10-K 1 v227306_10k.htm FORM 10-K
UNITED STATES
SECURITIES AND EXCHANGE COMMISSION
Washington, D.C. 20549
FORM 10-K
(MARK ONE)
x
¨
ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
FOR THE FISCAL YEAR ENDED – MARCH 31, 2011
TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
FOR THE TRANSITION PERIOD FROM __________ TO __________
Commission File Number: 001 – 15697
ELITE PHARMACEUTICALS, INC.
(Exact name of registrant as specified in its charter)
Delaware
22-3542636
(State or other jurisdiction of incorporation)
(IRS Employer Identification No.)
165 Ludlow Avenue, Northvale, New Jersey 07647
(Address of principal executive offices)
(201) 750 – 2646
(Registrant’s telephone number, including area code)
Securities Registered pursuant to Section 12(b) of the Act:
Title of Each Class
None
Name of Exchange on Which Registered
~
Securities Registered pursuant to Section 12(g) of the Act:
Common Stock, $0.001 par value
�Indicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act
Indicate by check mark if the registrant is not required to file reports pursuant to Section 13 or 15(d) of the Act
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 registrant was required
to file such reports) and (2) has been subject to such filing requirements for at least the past 90 days.
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 ST (§ 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). The registrant is not yet subject to this requirement.
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.
Yes ¨
Yes ¨
No x
No x
Yes x
No ¨
Yes ¨
No x
Yes ¨
No ¨
Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, or a smaller reporting company. See definition of “large
accelerated filer”, “accelerated filer” and smaller reporting company” in Rule 12b2 of the Exchange Act. (Check one):
Large Accelerated Filer
¨
Accelerated Filer
¨
Non-Accelerated Filer
¨
Smaller Reporting Company
x
Indicate by check mark whether the registrant is a shell company (as defined in Rule 12b-2 of the Act).
Yes ¨ No x
State the aggregate market value of the voting common equity held by non-affiliates computed by reference to the price at which the common equity
was last sold as of the last business day of the registrant’s most recently completed second fiscal quarter (for purposes of determining this amount,
only directors, executive officers and, based on Schedule 13(d) filings as of September 30, 2010, 10% or greater stockholders, and their respective
affiliates, have been deemed affiliates. This determination of affiliate status is not necessarily a conclusive determination for other purposes).
Title of Class
Common Stock - $0.001 par value
Aggregate Market Value
5,559,405
As of Close of Business on
September 30, 2010
Indicate the number of shares outstanding of each of the registrant’s classes of common stock, as of the latest practical date
�Title of Class
Common Stock - $0.001 par value
Shares Outstanding
243,363,531
As of Close of Business on
June 24, 2011
DOCUMENTS INCORPORATED BY REFERENCE
List hereunder the following documents if incorporated by reference and the Part of the Form 10-K (e.g., Part I, Part II, etc.) into which the document
is incorporated: (1) Any annual report to security holders; (2) Any proxy or information statement; and (3) Any prospectus filed pursuant to Rule
424(b) or (c) under the Securities Act of 1933, as amended. The listed documents should be clearly described for identification purposes (e.g., annual
report to security holders for fiscal year ended December 24, 1980).
FORWARD LOOKING STATEMENTS
This Annual Report on Form 10K and the documents incorporated herein contain “forwardlooking statements”. Such forwardlooking
statements involve known and unknown risks, uncertainties and other factors which may cause the actual results, performance or achievements of
the Company, or industry results, to be materially different from any future results, performance or achievements expressed or implied by such
forwardlooking statements. Many of these risks and uncertainties are discussed in this report, particularly in the sections titled “Business”,
“Risk Factors” and “Management’s Discussion and Analysis of Financial Conditions and Results of Operations”. When used in this Annual
Report, statements that are not statements of current or historical fact may be deemed to be forwardlooking statements. Without limiting the
foregoing, the words “plan”, “intend”, “may,” “will,” “expect,” “believe”, “could,” “anticipate,” “estimate,” or “continue” or similar
expressions or other variations or comparable terminology are intended to identify such forward-looking statements. Readers are cautioned not to
place undue reliance on these forwardlooking statements, which speak only as of the date hereof. Except as required by law, the Company
undertakes no obligation to update any forward-looking statements, whether as a result of new information, future events or otherwise.
Any reference to “Elite”, the “Company”, “we”, “us”, “our” or the “Registrant” means Elite Pharmaceuticals Inc. and its subsidiaries.
�Table of Contents
PART I
ITEM 1
BUSINESS
ITEM 1A.
RISK FACTORS
ITEM 1B. UNRESOLVED STAFF COMMENTS
ITEM 2.
PROPERTIES
ITEM 3.
LEGAL PROCEEDINGS
ITEM 4.
REMOVED AND RESERVED
PART II
ITEM 5.
MARKET FOR COMPANY’S COMMON EQUITY AND RELATED STOCKHOLDER MATTERS
ITEM 6
SELECTED FINANCIAL DATA
ITEM 7.
MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATION
ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK
ITEM 8.
FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA
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55
ITEM 9.
CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE 55
ITEM 9A.
CONTROLS AND PROCEDURES
ITEM 9B. OTHER INFORMATION
PART III
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 ACCOUNTING FEES AND SERVICES
PART IV
ITEM 15.
EXHIBITS, FINANCIAL STATEMENTS AND SCHEDULES
SIGNATURES
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�ITEM 1
BUSINESS
General
PART I
Elite Pharmaceuticals, Inc. (“Elite Pharmaceuticals”) was incorporated on October 1, 1997 under the laws of the State of Delaware, and its
whollyowned subsidiaries, Elite Laboratories, Inc. (“Elite Labs”) and Elite Research, Inc. (“Elite Research”), were incorporated on August 23,
1990 and December 20, 2002, respectively, under the laws of the State of Delaware.
On October 24, 1997, Elite Pharmaceuticals merged with and into our predecessor company, Prologica International, Inc. (“Prologica”), an inactive
publicly held Pennsylvania corporation. At the same time, Elite Labs merged with a whollyowned subsidiary of Prologica. Following these
mergers, Elite Pharmaceuticals survived as the parent to its wholly-owned subsidiary, Elite Labs.
On September 30, 2002, pursuant to a termination agreement, dated as of September 30, 2002 (the “Elan Termination Agreement”), between us and
Elan Corporation, plc and Elan International Services, Ltd. (together “Elan”), we acquired from Elan its 19.9% interest in Elite Research, Ltd.
( “ERL”), a joint venture formed between Elite and Elan in which our initial interest was 80.1% of the outstanding capital stock (100% of the
outstanding common stock). As a result of the termination of the joint venture, we owned 100% of ERL’s capital stock. On December 31, 2002,
ERL (a Bermuda Corporation) was merged into Elite Research, our wholly-owned subsidiary.
The address of our principal executive offices and our telephone and facsimile numbers at that address are:
Elite Pharmaceuticals, Inc.
165 Ludlow Avenue
Northvale, New Jersey 07647
Phone No.: (201) 750-2646
Facsimile No.: (201) 750-2755.
We file registration statements, periodic and current reports, proxy statements and other materials with the Securities and Exchange Commission (the
“ SEC”). You may read and copy any materials we file with the SEC at the SEC’s Public Reference Room at 100 F Street, N.W., Washington, DC
20549, on official business days during the hours of 10:00 am to 3:00 pm. You may obtain information on the operation of the Public Reference
Room by calling the SEC at 1-800-SEC-0330. The SEC maintains a web site at www.sec.gov that contains reports, proxy and information
statements and other information regarding issuers, such as us, that file electronically with the SEC. You may also visit our website at
www.elitepharma.com for information regarding the Company including information relating to our SEC filings.
Business Overview and Strategy
We are a specialty pharmaceutical company principally engaged in the development and manufacture of oral, controlled-release products, using
proprietary technology and the development and manufacture of generic pharmaceuticals. Our strategy includes improving off-patent drug products for
life cycle management and developing generic versions of controlled-release drug products with high barriers to entry. Our technology is applicable to
develop delayed-, sustained- or targeted-release pellets, capsules, tablets, granules and powders.
5
�We have one product, Phentermine 37.5mg tablets, currently being sold commercially.
During the fiscal years ended March 31, 2011 (“Fiscal 2011”) and March 31, 2010 (“Fiscal 2010”), the Company manufactured and sold Lodrane
24® and Lodrane 24D® (the “Lodrane Products”). On March 3, 2011, the U.S. Food and Drug Administration (“USFDA”) announced its
intention to remove approximately 500 cough/cold and allergy related products from the U.S. market. The Lodrane Products were included in the
FDA list of 500 products. After this announcement by the USFDA, the Company’s customer for the Lodrane Products cancelled all outstanding
orders and manufacturing of the Lodrane Products has ceased. A Current Report on Form 8K was filed with the SEC on March 4, 2011 in relation
to this announcement by the US-FDA, such filing being herein incorporated by reference.
The Lodrane Products were responsible for 97% and 100% of the Company’s revenues for Fiscal 2011 and Fiscal 2010, respectively.
ECR (the owner and marketer of the Lodrane Products) has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products
and issued a press release on March 3, 2011 stating that they will continue to actively pursue approval for the Lodrane products. In addition, on
April 29, 2011, ECR filed a Petition for Review with the United States Court of Appeals for the District of Columbia, petitioning such court to
review and set aside the final order of the US-FDA with relation to the Lodrane Products.
