2OCT200908064695
Annual Report
Fiscal Year 2016
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!"4".I"$%75C%5678%
UNITED STATES SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
FORM 10-K
(Mark One)
!!!! ANNUAL REPORT UNDER SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT
OF 1934
For the fiscal year ended June 30, 2016
OR
"""" TRANSITION REPORT UNDER SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE
ACT OF 1934
For the transition period from to
Commission File No. 001-31298
LANNETT COMPANY, INC.
(Exact name of registrant as specified in its charter)
State of Delaware
State of Incorporation
23-0787699
I.R.S. Employer I.D. No.
9000 State Road
Philadelphia, Pennsylvania 19136
Registrant’s telephone number, including area code: (215) 333-9000
(Address of principal executive offices and telephone number)
Securities registered under Section 12(b) of the Exchange Act:
Common Stock, $.001 Par Value
(Title of class)
Securities registered under Section 12(g) of the Exchange Act: None
Indicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act. Yes !
No "
Indicate by check mark if the registrant is not required to file reports pursuant to Section 13 or Section 15(d) of the Act. Yes "
No !
Indicate by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities
Exchange Act of 1934 during the preceding 12 months (or for such shorter period that the registrant was required to file such reports)
and (2) has been subject to such filing requirements for the past 90 days. Yes ! No "
Indicate by check mark if disclosure of delinquent filers pursuant to Item 405 of Regulation S-K is not contained herein and will
not be contained, to the best of registrant’s knowledge, in definitive proxy or information statements incorporated by reference in
Part III of this Form 10-K or any amendment to this Form 10-K. "
Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, a non-accelerated filer, or a smaller
reporting company. See definitions of “large accelerated filer,” “accelerated filer,” and “smaller reporting company” in Rule 12b-2 of
the Exchange Act. (Check one):
Large accelerated filer !
Non-accelerated filer "
(Do not check if a smaller reporting company)
Accelerated filer "
Smaller reporting company "
Indicate by check mark whether the registrant has submitted electronically and posted on its corporate Web site, if any, every
Interactive Data File required to be submitted and posted 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 and post such files). Yes ! No "
Indicate by check mark whether the registrant is a shell company (as defined in Rule 12B-12 of the Exchange Act). Yes "
No !
Aggregate market value of common stock held by non-affiliates of the registrant, as of December 31, 2015 was $1,248,715,702
based on the closing price of the stock on the NYSE.
As of July 31, 2016, there were 36,892,377 shares of the registrant’s common stock, $.001 par value, outstanding.
�PART I
PART II
PART III
PART IV
ITEM 1. DESCRIPTION OF BUSINESS
ITEM 1A. RISK FACTORS
ITEM 2. DESCRIPTION OF PROPERTY
ITEM 3. LEGAL PROCEEDINGS
ITEM 4. MINE SAFETY DISCLOSURES
ITEM 5. MARKET FOR COMMON EQUITY AND RELATED STOCKHOLDER MATTERS
ITEM 6. SELECTED FINANCIAL DATA
ITEM 7. MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND
RESULTS OF OPERATIONS
ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK
ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA
ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND
FINANCIAL DISCLOSURE
ITEM 9A. CONTROLS AND PROCEDURES
ITEM 9B. OTHER INFORMATION
ITEM 10. DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE
ITEM 11. EXECUTIVE COMPENSATION
ITEM 12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT
AND RELATED STOCKHOLDER MATTERS
ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS, AND DIRECTOR
INDEPENDENCE
ITEM 14. PRINCIPAL ACCOUNTANT FEES AND SERVICES
ITEM 15. EXHIBITS, FINANCIAL STATEMENT SCHEDULES
SIGNATURES
4
22
36
36
36
37
39
40
57
57
57
57
58
59
63
85
87
88
89
94
CAUTIONARY STATEMENT REGARDING FORWARD-LOOKING STATEMENTS
This Annual Report on Form 10-K contains forward-looking statements. Any statements made in this Annual Report that are not
statements of historical fact or that refer to estimated or anticipated future events are forward-looking statements. We have based our
forward-looking statements on management’s beliefs and assumptions based on information available to them at this time. Without
limiting the generality of the foregoing, words such as “may,” “will,” “expect,” “believe,” “anticipate,” “intend,” “could,” “would,”
“estimate,” “continue,” or “pursue,” or the negative other variations thereof or comparable terminology, are intended to identify
forward-looking statements. Such forward-looking statements reflect our current perspective of our business, future performance,
existing trends and information as of the date of this filing. These include, but are not limited to, our beliefs about future revenue and
expense levels, growth rates, prospects related to our strategic initiatives and business strategies, express or implied assumptions about
government regulatory action or inaction, anticipated product approvals and launches, business initiatives and product development
activities, assessments related to clinical trial results, product performance and competitive environment, anticipated financial
performance and integration of acquisitions. The statements are not guarantees of future performance and involve certain risks,
uncertainties and assumptions that are difficult to predict. We caution the reader that certain important factors may affect our actual
operating results and could cause such results to differ materially from those expressed or implied by forward-looking statements. We
believe the risks and uncertainties discussed under the “Item 1A - Risk Factors” and other risks and uncertainties detailed herein and
from time to time in our SEC filings may affect our actual results.
We disclaim any obligation to publicly update any forward-looking statements, whether as a result of new information, future events
or otherwise. We also may make additional disclosures in our Quarterly Reports on Form 10-Q, Current Reports on Form 8-K and in
other filings that we may make from time to time with the SEC. Other factors besides those listed here could also adversely affect us.
2
3
�ITEM 1.
DESCRIPTION OF BUSINESS
Business Overview
PART I
Lannett Company, Inc. and subsidiaries (the “Company,” “Lannett,” “we,” or “us”) was incorporated in 1942 under the laws of the
Commonwealth of Pennsylvania and reincorporated in 1991 as a Delaware corporation. We develop, manufacture, market and
distribute generic versions of brand pharmaceutical products. We report financial information on a quarterly and fiscal year basis with
the most recent being the fiscal year ended June 30, 2016. All references herein to a “fiscal year” or “Fiscal” refer to the applicable
fiscal year ended June 30.
The Company has experienced total net sales growth at a compounded annual growth rate in excess of 28% over the past fifteen years.
In that time period, total net sales increased from $12.1 million in fiscal year 2001 to $542.5 million in fiscal year 2016. This growth
has been achieved through filing and receiving approvals for abbreviated new drug applications (“ANDAs”), favorable product
pricing environments, strategic partnerships and launches of additional manufactured drugs, opportunities resulting from our strong
historical record of regulatory compliance, as well as the June 1, 2015 acquisition of Silarx Pharmaceuticals, Inc. (“Silarx”) and the
recent Kremers Urban Pharmaceuticals Inc. (“KUPI”) acquisition.
All products that we currently manufacture and/or distribute are prescription products with the exception of a small portfolio of over-
the-counter products manufactured by Silarx Pharmaceuticals, Inc., our wholly-owned subsidiary. Our top five products in fiscal
years 2016, 2015 and 2014 accounted for 57%, 78% and 74% of total net sales, respectively.
On November 25, 2015, the Company completed the acquisition of KUPI, the former U.S. specialty generic pharmaceuticals
subsidiary of global biopharmaceuticals company UCB S.A. KUPI is a specialty pharmaceuticals manufacturer focused on the
development of products that are difficult to formulate or utilize specialized delivery technologies. Strategic benefits of the
acquisition include expanded manufacturing capacity, a diversified product portfolio and pipeline and complementary research and
development (“R&D”) expertise.
Competitive Strengths
Vertically Integrated Manufacturer, Supplier and Distributor of Narcotics and Controlled Drugs. In July 2008, the U.S. Drug
Enforcement Administration (“DEA”) granted Cody Laboratories, Inc. (“Cody Labs”) a license to directly import concentrated poppy
straw for conversion into opioid-based active pharmaceutical ingredients (“APIs”) for commercial use in various dosage forms for
pain management. This license, along with Cody Labs’ expertise in API development and manufacture, allows the Company to
perform in a market with high barriers to entry, no foreign dosage form competition and limited domestic competition. Because of
this vertical integration, the Company has direct control of its supply and can avoid increased costs associated with buying APIs from
third-party manufacturers, thereby achieving higher margins.
Proven Ability to Develop Successful Products and Achieve Scale in Production. We believe that our ability to select viable products
for development, efficiently develop such products, including obtaining any applicable regulatory approvals, vertically integrate into
certain markets and achieve economies of scale in production are critical to our success in the generic pharmaceutical industry. We
intend to focus on long-term profitability driven in part by securing market positions with few vertically integrated competitors.
Efficient Development Systems and Manufacturing Expertise for New Products. We believe that our manufacturing expertise, low
overhead expenses, efficient product development and marketing capabilities can help us remain competitive in the generic
pharmaceutical market. We intend to dedicate significant capital toward developing new products because we believe our success is
linked to our ability to continually introduce new generic products into the marketplace. Competition from new and other market
participants for the manufacture and distribution of certain products would likely affect our market share with respect to such products
as well as force us to reduce our selling price for such products due to their increased availability. As a result, we believe that our
success depends on our ability to properly assess the competitive market for new products, including market share, the number of
competitors and the generic unit price erosion. We intend to reduce our exposure to competitive influences that may negatively affect
our sales and profits, including the potential saturation of the market for certain products, by continuing to emphasize maintenance of
a strong product selection R&D pipeline.
Mutually Beneficial Supply and Distribution Arrangements. In 2004, we entered into an exclusive ten-year distribution agreement
(the “JSP Distribution Agreement”) with Jerome Stevens Pharmaceuticals (“JSP”) covering four different product lines. On
August 19, 2013, the Company entered into an agreement with JSP to extend its initial contract to continue as the exclusive distributor
in the United States of three JSP products: Butalbital, Aspirin, Caffeine with Codeine Phosphate Capsules USP; Digoxin Tablets USP;
and Levothyroxine Sodium Tablets USP. The amendment to the original agreement extends the initial contract, which was due to
expire on March 22, 2014, for five years. In connection with the amendment, the Company issued a total of 1.5 million shares of the
Company’s common stock to JSP and its designees. In accordance with its policy related to renewal and extension costs for
recognized intangible assets, the Company recorded a $20.1 million expense in cost of sales, which represented the fair value of the
shares on August 19, 2013.
If the parties agree to a second five year extension from March 23, 2019 to March 23, 2024, the Company is required to issue to JSP
or its designees an additional 1.5 million shares of the Company’s common stock. Both Lannett and JSP have the right to terminate
the contract if one of the parties does not cure a material breach of the contract within thirty (30) days of notice from the non-
breaching party. Levothyroxine Sodium and Digoxin collectively accounted for 34% of our total net sales in fiscal year 2016.
During the renewal term of the JSP Distribution Agreement, the Company is required to use commercially reasonable efforts to
purchase minimum dollar quantities of JSP products. There is no guarantee that the Company will continue to meet the minimum
purchase requirement for Fiscal 2017 and thereafter. If the Company does not meet the minimum purchase requirements, JSP’s sole
remedy is to terminate the agreement.
Dependable Supplier to our Customers. We believe we are viewed within the generic pharmaceutical industry as a strong, dependable
supplier. We have cultivated strong and dependable customer relationships by maintaining adequate inventory levels, employing a
responsive order filling system and prioritizing timely fulfillment of those orders. A majority of our orders are filled and shipped on
or the day after we receive the order.
Strong Track Record of Obtaining Regulatory Approvals for New Products. During the past three fiscal years, we have received
several approved ANDA /ANDA supplements from the Food and Drug Administration (the “FDA”). Although the timing of ANDA
approvals by the FDA is uncertain, we currently expect to receive several more during Fiscal 2017. These regulatory approvals will
enable us to manufacture and supply a broader portfolio of generic pharmaceutical products.
Reputation for Regulatory Compliance. We have a strong track record of regulatory compliance. We believe that we have strong
effective regulatory compliance capabilities and practices due to the hiring of qualified individuals and the implementation of strong
current Good Manufacturing Practices (“cGMP”). Our agility in responding quickly to market events and a reputation for regulatory
compliance position us to avail ourselves of market opportunities as they are presented to us.
In addition, narcotics which are classified by the DEA as “controlled drugs” are subject to a rigorous regulatory compliance regimen.
We have been granted a license from the DEA to import raw concentrated poppy straw for conversion into commercial APIs. Such
licenses are renewed annually and non-compliance could result in a license not being renewed. As a result, we believe that our strong
reputation for regulatory compliance allows us to have a competitive edge in managing the production and distribution of controlled
drugs.
Business Strategies
Continue to Broaden our Product Lines Through Internal Development and Strategic Partnerships.
We are focused on increasing our market share in the generic pharmaceutical industry while concentrating additional resources on the
development of new products, with an emphasis on controlled substance products. We continue to improve our financial performance
by expanding our line of generic products, increasing unit sales to current customers, creating manufacturing efficiencies and
managing our overhead and administrative costs.
We have four strategies for expanding our product offerings: (1) deploying our experienced R&D staff to develop products in-house;
(2) entering into product development agreements or strategic alliances with third-party product developers and formulators;
(3) purchasing ANDAs from other generic manufacturers; and (4) marketing drugs under brand-names. We expect that each strategy
will facilitate our identification, selection and development of additional pharmaceutical products that we may distribute through our
existing network of customers.
Key highlights related to product developments during Fiscal 2016 included the Company announcing a strategic partnership with
YiChang HEC ChangJiang Pharmaceutical Co., Ltd, an HEC Group company, to co-develop a generic insulin pharmaceutical product
for the U.S. market. The product is currently in late stage development. The Company will manage the remaining clinical and
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�regulatory steps specific for a U.S. Food and Drug Administration (FDA) license to market and will have the exclusive U.S. marketing
rights to the product.
Drug Master File (“DMF”) list. In our distribution of these products, we compete with generic products from Mylan, Impax, West-
Ward and until recently Sun, as well as the brand product Lanoxin distributed by Concordia.
We have several existing supply and development agreements with both international and domestic companies; in addition, we are
currently in negotiations on similar agreements with additional companies through which we can market and distribute future
products. We intend to capitalize on our strong customer relationships to build our market share for such products.
Mergers and Acquisitions.
We are active in evaluating potential mergers and acquisitions opportunities that are a strategic fit and accretive to our business. We
are particularly interested in opportunities that globalize our business, further vertically integrate our operations, or enhance
shareholder value through tax favorable jurisdiction treatment. During Fiscal 2016, we completed the acquisition of KUPI, the former
subsidiary of global biopharmaceuticals company UCB S.A. KUPI is a U.S. specialty pharmaceuticals manufacturer focused on the
development of products that are difficult to formulate or utilize specialized delivery technologies. Strategic benefits of the
acquisition include expanded manufacturing capacity, a diversified product portfolio and pipeline and complementary R&D expertise.
Improve our Operating Profile in Certain Targeted Specialty Markets.
In certain situations, we may increase our focus on particular specialty markets within the generic pharmaceutical industry. By
narrowing our focus to specialty markets, we can provide product alternatives in categories with relatively fewer market participants.
We plan to strengthen our relationships with strategic partners, including providers of product development research, raw materials,
APIs and finished products. We believe that mutually beneficial strategic relationships in such areas, including potential financing
arrangements, partnerships, joint ventures or acquisitions, could enhance our competitive advantages in the generic pharmaceutical
market.
Leverage Ability to Vertically Integrate as a Manufacturer, Supplier and Distributor of Controlled Substance Products.
One initiative that is at the core of the Company’s strategy is to continue leveraging the asset we acquired in 2007, Cody Labs. In
July 2008, the DEA granted Cody Labs a license to directly import concentrated poppy straw for conversion into opioid-based
commercial APIs for use in various dosage forms for pain management. The value of this license comes from the fact that, to date,
only a limited number of companies in the U.S. have been granted this license. This license, along with Cody Labs’ expertise in API
development and manufacture, allows the Company to perform in a market with high barriers to entry, no foreign dosage form
competition and limited domestic competition. Because of this vertical integration, the Company has direct control of its supply and
can avoid increased costs associated with buying APIs from third-party manufacturers, thereby achieving higher margins. The
Company can also leverage this vertical integration not only for direct supply of opioid-based APIs, but also for the manufacture of
non-opioid-based APIs.
The Company believes that the demand for controlled substance, pain management drugs will continue to grow as the “Baby Boomer”
generation ages. By concentrating additional resources in the development of opioid-based APIs and abuse deterrent features to
current dosage forms, the Company is well-positioned to take advantage of this opportunity. The Company is currently vertically
integrated on two products with several others in various stages of development.
Key Products
Levothyroxine Sodium Tablets
Levothyroxine Sodium tablets, which are used for the treatment of thyroid deficiency by patients of various ages and demographic
backgrounds, is the second most prescribed drug in the United States. The product is manufactured by JSP and distributed by us under
the JSP Distribution Agreement and is produced and marketed in 12 potencies. Net sales of Levothyroxine Sodium tablets totaled
$162.4 million in fiscal year 2016. Levothyroxine is a narrow therapeutic index drug and very difficult to formulate which results in a
less competitive market environment for this molecule. In our distribution of these products, we compete with two brand
Levothyroxine Sodium products, AbbVie’s Synthroid and Pfizer’s Levoxyl, as well as generic products from Mylan and Sandoz.
Digoxin Tablets
Digoxin tablets, which are used to treat congestive heart failure in patients of various ages and demographics, are produced and
marketed with two different potencies. This product is manufactured by JSP and we distribute it under the JSP Distribution
Agreement. Net sales of this product totaled $23.9 million in fiscal year 2016. The product is highly potent based on Environment,
Health & Safety (“EHS”), regulations and its API availability is limited given there are only two active suppliers, based on the FDA
Acetazolamide Tablets
Acetazolamide tablets are used for the treatment of glaucoma. The product is a carbonic anhydrase inhibitor that reduces fluid pressure
in the eyeball. It also increases the removal of water from the body by the kidneys and may block certain nerve discharges that may
contribute to seizures. Net sales of Acetazolamide tablets totaled $25.3 million in fiscal year 2016. Currently, our primary generic
competitor for this drug is Taro Pharmaceutical Industries.
Butalbital Products
We distribute three products containing Butalbital. We have manufactured and sold Butalbital with Aspirin and Caffeine capsules for
more than 25 years. Butalbital with Aspirin, Caffeine and Codeine Phosphate capsules are manufactured by JSP and distributed under
the JSP Distribution Agreement. Additionally, in September 2012, the Company was approved to sell Butalbital, Acetaminophen and
Caffeine Tablets. Butalbital products, which are orally administered in capsule or tablet dosage forms, are prescribed to treat
migraines and tension headaches caused by contractions of the muscles in the neck and shoulder area. The drug is prescribed
primarily for adults of various demographics. Migraines are an increasingly prevalent condition in the United States, and we believe
the demand for effective medical treatments will continue to increase. Net sales of Butalbital products totaled $21.8 million in fiscal
year 2016. Although new innovator drugs to treat migraines have been introduced by brand-name drug companies, we believe that
there is still a loyal following of doctors and consumers who prefer to use Butalbital products for treatment. In our distribution of
these products, we compete with products from Mallinckrodt, Mikart, Qualitest, Watson, West-Ward, Actavis and Breckenridge.
Ursodiol Capsules
Ursodiol Capsules are produced and marketed in 300 mg capsules and are used for the treatment of gallstones. Net sales of Ursodiol
capsules totaled $67.3 million in fiscal year 2016. We compete with a generic product from Epic and Mylan, as well as the brand
product Actigall distributed by Actavis.
Omeprazole Capsules
Omeprazole is a proton pump inhibitor that decreases the amount of acid produced in the stomach. The product is a generic version of
the branded drug Prilosec®. It is indicated for heartburn or irritation of the esophagus caused by gastroesophageal reflux disease.
KUPI produces Omeprazole DR capsules in 10mg, 20mg and 40mg dosages. Net sales of Omeprazole capsules totaled $23.7 million
in fiscal year 2016. In distributing this product, we compete primarily with Sandoz, Dr. Reddy’s and Zydus.
Methylphendiate Hydrochloride ER
Methylphenidate ER is a central nervous system stimulant indicated for the treatment of Attention Deficit Hyperactivity Disorder
(“ADHD”) in children six years of age and older, adolescents and adults up to the age of 65. The product is a generic version of the
branded drug Concerta®, which is currently marketed by Janssen Pharmaceuticals, Inc. and competes with a generic product marketed
by Mallinckrodt Pharmaceuticals and an Authorized Generic (“AG”) marketed by Actavis. The product was approved by the FDA in
2013 with a therapeutic equivalence rating of AB, meaning the FDA deemed it therapeutically equivalent to the brand-name drug,
Concerta®. Net sales of Methylphenidate ER tablets totaled $28.3 million in fiscal year 2016.
During a teleconference in November 2014, the FDA informed KUPI that it had concerns about whether generic versions of
Concerta® (methylphenidate hydrochloride extended release tablets), including KUPI’s Methylphenidate ER product, are
therapeutically equivalent to Concerta®. FDA indicated that its concerns were based in part on adverse event reports concerning lack
of effect and its analyses of pharmacokinetic data. FDA informed KUPI that it was changing the therapeutic equivalence rating of its
product from “AB” (therapeutically equivalent) to “BX.” A BX-rated drug is a product for which data are insufficient to determine
therapeutic equivalence; it is still approved and can be dispensed, but it may not be automatically substitutable at the pharmacy for the
brand-name drug under certain state laws. The FDA has indicated that there are no safety issues with KUPI’s product.
During the November 2014 teleconference, FDA also asked KUPI to either voluntarily withdraw its product or to conduct new
bioequivalence (“BE”) testing in accordance with the recommendations for demonstrating bioequivalence to Concerta proposed in a
new draft BE guidance that FDA issued earlier that November. FDA had approved the KUPI product (and originally granted it an AB
rating) in 2013, on the basis of KUPI data showing its product met bioequivalence criteria set forth in draft bioequivalence guidance
that FDA had issued in 2012. FDA’s position concerning the KUPI product was the subject of a public announcement by the agency.
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�KUPI agreed to conduct new bioequivalence studies per the new draft bioequivalence guidance. KUPI submitted the data from those
studies to FDA in May 2015. The Company continues to pursue the FDA to obtain its decision on the submitted study as well as its
response on whether it will restore the AB-rating for our product.
specialized manufacturing suites are a few examples of the sophisticated product development, manufacturing and packaging
equipment used in the production process. In addition, our Quality Control laboratory facilities are equipped with high precision
instruments, such as automated liquid chromatographs (“HPLC” and “UPLC”), gas chromatographs and laser particle size analyzers.
Pain Management Products
Cocaine Topical® Solution (“C-Topical®”) is produced and marketed under a preliminary new drug application (“PIND”) in two
different strengths and two different size containers. C-Topical® is utilized primarily for the anesthetization of the patient during ear,
nose or throat surgery and sinoplasty. The Company has completed a Phase III clinical trial and our Clinical Research Organization
(“CRO”) is assembling the data for our New Drug Application (“NDA”) for C-Topical® and continues to actively market the product
utilizing a group of brand representatives in key market locations throughout the United States.
Morphine Sulfate Oral Solution is produced and marketed in three different size containers. We manufacture this product at Cody
Labs and are currently finishing the manufacturing methods and capabilities to make the API. This drug is prescribed primarily for
the management of pain in adults.
Oxycodone HCl Oral Solution (“Oxycodone”) was produced until August 20, 2012 and marketed until October 4, 2012 in two
different size containers, at which point, as a result of FDA enforcement actions against all market participants, the Company
voluntarily exited the market. Prior to the enforcement actions the Company had submitted an ANDA to the FDA and subsequently
received approval and commenced shipping Oxycodone in September 2014. This drug is prescribed primarily for the management
and relief of moderate to moderately severe pain.
Other products in the pain management franchise include Hydromorphone HCl tablets, where we are vertically integrated, and
Codeine Sulfate tablets. Additionally, the Company added several pain management products through the Silarx acquisition. Net
sales of pain management products totaled $29.8 million in fiscal year 2016.
Validated Pharmaceutical Capabilities
Lannett’s 31,000 square foot manufacturing facility sits on 3.5 acres of Company-owned land. In addition, we own a 63,000 square
foot building residing on 3.0 acres of Company-owned land. This facility is located within one mile of our manufacturing facility.
The facility houses our Quality Control (“QC”) laboratories, packaging and research and development and has capacity for additional
manufacturing space, if needed. We also own a 66,000 square foot building on 7.3 acres of land, which is used for certain
administrative functions, warehouse space and shipping. It also has capacity for additional manufacturing space, if needed. All three
of these buildings are located in Philadelphia, Pennsylvania.
The manufacturing facility of our wholly-owned subsidiary, Cody Labs, consists of an approximately 73,000 square foot facility
located on 15.0 acres of land in Cody, Wyoming. Cody Labs leases the facility from Cody LCI Realty, LLC (“Realty”), which is 50%
owned by Lannett and 50% owned by a former officer of Cody Labs. Cody Labs’ manufacturing facility currently has little capacity
for further expansion.
In June 2015, we completed the acquisition of Silarx. The Silarx manufacturing facility consists of an 110,000 square foot facility
located in Carmel, New York and sits on 25.8 acres of land. The facility currently houses manufacturing, packaging, research and
development and has capacity for additional manufacturing space, if needed.
In November 2015, we completed the acquisition of KUPI. KUPI’s 432,000 square foot Seymour, Indiana facility contains
approximately 107,000 square feet of manufacturing space as well as a leased 116,000 square foot temperature/humidity controlled
storage warehouse. Seymour has had satisfactory inspections conducted by the FDA and EMA and similar regulatory authorities of
Japan, Taiwan, Brazil, Korea and Turkey. Since 2008, KUPI has invested more than $75 million into improvements to the facility and
new equipment. This investment enabled the facility to increase production from approximately 1.2 billion doses in 2008 to over
2.7 billion doses in 2014. KUPI recently completed a $20 million, 20,000 square foot expansion of the facility which, in combination
with an additional planned expansion in 2016, is expected to increase capacity to 3.9 billion doses by 2017. KUPI added a large vault
for storing controlled substances in 2011 and is also planning to expand its vault capabilities relating to Schedule II (“CII”) products in
conformance with DEA requirements. The facility also includes four packaging lines, one of which is a high speed line added in
2012. The serialization has been completed on three lines and we expect to complete the fourth line in the near future.
We have adopted many processes in support of regulations relating to cGMPs in the last several years and we believe we are operating
our facilities in substantial compliance with the FDA’s cGMP regulations. In designing our facilities, full attention was given to
material flow, equipment and automation, quality control and inspection. A granulator, an automatic film coating machine, high-
speed tablet presses, blenders, encapsulators, fluid bed dryers, high shear mixers, high-speed bottle filling and high potency or
We continue to pursue “Quality by Design” for improving and maintaining quality control and quality assurance programs in our
pharmaceutical development and manufacturing facilities, which is outlined in the FDA report entitled, “Pharmaceutical Quality for
the 21st Century: A Risk-Based Approach.” The FDA periodically inspects our production facilities to determine our compliance
with the FDA’s manufacturing standards. Typically, after completing its inspection, the FDA will issue a report, entitled a
“Form 483,” containing observations arising from an inspection. The FDA’s observations may be minor or severe in nature and the
degree of severity is generally determined by the time necessary to remediate the cGMP violation, any consequences to the consumer
of the products and whether the observation is subject to a Warning Letter from the FDA. By strictly complying with cGMPs and the
various FDA guidelines, Good Laboratory Practices (“GLPs”), as well as adherence to our Standard Operating Procedures, we have
never received a cGMP Warning Letter in more than 70 years of business.
Research and Development Process
Over the past several years, we have invested heavily in R&D projects. The costs of these R&D efforts are expensed during the
periods incurred. We believe that such costs may be recovered in future years when we receive approval from the FDA to
manufacture and distribute such products. We have embarked on a plan to grow in future years, which includes organic growth to be
achieved through our R&D efforts. We expect that our growing list of generic products under development will drive future growth.
Over the past several years, we have hired additional personnel in product development, production and formulation. The following
steps outline the numerous stages in the generic drug development process:
1.) Formulation and Analytical Method Development. After a drug candidate is selected for future sale, product development
scientists perform various experiments in order for the binding agents or lubricants to incorporate APIs into a dosage form
that will then, not only be therapeutically equivalent to the brand name drug, but match its size and shape as well. These
experiments will result in the creation of a number of product formulations to determine which formula will be most suitable
for our subsequent development process. Various formulations are tested in the laboratory to measure results against the
innovator brand drug. During this time, we may use reverse engineering methods on samples of the innovator drug to
determine the type and quantity of inactive ingredients. During the formulation phase, our R&D chemists begin to develop
an analytical, laboratory testing method. The successful development of this test method will allow us to test developmental
and commercial batches of the product in the future. All of the information used in the final formulation, including the
analytical test methods adopted for the generic drug candidate, will be included as part of the Chemistry, Manufacturing and
Controls (“CMC”) section of the ANDA submitted to the FDA.
2.) Scale-up and Tech Transfer. After product development, scientists and the R&D chemists agree on a final formulation for
use in moving the drug candidate forward in the developmental process, we then attempt to increase the batch size of the
product. The batch size represents the standard magnitude to be used in manufacturing a batch of the product. The
determination of batch size affects the amount of raw material that is used in the manufacturing process and the number of
expected dosages to be created during the production cycle. We attempt to determine batch size based on the amount of
active ingredient in each dosage, the available production equipment and unit sales projections. The scaled-up batch is then
generally produced in our commercial manufacturing facilities. During this manufacturing process, we document the
equipment used, the amount of time in each major processing step and any other steps needed to consistently produce a batch
of that product. This information, generally referred to as the validated manufacturing process, is included in the ANDA.
3.) Bioequivalency and Clinical Testing. After a successful scale-up of the generic drug batch, we schedule and perform
generally required bioequivalency testing on the product and in some cases, clinical testing if required by the FDA. These
procedures, which are generally outsourced to third parties, include testing the absorption of the generic product in the human
bloodstream compared to the absorption of the innovator drug. The results of this testing are then documented and reported
to us to determine the “success” of the generic drug product. Success, in this context, means that we are able to demonstrate
that our product is comparable to the innovator product in dosage form, strength, route of administration, quality,
performance characteristics and intended use.
Bioequivalence (meaning that the product performs in the same manner and in the same amount of time as the innovator
drug) and a stable formula are the primary requirements for a generic drug approval (assuming the manufacturing plant is in
compliance with the FDA’s cGMP regulations). With the exception of 505(b)(2) NDA filings, lengthy and costly clinical
trials proving safety and efficacy, which are required by the FDA for innovator drug approvals, are typically unnecessary for
generic companies. If the results are successful, we will continue the collection of information and documentation for
assembly of the drug application.
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�4.) Submission of the ANDA for FDA Review and Approval. The ANDA process became formalized under The Drug Price
Competition and Patent Term Restoration Act of 1984, also known as the Hatch-Waxman Act (“Hatch-Waxman Act”). The
Hatch-Waxman Act amended the Federal Food, Drug and Cosmetic Act (“FDCA”) to permit the FDA to review and approve
an ANDA for a generic equivalent of a new drug product, which previously received FDA approval through its new drug
approval process, without having the generic drug company conduct costly clinical trials. An ANDA is a comprehensive
submission that contains, among other things, data and information pertaining to the active pharmaceutical ingredient, drug
product formulation, specifications and stability of the generic drug, as well as analytical methods, manufacturing process
validation data and quality control procedures.
We currently file our ANDAs and NDAs electronically. On July 9, 2012, the Food and Drug Administration Safety and Innovation
Act was enacted, which included the Generic Drug User Fee Amendments of 2012 (“GDUFA”). Under these Amendments the FDA
committed to reviewing 90% of complete electronic generic applications within 10 months after the date of submission. Applications
filed after October 2014 will be reviewed under this process. While we have received approval for some of our ANDAs in as little as
14 months, we have also waited longer than 77 months before receiving approval. The FDA has advised that electronic submissions
of applications may shorten the approval process, however ANDAs and NDAs submitted for our products may not receive FDA
approval on a timely basis, or at all.
When a generic drug company files an ANDA with the FDA, it must certify either that (i) no patent was filed for the listed drug (a
“paragraph I” certification), (ii) the patent has expired (a “paragraph II” certification), (iii) the patent will expire on a specified date
and the ANDA filer will not market the drug until that date (a “paragraph III” certification), or (iv) the patent is invalid or would not
be infringed by the manufacture, use, or sale of the new drug (a “paragraph IV” certification). A paragraph IV certification must be
provided to each owner of the patent that is the subject of the certification and to the holder of the approved NDA to which the ANDA
refers. A paragraph IV certification can trigger an automatic 30 month stay of the ANDA if the innovator company files a claim
which would delay the approval of the generic company’s ANDA.
As of June 30, 2016, we have 12 paragraph IV certifications pending with the FDA. Four of the paragraph IV certifications are
currently being challenged. In response to our paragraph IV certification with respect to the Zomig® nasal spray product,
AstraZeneca AB, AstraZeneca UK Limited and Impax Laboratories, Inc. filed two patent infringement complaints against the
Company in July 2014. In response to our paragraph IV certification with respect to Thalomid®, Celegene Corporation and
Children’s Medical Center Corporation filed a patent infringement lawsuit against the Company in January 2015. In response to our
paragraph IV certification with respect to Dilaudid®, Purdue Pharmaceutical Products L.P, Purdue Pharma L.P and Purdue Pharma
Technologies Inc. filed a patent infringement lawsuit against the Company in August 2015. The Company is in various stages of
responding to the patent infringement claims; and in the case of Dilaudid, a settlement has been reached in principle and details are
being finalized. Refer to Note 12 “Legal and Regulatory Matters” for additional information.
Sales and Customer Relationships
We sell our pharmaceutical products to generic pharmaceutical distributors, drug wholesalers, chain drug retailers, private label
distributors, mail-order pharmacies, other pharmaceutical manufacturers, managed care organizations, hospital buying groups,
governmental entities and health maintenance organizations. We promote our products through direct sales, trade shows and bids.
Our practice of maintaining adequate inventory levels, employing a responsive order filling system and prioritizing timely fulfillment
of those orders have contributed to a strong reputation among our customers as a dependable supplier of high quality generic
pharmaceuticals.
Management
We have been focused on enhancing the quality of our management team in anticipation of continuing growth. As part of our growth,
we have established corporate and non-corporate officer positions. We recently promoted two internal candidates to officer positions.
We have hired experienced personnel from large, established, brand pharmaceutical companies as well as competing generic
companies to complement the skills and knowledge of the existing management team. As we continue to grow, additional personnel
may need to be added to our management team. We intend to hire the best people available to expand the knowledge base and
expertise within our personnel ranks.
Current Products
As of the date of this filing, we manufactured and/or distributed the following products:
Acetazolamide Tablets
Butalbital, Acetaminophen and Caffeine Tablets
Butalbital, Aspirin and Caffeine Capsules
C-Topical ® Solution
Digoxin Tablets*
Glycolax Rx
Name of Product(1)
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2
3
4
5
6
7
8
9
10
11
12
13
14
15
16
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Isosorbide Mononitrate CR
Levothyroxine Sodium Tablets*
Methylphenidate HCL CD
Methylphenidate ER
Nifedipine CR
Omeprazole DR
Oxbutynin ER
Pantoprazole DR
Pilocarpine HCl Tablets
Triamterene w/Hydrochlorothiazide Capsules
Ursodiol Capsules
Medical Indication
Glaucoma
Migraine
Migraine
Anesthetic
Congestive Heart Failure
Gastrointestinal
Cardiovascular
Thyroid Deficiency
Central Nervous System
Central Nervous System
Cardiovascular
Gastrointestinal
Urinary
Gastrointestinal
Dryness of the Mouth
Hypertension
Gallstone
Equivalent Brand
Diamox®
Fioricet®
Fiorinal®
N/A
Lanoxin®
MiraLAX®
Imdur®
Levoxyl®/ Synthroid®
Metadate® CD™
Concerta®
Procardia®
Prilosec®
Ditropan®
Protonix®
Salagen®
Dyazide®
Actigall ®
*Distributed under the JSP Distribution Agreement
(1) Products not listed each represented less than 1% of total net sales in Fiscal 2016.
Unlike brand, innovator companies, we generally do not develop new molecules. However, we have filed and received two patents
for APIs at our Cody, Wyoming manufacturing facility, with additional patents in process. Additionally, the Company has completed
the Phase III clinical trial and our CRO is assembling the data for our New Drug Appication. The Company continues to actively
market the product utilizing a group of brand representatives in key market locations throughout the United States.
In fiscal year 2016, we received several ANDA/ANDA supplement approvals from the FDA. The following summary contains more
specific details regarding our latest ANDA approvals. Market data was obtained from Wolters Kluwer and IMS.
In August 2015, we received a letter from the FDA with approval to market and launch Aripiprazole Oral Solution 1 mg/ML, the
generic version of the antidepressant drug ABILIFY®. According to IMS, annual total U.S. sales of Aripiprazole 1mg/mL Oral
Solution at Average Wholesale Price (“AWP”) were approximately $76.0 million. However, when the brand-name drug was
discontinued just prior to our approval being received from the FDA, the market opportunity declined.
In October 2015, we received a letter from the FDA with approval to market and launch Memantine Hydrochloride Oral Solution 2
mg/mL, the therapeutic equivalent to the reference listed drug Namenda® Oral Solution, 2mg/mL of Forest Pharmaceuticals.
According to IMS, for the year ended June 2015, total U.S. sales of Memantine Hydrochloride Oral Solution 2 mg/mL at AWP were
approximately $12.0 million.
In February 2016, we received a letter from the FDA with approval to market and launch Temozolomide Capsules 5 mg, 20 mg, 100
mg, 140 mg, 180 mg and 250 mg, the therapeutic equivalent to the reference drug listed Temodar® Capsules of Merck & Co.
According to IMS, total U.S. sales in 2015 of Temozolomide Capsules 5 mg, 20 mg, 100 mg, 140 mg, 180 mg and 250 mg at AWP
were approximately $206.0 million.
In February 2016, we received a letter from the FDA with approval to market and launch Sumatriptan Nasal Spray USP, 5 mg/spray
and 20 mg/spray, the therapeutic equivalent to the reference listed drug Imitrex® Nasal Spray, of GlaxoSmithKline. According to
IMS, total U.S. sales in 2015 of Sumatriptan Nasal Spray USP, 5 mg/spray and 20mg/spray at AWP were approximately $62.0
million.
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�In March 2016, we received a letter from the FDA with approval to market and launch Potassium Chloride Extended-release Capsules
USP, 8 mEq and 10 mEq, the therapeutic equivalent to the reference listed drug of Actavis Labs FL, Inc. According to IMS, total U.S.
sales in 2015 of Potassium Chloride Extended-release Capsules USP, 8 mEq and 10 mEq at AWP were approximately $89.0 million.
In June 2016, we received a letter from the FDA with approval to market and launch Neomycin Sulfate Tablets USP, 500 mg, the
therapeutic equivalent to the reference listed drug, Neomycin Sulfate Tablets USP, 500 mg, of Teva Pharmaceuticals USA, Inc.
According to IMS, total U.S. sales in 2015 of Neomycin Sulfate Tablets USP, 500 mg, at AWP were approximately $3.0 million.
In June 2016, we received a letter from the FDA with approval to market and launch Diazepam Oral Solution, 5 mg/5 mL, the
therapeutic equivalent to the reference listed drug, Diazepam Oral Solution, 5mg/5mL, of Roxane Laboratories, Inc. According to
IMS, total U.S. sales in 2015 of Diazepam Oral Solution, 5 mg/5 mL, at AWP were approximately $4.0 million.
We have additional products currently under development which are orally administered solid oral-dosage products (i.e.,
tablet/capsule) or oral solutions, nasal, topicals or parentarels, as well as other dosage forms designed to be generic equivalents to
brand-named innovator drugs. Our developmental drug products are intended to treat a diverse range of indications. The products
under development are at various stages in the development cycle—formulation, scale-up, clinical testing and FDA review.
The cost associated with each product that we are currently developing is dependent on numerous factors, including but not limited to,
the complexity of the active ingredient’s chemical characteristics, the price of the raw materials and the FDA-mandated requirement
of bioequivalence studies (depending on the FDA’s Orange Book classification). With the introduction of GDUFA and additional
guidance issued by the FDA, the cost to develop a new generic product varies but now totals several million dollars.
In addition, we currently own several ANDAs that are dormant for products which we currently do not manufacture and market.
Occasionally, we review such ANDAs to determine if the market potential for any of these older drugs has recently changed to make
it attractive for us to reconsider manufacturing and selling. If we decide to introduce one of these products into the consumer market,
we must review the original ANDA and related documentation to ensure that the approved product specifications, formulation and
other factors meet current FDA requirements for the marketing of the applicable drug. Generally, in these situations, we file a
supplement to the FDA for the applicable ANDA, informing the FDA of any significant changes in the manufacturing process, the
formulation, the raw material supplier, or another major feature of the previously approved ANDA. We would then redevelop the
product and submit it to the FDA for supplemental approval. The FDA’s approval process for an ANDA supplement is similar to that
of a new ANDA.
In addition to the efforts of our internal product development group, we have contracted with numerous outside firms for the
formulation and development of several new generic drug products. These outsourced R&D products are at various stages in the
development cycle—formulation, analytical method development and testing and manufacturing scale-up. These products include
orally administered solid dosage products, injectables and nasal delivery products that are intended to treat a diverse range of medical
indications. We intend to ultimately transfer the formulation technology and manufacturing process for some of these R&D products
to our own commercial manufacturing sites. We initiated these outsourced R&D efforts to complement the progress of our own
internal R&D efforts.
The following table summarizes key information related to our R&D products at June 30, 2016. The column headings are defined as
follows:
development. While we manage all R&D from our principal executive office in Philadelphia, Pennsylvania, we have also been taking
steps to capitalize on favorable development costs in other countries. We have strategic relationships with various companies that
either act as contract research organizations or API suppliers as well as dosage form manufacturers. In addition, U.S.-based research
organizations have been engaged for product development to enhance our internal development. Fixed payment arrangements are
established between Lannett and these research organizations and in some cases include a royalty provision. Development payments
are normally scheduled in advance, based on attaining development milestones.
Raw Materials and Finished Goods Suppliers
Our use of raw materials in the production process consists of using pharmaceutical chemicals in various forms that are generally
available from several sources. FDA approval is required in connection with the process of using active ingredient suppliers. In
addition to the raw materials we purchase for the production process, we purchase certain finished dosage inventories. We sell these
finished dosage form products directly to our customers along with the finished dosage form products manufactured in-house. We
generally take precautionary measures to avoid a disruption in raw materials and finished goods, such as finding secondary suppliers
for certain raw materials or finished goods when available.
The Company’s primary finished goods inventory supplier is JSP, in Bohemia, New York. Purchases of finished goods from JSP
accounted for 52% of our inventory purchases in fiscal year 2016, 68% in fiscal year 2015 and 62% in fiscal year 2014. On March 23,
2004, the Company entered into an agreement with JSP for the exclusive distribution rights in the United States to the current line of
JSP products, in exchange for 4.0 million shares of the Company’s common stock. The JSP products covered under the agreement
included Butalbital, Aspirin, Caffeine with Codeine Phosphate Capsules; Digoxin Tablets; and Levothyroxine Sodium Tablets, sold
generically and under the brand-name Unithroid®. On August 19, 2013, the Company entered into an agreement with JSP to extend
its initial contract to continue as the exclusive distributor in the United States of three JSP products: Butalbital, Aspirin, Caffeine with
Codeine Phosphate Capsules USP; Digoxin Tablets USP; and Levothyroxine Sodium Tablets USP. The amendment to the original
agreement extends the initial contract, which was due to expire on March 22, 2014, for five years through March 2019. In connection
with the amendment, the Company issued a total of 1.5 million shares of the Company’s common stock to JSP and its designees. The
Company recorded a $20.1 million expense in cost of sales, which represents the fair value of the shares on August 19, 2013. If the
parties agree to a second five year extension from March 23, 2019 to March 23, 2024, the Company is required to issue to JSP or its
designees an additional 1.5 million shares of the Company’s common stock. Both Lannett and JSP have the right to terminate the
contract if one of the parties does not cure a material breach of the contract within thirty (30) days of notice from the non-breaching
party.
During the renewal term of the JSP Distribution Agreement, the Company is required to use commercially reasonable efforts to
purchase minimum dollar quantities of JSP products. There is no guarantee that the Company will continue to meet the minimum
purchase requirement for Fiscal 2017 and thereafter. If the Company does not meet the minimum purchase requirements, JSP’s sole
remedy is to terminate the agreement.
We have entered into definitive supply and development agreements with JSP, Summit Bioscience LLC, HEC Pharm Group, Pharma
Pass II LLC and various other international and domestic companies. The Company is currently in negotiations on similar agreements
with other companies and is actively seeking additional strategic partnerships, through which it will market and distribute products
manufactured in-house or by third parties. The Company plans to continue evaluating potential merger and acquisition opportunities
as well as product acquisitions that are a strategic fit and accretive to the business.
1.) Stage of R&D — defines the current stage of the R&D product in the development process, as of the date of this
Customers and Marketing
Form 10-K.
2.) Regulatory Requirement — defines whether the R&D product is or is expected to be a new ANDA submission or a
NDA.
3.) Number of Products — defines the number of products in R&D at the stage noted. In this context, a product means any
finished dosage form, including all potencies, containing the same API or combination of APIs and which represents a
generic version of the same Reference Listed Drug (“RLD”) or innovator drug, identified in the FDA’s Orange Book.
Stage of R&D
FDA Review
In Development
Regulatory Requirement
ANDA
ANDA/NDA
Number of Products
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We recorded R&D expenses of $45.1 million in fiscal year 2016, $30.3 million in fiscal year 2015 and $27.7 million in fiscal year
2014. These amounts included expenses associated with bioequivalence studies, internal development resources as well as outsourced
We sell our products primarily to wholesale distributors, generic drug distributors, mail-order pharmacies, group purchasing
organizations, chain drug stores and other pharmaceutical companies. The pharmaceutical industry’s largest wholesale distributors,
Amerisource Bergen, McKesson and Cardinal Health, accounted for 25%, 16% and 7%, respectively, of our total net sales in fiscal
year 2016 and 30%, 11% and 7%, respectively, of our total net sales in fiscal year 2015. Our largest chain drug store customer in
fiscal year 2016 and 2015 accounted for 5% and 6% of total net sales, respectively.
Sales to wholesale customers include “indirect sales,” which represent sales to third-party entities, such as independent pharmacies,
managed care organizations, hospitals, nursing homes and group purchasing organizations, collectively referred to as “indirect
customers.” We enter into definitive agreements with our indirect customers to establish pricing for certain covered products. Under
such agreements, the indirect customers independently select a wholesaler from which to purchase the products at these agreed-upon
prices. We will provide credit to the wholesaler for the difference between the agreed-upon price with the indirect customer and the
wholesaler’s invoice price. This credit is called a “chargeback.” For more information on chargebacks, see the section entitled
“Critical Accounting Policies” in Item 7, “Management’s Discussion and Analysis of Financial Condition and Results of Operations”
of this Form 10-K. These indirect sale transactions are recorded on our books as sales to wholesale customers.
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�We promote our products through direct sales, trade shows and group purchasing organizations’ bidding processes. We also market
our products through private label arrangements, under which we manufacture our products with a label containing the name and logo
of our customer. This practice is commonly referred to as “private label.” Private label allows us to leverage our internal sales efforts
by using the marketing services from other well-respected pharmaceutical competitors. The focus of our sales efforts is the
relationships we create with our customer accounts.
Strong and dependable customer relationships have created a positive platform for us to increase our sales volumes. Historically and
in fiscal years 2016, 2015 and 2014, our advertising expenses were immaterial. When our sales representatives make contact with a
customer, we will generally offer to supply the customer our products at fixed prices. If accepted, the customer’s purchasing
department will coordinate the purchase, receipt and distribution of the products throughout its distribution centers and retail outlets.
Once a customer accepts our supply of a product, the customer typically expects a high standard of service, including timely receipt of
products ordered, availability of convenient, user-friendly and effective customer service functions and maintaining open lines of
communication.
We believe that retail-level consumer demand dictates the total volume of sales for various products. In the event that wholesale and
retail customers adjust their purchasing volumes, we believe that consumer demand will be fulfilled by other wholesale or retail
sources of supply. As a result, we attempt to develop and maintain strong relationships with most of the major retail chains, wholesale
distributors and mail-order pharmacies in order to facilitate the supply of our products through whatever channel the consumer prefers.
Although we have agreements with customers governing the transaction terms of our sales, generally there are no minimum purchase
quantities applicable to these agreements.
Competition
The manufacturing and distribution of generic pharmaceutical products is a highly competitive industry. Competition is based
primarily on price. In addition to competitive pricing, our competitive advantages are our ability to provide strong and dependable
customer service by maintaining adequate inventory levels, employing a responsive order filling system and prioritizing timely
fulfillment of orders. We ensure that our products are available from national suppliers as well as our own warehouse. The
modernization of our facilities, hiring of experienced staff and implementation of inventory and quality control programs have
improved our competitive cost position.
We compete with other manufacturers and marketers of generic and brand-name drugs. Each product manufactured and/or sold by us
has a different set of competitors. The list below identifies the companies with which we primarily compete with respect to each of
our major products:
Product
Acetazolomide Tablets
Primary Competitors
Taro
Butalbital, Acetaminophen and Caffeine Tablets
Mallinckrodt, Mikart, Qualitest, Watson and
West-Ward
Butalbital with Aspirin and Caffeine, with and without Codeine Phosphate Capsules Actavis and Breckenridge
C-Topical® Solution
Digoxin Tablets
Levothyroxine Sodium Tablets
Methylphenidate ER Tablets
Omeprazole Capsules
Ursodiol Capsules
Compounding pharmacies and alternative
drugs
Mylan, Impax, West-Ward, Sun and
Concordia
AbbVie, Pfizer, Mylan and Sandoz
Janssen, Mallinckrodt and Actavis
Sandoz, Dr. Reddy’s and Zydus
Epic, Mylan and Actavis
Government Regulation
Pharmaceutical manufacturers are subject to extensive regulation by the federal government, principally by the FDA and, in cases of
controlled substance products the DEA and to a lesser extent by other federal regulatory bodies and state governments. The Federal
Food, Drug and Cosmetic Act (the “FDCA”), the Controlled Substance Act (the “CSA”) and other federal statutes and regulations
govern or influence the testing, manufacture, safety, labeling, storage, record keeping, approval, pricing, advertising and promotion of
our generic drug products. Non-compliance with applicable regulations can result in fines, product recalls and seizure of products,
total or partial suspension of production, personal and/or corporate prosecution and debarment and refusal of the government to
approve new drug applications. The FDA also has the authority to revoke previously approved drug applications after a hearing.
