and could, therefore, materially impact our financial position and profitability.
If the value of the liabilities assumed by us, including contingent liabilities, is determined to be significantly different from the amounts previously
recorded in purchase accounting, we may need to record additional expenses, which could materially impact our financial position and profitability.
54
Legal Contingencies
We are involved in various legal proceedings primarily related to product liability and commercial liability arising in the normal course of our
business. These contingencies are described in detail in Note 32 to our consolidated financial statements.
These and other contingencies are, by their nature, uncertain and based upon complex judgments and probabilities. The factors we consider
in developing our provision for litigation and other contingent liability amounts include the merits and jurisdiction of the litigation, the nature and the
number of other similar current and past litigation cases, the nature of the product and the current assessment of the science subject to the litigation, and
the likelihood of settlement and current state of settlement discussions, if any. In addition, we record a provision for product liability claims incurred,
but not filed, to the extent we can formulate a reasonable estimate of their costs based primarily on historical claims experience and data regarding
product usage. We also consider the insurance coverage we have to diminish the exposure for periods covered by insurance. In assessing our insurance
coverage, we consider the policy coverage limits and exclusions, the potential for denial of coverage by the insurance company, the financial condition
of the insurers, and the possibility of and length of time for collection. Any provision and the related estimated insurance recoverable have been reflected
on a gross basis as liabilities and assets, respectively, on our consolidated balance sheets. As of March 31, 2019, we have a provision of ¥46.8 billion
for outstanding legal cases and other disputes.
Income Taxes
We prepare and file our tax returns based on an interpretation of tax laws and regulations, and we record estimates based on these judgments
and interpretations. In the normal course of business, our tax returns are subject to examination by various taxing authorities, which may result in
additional tax, interest or penalty assessment by these authorities. Inherent uncertainties exist in estimates of many tax positions due to changes in tax
law resulting from legislation, regulation, and/or as concluded through the various jurisdictions’ tax court systems. When we conclude that it is not
probable that a taxing authority will accept an uncertain tax position, we recognize the best estimate of the expenditure required to settle a tax uncertainty.
The amount of unrecognized tax benefits is adjusted for changes in facts and circumstances. For example, adjustments could result from significant
amendments to existing tax law, the issuance of regulations or interpretations by the taxing authorities, new information obtained during a tax examination,
or resolution of a tax examination. We believe our estimates for uncertain tax positions are appropriate and sufficient based on currently known facts
and circumstances.
We also assess our deferred tax assets to determine the realizable amount at the end of each period. In assessing the recoverability of deferred
tax assets, we consider the scheduled reversal of taxable temporary differences, projected future taxable profits, and tax planning strategies. Based on
the level of historical taxable profits and projected future taxable profits during the periods in which the temporary differences become deductible, we
determine the amount the tax benefits we believe are realizable. As of March 31, 2019, we had unrecognized deferred tax benefits of ¥259.4 billion. A
change in our assumptions in future periods could have a significant impact on our income tax provision.
Restructuring Costs
We incur restructuring costs associated with planned initiatives to reduce our costs and in connection with the integration of our acquisitions.
Our most significant restructuring costs are severance payments and lease termination costs. We establish a provision for restructuring costs when the
plan has been approved, the cost can be estimated and the amount is probable of payment. The recognition of restructuring provision requires a number
of estimates including timing of payments and the number of individuals that will ultimately remain with the company to receive severance. As a result
of these estimates, the actual restructuring costs could differ from our estimates.
We expect to incur additional restructuring costs in the future related to the integration efforts associated with our acquisitions and divestitures.
As of March 31, 2019, we have a provision of ¥49.7 billion for restructuring costs. See Note 23 to our audited consolidated financial statements included
in this annual report for a further description of our restructuring provisions and the change between periods.
55
Results of Operations
The following table provides selected consolidated statements of income information for the years ended March 31, 2017, 2018 and 2019.
Revenue
Cost of Sales
Selling, general and administrative expenses
Research and development expenses
Amortization and impairment losses on intangible assets associated with products
Other operating income
Other operating expenses
Operating profit
Finance income
Finance expenses
Share of loss of investments accounted for using the equity method
Profit before tax
Income tax (expense) benefit
Net profit for the year
For the fiscal year ended March 31,
2017
2018
2019
(billions of yen)
¥
1,732.1
¥
1,770.5
¥
2,097.2
(558.8)
(619.1)
(312.3)
(156.7)
143.5
(72.9)
155.9
12.3
(23.2)
(1.5)
143.3
(27.8)
(495.9)
(628.1)
(325.4)
(122.1)
169.4
(126.6)
241.8
39.5
(31.9)
(32.2)
217.2
(30.5)
¥
115.5
¥
186.7
¥
(659.7)
(717.6)
(368.3)
(203.4)
159.9
(103.2)
205.0
16.8
(83.3)
(43.6)
94.9
14.1
109.0
Fiscal Year Ended March 31, 2019 compared with the Fiscal Year Ended March 31, 2018
Our results of operations for the fiscal year ended March 31, 2019 have been significantly impacted the Shire Acquisition. The following
summarizes the impact on our results of operations in the year end March 31, 2019 and on the change in our results between years.
For the fiscal year ended March 31,
Consolidated financial results
Impact from the Shire Acquisition
2018
2019
Change
versus
previous
year
Shire
operations
Purchase
accounting
Acquisition/
integration
costs
Total
impact
from Shire
Acquisition
Remaining
change
Change
versus
previous
year
(billions of yen)
¥ 1,770.5
¥ 2,097.2
¥
326.7
¥
309.2
¥
— ¥
— ¥
309.2
¥
(495.9)
(659.7)
(163.8)
(101.6)
(81.7)
—
(183.3)
Research and development expenses
(325.4)
(368.3)
(628.1)
(717.6)
(89.5)
(42.9)
(98.5)
(43.0)
(0.6)
—
(23.8)
(122.9)
(1.6)
(44.6)
(122.1)
(203.4)
(81.2)
(0.0)
(99.2)
169.4
159.9
(126.6)
(103.2)
241.8
39.5
(31.9)
205.0
16.8
(83.3)
(9.5)
23.4
(36.8 )
(22.7)
(51.4)
(1.4)
(4.9)
59.8
0.0
(10.6)
(32.2)
(43.6)
(11.4)
0.3
—
—
(59.6)
(85.0)
—
(41.3)
(99.2)
(1.4)
(64.5)
(206.8)
0.2
(56.1)
—
0.3
(11.7)
(126.3)
26.1
(262.5)
58.7
140.2
(14.1)
—
—
(181.6)
0.2
(4.2)
—
(185.6)
44.0
Profit before income tax
Income tax (expense) benefit
217.2
(30.5)
94.9
14.1
(122.3)
44.6
49.4
(11.3)
Net profit for the year
¥
186.7
¥
109.0
¥
(77.7)
¥
38.1
¥
(141.7) ¥
(100.2) ¥
(203.8)
¥
126.1
56
Revenue
Cost of sales
Selling, general and
administrative expenses
Amortization and impairment losses
on intangibles assets associated with
products
Other operating income
Other operating expenses
Operating profit
Finance income
Finance expense
Share of (loss) profit of investments
accounted for using the equity
method
17.5
19.6
33.4
1.7
18.0
(8.2)
88.0
170.0
(22.9)
4.8
Revenue. Revenue increased ¥326.7 billion, or 18.5%, to ¥2,097.2 billion for the fiscal year ended March 31, 2019, including ¥309.2 billion resulting
from the Shire Acquisition.
The remaining increase of ¥17.5 billion, or 1.0%, resulted from the continued expansion from three business areas (GI, oncology, and
neuroscience), which was partially offset by the divestitures and the unfavorable impact of foreign currency movements.
The following shows revenue by geographic region:
Revenue:
Japan
United States
Europe and Canada
Russia/CIS
Latin America
Asia (excluding Japan)
Other(1)
Total
_____________
Note:
(1)
Other region includes Middle East, Oceania and Africa.
For the fiscal year ended March 31,
2018
2019
(billions of yen, except percentages)
¥
580.3
598.3
313.7
68.2
75.7
104.0
30.2
32.8%
¥
33.8
17.7
3.9
4.3
5.9
1.7
571.0
829.0
405.6
59.7
88.1
105.4
38.3
27.2%
39.5
19.3
2.8
4.2
5.0
1.8
¥
1,770.5
100.0%
¥
2,097.2
100.0%
57
We rely on our key prescription drug products to generate a significant portion of our revenue. The following products had the most
significant impact on our results of operations.
For the fiscal year ended March 31,
2018
2019
Change versus the previous year
(billions of yen, except for percentages)
GI:
ENTYVIO
DEXILANT
PANTOPROZOLE
TAKECAB
AMITIZA
Oncology:
VELCADE
LEUPRORELIN
NINLARO
ADCETRIS
ICLUSIG
ALUNBRIG
Neuroscience:
TRINTRELLIX
Others:
AZILVA
ALOGLIPTIN
ULORIC
COLCRYS
Products acquired from Shire:
IMMUNOGLOBULIN
VYVANSE
ADVATE
ALBUMIN
GATTEX/REVESTIVE
ADYNOVATE
TAKHZYRO
NATPARA
¥
201.4
¥
269.2
¥
65.7
65.8
48.5
33.8
137.3
108.1
46.4
38.5
23.1
2.8
48.4
64.0
50.2
46.8
40.3
—
—
—
—
—
—
—
—
69.2
61.6
58.2
33.0
127.9
110.1
62.2
42.9
28.7
5.2
57.6
70.8
54.8
51.1
30.0
62.2
49.4
32.1
15.8
12.8
10.7
9.7
7.1
67.8
3.5
(4.2)
9.8
(0.9)
(9.4)
2.0
15.7
4.4
5.6
2.4
9.2
6.8
4.6
4.3
33.7%
5.3
(6.4)
20.1
(2.5)
(6.9)
1.9
33.9
11.4
24.1
84.0
19.0
10.6
9.1
9.1
(10.3)
(25.4)
62.2
49.4
32.1
15.8
12.8
10.7
9.7
7.1
N/A
N/A
N/A
N/A
N/A
N/A
N/A
N/A
Change in revenue was primarily attributable to the following products:
•
•
GI. In GI, revenue was driven by Takeda's top-selling product ENTYVIO (for ulcerative colitis and Crohn’s disease) with sales of ¥269.2
billion in the fiscal year ended March 31, 2019, an increase of ¥67.8 billion, or 33.7%. This increase was mainly attributable to ENTYVIO's
steady expansion of patient share in the bio-naïve segment. Takeda obtained an NDA approval in July 2018 in Japan for the treatment
of patients with moderately to severely active ulcerative colitis and launched the product in November 2018. Sales of TAKECAB (for
acid-related diseases) were ¥58.2 billion in the fiscal year ended March 31, 2019, an increase of ¥9.8 billion, or 20.1%, versus the
previous year. The increase was driven by the expansion of new prescriptions in the Japanese market due to TAKECAB's efficacy in
reflux esophagitis and the prevention of recurrence of gastric ulcers during low-dose aspirin administration.
Oncology. In oncology, sales of NINLARO (for multiple myeloma) were ¥62.2 billion, an increase of ¥15.7 billion, or 33.9%, versus
the previous year. Strong performance in several regions, particularly in the United States continued to contribute to the growth.
NINLARO is a once-weekly oral proteasome inhibitor with a profile of efficacy, safety, and convenience. Additionally, sales of ADCETRIS
(for malignant lymphomas) increased by ¥4.4 billion, or 11.4%, reflecting strong performance particularly in Japan and Brazil. Sales
of ICLUSIG (for leukemia) and ALUNBRIG (for lung cancer), obtained through the acquisition of ARIAD in February 2017, grew by
¥5.6 billion, or 24.1% and ¥2.4 billion, or 84.0%, respectively. Sales of VELCADE (for multiple myeloma), which lost market exclusivity
in the United States in previous year, decreased by ¥9.4 billion, or 6.9%.
58
•
Neuroscience. In neuroscience, sales of TRINTELLIX (for major depressive disorder) were ¥57.6 billion in the fiscal year ended March
31, 2019, an increase of ¥9.2 billion, or 19.0%, versus the previous year. Prescribers and patients increasingly made TRINTELLIX part
of their comprehensive approach to treat major depressive disorder.
The decrease in revenue resulting from divestitures was primarily due to the sale of seven long-listed products in Japan to Teva Takeda Yakuhin
Ltd. in May 2017, the disposition of Guangdong Techpool Bio-Pharma Co., Ltd. in May 2018, and the termination Takeda’s co-promotion and distribution
of XELJANZ in Japan in March 2018.
Shire contributed ¥309.2 billion to our revenue from the date of acquisition. As part of the integration, Takeda's distribution channel policies
were applied to the products acquired from Shire. This resulted in a one-time destocking at wholesalers as they lowered their days-on-hand of inventory
of commercial products, which resulted in lower revenue for products acquired from Shire. The sales were primarily from the following products:
•
•
•
•
GI. In GI, revenue was ¥21.5 billion primarily from the sales of GATTEX/REVESTIVE (for the treatment of short bowel syndrome)
that were ¥12.8 billion.
Rare diseases. In rare diseases, revenue was ¥111.2 billion including sales of ADVATE and ADYNOVATE (both for the treatment of
hemophilia A), TAKHZYRO (for the preventive treatment of hereditary angioedema), and NATPARA (for the treatment of
hypoparathyroidism) of ¥32.1 billion, ¥10.7 billion, ¥9.7 billion, and ¥7.1 billion, respectively.
Plasma derived therapies. In plasma derived therapies, revenue was ¥96.3 billion including sales of IMMUNOGLOBULIN (mainly
for the treatment of primary immunodeficiency and multifocal motor neuropathy) and ALBUMIN (primarily used for the hypovolemia
and hypoalbuminemia) of ¥62.2 billion and ¥15.8 billion, respectively.
Neuroscience. In Neuroscience, revenue was ¥60.1 billion including sales of VYVANSE (for the treatment of ADHD and moderate to
severe binge eating disorder) of ¥49.4 billion.
Cost of sales. Cost of sales increased ¥163.8 billion, or 33.0%, to ¥659.7 billion for the fiscal year ended March 31, 2019. This includes ¥101.6
billion related to sales of products acquired as part of the Shire Acquisition and the impact of ¥81.7 billion mainly due to non-cash charge from the
unwinding of the fair value step up on the inventory from the Shire Acquisition. This increase was offset by a decrease in remaining cost of sales of
¥19.6 billion, or 3.9%, primarily due to a more favorable product mix.
Selling, general and administrative (“SG&A”) expenses. SG&A expenses increased ¥89.5 billion, or 14.2%, to ¥717.6 billion for the fiscal
year ended March 31, 2019, primarily due to acquisition of Shire’s operations in our results of ¥98.5 billion and related acquisition costs of ¥23.8 billion.
This increase was partially offset by a decrease of remaining SG&A expenses of ¥33.4 billion due to a favorable impact of our global operating expense
reduction initiative as well as lower long-term share-based incentive payments to management.
Research and development expenses. Research and development expenses increased ¥42.9 billion, or 13.2%, to ¥368.3 billion, primarily
resulting from the acquisition of Shire. The remainder of our research and development expenses remained steady compared to the previous year.
Amortization and impairment losses on intangible assets associated with products. Amortization and impairment losses on intangible assets
associated with products increased by ¥81.2 billion, or 66.5%, to ¥203.4 billion for the fiscal year ended March 31, 2019. This represents an increase
of ¥99.2 billion related to amortization of intangible assets recorded in the Shire Acquisition and a ¥22.6 billion reversal of the COLCRYS impairment
recorded in the previous year. This increase was offset by lower amortization expense of ¥36.7 billion, which related to the VELCADE intangible asset
being fully amortized within the previous year.
Other operating income. Other operating income decreased ¥9.5 billion, or 5.6%, to ¥159.9 billion for the fiscal year ended March 31, 2019.
The decrease was primarily due to the net impact of ¥106.3 billion gain on the sale of Wako Pure Chemical Industries, Ltd. recorded in the previous
year, whereas we recorded a ¥50.3 billion gain on sale of property, plant and equipment and investment property including Takeda’s old headquarter
building in Tokyo as well as a ¥38.2 billion gain on sale of shares of the subsidiary, to which respective real estate businesses were transferred in the
current year.
Other operating expenses. Other operating expenses decreased ¥23.4 billion, or 18.5%, to ¥103.2 billion for the fiscal year ended March
31, 2019 which was a decrease of ¥88.0 billion partially offset by ¥59.6 billion of Shire integration costs. The decrease was primarily due to a decrease
of ¥22.8 billion in restructuring expense and other costs incurred in the prior year that did not reoccur in the current fiscal year such as a ¥41.5 billion
loss on the liquidation of a foreign subsidiary.
Net financial income / (expense). Net financial expense was a ¥66.4 billion in the current year, an increase of ¥74.1 billion compared to the
previous year, which includes ¥41.3 billion mainly related to interest on borrowings used to partially fund the Shire Acquisition. The remaining increase
is primarily due to a gain on an investment of ¥30.4 billion that was included in financial income in the prior year and is no longer be included in financial
income upon adoption of a new accounting standard.
Shares of loss of associates accounted for using the equity method. Shares of loss of associates accounted for using the equity method were
¥43.6 billion, an increase of ¥11.4 billion from the previous year. This primarily relates to Takeda’s share of an impairment charge recognized by Teva
Takeda Pharma Ltd. Teva Takeda Pharma Ltd. operates a business of long-listed products and generics and conducted a revaluation of its assets in
response to changes in the business environment.
59
Income tax expenses. Income tax expenses decreased ¥44.6 billion, or 146.3% from ¥30.5 billion for the fiscal year ended March 31, 2018
to tax benefit of ¥14.1 billion for the fiscal year ended March 31, 2019. This decrease was mainly due to tax benefit of ¥58.7 billion resulting from the
Shire Acquisition. Excluding the Shire Acquisition impact, the remaining income tax expenses increased ¥14.1 billion mainly due to an increase in profit
before tax, as well as the impact from the enactment of the Tax Cuts and Jobs Act (Tax Reform) in the U.S. in the previous year. These factors were
partially offset by capital loss related to restructuring of subsidiaries in the current year.
Fiscal Year Ended March 31, 2018 compared with the Fiscal Year Ended March 31, 2017
Revenue. Revenue increased ¥38.5 billion, or 2.2%, from ¥1,732.1 billion for the fiscal year ended March 31, 2017 to ¥1,770.5 billion for
the fiscal year ended March 31, 2018. During the fiscal year ended March 31, 2018, our revenue decreased by ¥94.3 billion as a result of divestitures,
which primarily consisted of ¥79.1 billion attributable to the divestiture of Wako Pure Chemical in April 2017 and ¥11.1 billion attributable to the
termination of the commercialization agreement for CONTRAVE in the U.S. in August 2016. Excluding the impact of divestitures, our revenues increased
by ¥132.8 billion primarily due to growth in our core therapeutic areas of GI, oncology and neuroscience, which includes the favorable impact of the
strengthening of the U.S. dollar and Euro against the yen as compared to the prior year.
The following shows revenue by geographic region:
Revenue:
Japan
United States
Europe and Canada
Russia/CIS
Latin America
Asia (excluding Japan)
Other(1)
Total
_____________
Note:
(1)
Other region includes Middle East, Oceania and Africa.
For the fiscal year ended March 31,
2018
2017
(billions of yen, except for percentages)
¥
655.3
520.2
279.7
57.5
72.5
112.8
34
37.8% ¥
30.0
16.1
3.3
4.2
6.5
2.0
580.3
598.3
313.7
68.2
75.7
104.0
30.2
32.8%
33.8
17.7
3.9
4.3
5.9
1.7
¥
1,732.1
100.0% ¥
1,770.5
100.0%
The following table shows revenue, including royalty income and service income, for our key prescription drug products by geographic
region:
For the fiscal year ended March 31,
2017
2018
Change versus previous year
(billions of yen, except for percentages)
ENTYVIO
United States
Europe and Canada
Emerging Markets
Total
NINLARO
Japan
United States
Europe and Canada
Emerging Markets
Total
VELCADE
United States
Other than United States
Total
ADCETRIS
Japan
¥
¥
¥
¥
¥
¥
¥
60
¥
133.6
¥
99.6
39.5
4.0
143.2
¥
— ¥
29.1
0.2
0.1
29.4
112.9
24.7
137.6
3.3
¥
¥
¥
¥
60.2
7.5
201.4
2.5
39.4
4.0
0.6
46.4
113.7
23.6
137.3
3.8
¥
¥
¥
¥
¥
¥
34.0
20.7
3.5
58.2
2.5
10.3
3.8
0.5
17.0
0.8
(1.1)
(0.3)
0.5
34.1%
52.4
87.5
40.6 %
N/A
35.4 %
1,900.0
500.0
57.8 %
0.7 %
(4.5)
(0.2)%
15.2 %
Europe
Emerging Markets
Total
TAKECAB
Japan(1)
Total
TRINTELLIX(2)
United States
Total
LEUPRORELIN
Japan (product name: LEUPLIN)(1)
United States
Europe and Canada
Emerging Markets
Total
DEXILANT
United States
Europe and Canada
Emerging Markets
Total
AZILVA
Japan(1)
Total
ALOGLIPTIN
Japan (product name: NESINA)(1)
United States
Europe and Canada
Emerging Markets
Total
ULORIC
United States
Europe and Canada
Emerging Markets
Total
COLCRYS
United States
Total
AMITIZA
United States
Europe and Canada
Total
PANTOPRAZOLE
United States
Europe and Canada
Emerging Markets
Total
LANSOPRAZOLE
Japan(1)(3)
For the fiscal year ended March 31,
2017
2018
Change versus previous year
(billions of yen, except for percentages)
17.5
9.3
30.1
34.1
34.1
31.9
31.9
48.6
18.3
31.1
16.3
114.2
49.7
5.7
7.3
¥
¥
¥
¥
¥
¥
¥
¥
¥
20.1
14.3
38.5
48.5
48.5
48.4
48.4
¥
¥
41.2
19.7
34.5
12.7
108.1
49.5
¥
6.4
9.9
62.6
¥
65.7
¥
¥
¥
¥
¥
¥66.9
66.9
32.9
5.2
6.1
4.9
49.1
41.4
0.7
0.1
¥64.0
64.0
26.6
6.0
9.0
8.6
50.2
45.8
¥
0.8
0.3
42.2
¥
46.8
¥
¥38.9
38.9
33.7
0.1
33.8
10.1
30.5
33.7
74.2
8.1
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥40.3
40.3
33.7
0.1
33.8
7.2
30.6
28.0
65.8
4.6
2.6
5.0
8.4
N/A
N/A
16.5
16.5
N/A
1.4
3.4
(3.6)
N/A
(0.2)
0.7
2.6
3.1
N/A
N/A
N/A
0.8
2.9
3.7
N/A
4.4
0.1
0.2
4.6
¥1.4
1.4
—
—
—
(2.9)
0.1
(5.7)
(8.4)
N/A
14.9
53.8
27.9 %
N/A
N/A
51.7 %
51.7 %
N/A
7.7 %
10.9
(22.1)
N/A
(0.4)%
12.3
35.6
5.0 %
N/A
N/A
N/A
15.4 %
47.5
75.5
N/A
10.6 %
14.3
200.0
10.9 %
3.6 %
3.6 %
0.0 %
—
0.0 %
(28.7)%
0.3
(16.9)
(11.3)%
N/A
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
61
United States
Europe and Canada
Emerging Markets
Total
CANDESARTAN
Japan(1)
United States
Europe and Canada
Emerging Markets
Total
For the fiscal year ended March 31,
2017
2018
Change versus previous year
(billions of yen, except for percentages)
20.0
7.1
9.2
44.4
14.8
0.6
9.3
9.5
¥
¥
34.2
¥
15.2
7.2
9.7
36.8
2.6
0.7
9.5
9.2
22.0
¥
¥
¥
(4.8)
0.1
0.5
N/A
N/A
0.1
0.2
(0.3)
N/A
(24.0)%
1.4
5.4
N/A
N/A
16.7 %
2.2
(3.2)
N/A
_____________
Notes:
(1)
Beginning from the fiscal year ended March 31, 2019, sales of certain products in Japan are disclosed on a net basis, deducting items such as
discounts and rebates, in alignment with the global managerial approach applied to individual product sales for the fiscal year ended March 31,
2018. Sales of individual products have been revised retroactively on a net basis to enable year-on-year comparisons. This reclassification has
no impact on Takeda’s financial statements and does not represent a correction of figures from the prior fiscal periods. Figures for the fiscal year
ended March 31, 2017 have not been reclassified retroactively.
TRINTELLIX is the brand name used since June 2016 for the product previously marketed as BRINTELLIX in the United States. The formulations,
indication and dosages of TRINTELLIX remain the same as that of BRINTELLIX.
Products excluding fixed dose combinations were transferred to Teva Takeda Yakuhin Ltd., a wholly-owned subsidiary of Teva Takeda Pharma
Ltd., a joint venture in Japan we formed with Teva Pharmaceutical Industries Ltd., in April 2016. Fixed dose combinations were sold to Teva
Takeda Yakuhin Ltd. in May 2017. Amounts presented above represent supply sales to Teva Takeda Yakuhin Ltd., following such transfers.
(2)
(3)
Change in revenue in our three key therapeutic areas of GI, oncology and neuroscience was primarily attributable to the following products:
•
•
•
GI. In the therapeutic area of GI, revenue grew 23.5% compared to the previous fiscal year. Revenue attributable to ENTYVIO was
¥201.4 billion in the fiscal year ended March 31, 2018, an increase of ¥58.2 billion, or 40.6%, compared to the previous fiscal year as
a result of increase in sales volume, making ENTYVIO our top-selling product. Revenue attributable to TAKECAB was ¥48.5 billion
(or ¥55.1 billion on a gross basis) in the fiscal year ended March 31, 2018, compared to ¥34.1 billion on a gross basis in the previous
fiscal year, with prescriptions in Japan as a result of a higher overall volume due to TAKECAB’s efficacy in reflux esophagitis and the
prevention of recurrence of gastric ulcers during low-dose aspirin administration.
Oncology. In the therapeutic area of oncology, revenue grew 14.6% compared to the previous fiscal year. Revenue attributable to
NINLARO was ¥46.4 billion, an increase of ¥17.1 billion, or 58.1% compared to the previous fiscal year, reflecting market penetration
across several regions, particularly in the United States. Revenue attributable to ICLUSIG, which was obtained through the acquisition
of ARIAD in February 2017, was ¥23.1 billion, its first full-year contribution to our revenue growth in this key therapeutic area.
ALUNBRIG, also obtained through the acquisition of ARIAD, was launched in the United States in May 2017, and revenue attributable
to it in the fiscal year ended March 31, 2018 was ¥2.8 billion. Revenue attributable to VELCADE decreased slightly to ¥137.3 billion
in the fiscal year ended March 31, 2018 from ¥137.6 billion in the previous fiscal year.
Neuroscience. In the therapeutic area of neuroscience, revenue grew 24.5% compared to the previous fiscal year. Revenue attributable
to TRINTELLIX was ¥48.4 billion, an increase of ¥16.5 billion, or 51.6%, versus the previous year, reflecting higher volumes as a result
of expansion of market share in the U.S. branded antidepressant market, driven by our patient engagement initiatives.
Cost of sales. Cost of sales decreased ¥62.8 billion, or 11.2%, from ¥558.8 billion for the fiscal year ended March 31, 2017 to ¥495.9 billion
for the fiscal year ended March 31, 2018. Cost of sales as a percentage of revenue decreased from 32.3% in the fiscal year ended March 31, 2017 to
28.0% in the fiscal year ended March 31, 2018. The decreases in cost of sales, both overall and relative to revenues, was primarily due to the disposition
of Wako Pure Chemical in April 2017, which generally had lower-margin products, as well as the effect of other changes to our product mix due to the
faster growth of higher margin products, such as ENTYVIO and NINLARO, relative to other products.
Selling, general and administrative expenses. Selling, general and administrative expenses increased ¥9.0 billion, or 1.5%, from ¥619.1 billion
for the fiscal year ended March 31, 2017 to ¥628.1 billion for the fiscal year ended March 31, 2018, mainly due to increased long-term incentive payments
to management, higher co-promotion expenses related to increased sales of TAKECAB in Japan and higher compensation costs, which contributed ¥2.6
billion, ¥4.8 billion and ¥3.8 billion, respectively. However, selling, general and administrative expenses increased at a lower rate than revenue, reflecting
our overall cost reduction efforts.
Research and development expenses. Research and development expenses increased ¥13.1 billion, or 4.2%, from ¥312.3 billion for the fiscal
year ended March 31, 2017 to ¥325.4 billion for the fiscal year ended March 31, 2018, mainly due to our pursuit of increased research and development
projects and the effect of a weaker Japanese yen.
62
Amortization and impairment losses on intangible assets associated with products. Amortization and impairment losses on intangible assets
associated with products decreased ¥34.6 billion, or 22.1%, from ¥156.7 billion for the fiscal year ended March 31, 2017 to ¥122.1 billion for the fiscal
year ended March 31, 2018. This was primarily driven by a decrease of impairment losses on intangible assets of ¥48.2 billion, including a ¥22.6 billion
reversal of the previous impairment related to COLCRYS, reflecting updated estimates about the amount of impairment due to better-than-expected sales
performance. This was offset in part by increased amortization of intangible assets of ¥13.6 billion, resulting from the inclusion of amortization of
intangible assets acquired in the ARIAD acquisition.
Other operating income. Other operating income increased by ¥25.9 billion, or 18.0%, from ¥143.5 billion for the fiscal year ended March 31,
2017 to ¥169.4 billion for the fiscal year ended March 31, 2018, driven mainly by ¥106.3 billion representing a gain on the sale of Wako Pure Chemical
in April 2017, ¥27.5 billion representing a gain on divestments to Teva Takeda Yakuhin Ltd. and ¥18.8 billion representing a gain on sales of property,
plant and equipment and investment property. Other operating income in the previous fiscal year was primarily driven by a ¥115.4 billion gain on
divestments to Teva Takeda Yakuhin Ltd and a ¥12.0 billion gain from the reversal of contingent consideration liability reflecting decreased expected
sales of COLCRYS.
Other operating expenses. Other operating expenses increased ¥53.7 billion, or 73.6%, to ¥126.6 billion for the fiscal year ended March 31,
2018, as compared to ¥72.9 billion for the fiscal year ended March 31, 2017. This was driven by a loss on liquidation of a foreign subsidiary of
¥41.5 billion primarily reflecting the recognition of cumulative translation losses and an increase in fair value of contingent consideration of ¥10.5 billion
driven by an increase in projected sales primarily for COLCRYS.
Income tax (expenses). Income tax expenses increased ¥2.7 billion, or 9.6%, from ¥27.8 billion for the fiscal year ended March 31, 2017 to
¥30.5 billion for the fiscal year ended March 31, 2018. This increase was mainly due to the tax impact of ¥22.8 billion resulting from the increase in
profit before tax compared to the previous fiscal year, as well as the effect of additional tax benefits recognized for the year ended March 31, 2017,
resulting from reduction of share capital of a subsidiary, which was responsible for an increase of ¥8.9 billion. These increases were offset in part by
the positive impact of the enactment of U.S. tax reforms, principally related to the revaluation of net deferred tax liability at a lower enacted tax rate
and improved recoverability of deferred tax assets, which resulted in a decrease of ¥27.5 billion.
B.
Liquidity and Capital Resources.
Sources and Uses of Liquidity
Our liquidity requirements mainly relate to operating cash, capital expenditures, contractual obligations, repayment of indebtedness and
payment of interest and dividends. Our operating cash requirements include cash outlays for research and development expenses, milestone payments,
sales and marketing expenses, personnel and other general and administrative costs and raw material costs. Income tax payments also require significant
cash outlays as well as working capital financing.
Our capital expenditures for tangible assets consist primarily of enhancing and streamlining our production facilities, replacing fully depreciated
items, and promoting efficiency of our operations. Our capital expenditures for intangible assets represent mainly milestone payments related to licensed
products, where such assets have been acquired from third-party partners, as well as software development expenditures. Our capital expenditures, which
consist of additions to property, plant and equipment and intangible assets recorded on our consolidated balance sheets, were ¥148.1 billion, ¥124.1
billion and ¥244.6 billion for the fiscal years ended March 31, 2017, 2018, and 2019, respectively. As of March 31, 2019, we had contractual commitments
for the acquisition of property, plant and equipment of ¥34.0 billion.
Our dividend payments for the fiscal years ended March 31, 2017, 2018 and 2019 were ¥141.7 billion, ¥141.9 billion and ¥143.0 billion,
respectively. It is our intention to continue to return capital to shareholders using dividends at an annual level of ¥180 per share, consisting of interim
and fiscal year-end dividends of ¥90 per share. See “Item 8. Financial Information-A. Consolidated Statements and Other Financial Information-
Dividends” for a description of our dividend policy.
We are required to make interest and principal payments on our outstanding borrowings. As of March 31, 2019, we have ¥122.7 billion of
interest due within one year and ¥988.1 billion of principal payments on our borrowings due within one year. See “-Borrowings and Financial Obligations.”
Our sources of liquidity include cash and cash equivalents on hand, short-term commercial paper, committed borrowing lines from financial
institutions and long-term debt financing from global capital markets. We monitor and adjust the amount of foreign cash based on projected cash flow
requirements. As the majority of our business is conducted outside Japan, we hold a significant portion of cash outside of Japan. Our ability to use foreign
cash to fund cash flow requirements in Japan may be impacted by local regulations and, to a lesser extent, income taxes associated with transferring
cash to Japan.
As of March 31, 2019, we held ¥702.1 billion in cash and cash equivalents on hand and ¥300.0 billion in undrawn commitment line. We
believe that working capital is sufficient for our current business requirements. Furthermore, we continually seek to ensure that our level of liquidity
and access to capital market funding continues to be maintained to successfully support our business operations.
Consolidated Cash Flows
The following table shows information about our consolidated cash flows during the fiscal years ended March 31, 2017, 2018 and 2019:
63
Net cash from operating activities
Net cash used in investing activities
Net cash from (used in) financing activities
Net increase (decrease) in cash and cash equivalents
Cash and cash equivalents at the beginning of the year
Effects of exchange rate changes on cash and cash equivalents
¥
¥
Net increase (decrease) in cash and cash equivalents resulting from a transfer to assets held for
sale
For the fiscal year ended March 31,
2017
2018
2019
(billions of yen)
261.4
¥
377.9
¥
328.5
(655.7)
289.9
(93.3)
(326.2)
(2,835.7)
2,946.2
(104.4) ¥
(41.7) ¥
451.4
(5.7)
(21.8)
319.5
(4.6)
21.3
439.0
294.5
(31.3)
(0.1)
702.1
Cash and cash equivalents at the end of the year
¥
319.5
¥
294.5
¥
Fiscal Year Ended March 31, 2019 compared with the Fiscal Year Ended March 31, 2018
Net cash from operating activities was ¥328.5 billion for the fiscal year ended March 31, 2019 compared to ¥377.9 billion for the fiscal year
ended March 31, 2018. The decrease of ¥49.4 billion was driven by a decrease in net profit of ¥77.7 billion and the impacts of certain unfavorable
adjustments including the lower income tax expenses of ¥44.6 billion primarily attributable to non-cash tax benefit on the impact of purchase accounting
of the Shire acquisition, the loss on liquidation of foreign operations of ¥41.5 billion recorded in the previous fiscal year, as well as the effect of changes
in assets and liabilities such as higher employee bonus payments in the fiscal year ended March 31, 2019.
These were partially offset by certain favorable non-cash adjustments such as the increase in depreciation and amortization of ¥90.3 billion
mainly attributable to intangible assets recorded upon the acquisition of Shire and the decrease in inventories by ¥45.0 billion primarily attributable to
unwinding of the fair value step up recorded in relation to the Shire Acquisition. This also includes other favorable adjustments such as the increase in
net financial income and expenses by ¥74.1 billion primarily due to the financial expense recorded in connection with the acquisition of Shire.
Net cash used in investing activities was ¥2,835.7 billion for the fiscal year ended March 31, 2019, compared to ¥93.3 billion for the fiscal
year ended March 31, 2018. This significant increase was primarily attributable to ¥2,891.9 billion of net consideration paid for the acquisition of Shire.
This was offset by ¥50.7 billion proceeds from the sale of real estate primarily attributable to the sale of our former headquarters building in the current
fiscal year.
Net cash used in financing activities was ¥2,946.2 billion for the fiscal year ended March 31, 2019, compared to net cash used in financing
activities of ¥326.2 billion for the fiscal year ended March 31, 2018. The current fiscal year mainly includes an increase of short-term loans of ¥367.3
billion and ¥2,795.9 billion proceeds from bonds and long-term loans of mainly for the acquisition of Shire.
Fiscal Year Ended March 31, 2018 compared with the Fiscal Year Ended March 31, 2017
Net cash from operating activities increased by ¥116.5 billion from ¥261.4 billion in the fiscal year ended March 31, 2017 to ¥377.9 billion
in the fiscal year ended March 31, 2018, primarily due to the impact of a higher net profit of ¥71.2 billion and the effect of certain favorable non-cash
expenses and other adjustments, including a gain on divestment of a business of ¥87.9 billion, a loss on liquidation of foreign operations of ¥41.5 billion
as well as a ¥30.7 billion loss relating to the share of loss of associates. Additional sources of operating cash flow were a ¥9.8 billion decrease in
inventories as a result of management effort to reduce inventory levels during the fiscal year ended March 31, 2018. These sources of cash were partially
offset by a higher impairment loss of ¥37.8 billion in fiscal year ended March 31, 2017 and a gain on sale of a business of ¥106.6 billion during the
fiscal year ended March 31, 2018.
Net cash used in investing activities was ¥93.3 billion for the fiscal year ended March 31, 2018, compared to ¥655.7 billion for the fiscal
year ended March 31, 2017. This decrease was primarily attributable to ¥583.1 billion of net consideration paid for the acquisition of ARIAD in the
fiscal year ended March 31, 2017. The decrease also reflects the effect of a payment of ¥71.8 billion into a restricted cash account in the fiscal year
ended March 31, 2018 in preparation for the acquisition of TiGenix NV. This was offset by ¥84.5 billion proceeds from the divestment of Wako Pure
Chemical in the same fiscal year.
Net cash used in financing activities was ¥326.2 billion for the fiscal year ended March 31, 2018, compared to net cash from financing
activities of ¥289.9 billion for the fiscal year ended March 31, 2017. This was primarily the result of repayments of ¥403.9 billion of short-term bridge
loans, ¥337.2 billion of proceeds from long-term loans related mainly to the refinancing of the bridge loan for the ARIAD acquisition, and repayments
of other long-term loans of ¥80.0 billion in the fiscal year ended March 31, 2018, compared to ¥407.0 billion of proceeds primarily from such short-
term bridge loans in the previous fiscal year.
64
Borrowings and Financial Obligations
Our total bonds and loans are ¥985.7 billion and ¥5,751.0 billion as of March 31, 2018 and 2019, respectively. These borrowings include
unsecured bonds and senior notes issued by Takeda in prior years, syndicated loans entered into by Takeda in prior years, borrowings obtained to fund
a portion of the Shire acquisition, and debt assumed in connection with the Shire acquisition and included in our consolidated statement of financial
position. Our borrowings are mainly linked to acquisitions and therefore are not exposed to seasonality.
The increase in bonds and loans relates to financing obtained to fund a portion of the Shire Acquisition and the debt assumed from Shire. In
connection with the Shire Acquisition, we entered into various borrowing arrangements as described in further detail below, including bridge financing
that was subsequently repaid. The borrowings entered into during the fiscal year ended March 31, 2019 that remain outstanding at the end of the fiscal
year are as follows:
•
•
•
•
Term Loan Credit Agreement with a total aggregate principal amount of $7.5 billion denominated in U.S. dollar and Euro was entered
into on June 8, 2018 and fully drawn in early January 2019. The proceeds drawn were used to fund a portion of the cash consideration
payable in connection with the Shire Acquisition. The borrowings under the Term Loan Credit Agreement are unsecured and accrue
interest based on floating rates, and will mature on January 3, 2024.
Euro denominated senior notes with a total aggregate principal amount of €7.5 billion were issued in November 2018 together with
U.S. dollar denominated senior notes with a total aggregate principal amount of $5.5 billion (collectively, the “2018 Notes”). The
2018 Notes were issued in the following series:
◦
◦
€1,250.0 million aggregate principal amount of 0.375% Senior Notes due November 21, 2020, €1,000.0 million aggregate
principal amount of the Senior Floating Rate Notes due November 21, 2020, €1,500.0 million aggregate principal amount
of 1.125% Senior Notes due November 21, 2022, €750.0 million aggregate principal amount of the Senior Floating Rate
Notes due November 21, 2022, €1,500.0 million aggregate principal amount of 2.250% Senior Notes due November 21,
2026, and €1,500.0 million aggregate principal amount of 3.000% Senior Notes due November 21, 2030.
$1,000.0 million aggregate principal amount of 3.800% Senior Notes due November 26, 2020, $1,250.0 million aggregate
principal amount of 4.000% Senior Notes due November 26, 2021, $1,500.0 million aggregate principal amount of 4.400%
Senior Notes due November 26, 2023, and $1,750.0 million aggregate principal amount of 5.000% Senior Notes due
November 26, 2028.
The 2018 Notes were issued in private placements in reliance on exemptions from registration under the U.S. Securities Act of 1933
(the “Securities Act”). Interest on the series of 2018 Notes, which are subject to fixed rates, is payable annually (in the case of the
Euro-denominated 2018 Notes) or semi-annually (in the case of the dollar-denominated 2018 Notes) in arrears. Interest on the series
of 2018 Notes which are subject to floating rates is determined by reference to three-month EURIBOR plus an applicable spread, reset
quarterly, and is payable quarterly in arrears.
An unsecured JBIC Loan Agreement for an aggregate principal amount $3.7 billion was entered into December 2018. The JBIC Loan
was fully drawn down in early January 2019 and will mature on December 11, 2025. The borrowings under the Term Loan Credit
Agreement are unsecured and accrue interest based on floating rates.
A ¥500 billion Senior Short-Term Loan ("SSTL") Facility Agreement entered into in October 2018. The SSTL was fully drawn in
early January 2019 and the proceeds were used to fund a portion of the cash consideration payable in connection with the Shire
Acquisition. The SSTL has a maturity of up to six months from the date of draw down at our option. In October 2018, we entered into
a Subordinated Loan Agreement providing for borrowings up to the same principal amount of the SSTL in order to allow for the
refinancing of any borrowings under the SSTL. However, the SSTL was repaid in June 2019 using the proceeds from the offering of
our Hybrid Bonds, described below, and no borrowings were made under the Subordinated Loan Agreement. Both the SSTL and
Subordinated Loan Agreement were cancelled in June 2019.
In connection with the Shire Acquisition, various borrowing arrangements previously held by Shire as described in further detail below were
assumed and are included in our consolidated statement of financial position. Such borrowings that remain outstanding at the end of the fiscal year are
as follows:
•
•
USD denominated senior notes (the “SAIIDAC Notes”) issued by Shire Acquisitions Investments Ireland Designated Activity Company
(“SAIIDAC”), a wholly-owned subsidiary of Shire, and guaranteed by us. The SAIIDAC Notes have a total aggregate principal amount
of $12.1 billion as of March 31, 2019. Interest is payable semi-annually in arrears. The following series of SAIIDAC Notes were
outstanding as of March 31, 2019: $3,300.0 million aggregate principal amount of 1.900% notes due September 23, 2019, $3,300.0
million aggregate principal amount of 2.400% notes due September 23, 2021, $2,500.0 million aggregate principal amount of 2.875%
notes due September 23, 2023 and $3,000.0 million aggregate principal amount of 3.200% notes due 2026.
USD denominated senior notes (the "Baxalta Notes") issued by Baxalta and guaranteed by us. The Baxalta Notes have a total aggregate
principal amount of $1.925 billion as of March 31, 2019. Interest on the Baxalta Notes is payable semi-annually in arrears. The following
series of Baxalta Notes were outstanding as of March 31, 2019: $404.5 million aggregate principal amount of 2.875% senior notes
due June 23, 2020, $219.4 million aggregate principal amount of 3.600% senior notes due June 23, 2022, $800.5 million aggregate
principal amount of 4.000% senior notes due June 23, 2025 and $500.4 million aggregate principal amount of 5.250% senior notes
due June 23, 2045.
65
On June 6, 2019, we issued hybrid bonds (subordinated bonds) (“Hybrid Bonds”) with an aggregate principal amount of ¥500 billion. We
used the proceeds from this Hybrid Bond offering to repay the SSTL.
The Hybrid Bonds will mature on June 6, 2079. Under the terms and conditions of the Hybrid Bond, we may make an early repayment of all
of the principal of the Hybrid Bonds on each interest payment date beginning October 6, 2024. Interest is payable semi-annually at a rate per annum
subject to revision. The Hybrid Bonds are unsecured and we are not subject to any financial covenants.
We currently have a Japanese unsecured commercial paper program in place to facilitate short-term liquidity management. We further have
short-term commitment line of ¥300 billion which are undrawn as of March 31, 2019.
We have certain borrowings outstanding as of March 31, 2019, that have restrictive financial covenants. The most restrictive of these covenants
is that our profit before tax must not be negative for two consecutive years, which is contained in the JBIC Loan Agreement described above. As of
March 31, 2019, we are in compliance with all such covenants. There are no restrictions on the ability to draw from the commitment line.
For further description of our borrowings, see Note 20 to our audited consolidated financial statements included in this annual report.
Credit Ratings
Our credit ratings, which reflect each rating agency’s opinion of our financial strength, operating performance and ability to meet our obligations,
as of the date of this annual report are as follows:
Rating agency
S&P Global Ratings
Category
Issuer credit rating/foreign currency long-term
and local currency long-term
Rating
BBB+
Issuer credit rating (short-term)
Moody’s
Long-term issuer rating and Long-term senior
unsecured rating
A-2
Baa2
Rating structure
Fourth highest of 11 rating categories and first within the
category based on modifiers (e.g. BBB+, BBB and BBB- are
within the same category).
Second highest of six rating categories
Fourth highest of nine rating categories and second highest
within the category based on modifiers (e.g., Baa1, Baa2 and
Baa3 are within the same category).
The ratings are not a recommendation to buy, sell or hold securities. The ratings are subject to revision or withdrawal at any time by the
assigning rating agency. Each of the financial strength ratings should be evaluated independently.
C.
Research and Development, Patents and Licenses, etc.
The information required by this item is set forth in "Item 4.B Business Overview - Research and Development" of this annual report.
D.
Trend Information.
The information required by this item is set forth in "Item 5.A Operating and Financial Review and Prospects - Operating Results" of this
annual report.
E.
Off-Balance Sheet Arrangements.
Milestone Payments
Under the terms of our collaborations with third parties for the development of new products, we may be required to make payments for the
achievement of certain milestones related to the development of pipeline products and the launch and subsequent marketing of new products. As of
March 31, 2018, and 2019, the contractual amount of potential milestone payments totaled ¥517.0 billion and ¥655.5 billion, respectively, in each case
excluding potential commercial milestone payments for pipeline products under development.
66
F.
Tabular Disclosure of Contractual Obligations.
The following table summarizes our contractual obligations as of March 31, 2019:
Bonds and loans: (2) (3)
Bonds
Loans
Purchase obligations for property, plant and equipment
Finance lease obligations
Operating lease obligations
Contributions to defined benefit plans(4)
Total(5) (6)
___________
Notes:
Total contractual
amount(1)
Less than one
year
One to three
years
Three to five
years
More than five
years
(billions of yen)
¥
3,790.2
¥
2,780.3
34.0
333.1
233.6
7.8
507.2
603.6
34.0
6.9
31.2
7.8
¥
1,197.7
¥
849.0
¥
1,236.3
228.1
—
18.4
52.7
—
978.4
—
19.4
38.4
—
970.2
—
288.5
111.3
—
¥
7,179.0
¥
1,190.7
¥
1,496.9
¥
1,885.2
¥
2,606.3
(1) Obligations denominated in currencies other than yen have been translated into yen using period-end exchange rates for the fiscal year ended
March 31, 2019 and may fluctuate due to changes in exchange rates.
Includes interest payment obligations.
(2) Repayment obligations may be accelerated if we breach the relevant covenants under the relevant instruments.
(3)
(4) Pension and post-retirement contributions cannot be determined beyond the fiscal year ending March 31, 2020 because the timing of funding
is uncertain and dependent on future movements in interest rates and investment returns, changes in laws and regulations and other variables.
(5) Does not include contractual obligations whose timing we are unable to estimate, including defined benefit contribution obligations, litigation
reserves and long-term income tax liability and does not include liabilities recorded at fair value as amounts will fluctuate based on any
changes in fair value including derivative liabilities and contingent consideration. Milestone payments that are dependent on the occurrence
of certain future events are not included.
(6) Does not include purchase orders entered into for purchases made in the normal course of business.
G.
Safe Harbor.
Statements in Item 5.E and Item 5.F of this annual report that are not statements of historical fact, constitute “forward-looking statements.”
See Special Note Regarding Forward-Looking Statements” on page 2 of this annual report. The Company is relying on the safe harbor provided in
Section 27A of the Securities Act of 1933, as amended, and Section 21E of the Exchange Act, as amended, in making such forward-looking statements.
Item 6. Directors, Senior Management and Employees
A.
Directors and Senior Management.
Directors
The following table provides information about Directors of the Company as of the date of this annual report.
Name
(Date of birth)
Christophe Weber
(November 14, 1966)
Responsibilities and
status within Takeda
Representative Director,
President and Chief Executive
Officer
("CEO")
End of term
Note 1
Business experience
Christophe Weber is President and CEO of Takeda. He joined
Takeda in April 2014 as Chief Operating Officer and Corporate
Officer, was named President and Representative Director in June
2014 and was subsequently appointed Chief Executive Officer in
April 2015. Prior to joining Takeda, Mr. Weber held positions of
including
responsibility at GlaxoSmithKline,
increasing
President and General Manager at GlaxoSmithKline Vaccines,
Chief Executive Officer of GlaxoSmithKline Biologicals SA in
Belgium, and member of the GlaxoSmithKline global Corporate
Executive Team. From 2008 to 2010, Mr. Weber served as Asia
Pacific SVP and Regional Director at GlaxoSmithKline Asia
Pacific in Singapore.
67
Name
(Date of birth)
Costa Saroukos
(April 15, 1971)
Responsibilities and
status within Takeda
Director and
Chief Financial Officer
(“CFO”)
Masato Iwasaki, Ph.D.
(November 6, 1958)
Director and President, Japan
Pharma Business Unit
Andrew S. Plump, M.D.,
Ph.D.