Elite also purchased from Mikah Pharma LLC, an approved Abbreviated New Drug Applications (“ANDAs”) for Hydromorphone 8 mg and
Naltrexone 50mg tablets. Transfer of production of this product from the previous ANDA holder, Mikah Pharma to our manufacturing facilities is
currently in process. Elite also completed a contract manufacturing agreement with Mikah Pharma for two generic products: Isradipine Capsules USP,
2.5 mg and 5 mg and Phendimetrazine Tartrate Tablets USP, 35 mg and with ThePharmaNetwork for methadone 10 mg.
The Company has a pipeline of additional generic drug candidates under active development, including, without limitation, ELI-216, an abuse
resistant oxycodone product, and ELI-154, a once-a-day oxycodone product.
Elite’s facility in Northvale, New Jersey (the “Facility”) operates under Good Manufacturing Practice (“GMP”) and is a United States Drug
Enforcement Agency (“DEA”) registered facility for research, development and manufacturing.
Strategy
Elite is focusing its efforts on the following areas: (i) development of Elite’s pain management products, (ii) manufacturing of a line of generic
pharmaceutical products with approved ANDA’s; (iii) development of additional generic pharmaceutical products ; (iv) the development of the other
products in our pipeline including the products pursuant to the Epic Strategic Alliance Agreement and other partners; (v) commercial exploitation of
our products either by license and the collection of royalties, or through the manufacture of our formulations, and (vi) development of new products
and the expansion of our licensing agreements with other pharmaceutical companies, including co-development projects, joint ventures and other
collaborations.
Elite is focusing on the development of various types of drug products, including branded drug products which require new drug applications
( “NDAs”) under Section 505(b)(1) or 505(b)(2) of the Drug Price Competition and Patent Term Restoration Act of 1984 (the “Drug Price
Competition Act”) as well as generic drug products which require abbreviated new drug applications (“ANDAs”).
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�Elite believes that its business strategy enables it to reduce its risk by having a diverse product portfolio that includes both branded and generic
products in various therapeutic categories and to build collaborations and establish licensing agreements with companies with greater resources
thereby allowing us to share costs of development and improve cash-flow.
Elite’s Purchase of a Generic Hydromorphone HCl Product
On May 18, 2010, Elite executed an asset purchase agreement with Mikah Pharma LLC (“Mikah”) (the “Hydromorphone Agreement”). Pursuant to
the Hydromorphone Agreement, the Company acquired from Mikah an Abbreviated New Drug Application for Hydromorphone Hydrochloride
Tablets USP, 8 mg (“Hydromorphone 8mg”), for aggregate consideration of $225,000, comprised of an initial payment of $150,000, which was
made on May 18, 2010. A second payment of $75,000 was due to be paid to Mikah on June 15, 2010, with the Company having the option to
make this payment in cash or by issuing to Mikah 937,500 shares of the Company’s common stock. The Company elected and did issue 937,500
shares of Common Stock during the quarter ended December 31, 2010, in full payment of the $75,000 due to Mikah pursuant to the asset purchase
agreement dated May 18, 2010. A current report on form 8K was filed on May 24, 2010 in relation to this announcement, such filing being
incorporated herein by this reference.
For further details on the Hydromorphone Agreement, please refer to Exhibit 10.4 to the Quarterly Report on Form 10-Q, filed with the SEC on
November 15, 2010, and incorporated herein by reference.
On May 31, 2011, the Company received a letter from the US Food and Drug Administration (FDA) responding to a Changes Being Effected in 30
Days (“CBE 30”) supplement filed by the Company with the agency to change the manufacturing and packaging location of the Hydromorphone
Hydrochloride Tablets USP, 8 mg ANDA purchased from Mikah Pharma. The letter from the FDA informed the Company that the agency has
reclassified the application as a prior approval supplemental application which will delay the commercialization.
A current report on form 8K was filed on June 6, 2011 in relation to this announcement, such filing being incorporated herein by this reference.
As a result of the delay in commercialization resulting from the reclassification of the Company’s application, the Company recorded an impairment
of the ANDA asset acquired from Mikah Pharma pursuant to the Hydromorphone Agreement in an amount equal to the entire purchase price of the
acquisition.
This product is included in the license and manufacturing agreements executed with Precision Dose Inc (“Precision Dose”) and its wholly owned
subsidiary, TAGI Pharma Inc (“TAGI”) and dated September 10, 2010. A current report on form 8K was filed on September 16, 2010, in relation
to the signing of this agreement, such filing being herein incorporated by reference.
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�Elite’s Purchase of a Generic Naltrexone Product
On August 27, 2010, Elite executed an asset purchase with Mikah (the “Naltrexone Agreement”). Pursuant to the Naltrexone Agreement, Elite
acquired from Mikah the Abbreviated New Drug Application number 75-274 (Naltrexone Hydrochloride Tablets USP, 50 mg), and all amendments
thereto (the “ANDA”), that have to date been filed with the FDA seeking authorization and approval to manufacture, package, ship and sell the
products described in the ANDA within the United States and its territories (including Puerto Rico) for aggregate consideration of $200,000. In lieu
of cash, Mikah agreed to accept from Elite product development services to be performed by Elite. A current report on form 8K was filed on August
27, 2010 in relation to this announcement, such filing being incorporated herein by this reference. Please also refer to exhibit 10.5 of the Quarterly
Report on Form 10-Q filed with SEC on November 15, 2010, such filing being incorporated herein by this reference.
The transfer of production of Naltrexone Hydrochloride Tablets USP, 50mg (“Naltrexone 50mg Tablets”) from Mikah to the Facility is currently in
progress. Similar to Hydromorphone 8 mg, The Company also recorded an impairment of this product, Naltrexone 50 mg, in an amount equal to
the entire purchase price of the acquisition since it could also be affected in the same manner as hydromorphone.
Elite’s Purchase of a Generic Phentermine Product
On September 10, 2010, Elite, together with its subsidiary, Elite Laboratories, Inc., executed a Purchase Agreement (the “Phentermine Purchase
Agreement”) with Epic Pharma LLC (the “Seller”) for the purpose of acquiring from the seller an Abbreviated New Drug Application for a generic
phentermine product (the “Phentermine ANDA”), with such being filed with, but not yet approved by the FDA at the time the Phentermine
Purchase Agreement was executed. On February 4, 2011, the Company announced the approval by the FDA of the Phentermine ANDA. The
acquisition of the Phentermine ANDA closed on March 31, 2011 and Elite paid the full acquisition price of $450,000 from the purchase agreement
with Epic Pharma. Current reports on form 8K were filed on September 10, 2010 and February 4, 2011 in relation to the Phentermine Purchase
Agreement and the Phentermine ANDA, with such filings being incorporated herein by this reference. Please also refer to exhibit 10.7 of the
Quarterly Report on Form 10-Q filed with SEC on November 15, 2010, such filing being incorporated herein by this reference.
This product is being marketed and distributed by Precision Dose Inc (“Precision Dose”) and its wholly owned subsidiary, TAGI Pharma Inc.
(“TAGI”) pursuant license and manufacturing agreements dated September 10, 2010. A current report on form 8K was filed on September 16, 2010
in relation to signing of this agreement, such filing being incorporated herein by this reference
Licensing Agreement with Precision Dose Inc.
On September 10, 2010, Elite Pharmaceuticals Inc. (“Elite”) executed a License Agreement with Precision Dose, Inc. (“Precision Dose”) to market
and sell four Elite generic products, consisting of Hydromorphone, Naltrexone, Phentermine 37.5mg tablets (“Phentermine 37.5mg”) and one
additional generic products for which an ANDA has been filed but not yet approved by the FDA., through its wholly-owned subsidiary, TAGI
Pharma, Inc. in the United States, Puerto Rico and Canada. Precision Dose will have the exclusive right to market the products in the United States
and Puerto Rico and a nonexclusive right to market the products in Canada. Pursuant to the License Agreement, Elite will receive a license fee and
milestone payments. The license fee will be computed as a percentage of the gross profit, as defined in the License Agreement, earned by Precision
Dose as a result of sales of the products. The license fee is payable monthly for the term of the License Agreement. The milestone payments will be
paid in 6 installments. The first installment was paid upon execution of the License Agreement. The remaining installments are to be paid upon
FDA approval and initial shipment of the products to Precision Dose. The term of the License Agreement is 15 years and may be extended for 3
successive terms, each of 5 years. A current report on form 8K was filed on September 10, 2010 in relation to this announcement, such filing being
incorporated herein by this reference. Please also refer to exhibits 10.8 and 10.9 of the Quarterly Report on Form 10Q filed with SEC on November
15, 2010, such filings being incorporated herein by this reference.
8
�Research and Development
During each of the last two fiscal years, we have focused on research and development activities. We spent $1,385,211 for the fiscal year ended
March 31, 2011 (“Fiscal 2011”) and $794,433 for the fiscal year ended March 31, 2010 (“Fiscal 2010”) on research and development activities.
It is our general policy not to disclose products in our development pipeline or the status of such products until a product reaches a stage that we
determine, for competitive reasons, in our discretion, to be appropriate for disclosure and because the disclosure of such information might suggest
the occurrence of future matters or events that may not occur.
Commercial Products
On April 7, 2011, Elite Pharmaceuticals, Inc. announced that the company made the initial shipment of phentermine HCl 37.5 mg tablets to TAGI
Pharma, a wholly owned subsidiary of Precision Dose. This triggered a milestone payment under the License, Manufacturing and Supply
Agreement with Precision Dose. Phentermine tablets are now a commercial product being distributed by our partner, TAGI Pharma.
A Current Report on form 8-K was filed on April 7, 2011 in relation to this announcement, such filing being incorporated herein by this reference.
Contract Manufacturing
Subsequent to March 31, 2011 and prior to the date of filing of this Annual Report on Form 10-K, Elite entered into two separate contractual
relationships for the contract manufacturing by Elite for three different generic products. As these contracts were executed after March 31, 2011, they
had no effect on the results presented in this Annual Report on Form 10-K.