Generally, FDA approval is required before a prescription drug can be marketed. A new drug is one not generally recognized by
qualified experts as safe and effective for its intended use. New drugs are typically developed and submitted to the FDA by
companies expecting to brand the product and sell it. The FDA review process for new drugs is very extensive and requires a
substantial investment to research and test the drug candidate. However, less burdensome approval procedures are generally used for
generic equivalents. Typically, the investment required to develop a generic drug is less costly than the innovator drug.
There are currently three ways to obtain FDA approval of a drug:
• New Drug Applications (NDA): Unless one of the two procedures discussed in the following sections is available, a
manufacturer must conduct and submit to the FDA complete clinical studies to establish a drug’s safety and efficacy. The
new drug approval process generally involves:
•
•
•
•
•
completion of preclinical laboratory and animal testing in compliance with the FDA’s GLP regulations;
submission to the FDA of an Investigational New Drug (“IND”) application for human clinical testing, which
must become effective before human clinical trials may begin;
performance of adequate and well-controlled human clinical trials to establish the safety and efficacy of the
proposed drug product for each intended use;
satisfactory completion of an FDA pre-approval inspection of the facility or facilities at which the product is
produced to assess compliance with the FDA’s cGMP regulations; and
submission to and approval by the FDA of an NDA.
The results of preclinical tests, together with manufacturing information and analytical data, are submitted to the
FDA as part of an IND, which must become effective before human clinical trials may begin. Further, each clinical
trial must be reviewed and approved by an independent Institutional Review Board. Human clinical trials are
typically conducted in three sequential phases that may overlap. These phases generally include:
• Phase I, during which the drug is introduced into healthy human subjects or, on occasion, patients and is tested
for safety, stability, dose tolerance and metabolism;
• Phase II, during which the drug is introduced into a limited patient population to determine the efficacy of the
product in specific targeted indications, to determine dosage tolerance and optimal dosage and to identify
possible adverse effects and safety risks; and
• Phase III, during which the clinical trial is expanded to a larger and more diverse patient group at
geographically dispersed clinical trial sites to further evaluate clinical efficacy, optimal dosage and safety.
The drug sponsor, the FDA, or the independent Institutional Review Board at each institution at which a clinical trial
is being performed may suspend a clinical trial at any time for various reasons, including a belief that the subjects
are being exposed to an unacceptable health risk.
The results of preclinical animal studies and human clinical studies, together with other detailed information, are
submitted to the FDA as part of the NDA. The NDA also must contain extensive manufacturing information. The
FDA may disapprove the NDA if applicable FDA regulatory criteria are not satisfied or it may require additional
clinical data. Once approved, the FDA may withdraw the product approval if compliance with pre- and post-market
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�regulatory standards is not maintained or if problems occur or are identified after the product reaches the
marketplace. In addition, the FDA may require post-marketing studies to monitor the effect of approved products
and may limit further marketing of the product based on the results of these post-marketing studies.
The FDA has broad post-market regulatory and enforcement powers, including the ability to levy fines and civil
penalties, suspend or delay issuance of approvals, seize or recall products and withdraw approvals.
Satisfaction of FDA new drug approval requirements typically takes several years and the actual time required may
vary substantially based upon the type, complexity and novelty of the product or disease. Government regulation
may delay or prevent marketing of potential products for a considerable period of time and/or require additional
procedures which increase manufacturing costs. Success in early stage clinical trials does not assure success in later
stage clinical trials. Data obtained from clinical activities is not always conclusive and may be subject to varying
interpretations that could delay, limit, or prevent regulatory approval. Even if a product receives regulatory
approval, later discovery of previously unknown problems with a product may result in restrictions on the product or
even complete withdrawal of the product from the market.
•
Abbreviated New Drug Applications: An ANDA is similar to an NDA except that the FDA generally waives the requirement
of complete clinical studies of safety and efficacy. However, it may require bioavailability and bioequivalence studies.
Bioavailability indicates the rate of absorption and levels of concentration of a drug in the bloodstream needed to produce a
therapeutic effect. Bioequivalence compares one drug product with another and indicates if the rate of absorption and the
levels of concentration of a generic drug in the body are within prescribed statistical limits to those of a previously approved
drug. Under the Hatch-Waxman Act, an ANDA may be submitted for a drug on the basis that it is the equivalent of an
approved drug regardless of when such other drug was approved. The FDA will approve the generic product as suitable for
an ANDA application if it finds that the generic product does not raise new questions of safety and effectiveness as compared
to the innovator product. A product is not eligible for ANDA approval if the FDA determines that it is not equivalent to the
referenced innovator drug, if it is intended for a different use, or if it is not subject to an approved Suitability Petition.
However, such a product might be approved under an NDA, with supportive data from clinical trials.
In addition to establishing a new ANDA procedure, the Hatch-Waxman Act created statutory protections for approved brand-
name drugs. Under the Hatch-Waxman Act, an ANDA for a generic drug may not be made effective until all relevant
product and use patents for the brand-name drug have expired or have been determined to be invalid. Prior to this act, the
FDA gave no consideration to the patent status of a previously approved drug. Upon NDA approval, the FDA lists in its
Orange Book the approved drug product and any patents identified by the NDA applicant that relate to the drug product. Any
applicant who files an ANDA seeking approval of a generic equivalent version of a drug listed in the FDA’s Orange Book
before expiration of the referenced patent(s), must certify to the FDA that (1) no patent information on the drug product that
is the subject of the ANDA has been submitted to the FDA; (2) such patent has expired; (3) the date on which such patent
expires; or (4) such patent is invalid or will not be infringed upon by the manufacture, use, or sale of the drug product for
which the ANDA is submitted.
This last certification is known as a paragraph IV certification. A notice of the paragraph IV certification must be provided to
each owner of the patent that is the subject of the certification and to the holder of the approved NDA to which the ANDA
refers. Before the enactment of the Medicare Prescription Drug Improvement and Modernization Act of 2003 (the “MMA”),
which amended the Hatch-Waxman Act, if the NDA holder or patent owner(s) asserted a patent challenge within 45 days of
its receipt of the certification notice, the FDA was prevented from approving that ANDA until the earlier of 30 months from
the receipt of the notice of the paragraph IV certification, the expiration of the patent, when the infringement case concerning
each such patent was favorably decided in an ANDA applicant’s favor, or such shorter or longer period as may be ordered by
a court. This prohibition is generally referred to as the 30-month stay. In some cases, NDA owners and patent holders have
obtained additional patents for their products after an ANDA had been filed but before that ANDA received final marketing
approval and then initiated a new patent challenge, which resulted in more than one 30-month stay. The MMA amended the
Hatch-Waxman Act to eliminate certain unfair advantages of patent holders in the implementation of the Hatch-Waxman Act.
As a result, the NDA owner remains entitled to an automatic 30-month stay if it initiates a patent infringement lawsuit within
45 days of its receipt of notice of a paragraph IV certification, but only if the patent infringement lawsuit is directed to
patents that were listed in the FDA’s Orange Book before the ANDA was filed. An ANDA applicant is now permitted to
take legal action to enjoin or prohibit the listing of certain of these patents as a counterclaim in response to a claim by the
NDA owner that its patent covers its approved drug product. As of June 30, 2016, we have 12 paragraph IV certifications
pending with the FDA. Four of the paragraph IV certifications are currently being challenged. In response to our paragraph
IV certification with respect to the Zomig® nasal spray product, AstraZeneca AB, AstraZeneca UK Limited and Impax
Laboratories, Inc. filed two patent infringement complaints against the Company in July 2014. In response to our paragraph
IV certification with respect to Thalomid®, Celegene Corporation and Children’s Medical Center Corporation filed a patent
infringement lawsuit against the Company in January 2015. In response to our paragraph IV certification with respect to
Dilaudid®, Purdue Pharmaceutical Products L.P, Purdue Pharma L.P and Purdue Pharma Technologies Inc. filed a patent
infringement lawsuit against the Company in August 2015. The Company is in various stages of responding to the patent
infringement claims; and in the case of Dilaudid, a settlement has been reached in principle and details are being finalized.
Refer to Note 12 “Legal and Regulatory Matters” for additional information.
If an ANDA applicant is the first-to-file a substantially complete ANDA with a paragraph IV certification and provides
appropriate notice to the FDA, the NDA holder and all patent owner(s) for a particular generic product, the applicant may be
awarded a 180-day period of marketing exclusivity against other companies that subsequently file ANDAs for that same
product. A substantially complete ANDA is one that contains all the information required by the Hatch-Waxman Act and the
FDA’s regulations, including the results of any required bioequivalence studies. The FDA may refuse to accept the filing of
an ANDA that is not substantially complete or may determine during substantive review of the ANDA that additional
information, such as an additional bioequivalence study, is required to support approval.
Such a determination may affect an applicant’s first-to-file status and eligibility for a 180-day period of marketing exclusivity
for the generic product. The MMA also modified the rules governing when the 180-day marketing exclusivity period is
triggered or forfeited and shared. Prior to the legislation, the 180-day marketing exclusivity period was triggered upon the
first commercial marketing of the ANDA or a court decision holding the patent invalid, unenforceable, or not infringed. For
ANDAs accepted for filing before March 2000, that court decision had to be final and non-appealable (other than a petition to
the U.S. Supreme Court for a writ of certiorari). In March 2000, the FDA changed its position in response to two court cases
that challenged the FDA’s original interpretation of what constituted a court decision under the Hatch-Waxman Act. Under
the changed policy, the 180-day marketing exclusivity period began running immediately upon a district court decision
holding the patent at issue invalid, unenforceable, or not infringed, regardless of whether the ANDA had been approved and
the generic product had been marketed. In codifying the FDA’s original policy, the MMA retroactively applies a final and
non-appealable court decision trigger for all ANDAs filed before December 8, 2003 leaving intact the first commercial
marketing trigger. As for ANDAs filed after December 8, 2003, the marketing exclusivity period is only triggered upon the
first commercial marketing of the ANDA product, but that exclusivity may be forfeited under certain circumstances,
including, if the ANDA is not marketed within 75 days after a final and non-appealable court decision by the first-to-file or
other ANDA applicant, or if the FDA does not tentatively approve the first-to-file applicant’s ANDA within 30 months.
In addition to patent exclusivity, the holder of the NDA for the listed drug may be entitled to a period of non-patent market
exclusivity, during which the FDA cannot approve an ANDA. If the listed drug is a new chemical entity (“NCE”), the FDA
may not accept an ANDA for a bioequivalent product for up to five years following approval of the NDA for the NCE. If the
listed drug is not a new chemical entity but the holder of the NDA conducted clinical trials essential to approval of the NDA
or a supplement thereto, the FDA may not approve an ANDA for a bioequivalent product before expiration of three years.
Certain other periods of exclusivity may be available if the listed drug is indicated for treatment of a rare disease or is studied
for pediatric indications.
•
Section 505(b)(2) New Drug Applications: For a drug that is identical to a previously approved drug, a prospective
manufacturer need not go through the full NDA procedure. Instead, it may demonstrate safety and efficacy by relying on
published literature and reports where at least some of information required for approval comes from studies not conducted
by or for the applicant and for which the applicant has not obtained a right of reference. The Hatch-Waxman Act permits the
applicant to rely upon certain preclinical or clinical studies conducted for an approved product. The manufacturer must also
submit, if the FDA so requires, bioavailability or bioequivalence data illustrating that the generic drug formulation produces
the same effects, within an acceptable range, as the previously approved innovator drug. Because published literature to
support the safety and efficacy of post-1962 drugs may not be available, this procedure is of limited utility to generic drug
manufacturers and the resulting approved product will not be interchangeable with the innovator drug as an ANDA drug
would be unless bioequivalency testing were undertaken and approved by FDA. Moreover, the utility of
Section 505(b)(2) applications have with the exception of “Grandfathered drugs” been diminished by the availability of the
ANDA process, as described above.
Additionally, certain products marketed prior to the FDCA may be considered GRASE (“Generally Recognized As Safe and
Effective”) or Grandfathered. GRASE products are those “old drugs that do not require prior approval from FDA in order to be
marketed because they are generally recognized as safe and effective based on published scientific literature.” Similarly,
Grandfathered products are those which “entered the market before the passage of the 1938 act or the 1962 amendments to the act.”
Under the grandfather clause, such a product is exempted from the “effectiveness requirements [of the act] if its composition and
labeling have not changed since 1962 and if, on the day before the 1962 amendments became effective, it was (1) used or sold
commercially in the United States, (2) not a new drug as defined by the act at that time and (3) not covered by an effective
application.”
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�Manufacturing cGMP Requirements
Among the requirements for a new drug approval, a company’s manufacturing methods must conform to FDA cGMP regulations
before a facility may be used to manufacture a product. The FDA performs pre-approval inspections to assess a company’s
manufacturing methods as part of a new drug approval process. These inspections include reviews of procedures and operations used
in the manufacture and testing of our products to assess compliance with application regulations. The cGMP regulations must be
followed at all times during which the approved drug is manufactured and the manufacturing facilities are subject to periodic
inspections by the FDA and other authorities. FDA’s cGMP regulations require, among other things, quality control and quality
assurance as well as the corresponding maintenance of records and documentation. In complying with the standards set forth in the
cGMP regulations, we must continue to expend time, money and effort in the areas of production and quality control to ensure full
technical compliance.
Failure to comply with statutory and regulatory requirements subject a manufacturer to possible legal or regulatory action, including
but not limited to, the seizure or recall of non-complying drug products, injunctions, consent decrees placing significant restrictions on
or suspending manufacturing operations and/or civil and criminal penalties. Adverse experiences with the product must be reported to
the FDA and could result in the imposition of market restriction through labeling changes or in product removal. Product approvals
may be withdrawn if compliance with regulatory requirements is not maintained or if problems concerning safety or efficacy of the
product occur following approval.
Other Regulatory Requirements
With respect to post-market product advertising and promotion, the FDA imposes a number of complex regulations on entities that
advertise and promote pharmaceuticals, which include, among others, standards for direct-to-consumer advertising, off-label
promotion, industry-sponsored scientific and educational activities and promotional activities involving the internet. The FDA has
very broad enforcement authority under the FDCA and failure to abide by these regulations can result in penalties, including the
issuance of a warning letter directing entities to correct deviations from FDA standards, a requirement that future advertising and
promotional materials be pre-cleared by the FDA and state and/or federal civil and criminal investigations and prosecutions.
We are also subject to various laws and regulations regarding laboratory practices, the experimental use of animals and the use and
disposal of hazardous or potentially hazardous substances in connection with our research. In each of these areas, as above, the FDA
has broad regulatory and enforcement powers, including the ability to levy fines and civil penalties, suspend or delay issuance of
approvals, seize or recall products and withdraw approvals. Any one or a combination of FDA regulatory or enforcement actions
against the Company could have a material adverse effect on our financial results.
DEA Regulation
We maintain registrations with the DEA that enable us to receive, manufacture, store and distribute controlled substances in
connection with our operations. Controlled substances are those drugs that appear on one of five schedules promulgated and
administered by the DEA under the CSA. The CSA governs, among other things, the distribution, recordkeeping, handling, security
and disposal of controlled substances. We are subject to periodic and ongoing inspections by the DEA and similar state drug
enforcement authorities to assess our ongoing compliance with the DEA’s regulations. Any failure to comply with these regulations
could lead to a variety of sanctions, including the revocation or a denial of renewal of our DEA registration, injunctions, or civil or
criminal penalties.
arrangements, payment of cash and waivers of payments. Several courts have interpreted the statute’s intent requirement to mean that
if any one purpose of an arrangement involving remuneration is to induce referrals of federal health care covered business, the statute
has been violated. Penalties for violations include criminal penalties and civil sanctions such as fines, imprisonment and possible
exclusion from Medicare, Medicaid and other federal health care programs. In addition, some kickback allegations have been claimed
to violate the Federal False Claims Act, discussed in more detail below.
The Anti-Kickback Statute is broad and prohibits many arrangements and practices that are lawful in businesses outside of the health
care industry. Recognizing that the Anti-Kickback Statute is broad and may technically prohibit many innocuous or beneficial
arrangements, Congress authorized the Office of Inspector General of the U.S. Department of Health and Human Services (“OIG”) to
issue a series of regulations, known as “safe harbors.” These safe harbors, issued by the OIG beginning in July 1991, set forth
provisions that, if all their applicable requirements are met, will assure health care providers and other parties that they will not be
prosecuted under the Anti-Kickback Statute. The failure of a transaction or arrangement to fit precisely within one or more safe
harbors does not necessarily mean that it is illegal or that prosecution will be pursued.
However, conduct and business arrangements that do not fully satisfy each applicable safe harbor may result in increased scrutiny by
government enforcement authorities such as OIG.
Many states have adopted laws similar to the Anti-Kickback Statute. Some of these state prohibitions apply to referral of patients for
health care items or services reimbursed by any source, not only the Medicare and Medicaid programs.
Government officials have focused their enforcement efforts on marketing of health care services and products, among other activities
and recently have brought cases against companies and certain sales, marketing and executive personnel, for allegedly offering
unlawful inducements to potential or existing customers in an attempt to procure their business.
Another development affecting the health care industry is the increased use of the Federal False Claims Act (“FFCA”) and in
particular, action brought pursuant to the FFCA’s “Whistleblower” or “Qui Tam” provisions. The FFCA imposes liability on any
person or entity who, among other things, knowingly presents, or causes to be presented, a false or fraudulent claim for payment by a
federal health care program. The Qui Tam provisions of the FFCA allow a private individual to bring actions on behalf of the federal
government alleging that the defendant has submitted a false claim to the federal government and to share in any monetary recovery.
In recent years, the number of suits brought against health care providers by private individuals has increased dramatically. In
addition, various states have enacted false claims law analogous to the FFCA, although many of these state laws apply where a claim
is submitted to any third-party payer and not merely a federal health care program.
When an entity is determined to have violated the FFCA, it may be required to pay up to three times the actual damages sustained by
the government, plus civil penalties. Liability arises, primarily, when an entity knowingly submits or causes another to submit a false
claim for reimbursement to the federal government. The federal government has used the FFCA to assert liability on the basis of
inadequate care, kickbacks and other improper referrals and improper use of Medicare numbers when detailing the provider of
services, in addition to the more predictable allegations as to misrepresentations with respect to the services rendered. In addition, the
federal government has prosecuted companies under the FFCA in connection with off-label promotion of products. Our future
activities relating to the reporting of wholesale or estimated retail prices of our products, the reporting of discount and rebate
information and other information affecting federal, state and third-party reimbursement of our products and the sale and marketing of
our products may be subject to scrutiny under these laws. We are unable to predict whether we will be subject to actions under the
FFCA or a similar state law, or the impact of such actions. However, the costs of defending such claims, as well as any sanctions
imposed, could significantly affect our financial performance.
Fraud and Abuse Laws
Foreign Corrupt Practices Act
Because of the significant federal funding involved in Medicare and Medicaid, Congress and state legislatures have enacted and
actively enforce, a number of laws whose purpose is to eliminate fraud and abuse in federal health care programs. Our business is
subject to compliance with these laws, such as Sarbanes-Oxley Act of 2002, Dodd-Frank and the Foreign Corrupt Practices Act
(“FCPA”).
The Foreign Corrupt Practices Act of 1977, as amended (“FCPA”), was enacted for the purpose of making it unlawful for certain
classes of persons and entities to make payments to foreign government officials to assist in obtaining or retaining business.
Specifically, the anti-bribery provisions of the FCPA prohibit the bribery of government officials.
Anti-Kickback Statutes, Sunshine Act and Federal False Claims Act
The federal health care programs fraud and abuse law (sometimes referred to as the “Anti-Kickback Statue”) prohibits persons from
knowingly and willfully soliciting, offering, receiving, or providing remuneration, directly or indirectly, in exchange for or to induce
either the referral of an individual, or the furnishing or arranging for a good or service, for which payment may be made under a
federal health care program such as Medicare or Medicaid. The definition of “remuneration” has been broadly interpreted to include
anything of value, including for example gifts, certain discounts, the furnishing of free supplies, equipment or services, credit
HIPAA and Other Fraud and Privacy Regulations
The Health Insurance Portability and Accountability Act of 1996 (“HIPAA”) created two new federal crimes: health care fraud and
false statements relating to health care matters. The HIPAA health care fraud statute prohibits, among other things, knowing and
willfully executing, or attempting to execute, a scheme to defraud any health care benefit program, including private payors. A
violation of this statute is a felony and may result in fines, imprisonment and/or exclusion from government-sponsored programs. The
HIPAA false statements statute prohibits knowingly and willfully falsifying, concealing, or covering up a material fact or making any
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�materially false, fictitious, or fraudulent statement or representation in connection with the delivery of or payment for health care
benefits, items, or services. A violation of this statute is a felony and may result in fines and/or imprisonment.
currently believes that it has acted in compliance with all applicable laws and regulations and continues to cooperate with the federal
investigation.
Pricing
Other Applicable Laws
We are also subject to federal, state and local laws of general applicability, including laws regulating working conditions and the
storage, transportation, or discharge of items that may be considered hazardous substances, hazardous waste, or environmental
contaminants. We monitor our compliance with laws and we believe we are in substantial compliance with all regulatory bodies.
As a publicly-traded company, we are also subject to significant regulations and laws, included in the Sarbanes-Oxley Act of 2002.
Since its enactment, we have developed and instituted a corporate compliance program based on what we believe are the current best
practices and we continue to update the program in response to newly implemented or changing regulatory requirements.
Employees
As of June 30, 2016, we had 1,149 employees.
Securities and Exchange Act Reports
We maintain a website at www.lannett.com. We make available on or through our website our current and periodic reports, including
any amendments to those reports, that are filed with the Securities and Exchange Commission (the “SEC”) in accordance with the
Securities Exchange Act of 1934, as amended (the “Exchange Act”). These reports include annual reports on Form 10-K, quarterly
reports on Form 10-Q and current reports on Form 8-K. This information is available on our website free of charge as soon as
reasonably practicable after we electronically file the information with, or furnish it to, the SEC. The contents of our website are not
incorporated by reference in this Form 10-K and shall not be deemed “filed” under the Exchange Act.
In the United States, our sales are dependent upon the availability of coverage and reimbursement for our products from third-party
payors, including federal and state programs such as Medicare and Medicaid and private organizations such as commercial health
insurance and managed care companies. Such third-party payors increasingly challenge the price of medical products and services
and instituting cost containment measures to control or significantly influence the purchase of medical products and services.
Over the past several years, the rising costs of providing health care services has triggered legislation to make certain changes to the
way in which pharmaceuticals are covered and reimbursed, particularly by government programs. For instance, recent federal
legislation and regulations have created a voluntary prescription drug benefit, Medicare Part D, which revised the formula used to
reimburse health care providers and physicians under Medicare Part B and imposed significant revisions to the Medicaid Drug Rebate
Program. These changes have resulted in and may continue to result in, coverage and reimbursement restrictions and increased rebate
obligations by manufacturers.
In addition, there continues to be legislative and regulatory proposals at the federal and state levels directed at containing or lowering
the cost of health care. Examples of how limits on drug coverage and reimbursement in the United States may cause reduced
payments for drugs in the future include:
•
•
•
•
•
changing Medicare reimbursement methodologies;
revising drug rebate calculations under the Medicaid program;
reforming drug importation laws;
fluctuating decisions on which drugs to include in formularies; and
requiring pre-approval of coverage for new or innovative drug therapies.
We cannot predict the likelihood or pace of such additional changes or whether there will be significant legislative or regulatory
reform impacting our products, nor can we predict with precision what effect such governmental measures would have if they were
ultimately enacted into law. However, in general, we believe that legislative and regulatory reform activity likely will continue.
Current or future federal or state laws and regulations may influence the prices of drugs and, therefore, could adversely affect the
prices that we receive for our products. Programs in existence in certain states seek to set prices of all drugs sold within those states
through the regulation and administration of the sale of prescription drugs. Expansion of these programs, in particular, state Medicaid
programs, or changes required in the way in which Medicaid rebates are calculated under such programs, could adversely affect the
price we receive for our products and could have a material adverse effect on our business, results of operations and financial
condition. Further, generic pharmaceutical drug prices have been the focus of increased scrutiny by certain states’ attorney generals,
the U.S. Department of Justice and Congress. Decreases in health care reimbursements or prices of our prescription drugs could limit
our ability to sell our products or decrease our revenues, which could have a material adverse effect on our business, results of
operations and financial condition.
The Company believes that under the current regulatory environment, the generic pharmaceutical industry as a whole will be the target
of increased governmental scrutiny, especially with respect to state and federal anti-trust and price fixing claims.
In July 2014, the Company and at least one of its competitors each received a subpoena and interrogatories from the Connecticut
Attorney General’s Office concerning its investigation into the pricing of Digoxin. In June 2016, the Connecticut Attorney General
issued interrogatories and a subpoena to an employee of the Company. The Company maintains that it acted in compliance with all
applicable laws and regulations and continues to cooperate with the Connecticut Attorney General’s investigation.
In Fiscal 2015, the Company and certain affiliated individuals each were served with a grand jury subpoena relating to a federal
investigation of the generic pharmaceutical industry into possible violations of the Sherman Act. The subpoenas request corporate
documents of the Company relating to corporate, financial and employee information, communications or correspondence with
competitors regarding the sale of generic prescription medications and the marketing, sale, or pricing of certain products, generally for
the period of 2005 through the dates of the subpoenas. Based on reviews performed to date by outside counsel, the Company
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�ITEM 1A.
RISK FACTORS
General Risks Relating to the Company
We materially rely on an uninterrupted supply of finished products from JSP for a significant amount of our sales. If we were
to experience an interruption of that supply, our operating results would suffer.
In fiscal year 2016, 35% of our total net sales are of distributed products manufactured by JSP. Two of these products are
Levothyroxine Sodium and Digoxin, which accounted for 30% and 4%, respectively, of our Fiscal 2016 total net sales and 38% and
12%, respectively, of our total net sales for Fiscal 2015. On August 19, 2013, the Company entered into an agreement with JSP to
extend its initial contract to continue as the exclusive distributor in the United States of three JSP products: Butalbital, Aspirin,
Caffeine with Codeine Phosphate Capsules USP; Digoxin Tablets USP; and Levothyroxine Sodium Tablets USP. The amendment to
the original agreement extended the initial contract, which was due to expire on March 22, 2014, for five years through March 2019.
Both Lannett and JSP have the right to terminate the contract if one of the parties does not cure a material breach of the contract
within thirty (30) days of notice from the non-breaching party. If the supply of these products is interrupted in any way by any form
of temporary or permanent business interruption to JSP, including but not limited to fire or other naturally-occurring, damaging event
to their physical plant and/or equipment, condemnation of their facility, legislative or regulatory cease and desist declaration regarding
their operations, FDA action and any interruption in their source of API for their products, our operating results could be materially
adversely affected. We do not have, at this time, a second source for these products.
Our gross profit may fluctuate from period to period depending upon our product sales mix, our product pricing and our
costs to manufacture or purchase products.
Our future results of operations, financial condition and cash flows depend to a significant extent upon our product sales mix. Sales of
certain products that we manufacture tend to create higher gross margins than the products we purchase and resell. As a result, our
sales mix will significantly impact our gross profit from period to period.
Factors that may cause our sales mix to vary include:
•the number of new product introductions;
•marketing exclusivity, if any, which may be obtained on certain new products;
•the level of competition in the marketplace for certain products;
•the availability of raw materials and finished products from our suppliers; and
•the scope and outcome of governmental regulatory action that may involve us.
The Company is continuously seeking to keep product costs low, however there can be no guarantee that gross profit percentages will
stay consistent in future periods. Pricing pressure from competitors, changes in product mix and the costs of producing or purchasing
new drugs may also fluctuate in future periods.
Acquisitions could result in operating difficulties, dilution and other harmful consequences that may adversely impact our
business and results of operations.
Acquisitions are an important element of our overall corporate strategy and use of capital and we expect our current pace of
acquisitions to continue or increase. These transactions could be material to our financial condition and results of operations. We also
expect to continue to evaluate and enter into discussions regarding a wide array of potential strategic transactions. The process of
integrating an acquired company, business, or technology may create unforeseen operating difficulties and expenditures. The areas
where we may face risks include but are not limited to (i) diversion of management time and focus from operating our business to
acquisition integration challenges, (ii) implementation or remediation of controls, procedures and policies at the acquired company,
(iii) integration of the acquired company’s accounting, human resource and other administrative systems and coordination of product,
engineering and sales and marketing functions, (iv) transition of operations, users and customers onto our existing platforms,
(v) failure to obtain required approvals from governmental authorities under competition and antitrust laws on a timely basis, if at all,
which could, among other things, delay or prevent us from completing a transaction, or otherwise restrict our ability to realize the
expected financial or strategic goals of an acquisition, (vi) cultural challenges associated with integrating employees from the acquired
company into our organization and retention of employees from the businesses we acquire and (vii) liability for activities of the
acquired company before the acquisition, including infringement claims, violations of laws, commercial disputes, tax liabilities, claims
from current and former employees and customers and other known and unknown liabilities.
Our failure to address these risks or other problems encountered in connection with our past or future acquisitions could cause us to
fail to realize the anticipated benefits of such acquisitions, incur unanticipated liabilities and harm our business generally. Future
acquisitions could also result in dilutive issuances of our equity securities, the incurrence of debt, contingent liabilities, or amortization
expenses, or write-offs of goodwill, any of which could harm our financial condition. Also, the anticipated benefit of many of our
acquisitions may not materialize.
The generic pharmaceutical industry is highly competitive.
We face strong competition in our generic product business. Revenues and gross profit derived from the sales of generic
pharmaceutical products tend to follow a pattern based on certain regulatory and competitive factors. As patents for brand-name
products and related exclusivity periods expire or fall under patent challenges, the first generic manufacturer to receive regulatory
approval for generic equivalents of such products is generally able to achieve significant market penetration. As competing off-patent
manufacturers receive regulatory approvals on similar products or as brand manufacturers launch generic versions of such products
(for which no separate regulatory approval is required), market share, revenues and gross profit typically decline, in some cases
dramatically. Accordingly, the level of market share, revenue and gross profit attributable to a particular generic product is normally
related to the number of competitors in that product’s market and the timing of that product’s regulatory approval and launch, in
relation to competing approvals and launches. Consequently, we must continue to develop and introduce new products in a timely and
cost-effective manner to maintain our revenues and gross margins.
Extensive industry regulation has had and will continue to have, a significant impact on our business in the area of cost of
goods, especially our product development, manufacturing and distribution capabilities.
All pharmaceutical companies, including Lannett, are subject to extensive, complex, costly and evolving regulation by the federal
government, including the FDA and in the case of controlled drugs, the DEA and state government agencies. The FDCA, the CSA
and other federal statutes and regulations govern or influence the development, testing, manufacturing, packing, labeling, storing,
record keeping, safety, approval, advertising, promotion, sale and distribution of our products.
The process for obtaining governmental approval to manufacture and market pharmaceutical products is rigorous, time-consuming and
costly and we cannot predict the extent to which we may be affected by legislative and regulatory developments. We are dependent
on receiving FDA and other governmental or third-party approvals prior to manufacturing, marketing and shipping our products. The
FDA approval process for a particular product candidate can take several years and requires us to dedicate substantial resources to
securing approvals and we may not be able to obtain regulatory approval for our product candidates in a timely manner, or at all. In
order to obtain approval for our generic product candidates, we must demonstrate that our drug product is bioequivalent to a drug
previously approved by the FDA through the drug approval process, known as an innovator drug. Bioequivalency may be
demonstrated in vivo or in vitro by comparing the generic product candidate to the innovator drug product in dosage form, strength,
route of administration, quality, dissolution performance characteristics and intended use. The FDA may not agree that the
bioequivalence studies we submit in the ANDA applications for our generic drug products are adequate to support approval. If it
determines that an ANDA application is not adequate to support approval, the FDA could deny our application or request additional
information, including clinical trials, which could delay approval of the product and impair our ability to compete with other versions
of the generic drug product.
Consequently, there is always the chance that we will not obtain FDA or other necessary approvals, or that the rate, timing and cost of
such approvals will adversely affect our product introduction plans or results of operations. We carry inventories of certain products
in anticipation of launch and if such products are not subsequently launched, we may be required to write-off the related inventory.
Furthermore, the FDA also has the authority to revoke drug approvals previously granted and remove these products from the market
for a variety of reasons, including a failure to comply with applicable regulations, the discovery of previously unknown problems with
the product, or because the ingredients in the drug are no longer approved by the FDA.
Additionally, certain products marketed prior to the FDCA may be considered GRASE or Grandfathered. GRASE products are those
“old drugs that do not require prior approval from FDA in order to be marketed because they are generally recognized as safe and
effective based on published scientific literature.” Similarly, Grandfathered products are those which “entered the market before the
passage of the 1906 Act, 1938 Act or the 1962 amendments to the Act.” Under the Grandfathered drug clause, such a product is
exempted from the “effectiveness requirements [of the act] if its composition and labeling have not changed since 1962 and if, on the
day before the 1962 amendments became effective, it was (1) used or sold commercially in the United States, (2) not a new drug as
defined by the act at that time and (3) not covered by an effective application.” Recently, the FDA has increased its efforts to force
companies to file and seek FDA approval for GRASE or Grandfathered products. Efforts have included issuing notices to companies
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�currently producing these products to cease its distribution of said products. Lannett currently manufactures and markets one product
that is considered a GRASE or Grandfathered product, C-Topical® Solution. The Company has completed the Phase III clinical trial
and our CRO is assembling the data for our New Drug Application. The FDA is currently undertaking activities to force all
companies who manufacture certain GRASE products to file applications and seek approval for these products or remove their
products from the market.
In addition, we, as well as many of our significant suppliers of distributed product and raw materials, are subject to periodic inspection
of facilities, procedures and operations and/or the testing of the finished products by the FDA, the DEA and other authorities, which
conduct periodic inspections to confirm that pharmaceutical companies are in compliance with all applicable regulations. The FDA
conducts pre-approval and post-approval reviews and plant inspections to determine whether systems and processes are in compliance
with cGMP and other FDA regulations. Following such inspections, the FDA may issue notices on Form 483 that could cause us or
our suppliers to modify certain activities identified during the inspection. A Form 483 notice is generally issued at the conclusion of a
FDA inspection and lists conditions the FDA inspectors believe may violate cGMP or other FDA regulations. The DEA and
comparable state-level agencies also heavily regulate the manufacturing, holding, processing, security, record-keeping and distribution
of drugs that are considered controlled substances. Some of the pain management products we manufacture contain controlled
substances. The DEA periodically inspects facilities for compliance with its rules and regulations. If our manufacturing facilities or
those of our suppliers fail to comply with applicable regulatory requirements, it could result in regulatory action and additional costs.
Our inability or the inability of our suppliers to comply with applicable FDA and other regulatory requirements can result in, among
other things, delays in or denials of new product approvals, warning letters, fines, consent decrees restricting or suspending
manufacturing operations, injunctions, civil penalties, recall or seizure of products, total or partial suspension of sales and/or criminal
prosecution. Any of these or other regulatory actions could materially harm our operating results and financial condition. Although
we have instituted internal compliance programs, if these programs do not meet regulatory agency standards or if compliance is
deemed deficient in any significant way, it could materially harm our business. Additionally, if the FDA were to undertake additional
enforcement activities with Lannett’s GRASE product, their actions could result in, among other things, removal of some of the
product from the market, seizure of the product and total or partial suspension of sales. Any of these regulatory actions could
materially harm our operating results and financial condition.
Our manufacturing operations as well as our suppliers manufacturing operations are subject to licensing by the FDA and/or
DEA. If we or our suppliers are unable to maintain the proper agency licensing arrangements, our operating results would be
materially negatively impacted.
All of our manufacturing operations as well as those of our suppliers rely on maintaining active licenses to produce and develop
generic drugs. Specifically, our Cody Labs operations rely on a DEA license to directly import and convert raw concentrated poppy
straw into several APIs or dosage forms. This license is granted for a one year period and must be renewed successfully each year in
order for us to maintain Cody’s current operations and allow the Company to continue to work towards becoming a fully integrated
narcotics supplier. If the Company is unable to successfully renew its FDA and/or DEA licenses, the financial results of Lannett
would be negatively impacted.
If we are unable to successfully develop or commercialize new products, our operating results will suffer.
Our future results of operations will depend to a significant extent upon our ability to successfully commercialize new generic
products in a timely manner. There are numerous difficulties in developing and commercializing new products, including:
•developing, testing and manufacturing products in compliance with regulatory standards in a timely manner;
•receiving requisite regulatory approvals for such products in a timely manner;
•the availability, on commercially reasonable terms, of raw materials, including APIs and other key ingredients;
•developing and commercializing a new product is time consuming, costly and subject to numerous factors that may delay or
prevent the successful commercialization of new products; and
•commercializing generic products may be substantially delayed by the listing with the FDA of patents that have the effect of
potentially delaying approval of the off-patent product by up to 30 months and in some cases, such patents have been
issued and listed with the FDA after the key chemical patent on the brand drug product has expired or been litigated,
causing additional delays in obtaining approval.
As a result of these and other difficulties, products currently in development by Lannett may or may not receive the regulatory
approvals necessary for marketing. If any of our products, when developed and approved, cannot be successfully or timely
commercialized, our operating results could be adversely affected. We cannot guarantee that any investment we make in developing
products will be recouped, even if we are successful in commercializing those products.
The loss of key personnel could cause our business to suffer.
The success of our present and future operations will depend, to a significant extent, upon the experience, abilities and continued
services of our key personnel. If we lose the services of our key personnel, or if they are unable to devote sufficient attention to our
operations for any other reason, our business may be significantly impaired. If the employment of any of our current key personnel is
terminated, we cannot assure you that we will be able to attract and replace the employee with the same caliber of key personnel. As
such, we have entered into employment agreements with all of our senior executive officers in order to help retain these key
individuals.
If brand pharmaceutical companies are successful in limiting the use of generics through their legislative and regulatory
efforts, our sales of generic products may suffer.
Many brand pharmaceutical companies increasingly have used state and federal legislative and regulatory means to delay generic
competition. These efforts have included:
•pursuing new patents for existing products which may be granted just before the expiration of one patent which could
extend patent protection for additional years or otherwise delay the launch of generics;
•using the Citizen Petition process to request amendments to FDA standards;
•seeking changes to U.S. Pharmacopeia, an organization which publishes industry recognized compendia of drug standards;
•attaching patent extension amendments to non-related federal legislation;
•engaging in state-by-state initiatives to enact legislation that restricts the substitution of some generic drugs, which could
have an impact on products that we are developing;
•persuading regulatory bodies to withdraw the approval of brand-name drugs for which the patents are about to expire and
converting the market to another product of the brand company on which longer patent protection exists;
•entering into agreements whereby other generic companies will begin to market an authorized generic, a generic equivalent
of a branded product, at the same time or after generic competition initially enters the market;
•filing suits for patent infringement and other claims that may delay or prevent regulatory approval, manufacture and/or scale
of generic products; and,
•introducing “next-generation” products prior to the expiration of market exclusivity for the reference product, which often
materially reduces the demand for the generic or the reference product for which we seek regulatory approval.
In the U.S., some companies have lobbied Congress for amendments to the Hatch-Waxman Act that would give them additional
advantages over generic competitors. For example, although the term of a company’s drug patent can be extended to reflect a portion
of the time an NDA is under regulatory review, some companies have proposed extending the patent term by a full year for each year
spent in clinical trials rather than the one-half year that is currently permitted.
If proposals like these were to become effective, or if any other actions by our competitors and other third parties to prevent or delay
activities necessary to the approval, manufacture, or distribution of our products are successful, our entry into the market and our
ability to generate revenues associated with new products may be delayed, reduced, or eliminated, which could have a material
adverse effect on our business, financial condition, results of operations, cash flows and/or share price.
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�The generic pharmaceutical industry is characterized by intellectual property litigation and third parties may claim that we
infringe on their proprietary rights which could result in litigation that could be costly, result in the diversion of
management’s time and efforts, require us to pay damages or prevent us from marketing our existing or future products.
Our commercial success will depend in part on not infringing or violating the intellectual property rights of others. The manufacture,
use and sale of new products that are the subject of conflicting patent rights have been the subject of substantial litigation in the
pharmaceutical industry. These lawsuits relate to the validity and infringement of patents or proprietary rights of third parties. We may
have to defend against charges that we violated patents or proprietary rights of third parties. This is especially true in the case of
generic products on which the patent covering the brand product is expiring, an area where infringement litigation is prevalent and in
the case of new brand products in which a competitor has obtained patents for similar products. Our competitors, some of which have
substantially greater resources than we do and have made substantial intellectual property investments in competing technologies, may
have applied for or obtained, or may in the future apply for and obtain, patent rights and other intellectual property that will prevent,
limit or otherwise interfere with our ability to make, use and sell our products.
We may not be aware of whether our products do or will infringe existing or future patents or the intellectual property rights of others.
In addition, patent applications can be pending for many years and may be confidential for a number of months after filing and
because pending patent claims can be revised before issuance, there may be applications of others now pending of which we are
unaware that may later result in issued patents that will prevent, limit or otherwise interfere with our ability to make, use or sell our
products. Even if we prevail, litigation may be costly and time-consuming and could divert the attention of our management and
technical personnel. Any potential intellectual property litigation also could force us to do one or more of the following:
•stop making, selling or using products or technologies that allegedly infringe the asserted intellectual property;
•lose the opportunity to license our technology to others or to collect royalty payments based upon successful protection and
assertion of our intellectual property rights against others;
•incur significant legal expenses;
•pay substantial damages or royalties to the party whose intellectual property rights we may be found to be infringing;
•pay the attorney fees and costs of litigation to the party whose intellectual property rights we may be found to be infringing;
•redesign or rename, in the case of trademark claims, those products that contain the allegedly infringing intellectual
property, which could be costly, disruptive and/or infeasible; or
•attempt to obtain a license to the relevant intellectual property from third parties, which may not be available on reasonable
terms or at all.
Any litigation or claim against us, even those without merit, may cause us to incur substantial costs and could place a significant strain
on our financial resources, divert the attention of management from our core business and harm our reputation. For a description of
intellectual property-related litigation matters, see Note 12 “Legal and Regulatory Matters.” If we are found to infringe the
intellectual property rights of third parties, we could be required to pay substantial damages and/or substantial royalties and could be
prevented from selling our products unless we obtain a license or are able to redesign our products to avoid infringement. If we fail to
obtain any required licenses or make any necessary changes to our products or technologies, we may have to withdraw existing
products from the market or may be unable to commercialize one or more of our products, all of which could have a material adverse
effect on our business, results of operations and financial condition.
Although the parties to patent and intellectual property disputes in the pharmaceutical industry have often settled their disputes
through licensing or similar arrangements, the costs associated with these arrangements may be substantial and could include ongoing
royalties. Any such license may not be available on reasonable terms, if at all and there can be no assurance that we would be able to
redesign our products in a way that would not infringe the intellectual property rights of others. Even if we were able to obtain rights
to the third-party’s intellectual property, these rights may be non-exclusive, thereby giving our competitors access to the same
intellectual property. As a result, an adverse determination in a judicial or administrative proceeding or failure to obtain necessary
licenses could prevent us from manufacturing and selling a number of our products, or force us to redesign or rename our products to
avoid infringing the intellectual property rights of third parties, which, even if it is possible to so redesign or rename our products,
which could harm our business, financial condition, results of operations and cash flows.
If we are unable to obtain sufficient supplies from key suppliers that in some cases may be the only source of finished products
or raw materials, our ability to deliver our products to the market may be impeded.
We are required to identify the supplier(s) of all the raw materials for our products in our applications with the FDA. To the extent
practicable, we attempt to identify more than one supplier in each drug application. However, some products and raw materials are
available only from a single source and, in some of our drug applications, only one supplier of products and raw materials has been
identified, even in instances where multiple sources exist. To the extent any difficulties experienced by our suppliers cannot be
resolved within a reasonable time and at reasonable cost, or if raw materials for a particular product become unavailable from an
approved supplier and we are required to qualify a new supplier with the FDA, our profit margins and market share for the affected
product could decrease and our development and sales and marketing efforts could be delayed.
Our policies regarding returns, allowances and chargebacks and marketing programs adopted by wholesalers may reduce our
revenues in future fiscal periods.
Based on industry practice, generic drug manufacturers have liberal return policies and have been willing to give customers post-sale
inventory allowances. Under these arrangements, from time to time we give our customers credits on our generic products that our
customers hold in inventory after we have decreased the market prices of the same generic products due to competitive
pricing. Therefore, if new competitors enter the marketplace and significantly lower the prices of any of their competing products, we
would likely reduce the price of our products. As a result, we would likely be obligated to provide credits to our customers who are
then holding inventories of such products, which could reduce sales revenue and gross margin for the period the credit is
provided. Like our competitors, we also give credits for chargebacks to wholesalers that have contracts with us for their sales to
hospitals, group purchasing organizations, pharmacies or other customers.
A chargeback is the difference between the price the wholesaler pays and the price that the wholesaler’s end-customer pays for a
product. Although we establish reserves based on our prior experience and our best estimates of the impact that these policies may
have in subsequent periods, we cannot ensure that our reserves are adequate or that actual product returns, allowances and
chargebacks will not exceed our estimates.
Health care initiatives and other third-party payor cost-containment pressures could cause us to sell our products at lower
prices, resulting in decreased revenues.
Some of our products are purchased or reimbursed by state and federal government authorities, private health insurers and other
organizations, such as health maintenance organizations, or HMOs and managed care organizations, or MCOs. Third-party payors
increasingly challenge pharmaceutical product pricing. There also continues to be a trend toward managed health care in the United
States. Pricing pressures by third-party payors and the growth of organizations such as HMOs and MCOs could result in lower prices
and a reduction in demand for our products.
In addition, legislative and regulatory proposals and enactments to reform health care and government insurance programs could
significantly influence the manner in which pharmaceutical products and medical devices are prescribed and purchased. We expect
there will continue to be federal and state laws and/or regulations, proposed and implemented, that could limit the amounts that federal
and state governments will pay for health care products and services. The extent to which future legislation or regulations, if any,
relating to the health care industry or third-party coverage and reimbursement may be enacted or what effect such legislation or
regulation would have on our business remains uncertain. For example, the American Recovery and Reinstatement Act of 2009, also
known as the Stimulus Package, includes $1.1 billion in funding to study the comparative effectiveness of health care treatments and
strategies. The Stimulus Package funding is expected to be used for, among other things, to conduct, support or synthesize research
that compares and evaluates the risk and benefits, clinical outcomes, effectiveness and appropriateness of products. Although
Congress has indicated that this funding is intended for improvement in quality of health care, it remains unclear how the research will
impact coverage, reimbursement or other third-party payor policies. Such measures or other health care system reforms that are
adopted could have a material adverse effect on our industry generally and our ability to successfully commercialize our products or
could limit or eliminate our spending on development projects and affect our ultimate profitability.
We may need to change our business practices to comply with changes to fraud and abuse laws.
We are subject to various federal and state laws pertaining to health care fraud and abuse, including the Anti-Kickback Statute, which
apply to our sales and marketing practices and our relationships with physicians. At the federal level, the Anti-Kickback Statute
prohibits any person or entity from knowingly and willfully soliciting, receiving, offering, or paying any remuneration, including a
bribe, kickback, or rebate, directly or indirectly, in return for or to induce the referral of patients for items or services covered by
federal health care programs, or the furnishing, recommending, or arranging for products or services covered by federal health care
programs. Federal health care programs have been defined to include plans and programs that provide health benefits funded by the
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�federal government, including Medicare and Medicaid, among others. The definition of “remuneration” has been broadly interpreted
to include anything of value, including, for example, gifts, discounts, the furnishing of supplies or equipment, credit arrangements,
payments of cash and waivers of payments. Several courts have interpreted the federal Anti-Kickback Statute’s intent requirement to
mean that if even one purpose in an arrangement involving remuneration is to induce referrals or otherwise generate business
involving goods or services reimbursed in whole or in part under federal health care programs, the statute has been violated. The
federal government has issued regulations, commonly known as safe harbors that set forth certain provisions which, if fully met, will
assure parties that they will not be prosecuted under the federal Anti-Kickback Statute. The failure of a transaction or arrangement to
fit within a specific safe harbor does not necessarily mean that the transaction or arrangement will be illegal or that prosecution under
the federal Anti-Kickback Statute will be pursued, but such transactions or arrangements face an increased risk of scrutiny by
government enforcement authorities and an ongoing risk of prosecution. If our sales and marketing practices or our relationships with
physicians are considered by federal or state enforcement authorities to be knowingly and willfully soliciting, receiving, offering, or
providing any remuneration in exchange for arranging for or recommending our products and services and such activities do not fit
within a safe harbor, then these arrangements could be challenged under the federal Anti-Kickback Statute.
If our operations are found to be in violation of the federal Anti-Kickback Statute we may be subject to civil and criminal penalties
including fines of up to $25 thousand per violation, civil monetary penalties of up to $50 thousand per violation, assessments of up to
three times the amount of the prohibited remuneration, imprisonment and exclusion from participating in the federal health care
programs. In addition, HIPAA and its implementing regulations created two new federal crimes: health care fraud and false
statements relating to health care matters. The HIPAA health care fraud statute prohibits, among other things, knowingly and willfully
executing, or attempting to execute, a scheme to defraud any health care benefit program, including private payors. A violation of this
statue is a felony and may result in fines, imprisonment and/or exclusion from government-sponsored programs. The HIPAA false
statements statute prohibits, among other things, knowingly and willfully falsifying, concealing or covering up a material fact or
making any materially false, fictitious or fraudulent statement or representation in connection with the delivery of or payment for
health care benefits, items, or services.
A violation of this statute is a felony and may result in fines and/or imprisonment. A number of states also have anti-fraud and anti-
kickback laws similar to the federal Anti-Kickback Statute that prohibit certain direct or indirect payments if such arrangements are
designed to induce or encourage the referral of patients or the furnishing of goods or services. Some states’ anti-fraud and anti-
kickback laws apply only to goods and services covered by Medicaid. Other states’ anti-fraud and anti-kickback laws apply to all
health care goods and services, regardless of whether the source of payment is governmental or private. Due to the breadth of these
laws and the potential for changes in laws, regulations, or administrative or judicial interpretations, we may have to change our
business practices or our existing business practices could be challenged as unlawful, which could materially adversely affect our
business.