(October 13, 1965)
Director and President,
Research and Development
Olivier Bohuon
(January 3, 1959)
External Director
End of term
Note 1
Note 1
Note 1
Note 1
Business experience
finance
leadership positions with
Costa Saroukos has been Takeda’s Chief Financial Officer since
April 2018. He was appointed as Corporate Officer in April 2018
and Director in June 2019. Mr. Saroukos has over 20 years of
experience in both the private and public sectors, having held a
number of
financial
responsibility for businesses in over 100 countries across Asia-
Pacific, Europe, Africa and the Middle East. Mr. Saroukos has
been with Takeda since May 2015, as CFO of the Europe and
Canada business unit, significantly contributing
the
transformation of the business unit towards a specialty healthcare
provider. Prior to joining Takeda, Mr. Saroukos was at Allergan
as Head of Finance and Business Development for the Asia-Pacific
region, including China and Japan. He was also Finance Director
for Greater China and Japan. Previously, he spent 13 years at
Merck & Co. in roles of increasing responsibility, including
Executive Finance Director for EEMEA (Eastern Europe, Middle
East and Africa), Finance Director of South Korea and Head of
Internal Audit Asia Pacific and Global Joint Ventures.
to
Masato Iwasaki is the President of Takeda’s Japan Pharma
Business Unit. He joined Takeda in 1985 and had an extensive
career in roles of increasing responsibility in sales and marketing
under
the Pharmaceutical Marketing Division. In 2003,
Dr. Iwasaki was appointed Manager of Strategic Product Planning
and Project Leader for the Cardiovascular and Metabolic
franchise. He was appointed Senior Vice President of the Strategic
Product Planning department in 2008. In 2010, Dr. Iwasaki was
named Corporate Officer. Dr. Iwasaki has been a Director and
Member of our board of directors since 2012 and was named
President of the Japan Pharma Business Unit in 2015.
Andrew S. Plump, MD., Ph.D., is the President of Research and
Development at Takeda. Dr. Plump joined Takeda as Chief
Medical and Scientific Officer (“CMSO”) in 2015. In his position,
he leads our global research and development organization, where
he provides strategic direction and oversight. Prior to joining
Takeda, Dr. Plump served as Senior Vice President, Research and
Translational Medicine, Deputy to the President of research and
development at Sanofi, where he was responsible for global
research and translational medicine across all therapeutic areas.
Dr. Plump also spent more than 10 years at Merck in a Clinical
Pharmacology group, working on programs in neurodegeneration,
immunology, metabolism and infectious diseases.
Olivier Bohuon has been an External Director with Takeda since
January 2019. Prior to his appointment, Mr. Bohuon was an
External Director of Shire. Mr. Bohuon currently also holds the
position of External Director and Vice Chairman at LEO Pharma
A/S. Mr. Bohuon has previously served as External Director at
Virbac SA, External Director at Smiths Group plc, Chief
Executive Officer of Smith & Nephew plc, Chief Executive
Officer and President of Pierre Fabre Group SA and as President
of Abbott Pharmaceuticals; a division of US-based Abbott
Laboratories. He has also held diverse commercial leadership
positions at GlaxoSmithKline and its predecessor companies in
France.
68
Name
(Date of birth)
Ian Clark
(August 27, 1960)
Responsibilities and
status within Takeda
External Director
Yoshiaki Fujimori
(July 3, 1951)
External Director
Steven Gillis, PhD
(April 25, 1953)
External Director
Masahiro Sakane
(January 7, 1941)
External Director
Toshiyuki Shiga
(September 16, 1953)
External Director
End of term
Note 1
Business experience
Ian Clark has been an External Director with Takeda since January
2019. Prior to his appointment, Mr. Clark was an External
Director of Shire plc. He also currently holds External
Directorships
Inc., Corvus
at Agios Pharmaceuticals,
Pharmaceuticals, Inc., Guardant Health, Inc., AVROBIO Inc. and
Forty Seven Inc. Mr. Clark served as CEO and Director of
Genentech Inc. (part of the Roche Group) and Head of North
American Commercial Operations for Roche until 2016. From
2003 to 2010 he held the positions of Head of Global Product
Strategy and Chief Marketing Officer, Executive Vice President
—Commercial Operations and Senior Vice President and General
Manager—BioOncology at Genentech.
Note 1
Note 1
Note 1
Yoshiaki Fujimori has served as External Director of Takeda since
June 2016. Mr. Fujimori currently also serves as Advisor of LIXIL
Group Corporation. He previously served as External Director of
Tokyo Electric Power Company, Incorporated (currently Tokyo
Electric Power Company Holdings, Incorporated) and in a number
of senior leadership positions within the LIXIL Group, including
Representative Director, Chairman and CEO of LIXIL
Corporation. Mr. Fujimori has also served in a number of senior
positions in the General Electric Group, including Chairman of
GE Japan Corporation and Chairman, President and CEO of
General Electric Japan Ltd.
Dr. Steven Gillis has been and External Director with Takeda since
January 2019. Prior to his appointment, Dr. Gillis was an External
Director of Shire plc. He also currently holds the positions of
Managing Director at ARCH Venture Partners, External Director
of Pulmatrix, Inc., and External Director and Chairman, VBI
Vaccines, Inc. Dr. Gillis was a founder and Director of Corixa
Corporation, acquired by GlaxoSmithKline in 2005, and before
that a founder and Director of Immunex Corporation.
Masahiro Sakane has served as External Director of Takeda since
June 2014 and was appointed Chairman of the Board in June 2017.
Mr. Sakane currently also serves as Councilor of Komatsu Ltd.,
and External Director of Kajima Corporation. Mr. Sakane started
his career at Komatsu Ltd. in April 1963. In the Komatsu group,
he served in several senior leadership positions including
Chairman of the Board and Representative Director and President
and Representative Director of Komatsu Ltd. and Chief Operating
Officer ("COO") of Komatsu Dresser Company (currently
Komatsu America Corp.). Mr. Sakane has also served as External
Director of Nomura Holdings, Inc., External Director of Nomura
Securities Co., Ltd., External Director of Tokyo Electron Limited,
External Director of Asahi Glass Company, Ltd. and Vice
Chairman of Keidanren (Japan Business Federation).
Note 1
Toshiyuki Shiga has served as External Director of Takeda since
June 2016. Mr. Shiga currently also serves as Chairman and CEO
of INCJ, Ltd. and Director of Nissan Motor Co., Ltd. Mr. Shiga
started his career at Nissan Motor Co., Ltd. in April 1976. At
Nissan Motor Co., Ltd., he served in a number of leadership
positions including Vice Chairman, Chief Operating Officer and
Senior Vice President (Officer). He has also served as Chairman
of Japanese Automobile Manufacturers Association, Inc.Vice
Chairman of KEIZAI DOYUKAI (Japan Association of
Corporate Executives) and Chairman and CEO of Innovation
Network Corporation of Japan.
69
Name
(Date of birth)
Jean-Luc Butel
(November 8, 1956)
Responsibilities and
status within Takeda
External Director
Shiro Kuniya
(February 22, 1957)
External Director
Yasuhiko Yamanaka
(January 18, 1956)
Director (Audit and
Supervisory
Committee member)
Koji Hatsukawa
(September 25, 1951)
External Director (Head of
Audit and Supervisory
Committee)
Emiko Higashi
(November 6, 1958)
External Director (Audit and
Supervisory Committee
Member)
End of term
Note 1
Note 1
Note 2
Note 2
Note 3
Business experience
Jean-Luc Butel served as External Director and member of the
Audit and Supervisory Committee of Takeda from June 2016 to
June 2019. He was appointed External Director who is not a
member of the Audit and Supervisory Committee of Takeda in
June 2019. He currently also serves as Global Healthcare
Advisor, President of K8 Global Pte. Ltd and External Director
of Novo Holdings A/S. Mr. Butel previously served as
President, International, Corporate Vice President and
Operating Committee Member of Baxter International Inc. and
has held leadership positions at Medtronic, Inc., Johnson &
Johnson, Becton, Dickinson and Company and Nippon Becton
Dickinson Company, Ltd.
Shiro Kuniya served as External Director and Head of the
Audit and Supervisory Committee of Takeda from June 2016 to
June 2019. He was appointed External Director who is not a
member of the Audit and Supervisory Committee of Takeda in
June 2019. He currently also serves as Managing Partner of Oh-
Ebashi LPC & Partners, External Director of NEXON Co., Ltd.,
External Director of EBARA CORPORATION and External
Director of Sony Financial Holdings Inc. Mr. Kuniya was
registered as an attorney-at-law (Osaka Bar Association) and
joined Oh-Ebashi Law Offices in April 1982 and was also admitted
to practice law in New York State in the United States in May
1987. He has also previously served as our Outside Corporate
Auditor as well as Chairman of the Inter-Pacific Bar Association,
Outside Corporate Auditor of NIDEC CORPORATION and
Outside Corporate Auditor of Sunstar Inc.
Yasuhiko Yamanaka has served as Director and member of the
Audit and Supervisory Committee of Takeda since June 2016.
Mr. Yamanaka joined Takeda in April 1979 and has served in a
number of leadership positions within the company, including
Corporate Auditor, Special Missions, Special Missions assigned
by President, Assistant to CEO, Globalization of the Company,
Managing Director and Director.
Koji Hatsukawa has served as External Director and member of
the Audit and Supervisory Committee of Takeda since June 2016.
He was appointed Head of Audit and Supervisory Committee in
June 2019. He currently also serves as Outside Audit and
Supervisory Board Member of Fujitsu Limited and Audit and
Supervisory Board Member of The Norinchukin Bank.
Mr. Hatsukawa started his career at Price Waterhouse accounting
office in March 1974. Mr. Hatsukawa has previously served CEO
of PricewaterhouseCoopers Aarata and has held leadership
positions at ChuoAoyama PricewaterhouseCoopers and Aoyama
Audit Corporation. In addition, he has also served as an Audit and
Supervisory Board Member of The Norinchukin Bank and Outside
Audit and Supervisory Board Member of Accordia Golf co., Ltd.
Emiko Higashi served as External Director who is not a member
of the Audit and Supervisory Committee of Takeda from June 2016
to June 2019. She was appointed External Director who is a
member of the Audit and Supervisory Committee of Takeda in
June 2019. She currently also serves as Managing Director of
Tomon Partners, LLC, External Director of MetLife Insurance
K.K., External Director of KLA-Tencor Corporation and External
Director of Rambus Inc. Ms. Higashi previously served as
External Director of InvenSense Inc., CEO of Gilo Ventures, LLC,
Managing Director of Investment Banking, Merrill Lynch & Co.
and Director of Wasserstein Perella & Co., Inc.
70
Name
(Date of birth)
Michel Orsinger
(September 15, 1957)
Responsibilities and
status within Takeda
External Director (Audit and
Supervisory Committee
Member)
End of term
Note 3
Business experience
Michel Orsinger has served as External Director who is not a
member of the Audit and Supervisory Committee of Takeda from
June 2016 to June 2019. He was appointed External Director who
is a member of the Audit and Supervisory Committee of Takeda
in June 2019. He previously served as a Member of Global
Management Team of Johnson & Johnson, Worldwide Chairman,
Global Orthopedics Group of DePuy Synthes Companies of
Johnson & Johnson and President and Chief Executive Officer
and Chief Operating Officer of Synthes, Inc. (currently Johnson &
Johnson). He has also held several leadership positions at Novartis
AG, including Chief Executive Officer and President of OTC
Division Worldwide, Consumer Health; President of Global
Medical Nutrition, Consumer Health; and Regional President of
Europe, Middle East and Africa, Consumer Health.
_____________
Notes:
(1) The term of office for Directors who are not members of the audit and supervisory committee is from the end of the ordinary general meeting
of shareholders for the fiscal year ended March 31, 2019 through the end of the ordinary general meeting of shareholders for the fiscal year
ending March 31, 2020.
(2) The term of office for Directors who are also audit and supervisory committee members is two years. The term of office for these Directors
who are also audit and supervisory committee members is from the end of the ordinary general meeting of shareholders for the fiscal year
ended March 31, 2018 through the end of the ordinary general meeting of shareholders for the fiscal year ending March 31, 2020.
(3) Notwithstanding the Note (2) above, the term of office for Emiko Higashi and Michel Orsinger, Directors who are audit and supervisory
committee members, is from the end of the ordinary general meeting of shareholders for the fiscal year ended March 31, 2019 through the
end of the ordinary general meeting of shareholders for the fiscal year ending March 31, 2020. Since they were appointed as substitutes for
Shiro Kuniya and Jean-Luc Butel, who resigned as Directors who are audit and supervisory committee members at the end of the ordinary
general meeting of shareholders for the fiscal year ended March 31, 2018, their term of office will remain until the expiration of Shiro Kuniya
and Jean-Luc Butel as Directors who are audit and supervisory committee members, in accordance with the provision of the Articles of
Incorporation of Takeda.
Executive Officers
The following table provides information about the Company’s Executive Officers who are not also directors as of the date of this annual
report.
Name
(Date of birth)
Marcello Agosti
(June 2, 1971)
Responsibilities and
status within Takeda
Global Business
Development Officer
Business experience
In January 2019, Marcello Agosti became Global Business Development Officer. Mr.
Agosti is responsible for Takeda’s Business Development activities, including mergers
and acquisitions and corporate development.
Mr. Agosti has led the Shire Acquisition and several other acquisitions for Takeda,
including ARIAD Pharmaceuticals, transforming Takeda’s global oncology portfolio and
TiGenix, and strengthening the company’s GI leadership position. Mr. Agosti has also
led Takeda’s Global Commercial organization since 2015, which included the successful
launch of Takeda’s first global brand, ENTYVIO, now approved in more than 60 countries.
He has also held a number of leadership positions in Europe as Country Manager in France
and in Italy and as Area Head of Southern and Eastern Europe.
Prior to joining Takeda, Mr. Agosti worked in business development at Novartis in the
U.K. and Switzerland was also a consultant at McKinsey & Co.
71
Name
(Date of birth)
Teresa Bitetti
(September 21, 1962)
Responsibilities and
status within Takeda
President, Global Oncology
Business Unit
Business experience
In April 2019, Teresa Bitetti joined Takeda as President of the Global Oncology Business
Unit. She is responsible for oncology business activities.
Milano Furuta
(February 26, 1978)
Corporate Strategy Officer
and Chief of Staff
Helen Giza
(January 24, 1968)
Chief Integration and
Divestiture
Management Officer
Prior to joining Takeda, Ms. Bitetti was the Senior Vice President, Head of Worldwide
Oncology Commercialization at Bristol-Myers Squibb. In this role, Ms. Bitetti
significantly enhanced the long term strategic direction of the immuno-oncology portfolio.
In addition, she further enhanced the model of collaboration with the research and
development team to ensure the long term success of its marketed and pipeline Oncology
products. Some of her key leadership roles included, Senior Vice President and Head of
U.S. Oncology where she was responsible for the launch of Opdivo, President and GM
of BMS Canada, and Worldwide Head of the BMS Virology business.
Prior to joining Bristol-Myers Squibb, Ms. Bitetti held various roles of increasing
responsibility at Mobil Oil Corporation where she was part of the Capital Markets Group
and was responsible for the investment of Mobil's worldwide pension assets.
Milano Furuta joined Takeda’s corporate strategy and business development team in Japan
in 2010 and played a central role in the acquisition of a Switzerland-based pharmaceutical
company. After working on its post-merger integration and other corporate projects in
Switzerland, Mr. Furuta moved to Mexico where he led the Diabetes Business Unit and
launched new products in the areas of cardiovascular and metabolism area.
More recently, as Country Manager of Sweden, Mr. Furuta optimized commercial
organization and launched new oncology products which drove the growth of the specialty
care portfolio. From January 2019, he began his new role as Corporate Strategy Officer
and Chief of Staff.
Before joining Takeda, Mr. Furuta worked as an equity research analyst at an investment
management firm in the U.S. for two years. Previously, he spent six years in banking and
private equity investment in Japan, where he was engaged with several types of financial
transactions including leveraged buyouts and debt restructuring.
In January 2019, Helen Giza became Chief Integration and Divestiture Management
Officer. Ms. Giza is responsible for overseeing the success of the Shire integration into
Takeda, as well as the organization’s divestiture activities. Initially named as Takeda’s
Head of Integration in May 2018, Ms. Giza set up an integration team and built capabilities
that are being leveraged post-close to ensure the combination happens at pace, and in a
thoughtful, decisive and thorough manner.
Previously, Ms. Giza served as Senior Vice President, CFO of the U.S. Business Unit for
Takeda Pharmaceuticals, U.S.A, Inc. Ms. Giza has been involved in Takeda’s
transformation efforts serving as Executive sponsor of U.S. BPR (Business process re-
design) implementation and Takeda Business Services initiative and was actively involved
in the Global Opex program.
Ms. Giza was also the Vice President of Finance and Controller at TAP Pharmaceutical
Products Inc., a former joint venture between Takeda and Abbott.
Prior to joining TAP, Ms. Giza spent eight years in the automotive supply industry in the
U.K., holding a variety of finance leadership positions in large multinational companies.
She joined Abbott U.K. in 1999 as plant controller and went on to hold finance roles in
Abbott’s international division.
72
Name
(Date of birth)
Gerard Greco, Ph.D.
(February 8, 1962)
Responsibilities and
status within Takeda
Global Quality Officer
Business experience
In September 2014, Dr. Gerard Greco joined Takeda as Global Quality Officer. Dr. Greco
has more than 35 years of experience in quality leadership roles in the pharmaceutical
industry.
At Takeda, Dr. Greco has introduced key transformations by creating a Global Quality
Organization that aligns the quality units and establishes consistent quality systems and
programs across the network.
Prior to joining Takeda, Dr. Greco held positions of increasing responsibility at Johnson
& Johnson, Wyeth Pharmaceuticals, Pfizer Inc. and Teva Pharmaceuticals, where he
served as Senior Vice President of Global Quality Operations.
Haruhiko Hirate
(August 8, 1957)
Corporate
Communications and Public
Affairs Officer
Haruhiko Hirate became Takeda’s Corporate Communications and Public Affairs Officer
in October 2014. He previously served as President of North Asia in 2011, and has held
Corporate Officer and Senior Vice President positions at Takeda since 2010.
Julie Kim
(June 6, 1970)
President, Plasma-Derived
Therapies Business Unit
Prior to joining Takeda, Mr. Hirate held the position of Representative Senior Managing
Director at GlaxoSmithKline in Japan and, before that, Representative Director and
President of Banyu Pharmaceuticals, the Japanese subsidiary of Merck & Co. He joined
Banyu Pharmaceuticals in 2004 from his role as Senior Vice President at Merck & Co,
based in the U.S. He had previously held the position of Representative Director and
President at Roche Diagnostics based in Japan and before that, Asia Pacific Regional
President of Draeger.
Mr. Hirate began his career with Nissei Sangyo, a subsidiary of Hitachi, in 1980. During
his career at Hitachi group companies, he worked with former Boehringer Manheim, and
a series of overseas projects in the U.S. and Asia between 1980 and 1996.
Well respected in the Japanese pharmaceutical industry, Mr. Hirate served as Director at
the Federation of Pharmaceutical Manufacturers Associations of Japan and Chairman of
the Pharmaceutical Research and Manufacturers of America (“PhRMA”) Japan. In 2012,
he became a member of the Japan Association of Corporate Executives. In 2014, he
became Chairman of the International Affairs Committee at the Japan Pharmaceutical
Manufacturers Association.
In January 2019, Julie Kim joined Takeda as President of the Plasma-Derived Therapies
Business Unit and serves as a member of the Takeda Executive Team. She is responsible
for building a sustainable, high growth business focused on meeting the large and growing
global demand for plasma-derived products.
Previously at Shire/Baxalta/Baxter, Julie has held a diverse number of senior roles. She
led the access function for the entire Shire portfolio outside of the US, ran Global
Franchises for Shire Hematology and Baxter Immunology, managed country
organizations as North/South Europe Cluster Head for Baxalta Immunology and General
Manager for Baxter UK/Ireland, among other roles. Julie started her career as a consultant
in the US healthcare space.
Julie is a member of the Global Board for the Plasma Protein Therapeutics Association
(PPTA, a plasma industry organization). She is also a member of the Board for the Jeffrey
Modell World Immunodeficiency Network, part of the Jeffrey Modell Foundation.
73
Name
(Date of birth)
Mwana Lugogo
(January 30, 1970)
Responsibilities and
status within Takeda
Chief Ethics and
Compliance Officer
Ricardo Marek
(May 30, 1970)
President, Growth and
Emerging Markets Business
Unit
Yoshihiro Nakagawa
(July 26, 1960)
Global General Counsel
Giles Platford
(April 26, 1978)
President, Europe and
Canada Business Unit
Business experience
In October 2014, Mwana Lugogo became Takeda’s Chief Ethics & Compliance Officer.
Having joined Takeda in 2012, she initially established the Compliance function for our
Growth & Emerging Markets Business Unit.
In 2015, Ms. Lugogo was appointed to lead the newly-created Global Compliance
function. In this role, she is the custodian of Takeda’s Global Code of Conduct and is
responsible for the global ethics & compliance program. She also ensures that ethical
and reputational risks related to Takeda’s business are identified and addressed.
Before joining Takeda, Ms. Lugogo worked as an attorney in private practice in the U.S.,
U.K. and Central Asia for six years. In 2002, she moved into the corporate world with
Interbrew in Belgium. She moved to Switzerland in 2009, when she joined the Legal
department at Baxter Healthcare, responsible for Central and Eastern Europe, and
Emerging Markets.
Ricardo Marek is President of Growth and Emerging Markets ("GEM") Business Unit.
Mr. Marek has over 25 years of experience in various industries and leadership roles. He
has been with Takeda for eight years and over this time he simultaneously held the roles
of Area Head for Latin America (“LATAM”) since 2014, President for Brazil since 2013.
Prior to that, he was CFO of Brazil.
He led the realignment and restructuring of the LATAM area, positioning it as one of the
top performers across EM BU, and Takeda Brazil as one of the top 10 pharmaceutical
companies in the country. He also secured a number of acquisitions as well as launched
the Oncology business in the region for Takeda’s potentially life-saving and life-
transforming medicines. Under his leadership, Takeda was recognized for the first time
as a top employer in all seven countries across the LATAM region, and also received
several other HR awards, such as Great Place to Work.
Before joining Takeda in 2011, he was CFO for Organon International in the U.S., and
Managing Director and Vice President Finance for the Akzo Nobel Group in Brazil. He
also has experience in other industries such as chemicals and aerospace.
In October 2014, Yoshihiro Nakagawa was appointed Corporate Officer and Global
General Counsel of Takeda. He is responsible for the company’s global legal and
intellectual property organizations.
Mr. Nakagawa joined the company in 1983. At that time, he served in varying roles of
responsibility including reviewing, negotiating and drafting intellectual property and
technology-related licensing agreements as a member of the Patent & Trademark
Department.
In 1995, he moved to the Legal Department, then spent more than two years in London
as Company Secretary for Takeda Europe Holdings. Prior to his current appointment,
Mr. Nakagawa served as Senior Vice President of the Legal Department at Takeda
headquarters in Japan.
Giles Platford is President of Europe and Canada Business Unit for Takeda.
A seasoned industry leader with over 15 years of pharmaceutical experience, Giles was
formerly President of Emerging Markets for Takeda, where he oversaw the launch of
Takeda’s innovative pipeline across the region, and led the design and roll-out of Takeda’s
global access to medicines program.
Previously, Giles headed the Middle East, Turkey and Africa region where he strengthened
controls and compliance whilst re-engineering the business for growth. He also held
various leadership positions including General Manager Brazil, where he transformed
Takeda into a top 10 pharma industry player, being externally recognized for the first time
as one of the country’s top employers and best companies to work for.
Before joining Takeda in 2009, Giles spent eight years in Asia Pacific, where he assumed
a number of business development, commercial and general Management roles.
74
Name
(Date of birth)
Ramona Sequeira
(November 21, 1965)
Responsibilities and
status within Takeda
President, United States
Business Unit
Camilla Soenderby
(February 19, 1972)
Chief Patient Value and
Product Strategy Officer
Padma Thiruvengadam
(January 18, 1965)
Chief Human Resources
Officer
Business experience
Ramona Sequeira, President, United States Business Unit, is responsible for the
company’s commercial operations in the U.S. Ms. Sequeira joined Takeda in 2015.
Through her work with Takeda and prior to that with Eli Lilly, Ms. Sequeira has over 25
years of experience in the pharmaceutical industry. She has led businesses in Canada,
Europe and the U.S.
Ms. Sequeira is committed to the industry’s role in shaping a positive environment that
rewards pharmaceutical innovation and ensures patients have access to innovative
medicines that can help them have better health. She is a member of the PhRMA Board
of Directors, and was appointed, Chair, State Committee, PhRMA in April 2018. She is
also a member of the Board of Directors for Matter, a Chicago-based healthcare technology
incubator, and was previously a board member of the Association of the British
Pharmaceutical Industry. In addition, Ms. Sequeira is a member of the Board of Trustees
for Lake Forest Academy, a college preparatory boarding and day school for grades 9
through 12 located in Lake Forest, Illinois. She is also a member of the Chicago Executive
Club’s board.
Prior to Takeda, Ms. Sequeira received a B.Sc. with honors in molecular genetics and
molecular biology from the University of Toronto, and later received an MBA from
McMaster University in Canada.
In January 2019, Camilla Soenderby joined Takeda as Chief Patient Value and Product
Strategy Officer. Having previously joined Shire in March 2018, Camilla led and oversaw
Global Product Strategy, which comprised six franchises (rare diseases and specialty
conditions) as well as Global Market Access, Global Patient Services and Global
Commercial Operations.
Prior to joining Shire, Camilla was Region Head for Roche Pharma with profit and loss
responsibility for 11 countries in Central, South and Eastern Europe. Prior to that, she
worked as General Manager for Abbott (now AbbVie), first in Sweden and later in the
United Kingdom. She also held several operational and strategic roles of increasing
responsibility at Schering Plough in Asia Pacific, including General Manager for Taiwan.
Camilla began her career as a management consultant at McKinsey & Company focusing
on the bio-pharmaceutical and medical device industries.
Padma Thiruvengadam is a senior human resources executive with more than 25 years
of experience developing and implementing leading-edge people strategies and
organizational solutions. She was appointed as Takeda’s Chief Human Resources Officer
in June 2018 and is responsible for all HR strategies and programs supporting the
company’s global business.
Prior to joining Takeda, she served as Chief People Officer for Lego, with responsibility
for Human Resources and global organizational capability building.
Previously, Ms. Thiruvengadam was Corporate Vice President ("CVP") and Chief Human
Resources Officer with Integra Life Sciences. She joined Pfizer, first as Vice President,
Human Resources for Oncology and subsequently led global integration activities for
Pfizer Oncology following a major acquisition and later as Vice President, Asia Pacific
and Canada for the group’s Oncology Business Unit. Earlier in her career she worked as
a Senior Vice President and Human Resources Executive at Bank of America.
75
Name
(Date of birth)
Rajeev Venkayya,M.D.
(March 6, 1967)
Responsibilities and
status within Takeda
President, Global Vaccine
Business Unit
Business experience
Dr. Rajeev Venkayya serves as President of the Vaccine Business Unit. He joined Takeda
in 2012 to launch the global vaccine business, building upon a longstanding business in
Japan. Since then, he has formed a global organization and established a high-impact
vaccine pipeline that includes promising late-stage candidates for dengue and norovirus,
gained through the acquisitions of LigoCyte and Inviragen Inc. He concurrently serves
on the boards of two NGOs: CEPI (Coalition for Epidemic Preparedness Innovations),
and IAVI (International AIDS Vaccine Initiative).
Prior to Takeda, Dr. Venkayya served as Director of Vaccine Delivery in the Global Health
Program at the Bill & Melinda Gates Foundation, where he was responsible for the
Foundation’s efforts in polio eradication and new vaccine introduction, and a grant
portfolio of $500 million/year. While at the foundation, he served on the board of the
Global Alliance for Vaccines and Immunization (“GAVI”).
Dr. Venkayya was previously the Special Assistant to the President for Biodefense at the
White House. In this capacity, he oversaw U. S. preparedness for bioterrorism and
biological threats, and was responsible for the development and implementation of the
National Strategy for Pandemic Influenza. He first came to Washington though the non-
partisan White House Fellowship program in 2002.
Dr. Venkayya was trained in pulmonary and critical care medicine and served as an
Assistant Professor of Medicine in the Division of Pulmonary and Critical Care Medicine
at the University of California, San Francisco. He also served as co-director of the Medical
Intensive Care Unit and Director of the High-Risk Asthma Clinic at San Francisco General
Hospital.
Thomas Wozniewski,
Ph.D.
(July 26, 1962)
Global Manufacturing and
Supply Officer
In July 2014, Thomas Wozniewski, Ph.D. joined Takeda as Global Manufacturing and
Supply Officer. He has more than 20 years of experience in the pharmaceutical industry.
Dr. Wozniewski joined Takeda from Bayer Healthcare Switzerland, where he was Head
of Product Supply Consumer Care. In this role, he was responsible for the end-to-end
supply chain for all Bayer global OTC products. Prior to this, he served as Head of Global
Pharmaceuticals Product Supply at Bayer Healthcare AG and Schering AG in Germany.
While at Schering AG, he was also Head of Global Quality, Environment and Safety,
leading the development and implementation of an Integrated Management System for
the company. Dr. Wozniewski also worked at Boehringer Ingelheim, where he held several
positions in quality and production.
B.
Compensation.
The following table provides information about our executive officers whose compensation was greater than ¥100 million on an individual
basis in the fiscal year ended March 31, 2019.
Name
(Position)
Total
consolidated
compensation
(millions of yen)
Christophe Weber (Director)
Masato Iwasaki (Director)
1,758
193
Company
Takeda
Takeda
(Director portion)
Takeda
(Employee portion)(4)
Andrew S. Plump (Director)
795
Takeda
Amount of consolidated compensation by type (millions of yen)
Base
compensation
269(2)
16
27
12
Bonus
638
67
32
—
Long-term
incentive(1)
Other
851(3)
51(5)
—
—
—
—
—
—
Takeda Pharmaceuticals
International, Inc.(6)
115
378
255(7)
35(8)
_____________
Notes:
76
(1)
(2)
(3)
(4)
(5)
(6)
(7)
(8)
Compensation expense related to the long-term incentive plan is recognized over multiple fiscal years, depending on the length of the period
eligible for earning compensation. This column shows amounts recognized as expenses during the fiscal year ended March 31, 2019.
Base compensation includes the grossed up amount paid for residence and pension allowance for the relevant officer (¥112 million).
The amount recognized as an expense during the fiscal year, representing stock incentive plan (Board Incentive Plan) grants awarded in fiscal
years 2015 - 2018.
Shows the salary and other amounts earned as the President, Japan Pharma Business Unit. This employee portion of the bonus amount is not
included in the limit outlined in the proposal "Payment of Bonuses to Directors who are not Audit and Supervisory Committee Members" as
proposed at the 143th General Meeting of Shareholders held on June 27.
The amount recognized as an expense during the fiscal year, representing stock incentive plan (Board Incentive Plan) grants awarded in fiscal
years 2015 - 2018.
Shows the salary and other amounts earned as the President, Research and Development of Takeda Pharmaceuticals International, Inc.
The amount recognized as an expense during the fiscal year, representing stock incentive plan (Employee Stock Ownership Plan) grants awarded
in fiscal years 2015 - 2018.
Amounts of local retirement plan contributions and other additional benefits paid by Takeda Pharmaceuticals International, Inc. during the fiscal
year ended March 31, 2019, as well as the amount equal to taxes on such amounts.
Share-based Compensation Payments
We maintain certain share-based compensation payment plans for the benefit of our directors and certain of our employees. In the fiscal
years ended March 31, 2017, 2018 and 2019, we recorded total compensation expense related to our share-based payment plans of ¥17.4 billion,
¥22.2 billion and ¥18.8 billion, respectively, in our consolidated statements of income. For detailed information about our share-based compensation
plans, including our stock option plan, stock incentive plan, phantom stock appreciation rights and restricted stock units, see Note 28 to our audited
consolidated financial statements included in this annual report.
C.
Board Practices.
See “—A. Directors and Senior Management.” for information about the terms of service of the members of our Board of Directors and the
committees thereof.
Corporate Governance Structure
Under the Companies Act, joint stock corporations in Japan may adopt a corporate governance structure comprised of a board of directors
and an audit and supervisory committee, commonly referred to as the audit and supervisory committee system, in lieu of the traditional structure comprised
of a board of directors and a board of corporate auditors or the alternative structure comprised of a board of directors and three statutory committees.
The members of the audit and supervisory committee consist of three or more directors. We adopted the audit and supervisory committee system in June
2016, in order to increase transparency and independency of our board of directors, and further enhance our corporate governance, by establishing the
systems of audit and supervision conducted by the Audit and Supervisory Committee and increasing the proportion of the number of External Directors
and the diversity of our board of directors. This governance structure also enables us to enhance the separation of business execution and supervision
by delegating certain decision-making authority to individual members of our board of directors, realizing increased agility in decision-making and
helping the board of directors focus more on discussions of business strategies and particularly important business matters.
Board of Directors
Pursuant to the audit and supervisory committee system, our board of directors is comprised of directors who are audit and supervisory
committee members and directors who are not. Our articles of incorporation provide for a board of directors consisting of no more than 12 members
who are not audit and supervisory committee members and no more than four directors who are audit and supervisory committee members. All directors
are elected by our shareholders at a general meeting of shareholders, with directors who are audit and supervisory committee members elected separately
from other directors. The term of office for directors who are not audit and supervisory committee members expires at the close of the ordinary general
meeting of shareholders held with respect to the last fiscal year ended within one year after their election, and the term of office for directors who are
audit and supervisory committee members expires at the close of the ordinary general meeting of shareholders held with respect to the last fiscal year
ended within two years after their election. The current terms of our directors are set forth under "Item 6. Directors, Senior Management and Employees
—A. Directors and Senior Management." All directors may serve any number of consecutive terms. None of our directors have entered service contracts
with us or any of our subsidiaries providing for benefits upon termination of employment.
Our board of directors has the ultimate responsibility for the administration of our affairs. Our board of directors, however, may delegate
by its resolution some or all of its decision-making authority in respect of the execution of operational matters (excluding certain matters specified in
the Companies Act) to individual directors and has delegated such decision-making authority as described below. Our board of directors elect one or
more representative directors from among its members who are not audit and supervisory committee members. Each of the representative directors has
the authority to represent us in the conduct of our affairs.
Audit and Supervisory Committee
Our directors who are audit and supervisory committee members are not required to be certified public accountants. They may not serve
concurrently as executive directors, managers or any other type of employee for us or for any of our subsidiaries, or as accounting advisors or corporate
77
executive officers for any of our subsidiaries. In addition, more than half of our directors who are audit and supervisory committee members at any one
time must be external directors as defined under the Companies Act, who have not served as executive directors, corporate executive officers, managers
or any other type of employee for us or any of our subsidiaries for ten years prior to their election and fulfill certain other requirements specified in the
Companies Act.
The audit and supervisory committee has a statutory duty to audit the administration of our affairs by our directors, to examine the financial
statements and business reports to be submitted to the shareholders by a representative director, to prepare an audit report each year, to determine details
of proposals concerning the appointment and dismissal of independent auditors and the refusal to reappoint independent auditors for submission to
general meetings of shareholders and to determine the opinion on election, removal, resignation of or compensation for directors who are not audit and
supervisory committee members, which may be expressed at a general meeting of shareholders. An audit and supervisory committee member may note
his or her opinion in the audit report issued by the audit and supervisory committee if such an opinion differs from that expressed in the audit report.
Additionally, our Audit and Supervisory Committee serves as our “audit committee” for the purposes of Rule 10A-3 under the Exchange Act. We are
required to appoint and have appointed an independent auditor, who has a statutory duty of examining the financial statements to be submitted to the
shareholders by a Representative Director and preparing its audit report thereon. KPMG AZSA LLC currently acts as our independent auditor.
Takeda Executive Team
As management tasks continue to diversify, we have established a Takeda executive team under the President and Chief Executive Officer,
consisting of certain directors and employees in senior positions who manage and supervise our key functions, as well as a business review committee,
which is responsible for consideration and determination of general management matters, a portfolio review committee, which is responsible for research
and development and products-related matters, and a risk, ethics and compliance committee, which is responsible for internal audit, risk management
and compliance matters. Our board of directors has delegated all of its decision-making authority in respect of operational matters (excluding certain
matters specified in the Companies Act, as well as substantive matters valued at ¥100 billion or more or those matters which will have substantial impact
on us or our stakeholders) to the President and Chief Executive Officer, two directors belonging to the business review committee and one director
belonging to the portfolio review committee.
Nomination Committee and Compensation Committee
We also have voluntarily established a nomination committee and a compensation committee as advisory committees of the board of directors.
The majority of each committee's members must be “External Members” (either external directors or external experts). Furthermore, at least one director
who is an Audit and Supervisory Committee member must be assigned to each committee and each committee must be chaired by an external director.
As of the date of this annual report, the nomination committee consists of one external director who serves as chairman, two other external directors
and one other director who is not an external director, and the compensation committee consists of one external director who serves as chairman, one
other external director and one other director who is not an external director. Together, the committees serve to ensure transparency and objectivity in
decision-making relating to personnel matters for directors who are not external directors (including appropriate standards and procedures for appointment
and reappointment and establishing and administering appropriate succession plans) and the compensation system (including appropriate levels of
compensation for the directors, appropriate performance targets within the bonus system for directors and appropriate bonuses based on business results).
Also, by resolution of the Board of Directors, the authority to decide the amount of individual remuneration of Internal Directors who are not Audit and
Supervisory Committee members is delegated to the compensation committee, through which we have realized a more transparent process in determining
individual remuneration.
Limitation of Liability of Directors
Our articles of incorporation provide that we may enter into agreements with our directors (excluding executive directors as defined under
the Companies Act) to limit their respective liabilities to us arising from their failure to execute their duties in good faith and without gross negligence,
subject to applicable laws and regulations. We have entered into such agreements with our external directors, which limit the maximum amount of their
respective liabilities to us to the minimum amount stipulated by applicable laws and regulations, so long as those directors act in good faith and without
gross negligence in performing their duties.
D.
Employees.
As of March 31, 2019, we had 49,578 employees on a consolidated basis, of which 6,941 employees were based in Japan and 42,637 employees
were based outside Japan.
We have concluded a collective bargaining agreement with the Takeda Pharmaceutical Workers Union, through which we have established
sound relations with our employees in Japan. We hold regular dialogues with the union concerning, among other issues, conditions of employment and
human resources practices. Similarly, all of our group companies hold discussions with their respective workers unions and employee representatives
in accordance with local laws. We have an employee stock ownership association for employees of Takeda.
78
E.
Share Ownership.
The following table shows the number of shares owned by our directors as of March 31, 2019.
Directors
Name
Christophe Weber
Costa Saroukos
Masato Iwasaki
Andrew Plump
Masahiro Sakane
Olivier Bohuon
Ian Clark
Yoshiaki Fujimori
Steven Gillis
Toshiyuki Shiga
Shiro Kuniya
Jean-Luc Butel
Yasuhiko Yamanaka
Koji Hatsukawa
Emiko Higashi
Michel Orsinger
Total
Number of shares held
(of which, number of shares scheduled to
be issued pursuant to equity -
settled share-based compensation plans)
(thousands of shares)
293.6
(145.4)
12.6
(12.6)
21.8
(8.6)
52.8
(52.8)
5.4
(4.5)
—
—
—
—
6.7
(4.5)
—
—
6.3
(4.5)
6.3
(4.5)
6.5
(6.5)
25.6
(7.6)
5.7
(4.5)
6.5
(6.5)
6.5
(6.5)
456.6
(269.3)
Each of our directors held less than one percent of our total issued shares as of March 31, 2019. Shares held by directors have equal voting
rights as common stock held by other holders.
For detailed information about our share-based compensation plans, including our stock option plan, stock incentive plan, phantom stock
appreciation rights and restricted stock units, see Note 28 to our audited consolidated financial statements included in this annual report.
79
Item 7. Major Shareholders and Related Party Transactions
A.
Major Shareholders.
The following table sets forth the number of shares held of record by each of our principal shareholders as well as the percentage of our
issued shares held by each of our principal shareholders as of March 31, 2019.
Shareholder
The Bank Of New York Mellon as Depositary Bank for Depositary Receipt Holders(2)
The Master Trust Bank of Japan, Ltd. (Trust account)
Japan Trustee Services Bank, Ltd. (Trust account)
Nippon Life Insurance Company
Japan Trustee Services Bank, Ltd. (Trust account 5)
JP Morgan Chase Bank 380055
SSBTC Client Omnibus Account
State Street Bank West Client-Treaty 505234
State Street Bank and Trust Company 505001
Japan Trustee Services Bank, Ltd. (Trust account 1)
Total
___________
Notes:
Number of shares
held of record
(thousands, except percentages)
Percentage of
issued shares(1)
118,250
109,549
85,405
35,360
34,260
30,324
26,787
24,673
23,775
22,798
7.56%
7.00
5.46
2.26
2.19
1.94
1.71
1.58
1.52
1.46
511,183
32.66%
(1)
(2)
Percentage of issued shares excludes treasury stock held as of March 31, 2019. As of March 31, 2019, we held 10,225,845 shares of common
stock as treasury stock, which include 165,150 shares held by us, 9,975,569 shares held in trust for our stock-based compensation plans and
85,126 shares held by equity-method affiliates (based on our ownership percentage in them). The total number of issued shares, less treasury
stock, used to calculate percentages in the above table include such shares held in trust or by equity-method affiliates.
During the year ended March 31, 2019, The Bank of New York Mellon acquired 118,250 thousand (or 7.56%) of our shares which represents
a significant change from the past three years. This primarily represents shares issued to former shareholders of Shire in the form of ADSs in
connection with the Shire Acquisition.
Our major shareholders of common stock have the same voting rights as other holders of common stock.
As of March 31, 2019, there were 322 record holders of our common stock with addresses in the United States, whose shareholdings
represented approximately 28% of our outstanding common stock on that date. One such shareholder was The Bank of New York Mellon as depositary
for holders of American Depositary Shares, which held 118.2 million shares, or 7.56% of the total number of shares in issue, as of such date. Because
some of these shares were held by brokers or other nominees, the number of record holders with addresses in the United States might not fully reflect
the number of beneficial owners in the United States.
To the extent known to us, we are not directly or indirectly owned or controlled by any other corporation, by any foreign government or
by any other natural or legal person severally or jointly.
To our knowledge, there are no arrangements, the operation of which may at a subsequent date result in a change in control of us.
B.
Related Party Transactions.
From time to time, we enter into agreements and engage in transactions with a number of subsidiaries and affiliates in the ordinary course
of our business. Takeda has one major affiliate, Teva Takeda Pharma Ltd., to which Takeda sells products and acts as a sales agent. Total transactions
with Teva Takeda Pharma Ltd. for the year ended March 31,2019 was ¥10.4 billion. The terms and conditions of the related party transactions are entered
into on terms consistent with third-party transactions and considering market prices. In addition, the receivables and payables are settled in cash and
consistent with terms of third party settlements.
C.
Interests of Experts and Counsel.
Not applicable.
Item 8. Financial Information
A.
Consolidated Statements and Other Financial Information.
80
Our audited consolidated financial statements are included under “Item 18—Financial Statements”.
Legal Proceedings
The information required by this item is set forth in our consolidated financial statements included in this annual report. See Note 32 to
our audited consolidated financial statements included in this annual report for a detailed discussion of legal proceedings.
Dividends
Our capital resource management is based on the following:
•
•
•
•
investments in our internal research and development pipeline, foundational technology and ability to develop and bring to market
new products;
dividends as an important tool for returning capital to shareholders, while emphasizing capital gains for shareholders through
increased corporate value;
the maintenance of an investment-grade credit rating; and
disciplined alliances and acquisitions in order to strengthen our business around our key therapeutic areas.
As noted above, the return of capital to shareholders is one focus area for our management, and we believe our dividend policy is an
important tool for accomplishing our goals.
The following table sets forth the dividends paid with respect to each of our fiscal years indicated.
Dividends declared and paid
April 1, 2016 to March 31, 2017
Q1 2016
Q3 2016
April 1, 2017 to March 31, 2018
Q1 2017
Q3 2017
April 1, 2018 to March 31, 2019
Q1 2018
Q3 2018
Dividends declared and paid
April 1, 2019, to March 31, 2020
Q1 2019
B.
Significant Changes.
Total
dividends
(billions of
yen)
Dividends
per share
(yen)
Basis date
Effective date
71.1
71.1
71.1
71.2
71.5
71.5
90.00
90.00
90.00
90.00
90.00
90.00
March 31, 2016
June 30, 2016
September 30, 2016
December 1, 2016
March 31, 2017
June 29, 2017
September 30, 2017
December 1, 2017
March 31, 2018
June 29, 2018
September 30, 2018
December 3, 2018
Total
dividends
(billions of
yen)
Dividends
per share
(yen)
Basis date
Effective date
¥
140.8
¥
90.00
March 31, 2019
June 28, 2019
No significant change has occurred since the date of the annual financial statements.
Item 9. The Offer and Listing
A.
Offer and Listing Details.
See Item 9.C of this annual report.
B.
Plan of Distribution.
Not applicable.
C.
Markets.
81
In Japan, our common stock has been listed since 1949 on the Tokyo Stock Exchange. Our common stock is also listed on the Nagoya Stock
Exchange, the Fukuoka Stock Exchange and the Sapporo Securities Exchange. On each of these markets, our common stock trades under the securities
identification code “4502.”
ADSs, each representing 0.5 shares of our common stock, have been listed on the New York Stock Exchange since 2018 and trade under
the symbol “TAK.”
D.
Selling Shareholders.
Not applicable.
E.
Dilution.
Not applicable.
F.
Expenses of the Issue.
Not applicable.
Item 10. Additional Information
A.
Share Capital.
Not applicable.
B.
Memorandum and Articles of Association.
We are a joint-stock corporation incorporated in Japan under the Companies Act. The rights of our shareholders are represented by shares
of our common stock as described below, and shareholders’ liability is limited to the amount of subscription for such shares. As of March 31, 2019, our
authorized share capital consisted of 3,500,000,000 shares of common stock of which 1,565,005,908 shares were issued.
Only the holders of our common stock will be entitled to the shareholder rights described below. In order to exercise the rights described
below, holders of our ADSs will be required to withdraw their ADSs in favor of shares of our common stock in order to exercise their rights as shareholders.
Company Purpose
Article 3 of our Articles of Incorporation, which are included as an exhibit hereto, set forth our objects and purposes, which are to engage
in the following businesses:
• Manufacture, purchase and sale of medicines, chemicals for non-medicinal uses, quasi-medicines, medical instruments, appliances and
supplies, measuring equipments, cosmetics, food products, beverages, food additives, livestock feed additives and other chemical
products, and instruments, appliances and equipment relating to any of the foregoing products;
•
Trucking and freight forwarding;
• Warehousing;
•
Publishing;
• Management, purchase, sale and lease of real estate; and
•
Business ancillary or related to any of those specified in each foregoing clause.
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Book-Entry Transfer System
The Japanese book-entry transfer system for listed shares of Japanese companies under the Book-Entry Act of Japan (the “Book-Entry Act”)
applies to the shares of our common stock. Under this system, shares of all Japanese companies listed on any Japanese stock exchange are dematerialized.
Under the book-entry transfer system, in order for any person to hold, sell or otherwise dispose of listed shares of Japanese companies, they must have
an account at an account management institution unless such person has an account at Japan Securities Depository Center, Incorporated (the “JASDEC”).
“Account management institutions” are financial instruments business operators (i.e., securities firms), banks, trust companies and certain other financial
institutions that meet the requirements prescribed by the Book-Entry Act, and only those financial institutions that meet the further stringent requirements
of the Book-Entry Act can open accounts directly at JASDEC.
The following description of the book-entry transfer system assumes that the relevant person has no account at JASDEC.
Under the Book-Entry Act, any transfer of shares is affected through book-entry, and the title to the shares passes to the transferee at the
time when the transferred number of shares is recorded in the transferee’s account at an account management institution. The holder of an account at an
account management institution is presumed to be the legal owner of the shares held in such account.
Under the Companies Act, in order to assert shareholders’ rights against us, the transferee must have its name and address registered in the
register of our shareholders, except in limited circumstances. Under the book-entry transfer system, such registration is generally made upon receipt of
an all shareholders notice (soukabunushi tsuchi) (as described in “— Register of Shareholders”) from JASDEC. For this purpose, shareholders are
required to file their names and addresses with our transfer agent through the account management institution and JASDEC. See “— Register of
Shareholders” for more information.
Non-resident shareholders are required to appoint a standing proxy in Japan or provide a mailing address in Japan. Each such shareholder
must give notice of its standing proxy or a mailing address to the relevant account management institution. Such notice will be forwarded to our transfer
agent through JASDEC. Japanese securities firms and commercial banks customarily act as standing proxies and provide related services for standard
fees. Notices from us to non-resident shareholders are delivered to the standing proxies or mailing addresses.
Register of Shareholders
Under the book-entry transfer system, the registration of names, addresses and other information of shareholders in the register of our
shareholders will be made by us upon the receipt of an all shareholders notice (with the exception that in the event of the issuance of new shares, we
will register the names, addresses and other information of our shareholders in the register of our shareholders without an all shareholders notice from
JASDEC) given to us by JASDEC, which will give us such all shareholders notice based on information provided by the account management institutions.
Such all shareholders notice will be made only in cases prescribed under the Book-Entry Act such as when we fix the record date and when we make a
request to JASDEC with any justifiable reason. Therefore, a shareholder may not assert shareholders’ rights against us immediately after such shareholder
acquires our shares, unless such shareholder’s name and address are registered in the register of our shareholders upon our receipt of an all shareholders
notice; provided, however, that, in respect of the exercise of rights of minority shareholders as defined in the Book-Entry Act, a shareholder may exercise
such rights upon giving us an individual shareholder notice (kobetsukabunushi tsuchi) through JASDEC only during a certain period prescribed under
the Book-Entry Act.
Distribution of Surplus
Under the Companies Act, the distribution of dividends takes the form of distribution of Surplus (as defined in “—Restriction on Distribution
of Surplus”), and a distribution of Surplus may be made in cash and/or in kind, with no restrictions on the timing and frequency of such distributions.
The Companies Act generally requires a joint-stock corporation to make distributions of Surplus authorized by a resolution of a general meeting of
shareholders. However, in accordance with the Companies Act, our Articles of Incorporation provide that the board of directors has the authority to
make decisions regarding distributions of Surplus, except for limited exceptions, as provided by the Companies Act, as long as the company that has
both of an independent auditor and an audit and supervisory committee satisfies the following requirements:
(a)
(b)
the normal term of office of directors who are not audit and supervisory committee members expires at the close of the ordinary general
meeting of shareholders held with respect to the last fiscal year ended within one year after their election (our Articles of Incorporation
currently satisfies this requirement); and
its non-consolidated annual financial statements and certain documents for the latest fiscal year fairly present its assets and profit or loss,
as required by the ordinances of the Ministry of Justice.
A resolution of a general meeting of shareholders or the board of directors authorizing a distribution of Surplus must specify the kind and
aggregate book value of the assets to be distributed, the manner of allocation of such assets to shareholders and the effective date of the distribution. If
a distribution of Surplus is to be made in kind, we may, pursuant to a resolution of a general meeting of shareholders or the board of directors, grant a
right to the shareholders to require us to make such distribution in cash instead of in kind. If no such right is granted to shareholders, the relevant
distribution of Surplus must be approved by a special resolution of a general meeting of shareholders. See “— Voting Rights” for more details regarding
a special resolution. Our Articles of Incorporation provide that we are relieved of our obligation to pay any distributions in cash that go unclaimed for
three years after the date they first become payable.