On June 1, 2011, Elite Pharmaceuticals Inc. (“Elite”) executed a Manufacturing and Supply Agreement (the “Agreement”) with Mikah Pharma, LLC
(“Mikah”) to undertake and perform certain services relating to two generic products: Isradipine Capsules USP, 2.5 mg and 5 mg and
Phendimetrazine Tartrate Tablets USP, 35 mg (the “Products”), including (a) developing and preparing the documentation required for the transfer of
the manufacturing process to Elite’s facility and the appropriate regulatory filing for the ANDA, and (b) manufacturing finished dosage forms
appropriate for commercial sale, marketing and distribution in the United States of America, its territories, possessions, and commonwealths in
accordance with the requirements of this Agreement; Elite shall perform, at its sole cost and expense, all Technology Transfer, validation and
qualification services (including: equipment, methods and facility qualification), validation and stability services required by Applicable Laws to
commence manufacturing the Products for commercial sale by Mikah or its designees in accordance with the terms of this Agreement. During the
term of this Agreement and subject to the provisions herein, Mikah shall purchase from Elite and Elite agrees to manufacture and supply solely and
exclusively to Mikah, such Product as Mikah may order from time to time pursuant to this Agreement. Mikah will compensate Elite at an agreed
upon transfer price for the manufacturing and packaging of the Products. For the Isradipine product, Elite will also receive a 10% royalty on net
profits of the finished Product. The payment is to be calculated and paid quarterly. Elite will also receive a onetime milestone payment for each
Product for the work associated with the Technology transfer. The milestone payment shall be made upon the successful manufacturing and testing of
the exhibit batch. The Manufacturing and Supply Agreement has a term of five (5) years and shall automatically renew for additional periods of one
(1) year unless Mikah provides written notice of termination to Elite at least six (6) months prior to the expiration of the Term or any Renewal
Term.
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�Transfer of the manufacturing site to Elite’s Facility is in progress as of the date of filing of this Annual Report on Form 10K.
A Current Report on Form 8-K was filed on June 7, 2011 in relation to this announcement, such filing being herein incorporated by this reference.
On June 29, 2011, Elite Pharmaceuticals, Inc. announced that it entered into a commercial manufacturing and supply agreement with
ThePharmaNetwork, LLC and its wholly owned subsidiary, Ascend Laboratories LLC (together “TPN”). Under the terms of the agreement, Elite
will perform manufacturing and packaging for TPN’s Methadone Hydrochloride, 10mg tablets.
The Company expects to commence commercial contract manufacturing and packaging operations pursuant to this agreement during 2011.
A Current Report on Form 8-K was filed on June 29, 2011 in relation to this announcement, such filing being herein incorporated by this reference.
Manufacturing Site Transfers in Progress
Elite is currently engaged in the transfer of the manufacturing site for the following two generic products for which it purchased approved ANDA’s
during the fiscal year ended March 31, 2011: Hydromorphone 8mg and Naltrexone 50mg tablets.
Please refer to the sections above titled “Elite’s Purchase of a Generic Hydromorphone HCl Product” and “Elite’s Purchase of a Generic Naltrexone
Product” for further details on the transfer of the manufacturing site for Hydromorphone 8mg and Naltrexone 50mg, respectively.
Discontinued Products
Elite manufactured two oncedaily allergy products, Lodrane 24® and Lodrane 24D®, that were codeveloped with our partner, ECR Pharmaceuticals
( “ECR”). Elite entered into development agreements for these two products with ECR in June 2001 whereby Elite agreed to commercially develop
two products in exchange for development fees, certain payments, royalties and manufacturing rights. The products are being marketed by ECR
which also has the responsibility for regulatory matters. In addition to receiving revenues for the manufacture of these products, Elite receives a
royalty on in-market sales.
Lodrane 24®, was first commercially offered in November 2004 and Lodrane 24D® was first commercially offered in December, 2006. Elite’s
revenues for manufacturing these products and a royalty on sales for the years ended March 31, 2011 and 2010 aggregated $3,917,721 and,
$3,339,870, respectively.
Since January, 2010, the Company has performed laboratory stability studies of Lodrane24® and Lodrane 24D®, for ECR, on a contract
basis. Elite’s revenues from such contract laboratory services were $348,242 and $4,429 for Fiscal 2011 and Fiscal 2010, respectively.
10
�On March 3, 2011, the U.S. Food and Drug Administration (“USFDA”) announced its intention to remove approximately 500 cough/cold and
allergy related products from the U.S. market. The Lodrane Products were included in the FDA list of 500 products. After this announcement by the
USFDA, the Company’s customer for the Lodrane Products cancelled all outstanding orders and manufacturing of the Lodrane Products has ceased.
A Current Report on Form 8-K was filed with the SEC on March 4, 2011 in relation to this announcement by the US-FDA, such filing being herein
incorporated by reference.
ECR (the owner and marketer of the Lodrane Products) has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products
and issued a press release on March 3, 2011 stating that they will continue to actively pursue approval for the Lodrane products. In addition, on
April 29, 2011, ECR filed a Petition for Review with the United States Court of Appeals for the District of Columbia, petitioning such court to
review and set aside the final order of the US-FDA with relation to the Lodrane Products.
Products Under Development
ELI-154 and ELI-216
For ELI-154, Elite has developed a once-daily oxycodone formulation using its proprietary technology. An investigational new drug application, or
IND, has been filed and Elite has completed two pharmacokinetic studies in healthy subjects that compared blood levels of oxycodone from dosing
ELI154 and the twiceaday product that is on the market currently, OxyContin® marketed in the U.S. by Purdue Pharma LP. These studies
confirmed that ELI-154, when compared to twice-daily delivery, demonstrated an equivalent onset, more constant blood levels of the drug over the
24 hour period and equivalent blood levels to the twiceaday product at the end of 24 hours. Elite has successfully manufactured multiple batches
on commercial scale equipment and we have discussions ongoing in Europe for the licensing of this product. We are looking for a partner who can
complete the clinical studies required for Europe and who can sell and distribute the product in key European territories.
ELI216 utilizes Elite Pharmaceuticals’ patentpending abusedeterrent technology that is based on a pharmacological approach. ELI216 is a
combination of a narcotic agonist, oxycodone hydrochloride, in a sustained-release formulation intended for use in patients with moderate to severe
chronic pain, and an antagonist, naltrexone hydrochloride, formulated to deter abuse of the drug. Both of these compounds, oxycodone
hydrochloride and naltrexone hydrochloride, have been on the market for a number of years and sold separately in various dose strengths. Elite has
filed an IND for the product and has tested the product in a series of pharmacokinetic studies. In singledose studies for ELI216, it was
demonstrated that no quantifiable blood levels of naltrexone hydrochloride were released at a limit of quantification (“LOQ”) of 7.5 pg/ml. As
described below, when crushed, naltrexone hydrochloride was released at levels that would be expected to eliminate the euphoria from the crushed
oxycodone hydrochloride. This data is consistent with the premise of Elite’s abuse resistant technology, that essentially no naltrexone is released
and absorbed when administered as intended. Products utilizing the pharmacological approach to deter abuse such as Suboxone®, a product
marketed in the United States by Reckitt Benckiser Pharmaceuticals, Inc., and Embeda®, a product marketed in the United States by Pfizer, have
been approved by the FDA.
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�ELI216 demonstrates a euphoriablocking effect when the product is crushed. A study completed in 2007 was designed to determine the optimal
ratio of oxycodone hydrochloride and the opioid antagonist, naltrexone hydrochloride, to significantly block the euphoric effect of the opioid if the
product is abused by physically altering it (i.e., crushing). The study also helped determine the appropriate levels of naltrexone hydrochloride
required to reduce or eliminate the euphoria experienced by subjects who might take crushed product to achieve a “high”.
Elite met with the FDA for a Type C clinical guidance meeting regarding the NDA development program for ELI216. Elite has incorporated the
FDA’s guidance into its developmental plan. Elite has obtained a special protocol assessment, or SPA, with the FDA for the ELI216 Phase III
protocol. Elite will conduct additional Phase I studies including, but not limited to, food effect, ascending dose and multi-dose studies.
Elite has developed ELI154 and ELI216 and retains the rights to these products. Elite has currently chosen to develop these products itself but
expects to license these products at a later date to a third party who could provide funding for the remaining clinical studies, including a Phase III
study, and who could provide sales and distribution for the product. The drug delivery technology underlying ELI-154 was originally developed
under a joint venture with Elan which terminated in 2002.
According to the Elan Termination Agreement, Elite acquired all proprietary, development and commercial rights for the worldwide markets for the
products developed by the joint venture, including ELI-154. Upon licensing or commercialization of ELI-154, Elite will pay a royalty to Elan
pursuant to the Termination Agreement. If Elite were to sell the product itself, Elite would pay a 1% royalty to Elan based on the product’s net
sales, and if Elite enters into an agreement with another party to sell the product, Elite will pay a 9% royalty to Elan based on Elite’s net revenues
from this product. (Elite’s net product revenues would include license fees, royalties, manufacturing profits and milestones) Elite is allowed to recoup
all development costs including research, process development, analytical development, clinical development and regulatory costs before payment of
any royalties to Elan.
Epic Strategic Alliance Agreement
On March 18, 2009, Elite and Epic Pharma, LLC and Epic Investments, LLC, a subsidiary of Epic Pharma LLC (collectively, “Epic”) entered into
the Epic Strategic Alliance Agreement (amended on April 30, 2009, June 1, 2009 and July 28, 2009). Epic is a pharmaceutical company that
operates a business synergistic to that of Elite in the research and development, manufacturing and sales and marketing of oral immediate release and
controlled-release drug products.