Certain federal and state governmental agencies, including the U.S. Department of Justice and the U.S. Department of Health and
Human Services, have been investigating issues surrounding pricing information reported by drug manufacturers and used in the
calculation of reimbursements as well as sales and marketing practices. For example, many government and third-party payors,
including Medicare and Medicaid, reimburse doctors and others for the purchase of certain pharmaceutical products based on the
product’s AWP reported by pharmaceutical companies. The federal government, certain state agencies and private payors are
investigating and have begun to file court actions related to pharmaceutical companies’ reporting practices with respect to AWP,
alleging that the practice of reporting prices for pharmaceutical products has resulted in a false and overstated AWP, which in turn is
alleged to have improperly inflated the reimbursement paid by Medicare beneficiaries, insurers, state Medicaid programs, medical
plans and others to health care providers who prescribed and administered those products. In addition, some of these same payors are
also alleging that companies are not reporting their “best price” to the states under the Medicaid program.
We may become subject to federal and state false claims litigation brought by private individuals and the government.
We are subject to state and federal laws that govern the submission of claims for reimbursement. The FFCA, also known as Qui Tam,
imposes civil liability and criminal fines on individuals or entities that knowingly submit, or cause to be submitted, false or fraudulent
claims for payment to the government. Violations of the FFCA and other similar laws may result in criminal fines, imprisonment and
civil penalties for each false claim submitted and exclusion from federally funded health care programs, including Medicare and
Medicaid. The FFCA also allows private individuals to bring a suit on behalf of the government against an individual or entity for
violations of the FFCA. These suits, also known as Qui Tam actions, may be brought by, with only a few exceptions, any private
citizen who has material information of a false claim that has not yet been previously disclosed. These suits have increased
significantly in recent years because the FFCA allows an individual to share in any amounts paid to the federal government in fines or
settlement as a result of a successful Qui Tam action. If our past or present operations are found to be in violation of any of such laws
or any other governmental regulations that may apply to us, we may be subject to penalties, including civil and criminal penalties,
damages, fines, exclusion from federal health care programs and/or the curtailment or restructuring of our operations. Any penalties,
damages, fines, curtailment, or restructuring of our operations could adversely affect our ability to operate our business and our
financial results, action against us for violation of these laws, even if we successfully defend against them, could cause us to incur
significant legal expenses and divert our management’s attention from the operation of our business.
Sales of our products may continue to be adversely affected by the continuing consolidation of our distribution network and
the concentration of our customer base.
Our principal customers are wholesale drug distributors and major retail drug store chains. These customers comprise a significant
part of the distribution network for pharmaceutical products in the U.S. This distribution network is continuing to undergo significant
consolidation marked by mergers and acquisitions among wholesale distributors and the growth of large retail drug store chains. As a
result, a small number of large wholesale distributors control a significant share of the market and the number of independent drug
stores and small drug store chains has decreased. We expect that consolidation of drug wholesalers and retailers will increase pricing
and other competitive pressures on drug manufacturers, including Lannett.
Our three largest customers accounted for 25%, 16% and 7%, respectively, of our total net sales for the fiscal year ended June 30,
2016 and 30%, 11% and 7%, respectively, of our total net sales for the fiscal year ended June 30, 2015. The loss of any of these
customers could materially adversely affect our business, results of operations and financial condition and our cash flows. In addition,
the Company generally does not enter into long-term supply agreements with its customers that would require them to purchase our
products.
A relatively small group of products may represent a significant portion of our revenues, gross profit, or net earnings from
time to time.
Sales of a limited number of our products from time to time represent a significant portion of our revenues, gross profit and net
earnings. For the fiscal years ended June 30, 2016, 2015 and 2014, our top five products in terms of sales, in the aggregate,
represented approximately 57%, 78% and 74%, respectively, of our total net sales. If the volume or pricing of our largest selling
products decline in the future, our business, financial condition, results of operations, cash flows and/or share price could be materially
adversely affected. See Item 1. Description of Business for more information on our top products.
We are increasingly dependent on information technology and our systems and infrastructure face certain risks, including
cybersecurity and data leakage risks.
Significant disruptions to our information technology systems or breaches of information security could adversely affect our business.
We are increasingly dependent on information technology systems and infrastructure to operate our business. In the ordinary course of
business, we collect, store and transmit large amounts of confidential information (including trade secrets or other intellectual
property, proprietary business information and personal information) and it is critical that we do so in a secure manner to maintain the
confidentiality and integrity of such confidential information. We could be susceptible to third-party attacks on our information
technology systems, which attacks are of ever increasing levels of sophistication and are made by groups and individuals with a wide
range of motives and expertise, including state and quasi-state actors, criminal groups, “hackers” and others. Maintaining the security,
confidentiality and integrity of this confidential information (including trade secrets or other intellectual property, proprietary,
business information and personal information) is important to our competitive business position. There can be no assurance that we
can prevent service interruptions or security breaches in our systems or the unauthorized or inadvertent wrongful use or disclosure of
confidential information that could adversely affect our business operations or result in the loss, misappropriation and/or unauthorized
access, use or disclosure of, or the prevention of access to, confidential information. A breach of our security measures or the
accidental loss, inadvertent disclosure, unapproved dissemination, misappropriation or misuse of trade secrets, proprietary
information, or other confidential information, whether as a result of theft, hacking, fraud, trickery or other forms of deception, or for
any other cause, could enable others to produce competing products, use our proprietary technology or information and/or adversely
affect our business position. Further, any such interruption, security breach, or loss, misappropriation and/or unauthorized access, use
or disclosure of confidential information could result in financial, legal, business and reputational harm to us and could have a material
adverse effect on our business, financial condition and results of operations.
The design, development, manufacture and sale of our products involves the risk of product liability claims by consumers and
other third parties and insurance against such potential claims is expensive and may be difficult to obtain.
The design, development, manufacture and sale of our products involve an inherent risk of product liability claims and the associated
adverse publicity. Insurance coverage is expensive and may be difficult to obtain and may not be available in the future on acceptable
terms, or at all. Although we currently maintain product liability insurance for our products in amounts we believe to be commercially
reasonable, if the coverage limits of these insurance policies are not adequate, a claim brought against Lannett, whether covered by
insurance or not, could have a material adverse effect on our business, results of operations, financial condition and cash flows.
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�Rising insurance costs, as well as the inability to obtain certain insurance coverage for risks faced by us, could negatively
impact profitability.
The cost of insurance, including workers compensation, product liability and general liability insurance, has risen in recent years and
may increase in the future. In response, we may increase deductibles and/or decrease certain coverage to mitigate these costs. These
increases and our increased risk due to increased deductibles and reduced coverage, could have a negative impact on our results of
operations, financial condition and cash flows.
Additionally, certain insurance coverage may not be available to us for risks faced by us. Sometimes the coverage we obtain for
certain risks may not be adequate to fully reimburse the amount of damage that we could possibly sustain. Should either of these
events occur, the lack of insurance to cover our entire cost would adversely affect our results of operations and financial condition.
Federal regulation of arrangements between manufacturers of brand and generic products could adversely affect our
business.
As part of the Medicare Prescription Drug, Improvement and Modernization Act of 2003, companies are now required to file with the
Federal Trade Commission (“FTC”) and the Department of Justice certain types of agreements entered into between brand and generic
pharmaceutical companies related to the manufacture, marketing and sale of generic versions of brand drugs. This new requirement
could affect the manner in which generic drug manufacturers resolve intellectual property litigation and other disputes with brand
pharmaceutical companies and could result generally in an increase in private-party litigation against pharmaceutical companies or
additional investigations or proceedings by the FTC or other governmental authorities. The impact of this new requirement and the
potential private-party lawsuits associated with arrangements between brand-name and generic drug manufacturers is uncertain and
could adversely affect our business.
If our goodwill or indefinite-lived intangible assets become impaired, we may be required to record a significant charge to
earnings.
Under accounting principles generally accepted in the U.S. (“GAAP”), we review our goodwill and indefinite lived intangible assets
for impairment at least annually and when there are changes in circumstances. In the fourth quarter of Fiscal 2016, we recorded an
$8.0 million impairment charge related to certain intellectual property research and development (“IPR&D”) assets acquired as part of
the KUPI acquisition mainly related to delays in expected launch dates as well as competitive pricing factors for two products in
development. We may be required to record additional significant charges to earnings in our financial statements during the period in
which any impairment of our goodwill or indefinite lived intangible assets is determined, resulting in a negative effect on our results
of operations.
Risks Related to our Recent Acquisition (the “Acquisition”) of Kremers Urban Pharmaceuticals, Inc. (“KUPI”)
The integration of the Lannett business with the KUPI business may present significant challenges.
There is a significant degree of difficulty inherent in the process of integrating the Lannett and KUPI businesses. These difficulties
include, among others:
•the challenge of integrating the Lannett and KUPI businesses while also effectively carrying on the ongoing operations of
each business;
•the challenge of integrating the business cultures of each company;
•the challenges of managing customer relationships smoothly and maintaining customer accounts, particularly in instances
where both companies serve the same customer;
•difficulties encountered in any internal reorganization that we may undertake;
•the challenge and cost of integrating the information technology and financial management systems of each company; and
•the potential difficulty in retaining key personnel.
The process of integrating operations could cause an interruption of, or loss of momentum in, the activities of one or more of Lannett’s
or KUPI’s businesses and may require us to incur substantial costs. For example, in October 2015, KUPI received notice from a
significant customer, representing approximately 20% of pre-acquisition net revenues, of its intention to re-source with alternative
suppliers certain products it currently purchases from KUPI. Any inability to recoup these sales from other existing and new
customers may result in an adverse impact on our financial results. Members of senior management may be required to devote
considerable amounts of time and attention to this integration process, which will decrease the time they will have to manage our
business, service existing customers, attract new customers, develop new services or strategies and manage risk. If senior management
is not able to effectively manage the integration process, or if any significant business activities are interrupted as a result of the
integration process, the combined business could suffer.
Additionally, we must integrate the accounting systems of Lannett and KUPI, which may be incompatible and which may take
different approaches to similar accounting policies, including revenue recognition. The changes in accounting policies and integrating
these disparate accounting systems and records have placed and will continue to place, significant additional demands on our
management, administrative and operational resources, including our accounting resources. We cannot guarantee that this integration
will be able to identify and resolve all issues in the integration time frame contemplated, or at all, or that the integration will not cost
more than we have budgeted. Any delay in integrating our accounting systems may have an adverse effect on our results of operations
or financial condition.
We cannot assure you that we will successfully or cost-effectively integrate the Lannett and KUPI businesses. The failure to do so
could have a material adverse effect on our financial condition and results of operations.
We may not realize the anticipated synergies, cost savings and growth opportunities from the Acquisition.
The benefits that we expect to achieve as a result of the Acquisition will depend, in part, on the ability of the combined company to
realize anticipated growth opportunities and cost synergies. Our success in realizing these growth opportunities and cost synergies and
the timing of this realization, depends on the successful integration of the historical Lannett business and operations and the historical
KUPI business and operations. Even if we are able to integrate the Lannett and KUPI businesses and operations successfully, this
integration may not result in the realization of the full benefits of the growth opportunities and cost synergies that we currently expect
from this integration within the anticipated time frame or at all. Moreover, we may incur substantial expenses in connection with this
integration. While we anticipate that certain expenses will be incurred, such expenses are difficult to estimate accurately and may
exceed current estimates. Accordingly, the benefits from the Acquisition may be offset by costs or delays incurred in integrating the
businesses.
Our actual financial position and results of operations may differ materially from the unaudited pro forma combined financial
data filed previously with the SEC.
The unaudited pro forma combined financial information that we filed previously with the SEC is presented for illustrative purposes
only and may not be an indication of what our financial position or results of operations would have been had the Acquisition been
completed on the dates indicated. The unaudited pro forma combined financial information has been derived from the audited and
unaudited financial statements of Lannett and KUPI and certain adjustments and assumptions have been made regarding Lannett after
giving effect to the Acquisition. Actual results are expected to differ from these preliminary estimates once we have completed the
valuation studies necessary to finalize the required purchase price allocations.
Differences between preliminary estimates in the unaudited pro forma combined financial information and the final acquisition
accounting may occur and could have a material impact on the pro forma combined financial information and our financial position
and future results of operations. In addition, the assumptions used in preparing the pro forma combined financial information may not
prove to be accurate and other factors may affect our financial condition or results of operations. Any potential decline in our
financial condition or results of operations may have a material effect on our ability to service and ultimately repay our indebtedness.
The Company is in the process of seeking restoration by the FDA of an AB rating for its methylphenidate hydrochloride extended
release product. Such restoration could take significant time, if it occurs at all, and failure to timely reestablish an AB rating may
adversely affect our financial results.
In November 2014, the FDA asked KUPI to conduct new bioequivalence testing of its Methylphenidate ER product using proposed
bioequivalence criteria or to voluntarily withdraw the product from the market. The FDA concurrently made the same request to the
other non-AG competitor (Mallinckrodt) regarding its Methylphenidate product. The FDA also changed the therapeutic
bioequivalence rating for KUPI’s and Mallinckrodt’s products from AB to BX at such time. A product that is BX-rated is still
approved and can be dispensed, but it may not be automatically substitutable at the pharmacy for the brand-name drug under certain
state laws. The FDA explained that while there were no safety or efficacy concerns, an FDA internal analysis (based on reports of lack
of effect and differences in pharmacokinetic (“PK”) profiles and delivery systems) suggested that KUPI’s generic Methylphenidate
ER product may not be therapeutically equivalent to Concerta®. In June 2015, KUPI submitted the final results of new bioequivalence
studies designed to assess whether KUPI’s Methylphenidate ER product meets the FDA’s newly-revised bioequivalence criteria. The
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�Company continues to market Methylphenidate ER under the BX rating. The Company also continues to pursue the FDA to obtain its
decision on the submitted study, as well as its response on whether it will restore the AB-rating for our product.
The Amended Senior Secured Credit Facility imposes operating and financial restrictions, which may prevent us from pursuing
certain business opportunities and taking certain actions that may be potentially profitable or in our best interests.
The FDA has not indicated when it will reach a decision on whether to revise the bioequivalence rating of Methylphenidate ER and no
assurance can be made that any such decision will result in Methylphenidate ER’s AB rating being restored. If the FDA should decide
to retain the BX rating of Methylphenidate ER, the Company will have to continue marketing the drug under its current rating. In
addition, if the Company is unable to regain an AB therapeutic rating, there is no assurance that the FDA will allow the Company to
retain the BX rating over the longer term. This could result in the Company having to potentially reformulate Methylphenidate ER or
otherwise discontinue sales.
As a result of the change in rating to BX from AB, the Company’s net sales of Methylphenidate ER have materially decreased. We
can provide no assurance that net sales of Methylphenidate ER will not continue to fall significantly. We can also provide no
assurance that the FDA will re-establish an AB rating for the Company’s Methylphenidate ER product in a timely manner, if at all. If
the FDA does not re-establish an AB rating for the Company’s Methylphenidate ER product in a timely manner, or at all, our financial
results could be adversely affected.
KUPI has received notification regarding state inquiries into its pricing practices.
In August 2015, KUPI received a letter from the Texas Office of the Attorney General alleging that KUPI had inaccurately reported
certain price information in violation of the Texas Medicaid Fraud Prevention Act. The Company is currently cooperating with the
Texas Attorney General’s Office, however, the outcome of the investigation could result in serious fines being levied on us, along
with harm to our reputation. Any negative outcome from this or any other investigation related to our pricing could have a material
adverse effect on our business, financial condition and results of operations.
Risks Related to our Indebtedness
Our substantial indebtedness may adversely affect our financial health.
We currently have substantial indebtedness. As of June 30, 2016, we had total indebtedness of $1.2 billion. Our total indebtedness
consists of a $1.1 billion amended term loan facility (the “Amended Term Loan Facility”) as well as a $125.0 million revolving credit
facility (the “Revolving Credit Facility”). The Amended Term Loan Facility consists of an initial $910.0 million senior secured term
loan facility (the “Senior Secured Term Loan Facility”), which was amended in June 2016 to include an additional $150.0 million
incremental term loan (the “Incremental Term Loan”). The Amended Term Loan Facility, together with the Revolving Credit Facility
comprises the amended senior secured credit facility (the “Amended Senior Secured Credit Facility”).
Our substantial indebtedness may have important consequences for us. For example, it may:
•make it more difficult for us to make payments on our indebtedness;
•increase our vulnerability to general economic and industry conditions, including recessions and periods of significant
inflation and financial market volatility;
•expose us to the risk of increased interest rates, because any borrowings we make under the Revolving Facility and other
borrowings under the Term Loan Facility under certain circumstances, will bear interest at variable rates;
•require us to use a substantial portion of cash flow from operations to service our indebtedness, thereby reducing our ability
to fund working capital, capital expenditures and other expenses;
•limit our flexibility in planning for, or reacting to, changes in our business and the industry in which we operate;
•place us at a competitive disadvantage compared to competitors that have less indebtedness; and
•limit our ability to borrow additional funds that may be needed to operate and expand our business.
The operating and financial restrictions and covenants in our Amended Senior Secured Credit Facility restrict and future debt
instruments may restrict, subject to certain important exceptions and qualifications, our and our subsidiaries’ ability to, among other
things:
•incur or guarantee additional indebtedness;
•make certain investments or acquisitions;
•grant or permit certain liens on our assets;
•enter into certain transactions with affiliates;
•pay dividends, redeem our equity or make other restricted payments;
•prepay, repurchase or redeem contractually subordinated debt and certain other debt;
•merge, consolidate or transfer substantially all of our assets;
•transfer, sell or dispose of property and assets; and
•change the business we conduct or enter into new kinds of business.
These covenants could adversely affect our ability to finance our future operations or capital needs, withstand a future downturn in our
business or the economy in general, engage in business activities, including future opportunities that may be in our interest and plan
for or react to market conditions or otherwise execute our business strategies. Our ability to comply with these covenants may be
affected by events beyond our control. A breach of any of these covenants could result in a default in respect of the related
indebtedness. If an event of default occurs, the relevant lenders or holders of such indebtedness could elect to declare the
indebtedness, together with accrued interest, fees and other liabilities, to be immediately due and payable and proceed against any
collateral securing that indebtedness. Acceleration of our other indebtedness could result in a default under the terms of the Amended
Senior Secured Credit Facility. There is no guarantee that we would be able to satisfy our obligations if any of our indebtedness is
accelerated.
In addition, the limitations imposed in the Amended Senior Secured Credit Facility on our ability to incur certain additional debt and
to take other corporate actions might significantly impair our ability to obtain other financing. If, for any reason, we are unable to
comply with the restrictions in the Amended Senior Secured Credit Facility, we may not be granted waivers or amendments to such
restrictions or we may not be able to refinance our debt on terms acceptable to us, or at all. The lenders under the Amended Senior
Secured Credit Facility also have the right in these circumstances to terminate any commitments they have to provide further
borrowings. If we were unable to pay such amounts, the lenders under the Amended Senior Secured Credit Facility could recover
amounts owed to them by foreclosing against the collateral pledged to them. We have pledged a substantial portion of our assets to the
lenders under the Amended Senior Secured Credit Facility, including the equity of our subsidiaries.
Our Amended Senior Secured Credit Facility contains a financial covenant and other restrictive covenants that limit our
flexibility. We may not be able to comply with these covenants, which could result in the amounts outstanding under our Amended
Senior Secured Credit Facility becoming immediately due and payable.
Our Revolving Credit Facility requires us to comply with a first lien net leverage ratio not to exceed 4.25:1.00 when there are
outstanding loans and letters of credit (other than (i) drawn letters of credit that have been cash collateralized, (ii) up to $5.0 million of
undrawn letters of credit and (iii) with respect to each test period ending on or prior to December 31, 2016, up to $22.8 million of
loans under the Revolving Credit Facility made on the Acquisition closing date) thereunder that exceed 30% of the aggregate
commitment amount under the Revolving Credit Facility of $125.0 million as of the last day of the applicable fiscal quarter (with two
step downs occurring as of December 31, 2017 and as of December 31, 2019 of 3.75:1.00 and 3.25:1.00, respectively). In addition, the
Term Loan A Facility is subject to a financial performance covenant, which provides that the Company shall not permit its secured net
leverage ratio as of the last day of any four consecutive fiscal quarters to be greater than 4.25:1.00 (with two step downs occurring as
of December 31, 2017 and as of December 31, 2019 to 3.75:1.00 and 3.25:1.00, respectively). Accordingly, if our liquidity and
performance significantly worsens, we could become non-compliant with such covenants.
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�Despite our substantial indebtedness level, we and any of our existing or future subsidiaries may still be able to incur substantially
more debt, which could exacerbate the risks associated with our substantial leverage.
The terms of the agreements governing the Amended Senior Secured Credit Facility permit us and our subsidiaries to incur a
substantial amount of additional debt, including secured debt. Although the agreement that governs the Amended Senior Secured
Credit Facility contain restrictions on the incurrence of additional indebtedness, these restrictions are subject to a number of
qualifications and exceptions and the indebtedness incurred in compliance with these restrictions could be substantial. Additionally,
the Amended Senior Secured Credit Facility may be increased from time to time, subject to certain conditions. All of those borrowings
would be secured indebtedness. If new debt is added to our and our subsidiaries’ current debt levels, the risks that we now face as a
result of our leverage would intensify and we may not be able to meet all of our debt obligations, in whole or in part.
In addition, our Amended Senior Secured Credit Facility contains other restrictive covenants, including covenants that limit and in
some circumstances prohibit, our ability to, among other things, incur additional debt, sell, transfer or otherwise dispose of our assets,
pay dividends, make investments, loans, advances and acquisition, guarantee debt or obligations, create liens, enter into transactions
with our affiliates and enter into certain merger, consolidation or other fundamental transactions.
If we fail to meet any covenants in our Amended Senior Secured Credit Facility and cannot secure a waiver for such failure, the
lenders under our Amended Senior Secured Credit Facility would be entitled to exercise various rights, including causing the amounts
outstanding under the entire Amended Senior Secured Credit Facility to become immediately due and payable.
We are also subject to requirements to make mandatory prepayments, with the net proceeds of certain asset sales, excess cash flows
and debt issuances. These requirements could limit our ability to obtain future financing, make acquisitions or needed capital
expenditures, withstand any downturns in our business or the economy in general, conduct operations or otherwise take advantage of
business opportunities that may arise, any of which could place us at a competitive disadvantage relative to our competitors that have
less debt and are not subject to such restrictions.
Our variable rate indebtedness subjects us to interest rate risk, which could cause our debt service obligations to increase
significantly.
Borrowings under the Amended Senior Secured Credit Facility are at variable rates of interest and expose us to interest rate risk.
Interest rates are currently at historically low levels. If interest rates increase, our debt service obligations on our variable rate
indebtedness will increase even though the amount borrowed remained the same and our net income and cash flows, including cash
available for servicing our indebtedness, will correspondingly decrease. Based on total indebtedness as of June 30, 2016 and the
assumption that interest rates are above the interest rate floor set forth in the Amended Senior Secured Credit Facility, each 1/8th
percentage point change in interest rates would result in a $1.5 million change in annual interest expense on our indebtedness under
the Amended Senior Secured Credit Facility.
Due to many factors beyond our control, we may not be able to generate sufficient cash to service all of our indebtedness and meet
our other ongoing liquidity needs and we may be forced to take other actions to satisfy our obligations under our debt agreements,
which may not be successful.
Our ability to make payments on and to refinance, our indebtedness and to fund planned capital expenditures will depend on our
ability to generate cash in the future. This is subject to general economic, financial, competitive, legislative, regulatory and other
factors, many of which are beyond our control.
Our business may not generate sufficient cash flow from operations and we may not have available to us future borrowings in an
amount sufficient, to enable us to pay our indebtedness or to fund our other liquidity needs. In these circumstances, we may need to
refinance all or a portion of our indebtedness on or before maturity. Any refinancing of our debt could be at higher interest rates and
may require us to comply with more onerous covenants, which could further restrict our business operations. Our ability to refinance
our indebtedness or obtain additional financing will depend on, among other things:
•our financial condition at the time;
•restriction in the agreements governing our indebtedness; and
•the condition of the financial markets and the industry in which we operate.
As a result, we may not be able to refinance any of our indebtedness on commercially reasonable terms or at all. In such a case, we
could be forced to sell assets, reduce or delay capital expenditures or issue equity securities to make up for any shortfall in our
payment obligations under unfavorable circumstances. The terms of the Amended Senior Secured Credit Facility limit our ability to
sell assets. In addition, we may not be able to sell assets quickly enough or for sufficient amounts to enable us to meet our obligations.
Any failure to make scheduled payments of interest and principal on our outstanding indebtedness when due would permit the holders
of such indebtedness to declare an event of default and accelerate the indebtedness. This could result in the lenders under the
Amended Senior Secured Credit Facility terminating their commitments to lend us money and foreclosing against the assets securing
the borrowings and we could be forced into bankruptcy or other insolvency proceedings. In addition, any failure to make payments of
interest and principal on our outstanding indebtedness on a timely basis would likely result in a reduction of our credit rating, which
could harm our ability to incur additional indebtedness on acceptable terms.
34
35
�ITEM 2.
DESCRIPTION OF PROPERTY
PART II
Lannett owns five facilities in Philadelphia, Pennsylvania. Certain administrative functions, manufacturing and production facilities
and our quality control laboratory are located in a 31,000 square foot facility at 9000 State Road, Philadelphia, PA. The second
facility consists of 63,000 square feet and is located within one mile of the State Road facility at 9001 Torresdale Avenue,
Philadelphia, PA. Our research laboratory and packaging functions are located at this location. Additionally, the facility has capacity
for additional manufacturing space, if needed. We also own a building at 13200 Townsend Road Philadelphia, PA consisting of
66,000 square feet on 7.3 acres of land which is used for certain administrative functions, warehouse space and shipping. It also has
capacity for additional manufacturing space, if needed.
On December 20, 2013, the Company acquired two separate properties located in Philadelphia, Pennsylvania for $4.0 million and $5.0
million. The buildings are 196,000 and 400,000 square feet. In connection with the purchase of these two buildings, the Company
expects to incur capital expenditures for fit out costs over the next several years.
The manufacturing facility of our wholly-owned subsidiary, Cody Labs, consists of a 73,000 square foot structure located on
approximately 15.0 acres in Cody, Wyoming. Cody Labs’ manufacturing facility currently has capacity for further expansion, both
inside and outside the existing structure.
In connection with the acquisition of Silarx, the Company acquired an 110,000 square foot manufacturing facility located in Carmel,
New York, which sits on 25.8 acres of land. The facility currently houses manufacturing, packaging, research and development and
has capacity for additional manufacturing space, if needed.
In November 2015, we completed the acquisition of KUPI. KUPI’s 432,000 square foot Seymour, Indiana facility contains
approximately 107,000 square feet of manufacturing space as well as a leased 116,000 square foot temperature/humidity controlled
storage warehouse. The Seymour facility has had satisfactory inspections conducted by the FDA and EMA and similar regulatory
authorities of Japan, Taiwan, Brazil, Korea and Turkey. Since 2008, KUPI has invested more than $75 million into improvements to
the facility and new equipment. This investment enabled the facility to increase production from approximately 1.2 billion doses in
2008 to over 2.7 billion doses in 2014. KUPI recently completed a $20 million, 20,000 square foot expansion of the facility which, in
combination with an additional planned expansion in 2016, is expected to increase capacity to 3.9 billion doses by 2017. KUPI added
a large vault for storing controlled substances in 2011 and is also planning to expand its vault capabilities relating to Schedule II
(“CII”) products in conformance with DEA requirements. The facility also includes four packaging lines, one of which is a high
speed line added in 2012. The serialization has been completed on three lines and we expect to complete the fourth line in the near
future.
ITEM 3.
LEGAL PROCEEDINGS
ITEM 5.
MARKET FOR COMMON EQUITY AND RELATED STOCKHOLDER MATTERS
Market Information
The Company’s common stock trades on the NYSE. The following table sets forth certain information with respect to the high and
low sales prices per share of the Company’s common stock during Fiscal 2016 and 2015, as quoted by the NYSE.
Fiscal Year Ended June 30, 2016
First quarter
Second quarter
Third quarter
Fourth quarter
First quarter
Second quarter
Third quarter
Fourth quarter
Fiscal Year Ended June 30, 2015
High
Low
$
$
$
$
$
$
$
$
62.90
49.44
40.66
26.25
High
51.66
59.44
71.26
72.44
$
$
$
$
$
$
$
$
40.85
33.13
16.91
17.05
33.51
39.05
40.34
52.10
Low
Holders
As of June 30, 2016, there were 523 holders of record of the Company’s common stock.
Information pertaining to legal proceedings can be found in Note 12 “Legal and Regulatory Matters” under Item 15. Exhibits and
Financial Statement Schedules and is incorporated by reference herein.
Dividends
ITEM 4.
MINE SAFETY DISCLOSURES
Not applicable
The Company did not pay cash dividends in Fiscal 2016 or Fiscal 2015. The Company intends to use available funds for working
capital, plant and equipment additions, various product extension ventures and mergers and acquisitions or other growth opportunities.
In addition, the Company is subject to certain restrictions on dividends under its Amended Senior Secured Credit Facility. The
Company does not expect to pay, nor should stockholders expect to receive, cash dividends in the foreseeable future.
36
37
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The following financial information as of and for the five years ended June 30, 2016, has been derived from our consolidated financial
statements. This information should be read in conjunction with our consolidated financial statements and related notes thereto
included elsewhere herein. Certain prior year amounts have been reclassified to conform to the current year financial statement
presentation.
Lannett Company, Inc. and Subsidiaries
Financial Highlights
(In thousands, except per share data)
As of and for the Fiscal Year Ended June 30,
Operating Highlights
Net sales
Settlement agreement
Total net sales
Gross profit
Operating income
Net income attributable to Lannett Company,
Inc.
Basic earnings per common share attributable to
Lannett Company, Inc.
Diluted earnings per common share attributable
to Lannett Company, Inc.
$
$
$
$
$
$
$
$
Balance Sheet Highlights
Total Assets
Total Debt
Long-Term Debt, net
Total Stockholders’ Equity
$ 1,764,018
$ 1,061,848
883,612
$
554,457
$
2016
2015
2014
2013
2012
566,091
$
(23,598) $
$
542,493
$
286,493
$
130,758
44,782
1.23
1.20
$
$
$
$
$
$
$
406,837
—
406,837
306,356
226,487
149,919
4.18
4.04
508,766
1,009
874
463,766
$
$
$
$
$
$
$
$
$
$
$
$
273,771
—
273,771
154,408
88,089
57,101
1.70
1.62
342,773
1,138
1,009
294,765
$
$
$
$
$
$
$
$
$
$
$
$
151,054
—
151,054
57,420
18,757
13,317
0.47
0.46
167,752
6,514
5,844
128,809
$
$
$
$
$
$
$
$
$
$
$
$
122,990
—
122,990
38,947
6,910
3,948
0.14
0.14
142,592
7,161
6,513
111,313
Settlement agreement relates to a Settlement Agreement Release and Mutual Release with one of the Company’s former customers.
Refer to Note 22 “Settlement Agreement” for additional information.
On November 25, 2015, the Company completed the acquisition of KUPI. The Company’s Consolidated Statements of Operations for
Fiscal 2016 includes the impact of KUPI from that date.
8
38
3
39
�ITEM 7.
OPERATIONS
MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF
The following discussion and analysis describes material changes in the financial condition and results of operations, as well as
liquidity and capital resources of the Company. Additionally, it addresses accounting policies that management has deemed are
“critical accounting policies.” This discussion and analysis is intended as a supplement to and should be read in conjunction with the
Consolidated Financial Statements, the Notes to the Consolidated Financial Statements and other sections of this Form 10-K.
The following discussion contain forward-looking statements. You should refer to the “Cautionary Statement Regarding Forward-
Looking Statements” set forth in Part I of this Annual Report.
million settlement agreement, decreased $19.9 million to $286.5 million, compared to the prior year period and gross profit percentage
decreased to 53% compared to 75% in Fiscal 2015. Excluding the impact of KUPI and the settlement agreement, gross profit as a
percentage of net sales decreased to 71%. R&D expenses increased 48% to $45.1 million compared to the prior year period while
SG&A expenses increased 51% to $68.3 million. Acquisition and integration-related expenses increased to $27.2 million from $4.3
million in the prior year period. Restructuring expenses increased to $7.2 million as a result of implementing the 2016 Restructuring
Program. Operating income for Fiscal 2016, which included an $8.0 million intangible asset impairment charge, was $130.8 million
compared to $226.5 million in the prior year period. Net income attributable to Lannett Company, Inc. for Fiscal 2016, which
included a $3.0 million loss on extinguishment of debt, was $44.8 million, or $1.20 per diluted share. Comparatively, net income
attributable to Lannett Company, Inc. in the prior year was $149.9 million, or $4.04 per diluted share.
All references to “Fiscal 2016” or “Fiscal Year 2016” shall mean the fiscal year ended June 30, 2016 and all references to “Fiscal
2015” or “Fiscal Year 2015” shall mean the fiscal year ended June 30, 2015.
Results of Operations — Fiscal 2016 compared to Fiscal 2015
A more detailed discussion of the Company’s financial results can be found below.
Company Overview
Lannett Company, Inc. (a Delaware corporation) and its subsidiaries (collectively, the “Company”, “Lannett”, “we” or “us”) develop,
manufacture, package, market and distribute solid oral and extended release (tablets and capsules), topical, nasal and oral solution
finished dosage forms of drugs, that address a wide range of therapeutic areas. Certain of these products are manufactured by others
and distributed by the Company. The Company also manufactures active pharmaceutical ingredients through its Cody Labs
subsidiary, providing a vertical integration benefit. Additionally, the Company is pursuing partnerships, research contracts and
internal expansion for the development and production of other dosage forms including: ophthalmic, nasal, patch, foam, buccal,
sublingual, soft gel, injectable and oral dosages.
On November 25, 2015, the Company completed the acquisition of Kremers Urban Pharmaceutical, Inc. (“KUPI”), the former
subsidiary of global biopharmaceuticals company UCB S.A. KUPI is a specialty pharmaceuticals manufacturer focused on the
development of products that are difficult to formulate or utilize specialized delivery technologies. Strategic benefits of the
acquisition include expanded manufacturing capacity, a diversified product portfolio and pipeline and complementary research and
development expertise.
The Company operates pharmaceutical manufacturing plants in Philadelphia, Pennsylvania; Cody, Wyoming; Carmel, New York and
Seymour, Indiana. The Company’s customers include generic pharmaceutical distributors, drug wholesalers, chain drug stores,
private label distributors, mail-order pharmacies, other pharmaceutical manufacturers, managed care organizations, hospital buying
groups, governmental entities and health maintenance organizations.
2016 Restructuring Plan
On February 1, 2016, in connection with the acquisition of KUPI, the Company announced a plan related to the future integration of
KUPI and the Company’s operations (the “2016 Restructuring Program”). The plan focuses on the closure of KUPI’s corporate
functions and the consolidation of manufacturing, sales, research and development and distribution functions. The Company estimates
that it will incur an aggregate of up to approximately $23.0 million in restructuring charges for actions that have been announced or
communicated since the 2016 Restructuring Program began. Of this amount, approximately $14.0 million relates to employee
separation costs, approximately $1.0 million relates to contract termination costs and approximately $8.0 million relates to facility
closures costs and other actions.
The plan is expected to result in cost synergies of approximately $45.0 million during the 12 months following the close of the
acquisition, including $32.9 million realized in Fiscal 2016 and is currently estimated to generate annualized synergies of
approximately $50.0 million by the end of Fiscal 2018. It is expected to achieve an ultimate annual run rate of synergies totaling
approximately $65.0 million by the end of Fiscal 2020.
These amounts are preliminary estimates based on the information currently available to management. It is possible that additional
charges and future cash payments could occur in relation to the restructuring actions.
Financial Summary
For Fiscal 2016, net sales increased to $566.1 million, which included $165.6 million of net sales from the recent KUPI acquisition in
November 2015. Excluding the impact of KUPI, net sales decreased 2% as compared to Fiscal 2015 primarily due to pricing
pressures and increased competition, partially offset by increased volumes. Total net sales, which included a $23.6 million reduction
for a settlement agreement, increased to $542.5 million from $406.8 million in the prior year period. Gross profit, including the $23.6
Total net sales, which included a $23.6 million reduction for a settlement agreement, increased to $542.5 million from $406.8 million
in the prior year period. The settlement agreement relates to a Settlement Agreement Release and Mutual Release with one of the
Company’s former customers. Refer to Note 22 “Settlement Agreement” for additional information.
Net sales increased 39% to $566.1 million for the fiscal year ended June 30, 2016. The following table identifies the Company’s
approximate net product sales by medical indication for the fiscal years ended June 30, 2016 and 2015:
(In thousands)
Medical Indication
Antibiotic
Cardiovascular
Central Nervous System
Gallstone
Gastrointestinal
Glaucoma
Gout
Migraine
Muscle Relaxant
Obesity
Pain Management
Respiratory
Thyroid Deficiency
Urinary
Other
Contract manufacturing revenue
Net sales
Settlement agreement
Total net sales
Fiscal Year Ended June 30,
2016
2015
$
$
14,558
53,541
36,291
67,348
52,699
25,336
303
21,776
5,403
3,809
29,804
9,982
162,411
17,398
43,389
22,043
566,091
(23,598)
542,493
$
$
12,306
55,166
—
65,262
—
21,145
6,833
25,729
8,779
4,004
27,461
—
153,460
212
26,480
—
406,837
—
406,837
Revenues from the KUPI acquisition of $165.6 million and increased volumes of $38.7 million contributed to the overall increase in
net sales, partially offset by product price decreases of $45.0 million. Although the Company has benefited in the past from favorable
pricing trends, the trends are stabilizing and in, some instances, beginning to reverse. During the period, the Company experienced
pricing pressure and increased competition on several products. The level of competition in the marketplace is constantly changing
and the Company cannot predict with certainty the extent to which pricing pressures will continue.
40
41
�The following chart details price and volume changes by medical indication:
Medical indication
Antibiotic
Cardiovascular
Central Nervous System
Gallstone
Gastrointestinal
Glaucoma
Gout
Migraine
Muscle Relaxant
Obesity
Pain Management
Respiratory
Thyroid Deficiency
Urinary
Sales volume
change %
Sales price
change %
Acquisition
change %
33%
(20)%
—%
13%
—%
19%
(95)%
(3)%
(34)%
(5)%
(7)%
—%
17%
500%
(15)%
(25)%
—%
(10)%
—%
1%
—%
(13)%
(4)%
—%
15%
—%
(11)%
(176)%
—%
42%
100%
—%
100%
—%
—%
—%
—%
—%
—%
100%
—%
7783%
Cardiovascular. Net sales of drugs used for cardiovascular treatment decreased by $1.6 million, primarily as a result of decreased
volumes due to several new entrants in the market for products used to treat congestive heart failure, as well as pricing pressures. The
decreases were partially offset by net sales from cardiovascular products acquired in the KUPI acquisition.
Central Nervous System. Net sales of central nervous system products increased by $36.3 million. The increase in net sales was
attributable to net sales from the Methylphenidate Hydrochloride Extended Release tablets, a product acquired in the KUPI
acquisition.
Methylphendidate Hydrochloride Extended Release Tablets
During a teleconference in November 2014, the FDA informed KUPI that it had concerns about whether generic versions of Concerta
(methylphenidate hydrochloride extended release tablets), including KUPI’s Methylphenidate ER product, are therapeutically
equivalent to Concerta. The FDA indicated that its concerns were based in part on adverse event reports concerning lack of effect and
its analyses of pharmacokinetic data. The FDA informed KUPI that it was changing the therapeutic equivalence rating of its product
from “AB” (therapeutically equivalent) to “BX.” A BX-rated drug is a product for which data are insufficient to determine
therapeutic equivalence; it is still approved and can be prescribed, but the FDA does not recommend it as automatically substitutable
for the brand-name drug at the pharmacy. The FDA has indicated that there are no safety issues with KUPI’s product.
During the November 2014 teleconference, the FDA also asked KUPI to either voluntarily withdraw its product or to conduct new
bioequivalence (“BE”) testing in accordance with the recommendations for demonstrating bioequivalence to Concerta proposed in a
new draft BE guidance that the FDA issued earlier that November. The FDA had approved the KUPI product (and originally granted
it an AB rating) in 2013, on the basis of KUPI data showing its product met BE criteria set forth in draft BE guidance that the FDA
had issued in 2012. The FDA’s position concerning the KUPI product was the subject of a public announcement by the agency. The
Company agreed to conduct new BE studies per the new draft BE guidance. KUPI submitted the data from those studies to the FDA
in May 2015. The Company continues to pursue the FDA to obtain its decision on the submitted study as well as its response on
whether it will restore the AB-rating for our product.
There can be no assurance as to when or if the Company will receive the “AB” rating. However, if the Company were to receive the
“AB” rating, net sales of the product could increase subject to market factors existing at that time. The Company also agreed to
potential acquisition-related contingent payments to UCB related to Methylphenidate ER if the FDA reinstates the AB-rating and
certain sales thresholds are met.
Gallstone. Net sales of drugs used for gallstones increased by $2.1 million. The increase in net sales was primarily attributable to
increased volumes, partially offset by price decreases.
Gastrointestinal. Net sales of gastrointestinal products increased by $52.7 million. The increase in net sales was primarily
attributable to sales of gastrointestinal products acquired in the KUPI acquisition.
Glaucoma. Net sales of drugs used for the treatment of glaucoma increased by $4.2 million. The increase in net sales was primarily
attributable to increased volumes.
Gout. Net sales of drugs used to treat gout decreased by $6.5 million. The decrease in net sales was attributable to decreased volumes
resulting from the loss of a customer contract.
Pain Management. Net sales of pain management products increased $2.3 million. The increase in net sales was mainly attributable
to price increases on the Company’s C-Topical® Solution product as well as a higher average net sales price. Net sales was lower in
the prior year period as a result of an increase in return reserves related to a voluntary recall of one lot of product manufactured at the
Company’s facility in Cody, Wyoming due to incorrect labeling. The Company has completed its C-Topical® Solution Phase III trial
and anticipates filing an NDA application with the FDA in calendar year 2017.
Respiratory. Net sales of respiratory products increased by $10.0 million. The increase in net sales was attributable to sales of
respiratory products acquired in the KUPI acquisition.
Thyroid Deficiency. Net sales of drugs used for the treatment of thyroid deficiency increased by $9.0 million, primarily as a result of
increased volumes, partially offset by a price concession to secure a long-term customer commitment.
Urinary. Net sales of urinary products increased by $17.2 million. The increase in net sales was primarily attributable to net sales of
urinary products acquired in the KUPI acquisition.
Contract manufacturing revenue. Contract manufacturing revenue for Fiscal 2016 totaled $22.0 million, which was the result of the
acquisition of KUPI.
The Company sells its products to customers in various distribution channels. The table below presents the Company’s net sales to
each distribution channel for the fiscal year ended June 30:
(In thousands)
Customer Distribution Channel
Wholesaler/Distributor
Retail Chain
Mail-Order Pharmacy
Contract manufacturing revenue
Net sales
Settlement agreement
Total net sales
June 30,
2016
June 30,
2015
$
$
419,375
84,614
40,059
22,043
566,091
(23,598)
542,493
$
$
297,675
65,130
44,032
—
406,837
—
406,837
Net sales to wholesaler/distributor and retail chain increased primarily as a result of additional net sales related to the KUPI
acquisition. Mail-order pharmacy net sales decreased primarily as a result of lower cardiovascular drug sales as well as drugs used for
the treatment of gallstones to a specific mail-order pharmacy customer.
Cost of Sales, including amortization of intangibles. Cost of sales for Fiscal 2016 increased $155.5 million to $256.0 million.
The increase primarily reflected additional costs from the acquisition of KUPI, as well as the effects of purchase accounting related to
the amortization of inventory step-up totaling $17.0 million and increased provisions for excess and obsolete inventory totaling $9.4
million. Product royalties included in cost of sales totaled $17.0 million for Fiscal 2016 and $175 thousand for Fiscal 2015. The
increase was primarily the result of additional product royalties from the acquisition of KUPI. Amortization of intangible assets
included in cost of sales totaled $18.6 million for Fiscal 2016 and $137 thousand for Fiscal 2015. The increase primarily reflected
additional amortization of the acquired intangibles from the acquisition of KUPI and Silarx.
Gross Profit. Gross profit for the fiscal year ended June 30, 2016 decreased 6% to $286.5 million or 53% of total net sales. In
comparison, gross profit for the fiscal year ended June 30, 2015 was $306.4 million or 75% of total net sales. The decrease in gross
profit percentage for Fiscal 2016 was attributable to the settlement agreement, the dilutive impact of gross profit margins of KUPI
products, additional amortization of intangibles, as well as amortization of inventory step-up and depreciation of property, plant and
equipment step-up related to the acquisition of KUPI. Product mix and pricing pressures also contributed to lower gross profit as a
percentage of total net sales during Fiscal 2016. Excluding the impact of KUPI and the settlement agreement, gross profit as a
percentage of total net sales decreased to 71%.
Research and Development Expenses. Research and development expenses increased 48% to $45.1 million for the fiscal year ended
June 30, 2016 compared to $30.3 million in the prior year period. The increase was primarily due to the acquisitions of KUPI and
Silarx, which resulted in additional research and development expenses. The increase was partially offset by lower contract laboratory
and bio-equivalency studies expenses.
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�Selling, General and Administrative Expenses. Selling, general and administrative expenses increased 51% to $68.3 million for the
fiscal year ended June 30, 2016 compared with $45.2 million in the prior year period. The increase was primarily due to the
acquisition of KUPI and Silarx, which resulted in additional selling, general and administrative expenses. Additional compensation-
related costs, including separation benefits for two former executive officers, also contributed to the increase.
The Company is focused on controlling operating expenses and has implemented its 2016 Restructuring Plan as noted above, however
increases in personnel and other costs to facilitate enhancements in the Company’s infrastructure and expansion may continue to
impact operating expenses in future periods.
Acquisition and Integration-related Expenses. Acquisition and integration-related expenses increased $22.9 million compared to the
prior year period. The increase was primarily due to costs associated with the acquisition of KUPI, including investment banking,
legal and accounting fees as well as post-acquisition integration costs. In the fourth quarter of Fiscal Year 2016, the Company also
recorded compensation-related expense, of which $2.5 million was classified as integration-related expenses.
Restructuring Expenses. Restructuring expenses increased $7.2 million compared to the prior year period as a result of implementing
the 2016 Restructuring Program on February 1, 2016.
Intangible Assets Impairment Charge. As part of the Company’s annual impairment analysis performed in the fourth quarter of
Fiscal 2016, the Company recorded an $8.0 million impairment charge related to certain intangible assets acquired as part of the KUPI
acquisition. The impairment was mainly related to delays in expected launch dates as well as competitive pricing factors for two
products in development.
Other Income (Loss). Interest expense in Fiscal 2016 totaled $65.9 million compared to $207 thousand in the prior year period. The
increase was due to interest on debt obligations used to finance the acquisition of KUPI, as well as amortization of debt discount and
other debt issuance costs. The weighted average interest rate for Fiscal 2016 was 9.1%. Investment income in Fiscal 2016 totaled
$368 thousand compared to investment income of $1.1 million in the prior year period. The Company also recorded a $3.0 million
loss on extinguishment of debt related to the repurchase of the 12.0% Senior Notes in the fourth quarter of Fiscal 2016.
Income Tax. The Company recorded income tax expense for the fiscal year ended June 30, 2016 of $17.3 million compared to $77.4
million for the fiscal year ended June 30, 2015. The effective tax rate for the fiscal year ended June 30, 2016 was 27.9%, compared to
34.0% for the prior year period. The decrease in the effective tax rate in the fiscal year ended June 30, 2016 as compared to the fiscal
year ended June 30, 2015 was primarily due to state deferred tax benefits recorded in Fiscal 2016 as a result of the KUPI acquisition,
as compared to overall state deferred tax expense in Fiscal 2015. In addition, research and development tax credits and domestic
manufacturing deductions relative to pre-tax income also contributed to the lower effective tax rate for Fiscal 2016 compared to Fiscal
2015.
At June 30, 2016, the Company had recognized a net deferred tax asset of $52.4 million. The net deferred tax asset is net of a
valuation allowance of $3.9 million that is primarily related to the Cody notes receivable impairment recorded in conjunction with the
acquisition of Cody Labs. The Company expects the remaining net deferred tax assets to be fully realizable based on the Company’s
history and future expectations of taxable income.
Net Income. For the fiscal year ended June 30, 2016, the Company reported net income attributable to Lannett Company, Inc. of
$44.8 million, or $1.23 basic and $1.20 per diluted share. Comparatively, net income attributable to Lannett Company, Inc. in the
prior year was $149.9 million, or $4.18 basic and $4.04 per diluted share.
Results of Operations — Fiscal 2015 compared to Fiscal 2014
Net sales increased 49% to $406.8 million for the fiscal year ended June 30, 2015. The following table identifies the Company’s
approximate net product sales by medical indication for the fiscal years ended June 30, 2015 and 2014:
(In thousands)
Medical Indication
Antibiotic
Cardiovascular
Gallstone
Glaucoma
Gout
Migraine
Muscle Relaxant
Obesity
Pain Management
Thyroid Deficiency
Urinary
Other
Total net sales
Fiscal Year Ended June 30,
2015
2014
$
$
12,306
55,166
65,262
21,145
6,833
25,729
8,779
4,004
27,461
153,460
212
26,480
406,837
$
$
13,572
62,121
6,578
11,987
10,822
14,527
—
4,032
27,174
102,248
—
20,710
273,771
Product price increases contributed $157.3 million to the overall increase in net sales, partially offset by decreased volumes of $24.2
million. The Company experienced favorable trends in product pricing on several key products during the period, as discussed below.
The following chart details price and volume changes by medical indication:
Medical indication
Antibiotic
Cardiovascular
Gallstone
Glaucoma
Gout
Migraine
Muscle Relaxant
Obesity
Pain Management
Thyroid Deficiency
Sales volume
change %
Sales price
change %
1%
(42)%
(15)%
(4)%
(37)%
(10)%
100%
9%
4%
(4)%
(10)%
30%
907%
81%
—%
87%
—%
(10)%
(3)%
54%
Thyroid Deficiency. Net sales of drugs used for the treatment of thyroid deficiency increased by $51.2 million, primarily as a result of
price increases on key products.