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Restriction on Distribution of Surplus
Under the Companies Act, we may distribute Surplus up to the excess of the aggregate of (a) and (b) below, less the aggregate of (c) through
(f) below, as of the effective date of such distribution, if our net assets are not less than ¥3,000,000:
(a)
(b)
(c)
(d)
(e)
(f)
the amount of Surplus, as described below;
in the event that extraordinary financial statements as of, or for a period from the beginning of the fiscal year to, the specified date are
approved, the aggregate amount of (i) the aggregate amount as provided for by an ordinance of the Ministry of Justice as the net profit for
such period described in the statement of income constituting the extraordinary financial statements, and (ii) the amount of consideration
that we received for the treasury stock that we disposed of during such period;
the book value of our treasury stock;
in the event that we disposed of treasury stock after the end of the previous fiscal year, the amount of consideration that we received for
such treasury stock;
in the event described in (b) in this paragraph, the aggregate amount as provided for by an ordinance of the Ministry of Justice as the net
loss for such period described in the statement of income constituting the extraordinary financial statements; and
certain other amounts set forth in the ordinances of the Ministry of Justice, including (if the sum of one-half of goodwill and the deferred
assets exceeds the total of share capital, additional paid-in capital and legal earnings reserve, each such amount as it appears on the balance
sheet as of the end of the previous fiscal year) all or a certain part of such excess amount as calculated in accordance with the ordinances
of the Ministry of Justice.
For the purposes of this section, the amount of “Surplus” is the excess of the aggregate of (I) through (IV) below, less the aggregate of
(V) through (VII) below:
(I)
(II)
(III)
(IV)
the aggregate of other capital surplus and other retained earnings at the end of the previous fiscal year;
in the event that we disposed of treasury stock after the end of the previous fiscal year, the difference between the book value of such
treasury stock and the consideration that we received for such treasury stock;
in the event that we reduced our share capital after the end of the previous fiscal year, the amount of such reduction less the portion thereof
that has been transferred to additional paid-in capital and/or legal earnings reserve (if any);
in the event that we reduced additional paid-in capital and/or legal earnings reserve after the end of the previous fiscal year, the amount
of such reduction less the portion thereof that has been transferred to share capital (if any);
(V)
in the event that we cancelled treasury stock after the end of the previous fiscal year, the book value of such treasury stock;
(VI)
in the event that we distributed Surplus after the end of the previous fiscal year, the aggregate of the following amounts:
(1)
(2)
(3)
the aggregate amount of the book value of the distributed assets, excluding the book value of such assets that would be
distributed to shareholders but for their exercise of the right to receive dividends in cash instead of dividends in kind;
the aggregate amount of cash distributed to shareholders who exercised the right to receive dividends in cash instead of
dividends in kind; and
the aggregate amount of cash paid to shareholders holding fewer shares than the shares that were required in order to receive
dividends in kind;
(VII)
the aggregate amounts of (1) through (4) below, less (5) and (6) below:
(1)
(2)
(3)
(4)
(5)
in the event that the amount of Surplus was reduced and transferred to additional paid-in capital, legal earnings reserve and/
or share capital after the end of the previous fiscal year, the amount so transferred;
in the event that we distributed Surplus after the end of the previous fiscal year, the amount set aside in additional paid-in
capital and/or legal earnings reserve;
in the event that we disposed of treasury stock in the process of (x) a merger in which we acquired all rights and obligations
of a company, (y) a corporate split in which we acquired all or a part of the rights and obligations of a split company or (z) a
share exchange in which we acquired all shares of a company after the end of the previous fiscal year, the difference between
the book value of such treasury stock and the consideration that we received for such treasury stock;
in the event that the amount of Surplus was reduced in the process of a corporate split in which we transferred all or a part of
our rights and obligations after the end of the previous fiscal year, the amount so reduced;
in the event of (x) a merger in which we acquired all rights and obligations of a company, (y) a corporate split in which we
acquired all or a part of the rights and obligations of a split company or (z) a share exchange in which we acquired all shares
of a company after the end of the previous fiscal year, the aggregate amount of (i) the amount of other capital surplus after
such merger, corporate split or share exchange, less the amount of other capital surplus before such merger, corporate split or
share exchange, and (ii) the amount of other retained earnings after such merger, corporate split or share exchange, less the
amount of other retained earnings before such merger, corporate split or share exchange; and
84
(6)
in the event that an obligation to cover a deficiency, such as the obligation of a person who subscribed for newly issued shares
with an unfair amount to be paid in, was fulfilled after the end of the previous fiscal year, the amount of other capital surplus
increased by such payment.
In Japan, the “ex-dividend” date and the record date for any distribution of Surplus come before the date a company determines the amount
of distribution of Surplus to be paid.
For information as to Japanese taxes on dividends, please refer to “Taxation — Japanese Taxation.”
Capital and Reserves
Under the Companies Act, the paid-in amount of any newly-issued shares of stock is required to be accounted for as share capital, although
we may account for an amount not exceeding one-half of such paid-in amount as additional paid-in capital. We may generally reduce additional paid-
in capital and/or legal earnings reserve by resolution of a general meeting of shareholders, subject to completion of protection procedures for creditors
in accordance with the Companies Act, and, if so decided by the same resolution, we may account for the whole or any part of the amount of such
reduction as share capital. We may generally reduce share capital by a special resolution of a general meeting of shareholders subject to completion of
protection procedures for creditors in accordance with the Companies Act, and, if so decided by the same resolution, we may account for the whole or
any part of the amount of such reduction as additional paid-in capital or legal earnings reserve.
Stock Splits
Under the Companies Act, we may at any time split shares in issue into a greater number of the same class of shares by a resolution of the
board of directors or by determination of an individual director to whom the authority to make such determination has been delegated by resolution of
the board of directors. A company that has issued only one class of shares may amend its articles of incorporation to increase the number of the authorized
shares to be issued up to a number in proportion to the stock split by resolution of the board of directors or by determination of an individual director
to whom the authority to make such determination has been delegated by resolution of the board of directors, rather than a special resolution of a general
meeting of shareholders, which is otherwise required for amending the articles of incorporation. When a stock split is to be made, we must give public
notice of the stock split, specifying the record date therefor, at least two weeks prior to such record date.
Under the book-entry transfer system, on the effective date of the stock split, the numbers of shares recorded in all accounts held by our
shareholders at account management institutions will be increased in accordance with the applicable ratio.
Gratuitous Allocations
Under the Companies Act, we may allot any class of shares to our existing shareholders without any additional contribution by resolution
of the board of directors or by determination of an individual director to whom the authority to make such determination has been delegated by resolution
of the board of directors; provided that although our treasury stock may be allotted to our shareholders, any allotment of shares will not accrue to shares
of our treasury stock.
When a gratuitous allocation is to be made and we set a record date therefor, we must give public notice of the gratuitous allocation, specifying
the record date therefor, at least two weeks prior to the record date.
Under the book-entry transfer system, on the effective date of the gratuitous allocation, the number of shares of our common stock recorded
in accounts held by our shareholders at account management institutions will be increased in accordance with a notice from us to JASDEC.
Reverse Stock Split
Under the Companies Act, we may at any time consolidate our shares into a smaller number of shares by a special resolution of the general
meeting of shareholders. We must disclose the reason for the reverse stock split at the general meeting of shareholders. When a reverse stock split is to
be made, we must give public notice of the reverse stock split, at least two weeks (or, in certain cases where any fractions of shares are left as a result
of a reverse stock split, 20 days) prior to the effective date of the reverse stock split.
Under the book-entry transfer system, on the effective date of the reverse stock split, the numbers of shares recorded in all accounts held by
our shareholders at account management institutions will be decreased in accordance with the applicable ratio.
Unit Share System
General
Our Articles of Incorporation provide that 100 shares constitute one “unit” of common stock. Our board of directors or an individual director
to whom the authority to make such determination has been delegated by resolution of the board of directors is permitted to reduce the number of shares
that will constitute one unit or to abolish the unit share system entirely by amending our Articles of Incorporation, without shareholders’ approval, with
public notice without delay after the effective date of such amendment.
85
Transferability of Shares Constituting Less Than One Unit
Under the book-entry transfer system, shares constituting less than one unit are transferable. Under the rules of the Japanese stock exchanges,
however, shares constituting less than one unit do not comprise a trading unit, except in limited circumstances, and accordingly may not be sold on the
Japanese stock exchanges.
Voting Rights of a Holder of Shares Constituting Less Than One Unit
A holder of shares constituting less than one unit cannot exercise any voting rights pertaining to those shares. In calculating the quorum for
various voting purposes, the aggregate number of shares constituting less than one unit will be excluded from the number of outstanding shares. A holder
of shares representing one or more full units will have one vote for each full unit represented.
A holder of shares constituting less than one unit does not have any rights related to voting, such as the right to participate in a demand for the
resignation of a director, the right to participate in a request for the convocation of a general meeting of shareholders and the right to join with other
shareholders to propose a matter to be included in the agenda of a general meeting of shareholders.
Rights of a Holder of Shares Constituting Less Than One Unit to Require Us to Purchase Shares and to Sell Shares
Under the Companies Act, a holder of shares constituting less than one full unit may at any time request that we purchase such shares. In
addition, our Articles of Incorporation provide that, pursuant to our Share Handling Regulations, a holder of shares constituting less than one full unit
has the right to request that we sell to such holder such number of shares constituting less than one full unit which, when added to the shares constituting
less than one full unit currently owned by such holder, will constitute one full unit.
Under the book-entry system, such a request must be made to us through the relevant account managing institution. The price at which shares
of common stock constituting less than one unit will be purchased or sold by us pursuant to such a request will be equal to (a) the closing price of shares
of our common stock reported by the Tokyo Stock Exchange on the day when the request is received by our transfer agent or (b) if no sale takes place
on the Tokyo Stock Exchange on that day, the price at which the sale of shares of our common stock is executed on such stock exchange immediately
thereafter.
General Meeting of Shareholders
Our ordinary general meeting of shareholders is usually held every June in Japan. The record date for an ordinary general meeting of shareholders
is March 31 of each year. In addition, we may hold an extraordinary general meeting of shareholders whenever necessary by giving at least two weeks’
advance notice to shareholders.
Notice of convocation of a general meeting of shareholders setting forth the time, place, purpose thereof and certain other matters set forth in
the Companies Act and relevant ordinances must be mailed to each shareholder having voting rights (or, in the case of a non-resident shareholder, to
his or her standing proxy or mailing address in Japan) at least two weeks prior to the date set for such meeting. Such notice may be given to shareholders
by electronic means, subject to the consent of the relevant shareholders.
Any shareholder or group of shareholders holding at least 3% of the total number of voting rights for a period of six months or more may require,
with an individual shareholder notice (as described in “— Register of Shareholders”), the convocation of a general meeting of shareholders for a particular
purpose. Unless such general meeting of shareholders is convened without delay or a convocation notice of a meeting which is to be held not later than
eight weeks from the day of such demand is dispatched, the requiring shareholder may, upon obtaining a court approval, convene such general meeting
of shareholders.
Any shareholder or group of shareholders holding at least 300 voting rights or 1% of the total number of voting rights for a period of six months
or more may propose a matter to be included in the agenda of a general meeting of shareholders, and may propose to describe such matter together with
a summary of the proposal to be submitted by such shareholder in a convocation notice to our shareholders, by submitting a request to a director at least
eight weeks prior to the date set for such meeting, with an individual shareholder notice (as described in “— Register of Shareholders”).
The Companies Act enables a company to amend its articles of incorporation in order to loosen the requirements for the number of shares held
and shareholding period, as well as the period required for dispatching a convocation notice or submission of requests, all of which are required for any
shareholder or group of shareholders to request the convocation of a general meeting of shareholders or to propose a matter to be included in the agenda
of a general meeting of shareholders. Our Articles of Incorporation do not provide for loosening such requirements.
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Voting Rights
A shareholder of record is entitled to one vote per unit (100 shares) of common stock, except that neither we nor any corporation, partnership
or other similar entity in which we hold, directly or indirectly, 25% or more of the voting rights shall exercise any voting rights in respect of shares held
by us or such entity, as the case may be. Except as otherwise provided by law or by our Articles of Incorporation, a resolution can be adopted at a general
meeting of shareholders by a majority of the voting rights represented at the meeting. Shareholders may also exercise their voting rights through proxies,
provided that the proxy is granted to one of our shareholders having voting rights. The Companies Act and our Articles of Incorporation provide that
the quorum for the election of directors is one-third of the total number of voting rights. Our Articles of Incorporation provide that the shares may not
be voted cumulatively for the election of directors.
The Companies Act provides that a special resolution of the general meeting of shareholders is required for certain significant corporate
transactions, including:
•
•
•
•
•
•
•
•
•
•
•
•
any amendment to our Articles of Incorporation (except for amendments that may be made without the approval of shareholders under
the Companies Act);
a reduction of share capital, subject to certain exceptions under which a shareholders’ resolution is not required, such as a reduction of
share capital for the purpose of replenishing capital deficiencies;
transfer of the whole or a part of our equity interests in any of our subsidiaries, subject to certain exceptions under which a shareholders’
resolution is not required;
a dissolution, merger or consolidation, subject to certain exceptions under which a shareholders’ resolution is not required;
the transfer of the whole or a substantial part of our business, subject to certain exceptions under which a shareholders’ resolution is
not required;
the taking over of the whole of the business of any other corporation, subject to certain exceptions under which a shareholders’ resolution
is not required;
a corporate split, subject to certain exceptions under which a shareholders’ resolution is not required;
a share exchange (kabushiki kokan) or share transfer (kabushiki iten) for the purpose of establishing 100% parent-subsidiary relationships,
subject to certain exceptions under which a shareholders’ resolution is not required;
any issuance of new shares or transfer of existing shares held by us as treasury stock at a “specially favorable” price and any issuance
of stock acquisition rights or bonds with stock acquisition rights at a “specially favorable” price or on “specially favorable” conditions
to any persons other than shareholders;
any acquisition by us of our own shares from specific persons other than our subsidiaries;
reverse stock split; or
the removal of directors who are audit and supervisory committee members.
Except as otherwise provided by law or in our Articles of Incorporation, a special resolution of the general meeting of shareholders requires
the approval of the holders of at least two-thirds of the voting rights of all shareholders present or represented at a meeting where a quorum is present.
Our Articles of Incorporation provide that a quorum exists when one-third of the total number of voting rights is present or represented.
Liquidation Rights
If we are liquidated, the assets remaining after payment of all taxes, liquidation expenses and debts will be distributed among shareholders in
proportion to the number of shares they hold.
Rights to Allotment of Shares
Holders of shares of our common stock have no pre-emptive rights. Authorized but unissued shares may be issued at the times and on the terms
as the board of directors or an individual director to whom the authority to make such determination has been delegated by resolution of the board of
directors determines, so long as the limitations with respect to the issuance of new shares at “specially favorable” prices (as described in “— Voting
Rights”) are observed. Our board of directors or an individual director to whom the authority to make such determination has been delegated by resolution
of the board of directors may, however, determine that shareholders shall be given rights to allotment regarding a particular issue of new shares, in which
case such rights must be given on uniform terms to all holders of the shares as of a record date for which not less than two weeks’ prior public notice
must be given. Each shareholder to whom such rights are given must also be given notice of the expiration date thereof at least two weeks prior to the
date on which such rights expire. The rights to allotment of new shares may not be transferred. However, the Companies Act enables us to allot stock
acquisition rights to shareholders without consideration therefor, and such stock acquisition rights are transferable. See “— Stock Acquisition Rights”
below.
In cases where a particular issuance of new shares (i) violates laws and regulations or our Articles of Incorporation, or (ii) will be performed
in a manner materially unfair, and shareholders may suffer disadvantages therefrom, such shareholders may file an injunction with a court of law to
enjoin such issuance.
87
Stock Acquisition Rights
Subject to certain conditions and to the limitations on issuances at a “specially favorable” price or on “specially favorable” conditions described
in “— Voting Rights,” we may issue stock acquisition rights (shinkabu yoyakuken) and bonds with stock acquisition rights (shinkabu yoyakuken-tsuki
shasai) by a resolution of the board of directors or by determination of an individual director to whom the authority to make such determination has
been delegated by resolution of the board of directors. Holders of stock acquisition rights may exercise their rights to acquire a certain number of shares
within the exercise period as set forth in the terms of their stock acquisition rights. Upon exercise of stock acquisition rights, we will be obligated either
to issue the relevant number of new shares or, alternatively, to transfer the necessary number of shares of treasury stock held by us.
Record Date
The record date for annual dividends and the determination of shareholders entitled to vote at the ordinary general meeting of our shareholders
is March 31. The record date for interim dividends is September 30.
In addition, by a resolution of the board of directors or by determination of an individual director to whom the authority to make such determination
has been delegated by resolution of the board of directors, we may set a record date for determining the shareholders entitled to other rights and for other
purposes by giving at least two weeks’ prior public notice.
Under the rules of JASDEC, we are required to give notice of each record date to JASDEC promptly after setting such record date. JASDEC
is required to promptly give us notice of the names and addresses of the holders of shares of our common stock, the number of shares of our common
stock held by them and other relevant information as at each record date.
Purchase of Our Own Shares
Under the Companies Act and our Articles of Incorporation, we may acquire our own shares:
•
•
•
by purchase on any stock exchange on which our shares are listed or by way of tender offer, pursuant to a resolution of our board of
directors subject to certain requirements;
by purchase from a specific party other than any of our subsidiaries, pursuant to a special resolution of a general meeting of shareholders;
and
by purchase from any of our subsidiaries, pursuant to a resolution of the board of directors or determination of an individual director
to whom the authority to make such determination has been delegated by resolution of the board of directors.
If we acquire our own shares from a specific party other than any of our subsidiaries as specified above at a price higher than the greater of
(i) (a) the closing price of the shares at the market trading such shares on the day immediately preceding the day on which the relevant special resolution
of a general meeting of shareholders is made or (b) if no sale takes place at such market on that day, the price at which the sale of the shares is effected
on such market immediately thereafter and (ii) in the event that such shares are subject to a tender offer, the price set in the contract regarding such
tender offer on that day, shareholders may request that we include him or her as the seller of his or her shares in the proposed purchase. Any such
acquisition of shares must satisfy certain requirements, such as that we may only acquire our own shares in an aggregate amount up to the amount that
we may distribute as Surplus. See “— Distribution of Surplus” above for more details regarding this amount.
Our own shares acquired by us may be held by us as treasury stock for any period or may be cancelled by resolution of the board of directors
or by determination of an individual director to whom the authority to make such determination has been delegated by resolution of the board of directors.
We may also transfer the shares held by us to any person, subject to a resolution of the board of directors or determination of an individual director to
whom the authority to make such determination has been delegated by resolution of the board of directors, and subject also to other requirements similar
to those applicable to the issuance of new shares, as described in “— Rights to Allotment of Shares” above. We may also utilize our treasury stock (x) for
the purpose of transfer to any person upon exercise of stock acquisition rights or (y) for the purpose of acquiring another company by way of merger,
share exchange, or corporate split through exchange of treasury stock for shares or assets of the acquired company.
Request by Controlling Shareholder to Sell All Shares
Under the Companies Act and our Articles of Incorporation, in general, a shareholder holding 90% or more of our voting rights, directly or
through wholly-owned subsidiaries, shall have the right to request that all other shareholders other than us (and all other holders of stock acquisition
rights other than us, as the case may be) sell all shares (and all stock acquisition rights, as the case may be) held by them with our approval, which must
be made by a resolution of the board of directors or by determination of an individual director to whom the authority to make such determination has
been delegated by resolution of the board of directors (kabushiki tou uriwatashi seikyu or a “Share Sales Request”). In order to make a Share Sales
Request, such controlling shareholder will be required to issue a prior notice to us. If we approve such Share Sales Request, we will be required to make
a public notice to all holders and registered pledgees of shares (and stock acquisition rights, as the case may be) not later than 20 days before the effective
date of such sales.
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Sale by Us of Shares Held by Shareholders Whose Addresses Are Unknown
Under the Companies Act, we are not required to send a notice to a shareholder if notices to such shareholder fail to arrive for a continuous
period of five or more years at the registered address of such shareholder in the register of our shareholders or at the address otherwise notified to us.
In addition, we may sell or otherwise dispose of the shares held by a shareholder whose location is unknown. Generally, if
•
•
notices to a shareholder fail to arrive for a continuous period of five or more years at the shareholder’s registered address in the register
of our shareholders or at the address otherwise notified to us, and
the shareholder fails to receive distribution of Surplus on the shares for a continuous period of five or more years at the address registered
in the register of our shareholders or at the address otherwise notified to us,
we may sell or otherwise dispose of the shareholder’s shares at the market price after giving at least three months’ prior public and individual notices,
and hold or deposit the proceeds of such sale or disposal for the shareholder.
Reporting of Substantial Shareholdings
The Financial Instruments and Exchange Law of Japan and its related regulations require any person who has become beneficially, solely or
jointly, a holder of more than 5% of total issued shares of our common stock, to file with the director of a relevant local finance bureau of the Ministry
of Finance within five business days a report concerning such shareholdings. With certain exceptions, a similar report must also be filed in respect of
any subsequent change of 1% or more in any such holdings or any change in material matters set out in reports previously filed. For this purpose, shares
of our common stock issuable to such person upon exchange of exchangeable securities, conversion of convertible securities or exercise of warrants or
stock acquisition rights (including those incorporated in bonds with stock acquisition rights) are taken into account in determining both the number of
our shares held by the holder and our total issued shares.
C.
Material Contracts.
TiGenix NV
In connection with our acquisition of TiGenix NV, on January 5, 2018, we entered into an Offer and Support Agreement with TiGenix NV,
whereby we commenced an all cash voluntary and conditional public takeover bid for 100% of the securities with voting rights or giving access to voting
rights of TiGenix NV that are not already owned by Takeda or its affiliates, at a price of €1.78 per share in cash and an equivalent price for the ADSs,
warrants to acquire shares and 9% senior unsecured convertible bonds due March 6, 2018 of TiGenix NV. On July 31, 2018, we acquired all outstanding
ordinary shares as well as the ADSs and warrants of TiGenix NV following the expiration of the squeeze-out period and TiGenix NV became a wholly-
owned subsidiary of Takeda. Following the acquisition of all outstanding ordinary shares, ADSs and warrants of TiGenix NV, TiGenix NV was delisted
from Euronext Brussels and from Nasdaq.
Shire Acquisition
In connection with the Shire Acquisition, on May 8, 2018, we entered into a Co-operation Agreement with Shire, governing certain matters
leading to the closing of the Shire Acquisition. The Shire Acquisition was completed on January 8, 2019. On May 8, 2018, we entered into the Bridge
Credit Agreement totaling commitments of $30.85 billion with, among others, JPMorgan Chase Bank N.A., Sumitomo Mitsui Banking Corporation and
MUFG Bank, Ltd. On June 8, 2018, we entered into the Term Loan Credit Agreement for an aggregate principal amount of $7.5 billion with, among
others, JPMorgan Chase Bank N.A., Sumitomo Mitsui Banking Corporation, MUFG Bank, Ltd. and Mizuho Bank, Ltd., and on the same date entered
into Amendment No. 1 to the Bridge Credit Agreement to make certain technical changes thereto. On October 26, 2018, we entered into the SSTL with
an aggregate commitment of ¥500.0 billion, with Sumitomo Mitsui Banking Corporation, MUFG Bank, Ltd., Mizuho Bank, Ltd., The Norinchukin
Bank and Sumitomo Mitsui Trust Bank, Limited, and on the same date entered into Amendment No. 2 to the Bridge Credit Agreement to make certain
technical changes thereto. On October 26, 2018, we also entered into the Subordinated Loan Agreement, with aggregate commitments of ¥500.0 billion,
with Sumitomo Mitsui Banking Corporation, MUFG Bank, Ltd., Mizuho Bank, Ltd., The Norinchukin Bank and Sumitomo Mitsui Trust Bank, Limited,
which may be used, at our option to refinance all or a portion of the borrowings under the SSTL following the completion of the Shire Acquisition. On
November 21, 2018, we entered into a Fiscal Agency Agreement with MUFG Bank, Ltd., as Fiscal Agent, under which we issued a total aggregate
principal amount of €7.5 billion of senior notes on the same day. On November 26, 2018, we entered into an Indenture with MUFG Union Bank, N.A.,
as Trustee (the "Indenture"), under which we issued a total aggregate principal amount of $5.5 billion of senior notes on the same day. On December 3,
2018, we entered into the JBIC Loan with the Japan Bank for International Cooperation, for an aggregate principal amount of up to $3.7 billion. On
December 20, 2018 we entered into Amendment No. 1 to the Term Loan Credit Agreement to make certain technical changes thereto and entered into
Amendment No. 1 to the SSTL to make certain technical changes thereto. On December 21, 2018, we cancelled in full the remaining commitments
under the Bridge Credit Agreement. On December 25, we entered into Amendment No. 1 to the JBIC Loan to make certain technical changes thereto.
On June 6, 2019, we issued the Hybrid Bonds with an aggregate principal amount of ¥500 billion, and we used the proceeds from the Hybrid Bonds
offering to repay the SSTL. The Hybrid Bonds will mature on June 6, 2079 and, under the terms and conditions of the Hybrid Bonds, we may make an
early repayment of all of the principal of the Hybrid Bonds on each interest payment date beginning October 6, 2024. Interest on the Hybrid Bonds is
payable semi-annually at a rate per annum subject to revision. The Hybrid Bonds are unsecured and we are not subject to any financial covenants related
to these bonds.
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The Term Loan Credit Agreement and Amendment No. 1 thereto, the Fiscal Agency Agreement, the Indenture and the JBIC Loan and Amendment
No. 1 thereto are filed as exhibits hereto. English-language translations of the Subordinated Loan Agreement and the terms and conditions of the Hybrid
Bonds are also filed as exhibits hereto.
For a description of the agreements mentioned above as well as the effect of the Shire Acquisition on our financial condition and results of
operations, see “Item 5. Operating and Financial Review and Prospects—A. Operating Results—Acquisitions.”
Letter Agreement with Baxter
On January 11, 2016, Baxter International Inc. (“Baxter”), Shire and Baxalta entered into a letter agreement (the “Letter Agreement”) in
connection with the Shire’s acquisition of Baxalta, which, among other things, addresses certain aspects of a tax matters agreement entered into between
Baxter and Baxalta prior to their separation in July 2015.
Under the Letter Agreement, from and after the closing of Shire’s acquisition of Baxalta (which occurred on June 3, 2016), Baxalta agreed to
indemnify, and Shire agreed to guarantee such indemnity to, Baxter and each of its affiliates and each of their respective officers, directors and employees
against certain tax-related losses resulting from the acquisition (other than losses resulting from any disposition of Baxalta common stock by Baxter (i)
that are not attributable to the acquisition and (ii) other than in the initial distribution on July 1, 2015 and certain debt-for-equity exchanges, exchange
offers, contribution of Baxalta shares to Baxter’s U.S. pension fund or a dividend distribution to Baxter’s stockholders (in each case as contemplated
by the Letter Agreement).
The Letter Agreement is filed as an exhibit hereto.
Licensing and Collaboration Agreements
In the ordinary course of our business, we enter into agreements for licensing or collaboration in the development and commercialization of
products. Our business does not materially depend on any one of these agreements. Instead, they overall form a portion of our strategy to leverage a
mix of internal and external resources to develop and commercialize new products. Certain of the agreements which have led to successful
commercialization to date are summarized in “Item 4. Information on the Company—B. Business Overview—Licensing and Collaboration.” Our
Licensing and Collaboration Agreement with Seattle Genetics, Inc. is filed as an exhibit hereto to provide investors with an example of one such
agreement. We believe this agreement is representative of our licensing and collaboration agreements for marketed products in that it provides for the
payment of development and commercial milestone payments and sales-based royalties and sets forth the parties’ responsibilities relating to the terms
of co-development, co-manufacturing and co-marketing efforts, as well as providing for geographic limitations and limitations on term for the relevant
licensing and collaboration efforts. The specific terms of each of our licensing or collaboration agreements are negotiated individually. Agreements for
compounds still in development may have additional terms governing, for example, equity investments or other capital relationships.
D.
Exchange Controls.
The Foreign Exchange and Foreign Trade Act of Japan and related cabinet orders and ministerial ordinances, which we refer to collectively as
the Foreign Exchange Regulations, govern certain aspects relating to the acquisition and holding of shares by “exchange non-residents” and by “foreign
investors” (as these terms are defined below). It also applies in some cases to the acquisition and holding of ADSs representing shares of our common
stock acquired and held by exchange non-residents and by foreign investors. In general, the Foreign Exchange Regulations currently in effect do not
affect transactions between exchange non-residents to purchase or sell shares or ADSs outside Japan using currencies other than Japanese yen.
Exchange residents are defined in the Foreign Exchange Regulations as:
(i)
(ii)
individuals who reside within Japan; or
corporations whose principal offices are located within Japan.
Exchange non-residents are defined in the Foreign Exchange Regulations as:
(i)
(ii)
individuals who do not reside in Japan; or
corporations whose principal offices are located outside Japan.
Generally, branches and other offices of non-resident corporations located within Japan are regarded as exchange residents. Conversely, branches
and other offices of Japanese corporations located outside Japan are regarded as exchange non-residents.
Foreign investors are defined in the Foreign Exchange Regulations as:
(i)
(ii)
(iii)
individuals who do not reside in Japan;
corporations or other entities organized under the laws of foreign countries or whose principal offices are located outside Japan;
corporations of which 50% or more of the total voting rights are held, directly or indirectly, by individuals and/or corporations falling
within (i) and/or (ii) above; or
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(iv)
corporations or other entities having a majority of either (A) directors or other persons equivalent thereto or (B) directors or other
persons equivalent thereto having the power of representation who are non-resident individuals.
Acquisition of Shares
Acquisition by an exchange non-resident of shares of a Japanese corporation from an exchange resident requires post facto reporting by the
exchange resident to the Minister of Finance of Japan through the Bank of Japan. No such reporting requirement is imposed, however, if:
(i)
(ii)
the aggregate purchase price of the relevant shares is ¥100 million or less;
the acquisition is affected through any bank, financial instruments business operator or other entity prescribed by the Foreign Exchange
Regulations acting as an agent or intermediary; or
(iii)
the acquisition constitutes an “inward direct investment” described below.
Inward Direct Investment in Shares of Listed Corporations
If a foreign investor acquires shares of a Japanese company that are listed on a Japanese stock exchange, such as the shares of our common
stock, or that are traded on an over-the-counter market in Japan and, as a result of the acquisition, the foreign investor, in combination with any existing
holdings, directly or indirectly holds 10% or more of the issued shares of the relevant company, such acquisition constitutes an “inward direct investment”
and the foreign investor in general must file a report of the acquisition with the Minister of Finance and any other competent Ministers having jurisdiction
over that Japanese company by the 15th day of the month immediately following the month to which the date of such acquisition belongs. In limited
circumstances, such as where the foreign investor is in a country that is not listed on an exemption schedule in the Foreign Exchange Regulations, or
where that Japanese company is engaged in certain businesses designated by the Foreign Exchange Regulations (including the manufacturing of biological
preparations), a prior notification of the acquisition must be filed with the Minister of Finance and any other competent Ministers (including the Minister
of Health, Labour and Welfare). The proposed acquisition may not be consummated until 30 days have passed from the date of filing of such notification,
although this period will be shortened to two weeks unless such Ministers deem it necessary to review the proposed acquisition. The relevant Ministers
may extend the screening period up to five months if they deem it necessary to review the proposed acquisition and may recommend any modification
or abandonment of the proposed acquisition and, if such recommendation is not accepted, they may order the modification or abandonment of such
acquisition.
Acquisition of shares by foreign investors by way of stock split is not subject to any of the foregoing notification or reporting requirements.
Dividends and Proceeds of Sale
Under the Foreign Exchange Regulations, dividends paid on, and the proceeds from sales in Japan of, shares held by exchange non-residents
may generally be converted into any foreign currency and repatriated abroad.
E. Taxation.
Material U.S. Federal Income Tax Consequences
This section describes the material United States federal income tax consequences of owning ADSs. It applies to you only if you are a U.S.
holder (as defined below) and you hold your ADSs as capital assets for tax purposes. This discussion addresses only United States federal income taxation
and does not discuss all of the tax consequences that may be relevant to you in light of your individual circumstances, including foreign, state or local
tax consequences, estate and gift tax consequences, and tax consequences arising under the Medicare contribution tax on net investment income or the
alternative minimum tax. This section does not apply to you if you are a member of a special class of holders subject to special rules, including:
•
•
•
•
•
•
•
•
a dealer in securities,
a trader in securities that elects to use a mark-to-market method of accounting for securities holdings,
a tax-exempt organization,
a life insurance company,
a person that actually or constructively owns 10% or more of the combined voting power of our voting stock or of the total value of our
stock,
a person that holds ADSs as part of a straddle or a hedging or conversion transaction,
a person that purchases or sells ADSs as part of a wash sale for tax purposes, or
a person whose functional currency is not the U.S. dollar.
This section is based on the Internal Revenue Code of 1986, as amended, its legislative history, existing and proposed regulations, published
rulings and court decisions, all as currently in effect, as well as on the Convention Between the Government of the United States of America and the
Government of Japan for the Avoidance of Double Taxation and the Prevention of Fiscal Evasion with Respect to Taxes on Income (the “Treaty”). These
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laws are subject to change, possibly on a retroactive basis. In addition, this section is based in part upon the assumption that each obligation in the deposit
agreement will be performed in accordance with its terms.
If an entity or arrangement that is treated as a partnership for United States federal income tax purposes holds the ADSs, the United States
federal income tax treatment of a partner will generally depend on the status of the partner and the tax treatment of the partnership. A partner in a
partnership holding the ADSs should consult its tax advisor with regard to the United States federal income tax treatment of an investment in the ADSs.
You are a U.S. holder if you are a beneficial owner of ADSs and you are for United States federal income tax purposes:
•
•
•
•
a citizen or resident of the United States,
a domestic corporation,
an estate whose income is subject to United States federal income tax regardless of its source, or
a trust if a United States court can exercise primary supervision over the trust’s administration and one or more United States persons
are authorized to control all substantial decisions of the trust.
You should consult your own tax advisor regarding the United States federal, state and local tax consequences of owning and disposing of
ADSs in your particular circumstances.
In general, and taking into account the earlier assumptions, for United States federal income tax purposes, if you hold ADRs evidencing
ADSs, you will be treated as the owner of the shares represented by those ADRs. Exchanges of shares for ADRs, and ADRs for shares, generally will
not be subject to United States federal income tax.
The tax treatment of your ADSs will depend in part on whether or not we are classified as a passive foreign investment company, or PFIC,
for United States federal income tax purposes. Except as discussed below under “—PFIC Rules”, this discussion assumes that we are not classified as
PFIC for United States federal income tax purposes.
Distributions. Under the United States federal income tax laws, if you are a U.S. holder, the gross amount of any distribution we pay out of
our current or accumulated earnings and profits (as determined for United States federal income tax purposes), other than certain pro-rata distributions
of our shares, will be treated as a dividend that is subject to United States federal income taxation. If you are a noncorporate U.S. holder, dividends that
constitute qualified dividend income will be taxable to you at the preferential rates applicable to long-term capital gains provided that you hold the ADSs
for more than 60 days during the 121-day period beginning 60 days before the ex-dividend date and meet other holding period requirements. Dividends
that we distribute with respect to the ADSs will be qualified dividend income if the ADSs are readily tradable on an established securities market in the
United States in the year that we distribute the dividend. Our ADSs will be listed on the NYSE, in which case the ADSs will be treated as readily tradable
on an established securities market in the United States. We therefore expect that dividends that we distribute on our ADSs will be qualified dividend
income.
You must include any Japanese tax withheld from the dividend payment in this gross amount even though you do not in fact receive it. The
dividend is taxable to you when the depositary receives the dividend, actually or constructively. The dividend will not be eligible for the dividends-
received deduction generally allowed to United States corporations in respect of dividends received from other United States corporations. The amount
of the dividend distribution that you must include in income will be the U.S. dollar value of the yen payments made, determined at the spot yen/U.S.
dollar rate on the date the depositary actually or constructively receives the dividend, even if the depositary (a) converts the yen into U.S. dollars at a
different rate or (b) does not convert the dividend payment into U.S. dollars. If the depositary converts the yen into U.S. dollars at a different rate, then
you will recognize U.S. source ordinary income (that would not be treated as qualified dividends) or loss equal to the difference between the U.S. dollars
that you receive and the U.S. dollar amount that you included as dividend income. If the depositary does not convert the dividend payment into U.S.
dollars, then you will recognize U.S. source ordinary income (that would not be treated as qualified dividends) or loss upon a conversion of the yen into
U.S. dollars equal to the difference between the U.S. dollars that you receive in the conversion and the U.S. dollar amount that you included as dividend
income.
Distributions in excess of current and accumulated earnings and profits, as determined for United States federal income tax purposes, will
be treated as a non-taxable return of capital to the extent of your basis in the ADSs and thereafter as capital gain. However, we do not expect to calculate
earnings and profits in accordance with United States federal income tax principles. Accordingly, you should expect to generally treat distributions we
make as dividends.
Subject to certain limitations, the Japanese tax withheld in accordance with the Treaty and paid over to Japan will be creditable or deductible
against your United States federal income tax liability. Special rules apply in determining the foreign tax credit limitation with respect to dividends that
are subject to the preferential tax rates. To the extent a reduction or refund of the tax withheld is available to you under Japanese law or under the Treaty,
the amount of tax withheld that could have been reduced or that is refundable will not be eligible for credit against your United States federal income
tax liability.
Dividends will generally be income from sources outside the United States and will generally be “passive” income for purposes of computing
the foreign tax credit allowable to you. However, if (a) we are 50% or more owned, by vote or value, by United States persons and (b) at least 10% of
our earnings and profits are attributable to sources within the United States, then for foreign tax credit purposes, a portion of our dividends would be
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treated as derived from sources within the United States. With respect to any dividend paid for any taxable year, the United States source ratio of our
dividends for foreign tax credit purposes would be equal to the portion of our earnings and profits from sources within the United States for such taxable
year, divided by the total amount of our earnings and profits for such taxable year.
Distributions of additional shares to you with respect to ADSs that are made as part of a pro rata distribution to all of our shareholders
generally will not be subject to United States federal income tax.
Capital Gains. If you are a U.S. holder and you sell or otherwise dispose of your ADSs, you will recognize capital gain or loss for United
States federal income tax purposes equal to the difference between the U.S. dollar value of the amount that you realize and your tax basis, determined
in U.S. dollars, in your ADSs. Capital gain of a noncorporate U.S. holder is generally taxed at preferential rates where the property is held for more than
one year. The gain or loss will generally be income or loss from sources within the United States for foreign tax credit limitation purposes.
PFIC Rules. We believe that ADSs should not currently be treated as stock of a PFIC for United States federal income tax purposes and we
do not expect to become a PFIC in the foreseeable future. However, this conclusion is a factual determination that is made annually and thus may be
subject to change. It is therefore possible that we could become a PFIC in a future taxable year.
In general, if you are a U.S. holder, we will be a PFIC with respect to you if for any taxable year in which you held our ADSs:
•
•
at least 75% of our gross income for the taxable year is passive income or
at least 50% of the value, determined on the basis of a quarterly average, of our assets is attributable to assets that produce or are held
for the production of passive income.
“Passive income” generally includes dividends, interest, gains from the sale or exchange of investment property, rents and royalties (other
than certain rents and royalties derived in the active conduct of a trade or business) and certain other specified categories of income. If a foreign corporation
owns at least 25% by value of the stock of another corporation, the foreign corporation is treated for purposes of the PFIC tests as owning its proportionate
share of the assets of the other corporation, and as receiving directly its proportionate share of the other corporation’s income.
If we are treated as a PFIC, and you are a U.S. holder that did not make a mark-to-market election, as described below, you will generally
be subject to special rules with respect to:
•
•
any gain you realize on the sale or other disposition of your ADSs and
any excess distribution that we make to you (generally, any distributions to you during a single taxable year, other than the taxable year
in which your holding period in the ADSs begins, that are greater than 125% of the average annual distributions received by you in
respect of the ADSs during the three preceding taxable years or, if shorter, your holding period for the ADSs that preceded the taxable
year in which you receive the distribution).
Under these rules:
•
•
•
•
the gain or excess distribution will be allocated ratably over your holding period for the ADSs,
the amount allocated to the taxable year in which you realized the gain or excess distribution or to prior years before the first year in
which we were a PFIC with respect to you will be taxed as ordinary income,
the amount allocated to each other prior year will be taxed at the highest tax rate in effect for that year, and
the interest charge generally applicable to underpayments of tax will be imposed in respect of the tax attributable to each such year.
Special rules apply for calculating the amount of the foreign tax credit with respect to excess distributions by a PFIC.
If we are a PFIC in a taxable year and our ADSs are treated as “marketable stock” in such year, you may make a mark-to-market election
with respect to your ADSs. If you make this election, you will not be subject to the PFIC rules described above. Instead, in general, you will include as
ordinary income each year the excess, if any, of the fair market value of your ADSs at the end of the taxable year over your adjusted basis in your ADSs.
You will also be allowed to take an ordinary loss in respect of the excess, if any, of the adjusted basis of your ADSs over their fair market value at the
end of the taxable year (but only to the extent of the net amount of previously included income as a result of the mark-to-market election). Your basis
in the ADSs will be adjusted to reflect any such income or loss amounts. Any gain that you recognize on the sale or other disposition of your ADSs
would be ordinary income and any loss would be an ordinary loss to the extent of the net amount of previously included income as a result of the mark-
to-market election and, thereafter, a capital loss.
Your ADSs will generally be treated as stock in a PFIC if we were a PFIC at any time during your holding period in your ADSs, even if we
are not currently a PFIC.
In addition, notwithstanding any election you make with regard to the ADSs, dividends that you receive from us will not constitute qualified
dividend income to you if we are a PFIC (or are treated as a PFIC with respect to you) either in the taxable year of the distribution or the preceding
taxable year. Dividends that you receive that do not constitute qualified dividend income are not eligible for taxation at the preferential rates applicable
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to qualified dividend income. Instead, you must include the gross amount of any such dividend paid by us out of our accumulated earnings and profits
(as determined for United States federal income tax purposes) in your gross income, and it will be subject to tax at rates applicable to ordinary income.
If you own ADSs during any year that we are a PFIC with respect to you, you may be required to file Internal Revenue Service (“IRS”)
Form 8621.
Japanese Taxation
The following is a general summary of the principal Japanese tax consequences (limited to national tax) to owners of shares of our common
stock, in the form of shares or ADSs, who are non-resident individuals of Japan or who are non-Japanese corporations without a permanent establishment
in Japan, collectively referred to in this section as non-resident holders. The statements below regarding Japanese tax laws are based on the laws and
treaties in force and as interpreted by the Japanese tax authorities as of the date of this annual report, and are subject to changes in applicable Japanese
laws, tax treaties, conventions or agreements, or in the interpretation of them, occurring after that date. This summary is not exhaustive of all possible
tax considerations that may apply to a particular investor, and potential investors are advised to satisfy themselves as to the overall tax consequences of
the acquisition, ownership and disposition of shares of our common stock, including, specifically, the tax consequences under Japanese law, under the
laws of the jurisdiction of which they are resident and under any tax treaty, convention or agreement between Japan and their country of residence, by
consulting their own tax advisors.
For the purpose of Japanese tax law and the tax treaty between the United States and Japan, a U.S. holder of ADSs will generally be treated as
the owner of the shares underlying the ADSs evidenced by the ADRs.
Generally, a non-resident holder of shares or ADSs will be subject to Japanese income tax collected by way of withholding on dividends (meaning
in this section distributions made from our retained earnings for the Companies Act purposes) we pay with respect to shares of our common stock and
such tax will be withheld prior to payment of dividends. Stock splits generally are not subject to Japanese income or corporation taxes.
In the absence of any applicable tax treaty, convention or agreement reducing the maximum rate of Japanese withholding tax or allowing
exemption from Japanese withholding tax, the rate of the Japanese withholding tax applicable to dividends paid by Japanese corporations on their shares
of stock to non-resident holders is generally 20.42% (or 20% for dividends due and payable on or after January 1, 2038) under Japanese tax law. However,
with respect to dividends paid on listed shares issued by a Japanese corporation (such as shares or ADSs) to non-resident holders, other than any individual
shareholder who holds 3% or more of the total number of shares issued by the relevant Japanese corporation (to whom the aforementioned withholding
tax rate will still apply), the aforementioned withholding tax rate is reduced to (i) 15.315% for dividends due and payable up to and including December 31,
2037 and (ii) 15% for dividends due and payable on or after January 1, 2038. The withholding tax rates described above include the special reconstruction
surtax (2.1% multiplied by the original applicable withholding tax rate, i.e., 15% or 20%, as the case may be), which is imposed during the period from
and including January 1, 2013 to and including December 31, 2037, to fund the reconstruction from the Great East Japan Earthquake.
If distributions were made from our capital surplus, rather than retained earnings, for the Companies Act purposes, the portion of such distributions
in excess of the amount corresponding to a pro rata portion of return of capital as determined under Japanese tax laws would be deemed dividends for
Japanese tax purposes, while the rest would be treated as return of capital for Japanese tax purposes. The deemed dividend portion, if any, would generally
be subject to the same tax treatment as dividends as described above, and the return of capital portion would generally be treated as proceeds derived
from the sale of shares and subject to the same tax treatment as sale of shares of our common stock as described below. Distributions made in consideration
of repurchase by us of our own shares or in connection with certain reorganization transactions will be treated substantially in the same manner.
Japan has income tax treaties whereby the withholding tax rate (including the special reconstruction surtax) may be reduced, generally to 15%,
for portfolio investors, with, among others, Canada, Denmark, Finland, Germany, Ireland, Italy, Luxembourg, New Zealand, Norway, Singapore and
Spain, while the income tax treaties with, among others, Australia, Belgium, France, Hong Kong, the Netherlands, Portugal, Sweden, Switzerland, the
United Arab Emirates, the United Kingdom and the United States generally reduce the withholding tax rate to 10% for portfolio investors. In addition,
under the income tax treaty between Japan and the United States, dividends paid to pension funds which are qualified U.S. residents eligible to enjoy
treaty benefits are exempt from Japanese income taxation by way of withholding or otherwise unless the dividends are derived from the carrying on of
a business, directly or indirectly, by the pension funds. Similar treatment is applicable to dividends paid to pension funds under the income tax treaties
between Japan and the Netherlands, Switzerland and the United Kingdom. Under Japanese tax law, any reduced maximum rate applicable under a tax
treaty shall be available when such maximum rate is below the rate otherwise applicable under the Japanese tax law referred to in the second preceding
paragraph with respect to the dividends to be paid by us on our shares or ADSs.
Non-resident holders of our shares who are entitled under an applicable tax treaty to a reduced rate of, or exemption from, Japanese withholding
tax on any dividends on our shares, in general, are required to submit, through the withholding agent to the relevant tax authority prior to the payment
of dividends, an Application Form for Income Tax Convention regarding Relief from Japanese Income Tax and Special Income Tax for Reconstruction
on Dividends together with any required forms and documents. A standing proxy for a non-resident holder of shares of our common stock or ADSs may
be used in order to submit the application on a non-resident holder’s behalf. In this regard, a certain simplified special filing procedure is available for
non-resident holders to claim treaty benefits of reduction of or exemption from Japanese withholding tax, by submitting a Special Application Form for
Income Tax Convention regarding Relief from Japanese Income Tax and Special Income Tax for Reconstruction on Dividends of Listed Stock, together
with any required forms or documents. If the depositary needs investigation to identify whether any non-resident holders of ADSs are entitled to claim
treaty benefits of exemption from or reduction of Japanese withholding tax, the depositary or its agent submits an application form before payment of
dividends so that the withholding cannot be made in connection with such holders for eight months after the record date concerning such payment of
dividends. If it is proved that such holders are entitled to claim treaty benefits of exemption from or reduction of Japanese withholding tax within the
94
foregoing eight-month period, the depositary or its agent submits another application form together with certain other documents so that such holder
can be subject to exemption from or reduction of Japanese withholding tax. To claim this reduced rate or exemption, such non-resident holder of ADSs
will be required to file a proof of taxpayer status, residence and beneficial ownership, as applicable, and to provide other information or documents as
may be required by the depositary. Non-resident holders who are entitled, under any applicable tax treaty, to a reduced rate of Japanese withholding tax
below the rate otherwise applicable under Japanese tax law, or exemption therefrom, as the case may be, but fail to submit the required application in
advance may nevertheless be entitled to claim a refund from the relevant Japanese tax authority of withholding taxes withheld in excess of the rate under
an applicable tax treaty (if such non-resident holders are entitled to a reduced treaty rate under the applicable tax treaty) or the full amount of tax withheld
(if such non-resident holders are entitled to an exemption under the applicable tax treaty), as the case may be, by complying with a certain subsequent
filing procedure. We do not assume any responsibility to ensure withholding at the reduced treaty rate, or exemption therefrom, for shareholders who
would be eligible under an applicable tax treaty but who do not follow the required procedures as stated above.
Gains derived from the sale of our shares or ADSs outside Japan by a non-resident holder that is a portfolio investor will generally not be subject
to Japanese income or corporation taxes. Japanese inheritance and gift taxes, at progressive rates, may be payable by an individual who has acquired
from another individual our shares or ADSs as a legatee, heir or done, even if none of the acquiring individual, the decedent or the donor is a Japanese
resident.
F.
Dividends and Paying Agents.
Not applicable.
G.
Statement by Experts.
Not applicable.
H.
Documents on Display.
We have filed this annual report with the SEC under the Exchange Act with respect to the ADSs. We are subject to the information requirements
of the Exchange Act and, in accordance therewith, we are required to file annual reports on Form 20-F and furnish other reports and information on
Form 6-K with the SEC.
You may review a copy of our filings without charge at the SEC’s web site at www.sec.gov that contains reports and other information
regarding registrants that file electronically with the SEC. You can also view such filings on our web site at https://www.takeda.com/investors/reports/
sec-filings/. As a foreign private issuer, we are exempt from the rules under the Exchange Act prescribing the furnishing and content of proxy statements
to shareholders.
I.
Subsidiary Information.
Not applicable.
Item 11. Quantitative and Qualitative Disclosures about Market Risk
We are exposed to market risks primarily from changes in foreign currency exchange rates, interest rate changes and changes in the value
of our investment securities. The information required under this Item 11 is set forth in Note 27 to our audited consolidated financial statements included
in this annual report.
Item 12. Description of Securities Other Than Equity Securities
A.
Debt Securities
Not applicable.
B.
Warrants and Rights
Not applicable.
C.
Other Securities
Not applicable.
D.