Under the Epic Strategic Alliance Agreement (i) at least eight additional generic drug products will be developed by Epic at the Facility with the
intent of filing abbreviated new drug applications for obtaining FDA approval of such generic drugs, (ii) Elite will be entitled to 15% of the profits
generated from the sales of such additional generic drug products upon approval by the FDA, and (iii) Epic and Elite will share certain resources,
technology and know-how in the development of drug products, which Elite believes will benefit the continued development of its current drug
products.
For additional information regarding the Epic Strategic Alliance Agreement, please see our disclosures under “Epic Strategic Alliance Agreement” in
Item 7 of Part II of this Annual Report on Form 10-K, and in our Current Reports on Form 8-K, filed with the SEC on March 23, 2009, May 6,
2009 and June 5, 2009, which are incorporated herein by reference.
12
�Novel Labs Investment
At the end of 2006, Elite entered into a joint venture with VGS Pharma, LLC (“VGS”) and created Novel Laboratories, Inc. (“Novel”), a
privately-held company specializing in pharmaceutical research, development, manufacturing, licensing, acquisition and marketing of specialty
generic pharmaceuticals. Novel's business strategy is to focus on its core strength in identifying and timely executing niche business opportunities in
the generic pharmaceutical area. Elite owns approximately 10% of the outstanding shares of Class A Voting Common Stock of Novel. To date, Elite
has received no distributions or dividends from this investment.
Patents
Since our incorporation, we have secured seven United States patents of which two have been assigned for a fee to another pharmaceutical company.
Elite’s patents are:
PATENT
U.S. patent 5,871,776
U.S. patent 5,902,632
U.S. patent 5,837,284 (assigned to Celgene Corporation)
U.S. patent 6,620,439
U.S. patent 6,635,284 (assigned to Celgene Corporation)
U.S. patent 6,926,909
U.S. patent 6,984,402
EXPIRATION DATE
October 28, 2016
July 31, 2017
November 17, 2018
October 3, 2020
March 11, 2018
April 4, 2023
April 10, 2023
We have pending applications for four additional U.S. patents. The pending patent applications relate to two different controlledrelease
pharmaceutical products on which we are working. Three of these patents are for an opioid agonist and antagonist product that we are developing to
be used with oxycodone and other opioids to minimize the abuse potential for the opioids. Another U.S. patent is for formulation of oral sustained
release opioids intended to improve the delivery of the opioids. We intend to apply for patents for other products in the future; however, there can be
no assurance that any of the pending applications or other applications which we may file will be granted. We have also filed corresponding foreign
applications for key patents.
Prior to the enactment in the United States of new laws adopting certain changes mandated by the General Agreement on Tariffs and Trade
( “GATT”), the exclusive rights afforded by a U.S. Patent were for a period of 17 years measured from the date of grant. Under GAAT, the term of any
U.S. Patent granted on an application filed subsequent to June 8, 1995 terminates 20 years from the date on which the patent application was filed in
the United States or the first priority date, whichever occurs first. Future patents granted on an application filed before June 8, 1995, will have a term
that terminates 20 years from such date, or 17 years from the date of grant, whichever date is later.
Under the Drug Price Competition Act, a U.S. product patent or use patent may be extended for up to five years under certain circumstances to
compensate the patent holder for the time required for FDA regulatory review of the product. Such benefits under the Drug Price Competition Act are
available only to the first approved use of the active ingredient in the drug product and may be applied only to one patent per drug product. There
can be no assurance that we will be able to take advantage of this law.
13
�Also, different countries have different procedures for obtaining patents, and patents issued by different countries provide different degrees of protection
against the use of a patented invention by others. There can be no assurance, therefore, that the issuance to us in one country of a patent covering an
invention will be followed by the issuance in other countries of patents covering the same invention, or that any judicial interpretation of the
validity, enforceability, or scope of the claims in a patent issued in one country will be similar to the judicial interpretation given to a corresponding
patent issued in another country. Furthermore, even if our patents are determined to be valid, enforceable, and broad in scope, there can be no
assurance that competitors will not be able to design around such patents and compete with us using the resulting alternative technology.
We also rely upon unpatented proprietary and trade secret technology that we seek to protect, in part, by confidentiality agreements with our
collaborative partners, employees, consultants, outside scientific collaborators, sponsored researchers, and other advisors. There can be no assurance
that these agreements provide meaningful protection or that they will not be breached, that we will have adequate remedies for any such breach, or
that our trade secrets, proprietary know-how, and technological advances will not otherwise become known to others. In addition, there can be no
assurance that, despite precautions taken by us, others have not and will not obtain access to our proprietary technology.
Trademarks
We currently plan to license our products to other entities engaged in the marketing of pharmaceuticals and not to sell under our own brand name
and so we do not currently intend to register any trademarks related to our products.
Government Regulation and Approval
The design, development and marketing of pharmaceutical compounds, on which our success depends, are intensely regulated by governmental
regulatory agencies, in particular the FDA. Noncompliance with applicable requirements can result in fines and other judicially imposed sanctions,
including product seizures, injunction actions and criminal prosecution based on products or manufacturing practices that violate statutory
requirements. In addition, administrative remedies can involve voluntary withdrawal of products, as well as the refusal of the FDA to approve
ANDAs and NDAs. The FDA also has the authority to withdraw approval of drugs in accordance with statutory due process procedures.
Before a drug may be marketed, it must be approved by the FDA either by an NDA or an ANDA, each of which is discussed below.
Please note that on March 3, 2011, the U.S. Food and Drug Administration (“USFDA”) announced its intention to remove approximately 500
cough/cold and allergy related products from the U.S. market, with such list of 500 products including the Lodrane Products. After this
announcement by the USFDA, the Company’s customer for the Lodrane Products cancelled all outstanding orders and manufacturing of the Lodrane
Products has ceased.
The Lodrane Products were responsible for approximately 97% of the Company’s gross revenues in Fiscal 2011 and while the timing of the
announcement by the USFDA at the end of Fiscal 2011 resulted in such having a minimal effect on the Company’s results for Fiscal 2011, the
announcement has a material adverse effect on revenues for periods beginning after March 31, 2011.
A Current Report on Form 8-K was filed with the SEC on March 4, 2011 in relation to this announcement by the US-FDA, such filing being herein
incorporated by reference.
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�ECR (the owner and marketer of the Lodrane Products) has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products
and issued a press release on March 3, 2011 stating that they will continue to actively pursue approval for the Lodrane products. In addition, on
April 29, 2011, ECR filed a Petition for Review with the United States Court of Appeals for the District of Columbia, petitioning such court to
review and set aside the final order of the US-FDA with relation to the Lodrane Products.
NDAs and NDAs under Section 505(b) of the Drug Price Competition Act
The FDA approval procedure for an NDA is generally a two-step process. During the Initial Product Development stage, an investigational new drug
application (“IND”) for each product is filed with the FDA. A 30day waiting period after the filing of each IND is required by the FDA prior to the
commencement of initial clinical testing. If the FDA does not comment on or question the IND within such 30-day period, initial clinical studies
may begin. If, however, the FDA has comments or questions, they must be answered to the satisfaction of the FDA before initial clinical testing may
begin. In some instances this process could result in substantial delay and expense. Initial clinical studies generally constitute Phase I of the NDA
process and are conducted to demonstrate the product tolerance/safety and pharmacokinetic in healthy subjects.
After Phase I testing, extensive efficacy and safety studies in patients must be conducted. After completion of the required clinical testing, an NDA is
filed, and its approval, which is required for marketing in the United States, involves an extensive review process by the FDA. The NDA itself is a
complicated and detailed application and must include the results of extensive clinical and other testing, the cost of which is substantial. However,
the NDA filings contemplated by us, which are already marketed drugs, would be made under Sections 505 (b)(1) or 505 (b)(2) of the Drug Price
Competition Act, which do not require certain studies that would otherwise be necessary; accordingly, the development timetable should be
shorter. While the FDA is required to review applications within a certain timeframe, during the review process, the FDA frequently requests that
additional information be submitted. The effect of such request and subsequent submission can significantly extend the time for the NDA review
process. Until an NDA is actually approved, there can be no assurance that the information requested and submitted will be considered adequate by
the FDA to justify approval. The packaging and labeling of our developed products are also subject to FDA regulation. It is impossible to anticipate
the amount of time that will be needed to obtain FDA approval to market any product.
Whether or not FDA approval has been obtained, approval of the product by comparable regulatory authorities in any foreign country must be
obtained prior to the commencement of marketing of the product in that country. We intend to conduct all marketing in territories other than the
United States through other pharmaceutical companies based in those countries. The approval procedure varies from country to country, can involve
additional testing, and the time required may differ from that required for FDA approval. Although there are some procedures for unified filings for
certain European countries, in general each country has its own procedures and requirements, many of which are time consuming and expensive.
Thus, there can be substantial delays in obtaining required approvals from both the FDA and foreign regulatory authorities after the relevant
applications are filed. After such approvals are obtained, further delays may be encountered before the products become commercially available.
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�ANDAs
The FDA approval procedure for an ANDA differs from the procedure for a NDA in that the FDA waives the requirement of conducting complete
clinical studies, although it normally requires bioavailability and/or bioequivalence studies. “Bioavailability” indicates the rate and extent of
absorption and levels of concentration of a drug product in the blood stream needed to produce a therapeutic effect. “Bioequivalence” compares the
bioavailability of one drug product with another, and when established, indicates that the rate of absorption and levels of concentration of the active
drug substance in the body are equivalent for the generic drug and the previously approved drug. An ANDA may be submitted for a drug on the basis
that it is the equivalent of a previously approved drug or, in the case of a new dosage form, is suitable for use for the indications specified.