Gallstone. Net sales of drugs used for gallstones increased by $58.7 million. The increase in net sales was primarily attributable to
price increases on key products.
Migraine. Net sales of drugs used to treat migraines increased by $11.2 million. The increase in net sales was primarily attributable
to price increases on key products, partially offset by decreased volumes.
Glaucoma. Net sales of drugs used for the treatment of glaucoma increased by $9.2 million. The increase in net sales was primarily
attributable to price increases on key products.
Muscle Relaxant. Net sales of muscle relaxant products increased by $8.8 million due to the launch of a new product in the first
quarter of Fiscal 2015.
Pain Management. Net sales of pain management products increased $287 thousand. The increase in net sales was primarily
attributable to increased volumes of C-Topical® Solution and Oxycodone HCl Oral Solution. A lower average net sales price
resulting from an increase in return reserves related to a voluntary recall in April 2015 of one lot of product manufactured at the
Company’s facility in Cody, Wyoming, due to incorrect labeling and lower volumes on other pain management products partially
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45
�offset the increase in net sales. The Company continues to actively market its C-Topical® Solution product utilizing a group of brand
representatives in anticipation of an NDA filing.
Cardiovascular. Net sales of drugs used for cardiovascular treatment decreased by $7.0 million, primarily as a result of lower
volumes, partially offset by price increases on products used to treat congestive heart failure. The Company experienced lower
volumes and additional competition beginning in the third quarter of Fiscal 2015.
The Company sells its products to customers in various distribution channels. The table below presents the Company’s net sales to
each distribution channel for the fiscal year ended June 30:
(In thousands)
Customer Distribution Channel
Wholesaler/Distributor
Retail Chain
Mail-Order Pharmacy
Total net sales
June 30,
2015
June 30,
2014
$
$
297,675
65,130
44,032
406,837
$
$
172,503
80,710
20,558
273,771
Total net sales to wholesaler/distributor increased as a result of increased sales in a variety of products for thyroid deficiency,
gallstone and cardiovascular, as discussed above. Additionally, the increase in total net sales to wholesaler/distributor was impacted
by the strategic partnership between Amerisource Bergen and Walgreens, whereby Amerisource Bergen began product distribution on
behalf of Walgreens in third quarter of Fiscal Year 2014. Other strategic partnerships between industry wholesalers and retailers also
impacted total net sales to wholesaler/distributor and retail chain. Mail-order pharmacy total net sales increased primarily as a result
of increased sales of drugs used for the treatment of thyroid deficiency, as discussed above.
Cost of Sales, including amortization of intangibles. Cost of sales for Fiscal 2015 decreased $18.9 million to $100.5 million. The
decrease was primarily attributable to the nonrecurring $20.1 million charge related to the JSP contract renewal recorded in the first
quarter of Fiscal Year 2014 as well as lower amortization. The decrease was partially offset by increased provisions for excess and
obsolete inventory totaling $6.7 million. Amortization expense included in cost of sales totaled $137 thousand for Fiscal 2015 and
$1.4 million for Fiscal 2014.
Gross Profit. Gross profit for the fiscal year ended June 30, 2015 increased 98% to $306.4 million or 75% of total net sales. In
comparison, gross profit for the fiscal year ended June 30, 2014 was $154.4 million or 56% of total net sales. The gross profit
percentage change for the fiscal year ended June 30, 2015 was mainly attributable to product price increases. The remaining increase
was due to the charge related to the JSP contract renewal, which negatively impacted gross margin percentage by 7% in Fiscal Year
2014.
While the Company is continuously seeking to keep product costs low, there can be no guarantee that gross profit percentages will
stay consistent in future periods. Pricing pressure from competitors and costs of producing or purchasing new drugs may also
fluctuate in future periods. Changes in future product sales mix may also occur.
Research and Development. Research and development expenses increased 9% to $30.3 million for the fiscal year ended June 30,
2015 compared to $27.7 million in the prior-year period. The increase was primarily due to increased product development costs
totaling $2.0 million as well as costs associated with bio-equivalency studies and the clinical trial for the Company’s C-Topical®
Solution product totaling $1.9 million. The increase was partially offset by decreased third-party contract lab expenses totaling $2.7
million. Compensation-related and other miscellaneous expenses also contributed to the increase.
Selling, General and Administrative. Selling, general and administrative expenses increased 17% to $45.2 million for the fiscal year
ended June 30, 2015 compared with $38.6 million in the prior year period. The increase was primarily due to additional
compensation-related expenses totaling $3.1 million. Legal expenses also contributed an additional increase of $1.5 million.
The Company is focused on controlling selling, general and administrative costs; however increases in personnel and other costs to
facilitate changes in the Company’s infrastructure and expansion may impact selling, general and administrative expenses in future
periods.
Acquisition and Integration-related Expenses. Acquisition and integration-related expenses increased $4.3 million compared to the
prior year period. The increase was due to costs associated with the acquisition of Silarx, KUPI and other prospective acquisitions.
Other Income (Loss). The Company recorded a net gain on investment securities during the fiscal year ended June 30, 2015 totaling
$705 thousand compared to a net gain on investment securities totaling $1.9 million in the prior year period.
Income Tax. The Company recorded income tax expense for the fiscal year ended June 30, 2015 of $77.4 million compared to $32.9
million for the fiscal year ended June 30, 2014. The effective tax rate for the fiscal year ended June 30, 2015 was 34.0%, compared to
36.5% for the prior-year period. The decrease in the effective tax rate in the fiscal year ended June 30, 2015 as compared to the fiscal
year ended June 30, 2014 was due primarily to the effect of changes in local tax laws and domestic manufacturing deductions recorded
in Fiscal 2015. Research-related tax credits also contributed to the lower rate.
At June 30, 2015, the Company had recognized a net deferred tax asset of $28.8 million. The net deferred tax asset is net of a
valuation allowance of $2.3 million that is primarily related to the Cody notes receivable impairment recorded in conjunction with the
acquisition of Cody Labs. The Company expects the remaining net deferred tax assets to be fully realizable based on the Company’s
history and future expectations of taxable income.
Net Income. For the fiscal year ended June 30, 2015, the Company reported net income attributable to Lannett Company, Inc. of
$149.9 million, or $4.18 basic and $4.04 per diluted share. Comparatively, net income attributable to Lannett Company, Inc. in the
prior year was $57.1 million, or $1.70 basic and $1.62 per diluted share, which included the charge related to the JSP contract renewal
equal to $0.36 per diluted share.
Liquidity and Capital Resources
Cash Flow
Until November 25, 2015, the date of the KUPI acquisition, the Company had historically financed its operations with cash flow
generated from operations supplemented with borrowings from various government agencies and financial institutions. At June 30,
2016, working capital was $306.1 million as compared to $327.0 million at June 30, 2015, a decrease of $20.9 million. Current
product portfolio sales as well as sales related to future product approvals are anticipated to continue to generate positive cash flow
from operations, which we expect will be sufficient to service our outstanding debt.
Net cash from operating activities of $135.3 million for the fiscal year ended June 30, 2016 reflected net income of $44.9 million,
adjustments for non-cash items of $48.1 million, as well as cash provided by changes in operating assets and liabilities of $42.3
million. In comparison, net cash from operating activities of $128.5 million for the fiscal year ended June 30, 2015 reflected net
income of $150.0 million, offset by cash used by changes in operating assets and liabilities of $21.5 million.
Significant changes in operating assets and liabilities from June 30, 2015 to June 30, 2016 are comprised of:
• A decrease in accounts receivable of $15.1 million due to lower gross accounts receivable outstanding and the timing of
collections during the quarter ended June 30, 2016 compared to the quarter ended June 30, 2015. The Company’s days sales
outstanding (“DSO”) at June 30, 2016, based on gross sales for the fiscal year ended June 30, 2016 and gross accounts
receivable at June 30, 2016, was 77 days. The level of DSO at June 30, 2016 was comparable to the Company’s expectation
that DSO will be in the 70 to 80 day range based on customer payment terms.
• A decrease in inventories of $15.3 million primarily due to the timing of customer order fulfillment.
• A decrease in accrued payroll and payroll-related costs of $20.9 million primarily related to payments made in the third
quarter of Fiscal 2016 in connection with compensation accrued by KUPI prior to the acquisition as well as payments made
in August 2015 in connection with incentive compensation accrued in Fiscal Year 2015.
• A decrease in other assets of $7.7 million primarily related to compensation-related reimbursements received from UCB.
• An increase in settlement liability of $18.6 million related to a settlement charge recorded in the third quarter of Fiscal 2016,
partially offset by payments made pursuant to the agreement.
Significant changes in operating assets and liabilities from June 30, 2014 to June 30, 2015 are comprised of:
• An increase in accounts receivable of $25.4 million mainly due to an increase in gross accounts receivable resulting from
increased sales partially offset by increases in total revenue-related reserves. The Company’s days sales outstanding
(“DSO”) at June 30, 2015, based on gross sales for the fiscal year ended June 30, 2015 and gross accounts receivable at June
30, 2015, was 66 days. The level of DSO at June 30, 2015 was comparable to the Company’s expectation that DSO will be
in the 60 to 70 day range based on 60-70 day payment terms for most customers.
• A decrease in accrued payroll and payroll related costs of $2.5 million primarily related to tax withholdings on a restricted
stock vesting on June 30, 2014, partially offset by an increase in accrued incentive compensation costs in Fiscal Year 2015
compared to Fiscal Year 2014.
• A decrease in accounts payable of $2.5 million due to the timing of payments at the beginning of Fiscal Year 2015.
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47
�• A decrease in income taxes payable of $5.1 million primarily due to the timing of estimated tax payments made during Fiscal
2015 and excess tax benefits on stock options exercised, partially offset by Fiscal 2015 taxable income.
• An increase in rebates payable of $3.0 million due to an increase in rebates accrued resulting from sales qualifying for
existing rebates programs.
Net cash used in investing activities of $959.1 million for the fiscal year ended June 30, 2016 is mainly the result of the acquisition of
KUPI totaling $934.2 million (net of cash acquired), purchases of investment securities of $40.5 million and purchases of property,
plant and equipment of $24.3 million, partially offset by proceeds from the sale of investment securities of $39.9 million. Net cash
used in investing activities of $45.8 million for the year ended June 30, 2015 is mainly the result of the acquisition of Silarx totaling
$41.9 million, purchases of investment securities of $47.8 million and purchases of property, plant and equipment of $31.7 million,
partially offset by proceeds from the sale of investment securities of $75.8 million.
Net cash provided by financing activities of $848.2 million for the fiscal year ended June 30, 2016 was primarily due to proceeds from
the issuance of debt totaling $1.0 billion, short-term borrowings under the revolving credit facility of $125.0 million, proceeds from
issuance of stock pursuant to stock compensation plans of $4.1 million and excess tax benefits on stock option exercises of $1.5
million, partially offset by debt repayments of $295.0 million, payments of debt issuance costs totaling $34.7 million and purchases of
treasury stock totaling $1.3 million. Net cash provided by financing activities of $12.3 million for the year ended June 30, 2015 was
primarily due to proceeds from the issuance of stock pursuant to stock compensation plans of $4.9 million and excess tax benefits on
stock options exercises of $8.1 million.
Credit Facility and Other Indebtedness
The Company has previously entered into and may enter future agreements with various government agencies and financial
institutions to provide additional cash to help finance the Company’s various capital investments and potential strategic opportunities.
These borrowing arrangements as of June 30, 2016 are as follows:
Amended Senior Secured Credit Facility
On November 25, 2015, in connection with its acquisition of KUPI, Lannett entered into a credit and guaranty agreement (the “Credit
and Guaranty Agreement”) among certain of its wholly-owned domestic subsidiaries, as guarantors, Morgan Stanley Senior Funding,
Inc., as administrative agent and collateral agent and other lenders providing for a senior secured credit facility (the “Senior Secured
Credit Facility”). The Senior Secured Credit Facility consisted of Term Loan A in an aggregate principal amount of $275.0 million,
Term Loan B in an aggregate principal amount of $635.0 million and a revolving credit facility providing for revolving loans in an
aggregate principal amount of up to $125.0 million. On April 8, 2016, the Company drew down the full $125.0 million Revolving
Credit Facility for working capital and other general purposes. The entire balance of the Revolving Credit Facility loan is outstanding
as of June 30, 2016.
On June 17, 2016, Lannett amended the Senior Secured Credit Facility and the Credit and Guaranty Agreement to raise an incremental
term loan in the principal amount of $150.0 million (the “Incremental Term Loan”) and amended certain sections of the agreement
(the “Amended Senior Secured Credit Facility”). The terms of this Incremental Term Loan are substantially the same as those
applicable to the Term Loan B. The Company used the proceeds of the Incremental Term Loan and cash on hand to repurchase the
outstanding $250.0 million aggregate principal amount of Lannett’s 12.0% Senior Notes due 2023 (the “Senior Notes”) issued in
connection with the KUPI acquisition.
The Term Loan A Facility will mature on November 25, 2020. The Term Loan A Facility amortizes in quarterly installments (a)
through December 31, 2017 in amounts equal to 1.25% of the original principal amount of the Term Loan A Facility and (b) from
January 1, 2018 through September 30, 2020 in amounts equal to 2.50% of the original principal amount of the Term Loan A Facility,
with the balance payable on November 25, 2020. The Term Loan B Facility will mature on November 25, 2022. The Term Loan B
Facility amortizes in equal quarterly installments in amounts equal to 1.25% of the original principal amount of the Term Loan B
Facility with the balance payable on November 25, 2022. Any outstanding Revolving Loans will mature on November 25, 2020.
The Amended Senior Secured Credit Facility is guaranteed by all of Lannett’s significant wholly-owned domestic subsidiaries (the
“Subsidiary Guarantors”) and is collateralized by substantially all present and future assets of Lannett and the Subsidiary Guarantors.
The interest rates applicable to the Amended Term Loan Facility are based on a fluctuating rate of interest of the greater of an adjusted
LIBOR and 1.00%, plus a borrowing margin of 4.75% (for Term Loan A Facility) or 5.375% (for Term Loan B Facility). The interest
rates applicable to the Revolving Credit Facility is based on a fluctuating rate of interest of an adjusted LIBOR plus a borrowing
margin of 4.75%. The interest rate applicable to the unused commitment for the Revolving Credit Facility was initially 0.50%.
Beginning March 2016, the interest margins and unused commitment fee on the Revolving Credit Facility are subject to a leveraged
based pricing grid.
The Amended Senior Secured Credit Facility contains a number of covenants that, among other things, limit the ability of Lannett and
its restricted subsidiaries to: incur more indebtedness; pay dividends; redeem stock or make other distributions of equity; make
investments; create restrictions on the ability of Lannett’s restricted subsidiaries that are not Subsidiary Guarantors to pay dividends to
Lannett or make intercompany transfers; create negative pledges; create liens; transfer or sell assets; merge or consolidate; enter into
sale leasebacks; enter into certain transactions with Lannett’s affiliates; and prepay or amend the terms of certain indebtedness.
The Amended Senior Secured Credit Facility contains a financial performance covenant that is triggered when the aggregate principal
amount of outstanding Revolving Credit Facility and outstanding letters of credit as of the last day of the most recent fiscal quarter is
greater than 30% of the aggregate commitments under the Revolving Credit Facility. The covenant provides that Lannett shall not
permit its first lien net senior secured leverage ratio as of the last day of any four consecutive fiscal quarters (i) from and after
December 31, 2015, to be greater than 4.25:1.00 (ii) from and after December 31, 2017 to be greater than 3.75:1.00 and (iii) from and
after December 31, 2019 to be greater than 3.25:1.00.
The Amended Senior Secured Credit Facility also contains a financial performance covenant for the benefit of the Term Loan A
Facility lenders which provides that Lannett shall not permit its net senior secured leverage ratio as of the last day of any four
consecutive fiscal quarters (i) prior to December 31, 2017, to be greater than 4.25:1.00, (ii) as of December 31, 2017 and prior to
December 31, 2019 to be greater than 3.75:1.00 and (iii) as of December 31, 2019 and thereafter to be greater than 3.25:1.00.
The Amended Senior Secured Credit Facility also contains certain affirmative covenants, including financial and other reporting
requirements.
12.0% Senior Notes due 2023
On November 25, 2015, Lannett issued $250.0 million aggregate principal amount of its unsecured 12.0% Senior Notes due 2023
under an Indenture. Interest on the Senior Notes accrued at the rate of 12.0% per annum and was payable semi-annually on June 15
and December 15 of each year. The Senior Notes had a maturity date of December 15, 2023. The Senior Notes were guaranteed by
each of Lannett’s current and future domestic subsidiaries that guarantee Lannett’s obligations under the Amended Senior Secured
Credit Facility. The Senior Notes may have been redeemed at par, in whole but not in part, at any time prior to October 1, 2016.
On May 26, 2016, the Company repurchased $50.0 million of the $250.0 million aggregate principal amount of the Senior Notes. On
June 20, 2016, the Company completed the repurchase of the remaining $200.0 million of Senior Notes. The repurchase of the $250.0
million aggregate principal amount of the Senior Notes resulted in a loss on extinguishment of approximately $3.0 million.
Cody Mortgage
The Company is the primary beneficiary of a VIE called Realty. The VIE owns land and a building which is being leased to Cody
Labs. A mortgage loan with First National Bank of Cody has been consolidated in the Company’s financial statements, along with the
related land and building. As of June 30, 2016 and June 30, 2015, the effective rate was 4.5% per annum. The mortgage is
collateralized by the land and building with a net book value of $1.5 million. As of June 30, 2016, $874 thousand is outstanding under
the mortgage loan, of which $141 thousand is classified as currently due.
Other Liquidity Matters
Material Suppliers
During the renewal term of the JSP Distribution Agreement, the Company is required to use commercially reasonable efforts to
purchase minimum dollar quantities of JSP products. There is no guarantee that the Company will continue to meet the minimum
purchase requirement for Fiscal 2017 and thereafter. If the Company does not meet the minimum purchase requirements, JSP’s sole
remedy is to terminate the agreement.
Future Acquisitions
We are continuously evaluating the potential for product and company acquisitions as a part of our future growth strategy. In
conjunction with a potential acquisition, the Company may utilize current resources or seek additional sources of capital to finance
any such acquisition, which could have an impact on future liquidity.
We, or any of our affiliates may also, from time to time depending on market conditions and prices, contractual restrictions, our
financial liquidity and other factors, seek to prepay outstanding debt or repurchase our outstanding debt through open market
48
49
�purchases, privately negotiated purchases, or otherwise. The amounts involved in any such transactions, individually or in the
aggregate, may be material and may be funded from available cash or from additional borrowings.
Contractual Obligations
The following table represents annual contractual obligations as of June 30, 2016:
(In thousands)
Long-Term Debt
Operating Lease Obligations
Purchase Obligations
Contingent Consideration
Settlement Agreement
Interest on Obligations
Total
Total
$ 1,161,225
12,278
95,451
35,000
21,000
351,857
$ 1,676,811
$
Less than 1
year
178,236
1,578
41,201
35,000
7,000
70,623
333,638
$
1-3 years
3-5 years
More than 5
Years
$
$
127,117
2,222
54,250
—
14,000
130,405
327,994
$
$
285,270
2,160
—
—
—
103,387
390,817
$
$
570,602
6,318
—
—
—
47,442
624,362
Long-term debt and interest on obligations amounts above primarily relate to the Company’s Amended Senior Secured Credit Facility.
Refer to Note 11 “Long-Term Debt” for additional information.
Interest on obligations was calculated based on interest rates in effect at June 30, 2016.
The purchase obligations above are primarily due to the agreement with Jerome Stevens Pharmaceuticals, Inc. (“JSP”). If the
minimum purchase requirement is not met, JSP has the right to terminate the contract within 60 days of Lannett’s failure to meet the
requirement. If JSP terminates the contract, Lannett does not pay any fee, but could lose its exclusive distribution rights in the United
States. If Lannett’s management believes that it is not in the Company’s best interest to fulfill the minimum purchase requirements, it
can also terminate the contract without any penalty. If either party were to terminate the purchase agreement, there would be a
significant impact on the financial position, results of operations and operating cash flows of the Company. See Note 21 “Material
Contracts with Suppliers” to our Consolidated Financial Statements for more information on the terms, conditions and financial
impact of the JSP Distribution Agreement.
Operating lease obligations primarily relate to a 116,000 square foot leased warehouse in Seymour, Indiana as well as a 25 year lease
with Forward Cody, which commenced in April 2015.
Contingent consideration of $35.0 million relates to a 50/50 split of additional tax liabilities UCB will incur associated with the IRS
Section 338(H)(1) tax election. Refer to Note 2 “Summary of Significant Accounting Policies” for additional information.
Settlement agreement relates to a Settlement Agreement Release and Mutual Release with one of the Company’s former customers.
Refer to Note 22 “Settlement Agreement” for additional information.
Research and Development Arrangements
In the normal course of business, the Company has entered into certain research and development and other arrangements. As part of
these arrangements, the Company has agreed to certain contingent payments which generally become due and payable only upon the
achievement of certain developmental, regulatory, commercial and/or other milestones. In addition, under certain arrangements, we
may be required to make royalty payments based on a percentage of future sales, or other metric, for products currently in
development in the event that the Company begins to market and sell the product. Due to the inherent uncertainty related to these
developmental, regulatory, commercial and/or other milestones, it is unclear if the Company will ever be required to make such
payments. As such, these contingencies are not reflected in the expected cash requirements for Contractual Obligations in the table
above.
Prospects for the Future
As we enter our new fiscal year, we are a formidable generic drug company. We have earned the respect of our customers by our
continuous growth in product offerings and our extraordinary service as a reliable supplier. The lack of regulatory issues and the
ability to respond to our customers’ needs make our Company a desirable supplier. In 2016, we once again won the prestigious Diana
Award for Best Generic Manufacturer from the Healthcare Distribution Alliance.
Over the past several years, Lannett continued to experience substantial improvement in many important financial metrics. Each year,
our knowledge, staffs’ skills and talent increase. The Company is strengthening and building momentum to grow within the generic
pharmaceutical industry organically and through mergers and acquisitions. The recently completed acquisitions of Silarx and KUPI
display our ability to grow through M&A.
One initiative at the core of the Company’s long term strategy is our plan to vertically integrate our supply chain. Acquired in 2007
we continue leveraging Cody Labs. In July 2008, the DEA granted Cody Labs a license to directly import concentrated poppy straw
for extraction into opioid-based active pharmaceutical ingredients (“APIs”) such as Morphine Base, Hydromorphone, Hydrocodone
and Oxycodone, for use in various dosage forms for pain management.
The value of this license comes from the successful development of patentable processes. Cody Labs has filed and received numerous
patents using their expertise in API development and manufacture. Our technical skills allow the Company to perform in a market
with high barriers to entry and limited foreign and domestic competition.
Because of this vertical integration, the Company has direct control of those APIs manufactured by Cody. In this fashion we can
avoid increased costs, add to the Company’s overall margins and avoid supply chain interruptions associated with buying APIs from
third-party manufacturers. The Company can also leverage this vertical integration not only for direct supply of opioid-based APIs,
but also for the manufacture of non-opioid-based controlled drugs such as Cocaine HCl.
The Company believes that demand for controlled substances and pain management drugs, having grown from $3 billion in 2005 to
over $31 billion today, will continue based upon the “Baby Boomer” demographics. By concentrating additional resources in the
development of opioid-based APIs and dosage forms, the Company is well-positioned to take advantage of this opportunity. The
Company is currently vertically integrated on three products, with several others in various stages of development.
One product that the Company manufactures is a brand drug for use in surgery. Our C-Topical® Solution brand of cocaine
hydrochloride involves the successful patented synthetic process developed by Cody. This product is being manufactured and
marketed under the product name C-Topical® Solution. This product is an analgesic topical solution, with vasoconstriction as a side
effect, for use primarily by ear, nose and throat physicians during surgical procedures. This product represents the Company’s first
foray into the brand market. Currently, we have completed the Phase III study and our CRO is assembling the data for our New Drug
Application. As the Company continues to invest in and focus on process and manufacturing optimization, Cody Labs will continue
to be an important part of our future growth plan.
Selling brand versus generic products require a dedicated sales force to detail and educate physicians on the product. The Company
strongly believes that C-Topical®, once FDA has granted approval, will be an important contributor to total revenue, with higher than
average profit margins as a result of vertical integration. The Company’s strategic goal is to continue investing in controlled
substance product development. Revenues from manufactured products derived from controlled substances carry higher-than-average
gross margins.
In addition to focusing on the development and manufacture of opioid-based APIs and dosage forms, the Company has made a
decision to develop products which require a paragraph four (“P-IV”) certification when filing the ANDA. A P-IV certification is
required when an ANDA is submitted for a product for which the innovator’s patent has not yet expired. The certification must state
whether the patent on the reference listed drug (“RLD”) is being challenged on grounds of it being invalid, or if the patent is being
circumvented. This path to product approval represents an opportunity for our Company, because we do not have to wait until a
particular patent expires to potentially enter the market. Secondly, if our Company is the first-to-file a P-IV certification on a product
and we successfully invalidate or circumvent the patent, the FDA may grant 180 days of market exclusivity. This allows us to be the
sole competitor to the brand currently on the market for six months unless the innovator company sells an authorized generic. During
this market exclusivity period, we could capture a significant portion of the market from the brand company at reasonably higher
prices than our older products.
The Company filed its first ANDA with a P-IV certification in Fiscal 2013. As of June 30, 2016, we have 12 P-IV certifications
pending with the FDA, of which five were filed by Lannett, four by Silarx and three by KUPI. Four of the P-IV certifications are
currently being challenged. In response to our P-IV certification with respect to the Zomig® nasal spray product, AstraZeneca AB,
AstraZeneca UK Limited and Impax Laboratories, Inc. filed two patent infringement complaints against the Company in July 2014.
In response to our P-IV certification with respect to Thalomid®, Celgene Corporation and Children’s Medical Center Corporation
filed a patent infringement lawsuit against the Company in January 2015. In response to our P-IV certification with respect to
Dilaudid® Oral Solution, Purdue Pharmaceutical Products L.P, Purdue Pharma L.P and Purdue Pharma Technologies Inc. filed a
patent infringement lawsuit against the Company in August 2015. The Company is in various stages of responding to the patent
infringement claims; and in the case of Dilaudid, a settlement has been reached in principle and details are being finalized. Refer to
Note 12 “Legal and Regulatory Matters” for additional information.
50
51
�The Company has a business development group focused on mergers, acquisitions and other strategic alliances. The Company is
party to supply and development agreements with JSP, Summit Bioscience LLC, HEC Pharm Group, Pharma Pass II LLC and various
other international and domestic companies. The Company is currently in negotiations of similar agreements with other companies
and is actively seeking additional strategic partnerships, through which it will market and distribute products manufactured in-house or
by third parties. The Company plans to continue evaluating potential merger and acquisition opportunities as well as product
acquisitions that are a strategic fit and accretive to the business.
After we closed upon the Kremers Urban acquisition, we established a very aggressive integration plan. We are pleased to say that
our integration plans are moving swiftly and we will be benefitting from the synergies created through integration.
We are pleased to advise that the FDA will be inspecting our overseas pharmacokinetic subsidiary Darmantest Laboratory as well as
Firmplace, a joint venture stability lab this fall. These operations may affect lower cost benefits for stability and bioequivalency
studies in the future.
Critical Accounting Policies
The preparation of our consolidated financial statements in accordance with accounting principles generally accepted in the United
States and the rules and regulations of the SEC requires the use of estimates and assumptions. A listing of the Company’s significant
accounting policies are detailed in Note 2 “Summary of Significant Accounting Policies.” A subsection of these accounting policies
have been identified by management as “Critical Accounting Policies.” Critical accounting policies are those which require
management to make estimates using assumptions that were uncertain at the time the estimates were made and for which the use of
different assumptions, which reasonably could have been used, could have a material impact on the financial condition or results of
operations.
Management has identified the following as “Critical Accounting Policies”: Revenue Recognition, Inventories, Income Taxes,
Valuation of Long-Lived Assets, including Goodwill and Intangible Assets, In-Process Research and Development and Share-based
Compensation.
Revenue Recognition
The Company recognizes revenue when title and risk of loss have transferred to the customer and provisions for estimates, including
rebates, promotional adjustments, price adjustments, returns, chargebacks and other potential adjustments are reasonably
determinable. The Company also considers all other relevant criteria specified in SEC Staff Accounting Bulletin No. 104, Topic No.
13, “Revenue Recognition,” in determining when to recognize revenue.
When revenue is recognized, a simultaneous adjustment to gross sales is made for chargebacks, rebates, returns, promotional
adjustments and other potential adjustments. These provisions are primarily estimated based on historical experience, future
expectations, contractual arrangements with wholesalers and indirect customers and other factors known to management at the time of
accrual. Accruals for provisions are presented in the Consolidated Financial Statements as a reduction to gross sales with the
corresponding reserve presented as a reduction of accounts receivable or included as rebates payable. The reserves presented as a
reduction of accounts receivable totaled $176.1 million and $69.4 million at June 30, 2016 and June 30, 2015, respectively. Rebates
payable at June 30, 2016 and June 30, 2015 included $21.9 million and $7.6 million, respectively, for certain rebate programs,
primarily related to Medicare Part D and Medicaid and certain sales allowances and other adjustments paid to indirect customers.
The following table identifies the activity and ending balances of each major category of revenue reserve for fiscal years 2016, 2015
and 2014:
Reserve Category
(In thousands)
Balance at June 30, 2013
Current period provision
Credits issued during the period
Balance at June 30, 2014
Additions related to the Silarx acquisition
Current period provision
Credits issued during the period
Balance at June 30, 2015
Additions related to the KUPI acquisition
Current period provision
Credits issued during the period
Balance at June 30, 2016
Chargeback
s
Rebates
Returns
Other
Total
$
$
7,267
144,578
(121,525)
30,320
1,042
338,668
(334,229)
35,801
49,333
646,926
(645,565)
86,495
$
$
3,581
56,346
(44,836)
15,091
1,176
83,364
(79,133)
20,498
38,471
189,210
(194,095)
54,084
$
$
6,689
6,632
(3,980)
9,341
712
17,707
(8,551)
19,209
20,498
21,298
(20,412)
40,593
$
$
1,000
21,462
(20,675)
1,787
—
30,661
(30,920)
1,528
6,455
49,976
(41,108)
16,851
$
$
18,537
229,018
(191,016)
56,539
2,930
470,400
(452,833)
77,036
114,757
907,410
(901,180)
198,023
For the fiscal years ended June 30, 2016, 2015 and 2014, as a percentage of gross sales the provision for chargebacks was 44.6%,
38.6% and 28.8%, respectively, the provision for rebates was 13.0%, 9.5% and 11.2%, respectively, the provision for returns was
1.5%, 2.0% and 1.3%, respectively and the provision for other adjustments was 3.4%, 3.5% and 4.3%, respectively.
The increase in total reserves from June 30, 2015 to June 30, 2016 was due to increases in all reserve categories primarily as a result
of reserves acquired in connection with the acquisition of KUPI. The activity in the “Other” category includes shelf-stock, shipping
and other sales adjustments including prompt payment discounts. Historically, we have not recorded any material amounts in the
current period related to reversals or additions of prior period reserves. If the Company were to record a material reversal or addition
of any prior period reserve amount, it would be separately disclosed.
Provisions for chargebacks, rebates, returns and other adjustments require varying degrees of subjectivity. While rebates generally are
based on contractual terms and require minimal estimation, chargebacks and returns require management to make more subjective
assumptions. Each major category is discussed in detail below:
Chargebacks
The provision for chargebacks is the most significant and complex estimate used in the recognition of revenue. The Company
sells its products directly to wholesale distributors, generic distributors, retail pharmacy chains and mail-order pharmacies. The
Company also sells its products indirectly to independent pharmacies, managed care organizations, hospitals, nursing homes and
group purchasing organizations, collectively referred to as “indirect customers.” The Company enters into agreements with its
indirect customers to establish pricing for certain products. The indirect customers then independently select a wholesaler from
which to purchase the products. If the price paid by the indirect customers is lower than the price paid by the wholesaler, the
Company will provide a credit, called a chargeback, to the wholesaler for the difference between the contractual price with the
indirect customers and the wholesaler purchase price. The provision for chargebacks is based on expected sell-through levels by
the Company’s wholesale customers to the indirect customers and estimated wholesaler inventory levels. As sales to the large
wholesale customers, such as Cardinal Health, AmerisourceBergen and McKesson increase (decrease), the reserve for
chargebacks will also generally increase (decrease). However, the size of the increase (decrease) depends on product mix and
the amount of sales made to indirect customers with which the Company has specific chargeback agreements. The Company
continually monitors the reserve for chargebacks and makes adjustments when management believes that expected chargebacks
may differ from the actual chargeback reserve.
Rebates
Rebates are offered to the Company’s key chain drug store, distributor and wholesaler customers to promote customer loyalty
and increase product sales. These rebate programs provide customers with credits upon attainment of pre-established volumes or
attainment of net sales milestones for a specified period. Other promotional programs are incentive programs offered to the
customers. Additionally, as a result of the Patient Protection and Affordable Care Act (“PPACA”) enacted in the U.S. in March
2010, the Company participates in a new cost-sharing program for certain Medicare Part D beneficiaries designed primarily for
the sale of brand drugs and certain generic drugs if their FDA approval was granted under a New Drug Application (“NDA”) or
505(b) NDA versus an ANDA. Because our drugs used for the treatment of thyroid deficiency and our Morphine Sulfate Oral
Solution product were both approved by the FDA as 505(b)(2) NDAs, they are considered “brand” drugs for purposes of the
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53
�PPACA. Drugs purchased within the Medicare Part D coverage gap (commonly referred to as the “donut hole”) result in
additional rebates. The Company estimates the reserve for rebates and other promotional credit programs based on the specific
terms in each agreement when revenue is recognized. The reserve for rebates increases (decreases) as sales to certain wholesale
and retail customers increase (decrease). However, since these rebate programs are not identical for all customers, the size of the
reserve will depend on the mix of sales to customers that are eligible to receive rebates.
assigned to each class of assets acquired and liabilities assumed are based on, among other factors, the expected future period of
benefit of the asset, the various characteristics of the asset and projected future cash flows. Significant judgment is employed in
determining the assumptions utilized as of the acquisition date and for each subsequent measurement period. Accordingly, changes in
assumptions described above, could have a material impact on our consolidated results of operations.
Returns
Consistent with industry practice, the Company has a product returns policy that allows customers to return product within a
specified time period prior to and subsequent to the product’s expiration date in exchange for a credit to be applied to future
purchases. The Company’s policy requires that the customer obtain pre-approval from the Company for any qualifying return.
The Company estimates its provision for returns based on historical experience, changes to business practices, credit terms and
any extenuating circumstances known to management. While historical experience has allowed for reasonable estimations in the
past, future returns may or may not follow historical trends. The Company continually monitors the reserve for returns and
makes adjustments when management believes that actual product returns may differ from the established reserve. Generally,
the reserve for returns increases as net sales increase.
Other Adjustments
Other adjustments consist primarily of price adjustments, also known as “shelf-stock adjustments” and “price protections,”
which are both credits issued to reflect increases or decreases in the invoice or contract prices of the Company’s products. In the
case of a price decrease, a credit is given for product remaining in customer’s inventories at the time of the price reduction.
Contractual price protection results in a similar credit when the invoice or contract prices of the Company’s products increase,
effectively allowing customers to purchase products at previous prices for a specified period of time. Amounts recorded for
estimated shelf-stock adjustments and price protections are based upon specified terms with direct customers, estimated changes
in market prices and estimates of inventory held by customers. The Company regularly monitors these and other factors and
evaluates the reserve as additional information becomes available. Other adjustments also include prompt payment discounts.
Inventories
Inventories are stated at the lower of cost or market determined by the first-in, first-out method. Inventories are regularly reviewed
and provisions for excess and obsolete inventory are recorded based primarily on current inventory levels and estimated sales
forecasts. During the fiscal years ended June 30, 2016, 2015 and 2014, the Company recorded provisions for excess and obsolete
inventory of $9.4 million, $6.7 million and $2.9 million, respectively.
Income Taxes
The Company uses an asset and liability approach to account for income taxes as prescribed by ASC 740, Income Taxes. Deferred
taxes are recorded to reflect the tax consequences on future years of events that the Company has already recognized in the financial
statement or tax returns. Deferred income tax assets and liabilities are adjusted to recognize the effect of changes in tax law or tax
rates in the period during which the new law is enacted. Under ASC 740, Income Taxes, a valuation allowance is required when it is
more likely than not that all or some portion of the deferred tax assets will not be realized through generating sufficient future taxable
income. Failure to achieve forecasted taxable income in applicable tax jurisdictions could affect the ultimate realization of deferred
tax assets and could result in an increase in the Company’s effective tax rate on future earnings.
The Company may recognize the tax benefit from an uncertain tax position claimed on a tax return only if it is more likely than not
that the tax position will be sustained on examination by the taxing authorities, based on the technical merits of the position. The tax
benefits recognized in the financial statements from such a position should be measured based on the largest benefit that has a greater
than 50% likelihood of being realized upon ultimate settlement. The benefit from uncertain tax positions recorded in the financial
statements was immaterial for all periods presented.
The Company’s future effective income tax rate is highly reliant on future projections of taxable income, tax legislation and potential
tax planning strategies. A change in any of these factors could materially affect the effective income tax rate of the Company in future
periods.
Business Combinations
Acquired businesses are accounted for using the acquisition method of accounting, which requires that the assets acquired and
liabilities assumed be recorded at the date of acquisition at their respective estimated fair values. The fair values and useful lives
Valuation of Long-Lived Assets, including Goodwill and Intangible Assets
The Company’s long-lived assets primarily consist of property, plant and equipment, definite and indefinite-lived intangible assets and
goodwill.
Property, plant and equipment are stated at cost less accumulated depreciation. Depreciation is computed on a straight-line basis over
the assets’ estimated useful lives, generally for periods ranging from 5 to 39 years. Definite-lived intangible assets are stated at cost
less accumulated amortization and are amortized on a straight-line basis over the assets’ estimated useful lives, generally for periods
ranging from 10 to 15 years. The Company continually evaluates the reasonableness of the useful lives of these assets.
Property, plant and equipment and definite-lived intangible assets are reviewed for impairment whenever events or changes in
circumstances (“triggering events”) indicate that the carrying amount of the asset may not be recoverable. The nature and timing of
triggering events by their very nature are unpredictable; however, management regularly considers the performance of an asset as
compared to its expectations, industry events, industry and economic trends, as well as any other relevant information known to
management when determining if a triggering event occurred. If a triggering event is determined to have occurred, the first step in the
impairment test is to compare the asset’s carrying value to the undiscounted cash flows expected to be generated by the asset. If the
carrying value exceeds the undiscounted cash flow of the asset, then an impairment exists. An impairment loss is measured as the
excess of the asset’s carrying value over its fair value, which in most cases is calculated using a discounted cash flow model.
Discounted cash flow models are highly reliant on various assumptions which are considered Level 3 inputs, including estimates of
future cash flows (including long-term growth rates), discount rates and the probability of achieving the estimated cash flows. The
judgments made in determining the estimated fair value can materially impact our results of operations.
Goodwill and indefinite-lived intangible assets, including in-process research and development, are not amortized. Instead, goodwill
and indefinite-lived intangible assets are tested for impairment annually during the fourth quarter of each fiscal year, or more
frequently whenever events or changes in circumstances (“triggering events”) indicate that the asset might be impaired. The Company
first performs a qualitative assessment to determine if the quantitative impairment test is required. If changes in circumstances
indicate an asset may be impaired, the Company performs the quantitative test. The quantitative impairment test consists of a Step I
analysis that requires a comparison between the reporting unit’s fair value and carrying amount. If the fair value of the reporting unit
exceeds its carrying amount, impairment does not exist and no further analysis is required. A Step II analysis would be required if the
fair value of the reporting unit is lower than its carrying amount. If the carrying amount of a reporting unit exceeds the fair value, Step
II of the quantitative impairment test requires the allocation of the reporting unit fair value to all of its assets and liabilities using the
acquisition method prescribed under authoritative guidance for business combinations with any residual fair value being allocated to
goodwill or indefinite-lived intangibles. An impairment charge is recognized only when the implied fair value of the reporting unit’s
goodwill or indefinite-lived intangible is less than its carrying amount. The judgments made in determining the estimated fair value of
goodwill and indefinite-lived intangible asset can materially impact our results of operations. The Company’s fair value assessments
are highly reliant on various assumptions which are considered Level 3 inputs, including estimates of future cash flows (including
long-term growth rates), discount rates and the probability of achieving the estimated cash flows. The Company has one reportable
segment and one reporting unit, generic pharmaceuticals.
In-Process Research and Development
Acquired businesses are accounted for using the acquisition method of accounting. The acquisition purchase price is allocated to the
net assets of the acquired business at their respective fair values. Amounts allocated to in-process research and development are
recorded at fair value and are considered indefinite-lived intangible assets subject to the impairment testing in accordance with the
Company’s impairment testing policy for indefinite-lived intangible assets as described above. As products in development are
approved for sale, amounts will be allocated to product rights and will be amortized over their estimated useful lives. Definite-lived
intangible assets are amortized over the expected life of the asset. The judgments made in determining the estimated fair value of in-
process research and development, as well as asset lives, can materially impact our results of operations. The Company’s fair value
assessments are highly reliant on various assumptions which are considered Level 3 inputs, including estimates of future cash flows
(including long-term growth rates), discount rates and the probability of achieving the estimated cash flows. During the fourth quarter
of Fiscal 2016, as part of the Company’s annual test of goodwill and indefinite-lived intangibles, an impairment charge equal to $8.0
million was recorded. In Fiscal 2015, no impairment charges were recorded.
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55
�Share-based Compensation
Share-based compensation costs are recognized over the vesting period, using a straight-line method, based on the fair value of the
instrument on the date of grant less an estimate for expected forfeitures. The Company uses the Black-Scholes valuation model to
determine the fair value of stock options and the market price on the grant date to value restricted stock. The Black-Scholes valuation
model includes various assumptions, including the expected volatility, the expected life of the award, dividend yield and the risk-free
interest rate. These assumptions involve inherent uncertainties based on market conditions which are generally outside the Company’s
control. Changes in these assumptions could have a material impact on share-based compensation costs recognized in the financial
statements.
The following table presents the weighted average assumptions used to estimate fair values of the stock options granted during the
years ended June 30 and the estimated annual forfeiture rates used to recognize the associated compensation expense:
Risk-free interest rate
Expected volatility
Expected dividend yield
Forfeiture rate
Expected term
June 30,
2016
June 30,
2015
June 30,
2014
1.7%
48.3%
0.0%
6.5%
1.7%
52.1%
0.0%
6.5%
2.1%
62.8%
0.0%
7.5%
5.2 years
5.5 years
5.9 years
Expected volatility is based on the historical volatility of the price of our common shares during the historical period equal to the
expected term of the option. The Company uses historical information to estimate the expected term, which represents the period of
time that options granted are expected to be outstanding. The risk-free rate for the period equal to the expected life of the option is
based on the U.S. Treasury yield curve in effect at the time of grant. The forfeiture rate assumption is the estimated annual rate at
which unvested awards are expected to be forfeited during the vesting period. This assumption is based on our actual forfeiture rate
on historical awards. Periodically, management will assess whether it is necessary to adjust the estimated rate to reflect changes in
actual forfeitures or changes in expectations. Additionally, the expected dividend yield is equal to zero, as the Company has not
historically issued and has no immediate plans to issue, a dividend.
Recent Accounting Pronouncements
In May 2014, the FASB issued ASU 2014-09, Revenue from Contracts with Customers. The core principle of the guidance is that an
entity should recognize revenue to depict the transfer of promised goods or services to customers in an amount that reflects the
consideration to which the entity expects to be entitled in exchange for those goods or services. The authoritative guidance is effective
for annual reporting periods beginning after December 15, 2016. In July 2015, the FASB extended the effective date of the guidance
by one year to December 15, 2017. The Company is currently in the process of assessing the impact this guidance will have on the
consolidated financial statements.
In April 2015, the FASB issued ASU 2015-03, Simplifying the Presentation of Debt Issuance Costs which changes the presentation of
debt issuance costs in financial statements. ASU 2015-03 requires an entity to present such costs in the balance sheet as a direct
deduction from the related debt liability rather than as an asset. Amortization of the costs will continue to be reported as interest
expense. It is effective for fiscal years and interim periods within those fiscal years beginning after December 15, 2015. Early
adoption is permitted. The new guidance will be applied retrospectively to each prior period presented. The Company has elected to
early adopt ASU 2015-03 as of December 31, 2015.
In July 2015, the FASB issued ASU 2015-11, Inventory — Simplifying the Measurement of Inventory. ASU 2015-11 requires
inventory to be subsequently measured using the lower of cost or net realizable value, thereby eliminating the market value approach.
Net realizable value is defined as the “estimated selling prices in the ordinary course of business, less reasonably predictable costs of
completion, disposal and transportation.” ASU 2015-11 is effective for reporting periods beginning after December 15, 2016 and is
applied prospectively. Early adoption is permitted. The Company is currently in the process of assessing the impact this guidance
will have on the consolidated financial statements.
In September 2015, the FASB issued ASU 2015-16, Business Combinations — Simplifying the Accounting for Measurement-Period
Adjustments. ASU 2015-16 requires that an acquirer recognize adjustments to provisional amounts that are identified during the
measurement period in the reporting period in which the adjustment amounts are determined. ASU 2015-16 also requires that the
acquirer record, in the same period’s financial statements, the effect on earnings of changes in depreciation, amortization, or other
income effects, if any, as a result of the change to the provisional amounts, calculated as if the accounting had been completed at the
acquisition date. ASU 2015-16 is effective for reporting periods beginning after December 15, 2015 and is applied prospectively.
Early adoption is permitted. The Company has elected to early adopt ASU 2015-16 as of March 31, 2016.
In November 2015, the FASB issued ASU 2015-17, Income Taxes — Balance Sheet Classification of Deferred Taxes. ASU 2015-17
requires all deferred tax assets and liabilities to be classified as noncurrent on the balance sheet. The guidance may be applied either
prospectively or retrospectively. ASU 2015-17 is effective for fiscal years and interim periods within those fiscal years beginning
after December 15, 2016. Early adoption is permitted. The Company is currently in the process of assessing the impact this guidance
will have on the consolidated financial statements.
In February 2016, the FASB issued ASU 2016-02, Leases. ASU 2016-02 requires an entity to recognize right-of-use assets and
liabilities on its balance sheet for all leases with terms longer than 12 months. Lessees and lessors are required to disclose quantitative
and qualitative information about leasing arrangements to enable a user of the financial statements to assess the amount, timing and
uncertainty of cash flows arising from leases.
ASU 2016-02 is effective for annual reporting periods beginning after December 15, 2018, including interim periods within that
reporting period and requires a modified retrospective application, with early adoption permitted. The Company is currently in the
process of assessing the impact this guidance will have on the consolidated financial statements.
In March 2016, the FASB issued ASU 2016-09, Compensation — Stock Compensation: Improvements to Employee Share-Based
Payment Accounting. ASU 2016-09 clarifies several aspects of accounting for share-based compensation including the accounting for
excess tax benefits and deficiencies, accounting for forfeitures and the classification of excess tax benefits on the cash flow statement.
ASU 2016-09 is effective for fiscal years beginning after December 15, 2016 and in interim periods within those fiscal years, with
early adoption permitted. The Company is currently in the process of assessing the impact this guidance will have on the consolidated
financial statements.
ITEM 7A.
QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK
On November 25, 2015, in connection with the acquisition of KUPI, the Company entered into a Senior Secured Credit Facility,
which was subsequently amended in June 2016. Based on the variable-rate debt outstanding at June 30, 2016, each 1/8% increase in
interest rates would yield $1.5 million of incremental annual interest expense.
A mortgage loan with First National Bank of Cody has been consolidated in the Company’s financial statements, along with the
related land and building. The mortgage requires monthly principal and interest payments of $15 thousand. As of June 30, 2016 and
June 30, 2015, the effective interest rate was 4.5% per annum. The mortgage is collateralized by the land and building with a net book
value of $1.5 million. As of June 30, 2016, $874 thousand is outstanding under the mortgage loan.
The Company invests in equity securities, U.S. government agency securities and corporate bonds, which are exposed to market and
interest rate fluctuations. The market value, interest and dividends earned on these investments may vary based on fluctuations in
interest rate and market conditions.
ITEM 8.
FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA
The Consolidated Financial Statements and Report of the Independent Registered Public Accounting Firm is set forth in Item 15 of
this Annual Report on Form 10-K under the caption “Consolidated Financial Statements” and incorporated herein by reference.
CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL
ITEM 9.
DISCLOSURE
None.
ITEM 9A.
CONTROLS AND PROCEDURES
Disclosure Controls and Procedures
We carried out an evaluation under the supervision and with the participation of our management, including our chief executive
officer and chief financial officer, of the effectiveness of the design and operation of our disclosure controls and procedures, as such
term is defined under Rule 13a-15(e) promulgated under the Securities Exchange Act of 1934 (the “Exchange Act”), as amended, for
financial reporting as of June 30, 2016. Based on that evaluation, our chief executive officer and chief financial officer concluded that
these controls and procedures are effective to ensure that information required to be disclosed by the Company in reports that it files or
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�submits under the Exchange Act is recorded, processed, summarized and reported as specified in Securities and Exchange
Commission rules and forms and is accumulated and communicated to our management to allow timely decisions regarding required
disclosures. There were no changes in these controls or procedures identified in connection with the evaluation of such controls or
procedures that occurred during our last fiscal quarter, or in other factors that have materially affected, or are reasonably likely to
materially affect these controls or procedures.
Our disclosure controls and procedures are designed to ensure that information required to be disclosed by us in the reports that we file
or submit under the Exchange Act is recorded, processed, summarized and reported, within the time periods specified in the rules and
forms of the Securities and Exchange Commission. These disclosure controls and procedures include, among other things, controls
and procedures designed to ensure that information required to be disclosed by us in the reports that we file under the Exchange Act is
accumulated and communicated to our management, including our chief executive officer and chief financial officer, as appropriate to
allow timely decisions regarding required disclosure.
Management’s Report on Internal Control over Financial Reporting
The report of management of the Company regarding internal control over financial reporting is set forth in Item 15 of this Annual
Report on Form 10-K under the caption “Consolidated Financial Statements: Management’s Report on Internal Control Over
Financial Reporting “ and incorporated herein by reference.