American Depositary Shares
95
Each ADS represents one-half of one share of our common stock deposited with our depositary’s (The Bank of New York Mellon) custodian
(Sumitomo Mitsui Banking Corporation) in Japan. Each ADS will also represent any other securities, cash or other property which may be held by the
depositary from time to time. The deposited shares of our common stock, together with any other securities, cash or other property held by the depositary
are referred to as the “deposited securities.”
Fees and Expenses
Persons depositing or withdrawing shares of our common stock or ADS holders
must pay:
$5.00 (or less) per 100 ADSs (or portion of 100 ADSs)
$0.05 (or less) per ADS
A fee equivalent to the fee that would be payable if securities distributed
to ADS holders had been shares of our common stock and the shares of
our common stock had been deposited for issuance of ADSs
$0.05 (or less) per ADS per calendar year
Registration or transfer fees
Expenses of the depositary
Taxes and other governmental charges the depositary or the custodian has
to pay on any ADSs or shares of our common stock underlying ADSs,
such as stock transfer taxes, stamp duty or withholding taxes
Any charges incurred by the depositary or its agents for servicing the
deposited securities
For:
Issue of ADSs, including issues resulting from a distribution of shares of
our common stock or rights or other property
Cancellation of ADSs for the purpose of withdrawal, including if the
deposit agreement terminates
Any cash distribution to ADS holders
Distribution of securities distributed to holders of deposited securities
(including rights) that are distributed by the depositary to ADS holders
Depositary services
Transfer and registration of shares of our common stock on our share
register to or from the name of the depositary or its agent when persons
deposit or withdraw shares of our common stock
Cable and facsimile transmissions (when expressly provided in the deposit
agreement)
Converting foreign currency to U.S. dollars
As necessary
As necessary
The depositary collects its fees for delivery and surrender of ADSs directly from investors depositing shares of our common stock or
surrendering ADSs for the purpose of withdrawal or from intermediaries acting for them. The depositary collects fees for making distributions to investors
by deducting those fees from the amounts distributed or by selling a portion of distributable property to pay the fees. The depositary may collect its
annual fee for depositary services by deduction from cash distributions or by directly billing investors or by charging the book-entry system accounts
of participants acting for them. The depositary may collect any of its fees by deduction from any cash distribution payable (or by selling a portion of
securities or other property distributable) to ADS holders that are obligated to pay those fees. The depositary may generally refuse to provide fee-
attracting services until its fees for those services are paid.
In performing its duties under the deposit agreement, the depositary may use brokers, dealers, foreign currency dealers or other service
providers that are owned by or affiliated with the depositary and that may earn or share fees, spreads or commissions.
The depositary may convert currency itself or through any of its affiliates and, in those cases, acts as principal for its own account and not
as agent, advisor, broker or fiduciary on behalf of any other person and earns revenue, including, without limitation, transaction spreads, that it will
retain for its own account. The revenue is based on, among other things, the difference between the exchange rate assigned to the currency conversion
made under the deposit agreement and the rate that the depositary or its affiliate receives when buying or selling foreign currency for its own account.
The depositary makes no representation that the exchange rate used or obtained in any currency conversion under the deposit agreement will be the most
favorable rate that could be obtained at the time or that the method by which that rate will be determined will be the most favorable to ADS holders,
subject to the depositary’s obligations under the deposit agreement. The methodology used to determine exchange rates used in currency conversions
is available upon request.
Payment of Taxes
ADS holders will be responsible for any taxes or other governmental charges payable on their ADSs or on the deposited securities represented
by any of their ADSs. The depositary may refuse to register any transfer of ADSs or allow an ADS holder to withdraw the deposited securities represented
by his or her ADSs until those taxes or other charges are paid. It may apply payments owed to such ADS holder or sell deposited securities represented
by such ADS holder’s ADSs to pay any taxes owed and such ADS holder will remain liable for any deficiency. If the depositary sells deposited securities,
it will, if appropriate, reduce the number of ADSs to reflect the sale and pay to ADS holders any proceeds, or send to ADS holders any property, remaining
after it has paid the taxes.
96
Direct and Indirect Payments by the Depositary
Pursuant to contractual arrangements between us and the depositary in place through January 8, 2019, the depositary had previously agreed
to reimburse us for certain costs and expenses generally arising out of the establishment and maintenance of the ADS program. Costs and expenses for
which the depositary has agreed to reimburse us for the fiscal year ending March 31, 2019 (through January 8, 2019), were approximately $250,000.
Beginning on January 8, 2019, the depositary has agreed to make revenue sharing payments to us based on a fixed portion of the net issuance,
net cancellation cash dividend and net depositary servicing fees received by it under the deposit agreement, subject to a minimum annual payment based
on the total of such fees received by the depositary. No payments were received under this revenue sharing arrangement in the fiscal year ended March
31, 2019.
The depositary has also agreed to waive fees and expenses for services provided to us, to ADS holders or to their respective brokers by the
depositary in connection with the establishment, administration and ongoing servicing of the ADS program. Furthermore, the depositary has agreed to
waive fees for certain value-added services, including training for our staff, investor relations advisory services and access to the depositary’s analytics
and reporting platform. Accordingly, in the fiscal year ended March 31, 2019, the depositary waived approximately $52,000 of fees and expenses.
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.
Disclosure Controls and Procedures
We have carried out an evaluation under the supervision and with the participation of our management, including our CEO and CFO, of the
effectiveness of the design and operation of our disclosure controls and procedures, as defined in Rules 13a-15(e) and 15d-15(e) under the Securities
Exchange Act of 1934 (the “Exchange Act”), as of March 31, 2019. Disclosure controls and procedures require that information to be disclosed in the
reports we file or submit under the Exchange Act is recorded, processed, summarized and reported as and when required, within the time periods specified
in the applicable rules and forms, and that such information is accumulated and communicated to our management, including the CEO and CFO, as
appropriate to allow timely decisions regarding required disclosure. There are inherent limitations to the effectiveness of any system of disclosure controls
and procedures, including the possibility of human error and the circumvention or overriding of the controls and procedures. Accordingly, even effective
disclosure controls and procedures can only provide reasonable assurance of achieving their control objectives. Based upon our evaluation, the CEO
and CFO have concluded that, as of March 31, 2019, the disclosure controls and procedures were effective at the reasonable assurance level.
Management’s Annual Report on Internal Control Over Financial Reporting
This annual report does not include a report of management’s assessment regarding internal control over financial reporting due to a transition
period established by rules of the Securities and Exchange Commission for newly public companies.
Attestation Report of the Registered Public Accounting Firm
This annual report does not include an attestation report of our registered public accounting firm due to a transition period established by
rules of the Securities and Exchange Commission for newly public companies.
Changes in Internal Control Over Financial Reporting
There were no changes in our internal control over financial reporting (as defined in Rules 13a-15(f) and 15d-15(f) under the Exchange Act)
that occurred during the fiscal year ended March 31, 2019 that have materially affected, or were reasonably likely to materially affect, our internal control
over financial reporting.
Item 16A. Audit Committee Financial Expert.
Our board of directors has determined that Mr. Koji Hatsukawa, an external director and member of our Audit and Supervisory Committee,
is an “audit committee financial expert” as defined in Item 16A of Form 20-F and is “independent” as defined in the listing standards of the New York
Stock Exchange as applicable through Rule 10A-3 under the Exchange Act.
97
Item 16B. Code of Ethics.
We have adopted the Takeda Global Code of Conduct, which applies to all of our employees, including our principal executive officer,
principal financial officer, principal accounting officer and persons performing similar functions. The Takeda Global Code of Conduct is posted on our
corporate website at http://www.takeda.com/who-we-are/corporate-governance/compliance. No waivers to the Global Code of Conduct were granted
to our principal executive officer, principal financial officer, principal accounting officer and persons performing similar functions in the fiscal year
ended March 31, 2019.
Item 16C. Principal Accountant Fees and Services.
Audit and Non‑Audit Fees
The following table sets forth the fees billed to us by our independent certified public accountant, KPMG AZSA LLC (including its Japanese
and non-Japanese affiliates), in the fiscal years ended March 31, 2018 and 2019:
Audit fees (1)
Audit‑related fees (2)
Tax fees (3)
Other fees
Total fees
For the fiscal year ended
March 31,
2018
2019
(billions of yen)
¥
¥
1.43
0.03
0.03
0.03
1.52
¥
¥
3.75
0.05
0.01
—
3.81
____________
Notes:
(1)
Audit fees were related to the audit of our consolidated financial statements and other services provided in connection with statutory and regulatory
filings or engagements.
Audit‑related fees were related to assurance services with respect to our debt issuances.
Tax fees were related to tax compliance and other tax-related services.
(2)
(3)
Pre‑Approval Policies and Procedures
Pursuant to Rule 2-01(c)(7)(i) of Regulation S-X, we have adopted policies and procedures under which all services (including permissible
non-audit services) for which we or our subsidiaries engage our independent certified public accountant, KPMG AZSA LLC, and its affiliates must be
approved by our Audit and Supervisory Committee prior to entering into an engagement.
All audit services are subject to the pre-approval by the Audit and Supervisory Committee in principle, regardless of monetary value. Audit
services include statutory or financial statement audits for us and our subsidiaries, services associated with the audit of our management’s report on
internal controls over financial reporting and services associated with the review of our quarterly financial statements. On a yearly basis, our management,
following a review by our Chief Financial Officer, presents the proposed audit services to our Audit and Supervisory Committee for approval, and
proposes audit fees on an entity basis to the Audit and Supervisory Committee for its consent. Once such services and fees are approved or consented
to, as applicable, any additional audit services must be separately presented to and approved by our Audit and Supervisory Committee.
Permissible non-audit services, which are limited to certain services permissible under applicable regulation and our internal rules, are pre-
approved by the Audit and Supervisory Committee for individual services below ¥25 million annually, subject to an aggregate annual limit of up to ¥250
million for all such services. These services are subject to review by our management for compliance with our internal policies. All non-audit services
exceeding the applicable monetary limits or which are not clearly within the scope of permitted non-audit services must be presented to and pre-approved
by the Audit and Supervisory Committee. All services relating to tax or internal control are also subject to separate presentation to and pre-approval by
the Audit and Supervisory Committee regardless of monetary value.
Item 16D. Exemptions from the Listing Standards for Audit Committees.
As of the date of this annual report, we do not rely on any of the exemptions contained in paragraph (b)(1)(iv), the general exemption
contained in paragraph (c)(3) or the last sentence of paragraph (a)(3) of Rule 10A-3 under the Exchange Act (“Rule 10A-3”).
Paragraph (b)(iv)(A)(2) of Rule 10A-3 permits a minority of the members of a listed issuer’s audit committee to be exempt from the
independence requirements under Rule 10A-3 for a period of one year from the date of effectiveness of such issuer’s initial registration statement under
Section 12 of the Exchange Act or the registration statement under the Securities Act covering an initial public offering of securities to be listed by such
issuer. From the time of the effectiveness of our registration statement on Form 20-F on December 21, 2018 until the election of directors at of our most
recent annual general meeting of shareholders held on June 27, 2019, we relied on this exemption with respect to the former membership of one of our
98
directors on our Audit and Supervisory Committee, which is our “audit committee” for the purposes of Rule 10A-3. Following such election of directors,
each of the members of our Audit and Supervisory Committee now satisfy the independence requirements of Rule 10A-3. We do not believe that our
reliance on this transitional exemption has materially affected the ability of our Audit and Supervisory Committee to act independently or satisfy any
of the other requirements under Rule 10A-3.
Item 16E. Purchases of Equity Securities by the Issuer and Affiliated Purchasers.
The following table sets forth purchases of our common stock by us and our affiliated purchasers during the fiscal year ended March 31,
2019:
April 1 to April 30, 2018
May 1 to May 31, 2018
June 1 to June 30, 2018
July 1 to July 31, 2018
August 1 to August 31, 2018
September 1 to September 30, 2018
October 1 to October 31, 2018
November 1 to November 30, 2018
December 1 to December 31, 2018
January 1 to January 31, 2019
February 1 to February 28, 2019
March 1 to March 31, 2019
Total
Total number of
shares purchased
Average price
paid per share
Total number of
shares purchased
as part of publicly
announced plans
or programs
Maximum
number of shares
that may yet be
purchased under
the plans
or programs
228
¥
246,075
299
478
381
227
517
410
424
610
484
372
250,505
¥
5,091
4,674
4,303
4,673
4,711
4,640
4,674
4,557
3,856
4,281
4,403
4,597
4,671
—
—
245,800
—
—
—
—
—
—
—
—
—
245,800
—
—
—
—
—
—
—
—
—
—
—
—
—
Purchases in the above table reflect (1) purchases of shares in relation to stock-based incentive compensation plans and (2) purchases of shares
constituting less than one “unit” (100 shares).
We have two stock-based incentive compensation plans for its directors and members of senior management, the Board Incentive Plan (the “BIP”)
and the Employee Stock Ownership Plan (the “ESOP”). See “Item 6.B. Directors, Senior Management and Employees-Compensation.” For grants under
the BIP, we, through a wholly-owned trust, buy shares of our common stock in the market on the grant date, and use these shares to settle awards. Grants
under the ESOP have been settled using shares newly issued by us, although it is possible in the future that we will adopt a similar trust structure for
the ESOP.
The wholly-owned trust purchases shares of our common stock using funds transferred to the trust by us (less trust fees and trust expenses) at the
market price of the shares during the share purchase period. As the total number of shares therefore fluctuates with the market price of our shares, the
total number of shares which may be purchased under the BIP is not given above.
In May 2018, we approved the transfer of approximately ¥1.09 billion to the wholly-owned trust and, in the same month, the wholly-owned trust
used such funds to purchase 245,800 shares in respect of grants under the BIP. As of the date of this annual report, the transfer of a total of an additional
¥5 billion to the wholly-owned trust for the purpose of purchasing shares of our common stock at the market in order to settle grants under the BIP for
the three fiscal years ending March 31, 2022 has been approved by our annual general meeting of shareholders. The wholly-owned trust is scheduled
to purchase shares up to such amount, less trust fees and trust expenses, during the period from August 2, 2019 to the end of August 2019.
A total of 4,705 shares were purchased other than through publicly announced plans or programs during the fiscal year ended March 31, 2019,
due to our purchase of shares constituting less than one “unit” (100 shares) from holders of shares constituting less than one unit at the current market
price of those shares.
Item 16F. Change in Registrant’s Certifying Accountant.
Not applicable.
99
Item 16G. Corporate Governance.
Our ADSs have been listed on the NYSE since 2018. NYSE-listed companies are required to comply with corporate governance standards
under Section 303A of the NYSE Listed Company Manual. However, as a foreign private issuer, we are permitted to follow home country practices in
lieu of certain provisions of Section 303A. Below, we provide a brief description of significant differences between the NYSE listing standards applicable
to U.S. domestic issuers and our corporate governance policies pursuant to 303A.11 of the NYSE Listed Company Manual.
Composition of the Board (303A.01)
Under the NYSE listing standards, U.S. domestic issuers are required to have a majority of directors meeting the independence tests set
forth in the NYSE listed company manual.
Takeda is a “company with audit and supervisory committee” as defined in the Companies Act. Companies with audit and supervisory
committees are not required to have a majority of independent directors. Such companies must have a board of directors as well as an audit and supervisory
committee consisting of at least three of its directors. A majority of the members of the audit and supervisory committee must be “external directors”
as defined under the Companies Act, which differs from the director independence standards under the NYSE listed company manual. Additionally,
under the regulations of the Tokyo Stock Exchange, we are required to have at least one director who is “independent” for the purposes of such regulations,
which are more stringent than the requirements for “external directors” under the Companies Act.
Our board of directors consists of 16 directors, of which 11 are “external directors” under the Companies Act. Our Audit and Supervisory
Committee is comprised of four of our directors, three of whom qualify as “external directors” under this standard. Each of our external directors also
qualifies as “independent” as described under “Director Independence (303A.02)” below, and each of the members of our Audit and Supervisory
Committee qualifies as “independent” for purposes of Rule 10A-3 under the Exchange Act.
for a director who is an Audit and Supervisory Committee member is two years, whereas the term of office for other directors is one year.
Directors who are Audit and Supervisory Committee members are elected separately from our other directors. The term of office
Director Independence (303A.02)
We deem a director as being an “independent director” when such director also meets independence requirements stipulated in the regulations
of the Tokyo Stock Exchange, on which our common stock is listed, and independence requirements established internally. These requirements differ
in certain respects from the requirements under the NYSE listed company manual.
Executive Sessions (303A.03)
The NYSE listed company manual requires that non-management directors of U.S. domestic issuers meet in regularly scheduled executive
sessions without management. Although not required under Japanese law or Tokyo Stock Exchange rule, our independent external directors hold regularly
scheduled executive sessions without management.
Composition of Committees (303A.04, 05, 06 and 07)
The NYSE listed company manual requires that U.S. domestic issuers establish a nomination/corporate governance committee and a
compensation committee, each of which much be composed entirely of independent directors. The NYSE listed company manual also requires that all
listed companies, including a foreign private issuer (as defined in the Exchange Act) such as us, establish an audit committee satisfying the requirements
of Rule 10A-3 under the Exchange Act. Audit committees of U.S. domestic issuers are also subject to certain additional requirements under Section
303A.07 of the NYSE listed company manual.
Although the Companies Act does not require companies with audit and supervisory committees to establish nomination committees or
compensation committees, we have established such committees in order to ensure transparency. Our nomination committee consists of four directors
(of which, three are independent external directors for the purposes of Japanese law and the rules of the Tokyo Stock Exchange). Director candidates
nominated by our nomination committee must be approved at our general meeting of shareholders. Unlike the nomination/corporate governance
committees of U.S. domestic issuers, our nomination committee is not also responsible for corporate governance policies.
Our compensation committee consists of three directors (of which, two are independent external directors for the purposes of Japanese law
and the rules of the Tokyo Stock Exchange). The maximum total amount of compensation for our directors must be approved at our general meeting of
shareholders, provided that the maximum total amounts for directors who are Audit and Supervisory Committee members and for other directors must
be separately approved. The individual amounts of compensation for our directors (other than Audit and Supervisory Committee members) is determined
in accordance with the compensation standards determined by our board of directors or a resolution of our board of directors. The individual amounts
of compensation for our Audit and Supervisory Committee members are determined by discussion among the Audit and Supervisory Committee members.
Our Audit and Supervisory Committee consists of four directors (of which, three are independent external directors for the purposes of
Japanese law and the rules of the Tokyo Stock Exchange), and all of whom currently satisfy the independence requirements of Rule 10A-3 under the
Exchange Act. Our Audit and Supervisory Committee does not necessarily satisfy all of the additional audit committee requirements applicable to NYSE-
listed U.S. domestic companies under Section 303A.07, nor is it required to under the standards applicable to foreign private issuers under Section 303A.
100
Equity Compensation Plans (303A.08)
U.S. domestic issuers listed on NYSE are required to obtain the approval of shareholders for equity compensation plans and any material
changes thereto, subject to certain limited exceptions.
Under Japanese law and the regulations of the Tokyo Stock Exchange, the adoption of an equity compensation plan, including for directors,
requires shareholder approval. Pursuant to the approval of our general meeting of shareholders, we grant certain stock-based compensation to the
directors. Stock acquisition rights or shares of common stock may be granted by resolution of the board of directors, except that, if stock acquisition
rights or shares of common stock are to be granted on particularly favorable conditions, a special resolution of the general meeting of shareholders is
required. The passage of a special resolution of the general meeting of shareholders requires the approval of two-thirds or more of the voting rights
represented at a quorate general meeting of shareholders.
Corporate Governance Guidelines (303A.09)
U.S. domestic issuers listed on the NYSE must adopt and disclose corporate governance guidelines as set forth in the NYSE listed company
manual. Japanese law and the regulations of the Tokyo Stock Exchange require us to disclose our basic views on corporate governance. In accordance
with these requirements, we publish our Corporate Governance Report annually, which is posted on our website and furnished to the SEC under cover
of Form 6-K, although this may not necessarily cover all of the same items as contemplated by the NYSE listed company manual.
Code of Business Conduct and Ethics (303A.10)
U.S. domestic issuers listed on NYSE are required to adopt and disclose a code of business conduct and ethics for directors, officers and
employees, and promptly disclose any waivers of the code for directors or executive officers. Although not required to do so under the NYSE listed
company manual, we have established a global code of business conduct and ethics, known as the Takeda Global Code of Conduct, which is posted on
our website. Although the Takeda Global Code of Conduct functions as a code of business conduct and ethics, it is not required to cover all of the same
areas as that of a U.S. domestic issuer under the NYSE listed company manual. Pursuant to the requirements of Form 20-F, waivers, if any, to the Takeda
Global Code of Conduct given to our directors or senior management are disclosed by us in our annual reports on Form 20-F.
Item 16H. Mine Safety Disclosure
Not applicable.
Item 17. Financial Statements
The Company has responded to Item 18 in lieu of this item.
Item 18. Financial Statements
The information required by this item is set forth in our consolidated financial statements included in this annual report.
Item 19. Exhibits
Exhibit
No.
Exhibit 1.1
Exhibit 1.2
Exhibit 1.3
Exhibit 2.1
Exhibit 2.2
Exhibit 2.3
Exhibit
Articles of Incorporation of Takeda Pharmaceutical Company Limited (English Translation) (incorporated by reference to
Exhibit 1.1 to Amendment No. 1 to the Registration Statement on Form 20-F of the registrant, filed on December 17, 2018).
Regulations of the Board of Directors of Takeda Pharmaceutical Company Limited (English Translation) (incorporated by
reference to Exhibit 1.2 to Amendment No. 1 to the Registration Statement on Form 20-F of the registrant, filed on December
17, 2018).
Share Handling Regulations of Takeda Pharmaceutical Company Limited (English Translation) (incorporated by reference to
Exhibit 1.3 to Amendment No. 1 to the Registration Statement on Form 20-F of the registrant, filed on December 17, 2018).
Form of Amended and Restated Deposit Agreement among the Takeda Pharmaceutical Company Limited, The Bank of New
York Mellon, as Depositary, and all Owners and Holders from time to time of American Depositary Shares issued thereunder
(incorporated by reference to Exhibit 2.1 to Amendment No. 1 to the Registration Statement on Form 20-F of the registrant,
filed on December 17, 2018).
Indenture, dated as of September 23, 2016, among Shire Acquisitions Investments Ireland DAC, Shire plc, as guarantor, and
Deutsche Bank Trust Company Americas, as trustee (incorporated by reference to Exhibit 4.1 of Shire plc’s Current Report on
Form 8-K filed on September 23, 2016).
First Supplemental Indenture, dated as of September 23, 2016, to the Indenture, dated as of September 23, 2016, among Shire
Acquisitions Investments Ireland DAC, Shire plc, as guarantor, and Deutsche Bank Trust Company Americas, as trustee
(incorporated by reference to Exhibit 4.2 of Shire plc’s Current Report on Form 8-K filed on September 23, 2016).
101
Exhibit
No.
Exhibit 2.4
Exhibit 2.5*
Exhibit 2.6
Exhibit 2.7
Exhibit 2.8
Exhibit 2.9
Exhibit 2.10
Exhibit 2.11
Exhibit 2.12
Exhibit 2.13*
Exhibit 2.14
Exhibit 2.15*
Exhibit 2.16
Exhibit 2.17
Exhibit 2.18
Exhibit 2.19
Exhibit 2.20*
Exhibit 2.21
Exhibit 2.22
Exhibit 4.1**
Exhibit 4.2
Exhibit 8.1
Exhibit
Second Supplemental Indenture, dated as of December 1, 2016, to the Indenture dated as of September 23, 2016, among Shire
Acquisitions Investments Ireland DAC, Shire plc, as guarantor, Baxalta Incorporated, as subsidiary guarantor, and Deutsche
Bank Trust Company Americas, as trustee (incorporated by reference to Exhibit 4.1 of Shire plc’s Current Report on Form 8-K
filed on December 2, 2016).
Third Supplemental Indenture, dated as of February 4, 2019, to the Indenture dated as of September 23, 2016, among Shire
Acquisitions Investments Ireland DAC, Takeda Pharmaceutical Company Limited, as guarantor, Shire plc, as guarantor,
Baxalta Incorporated, as subsidiary guarantor, and Deutsche Bank Trust Company Americas, as trustee.
Form of 1.900% Senior Notes due 2019 of Shire Acquisitions Investments Ireland DAC (incorporated by reference to Exhibit
4.1 of Shire plc’s Current Report on Form 8-K filed on September 21, 2016).
Form of 2.400% Senior Notes due 2021 of Shire Acquisitions Investments Ireland DAC (incorporated by reference to Exhibit
4.2 of Shire plc’s Current Report on Form 8-K filed on September 21, 2016).
Form of 2.875% Senior Notes due 2023 of Shire Acquisitions Investments Ireland DAC (incorporated by reference to Exhibit
4.3 of Shire plc’s Current Report on Form 8-K filed on September 21, 2016).
Form of 3.200% Senior Notes due 2026 of Shire Acquisitions Investments Ireland DAC (incorporated by reference to Exhibit
4.4 of Shire plc’s Current Report on Form 8-K filed on September 21, 2016).
Indenture between Baxalta Incorporated and The Bank of New York Mellon Trust Company, N.A., as Trustee, dated as of June
23, 2015 (incorporated by reference to Exhibit 4.1 of Baxalta Incorporated’s Current Report on Form 8-K filed on June 23,
2015).
First Supplemental Indenture, to the Indenture dated as of June 23, 2015, between Baxalta Incorporated and The Bank of New
York Mellon Trust Company, N.A., as Trustee, dated as of June 23, 2015 (incorporated by reference to Exhibit 4.2 of Baxalta
Incorporated’s Current Report on Form 8-K filed on June 23, 2015).
Second Supplemental Indenture, to the Indenture dated as of June 23, 2015, between Baxalta Incorporated, Shire plc and The
Bank of New York Mellon Trust Company, N.A., as Trustee, dated as of June 3, 2016 (incorporated by reference to Exhibit 4.3
of Shire plc’s Current Report on Form 8-K filed on June 3, 2016).
Third Supplemental Indenture, to the Indenture dated as of June 23, 2015, between Baxalta Incorporated, Shire plc, Takeda
Pharmaceutical Company Limited and The Bank of New York Mellon Trust Company, N.A., as Trustee, dated as of February
4, 2019.
Term Loan Credit Agreement among Takeda Pharmaceutical Company Limited, as Borrower, Various Financial Institutions,
as Lenders, and JPMorgan Chase Bank, N.A., as Administrative Agent, dated as of June 8, 2018 (incorporated by reference to
Exhibit 10.7 to Amendment No. 1 to the Registration Statement on Form 20-F of the registrant, filed on December 17, 2018).
Amendment No. 1, dated as of December 20, 2018, to the Term Loan Credit Agreement among Takeda Pharmaceutical
Company Limited, as Borrower, Various Financial Institutions, as Lenders, and JPMorgan Chase Bank, N.A., as
Administrative Agent, dated as of June 8, 2018.
Fiscal Agency Agreement, dated as of November 21, 2018, between Takeda Pharmaceutical Company Limited and MUFG
Bank, Ltd., as Fiscal Agent (incorporated by reference to Exhibit 10.11 to Amendment No. 1 to the Registration Statement on
Form 20-F of the registrant, filed on December 17, 2018).
Indenture, dated as of November 26, 2018, between Takeda Pharmaceutical Company Limited and MUFG Union Bank, N.A.,
as Trustee (incorporated by reference to Exhibit 10.12 to Amendment No. 1 to the Registration Statement on Form 20-F of the
registrant, filed on December 17, 2018).
Registration Rights Agreement, dated as of November 26, 2018, among Takeda Pharmaceutical Company Limited, J.P.
Morgan Securities LLC, SMBC Nikko Securities America, Inc., Morgan Stanley MUFG Securities Co., Ltd., Mizuho
Securities USA LLC and Merrill Lynch, Pierce, Fenner & Smith Incorporated, as representatives of the several initial
purchasers (incorporated by reference to Exhibit 10.13 to Amendment No. 1 to the Registration Statement on Form 20-F of the
registrant, filed on December 17, 2018).
Loan Agreement, dated December 3, 2018, between Takeda Pharmaceutical Company Limited and Japan Bank for
International Cooperation (incorporated by reference to Exhibit 10.14 to Amendment No. 1 to the Registration Statement on
Form 20-F of the registrant, filed on December 17, 2018).
Amendment No. 1, dated as of December 25, 2018, to the Loan Agreement, dated December 3, 2018, between Takeda
Pharmaceutical Company Limited and Japan Bank for International Cooperation.
(English Translation) Terms and Conditions of Hybrid Bonds issued by Takeda Pharmaceutical Company Limited on June 6,
2019 (incorporated by reference to Annex 1 to Exhibit 1 to the current report on Form 6-K of the Registrant furnished to the
Commission on May 31, 2019).
A description of the rights of each class of securities that is registered under Section 12 of the Exchange Act as of the end of
the period covered by this report. The information required hereby is incorporated by reference to Items 9, 10 and 12 of
Amendment No. 1 to the Registration Statement on Form 20-F of the registrant, filed on December 17, 2018.
Collaboration Agreement dated December 14, 2009 by and between Seattle Genetics, Inc. and Millennium Pharmaceuticals,
Inc. (incorporated by reference to Exhibit 10.1 to Amendment No. 1 to the Registration Statement on Form 20-F of the
registrant, filed on December 17, 2018).
Letter Agreement among Shire plc, Baxalta Incorporated and Baxter International Inc. dated January 11, 2016 (incorporated
by reference to Exhibit 10.1 to Shire plc's Current Report on Form 8-K filed on January 11, 2016).
List of subsidiaries of Takeda Pharmaceutical Company Limited, as of March 31, 2019: See “Item 4. Information on the
Company—C. Organizational Structure.”
102
Exhibit
No.
Exhibit 12.1*
Exhibit 12.2*
Exhibit 13.1*
Exhibit 13.2*
Exhibit
Certification of the principal executive officer required by 17 C.F.R. 240. 13a-14(a).
Certification of the principal financial officer required by 17 C.F.R. 240. 13a-14(a).
Certification of the chief executive officer required by 18 U.S.C. Section 1350.
Certification of the chief financial officer required by 18 U.S.C. Section 1350.
*
**
Filed herewith.
Pursuant to a request for confidential treatment, portions of this Exhibit have been redacted from the publicly filed document and have been
furnished separately to the SEC as required by Rule 24b-2 under the Securities Exchange Act of 1934.
We have not included as exhibits certain instruments with respect to our long-term debt where the amount of debt authorized under each
such debt instrument does not exceed 10% or our total assets. We will furnish a copy of any such instrument to the SEC upon request.
103
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.
SIGNATURES
TAKEDA PHARMACEUTICAL COMPANY
LIMITED
By:
/s/ Costa Saroukos
Name: Costa Saroukos
Title: Chief Financial Officer
Date: June 27, 2019
104
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Index
Report of Independent Registered Public Accounting Firm
Consolidated Statements of Income for the years ended March 31, 2017, 2018 and 2019
Consolidated Statements of Other Comprehensive Income for the years ended March 31, 2017, 2018 and 2019
Consolidated Statements of Financial Position as of March 31, 2018 and 2019
Consolidated Statements of Changes in Equity for the years ended March 31, 2017, 2018 and 2019
Consolidated Statements of Cash Flows for the years ended March 31, 2017, 2018 and 2019
Notes to Consolidated Financial Statements
Page
F-2
F-3
F-4
F-5 - F-6
F-7 - F-9
F-10
F-11 - F-78
F-1
Report of Independent Registered Public Accounting Firm
To the Stockholders and Board of Directors
Takeda Pharmaceutical Company Limited:
Opinion on the Consolidated Financial Statements
We have audited the accompanying consolidated statements of financial position of Takeda Pharmaceutical Company Limited and subsidiaries (the
“Company”) as of March 31, 2019 and 2018, the related consolidated statements of income, other comprehensive income, changes in equity, and
cash flows for each of the years in the three‑year period ended March 31, 2019, and the related notes (collectively, the consolidated financial
statements). In our opinion, the consolidated financial statements present fairly, in all material respects, the financial position of the Company as of
March 31, 2019 and 2018, and the results of its operations and its cash flows for each of the years in the three‑year period ended March 31, 2019, in
conformity with International Financial Reporting Standards as issued by the International Accounting Standards Board.
Basis for Opinion
These consolidated financial statements are the responsibility of the Company’s management. Our responsibility is to express an opinion on these
consolidated financial statements based on our audits. We are a public accounting firm registered with the Public Company Accounting Oversight
Board (United States) (PCAOB) and are required to be independent with respect to the Company in accordance with the U.S. federal securities laws
and the applicable rules and regulations of the Securities and Exchange Commission and the PCAOB.
We conducted our audits in accordance with the standards of the PCAOB. Those standards require that we plan and perform the audit to obtain
reasonable assurance about whether the consolidated financial statements are free of material misstatement, whether due to error or fraud. Our audits
included performing procedures to assess the risks of material misstatement of the consolidated financial statements, whether due to error or fraud,
and performing procedures that respond to those risks. Such procedures included examining, on a test basis, evidence regarding the amounts and
disclosures in the consolidated financial statements. Our audits also included evaluating the accounting principles used and significant estimates
made by management, as well as evaluating the overall presentation of the consolidated financial statements. We believe that our audits provide a
reasonable basis for our opinion.
/s/ KPMG AZSA LLC
We have served as the Company’s auditor since 2007.
Tokyo, Japan
June 27, 2019
F- 2
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Income for the Year Ended March 31,
JPY (millions, except per share data)
Note
2017
2018
2019
4
¥
1,732,051
¥
1,770,531
¥
2,097,224
Revenue
Cost of sales
Selling, general and administrative expenses
Research and development expenses
Amortization and impairment losses on intangible assets associated with products
12
Other operating income
Other operating expenses
Operating profit
Finance income
Finance expenses
Share of loss of investments accounted for using the equity method
Profit before tax
Income tax (expense) benefit
Net profit for the year
Attributable to:
Owners of the Company
Non-controlling interests
Net profit for the year
Earnings per share (JPY)
Basic earnings per share
Diluted earnings per share
5
5
6
6
14
7
8
8
8
¥
¥
¥
¥
(558,755)
(619,061)
(312,303)
(156,717)
143,533
(72,881)
155,867
12,274
(23,249)
(1,546)
143,346
(27,833)
115,513
114,940
573
115,513
147.15
146.26
¥
¥
¥
¥
(495,921)
(628,106)
(325,441)
(122,131)
169,412
(126,555)
241,789
39,543
(31,928)
(32,199)
217,205
(30,497)
186,708
186,886
(178)
186,708
239.35
237.56
¥
¥
¥
¥
(659,690)
(717,599)
(368,298)
(203,372)
159,863
(103,159)
204,969
16,843
(83,289)
(43,627)
94,896
14,118
109,014
109,126
(112)
109,014
113.50
112.86
See accompanying notes to consolidated financial statements.
F- 3
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Other Comprehensive Income for the Year Ended March 31,
Net profit for the year
Other comprehensive income (loss)
Items that will not be reclassified to profit or loss:
Changes in fair value of financial assets measured at fair value through other
comprehensive income
Remeasurement gain (loss) of defined benefit plans
Items that may be reclassified subsequently to profit or loss:
Exchange differences on translation of foreign operations
Net changes on revaluation of available-for-sale financial assets
Cash flow hedges
Hedging cost
Share of other comprehensive income (loss) of investments accounted for using the
equity method
Other comprehensive income (loss) for the year, net of tax
Total comprehensive income for the year
Attributable to:
Owners of the Company
Non-controlling interests
Total comprehensive income for the year
JPY (millions)
Note
2017
2018
2019
¥
115,513
¥
186,708
¥
109,014
9
9
9
9
9
9
9, 14
9
¥
¥
¥
—
15,554
15,554
(51,820)
9,521
4,634
(222)
(38)
(37,925)
(22,371)
93,142
93,552
(410)
93,142
¥
¥
¥
—
724
724
46,611
4,714
1,919
1,606
382
55,232
55,956
242,664
242,444
220
242,664
¥
¥
¥
6,000
(11,665)
(5,665)
34,639
—
(33,793)
(4,909)
(94)
(4,157)
(9,822)
99,192
99,456
(264)
99,192
See accompanying notes to consolidated financial statements.
F- 4
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Financial Position as of March 31,
Assets
Non-current assets:
Property, plant and equipment
Goodwill
Intangible assets
Investments accounted for using the equity method
Other financial assets
Other non-current assets
Deferred tax assets
Total non-current assets
Current assets:
Inventories
Trade and other receivables
Other financial assets
Income tax receivables
Other current assets
Cash and cash equivalents
Assets held for sale
Total current assets
Total assets
JPY (millions)
Note
2018
2019
10
11
12
14
15
7
16
17
15
18
19
¥
536,801
¥
1,316,531
1,029,248
1,014,264
107,949
196,436
77,977
64,980
4,161,403
4,860,368
114,658
192,241
87,472
88,991
3,027,655
10,821,664
212,944
420,247
80,646
8,545
57,912
294,522
3,992
986,744
741,907
23,276
7,212
109,666
702,093
479,760
1,078,808
3,050,658
¥
4,106,463
¥ 13,872,322
See accompanying notes to consolidated financial statements.
F- 5
Liabilities and Equity
Liabilities:
Non-current liabilities:
Bonds and loans
Other financial liabilities
Net defined benefit liabilities
Accrued income taxes
Provisions
Other non-current liabilities
Deferred tax liabilities
Total non-current liabilities
Current liabilities:
Bonds and loans
Trade and other payables
Other financial liabilities
Accrued income taxes
Provisions
Other current liabilities
Liabilities held for sale
Total current liabilities
Total liabilities
Equity:
Share capital
Share premium
Treasury shares
Retained earnings
Other components of equity
Other comprehensive income related to assets held for sale
Equity attributable to owners of the company
Non-controlling interests
Total equity
Total liabilities and equity
JPY (millions)
Note
2018
2019
20
21
22
23
24
7
20
25
21
23
24
19
¥
985,644
¥
4,766,005
91,223
87,611
—
28,042
68,300
90,725
1,351,545
18
240,259
29,613
67,694
132,781
263,930
3,214
737,509
2,089,054
77,914
90,740
(74,373)
1,557,307
350,631
(4,795)
235,786
156,513
61,900
35,364
75,174
867,061
6,197,803
984,946
327,394
47,340
119,485
392,733
437,888
201,145
2,510,931
8,708,734
1,643,585
1,650,232
(57,142)
1,569,365
353,542
—
1,997,424
5,159,582
19,985
4,006
2,017,409
5,163,588
¥
4,106,463
¥ 13,872,322
See accompanying notes to consolidated financial statements.
F- 6
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Changes in Equity
JPY (millions)
Equity attributable to owners of the Company
Other components of equity
Share
Capital
Share
Premium
Treasury
Shares
Retained
Earnings
Exchange
Differences on
Translation of
Foreign
Operations
Changes in fair
value of financial
assets measured
at fair value
through other
comprehensive
income
Net Changes on
Revaluation of
Available-for-
Sale Financial
Assets
Cash Flow
Hedges
Hedging
Cost
Re-measurement
Gain or Loss on
Defined
Benefit Plans
Total
Other
comprehensive
income related
to assets held for
sale
Non-
Controlling
Interests
Total
Total Equity
As of April 1, 2016
¥
64,766
¥
68,829
¥ (35,974)
¥ 1,523,127
¥
272,361
¥
— ¥
58,523
¥
(3,162)
¥
222
¥
— ¥ 327,944
¥
— ¥1,948,692
¥
62,511
¥
2,011,203
Net profit for the year
Other comprehensive income
(loss)
Comprehensive income (loss)
for the year
Transactions with owners:
—
—
—
—
—
—
Issuance of new shares
437
437
—
—
—
—
114,940
—
—
(50,811)
114,940
(50,811)
Acquisition of treasury
shares
Disposal of treasury shares
Dividends (Note 26)
Changes in ownership
Transfers from other
components of equity
Share-based compensation
(Note 28)
Exercise of share-based
awards (Note 28)
Total transactions with owners
—
—
—
—
—
—
—
437
—
(0)
—
—
—
15,322
(23,117)
4
—
—
—
—
(9,615)
10,353
—
—
—
(141,804)
—
15,554
—
—
6,144
(12,760)
(126,250)
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
9,457
9,457
—
—
—
—
—
—
—
—
—
—
—
—
—
4,634
(222)
15,554
(21,388)
4,634
(222)
15,554
(21,388)
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
(15,554)
(15,554)
—
—
—
—
(15,554)
(15,554)
—
—
—
—
—
—
—
—
—
—
—
—
114,940
573
115,513
(21,388)
(983)
(22,371)
93,552
(410)
93,142
874
(23,117)
4
(141,804)
—
—
15,322
738
—
—
—
(1,910)
(5,487)
—
—
—
874
(23,117)
4
(143,714)
(5,487)
—
15,322
738
(147,983)
(7,397)
(155,380)
As of March 31, 2017
¥
65,203
¥
74,973
¥ (48,734)
¥ 1,511,817
¥
221,550
¥
— ¥
67,980
¥
1,472
¥
— ¥
— ¥ 291,002
¥
— ¥1,894,261
¥
54,704
¥
1,948,965
See accompanying notes to consolidated financial statements.
F- 7
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Changes in Equity
JPY (millions)
Equity attributable to owners of the Company
Other components of equity
Share
Capital
Share
Premium
Treasury
Shares
Retained
Earnings
Exchange
Differences on
Translation of
Foreign
Operations
Changes in fair
value of financial
assets measured
at fair value
through other
comprehensive
income
Net Changes on
Revaluation of
Available-for-
Sale Financial
Assets
Cash Flow
Hedges
Hedging
Cost
Re-measurement
Gain or Loss on
Defined
Benefit Plans
Total
Other
comprehensive
income related
to assets held for
sale
Non-
Controlling
Interests
Total
Total Equity
¥
65,203
¥
74,973
¥ (48,734)
¥ 1,511,817
¥
221,550
¥
— ¥
67,980
¥
1,472
¥
— ¥
— ¥ 291,002
¥
— ¥ 1,894,261
¥
54,704
¥
1,948,965
—
—
—
—
—
—
186,886
—
—
46,252
186,886
46,252
Issuance of new shares
12,711
12,609
As of April 1, 2017
Net profit for the year
Other comprehensive income
Comprehensive income for the
year
Transactions with owners:
Acquisition of treasury
shares
Disposal of treasury shares
Dividends (Note 26)
Changes in ownership
Transfers from other
components of equity
Share-based compensation
(Note 28)
Exercise of share-based
awards (Note 28)
Transfers to other
comprehensive income
related to assets held for
sale
—
—
—
—
—
—
—
—
—
—
—
—
(41,545)
1
—
—
—
—
—
0
—
—
—
18,610
(15,452)
15,905
—
—
—
—
—
(142,120)
—
724
—
—
—
Total transactions with owners
12,711
15,767
(25,639)
(141,396)
—
—
—
—
—
—
—
—
4,795
4,795
—
—
—
—
—
—
—
—
—
—
—
—
—
—
5,057
5,057
—
—
—
—
—
—
—
—
—
—
—
1,919
—
1,606
—
724
—
55,558
1,919
1,606
724
55,558
—
—
—
—
—
—
—
—
—
—
(724)
(724)
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
(724)
4,795
4,071
(4,795)
(4,795)
—
—
—
—
—
—
—
—
—
—
—
186,886
55,558
(178)
398
186,708
55,956
242,444
220
242,664
25,320
(41,545)
1
—
—
—
25,320
(41,545)
1
(142,120)
(2,189)
(144,309)
—
—
18,610
453
—
(32,750)
(32,750)
—
—
—
—
—
18,610
453
—
(139,281)
(34,939)
(174,220)
As of March 31, 2018
¥
77,914
¥
90,740
¥ (74,373)
¥ 1,557,307
¥
272,597
¥
— ¥
73,037
¥
3,391
¥
1,606
¥
— ¥ 350,631
¥
(4,795)
¥ 1,997,424
¥
19,985
¥
2,017,409
See accompanying notes to consolidated financial statements.
F- 8
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Changes in Equity
JPY (millions)
Equity attributable to owners of the Company
Other components of equity
Share
Capital
Share
Premium
Treasury
Shares
Retained
Earnings
Exchange
Differences on
Translation of
Foreign
Operations
Changes in fair
value of financial
assets measured
at fair value
through other
comprehensive
income
Net Changes on
Revaluation of
Available-for-
Sale Financial
Assets
Cash Flow
Hedges
Hedging
Cost
Re-
measurement
Gain or Loss on
Defined
Benefit Plans
Other
comprehensive
income related
to assets held for
sale
Total
Non-
Controlling
Interests
Total
Equity
Total
As of April 1, 2018
¥
77,914
¥
90,740
¥ (74,373)
¥ 1,557,307
¥
272,597
¥
— ¥
73,037
¥
3,391
¥
1,606
¥
— ¥ 350,631
¥
(4,795)
¥1,997,424
¥
19,985
¥
2,017,409
Cumulative effects of
changes in accounting
policies (Note 2)
—
—
—
15,401
Adjusted opening balance
77,914
90,740
(74,373)
1,572,708
Net profit for the year
Other comprehensive income
(loss)
Comprehensive income
(loss) for the year
Transactions with owners:
—
—
—
—
—
—
Issuance of new shares
1,565,671
1,565,671
—
—
—
—
(1,172)
3
—
—
—
—
109,126
—
109,126
—
—
—
(142,697)
(2,337)
32,565
—
—
—
—
(0)
—
—
—
20,102
—
—
—
—
—
—
—
—
(26,281)
18,400
—
—
Acquisition of treasury
shares
Disposal of treasury shares
Dividends (Note 26)
Changes in ownership
Transfers from other
components of equity
Share-based compensation
(Note 28)
Exercise of share-based
awards (Note 28)
Basis adjustment related to
acquisitions
Total transactions with
owners
—
272,597
—
29,964
29,964
—
—
—
—
230
—
—
—
—
84,672
84,672
—
5,938
5,938
—
—
—
—
—
(44,230)
—
—
—
(73,037)
—
—
—
—
—
—
—
—
—
—
—
—
—
—
(1,378)
2,013
—
—
1,606
—
—
—
—
10,257
360,888
—
—
25,658
(10)
25,648
(4,795)
2,023,082
19,975
2,043,057
—
109,126
(112)
109,014
(33,793)
(4,909)
(11,665)
(14,465)
4,795
(9,670)
(152)
(9,822)
(33,793)
(4,909)
(11,665)
(14,465)
4,795
99,456
(264)
99,192
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
34,739
4,715
—
—
—
—
—
—
—
—
—
230
11,665
(32,565)
—
—
—
—
—
39,454
34,739
4,715
11,665
7,119
—
—
—
—
—
—
—
—
—
—
3,131,342
(1,172)
3
—
—
—
3,131,342
(1,172)
3
(142,697)
(169)
(142,866)
(2,107)
(15,536)
(17,643)
—
20,102
(7,881)
39,454
—
—
—
—
—
20,102
(7,881)
39,454
3,037,044
(15,705)
3,021,339
1,565,671
1,559,492
17,231
(112,469)
230
(44,230)
As of March 31, 2019
¥ 1,643,585
¥1,650,232
¥ (57,142)
¥ 1,569,365
¥
302,791
¥
46,380
¥
— ¥
2,959
¥
1,412
¥
— ¥ 353,542
¥
— ¥ 5,159,582
¥
4,006
¥
5,163,588
See accompanying notes to consolidated financial statements.
F- 9
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
Consolidated Statements of Cash Flows for the Year Ended March 31,
Note
2017
JPY (millions)
2018
2019
Cash flows from operating activities:
Net profit for the year
Depreciation and amortization
Impairment losses
Equity-settled share-based compensation
Gain on sales and disposal of property, plant and equipment
Gain on divestment of business and subsidiaries
Loss (gain) on liquidation of foreign operations
Change in fair value of contingent consideration liabilities
Finance (income) expenses, net
Share of loss of associates accounted for using the equity method
Income tax expenses (benefit)
Changes in assets and liabilities:
Increase in trade and other receivables
Decrease in inventories
Increase (decrease) in trade and other payables
Increase (decrease) in provisions
Other, net
Cash generated from operations
Income taxes paid
Tax refunds and interest on tax refunds received
Net cash from operating activities
Cash flows from investing activities:
Interest received
Dividends received
Acquisition of property, plant and equipment
Proceeds from sales of property, plant and equipment
Acquisition of intangible assets
Acquisition of investments
Proceeds from sales and redemption of investments
Acquisition of business, net of cash and cash equivalents acquired
Proceeds from sales of business, net of cash and cash equivalents divested
Payments into restricted deposits
Proceeds from withdrawal of restricted deposits
Payments into time deposits
Proceeds from withdrawal of time deposits
Other, net
Net cash used in investing activities
Cash flows from financing activities:
Net increase (decrease) in short-term loans
Proceeds from bonds and long-term loans
Repayments of bonds and long-term loans
Purchase of treasury shares
Interest paid
Dividends paid
Acquisition of non-controlling interests
Repayments of obligations under finance lease
Facility fees paid for loan agreements
Other, net
Net cash from (used in) financing activities
Net increase (decrease) in cash and cash equivalents
Cash and cash equivalents at the beginning of the year
(Consolidated statements of financial position)
Cash and cash equivalents reclassified back from assets held for sale
Cash and cash equivalents at the beginning of the year
Effects of exchange rate changes on cash and cash equivalents
Cash and cash equivalents at the end of the year
Cash and cash equivalents reclassified to assets held for sale
Cash and cash equivalents at the end of the year
(Consolidated statements of financial position)
¥
31
27
27
27
27
18
19
19
18
¥
115,513
171,426
51,361
15,385
(129)
(115,363)
—
(18,441)
10,975
1,546
27,833
(37,315)
3,886
42,557
20,547
12,333
302,114
(53,227)
12,476
261,363
2,001
3,674
(61,660)
2,629
(50,367)
(12,106)
5,268
(589,144)
64,405
—
—
(70,000)
70,000
(20,391)
(655,691)
406,971
260,226
(191,763)
(23,117)
(6,971)
(141,688)
(4,822)
(4,013)
—
(4,927)
289,896
(104,432)
451,426
—
451,426
(5,742)
341,252
(21,797)
¥
186,708
182,127
13,544
18,610
(434)
(134,100)
41,465
10,523
(7,615)
32,199
30,497
(647)
13,719
6,862
(6,530)
20,809
407,737
(54,874)
24,991
377,854
2,412
7,699
(67,005)
2,965
(61,257)
(16,883)
40,743
(28,328)
85,080
(71,774)
—
—
—
13,006
(93,342)
(403,931)
393,453
(140,000)
(18,756)
(8,365)
(141,893)
—
(2,658)
—
(4,076)
(326,226)
(41,714)
319,455
21,797
341,252
(4,565)
294,973
(451)
109,014
272,446
10,120
20,084
(45,220)
(82,975)
(2,669)
(5,966)
66,446
43,627
(14,118)
(13,382)
58,678
(16,413)
47,063
(73,347)
373,388
(51,536)
6,627
328,479
6,305
2,739
(77,677)
50,717
(56,437)
(17,099)
65,035
(2,958,686)
85,131
—
71,844
—
—
(7,570)
(2,835,698)
367,319
2,795,926
—
(1,172)
(34,914)
(142,952)
(2,392)
(1,741)
(19,507)
(14,330)
2,946,237
439,018
294,522
451
294,973
(31,269)
702,722
(629)
319,455
294,522
702,093
See accompanying notes to consolidated financial statements.