The timing of final FDA approval of an ANDA depends on a variety of factors, including whether the applicant challenges any listed patents for the
drug and whether the brand-name manufacturer is entitled to one or more statutory exclusivity periods, during which the FDA may be prohibited
from accepting applications for, or approving, generic products. In certain circumstances, a regulatory exclusivity period can extend beyond the life of
a patent, and thus block ANDAs from being approved on the patent expiration date.
In May 1992, Congress enacted the Generic Drug Enforcement Act of 1992, which allows the FDA to impose debarment and other penalties on
individuals and companies that commit certain illegal acts relating to the generic drug approval process. In some situations, the Generic Drug
Enforcement Act requires the FDA to not accept or review ANDAs for a period of time from a company or an individual that has committed certain
violations. It also provides for temporary denial of approval of applications during the investigation of certain violations that could lead to debarment
and also, in more limited circumstances, provides for the suspension of the marketing of approved drugs by the affected company. Lastly, the Generic
Drug Enforcement Act allows for civil penalties and withdrawal of previously approved applications. Neither we nor any of our employees have ever
been subject to debarment. We do not believe that we receive any services from any debarred person.
Controlled Substances
We are also subject to federal, state, and local laws of general applicability, such as laws relating to working conditions. We are also licensed by,
registered with, and subject to periodic inspection and regulation by the Drug Enforcement Agency (“DEA”) and New Jersey state agencies, pursuant
to federal and state legislation relating to drugs and narcotics. Certain drugs that we currently develop or may develop in the future may be subject
to regulations under the Controlled Substances Act and related statutes. As we manufacture such products, we may become subject to the
Prescription Drug Marketing Act, which regulates wholesale distributors of prescription drugs.
GMP
All facilities and manufacturing techniques used for the manufacture of products for clinical use or for sale must be operated in conformity with GMP
regulations issued by the FDA. We engage in manufacturing on a commercial basis for distribution of products, and operate our facilities in
accordance with GMP regulations. If we hire another company to perform contract manufacturing for us, we must ensure that our contractor’s facilities
conform to GMP regulations.
Compliance with Environmental Laws
We are subject to comprehensive federal, state and local environmental laws and regulations that govern, among other things, air polluting
emissions, waste water discharges, solid and hazardous waste disposal, and the remediation of contamination associated with current or past
generation handling and disposal activities, including the past practices of corporations as to which we are the legal successor or in possession. We
do not expect that compliance with such environmental laws will have a material effect on our capital expenditures, earnings or competitive position
in the foreseeable future. There can be no assurance, however, that future changes in environmental laws or regulations, administrative actions or
enforcement actions, or remediation obligations arising under environmental laws will not have a material adverse effect on our capital expenditures,
earnings or competitive position.
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�Competition
We have competition with respect to our two principal areas of operation. We develop and manufacture generic products and products using
controlled-release drug technology for other pharmaceutical companies, and we develop and market (either on our own or by license to other
companies) generic and proprietary controlled-release pharmaceutical products. In both areas, our competition consists of those companies which
develop controlledrelease drugs and alternative drug delivery systems. We do not represent a significant presence in the pharmaceutical industry.
An increasing number of pharmaceutical companies have become interested in the development and commercialization of products incorporating
advanced or novel drug delivery systems. We expect that competition in the field of drug delivery will significantly increase in the future since
smaller specialized research and development companies are beginning to concentrate on this aspect of the business. Some of the major
pharmaceutical companies have invested and are continuing to invest significant resources in the development of their own drug delivery systems and
technologies and some have invested funds in such specialized drug delivery companies. Many of these companies have greater financial and other
resources as well as more experience than we do in commercializing pharmaceutical products. Certain companies have a track record of success in
developing controlledrelease drugs. Significant among these are Sandoz (a Novartis company), Durect Corporation, Mylan Laboratories, Inc., Par
Pharmaceuticals, Inc., Alkermes, Inc., Teva Pharmaceuticals Industries Ltd., Aptalis Pharma, Impax Laboratories, Inc., and Watson
Pharmaceuticals. Each of these companies has developed expertise in certain types of drug delivery systems, although such expertise does not carry
over to developing a controlledrelease version of all drugs. Such companies may develop new drug formulations and products or may improve
existing drug formulations and products more efficiently than we can. In addition, almost all of our competitors have vastly greater resources than we
do. While our product development capabilities and, if obtained, patent protection may help us to maintain our market position in the field of
advanced drug delivery, there can be no assurance that others will not be able to develop such capabilities or alternative technologies outside the
scope of our patents, if any, or that even if patent protection is obtained, such patents will not be successfully challenged in the future.
In addition to competitors that are developing products based on drug delivery technologies, there are also companies that have announced that they
are developing opioid abusedeterrent products that might compete directly or indirectly with Elite’s products. These include, but are not limited to
Pfizer Inc., Pain Therapeutics (which has an agreement with Durect Corporation and Pfizer Inc.), Collegium Pharmaceuticals, Inc., Purdue Pharma
LP, and Acura Pharmaceuticals, Inc.
We also face competition in the generic pharmaceutical market. The principal competitive factors in the generic pharmaceutical market include: (i)
introduction of other generic drug manufacturers’ products in direct competition with our products under development, (ii) introduction of authorized
generic products in direct competition with any of our products under development, particularly if such products are approved and sold during
exclusivity periods, (iii) consolidation among distribution outlets through mergers and acquisitions and the formation of buying groups, (iv) ability
of generic competitors to quickly enter the market after the expiration of patents or exclusivity periods, diminishing the amount and duration of
significant profits, (v) the willingness of generic drug customers, including wholesale and retail customers, to switch among pharmaceutical
manufacturers, (vi) pricing pressures and product deletions by competitors, (vii) a company’s reputation as a manufacturer and distributor of quality
products, (viii) a company’s level of service (including maintaining sufficient inventory levels for timely deliveries), (ix) product appearance and
labeling and (x) a company’s breadth of product offerings.
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�Sources and Availability of Raw Materials; Manufacturing
A significant portion of our raw materials may be available only from foreign sources. Foreign sources can be subject to the special risks of doing
business abroad, including:
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greater possibility for disruption due to transportation or communication problems;
the relative instability of some foreign governments and economies;
interim price volatility based on labor unrest, materials or equipment shortages, export duties, restrictions on the transfer of funds, or
fluctuations in currency exchange rates; and
uncertainty regarding recourse to a dependable legal system for the enforcement of contracts and other rights.
Please see the Risk Factor entitled “Even after regulatory approval, we will be subject to ongoing significant regulatory obligations and oversight” at
Item 1A.
While we currently obtain the raw materials that we need from over 20 suppliers, some materials used in our products are currently available from
only one supplier or a limited number of suppliers. The FDA requires identification of raw material suppliers in applications for approval of drug
products. If raw materials were unavailable from a specified supplier, FDA approval of a new supplier could delay the manufacture of the drug
involved.
We have acquired pharmaceutical manufacturing equipment for manufacturing our products. We have registered our facilities with the FDA and the
DEA.
Dependence on One or a Few Major Customers
Each year we have had one or a few customers that have accounted for a large percentage of our limited revenues therefore the termination of a contract
with a customer may result in the loss of substantially all of our revenues. We are constantly working to develop new relationships with existing or
new customers, but despite these efforts we may not, at the time that any of our current contracts expire, have other contracts in place generating
similar or material revenue. We have agreements with ECR and Precision Dose for the sales and distribution of products that we manufacture. We
receive revenues to manufacture these products and also receive a profit split or royalties based on in-market sales of the products.
In April 2011, we ceased production of the Lodrane Products, which are the subject of the agreements with ECR, pursuant to the USFDA’s
announcement of its intention to remove approximately 500 cough/cold and allergy related products from the US market, including the Lodrane
Products. While the announcement by the USFDA had a minimal effect on the Company’s results for Fiscal 2011, the Lodrane Products for which
production has ceased were responsible for 97% of the Company’s revenues. The announcement by the USFDA accordingly has a material adverse
effect on the Company’s revenues for periods beginning after March 31, 2011.
ECR has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products and issued a press release on March 3, 2011
stating that they will continue to actively pursue approval for the Lodrane products. In addition, on April 29, 2011, ECR filed a Petition for Review
with the United States Court of Appeals for the District of Columbia, petitioning such court to review and set aside the final order of the US-FDA
with relation to the Lodrane Products.
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�The agreement with Precision Dose is currently the only commercially active contractual relationship from which the Company generates revenue.
Employees
As of June 15, 2011, we had 17 full time employees. Fulltime employees are engaged in operations, administration, research and
development. None of our employees is represented by a labor union and we have never experienced a work stoppage. We believe our relationship
with our employees to be good. However, our ability to achieve our financial and operational objectives depends in large part upon our continuing
ability to attract, integrate, retain and motivate highly qualified personnel, and upon the continued service of our senior management and key
personnel.
ITEM 1A.
RISK FACTORS
In addition to the other information contained in this report, the following risk factors should be considered carefully in evaluating an investment in
us and in analyzing our forward-looking statements.
RISKS RELATED TO OUR BUSINESS
We have a relatively limited operating history, which makes it difficult to evaluate our future prospects.
Although we have been in operation since 1990, we have a relatively short operating history and limited financial data upon which you may evaluate
our business and prospects. In addition, our business model is likely to continue to evolve as we attempt to expand our product offerings and our
presence in the generic pharmaceutical market. As a result, our potential for future profitability must be considered in light of the risks, uncertainties,
expenses and difficulties frequently encountered by companies that are attempting to move into new markets and continuing to innovate with new
and unproven technologies. Some of these risks relate to our potential inability to:
develop new products;
obtain regulatory approval of our products;
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attract, retain and motivate qualified personnel; and
respond to competitive developments.