Attestation Report of Independent Registered Public Accounting Firm
The attestation report of the Company’s independent registered public accounting firm regarding internal control over financial
reporting is set forth in Item 15 of this Annual Report on Form 10-K under the caption “Consolidated Financial Statements: Report of
Independent Registered Public Accounting Firm” and incorporated herein by reference.
Changes in Internal Control over Financial Reporting
During the quarter ended June 30, 2016, there were no changes in the Company’s internal control over financial reporting (as defined
in Rule 13a-15(f) of the Exchange Act) that materially affected, or are reasonably likely to materially affect, the Company’s internal
control over financial reporting.
ITEM 9B.
OTHER INFORMATION
None.
ITEM 10.
DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE
PART III
Directors and Executive Officers
The directors and executive officers of the Company are set forth below:
Age
Position
Directors:
Jeffrey Farber
Arthur P. Bedrosian
David Drabik
Paul Taveira
James M. Maher
Albert Paonessa, III
Officers:
Arthur P. Bedrosian
Martin P. Galvan
Kevin R. Smith
John M. Abt
Dr. Mahendra Dedhiya
Robert Ehlinger
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70
64
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51
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Chairman of the Board
Director
Director
Director
Director
Director
Chief Executive Officer
Vice President of Finance, Chief Financial Officer and Treasurer
Senior Vice President of Sales and Marketing
Vice President of Quality
Chief Scientific Affairs
Vice President and Chief Information Officer
Jeffrey Farber was appointed a Director of the Company in May 2006 and was appointed Chairman of the Board of Directors in July
2012. Jeffrey Farber joined the Company in August 2003 as Secretary. Since 1994, Mr. Farber has been President and the owner of
Auburn Pharmaceutical (“Auburn”), a national generic pharmaceutical distributor. Prior to starting Auburn, Mr. Farber served in
various positions at Major Pharmaceutical (“Major”), where he was employed for over 15 years. At Major, Mr. Farber was involved
in sales, purchasing and eventually served as President of the Midwest division. Mr. Farber also spent time working at Major’s
manufacturing division, Vitarine Pharmaceuticals, where he served on its Board of Directors. Mr. Farber joined the Board of
Directors of the Karmanos Cancer Center in June 2015. The Karmanos Cancer Center is a not-for-profit national cancer center in
Michigan. Mr. Farber graduated from Western Michigan University with a Bachelors of Science Degree in Business Administration
and participated in the Pharmacy Management Graduate Program at Long Island University.
The Governance and Nominating Committee concluded that Mr. Farber is qualified and should continue to serve, due, in part, to his
significant experience in the generic drug industry and his ongoing role as the owner of a highly regarded and successful generic drug
distributor. His skills include a thorough knowledge of the generic drug marketplace and drug supply chain management.
David Drabik was elected a Director of the Company in January 2011. Mr. Drabik is a National Association of Corporate Directors
Governance Fellow. Since 2002, Mr. Drabik has been President of Cranbrook & Co., LLC (“Cranbrook”), an advisory firm primarily
serving the private equity and venture capital community. At Cranbrook, Mr. Drabik assists and advises its clientele on originating,
structuring and executing private equity and venture capital transactions. From 1995 to 2002, Mr. Drabik served in various roles and
positions with UBS Capital Americas (and its predecessor UBS Capital LLC), a New York City based private equity and venture
capital firm that managed $1.5 billion of capital. From 1992 to 1995, Mr. Drabik was a banker with Union Bank of Switzerland’s
Corporate and Institutional Banking division in New York City. Mr. Drabik graduated from the University of Michigan with a
Bachelors of Business Administration degree.
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�The Governance and Nominating Committee concluded that Mr. Drabik is well qualified and should be nominated to serve as a
Director due, in part, to his understanding and involvement in investment banking. As a global investment bank professional with
extensive experience advising senior management, his skills include business analytics, financing and a strong familiarity with SEC
documentation. Mr. Drabik is an independent director as defined by the rules of the NYSE.
Paul Taveira was appointed a Director of the Company in May 2012. Mr. Taveira has been Chief Executive Officer of the National
Response Corporation, an international firm specializing in environmental services, since June 2015. He previously served on the
Board of Directors and as the Chief Executive Officer of A&D Environmental Services Inc., an environmental and industrial services
company. From 2007 to 2009, Mr. Taveira was a Managing Partner of Precision Source LLC, a manufacturer of precision parts for
various industries across the United States. From 1997 to 2007, Mr. Taveira held several positions at PSC Inc., a national provider of
environmental services, including President, Vice President and Regional General Manager. From 1987 to 1997, Mr. Taveira held
several management positions with Clean Harbors Inc., an international provider of environmental and energy services. Mr. Taveira
graduated from Worcester State University with a Bachelor of Science degree in Biology.
The Governance and Nominating Committee concluded that Mr. Taveira is well qualified and should be nominated to serve as a
Director due, in part, to his understanding and experience as a Chief Executive Officer and Director of A&D Environmental Services
Inc. Additionally, Mr. Taveira has experience as a Managing Partner of Precision Source LLC, a manufacturer of precision parts for
various industries across the United States. Mr. Taveira is an independent director as defined by the rules of the NYSE.
James M. Maher was appointed as a Director of the Company in June 2013. He spent his entire 37 year professional career with
PricewaterhouseCoopers (PwC) LLP, including 27 years as a partner, before retiring in June 2012. Most recently, Maher served as the
managing partner of PwC’s U.S. assurance practice, comprised of more than 1,100 partners and 12,000 staff. Previously, he served as
the regional assurance leader for the metro assurance practice. During his tenure at PwC, Maher worked closely with senior
management at several multinational companies, dealing extensively with significant acquisitions, divestitures, initial public offerings
and secondary offerings. Maher earned a bachelor’s degree in Accounting from LIU Post.
The Governance and Nominating Committee concluded that Mr. Maher is well qualified and should be nominated to serve as a
Director, due to his extensive experience at PricewaterhouseCoopers. Additionally, Mr. Maher has significant experience in dealing
with acquisitions, divestitures, initial public offerings and secondary offerings. Mr. Maher is an independent director as defined by the
rules of the NYSE.
Albert Paonessa, III was appointed as a Director of the Company in July 2015. Mr. Paonessa retired from Anda, Inc., the fourth
largest distributor of generic drugs in the U.S. in January 2015 after serving as President for the past 10 years. He previously served
as Anda’s Senior Vice President of Sales and before that as Vice President of IT. Earlier, Mr. Paonessa was Vice President of
Operations for VIP Pharmaceuticals, which was acquired by Anda’s parent company Andrx, in 2000. Mr. Paonessa earned a Bachelor
of Arts degree in Interpersonal Communications from Bowling Green State University.
The Governance and Nominating Committee concluded that Mr. Paonessa is well qualified and should be nominated to serve as a
Director due, in part, to his significant experience in different executive roles within the generic pharmaceutical industry.
Additionally, Mr. Paonessa has a strong operational and technical background, especially in the areas of sales, IT, planning and
budgeting and business development. Mr. Paonessa is an independent director as defined by the rules of the NYSE.
Arthur P. Bedrosian, J.D. was promoted to President of the Company in May 2002 and CEO in January of 2006. Previously, he
served as the Company’s Vice President of Business Development from January 2002 to April 2002. Mr. Bedrosian was elected as a
Director in February 2000 and served to January 2002. Mr. Bedrosian was re-elected a Director in January 2006. Mr. Bedrosian has
operated generic drug manufacturing, sales and marketing businesses in the healthcare industry for many years. Prior to joining the
Company, from 1999 to 2001, Mr. Bedrosian served as President and Chief Executive Officer of Trinity Laboratories, Inc., a medical
device and drug manufacturer. Mr. Bedrosian also operated Pharmaceutical Ventures Ltd, a healthcare consultancy, Pharmeral, Inc. a
drug representation company selling generic drugs and Interal Corporation, a computer consultancy to Fortune 100 companies. Mr.
Bedrosian holds a Bachelor of Arts Degree in Political Science from Queens College of the City University of New York and a Juris
Doctorate from Newport University in California.
The Governance and Nominating Committee concluded that Mr. Bedrosian is qualified to serve as a director, in part, because his
experience as our Chief Executive Officer has been instrumental in the Company’s growth and provides the board with a compelling
understanding of our operations, challenges and opportunities. In addition, his background includes over 40 years in the generic
pharmaceutical industry that encompasses a broad background and knowledge in the underlying scientific, sales, marketing and supply
chain management which brings special expertise to the board in developing our business strategies. His recent qualification to
FINRA’s list of arbitrators recognizes his expertise and experience.
Martin P. Galvan, CPA was appointed as the Company’s Vice President of Finance, Chief Financial Officer and Treasurer in August
2011. Most recently, he was Chief Financial Officer of CardioNet, Inc., a medical technology and service company. From 2001 to
2007, Mr. Galvan was employed by Viasys Healthcare Inc., a healthcare technology company that was acquired by Cardinal Health,
Inc. in June 2007. Prior to the acquisition, he served as Executive Vice President, Chief Financial Officer and Director Investor
Relations. From 1999 to 2001, Mr. Galvan served as Chief Financial Officer of Rodel, Inc., a precision surface technologies company
in the semiconductor industry. From 1979 to 1998, Mr. Galvan held several positions with Rhone-Poulenc Rorer Inc., a
pharmaceutical company, including Vice President, Finance — The Americas; President & General Manager, RPR Mexico & Central
America; Vice President, Finance, Europe/Asia Pacific; and Chief Financial Officer, United Kingdom & Ireland. Mr. Galvan began
his career with the international accounting firm Ernst & Young LLP. He earned a Bachelor of Arts degree in economics from
Rutgers University and is a member of the American Institute of Certified Public Accountants.
Kevin R. Smith joined the Company in January 2002 as Vice President of Sales and Marketing. Prior to this, from 2000 to 2001, he
served as Director of National Accounts for Bi-Coastal Pharmaceutical, Inc., a pharmaceutical sales representation company. Prior to
this, from 1999 to 2000, he served as National Accounts Manager for Mova Laboratories Inc., a pharmaceutical manufacturer. Prior
to this, from 1991 to 1999, Mr. Smith served as National Sales Manager at Sidmak Laboratories, a pharmaceutical manufacturer. Mr.
Smith has extensive experience in the generic sales market and brings to the Company a vast network of customers, including retail
chain pharmacies, wholesale distributors, mail-order wholesalers and generic distributors. Mr. Smith has a Bachelor of Science
Degree in Business Administration from Gettysburg College.
John M. Abt joined the Company in March 2015 as Vice President of Quality. Prior to joining the Company, Mr. Abt held senior
level positons in both quality and operations and has extensive knowledge in pharmaceutical manufacturing, quality, strategy, business
improvement and site transformation. He most recently served as Teva Pharmaceuticals’ Vice President Global Quality Strategy,
overseeing the development and implementation of strategy and associated initiatives for the global quality organization. Before that,
he held a number of leadership positions of increasing responsibility in operations, continuous improvement, quality systems and
compliance. He earned his Masters of Administrative Science in Business Management from John Hopkins University and a Bachelor
of Science in Biochemistry from Niagara University.
Dr. Mahendra Dedhiya joined the Company as Chief Scientific Affairs in June 2015. Prior to joining the Company, Dr. Dedhiya
served as Silarx Pharmaceuticals’ Executive Vice President of Scientific Affairs from 2014 to 2015, overseeing research and
development and regulatory affairs among other responsibilities. Before that, he held a number of positions of increasing
responsibility for Forest Pharmaceuticals from 2001 to 2014, rising to Executive Director. Prior to his tenure at Forest
Pharmaceuticals, Dr. Dedhiya served as Director of Product Development at Roxane Laboratories and held a number of positions at
other Pharmaceutical Companies. He earned a Doctor of Philosophy degree from the University of Michigan in Pharmaceutics, a
Master of Science degree in Medicinal Chemistry from the University of Rhode Island, a Bachelor of Science from University of
Poona and MBA from University of Bridgeport.
Robert Ehlinger joined the Company in July 2006 as Chief Information Officer. In June 2011, Mr. Ehlinger was promoted to Vice
President of Logistics and Chief Information Officer. Prior to joining Lannett, Mr. Ehlinger was the Vice President of Information
Technology at MedQuist, Inc., a healthcare services provider, where his career spanned 10 years in progressive operational and
technology roles. Prior to MedQuist, Mr. Ehlinger was with Kennedy Health Systems as their Corporate Director of Information
Technology supporting acute care and ambulatory care health information systems and biomedical support services. Earlier on, Mr.
Ehlinger was with Dowty Communications where he held various technical and operational support roles prior to assuming the role of
International Distribution Sales Executive managing the Latin America sales distribution channels. Mr. Ehlinger received a
Bachelor’s of Arts degree in Physics from Gettysburg College in Gettysburg, PA.
To the best of the Company’s knowledge, there have been no events under any bankruptcy act, no criminal proceedings and no
judgments or injunctions that are material to the evaluation of the ability or integrity of any director, executive officer, or significant
employee during the past ten years.
Section 16(a) Beneficial Ownership Reporting Compliance
Section 16(a) of the Securities Exchange Act of 1934 requires the Company’s directors, officers and persons who own more than 10%
of a registered class of the Company’s equity securities to file with the SEC reports of ownership and changes in ownership of
common stock and other equity securities of the Company. Officers, directors and greater-than-10% stockholders are required by SEC
regulations to furnish the Company with copies of all Section 16(a) forms they file.
Based solely on review of the copies of such reports furnished to the Company or written representations that no other reports were
required, the Company believes that during Fiscal 2016 all filing requirements applicable to its officers, directors and greater-than-
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�10% beneficial owners under Section 16(a) of the Exchange Act were complied with in a timely manner, except for a Form 4 for Dr.
Mahendra Dedhiya related to a purchase of shares on February 5, 2016, a Form 4 for John Abt related to shares withheld by the
Company to satisfy tax withholding obligations for a restricted stock vesting on March 30, 2016 and Form 4s for various executive
officers related to shares withheld by the Company to satisfy tax withholding obligations for restricted stock vestings on April 24,
2016.
ITEM 11.
EXECUTIVE COMPENSATION
Compensation Discussion and Analysis
Code of Ethics
The Company has adopted the Code of Professional Conduct (the “code of ethics”), a code of ethics that applies to the Company’s
Chief Executive Officer and Chief Financial Officer, as well as all other company personnel. The code of ethics is publicly available
on our website at www.lannett.com. If the Company makes any substantive amendments to the code of ethics or grants any waiver,
including any implicit waiver, from a provision of the code to our Chief Executive Officer, Chief Financial Officer, or any other
executive, we will disclose the nature of such amendment or waiver on our website or in a report on Form 8-K.
Audit Committee
The Audit Committee has responsibility for overseeing the Company’s financial reporting process on behalf of the Board. In addition,
Audit Committee responsibilities include selection of the Company’s independent auditors, conferring with the independent auditors
regarding their audit of the Company’s consolidated financial statements, pre-approving and reviewing the independent auditors’ fees
and considering whether non-audit services are compatible with maintaining their independence and considering the adequacy of
internal financial controls. The Audit Committee operates pursuant to a written charter adopted by the Board, which is available on
the Company’s website at www.lannett.com. The charter describes the nature and scope of the Audit Committee’s responsibilities.
The members of the Audit Committee consist of Paul Taveira, David Drabik and James M. Maher. All members of the Audit
Committee are independent directors as defined by the rules of the NYSE.
Financial Expert on Audit Committee: The Board has determined that James M. Maher, current director and chairman of the audit
committee, is the audit committee financial expert as defined in section 3(a)(58) of the Exchange Act and the related rules of the
Commission.
This Compensation Discussion and Analysis (CD&A) describes our 2016 Executive Compensation Program. It provides an overview
of the compensation program for the following Named Executive Officers (NEOs) and how the Compensation Committee of the
Board of Directors (the Committee) made its decisions for our 2016 fiscal year (July 1, 2015 — June 30, 2016).
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
John M. Abt
Robert Ehlinger
Michael Bogda
William Schreck
Title/Role
Chief Executive Officer (CEO)
Vice President of Finance, Chief Financial Officer and Treasurer
Senior Vice President of Sales and Marketing
Vice President of Quality
Vice President of Logistics and Chief Information Officer
Former President*
Former Chief Operating Officer*
* Mr. Bogda departed the Company effective June 3, 2016
** Mr. Schreck departed the Company effective September 11, 2015
Say on Pay Results in 2015
At our annual shareholders meeting in January 2012, our shareholders supported a triennial cycle for “say-on-pay” advisory votes
relating to our Executive Compensation Program for NEOs. At that time, and again in January 2015, we provided our shareholders
with the opportunity to approve, or to vote against, the compensation of our NEOs, as required by the Dodd-Frank Wall Street Reform
and Consumer Protection Act (Dodd-Frank Act). At our January 2015 meeting, approximately 96% of the shareholders who voted on
the “say-on-pay” proposal supported our program.
Although this vote is non-binding, its outcome, along with shareholder feedback and the competitive business environment, plays an
important role in how the Committee makes decisions about the program’s structure. To this end, during the past few years, the
Committee conducted periodic reviews of the Executive Compensation Program, monitored industry practices and sought feedback
from some of our largest investors.
The following pages of this CD&A highlight performance results since Fiscal 2013 that have had a direct impact on the compensation
paid to our NEOs over the same period of time. It looks specifically at the performance measures used in the short- and long-term
incentive awards under the Executive Compensation Program that the Committee believes drive shareholder value. It also describes
recently approved changes for Fiscal 2017 to further align our Executive Compensation Program with our objectives and best
competitive practice.
A Word About Risk
The Committee believes that incentive plans, along with the other elements of the Executive Compensation Program, provide
appropriate rewards to our NEOs to keep them focused on our goals. The Committee also believes that the program’s structure, along
with its oversight, continues to provide a setting that does not encourage the NEOs to take excessive risks in their business decisions.
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�Fiscal 2016 Executive Compensation Program Changes
Overview of the Executive Compensation Program
As our Company grows, the Committee is committed to the evolution and improvement of our Executive Compensation Program to
ensure alignment with our business strategy and shareholder interests, as well as best competitive practices. The Committee made the
following adjustments to the program’s core compensation elements for 2016:
What’s Changed
Short-Term Incentives
(Annual Bonus)
Long-Term Incentives
How It’s Changed
Explanation
•
•
•
Increased Threshold performance hurdles
from 80% of Target to 90% of Target, to
account for the anticipated lack of growth
in Fiscal 2016 performance results.
Increased the target award opportunity for
the CEO from 75% of salary to 80% of
salary, to improve pay competitiveness.
Increased target award opportunities for
several NEOs to improve pay
competitiveness, with grants for Fiscal
2016 performance to be provided through
a value mix of 65% restricted stock and
35% stock options.
• Grant levels will continue to be tied to
Company performance, and can range
from 0% to 150% of target awards based
on actual results versus pre-established
goals.
• Grants under this program occurred in
July 2016, following the determination of
actual results for Fiscal 2016.
No changes were made to performance
metrics or weightings. Following several
years of extraordinary growth, Fiscal 2016
financial performance results were expected
to be slightly below Fiscal 2015 levels. As a
result, the Committee increased the
Threshold performance hurdle, relative to
Target, to focus NEOs on achieving Fiscal
2016 performance targets.
The Committee continued to link equity grant
levels to Company performance to strengthen
alignment with shareholder interests. The
increased emphasis on restricted stock
relative to stock options helps manage equity
plan share usage and dilution levels, focuses
executives on long-term shareholder value
creation, and further reinforces the
Company’s leadership retention strategy.
Our Philosophy
A fundamental objective of our Executive Compensation Program is to focus our executives on creating long-term shareholder value
— all aspects of our program are rooted in this goal and designed around the following guiding principles:
•
Pay for performance: A significant portion of compensation should be variable and directly linked to corporate and individual
performance goals and results.
• Competitiveness: Compensation should be sufficiently competitive to attract, motivate and retain an executive team fully capable
of driving exceptional performance.
• Alignment: The interests of executives should be aligned with those of our shareholders through equity-based compensation and
performance measures that help to drive shareholder value over the long term.
To support these guiding principles, our program includes the following compensation elements:
Pay Element
Base Salary
Form
Cash
(Fixed)
Short-Term Incentives
(Annual Bonus)
Cash
(Variable)
Long-Term Incentives
Equity
(Variable)
Purpose
Provides a competitive level of compensation that reflects position
responsibilities, strategic importance of the position and individual
experience.
Provides a cash-based award that recognizes the achievement of
corporate goals in support of the annual business plan, as well as specific,
qualitative and quantitative individual goals for the most recently
completed fiscal year.
Provides incentives for management to execute on financial and strategic
goals that drive long-term shareholder value creation and support the
Company’s retention strategy.
Target Compensation Mix
Our Commitment to Sound Corporate Governance
In order to align our executive compensation program with long-term shareholder interests, we have adopted a variety of sound
corporate governance practices, as illustrated in the following table:
The charts below show that most of our NEO’s target compensation for Fiscal 2016 is variable (74% for our CEO and an average of
62% for our other NEOs). Variable pay includes the target value of short-term cash incentives (“STI”), stock options, and restricted
stock.
What We Do
• Emphasize variable incentives to align pay with
performance
• Tie incentive compensation to multiple performance
metrics that reinforce key business objectives
• Place primary emphasis on equity compensation to
align executive and shareholder interests
•
What We Don’t Do
Provide multi-year pay guarantees within
employment agreements
• Allow stock option repricing without shareholder
approval
• Permit stock hedging or pledging activities
• Use stock ownership guidelines for executive officers
• Provide uncapped incentive awards
and non-employee directors
• Maintain a clawback policy allowing for the
• Pay tax gross-ups on any awards
recoupment of excess compensation in the event of a
material financial restatement and fraud or misconduct
• Engage an independent compensation consultant to
• Provide excessive executive perquisites
advise the Compensation Committee
Based upon Fiscal 2016 compensation as reported in the Summary Compensation Table on page 77 of this Form 10-K, variable pay
represents 75% of total pay for our CEO and 66% of average total pay for our other NEOs. This mix reflects below-target annual
incentives earned in Fiscal 2016 under the Annual Bonus Plan (shown as STI), above-target equity grants in Fiscal 2016 based on
Fiscal 2015 Company performance, and one-time special recognition cash awards for the successful closing of the KUPI transaction
66
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�and related integration activities during Fiscal 2016. The emphasis on variable pay would be lower if comparisons included equity
grants in the year earned, since equity grants in Fiscal 2017 based on Fiscal 2016 performance were well below target levels.
How Compensation Decisions Are Made
•
•
The Role of the Compensation Committee. The Committee, composed entirely of independent directors, is responsible for
making executive compensation decisions for the NEOs. The Committee works closely with its independent compensation
consultant, Pearl Meyer & Partners (“Pearl Meyer”), and management to examine pay and performance matters throughout the
year. The Committee’s charter, which sets out its objectives and responsibilities, can be found at our website at www.lannett.com
under Investor Relations.
The Committee has authority and responsibility to establish and periodically review our Executive Compensation Program and
compensation philosophy. Importantly, the Committee also has the sole responsibility for approving the corporate performance
goals upon which compensation for the CEO is based, evaluating the CEO’s performance and determining and approving the
CEO’s compensation, including equity-based compensation, based on the achievement of his goals. The Committee also reviews
and approves compensation levels for other NEOs, taking into consideration recommendations from the CEO.
In making its determinations, the Committee considers market data and advice from Pearl Meyer, as well as budgets, reports,
performance assessments and other information provided by management. It also considers other factors, such as the experience,
skill sets, and contributions of each NEO towards our overall success. However, the Committee is ultimately responsible for all
compensation-related decisions for the NEOs and may exercise its own business judgment when evaluating performance results
and making compensation decisions.
Timing of Committee Meetings and Grants; Option and Share Pricing
The Committee meets as necessary to fulfill its responsibilities, and the timing of these meetings is established during the year.
The Committee holds special meetings from time to time as its workload requires. Annual equity grants typically occur after
finalizing fiscal year end performance results. Historically, annual grants of equity awards were typically approved at a meeting
of the Committee in August/September of each year to reward prior year performance. Beginning with grants made in Fiscal
2015, equity grants occur in the July/August time frame, reflecting the Company’s status change to a large accelerated filer (with
an expedited filing date requirement) as a result of our strong growth and significant increase in equity market capitalization.
Individual grants (for example, associated with the timing of a new NEO or promotion to an NEO position) may occur at any time
of year. The exercise price of each stock option and fair value of restricted stock awarded to our NEOs is the closing price of our
common stock on the date of grant.
The Role of the CEO. The CEO does not play any role in the Committee’s determination of his own compensation. However, he
presents the Committee with recommendations for each element of compensation including base salaries and short- and long-term
incentive awards for the other NEOs, as well as non-executive employees who are eligible for equity grants. The CEO bases
these recommendations upon his assessment of each individual’s performance, as well as market practice. The Committee has
full discretion to modify the recommendations of the CEO in the course of its approvals.
•
The Role of the Independent Consultant. The Committee consults, as needed, with an outside compensation consulting firm.
As it makes decisions about executive compensation, the Committee reviews data and advice from its consultant about current
compensation practices and trends among publicly-traded companies in general and comparable generic pharmaceutical
companies in particular.
The Committee also reviews recommendations from its outside consultant and makes recommendations to the Board about the
compensation for non-employee directors.
In Fiscal 2015, Pearl Meyer was retained by the Committee, as its independent consultant, to review the competitiveness of the
Executive Compensation Program. Pearl Meyer provided the Committee with compensation data with respect to similarly sized
biopharmaceutical and life sciences companies and consulted with the Committee about a variety of issues related to competitive
compensation practices and incentive plan designs. Pearl Meyer was also retained by the Committee in Fiscal 2016 to review the
competitiveness of the Executive Compensation Program and to provide ongoing advice relating to the Executive Compensation
Program. The Committee assessed the independence of Pearl Meyer pursuant to the SEC rules and concluded that no conflict of
interest exists that would prevent Pearl Meyer from independently advising the Committee.
Peer Group & Benchmarking
The Committee evaluates industry-specific and general market compensation practices and trends to ensure the Executive
Compensation Program is appropriately competitive. When making decisions about the program for Fiscal 2016, the Committee
considered publicly-available data, as well as a market study conducted by Pearl Meyer in July 2015. The Pearl Meyer study
developed market values using a blend of peer group proxy pay data for the companies shown below as well as published survey data
for the broader life sciences industry. Using this information, the Committee compared our program to the compensation practices of
other companies which the Committee believes are comparable to the Company in terms of size, scope and business complexity (the
peer group). As shown below, the Company ranked in the upper half of the peer group in terms of revenues and profitability and
slightly below the 50th percentile for equity market capitalization.
Company Name
Aceto Corp.
Akorn, Inc.
Albany Molecular Research Inc.
Amphastar Pharmaceuticals, Inc.
Cambrex Corporation.
Depomed, Inc.
Impax Laboratories Inc.
INSYS Therapeutics, Inc.
The Medicines Company
Pernix Therapeutics Holdings, Inc.
Sagent Pharmaceuticals, Inc.
Lannett Company, Inc.
% Rank
Fiscal Year
End # of
Employees
270
1,644
2,220
1,460
1,228
494
1,290
510
614
274
440
1,149
55%
Equity
Fiscal Year
Fiscal
Market Cap.
6/30/2016
($mm)
End Operating Year End
Income
($mm)
Sales
($mm)
Cumulative
3 YR TSR
6/30/2016
$
$
$
$
$
$
$
$
$
$
$
$
648
3,402
466
723
1,654
1,199
2,127
926
2,340
27
492
874
45%
$
$
$
$
$
$
$
$
$
$
$
$
$
54
$
150
23
$
(3) $
$
107
$
1
$
97
102
$
(257) $
(71) $
$
$
9
131
91%
547
593
402
252
434
343
860
331
309
176
318
542
73%
57%
111%
13%
N/A
270%
249%
45%
180%
9%
-88%
-29%
100%
60%
Following the KUPI acquisition, and based on recommendations from Pearl Meyer, the Committee approved changes to the peer
group for Fiscal 2017 to account for the Company’s significant increase in size. The Committee approved the exclusion of former
peers Albany Molecular Research Inc., Pernix Therapeutics Holdings Inc., and Sagent Pharmaceuticals Inc., on the basis of size and
business focus. The Committee also approved the addition of Horizon Pharma plc, Jazz Pharmaceuticals plc, Prestige Brand Holdings
Inc., and United Therapeutics Corporation. These additional companies compete with us for business and executive talent, and were
added to the peer group to round out the sample size. Compared with the revised peer group, the Company is near the 50th percentile
in terms of net sales and between the 50th and 75th percentiles in terms of operating income.
The Committee uses external market data as a reference point to ensure the Company’s executive compensation program is
sufficiently competitive to attract, retain, and motivate highly experienced and talented NEOs. The Committee generally seeks to
position target total direct compensation for NEOs at or near 50th percentile market values for comparable positions, but does not
utilize a purely formulaic benchmarking approach. Based on the July 2015 Pearl Meyer study, target total direct compensation,
68
69
�including the sum of base salary plus target short-term and long-term incentives, was within a competitive range (defined as +/- 10%)
of 50th percentile market values for then-current NEOs except for Messrs. Bedrosian and Galvan, who were below the competitive
range, and Mr. Abt, who was recently recruited to the Company and was above the competitive range. Excluding Mr. Bedrosian,
whose target pay was below the 25th percentile, aggregate target total direct compensation was equal to 96% of the 50th percentile.
As previously noted, when evaluating our executive compensation program, the Committee considers a variety of other factors in
addition to external market data, such as Company and individual performance, and each NEO’s qualifications, skill sets, and past and
expected future contributions towards our success.
2016 Executive Compensation Program Decisions
Base Salary
We attribute much of our success to our highly-experienced executive management team, and the strength of their leadership has been
clearly demonstrated by our exceptional long-term performance results and growth. In order to remain competitive among our
industry peers, the Committee believes it must set compensation at market-competitive levels that reflect the executive’s experience,
role and responsibilities. In Fiscal 2016, the Committee approved base salary increases to Messrs. Bedrosian, Galvan, and Smith to
bring them to the 50th percentile of comparable organizations, as reported in Pearl Meyer’s July 2015 market pay analysis, and modest
merit increases for Messrs. Ehlinger and Abt. No base salary increases were provided for Messrs. Bogda and Schreck, both of whom
departed from the Company during Fiscal 2016.
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
Robert Ehlinger
John Abt*
2015 Base Salary
2016 Base Salary
% Change
$
$
$
$
$
555,170
326,510
286,340
236,900
286,000
$
$
$
$
$
615,129
354,916
314,974
242,823
289,632
11%
9%
10%
3%
1%
* Mr. Abt was hired during Fiscal 2015
Short-Term Incentives (Annual Bonus)
The Company’s NEOs participate in an annual bonus program, which is designed to reinforce the annual business plan and budgeted
goals and to recognize yearly performance achievements focused primarily on financial and operating results. Actual payouts can
range from 0% (below threshold) to 200% (superior performance) of target awards and are paid in cash. The Committee sets each
NEO’s threshold, target and superior bonus opportunity as a percentage of base salary, as follows:
NEO
Arthur P. Bedrosian
Martin P. Galvan, Kevin Smith, John Abt
Robert Ehlinger
Annual Bonus Opportunity As a % of Salary
Target
(100% of Target)
Superior
(200% of Target)
Threshold
(25% of Target)
20%
15%
12.5%
80%
60%
50%
160%
120%
100%
In Fiscal 2016, Mr. Bedrosian’s target award opportunity was increased from 75% of salary to 80% of salary to align more closely
with 50th percentile market values. Expressed as percentages of salary, Fiscal 2016 award opportunities for all other NEOs were the
same as those established in Fiscal 2015.
The overall annual bonus plan for Fiscal 2016 is comprised of two components:
• Corporate Financial & Operational Goals: 90% (95% for the CEO) of the total target award opportunity is tied to
operating results versus targets established by the Committee to promote a focus on Company-wide profitable growth and
collaboration:
Performance Metric
Adjusted Operating Income
Adjusted Earnings Per Share (EPS)
Adjusted Net Sales
Individual Objectives
Weighting (Out of 100%)
CEO
Other NEOs
50%
25%
20%
5%
50%
20%
20%
10%
Fiscal 2016 performance metrics and weightings were the same as those established in Fiscal 2015. Adjusted Operating Income
is defined as operating income excluding bonus and stock-based compensation expense, as further adjusted for certain non-
recurring items. Adjusted EPS is defined as diluted EPS excluding bonus and stock-based compensation expense, as further
adjusted for certain non-recurring items. Adjusted Net Sales is defined as Net Sales excluding the impact of a customer
settlement charge. Any adjustments are reviewed and approved by the Committee.
•
Individual Objectives: 10% (5% for the CEO) of the total target award opportunity is based on the achievement of pre-
established quantitative and qualitative individual goals, to promote individual accountability and “line of sight.” Fiscal 2016
goals were tied to various strategic, financial and operational objectives, taking into consideration each NEO’s job function and
responsibilities. For competitive harm reasons, the Company does not disclose specific details on individual goals and strategic
objectives, although major accomplishments in Fiscal 2016 for each NEO are listed on page 72.
2016 Short-Term Incentives (Annual Bonus): Results and Payouts
• Corporate Financial & Operational Results (Collectively Weighted 90% to 95% of Target Award). Following several years
of extraordinary growth, Fiscal 2016 performance results were expected to be at or below Fiscal 2015 levels. Fiscal 2016 Target
goals for Adjusted Operating Income and Adjusted EPS were set at Fiscal 2015 actual levels, and the Adjusted Net Sales Target
was set slightly above Fiscal 2015 actual results. These goals were established prior to the KUPI acquisition, and therefore, all
Fiscal 2016 performance goals and actual results exclude the KUPI transaction. Based on the established Target goals, the
Committee increased the hurdle for Fiscal 2016 Threshold performance goals from 80% of Target to 90% of Target goals. The
Committee viewed these performance hurdles as very challenging in light of then-current internal forecasts and economic
conditions. For Fiscal 2016, the Committee established financial performance goals ranging from 90% of Target (Threshold) to
120% of Target (Superior):
Performance Metric
Adjusted Operating Income ($
millions)
Adjusted Earnings Per Share
(EPS)
Adjusted Net Sales ($
millions)
Weighting
(Out of 100%)
50%
20% (25% for CEO)
20%
Performance Goals (Excluding KUPI Transaction)
Actual
Superior
Target
Threshold
$
$
$
220.7
3.93
393.3
$
$
$
245.2
4.37
437.0
$
$
$
294.2
5.24
524.4
$
$
$
207.1
3.79
400.4
Excluding the impact of the KUPI acquisition, actual Fiscal 2016 performance results were below Threshold levels for Adjusted
Operating Income and Adjusted EPS, and between Threshold and Target levels for Adjusted Net Sales. Actual Adjusted
Operating Income for Fiscal 2016 excluded pre-tax items totaling $76 million, including acquisition-related expenditures,
purchase accounting-related expenses due to the KUPI acquisition, and other non-recurring one-time items.
70
71
�Actual Adjusted EPS excluded the same $76 million in pre-tax items that were excluded from Adjusted Operating Income plus
$70 million in interest expense and the tax effects for all of these items. The Adjusted Net Sales performance metric excluded
items totaling $142 million, including KUPI sales of approximately $166 million between the date of acquisition and fiscal year
end and $24 million related to a customer settlement.
•
Individual Results (Collectively Weighted 5% of Target Award for the CEO and 10% for other Current NEOs).
NEO
Arthur P. Bedrosian
Performance Highlights
• Doubled the size of the Company through acquisitions
• Reduced product concentrations
• Restored relations with major KUPI customer
• Refinanced $250 million 12% Senior Note within six months of closing the Acquisition
• Led and managed C-Suite leadership/succession planning with Human Resources
Martin P. Galvan
• Delivered accurate financial reports on a required monthly, quarterly and annual basis as an accelerated
Kevin Smith
filer with the SEC while integrating the two M&A transactions
• Worked with CEO to refinance $250 million Senior Note
• Contributed to the integration of Silarx and KUPI
• Assembled and mentored an executive M&A and banking team
• Doubled sales of Silarx products and integrated KUPI acquisition and reorganized sales team
•
• Transitioned CSO into in-house sales team for C-Topical brand sales
Introduced Silarx and KUPI products and increased market share on Lannett products
John Abt
•
Introduced new quality initiatives at all sites in systemic Quality procedures
Robert Ehlinger
• Headed the Integration Management Office to integrate the two M&A transactions
• Assembled team to upgrade SAP at Lannett
•
• Assembled and headed the separation and eventual integration of SAP from UCB to Lannett
• Made IT software compatible with internal SOX compliance initiatives
Introduced SAP at both Silarx and Cody Labs sites
Individual goals are not shown for Messrs. Bogda and Schreck, both of whom departed from the Company during Fiscal 2016 and did
not receive a bonus.
Total Annual Bonus
Based on our performance results and individual contributions, the NEOs earned below-Target awards for the corporate operational
component and awards between Threshold and Target levels for the individual component under the Annual Bonus Plan. Overall
awards for current NEOs were equal to approximately 11.3% (9.3% for the CEO) of target amounts. Total awards for each of the
NEOs were as follows:
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
John Abt
Robert Ehlinger
Operational Results Portion of the
Bonus (90% to 95%)
$
$
$
$
$
36,734
19,870
17,634
16,215
11,329
Individual Results Portion
of the Bonus (5% to 10%)
9,183
$
3,974
$
3,527
$
3,243
$
2,266
$
Total Actual Bonus
45,917
23,844
21,161
19,458
13,595
$
$
$
$
$
Short-term incentive awards earned in Fiscal 2016 were well-below awards earned in Fiscal 2015, reflecting below-target performance
results in Fiscal 2016 as compared with near-superior performance in Fiscal 2015.
Special Recognition Awards for KUPI Transaction
To recognize the successful closing of the KUPI acquisition and related integration activities during Fiscal 2016, the Committee
approved one-time cash awards to our NEOs and other key employees who were actively involved with the transaction. The
Committee approved an aggregate award pool equal to approximately $2.7 million, with approximately 66% allocated to our NEOs.
Special recognition awards to our NEOs were as follows:
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
John Abt
Robert Ehlinger
Percentage of Total Special
Recognition Award Pool
Special Recognition Transaction
Incentive
27.9% $
15.8% $
7.0% $
6.1% $
9.0% $
811,484
492,928
178,840
154,321
229,228
In approving these awards, the Committee considered the efforts and contributions of each executive towards the KUPI transaction,
which nearly doubled the size of the Company and greatly expanded the product portfolio, and the significant progress achieved in
terms of integration activities during Fiscal 2016.
Long-Term Incentives
In Fiscal 2015, the Committee approved a new long-term incentive program that ties equity grant levels to Company performance,
using the same financial and operational metrics as under the Annual Bonus Plan. Each NEO had a target award opportunity equal to
100% of base salary, provided through an equally weighted value mix of stock options and restricted stock. Actual grants can range
from 0% (for below threshold results) to 150% (for superior performance) of target award levels:
Fiscal 2015 Performance Result
Below Threshold
Threshold (80% of Budget)
Target (100% of Budget)
Superior (120% of Budget)
Percentage of Target Equity Grants Earned
(as % of Target Grant)
0% (subject to Committee discretion)
50%
100%
150%
Grants Made in Fiscal 2016 (Based on Fiscal 2015 Performance)
In Fiscal 2015, the Company achieved above-target financial performance results and NEOs exceeded individual performance goals.
As a result, the Committee approved the following grants to NEO in Fiscal 2016, effective as of July 22, 2015:
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
John Abt
Robert Ehlinger
Michael Bogda*
William Schreck*
Equity Grants Earned Based on Fiscal 2015 Performance
# of Stock Options
# of Restricted Shares
15,280
8,990
7,880
1,970
6,300
7,710
9,810
6,880
4,040
3,550
880
2,830
3,470
4,410
* Messrs. Bogda and Schreck departed from the Company during Fiscal 2016. Per the terms of their Separation Agreements,
Messrs. Bogda’s and Schreck’s awards fully vested upon their departure.
These stock options vest in three equal annual increments, beginning on the first anniversary of grant and expire on the tenth
anniversary from the date of grant. Each stock option has an exercise price of $59.20, equal to our closing stock price on the date of
grant. Restricted stock also vests in three equal annual increments, beginning on the first anniversary of grant. These grants are
included in the Summary Compensation Table and Grants of Plan-Based Awards Table in the Form 10-K and proxy filings for Fiscal
2016, per current SEC reporting requirements. Mr. Bedrosian also received a grant of 4,223 common shares on July 22, 2015, along
with all other members of our Board of Directors, to recognize Fiscal 2015 board service.
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73
�Grants Made in Fiscal 2017 (Based on Fiscal 2016 Performance)
In Fiscal 2016, the Committee increased target long-term incentive award opportunities to 200% of salary for Mr. Bedrosian and
125% of salary for Messrs. Galvan and Smith to more closely align with 50th percentile market values. Expressed as percentages of
salary, no changes were made to target award opportunities for Messrs. Abt, and Ehlinger. Consistent with the change made to the
Fiscal 2016 Annual Bonus Plan, the Committee also increased Threshold hurdles for Fiscal 2016 performance goals from 80% of
Target to 90% of Target. The Committee also modified the mix for any earned awards, with 65% of the grant value provided in the
form of restricted stock and 35% in the form of stock options. This change was made to help manage equity plan share usage and
dilution levels and to enhance executive retention. Actual grants could range from 0% (for below threshold results) to 150% (for
superior performance) of target award levels:
Fiscal 2016 Performance Result
Below Threshold
Threshold (90% of Target)
Target (100% of Target)
Superior (120% of Target)
Percentage of Target Equity Grants Earned
(as % of Target Grant)
0% (subject to Committee discretion)
50%
100%
150%
In Fiscal 2016, and excluding the KUPI acquisition, the Company achieved financial performance results between Threshold and
Target levels for Adjusted Net Sales and below Threshold levels for profitability. Based on Company financial and individual
performance results, the Committee approved the following grants to NEO in Fiscal 2017, with grant date values ranging from
approximately 15% to 18% of target award levels, and effective as of July 27, 2016:
to designated beneficiaries. Premiums paid for coverage above $50,000 are treated as imputed income. Lannett also provides
short- and long-term disability insurance which would, in the event of disability, pay the NEO 60% of his base salary up to the
plan limits of $2,000 per week for short-term disability and $15,000 per month for long-term disability. The NEOs are also
provided with car allowances.
•
•
Post-Termination Pay. The Committee believes that reasonable severance and change-in-control benefits are necessary in order
to recruit and retain qualified senior executives and are generally required by the competitive recruiting environment within our
industry and the marketplace in general. These severance benefits reflect the fact that it may be difficult for our NEOs to find
comparable employment within a short period of time, and are designed to alleviate concerns about the loss of his or her position
without cause. The Committee also believes that a change-in-control arrangement will provide security that will likely reduce the
reluctance of an NEO to pursue a change in control transaction that could be in the best interest of our shareholders. Lannett’s
severance plan is designed to pay severance benefits to a NEO for a qualifying separation. For the CEO, the severance plan
provides for payment of three times base salary, plus a pro-rated annual cash bonus for the current year calculated as if all targets
and goals are achieved. For the other NEOs, the severance plan provides for a payment of 18-months of base salary, plus a pro-
rated annual cash bonus for the current year calculated as if all targets and goals are achieved.
Tax and Accounting Implications. Section 162(m) of the Internal Revenue Code of 1986, as amended, precludes the
deductibility of a NEO’s compensation that exceeds $1,000,000 per year unless the compensation is paid under a performance-
based plan that has been approved by shareholders. The Committee believes that it is generally preferable to comply with the
requirements of 162(m) through, for example, the use of certain types of equity grants under our 2014 Long-Term Incentive Plan.
However, to maintain flexibility in compensating NEOs in a manner consistent with our compensation philosophy, the Committee
may elect to provide compensation outside those requirements when it deems appropriate. The Committee believes that
shareholder interests are best served by not restricting the Committee’s discretion in this regard, even though such compensation
may result in non-deductible compensation expenses to the Company.
Equity Grants Earned Based on Fiscal 2016 Performance
# of Stock Options
# of Restricted Shares
Looking Ahead: Executive Compensation Program Changes for Fiscal 2017
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
John Abt
Robert Ehlinger
4,088
1,769
1,570
1,155
968
3,718
1,609
1,428
1,050
881
These stock options vest in three equal annual increments, beginning on the first anniversary of grant and expire on the tenth
anniversary from the date of grant. Each stock option has an exercise price of $31.30, equal to our closing stock price on the date of
grant. Restricted stock also vests in three equal annual increments, beginning on the first anniversary of grant. These grants will be
included in the Summary Compensation Table and Grants of Plan-Based Awards Table in the Form 10-K and proxy filings for Fiscal
2017, per current SEC reporting requirements.
Other Policies, Programs and Guidelines
The Company currently maintains a clawback policy under the Sarbanes-Oxley Act, with incentive awards for the CEO and CFO
subject to recoupment in the event of a material financial restatement triggered by fraud or misconduct. Additionally, any employee
who violates the provisions of the Company’s Code of Business Conduct and Ethics is subject to disciplinary penalties that may
include termination of employment. The Committee intends to comply with any regulatory requirements pertaining to clawback
provisions under the Dodd-Frank Act once rules are finalized by the SEC and New York Stock Exchange.
NEOs, like all other employees, have retirement programs and other benefits as part of their overall compensation package. The
Committee believes that these programs and benefits support our compensation philosophy, part of which is to provide compensation
that is sufficiently competitive to attract, motivate and retain an executive team fully capable of driving exceptional performance. The
Committee periodically reviews these programs to validate that they are reasonable and consistent with market practice. Attributed
costs of the personal benefits available to the NEOs are included in column (i) of the Summary Compensation Table on page 77.
• Retirement Benefits. Each of our NEOs is eligible to participate in a 401(k) plan that is available to all employees. The
Company provides matching contributions on a $0.50 basis up to 8% of the contributing employee’s base salary, subject to
limitations of the 401(k) plan and applicable law.
• Other Benefits. Our NEOs are eligible to participate in the same health benefits available to all other employees — there are no
special medical plans for our NEOs. Lannett provides life insurance for NEOs which would, in the event of death, pay $115,000
For Fiscal 2017, the Committee decided to increase base salaries for certain NEOs, modify the short-term incentive (Annual Bonus)
design, and modify the long-term incentive plan design, as shown below:
•
Base Salaries. For Fiscal 2017, the Committee approved the following market adjustments to position base salaries for our NEOs
at or near 50th percentile market values, which increased significantly for most executives following the KUPI transaction and the
doubling in Company size:
NEO
Arthur P. Bedrosian
Martin P. Galvan
Kevin Smith
Robert Ehlinger
John Abt
2016 Base Salary
615,129
354,916
314,974
242,823
289,632
$
$
$
$
$
2017 Annual Base Salary % Change
$
$
$
$
$
735,000
415,000
370,000
280,000
289,632
19%
17%
17%
15%
—%
•
Short-Term Incentives (Annual Bonus). For Fiscal 2017, performance metrics and weightings are the same as those for Fiscal
2016. The target annual bonus opportunity for Mr. Bedrosian increased to 90% of base salary. For other NEOs, target annual
bonus opportunities, expressed as percentages of base salary, are the same as in Fiscal 2016. Based on established Target
performance goals for Fiscal 2017, the Committee chose to maintain Threshold performance levels at 90% of Target and Superior
performance levels at 120% of Target.
74
75
�•
Long-Term Incentives. Equity grant levels will be based on the Company’s Fiscal 2017 financial performance using the same
metrics as under the Annual Bonus Plan. Based on established Target performance goals for Fiscal 2017, and consistent with the
Fiscal 2017 Annual Bonus Plan design, the Committee established Threshold performance at 90% of Target levels and Superior
performance at 120% of Target levels. Expressed as percentages of base salary, target long-term incentive award opportunities
will equal 300% for Mr. Bedrosian, 200% for Mr. Galvan, 150% for Mr. Smith, and 100% for Messrs. Abt and Ehlinger. Actual
grant levels will range from 0% to 150% of target levels, based on Fiscal 2017 performance, as follows:
COMPENSATION OF EXECUTIVE OFFICERS
Overview
Fiscal 2017 Performance Result
Below Threshold
Threshold (90% of Target)
Target (100% of Target)
Superior (120% of Target)
Percentage of Target Award Opportunity
Earned
0% (subject to Committee discretion)
50%
100%
150%
For any award values earned, the Company is considering the following equity award mix: 45% will be provided in the form of
restricted stock that vests based on continued service, 30% stock options, and 25% will be provided in the form of performance-based
restricted stock tied to our 3-year total shareholder return (TSR) relative to industry peers. Grants, if any, will occur following the end
of Fiscal 2017, with stock options and time-based restricted stock vesting in three equal annual increments based on continued service
with the Company, and performance-based restricted shares only vesting if our 3-year TSR is at or above the 50th percentile of
companies included in our 2016 industry peer group. This expected change in award mix was made to further align executive and
shareholder interests.
•
Financial Planning Allowance. Beginning in Fiscal 2017, the Committee approved an annual financial planning allowance of
up to $15,000 per NEO. The executive is responsible for any tax liability associated with the financial planning benefit.
REPORT OF THE COMPENSATION COMMITTEE
The Compensation Committee has reviewed, discussed and approved the CD&A as set forth above with management. Taking this
review and discussion into account, the undersigned Committee members recommend to the Board of Directors that the CD&A be
included in the annual report on Form 10-K.
Paul Taveira, Chairman
David Drabik
James Maher
Albert Paonessa III
The tables and narratives set forth below provide specified information concerning the compensation of our Named Executive Officers
(NEOs) for the fiscal year ended June 30, 2016.
Summary Compensation Table
This table summarizes all compensation paid to or earned by our NEOs for fiscal years 2016, 2015 and 2014.