F- 10
TAKEDA PHARMACEUTICAL COMPANY LIMITED AND ITS SUBSIDIARIES
1. Reporting Entity
Notes to Consolidated Financial Statements
Takeda Pharmaceutical Company Limited (the "Company") is a public company incorporated in Japan. The Company and its subsidiaries
(collectively, "Takeda") is a global, values-based, research and development ("R&D") driven biopharmaceutical company with an innovative
portfolio, engaged primarily in the research, development, manufacturing and marketing of pharmaceutical products. Takeda's principal
pharmaceutical products include medicines in the following core business areas: gastroenterology ("GI"), rare diseases, plasma-derived therapies,
oncology, and neuroscience.
Takeda has grown both organically and through acquisitions, completing a series of major transactions that have brought therapeutic, geographic and
pipeline growth, specifically the acquisition of Shire plc ("Shire") in January 2019 for 6,213,335 million JPY (Note 31). Shire was a leading global
biotechnology company focused on serving people with rare diseases and other highly specialized conditions.
2. Basis of Preparation
Compliance with International Financial Reporting Standards
Takeda’s consolidated financial statements have been prepared in accordance with International Financial Reporting Standards ("IFRS"), as issued by
the International Accounting Standards Board (“IASB”). The term IFRS also includes International Accounting Standards (“IASs”) and the related
interpretations of the interpretations committees ("SIC" and "IFRIC").
Approval of Financial Statements
The Company's consolidated financial statements as of and for the year ended March 31, 2019 were approved on June 27, 2019 by Representative
Director, President & Chief Executive Officer (“CEO”) Christophe Weber and Director & Chief Financial Officer ("CFO") Costa Saroukos.
Basis of Measurement
The consolidated financial statements have been prepared on a historical cost basis, except for certain assets and liabilities recorded at fair value
including investments, derivatives, and contingent considerations.
Functional and Presentation Currency
The consolidated financial statements are presented in Japanese Yen ("JPY"), which is the functional currency of the Company. All financial
information presented in JPY has been rounded to the nearest million JPY, except when otherwise indicated.
New Accounting Standards and Interpretations Adopted
During the year ended March 31, 2019, Takeda has adopted the following new accounting standards:
IFRS 9 Financial instruments (“IFRS 9”)
IFRS 9 was issued in its final form in July 2014 and has been implemented by Takeda as of April 1, 2018. IFRS 9 replaces the majority of the
requirements of IAS 39 ‘Financial Instruments: Recognition and Measurement’ (“IAS 39”) and covers the recognition, classification, measurement
and de-recognition of financial assets and financial liabilities; introduces a new impairment model for financial assets based on expected losses rather
than incurred losses and provides a new hedge accounting model. The principal impact for Takeda was the re-measurement of certain available-for-
sale financial instruments to fair value on initial application on April 1, 2018.
Takeda applied IFRS 9 with respect to classification and measurement (including impairment) without restating previous years, with the exception of
hedge accounting impacts which generally have been applied prospectively. The cumulative effects of initially applying IFRS 9 were recognized in
equity as of the date of initial application of IFRS 9 (April 1, 2018). As a result of the adoption on the date of initial application, the opening balance
of retained earnings and other components of equity increased by 14,073 million JPY and 10,257 million JPY, respectively, while other financial
assets (non-current), other financial assets (current), and deferred tax liabilities increased by 32,809 million JPY, 856 million JPY and 9,345 million
JPY, respectively, and non-controlling interests decreasing by 10 million JPY. Comparative period presented for 2017 and 2018 has not been updated
as a result of the adoption of IFRS 9, with the exception of hedge accounting impacts. See Note 3 for further details on the accounting policy under
IAS 39 and IFRS 9.
Takeda elected to designate irrevocably all of its equity instruments as financial assets measured at fair value through other comprehensive income
(FVTOCI). This designation has been made based on the Company’s intent to hold these investments for the foreseeable future. Changes in the fair
F- 11
value of financial assets at FVTOCI are recognized in other comprehensive income, and the cumulative amount of the other comprehensive income is
transferred to retained earnings when the instruments are derecognized due to liquidation or sale.
The classification of other financial assets under IFRS 9 is generally based on the business model in which a financial asset is managed and its
contractual cash flow characteristics. The determination of the business model has been made based on the facts and circumstances that existed at the
date of initial application.
The impairment of financial assets measured at amortized cost is assessed using an expected credit loss (ECL) model where previously the incurred
loss model was used. There was no significant impact on the impairment of receivables upon the adoption of the new standard.
Takeda has not designated any financial liabilities as at fair value through profit or loss. There are no changes in classification and measurement for
Takeda’s financial liabilities following the adoption of IFRS 9.
The adoption of IFRS 9 has not had a material impact on Takeda’s financial liabilities and derivatives.
The new hedge accounting model introduced by the standard requires hedge accounting relationships to be based upon Takeda’s own risk
management objectives and strategy, and to apply a more qualitative and forward-looking approach to assessing hedge effectiveness. The model is to
be discontinued only when the hedging relationships no longer qualify for hedge accounting. All hedging relationships designated under IAS 39 as of
March 31, 2018 met the criteria for hedge accounting under IFRS 9 as of April 1, 2018, and are therefore regarded as continuing hedging
relationships.
In addition, under IAS 39, the currency basis spread was included in cash flow hedges under other component of equity. Under IFRS 9, this basis
spread and time value of the currency options are separately accounted for and presented as hedging cost under other component of equity. The hedge
accounting impacts from IFRS 9 are generally applied prospectively, with the exception of certain aspects being treated retrospectively. Takeda
retrospectively applied the accounting treatment of hedging cost and adjusted the comparative information. The amounts retrospectively recorded as
hedging cost resulted in a 222 million JPY increase to and a 1,606 million JPY deduction from cash flow hedge reserves as of March 31, 2017 and
2018, respectively.
Classification and carrying amounts of financial assets under IAS 39 and IFRS 9 as of the date of adoption were changed as presented in the table
below.
Cash and cash equivalents
Loans and receivables
¥
294,522 Financial assets measured
¥
294,522
IAS 39
JPY (millions)
Carrying
Amount
IFRS 9
JPY (millions)
Carrying
Amount
Derivative assets
Financial assets measured
at fair value through
profit or loss
at amortized cost
762 Financial assets measured
at fair value through
profit or loss
Derivative assets to which hedge accounting
Derivative assets to which
2,527 Derivative assets to which
is applied
hedge accounting is
applied
hedge accounting is
applied
Trade and other receivables, other financial
Loans and receivables
516,853 Financial assets measured
assets
Equity instruments
Convertible notes
Available-for-sale financial
169,814 Financial assets measured
at amortized cost
assets
Loans and receivables
Financial assets measured
at fair value through
profit or loss
at fair value through
other comprehensive
income
5,303 Financial assets measured
2,070
at fair value through
profit or loss
762
2,527
516,853
203,276
7,576
Total
¥
991,851
¥
1,025,516
F- 12
The following changes were made to the carrying amount of the financial assets as of the application date.
JPY (millions)
JPY (millions)
IAS 39
Loans and receivables
Carrying Amount
816,678
¥
Re-
Classification
¥
(5,303) ¥
Financial assets measured
at fair value through
profit or loss
Derivative assets to which
hedge accounting is
applied
Available-for-sale
financial assets
2,527
169,814
—
—
Re-Measurement
IFRS 9
Carrying Amount
— Financial assets measured
at amortized cost
¥
at fair value through
profit or loss
— Derivative assets to which
hedge accounting is
applied
811,375
8,338
2,527
33,462 Financial assets measured
203,276
at fair value through other
comprehensive income
2,832
5,303
203 Financial assets measured
Total
¥
991,851
¥
— ¥
33,665
¥
1,025,516
IFRS 15 Revenue from Contracts with Customers (“IFRS 15”)
Takeda adopted IFRS 15 on April 1, 2018. The new standard provides a single, principles-based approach to the recognition of revenue from all
contracts with customers. The standard focuses on the identification of performance obligations in a contract and requires revenue to be recognized
when or as those performance obligations are satisfied. The standard also has more detailed disclosure requirements. IFRS 15 did not have a material
impact on the amount or timing of recognition of revenue.
The amount and timing of the recognition of sales and the basis for the estimates of sales deductions generally remained consistent as it relates to
revenue derived from the sale of pharmaceutical products.
The previous revenue recognition for considerations received related to revenue received from out-licensing agreements required the transfer of
ownership and related royalty income to be recognized on an accrual basis in accordance with the substance of the agreement as remaining
performance obligations. The basis of allocation to the transfer of ownership and an allocation of revenue over the remaining performance
obligations, and therefore timing of recognition for consideration received, has changed as a result of adoption. The impact of this change is not
material.
Takeda elected the modified retrospective method upon adoption of IFRS 15, which requires the recognition of the cumulative effect of initially
applying IFRS 15 in opening equity at the date of initial application. As a result of the adoption of IFRS 15, due to the difference in allocation of
revenue to performance obligations for considerations received related to out-licensing agreements, other non-current liabilities, other current
liabilities, and deferred tax assets decreased by 1,247 million JPY, 495 million JPY and 414 million JPY respectively, and opening retained earnings
increased by 1,328 million JPY.
For the year ended March 31, 2019, the impact from adoption of IFRS 15 on the consolidated financial statements was immaterial compared to the
consolidated financial statements under IAS 18.
New Accounting Standards and Interpretations Issued and Not Yet Adopted
New or amended accounting standards and interpretations that have been issued as of the date of approval of the consolidated financial statements but
are not effective and have not yet been adopted by Takeda as of March 31, 2019 are discussed below:
IFRS 16 Leases (“IFRS 16”)
The standard will require lease liabilities and right of use (ROU) assets to be recognized on the balance sheet for almost all leases. Of the costs from
operating leases currently included within cost of sales, selling, general and administrative expenses, research and development expenses, and other
operating expenses, the portion related to the financing element will be reclassified and reported as finance expenses. In the statement of cash flow,
the lease payments currently included within cash outflows from operating activities will be reported within cash flows from financing activities.
IFRS 16 is effective for Takeda on April 1, 2019.
As a lessee, this standard can be applied retrospectively to each prior reporting period (retrospective approach) or retrospectively with the cumulative
effect of initially applying this standard recognized at the date of initial application (modified retrospective approach). Takeda has elected to apply the
standard applying the modified retrospective approach. Under the modified retrospective approach, the lease liabilities will be measured at the
present value of the remaining lease payments, discounted at the incremental borrowing rate as of April 1, 2019. The ROU assets will be recognized
at an amount equal to the lease liability, adjusted for any prepaid or accrued lease payments, onerous lease provisions and business combination
related fair value adjustments.
F- 13
On April 1, 2019, Takeda expects to recognize additional lease liabilities of approximately 220 billion JPY and corresponding ROU assets of
approximately 200 billion JPY excluding existing finance leases. The additional liabilities and ROU assets include the impact of the operating leases
obtained as a result of the Shire Acquisition.
IFRIC 23 Uncertainty over Income Tax Treatments (“IFRIC 23”)
The interpretation clarifies that if it is considered probable that a tax authority will accept an uncertain tax treatment, the tax charge should be
calculated on that basis. If it is not considered probable, the effect of the uncertainty should be estimated and reflected in the tax charge. In assessing
the uncertainty, it is assumed that the tax authority will have full knowledge of all information related to the matter. IFRIC 23 is effective for Takeda
on April 1, 2019.
Other Standards
In addition, the following amendments and interpretations have been issued:
•
•
•
•
•
Amendments to IFRS 10 and IAS 28 ‘Sale or Contribution of Assets between an Investor and its Associate or Joint Venture’. The IASB has
deferred these amendments until a date to be determined by the IASB.
Amendments to IFRS 9: Prepayment Features with Negative Compensation
Amendments to IAS 19: Plan Amendment, Curtailment or Settlement
Amendments to IAS 28: Long-term interests in associates and joint ventures
Annual Improvements 2015-2017 Cycle (issued in December 2017) including improvements to IFRS 3 Business Combinations, IFRS 11
Joint Arrangements, IAS 12 Income Taxes and IAS 23 Borrowing Costs
The adoption of the amendments to IFRIC 23 and these additional amendments and interpretations are not expected to have a significant impact on
Takeda’s consolidated financial statements. For those amendments and interpretations where early adoption is permitted, Takeda does not plan to
early adopt.
Use of Judgments, Estimates, and Assumptions
The preparation of consolidated financial statements in accordance with IFRS requires management to make certain judgments, estimates, and
assumptions that affect the application of accounting policies and the reported amount of assets, liabilities, revenues and expenses, and the disclosure
of contingent assets and liabilities. Actual results could differ from these estimates.
These estimates and underlying assumptions are reviewed on a continuous basis. Changes in these accounting estimates are recognized in the period
in which the estimates are revised and in any future periods affected.
Information about judgments and estimates that have been made in the process of applying accounting policies and that have significant effects on
the amounts reported in the consolidated financial statements, and information about accounting estimates and assumptions that have significant
effects on the amounts reported in the consolidated financial statements, are as follows:
Recognition and measurement of taxes based on uncertain tax positions (Note 7)
Recoverability of deferred tax assets (Note 7)
Impairment of property, plant and equipment; goodwill; and other intangible assets (Note 10, Note 11, and Note 12, respectively)
•
•
•
• Measurement of fair value of assets acquired and liabilities assumed and contingent consideration in business combinations (Note 21 and
Note 31)
• Measurement of defined benefit obligations (Note 22)
• Measurement of provisions, including estimation of rebates and return reserves associated with Takeda’s product sales (Note 23)
•
•
Valuation assumptions relating to share-based compensation (Note 28)
Probability of an outflow of resources embodying economic benefits on contingent liabilities (Note 32)
3. Significant Accounting Policies
Basis of Consolidation
The consolidated financial statements include the accounts of the Company and its subsidiaries that are directly or indirectly controlled by the
Company. All significant intercompany balances and transactions have been eliminated in consolidation.
Takeda controls an entity when it is exposed or has rights to variable returns from involvement with the entity and has the ability to affect those
returns using its power, which is the current ability to direct the relevant activities, over the entity. To determine whether Takeda controls an entity,
status of voting rights or similar rights, contractual agreements and other specific factors are considered.
The financial statements of the subsidiaries are included in the consolidated financial statements from the date when control is obtained until the date
when control is lost. The financial statements of subsidiaries have been adjusted in order to ensure consistency with the accounting policies adopted
by the Company as necessary.
F- 14
Changes in ownership interest in subsidiaries that do not result in loss of control are accounted for as equity transactions. Any difference between the
adjustment to non-controlling interests and the fair value of consideration transferred or received, is recognized directly in equity attributable to
owners of the Company. When control over a subsidiary is lost, the investment retained after the loss of control is re-measured at fair value as of the
date when control is lost, and any gain or loss on such re-measurement and disposal of the interest sold is recognized in profit or loss.
Investments in Associates and Joint Arrangements
Associates are entities over which Takeda has significant influence over the decisions on financial and operating policies, but does not have control or
joint control. Investments in associates are accounted for using the equity method and recognized at cost on the acquisition date. The carrying amount
is subsequently increased or decreased to recognize Takeda’s share of profit or loss and other comprehensive income of the affiliate. Intra-group
profits on transactions with associates accounted for using the equity method are eliminated against the investment to the extent of Takeda’s equity
interest in the associates. Intra-group losses are eliminated in the same way as intra-group profits unless there is evidence of impairment.
Joint arrangement is an arrangement of which two or more parties have joint control. Joint control is the contractually agreed sharing of control of an
arrangement, which exists only when decisions about the relevant activities require the unanimous consent of the parties sharing control. Takeda
classifies joint arrangement into either joint operations or joint ventures. The classification of a joint arrangement as a joint operation or a joint
venture depends upon the rights and obligations of the parties to the arrangement. Joint operation is a joint arrangement whereby the parties that have
joint control of the arrangement have rights to the assets, and obligations for the liabilities, relating to the arrangement. Joint venture is a joint
arrangement whereby the parties that have joint control of the arrangement have rights to the net assets of the arrangement. The assets, liabilities,
revenues and expenses in joint operations are recognized in relation to Takeda’s interest. The investment in joint ventures is accounted for using the
equity method. At each reporting date, the Company determines whether there is objective evidence that the investment in the associate or joint
venture is impaired. If there is such evidence, the Company calculates the amount of impairment as the difference between the recoverable amount of
the associate or joint venture and its carrying value, and then recognizes the loss within profit or loss.
Business Combinations
Business combinations are accounted for using the acquisition method. The identifiable assets acquired and the liabilities assumed are measured at
the fair values at the acquisition date. Goodwill is measured as the excess of the sum of the fair value of consideration transferred, the amount of any
non-controlling interests in the acquiree and the fair value of the acquirer's previously held equity interest in the acquiree less the fair value of
identifiable assets acquired, net of liabilities assumed at the acquisition date. As part of business combinations, when the acquired entity consists of
foreign operations with multiple functional currencies, Takeda allocates goodwill recognized upon the acquisition to the foreign operations based on
the estimated cash flows of the acquired foreign operations.
The consideration transferred for the acquisition of a subsidiary is measured as the fair value of the assets transferred, the liabilities incurred to
former owners of the acquiree, and the equity interests issued by Takeda. Non-controlling interests is initially measured either at fair value or at the
non-controlling interests’ proportionate share of the recognized amounts of the acquiree’s identifiable net assets on a transaction-by-transaction basis.
The consideration for certain acquisitions includes amounts contingent upon future events, such as the achievement of development milestones and
sales targets.
Any contingent consideration included in the consideration payable for a business combination is recorded at fair value at the date of acquisition.
These fair values are generally based on risk-adjusted future cash flows discounted using appropriate discount rates. The fair values are reviewed at
the end of each reporting period. The changes in the fair value based on the time value of money are recognized in finance expenses and the other
changes are recognized in other operating income or other operating expenses in the consolidated statements of income.
Acquisition related costs are recognized as expenses in the period they are incurred. Changes in Takeda’s ownership interests in subsidiaries arising
from transactions between Takeda and non-controlling interests that do not result in Takeda losing control over a subsidiary are treated as equity
transactions and therefore, do not result in adjustments to goodwill.
Foreign Currency Translations
Foreign Currency Transactions
Foreign currency transactions are translated into the functional currency of each entity within Takeda using the exchange rates at the dates of the
transactions or rates that approximate the exchange rates at the dates of the transactions. Monetary assets and liabilities denominated in foreign
currencies are translated into the functional currency using the spot rates of exchange at the end of each reporting period. Non-monetary assets and
liabilities that are measured at fair value in foreign currencies are translated using historical exchange rates at the date when the fair value was
determined. Non-monetary assets and liabilities measured based on historical cost that are denominated in foreign currencies are translated at the
exchange rate at the date of the initial transaction. Exchange differences arising from the translation or settlement are recognized in profit or loss
except when related to financial assets measured at fair value through other comprehensive income, as well as financial instruments designated as
hedges of net investments in foreign operations and cash flow hedges subsequently recognized as other comprehensive income. The gain or loss
arising from translation of non-monetary items measured at fair value is treated in line with the recognition of the gain or loss on the change in fair
value of the item (i.e., translation differences on items whose fair value gain or loss is recognized in other comprehensive income or profit or loss, are
also recognized in other comprehensive income or profit or loss, respectively).
F- 15
Foreign Operations
The assets and liabilities of foreign operations are translated using the spot exchange rates at the end of the reporting period, while income and
expenses of foreign operations presented in profit or loss and other comprehensive income are translated using the exchange rates at the dates of the
transactions or rates that approximate the exchange rates at the dates of the transactions.
Exchange differences arising from translation are recognized as other comprehensive income. In cases in which foreign operations are disposed of,
the cumulative amount of exchange differences related to the foreign operations is recognized as part of the gain or loss on disposal.
Revenue
Revenue on sales of Takeda products and services is recognized when control of the products is passed to the customer in an amount that reflects the
consideration to which we expect to be entitled in exchange for those products. Control is generally transferred at the point in time of shipment to or
receipt of the products by customer, or when the services are performed. The amount of revenue to be recognized is based on the consideration
Takeda expects to receive in exchange for its goods and services. If a contract contains more than one contractual promise to a customer
(performance obligation), the consideration is allocated based on the standalone selling price of each performance obligation.
The consideration Takeda receives in exchange for its goods or services may be fixed or variable. Variable consideration is only recognized when it is
highly probable that a significant reversal will not occur. The most common elements of variable consideration are listed below:
•
•
•
Rebates and discounts granted to government agencies, wholesalers, retail pharmacies, managed healthcare organizations and other
customers are estimated and recorded as a deduction from revenue at the time the related revenues are recorded. They are calculated on the
basis of historical experience and the specific terms in the individual agreements.
Cash discounts are offered to customers and are provisioned and recorded as revenue deductions at the time the related sales are recorded.
Sales return provisions are recognized when Takeda sells a product which provides the customer a right of return. Sales return provisions
are recorded as revenue deductions when there is historical experience of Takeda agreeing to customer returns and Takeda can reasonably
estimate expected future returns. In doing so, the estimated rate of return is applied, determined based on historical experience of customer
returns and considering any other relevant factors. The rate is multiplied by the amounts invoiced in order to estimate expected future
returns.
Takeda generally receives payments from customers within 120 days after the point in time when goods are delivered to the customers. Takeda
usually performs those transactions as a principal, but Takeda also sells products on behalf of others, and revenue is recognized at an amount of sales
commission that Takeda expects to be entitled as an agent.
Takeda also generates revenue in the form of royalty payments, upfront payments, and milestone payments from the out-licensing of intellectual
property (IP). Royalty revenue earned through a license is recognized when the underlying sales have occurred. Revenue from upfront payment is
generally recognized when Takeda provides a right to use IP. Revenue from milestone payments is recognized at the point in time when it is highly
probable that the respective milestone event criteria is met, and a significant reversal in the amount of revenue recognized will not occur. Revenue
from other services such as research and development of compounds that are out-licensed is recognized over the service period.
Takeda generally receives payments from customers within 60 days after entering into out-licensing contracts or confirmation by customers that
conditions for the milestone payments are met. Takeda licenses its own intellectual property rights to customers, and performed those transactions as
a principal. Takeda also provides other services as a principal.
Government Grants
Government grants are recognized when there is reasonable assurance that Takeda will comply with the conditions attached to them and receive the
grants. Government grants for the purchasing of property, plant and equipment are recognized as deferred income and then recognized as profit or
loss and offset the related expenses on a systematic basis over the useful lives of the related assets.
Government grants for expenses incurred are recognized as profit or loss and offset the related expenses over the periods in which Takeda recognizes
costs for which the grants are intended to compensate.
Advertising and Sales Promotion Expenses
Costs of advertising and sales promotion are expensed as incurred. Advertising and sales promotion expense was 112,842 million JPY, 115,708
million JPY, and 106,755 million JPY for the years ended March 31, 2017, 2018 and 2019, respectively.
Research and Development Expenses
Research costs are expensed in the period incurred. Internal development expenditures are capitalized when the criteria for recognizing an asset are
met in accordance with IAS 38 ‘Intangible Assets,’ usually when a regulatory filing has been made in a major market and approval is considered
highly probable. Where regulatory and other uncertainties are such that the criteria are not met, the expenditures are recognized in the income
statement. Property, plant and equipment used for research and development is capitalized and depreciated over the estimated life of the asset.
F- 16
Income Taxes
Income taxes consist of current taxes and deferred taxes. Current and deferred taxes are recognized in profit or loss, except for income taxes resulting
from business combinations, and income taxes recognized in either other comprehensive income or equity related to items that are recognized, in the
same or different period, outside of profit or loss.
Current Taxes
The current tax payable or receivable is based on taxable profit for the year. Taxable profit differs from reported profit because taxable profit excludes
items that are either never taxable or tax deductible or items that are taxable or tax deductible in a different period. Accrued income taxes and income
tax receivable, including those from prior fiscal years, are measured at the amount that is expected to be paid to or received from the taxation
authorities, reflecting uncertainty related to income taxes, if any. Takeda’s current taxes also include liabilities related to uncertain tax positions.
Takeda’s current tax assets and liabilities are calculated using tax rates that have been enacted or substantively enacted by the reporting date.
Deferred Taxes
Deferred taxes are calculated based on the temporary differences between the carrying amounts of assets and liabilities for financial reporting
purposes and the amounts used for taxation purposes at the end of the reporting period. Deferred tax assets are recognized for deductible temporary
differences, unused tax credits and unused tax losses to the extent that it is probable that future taxable profit will be available against which the
assets can be utilized. This requires us to evaluate and assess the probability of future taxable profit and our business plan, which are inherently
uncertain. Uncertainty of estimates of future taxable profit could increase due to changes in economies in which we operate, changes in market
conditions, effects of currency fluctuations, or other factors. Takeda’s deferred taxes also include liabilities related to uncertain tax positions.
Deferred tax liabilities are generally recognized for taxable temporary differences.
Deferred tax assets and liabilities are not recognized for the following temporary differences:
•
•
•
•
Taxable temporary differences arising on the initial recognition of goodwill
The initial recognition of assets and liabilities in transactions that are not business combinations and affect neither accounting profit nor
taxable profit (loss) at the time of the transaction
Deductible temporary differences arising from investments in subsidiaries and associates, when it is not probable that the temporary
differences will reverse in the foreseeable future and that taxable profit will be available against which the temporary differences can be
utilized
Taxable temporary differences arising from investments in subsidiaries and associates when the timing of the reversal of the temporary
differences is controllable and it is not probable that they will reverse in the foreseeable future
Deferred tax assets and liabilities are measured at the tax rates that are expected to apply to the periods in which the temporary differences are
expected to reverse based on the tax rates and tax laws that have been enacted or substantively enacted by the end of the reporting period. Deferred
tax assets and liabilities are offset when there is a legally enforceable right to offset current tax assets against current tax liabilities and the deferred
tax assets and liabilities for those related to income taxes levied by the same taxation authority on the same taxable entity.
Earnings per Share
Basic earnings per share is calculated by dividing profit or loss for the year attributable to owners of ordinary shares of the Company, by the
weighted-average number of ordinary shares outstanding during the reporting period, adjusted by the number of treasury shares. Diluted earnings per
share is calculated by adjusting all the effects of dilutive potential ordinary shares.
Property, Plant and Equipment
Property, plant and equipment are measured using the cost model and is stated at cost less accumulated depreciation and accumulated impairment
loss. Acquisition cost includes mainly the costs directly attributable to the acquisition and the initial estimated dismantlement, removal, and
restoration costs associated with the asset. Except for assets that are not subject to depreciation, such as land and construction in progress, assets are
depreciated mainly using the straight-line method over the estimated useful life of the asset. Leased assets are depreciated using the straight-line
method over the shorter of the lease term or the estimated useful life unless it is reasonably certain that Takeda will obtain ownership by the end of
the lease term. The depreciation of these assets begins when they are available for use.
The estimated useful life of major asset items is as follows:
•
Buildings and structures
• Machinery and vehicles
•
Tools, furniture and fixtures
3 to 50 years
2 to 20 years
2 to 20 years
F- 17
Goodwill
Goodwill arising from business combinations is stated at its cost less accumulated impairment losses. Goodwill is not amortized. Goodwill is
allocated to cash-generating units or groups of cash-generating units based on expected synergies and tested for impairment annually or whenever
there is any indication of impairment. Impairment losses on goodwill are recognized in the consolidated statements of income and no subsequent
reversal will be made.
Intangible Assets Associated with Products
Marketed Products
An intangible asset associated with a marketed product is amortized on a straight-line basis over the estimated useful life, which is based on expected
exclusivity period, ranging from 3 to 20 years. Amortization of intangible assets is included in amortization and impairment losses on intangible
assets associated with products in the consolidated statements of income. Amortization and impairment losses on intangible assets associated with
products is separately stated in the consolidated statement of income because intangible assets associated with products have various comprehensive
rights and contribute to our ability to sell, manufacture, research, market and distribute products, compounds and benefit multiple business functions.
In-Process R&D
Takeda regularly enters into collaboration and in-license agreements with third parties for products and compounds for research and development
projects. Payments for collaboration agreements generally take the form of subsequent development milestone payments. Payments for in-license
agreements generally take the form of up-front payments and subsequent development milestone payments.
Up-front payments for in-license agreements are capitalized upon commencement of the in-license agreements, and development milestone payments
are capitalized when the milestone is triggered.
These intangible assets relating to products in development that are not yet available for use are not amortized. These intangible assets are assessed
for impairment on an annual basis, or more frequently if indicators of a potential impairment exist. An impairment is recorded if the carrying value
exceeds the recoverable amount of the intangible assets. Intangible assets relating to products which fail during development, or for which
development ceases for any reason are written down to their recoverable amount which is typically nil.
If and when Takeda obtains approval for the commercial application of a product in development, the related in-process research and development
assets will be reclassified to intangible assets associated with marketed products and amortized over its estimated useful life from marketing
approval.
Intangible Assets – Software
Software is recognized at cost and amortized on a straight-line basis over the expected useful life. The useful life used for this purpose is 3 to 10
years. Amortization of intangible assets – software is included in cost of sales, selling, general and administrative expenses, and research and
development expenses in the consolidated statements of income.
Leases
Leases are classified as finance leases if substantially all the risks and rewards incidental to ownership are transferred to the lessee. Leases other than
finance leases are classified as operating leases.
As Lessee
At the commencement of the lease term, Takeda recognizes finance leases as assets and liabilities in the consolidated statements of financial position
at amounts equal to the fair value of the leased property or, if lower, the present value of the minimum lease payments, each determined at the
inception of the lease. Lease payments for operating leases are recognized as expenses on a straight-line basis over the lease term, unless another
systematic basis is more representative of the time pattern of the user's benefit is available.
Impairment of Non-Financial Assets
Takeda assesses whether there is any indication of impairment for non-financial assets at the end of each reporting period, excluding inventories,
deferred tax assets, assets held for sale, and assets arising from employee benefits. If any such indication exists, or in cases in which an impairment
test is required to be performed each year, the recoverable amount of the asset is estimated. In cases in which the recoverable amount cannot be
estimated for each asset, they are estimated at the cash-generating unit level. The recoverable amount of an asset or a cash-generating unit is
determined at the higher of its fair value less costs of disposal, or its value in use. In determining the value in use, the estimated future cash flows are
discounted to their present value using a discount rate that reflects the time value of money and the risks specific to the asset. If the carrying amount
of the asset or cash-generating unit exceeds the recoverable amount, impairment loss is recognized in profit or loss and the carrying amount is
reduced to the recoverable amount. An asset or a cash-generating unit other than goodwill, for which impairment losses were recognized in prior
years, is assessed at the end of the reporting period to determine whether there is any indication that the impairment loss recognized in prior periods
F- 18
may no longer exist or may have decreased. If any such indication exists, the recoverable amount of the asset or cash-generating unit is estimated. In
cases in which the recoverable amount exceeds the carrying amount of the asset or cash-generating unit, the impairment loss is reversed up to the
lower of the estimated recoverable amount or the carrying amount that would have been determined if no impairment loss had been recognized in
prior years. The reversal of impairment loss is immediately recognized in profit or loss.
Inventories
Inventories are measured at the lower of cost and net realizable value. The cost of inventories is determined mainly using the weighted-average cost
formula. The cost of inventories includes purchase costs, costs of conversion, and other costs incurred in bringing the inventories to the present
location and condition. Net realizable value is the estimated selling price in the ordinary course of business less the estimated costs of completion and
the estimated costs necessary to make the sale. Pre-launch inventory is held as an asset when there is a high probability of regulatory approval for the
product. Before that point, a provision is made against the carrying value to its recoverable amount; the provision is then reversed at the point when a
high probability of regulatory approval is determined.
Cash and cash equivalents
Cash and cash equivalents consist of cash on hand, demand deposits and short-term, highly liquid investments that are readily convertible to known
amounts of cash and subject to insignificant risk of change in value and due within three months from the date of acquisition.
Assets Held for Sale
An asset or disposal group for which the cash flows are expected to arise principally from sale rather than continuing use is classified as an asset held
for sale when it is highly probable that the asset or disposal group will be sold within one year, the asset or disposal group is available for immediate
sale in its present condition, and the management of Takeda is committed to the sale. In such cases, the asset held for sale is measured at the lower of
its carrying amount and fair value less costs to sell.
Property, plant and equipment and intangible assets classified as held for sale are not depreciated or amortized. Assets and liabilities classified as held
for sale are presented separately as current items in the consolidated statements of financial position.
Post-employment Benefit
Takeda sponsors lump-sum payments on retirement, pensions and other plans such as post-retirement medical care as post-employment benefit plans.
They are classified into defined benefit plans and defined contribution plans.
Defined Benefit Plans
Takeda uses the projected unit credit method to determine the present value, the related current service cost, and the past service cost by each defined
benefit obligation. The discount rate is determined by reference to market yields on high quality corporate bonds at the end of the reporting period.
The net defined benefit liabilities (assets) in the consolidated statements of financial position are calculated by deducting the fair value of the plan
assets from the present value of the defined benefit obligations. Past service cost defined as the change in the present value of the defined benefit
obligation resulting from a plan amendment or curtailment is recognized in profit or loss upon occurrence of the plan amendment or curtailment.
Re-measurement of net defined benefit plans is recognized in full in other comprehensive income and transferred to retained earnings in the period in
which they are recognized.
Defined Contribution Plans
The costs for defined contribution plans are recognized as expenses when the employees render the related service.
Provisions
Takeda recognizes rebates and return reserves if Takeda receives consideration from a customer and expects to refund some or all of that
consideration to the customer. In addition, provisions are recognized when Takeda has present legal or constructive obligations as a result of past
events, it is probable that outflows of resources embodying economic benefits will be required to settle the obligations and reliable estimates can be
made of the amount of the obligations. Takeda’s provisions consist primarily of rebates and return reserves, as well as provisions for litigation and
restructuring.
Financial Instruments
Takeda’s financial instruments include financial instruments related to lease contracts, trade and other receivables and payables, liabilities for
contingent consideration under business combinations, derivative instruments, and rights and obligations under employee benefit plans, which are
dealt with in specific accounting policies.
F- 19
Financial Assets – Subsequent to April 1, 2018
Initial Recognition and Measurement
Financial assets are recognized in the consolidated statements of financial position when Takeda becomes a party to the contractual provisions of the
instruments. Financial assets, except for investments in debt instruments recorded at fair value through profit or loss (FVTPL), are initially measured
at fair value plus transaction costs that are directly attributable to the acquisition.
Investments in debt instruments recorded at amortized cost: Assets such as trade and other receivables that are held within a business model whose
objective is to hold financial assets in order to collect contractual cash flows and whose contractual terms give rise on specified dates to cash flows
that are solely payments of principal and interest on the principal amount outstanding are measured at amortized cost. Trade receivables are initially
recognized at their invoiced amounts, including any related sales taxes less adjustments for revenue deductions such as impairment loss allowance
and cash discounts.
Investments in debt instruments recorded at fair value through other comprehensive income (FVTOCI): Assets that are held within a business model
objective whose objective is achieved by both collecting contractual cash flows and selling financial assets whose contractual terms give rise on
specified dates to cash flows that are solely payments of principal and interest on the principal amount outstanding are measured at FVTOCI.
Investments in debt instruments recorded at fair value through profit or loss (FVTPL): Assets that do not meet the criteria for amortized cost or
FVTOCI are measured at FVTPL.
Equity instruments recorded at FVTOCI: On initial recognition, Takeda made an irrevocable FVTOCI election (on an instrument-by-instrument
basis) to present the subsequent changes in the fair value of equity instruments in other comprehensive income for certain equity instruments held for
the long term for strategic purposes. At the reporting date, Takeda designates all of its equity instruments as financial assets at FVTOCI.
Subsequent Measurement and Derecognition
Takeda derecognizes a financial asset only when the contractual right to receive the cash flows from the asset expires or when Takeda transfers
the financial asset and substantially all the risks and rewards of ownership of the asset to another entity.
Investments in debt instruments recorded at amortized cost: These assets are subsequently measured at amortized cost using the effective interest
method. The amortized cost is reduced by impairment losses. Interest income, foreign exchange gains and losses and impairment are recognized in
profit or loss. Any gain or loss on derecognition is recognized in profit or loss.
Investments in debt instruments recorded at FVTOCI: These assets are subsequently measured at fair value. Interest income calculated using the
effective interest method, foreign exchange gains and losses and impairment are recognized in profit or loss. Other net gains and losses are
recognized in OCI. Upon derecognition of the investments, the gains and losses accumulated in OCI related to the investment is reclassified to profit
or loss.
Investments in debt instruments recorded at FVTPL: These assets are subsequently measured at fair value, and a gain or loss on debt instruments that
is subsequently measured at FVTPL is recognized in profit or loss.
Equity instruments recorded at FVTOCI: These assets are subsequently measured at fair value. Dividends are recognized as income in profit or loss
unless the dividend clearly represents a recovery of part of the cost of the investment. Other net gains and losses are recognized in OCI and are never
reclassified to profit or loss. Upon derecognition of the investments, the amounts in OCI related to the investment is reclassified within equity to
retained earnings.
Impairment
Loss allowances for trade receivables are established using an ECL model. The provisions are based on a forward-looking ECL, which includes
possible default events on the trade receivables over the entire holding period of the trade receivables. Takeda has elected to measure provisions for
trade receivables, contract assets and lease receivables at an amount equal to lifetime ECL. Takeda uses a provisions matrix based on historical loss
rates adjusted for forward looking information to calculate ECL. These provisions represent the difference between the contractual amount of the
trade receivables and the lease receivables in the consolidated financial statements of financial position and the estimated collectible net amount.
Financial Assets – Prior to April 1, 2018
Initial Recognition and Measurement
Financial assets are recognized in the consolidated statements of financial position when Takeda becomes a party to the contractual provisions of the
instruments. Financial assets, except for financial assets at fair value through profit or loss, are initially measured at fair value plus transaction costs
that are directly attributable to the acquisition.
F- 20
At the initial recognition, the financial assets are classified based on the nature and purpose in accordance with the following:
•
•
•
Financial assets at fair value through profit or loss: Either held-for-trading financial assets or financial assets designated as financial assets
at fair value through profit or loss.
Loans and receivables: Non-derivative financial assets with fixed or determinable payments that are not quoted in an active market.
Available-for-sale financial assets: Non-derivative financial assets that are either designated as available-for-sale financial assets or not
classified as (a) financial assets at fair value through profit or loss, or (b) loans and receivables.
Subsequent Measurement
•
•
•
Financial assets at fair value through profit or loss – Financial assets at fair value through profit or loss are measured at fair value, and any
gains or losses arising on re-measurement are recognized in profit or loss.
Loans and receivables – Loans and receivables are measured at amortized cost using the effective interest method less any impairment loss.
Interest income is recognized principally by applying the effective interest rate, unless the recognition of interest is immaterial as in the
case of short-term receivables.
Available-for-sale financial assets – Available-for-sale financial assets are measured at fair value as of the end of the reporting period, and
the gains and losses arising from changes in fair value are recognized in other comprehensive income. Exchange differences on monetary
assets are recognized in profit or loss. Dividends on available-for-sale financial assets (equity instruments) are recognized in profit or loss
in the reporting period when Takeda’s right to receive the dividends is established. Upon derecognition of the investments, the amounts in
OCI related to the investment is reclassified to profit or loss.
Impairment
Financial assets are considered impaired when there is objective evidence that one or more events occurred after the initial recognition of the
financial asset and it is reasonably anticipated to have had a negative impact on the estimated future cash flows of the asset. For available-for-sale
equity instrument, a significant or prolonged decline in the fair value below its cost is considered objective evidence of impairment. Even when there
is no objective evidence of impairment individually, certain categories of financial assets, such as trade receivables, are collectively assessed for
impairment. For financial assets measured at amortized cost, the impairment loss is the difference between the carrying amount of the asset and the
present value of the estimated future cash flows discounted at the original effective interest rate on the asset. In a subsequent period, if the amount of
the impairment loss decreases and the decrease can be related objectively to an event occurring after the impairment was recognized; the previously
recognized impairment loss is reversed through profit or loss. When an available-for-sale financial asset is determined to be impaired, the cumulative
gain or loss that was previously accumulated in accumulated other comprehensive income (loss) is reclassified to profit or loss in the same period. In
respect to available-for-sale equity investments, impairment loss previously recognized in profit or loss is not reversed through profit or loss. In
respect to available-for-sale debt instruments, if the amount of the fair value increases in a subsequent period and the increase can be related
objectively to an event occurring after the impairment was recognized; the previously recognized impairment loss is reversed through profit or loss.
Derecognition
Takeda derecognizes a financial asset only when the contractual right to receive the cash flows from the asset expires or when Takeda transfers the
financial asset and substantially all the risks and rewards of ownership of the asset to another entity. On derecognition of a financial asset, the
difference between the carrying amount and the consideration received or receivable is recognized in profit or loss, and the cumulative gain or loss
that was previously accumulated in accumulated other comprehensive income (loss) is reclassified to profit or loss.
Financial Liabilities
Initial Recognition and Measurement
Financial liabilities are recognized in the consolidated statements of financial position when Takeda becomes party to contractual provisions of
financial instruments. Financial liabilities are classified, at initial recognition, as financial liabilities at fair value through profit or loss, bonds and
loans, or payables.
Financial liabilities, except for financial liabilities at fair value through profit or loss, are initially measured at fair value less transaction costs that are
directly attributable to the issuance.
Subsequent Measurement
Financial liabilities recorded at FVTPL: Financial liabilities at fair value through profit or loss are measured at fair value, and any gains or losses
arising on re-measurement are recognized in profit or loss. Financial liabilities at fair value through the profit and loss includes derivatives and
contingent consideration related to business combinations.
Other financial liabilities, including bonds and loans: Other financial liabilities are measured at amortized cost mainly using the effective interest
method.
F- 21
Derecognition
Takeda derecognizes a financial liability only when the obligation specified in the contract is discharged, cancelled, or expires. On derecognition of a
financial liability, the difference between the carrying amount and the consideration paid or payable is recognized in profit or loss.
Derivatives
Takeda hedges the risks arising mainly from their exposure to fluctuations in foreign currency exchange rates and interest rates using derivative
financial instruments such as foreign exchange forward contracts, interest rate swaps, currency options, and currency swaps. Takeda does not enter
into derivative transactions for trading or speculative purposes. Derivatives are measured at FVTPL unless the derivative contracts are designated as
hedging instruments. The gains and losses on derivatives that are not designed as hedging instruments are recognized in profit or loss. The treatment
of the change in fair value for derivatives designated as hedging instruments varies based on the type of hedge as described below.
Hedge Accounting- Subsequent to April 1, 2018
For foreign currency exposure as a result of translation risk, Takeda designates certain non-derivatives, such as foreign currency denominated debt, as
net investment hedges of foreign operations. For foreign currency exposure due to foreign currency denominated transactions, Takeda designates
certain derivatives, such as foreign currency forwards, as cash flow hedges of forecasted transactions. Within the designation documentation at
inception, Takeda documents the risk management objective, nature of the risk being hedged, and relationship between hedging instruments and
hedged risk based on the strategy for undertaking the hedging relationships. At inception and on a quarterly basis, Takeda also assesses whether the
hedging instruments are highly effective in offsetting changes in the fair value or the cash flows of the hedged item.
Cash flow hedges – the effective portion of changes in the fair value of derivatives designated and qualifying as cash flow hedges is recognized in
other comprehensive income. The gain or loss relating to the ineffective portion is recognized immediately in profit or loss. The cumulative gain or
loss that was previously recognized in other comprehensive income is reclassified to profit or loss in the same period when the cash flows of the
hedged items are recognized in profit or loss and in the same line item in the consolidated statements of income. The currency basis spread and the
time value of the foreign currency options are accounted for and presented as hedging cost under other components of equity separately from cash
flow hedges.
Net investment hedges – the gain or loss on hedging instruments is recognized in other comprehensive income. At the time of disposal of the foreign
operations, the cumulative gain or loss recognized in other comprehensive income is reclassified to profit or loss.
Hedge accounting is discontinued when the hedging instrument expires or is sold, terminated or exercised, or when the hedge no longer qualifies for
hedge accounting.
Hedge Accounting - Prior to April 1, 2018
The policy applied prior to April 1, 2018 is similar to that applied subsequent to April 1, 2018. However, for all cash flow hedges, the currency basis
spread was accounted for and presented under cash flow hedges.
Transaction costs of financial liabilities
Transaction costs relating to the financial liabilities of debt issued are recorded against the corresponding debt and amortized to the consolidated
statements of income over the period to the earliest redemption date of the debt, using the effective interest rate method. On extinguishment of the
related debt, any unamortized deferred transaction costs are written off and charged to interest expense in the consolidated statements of income.
Share-based Payments
Takeda has implemented share-based payment programs and provides equity and cash-settled share-based payments.
Equity-settled Share-based Payments
Equity-settled share-based payments are granted based on the service performed by the employees, directors, and senior management. The service
received and the corresponding increase in equity are measured at the fair value of the equity instruments at the grant date. The fair value of the
equity instruments granted to employees, directors, and senior management are recognized as expense over the vesting period of the awards with a
corresponding amount as an increase in equity.
Cash-settled Share-based Payments
Cash-settled share-based payments are granted based on the service performed by the employees, directors, and senior management. The service
received and the corresponding liability are measured at the fair value of the corresponding liability. The fair value of the liability-classified awards
granted to employees, directors, and senior management are recognized as expense over the vesting period of the awards with a corresponding
amount as an increase in liability. Takeda re-measures the fair value of the liability at the end of each reporting period and at the date of settlement,
and recognizes any changes in fair value in profit or loss.
F- 22
Capital
Ordinary Shares
Proceeds from the issuance of ordinary shares by the Company are included in share capital and share premium.
Treasury Shares
When the Company acquires treasury shares, the consideration paid is recognized as a deduction from equity. When the Company sells the treasury
shares, the difference between the carrying amount and the consideration received is recognized in share premium.
4. Operating Segment and Revenue Information
Takeda comprises a single operating segment and is engaged in the research, development, manufacturing and marketing of pharmaceutical products,
over-the-counter ("OTC") medicines and quasi-drug consumer products, and other healthcare products. This is consistent with how the financial
information is viewed in allocating resources, measuring performance, and forecasting future periods by the CEO who is Takeda’s Chief Operating
Decision Maker.
Takeda’s revenue from contracts with customers is comprised of the following:
Sales of pharmaceutical products
Royalty and service income
Total
Geographic Information
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
¥
1,671,911
60,140
1,732,051
¥
¥
1,693,838
76,693
1,770,531
¥
¥
2,026,273
70,951
2,097,224
Takeda’s revenue from contracts with customers is based in the following geographic locations:
JPY (millions)
For the Year Ended March 31
Japan
¥
655,344
United States
520,161
¥
Europe and
Canada
279,693
¥
Russia/ CIS
57,550
¥
¥
580,349
571,016
598,341
828,985
313,723
405,641
68,240
59,741
Latin
America
72,516
75,658
88,115
2017
2018
2019
Asia
Other
¥
112,799
¥
33,988
¥
104,026
105,411
30,194
38,315
Total
1,732,051
1,770,531
2,097,224
Other includes the Middle East, Oceania and Africa.
Takeda’s non-current assets are held in the following geographic locations:
JPY (millions)
As of March 31
2018
2019
Japan
United States
Switzerland
Other
¥
413,457
¥
1,231,051
¥
70,175
¥
902,226
¥
400,342
6,649,357
1,523,527
1,818,875
Total
2,616,909
10,392,101
Non-current assets exclude financial instruments, deferred tax assets and net defined benefit assets. Goodwill recognized as a result of the Shire
acquisition during the year ended March 31, 2019 was allocated to United States, Switzerland and Other.
Information Related to Major Customers
During the year ended March 31, 2017, 2018, and 2019, Medipal Holdings Corporation and its subsidiaries (collectively, “Medipal Group”)
represented more than 10% of Takeda’s sales. The sales to the Medipal Group were 265,646 million JPY, 220,249 million JPY, and 225,962 million
JPY for the years ended March 31, 2017, 2018 and 2019, respectively.
These customers represented an aggregate 49,565 million JPY and 58,965 million JPY of trade receivables as of March 31, 2018 and 2019,
respectively.
F- 23
Other Revenue Information
Contract Balances
JPY (millions)
As of
April 1, 2018
As of
March 31, 2019
Receivables from contracts with customers
Receivables included in trade and other receivables (net of impairment loss allowance) (Note 17)
¥
360,833
¥
657,681
Receivables included in assets held for sale (net of impairment loss allowance)
Contract assets
Unbilled receivables
Contract liabilities
Deferred income (Note 24)
Advance payments
1,277
—
4,321
541
—
4,237
6,819
1,101
The revenue recognized during the year ended March 31, 2019 that was included in the contract liability balance as of April 1, 2018 was 781 million
JPY. The revenue recognized during the year ended March 31, 2019 from performance obligations satisfied (or partially satisfied) in previous periods
was 53,931 million JPY, and primarily relates to royalty income.
Takeda’s contract assets relate to the right to receive consideration where performance was completed based on the contract, and trade receivables are
recognized when the right to receive consideration becomes unconditional. The change during the year was mainly due to business combinations.
Takeda’s contract liabilities primarily relate to out-licensing arrangements where Takeda receives cash consideration prior to the completion of its
performance obligations under the agreements.
Receivables from contracts with customers primarily increased as a result of the acquisition of Shire, upon which 304,720 million JPY of such
receivables were recorded.
Transaction price allocated to the remaining performance obligations
As of
April 1,
2018
Changes
during the
period
As of
March 31,
2019
Duration of the remaining performance obligations
Within a year
After a year but
before 5 years
After 5 years
JPY (millions)
Contract liabilities
¥
4,862
¥
3,058
¥
7,920
¥
4,200
¥
1,015
¥
2,705
F- 24
5.
Other Operating Income and Expenses
JPY (millions)
For the Year Ended March 31
2017
2018
2019
Other operating income:
Change in fair value of contingent consideration liabilities (Note 21)
¥
18,441
¥
— ¥
Gain on sales of property, plant and equipment and investment property
Gain on divestment of business to Teva Takeda Yakuhin (Note 14)
Gain on sale of shares of subsidiaries
Other
Total
Other operating expenses:
Donations and contributions
Restructuring expense (Note 23)
Loss on liquidation of foreign operations
Change in fair value of contingent consideration liabilities (Note 21)
Loss on sale of shares of subsidiaries
Other
Total
762
115,363
—
8,967
18,814
27,481
106,337
16,780
143,533
¥
169,412
¥
159,863
¥
¥
3,763
¥
5,603
¥
54,589
—
—
—
14,529
¥
72,881
¥
44,736
41,465
10,523
—
24,228
126,555
¥
5,966
50,330
30,366
56,625
16,576
3,627
82,962
2,112
—
4,016
10,442
103,159
For the year ended March 31, 2018, the loss on liquidation of foreign operations primarily consists of the realization of cumulative translation loss
recorded in the consolidated statement of income upon the liquidation of certain foreign operations. The gain on the sale of shares of subsidiaries
relates to the sale of shareholding in Wako Pure Chemical Industries, Ltd.