If we do not effectively address the risks we face, our business model may become unworkable and we may not achieve or sustain profitability or
successfully develop any products.
We have not been profitable and expect future losses.
To date, we have not been profitable and we may never be profitable or, if we become profitable, we may be unable to sustain profitability. We have
sustained losses in each year since our incorporation in 1990. For the past two years, we incurred net losses of $13,582,159 and $8,056,874,
respectively and losses from operations of $1,936,321 and $445,758, respectively. We expect to continue to incur losses until we are able to generate
sufficient revenues to support our operations and offset operating costs.
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�There is doubt as to our ability to continue as a going concern.
On June 21, 2010, we had cash reserves of approximately $1.8 million. The completion of all transactions contemplated by the Epic Strategic
Alliance Agreement will provide additional funds to permit us to continue development of our product pipeline. We are anticipating that, with the
growth of the generic phentermine product, the contract manufacturing of methadone, Phendimetrazine and Isradipine, the launch of the generic
hydromorphone and naltrexone products and other opportunities in our pipeline, Elite could be profitable. In addition, the commercialization of the
Epic products developed under the Epic Strategic Alliance Agreement will add a new revenue source for Elite. However, there can be no assurances
as to the success of the development of such Epic products or the commercialization of such Epic products or the success or commercialization of
other pipeline products of Elite.
Despite the successful completion of the initial, second and third closings of the Epic Strategic Alliance Agreement, there can be no assurances that
we will be able to consummate quarterly payment closings pursuant to the terms and conditions of the Epic Strategic Alliance Agreement. If such
transactions are consummated, we will receive additional cash proceeds of $0.6875 million. Even if we were able to successfully complete the
quarterly payment closings of the Epic Strategic Alliance Agreement, we still may be required to seek additional capital in the future and there can be
no assurances that we will be able to obtain such additional capital on favorable terms, if at all. For additional information regarding the Epic
Strategic Alliance Agreement, please see our disclosures under “Epic Strategic Alliance Agreement” in Item 7 of Part II of this Annual Report on
Form 10-K, and in our Current Reports on Form 8-K, filed with the SEC on March 23, 2009, May 6, 2009, June 5, 2009 and July 1, 2010, which
are incorporated herein by reference.
If we are unable to obtain additional financing needed for the expenditures for the development and commercialization of our drug
products, it would impair our ability to continue to meet our business objectives.
We continue to require additional financing to ensure that we will be able to meet our expenditures to develop and commercialize our products. As
of June 21, 2011 we had cash and cash equivalents of approximately $1.8 million. Elite must be able to commercialize other products or pipeline
opportunities such as the generic hydromorphone and naltrexone products at that time or we will require additional funding in order to continue to
operate. If the quarterly payment closings of the transactions contemplated by the Epic Strategic Alliance Agreement are not closed on a timely
basis, or if another financing or strategic alternative providing sufficient resources to allow us to continue operations is not consummated upon
exhaustion of our current capital, we will be required to cease operations and liquidate our assets. No assurance can be given that we will be able to
commercialize the new opportunities or consummate the quarterly payment closings under the Epic Strategic Alliance Agreement on a timely basis,
or consummate such other financing or strategic alternative in the time necessary to avoid the cessation of our operations and liquidation of our
assets. Moreover, even if we consummate the quarterly payment closings under the Epic Strategic Alliance Agreement, or such other financing or
strategic alternative, we may be required to seek additional capital in the future and there can be no assurances that we will be able to obtain
additional capital on favorable terms, if at all.
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�If Novel Laboratories issues additional equity in the future our equity interest in Novel may be diluted, resulting in a decrease in our
share of any dividends or other distributions which Novel may issue in the future.
At the end of 2006, Elite entered into a joint venture with VGS Pharma, LLC (“VGS”) and created Novel Laboratories, Inc. (“Novel”), a
privately-held company specializing in pharmaceutical research, development, manufacturing, licensing, acquisition and marketing of specialty
generic pharmaceuticals. Novel's business strategy is to focus on its core strength in identifying and timely executing niche business opportunities in
the generic pharmaceutical area. Elite owns approximately 10% of the outstanding shares of Class A Voting Common Stock of Novel. To date, Elite
has received no distributions or dividends from this investment.
As a result of our determination not to fund our remaining contributions to Novel at the valuation set forth in the Novel Alliance Agreement and the
resulting purchase from us of a portion of our shares of Class A Voting Common Stock of Novel by VGS Pharma, LLC, our remaining ownership
interest in equity of Novel was reduced to approximately 10% of the outstanding shares of Novel. Novel may seek to raise additional operating
capital in the future and may do so by the issuance of equity. If Novel issues additional equity, our future equity interest in Novel will decrease and
we will be entitled to a decreased portion of any dividends or other distributions which Novel may issue in the future. Novel also has a company
sponsored stock option plan and any equity issued from this stock plan will also reduce Elite’s equity interest in Novel.
Substantially all of our product candidates are at an early stage of development and only a portion of these are in clinical development.
ELI-154 and ELI-216 are pre-Phase III and some of our generic products are still at an early stage of development. Other than generic phentermine,
which is a commercial drug product, and two additional generic drug products which Elite purchased in 2010, but are not yet commercialized, and a
generic product that has been filed but not yet approved by the FDA, we will need to perform additional development work for the additional product
candidates in our pipeline before we can seek the regulatory approvals necessary to begin commercial sales.
If we are unable to satisfy regulatory requirements, we may not be able to commercialize our product candidates.
We need FDA approval prior to marketing our product candidates in the United States of America. If we fail to obtain FDA approval to market our
product candidates, we will be unable to sell our product candidates in the United States of America and we will not generate any revenue from the
sale of such products.
This regulatory review and approval process, which includes evaluation of preclinical studies and clinical trials of our product candidates, is lengthy,
expensive and uncertain. To receive approval, we must, among other things, demonstrate with substantial evidence from well-controlled clinical
trials that our product candidates are both safe and effective for each indication where approval is sought. Satisfaction of these requirements typically
takes several years and the time needed to satisfy them may vary substantially, based on the type, complexity and novelty of the pharmaceutical
product. We cannot predict if or when we might submit for regulatory approval any of our product candidates currently under development. Any
approvals we may obtain may not cover all of the clinical indications for which we are seeking approval. Also, an approval might contain significant
limitations in the form of narrow indications, warnings, precautions, or contra-indications with respect to conditions of use.
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�The FDA has substantial discretion in the approval process and may either refuse to accept an application for substantive review or may form the
opinion after review of an application that the application is insufficient to allow approval of a product candidate. If the FDA does not accept our
application for review or approve our application, it may require that we conduct additional clinical, preclinical or manufacturing validation studies
and submit the data before it will reconsider our application. Depending on the extent of these or any other studies that might be required, approval
of any applications that we submit may be delayed by several years, or we may be required to expend more resources than we have available. It is
also possible that any such additional studies, if performed and completed, may not be considered sufficient by the FDA to make our applications
approvable. If any of these outcomes occur, we may be forced to abandon our applications for approval.
We will also be subject to a wide variety of foreign regulations governing the development, manufacture and marketing of our products. Whether or
not an FDA approval has been obtained, approval of a product by the comparable regulatory authorities of foreign countries must still be obtained
prior to manufacturing or marketing the product in those countries. The approval process varies from country to country and the time needed to
secure approval may be longer or shorter than that required for FDA approval. We cannot assure you that clinical trials conducted in one country will
be accepted by other countries or that approval of our product in one country will result in approval in any other country.
Before we can obtain regulatory approval, we need to successfully complete clinical trials, outcomes of which are uncertain.
In order to obtain FDA approval to market a new drug product, we must demonstrate proof of safety and effectiveness in humans. To meet these
requirements, we must conduct extensive preclinical testing and “adequate and wellcontrolled” clinical trials. Conducting clinical trials is a lengthy,
time-consuming, and expensive process. Completion of necessary clinical trials may take several years or more. Delays associated with products for
which we are directly conducting preclinical or clinical trials may cause us to incur additional operating expenses. The commencement and rate of
completion of clinical trials may be delayed by many factors, including, for example:
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ineffectiveness of our product candidate or perceptions by physicians that the product candidate is not safe or effective for a particular
indication;
inability to manufacture sufficient quantities of the product candidate for use in clinical trials;
delay or failure in obtaining approval of our clinical trial protocols from the FDA or institutional review boards;
slower than expected rate of patient recruitment and enrollment;
inability to adequately follow and monitor patients after treatment;
difficulty in managing multiple clinical sites;
unforeseen safety issues;
government or regulatory delays; and
clinical trial costs that are greater than we currently anticipate.
Even if we achieve positive interim results in clinical trials, these results do not necessarily predict final results, and positive results in early trials
may not be indicative of success in later trials. A number of companies in the pharmaceutical industry have suffered significant setbacks in advanced
clinical trials, even after achieving promising results in earlier trials. Negative or inconclusive results or adverse medical events during a clinical trial
could cause us to repeat or terminate a clinical trial or require us to conduct additional trials. We do not know whether our existing or any future
clinical trials will demonstrate safety and efficacy sufficiently to result in marketable products. Our clinical trials may be suspended at any time for a
variety of reasons, including if the FDA or we believe the patients participating in our trials are exposed to unacceptable health risks or if the FDA
finds deficiencies in the conduct of these trials.