Name and Principal Position
(a)
Arthur P. Bedrosian
Chief Executive Officer
Michael Bogda
Former President
Martin P. Galvan
Vice President of Finance and
Chief Financial Officer
William Schreck
Former Chief Operating Officer
Kevin Smith
Senior Vice President of Sales
and Marketing
Robert Ehlinger
Vice President of Logistics and
Chief Information Officer
John Abt
Vice President of Quality
Fiscal Year
(b)
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
Salary
(c)
Bonus
(d)
Stock
Awards
Options
Awards
(e)
(f)
incentive plan
All Other
compensation Compensation
(g)
(i)
Total
(j)
Non-equity
$ 615,129
555,170
539,000
$ 811,484
—
—
$ 657,298
620,494
995,450
$ 400,977
1,613,437
726,825
$
$ 477,354
280,000
—
— $ 205,424
—
—
—
—
$ 202,325
1,681,088
—
$ 354,916
326,510
317,000
$ 492,928
—
—
$ 239,168
275,775
637,450
$ 235,915
504,199
403,792
$
$
89,095
356,380
346,000
— $ 261,072
135,130
—
287,259
—
$ 257,434
487,393
363,413
$ 314,974
286,340
278,000
$ 178,840
—
—
$ 210,160
330,930
350,004
$ 206,787
436,973
363,413
$ 242,823
236,900
230,000
$ 229,228
—
—
$ 167,536
—
171,360
$ 165,324
168,066
282,654
$ 289,632
71,500
—
$ 154,321
—
—
$
52,688
152,685
—
$
51,697
—
—
$
$
$
$
$
$
$
$
45,917
802,576
808,500
— $
323,823
—
23,844
377,613
380,400
$
— $
412,158
367,622
21,160
331,156
333,600
13,595
216,470
161,000
19,458
69,427
—
$
$
$
78,382
70,102
64,286
$ 2,609,187
3,661,780
3,134,061
528,907
19,597
—
$ 1,414,010
2,304,509
—
28,917
38,377
20,645
$ 1,375,688
1,522,475
1,759,287
651,699
55,344
36,107
$ 1,259,300
1,446,404
1,400,400
24,869
35,786
23,399
36,400
29,261
28,054
16,341
2,285
—
$
$
$
956,790
1,421,185
1,348,416
854,906
650,698
873,068
584,137
295,897
—
(1) Mr. Bogda joined the Company as President in December 2014 and departed from the Company effective June 3, 2016
(2) Mr. Schreck retired from the Company effective September 11, 2015
76
77
�All Other Compensation
Grants of Plan-Based Awards in Fiscal 2016
The following summarizes the components of column (i) of the Summary Compensation Table above:
Name and Principal Position
Fiscal Year
Company
Match
Contributions
401(k) Plan
Auto
Allowance
Pay in
Lieu of
Vacation
Separation
Payments
Excess Life
Insurance
Total
Arthur P. Bedrosian
Chief Executive Officer
Michael Bogda
Former President
Martin P. Galvan
Vice President of Finance, Chief
Financial Officer and Treasurer
William Schreck
Former Chief Operating Officer
Kevin Smith
Senior Vice President of Sales and
Marketing
Robert Ehlinger
Vice President of Logistics and
Chief Information Officer
John Abt
Vice President of Quality
$
$
$
$
$
$
$
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
2016
2015
2014
$
$
$
$
$
$
$
8,000
10,715
9,438
9,292
6,000
—
10,197
8,893
9,380
2,626
9,514
10,411
8,678
9,423
9,737
8,030
8,030
8,160
5,403
—
—
$
$
$
$
$
$
$
13,500
13,500
13,500
12,981
13,555
—
10,800
10,800
10,800
2,492
10,800
10,800
13,500
13,500
13,500
10,800
10,800
10,800
10,800
2,285
—
$
$
$
$
$
$
55,598
44,841
40,425
18,078
—
—
7,508
18,288
—
31,355
34,267
13,973
2,423
12,665
—
17,312
10,173
8,747
— $
—
—
— $
—
—
$
488,352
—
—
— $
—
—
$
614,992
—
—
— $
—
—
— $
—
—
— $
—
—
$
$
$
$
$
$
$
1,284
1,046
923
204
42
—
412
396
465
234
762
923
268
198
162
258
258
347
138
—
—
78,382
70,102
64,286
528,907
19,597
—
28,917
38,377
20,645
651,699
55,344
36,107
24,869
35,786
23,399
36,400
29,261
28,054
16,341
2,285
—
Name
Grant Date
Arthur P. Bedrosian (1)
Chief Executive Officer
Michael Bogda
Former President
Martin P. Galvan
Vice President of Finance and Chief
Financial Officer
William Schreck
Former Chief Operating Officer
Kevin Smith
Senior Vice President of Sales and
Marketing
Robert Ehlinger
Vice President of Logistics and Chief
Information Officer
John Abt
Vice President of Quality
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
7/22/2015
Estimated Future Payouts Under
Non-Equity Incentive Plan
Awards
Target
($)
Maximum
($)
Threshold
($)
Estimated Future Payouts Under
Equity Incentive Plan Awards
Target
(#)
Maximum
(#)
Threshold
(#)
All Other Stock
Awards:
Number of
Shares of
Stocks or Units
(2)
(#)
All Other
Option Awards:
Number of
Securities
Underlying
Options (2)
(#)
Exercise or
Base Price
of Option
Awards (3)
($/sh)
Grant Date
Fair Value of
Stock and
Options
Awards (4)
($)
11,103
3,470
4,040
4,410
3,550
2,830
890
15,280 $
7,710 $
$
59.20 $
$
59.20 $
657,298
400,977
205,424
202,325
$
239,168
8,990 $
59.20 $
235,915
9,810 $
$
59.20 $
261,072
257,434
$
210,160
7,880 $
59.20 $
206,787
$
167,536
6,300 $
59.20 $
165,324
1,970 $
$
59.20 $
52,688
51,697
(1)
(2)
(3)
(4)
Includes 4,223 shares granted to all directors for Board service during Fiscal 2015.
Reflects stock options and restricted stock granted to NEOs during Fiscal 2016 to recognize the Company’s Fiscal 2015 performance, which vest in three equal annual increments.
The exercise price was equal to the Company’s closing stock price on the date of grant.
Stock options were valued using the Black-Scholes option pricing model. The assumptions used in fair value calculations are described in Note 17, “Share-Based Compensation,” in the Form 10-K. The grant
date fair value for other stock grants reflects the number of shares multiplied by the Company’s closing stock price on the applicable date of grant.
78
79
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.
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.
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—
—
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1
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.
3
1
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7
.
4
3
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.
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6
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$
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$
$
$
$
$
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—
—
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—
—
—
Options Exercised and Stock Vested During the Fiscal Year Ended June 30, 2016
The following table sets forth information concerning stock options exercised and stock awards that vested during Fiscal 2016 for
each of the NEOs.
Name and Principal Position
(a)
Arthur P. Bedrosian
Chief Executive Officer
Michael Bogda
Former President
Martin P. Galvan
Vice President of Finance and Chief Financial
Officer
William Schreck
Former Chief Operating Officer
Kevin Smith
Senior Vice President of Sales and Marketing
Robert Ehlinger
Vice President of Logistics and Chief
Information Officer
John Abt
Vice President of Quality
Options
Stock Awards
Number of Shares
Acquired
On Exercise
Value
Realized
on Exercise
Number of
Shares Acquired
on Vesting
Value
Realized
on Vesting
16,667
$
461,176
10,890
— $
— $
—
—
3,470
3,333
70,667
$
1,383,552
8,902
— $
—
4,000
$
$
$
$
$
574,908
85,397
162,443
509,947
194,940
65,090
$
1,159,625
— $
—
— $
—
750
$
13,268
—
—
—
—
—
—
0
0
0
,
0
3
0
0
0
,
4
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0
8
2
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81
�Employment and Separation Agreements
Potential Payments upon Termination or Change in Control
The Company has entered into employment agreements with its current NEOs. Each of the agreements provides for an annual base
salary and eligibility to receive a bonus. The salary and bonus amounts of these executives are determined by the review and approval
of the Compensation Committee in accordance with the Committee’s charter as approved by the Board of Directors. Additionally,
these executives are eligible to receive stock options and restricted stock awards. Under the agreements, these executive employees
may be terminated at any time with or without cause, or by reason of death or disability. In certain termination situations, the
Company is liable to pay these executives severance compensation as discussed in the table below. The Company previously
maintained employment agreements with Messrs. Bogda and Schreck, which expired upon their termination of employment.
Effective September 11, 2015, the Company entered into a Separation Agreement and General Release with Mr. Schreck, our former
Chief Operating Officer, upon his termination of employment. The agreement provides for a lump sum separation payment of
$614,992, equal to eighteen months of Mr. Schreck’s final base salary, pro-rated cash bonus, continued medical benefits coverage for
eighteen months, and immediate vesting of all unvested stock options and restricted stock awards. In exchange for these benefits,
Mr. Schreck agreed to release the Company from any claims and to cooperate in the resolution of any issues pertaining to filings,
investigations, or claims relating to events that occurred during his tenure with the Company. He also agreed to various restrictive
covenants during the eighteen month period following his separation from service.
Effective June 3, 2016, the Company entered into a Separation Agreement and General Release with Mr. Bogda, our former President,
upon his termination of employment. The agreement provides for a lump sum separation payment of $488,352, equal to twelve
months of Mr. Bogda’s final base salary, continued medical benefits coverage for twelve months, and immediate vesting of all
unvested stock options and restricted stock awards. In exchange for these benefits, Mr. Bogda agreed to release the Company from
any claims and to cooperate in the resolution of any issues pertaining to filings, investigations, or claims relating to events that
occurred during his tenure with the Company. He also agreed to various restrictive covenants during the twelve month period
following his resignation.
The following table assumes that the relevant triggering event occurred on June 30, 2016. The fair market values of share-based
compensation (i.e. Stock Options and Restricted Stock) were calculated using the closing price of Lannett Company, Inc. stock
($23.79) on June 30, 2016, which was the last trading day of Fiscal 2016. The “spread,” the difference between the fair market value
of Lannett Company’s stock on June 30, 2016, and the option exercise price, was used for valuing stock options.
$
$
Name
Arthur P. Bedrosian
Without Cause/With Good Reason (1) (2)
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
Michael Bogda
Without Cause/With Good Reason (1) (2) $
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
Martin P. Galvan
Without Cause/With Good Reason (1) (2)
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
William F. Schreck
Without Cause/With Good Reason (1) (2) $
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
Kevin R. Smith
Without Cause/With Good Reason (1) (2)
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
Robert Ehlinger
Without Cause/With Good Reason (1) (2) $
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
John Abt
Without Cause/With Good Reason (1) (2)
For Cause (3) (4)
Retirement / Death / Disability (3)
Change in Control (5)
$
$
Base Salary
Continuation
Annual Cash
Bonus
Acceleration and
Exercisability of
Unvested Stock
Options
Acceleration
of Unvested
Restricted
Stock
Insurance
Benefit
Continuation
Other
Benefits
Total
$
1,845,386
—
—
1,845,386
— $
—
—
—
$
532,375
—
—
532,375
— $
—
—
—
$
472,461
—
—
472,461
364,234 $
—
—
364,234
$
434,448
—
—
434,448
$
45,917
45,917
45,917
45,917
— $
—
—
—
$
23,844
23,844
23,844
23,844
— $
—
—
—
$
21,160
21,160
21,160
21,160
13,595 $
13,595
13,595
13,595
$
19,458
19,458
19,458
19,458
$
297,900
—
—
297,900
$
441,233
—
—
441,233
$
38,016
—
—
38,016
$
7,124
7,124
7,124
7,124
2,675,576
53,041
53,041
2,675,576
— $
—
—
—
— $
—
—
—
— $
—
—
—
— $
—
—
—
—
—
—
—
$
165,503
—
—
165,503
$
234,902
—
—
234,902
$
30,214
—
—
30,214
$
4,492
4,492
4,492
4,492
991,330
28,336
28,336
991,330
— $
—
—
—
$
148,950
—
—
148,950
115,853 $
—
—
115,853
— $
—
—
—
— $
—
—
—
$
250,985
—
—
250,985
67,326 $
—
—
67,326
$
56,858
—
—
56,858
— $
—
—
—
$
37,560
—
—
37,560
2,548 $
—
—
2,548
$
37,047
—
—
37,047
— $
—
—
—
$
5,088
5,088
5,088
5,088
5,392 $
5,392
5,392
5,392
$
2,344
2,344
2,344
2,344
—
—
—
—
936,205
26,248
26,248
936,205
568,948
18,987
18,987
568,948
550,156
21,802
21,802
550,156
(1) Each employment agreement ranges from 1-3 years and is automatically renewed unless notice is given by either party. Any non-renewal of the existing employment agreements by the
Company and any resignation of the Executive with Good Reason both constitute a termination without Cause. Under the existing employment agreements base salary continuation for a
period of 18-36 months, pro-rated cash bonus as if all targets and goals were achieved subject to any applicable cap on cash payments, acceleration of exercisability of unvested stock option
awards, acceleration of unvested restricted stock, and insurance benefit continuation for a period of 18 months (collectively “Severance Compensation”) will only be made if the Executive
executes and delivers to the Company, in a form prepared by the Company, a release of all claims against the Company and other appropriate parties, excluding the Company’s performance
obligation to pay Severance Compensation and the Executive’s vested rights under the Company sponsored retirement plans, 401(k) plans and stock ownership plans (“General Release”).
Severance Compensation is paid in equal monthly installments over a 12 month period to commence on the 90th day following the Termination Date provided the Executive has not revoked
the General Release prior to that date. Earned but unpaid base salary, accrued but unpaid annual bonus (if the Executive otherwise meets the eligibility requirements) and accrued but unpaid
paid time off and other miscellaneous items are to be paid in a single lump sum in cash no later than the earlier of: (1) the date required under applicable law; or (2) 60 days following the
Termination Date.
(2) Under the existing employment agreements, Good Reason is defined as giving written notice of his resignation within thirty (30) days after Executive has actual knowledge of the
occurrence, without the written consent of Executive, of one of the following events: (A) the assignment to Executive of duties materially and adversely inconsistent with Executive’s position
or a material and adverse alteration in the nature of his duties, responsibilities and/or reporting obligations, (B) a reduction in Executive’s Base Salary or a failure to pay any such amounts
when due; or (C) the relocation of Company headquarters more than 100 miles from its current location. Good Reason is also defined to include any other reason provided the Executive gives
at least thirty (30) days prior written notice to Company.
(3) Under the existing employment agreements, if the Executive is terminated For Cause; by death; by disability; resigns without Good Reason; or retires; earned but unpaid base salary,
accrued but unpaid annual bonus (if the Executive otherwise meets the eligibility requirements) and accrued but unpaid paid time off and other miscellaneous items are to be paid in a single
lump sum in cash no later than the earlier of: (1) the date required under applicable law; or (2) 60 days following the Termination Date.
(4) For Cause generally means Executive’s willful commission of an act constituting fraud, embezzlement, breach of fiduciary duty, material dishonesty with respect to the Company, gross
negligence or willful misconduct in performance of Executive duties, willful violation of any law, rule or regulation relating to the operation of the Company, abuse of illegal drugs or other
controlled substances or habitual intoxication, willful violation of published business conduct guidelines, code of ethics, conflict of interest or other similar policies, and Executive becoming
under investigation by or subject to any disciplinary charges by any regulatory agency having jurisdiction over the Company (including but not limited to the Drug Enforcement Administration
(DEA), Food and Drug Administration (FDA) or the Securities and Exchange Commission (SEC)) or if any complaint is filed against the Executive by any such regulatory agency.
(5) Under the existing employment agreements a Change in Control is defined as a “change in ownership of the Company,” “a change in effective control of the Company,” or “a change in
ownership of a substantial portion of the Company’s assets.” If the Executive is terminated by the Company without Cause or resigns with Good Reason within 24 months of a Change in
Control event, the Executive shall be entitled to earned but unpaid base salary, accrued but unpaid annual bonus (if the Executive otherwise meets the eligibility requirements) and accrued but
unpaid paid time off and other miscellaneous items. These items are to be paid in a single lump sum in cash no later than the earlier of: (1) the date required under applicable law; or (2) 60
days following the Termination Date. Additionally, the Executive shall be entitled to Severance Compensation to be paid in equal monthly installments over a 12 month period to commence
on the 90th day following the Termination Date provided the Executive has not revoked the General Release prior to that date. A written notice that the Executive’s employment term is not
extended within the 24-month period after a Change in Control shall be deemed a termination without Cause, unless the Executive and the Company execute a new employment agreement.
82
83
�COMPENSATION OF DIRECTORS
Our Board of Directors is actively involved in providing strategic direction and fiduciary oversight to the Company. During Fiscal
2016 we had a total of six Board members, which resulted in a significant workload for our directors, with our four independent
directors serving on an average of three committees each. Our Board of Directors held numerous meetings and teleconferences in
Fiscal 2016 in carrying out its responsibilities. One of the important roles the Board plays is in the area of mergers and acquisitions
(“M&A”). The Company has been involved with a significant amount of M&A activity over the past several years, including the
KUPI acquisition in Fiscal 2016 and the acquisition of Silarx Pharmaceuticals, Inc. in Fiscal 2015. The Board is actively involved in
transactional due diligence as well as on-going reviews of business development activities.
For Fiscal 2016, our non-employee directors received a cash retainer of $90,000, payable in monthly increments of $7,500, for Board
and committee service. For serving as Lead Independent Director, Mr. Drabik also received an additional retainer of $1,000 per
month, beginning in January 2016. No other cash retainers or meeting fees were provided.
Board members receive annual equity grants to recognize their service during the prior fiscal year. Grant levels may vary from year to
year based on Company performance. Given the Company’s strong performance and the significant efforts and contributions of our
directors in Fiscal 2015, in July 2015, each Board member serving in Fiscal 2015 received an award of 4,223 common shares with a
grant date value of $250,002, immediately vested at grant. These grants are shown in the table below, since they occurred in Fiscal
2016. Based on the Company’s performance and the significant efforts and contributions of our directors in Fiscal 2016, in July 2016,
each non-employee Board member received an award of 4,075 common shares with a grant date value of $124,980, immediately
vested at grant. Grant date values for this grant will be reported in the director compensation table for Fiscal 2017, since the grant
occurred after the end of Fiscal 2016. As an executive director, Mr. Bedrosian did not receive an additional grant for Fiscal 2016
board service.
Effective in July 2014, the Board of Directors approved stock ownership guidelines for non-employee directors equal to three times
their cash retainer. Non-employee directors must meet required ownership levels within five years of first becoming subject to the
guidelines. All directors other than Mr. Paonessa, who joined the board in Fiscal 2016, currently meet required ownership levels.
We maintain policies that prohibit Directors from pledging Lannett stock or engaging in activity considered hedging of our common
stock, and none of our Directors has pledged Lannett stock as collateral for a personal loan or other obligations.
The following table shows compensation information for Fiscal 2016 for non-employee members of our Board of Directors.
Name
Fees
Earned
($)
Stock
Awards (1)
($)
Options
Awards
($)
Non-Equity
Incentive Plan
Compensation
($)
Jeffrey Farber
$
90,000 $
250,002
David Drabik
96,000
250,002
Paul Taveira
90,000
250,002
James Maher
90,000
250,002
Albert Paonessa III
90,000
31,085
—
—
—
—
—
—
—
—
—
—
Change in
Pension Value
and
Nonqualified
Deferred
Compensation
($)
All Other
Compensation
($)
Total
($)
—
—
—
—
—
— $
340,002
—
—
—
—
346,002
340,002
340,002
121,085
ITEM 12.
RELATED STOCKHOLDER MATTERS
SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND
The following table sets forth, as of July 31, 2016, information regarding the security ownership of the directors and certain executive
officers of the Company and persons known to the Company to be beneficial owners of more than five (5%) percent of the Company’s
common stock. Although grants of restricted stock under the Company’s 2006, 2011 and 2014 Long Term Incentive Plans (“LTIPs”)
generally vest equally over a three year period from the grant date, the restricted shares are included below because the voting rights
with respect to such restricted stock are acquired immediately upon grant.
Name and Address of
Beneficial Owner /
Director / Executive
Officer
John M. Abt
13200 Townsend Road
Philadelphia, PA 19154
Arthur P. Bedrosian
13200 Townsend Road
Philadelphia, PA 19154
Mahendra Dedhiya
13200 Townsend Road
Philadelphia, PA 19154
David Drabik
13200 Townsend Road
Philadelphia, PA 19154
Robert Ehlinger
13200 Townsend Road
Philadelphia, PA 19154
Jeffrey Farber
13200 Townsend Road
Philadelphia, PA 19154
David Farber
13200 Townsend Road
Philadelphia, PA 19154
Jeffrey and Jennifer Farber Family Foundation
2354 Bellingham Drive
Troy, MI 48083
David and Nancy Farber Family Foundation
2354 Bellingham Drive
Troy, MI 48083
Farber Family LLC
2354 Bellingham Drive
Troy, MI 48083
Farber Investment LLC
2354 Bellingham Drive
Troy, MI 48083
Martin Galvan
13200 Townsend Road
Philadelphia, PA 19154
James M. Maher
13200 Townsend Road
Philadelphia, PA 19154
Albert Paonessa, III
13200 Townsend Road
Philadelphia, PA 19154
Kevin R. Smith
13200 Townsend Road
Philadelphia, PA 19154
Paul Taveira
13200 Townsend Road
Philadelphia, PA 19154
Office
VP of Quality
Excluding Options (*)
Including Options (**)
Shares Held
Directly
Shares Held
Indirectly
Total
Shares
Percent of
Class
Number of
Shares
Percent of
Class
6,110
––
6,110(1)
0.02%
6,766(1),(2)
0.02%
Chief Executive Officer
618,165
36,500
654,665(3)
1.77%
1,167,583(3),(4)
3.12%
Chief Scientific Affairs
2,976
Director
24,575
VP and Chief Information Officer
19,861
––
––
––
2,976(5)
0.01%
3,725(5),(6)
0.01%
24,575
0.07%
24,575
0.07%
19,861(7)
0.05%
28,627(7),(8)
0.08%
Chairman of the Board, Director
2,433,826
2,260,327
4,694,153(9)
12.72%
4,699,153(9),(10)
12.74%
1,940,870
2,432,455
4,373,325(11)
11.85%
4,373,325(11)
11.85%
1,603,498
––
1,603,498(12)
4.35%
1,603,498(12)
4.35%
1,583,499
––
1,583,499(13)
4.29%
1,583,499(13)
4.29%
528,142
––
528,142(14)
1.43%
528,142(14)
1.43%
38,000
Chief Financial Officer
38,370
Director
Director
21,798
7,105
SVP of Sales and Marketing
16,498
Director
24,798
––
––
––
––
––
––
38,000(15)
0.10%
38,000(15)
0.10%
38,370(16)
0.10%
183,366(16),(17)
0.50%
21,798
0.06%
21,798
0.06%
7,105
0.02%
7,105
0.02%
16,498(18)
0.04%
78,124(18),(19)
0.21%
24,798
0.07%
24,798
0.07%
(1) Reflects grant date award value for equity grants received in Fiscal 2016 to recognize Board service in 2015.
All directors and executive officers as a group (11
persons)
3,214,082
2,296,827
5,510,909
14.94%
6,245,620
16.60%
84
85
�Equity Compensation Plan Information
The following table summarizes the equity compensation plans as of June 30, 2016:
(1)
(2)
Includes 3,144 unvested shares received pursuant to restricted stock awards granted in March 2015, July 2015 and July 2016.
Includes 656 vested options to purchase common stock at an exercise price of $59.20 per share.
(3)
awards granted in April 2014, July 2014, July 2015 and July 2016.
Includes 36,500 shares owned by Arthur P. Bedrosian’s wife and daughter. Mr. Bedrosian disclaims beneficial ownership of these shares. Includes 14,972 unvested shares received pursuant to restricted stock
Includes 20,325 vested options to purchase common stock at an exercise price of $6.89 per share, 75,000 vested options to purchase common stock at an exercise price of $4.03 per share, 30,000 vested options to
(4)
purchase common stock at an exercise price of $2.80 per share, 75,000 vested options to purchase common stock at an exercise price of $6.94 per share, 89,500 vested options to purchase common stock at an exercise price of
$3.55 per share, 64,000 vested options to purchase common stock at an exercise price of $4.16 per share, 90,000 vested options to purchase common stock at an exercise price of $13.86 per share, 64,000 vested options to
purchase common stock at an exercise price of $34.77 per share and 5,093 vested options to purchase common stock at an exercise price of $59.20 per share.
Number of securities to
be issued upon exercise
of outstanding options,
warrants and rights
(a)
Weighted average
exercise price of
outstanding
options, warrants
and rights
(b)
Number of securities
remaining available for
future issuance under
equity compensation plans
(excluding securities
reflected in column (a))
(c)
1,730
$
16.77
2,365
—
2,365
Includes 870 unvested shares received pursuant to restricted stock awards granted in July 2016.
Includes 749 vested options to purchase common stock at an exercise price of $55.59 per share.
Includes 2,768 unvested shares received pursuant to restricted stock awards granted in July 2015 and July 2016.
(In thousands, except for weighted average exercise price)
Plan Category
Equity Compensation plans approved by security holders
(5)
(6)
(7)
(8)
Includes 6,666 vested options to purchase common stock at an exercise price of $34.77 per share and 2,100 vested options to purchase common stock at an exercise price of $59.20 per share.
Equity Compensation plans not approved by security holders
—
—
Includes 1,603,498 shares held by the Jeffrey Farber Family Foundation which is managed by Jeffrey Farber. Jeffrey Farber disclaims beneficial ownership of these shares. Includes 528,142 shares held by Farber
(9)
Family LLC (“FFLLC”) which is managed by Jeffrey and David Farber. David Farber and Jeffrey Farber each disclaim beneficial ownership of these shares. Includes 73,408 shares held by Jeffrey Farber as custodian for his
children, 17,279 shares held as joint custodian with David Farber for a relative and also includes 38,000 shares held by Farber Investment Company (“FIC”). Jeffrey Farber and David Farber each beneficially own 25% of
FIC and each disclaim beneficial ownership of all but 9,500 shares held by FIC.
Total
1,730
$
16.77
(10)
Includes 5,000 vested options to purchase common stock at an exercise price of $6.89 per share.
ITEM 13.
CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS AND DIRECTOR INDEPENDENCE
(11)
Includes 1,583,499 shares held by the David and Nancy Family Foundation. David Farber disclaims beneficial ownership of these shares. Includes 528,142 shares held by FFLLC which is managed by Jeffrey and
David Farber. David Farber and Jeffrey Farber each disclaim beneficial ownership of these shares. Includes 265,535 shares held by David Farber as custodian for his children and 17,279 shares held as joint custodian with
Jeffrey Farber for a relative. Also includes 38,000 shares held by FIC. Jeffrey Farber and David Farber each beneficially own 25% of FIC and each disclaim beneficial ownership of all but 9,500 shares held by FIC.
Review and Approval of Transactions with Related Persons
The responsibility for the review of transactions with “related persons” (as defined below) has been assigned to the Audit Committee
of the Board of Directors, which is comprised of three independent directors. “Related persons” are defined as directors and executive
officers or their immediate family members or stockholders owning more than five percent of the Company’s common stock. The
Audit Committee annually reviews related party transactions with any related person in which the amount exceeds $120,000.
The Company had total net sales of $3.1 million, $1.9 million and $2.3 million during the fiscal years ended June 30, 2016, 2015 and
2014, respectively, to a generic distributor, Auburn Pharmaceutical Company (“Auburn”). Jeffrey Farber, Chairman of the Board, is
the owner of Auburn. Accounts receivable includes amounts due from Auburn of $682 thousand and $733 thousand at June 30, 2016
and 2015, respectively.
As part of its review, the Audit Committee noted that the amount of total net sales to Auburn approximated 0.6%, 0.5% and 1.5% of
total net sales during the fiscal years ended June 30, 2016, 2015 and 2014, respectively.
The Audit Committee reviewed an analysis of sales prices charged to Auburn, which compared the average sales prices by product for
Auburn sales to the average sales prices by product to other Lannett customers during the same period. As a result of this analysis, the
Audit Committee ratified the net sales made to Auburn during the fiscal years ended June 30, 2016 and noted that the aggregate
impact of the difference in sales prices charged to Auburn compared to other customers was not significant.
(12)
Jeffrey and Jennifer Farber Family Foundation is managed by Jeffrey Farber.
(13)
David and Nancy Farber Family Foundation is managed by David and Nancy Farber.
(14)
Farber Family LLC is managed by Jeffrey Farber and David Farber.
(15)
Farber Investment LLC is beneficially owned 25% each by Jeffrey and David Farber and 50% by Larry Farber.
(16)
Includes 7,637 unvested shares received pursuant to restricted stock awards granted in April 2014, July 2014, July 2015 and July 2016.
(17)
Includes 40,000 vested options to purchase common stock at an exercise price of $4.73 per share, 32,000 vested options to purchase common stock at an exercise price of $4.16 per share, 50,000 vested options to
purchase common stock at an exercise price of $13.86 per share, 20,000 vested options to purchase common stock at an exercise price of $34.77 per share and 2,996 vested options to purchase common stock at an exercise
price of $59.20 per share.
(18)
Includes 7,795 unvested shares received pursuant to restricted stock awards granted in April 2014, July 2014, July 2015 and July 2016.
(19)
purchase common stock at an exercise price of $34.77 per share and 2,626 vested options to purchase common stock at an exercise price of $59.20 per share.
Includes 11,667 vested options to purchase common stock at an exercise price of $4.16 per share, 30,000 vested options to purchase common stock at an exercise price of $13.86 per share, 17,333 vested options to
* Percent of class calculation is based on 36,892,377 outstanding shares of common stock at July 31, 2016.
** Assumes that all options exercisable within sixty days have been exercised.
The following table sets forth, as of July 31, 2016, information regarding the names and addresses of the shareholders known to the
Company to be beneficial owners of more than five (5%) percent of the Company’s common stock.
Name and Address of Beneficial Owner
BlackRock, Inc.
55 East 52nd Street
New York, NY 10055
The Vanguard Group
100 Vanguard Blvd
Malvern, PA 19355
Number of
Shares
Percent of
Class
2,876,155(1)
7.80%
2,439,551(2)
6.61%
(1) Based on Schedule 13G/A filed by BlackRock, Inc. with the SEC on January 26, 2016. BlackRock, Inc. has sole voting power
over 2,811,893 shares, shared voting power over 0 shares, sole dispositive power over 2,876,155 shares and shared dispositive power
over 0 shares.
(2) Based on Schedule 13G/A filed by The Vanguard Group with the SEC on February 10, 2016. The Vanguard Group has sole
voting power over 59,111 shares, shared voting power over 1,800 shares, sole dispositive power over 2,380,540 shares and shared
dispositive power over 59,011 shares.
86
87
�ITEM 14.
PRINCIPAL ACCOUNTANT FEES AND SERVICES
Grant Thornton LLP served as the independent auditors of the Company during Fiscal 2016, 2015 and 2014. No relationship exists,
other than the usual relationship between independent public accountant and client. The following table identifies the fees incurred for
services rendered by Grant Thornton LLP in Fiscal 2016, 2015 and 2014.
(In thousands)
Fiscal 2016:
Fiscal 2015:
Fiscal 2014:
Audit Fees
Audit-Related
Tax Fees (1)
All Other Fees (2)
Total Fees
$
$
$
1,482
499
444
$
$
$
— $
—
$
— $
154
104
69
$
$
$
— $
10
$
— $
1,636
613
513
(1) Tax fees include fees paid for preparation of annual federal, state and local income tax returns, quarterly estimated income tax
payments and various tax planning services.
(2) Other fees include fees paid for review of various correspondences, miscellaneous studies, etc.
The non-audit services provided to the Company by Grant Thornton LLP were pre-approved by the Company’s Audit Committee.
Prior to engaging its auditor to perform non-audit services, the Company’s Audit Committee reviews the particular service to be
provided and the fee to be paid by the Company for such service and assesses the impact of the service on the auditor’s independence.
PART IV
ITEM 15.
EXHIBITS, FINANCIAL STATEMENT SCHEDULES
1.
Consolidated Financial Statements:
See accompanying Index to Consolidated Financial Statements.
2.
Consolidated Financial Statement Schedules:
Lannett Company, Inc.
Schedule II - Valuation and Qualifying Accounts
For the years ended June 30:
Description
(In thousands)
Allowance for Doubtful Accounts
2016
2015
2014
Inventory Valuation
2016
2015
2014
Deferred Tax Asset Valuation Allowance
2016
2015
2014
Balance at
Beginning of
Fiscal Year
Charged to
(Reduction of)
Expense
Deductions
Balance at
End of Fiscal
Year
$
$
$
$
$
$
374
115
41
4,957
2,384
2,002
2,326
2,289
2,140
$
$
$
236
259
74
9,354
6,700
2,918
1,601
37
149
$
$
$
—
—
—
7,387
4,127
2,536
—
—
—
610
374
115
6,924
4,957
2,384
3,927
2,326
2,289
88
89
�3.
Exhibits:
Those exhibits marked with a (*) refer to management contracts or compensatory plans or arrangements.
Exhibit
Number
2.1
Description
Method of Filing
Stock Purchase Agreement by and among Lannett
Company, Inc., Rohit Desai, the RD Nevada Trust, Silarx
Pharmaceuticals, Inc. and Stoneleigh Realty, LLC, dated
as of May 15, 2015
Incorporated by reference to Exhibit 2.1 on Form 8-K
dated May 18, 2015
2.2
Stock Purchase Agreement among UCB S.A., UCB
Manufacturing, Inc. and Lannett Company, Inc. dated as
of September 2, 2015
Amendment No. 2 to Stock Purchase Agreement
Certificate of Incorporation
By-Laws, as amended
Amendment No. 1 to Amended and Restated By-Laws
Amendment No. 2 to Amended and Restated By-Laws
Updated and Amended Certificate of Incorporation
Updated and Amended By-Laws
Amended and Restated Bylaws of Lannett Company Inc.,
as amended through January 21, 2015.
Amended and Restated Bylaws of Lannett Company Inc.,
as amended through July 6, 2015.
Specimen Certificate for Common Stock
2.3
3.1
3.2
3.3
3.4
3.5
3.6
3.7
3.8
4
4.1
Lannett Company, Inc. Indenture. Wilmington Trust,
4.2
4.3
10.1
10.2
10.3
10.4
National Association, Providing for the Issuance of Notes
in Series
First Supplemental Indenture dated as of November 25,
2015
Supplemental Indenture in Respect of Subsidiary
Guarantee
Line of Credit Note dated March 11, 1999 between the
Company and First Union National Bank
Philadelphia Authority for Industrial Development
Taxable Variable Rate Demand/Fixed Rate Revenue
Bonds, Series of 1999
Philadelphia Authority for Industrial Development
Tax-Exempt Variable Rate Demand/Fixed Revenue
Bonds (Lannett Company, Inc. Project) Series of 1999
Letter of Credit and Agreements supporting bond issues
between the Company and First Union National Bank
Incorporated by reference to Exhibit 2.2 on Form 8-K
dated September 4, 2015
Incorporated by reference to Exhibit 2.3 on Form 8-K
dated December 2, 2015
Incorporated by reference to the Proxy Statement filed
with respect to the Annual Meeting of Shareholders held
on December 6, 1991 (the “1991 Proxy Statement”).
Incorporated by reference to the 1991 Proxy Statement.
Incorporated by reference to Exhibit 3.3 on Form 8-K
dated January 16, 2014
Incorporated by reference to Exhibit 3.4 on Form 8-K
dated July 17, 2014
Incorporated by reference to Exhibit 3.5 to the Annual
Report on 2014 Form 10-K
Incorporated by reference to Exhibit 3.6 to the Annual
Report on 2014 Form 10-K
Incorporated by reference to Exhibit 3.7 on Form 8-K
dated April 3, 2015
Incorporated by reference to Exhibit 3.8 on Form 8-K
dated July 9, 2015
Incorporated by reference to Exhibit 4(a) to Form 8 dated
April 23, 1993 (Amendment No. 3 to Form 10-KSB for
Fiscal 1992) (“Form 8”)
Incorporated by reference to Exhibit 4.1 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 4.2 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 4.3 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10(ad) to the Annual
Report on 1999 Form 10-KSB
Incorporated by reference to Exhibit 10(ae) to the Annual
Report on 1999 Form 10-KSB
Incorporated by reference to Exhibit 10(af) to the Annual
Report on 1999 Form 10-KSB
Incorporated by reference to Exhibit 10(ag) to the Annual
Report on 1999 Form 10-KSB
Exhibit
Number
10.5*
2003 Stock Option Plan
Description
Method of Filing
10.6*
Employment Agreement with Kevin Smith
10.7*
Employment Agreement with Arthur Bedrosian
10.9
Agreement between Lannett Company, Inc and Siegfried
(USA), Inc.
10.10
Agreement between Lannett Company, Inc and Jerome
Stevens, Pharmaceutical, Inc.
10.11*
Terms of Employment Agreement with Stephen J.
Kovary
10.12
Agreement of Sale Between Anvil Construction
Company, Inc. and Lannett Company, Inc.
10.13*
2006 Long Term Incentive Plan
10.15*
2011 Long Term Incentive Plan
10.16*
Terms of Employment Agreement with Martin P. Galvan
10.17
Amended and Restated Loan Agreement dated April 29,
2011 between the Company and Wells Fargo Bank, N. A.
10.18
Loan Agreement dated May 26, 2011 between the
Company, the Pennsylvania Industrial Development
Authority (“PIDA”) and PIDC Financing Corporation
Second Amended and Restated Employment Agreement
10.19*
of Arthur P. Bedrosian
10.20*
Amended and Restated Employment Agreement of
Martin P. Galvan
10.21*
Amended and Restated Employment Agreement of
William F. Schreck
10.22*
Amended and Restated Employment Agreement of Kevin
Smith
10.23*
Amended and Restated Employment Agreement of
Ernest J. Sabo
10.24*
Amended and Restated Employment Agreement of
Robert Ehlinger
10.25
Amendment to Agreement dated March 23, 2004 by and
between Lannett Company, Inc. and Jerome Stevens
Pharmaceuticals, Inc.
10.26
Credit Agreement dated as of December 18, 2013 among
Lannett Company Inc., as the Borrower, Certain
Financial Institutions as the Lenders and Citibank, N.A.,
as Administrative Agent
10.27
Guaranty and Security Agreement dated as of
December 18, 2013, among Lannett Company, Inc., the
Subsidiaries of Lannett Company, Inc. identified therein
and Citibank, N.A., as Administrative Agent
Incorporated by reference to the Proxy Statement for
Fiscal Year Ending June 30, 2002
Incorporated by reference to Exhibit 10.6 to the Annual
Report on 2003 Form 10-KSB
Incorporated by reference to Exhibit 10 to the Quarterly
Report on Form 10-Q dated May 12, 2004.
Incorporated by reference to Exhibit 10.9 to the Annual
Report on 2003 Form 10-KSB
Incorporated by reference to Exhibit 2.1 to Form 8-K
dated April 20, 2004
Incorporated by reference to Exhibit 10.11 to the Annual
Report on 2009 Form 10-K
Incorporated by reference to Exhibit 10.12 to the Annual
Report on 2009 Form 10-K
Incorporated by reference to the Proxy Statement dated
January 5, 2007
Incorporated by reference to the Proxy Statement dated
January 19, 2011
Incorporated by reference to Exhibit 10.1 on Form 8-K
dated August 8, 2011
Incorporated by reference to Exhibit 10.17 to the Annual
Report on 2011 Form 10-K
Incorporated by reference to Exhibit 10.18 to the Annual
Report on 2011 Form 10-K
Incorporated by reference to Exhibit 10.19 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.20 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.21 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.22 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.23 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.24 on Form 8-K
dated January 3, 2013
Incorporated by reference to Exhibit 10.25 on Form 8-K
dated August 19, 2013
Incorporated by reference to Exhibit 10.26 on Form 8-K
dated December 19, 2013
Incorporated by reference to Exhibit 10.27 on Form 8-K
dated December 19, 2013
90
91
�Exhibit
Number
10.28*
Employment Agreement of Michael Bogda dated
December 1, 2014
Description
10.29
Lender Joinder and First Amendment to Credit
Agreement dated as of April 21, 2015 among Lannett
Company, Inc., as the Borrower, Certain Financial
Institutions as the Lenders and Citibank, N.A., as
Administrative Agent
10.30*
Employment Agreement of John Abt
10.31*
Employment Agreement of Rohit Desai
10.32*
Employment Agreement of Dr. Mahendra Dedhiya
10.33
Project Orion Commitment Letter
10.34*
Separation Agreement and General Release between
William F. Schreck and Lannett Company, Inc., dated
September 11, 2015
10.35
Project Orion Amended and Restated Commitment Letter
10.36
Credit and Guaranty Agreement dated as of
November 25, 2015
10.37
Credit Agreement Joinder
10.38
Pledge and Security Agreement dated as of
November 25, 2015
10.39
Supplement No. 1 to the Pledge and Security Agreement
10.40
Warrant to Purchase Common Stock
10.41
Registration Rights Agreement
10.42*
Separation Agreement and General Release between
Michael Bogda and Lannett Company, Inc., dated
April 11, 2016
10.43
Amendment No. 1 to Credit and Guaranty Agreement
dated June 17, 2016
10.44
Amendment No. 2 to Credit and Guaranty Agreement
Method of Filing
Incorporated by reference to Exhibit 10.28 on Form 8-K
dated December 5, 2014
Incorporated by reference to Exhibit 10.29 on Form 8-K
dated April 24, 2015
Exhibit
Number
32
Description
Method of Filing
Certifications of Chief Executive Officer and Chief
Financial Officer Pursuant to Section 906 of the
Sarbanes-Oxley Act of 2002
Filed Herewith
101.INS
XBRL Instance Document
101.SCH
XBRL Extension Schema Document
101.CAL
XBRL Calculation Linkbase Document
101.DEF
XBRL Definition Linkbase Document
101.LAB
XBRL Label Linkbase Document
101.PRE
XBRL Presentation Linkbase Document
Incorporated by reference to Exhibit 10.30 on Form 10-Q
dated May 8, 2015
Incorporated by reference to Exhibit 10.31 to the Annual
Report on 2015 Form 10-K
Incorporated by reference to Exhibit 10.31 to the Annual
Report on 2015 Form 10-K
Incorporated by reference to Exhibit 10.33 on Form 8-K
dated September 4, 2015
Incorporated by reference to Exhibit 10.34 on Form 8-K
dated September 15, 2015
Incorporated by reference to Exhibit 10.35 on Form 8-K
dated September 25, 2015
Incorporated by reference to Exhibit 10.36 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.37 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.38 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.39 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.40 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.41 on Form 8-K
dated December 2, 2015
Incorporated by reference to Exhibit 10.42 on Form 8-K
dated April 12, 2016
Incorporated by reference to Exhibit 10.43 on Form 8-K
dated June 20, 2016
Incorporated by reference to Exhibit 10.44 on Form 8-K
dated June 20, 2016
dated June 17, 2016
Subsidiaries of the Company
Consent of Grant Thornton, LLP
Certification of Chief Executive Officer Pursuant to
Section 302 of the Sarbanes-Oxley Act of 2002
Filed Herewith
Filed Herewith
Filed Herewith
21
23.1
31.1
31.2
Certification of Chief Financial Officer Pursuant to
Section 302 of the Sarbanes-Oxley Act of 2002
Filed Herewith
92
93
�Index to Consolidated Financial Statements and
Supplementary Financial Information
Management’s Report on Internal Control Over Financial Reporting
Reports of Independent Registered Public Accounting Firm
Consolidated Balance Sheets as of June 30, 2016 and 2015
Consolidated Statements of Operations for the Fiscal Years Ended June 30, 2016, 2015 and 2014
Consolidated Statements of Comprehensive Income for the Fiscal Years Ended June 30, 2016, 2015 and 2014
Consolidated Statements of Changes in Stockholders’ Equity for the Fiscal Years Ended June 30, 2016, 2015 and 2014
Consolidated Statements of Cash Flows for the Fiscal Years Ended June 30, 2016, 2015 and 2014
Notes to Consolidated Financial Statements for the three Fiscal Years ended June 30, 2016
Supplementary Financial Information
96
97
99
100
101
102
103
104
Pursuant to the requirements of Section 13 or 15(d) of the Securities Exchange Act of 1934, the registrant has duly caused this report
to be signed on its behalf by the undersigned, thereunto duly authorized.
SIGNATURES
Date: August 29, 2016
LANNETT COMPANY, INC.
By:
/s/ Arthur P. Bedrosian
Arthur P. Bedrosian,
Chief Executive Officer
Pursuant to the requirements of the Securities Exchange Act of 1934, this report has been signed by the following persons on behalf of
the registrant and in the capacities and on the dates indicated.
Date: August 29, 2016
By: /s/ Martin P. Galvan
Martin P. Galvan
Vice President of Finance, Chief Financial Officer and
Treasurer
Date: August 29, 2016
By: /s/ G. Michael Landis
G. Michael Landis
Director of Finance and Principal Accounting Officer
Date: August 29, 2016
By: /s/ Jeffrey Farber
Date: August 29, 2016
Jeffrey Farber,
Director, Chairman of the Board of Directors
By: /s/ Arthur P. Bedrosian
Arthur P. Bedrosian,
Director, Chief Executive Officer
Date: August 29, 2016
By: /s/ David Drabik
David Drabik,
Director, Chairman of Governance and Nominating
Committee, Lead Independent Director
Date: August 29, 2016
By: /s/ Paul Taveira
Date: August 29, 2016
Date: August 29, 2016
Paul Taveira,
Director, Chairman of Compensation Committee
By: /s/ James M. Maher
James M. Maher,
Director, Chairman of Audit Committee
By: /s/ Albert Paonessa III
Albert Paonessa III,
Director
94
95
�Management’s Report on Internal Control over Financial Reporting
Report of Independent Registered Public Accounting Firm
Management of Lannett Company Inc. (the “Company”) is responsible for establishing and maintaining adequate internal control over
financial reporting. Internal control over financial reporting is defined in Rule 13a-15(f) and 15d-15(f) under the Securities Exchange
Act of 1934, as amended. The Company’s internal control framework was designed to provide the Company’s management and
Board of Directors, reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for
external purposes in accordance with accounting principles generally accepted in the United States of America.
Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Projections of
any evaluation of effectiveness to future periods are subject to the risk that controls may become inadequate because of changes in
conditions, or that the degree of compliance with policies or procedures may deteriorate.
Management used the criteria set forth by the Committee of Sponsoring Organizations of the Treadway Commission (“COSO”) in
Internal Control — Integrated Framework (2013) in conducting its assessment as of June 30, 2016. As a result of this assessment,
management has concluded that, as of June 30, 2016, the Company’s internal control over financial reporting is effective.
Our evaluation of the effectiveness of internal control over financial reporting as of June 30, 2016 did not include an evaluation of the
internal control over financial reporting of Kremers Urban Pharmaceuticals. We excluded Kremers Urban Pharmaceuticals from our
assessment of internal control over financial reporting as of June 30, 2016 because it was acquired in a business combination
consummated on November 25, 2015 and we are in the process of integrating these operations into our internal control over financial
reporting. Kremers Urban Pharmaceuticals total assets acquired represent approximately 53% of consolidated total assets as of
June 30, 2016; total revenues acquired represent approximately 31% of consolidated total revenues for the year ended June 30, 2016.
The Company’s independent registered public accounting firm, Grant Thornton, LLP, has issued its report on the effectiveness of the
Company’s internal control over financial reporting as of June 30, 2016. Grant Thornton, LLP’s opinion on the Company’s internal
control over financial reporting appears on page 98 of this Form 10-K.
To the Board of Directors and Stockholders of
Lannett Company, Inc.
We have audited the accompanying consolidated balance sheets of Lannett Company, Inc. (a Delaware corporation) and Subsidiaries
(collectively, the Company) as of June 30, 2016 and 2015 and the related consolidated statements of operations, comprehensive
income, changes in stockholders’ equity and cash flows for each of the three fiscal years in the period ended June 30, 2016. Our
audits of the basic consolidated financial statements included the consolidated financial statement schedules listed in the index
appearing under Item 15. These financial statements and financial statement schedules are the responsibility of the Company’s
management. Our responsibility is to express an opinion on these financial statements and financial statement schedules based on our
audits.
We conducted our audits in accordance with the standards of the Public Company Accounting Oversight Board (United
States). Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the financial
statements are free of material misstatement. An audit includes examining, on a test basis, evidence supporting the amounts and
disclosures in the financial statements. An audit also includes assessing the accounting principles used and significant estimates made
by management, as well as evaluating the overall financial statement presentation. We believe that our audits provide a reasonable
basis for our opinion.
In our opinion, the consolidated financial statements referred to above present fairly, in all material respects, the financial position of
Lannett Company, Inc. and Subsidiaries as of June 30, 2016 and 2015 and the results of their operations and their cash flows for each
of the three fiscal years in the period ended June 30, 2016 in conformity with accounting principles generally accepted in the United
States of America. Also in our opinion, the related consolidated financial statement schedules, when considered in relation to the
basic consolidated financial statements taken as a whole, presents fairly, in all material respects, the information set forth therein.
We have also audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), the
Company’s internal control over financial reporting as of June 30, 2016, based on criteria established in 2013 Internal Control —
Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (COSO) and our report
dated August 29, 2016 expressed an unqualified opinion.
/s/ GRANT THORNTON LLP
Philadelphia, Pennsylvania
August 29, 2016
96
97
�Report of Independent Registered Public Accounting Firm
To the Board of Directors and Stockholders of
Lannett Company, Inc.
We have audited the internal control over financial reporting of Lannett Company, Inc. (a Delaware Corporation) and Subsidiaries
(the “Company”) as of June 30, 2016, based on criteria established in 2013 Internal Control — Integrated Framework issued by the
Committee of Sponsoring Organizations of the Treadway Commission (COSO). The Company’s management is responsible for
maintaining effective internal control over financial reporting and for its assessment of the effectiveness of internal control over
financial reporting, included in the accompanying Management’s Report on Internal Control over Financial Reporting. Our
responsibility is to express an opinion on the Company’s internal control over financial reporting based on our audit. Our audit of and
opinion on, the Company’s internal control over financial reporting does not include the internal control over financial reporting of
Kremers Urban Pharmaceuticals Inc., a wholly-owned subsidiary, whose financial statements reflect total revenues and assets
constituting 31% and 53%, respectively, of the related consolidated financial statement amounts as of and for the year ended June 30,
2016. As indicated in Management’s report, management’s assertion on the effectiveness of the Company’s internal control over
financial reporting excluded internal control over financial reporting of Kremers Urban Pharmaceuticals Inc.
We conducted our audit in accordance with the standards of the Public Company Accounting Oversight Board (United States). Those
standards require that we plan and perform the audit to obtain reasonable assurance about whether effective internal control over
financial reporting was maintained in all material respects. Our audit included obtaining an understanding of internal control over
financial reporting, assessing the risk that a material weakness exists, testing and evaluating the design and operating effectiveness of
internal control based on the assessed risk and performing such other procedures as we considered necessary in the
circumstances. We believe that our audit provides a reasonable basis for our opinion.