For the year ended March 31, 2019, the gain on sales of property, plant and equipment and investment property primarily relates to the sale of the
former headquarters in Tokyo. The gain on sale of shares of subsidiaries relates to the sale of shareholding in certain real estate properties, including
the former Osaka headquarters, and the gain on the sale of 100% of the shares held in Guangdong Techpool Bio-Pharma Co., Ltd.
F- 25
6.
Finance Income and Expenses
Finance Income:
Interest income
Interest income from financial assets measured at amortized cost
Interest income from financial assets measured at fair value through P&L
Total interest income
Dividend income
Dividend income from financial assets measured at fair value through OCI and disposed of
during the period
Dividend income from financial assets measured at fair value through OCI and held at end
of the period
Dividend income from financial assets measured at fair value through P&L
Total dividend income
Gain on sales of available-for-sale financial assets
Gain on foreign currency exchange, net
Other
Total
Finance Expenses:
Interest expense
Change in fair value of contingent consideration liabilities (Note 21)
Impairment of available-for-sale financial assets
Loss on derivative financial assets
Loss on foreign currency exchange, net
Financing fees for bridge loan for acquisition of Shire
Other
Total
7.
Income Taxes
Income Tax Expenses (Benefit)
The composition of income tax expense (benefit) is as follows:
Current tax expenses
Deferred tax expenses
Total
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
¥
2,019
¥
3,282
3,236
3,638
1,897
1,484
3,165
30,430
—
2,666
6,171
448
6,619
1,353
1,116
145
2,614
—
7,007
603
12,274
¥
39,543
¥
16,843
7,560
¥
10,036
¥
3,693
3,659
5,428
—
—
2,909
2,261
6,657
—
10,279
—
2,695
¥
23,249
¥
31,928
¥
48,158
3,743
—
11,365
—
16,102
3,921
83,289
¥
¥
JPY (millions)
For the Year Ended March 31
2017
60,239
(32,406)
27,833
¥
¥
2018
37,758
(7,261)
30,497
¥
¥
2019
61,606
(75,724)
(14,118)
¥
¥
Current tax expenses include the benefits arising from previously unrecognized tax losses, tax credits, and temporary differences of prior periods.
These effects decreased current tax expenses by 1,563 million JPY, 8,005 million JPY and 10,875 million JPY for the years ended March 31, 2017,
2018 and 2019, respectively.
Deferred tax expenses include the benefits arising from previously unrecognized tax losses, tax credits, and temporary differences of prior periods.
These effects decreased deferred tax expenses by 10,915 million JPY, 2,998 million JPY and 6,975 million JPY for the years ended March 31, 2017,
2018 and 2019, respectively.
F- 26
The Company is mainly subject to income taxes, inhabitant tax, and deductible enterprise tax in Japan. The statutory tax rate calculated based on
these taxes for the years ended March 31, 2017, 2018 and 2019 were 30.8%, 30.8% and 30.6% respectively. The tax law changed during the periods
presented, which resulted in the reduction in the statutory tax rate for the Company.
The following is a reconciliation from the Company's domestic (Japanese) tax rate to the effective tax rate for the year ended March 31:
Company’s domestic (Japanese) tax rate
Non-deductible expenses for tax purposes (1)
Changes in unrecognized deferred tax assets and
deferred tax liabilities (2)
Tax credits
Differences in applicable tax rates of overseas subsidiaries (3)
Changes in tax effects of undistributed profit of
overseas subsidiaries
Effect of changes in applicable tax rates
Tax contingencies (4)
Non-deductible impairment of goodwill
Changes in fair value of contingent consideration
Others
Effective tax rate
Unit: Percentage
2017
2018
2019
30.8
4.7
(5.0)
(6.4)
(7.1)
0.5
(1.8)
3.7
2.3
(3.7)
1.4
19.4
30.8
2.6
(0.6)
(4.7)
(5.4)
0.1
(12.6)
2.7
—
1.7
(0.6)
14.0
30.6
23.2
(61.5)
(13.4)
8.2
7.9
1.9
(10.0)
—
(1.8)
0.0
(14.9)
(1) The 23.2%, impact for the year ended March 31, 2019 includes the impact from intra territory eliminations, the pre-tax effect of which has been
eliminated in arriving at the Company’s consolidated income from continuing operations before income taxes as well as non-deductible transaction
costs related to the Shire acquisition.
(2) The (61.5)% impact for the year ended March 31, 2019 is primarily driven by a capital tax loss related to restructuring of subsidiaries.
(3) The 8.2% impact for the year ended March 31, 2019 is primarily driven by a unitary tax on overseas subsidiaries.
(4) The (10.0)% impact for the year ended March 31, 2019 primarily relates to the tax benefit driven by favorable audit settlements.
In the United States, the Tax Cuts and Jobs Act (“U.S. Tax Reform”) was enacted on December 22, 2017. The federal corporate tax rate was reduced
from 35% to 21% beginning January 1, 2018 under the new tax law. As a consequence of U.S. Tax Reform enactment, Takeda recognized tax benefits
of 27,516 million JPY during the year ended March 31, 2018, primarily from the revaluation of net deferred tax liabilities at lower future tax rates
and the improved recoverability of deferred tax attributes resulting from U.S. Tax Reform enacted federal law changes.
The decrease in Takeda’s effective tax rate from 19.4% to 14.0% between the years ended March 31, 2017 and 2018, was primarily due to a one-time
tax benefit from the enactment of U.S. Tax Reform principally related to the revaluation of net deferred tax liability at a lower enacted tax rate and
improved recoverability of deferred tax attributes resulting from U.S. Tax Reform during the year ended March 31, 2018 (in effect of changes in
applicable tax rates), partially offset by tax benefit from subsidiary capital redemption (in changes in unrecognized deferred tax assets and deferred
tax liabilities) during the prior year that did not occur in the current year.
The decrease in Takeda’s effective tax rate from 14.0% to (14.9)% between the years ended March 31, 2018 and 2019 was primarily due to a one-
time tax benefit from restructuring of subsidiaries (in changes in unrecognized deferred tax assets and deferred tax liabilities) and favorable audit
settlements (in tax contingencies), partially offset by an increase in non-deductible expenses for tax purposes and differences in applicable tax rates of
overseas subsidiaries and the impact of U.S. Tax Reform (in effect of changes in applicable tax rates) during the prior year that did not occur in the
current year.
Deferred Taxes
Deferred tax assets and liabilities reported in the consolidated statements of financial position are as follows:
Deferred tax assets
Deferred tax liabilities
Net deferred tax liabilities
F- 27
JPY (millions)
As of March 31
2018
2019
¥
¥
64,980
¥
88,991
(90,725)
(867,061)
(25,745) ¥
(778,070)
The major items and changes in deferred tax assets and liabilities are as follows:
As of April
1, 2017
Recognized
in Profit or
(Loss)
JPY (millions)
Recognized in
Other
Comprehensive
Income
Acquisitions
through
Business
Combinations
As of
March 31,
2018
Others(1)
Research and development expenses
¥
52,595
¥
(34,007) ¥
— ¥
— ¥
(225) ¥
Inventories
Property, plant and equipment
Intangible assets
Available-for-sale financial assets
Accrued expenses and provisions
Defined benefit plans
Deferred income
Unused tax losses
Tax credits
Investments in subsidiaries and associates
Other
Total
38,452
(33,574)
(254,908)
(28,241)
80,266
4,815
17,562
62,886
29,563
(35,461)
31,617
(6,561)
656
84,254
—
(10,373)
(3,032)
709
(16,114)
9,314
6,762
(24,347)
¥
(34,428) ¥
7,261
¥
—
—
—
4,074
—
(432)
—
—
—
—
(1,570)
2,072
¥
—
—
—
—
—
—
—
—
—
—
—
18
(111)
1,696
89
(1,560)
1,027
(503)
915
(2,456)
89
371
18,363
31,909
(33,029)
(168,958)
(24,078)
68,333
2,378
17,768
47,687
36,421
(28,610)
6,071
— ¥
(650) ¥
(25,745)
As of
April 1,
2018
Recognized in
Profit or
(Loss)
JPY (millions)
Recognized in
Other
Comprehensive
Income
Acquisitions
through
Business
Combinations
As of
March 31,
2019
Others(1)
Research and development expenses
¥
18,363
¥
(5,512) ¥
— ¥
17,605
¥
650
¥
31,106
Inventories
Property, plant and equipment
Intangible assets
Available-for-sale financial assets
Financial assets measured at FVTOCI
Accrued expenses and provisions
Defined benefit plans
Deferred income
Unused tax losses
Tax credits
Investments in subsidiaries and associates
Other
Total
31,909
(33,029)
(168,958)
(24,078)
—
68,333
2,378
17,768
47,687
36,421
(28,610)
6,071
19,628
4,514
47,320
—
—
(3,528)
303
283
30,418
(335)
(20,353)
2,986
—
—
—
—
(1,202)
—
3,241
—
—
—
—
720
(39,308)
(52,036)
(733,472)
—
15
37,472
10,314
6
52,705
38,562
(113,900)
(20,989)
(5,965)
(3,289)
(9,728)
24,078
6,264
(83,840)
(864,838)
—
(28,095)
(29,282)
1,958
104,235
448
(519)
(3,467)
(979)
(1,210)
(1,664)
16,684
17,538
127,343
73,669
(164,073)
(12,876)
¥ (25,745) ¥
75,724
¥
2,759
¥
(803,026) ¥
(27,782) ¥ (778,070)
(1) Other consists primarily of foreign currency translation differences, reclassification of deferred tax assets and liabilities classified as held for sale
and the tax impact of items recorded directly to equity. There was no amount of deferred tax recorded directly to equity for the period ended
March 31, 2018. The aggregate amount of deferred tax related to items recorded directly to equity for the period ended March 31, 2019 caused a
reduction in equity of 1,992 million JPY.
Takeda considers the probability that a portion, or all of the future deductible temporary differences, unused tax losses, or unused tax credits can be
utilized against future taxable profits upon recognition of deferred tax assets. In assessing the recoverability of deferred tax assets, Takeda considers
the scheduled reversal of taxable temporary differences, projected future taxable profits, and tax planning strategies.
Based on the level of historical taxable profits and projected future taxable profits during the periods in which the temporary differences become
deductible, Takeda determined that it is probable that the tax benefits can be utilized.
F- 28
The unused tax losses, deductible temporary differences, and unused tax credits for which deferred tax assets were not recognized are as follows:
Unused tax losses
Deductible temporary differences
Unused tax credits
JPY (millions)
As of March 31
2018
2019
¥
36,878
¥
840,867
11,593
7,954
45,135
6,054
The unused tax losses and unused tax credits for which deferred tax assets were not recognized will expire as follows:
Unused tax losses
Unused tax credits
1st year
2nd year
3rd year
4th year
5th year
After 5th year
Indefinite
Total
Less than 5 years
5 years or more
Indefinite
Total
JPY (millions)
As of March 31
2018
2019
¥
— ¥
92
8,901
505
301
25,189
1,890
¥
36,878
¥
—
1
22,690
163
615
741,044
76,354
840,867
JPY (millions)
As of March 31
2018
2019
¥
¥
3,201
¥
4,383
370
7,954
¥
1,200
4,460
394
6,054
The aggregate amounts of temporary differences associated with investments in subsidiaries for which deferred tax assets were not recognized were
140,647 million JPY and 1,728,537 million JPY as of March 31, 2018 and 2019, respectively.
The aggregate amounts of temporary differences associated with investments in subsidiaries for which deferred tax liabilities were not recognized
were 157,656 million JPY and 2,462,928 million JPY as of March 31, 2018 and 2019, respectively.
F- 29
8.
Earnings per Share
The basis for calculating basic and diluted earnings per share (“EPS”) (attributable to owners) is as follows:
As of March 31
2017
2018
2019
Net profit for the year attributable to owners of the Company:
Net profit for the year attributable to owners of the Company JPY (millions)
Net profit used for calculation of earnings per share JPY (millions)
¥
¥
114,940
114,940
¥
¥
186,886
186,886
¥
¥
Weighted-average number of ordinary shares outstanding during the year (thousands of
shares) [basic]
Dilutive effect (thousands of shares)
781,096
4,792
780,812
5,895
109,126
109,126
961,477
5,420
Weighted-average number of ordinary shares outstanding during the year (thousands of
shares) [diluted]
Earnings per share
Basic (JPY)
Diluted (JPY)
785,888
786,707
966,897
147.15
146.26
239.35
237.56
113.50
112.86
Basic EPS is calculated by dividing the net profit for the year attributable to owners of the Company, with the weighted average number of ordinary
shares outstanding during the year. This calculation excludes the average number of treasury shares. Diluted EPS is calculated by dividing the net
profit for the year attributable to owners of the Company, with the weighted-average number of ordinary shares outstanding during the year plus the
weighted-average number of ordinary shares that would be issued upon conversion of all the dilutive ordinary shares into ordinary shares.
There were 901 thousand shares, such as stock options that are anti-dilutive, not included in the calculation of diluted earnings per share for the year
ended March 31, 2017, and 814 thousand such anti-dilutive shares not included for the year ended March 31, 2019. There were no anti-dilutive shares
for the years ended March 31, 2018.
9.
Other Comprehensive Income (Loss)
Amounts arising during the year, reclassification adjustments to profit or loss, and tax effects for each component of other comprehensive income
(loss) are as follows:
Re-measurement gain or (loss) on defined benefit plans:
Amounts arising during the year
Tax effects
Re-measurement gain or (loss) on defined benefit plans
Exchange differences on translation of foreign operations:
Amounts arising during the year
Reclassification adjustments to profit or (loss)
Before tax effects
Tax effects
Exchange differences on translation of foreign operations
Net changes on revaluation of available-for-sale financial assets
Amounts arising during the year
Reclassification adjustments to profit or (loss)
Before tax effects
Tax effects
Net changes on revaluation of available-for-sale financial assets
F- 30
JPY (millions)
For the Year Ended March 31
2017
2018
2019
23,242
(7,688)
15,554
¥
¥
1,156
(432)
724
¥
¥
(14,906)
3,241
(11,665)
(51,252) ¥
8,125
¥
22
(51,230)
(590)
39,964
48,089
(1,478)
(51,820) ¥
46,611
¥
42,939
(3,134)
39,805
(5,166)
34,639
12,485
¥
24,413
¥
22
12,507
(2,986)
(23,773)
640
4,074
9,521
¥
4,714
¥
—
—
—
—
—
¥
¥
¥
¥
¥
¥
Changes in fair value of financial assets measured at fair value through OCI:
Amounts arising during the year
Tax effects
Changes in fair value of financial assets measured at fair value through OCI
Cash flow hedges:
Amounts arising during the year
Reclassification adjustments to profit or (loss)
Before tax effects
Tax effects
Cash flow hedges
Hedging cost:
Amounts arising during the year
Reclassification adjustments to profit or (loss)
Before tax effects
Tax effects
Hedging cost
Share of other comprehensive income of investments accounted for using the equity
method:
Amounts arising during the year
Reclassification adjustments to profit or (loss)
Before tax effects
Tax effects
Share of other comprehensive income of investments accounted for using the equity
method
Total other comprehensive income (loss) for the year
¥
¥
¥
¥
¥
¥
¥
¥
¥
— ¥
—
— ¥
— ¥
—
— ¥
7,202
(1,202)
6,000
7,254
¥
(1,460) ¥
(418)
6,836
(2,202)
4,240
2,780
(861)
(28,063)
(6,363)
(34,426)
633
4,634
¥
1,919
¥
(33,793)
(321) ¥
3,130
¥
—
(321)
99
(815)
2,315
(709)
(4,088)
(908)
(4,996)
87
(222) ¥
1,606
¥
(4,909)
(38) ¥
295
¥
(101)
—
(38)
—
(38) ¥
87
382
—
382
(22,371) ¥
55,956
¥
¥
7
(94)
—
(94)
(9,822)
F- 31
10.
Property, Plant and Equipment
Acquisition cost
As of April 1, 2017
Additions
Acquisitions through business
combinations
Transfers
Disposals and other decreases
Reclassification to assets held for
sale (Note 19)
Foreign currency translation
differences
Other
Buildings and
structures
Machinery and
vehicles
JPY (millions)
Tools,
furniture, and
fixtures
Land
Construction
in progress
¥515,202
19,778
¥
—
15,741
(864)
(1,830)
630
(328)
¥
384,184
11,327
—
19,184
(8,459)
(2,066)
5,020
(445)
¥
107,408
6,288
¥
69,586
63
—
1,615
(9,564)
(276)
767
313
—
72
(77)
(94)
541
(2)
¥
58,052
37,071
—
(37,382)
(376)
—
626
(307)
Total
1,134,432
74,527
—
(770)
(19,340)
(4,266)
7,584
(769)
As of March 31, 2018
¥
548,329
¥
408,745
¥
106,551
¥
70,089
¥
57,684
¥
1,191,398
Additions
Acquisitions through business
combinations
Transfers
Disposals and other decreases
Reclassification to assets held for
sale (Note 19)
Foreign currency translation
differences
Other
123,099
267,871
42,353
(35,073)
(2,272)
1,596
(4,418)
12,974
244,277
9,511
(23,933)
(167)
(2,611)
(1,698)
7,374
26,909
3,055
(10,132)
(9,784)
(1,271)
(624)
383
46,117
(11,519)
(3,397)
(69)
125
2
44,564
100,724
(55,388)
(374)
—
188,394
685,898
(11,988)
(72,909)
(12,292)
(3,841)
(6,002)
(809)
(7,547)
As of March 31, 2019
¥
941,485
¥
647,098
¥
122,078
¥
101,731
¥
142,560
¥
1,954,952
Accumulated depreciation and
accumulated impairment losses
As of April 1, 2017
Depreciation expenses
Impairment losses
Transfers
Disposals and other decreases
Reclassification to assets held for
sale (Note 19)
Foreign currency translation
differences
Other
As of March 31, 2018
Depreciation expenses
Impairment losses
Transfers
Disposals and other decreases
Reclassification to assets held for
sale (Note 19)
Foreign currency translation
differences
Other
¥
(222,794) ¥
(292,117) ¥
(89,197) ¥
(361) ¥
(2,619) ¥
(607,088)
(19,480)
(13,620)
637
701
525
(774)
106
(21,357)
(6,670)
(454)
5
7,126
846
(3,829)
21
(9)
90
9,268
171
(533)
(108)
—
—
—
—
—
(34)
—
—
(137)
—
—
—
—
—
(47,507)
(14,220)
732
17,095
1,542
(5,170)
19
¥
(254,699) ¥
(309,759) ¥
(86,988) ¥
(395) ¥
(2,756) ¥
(654,597)
(24,261)
(355)
(1,269)
27,045
1,109
1,203
2,249
(29,888)
(9,169)
(151)
374
23,225
168
3,535
1,179
(72)
895
9,953
9,342
831
246
—
—
—
—
—
21
—
—
(43)
—
—
—
9
—
(63,318)
(621)
—
60,223
10,619
5,599
3,674
As of March 31, 2019
¥
(248,978) ¥
(311,317) ¥
(74,962) ¥
(374) ¥
(2,790) ¥
(638,421)
F- 32
Carrying amount
As of April 1, 2017
As of March 31, 2018
As of March 31, 2019
Buildings and
structures
Machinery and
vehicles
Tools,
furniture, and
fixtures
Land
Construction
in progress
¥
292,408
¥
92,067
¥
18,211
¥
69,225
¥
55,433
¥
293,630
692,507
98,986
335,781
19,563
47,116
69,694
101,357
54,928
139,770
Total
527,344
536,801
1,316,531
JPY (millions)
Property, plant and equipment includes assets held under finance leases. The carrying amounts of these assets are as follows:
JPY (millions)
Buildings and
structures
Machinery
and vehicles
Tools,
furniture and
fixtures
As of April 1, 2017
As of March 31, 2018
As of March 31, 2019
¥
61,375
¥
2,702
¥
55,941
179,668
1,523
1,331
Takeda recognized the following impairment losses, which are reflected as follows, in the consolidated statements of income:
Cost of sales
Selling, general and administrative expenses
Research and development expenses
Other operating expenses
Total
JPY (millions)
For the Year Ended March 31
2017
2018
2019
(1,079) ¥
(365) ¥
—
(678)
(4,091)
—
—
(13,855)
(5,848) ¥
(14,220) ¥
¥
¥
494
330
220
(35)
(354)
(41)
(191)
(621)
Impairment loss for the year ended March 31, 2017 was primarily due to the impairment of construction in progress relating to construction of a
facility that was terminated following the decision to discontinue a product to be manufactured at this facility.
Impairment loss for the year ended March 31, 2018 was related primarily to buildings and structures in research equipment which were deemed as
underutilized assets, related to the R&D transformation strategy.
Impairment loss for the year ended March 31, 2019 resulted primarily from facilities for administrative and sales activities in Japan that were
divested in the year ended March 31, 2019.
The carrying amounts of the impaired assets were reduced to the recoverable amounts, which were measured at the fair value less costs of disposal
using values, such as expected sales amounts. This fair value is classified as Level 3 in the fair value hierarchy.
F- 33
11.
Goodwill
Acquisition cost
As of beginning of the year
Acquisitions (Note 31)
Deconsolidation
Foreign currency translation differences
Reclassification to assets held for sale (Note 19)
As of end of the year
Accumulated impairment losses
As of beginning of the year
Deconsolidation
Foreign currency translation differences
As of end of the year
Carrying amount
As of beginning of the year
As of end of the year
Goodwill is allocated to the following groups of cash-generating units (“CGU”):
Prescription drugs sold worldwide
Prescription drugs sold outside of the United States and Japan
Other
Total
JPY (millions)
2018
2019
¥
1,020,471
¥
1,029,291
3,256
(899)
6,512
(49)
3,105,512
(3,899)
30,499
—
1,029,291
¥
4,161,403
(897) ¥
899
(45)
(43) ¥
(43)
40
3
—
1,019,574
¥
1,029,248
1,029,248
4,161,403
JPY (millions)
As of March 31
2018
2019
527,481
¥
3,685,352
429,363
72,404
403,474
72,577
1,029,248
¥
4,161,403
¥
¥
¥
¥
¥
¥
Impairment loss for goodwill is recognized if the recoverable amount of goodwill is less than the carrying amount. The recoverable amount is the
greater of fair value less costs to sell, or value in use. Value in use is calculated by discounting the estimated future cash flows based on a three-year
projection approved by management using an appropriate growth rate and a discount rate. The projection includes assumptions about product
launches, competition from rival products and pricing policy as well as the possibility of generics entering the market and loss of exclusivity. In
setting these assumptions, Takeda considers past experience, external sources of information, knowledge of competitor activity, and industry trends.
The significant assumptions used to calculate the recoverable amount (value in use) are as follows:
Growth Rate
Based on country/market
specific long-term average
growth rate for the CGU
Discount Rate
(Post-tax)
Based on country/market
specific weighted average cost of
capital
Discount Rate
(Pre-tax)
Based on country/market
specific weighted average cost of
capital
1.5% – 2.7%
1.5% – 3.2%
1.3% – 2.8%
4.9% – 13.5%
5.6% – 14.4%
6.1% – 11.8%
7.0% – 16.9%
8.0% – 18.0%
8.8% – 15.5%
March 31, 2017
March 31, 2018
March 31, 2019
The value in use exceeded the relevant carrying amount in each group of CGUs, and a reasonable change in the assumptions would not result in an
impairment.
F- 34
12. Intangible Assets
Acquisition cost
As of April 1, 2017
Additions
Acquisitions through business combinations (Note 31)
Disposals and other decreases
Reclassification to assets held for sale (Note 19)
Deconsolidation
Foreign currency translation differences
As of March 31, 2018
Additions
Acquisitions through business combinations (Note 31)
Disposals and other decreases
Reclassification to assets held for sale (Note 19)
Deconsolidation
Foreign currency translation differences
As of March 31, 2019
Accumulated amortization and
accumulated impairment losses
As of April 1, 2017
Amortization
Impairment losses
Reversal of impairment losses
Disposals and other decreases
Reclassification to assets held for sale (Note 19)
Deconsolidation
Foreign currency translation differences
As of March 31, 2018
Amortization
Impairment losses
Disposals and other decreases
Reclassification to assets held for sale (Note 19)
Deconsolidation
Foreign currency translation differences
As of March 31, 2019
Carrying amount
As of April 1, 2017
As of March 31, 2018
As of March 31, 2019
JPY (millions)
Software
Intangible Assets
Associated with
Products
Other
Total
¥
69,154
¥
1,977,596
¥
23,337
¥
2,070,087
16,934
—
(1,975)
(158)
—
830
32,594
41,764
(4,517)
(2,655)
(2,356)
(21,565)
1
—
(8)
—
—
49,529
41,764
(6,500)
(2,813)
(2,356)
(1,126)
(21,861)
¥
84,785
¥
2,020,861
¥
22,204
¥
2,127,850
¥
¥
26,188
51,722
(2,522)
(120)
(220)
404
29,857
3,910,997
(131)
—
(28,794)
63,581
141
—
(11)
—
(4)
3
56,186
3,962,719
(2,664)
(120)
(29,018)
63,988
160,237
¥
5,996,371
¥
22,333
¥
6,178,941
(45,011) ¥
(951,122) ¥
(10,917) ¥
(1,007,050)
(8,045)
(88)
—
1,242
118
—
13
(126,108)
(19,080)
23,057
2,397
2,079
2,356
15,557
(41)
—
—
6
—
—
1
(134,194)
(19,168)
23,057
3,645
2,197
2,356
15,571
¥
(51,771) ¥
(1,050,864) ¥
(10,951) ¥
(1,113,586)
(13,774)
(53)
2,388
59
153
55
(194,727)
(8,645)
22
—
17,888
(8,325)
(61)
(208,562)
—
6
—
4
23
(8,698)
2,416
59
18,045
(8,247)
(62,943) ¥
(1,244,651) ¥
(10,979) ¥
(1,318,573)
24,143
¥
1,026,474
¥
12,420
¥
1,063,037
33,014
97,294
969,997
4,751,720
11,253
11,354
1,014,264
4,860,368
¥
¥
There were no material internally generated intangible assets recorded in the consolidated statements of financial position.
The intangible assets associated with products are comprised of the following:
F- 35
As of April 1, 2017
As of March 31, 2018
As of March 31, 2019
JPY (millions)
Marketed Products
In-Process R&D
Carrying amount
¥
645,449
¥
381,025
¥
698,329
4,248,285
271,668
503,435
1,026,474
969,997
4,751,720
Marketed products mainly represent license rights associated with commercialized products. These include, but are not limited to, intangible assets
associated with PANTOPRAZOLE acquired through the acquisition of Nycomed, which represent 318,281 million JPY and 253,272 million JPY as of
March 31, 2018 and 2019, respectively, intangible assets associated with ALUNBRIG and ICLUSIG acquired through the acquisition of ARIAD
Pharmaceuticals, Inc., which represent 204,378 million JPY and 192,200 million JPY as of March 31, 2018 and 2019, respectively and TAKHZYRO,
VYVANSE, GAMMAGARD, ADVATE, ADYNOVATE, and REPLAGAL, acquired through the acquisition of Shire, which represent 2,497,460 million
JPY as of March 31, 2019.
The remaining amortization period is 3 to 8 years as of March 31, 2019 for the assets acquired through the acquisition of Nycomed, 8 to 12 years for
the assets acquired through the acquisition of ARIAD Pharmaceuticals, Inc. and 1 to 20 years for the assets acquired through the acquisition of Shire.
In-process R&D mainly represents products in development and license rights obtained in connection with Takeda’s in-licensing and collaboration
agreements. These agreements relate to the right to sell products that are being developed (Note 13). These intangible assets are not subject to amortization.
These include intangible assets associated mainly with ALUNBRIG acquired through the acquisition of ARIAD Pharmaceuticals, Inc., which represent
182,002 million JPY and 189,184 million JPY as of March 31, 2018 and 2019, respectively and with SHP621 budesonide and SHP620 Maribavir acquired
through the acquisition of Shire, which represents 70,796 million JPY as of March 31, 2019.
Impairment
Takeda’s impairment assessment for intangible assets requires a number of significant judgments to be made by management to estimate the recoverable
amount, including the estimated pricing and costs, likelihood of regulatory approval, and the estimated market and Takeda’s share of the market. The
most significant assumption for intangible assets associated with marketed products is the product market share of the therapeutic area and estimated
pricing, whereas the most significant assumption with pre-marketed products and in-process R&D is the probability of regulatory approval. A change
in these assumptions may have a significant impact on the amount, if any, of an impairment charge recorded during a period. For example, negative
results from a clinical trial may change the assumption and result in an impairment. Products in development may be fully impaired when a trial is
unsuccessful and there is no alternative use for the development asset.
Takeda recorded impairment losses of 44,609 million JPY, a reversal of impairment losses 3,889 million JPY (net of impairment losses), and impairment
losses of 8,698 million JPY during the years ended March 31, 2017, 2018, and 2019, respectively. These losses are primarily recognized in amortization
and impairment losses on intangible assets associated with products in the consolidated statement of income.
During the year ended March 31, 2017, Takeda recorded impairment losses of 44,609 million JPY primarily resulting from a decision to terminate
development of certain products and competitive product launches. The recoverable amount of the impaired assets amounted to 45,275 million JPY.
Specifically, during the year ended March 31, 2017, Takeda recorded an impairment loss of 16,003 million JPY due to a decline in expected
profitability of COLCRYS, an impairment loss of 7,889 million JPY due to the termination of development of an oncology product, and an
impairment loss of 3,359 million JPY due to the termination of development of a vaccine product.
During the year ended March 31, 2018, Takeda recorded reversal of a previously recorded impairment losses of 23,057 million JPY mainly related to
COLCRYS based on more favorable sales performance. The recoverable amount of the assets related to the reversal was 49,113 million JPY. This
was offset by impairment losses of 19,168 million JPY primarily resulting from a decision to terminate development of certain products. The
recoverable amount of the impaired assets amounted to 3,185 million JPY.
During the year ended March 31, 2019, Takeda recorded impairment losses of 8,698 million JPY. The recoverable amount of the combined impaired
assets amounted to 29,667 million JPY. The impairment losses primarily resulted from the decision to terminate a collaboration agreement on development
of oncology products (Note 13).
Impairment losses were calculated by deducting the recoverable amount from the carrying amount.
The significant assumptions used to calculate the recoverable amount (value in use) are as follows:
March 31, 2017
March 31, 2018
March 31, 2019
Discount Rate
(Post-tax)
Discount Rate
(Pre-tax)
5.7% - 13.5%
8.3% - 16.9%
6.5% - 14.4%
9.4% - 18.5%
11.0%
14.2%
A part of the recoverable amount was measured at the fair value less costs of disposal (the amount that was expected to be received by selling the
assets). This fair value is classified as Level 3 in the fair value hierarchy.
F- 36
13.
Collaborations and Licensing Arrangements
Takeda is party to certain collaborations, in-licensing agreements and out-licensing arrangements.
Out-licensing agreements
Takeda has entered into various licensing arrangements where it has licensed certain product or intellectual property rights for consideration such as
up-front payments, equity interest of partners, development milestones, sales milestones and/or sales-based royalty payments. The receipt of the
variable considerations related to these substantive milestones is uncertain and contingent on the achievement of certain development milestones or
the achievement of a specified level of annual net sales by the licensee.
Collaborations and in-licensing arrangements
These agreements generally provide for commercialization rights to a product or products being developed by the counterparty, and, in exchange,
often resulted in an up-front payment being paid upon execution of the agreement and resulting an obligation that may require Takeda to make future
development, regulatory approval, or commercial milestone payments as well as sales-based royalty payments. In some of these arrangements,
Takeda and the licensee are both actively involved in the development and commercialization of the licensed product, and have exposure to risks and
rewards that are dependent on its commercial success.
Under the terms of these collaboration and licensing arrangements, Takeda made the following payments during the years ended March 31:
Initial up-front and milestone payments
Acquisition of shares of collaboration and in- licensing partners
JPY (millions)
2017
2018
2019
¥
62,282
¥
2,480
¥
32,594
15,074
29,857
5,994
The following is a description of Takeda’s significant collaborations and in-licensing agreements.
Mersana Therapeutics (“Mersana”)
In March 2014, Takeda entered into an agreement with Mersana related to the development of antibody drug conjugates, which was expanded in
January 2015 and again in February 2016. In January 2019, Takeda and Mersana terminated the partnership. Accordingly, Takeda recognized
impairment loss on intangible assets associated with products of 7,237 million JPY during the year ended March 31, 2019.
GlaxoSmithKline plc. (“GSK”)
In July 2017, Takeda entered into an exclusive licensing agreement with TESARO, Inc. ("TESARO") for the commercialization and clinical
development of Niraparib, a novel poly ADP-ribose polymerase inhibitor. TESARO was acquired by GSK during the year ended March 31, 2019.
The collaboration agreement grants Takeda the right to develop and commercialize all indications in Japan and all indications, except prostate cancer,
in South Korea, Taiwan, Russia and Australia. Under the terms of this agreement, Takeda has made an up-front payment and is required to make
additional milestone payments upon the achievement of certain regulatory and commercial goals. GSK will also be eligible to receive from Takeda
tiered royalties based on a double-digit percentage of net product sales.
Denali Therapeutics (“Denali”)
In January 2018, Takeda entered into a collaboration agreement with Denali to develop and commercialize up to three specified therapeutic product
candidates for neurodegenerative diseases. Each program is directed to a genetically validated target for neurodegenerative disorders, including
Alzheimer’s disease and other indications, and incorporates Denali’s Antibody Transport Vehicle platform for increased exposure of biotherapeutic
products in the brain. Under the terms of the agreement, Takeda made an up-front payment in exchange for certain option rights and the purchase of
Denali equity. In addition, Denali is eligible to receive development and commercial milestone payments. Denali will be responsible for all
development activities and costs prior to Investigational New Drug filing for each of the three programs. Takeda has the option to co-develop and co-
commercialize each of the three programs. If Takeda exercises the option, the parties will then jointly conduct clinical development and share all
costs equally. Denali will lead early clinical development activities and Takeda will lead late-stage clinical development activities. Takeda and Denali
will jointly commercialize the products in the United States and China, and Takeda will have exclusive commercialization rights in all other markets.
The parties will share global profits equally.
Wave Life Sciences Ltd. (“Wave”)
In February 2018, Takeda entered into an agreement with Wave to discover, develop and commercialize nucleic acid therapies for disorders of the
central nervous system (“CNS”). Under the agreement, Takeda has the option to co-develop and co-commercialize programs in areas of Huntington’s
disease (HD), amyotrophic lateral sclerosis (ALS), frontotemporal dementia (FTD) and spinocerebellar ataxia type 3 (SCA3). In addition, Takeda has
the right to license multiple preclinical programs targeting CNS disorders, including Alzheimer’s disease and Parkinson’s disease. Takeda made an
upfront payment and investment in Wave and has the potential to make future payments related to development and commercial milestone payments.
F- 37
Rani Therapeutics LLC (“Rani”)
In January 2019, Takeda acquired a collaboration agreement with Rani to conduct research on the use of the RANI PILL technology for oral delivery
of Factor VIII (FVIII) therapy for patients with hemophilia A. This collaboration agreement was acquired through the acquisition of Shire. The
agreement provides Takeda an exclusive option to negotiate a license to develop and commercialize the technology for delivery of FVIII therapy
following completion of feasibility studies and a 0.84% equity ownership in Rani.
Novimmune S.A. (“Novimmune”)
In January 2019, Takeda acquired a licensing agreement with Novimmune through its acquisition of Shire. The agreement provides Takeda a license
to the exclusive worldwide rights to develop and commercialize a bi-specific antibody for the treatment of hemophilia A and hemophilia A patients
with inhibitors. Under the terms of the agreement, Takeda will develop, and if approved, commercialize the product. Novimmune will be entitled to
receive additional potential milestone payments based on clinical, regulatory and commercial milestones and single-digit royalties.
AB Biosciences Inc. (“AB Biosciences”)
In January 2019, Takeda acquired a licensing agreement with AB Biosciences through its acquisition of Shire. The agreement grants Takeda a license
to exclusive worldwide rights to develop and commercialize a recombinant immunoglobulin product candidate and an exclusive, worldwide license
to AB Bioscience’s intellectual property relating to its pan receptor interacting molecule program. AB Biosciences is eligible to receive contingent
research, development, and commercialization milestone payments and tiered royalty payments.
14.
Investments Accounted for Using the Equity Method
Teva Takeda Pharma
Teva Takeda Pharma Ltd. ("Teva Takeda Pharma") is a business venture of Takeda and Teva Pharmaceutical Industries Ltd. ("Teva") headquartered in
Israel.
On April 1, 2016, Takeda sold its off-patented and long-listed products business in Japan to Teva Takeda Yakuhin Ltd. ("Teva Takeda Yakuhin”), a
subsidiary of Teva Takeda Pharma, and received 49.0% of shares of Teva Takeda Pharma as consideration for the business. The remainder of Teva
Takeda Pharma is owned by a subsidiary of Teva. The long-listed products business had a book value of 3,755 million JPY on the date of disposal.
Takeda has significant influence over Teva Takeda Pharma and has applied the equity method. Takeda accounted for the transaction based on IAS 28
'Investments in Associates and Joint Ventures’. Under this accounting, Takeda recognized a gain for the difference between the fair value
consideration received (shares of Teva Takeda Pharma) and the carrying value of the business to the extent it had disposed of the business and it
deferred the remainder of the gain (49)%. The gain on transfer of business recorded in other operating income for the year ended March 31, 2017 was
115,363 million JPY, which included the gain of 102,899 million JPY recognized at the date of disposal. The remainder of the gain was deferred and
is amortized over 15 years, which is the same period as the intangible assets identified in the purchase price allocation. The amortization of the gain is
recorded in other operating income.
Teva Takeda Pharma, which continues its generics business, and Teva Takeda Yakuhin, which operates the long-listed products business and its
generics business, are jointly engaged in business in Japan. Takeda recognizes revenue for product sales of goods related to its supply of the long-
listed products, to Teva Takeda Yakuhin and service revenue for its distribution using its channel to deliver products including generic products of
Teva Takeda Pharma and Teva Takeda Yakuhin, to healthcare providers.
The summarized consolidated financial information of Teva Takeda Pharma and Teva Takeda Yakuhin is as follows:
Revenue
Net loss for the year
Other comprehensive income (loss)
Total comprehensive loss for the year
Total comprehensive loss for the year (49.0%)
Other
Takeda’s share of loss for the year
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
105,547
¥
103,719
¥
(4,132)
—
(4,132)
(2,025)
(120)
(66,301)
—
(66,301)
(32,487)
(137)
89,686
(87,106)
—
(87,106)
(42,682)
211
¥
(2,145) ¥
(32,624) ¥
(42,471)
F- 38
Non-current assets
Current assets
Non-current liabilities
Current liabilities
Equity
Takeda’s share of equity (49.0%)
Goodwill
Deferred gain
Carrying amount of investments accounted for using the equity method
JPY (millions)
As of March 31
2018
2019
¥
¥
¥
¥
163,979
¥
97,865
(31,901)
(20,119)
209,824
102,814
66,094
(73,554)
¥
¥
95,354
¥
111,379
108,423
(15,615)
(18,695)
185,492
90,891
32,921
(39,881)
83,931
The results of Teva Takeda Pharma and Teva Takeda Yakuhin for the year ended March 31, 2018 included an impairment loss of 104,753 million JPY
of which, 35,725 million JPY represents Takeda’s share. The results for the year ended March 31, 2019 included an impairment loss of 117,890
million JPY, of which 50,183 million JPY represents Takeda’s share. These impairments relate to changes in the business environment such as the
revision of the pharmaceutical pricing system in Japan.
Takeda received dividends of 4,159 million JPY from Teva Takeda Pharma for the year ended March 31, 2018. There were no dividends received
from Teva Takeda Pharma for the year ended March 31, 2019. Teva Takeda Pharma cannot distribute its profits without the consent from the two
venture partners.
Associates that are individually immaterial to Takeda
Financial information for associates, which are individually immaterial to Takeda, is as follows: These amounts are based on the shareholding ratio of
Takeda.
Net profit (loss) for the year
Other comprehensive income (loss)
Total comprehensive income (loss) for the year
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
¥
599
(38)
561
¥
¥
425
382
807
¥
¥
(1,156)
(94)
(1,250)
The carrying amount of the investments in associates, which are individually immaterial to Takeda, is as follows:
Carrying amount of investments accounted for using the equity method
¥
12,595
¥
30,727
JPY (millions)
As of March 31
2018
2019
F- 39
15.
Other Financial Assets
Derivative assets
Investment in convertible notes at FVTPL
Investment in debt securities at FVTPL
Investment in equity instruments at FVTOCI
Available-for-sale financial assets
Restricted deposits
Other
Total
Non-current
Current
JPY (millions)
As of March 31
2018
2019
¥
3,289
¥
—
—
—
169,814
87,381
16,598
277,082
196,436
80,646
¥
¥
¥
¥
¥
¥
8,315
9,865
1,608
168,732
—
15,577
11,420
215,517
192,241
23,276
As of March 31, 2018, available-for-sale financial assets included 163,030 million JPY of investments in public companies. As of March 31, 2019,
equity instruments included 119,907 million JPY of investments in public companies. These are considered Level 1 in the fair value hierarchy as
defined in Note 27. The remainder of the equity instruments primarily relates to investments acquired in connection with collaborations and licensing
agreements (Note 13) and are considered Level 3 investments in the fair value hierarchy.
As of March 31, 2018, the restricted deposits mainly represent cash restricted for the acquisition of TiGenix NV (Note 31). These amounts were
subsequently released following the completion of the acquisition. As of March 31, 2019, the restricted deposits mainly represent amounts related to
Takeda’s business combinations.
16.
Inventories
Finished products and merchandise
Work-in-process
Raw materials and supplies
Total
JPY (millions)
As of March 31
2018
2019
¥
¥
86,254
¥
63,145
63,545
212,944
¥
280,738
544,411
161,595
986,744
The amount of inventory write-offs recognized was 11,621 million JPY, 10,292 million JPY, and 9,321 million JPY for the years ended March 31,
2017, 2018 and 2019 respectively, and were included within cost of sales. Inventory as of March 31, 2019 increased due to the recording of the
acquired inventory at fair value upon the acquisition of Shire (Note 31).
17.
Trade and Other Receivables
Trade receivables
Other receivables
Impairment loss allowance
Total
JPY (millions)
As of March 31
2018
2019
369,652
¥
660,999
59,414
(8,819)
84,226
(3,318)
420,247
¥
741,907
¥
¥
F- 40
18.
Cash and Cash Equivalents
Cash and deposits
Short-term investments
Total
JPY (millions)
As of March 31
2018
2019
¥
¥
243,324
51,198
294,522
¥
¥
462,890
239,203
702,093
19.
Assets and Disposal Groups Held for Sale
Takeda has classified certain assets as held for sale in the consolidated statement of financial position. Non-current assets and disposal groups are
transferred to assets held for sale when it is expected that their carrying amounts will be recovered principally through a sale and the sale is considered
highly probable. The non-current assets and disposal groups held for sale are held at the lower of carrying amount or fair value less costs to sell.
Gains or losses recognized from measuring the disposal groups classified as held for sale at the lower of their carrying amounts or fair value less costs
to sell when assets or disposal groups are classified to held for sale, are recorded as other operating income or expense.
Assets Held for Sale
Buildings and structures
Land
Investments accounted for using the equity method
Total
JPY (millions)
As of March 31
2018
2019
¥
¥
¥
98
65
18
181
¥
—
—
450
450
The assets held for sale as of March 31, 2018 primarily represent buildings and structures that were classified as held for sale during the year then ended
based on management decision to sell this property. No impairment was recorded upon classification of the building as held for sale. These items were
sold during the year ended March 31, 2019. The fair value of the assets is based on valuations by independent appraisers who hold recognized and
relevant professional qualifications in the respective location of assets held for sale. The valuations, which conform to the standards of the location, are
based on market evidence of transaction prices for similar assets.
The assets held for sale as of March 31, 2019 primarily represent an investment accounted for using the equity method in PRA Health Sciences that
were classified as held for sale based on management decision to sell the investment. No impairment was recorded upon classification of the investments
as held for sale. This investment was sold in May 2019. The fair value of the assets is based on expected sales price less costs of disposal.
The fair value of assets held for sale is classified as Level 3 in the fair value hierarchy.
F- 41
Disposal Groups Held for Sale
Property, plant and equipment
Intangible assets
Inventories
Trade and other receivables
Cash and cash equivalents
Other
Total assets
Net defined benefit liabilities
Provisions
Trade and other payables
Other
Total liabilities
JPY (millions)
As of March 31
2018
2019
— ¥
—
1,202
1,466
451
692
3,811
¥
— ¥
1,066
165
1,983
451
58
—
179
629
1,379
2,696
383
—
210
959
3,214
¥
1,552
¥
¥
¥
¥
The disposal groups held for sale as of March 31, 2018, consisted mainly of a group of assets, liabilities, and other comprehensive income related to
Takeda's consolidated subsidiary, Multilab Indústria e Comércio de Produtos Farmacêuticos Ltda., and reclassified as held for sale. The shares of the
subsidiary were sold in July 2018. The fair value of the disposal group is based on the publicly announced sales price less costs of disposal and is
classified as Level 2 in the fair value hierarchy as of March 31, 2018.
The disposal groups held for sales as of March 31, 2019, consisted mainly of a group of assets and liabilities related to Takeda's consolidated subsidiary,
Axcelead Drug Discovery Partners, Inc., and reclassified as held for sale following management decision to sell the subsidiary. The shares of the
subsidiary were sold in April 2019. The fair value of the disposal group is based on the agreed upon sales price with the third party less costs of disposal
and is classified as Level 3 in the fair value hierarchy as of March 31, 2019.
Takeda recorded a loss of 3,213 million JPY on the classification of the disposal group as held for sale for the year ended March 31, 2018. No loss on
the classification was recorded for the year ended March 31, 2019.
Items classified as held for sale at acquisition
There were certain asset and disposal groups that were acquired from Shire with the intention to be sold that were classified as held for sale at the
acquisition date. These relate to the Xiidra®(lifitegrast ophthalmic solution) product which Takeda has subsequently announced a sale agreement for,
as included in Note 33. These also include the research and development program referred to as SHP647 that the European Union had required to be
disposed as a condition to the acquisition of Shire by Takeda.
JPY (millions)
As of March 31
2019
455,340
13,682
7,592
476,614
102,947
78,836
17,810
199,593
¥
¥
¥
¥
Intangible assets
Inventories
Deferred tax assets
Total assets
Deferred tax liabilities
Provisions
Other financial liabilities
Total liabilities
F- 42
20.
Bonds and Loans
Bonds
Short-term loans
Long-term loans
Total
Non-current
Current
The composition of bonds is as follows:
JPY (millions)
Carrying value
Principal Amount in
contractual currency
(millions)
As of
March 31, 2018
As of
March 31, 2019
60,000 JPY
¥
59,967
¥
60,000 JPY
500 USD
1,750 EUR
5,750 EUR
5,500 USD
12,100 USD
1,925 USD
59,944
52,978
—
—
—
—
—
59,992
59,968
55,129
216,717
708,860
605,261
¥
172,889
¥
3,196,365
Instrument
14th Unsecured Straight Bonds
15th Unsecured Straight Bonds
USD Unsecured Senior Notes
2018 EUR Unsecured Senior
Notes – variable rate
2018 EUR Unsecured Senior
Notes – fixed rate
2018 USD Unsecured Senior
Notes – fixed rate
Unsecured Senior Notes
Assumed in Shire Acquisition
Unsecured Senior Notes
Assumed in Shire Acquisition
Total
JPY (millions)
As of March 31
2018
2019
172,889
¥
3,196,365
18
812,755
985,662
985,644
18
¥
¥
¥
500,002
2,054,584
5,750,951
4,766,005
984,946
¥
¥
¥
¥
Interest Rate (%)
Maturity
0.540%
0.704%
2.450%
Jul 2019
Jul 2020
Jan 2022
3 month EURIBOR + margin
(0.550-1.100%)
Nov 2020 - Nov 2022
0.375-3.000%
Nov 2020 - Nov 2030
3.800-5.000%
Nov 2020 - Nov 2028
1,278,490
1.900-3.200%
Sep 2019 - Sep 2026
211,948
2.875%-5.250%
Jun 2020 - Jun 2045
The composition of loans is as follows:
JPY (millions)
Carrying value
Principal Amount in
contractual currency
(millions)
As of
March 31, 2018
As of
March 31, 2019
Interest Rate (%)
Maturity
3 month LIBOR + 0.010%
Jul 2019 - Jul 2020
0.200–0.300%
Apr 2023 - Apr 2026
120,000 JPY ¥
120,000
¥
200,000 JPY
113,500 JPY
1,500 USD
500,000 JPY
7,500 USD
3,700 USD
200,000
113,500
159,255
—
—
—
120,000
200,000
113,500
165,599
500,000
819,482
0.350%
6 month LIBOR + 0.500%
1 month TIBOR + 0.100%
LIBOR + variable margin
(0.750-1.500%)
409,346
6 month LIBOR + 0.600%
Apr 2027
Apr 2027
Jul 2019
Jan 2024
Dec 2025
220,018
226,659
¥
812,773
¥
2,554,586
Instrument
Syndicated Loans 2013
Syndicated Loans 2016
Syndicated Loans 2017
USD Syndicated Loans 2017
Syndicated Loans 2019
USD Syndicated Loans 2019
USD Japan Bank for
International Cooperation 2019
Other
Total
The bonds and loans incurred by Takeda to fund a portion of the Shire Acquisition comprised of the following:
•
2018 EUR Unsecured Notes - variable rate comprised of 1,000 million EUR at 3 month EURIBOR + 0.550% interest maturing in
2020, 750 million EUR at 3 month EURIBOR + 1.100% interest maturing in 2022.
F- 43
•
•
•
•
•
2018 EUR Unsecured Notes - fixed rate comprised of 1,250 million EUR at 0.375% interest maturing in 2020, 1,500 million
EUR at 1.125% interest maturing in 2022, 1,500 million EUR at 2.250% interest maturing in 2026, and 1,500 million EUR at
3.000% interest maturing in 2030.
2018 USD Unsecured Notes - fixed rate comprised of 1,000 million USD at 3.800% annual interest maturing in 2020, 1,250
million USD at 4.000% annual interest maturing in 2021, 1,500 million USD at 4.400% annual interest maturing in 2023, and
1,750 million USD at 5.000% annual interest maturing in 2028.
Syndicated Loans 2019 comprised of a Senior Short-Term Loan Facility agreement with aggregate principal amounts up to
500,000 million JPY at 1 month TIBOR + 0.100% interest maturing in July 2019.
USD Syndicated Loans 2019 comprised of a Term Loan Credit Agreement with aggregate principal amounts up to 7,500 million
USD, out of which 3,500 million USD was made available in Euros. These syndicated loans mature in 2024, and have an interest
rate of LIBOR plus a variable margin based on the public debt rating. As of March 31, 2019, the principal amounts in USD and
EUR were 4,000 million USD and 3,057 million EUR, respectively.