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�Failures or perceived failures in our clinical trials will directly delay our product development and regulatory approval process, damage our business
prospects, make it difficult for us to establish collaboration and partnership relationships, and negatively affect our reputation and competitive
position in the pharmaceutical community.
Because of these risks, our research and development efforts may not result in any commercially viable products. Any delay in, or termination of, our
preclinical or clinical trials will delay the filing of our drug applications with the FDA and, ultimately, our ability to commercialize our product
candidates and generate product revenues. If a significant portion of these development efforts are not successfully completed, required regulatory
approvals are not obtained, or any approved products are not commercially successful, our business, financial condition, and results of operations
may be materially harmed.
If our collaboration or licensing arrangements are unsuccessful, our revenues and product development may be limited.
We have entered into several collaborations and licensing arrangements for the development of products. However, there can be no assurance that any
of these agreements will result in FDA approvals, or that we will be able to market any such finished products at a profit. Collaboration and
licensing arrangements pose the following risks:
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collaborations and licensing arrangements may be terminated, in which case we will experience increased operating expenses and capital
requirements if we elect to pursue further development of the related product candidate;
collaborators and licensees may delay clinical trials and prolong clinical development, under-fund a clinical trial program, stop a clinical
trial or abandon a product candidate;
expected revenue might not be generated because milestones may not be achieved and product candidates may not be developed;
collaborators and licensees could independently develop, or develop with third parties, products that could compete with our future
products;
the terms of our contracts with current or future collaborators and licensees may not be favorable to us in the future;
a collaborator or licensee with marketing and distribution rights to one or more of our products may not commit enough resources to the
marketing and distribution of our products, limiting our potential revenues from the commercialization of a product;
disputes may arise delaying or terminating the research, development or commercialization of our product candidates, or result in significant
and costly litigation or arbitration;
one or more third-party developers could obtain approval for a similar product prior to the collaborator or licensee resulting in unforeseen
price competition in connection with the development product; and
Epic may decide that the further or continuing development of one or more of the eight designated drug products being developed by Epic at
our facility is no longer commercially feasible, delaying a potential source of revenue to us pursuant to the Epic Strategic Alliance
Agreement. In addition, there can be no assurance that any drug product designated by the parties as a replacement would be as strong a
candidate for commercial viability as the drug product that it replaced.
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�If we are unable to protect our intellectual property rights or avoid claims that we infringed on the intellectual property rights of others,
our ability to conduct business may be impaired.
Our success depends on our ability to protect our current and future products and to defend our intellectual property rights. If we fail to protect our
intellectual property adequately, competitors may manufacture and market products similar to ours.
We currently hold five patents and we have four patents pending. We intend to file further patent applications in the future. We cannot be certain that
our pending patent applications will result in the issuance of patents. If patents are issued, third parties may sue us to challenge our patent protection,
and although we know of no reason why they should prevail, it is possible that they could. It is likewise possible that our patent rights may not
prevent or limit our present and future competitors from developing, using or commercializing products that are similar or functionally equivalent to
our products.
In addition, we may be required to obtain licenses to patents, or other proprietary rights of third parties, in connection with the development and use
of our products and technologies as they relate to other persons’ technologies. At such time as we discover a need to obtain any such license, we will
need to establish whether we will be able to obtain such a license on favorable terms, if at all. The failure to obtain the necessary licenses or other
rights could preclude the sale, manufacture or distribution of our products.
We rely particularly on trade secrets, unpatented proprietary expertise and continuing innovation that we seek to protect, in part, by entering into
confidentiality agreements with licensees, suppliers, employees and consultants. We cannot provide assurance that these agreements will not be
breached or circumvented. We also cannot be certain that there will be adequate remedies in the event of a breach. Disputes may arise concerning the
ownership of intellectual property or the applicability of confidentiality agreements. We cannot be sure that our trade secrets and proprietary
technology will not otherwise become known or be independently developed by our competitors or, if patents are not issued with respect to products
arising from research, that we will be able to maintain the confidentiality of information relating to these products. In addition, efforts to ensure our
intellectual property rights can be costly, time-consuming and/or ultimately unsuccessful.
Litigation is common in our industry, particularly the generic pharmaceutical industry, and can be protracted and expensive and could
delay and/or prevent entry of our products into the market, which, in turn, could have a material adverse effect on our business.
Litigation concerning patents and proprietary rights can be protracted and expensive. Companies that produce brand pharmaceutical products
routinely bring litigation against applicants that seek FDA approval to manufacture and market generic forms of their branded products. These
companies allege patent infringement or other violations of intellectual property rights as the basis for filing suit against an applicant. Because the
eight drug products being developed by Epic at the Facility are generics, such drug products may be subject to such litigation brought by companies
that produce brand pharmaceutical products. If Epic were to become subject to litigation in connection with any drug products it is developing at the
Facility under the Epic Strategic Alliance Agreement, Epic may choose to, or be required to, decrease or cease its development and
commercialization of such product for an indefinite period of time, which may prevent or delay the first commercial sale of such product and cause us
to receive reduced or no product fees payable to us by Epic based on the commercial sales of such product in accordance with the Epic Strategic
Alliance Agreement.
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�Likewise, other patent holders may bring patent infringement suits against us alleging that our products, product candidates and technologies infringe
upon intellectual property rights. Litigation often involves significant expense and can delay or prevent introduction or sale of our products.
There may also be situations where we use our business judgment and decide to market and sell products, notwithstanding the fact that allegations of
patent infringement(s) have not been finally resolved by the courts. The risk involved in doing so can be substantial because the remedies available
to the owner of a patent for infringement include, among other things, damages measured by the profits lost by the patent owner and not by the
profits earned by the infringer. In the case of a willful infringement, the definition of which is subjective, such damages may be trebled. Moreover,
because of the discount pricing typically involved with bioequivalent products, patented brand products generally realize a substantially higher profit
margin than bioequivalent products. An adverse decision in a case such as this or in other similar litigation could have a material adverse effect on
our business, financial position and results of operations and could cause the market value of our Common Stock to decline.
The pharmaceutical industry is highly competitive and subject to rapid and significant technological change, which could impair our
ability to implement our business model.
The pharmaceutical industry is highly competitive, and we may be unable to compete effectively. In addition, the pharmaceutical industry is
undergoing rapid and significant technological change, and we expect competition to intensify as technical advances in each field are made and
become more widely known. An increasing number of pharmaceutical companies have been or are becoming interested in the development and
commercialization of products incorporating advanced or novel drug delivery systems. We expect that competition in the field of drug delivery will
increase in the future as other specialized research and development companies begin to concentrate on this aspect of the business. Some of the major
pharmaceutical companies have invested and are continuing to invest significant resources in the development of their own drug delivery systems and
technologies and some have invested funds in specialized drug delivery companies. Many of our competitors have longer operating histories and
greater financial, research and development, marketing and other resources than we do. Such companies may develop new formulations and products,
or may improve existing ones, more efficiently than we can. Our success, if any, will depend in part on our ability to keep pace with the changing
technology in the fields in which we operate.
As we expand our presence in the generic pharmaceuticals market our product candidates may face intense competition from brand-name companies
that have taken aggressive steps to thwart competition from generic companies. In particular, brand-name companies continue to sell or license their
products directly or through licensing arrangements or strategic alliances with generic pharmaceutical companies (socalled “authorized generics”).
No significant regulatory approvals are required for a brand-name company to sell directly or through a third party to the generic market, and
brand-name companies do not face any other significant barriers to entry into such market. In addition, such companies continually seek to delay
generic introductions and to decrease the impact of generic competition, using tactics which include:
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obtaining new patents on drugs whose original patent protection is about to expire;
filing patent applications that are more complex and costly to challenge;
filing suits for patent infringement that automatically delay approval from the FDA;
filing citizens’ petitions with the FDA contesting approval of the generic versions of products due to alleged health and safety issues;
developing controlledrelease or other “nextgeneration” products, which often reduce demand for the generic version of the existing product
for which we may be seeking approval;
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�changing product claims and product labeling;
developing and marketing as over-the-counter products those branded products which are about to face generic competition; and
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These strategies may increase the costs and risks associated with our efforts to introduce our generic products under development and may delay or
prevent such introduction altogether.
If our product candidates do not achieve market acceptance among physicians, patients, health care payors and the medical community,
they will not be commercially successful and our business will be adversely affected.
The degree of market acceptance of any of our approved product candidates among physicians, patients, health care payors and the medical
community will depend on a number of factors, including:
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acceptable evidence of safety and efficacy;
relative convenience and ease of administration;
the prevalence and severity of any adverse side effects;
availability of alternative treatments;
pricing and cost effectiveness;
effectiveness of sales and marketing strategies; and
ability to obtain sufficient third-party coverage or reimbursement.
If we are unable to achieve market acceptance for our product candidates, then such product candidates will not be commercially successful and our
business will be adversely affected.
We are dependent on a small number of suppliers for our raw materials and any delay or unavailability of raw materials can materially
adversely affect our ability to produce products.
The FDA requires identification of raw material suppliers in applications for approval of drug products. If raw materials were unavailable from a
specified supplier, FDA approval of a new supplier could delay the manufacture of the drug involved. In addition, some materials used in our
products are currently available from only one supplier or a limited number of suppliers.
Further, a significant portion of our raw materials may be available only from foreign sources. Foreign sources can be subject to the special risks of
doing business abroad, including:
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greater possibility for disruption due to transportation or communication problems;
the relative instability of some foreign governments and economies;
interim price volatility based on labor unrest, materials or equipment shortages, export duties, restrictions on the transfer of funds, or
fluctuations in currency exchange rates; and
uncertainty regarding recourse to a dependable legal system for the enforcement of contracts and other rights.