A company’s internal control over financial reporting is a process designed to provide reasonable assurance regarding the reliability of
financial reporting and the preparation of financial statements for external purposes in accordance with generally accepted accounting
principles. A company’s internal control over financial reporting includes those policies and procedures that (1) pertain to the
maintenance of records that, in reasonable detail, accurately and fairly reflect the transactions and dispositions of the assets of the
company; (2) provide reasonable assurance that transactions are recorded as necessary to permit preparation of financial statements in
accordance with generally accepted accounting principles and that receipts and expenditures of the company are being made only in
accordance with authorizations of management and directors of the company; and (3) provide reasonable assurance regarding
prevention or timely detection of unauthorized acquisition, use, or disposition of the company’s assets that could have a material effect
on the financial statements.
Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Also, projections
of any evaluation of effectiveness to future periods are subject to the risk that controls may become inadequate because of changes in
conditions, or that the degree of compliance with the policies or procedures may deteriorate.
In our opinion, Lannett Company, Inc. and Subsidiaries maintained, in all material respects, effective internal control over financial
reporting as of June 30, 2016, based on criteria established in 2013 Internal Control — Integrated Framework issued by COSO.
We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), the
consolidated financial statements of the Company as of and for the year ended June 30, 2016 and our report dated August 29, 2016
expressed an unqualified opinion.
/s/ GRANT THORNTON LLP
Philadelphia, Pennsylvania
August 29, 2016
LANNETT COMPANY, INC.
CONSOLIDATED BALANCE SHEETS
(In thousands, except share and per share data)
June 30, 2016
June 30, 2015
$
$
$
ASSETS
Current assets:
Cash and cash equivalents
Investment securities
Accounts receivable, net
Inventories
Deferred tax assets
Other current assets
Total current assets
Property, plant and equipment, net
Intangible assets, net
Goodwill
Deferred tax assets
Other assets
TOTAL ASSETS
LIABILITIES
Current liabilities:
Accounts payable
Accrued expenses
Accrued payroll and payroll-related expenses
Rebates payable
Royalties payable
Restructuring liability
Settlement liability
Income taxes payable
Acquisition-related contingent consideration
Short-term borrowings and current portion of long-term debt
Total current liabilities
Long-term debt, net
Settlement liability
Other liabilities
TOTAL LIABILITIES
Commitments and contingencies (Note 12 and 13)
STOCKHOLDERS’ EQUITY
Common stock ($0.001 par value, 100,000,000 shares authorized; 37,150,165 and
36,783,381 shares issued; 36,604,202 and 36,264,585 shares outstanding at
June 30, 2016 and 2015, respectively)
Additional paid-in capital
Retained earnings
Accumulated other comprehensive loss
Treasury stock (545,963 and 518,796 shares at June 30, 2016 and 2015, respectively)
Total Lannett Company, Inc. stockholders’ equity
Noncontrolling Interest
Total stockholders’ equity
TOTAL LIABILITIES AND STOCKHOLDERS’ EQUITY
$
$
$
$
224,769
14,094
211,722
114,904
40,892
6,434
612,815
216,638
575,503
333,611
11,556
13,895
1,764,018
34,720
9,247
10,572
21,894
5,127
4,130
7,000
743
35,000
178,236
306,669
883,612
12,526
6,754
1,209,561
37
283,301
278,355
(295)
(7,349)
554,049
408
554,457
1,764,018
$
200,340
13,467
91,103
46,191
16,270
3,175
370,546
94,556
29,090
141
12,495
1,938
508,766
19,195
4,928
10,397
7,553
—
—
—
1,340
—
135
43,548
874
—
578
45,000
37
236,178
233,573
(295)
(6,080)
463,413
353
463,766
508,766
The accompanying notes are an integral part of the consolidated financial statements.
98
99
�LANNETT COMPANY, INC.
CONSOLIDATED STATEMENTS OF OPERATIONS
(In thousands, except share and per share data)
LANNETT COMPANY, INC.
CONSOLIDATED STATEMENTS OF COMPREHENSIVE INCOME
(In thousands)
Net income
Other comprehensive income (loss), before taxes:
Foreign currency translation gain (loss)
Total other comprehensive income (loss), net of taxes
Comprehensive income
Less: Total comprehensive income attributable to
noncontrolling interest
Comprehensive income attributable to Lannett Company, Inc.
$
2016
Fiscal Year Ended June 30,
2015
2014
$
44,857
$
149,992
$
57,163
—
—
44,857
(241)
(241)
149,751
75
44,782
$
73
149,678
$
(7)
(7)
57,156
62
57,094
The accompanying notes are an integral part of the consolidated financial statements.
Net sales
Settlement agreement
Total net sales
Cost of sales
Amortization of intangibles
JSP contract renewal cost
Gross profit
Operating expenses:
Research and development expenses
Selling, general and administrative expenses
Acquisition and integration-related expenses
Restructuring expenses
Intangible assets impairment charge
Total operating expenses
Operating income
Other income (loss):
Loss on extinguishment of debt
Investment income
Interest expense
Other
Total other income (loss)
Income before income taxes
Income tax expense
Net income
Less: Net income attributable to noncontrolling interest
Net income attributable to Lannett Company, Inc.
Earnings per common share attributable to Lannett Company, Inc.:
Basic
Diluted
2016
Fiscal Year Ended June 30,
2015
2014
$
$
$
$
566,091
(23,598)
542,493
237,371
18,629
—
286,493
45,054
68,325
27,190
7,166
8,000
155,735
130,758
(3,009)
368
(65,937)
(1)
(68,579)
62,179
17,322
44,857
75
44,782
1.23
1.20
$
$
$
$
406,837
—
406,837
100,344
137
—
306,356
30,342
45,206
4,321
—
—
79,869
226,487
—
1,130
(207)
12
935
227,422
77,430
149,992
73
149,919
4.18
4.04
$
$
$
$
273,771
—
273,771
97,839
1,424
20,100
154,408
27,713
38,606
—
—
—
66,319
88,089
—
2,202
(130)
(141)
1,931
90,020
32,857
57,163
62
57,101
1.70
1.62
Weighted average common shares outstanding:
Basic
Diluted
36,442,782
37,389,445
35,827,167
37,127,117
33,663,589
35,193,376
The accompanying notes are an integral part of the consolidated financial statements.
100
101
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T
LANNETT COMPANY, INC.
CONSOLIDATED STATEMENTS OF CASH FLOWS
(In thousands)
Fiscal Year Ended June 30,
2015
2016
2014
OPERATING ACTIVITIES:
Net income
Adjustments to reconcile net income to net cash provided by operating activities:
$
44,857 $ 149,992 $
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Depreciation and amortization
Deferred income benefit
Share-based compensation
Excess tax benefits on share-based compensation awards
Intangible assets impairment charge
Loss (gain) on sale of assets
Loss (gain) on investment securities
Loss on extinguishment of debt
Amortization of debt discount and other debt issuance costs
JSP contract renewal cost
Other noncash expenses
Changes in assets and liabilities which provided (used) cash; net of acquisitions:
Accounts receivable, net
Inventories
Income taxes payable
Other assets
Rebates payable
Royalties payable
Restructuring liability
Settlement liability
Accounts payable
Accrued expenses
Accrued payroll and payroll-related expenses
Net cash provided by operating activities
INVESTING ACTIVITIES:
Purchases of property, plant and equipment
Proceeds from sale of property, plant and equipment
Purchases of intangible assets
Acquisitions, net of cash acquired
Proceeds from sale of investment securities
Purchase of investment securities
Net cash used in investing activities
FINANCING ACTIVITIES:
Proceeds from issuance of long-term debt
Short-term borrowings under revolving credit facility
Repayments of long-term debt
Proceeds from issuance of stock
Payment of debt issuance costs
Excess tax benefits on share-based compensation awards
Proceeds from stock offering
Purchase of treasury stock
Distributions to noncontrolling shareholders
Net cash provided by financing activities
Effect on cash and cash equivalents of changes in foreign exchange rates
NET INCREASE IN CASH AND CASH EQUIVALENTS
CASH AND CASH EQUIVALENTS, BEGINNING OF PERIOD
CASH AND CASH EQUIVALENTS, END OF PERIOD
SUPPLEMENTAL DISCLOSURE OF CASH FLOW INFORMATION:
Interest paid
Income taxes paid
Issuance of unsecured 12.0% Senior Notes to finance KUPI acquisition
Issuance of a warrant to finance KUPI acquisition
Acquisition-related contingent consideration
33,433
(19,497)
11,562
(1,507)
8,000
92
11
3,009
12,484
—
523
15,149
15,296
1,717
7,719
4,525
1,524
4,130
18,598
(3,723)
(1,760)
(20,865)
135,277
(24,267)
16
—
(934,178)
39,895
(40,533)
(959,067)
5,583
(3,266)
6,397
(8,051)
—
(33)
(705)
—
110
—
—
(25,382)
1,358
5,127
(1,673)
2,995
—
—
—
(2,498)
1,027
(2,463)
128,518
(31,676)
94
(300)
(41,862)
75,770
(47,839)
(45,813)
1,048,610
125,000
(295,033)
4,134
(34,710)
1,507
—
(1,269)
(20)
848,219
—
24,429
200,340
224,769 $ 200,340 $
—
—
(129)
4,938
(435)
8,051
—
(121)
(15)
12,289
(241)
94,753
105,587
52,916 $
35,141 $
200,000 $
29,920 $
35,000 $
206 $
75,569 $
— $
— $
— $
$
$
$
$
$
$
5,984
(12,886)
9,026
(7,017)
—
142
(1,907)
—
111
20,100
—
(34,912)
(12,313)
11,432
154
3,491
—
—
—
(1,686)
2,271
5,950
45,103
(26,082)
48
—
—
23,374
(53,699)
(56,359)
—
—
(5,376)
5,369
(402)
7,017
71,478
(3,925)
—
74,161
(7)
62,898
42,689
105,587
130
34,311
—
—
—
The accompanying notes are an integral part of the consolidated financial statements.
102
103
�LANNETT COMPANY, INC.
NOTES TO CONSOLIDATED FINANCIAL STATEMENTS
Note 1. The Business And Nature of Operations
Lannett Company, Inc. (a Delaware corporation) and its subsidiaries (collectively, the “Company” or “Lannett”) develop,
manufacture, package, market and distribute solid oral and extended release (tablets and capsules), topical, nasal and oral solution
finished dosage forms of drugs, that address a wide range of therapeutic areas. Certain of these products are manufactured by others
and distributed by the Company, most notably under the Jerome Stevens Distribution Agreement. The Company also manufactures
active pharmaceutical ingredients through its Cody Laboratories, Inc. (“Cody Labs”) subsidiary, providing a vertical integration
benefit.
On November 25, 2015, the Company completed the acquisition of Kremers Urban Pharmaceuticals, Inc. (“KUPI”), the former U.S.
specialty generic pharmaceuticals subsidiary of global biopharmaceuticals company UCB S.A. KUPI is a specialty pharmaceuticals
manufacturer focused on the development of products that are difficult to formulate or utilize specialized delivery
technologies. Strategic benefits of the acquisition include expanded manufacturing capacity, a diversified product portfolio and
pipeline and complementary research and development expertise.
The Company operates pharmaceutical manufacturing plants in Philadelphia, Pennsylvania; Cody, Wyoming; Carmel, New York and
Seymour, Indiana. The Company’s customers include generic pharmaceutical distributors, drug wholesalers, chain drug stores,
private label distributors, mail-order pharmacies, other pharmaceutical manufacturers, managed care organizations, hospital buying
groups, governmental entities and health maintenance organizations.
Note 2. Summary of Significant Accounting Policies
Basis of Presentation
The Consolidated Financial Statements have been prepared in conformity with United States generally accepted accounting principles
(U.S.GAAP).
Principles of consolidation
The Consolidated Financial Statements include the accounts of Lannett Company, Inc. and its wholly owned subsidiaries, as well as
Cody LCI Realty, LLC (“Realty”), a variable interest entity (“VIE”) in which the Company has a 50% ownership
interest. Noncontrolling interest in the operations of Realty is recorded net of tax as net income attributable to the noncontrolling
interest. Additionally, all intercompany accounts and transactions have been eliminated.
Business Combinations
Acquired businesses are accounted for using the acquisition method of accounting, which requires that the assets acquired and
liabilities assumed be recorded at the date of acquisition at their respective estimated fair values. The fair values and useful lives
assigned to each class of assets acquired and liabilities assumed are based on, among other factors, the expected future period of
benefit of the asset, the various characteristics of the asset and projected future cash flows. Significant judgment is employed in
determining the assumptions utilized as of the acquisition date and for each subsequent measurement period. Accordingly, changes in
assumptions described above, could have a material impact on our consolidated results of operations.
contingent consideration. Because of the inherent subjectivity and complexity involved in these estimates and assumptions, actual
results could differ from those estimates.
Foreign currency translation
The Consolidated Financial Statements are presented in U.S. Dollars, the reporting currency of the Company. The financial
statements of the Company’s foreign subsidiary are maintained in local currency and translated into U.S. dollars at the end of each
reporting period. Assets and liabilities are translated at period-end exchange rates, while revenues and expenses are translated at
average exchange rates during the period. The adjustments resulting from the use of differing exchange rates are recorded as part of
stockholders’ equity in accumulated other comprehensive income (loss). Gains and losses resulting from transactions denominated in
foreign currencies are recognized in the Consolidated Statements of Operations under Other income (loss). Amounts recorded due to
foreign currency fluctuations are immaterial to the Consolidated Financial Statements.
Cash and cash equivalents
The Company considers all highly liquid investments with original maturities less than or equal to three months at the date of purchase
to be cash and cash equivalents. Cash and cash equivalents are stated at cost, which approximates fair value and consist of bank
deposits and certificates of deposit that are readily convertible into cash. The Company maintains its cash deposits and cash
equivalents at well-known, stable financial institutions. Such amounts frequently exceed insured limits.
Investment securities
The Company’s investment securities consist of publicly-traded equity securities which are classified as trading
investments. Investment securities are recorded at fair value based on quoted market prices from broker or dealer quotations or
transparent pricing sources at each reporting date. Gains and losses are included in the Consolidated Statements of Operations under
Other income (loss).
Allowance for doubtful accounts
The Company continuously monitors collections and payments from its customers and maintains a provision for estimated credit
losses. The Company determines its allowance for doubtful accounts by considering a number of factors, including the length of time
balances are past due, the Company’s previous loss history, the customer’s current ability to pay its obligations to the Company and
the condition of the general economy and the industry as a whole. The Company writes off accounts receivable when they are
determined to be uncollectible.
Inventories
Inventories are stated at the lower of cost or market determined by the first-in, first-out method. Inventories are regularly reviewed
and provisions for excess and obsolete inventory are recorded based primarily on current inventory levels and estimated sales
forecasts.
Property, Plant and Equipment
Property, plant and equipment are stated at cost less accumulated depreciation. Depreciation is computed on a straight-line basis over
the assets’ estimated useful lives. Depreciation expense for the fiscal years ended June 30, 2016, 2015 and 2014 was $13.9 million,
$5.4 million and $4.6 million, respectively.
Reclassifications
Intangible Assets
Certain prior year amounts have been reclassified to conform to the current year financial statement presentation.
Use of estimates
The preparation of financial statements in conformity with U.S. GAAP requires management to make estimates and assumptions that
affect the reported amounts of assets and liabilities at the date of the financial statements and the reported amounts of revenues and
expenses during the reporting period. Significant estimates and assumptions are required in the determination of revenue recognition
and sales deductions for estimated chargebacks, rebates, returns and other adjustments including a provision for the Company’s
liability under the Medicare Part D program. Additionally, significant estimates and assumptions are required when determining the
fair value of long-lived assets, including goodwill and intangible assets, income taxes, contingencies, share-based compensation and
Definite-lived intangible assets are stated at cost less accumulated amortization. Amortization of definite-lived intangible assets is
computed on a straight-line basis over the assets’ estimated useful lives, generally for periods ranging from 10 to 15 years. The
Company continually evaluates the reasonableness of the useful lives of these assets. Indefinite-lived intangible assets are not
amortized, but instead are tested at least annually for impairment. Costs to renew or extend the life of a recognized intangible asset are
expensed as incurred.
Valuation of Long-Lived Assets, including Intangible Assets
The Company’s long-lived assets primarily consist of property, plant and equipment and definite and indefinite-lived intangible assets.
Property, plant and equipment and definite-lived intangible assets are reviewed for impairment whenever events or changes in
104
105
�circumstances (“triggering events”) indicate that the carrying amount of the asset may not be recoverable. If a triggering event is
determined to have occurred, the asset’s carrying value is compared to the future undiscounted cash flows expected to be generated by
the asset. If the carrying value exceeds the undiscounted cash flow of the asset, then impairment exists. Indefinite-lived intangible
assets are tested for impairment at least annually during the fourth quarter of each fiscal year or more frequently if events or changes
in circumstances indicate that the asset might be impaired. An impairment loss is measured as the excess of the asset’s carrying value
over its fair value, which in most cases is calculated using a discounted cash flow model. Discounted cash flow models are highly
reliant on various assumptions which are considered Level 3 inputs, including estimates of future cash flows (including long-term
growth rates), discount rates and the probability of achieving the estimated cash flows.. The judgments made in determining estimated
fair values can materially impact our results of operations.
In-Process Research and Development
Amounts allocated to in-process research and development (“IPR&D”) in connection with a business combination are recorded at fair
value and are considered indefinite-lived intangible assets subject to impairment testing in accordance with the Company’s
impairment testing policy for indefinite-lived intangible assets. As products in development are approved for sale, amounts will be
allocated to product rights and will be amortized over their estimated useful lives. Definite-lived intangible assets are amortized over
the expected life of the asset. The judgments made in determining the estimated fair value of in-process research and development, as
well as asset lives, can materially impact our results of operations. The Company’s fair value assessments are highly reliant on
various assumptions which are considered Level 3 inputs, including estimates of future cash flows (including long-term growth rates),
discount rates and the probability of achieving the estimated cash flows. Changes in any of the Company’s assumptions may result in
a reduction to the estimated fair value of the IPR&D asset and could result in future impairment charges. In the fourth quarter of
Fiscal 2016, the Company recorded an $8.0 million impairment charge related to certain IPR&D assets acquired as part of the KUPI
acquisition. The impairment was mainly related to delays in expected launch dates as well as competitive pricing factors for two
products in development.
Goodwill
Goodwill, which represents the excess of purchase price over the fair value of net assets acquired, is carried at cost. Goodwill is tested
for impairment on an annual basis on the first day of the fourth quarter of each fiscal year or more frequently if events or changes in
circumstances indicate that the asset might be impaired. The Company first performs a qualitative assessment to determine if the
quantitative impairment test is required. If changes in circumstances indicate an asset may be impaired, the Company performs the
quantitative impairment test. In accordance with accounting standards, a two-step quantitative method is used for determining
goodwill impairment. In the first step, the Company determines the fair value of our reporting unit (generic pharmaceuticals). If the
net book value of our reporting unit exceeds its fair value, the second step of the impairment test which requires allocation of our
reporting unit’s fair value to all of its assets and liabilities using the acquisition method prescribed under authoritative guidance for
business combinations would then be performed. Any residual fair value is allocated to goodwill. An impairment charge is recognized
to the extent that our reporting unit’s goodwill is less than its carrying amount. The judgments made in determining the estimated fair
value of goodwill can materially impact our results of operations. The Company’s fair value assessments are highly reliant on various
assumptions which are considered Level 3 inputs, including estimates of future cash flows (including long-term growth rates),
discount rates and the probability of achieving the estimated cash flows.
Segment Information
The Company operates in one reportable segment, generic pharmaceuticals. As such, the Company aggregates its financial
information for all products. The following table identifies the Company’s net sales by medical indication for fiscal years ended
June 30, 2016, 2015 and 2014:
(In thousands)
Medical Indication
Antibiotic
Cardiovascular
Central Nervous System
Gallstone
Gastrointestinal
Glaucoma
Gout
Migraine
Muscle Relaxant
Obesity
Pain Management
Respiratory
Thyroid Deficiency
Urinary
Other
Contract manufacturing revenue
Net sales
Settlement agreement
Total net sales
Fiscal Year Ended June 30,
2015
2016
2014
$
$
14,558
53,541
36,291
67,348
52,699
25,336
303
21,776
5,403
3,809
29,804
9,982
162,411
17,398
43,389
22,043
566,091
(23,598)
542,493
$
$
12,306
55,166
—
65,262
—
21,145
6,833
25,729
8,779
4,004
27,461
—
153,460
212
26,480
—
406,837
—
406,837
$
$
13,572
62,121
—
6,578
—
11,987
10,822
14,527
—
4,032
27,174
—
102,248
—
20,710
—
273,771
—
273,771
Customer, Supplier and Product Concentration
The following table presents the percentage of total net sales, for the fiscal years ended June 30, 2016, 2015 and 2014, for certain of
the Company’s products, defined as products containing the same active ingredient or combination of ingredients, which accounted
for at least 10% of total net sales in any of those periods:
Product 1
Product 2
Product 3
June 30,
2016
June 30,
2015
June 30,
2014
30%
12%
4%
38%
16%
12%
37%
2%
20%
The following table presents the percentage of total net sales, for the fiscal years ended June 30, 2016, 2015 and 2014, for certain of
the Company’s customers which accounted for at least 10% of total net sales in any of those periods:
Customer A
Customer B
Customer C
June 30,
2016
June 30,
2015
June 30,
2014
25%
16%
—%
30%
11%
—%
19%
8%
13%
The Company’s primary finished product inventory supplier is Jerome Stevens Pharmaceuticals, Inc. (“JSP”), in Bohemia, New York.
Purchases of finished goods inventory from JSP accounted for 52%, 68% and 62% of the Company’s inventory purchases in fiscal
years 2016, 2015 and 2014, respectively. See Note 21 “Material Contracts with Suppliers” for more information.
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107
�Revenue Recognition
Share-based Compensation
The Company recognizes revenue when title and risk of loss have transferred to the customer and provisions for rebates, promotional
adjustments, price adjustments, returns, chargebacks and other potential adjustments are reasonably determinable. The Company also
considers all other relevant criteria specified in Securities and Exchange Commission Staff Accounting Bulletin No. 104, Topic
No. 13, “Revenue Recognition,” in determining when to recognize revenue.
Net Sales Adjustments
When revenue is recognized, a simultaneous adjustment to gross sales is made for chargebacks, rebates, returns, promotional
adjustments and other potential adjustments. These provisions are primarily estimated based on historical experience, future
expectations, contractual arrangements with wholesalers and indirect customers and other factors known to management at the time of
accrual. Accruals for provisions are presented in the Consolidated Financial Statements as a reduction to gross sales with the
corresponding reserve presented as a reduction of accounts receivable or included as rebates payable, depending on the nature of the
reserve. The reserves, presented as a reduction of accounts receivable, totaled $176.1 million and $69.4 million at June 30, 2016 and
2015, respectively. Rebates payable at June 30, 2016 and 2015 included $21.9 million and $7.6 million, respectively, for certain
rebate programs, primarily related to Medicare Part D and Medicaid and certain sales allowances and other adjustments paid to
indirect customers.
Cost of Sales, including Amortization of Intangibles
Cost of sales includes all costs related to bringing products to their final selling destination, which includes direct and indirect costs,
such as direct material, labor and overhead expenses. Additionally, cost of sales includes product royalties, depreciation, amortization
and costs to renew or extend recognized intangible assets, freight charges and other shipping and handling expenses.
Research and Development
Research and development costs are expensed as incurred, including all production costs until a drug candidate is approved by the
FDA. Research and development expenses include costs associated with internal projects as well as costs associated with third-party
research and development contracts.
Contingencies
Loss contingencies, including litigation related contingencies, are included in the Consolidated Statements of Operations when the
Company concludes that a loss is both probable and reasonably estimable. Legal fees related to litigation-related matters are expensed
as incurred and included in the Consolidated Statements of Operations under the Selling, general and administrative line item.
Contingent Consideration
Contingent consideration resulting from the KUPI acquisition was recorded at its estimated fair value on the acquisition date. The
Company has agreed to a 50/50 split of the additional tax liabilities UCB will incur associated with the IRS Section 338(H)(10) tax
election, up to $35.0 million. This election is expected to result in additional tax benefits to the Company of approximately $100.0
million. Future decreases, if any, in the estimated fair value of the contingent consideration will be recorded as gains in the
Consolidated Statements of Operations. Decreases in the estimated fair value of the contingent consideration obligation can result
from lower tax liabilities incurred by UCB associated with the IRS Section 338(H)(10) tax election. These fair value measurements
represent Level 3 measurements, as they are based on significant inputs not observable in the market.
Share-based compensation costs are recognized over the vesting period, using a straight-line method, based on the fair value of the
instrument on the date of grant less an estimate for expected forfeitures. The Company uses the Black-Scholes valuation model to
determine the fair value of stock options and the stock price on the grant date to value restricted stock. The Black-Scholes valuation
model includes various assumptions, including the expected volatility, the expected life of the award, dividend yield and the risk-free
interest rate. These assumptions involve inherent uncertainties based on market conditions which are generally outside the Company’s
control. Changes in these assumptions could have a material impact on share-based compensation costs recognized in the financial
statements.
Income Taxes
The Company uses the asset and liability method to account for income taxes as prescribed by Accounting Standards Codification
(“ASC”) 740, Income Taxes. Deferred tax assets and liabilities are determined based on the difference between the financial
statement and tax bases of assets and liabilities as measured by the enacted tax rates which will be in effect when these differences
reverse. Deferred tax expense (benefit) is the result of changes in deferred tax assets and liabilities. Deferred income tax assets and
liabilities are adjusted to recognize the effects of changes in tax laws or enacted tax rates in the period during which they are signed
into law. The factors used to assess the likelihood of realization are the Company’s forecast of future taxable income and available tax
planning strategies that could be implemented to realize the net deferred tax assets. Under ASC 740, Income Taxes, a valuation
allowance is required when it is more likely than not that all or some portion of the deferred tax assets will not be realized through
generating sufficient future taxable income. Failure to achieve forecasted taxable income in applicable tax jurisdictions could affect
the ultimate realization of deferred tax assets and could result in an increase in the Company’s effective tax rate on future earnings.
The Company may recognize the tax benefit from an uncertain tax position claimed on a tax return only if it is more likely than not
that the tax position will be sustained on examination by the taxing authorities, based on the technical merits of the position. The tax
benefits recognized in the financial statements from such a position should be measured based on the largest benefit that has a greater
than 50% likelihood of being realized upon ultimate settlement. The authoritative standards issued by the Financial Accounting
Standards Board (“FASB”) also provide guidance on de-recognition, classification, interest and penalties on income taxes, accounting
in interim periods and requires increased disclosures.
Earnings Per Common Share
Basic earnings per common share attributable to Lannett Company, Inc. is computed by dividing net income attributable to Lannett
Company, Inc. common stockholders by the weighted average number of shares outstanding during the period. Diluted earnings per
common share attributable to Lannett Company, Inc. is computed by dividing net income attributable to Lannett Company, Inc.
common stockholders by the weighted average number of shares outstanding during the period including additional shares that would
have been outstanding related to potentially dilutive securities. These potentially dilutive securities primarily consist of stock options,
unvested restricted stock and an outstanding warrant. Anti-dilutive securities are excluded from the calculation. Dilutive shares are
also excluded in the calculation in periods of net loss because the effect of including such securities would be anti-dilutive.
Comprehensive Income (Loss)
Comprehensive income (loss) includes all changes in equity during a period except those that resulted from investments by or
distributions to the Company’s stockholders. Other comprehensive income (loss) refers to gains and losses that are included in
comprehensive income (loss), but excluded from net income as these amounts are recorded directly as an adjustment to stockholders’
equity.
Restructuring Costs
Recent Accounting Pronouncements
The Company records charges associated with approved restructuring plans to remove duplicative headcount and infrastructure
associated with business acquisitions or to simplify business processes. Restructuring charges can include severance costs to eliminate
a specified number of employees, infrastructure charges to vacate facilities and consolidate operations and contract cancellation costs.
The Company records restructuring charges based on estimated employee terminations, site closure and consolidation plans. The
Company accrues severance and other employee separation costs under these actions when it is probable that a liability exists and the
amount is reasonably estimable.
In May 2014, the FASB issued ASU 2014-09, Revenue from Contracts with Customers. The core principle of the guidance is that an
entity should recognize revenue to depict the transfer of promised goods or services to customers in an amount that reflects the
consideration to which the entity expects to be entitled in exchange for those goods or services. The authoritative guidance is effective
for annual reporting periods beginning after December 15, 2016. In July 2015, the FASB extended the effective date of the guidance
by one year to December 15, 2017. The Company is currently in the process of assessing the impact this guidance will have on the
consolidated financial statements.
In April 2015, the FASB issued ASU 2015-03, Simplifying the Presentation of Debt Issuance Costs which changes the presentation of
debt issuance costs in financial statements. ASU 2015-03 requires an entity to present such costs in the balance sheet as a direct
deduction from the related debt liability rather than as an asset. Amortization of the costs will continue to be reported as interest
108
109
�expense. It is effective for fiscal years and interim periods within those fiscal years beginning after December 15, 2015. Early
adoption is permitted. The new guidance will be applied retrospectively to each prior period presented. The Company has elected to
early adopt ASU 2015-03 as of December 31, 2015.
In July 2015, the FASB issued ASU 2015-11, Inventory — Simplifying the Measurement of Inventory. ASU 2015-11 requires
inventory to be subsequently measured using the lower of cost or net realizable value, thereby eliminating the market value
approach. Net realizable value is defined as the “estimated selling prices in the ordinary course of business, less reasonably
predictable costs of completion, disposal and transportation.” ASU 2015-11 is effective for reporting periods beginning after
December 15, 2016 and is applied prospectively. Early adoption is permitted. The Company is currently in the process of assessing
the impact this guidance will have on the consolidated financial statements.
In September 2015, the FASB issued ASU 2015-16, Business Combinations — Simplifying the Accounting for Measurement-Period
Adjustments. ASU 2015-16 requires that an acquirer recognize adjustments to provisional amounts that are identified during the
measurement period in the reporting period in which the adjustment amounts are determined. ASU 2015-16 also requires that the
acquirer record, in the same period’s financial statements, the effect on earnings of changes in depreciation, amortization, or other
income effects, if any, as a result of the change to the provisional amounts, calculated as if the accounting had been completed at the
acquisition date. ASU 2015-16 is effective for reporting periods beginning after December 15, 2015 and is applied
prospectively. Early adoption is permitted. The Company has elected to early adopt ASU 2015-16 as of March 31, 2016.
In November 2015, the FASB issued ASU 2015-17, Income Taxes — Balance Sheet Classification of Deferred Taxes. ASU 2015-17
requires all deferred tax assets and liabilities to be classified as noncurrent on the balance sheet. The guidance may be applied either
prospectively or retrospectively. ASU 2015-17 is effective for fiscal years and interim periods within those fiscal years beginning
after December 15, 2016. Early adoption is permitted. The Company is currently in the process of assessing the impact this guidance
will have on the consolidated financial statements.
In February 2016, the FASB issued ASU 2016-02, Leases. ASU 2016-02 requires an entity to recognize right-of-use assets and
liabilities on its balance sheet for all leases with terms longer than 12 months. Lessees and lessors are required to disclose quantitative
and qualitative information about leasing arrangements to enable a user of the financial statements to assess the amount, timing and
uncertainty of cash flows arising from leases. ASU 2016-02 is effective for annual reporting periods beginning after December 15,
2018, including interim periods within that reporting period and requires a modified retrospective application, with early adoption
permitted. The Company is currently in the process of assessing the impact this guidance will have on the consolidated financial
statements.
In March 2016, the FASB issued ASU 2016-09, Compensation — Stock Compensation: Improvements to Employee Share-Based
Payment Accounting. ASU 2016-09 clarifies several aspects of accounting for share-based compensation including the accounting for
excess tax benefits and deficiencies, accounting for forfeitures and the classification of excess tax benefits on the cash flow statement.
ASU 2016-09 is effective for fiscal years beginning after December 15, 2016 and in interim periods within those fiscal years, with
early adoption permitted. The Company is currently in the process of assessing the impact this guidance will have on the consolidated
financial statements.
Note 3. Acquisitions
Kremers Urban Pharmaceuticals Inc.
On November 25, 2015, the Company completed the acquisition of KUPI, the former U.S. specialty generic pharmaceuticals
subsidiary of global biopharmaceuticals company UCB S.A., pursuant to the terms and conditions of a Stock Purchase Agreement.
KUPI is a specialty pharmaceuticals manufacturer focused on the development of products that are difficult to formulate or utilize
specialized delivery technologies. Strategic benefits of the acquisition include expanded manufacturing capacity, a diversified product
portfolio and pipeline and complementary research and development expertise.
Pursuant to the terms of the Stock Purchase Agreement, Lannett purchased 100% of the outstanding equity interests of KUPI for total
estimated consideration of approximately $1.2 billion.
The following table summarizes the fair value of total consideration transferred to KUPI shareholders at the acquisition date of
November 25, 2015:
(In thousands)
Cash purchase price paid to KUPI shareholders
Working capital adjustment
Certain amounts reimbursed by UCB
Total cash consideration transferred to KUPI shareholders
12.0% Senior Notes issued to UCB
Acquisition-related contingent consideration
Warrant issued to UCB
Total consideration to KUPI shareholders
$
$
1,030,000
(41,605)
(37,340)
951,055
200,000
35,000
29,920
1,215,975
The Company funded the acquisition and transaction expenses with proceeds from the issuance of the $910.0 million of term loans,
$22.8 million borrowings from a revolving credit facility, the issuance of $250.0 million Senior Notes (see Note 11 “Long-term
Debt”) and cash on hand of $94.6 million. Lannett also issued a warrant with an estimated fair value of $29.9 million.
As part of the acquisition, the Company and UCB have agreed to jointly make an election under Section 338(h)(10) of the Internal
Revenue Code of 1986, as amended and under the corresponding provisions of state law, to treat the acquisition as a deemed purchase
and sale of assets for income tax purposes. The Company has agreed to reimburse UCB for 50% of the incremental tax cost of
making such election, subject to a reimbursement cap of $35.0 million. This liability has been recorded as acquisition-related
contingent consideration on the Consolidated Balance Sheet. This election is expected to result in additional tax benefits to the
Company of approximately $100.0 million.
The Company also agreed to contingent payments related to Methylphenidate ER provided the FDA reinstates the AB-rating for such
product and certain sales thresholds are met.
The Company used the acquisition method of accounting to account for this transaction. Under the acquisition method of accounting,
the assets acquired and liabilities assumed in the transaction were recorded at the date of acquisition at their respective preliminary fair
values using preliminary assumptions that are subject to change as the Company obtains additional information during the
measurement period. The Company has not finalized its valuation of certain assets and liabilities recorded in connection with this
transaction, primarily related to revenue-related reserves and tax-related accounts. Thus, the estimated fair values recorded to date are
subject to change and any changes will be recorded as adjustments to the fair value of those assets and liabilities and residual amounts
will be allocated to goodwill. The final valuation adjustments may also require adjustment to the Consolidated Statements of
Operations and Cash Flows.
110
111
�The preliminary purchase price has been allocated to the assets acquired and liabilities assumed for the KUPI business as follows:
(In thousands)
Cash and cash equivalents
Accounts receivable, net of revenue-related reserves
Inventories
Other current assets
Property, plant and equipment
Product rights
Trade name
Other intangible assets
In-process research and development
Goodwill
Deferred tax assets
Other assets
Total assets acquired
Accounts payable
Accrued expenses
Accrued payroll and payroll-related expenses
Rebates payable
Royalties payable
Other liabilities
Total net assets acquired
$
Preliminary Purchase
Price Allocation as of
November 25, 2015 (a)
16,877
$
149,209
83,815
12,873
97,418
409,000
2,920
20,000
232,000
240,575
4,956
4,859
1,274,502
(19,249)
(4,161)
(20,731)
(9,816)
(3,798)
(5,369)
1,211,378
$
Measurement Period
Adjustments (b)
Preliminary Purchase
Price Allocation as of
June 30, 2016
$
— $
(13,846)
194
(1,635)
14,431
18,000
—
(1,000)
(107,000)
92,895
(770)
5,359
6,628
—
(1,918)
(309)
—
196
—
4,597
$
16,877
135,363
84,009
11,238
111,849
427,000
2,920
19,000
125,000
333,470
4,186
10,218
1,281,130
(19,249)
(6,079)
(21,040)
(9,816)
(3,602)
(5,369)
1,215,975
(a) As originally reported in the Company’s Quarterly Report on Form 10-Q for the period ended December 31, 2015.
(b) The measurement period adjustments relate to 1) finalizing working capital adjustments totaling $4.6 million 2) finalized
valuations for inventories and property, plant and equipment, 3) receipt of additional information related to product
development timelines and 4) revenue-related reserve estimates, all of which reflect facts and circumstances that existed as of
the acquisition date. These adjustments did not have a significant impact on the Company’s previously reported consolidated
financial statements.
Included in the preliminary purchase price allocation above are indemnification assets totaling approximately $20.7 million, of which
$10.4 million relates to compensation-related payments, $4.9 million relates to unrecognized tax benefits and $5.4 million for
chargeback and rebate-related items. The inventory balance above includes $19.1 million to reflect fair value step-up adjustments.
KUPI’s intangible assets primarily consist of product rights and in-process research and development. See Note 10 “Goodwill and
Intangible Assets.”
Amounts allocated to acquired in-process research and development represent an estimate of the fair value of purchased in-process
technology for research projects that, as of the closing date of the acquisition, had not yet reached technological feasibility and had no
alternative future use. The fair value of in-process research and development was based on the excess earnings method, which utilizes
forecasts of expected cash inflows (including estimates for ongoing costs) and other contributory charges, on a project-by-project basis
at the appropriate discount rate for the inherent risk in each project and will be tested for impairment in accordance with the
Company’s policy for testing indefinite-lived intangible assets. In the fourth quarter of Fiscal 2016, the Company recorded an $8.0
million impairment charge related to certain intangible assets acquired as part of the KUPI acquisition. The impairment was mainly
related to delays in expected launch dates as well as competitive pricing factors for two products in development.
Goodwill of $333.5 million arising from the acquisition consists primarily of the value of the employee workforce and the value of
products to be developed in the future. The goodwill was assigned to the Company’s only reporting unit. Goodwill recognized is
expected to be fully deductible for income tax purposes.
The amounts of KUPI Net Sales and Net income attributable to Lannett Company, Inc. included in the Company’s Consolidated
Statements of Operations from November 25, 2015 to June 30, 2016 are as follows:
(In thousands, except per share data)
Total net sales
Loss attributable to Lannett Company, Inc.
Loss per common share attributable to Lannett Company, Inc.:
Basic
Diluted
For the fiscal year ended
June 30,
2016
$
$
$
165,649
(3,431)
(0.09)
(0.09)
During the fiscal year ended June 30, 2016, the Company recorded $21.5 million of acquisition-related expenses directly related to the
KUPI acquisition.
Unaudited Pro Forma Financial Results
The following supplemental unaudited pro forma information presents the financial results as if the acquisition of KUPI had occurred
on July 1, 2014 for the fiscal years ended June 30, 2016 and 2015. This supplemental pro forma information has been prepared for
comparative purposes and does not purport to be indicative of what would have occurred had the acquisition been made on July 1,
2014, nor are they indicative of any future results:
(In thousands, except per share data)
Total net sales
Net income attributable to Lannett Company, Inc.
Earnings per common share attributable to Lannett Company, Inc.:
Basic
Diluted
For the fiscal year ended
June 30,
2016
689,754
61,916
1.70
1.66
$
$
$
2015
809,379
116,119
3.24
3.13
$
$
$
The supplemental pro forma earnings for the fiscal year ended June 30, 2016 were adjusted to exclude $28.9 million of acquisition-
related costs, of which $21.5 million was incurred by Lannett and $7.4 million was incurred by KUPI, as well as to exclude $17.0
million of expense related to the amortization of fair value adjustments to acquisition-date inventory.
The supplemental pro forma earnings for the fiscal year ended June 30, 2015 were adjusted to include $28.9 million of acquisition-
related costs, of which $21.5 million was incurred by Lannett and $7.4 million was incurred by KUPI, as well as to include $18.9
million of expense related to the amortization of fair value step-up adjustments to acquisition-date inventory.
Silarx
On June 1, 2015, the Company completed the acquisition of Silarx Pharmaceuticals, Inc., a New York corporation and Stoneleigh
Realty, LLC, a New York limited liability company (together “Silarx”), pursuant to the terms and conditions of a Stock Purchase
Agreement. Silarx manufactures and markets high-quality liquid pharmaceutical products, including generic prescription and over-
the-counter products. Silarx operates within a manufacturing facility located in Carmel, New York. Strategic benefits of the
acquisition include an FDA-approved manufacturing facility, research and development expertise and added diversity to Lannett’s
portfolio of existing and pipeline products.
Pursuant to the terms of the Stock Purchase Agreement, Lannett purchased 100% of the outstanding equity interests of Silarx for cash
consideration totaling $42.5 million. The Company used the acquisition method of accounting to account for this transaction. Under
the acquisition method of accounting, the assets acquired and liabilities assumed in the transaction were recorded at the date of
acquisition at their respective fair values using assumptions that were subject to change.
112
113
�The purchase price has been allocated to the assets acquired and liabilities assumed for the Silarx business as follows:
(In thousands)
Cash
Accounts receivable, net of revenue-related reserves
Inventories
Other current assets
Property, plant and equipment
Product rights
In-process research and development
Goodwill
Other current assets
Total assets acquired
Accounts payable
Income taxes payable
Total net assets acquired
$
$
664
4,396
2,705
467
7,247
10,000
18,000
141
9
43,629
(711)
(392)
42,526
Amounts allocated to acquired in-process research and development represent an estimate of the fair value of purchased in-process
technology for research projects that, as of the closing date of the acquisition, had not yet reached technological feasibility and had no
alternative future use. The fair value of in-process research and development was based on the excess earnings method, which utilizes
forecasts of expected cash inflows (including estimates for ongoing costs) and other contributory charges, on a project-by-project basis
at the appropriate discount rate for the inherent risk in each project and will be tested for impairment in accordance with the
Company’s policy for testing indefinite-lived intangible assets.
Product rights totaling $10.0 million are comprised of currently marketed products that have an estimated useful life of 15 years. The
goodwill of $141 thousand arising from the acquisition consists primarily of the value of the employee workforce and the value of
products to be developed in the future. The goodwill was assigned to the Company’s only reporting unit. Goodwill recognized is
expected to be fully deductible for income tax purposes.
Note 4. Restructuring Charges
2016 Restructuring Program
On February 1, 2016, in connection with the acquisition of KUPI, the Company announced a plan related to the future integration of
KUPI and the Company’s operations. The plan focuses on the closure of KUPI’s corporate functions and the consolidation of
manufacturing, sales, research and development and distribution functions. The Company estimates that it will incur an aggregate of
up to approximately $23.0 million in restructuring charges for actions that have been announced or communicated since the 2016
Restructuring Program began. Of this amount, approximately $14.0 million relates to employee separation costs, approximately $1.0
million relates to contract termination costs and approximately $8.0 million relates to facility closure costs and other actions. The 2016
Restructuring Program is expected to be completed by the end of Fiscal 2019. The expenses associated with the restructuring program
included in restructuring expenses during the twelve months ended June 30, 2016 were as follows:
(In thousands)
Employee separation costs
Contract termination costs
Facility closure costs
Total
Twelve
Months Ended June
30, 2016
$
$
5,789
701
676
7,166
A reconciliation of the changes in restructuring liabilities associated with the 2016 Restructuring Program from June 30, 2015 through
June 30, 2016 is set forth in the following table:
(In thousands)
Balance at June 30, 2015
Restructuring Charges
Payments
Balance at June 30, 2016
Note 5. Accounts Receivable
Employee
Separation Costs
$
— $
5,789
(1,956)
3,833
$
$
Contract
Termination
Costs
Facility Closure
Costs
Total
— $
701
(404)
297
$
— $
676
(676)
—
$
—
7,166
(3,036)
4,130
Accounts receivable consisted of the following components at June 30, 2016 and 2015:
(In thousands)
Gross accounts receivable
Less Chargebacks reserve
Less Rebates reserve
Less Returns reserve
Less Other deductions
Less Allowance for doubtful accounts
Accounts receivable, net
June 30,
2016
June 30,
2015
$
$
388,460
(86,495)
(32,189)
(40,593)
(16,851)
(610)
211,722
$
$
160,960
(35,801)
(12,945)
(19,209)
(1,528)
(374)
91,103
For the fiscal year ended June 30, 2016, the Company recorded a provision for chargebacks, rebates, returns and other deductions of
$646.9 million, $189.2 million, $21.3 million and $50.0 million, respectively. For the fiscal year ended June 30, 2015, the Company
recorded a provision for chargebacks, rebates, returns and other deductions of $338.7 million, $83.4 million, $17.7 million and $30.7
million, respectively. For the fiscal year ended June 30, 2014, the Company recorded a provision for chargebacks, rebates, returns and
other deductions of $144.6 million, $56.3 million, $6.6 million and $21.5 million, respectively.
Note 6. Inventories
Inventories, net of allowances, at June 30, 2016 and 2015 consisted of the following:
(In thousands)
Raw Materials
Work-in-process
Finished Goods
Total
June 30,
2016
June 30,
2015
$
$
47,881
20,207
46,816
114,904
$
$
22,385
5,246
18,560
46,191
During the fiscal years ended June 30, 2016, 2015 and 2014, the Company recorded provisions for excess and obsolete inventory of
$9.4 million, $6.7 million and $2.9 million, respectively. The reserve for excess and obsolete inventory was $6.9 million and $5.0
million at June 30, 2016 and 2015, respectively.
114
115
�Note 7. Property, Plant and Equipment
The Company’s financial assets and liabilities measured at fair value at June 30, 2016 and June 30, 2015 were as follows:
(In thousands)
Assets
Equity securities
Total Assets
Liabilities
Acquisition-related contingent consideration
Total Liabilities
(In thousands)
Assets
Equity securities
Total Investment Securities
Note 9. Investment Securities
Level 1
Level 2
Level 3
Total
June 30, 2016
14,094
14,094
$
$
—
$
— $
—
$
— $
14,094
14,094
—
$
— $
—
$
— $
35,000
35,000
$
$
35,000
35,000
Level 1
Level 2
Level 3
Total
June 30, 2015
13,467
13,467
$
$
—
$
— $
—
$
— $
13,467
13,467
$
$
$
$
$
$
The Company uses the specific identification method to determine the cost of securities sold, which consisted entirely of securities
classified as trading.
The Company had a net loss on investment securities of $11 thousand during the fiscal year ended June 30, 2016, which included an
unrealized loss related to securities still held at June 30, 2016 of $51 thousand.
The Company had a net gain on investment securities of $705 thousand during the fiscal year ended June 30, 2015, which included an
unrealized loss related to securities still held at June 30, 2015 of $1.1 million.
The Company had a net gain on investment securities during the fiscal year ended June 30, 2014 of $1.9 million, which included an
unrealized gain related to securities still held at June 30, 2014 of $745 thousand.
Property, plant and equipment at June 30, 2016 and 2015 consisted of the following:
(In thousands)
Land
Building and improvements
Machinery and equipment
Furniture and fixtures
Construction in progress
Property, plant and equipment, gross
Less accumulated depreciation
Property, plant and equipment, net
Useful Lives
—
10 - 39 years
5 - 10 years
5 - 7 years
—
June 30,
2016
June 30,
2015
$
$
7,190
108,316
114,501
2,856
37,373
270,236
(53,598)
216,638
$
$
5,891
51,446
47,681
1,748
28,228
134,994
(40,438)
94,556
During the fiscal years ended June 30, 2016, 2015 and 2014, the Company had no impairment charges related to property, plant and
equipment. Property, plant and equipment, net included amounts held in foreign countries in the amount of $1.0 million and $1.2
million at June 30, 2016 and 2015, respectively.
Note 8. Fair Value Measurements
The Company’s financial instruments recorded in the Consolidated Balance Sheets include cash and cash equivalents, accounts
receivable, investment securities, accounts payable, accrued expenses and debt obligations. Included in cash and cash equivalents are
certificates of deposit with maturities less than or equal to three months at the date of purchase and money market funds. The carrying
value of certain financial instruments, primarily cash and cash equivalents, accounts receivable, accounts payable and accrued
expenses, approximate their estimated fair values based upon the short-term nature of their maturity dates. The carrying amount of the
Company’s debt obligations approximates fair value based on current interest rates available to the Company on similar debt
obligations.
The Company follows the authoritative guidance of ASC Topic 820 Fair Value Measurements and Disclosures. Fair value is defined
as the exchange price that would be received for an asset or paid to transfer a liability (an exit price) in the principal or most
advantageous market for the asset or liability in an orderly transaction between market participants on the measurement date. The
authoritative guidance also establishes a fair value hierarchy which requires an entity to maximize the use of observable inputs and
minimize the use of unobservable inputs when measuring fair value. The Company’s financial assets and liabilities measured at fair
value are entirely within Level 1 of the hierarchy as defined below:
Level 1 — Quoted prices (unadjusted) in active markets for identical assets or liabilities that the reporting entity can access at the
measurement date.
Level 2 — Directly or indirectly observable inputs, other than quoted prices, such as quoted prices for similar assets or liabilities;
quoted prices for identical or similar instruments in markets that are not active; or model-derived valuations whose inputs are
observable or whose significant value drivers are observable.
Level 3 — Unobservable inputs that are supported by little or no market activity and that are material to the fair value of the asset
or liability. Financial instruments whose values are determined using pricing models, discounted cash flow methodologies, or
similar techniques, as well as instruments for which the determination of fair value requires significant judgment or estimation are
examples of Level 3 assets and liabilities.
If the inputs used to measure the financial assets and liabilities fall within more than one level described above, the categorization is
based on the lowest level input that is significant to the fair value measurement of the instrument.