Loan Agreement with the Japan Bank for International Cooperation (the "JBIC Loan") with aggregate principal amount of up to
3,700 million USD. The JBIC loan has interest of 6 month LIBOR + 0.600% interest, and matures in 2025.
The bonds and loans assumed from Shire with the acquisition are mainly comprised of the following:
•
•
•
Shire Unsecured Senior Notes, guaranteed by Takeda Pharmaceuticals Company Limited, comprised of 3,300 million USD at
1.900% interest maturing in 2019, 3,300 million USD at 2.400% interest maturing in 2021, 2,500 million USD at 2.875% interest
maturing in 2023, 3,000 million USD at 3.200% interest maturing in 2026.
Shire Unsecured Senior Notes, guaranteed by Takeda Pharmaceuticals Company Limited, comprised of 405 million USD at
2.875% interest maturing in 2020, 220 million USD at 3.600% interest maturing in 2022, 800 million USD at 4.000% interest
maturing in 2025, and 500 million USD at 5.250% interest maturing in 2045.
Shire Revolving Credit Facilities Agreement – On December 12, 2014, Shire entered into a 2,100 million USD revolving credit
facilities agreement with a number of financial institutions. This agreement was terminated in February 2019.
At their respective times of issuance, Takeda entered into a currency and interest rate swap agreement to hedge the JPY amount for 200 million USD
of the USD Unsecured Senior Notes and 925 million USD of the USD Syndicated Loans 2017. Takeda entered into an interest rate swap agreement to
fix the interest rate for 120,000 million JPY of the Syndicated Loans 2013 and 575 million USD of the USD Syndicated Loans 2017.
As of March 31, 2019, Takeda had borrowing availability of 300,000 million JPY.
The 2018 USD Senior Notes have registration rights that, among other things, require Takeda to file a registration statement with the US Securities
and Exchange Commission for an offer to exchange the 2018 USD Senior Notes for registered notes prior to August 23, 2019. To the extent that this
is not accomplished, Takeda will be required to pay penalty interest until remedied. There are long-term financing agreements that contain various
financial covenants which require Takeda to maintain certain financial ratios and other restrictions including the level of the company’s borrowings.
The most restrictive of these covenants is that profit before tax must not be negative for two consecutive years. Takeda was in compliance with all
such covenants as of March 31, 2019.
21.
Other Financial Liabilities
Derivative liabilities
Finance lease obligations
Contingent consideration liabilities arising from
business combinations
Other
Total
Non-current
Current
JPY (millions)
As of March 31
2018
2019
8,871
¥
53,149
30,569
28,247
120,836
91,223
29,613
¥
¥
¥
8,745
179,411
71,062
23,908
283,126
235,786
47,340
¥
¥
¥
¥
F- 44
Finance lease obligations
The future minimum payments related to the finance lease obligations are as follows:
Within one year
Between one year and five years
More than five years
Total
Less: Future finance charges
Present value of minimum lease payments
Non-current
Current
JPY (millions)
As of March 31
Minimum Lease Payments
Present Value of Minimum
Lease Payments
2018
2019
2018
2019
4,808
¥
6,925
¥
2,127
¥
14,335
80,018
37,738
288,470
4,704
46,318
99,161
¥
333,133
¥
53,149
¥
2,145
9,634
167,632
179,411
46,012
53,149
51,022
2,127
¥
¥
¥
153,722
179,411
177,266
2,145
¥
¥
¥
¥
¥
Financial liabilities associated with contingent consideration arrangements
Financial liabilities associated with contingent consideration arrangements represent consideration related to business combinations or license
agreements that is payable only upon future events such as the achievement of development milestones and sales targets, including pre-existing
contingent consideration arrangements of the companies that are acquired by Takeda. At each reporting date, the fair value of contingent
consideration is re-measured based on risk-adjusted future cash flows discounted using appropriate discount rate.
As of the year ended March 31, 2018, financial liabilities associated with contingent consideration arrangements primarily consists of contingent
consideration related to the performance of the COLCRYS business which was acquired in the acquisition of URL Pharma. Inc. in June 2012.
As of the year ended March 31, 2019, the balance primarily relates to pre-existing contingent consideration arrangements from Shire’s historical
acquisitions.
The pre-existing contingent consideration acquired from Shire through Shire’s historical acquisitions is due upon the achievement of certain
milestones related to the development, regulatory, first commercial sale and other sales milestones of products at various stages of development and
marketing, which could total up to 83,802 million JPY of undiscounted payments over a period of over 20 years. The fair value of the contingent
consideration payable could increase or decrease due to changes in certain assumptions which underpin the fair value measurements. The
assumptions include probability of milestones being achieved.
F- 45
The fair value of financial liabilities associated with contingent consideration arrangements are classified as Level 3 in the fair value hierarchy.
As of the beginning of the year
Additions arising from business combinations (Note 31)
Changes in the fair value during the period
Settled and paid during the period
Settled during the period and reclassified to other payables
Foreign currency translation differences
Other
As of the end of the year
Payment term (undiscounted)
Within one year
Between one and three years
Between three and five years
More than five years
JPY (millions)
For the Year Ended March 31
2018
2019
¥
28,976
¥
3,164
12,784
(12,606)
—
(1,243)
(506)
30,569
52,046
(2,223)
(7,734)
(1,648)
175
(123)
¥
30,569
¥
71,062
JPY (millions)
As of March 31
2018
2019
¥
10,620
¥
18,584
4,641
2,831
17,604
19,470
10,885
54,536
The following sensitivity analysis represents effect on the fair value of financial liabilities associated with contingent consideration arrangements
from changes in major assumptions:
Probability of technical milestones being achieved for Shire's historical contingent
consideration arrangements
Increase by 5%
¥
— ¥
3,204
JPY (millions)
As of March 31
2018
2019
Discount rate
22.
Employee Benefits
Defined Benefit Plans
Decrease by 5%
Increase by 0.5%
Decrease by 0.5%
—
(257)
256
(3,204)
(1,626)
1,626
The Company and some of its subsidiaries have various defined benefit plans such as lump-sum retirement payments plans and defined benefit
pension plans, which define the amount of benefits that an employee will receive on or after retirement, usually based on one or more factors, such as
age, years of employment, compensation, classes, and service.
The Company’s defined benefit plans account for the majority of Takeda’s defined benefit obligations and plan assets.
Defined benefit pension plans
Japan
The Company’s corporate defined benefit pension plan in Japan is a funded defined benefit pension plan, which is regulated by the Defined-Benefit
Corporate Pension Act, one of the Japanese pension laws. Benefits are paid in exchange for services rendered by employees who worked for more
than a specified period, typically three years, considering their years of service and the degree of their contribution to the Company.
The Company’s pension fund (the “Fund”) is an independent entity established in accordance with the Japanese pension laws, and Takeda has an
obligation to make contributions. The Director(s) of the Fund has the fiduciary duty to comply with laws; the directives by the Minister of Health,
Labor and Welfare, and the Director-Generals of Regional Bureaus of Health and Welfare made pursuant to those laws; and the by-laws of the Fund
F- 46
and the decisions made by the Board of Representatives of the Fund. Contributions are also regularly reviewed and adjusted as necessary to the
extent permitted by laws and regulations.
Foreign
Other types of defined benefit pension plans operated by Takeda are generally established and operated in the same manner as described above and in
accordance with local laws and regulations where applicable.
The present value of the defined benefit obligation is calculated annually based on actuarial valuations that are dependent upon a number of
assumptions, including discount rates and future salary (benefit) increases, in accordance with IAS 19 ‘Employee Benefits’. Service costs charged to
operating expense related to defined benefit plans represent the increase in the defined benefit liability arising from pension benefits earned by active
participants in the current period. Takeda is exposed to investment and other experience risks and may need to make additional contributions where it
is estimated that the benefits will not be met from regular contributions, expected investment income, and assets held.
The amounts recognized in the consolidated statements of income and the consolidated statements of financial position are as follows:
Consolidated statements of income
Japan
Foreign
Defined benefit costs
Consolidated statements of financial position
Present value of defined benefit obligations
Fair value of plan assets
Net defined benefit liabilities (assets)
Consolidated statement of financial position
Net defined benefit liabilities
Net defined benefit assets
Net amount of liabilities (assets) recognized in the consolidated statement of financial
position
Present value of defined benefit obligations
Fair value of plan assets
Net defined benefit liabilities (assets)
Consolidated statement of financial position
Net defined benefit liabilities
Net defined benefit assets
Net amount of liabilities (assets) recognized in the consolidated statement of financial
position
JPY (millions)
For the Year Ended March 31
2017
2018
2019
6,779
5,210
11,989
¥
¥
4,582
5,772
10,354
¥
¥
4,621
6,786
11,407
JPY (millions)
As of March 31, 2018
Japan
Foreign
Total
¥
198,686
230,421
(31,735) ¥
99,174
21,207
77,967
¥
¥
297,860
251,628
46,232
9,604
¥
78,007
¥
41,339
40
87,611
41,379
(31,735) ¥
77,967
¥
46,232
JPY (millions)
As of March 31, 2019
Japan
Foreign
Total
¥
198,293
223,191
(24,898) ¥
227,975
80,625
147,350
¥
¥
426,268
303,816
122,452
9,461
¥
147,435
¥
156,896
34,359
85
34,444
(24,898) ¥
147,350
¥
122,452
¥
¥
¥
¥
¥
¥
¥
¥
¥
¥
Net defined benefit assets were included in other non-current assets on the consolidated statements of financial position. Net defined benefit assets
included 771 million JPY in assets held for sale, and net defined benefit liabilities included 383 million JPY in liabilities held for sale as of March 31,
2019, related to disposal groups held for sale (Note 19).
F- 47
Defined benefit obligations
A summary of changes in present value of the defined benefit obligations for the periods presented is as follows:
At beginning of the year
Current service cost
Interest cost
Re-measurement gains and losses of defined benefit plans
From changes in demographic assumptions
From changes in financial assumptions
Experience adjustments
Past service cost
Settlement
Benefits paid
Effect of business combinations and
disposals
Foreign currency translation differences
At end of the year
At beginning of year
Current service cost
Interest cost
Re-measurement gains and losses of defined benefit plans
From changes in demographic assumptions
From changes in financial assumptions
Experience adjustments
Past service cost
Settlement
Benefits paid
Effect of business combinations and
disposals
Foreign currency translation differences
At end of the year
JPY (millions)
For the Year Ended March 31, 2018
Japan
Foreign
Total
¥
217,026
¥
90,424
¥
307,450
4,866
1,424
4,295
1,713
9,161
3,137
3,294
(1,179)
2,115
(3)
466
11
(2,515)
(13,134)
(12,749)
—
782
297
5
2,346
(3,093)
81
3,503
779
763
16
(169)
(16,227)
(12,668)
3,503
¥
198,686
¥
99,174
¥
297,860
JPY (millions)
For the Year Ended March 31, 2019
Japan
Foreign
Total
¥
198,686
¥
99,174
¥
297,860
4,774
1,390
1,499
2,577
301
71
(262)
5,041
2,356
(44)
13,101
(1,301)
—
—
9,815
3,746
1,455
15,678
(1,000)
71
(262)
(11,784)
(5,156)
(16,940)
1,041
—
116,060
(1,256)
117,101
(1,256)
¥
198,293
¥
227,975
¥
426,268
The remaining weighted average duration of the defined benefit obligations was 14.4 years and 15.2 years as of March 31, 2018 and 2019,
respectively.
Significant actuarial assumptions used to determine the present value are as follows:
2018
2019
Japan
Foreign
Japan
Foreign
Discount Rate
Future Salary Increases
0.7%
1.7%
0.6%
1.7%
0.2%
2.7%
0.2%
2.2%
F- 48
A 0.5% change in these actuarial assumptions would affect the present value of defined benefit obligations at the end of the reporting period, while
holding all other assumptions constant, by the amounts shown below:
2018
2019
Japan
Foreign
Japan
Foreign
Plan assets
JPY (millions)
Discount Rate
Future Salary Increases
Change in
assumption
Impact
Change in
assumption
Impact
+0.50 % ¥
(12,250)
+0.50 % ¥
-0.50 %
+0.50 %
-0.50 %
+0.50 %
-0.50 %
+0.50 %
-0.50 %
13,778
(7,371)
8,247
(12,608)
14,193
(19,158)
17,699
-0.50 %
+0.50 %
-0.50 %
+0.50 %
-0.50 %
+0.50 %
-0.50 %
517
(477)
479
(665)
499
(470)
2,745
(3,995)
The defined benefit plans are independent of Takeda and funded only by contributions from Takeda. Takeda's investment policies are designed to secure
the necessary returns in the long-term within acceptable risk levels to ensure payments of pension benefits to eligible participants, including future
participants. The acceptable risk level in the return rate on the plan assets is derived from a detailed study considering the mid- to long-term trends and
the changes in income such as contributions and payments. Based on policies and studies, after consideration of issues such as the expected rate of return
and risks, Takeda formulates a basic asset mix which aims at an optimal portfolio on a long-term basis with the selection of appropriate investment
assets.
A summary of changes in fair value of plan assets for the periods presented is as follows:
Balance at beginning of the year
Interest income on plan assets
Re-measurement of defined benefit plans
Return on plan assets
Contributions by the employer
Settlement
Benefits paid
Effect of business combinations and disposals
Foreign currency translation differences
Balance at end of the year
Takeda expects to contribute 7,770 million JPY to the defined benefit plans for the year ending March 31, 2020.
JPY (millions)
For the Year Ended March 31,
2018
2019
¥
265,031
¥
251,628
1,959
4,813
4,753
(3,564)
(11,507)
(11,225)
1,368
2,225
468
5,706
—
(12,923)
55,133
1,579
¥
251,628
¥
303,816
F- 49
The breakdown of fair value by asset class is as follows:
Equities:
Japan
Foreign
Bonds:
Japan
Foreign
Life insurance company general accounts
Cash and cash equivalent
Investments in trusts
Others
Total plan assets
JPY (millions)
As of March 31
2018
2019
With Quoted
Prices in Active
Markets
No Quoted
Prices in
Active
Markets
With Quoted
Prices in Active
Markets
No Quoted
Prices in
Active
Markets
¥
15,494
¥
2,804
¥
15,025
¥
6,396
58,286
1,568
2,278
—
8,452
—
514
19,157
38,716
68,551
—
—
29,412
20,680
1,040
12,011
—
9,663
—
404
3,444
74,309
16,523
34,250
88,178
—
18,683
9,606
¥
34,702
¥
216,926
¥
58,823
¥
244,993
Equities and bonds with no quoted prices in active markets includes pooled funds that are primarily invested in listed securities on active markets. Life
insurance company general accounts are accounts with guaranteed capital and minimum interest rate, in which life insurance companies manage funds
on a contractual basis.
Defined Contribution Plans
The Company and some of the Company’s subsidiaries offer defined contribution benefit plans.
Benefits of defined contribution plans are linked to contributions paid, the performance of each participant’s chosen investments, and the form in which
participants choose to redeem their benefits. Contributions made into these plans are generally paid into an independently administered fund.
Contributions payable by Takeda for these plans are charged to operating expenses. Takeda has no exposure to investment risks and other experience
risks with regard to defined contribution plans.
The amount of defined contribution costs was 20,897 million JPY, 19,525 million JPY, and 21,068 million JPY for the years ended March 31, 2017,
2018 and 2019, respectively. These amounts include contributions to publicly provided plans.
Other Employee Benefit Expenses
Major employee benefit expenses other than retirement benefits for each fiscal year are as follows:
Salary
Bonuses
Other
The above table does not include severance expenses.
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
226,985
¥
215,256
¥
272,930
68,935
75,949
70,708
81,616
89,439
93,711
F- 50
23.
Provisions
The movements in the provisions are as follows:
As of April 1, 2017
Increases
Decreases (utilized)
Decreases (reversed)
Decreases from deconsolidation
Reclassification to liabilities held for sale
Foreign currency translation differences
As of March 31, 2018
Increases
Acquisitions through business combinations
Decreases (utilized)
Decreases (reversed)
Decreases from deconsolidation
Foreign currency translation differences
As of March 31, 2019
Litigation
(Note 32)
Restructuring
JPY (millions)
Rebates and
Return
Reserves
Other
Total
¥
33,446
¥
27,118
¥
90,870
¥
22,470
¥
3,692
(12,372)
(286)
—
(676)
(622)
5,935
(19,183)
(128)
(133)
—
(993)
310,070
(284,164)
(9,557)
—
—
(5,378)
14,009
(11,579)
(2,045)
(107)
(390)
826
¥
23,182
¥
12,616
¥
101,841
¥
23,184
¥
10,382
29,570
(11,426)
(3,146)
(1,032)
(755)
30,547
14,506
(8,594)
(679)
—
1,285
441,188
217,002
(462,335)
(11,447)
(994)
8,107
13,198
17,912
(10,836)
(3,335)
(295)
(1,549)
173,904
333,706
(327,298)
(12,016)
(240)
(1,066)
(6,167)
160,823
495,315
278,990
(493,191)
(18,607)
(2,321)
7,088
¥
46,775
¥
49,681
¥
293,362
¥
38,279
¥
428,097
The current portion of the provision is 135,796 million JPY, 132,781 million JPY, and 392,733 million JPY as of April 1, 2017,
March 31, 2018 and 2019, respectively. The non-current portion of the provision is 38,108 million JPY, 28,042 million JPY and 35,364
million JPY, as of April 1, 2017, March 31, 2018 and 2019, respectively.
Restructuring
Takeda has various restructuring efforts in place during the years ended March 31, 2017, 2018 and 2019, in connection with the
following:
•
Transform its R&D function – Takeda has commenced various restructuring efforts during the years ended March 31,
2017, 2018 and 2019, in connection with efforts to transform its R&D function and to improve the efficiency of its
operations. These initiatives included consolidation of sites and functions and reduction in workforce.
Integration of Shire - In the year ended March 31, 2019, Takeda commenced various restructuring efforts following the
acquisition of Shire. The integration of Shire includes initiatives to consolidate systems, sites, and functions, and to
optimize the workforce.
Acquired restructuring programs – Takeda acquired various restructuring programs in connection with the Shire
Acquisition. These include Shire program related to completing the integration of Baxalta, Inc., which was acquired by
Shire in June 2016.
Various other efforts to improve the efficiency of its operations and related facilities
•
•
•
A restructuring provision is recorded when Takeda has a detailed formal plan for the restructuring. Takeda records the provision and associated
expenses based on estimated costs associated with the plan. The ultimate cost and the timing of any payments under the plan will be impacted by the
actual timing of the actions and the actions of employees impacted by the restructuring activities. The payments for non-current restructuring
provision are expected to be made within approximately 3 years.
F- 51
Restructuring expenses recorded are as follows:
Cash:
Severance
Consulting fees
Other
Total
Non-Cash:
Depreciation and impairment
Total
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
¥
¥
¥
32,290
¥
6,397
¥
7,271
11,611
51,172
3,417
54,589
¥
¥
¥
7,205
16,528
30,130
14,606
44,736
¥
¥
¥
17,574
19,040
44,906
81,520
1,442
82,962
The other restructuring costs mainly relate to retention and contract termination costs. The other restructuring costs for the year ending March 31, 2019
includes personnel costs of 20,754 million JPY mainly related to retention bonus and salary of employees fully dedicated to restructuring programs.
Rebates and Returns
Takeda has recognized a provision related mainly to sales rebates and returns for products and merchandises, which include sales-linked rebates such
as government health programs in the US. These are expected to be paid out generally within one year. Sales rebates and sales returns are reviewed and
updated monthly or when there is a significant change in its amount.
Other
Other provisions are primarily related to asset retirement obligations, contract termination fees and onerous contracts.
24.
Other Liabilities
Accrued expenses
Deferred income
Other
Total
Non-current
Current
JPY (millions)
As of March 31
2018
2019
¥
¥
¥
¥
231,497
¥
52,527
48,206
332,230
68,300
263,930
¥
¥
¥
406,956
45,431
60,675
513,062
75,174
437,888
Accrued expenses include accrued labor cost of 108,766 million JPY and 163,241 million JPY as of March 31, 2018 and 2019, respectively.
Deferred income includes government grants for the purchase of property, plant and equipment. The grants received were 23,937 million JPY and 21,145
million JPY during the years ended March 31, 2018 and 2019, respectively. The primary government grants relate to funding a portion of Takeda’s
investment in the development and production of new influenza vaccines. Takeda was reimbursed for investments it made in facilities. The grant income
is recognized over the life of the associated assets and is recorded as an offset to the depreciation expense (included in cost of sales, selling, general,
and administrative expenses, and research and development expenses). Deferred income also includes unearned co-promotion fees received in advance
of 21,656 million JPY and 16,756 million JPY as of March 31, 2018 and 2019, respectively. When the co-promotion fees are recognized, they will offset
selling, general and administrative expenses.
F- 52
25.
Trade and Other Payables
Trade payables
Other payables
Total
JPY (millions)
As of March 31
2018
2019
¥
¥
133,705
106,554
240,259
¥
¥
212,348
115,046
327,394
Trade payables relate to expenditures associated with Takeda’s manufacturing and other payables relate to other expenditures associated with its day-
to-day operations.
26.
Equity and Other Equity Items
Authorized shares as of April 1
Outstanding shares:
At April 1
Exercise of stock options
Issuance of shares (Note 31)
At March 31
(Thousands of Shares)
2018
2019
3,500,000
3,500,000
790,521
617
3,550
794,688
794,688
15
770,303
1,565,006
The shares issued by the Company are ordinary shares with no par value that have no restrictions on any rights. The number of treasury shares included
in the above outstanding shares was 9,680 thousand shares, 13,379 thousand shares, and 10,226 thousand shares as of April 1, 2017, March 31, 2018,
and 2019, respectively. The number of treasury shares as of March 31, 2018 and March 31, 2019 includes 13,133 thousand shares and 9,976 thousand
shares, respectively, held by the Employee Stock Ownership Plan ("ESOP") Trust and the Board Incentive Plan ("BIP") Trust. The ESOP and BIP Trust
acquired 246 thousand shares and sold 3,403 thousand shares during the year ended March 31, 2019.
During the year ended March 31, 2018, the Company issued 3,550 thousand shares through third- party allotment to the Master Trust Bank of Japan,
Ltd., which is the trust account for Takeda’s ESOP subsidiary. The issuance of these shares resulted in an increase in share capital of 11,388 million JPY
and share premium of 11,286 million JPY. The Master Trust Bank of Japan is a co-trustee of the ESOP. This issuance was approved by the resolution
of our Board of Directors. These shares were reacquired by the Company from the ESOP trust for distribution of share based compensation awards. The
reacquisition of the shares resulted in an increase in treasury shares of 22,773 million JPY.
During the year ended March 31, 2019, the Company issued 770,303 thousand ordinary shares to fund the acquisition of Shire (Note 31).
Dividends Declared and Paid
April 1, 2016, to March 31, 2017
Q1 2016
Q3 2016
April 1, 2017, to March 31, 2018
Q1 2017
Q3 2017
April 1, 2018, to March 31, 2019
Q1 2018
Q3 2018
JPY (millions)
Total Dividends
Dividends Per
Share JPY
Basis Date
Effective Date
¥
71,112
¥
71,122
71,133
71,165
71,507
71,509
90.00
90.00
90.00
90.00
90.00
90.00
March 31, 2016
June 30, 2016
September 30, 2016
December 1, 2016
March 31, 2017
June 29, 2017
September 30, 2017
December 1, 2017
March 31, 2018
June 29, 2018
September 30, 2018
December 3, 2018
Dividends declared for which the effective date falls in the following fiscal year are as follows:
Dividends Declared
April 1, 2019, to March 31, 2020
Q1 2019
JPY (millions)
Total Dividends
Dividends Per
Share JPY
Basis Date
Effective Date
¥
140,836
¥
90.00 March 31, 2019
June 28, 2019
F- 53
27.
Financial Instruments
Takeda promotes risk management to reduce the financial risks arising from business operations. The principal risks to which Takeda is exposed include
market risk, counterparty credit risk, and liquidity risk caused by changes in the market environment such as fluctuations in the price of foreign currency,
interest rates and market prices of commodities and other financial holdings. Each of these risks are managed in accordance with Takeda’s policies.
Financial Assets and Liabilities
Financial Assets Measured at Fair Value
Other financial assets -
Available-for-sale financial assets
Derivative financial instruments
Other
Total
Financial Assets Not Measured at Fair Value
Other financial assets -
Restricted deposits
Other
Trade and Other Receivables
Cash and cash equivalents
Total
Financial Liabilities Measured at Fair Value
Other financial liabilities -
Contingent considerations
Derivative financial instruments
Total
Financial Liabilities Not Measured at Fair Value
Other financial liabilities -
Finance leases
Other
Trade and Other Payables
Bonds and Loans
Total
JPY (millions)
As of March 31, 2018
Available-
for-sale
financial
assets
Derivative
hedging
instruments
Measured at
fair value
through
profit or loss
Other
Financial
Liabilities
Loans and
Receivables
Total
¥
¥
— ¥
169,814
¥
— ¥
— ¥
— ¥
169,814
—
—
—
—
2,527
—
762
2,070
—
—
3,289
2,070
— ¥
169,814
¥
2,527
¥
2,832
¥
— ¥
175,173
¥
87,381
¥
— ¥
— ¥
— ¥
— ¥
14,528
420,247
294,522
—
—
—
—
—
—
—
—
—
—
—
—
87,381
14,528
420,247
294,522
¥
816,678
¥
— ¥
— ¥
— ¥
— ¥
816,678
¥
¥
¥
¥
— ¥
—
— ¥
— ¥
—
— ¥
3,498
— ¥
3,498
¥
30,569
5,373
35,942
¥
¥
— ¥
30,569
—
8,871
— ¥
39,440
— ¥
— ¥
— ¥
— ¥
53,149
¥
—
—
—
—
—
—
—
—
—
—
—
—
28,247
240,259
985,662
53,149
28,247
240,259
985,662
— ¥
— ¥
— ¥
— ¥ 1,307,317
¥ 1,307,317
F- 54
JPY (millions)
As of March 31, 2019
Measured at
fair value
through other
comprehensive
income
Measured at
fair value
through
profit or loss
Measured at
amortized
cost
Derivative
hedging
instruments
Other
Financial
Liabilities
Total
¥
¥
— ¥
168,732
¥
— ¥
— ¥
— ¥
168,732
—
—
—
—
—
—
—
—
4,590
9,865
1,608
504
3,725
—
—
—
—
—
—
—
8,315
9,865
1,608
504
— ¥
168,732
¥
16,567
¥
3,725
¥
— ¥
189,024
¥
26,493
¥
— ¥
— ¥
— ¥
— ¥
26,493
741,907
702,093
—
—
—
—
—
—
—
—
741,907
702,093
Financial Assets Measured at Fair Value
Other financial assets -
Equity instruments
Derivative financial instruments
Investments in convertible notes
Investments in debt securities
Other
Total
Financial Assets Not Measured at Fair Value
Other financial assets -
Others
Trade and Other Receivables
Cash and cash equivalents
Total
¥ 1,470,493
¥
— ¥
— ¥
— ¥
— ¥ 1,470,493
Financial Liabilities Measured at Fair Value
Other financial liabilities -
Contingent considerations
Derivative financial instruments
Total
Financial Liabilities Not Measured at Fair
Value
Other financial liabilities -
Finance leases
Other
Trade and Other Payables
Bonds and Loans
Total
Fair Value Measurement
¥
¥
¥
¥
— ¥
—
— ¥
— ¥
—
— ¥
71,062
7,120
78,182
¥
¥
— ¥
— ¥
71,062
1,625
—
8,745
1,625
¥
— ¥
79,807
— ¥
— ¥
— ¥
— ¥
179,411
¥
179,411
—
—
—
—
—
—
—
—
—
—
—
—
23,908
327,394
23,908
327,394
5,750,951
5,750,951
— ¥
— ¥
— ¥
— ¥ 6,281,664
¥ 6,281,664
Derivative and non-derivative financial instruments measured at fair value are categorized in the following three-tier fair value hierarchy that reflects
the significance of the inputs in making the measurements. Level 1 is defined as observable inputs, such as quoted prices in active markets for an identical
asset or liability. Level 2 is defined as inputs other than quoted prices in active markets within Level 1 that are directly or indirectly observable. Level
3 is defined as unobservable inputs. Fair value information is not provided for financial instruments, if the carrying amount is a reasonable estimate of
fair value due to the relatively short period of maturity of these instruments.
F- 55
Assets:
Financial assets measured at fair value through profit or loss
Derivatives
Derivatives for which hedge accounting is applied
Available-for-sale financial assets
Total
Liabilities:
Financial liabilities measured at fair value through profit or loss
Derivatives
Contingent considerations arising from business combinations
Derivatives for which hedge accounting is applied
Total
Assets:
Financial assets measured at fair value through profit or loss
Derivatives
Investment in convertible notes
Investment in debt securities
Other
Derivatives for which hedge accounting is applied
Financial assets measured at fair value through OCI
Equity instruments
Total
Liabilities:
JPY (millions)
For the Year Ended March 31, 2018
Level 1
Level 2
Level 3
Total
— ¥
—
163,030
762
¥
— ¥
2,527
34
—
—
163,030
¥
3,323
¥
— ¥
762
2,527
163,064
166,353
— ¥
5,373
¥
— ¥
—
—
—
3,498
30,569
—
— ¥
8,871
¥
30,569
¥
5,373
30,569
3,498
39,440
¥
¥
¥
¥
JPY (millions)
For the Year Ended March 31, 2019
Level 1
Level 2
Level 3
Total
¥
— ¥
4,590
¥
— ¥
—
—
—
—
—
—
—
3,725
9,865
1,608
504
—
119,907
—
48,825
¥
119,907
¥
8,315
¥
60,802
¥
4,590
9,865
1,608
504
3,725
168,732
189,024
Financial liabilities measured at fair value through profit or loss
Derivatives
Contingent considerations arising from business
combinations
Derivative for which hedge accounting is applied
Total
¥
¥
— ¥
7,120
¥
— ¥
7,120
—
—
—
1,625
71,062
—
— ¥
8,745
¥
71,062
¥
71,062
1,625
79,807
For the year ended March 31, 2018, available-for-sale financial assets and other financial assets for which it was difficult to reliably measure the fair
value are excluded from the table. The carrying amounts of such assets as of March 31, 2018 were 6,750 million JPY and 2,070 million JPY
respectively. These assets were primarily unlisted equity investments and the fair value of the investments was difficult to reliably measure as they
are not traded on stock markets.
Valuation Techniques
The fair value of derivatives is measured at quoted prices or quotes obtained from financial institutions, whose significant inputs to the valuation model
used are based on observable market data.
The fair value of the investment in convertible notes is measured using techniques such as the discounted cash flow and option pricing models.
Equity investments and investments in debt securities are not held for trading. If equity instruments or investments in debt securities are quoted in an
active market, the fair value is based on price quotations at the period-end-date. If equity instruments or investments in debt securities are not quoted
F- 56
in an active market, the fair value is calculated utilizing a net asset-book value method or multiples of EBITDA approach based on available information
as of each period-end-date and company comparable. The principle input that is not observable and utilized for the calculation of the fair value of equity
instruments and investments in debt securities classified as Level 3 is the EBITDA rate used for the EBITDA multiples approach, which ranges from
4.6 times to 11.1 times. During the year ended March 31, 2019, a cumulative gain on equity investments of 44,230 million JPY was reclassified from
other comprehensive income to retained earnings upon the disposal of certain equity investments in publicly traded companies. The fair value of these
investments on the dates of disposal was 65,035 million JPY. The investments were disposed of after management’s assessment of these investments
relative to the investment strategy.
Contingent consideration, resulting from business combinations, is valued at fair value at the acquisition date as part of the business combination. When
the contingent consideration meets the definition of a financial liability, it is subsequently re-measured to fair value at each reporting date. The
determination of the fair value is based on models such as scenario-based methods and discounted cash flows. The key assumptions take into consideration
the probability of meeting each performance target, forecasted revenue projections, and the discount factor. The fair value measurement of contingent
considerations arising from business combinations is discussed in Note 21.
The joint venture net written option, included in other Level 3 assets for the year ended March 31, 2019 above is valued at fair value, and
subsequently re-measured to fair value at each reporting date. The determination of the fair value is based on the Monte Carlo Simulation model. The
key assumptions include probability weighting, estimated earnings and assumed market participant discount rates that taken into account for the fair
value.
Transfers between levels
Takeda recognizes transfers between levels of the fair value hierarchy, at the end of the reporting period during which the change has occurred. There
were no transfers among Level 1, Level 2, and Level 3 except transfers from Level 3 to Level 1 recorded in 2018 and 2019. These transfers resulted
from the investments in the companies whose shares were previously not listed on an equity or stock exchange and had no recent observable active
trades in the shares. During the years ended March 31, 2018 and 2019, the companies listed its equity shares on an exchange and are currently
actively traded in the market. As the equity shares have a published price quotation in an active market, the fair value measurement was transferred
from Level 3 to Level 1 on the fair value hierarchy during the years ended March 31, 2018 and March 31, 2019, respectively.
Level 3 fair values
The following table shows a reconciliation from the opening balances to the closing balances for Level 3 financial asset fair values for the year ended
March 31, 2019. There were no Level 3 financial assets reflected in the consolidated financial statements of Takeda for the years ended March 31,
2017 and 2018. The disclosure related to the Level 3 financial liabilities, which are related to contingent considerations arising from business
combinations, are included in Note 21.
Balance as of March 31, 2018
Adoption of IFRS 9
Balance as of April 1, 2018
Additions arising from business combinations
Gain recognized as finance income
Loss recognized as changes in fair value of financial assets measured at fair value through OCI and exchange differences
on translation of foreign operations
Purchases
Sales
Transfers to Level 1
Other
As of March 31, 2019
JPY (millions)
—
47,789
47,789
6,183
587
(4,060)
12,253
(1,844)
(111)
5
60,802
¥
¥
Financial instruments not recorded at fair value
The carrying amount and fair value of financial instruments that are not recorded at fair value in the consolidated statements of financial position are
as follows:
F- 57
Bonds
Long-term loans
Finance leases
JPY (millions) As of March 31
2018
2019
Carrying
Amount
Fair Value
Carrying
Amount
Fair Value
¥
172,889
¥
172,872
¥
3,196,365
¥
3,323,592
812,755
53,149
815,865
53,690
2,054,584
179,411
2,058,929
181,776
Long-term debt is recognized at its amortized cost. The fair value of bonds is measured at quotes obtained from financial institutions whose significant
inputs to the valuation model used are based on observable market data. The fair value of loans and finance leases is measured at the present value of
future cash flows discounted using the applicable market rate on the loans with consideration of the credit risk by each group classified in a specified
period. The fair value of bonds, long-term loans, and finance leases are classified as Level 2 in the fair value hierarchy.
Market Risk
Major market risks to which Takeda is exposed are 1) foreign currency risk, 2) interest rate risk and 3) price fluctuation risk. Financial instruments
affected by market risk include loans and borrowings, deposits, equity investments and derivative financial instruments.
Foreign Currency Risk
Takeda’s exposure to the risk of changes in foreign exchange rates primarily relates to its operations (when revenue or expense is denominated in a
foreign currency) and the Company’s net investments in foreign subsidiaries. The Company manages foreign currency risks in a centralized manner
using derivative financial instruments. The Company's policy does not permit the use of speculative foreign currency financial instruments or derivatives,
and Takeda does not enter into derivative contracts or financial instruments to manage its exposure currency translation risk.
Takeda uses forward exchange contracts, currency swaps, and currency options to hedge individually significant foreign currency transactions. Takeda
has also designated loans and bonds denominated in the US dollar and Euro, including the US dollar and Euro debt instruments used to fund the Shire
Acquisition, as hedges of net investments in foreign operations. As of March 31, 2018, the total fair value of the foreign currency denominated loans
and foreign currency denominated bonds was 61,200 million JPY and 31,930 million JPY, respectively. As of March 31, 2019, the total fair value of
the foreign currency denominated loans and foreign currency denominated bonds was 1,404,031 million JPY and 3,203,040 million JPY, respectively.
Takeda is exposed mainly to foreign currency risks of the US dollar and Euro. A depreciation of the JPY by 5% against the US dollar and Euro would
impact profit or loss by 5,156 million JPY, 12,533 million JPY, and 19,530 million JPY as of March 31, 2017, 2018 and 2019, respectively. These
amounts do not include the effects of foreign currency translation on financial instruments in the functional currency or on assets, liabilities, revenue,
and expenses of foreign operations. This analysis assumes that all other variables, in particular interest rates, remain constant. Takeda's exposure to
foreign currency changes for all other currencies is not material.
Forward exchange contracts:
Selling:
Euro
United States Dollar
Chinese Yuan
Other
Buying:
Euro
United States Dollar
Other
Currency swaps:
Buying:
United States Dollar
JPY (millions)
For the Year Ended March 31, 2018
Contract amount to be settled
in more than one year
Contract Amount
Fair Value
¥
98,198
39,799
20,528
1,854
173,627
9,585
5,105
¥
— ¥
—
—
—
—
—
—
(894)
100
(1,211)
(1)
(964)
(19)
95
124,028
123,993
(1,773)
F- 58
Forward exchange contracts:
Selling:
Euro
United States Dollar
Other
Buying:
Euro
United States Dollar
Currency swaps:
Buying:
United States Dollar
Currency collar options:
Russian Ruble
Brazilian Real
JPY (millions)
For the Year Ended March 31, 2019
Contract amount to be settled
in more than one year
Contract Amount
Fair Value
¥
219,580
¥
— ¥
200,571
722
357,550
227,262
123,993
11,463
13,507
—
—
—
—
544
(2,145)
(2)
(4,156)
3,254
123,959
2,621
—
—
(9)
(15)
The above currency swaps were related to bonds and loans denominated in foreign currency, which the Company designated as hedging instruments
in a cash flow hedges. The cash flow hedge reserve related to the currency swaps were reclassified to profit or loss in the same period as the hedged
expected future cash flows occur.
Interest Rate Risk
Takeda’s exposure to the risk of changes in benchmark interest rates and foreign exchange rate relates primarily to the outstanding borrowings with
floating interest rates. Takeda may use interest and currency swaps that fix the amount of future payments to manage interest and foreign exchange
rate risks through cash flow hedge strategies. The following summarizes interest and cross currency interest rate swaps designated as cash flow
hedges for the periods ended March 31:
2018
2019
JPY (millions)
For the Year Ended March 31
Notional Amount More than One Year
Fair Value
¥
300,938
¥
308,078
300,938
¥
248,078
(970)
2,100
The above swaps are related to the borrowings which the Company designated as hedging instruments in a cash flow hedge.
The following represents interest rate sensitivity analysis for the periods presented. This analysis assumes that all other variables, in particular foreign
currency exchange rates, remain constant.
JPY (millions)
As of March 31, 2018
Interest rate
As of March 31, 2019
Interest rate
+1%
-1%
+1%
-1%
Impact on net profit or loss before tax
¥
— ¥
— ¥
(4,632) ¥
Impact on other comprehensive income (before tax effects)
16,543
(16,543)
14,840
4,632
(14,840)
For the year ended March 31, 2018, there is an immaterial impact on net profit or loss because the amount of interest payments from all the
outstanding borrowings with floating rates are fixed using interest rate swaps. The ineffective portion of the hedges was immaterial.
F- 59
Price Fluctuation Risk Management
Commodity Price Risk
For its business operations, Takeda is exposed to risks from commodity price fluctuations. Takeda manages this risk primarily by utilizing fixed price
contracts, but may also use financial instruments to lock in a fixed price.
Market Price Risk
Market pricing and valuations of Takeda’s fixed-income financial assets and liabilities are impacted by changes in currency rates, interest rates and
credit spreads, which are managed as described above.
For equity instruments, the Company manages the risk of price fluctuations in the instruments by regularly reviewing share prices and financial
positions of the issuers. The analysis shows that if the market price of equity instruments held by Takeda and investments in trusts which hold equity
instruments on behalf of Takeda had increased by 10%, the hypothetical impact on other comprehensive income (before tax effect) would have been
16,303 million JPY and 11,991 million JPY as of March 31, 2018 and 2019 respectively. This analysis assumes that all other variables, in particular
interest rates and foreign currency exchange rates, remain constant.
Derivative Financial Instruments
As described above, Takeda is exposed to effects related to foreign exchange fluctuations in connection with our international business activities that
are denominated in various currencies and Takeda entities that have different functional currencies. Takeda is also exposed to currency and interest
rate fluctuations on our borrowings that we use to finance our business operations and our acquisitions. These borrowings are denominated in various
currencies and may bear interest at variable rates, resulting in the risk related to the currency and interest rate movements.
In order to manage the risk of currency exchange rate and interest rate fluctuations, Takeda may enter into derivative contracts with highly rated
financial institutions. Takeda enters into derivative contracts based our risk management policies, which determine the authority for entering into
such transactions and the transaction limits. The policy, which has been consistently followed, is that financial derivatives be used only for hedging
foreign currency and interest rate exposure and not for speculative purposes.
Takeda generally designates its derivatives as hedges for accounting purposes. In certain instances, Takeda enters into derivative contracts that do not
qualify for hedge accounting but are utilized to manage the underlying risk (‘‘economic hedges’’). Takeda does not use financial instruments for
trading purposes. The Company established guidelines for risk assessment procedures and controls for the use of financial instruments. They include
a clear segregation of duties with regard to execution on one side and administration, accounting and controlling on the other.
Summary of Financial Position and Financial Performance for Derivative and Hedging Activities
The following table details the items designated as hedging instruments as of March 31, 2019:
JPY (millions)
Carrying
Amount –
Assets
Carrying
Amount –
Liabilities
Line Item in the
Statement of Financial
Position where Hedging
Instrument is included
Average Rate
Used for the Fair
Value of the
Hedging
Notional
Cash Flow Hedges
Interest risk
Interest rate swaps
120,000 million JPY
¥
— ¥
Currency and interest risk
Currency and interest rate swaps
1,125 million USD
575 million USD
Net Investment Hedges
Foreign currency denominated
bonds and loans
12,881 million USD
10,540 million EUR
396
3,329
—
—
F- 60
917 Other financial liabilities
— Other financial assets
0.66%
2.83%
708 Other financial assets /
liabilities
109.97 JPY
0.03%
1,425,116 Bonds and loans
1,308,686 Bonds and loans
The following table details the amounts within other components of equity related to items designated as hedged items as of March 31, 2019:
Cash Flow Hedges
Interest risk
Interest rate swaps
Forward interest rate
Currency and interest risk
Currency and interest rate swaps
Currency risk
Hedge related to acquisition
Net Investment Hedges
Foreign currency denominated bonds and loans
JPY (millions)
Balance in cash flow
hedges and exchange
differences on translation
Balance in hedge cost
¥
(362) ¥
33
(109)
3,397
7,969
—
—
1,412
—
—
The following table details the amounts of changes in fair value of hedging instruments recorded in other comprehensive income and the amounts
reclassified from the hedging reserve to profit or loss as of March 31, 2019:
JPY (millions)
Amounts recognized in
OCI
Amounts reclassified to
Goodwill
Change in
Fair Value of
Hedges
Hedging
Costs
Cash Flow
Hedge
Hedging
Costs
Amount reclassified to profit or loss
Cash
Flow
Hedge
Hedging
Costs
Line item in which
reclassification
adjustment is included
¥
(2,177) ¥
— ¥
— ¥
— ¥
845
¥
— Financial expenses
—
7,204
—
627
—
—
—
—
53
— Financial expenses
(7,261)
(908) Financial income and
Financial expenses
(33,090)
(4,715)
35,773
4,715
(8,488)
—
—
—
—
—
—
—
Cash Flow Hedges
Interest risk
Interest rate swaps
Forward interest rate
Currency and interest risk
Currency and interest rate
swaps
Currency risk
Hedge related to
acquisition
Net Investment Hedges
Foreign currency denominated
bonds and loans
The amount relating to the ineffectiveness recorded in profit or loss was immaterial for the years ended March 31, 2018 and 2019. The amount of hedging
gains/losses recorded in other comprehensive income and reclassified to profit or loss as hedged future cash flows were no longer expected to occur
was immaterial for the years ended March 31, 2018 and 2019.
Capital Management
The capital structure of Takeda consists of shareholders’ equity (Note 26), bonds and loans (Note 20), and cash and cash equivalents (Note 18). The
fundamental principles of Takeda’s capital risk management are to build and maintain a steady financial base for the purpose of maintaining soundness
and efficiency of operations and achieving sustainable growth. According to these principles, Takeda conducts capital investment, profit distribution
such as dividends, and repayment of loans based on steady operating cash flows through the development and sale of competitive products. Takeda
balances and monitors its capital structure between debt and equity and adheres to a conservative financial discipline.
Credit Risk
Takeda is exposed to credit risk from its operating activities (primarily trade receivables) and from its financing activities, including deposits with banks
and financial institutions, foreign exchange transactions, and other financial instruments. The maximum exposure to credit risk, without taking into
F- 61
account of any collateral held at the end of the reporting period, is represented by the carrying amount of the financial instruments which is exposed to
credit risk on the consolidated statement of financial position.
Customer Credit Risk
Trade and other receivables are exposed to customer credit risk. Takeda monitors the status of overdue balances, reviews outstanding balances for each
customer and regularly examines the credibility of major customers in accordance with Takeda’s policies for credit management to facilitate the early
evaluation and the reduction of potential credit risks. If necessary, Takeda obtains rights to collateral or guarantees on the receivables.
The following represents the age of trade receivables that are past due but not impaired:
JPY (millions)
Amount Past Due
Total
Within 30
Days
Over 30 Days
but within 60
Days
Over 60 Days
but within 90
Days
Over 90 Days
but within
One Year
Over One
Year
As of March 31, 2018
¥
16,222
¥
6,453
¥
2,243
¥
782
¥
5,042
¥
1,702
The amounts in the above table are net of allowances for doubtful receivables. Takeda has provided loss allowances on trade receivables and other
receivables not past due based on an analysis of credit histories. Takeda establishes loss allowances that represent an estimate of expected losses at
the end of the reporting period.
The following represents the carrying amount of the trade receivables categorized by due date and the analysis of impairment loss allowance as of
March 31, 2019:
Gross carrying amount
Impairment loss allowance
Net carrying amount
Weighted average loss rate
¥
¥
Current
613,062
(2,350)
610,712
0.4%
JPY (millions) except for percentage
Over 30 Days
but within 60
Days
Amount Past Due
Over 60 Days
but within 90
Days
Within 30
Days
¥
17,244
(27)
17,217
0.2%
¥
7,441
(24)
7,417
0.3%
5,968
(99)
5,869
1.7%
¥
Over 90 Days
but within
One Year
14,336
(477)
13,859
3.3%
¥
Over One
Year
¥
2,948
(341)
2,607
11.6%
Total
660,999
(3,318)
657,681
0.5%
Management believes that the unimpaired amounts that are past due are still collectible in full, based on historical payment behavior and extensive
analysis of customer credit risk.
As of March 31, 2019, Takeda has provided loss allowance on trade receivables and other receivables not past due based on an analysis of credit histories.
Loss allowance for trade receivables are measured based on expected credit losses on a collective basis using the simplified approach. However, when
events that have a detrimental impact on the estimated future cash flows such as customers’ deterioration of financial conditions or failure of payment
overdue have occurred, expected credit losses are measured on an individual basis as credit-impaired financial assets. Takeda considers a financial asset
to be in default when the customer is unlikely to pay the obligation in full, without recourse by Takeda to take actions such as realizing collaterals, if
any.
The following is a summary of the change in the loss allowance for trade receivables and other assets for the years ended March 31, 2017 and 2018.
The loss allowance recognized for other than trade receivables is immaterial. Comparative amounts for 2017 and 2018 represent the allowance account
for impairment losses under IAS 39.
At beginning of the year
Increases
Decreases (written off)
Decreases (reversed)
Reclassification to assets held for sale
Foreign currency translation differences
At end of the year
F- 62
JPY (millions)
2017
2018
9,165
2,438
(1,185)
(712)
(40)
67
9,733
¥
¥
9,733
1,946
(1,941)
(1,130)
(45)
262
8,825
¥
¥
The following is a summary of the change in the impairment loss allowance for trade receivables for the year ended March 31, 2019. The impairment
loss allowance recognized for other than trade receivables is immaterial.
At beginning of the year
Increases
Decreases (written off)
Decreases (reversed)
Reclassification to assets held for sale
Foreign currency translation differences
At end of the year
Other Counterparty Credit Risk
¥
¥
JPY (millions)
Bad debt provision
calculated by simplified
approach
Bad debt provision
recognized to credit-
impaired financial asset
¥
3,661
1,305
(2,716)
(942)
(36)
119
¥
5,158
2,243
(5,257)
(208)
—
(9)
Total
8,819
3,548
(7,973)
(1,150)
(36)
110
1,391
¥
1,927
¥
3,318
Cash reserves of the subsidiaries are concentrated mostly with the Company and entities acting as the cash pool leader in the United States and Europe.
These cash reserves are primarily managed exclusively by investments in highly rated short-term bank deposits and bonds of highly rated issuers within
the investment limits determined by reviewing the investment ratings and terms under Takeda’s policies for fund management, resulting in limited credit
risk. Cash reserves, other than those subject to the group cash pooling system, are managed by each consolidated subsidiary in accordance with the
Company’s fund management policies.
For derivatives, Takeda enters into trading contracts only with financial counterparties rated investment grade or higher in order to minimize counterparty
risk.
Liquidity Risk
The Company manages liquidity risk and establishes an adequate management framework for liquidity risk to secure stable short-, mid-, and long-term
funds and sufficient liquidity for operations. Takeda manages liquidity risk by monitoring forecasted cash flows and actual cash flows. In addition,
Takeda has commitment lines with some counterparty financial institutions to manage liquidity risk (Note 20). Takeda strives to maximize the available
liquidity with a combination of liquid short-term investments and committed credit lines with strong rated counterparties. The objective is to maintain
levels in excess of project cash needs to mitigate the risk of contingencies.
The table below presents the balances of financial liabilities by maturity. The total contract amount below reflects cash flows presented on an undiscounted
cash flow basis, including interest expense. The amounts disclosed as of March 31, 2018 and 2019 are undiscounted cash flows using the respective
spot foreign exchange rates as of March 31, 2018 and 2019.