116
117
�Note 10. Goodwill and Intangible Assets
Note 11. Long-Term Debt
The changes in the carrying amount of goodwill for the twelve months ended June 30, 2016 are as follows:
Amended Senior Secured Credit Facility
(In thousands)
Balance at June 30, 2015
Goodwill acquired
Balance at June 30, 2016
Generic
Pharmaceuticals
141
$
333,470
333,611
$
Intangible assets, net as of June 30, 2016 and June 30, 2015, consisted of the following:
(In thousands)
Definite-lived:
Cody Labs import license
KUPI product rights
KUPI trade name
KUPI other intangible assets
Silarx product rights
Other product rights
Total definite-lived
Indefinite-lived:
KUPI in-process research
and development
Silarx in-process research
and development
Other product rights
Total indefinite-lived
Total intangible assets,
net
Weighted Gross Carrying Amount Accumulated Amortization
Avg. Life
(Yrs.)
June 30,
2015
June 30,
2016
June 30,
2016
June 30,
2015
Intangible Assets, Net
June 30,
June 30,
2015
2016
15
15
2
15
15
14
—
—
—
$
$
582 $
427,000
2,920
19,000
10,000
653
460,155 $
582 $
—
—
—
10,000
653
11,235 $
(309) $
(17,119)
(878)
(762)
(722)
(311)
(20,101) $
(269) $
—
—
—
(56)
(269)
(594) $
273 $
409,881
2,042
18,238
9,278
342
440,054 $
313
—
—
—
9,944
384
10,641
$
117,000 $
— $
— $
— $
117,000 $
—
18,000
449
135,449
18,000
449
18,449
—
—
—
—
—
—
18,000
449
135,449
18,000
449
18,449
$
595,604 $
29,684 $
(20,101) $
(594) $
575,503 $
29,090
For the fiscal years ended June 30, 2016, 2015 and 2014, the Company recorded amortization expense of $19.5 million, $137
thousand and $1.4 million, respectively.
As part of the Company’s annual impairment analysis performed during the fourth quarter of Fiscal 2016, the Company recorded an
impairment charge of $8.0 million related to certain intangible assets acquired as part of the KUPI acquisition resulting in a decrease
of IPR&D assets at June 30, 2016. The impairment was mainly related to delays in expected launch dates as well as competitive
pricing factors for two products in development.
Future annual amortization expense consists of the following:
(In thousands)
Fiscal Year Ending June 30,
2017
2018
2019
2020
2021
Thereafter
$
Annual Amortization Expense
31,942
31,064
30,479
30,472
30,472
285,625
440,054
$
On November 25, 2015, in connection with its acquisition of KUPI, Lannett entered into a credit and guaranty agreement (the “Credit
and Guaranty Agreement”) among certain of its wholly-owned domestic subsidiaries, as guarantors, Morgan Stanley Senior
Funding, Inc., as administrative agent and collateral agent and other lenders providing for a senior secured credit facility (the “Senior
Secured Credit Facility”).
The Senior Secured Credit Facility consisted of a Term Loan A facility in an aggregate principal amount of $275.0 million, a Term
Loan B facility in an aggregate principal amount of $635.0 million and a revolving credit facility providing for revolving loans in an
aggregate principal amount of up to $125.0 million. On April 8, 2016, the Company drew down the full $125.0 million Revolving
Credit Facility for working capital and other general purposes. The entire balance of the Revolving Credit Facility loan is outstanding
as of June 30, 2016.
On June 17, 2016, Lannett amended the Senior Secured Credit Facility and the Credit and Guaranty Agreement to raise an incremental
term loan in the principal amount of $150.0 million (the “Incremental Term Loan”) and amended certain sections of the agreement
(the “Amended Senior Secured Credit Facility”). The terms of this Incremental Term Loan are substantially the same as those
applicable to the Term Loan B facility. The Company used the proceeds of the Incremental Term Loan and cash on hand to
repurchase the outstanding $250.0 million aggregate principal amount of Lannett’s 12.0% Senior Notes due 2023 (the “Senior Notes”)
issued in connection with the KUPI acquisition.
The Term Loan A Facility will mature on November 25, 2020. The Term Loan A Facility amortizes in quarterly installments
(a) through December 31, 2017 in amounts equal to 1.25% of the original principal amount of the Term Loan A Facility and (b) from
January 1, 2018 through September 30, 2020 in amounts equal to 2.50% of the original principal amount of the Term Loan A Facility,
with the balance payable on November 25, 2020. The Term Loan B Facility will mature on November 25, 2022. The Term Loan B
Facility amortizes in equal quarterly installments in amounts equal to 1.25% of the original principal amount of the Term Loan B
Facility with the balance payable on November 25, 2022. Any outstanding Revolving Loans will mature on November 25, 2020.
The Amended Senior Secured Credit Facility is guaranteed by all of Lannett’s significant wholly-owned domestic subsidiaries (the
“Subsidiary Guarantors”) and is collateralized by substantially all present and future assets of Lannett and the Subsidiary Guarantors.
The interest rates applicable to the Amended Term Loan Facility are based on a fluctuating rate of interest of the greater of an adjusted
LIBOR and 1.00%, plus a borrowing margin of 4.75% (for Term Loan A Facility) or 5.375% (for Term Loan B Facility). The interest
rates applicable to the Revolving Credit Facility is based on a fluctuating rate of interest of an adjusted LIBOR plus a borrowing
margin of 4.75%. The interest rate applicable to the unused commitment for the Revolving Credit Facility was initially
0.50%. Beginning March 2016, the interest margins and unused commitment fee on the Revolving Credit Facility are subject to a
leveraged based pricing grid.
The Amended Senior Secured Credit Facility contains a number of covenants that, among other things, limit the ability of Lannett and
its restricted subsidiaries to: incur more indebtedness; pay dividends; redeem stock or make other distributions of equity; make
investments; create restrictions on the ability of Lannett’s restricted subsidiaries that are not Subsidiary Guarantors to pay dividends to
Lannett or make intercompany transfers; create negative pledges; create liens; transfer or sell assets; merge or consolidate; enter into
sale leasebacks; enter into certain transactions with Lannett’s affiliates; and prepay or amend the terms of certain indebtedness.
The Amended Senior Secured Credit Facility contains a financial performance covenant that is triggered when the aggregate principal
amount of outstanding Revolving Credit Facility and outstanding letters of credit as of the last day of the most recent fiscal quarter is
greater than 30% of the aggregate commitments under the Revolving Credit Facility. The covenant provides that Lannett shall not
permit its first lien net senior secured leverage ratio as of the last day of any four consecutive fiscal quarters (i) from and after
December 31, 2015, to be greater than 4.25:1.00 (ii) from and after December 31, 2017 to be greater than 3.75:1.00 and (iii) from and
after December 31, 2019 to be greater than 3.25:1.00.
The Amended Senior Secured Credit Facility also contains a financial performance covenant for the benefit of the Term Loan A
Facility lenders which provides that Lannett shall not permit its net senior secured leverage ratio as of the last day of any four
consecutive fiscal quarters (i) prior to December 31, 2017, to be greater than 4.25:1.00, (ii) as of December 31, 2017 and prior to
December 31, 2019 to be greater than 3.75:1.00 and (iii) as of December 31, 2019 and thereafter to be greater than 3.25:1.00.
The Amended Senior Secured Credit Facility also contains certain affirmative covenants, including financial and other reporting
requirements.
118
119
�12.0% Senior Notes due 2023
On November 25, 2015, in connection with the KUPI acquisition, Lannett issued $250.0 million aggregate principal amount of its
unsecured 12.0% Senior Notes due 2023 under an Indenture. Interest on the Senior Notes accrued at the rate of 12.0% per annum and
was payable semi-annually on June 15 and December 15 of each year. The Senior Notes had a maturity date of December 15, 2023.
The Senior Notes were guaranteed by each of Lannett’s current and future domestic subsidiaries that guarantee Lannett’s obligations
under the Amended Senior Secured Credit Facility.
On May 26, 2016, the Company repurchased $50.0 million of the $250.0 million aggregate principal amount of the Senior Notes. On
June 20, 2016, the Company completed the repurchase of the remaining $200.0 million of Senior Notes. The repurchase of the $250.0
million aggregate principal amount of the Senior Notes resulted in a loss on extinguishment of approximately $3.0 million.
In connection with the Senior Secured Credit Facility and the Senior Notes, the Company incurred an initial purchaser’s discount of
$72.1 million and debt issuance costs of $32.7 million. These costs are recorded as a reduction of long-term debt in the Consolidated
Balance Sheet. In connection with the amendment to the Senior Secured Credit Facility and raising the Incremental Term Loan, the
Company capitalized $14.0 million of initial purchaser’s discount and other fees and expensed $2.2 million of legal and other
expenses.
Citibank Line of Credit
On November 25, 2015, in connection with the financing of the KUPI acquisition, the Company terminated the Citibank Line of
Credit.
Note 12. Legal and Regulatory Matters
Richard Asherman
On April 16, 2013, Richard Asherman (“Asherman”), the former President of and a member in Realty, filed a complaint
(“Complaint”) in Wyoming state court against the Company and Cody Labs. At the same time, he also filed an application for a
temporary restraining order to enjoin certain operations at Cody Labs, claiming, among other things, that Cody Labs is in violation of
certain zoning laws and that Cody Labs is required to increase the level of its property insurance and to secure performance bonds for
work being performed at Cody Labs. Mr. Asherman claims Cody Labs is in breach of his employment agreement and is required to
pay him severance under his employment agreement, including 18 months of base salary, vesting of unvested stock options and
continuation of benefits. The Company estimates that the aggregate value of the claimed severance benefits is approximately $350
thousand to $400 thousand, plus the value of any stock options that he can prove was lost as a result of his termination. Mr. Asherman
also asserts that the Company is in breach of the Realty Operating Agreement and, among other requested remedies, he seeks to have
the Company (i) pay him 50% of the value of 1.66 acres of land that Realty previously agreed to donate to an economic development
entity associated with the City of Cody, Wyoming, which contemplated transaction has since been avoided and cancelled. Although
Mr. Asherman originally sought to require that Lannett acquire his interest in Realty for an unspecified price and/or to dissolve Realty,
those claims have been dismissed.
The Company strongly disputes the claims in the Complaint and has filed motions for summary judgment. Trial is currently
scheduled for October 2016. If Mr. Asherman is successful on his claim for breach of his employment agreement, he would be
entitled to his contractual severance — 18 months’ salary plus the vesting of any stock options which Mr. Asherman can prove were
capable of being exercised and were actually exercised within three months of his termination. The Company does not believe that he
is entitled to any payments with respect to the options, plus a continuation of benefits. At this time, the Company is unable to
reasonably estimate a range or aggregate dollar amount of any potential loss, if any, to the Company. The Company does not believe
that the ultimate resolution of the matter will have a significant impact on the Company’s financial position, results of operations or
cash flows.
Long-term debt, net consisted of the following:
(In thousands)
Term Loan A due 2020
Unamortized discount and other debt issuance costs
Term Loan A, net
Term Loan B due 2022
Unamortized discount and other debt issuance costs
Term Loan B, net
Revolving Credit Facility due 2020
Other
Total debt, net
Less short-term borrowings and current portion of long-term debt
Total long-term debt, net
Long-term debt amounts due, for the twelve month periods ending June 30 were as follows:
(In thousands)
2017
2018
2019
2020
2021
Thereafter
Total
June 30,
2016
June 30,
2015
Connecticut Attorney General Inquiry
—
—
—
—
—
—
—
1,009
1,009
(135)
874
$
$
268,125
(22,104)
246,021
767,226
(77,273)
689,953
125,000
874
1,061,848
(178,236)
883,612
$
$
Amounts Payable
to Institutions
$
$
178,236
60,118
66,999
67,006
218,264
570,602
1,161,225
In July 2014, the Company received interrogatories and subpoena from the State of Connecticut Office of the Attorney General
concerning its investigation into pricing of digoxin. According to the subpoena, the Connecticut Attorney General is investigating
whether anyone engaged in any activities that resulted in (a) fixing, maintaining or controlling prices of digoxin or (b) allocating and
dividing customers or territories relating to the sale of digoxin in violation of Connecticut antitrust law. In June 2016, the Connecticut
Attorney General issued interrogatories and a subpoena to an employee of the Company in order to gain access to documents and
responses previously supplied to the Department of Justice. The Company maintains that it acted in compliance with all applicable
laws and regulations and continues to cooperate with the Connecticut Attorney General’s investigation.
Federal Investigation into the Generic Pharmaceutical Industry
In fiscal year 2015, the Company and certain affiliated individuals each were served with a grand jury subpoena relating to a federal
investigation of the generic pharmaceutical industry into possible violations of the Sherman Act. The subpoenas request corporate
documents of the Company relating to corporate, financial and employee information, communications or correspondence with
competitors regarding the sale of generic prescription medications and the marketing, sale, or pricing of certain products, generally for
the period of 2005 through the dates of the subpoenas.
Based on reviews performed to date by outside counsel, the Company currently believes that it has acted in compliance with all
applicable laws and regulations and continues to cooperate with the federal investigation.
Patent Infringement (Paragraph IV Certification)
There is substantial litigation in the pharmaceutical industry with respect to the manufacture, use and sale of new products which are
the subject of conflicting patent and intellectual property claims. Certain of these claims relate to paragraph IV certifications, which
allege that an innovator patent is invalid or would not be infringed upon by the manufacture, use, or sale of the new drug.
Zomig®
The Company filed with the Food and Drug Administration an ANDA No. 206350, along with a paragraph IV certification, alleging
that the two patents associated with the Zomig® nasal spray product (U.S. Patent No. 6,750,237 and U.S. Patent No. 67,220,767) are
invalid.
120
121
�In July 2014, AstraZeneca AB, AstraZeneca UK Limited and Impax Laboratories, Inc. filed two patent infringement lawsuits in the
United States District Court for the District of Delaware, alleging that the Company’s filing of ANDA No. 206350 constitutes an act
of patent infringement and seeking a declaration that the two patents at issue are valid and infringed.
In September 2014, the Company filed a motion to dismiss one patent infringement lawsuit for lack of standing and responded to the
second lawsuit by denying that any valid patent claim would be infringed. In the second lawsuit, the Company also counterclaimed
for a declaratory judgment that the patent claims are invalid and not infringed. The Court has consolidated the two actions and denied
the motion to dismiss the first action without prejudice.
In July 2015, the Company filed with the United States Patent and Trademark Office (“USPTO”) a Petition for Inter Partes Review of
each of the patents in suit seeking to reject as invalid all claims of the patents in suit. The USPTO has issued a decision denying
initiation of the Inter Partes Review.
A court-ordered mediation before a magistrate judge was conducted in April 2016. The mediation did not result in a resolution of this
matter.
Thalomid®
The Company filed with the Food and Drug Administration an ANDA No. 206601, along with a paragraph IV certification, alleging
that the fifteen patents associated with the Thalomid drug product (U.S. Patent Nos. 6,045,501; 6,315,720; 6,561,976; 6,561,977;
6,755,784; 6,869,399; 6,908,432; 7,141,018; 7,230,012; 7,435,745; 7,874,984; 7,959,566; 8,204,763; 8,315,886; 8,589,188 and
8,626,53) are invalid, unenforceable and/or not infringed. On January 30, 2015, Celgene Corporation and Children’s Medical Center
Corporation filed a patent infringement lawsuit in the United States District Court for the District of New Jersey, alleging that the
Company’s filing of ANDA No. 206601 constitutes an act of patent infringement and seeking a declaration that the patents at issue are
valid and infringed. The Company filed an answer and affirmative defenses to the complaint.
AWP Litigation
The Company and some of our competitors have been named as defendants in two lawsuits filed in 2016 alleging that the Company
and a number of other generic pharmaceutical manufacturers caused the Average Wholesale Prices (AWPs) of our and their products
to be inflated, thereby injuring government programs, entities and persons who reimbursed prescription drugs based on AWPs. The
Company stopped using AWP as a basis for establishing prices in or around 2002 and the bulk of prescription drugs manufactured by
the Company was sold under private label and dispute the allegations set forth in these lawsuits. The Company does not believe that
the ultimate resolution of these lawsuits will have a significant impact on our financial position, results of operations or cash flows.
Private Antitrust and Consumer Protection Litigation
The Company and certain competitors have been named as defendants in 19 lawsuits filed in 2016 alleging that the Company and
certain generic pharmaceutical manufacturers have conspired to fix prices of generic digoxin and doxycycline. There is a proceeding
before the United States Judicial Panel on Multidistrict Litigation, regarding centralization of all of these related cases. Oral argument
was held on July 28, 2016. The Panel has not yet made a decision. The Company believes that it acted in compliance with all
applicable laws and regulations. Accordingly, the Company disputes the allegations set forth in these class actions. The Company
does not believe that the ultimate resolution of these lawsuits will have a significant impact on our financial position, results of
operations or cash flows.
Other Litigation Matters
The Company is also subject to various legal proceedings arising out of the normal course of its business including, but not limited to,
product liability, intellectual property, patent infringement claims and antitrust matters. It is not possible to predict the outcome of
these various proceedings. An adverse determination in any of these proceedings in the future could have a significant impact on the
financial position, results of operations and cash flows of the Company.
The Company has responded to the complaint by filing a motion challenging personal jurisdiction. The court has decided to allow
limited discovery on the issue of personal jurisdiction and has administratively terminated the motion while discovery is taken on the
issue.
Note 13. Commitments and Contingencies
Leases
Dilaudid®
The Company filed with the Food and Drug Administration an ANDA No. 207108, along with a paragraph IV certification, alleging
that US Patent 6,589,960 associated with the Dilaudid® (hydromorphone oral solution) would not be infringed by the Company’s
proposed hydromorphone oral solution product and/or that the patent is invalid. On August 8, 2015, Purdue Pharmaceutical Products
L.P, Purdue Pharma L.P and Purdue Pharma Technologies Inc. (“Purdue”) filed a patent infringement lawsuit in the United States
District Court for the District of New Jersey, alleging that the Company’s filing of ANDA No. 207108 constitutes an act of patent
infringement and seeking a declaration that the patent at issue was infringed by the submission of ANDA No, 207108. The Company
filed an answer and affirmative defenses to the complaint. The Company and Purdue have reached a settlement in principle and
details are being finalized.
Nexium®
KUPI was sued on December 5, 2013, by AstraZeneca AB, Aktiebolaget Hassle, AstraZeneca LP, KBI Inc. and KBI-E Inc., alleging
infringement of U.S. Patent Nos. 5,714,504, 6,369,085, 7,411,070 and 8,466,175 through submission of an ANDA to the U.S. Food
and Drug Administration for approval to market 20 mg and 40 mg esomeprazole magnesium delayed-release tablets. On May 2016,
the Company and AstraZeneca settled all claims related to this case.
Although the Company cannot currently predict the length or outcome of paragraph IV litigation, legal expenses associated with these
lawsuits could have a significant impact on the financial position, results of operations and cash flows of the Company.
Texas Medicare Litigation
In August 2015, KUPI received a letter from the Texas Office of the Attorney General alleging that they had inaccurately reported
certain price information in violation of the Texas Medicaid Fraud Prevention Act. UCB, KUPI’s previous parent company is handling
the defense and is evaluating the allegations and cooperating with the Texas Attorney General’s Office. Per the terms of the Stock
Purchase Agreement the Company is fully indemnified for any losses associated with this matter. In conjunction with information
received from UCB’s legal counsel, the Company is currently unable to estimate the timing or the outcome of this matter.
The Company leases certain manufacturing and office equipment, in the ordinary course of business. These assets are typically
renewed annually. Rental and lease expense was not material for all periods presented.
Future minimum lease payments under noncancelable operating leases (with initial or remaining lease terms in excess of one year) for
the twelve month periods ending June 30 thereafter are as follows:
(In thousands)
2017
2018
2019
2020
2021
Thereafter
Total
$
Amounts Due
1,578
1,142
1,080
1,080
1,080
6,318
12,278
$
122
123
�Note 14. Accumulated Other Comprehensive Loss
Note 17. Share-based Compensation
The Company’s Accumulated Other Comprehensive Loss was comprised of the following components as of June 30, 2016 and 2015:
(In thousands)
Foreign Currency Translation
Beginning Balance, June 30, 2015
Net (loss) on foreign currency translation (net of tax of $0 and $0)
Reclassifications to net income (net of tax of $0 and $0)
Other comprehensive (loss), net of tax
Ending Balance, June 30, 2016
Total Accumulated Other Comprehensive Loss
Note 15. Earnings Per Common Share
June 30,
2016
June 30,
2015
$
$
(295) $
—
—
—
(295)
(295) $
(54)
(241)
—
(241)
(295)
(295)
A dual presentation of basic and diluted earnings per common share is required on the face of the Company’s Consolidated Statement
of Operations as well as a reconciliation of the computation of basic earnings per common share to diluted earnings per common
share. Basic earnings per common share excludes the dilutive impact of potentially dilutive securities and is computed by dividing net
income (loss) attributable to Lannett Company, Inc. by the weighted average number of common shares outstanding for the
period. Diluted earnings per common share is computed using the treasury stock method and includes the effect of potential dilution
from the exercise of outstanding stock options and a warrant and treats unvested restricted stock as if it were vested. Potentially
dilutive securities have been excluded in the weighted average number of common shares used for the calculation of earnings per
share in periods of net loss because the effect of including such securities would be anti-dilutive. A reconciliation of the Company’s
basic and diluted earnings per common share was as follows:
(In thousands, except share and per share data)
For Fiscal Year Ended June 30,
2015
2014
2016
Net income attributable to Lannett Company, Inc.
$
44,782
$
149,919
$
57,101
Basic weighted average common shares outstanding
Effect of potentially dilutive options and restricted stock awards
Diluted weighted average common shares outstanding
36,442,782
946,663
37,389,445
35,827,167
1,299,950
37,127,117
33,663,589
1,529,787
35,193,376
Earnings per common share attributable to Lannett Company, Inc.:
Basic
Diluted
$
$
1.23
1.20
$
$
4.18
4.04
$
$
1.70
1.62
The number of anti-dilutive shares that have been excluded in the computation of diluted earnings per share for the fiscal years ended
June 30, 2016, 2015 and 2014 were 3.0 million, 83 thousand and 18 thousand, respectively.
Note 16. Warrant
In connection with the KUPI acquisition, Lannett issued to UCB Manufacturing a warrant to purchase up to a total of 2.5 million
shares of Lannett’s common stock (the “Warrant”).
The Warrant has a term of three years (expiring November 25, 2018) and an exercise price of $48.90 per share, subject to customary
adjustments, including for stock splits, dividends and combinations. The Warrant also has a “weighted average” anti-dilution
adjustment provision. The fair value included as part of the total consideration transferred to UCB at the acquisition date was $29.9
million. The fair value assigned to the Warrant was determined using the Black-Scholes valuation model. The Company concluded
that the warrant was indexed to its own stock and therefore the Warrant has been classified as an equity instrument.
At June 30, 2016, the Company had two share-based employee compensation plans (the 2011 Long-Term Incentive Plan “LTIP” and
the 2014 “LTIP”). Together these plans authorized an aggregate total of 4.5 million shares to be issued. The plans have a total of 2.4
million shares available for future issuances.
The Company issues share-based compensation awards with a vesting period ranging up to 3 years and a maximum contractual term
of 10 years. The Company issues new shares of stock when stock options are exercised. As of June 30, 2016, there was $8.0 million
of total unrecognized compensation cost related to non-vested share-based compensation awards. That cost is expected to be
recognized over a weighted average period of 1.6 years.
Stock Options
The Company measures share-based compensation cost for options using the Black-Scholes option pricing model. The following
table presents the weighted average assumptions used to estimate fair values of the stock options granted during the fiscal years ended
June 30, the estimated annual forfeiture rates used to recognize the associated compensation expense and the weighted average fair
value of the options granted:
Risk-free interest rate
Expected volatility
Expected dividend yield
Forfeiture rate
Expected term
Weighted average fair value
June 30,
2016
June 30,
2015
June 30,
2014
1.7%
48.3%
0.0%
6.5%
1.7%
52.1%
0.0%
6.5%
2.1%
62.8%
0.0%
7.5%
5.2 years
26.24
$
5.5 years
17.73
$
5.9 years
8.55
$
Expected volatility is based on the historical volatility of the price of our common shares during the historical period equal to the
expected term of the option. The Company uses historical information to estimate the expected term, which represents the period of
time that options granted are expected to be outstanding. The risk-free rate for the period equal to the expected life of the option is
based on the U.S. Treasury yield curve in effect at the time of grant. The forfeiture rate assumption is the estimated annual rate at
which unvested awards are expected to be forfeited during the vesting period.
This assumption is based on our actual forfeiture rate on historical awards. Periodically, management will assess whether it is
necessary to adjust the estimated rate to reflect changes in actual forfeitures or changes in expectations. Additionally, the expected
dividend yield is equal to zero, as the Company has not historically issued and has no immediate plans to issue, a dividend.
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125
�A stock option roll-forward as of June 30, 2016, 2015 and 2014 and changes during the years then ended, is presented below:
(In thousands, except for weighted average price and life data)
Awards
Price
Weighted-
Average
Exercise
Weighted
Average
Remaining
Contractual
Life (yrs.)
Aggregate
Intrinsic
Value
Outstanding at June 30, 2013
Granted
Exercised
Forfeited, expired or repurchased
Outstanding at June 30, 2014
Granted
Exercised
Forfeited, expired or repurchased
Outstanding at June 30, 2015
Granted
Exercised
Forfeited, expired or repurchased
Outstanding at June 30, 2016
2,319
780
(783)
(111)
2,205
513
(665)
(78)
1,975
58
(254)
(49)
$
1,730
$
5.71
13.90
6.41
6.49
7.84
36.71
6.47
18.33
15.39
59.20
12.62
32.66
16.77
$
$
$
$
$
24,375
33,201
86,983
6,168
19,524
Vested and expected to vest at June 30, 2016
Exercisable at June 30, 2016
1,714
$
1,238 $
16.61
$
12.31 $
19,495
17,462
Restricted Stock
7.2
6.3
6.2
5.6
The Company measures restricted stock compensation costs based on the stock price at the grant date less an estimate for expected
forfeitures. The annual forfeiture rate used to calculate compensation expense was 6.5% for fiscal year ended June 30, 2016, 2015 and
2014.
A summary of restricted stock awards as of June 30, 2016, 2015 and 2014 and changes during the fiscal years then ended, is presented
below:
(In thousands)
Non-vested at June 30, 2013
Granted
Vested
Forfeited
Non-vested at June 30, 2014
Granted
Vested
Forfeited
Non-vested at June 30, 2015
Granted
Vested
Forfeited
Non-vested at June 30, 2016
Employee Stock Purchase Plan
Weighted
Average Grant
-
date Fair Valu
e
Aggregate
Intrinsic Value
Awards
—
269
(252)
(1)
16
103
(14)
(7)
98
147
(66)
(12)
167
$
$
—
24.07
23.45
24.48
34.01
37.97
36.06
36.59
37.83
54.64
47.11
47.67
48.22
$
$
$
10,440
664
3,511
In February 2003, the Company’s stockholders approved an Employee Stock Purchase Plan (“ESPP”). Employees eligible to
participate in the ESPP may purchase shares of the Company’s stock at 85% of the lower of the fair market value of the common stock
on the first day of the calendar quarter, or the last day of the calendar quarter. Under the ESPP, employees can authorize the Company
to withhold up to 10% of their compensation during any quarterly offering period, subject to certain limitations.
The ESPP was implemented on April 1, 2003 and is qualified under Section 423 of the Internal Revenue Code. The Board of
Directors authorized an aggregate total of 1.1 million shares of the Company’s common stock for issuance under the ESPP. During
the fiscal year ended June 30, 2016 and 2015, 47 thousand shares and 12 thousand shares were issued under the ESPP, respectively.
As of June 30, 2016, 485 thousand total cumulative shares have been issued under the ESPP.
The following table presents the allocation of share-based compensation costs recognized in the Consolidated Statements of
Operations by financial statement line item:
(In thousands)
Selling, general and administrative expenses
Research and development expenses
Cost of sales
Total
Tax benefit at statutory rate
Note 18. Employee Benefit Plan
For Fiscal Year Ended June 30,
2015
2016
2014
$
$
$
9,529
760
1,273
11,562
4,220
$
$
$
5,145
523
729
6,397
2,159
$
$
$
7,388
675
963
9,026
3,375
The Company has a 401k defined contribution plan (the “Plan”) covering substantially all employees. Pursuant to the Plan provisions,
the Company is required to make matching contributions equal to 50% of each employee’s contribution, not to exceed 4% of the
employee’s compensation for the Plan year. Contributions to the Plan during the fiscal years ended June 30, 2016, 2015 and 2014
were $1.6 million, $855 thousand and $748 thousand, respectively.
Note 19. Income Taxes
The provision for income taxes consisted of the following for the fiscal years ended June 30:
(In thousands)
Current Income Tax Expense
Federal
State and Local
Total Current Income Tax Expense
Deferred Income Tax Expense (Benefit)
Federal
State and Local
Total Deferred Income Tax Benefit
Total Income Tax Expense
June 30,
2016
June 30,
2015
June 30,
2014
$
$
34,932
1,887
36,819
(17,529)
(1,968)
(19,497)
17,322
$
$
80,124
572
80,696
(5,245)
1,979
(3,266)
77,430
$
$
41,497
4,246
45,743
(11,613)
(1,273)
(12,886)
32,857
A reconciliation of the differences between the effective rates and federal statutory rates was as follows:
Federal income tax at statutory rate
State and local income tax, net
Nondeductible expenses
Foreign rate differential
Income tax credits
Domestic production activity deduction
Change in tax laws
Other
Effective income tax rate
June 30,
2016
June 30,
2015
June 30,
2014
35.0%
(0.1)%
0.8%
0.5%
(3.0)%
(5.2)%
—%
(0.1)%
27.9%
35.0%
0.1%
—%
0.1%
(0.4)%
(1.3)%
0.6%
(0.1)%
34.0%
35.0%
2.2%
0.4%
0.2%
(0.4)%
(0.5)%
—%
(0.4)%
36.5%
126
127
�The principal types of differences between assets and liabilities for financial statement and tax return purposes are accruals, reserves,
impairment of intangibles, accumulated amortization, accumulated depreciation and share-based compensation expense. A deferred
tax asset is recorded for the future benefits created by the timing of accruals and reserves and the application of different amortization
lives for financial statement and tax return purposes. A deferred tax asset valuation allowance is established if it is more likely than
not that the Company will be unable to realize certain of the deferred tax assets. A deferred tax liability is recorded for the future
liability created by different depreciation methods for financial statement and tax return purposes. As of June 30, 2016 and 2015,
temporary differences which give rise to deferred tax assets and liabilities were as follows:
(In thousands)
Deferred tax assets:
Accrued expenses
Share-based compensation expense
Reserve for returns
Reserves for rebates
Reserves for accounts receivable and inventory
Intangible impairment
Federal net operating loss
State net operating loss
Impairment on Cody note receivable
Accumulated amortization on intangible assets
Settlement Liability
Foreign net operating loss
Other
Total deferred tax asset
Valuation allowance
Total deferred tax asset less valuation allowance
Deferred tax liabilities:
Prepaid expenses
Property, plant and equipment
Other
Total deferred tax liability
Net deferred tax asset
June 30,
2016
June 30,
2015
1,636
5,074
14,583
19,235
6,305
3,312
736
1,469
1,941
5,301
7,014
579
901
68,086
(3,927)
64,159
263
11,381
67
11,711
52,448
$
$
98
2,688
6,520
6,648
3,790
4,342
801
—
1,905
8,526
—
421
185
35,924
(2,326)
33,598
115
4,687
31
4,833
28,765
$
$
The Fiscal 2016 deferred tax expense does not equal the change in net deferred tax assets as a result of deferred taxes recorded in
connection with the KUPI acquisition.
On April 10, 2007, the Company entered into a Stock Purchase Agreement to acquire Cody by purchasing all of the remaining shares
of common stock of Cody. As a result of the acquisition, the Company recorded deferred tax assets related to Cody’s federal net
operation loss (NOL) carry-forwards totaling $3.8 million at the date of acquisition with $1.9 million expiring in 2026 and $1.9
million in 2027.
The Company may recognize the tax benefit from an uncertain tax position claimed on a tax return only if it is more likely than not
that the tax position will be sustained on examination by the taxing authorities, based on the technical merits of the position. The tax
benefits recognized in the financial statements from such a position should be measured based on the largest benefit that has a greater
than 50% likelihood of being realized upon ultimate settlement. The authoritative standards issued by the FASB also provide
guidance on de-recognition of income tax assets and liabilities, classification of current and deferred income tax assets and liabilities,
accounting for interest and penalties associated with tax positions and income tax disclosures.
A reconciliation of the beginning and ending amount of gross unrecognized tax benefits (exclusive of interest and penalties) was as
follows:
(In thousands)
Balance at June 30, 2014
Additions for tax positions of the current year
Additions for tax positions of prior years
Reductions for tax positions of prior years
Settlements
Lapse of statute of limitations
Balance at June 30, 2015
Additions for tax positions of the current year
Additions for tax positions of prior years
Additions from acquisitions
Reductions for tax positions of prior years
Settlements
Lapse of statute of limitations
Balance at June 30, 2016
Balance
428
101
305
—
—
(256)
578
742
109
4,858
—
—
(43)
6,244
$
$
$
The cumulative amount of unrecognized tax benefits above that, if recognized, would impact the Company’s tax expense and effective
tax rate is $6.2 million, $578 thousand and $428 thousand for the fiscal years ended June 30, 2016, 2015 and 2014, respectively.
The Company has not recorded any interest and penalties for the period ended June 30, 2016 in the statement of operations and no
cumulative interest and penalties have been recorded either in the Company’s statement of financial position as of June 30, 2016 and
2015. The Company will recognize interest accrued on unrecognized tax benefits in interest expense and any related penalties in
operating expenses. The Company does not believe that the total unrecognized tax benefits will significantly increase or decrease in
the next twelve months.
The Company files income tax returns in the United States federal jurisdiction and various states. The Company’s tax returns for
Fiscal Year 2012 and prior generally are no longer subject to review as such years generally are closed. The Company believes that an
unfavorable resolution for open tax years would not be material to the financial position of the Company.
Note 20. Related Party Transactions
The Company had sales of $3.1 million, $1.9 million and $2.3 million during the fiscal years ended June 30, 2016, 2015 and 2014,
respectively, to a generic distributor, Auburn Pharmaceutical Company (“Auburn”). Jeffrey Farber, Chairman of the Board, is the
owner of Auburn. Accounts receivable includes amounts due from Auburn of $682 thousand and $733 thousand at June 30, 2016 and
2015, respectively.
In the Company’s opinion, the terms of these related party transactions were not more favorable than would have been to a non-related
party.
Note 21. Material Contracts with Suppliers
Jerome Stevens Pharmaceuticals Distribution Agreement:
The Company’s primary finished goods inventory supplier is JSP, in Bohemia, New York. Purchases of finished goods inventory
from JSP accounted for 52%, 68% and 62% of the Company’s inventory purchases in the fiscal year ending June 30, 2016, 2015 and
2014, respectively.
On August 19, 2013, the Company entered into an agreement with JSP to extend its initial contract to continue as the exclusive
distributor in the United States of three JSP products: Butalbital, Aspirin, Caffeine with Codeine Phosphate Capsules USP; Digoxin
Tablets USP; and Levothyroxine Sodium Tablets USP. The amendment to the original agreement extends the initial contract, which
was due to expire on March 22, 2014, for five years through March 2019. In connection with the amendment, the Company issued a
total of 1.5 million shares of the Company’s common stock to JSP and JSP’s designees. In accordance with its policy related to
renewal and extension costs for recognized intangible assets, the Company recorded a $20.1 million expense in cost of sales, which
represents the fair value of the shares on August 19, 2013. If the parties agree to a second five year extension from March 23, 2019 to
March 23, 2024, the Company is required to issue to JSP or its designees an additional 1.5 million shares of the Company’s common
128
129
�stock. Both Lannett and JSP have the right to terminate the contract if one of the parties does not cure a material breach of the
contract within thirty (30) days of notice from the non-breaching party.
During the renewal term of the JSP distribution agreement, the Company is required to use commercially reasonable efforts to
purchase minimum dollar quantities of JSP products. There is no guarantee that the Company will continue to meet the minimum
purchase requirement for Fiscal 2017 and thereafter. If the Company does not meet the minimum purchase requirements, JSP’s sole
remedy is to terminate the JSP Distribution Agreement.
Note 22. Settlement Agreement
On March 7, 2016, the Company entered into a Settlement Agreement Release and Mutual Release (“Settlement Agreement”) with
one of its former customers, pursuant to which Lannett and such customer resolved all disputes between the parties with respect to the
termination of the direct sales business relationship by Lannett on December 31, 2013.
Pursuant to the terms of the Settlement Agreement, Lannett will pay to one of its former customers the following amounts: (a) in
calendar year 2016, $8.0 million in cash; (b) in calendar year 2017, at the discretion of the customer, either $8.0 million in cash or a
$10.0 million credit memorandum to be applied against invoices for the purchase of products from Lannett or any of its subsidiaries
by such customer; and (c) in calendar year 2018, at the discretion of the customer, either $10.0 million in cash or a $12.0 million credit
memorandum to be applied against invoices for the purchase of products from Lannett or any of its subsidiaries by such customer.
As a result of the Settlement Agreement, the Company recorded a $23.6 million charge to the Consolidated Statement of Operations,
which represents the present value of the required payments. At June 30, 2016, the Company had a settlement liability of $19.5
million recorded on the Consolidated Balance Sheet, of which $7.0 million is due over the next twelve months.
Note 23. Quarterly Financial Information (Unaudited)
Lannett’s quarterly consolidated results of operations are shown below:
(In thousands, except per share data)
Fiscal 2016
Net sales
Settlement agreement
Total net sales
Cost of sales
Gross profit
Operating expenses
Operating income
Other loss
Income tax expense (benefit)
Less: Net income attributable to noncontrolling interest
Net income (loss) attributable to Lannett Company, Inc.
Earnings per common share attributable to Lannett Company Inc. (1)
Basic
Diluted
(In thousands, except per share data)
Fiscal 2015
Net sales
Cost of sales
Gross profit
Operating expenses
Operating income
Other income (loss)
Income tax expense
Less: Net income attributable to noncontrolling interest
Net income attributable to Lannett Company, Inc.
Earnings per common share attributable to Lannett Company Inc. (1)
Basic
Diluted
Fourth
Quarter
Third
Quarter
Second
Quarter
First
Quarter
$
$
$
$
168,887
—
168,887
88,957
79,930
49,535
30,395
(29,752)
(2,948)
20
3,571
$ 163,712 $
(23,598)
140,114
82,623
57,491
38,874
18,617
(26,830)
(2,743)
20
(5,490) $
$
127,059 $
—
127,059
55,414
71,645
41,320
30,325
(10,827)
5,958
20
13,520 $
106,433
—
106,433
29,006
77,427
26,006
51,421
(1,170)
17,055
15
33,181
0.10
0.10
$
$
(0.15) $
(0.15) $
0.37 $
$
0.36
0.91
0.89
Fourth
Quarter
Third
Quarter
Second
Quarter
First
Quarter
$
$
$
$
99,276 $
27,326
71,950
20,932
51,018
165
17,222
18
33,943 $
99,352 $
23,714
75,638
21,363
54,275
(42)
17,973
27
36,233 $
114,822
27,621
87,201
20,658
66,543
713
22,435
10
44,811
0.94 $
0.91 $
1.01 $
$
0.97
1.26
1.21
$
$
$
$
93,387
21,820
71,567
16,916
54,651
99
19,800
18
34,932
0.98
0.94
(In thousands, except per share data)
Fiscal 2014
Net sales
Cost of sales
Gross profit
Operating expenses
Operating income (loss)
Other income
Income tax expense (benefit)
Less: Net income attributable to noncontrolling interest
Net income (loss) attributable to Lannett Company, Inc.
Earnings (loss) per common share attributable to Lannett Company Inc. (1)
Basic
Diluted
Fourth
Quarter
Third
Quarter
Second
Quarter
First
Quarter
$
$
$
$
80,619 $
24,691
55,928
18,577
37,351
220
14,019
17
23,535 $
79,997 $
23,865
56,132
20,143
35,989
297
13,280
11
22,995 $
67,326 $
26,284
41,042
15,675
25,367
1,025
9,800
26
16,566 $
45,829
44,523
1,306
11,924
(10,618)
389
(4,242)
8
(5,995)
0.66 $
0.64 $
0.66 $
0.63 $
0.48 $
0.46 $
(0.20)
(0.20)
130
131
�(1) Due to differences in weighted average common shares outstanding, quarterly earnings per share may not add up to the totals
reported for the full fiscal year.
The decline in operating income in the third and fourth quarters of Fiscal 2016 is primarily attributable to a $23.6 million settlement
agreement and $8.0 million intangible assets impairment charge, respectively. Net income attributable to Lannett Company, Inc. in
the fourth quarter of Fiscal 2016 also included a $3.0 million loss on extinguishment of debt.
The decrease in the effective tax rate in the fourth quarter of Fiscal 2016 is primarily due to state deferred tax benefits recorded as a
result of the KUPI acquisition. In addition, research and development tax credits and domestic manufacturing deductions relative to
pre-tax income also contributed to the lower rate.
The decline in net sales from the second quarter of Fiscal 2015 to the third quarter of Fiscal 2015 was due to lower volumes and
increased competition in cardiovascular products.
Gross margin percentage improved during Fiscal 2014 as a result of favorable pricing trends, specifically on products within the
thyroid and cardiovascular medical indications.
On August 19, 2013, the Company entered into an agreement with JSP to extend its initial contract to continue as the exclusive
distributor in the United States of three JSP products: Butalbital, Aspirin, Caffeine with Codeine Phosphate Capsules USP; Digoxin
Tablets USP; and Levothyroxine Sodium Tablets USP. The amendment to the original agreement extends the initial contract, which
was due to expire on March 22, 2014, for five years. In connection with the amendment, the Company issued a total of 1.5 million
shares of the Company’s common stock to JSP and its designees. In accordance with its policy related to renewal and extension costs
for recognized intangible assets, the Company recorded a $20.1 million expense in cost of sales, which represents the fair value of the
shares on August 19, 2013.
The following list identifies the subsidiaries of the Company:
Subsidiaries of the Company
Subsidiary Name
State of Incorporation
Lannett Holdings, Inc.
Cody Laboratories, Inc.
Silarx Pharmaceuticals, Inc.
Kremers Urban Pharmaceuticals, Inc..
Delaware
Wyoming
New York
Indiana
Exhibit 21
132
�CONSENT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM
We have issued our reports dated August 29, 2016, with respect to the consolidated financial statements, schedule and internal control
over financial reporting included in the Annual Report of Lannett Company, Inc. and Subsidiaries on Form 10-K for the fiscal year
ended June 30, 2016. We consent to the incorporation by reference of said reports in the Registration Statements of Lannett
Company, Inc. and Subsidiaries on Form S-3 (File No. 333-184721) and on Forms S-8 (File No. 333-103235, File No. 333-103236,
File No. 333-147410, File No. 333-172304 and File No. 333-193509).
CERTIFICATION PURSUANT TO
18 U.S.C. SECTION 1350,
AS ADOPTED PURSUANT TO
SECTION 302 OF THE SARBANES-OXLEY ACT OF 2002
I, Arthur P. Bedrosian, certify that:
1.
I have reviewed this report on Form 10-K of Lannett Company, Inc.;
Exhibit 23.1
Exhibit 31.1
/s/ Grant Thornton LLP
Philadelphia, Pennsylvania
August 29, 2016
2. Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact
necessary to make the statements made, in light of the circumstances under which such statements were made, not misleading
with respect to the period covered by this report;
3. Based on my knowledge, the financial statements and other financial information included in this report, fairly present in all
material respects the financial condition, results of operations and cash flows of the registrant as of and for, the periods
presented in this report;
4. The registrant’s other certifying officer and I are responsible for establishing and maintaining disclosure controls and
procedures (as defined in Exchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as
defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the registrant and have:
(a) Designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be
designed under our supervision, to ensure that material information relating to the registrant, including its
consolidated subsidiaries, is made known to us by others within those entities, particularly during the period in
which this report is being prepared;
(b) Designed such internal control over financial reporting, or caused such internal control over financial reporting to
be designed under our supervision, to provide reasonable assurance regarding the reliability of financial reporting
and the preparation of financial statements for external purposes in accordance with generally accepted accounting
principles;
(c) Evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our
conclusions about the effectiveness of the disclosure controls and procedures, as of the end of the period covered
by this report based on such evaluation; and
(d) Disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during
the registrant’s most recent fiscal quarter (the registrant’s fourth fiscal quarter in the case of an annual report) that
has materially affected, or is reasonably likely to materially affect, the registrant’s internal control over financial
reporting; and
5. The registrant’s other certifying officer and I have disclosed, based on our most recent evaluation of internal control over
financial reporting, to the registrant’s auditors and the audit committee of the registrant’s board of directors (or persons
performing the equivalent functions):
(a) All significant deficiencies and material weaknesses in the design or operation of internal control over financial
reporting which are reasonably likely to adversely affect the registrant’s ability to record, process, summarize and
report financial information; and
(b) Any fraud, whether or not material, that involves management or other employees who have a significant role in
the registrant’s internal control over financial reporting.
Date: August 29, 2016
/s/ Arthur P. Bedrosian
Chief Executive Officer
�Exhibit 31.2
Exhibit 32
Certification Pursuant to
18 U.S.C. Section 1350,
as Adopted Pursuant to
Section 906 of the Sarbanes-Oxley Act of 2002
In connection with the Annual Report of Lannett Company, Inc. (the “Company”) on Form 10-K for the year ended June 30, 2016 as
filed with the Securities and Exchange Commission on the date hereof (the “Report”), I, Arthur P. Bedrosian, the Chief Executive
Officer of the Company and I, Martin P. Galvan, the Vice President of Finance, Chief Financial Officer and Treasurer of the
Company, hereby certify, pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of the Sarbanes-Oxley Act of 2002,
that:
1.
2.
The Report complies with the requirements of Section13(a) or 15(d) of the Securities Exchange Act of 1934; and
The information contained in the Report fairly presents, in all material respects, the financial condition and results of
operations of the Company.
Dated: August 29, 2016
Dated: August 29, 2016
/s/ Arthur P. Bedrosian
Arthur P. Bedrosian,
Chief Executive Officer
/s/ Martin P. Galvan
Martin P. Galvan,
Vice President of Finance,
Chief Financial Officer and Treasurer
CERTIFICATION PURSUANT TO
18 U.S.C. SECTION 1350,
AS ADOPTED PURSUANT TO
SECTION 302 OF THE SARBANES-OXLEY ACT OF 2002
I, Martin P. Galvan, certify that:
1.
I have reviewed this report on Form 10-K of Lannett Company, Inc.;
2. Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact
necessary to make the statements made, in light of the circumstances under which such statements were made, not misleading
with respect to the period covered by this report;
3. Based on my knowledge, the financial statements and other financial information included in this report, fairly present in all
material respects the financial condition, results of operations and cash flows of the registrant as of and for, the periods
presented in this report;
4. The registrant’s other certifying officer and I are responsible for establishing and maintaining disclosure controls and
procedures (as defined in Exchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as
defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the registrant and have:
(a) Designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be designed
under our supervision, to ensure that material information relating to the registrant, including its consolidated
subsidiaries, is made known to us by others within those entities, particularly during the period in which this report
is being prepared;
(b) Designed such internal control over financial reporting, or caused such internal control over financial reporting to be
designed under our supervision, to provide reasonable assurance regarding the reliability of financial reporting and
the preparation of financial statements for external purposes in accordance with generally accepted accounting
principles;
(c) Evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our
conclusions about the effectiveness of the disclosure controls and procedures, as of the end of the period covered by
this report based on such evaluation; and
(d) Disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during
the registrant’s most recent fiscal quarter (the registrant’s fourth fiscal quarter in the case of an annual report) that
has materially affected, or is reasonably likely to materially affect, the registrant’s internal control over financial
reporting; and
5. The registrant’s other certifying officer and I have disclosed, based on our most recent evaluation of internal control over
financial reporting, to the registrant’s auditors and the audit committee of the registrant’s board of directors (or persons
performing the equivalent functions):
(a) All significant deficiencies and material weaknesses in the design or operation of internal control over financial
reporting which are reasonably likely to adversely affect the registrant’s ability to record, process, summarize and
report financial information; and
(b) Any fraud, whether or not material, that involves management or other employees who have a significant role in the
registrant’s internal control over financial reporting.
Date: August 29, 2016
/s/ Martin P. Galvan
Vice President of Finance, Chief Financial Officer and Treasurer
�BOARD OF DIRECTORS
CORPORATE INFORMATION
Jeffrey Farber
Chairman of the Board
President, Auburn Pharmaceutical
Arthur P. Bedrosian, J.D.
Chief Executive Officer and Director,
Lannett Company, lnc.
David Drabik
President, Cranbrook & Co., LLC
Paul Taveira
Chief Executive Officer, National
Response Corporation
James M. Maher
Retired Partner
PricewaterhouseCoopers, LLP
Albert Paonessa, III
Retired President
Anda, Inc.
MANAGEMENT TEAM
Arthur P. Bedrosian, J.D.
Chief Executive Officer and Director
Kevin R. Smith
Senior Vice President of Sales and
Marketing
Martin P. Galvan
Vice President of Finance, Chief Financial Officer,
and Treasurer
Robert Ehlinger
Vice President of Logistics and Chief Information
Officer
John M. Abt
Vice President of Quality
Corporate Headquarters
9000 State Road
Philadelphia, PA 19136
(215) 333-9000
lndependent Registered Public Accounting Firm
Grant Thornton LLP
2001 Market Street
Two Commerce Square, Suite 3100
Philadelphia, PA 19103
Legal Counsel
Fox Rothschild LLP
2000 Market Street, 20th Floor
Philadelphia, PA 19103
lnvestor Relations
Robert Jaffe Co., LLC
144 South Elm Drive, Suite #4
Beverly Hills, CA 90212
(424) 288-4098
Computershare Trust Company, N.A.
P.O. Box 30170
College Station, TX 77842
(800) 522-6645
Securities Listing
The common stock of Lannett Company, lnc. is
traded on the New York Stock Exchange.
Annual Report on Form 10-K
Additional copies of this Annual Report on
Form 10-K may be obtained without charge and the
exhibits to the Form 10-K may be obtained for a
nominal fee by writing to:
Lannett Company, lnc.
lnvestor Relations
9000 State Road
Philadelphia, PA 19136
(This page has been left blank intentionally.)
�2OCT200908064695
Lannett Company, Inc.
9000 State Road
Philadelphia, PA 19136
P: (215)333-9000
F: (215)333-9004
www.lannett.com