F- 63
Carrying
Amount
Total
Within One
Year
JPY (millions)
Between
One and
Two Years
Between
Two and
Three
Years
Between
Three and
Four Years
Between
Four and
Five Years
More than Five
Years
¥
172,889
¥
179,567
¥
2,050
¥
61,824
¥
61,429
¥
54,264
¥
— ¥
812,773
872,738
5,556
66,611
76,879
6,881
81,882
Trade and other payables
240,259
53,149
8,871
(3,289)
240,259
99,161
6,364
(33,590)
240,259
4,808
5,639
—
5,410
40
(3,049)
(3,383)
—
3,495
(336)
(3,729)
—
2,709
1,021
—
2,721
—
(3,698)
(3,699)
—
634,929
—
80,018
—
(16,032)
As of March 31, 2018
Bonds and loans
Bonds
Loans
Finance leases
Derivative liabilities
Derivative assets
As of March 31, 2019
Bonds and loans
Bonds
Loans
¥
3,196,365
¥
3,790,239
¥
507,158
¥
572,336
¥
625,401
¥
358,700
¥
490,302
¥
1,236,342
2,554,586
2,780,332
603,589
152,453
75,627
190,754
787,720
970,189
Trade and other payables
Finance leases
Derivative liabilities
Derivative assets
327,394
179,411
8,745
(8,315)
327,394
333,133
7,106
(30,902)
327,394
6,925
7,246
(8,090)
—
8,996
(301)
(2,983)
—
9,360
161
—
9,575
—
—
9,807
—
(2,576)
(2,633)
(2,816)
—
288,470
—
(11,804)
Reconciliation of liabilities arising from financing activities
Bonds
Long-term
Loans
Short-term
Loans
JPY (millions)
Finance
Lease
Obligations
Derivative
Assets Used
for Hedge of
Debts
Derivative
Liabilities
Used for
Hedge of
Debts
Total
As of April 1, 2017
¥
179,836
¥
560,000
¥
405,054
¥
58,811
¥
— ¥
— ¥ 1,203,701
Cash flows from financing activities
Net increase (decrease) in short-term
loans
Proceeds from long-term loans
Repayments of long-term loans
Proceeds from bonds
Repayments of bonds
Repayments of obligations under finance
lease
Interest paid
Non-cash items
Foreign exchange movement
Change in fair value
New and amended finance leases
Others
As of March 31, 2018
—
—
—
55,951
(60,000)
—
—
—
(403,931)
337,955
(80,000)
—
—
—
—
—
—
—
—
—
—
—
—
—
—
—
(2,658)
(2,855)
(3,019)
(5,244)
(1,105)
(2,610)
—
—
—
348
—
—
—
—
—
(403,931)
(801)
—
—
—
—
—
—
337,154
(80,000)
56,299
(60,000)
(2,658)
(2,855)
(11,978)
2,226
375
2,251
—
375
2,086
(528)
2,754
—
—
—
—
¥
53,149
¥
(180)
¥
1,953
¥ 1,040,584
—
—
121
—
—
44
¥
172,889
¥
812,755
¥
—
—
—
18
F- 64
Bonds
172,889
Long-term
Loans
812,755
Short-term
Loans
18
JPY (millions)
Derivative
Assets Used
for Hedge of
Debts
Derivative
Liabilities
Used for
Hedge of
Debts
(180)
1,953
Finance
Lease
Obligations
53,149
—
—
1,580,400
—
1,215,526
—
367,319
—
—
—
—
—
—
—
—
—
—
—
(1,741)
(4,643)
1,461,627
4,170
138,674
8,685
—
—
—
—
—
—
Total
1,040,584
367,319
1,215,526
1,580,400
(1,741)
(4,643)
—
—
—
—
—
— 1,613,156
(23,562)
—
—
5,011
¥ 3,196,365
21,955
—
—
178
¥ 2,054,584
¥
(6,009)
—
—
—
500,002
¥
1,281
—
118,037
4,643
179,411
¥
—
(3,149)
—
—
(3,329) ¥
—
(1,245)
—
—
708
(6,335)
(4,394)
118,037
9,832
¥ 5,927,741
As of April 1, 2018
Cash flows from financing activities
Net increase (decrease) in short-term
loans
Proceeds from long-term loans
Proceeds from bonds
Repayments of obligations under
finance lease
Interest paid
Acquisitions through business
combinations
Non-cash items
Foreign exchange movement
Change in fair value
New and amended finance leases
Others
As of March 31, 2019
Others includes increase in debts due to application of amortized cost method.
28.
Share-based Payments
Takeda maintains certain share-based compensation payment plans for the benefit of its directors and certain of its employees. Takeda recorded total
compensation expense related to its share-based payment plans of 17,414 million JPY, 22,172 million JPY, and 18,787 million JPY for the years ended
March 31, 2017, 2018 and 2019, respectively, in its consolidated statements of income.
Equity-settled Plans
Stock Options
Takeda had maintained a stock option plan under which it granted awards to members of the board, corporate officer, and senior management through
the year ended March 31, 2014. There were no stock options granted during the years presented in these financial statements and all previously granted
awards are fully vested. These awards generally vested three years after the grant date. The stock options are exercisable for 10 years after the grant date
for options held by directors and 20 years for options held by corporate officers and senior management. The individual must be either a director of the
Company or an employee of Takeda to exercise the options, unless the individual retired due to the expiration of their term of office, mandatory retirement
or other acceptable reasons.
The total compensation expense recognized related to the stock option was 63 million JPY during the year ended March 31, 2017. There was no
compensation expense during the years ended March 31, 2018 or 2019 as all awards were fully vested.
The following table summarizes the stock option activities:
For the Year Ended March 31
2017
2018
2019
Number of
options
(shares)
Weighted
average
exercise price
(JPY)
Number of
options
(shares)
Weighted
average
exercise price
(JPY)
Number of
options
(shares)
Weighted
average
exercise price
(JPY)
As of beginning of the year
4,258,000
¥
Exercised
As of end of the year
(237,100)
4,020,900
3,920
2,121
4,026
4,020,900
¥
(617,100)
3,403,800
4,026
3,876
4,054
3,403,800
¥
(14,600)
3,389,200
4,054
3,721
4,055
F- 65
All of the stock options were exercisable as of March 31, 2017, 2018, and 2019.
The weighted-average share price at the date of exercise was 4,939 JPY, 5,965 JPY and 4,679 JPY during the year ended March 31, 2017, 2018 and
2019, respectively. The weighted-average exercise price and weighted-average remaining contractual life of the share options outstanding were 4,026
JPY and 15 years, 4,054 JPY and 14 years, and 4,055 JPY and 13 years, as of March 31, 2017, 2018 and 2019, respectively.
Stock Incentive Plans
Takeda has two stock-based incentive compensation plans for its directors and members of senior management, including the following:
Board incentive plan (BIP) -The BIP is a stock-based incentive plan for directors of the Company whereby Restricted Share and Performance Share
awards are granted to the directors. Each award is settled in a single share of stock of the Company. Under the BIP, Restricted Shares vest one third each
year over a three-year period and Performance Shares vest three years from the date of grant. The settlement of the awards is based on stock price,
foreign exchange rates (in countries other than Japan), and company dividends. Performance shares are also based on the achievement of certain
performance criteria, which are established at the grant date, including, among others, accumulated revenue, operating free cash flow, earnings per share
and R&D goals, which are transparent and objective indicators. Takeda, through a wholly owned trust, buys shares of the Company in the market on
the grant date, and uses these shares to settle the awards. The number of shares the individual receives (either through physical settlement or cash) is
based on the achievement of the performance criteria and vesting of the award. The trust settles the awards through the issuance of shares to individuals
in Japan. For individuals outside of Japan the trust sells the share the individual is eligible to receive and pays the cash to the individual.
Employee Stock Ownership Plan (ESOP) - The ESOP is a stock-based incentive plan for senior management whereby awards are granted to the employees.
Each award is settled in a single share of stock of the Company. The vesting of the awards under this plan is the same as the BIP for certain members
of senior management with the remainder of the employees’ awards vesting one third each year over a three-year period. The settlement of the awards
is based on stock price, foreign exchange rates (in countries other than Japan), and company dividends. Performance shares, are also based on the
achievement of certain performance criteria, which are established at the grant date including, among others, accumulated revenue, operating free cash
flow, earnings per share and targeted R&D goals, which are transparent and objective indicators. Takeda, through wholly owned trust, buys shares of
the Company in the market on the grant date and uses these shares to settle the awards. The number of shares the individual receives (either through
physical settlement or cash) is based on the achievement of the performance criteria and vesting of the award. The trust settles the awards through the
issuance of shares to individuals in Japan. For individuals outside of Japan the trust sells the share the individual is eligible to receive and pays cash to
the individual.
The total compensation expense recognized related to these plans was 15,322 million JPY, 18,610 million JPY and 20,084 million JPY during the
years ended March 31, 2017, 2018 and 2019, respectively.
The weighted average fair value of the awards at the grant date is as follows (in JPY):
For the Year Ended March 31
2017
2018
2019
BIP:
Weighted average fair value at grant date
¥
4,664
¥
5,709
¥
ESOP:
Weighted average fair value at grant date
4,438
5,709
4,631
4,678
The grant date fair value was calculated using the Company's share price on the grant date as it was determined to be approximately the same as the
fair value of the awards.
The following table summarizes the award activity related to the stock incentive plans (number of awards):
At beginning of the year
Granted
Forfeited/expired before
vesting
Settled
At end of the year
For the Year Ended March 31
2017
2018
2019
ESOP
4,809,442
4,328,364
(849,886)
(1,816,816)
6,471,104
BIP
281,154
192,818
—
(59,039)
414,933
ESOP
6,471,104
3,944,938
(602,245)
(2,922,035)
6,891,762
BIP
414,933
188,695
—
(170,368)
433,260
ESOP
6,891,762
5,021,627
(781,033)
(3,192,681)
7,939,675
BIP
433,260
252,647
(17,832)
(182,843)
485,232
There were no exercisable shares as of March 31, 2017, 2018, and 2019. The weighted average remaining contractual life of the outstanding awards
was one year as of each year end for both the BIP and the ESOP plans.
F- 66
Liability Settled Awards
Takeda has a phantom stock appreciation rights (PSARs) plan and a restricted stock units (RSUs) plan for certain of its employees. The value of these
awards is linked to share price of the Company and are settled in cash. The total compensation expense recorded associated with these plans was 2,029
million JPY and 3,562 million JPY during the years ended March 31, 2017 and 2018. A reversal of total compensation expense of 1,297 million JPY
was recorded during the year ended March 31, 2019. The total liability reflected in the consolidated statements of financial position as of March 31,
2018 and 2019, is 4,872 million JPY and 2,597 million JPY, respectively.
Phantom stock appreciation rights (PSARs)
The PSARs vest one third each year over a three-year period from the end of the fiscal year during which the awards were granted and can be exercised
for a period of ten years from the end of the fiscal year during which the awards were granted. The awards are settled through a cash payment to the
holder based on the difference between the share price of the Company at the date of exercise, and the share price at the date of grant.
The following table summarizes the award activity related to the PSARs:
For the Year Ended March 31
2017
2018
2019
Number of
PSARs
Weighted Average
Exercise Price
(JPY)
Number of
PSARs
Weighted
Average
Exercise Price
(JPY)
Number of
PSARs
Weighted
Average Exercise
Price
(JPY)
As of beginning of the year
10,257,155
¥
5,063
9,282,080
¥
5,017
4,584,937
¥
Granted
Forfeited before vesting
Exercised
Forfeited/expired after
vesting
As of end of the year
—
—
—
—
—
—
(618,494)
4,706
(4,335,961)
(356,581)
9,282,080
5,012
5,017
(361,182)
4,584,937
—
—
5,072
5,505
4,650
—
—
(214,296)
(195,294)
4,175,347
4,650
—
—
4,428
4,940
4,849
All PSARs were exercisable as of March 31, 2017, 2018, and 2019.
Restricted stock units (RSUs)
The RSUs vest one third each year over a three-year period from the end of the fiscal year during which the awards were granted. The RSUs are
settled upon vesting based on the share price at the vesting date plus any dividends paid on shares during the vesting period. There is no exercise
price payable by the holder.
The following table summarizes the award activity related to the RSUs (number of RSUs):
As of the beginning of the year
Granted
Forfeited/expired before vesting
Settled
As of the end of the year
For the Year Ended March 31
2017
1,220,234
255,116
(148,502)
(878,562)
448,286
2018
2019
448,286
254,710
(82,388)
(222,129)
398,479
398,479
279,436
(92,829)
(183,933)
401,153
There are no exercisable balances as of March 31, 2017, 2018, and 2019. The total intrinsic value of vested cash-settled share-based payments was
2,442 million JPY as of March 31, 2018. There was no intrinsic value of vested cash-settled share-based payments as of March 31, 2019.
29.
Subsidiaries and Associates
The number of consolidated subsidiaries increased by 240 in the year ended March 31, 2019, primarily due to acquisition of Shire and Tigenix and
decreased by 13 primarily due to divestitures including Guangdong Techpool Bio-Pharma Co., Ltd. The number of associates accounted for using the
equity method increased by 7 primarily due to the acquisition of Shire and decreased by 3 primarily due to divestitures.
F- 67
The following is a listing of the Company's consolidated subsidiaries as of March 31, 2019:
Company Name
Takeda Austria GmbH
Baxter AG
Baxalta Innovations GmbH
Takeda Distribuidora Ltda.
Shire Pharma Canada ULC
Takeda (China) Holdings Co., Ltd.
Shire BioScience (Shanghai) Co. Ltd
Takeda Pharmaceutical (China) Company Limited
Takeda Pharma A/S
Takeda France S.A.S.
Shire France S.A.S
Takeda GmbH
Shire Deutschland GmbH
Takeda Ireland Limited
Shire Pharmaceutical Holdings Ireland Limited
Shire Pharmaceuticals International Unlimited Company
Shire Pharmaceuticals Ireland Limited
Shire Acquisitions Investments Ireland Designated Activity Company
Shire Ireland Finance Trading Limited
Takeda Italia S.p.A.
Shire Italia S.p.A.
Takeda Consumer Healthcare Company Limited
Nihon Pharmaceutical Co., Ltd.
Shire Japan KK
Shire plc
Takeda Pharmaceuticals Korea Co., Ltd.
Takeda AS
Takeda Pharmaceuticals Limited Liability Company
Takeda Development Center Asia, Pte. Ltd.
Takeda Vaccines Pte. Ltd.
Shire Pharmaceuticals Iberica S.L.U.
Takeda Pharmaceuticals International AG
Baxalta GmbH
Baxalta Manufacturing S.à r.l.
Baxalta Recombinant S.à r.l
Shire International GmbH
Takeda UK Limited
Takeda Development Centre Europe Ltd.
Shire Pharmaceuticals Limited
Shire Pharmaceutical Development Limited
Takeda Pharmaceuticals International, Inc.
Takeda Pharmaceuticals U.S.A., Inc.
Millennium Pharmaceuticals, Inc.
ARIAD Pharmaceutical, Inc.
Takeda California, Inc.
Takeda Vaccines, Inc.
Takeda Development Center Americas, Inc.
F- 68
Country
Austria
Austria
Austria
Brazil
Canada
China
China
China
Denmark
France
France
Germany
Germany
Ireland
Ireland
Ireland
Ireland
Ireland
Ireland
Italy
Italy
Japan
Japan
Japan
Jersey
Korea
Norway
Russia
Singapore
Singapore
Spain
Switzerland
Switzerland
Switzerland
Switzerland
Switzerland
U.K
U.K
U.K.
U.K.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
Voting Share
Capital Hd
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
87.3%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
Company Name
Baxalta Incorporated
Baxalta US Inc.
Shire Human Genetic Therapies Inc
Shire ViroPharma Incorporated
Shire-NPS Pharmaceuticals, Inc.
Dyax Corp.
Meritage Pharma, Inc.
Shire Development LLC
Shire North American Group Inc.
301 immaterial subsidiaries
Country
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
U.S.A.
Voting Share
Capital Hd
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
100.0%
The following is a listing of the Company's associates accounted for using the equity method as of March 31, 2019:
Company Name
Cerevance, LLC
Teva Takeda Pharma Ltd.
Amato Pharmaceutical Products, Ltd.
16 immaterial associates
30.
Related Party Transactions
Transactions with Affiliates
Country
U.S.A.
Japan
Japan
Voting Share
Capital Hd
27.8%
49.0%
30.0%
Takeda has one major affiliate, Teva Takeda Pharma, to which Takeda sells products and acts as a sales agent. Total transactions with Teva Takeda
Pharma for the years ended March 31, 2018 and 2019 were 18,166 million JPY and 10,380 million JPY, respectively. Balances of receivables and
payables are as follows:
Trade receivables
Other receivables
Other payables
JPY (millions)
As of March 31
2018
2019
¥
4,187
¥
1,507
30,066
2,885
1,892
26,844
The terms and conditions of the related party transactions are entered into on terms consistent with third-party transactions and considering market
prices. In addition, the receivables and payables are settled in cash and consistent with terms of third-party settlements.
There is no outstanding balance of collateral or guarantee. Impairment loss allowances are not recognized for the receivables.
Compensation for Key Management Personnel
Key management personnel are defined as members of the Board and the Chief Financial Officer. The compensation for key management personnel
is as follows:
Basic compensation and bonuses
Share-based compensation (expensed amount)
Retirement benefits
Total
F- 69
JPY (millions)
For the Year Ended March 31
2017
2018
2019
¥
¥
1,478
¥
948
38
2,464
¥
1,332
1,176
26
2,534
2,226
1,305
73
3,604
31.
Business Combinations
Acquisitions during the Year Ended March 31, 2019
Shire plc
On January 8, 2019, Takeda completed the acquisition of 100% of the outstanding shares of Shire plc in a cash and equity transaction valued at 6,213,335
million JPY. Takeda paid $30.33 in cash for each Shire ordinary share and issued either 0.839 of a new share (a "New Takeda Share") or 1.678 American
Depositary Shares (“ADSs”) in Takeda (one ADS equals 0.5 New Takeda Share). Takeda incurred 23,750 million JPY of acquisition related costs, which
were expensed as incurred and recorded in selling, general and administrative expenses. Takeda has entered into several borrowing agreements to fund
the cash portion of the acquisition price (Note 20). Shire was a leading global biotechnology company focused on serving people with rare diseases.
This acquisition creates a global R&D driven biopharmaceutical with an attractive geographic footprint as well as strengthens Takeda’s core therapeutic
areas, bringing together complementary positions in gastroenterology (GI) and neuroscience. Some of the Shire's marketed products include
GAMMAGARD, HYQVIA and TAKHZYRO for Immunology, ADVATE, ADYNOVATE, VONVENDI and FEIBA for Hematology, VYVANSE and
ADDERALL XR for Neuroscience, LIALDA/MEZAVANT and PENTASA for Internal Medicine, ELAPRASE and REPLAGAL for Genetic Diseases. Shire’s
R&D focused on rare diseases.
The total consideration transferred was comprised of the following:
Cash
Takeda equity (770,303,013 shares)
Cash for cash settled awards
Total
JPY (millions)
Amount
¥
¥
3,029,431
3,131,282
52,622
6,213,335
The Company issued 770,303,013 ordinary shares allocated to the former shareholders of Shire as part of the purchase consideration. The issue price
was 4,065 JPY per share, of which 2,032.50 JPY per share is recorded as share capital and the remainder is recorded as share premium. The total increase
in equity was 3,131,282 million JPY, of which 1,565,641 million JPY is recorded as share capital and the remainder is recorded as share premium. The
fair value of the Takeda shares issued as part of the consideration paid was determined based on the trading price of Takeda shares at the opening of the
Tokyo Stock Exchange on the date of acquisition.
The total cash outflow was 2,891,937 million JPY, which represents the initial cash consideration transferred of 3,082,053 million JPY and basis
adjustment of 37,107 million JPY, less cash acquired of 227,223 million JPY.
The following represents the preliminary estimate of the fair value of assets acquired and liabilities assumed:
Cash and cash equivalents
Trade and other receivables
Inventories
Property, plant & equipment
Intangible assets
Assets held for sale
Other assets
Trade and other payables
Provisions
Bonds and loans
Deferred tax liabilities
Liabilities held for sale
Other liabilities
Basis adjustments
Goodwill
Net assets acquired
F- 70
JPY (millions)
Amount
¥
227,223
326,154
825,985
684,487
3,899,298
463,526
103,283
(61,382)
(342,202)
(1,603,199)
(809,667)
(196,294)
(354,139)
(37,107)
3,087,369
¥
6,213,335
Goodwill is calculated as the excess of the consideration transferred over the net assets recognized and represents the expected revenue and cost synergies
of the combined Takeda/Shire group. Goodwill recognized as a result of the acquisition is not deductible for tax purposes (Note 11).
Provisions include 29,570 million JPY associated with amounts payable related to legal proceedings (Note 32). Other liabilities also include pre-existing
contingent consideration related to Shire’s historical acquisitions. The assumed pre-existing contingent consideration is payable mainly upon the
achievement of certain milestones, and the fair value of the potential payments Takeda could be required to make is 52,046 million JPY (Note 21).
The estimated fair values primarily consisting of intangible assets, deferred tax liabilities and goodwill noted above are preliminary and are subject to
change. As Takeda finalizes the fair value of assets acquired and liabilities assumed, additional purchase price adjustments will be recorded during the
measurement period during fiscal year 2019. Fair value estimates are based on a complex series of judgments about future events and uncertainties and
rely heavily on estimates and assumptions. The judgments used to determine the estimated fair value assigned to each class of assets acquired and
liabilities assumed, as well as asset lives, can materially impact the Takeda’s results of operations. The finalization of the purchase accounting assessment
will result in a change in the valuation of assets acquired and liabilities assumed, and may have a material impact on Takeda’s results of operations and
financial position.
Takeda held foreign currency denominated deposits and entered into foreign currency options to hedge foreign currency risks for the acquisition of
Shire, and Takeda applied the hedge accounting to the instruments. Basis adjustment represents accumulated change in fair value of the hedging
instruments recorded in other comprehensive income of 37,107 million JPY that was added to the amount of goodwill at the acquisition date.
Takeda recorded 309,198 million JPY of revenue and 126,068 million JPY of net loss related to the operating results of Shire between the acquisition
date and March 31, 2019.
Pro forma information
The following pro forma financial information presents the combined results of the operations of Takeda and Shire as if the acquisition of Shire had
occurred as of April 1, 2018. The pro forma financial information is not necessarily indicative of what the consolidated results of operations would have
been had the respective acquisitions been completed on April 1, 2018. In addition, the pro forma financial information does not purport to project the
future results of operations of the combined Company.
Revenues
Net loss
JPY (millions)
For the Year Ended March 31, 2019
¥
3,412,468
(90,581)
For the purpose of the pro forma financial information, Shire’s historical financial information has been conformed from U.S. Generally Accepted
Accounting Principles to IFRS, and to Takeda’s accounting policies for material accounting policy differences.
TiGenix NV ("TiGenix")
On April 30, 2018, Takeda made an all cash voluntary public takeover bid for the entire issued ordinary shares, warrants, and ADSs (collectively the
“Securities”) of TiGenix not already owned by Takeda. On June 8, 2018, the Company acquired the Securities tendered in the first acceptance period
for 470.2 million EUR. In response to the takeover bid with the Securities already owned by Takeda, Takeda acquired 90.8% of the voting rights. Takeda
incurred 767 million JPY of acquisition related costs, which were expensed as incurred and recorded in selling, general and administrative expenses.
TiGenix is a biopharmaceutical company which develops novel stem cell therapies for treatment of medical conditions. This acquisition will expand
Takeda's late stage gastroenterology (GI) pipeline with the U.S. rights to Cx601 (darvadstrocel), a suspension of allogeneic expanded adipose-derived
stem cells (eASC) under investigation for the treatment of complex perianal fistulas in patients with non-active/mildly active luminal Crohn’s disease
(CD). Following the 2nd Takeover bid and a squeeze-out ended in July 2018, TiGenix became a wholly owned subsidiary of Takeda.
The total consideration transferred was comprised of the following:
Cash
The ordinary shares of TiGenix already owned by Takeda immediately prior to the acquisition date
Total
JPY (millions)
Amount
¥
¥
67,319
2,684
70,003
The total cash outflow was 66,749 million JPY, which represents the initial cash consideration transferred of 67,319 million JPY and basis adjustment
of 3,381 million JPY, less cash acquired of 3,951 million JPY.
F- 71
The following represents provisional fair value of assets acquired and liabilities assumed:
Intangible assets
Other assets
Deferred tax liabilities
Other liabilities
Basis adjustments
Goodwill
Net assets acquired
JPY (millions)
Amount
¥
¥
63,421
5,541
(8,043)
(5,678)
(3,381)
18,143
70,003
Goodwill comprises increased earnings expected from the future business development. Goodwill is not deductible for tax purposes.
The fair value primarily consisting of intangible assets, deferred tax liabilities and goodwill assumed as of the acquisition date have been recorded
provisionally based on the information available as of March 31, 2019. These amounts are subject to change as the Company is in the process of reviewing
further details of the basis for the fair value measurement. For the year ended March 31, 2019, goodwill at the acquisition date decreased by 1,831
million JPY as a result of the adjustment to the provisional fair value, while other assets and deferred tax liabilities decreased by 253 million JPY and
2,084 million JPY, respectively.
Takeda entered into a forward exchange contract to hedge foreign currency risks for the acquisition of TiGenix, and applied the hedge accounting to the
contract. Basis adjustment represents a fair value of the hedging instrument of 3,381 million JPY that was added to the amount of goodwill at the
acquisition date.
No gains or losses were recognized as a result of remeasurement of fair value of the ordinary shares of TiGenix already owned by Takeda immediately
prior to the acquisition date.
The revenue and net profit of TiGenix for the post-acquisition period, which were recognized in the consolidated financial statements for the year ended
March 31, 2019 were immaterial.
The impact on Takeda’s revenue and net profit for the year ended March 31, 2019 assuming the acquisitions date of TiGenix had been April 1, 2018
was immaterial.
Acquisitions during the Years ended March 31, 2018
During the year ended March 31, 2018, Takeda acquired a business for 28,328 million JPY, which was fully paid in cash.
Acquisitions during the Year Ended March 31, 2017
ARIAD Pharmaceuticals, Inc.
On February 16, 2017, Takeda acquired ARIAD Pharmaceuticals, Inc. (hereinafter referred to as “ARIAD") through a tender offer to purchase all issued
and outstanding shares of common stock in cash. ARIAD was focused on discovering, developing and commercializing precision therapies for patients
with rare cancers. The acquisition of ARIAD is a highly strategic deal as it transforms Takeda’s global oncology portfolio and pipeline by expanding
into solid tumors and reinforcing the existing strength in hematology. Brigatinib (US product name: ALUNBRIG) is a small molecule ALK (anaplastic
lymphoma kinase) inhibitor for non-small cell lung cancer. After the acquisition, Brigatinib was granted marketing authorization by the US Food and
Drug Administration (FDA) in April 2017. ICLUSIG, a treatment for CML (chronic myeloid leukemia) and Philadelphia chromosome positive ALL
(acute lymphoblastic leukemia), is commercialized globally (marketing rights of the product are out-licensed in some certain markets other than the
US). These two targeted and innovative medicines, with cost synergies, are expected to be value drivers for Takeda's oncology business. Additionally,
ARIAD has a robust early stage pipeline, and Takeda will leverage ARIAD's R&D capabilities and platform to generate immediate and long-term growth
in the pharmaceutical business.
F- 72
The following represents fair value of assets acquired, liabilities assumed, purchase consideration transferred:
Intangible assets
Other assets
Deferred tax liabilities
Other liabilities
Goodwill
Net Assets Acquired
The consideration transferred was comprised of the following:
Cash
Debt assumed
Assumption of share-based payment liabilities
Total
Reduced by:
Cash acquired
Deferred consideration
Proceeds from cash flow hedge
Net consideration paid
JPY (millions)
Amount
¥
¥
433,047
43,490
(92,419)
(38,852)
273,627
618,893
JPY (millions)
Amount
¥
¥
531,918
59,155
27,820
618,893
(29,869)
(1,509)
(4,411)
¥
583,104
Goodwill comprises higher earnings expected from the future business development. Goodwill is not deductible for tax purposes.
The fair value of the assets acquired and the liabilities assumed, as of March 31, 2017, was booked provisionally, and allocation of the purchase price
was completed during the year ended March 31, 2018. The purchase price allocation above reflects the fair value, and has been updated from the
provisional amounts. As a result of the adjustments to the provisional fair value, goodwill at the acquisition date decreased by 3,198 million JPY while
other liabilities increased by 2,827 million JPY and intangible assets, other assets and deferred tax liabilities decreased by 2,853 million JPY, 3,114
million JPY and 11,992 million JPY, respectively.
Acquisition-related costs of 3,194 million JPY, which includes agent fee and legal fee arising from the acquisition, were expensed as incurred and
recorded in selling, general and administrative expenses.
Net revenue and net loss of ARIAD during the post-acquisition period, which were recognized in the consolidated statement of income for the year
ended March 31, 2017, were immaterial. The impact on Takeda’s revenue and net profit of ARIAD for the period ended March 31, 2017 assuming the
acquisition date had been as of the beginning of the annual reporting period was immaterial.
In addition to the acquisition of ARIAD, Takeda acquired another business during the year for 6,040 million JPY. The aggregate net cash paid for
acquisitions during the year ended March 31, 2017 was 589,144 million JPY.
32.
Commitments and Contingent Liabilities
Operating Lease
Takeda is the lessee under several operating leases, primarily for office and other facilities, and certain office equipment. Future minimum lease
payments by maturity under non-cancellable operating leases that have initial or remaining lease terms in excess of one year are as follows:
Within one year
Between one and five years
More than five years
Total
F- 73
JPY (millions)
As of March 31
2018
2019
¥
12,053
¥
31,278
33,720
31,172
91,105
111,301
¥
77,051
¥
233,578
Total future minimum sublease payments expected to be received under non-cancellable subleases as of March 31, 2018 and 2019 were 34,482
million JPY and 13,140 million JPY, respectively.
Rent expense for operating lease contracts and sublease income recognized in profit or loss are as follows:
JPY (millions)
For the Year Ended March 31
2018
2019
2017
Rent expense
Sublease income
Total
Purchase commitments
¥
¥
11,758
(109)
11,649
¥
¥
21,384
(2,493)
18,891
¥
¥
27,444
(3,579)
23,865
The amount of contractual commitments for the acquisition of property, plant and equipment was 14,078 million JPY and 33,991 million JPY as of
March 31, 2018 and 2019, respectively.
Irish Revenue Authority assessment
Shire received a tax assessment from the Irish Revenue Authority on November 28, 2018 for 398 million EUR. This assessment relates to a potential
taxable gain from a 1,635 million USD break fee Shire received from AbbVie, Inc. ("AbbVie") in connection with the terminated offer to acquire
Shire made by AbbVie in 2014. Takeda is currently in the appeal process with regards to this assessment as it does not believe a tax liability should
arise from the break fee.
Milestone Payments
As discussed in Note 13, Takeda has certain contractual agreements related to the acquisition of intangible assets that require it to make payments of up
to 517,017 million JPY and 655,531 million JPY as of March 31, 2018 and 2019, respectively. These commitments include development milestone
payments in relation to R&D programs under development and expected maximum commercial milestone payments in relation to launched products.
As for the programs under development, the possibility to meet certain conditions for commercial milestone payments is uncertain and the related
commercial milestone payments were not included in the commitments.
Guarantees
The amount of contingent liabilities related to guarantees was 186 million JPY and 99 million JPY as of March 31, 2018 and 2019, respectively.
These are all related to transactions with financial institutions and are not recognized as financial liabilities in the consolidated statement of financial
position because the possibility of loss from contingent liabilities was remote.
Litigation
Takeda is involved in various legal and administrative proceedings. The most significant matters are described below.
Takeda may become involved in significant legal proceedings for which it is not possible to make a reliable estimate of the expected financial effect, if
any, which may result from ultimate resolution of the proceedings. In these cases, appropriate disclosures about such cases would be included in this
note, but no provision would be made for the cases.
With respect to each of the legal proceedings described below, other than those for which a provision has been made, Takeda is unable to make a reliable
estimate of the expected financial effect at this stage. This is due to a number of factors, including, but not limited to, the stage of proceedings, the
entitlement of parties to appeal a decision, if any, and lack of clarity as to the merits of theories of liability, the merits of Takeda’s defenses, the amount
and recoverability of damages and/or governing law. The Company does not believe that information about the amount sought by the plaintiffs, if that
is known, is, by itself, meaningful in every instance with respect to the outcome of those legal proceedings.
Legal expenses incurred and charges related to legal claims are recorded in selling, general and administrative expenses. Provisions are recorded, after
taking appropriate legal and other specialist advice, where an outflow of resources is considered probable and a reliable estimate can be made of the
likely outcome of the dispute. For certain product liability claims, Takeda will record a provision where there is sufficient history of claims made and
settlements to enable management to make a reliable estimate of the provision required to cover unasserted claims. As of March 31, 2019, Takeda’s
aggregate provisions for legal and other disputes were 46,775 million JPY. The ultimate liability for legal claims may vary from the amounts provided
and is dependent upon the outcome of litigation proceedings, investigations and possible settlement negotiations. Unless otherwise stated below, Takeda
is unable to predict the outcome or duration of these matters at this time.
Takeda’s position could change over time, and, therefore, there can be no assurance that any losses that result from the outcome of any legal proceedings
will not exceed, by a material amount, the amount of the provisions reported in these consolidated financial statement.
F- 74
Certain of the matters discussed below were originally brought against Shire or its subsidiaries prior to Takeda’s acquisition of Shire. Refer to Note 31
on Business Combination for discussion of Takeda’s purchase accounting for the acquisition of Shire.
Product Liability and Related Claims
Pre-clinical and clinical trials are conducted during the development of potential products to determine the safety and efficacy of products for use by
humans following approval by regulatory bodies. Notwithstanding these efforts, when drugs and vaccines are introduced into the marketplace,
unanticipated safety issues may become, or be claimed by some to be, evident. Takeda is currently a defendant in a number of product liability lawsuits
related to its products. For the product liability lawsuits and related claims, other than those for which a provision has been made, Takeda is unable to
make a reliable estimate of the expected financial effect at this stage.
The Company’s principal pending legal and other proceedings are disclosed below. The outcomes of these proceedings are not always predictable and
can be affected by various factors. For those legal and other proceedings for which it is considered at least reasonably possible that a loss has been
incurred, the Company discloses the possible loss or range of possible loss in excess of the recorded loss contingency provision, if any, where such
excess is both material and estimable.
ACTOS
Takeda has been named as a defendant in lawsuits in U.S. federal and state courts in which plaintiffs allege to have developed bladder cancer or other
injuries as a result of taking products containing type 2 diabetes treatment pioglitazone (U.S. brand name ACTOS). Eli Lilly and Company ("Lilly"),
which co-promoted ACTOS in the United States for a period of time, also has been named as a defendant in many of these lawsuits. Under the parties’
co-promotion agreement, Takeda has agreed to defend and indemnify Lilly in the U.S. matters. Outside the U.S., lawsuits and claims have also been
brought by persons claiming similar injuries.
In April 2015, Takeda reached an agreement with the lead plaintiffs’ lawyers that resolved the vast majority of ACTOS product liability lawsuits pending
against Takeda and Lilly in the U.S. The settlement covered all bladder cancer claims pending in any U.S. court as of the date of settlement. Claimants
with unfiled claims in the U.S. represented by counsel as of the date of settlement and within three days thereafter were also eligible to participate. The
settlement became effective when 95% of litigants and claimants opted-in. In connection with this broad settlement, Takeda has paid 2.4 billion USD
(approximately 288 billion JPY) into a qualified settlement fund. Takeda received insurance proceeds totaling approximately 58 billion JPY under various
policies covering product liability claims against Takeda. Takeda also established provisions for the remaining ACTOS claims and lawsuits.
In addition to remaining product liability claims, the following lawsuits have been filed against Takeda by public and private third-party payors, as well
as consumers, seeking damages for alleged economic losses:
A purported nation-wide class action lawsuit has been filed in federal court in California—the Painters’ Fund case—on behalf of third-party payors
and consumers seeking, among other things, reimbursement of monies spent on ACTOS. In April 2018, the court dismissed the Painters’ Fund case.
Plaintiffs appealed.
A purported California class action has been filed in federal court in California asserting claims similar to the Painters’ Fund case.
The States of Mississippi and Louisiana have filed lawsuits against Takeda and Lilly alleging that defendants did not warn about bladder cancer and
other risks of ACTOS. The lawsuits seek reimbursement of the cost of ACTOS, paid by the states on behalf of patients through programs such as
Medicaid, and for medical treatment of patients allegedly injured by ACTOS, attorneys’ fees and expenses, and punitive damages. The court granted
Takeda’s motion to dismiss the Louisiana case. The decision has been appealed. In November 2018, Takeda and Lilly agreed to settle the lawsuit brought
by the State of Mississippi. The lawsuit brought by the State of Louisiana remains pending.
Proton Pump Inhibitor (“PPI”) Related Claims
As of June 10, 2019 approximately 6,000 product liability lawsuits involving PREVACID and DEXILANT have been filed against Takeda in U.S.
federal and state courts. The federal lawsuits are consolidated for pre-trial proceedings in a multi-district litigation in federal court in New Jersey. The
plaintiffs in these cases allege they developed kidney injuries as a result of taking PREVACID and/or DEXILANT, and that Takeda failed to adequately
warn them of this potential risk. It remains unclear how many of the plaintiffs actually took PREVACID and/or DEXILANT. Similar cases are pending
against other manufacturers of drugs in the same PPI class as Takeda’s products, including AstraZeneca plc (“AstraZeneca”), Procter & Gamble Company
(“Procter & Gamble”) and Pfizer Inc. (“Pfizer”). Outside the U.S., three proposed class actions have been filed in three provinces in Canada (Quebec,
Ontario, and Saskatchewan). The defendants in these actions include Takeda, AstraZeneca, Janssen Pharmaceutical Companies (“Janssen”) and several
generic manufacturers. It is unclear how many additional actions, if any, may be filed against Takeda in the U.S., Canada or elsewhere.
ELAPRASE
In 2014, Shire’s Brazilian affiliate, Shire Farmaceutica Brasil Ltda, was served with a lawsuit brought by the State of Sao Paulo where the Brazilian
Public Attorney’s office has intervened alleging that Shire would be obligated to supply ELAPRASE for an indefinite period at no cost to patients who
participated in ELAPRASE clinical trials in Brazil, and seeking recoupment to the Brazilian government for amounts paid on behalf of these patients
to date, and moral damages associated with these claims.
F- 75
On May 6, 2016, the trial court judge ruled on the case and dismissed all the claims under the class action, which was appealed. On February 20, 2017,
the Court of Appeals in Sao Paulo issued a decision upholding the decision rendered by the lower court judge, dismissing, therefore, all the claims under
the class action. On July 12, 2017, the Public Prosecutor filed an appeal addressed to the Supreme Court. On October 10, 2017, the State of Sao Paulo
filed appeals addressed to the Superior Court of Justice and to the Supreme Court. On November 13, 2017, Shire submitted its answers to the
aforementioned appeals. On July 3, 2018 the President of Sao Paulo Court of Appeals issued a decision denying the remittance of all appeals to the
Superior Courts. Against such decision, both the State (on August 23, 2018) and the Public Prosecutor (on October 3, 2018) filed an appeal. By virtue
of such appeal, the case records were remitted to the Superior Court of Justice on February 27, 2019. Takeda is currently waiting the assignment of the
case to one of the Justices of the Superior Court of Justice.
Intellectual property
Intellectual property claims include challenges to the validity and enforceability of Takeda’s patents on various products or processes as well as
assertions of non-infringement of those patents. A loss in any of these cases could result in loss of patent protection for the product at issue. The
consequences of any such loss could be a significant decrease in sales of that product and could materially affect future results of operations for
Takeda.
PREVACID
In January 2018, Takeda received notice from Zydus Pharmaceuticals (USA) Inc. ("Zydus") that it has amended its application for a generic version of
SoluTab. In response, Takeda filed a patent infringement lawsuit against Zydus and in response, Zydus filed a counterclaim asserting that Takeda’s
challenge of Zydus’ abbreviated new drug application (“ANDA”) product violates antitrust laws. Takeda believes the counterclaim is without merit.
In June 2009, Apotex Pharmaceuticals Inc. ("Apotex") filed a lawsuit in Toronto, Canada, against Takeda and Abbott Laboratories ("Abbott") seeking
alleged damages for delayed market entry of its generic lansoprazole capsules due to a prior patent infringement lawsuit against Apotex. Previously,
Abbott and Takeda filed a patent infringement lawsuit against Apotex in response to Apotex’s regulatory submission to the Canadian Minister of Health
seeking permission to market generic lansoprazole capsules before the expiration of various Canadian patents relating to this drug. In January 2019, the
parties settled the lawsuit.
PANTOPRAZOLE
On January 15, 2016, Mylan Inc. ("Mylan") filed a suit at the Federal Court against Takeda claiming damages as a result of the dismissal of Takeda´s
previous PM(NOC) proceeding against Mylan. Mylan claimed damages due to being held-off the market with its generic pantoprazole magnesium
product during the time period of June 27, 2013 until June 15, 2015. The parties settled the lawsuit in May 2018.
AMITIZA
In March 2017, Sucampo Pharmaceuticals, Inc. ("Sucampo") (Takeda’s licensor) received a paragraph IV certification directed to AMITIZA from Amneal
Pharmaceuticals, and in August 2017 received a paragraph IV certification directed to AMITIZA from Teva Pharmaceutical Industries Ltd. ("Teva").
These parties contend that the patents listed in FDA’s Orange Book for AMITIZA are invalid and/or not infringed by their ANDA product. In response,
Sucampo and Takeda filed a patent infringement lawsuit against the parties. Patent litigation against other ANDA filers for AMITIZA were previously
settled, and patent litigation against Amneal Pharmaceuticals and Teva was settled in June 2018.
TRINTELLIX
Takeda has received notices from sixteen generic pharmaceutical companies that they have submitted ANDAs with paragraph IV certifications seeking
to sell generic versions of TRINTELLIX. To date, at least four generic companies are challenging the patents covering the compound, vortioxetine,
which expire in 2026. Takeda filed patent infringement lawsuits against the ANDA filers in federal court in Delaware.
ENTYVIO
F. Hoffmann-La Roche, Ltd. ("Roche") has filed patent infringement lawsuits against Takeda in Germany and Italy alleging that ENTYVIO infringes
a Roche patent issued in Germany and Italy. Takeda is vigorously defending these lawsuits. Additionally, Takeda has filed a lawsuit in the U.K. seeking
nullification of Roche’s patent in the U.K.
MYDAYIS
On October 12, 2017, Shire was notified that Teva Pharmaceuticals USA, Inc. had submitted an ANDA to the FDA seeking permission to market a
generic version of MYDAYIS. Within the requisite 45-day period, Shire filed a lawsuit in the U.S. District Court for the District of Delaware against
Teva Pharmaceuticals USA, Inc., Actavis Laboratories, Inc. and Teva Pharmaceutical Industries Limited (collectively the “Teva entities”). A Markman
hearing took place on January 23, 2019. A trial is scheduled to begin on December 9, 2019.
On March 8, 2018, Shire was notified that Impax Laboratories, Inc. (“Impax”) had submitted an ANDA to the FDA seeking permission to market a
generic version of MYDAYIS. Within the requisite 45-day period, Shire filed a lawsuit in the U.S. District Court for the District of Delaware against
Impax. A Markman hearing took place on January 23, 2019. A trial is scheduled to begin on December 9, 2019.
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On April 19, 2018, Shire was notified that SpecGX LLC (“SpecGX”) had submitted an ANDA to the FDA seeking permission to market a generic
version of MYDAYIS. Within the requisite 45-day period, Shire filed a lawsuit in the U.S. District Court for the District of Delaware against SpecGx.
Shire and SpecGx settled the lawsuit on January 28, 2019.
Petitions to institute inter partes reviews (“IPRs”) against U.S. Patent numbers 8,846,100 and 9,173,857 were filed by KVK Tech in January 2018 and
the petitions were granted in July 2018. Both of these patents are listed in the Orange Book as covering MYDAYIS and are among the patents-in-suit
in the infringement action brought against the Teva entities and Impax as noted above. A decision on the merits is expected on or before July 10, 2019.
ADYNOVATE
On December 5, 2016, Bayer Healthcare LLC (“Bayer”) filed a lawsuit in the US District Court for the District of Delaware against Baxalta Incorporated
and Baxalta US Inc. (collectively "Baxalta"), which are direct or indirect wholly owned subsidiaries of Shire, and Nektar Therapeutics (“Nektar”) filed
alleging infringement of U.S. Patent No. 9,364,520 in connection with the sales of ADYNOVATE [antihemophilic factor (recombinant), PEGylated].
The case was tried before a jury beginning on January 28, 2019. The jury found in favor of Bayer determining that the patent is infringed. The jury
further awarded damages in the amount of 155.2 million USD. Takeda is considering its further options. Takeda established a provision against this
case in purchase accounting (Note 31).
On September 15, 2017, Baxalta and Nektar filed a lawsuit in the US District Court for the District of Delaware against Bayer alleging infringement of
US Patent Nos. 7,199,223; 7,863,421; 8,143,378; 8,247,536; 8,519,102; 8,618,259; 8,889,831: This case was consolidated on December 7, 2018 with
Baxalta’s and Nektar’s lawsuit filed on August 31, 2018 alleging infringement of 7,026,440; 7,872,072; 8,273,833; 8,809,453; and 9,187,569 in connection
with the BAY-94 (subsequently approved and marketed as Jivi® (antihemophilic factor (recombinant PEGylated-aucl)). On July 2, 2018, an amended
complaint was filed adding US Patent No. 9,999,657. Markman hearings are scheduled to take place on June 21, 2019 and August 20, 2019. A trial is
scheduled to begin on April 27, 2020.
Other
In addition to the individual patent litigation cases described above, Takeda is party to a number of cases where Takeda has received notices that
companies have submitted ANDAs with paragraph IV certifications to sell generic versions of other Takeda products. These include other Takeda
products including Alogliptin. Takeda has filed patent infringement lawsuits against parties involved in these situations.
Sales, Marketing, and Regulation
Takeda has other litigations related to its products and its activities, the most significant of which are describe below.
ACTOS
There have been purported class action lawsuits filed in federal court in New York by several end payors and wholesalers against Takeda alleging
anticompetitive conduct to delay generic competition for ACTOS. In September 2015, the court granted defendants’ motions to dismiss the antitrust
claims asserted by the end payors. The end payors appealed this decision to the Federal 2nd Circuit Court of Appeals. The wholesalers’ lawsuit had been
stayed pending the appellate court’s decision in the end payors’ lawsuit. In February 2017, the appellate court reversed in part the dismissal of the end
payors’ case and allowed one of plaintiffs’ antitrust theories to proceed in the trial court. Specifically, the court ruled that plaintiffs sufficiently alleged
that Takeda’s characterizations of two patents in the FDA Orange Book were false, and that this resulted in delaying Teva’s launch of generic ACTOS.
Takeda disagrees with these allegations and believes the Orange Book listings were correct. The court, however, affirmed the trial court’s dismissal of
other antitrust theories. The end payors’ case, along with the wholesalers’ case, is proceeding in the trial court, where Takeda has filed a motion to dismiss
the remaining legal theory.
VANCOCIN
On April 6, 2012, ViroPharma Incorporated (“ViroPharma”) received a notification that the United States Federal Trade Commission (“FTC”) was
conducting an investigation into whether ViroPharma had engaged in unfair methods of competition with respect to VANCOCIN, which Shire acquired
in January 2014. Following its divestiture of VANCOCIN in August 2014, Shire retained certain liabilities including any potential liabilities related to
the VANCOCIN citizen petition.
On August 3, 2012, and September 8, 2014, ViroPharma and Shire respectively received Civil Investigative Demands from the FTC requesting additional
information related to this matter. Shire has fully cooperated with the FTC’s investigation.
On February 7, 2017, the FTC filed a complaint against Shire alleging that ViroPharma engaged in conduct in violation of U.S. antitrust laws arising
from a citizen petition ViroPharma filed in 2006 related to FDA’s policy for evaluating bioequivalence for generic versions of VANCOCIN. The complaint
seeks equitable relief, including an injunction and disgorgement. Shire filed a motion to dismiss on April 10, 2017. On March 20, 2018, the court granted
Shire’s motion. On April 11, 2018, the FTC filed a Notice of Appeal. On February 25, 2019, the Court of Appeals for the Third Circuit affirmed the
dismissal of the FTC’s complaint.
At this time, Takeda is unable to predict the outcome or duration of this case.
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Investigation of Patient Assistance Programs
In November 2016, the U.S. Department of Justice (through the U.S. Attorneys’ Office in Boston) issued a subpoena to ARIAD, which was acquired
by Takeda during the year ended March 31, 2017, seeking information from January 2010 to the present relating to ARIAD’s donations to 501(c) (3)
co-payment foundations, financial assistance programs, and free drug programs available to Medicare beneficiaries and the relationship between these
co-payment foundations and specialty pharmacies, hubs or case management programs. ARIAD is cooperating in the investigation.
In June 2019, the U.S. Department of Justice (through the U.S. Attorney’s Office in Boston, Massachusetts) issued a subpoena to Shire
Pharmaceuticals LLC, which was acquired by Takeda during the year ended March 31, 2019 (through Takeda’s acquisition of Shire plc). The
subpoena generally seeks information about Shire’s interactions with 501(c)(3) organizations that provide financial assistance to Medicare patients
taking Shire drugs, including the hereditary angioedema medications Firazyr and Cinryze. Shire is cooperating with the investigation.
33.
Subsequent Events
On May 9, 2019, Takeda announced the sale of Xiidra® (lifitegrast ophthalmic solution), which was obtained as part of the Shire acquisition, to buyer
Novartis. Xiidra® is currently marketed in the United States and Canada. Under the terms of the agreement, Takeda will receive total consideration of
up to 5.3 billion USD (approximately 590.0 billion JPY), including 3.4 billion USD in cash at closing and up to 1.9 billion USD in contingent payments.
The contingent payments become payable to Takeda at specified milestones based on sales of Xiidra® or a comparable generic product. Xiidra® was
recorded as held for sale at the date of the Shire acquisition, as Takeda intended to dispose of Xiidra®. The disposal group including Xiidra® was recorded
at the acquisition date based on the estimated consideration to be received in the transaction. The deal is expected to be closed in the second quarter
ended September 30, 2019.
On May 9, 2019, Takeda announced the sale of TachoSiltm (Fibrin Sealant Patch) to buyer Ethicon for 400 million EUR (approximately 50 billion
JPY). In addition, Takeda entered in a long-term manufacturing services agreement with the buyer. The transaction includes the sale of product rights
and transfer of related workforce. The deal is expected to be closed in the second quarter ended September 30, 2019.
On May 14, 2019, Takeda announced the issuance of 11,350 thousand shares at an issuance price of 4,318 JPY per share through third- party allotment
to The Master Trust Bank of Japan, Ltd., which is the trust account for Takeda’s ESOP subsidiary. This issuance was approved by the resolution of the
Board of Directors. These shares are issued with the intention to be reacquired by Takeda from the ESOP trust for distribution of share-based compensation
awards.
On June 6, 2019, Takeda issued hybrid bonds (subordinated bonds) (“Hybrid Bonds”) with an aggregate principal amount of 500 billion JPY. The
proceeds from this Hybrid Bonds offering were used to repay the existing syndicated loans comprised of the senior short-term loan facility that was
utilized to finance the acquisition of Shire. The Hybrid Bonds will mature on June 6, 2079. Under the terms and conditions of the Hybrid Bonds, Takeda
may make an early repayment of all of the principal of the Hybrid Bonds on each interest payment date beginning October 6, 2024. Interest is payable
semi-annually at a rate per annum subject to revision. The Hybrid Bonds are unsecured, and Takeda is not subject to any financial covenants related to
these bonds.
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