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�In addition, recent changes in patent laws in certain foreign jurisdictions (primarily in Europe) may make it increasingly difficult to obtain raw
materials for research and development prior to expiration of applicable United States or foreign patents. Any delay or inability to obtain raw
materials on a timely basis, or any significant price increases that cannot be passed on to customers, can materially adversely affect our ability to
produce products. This can materially adversely affect our business and operations.
Even after regulatory approval, we will be subject to ongoing significant regulatory obligations and oversight.
Even if regulatory approval is obtained for a particular product candidate, the FDA and foreign regulatory authorities may, nevertheless, impose
significant restrictions on the indicated uses or marketing of such products, or impose ongoing requirements for post-approval studies. Following any
regulatory approval of our product candidates, we will be subject to continuing regulatory obligations, such as safety reporting requirements, and
additional post-marketing obligations, including regulatory oversight of the promotion and marketing of our products. If we become aware of
previously unknown problems with any of our product candidates here or overseas or at our contract manufacturers’ facilities, a regulatory agency
may impose restrictions on our products, our contract manufacturers or on us, including requiring us to reformulate our products, conduct additional
clinical trials, make changes in the labeling of our products, implement changes to or obtain reapprovals of our contract manufacturers’ facilities or
withdraw the product from the market. In addition, we may experience a significant drop in the sales of the affected products, our reputation in the
marketplace may suffer and we may become the target of lawsuits, including class action suits. Moreover, if we fail to comply with applicable
regulatory requirements, we may be subject to fines, suspension or withdrawal of regulatory approvals, product recalls, seizure of products, operating
restrictions and criminal prosecution. Any of these events could harm or prevent sales of the affected products or could substantially increase the costs
and expenses of commercializing and marketing these products.
If key personnel were to leave us or if we are unsuccessful in attracting qualified personnel, our ability to develop products could be
materially harmed.
Our success depends in large part on our ability to attract and retain highly qualified scientific, technical and business personnel experienced in the
development, manufacture and marketing of oral, controlled-release drug delivery systems and generic products. Our business and financial results
could be materially harmed by the inability to attract or retain qualified personnel.
If we were sued on a product liability claim, an award could exceed our insurance coverage and cost us significantly.
The design, development and manufacture of our products involves an inherent risk of product liability claims. We have procured product liability
insurance; however, a successful claim against us in excess of the policy limits could be very expensive to us, damaging our financial position. The
amount of our insurance coverage, which has been limited due to our limited financial resources, may be materially below the coverage maintained
by many of the other companies engaged in similar activities. To the best of our knowledge, no product liability claim has been made against us as
of March 31, 2011.
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�RISKS RELATED TO OUR COMMON STOCK
Future sales of our Common Stock could lower the market price of our Common Stock.
Sales of substantial amounts of our shares in the public market could harm the market price of our Common Stock, even if our business is doing
well. A significant number of shares of our Common Stock are eligible for sale in the public market under Rule 144, promulgated under the
Securities Act of 1933, as amended (the “Securities Act”), subject in some cases to volume and other limitations. These sales, or the perception in
the market that the holders of a large number of shares intend to sell shares, could reduce the market price of our Common Stock.
Our stock price has been volatile and may fluctuate in the future.
The market price for the publicly traded stock of pharmaceutical companies is generally characterized by high volatility. There has been significant
volatility in the market prices for our Common Stock. For the twelve months ended March 31, 2011, the closing sale price on the OTC Bulletin
Board (“OTCBB”) of our Common Stock fluctuated from a high of $0.10 per share to a low of $0.04 per share. The price per share of our
Common Stock may not exceed or even remain at current levels in the future. The market price of our Common Stock may be affected by a number
of factors, including:
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Results of our clinical trials;
Approval or disapproval of our ANDAs or NDAs;
Announcements of innovations, new products or new patents by us or by our competitors;
Governmental regulation;
Patent or proprietary rights developments;
Proxy contests or litigation;
News regarding the efficacy of, safety of or demand for drugs or drug technologies;
Economic and market conditions, generally and related to the pharmaceutical industry;
Healthcare legislation;
Changes in third-party reimbursement policies for drugs;
Fluctuations in our operating results;
Commercial success of the eight drug products of Epic identified under the Epic Strategic Alliance Agreement; and
Our ability to consummate the third closing of the transactions contemplated by the Epic Strategic Alliance Agreement
Our Common Stock is considered a “penny stock”. The application of the “penny stock” rules to our Common Stock could limit the
trading and liquidity of our Common Stock, adversely affect the market price of our Common Stock and increase the transaction costs to
sell shares of our Common Stock.
Our common stock is a “lowpriced” security or “penny stock” under rules promulgated under the Securities Exchange Act of 1934, as amended. In
accordance with these rules, broker-dealers participating in transactions in low-priced securities must first deliver a risk disclosure document which
describes the risks associated with such stocks, the brokerdealers duties in selling the stock, the customer’s rights and remedies and certain market
and other information. Furthermore, the brokerdealer must make a suitability determination approving the customer for lowpriced stock
transactions based on the customer’s financial situation, investment experience and objectives. Brokerdealers must also disclose these restrictions in
writing to the customer, obtain specific written consent from the customer, and provide monthly account statements to the customer. The effect of
these restrictions will likely decrease the willingness of broker-dealers to make a market in our common stock, will decrease liquidity of our common
stock and will increase transaction costs for sales and purchases of our common stock as compared to other securities.
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�We voluntarily delisted our Common Stock from NYSE Amex in May 2009. Our Common Stock is now quoted on the OvertheCounter
Bulletin Board. The OvertheCounter Bulletin Board is a quotation system, not an issuer listing service, market or exchange, therefore,
buying and selling stock on the OvertheCounter Bulletin Board is not as efficient as buying and selling stock through an exchange. As
a result, it may be difficult to sell our Common Stock for an optimum trading price or at all.
The OvertheCounter Bulletin Board (the “OTCBB”) is a regulated quotation service that displays realtime quotes, last sale prices and volume
limitations in overthecounter securities. Because trades and quotations on the OTCBB involve a manual process, the market information for such
securities cannot be guaranteed. In addition, quote information, or even firm quotes, may not be available. The manual execution process may delay
order processing and intervening price fluctuations may result in the failure of a limit order to execute or the execution of a market order at a
significantly different price. Execution of trades, execution reporting and the delivery of legal trade confirmations may be delayed
significantly. Consequently, one may not be able to sell shares of our common stock at the optimum trading prices.
When fewer shares of a security are being traded on the OTCBB, volatility of prices may increase and price movement may outpace the ability to
deliver accurate quote information. Lower trading volumes in a security may result in a lower likelihood of an individual’s orders being executed,
and current prices may differ significantly from the price one was quoted by the OTCBB at the time of the order entry. Orders for OTCBB securities
may be canceled or edited like orders for other securities. All requests to change or cancel an order must be submitted to, received and processed by
the OTCBB. Due to the manual order processing involved in handling OTCBB trades, order processing and reporting may be delayed, and an
individual may not be able to cancel or edit his order. Consequently, one may not be able to sell shares of common stock at the optimum trading
prices.
The dealer’s spread (the difference between the bid and ask prices) may be large and may result in substantial losses to the seller of securities on the
OTCBB if the common stock or other security must be sold immediately. Further, purchasers of securities may incur an immediate “paper” loss
due to the price spread. Moreover, dealers trading on the OTCBB may not have a bid price for securities bought and sold through the
OTCBB. Due to the foregoing, demand for securities that are traded through the OTCBB may be decreased or eliminated.
Raising of additional funding through sales of our securities could cause existing holders of our Common Stock to experience substantial
dilution.
Any financing that involves the further sale of our securities could cause existing holders of our Common Stock to experience substantial dilution.
On the other hand, if we incurred debt, we would be subject to risks associated with indebtedness, including the risk that interest rates might
fluctuate and cash flow would be insufficient to pay principal and interest on such indebtedness.
The issuance of additional warrants and shares to Epic under the Epic Strategic Alliance Agreement will cause existing holders of our
Common Stock to experience substantial dilution.
If Elite and Epic consummate the quarterly payment closings under the Epic Strategic Alliance Agreement, Elite will issue to Epic an aggregate of
687.5 shares of Series E Preferred Stock, convertible into an aggregate of approximately 27 million shares of Common Stock, based on a conversion
price as of June 30, 2011. If Epic converts the shares of Series E Preferred Stock into shares of Common Stock, the existing holders of our Common
Stock will experience substantial dilution.
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�In addition, with respect to the products developed by Epic under the Epic Strategic Alliance Agreement, Elite may issue to Epic (a) warrants to
purchase up to an aggregate of 56,000,000 shares of its Common Stock upon the receipt by Elite from Epic of written notices of Epic’s receipt of an
acknowledgment from the FDA that the FDA accepted for filing an ANDA for certain controlled-release and immediate-release products developed by
Epic at the Facility and (b) up to an aggregate of 40,000,000 additional shares of its Common Stock following the receipt by Elite from Epic of
written notices of Epic’s receipt from the FDA of approval for certain controlledrelease and immediaterelease products developed by Epic at the
Facility. If these events occur, the existing holders of our Common Stock will also experience substantial dilution upon the issuance of the additional
shares of Common Stock and the shares of Common Stock underlying the warrants, if the warrants are exercised.
The issuance of additional shares of our Common Stock or our preferred stock could make a change of control more difficult to achieve.
The issuance of additional shares of our Common Stock or the issuance of shares of an additional series of preferred stock could be used to make a
change of control of us more difficult and expensive. Under certain circumstances, such shares could be used to create impediments to, or frustrate
persons seeking to cause, a takeover or to gain control of us. Such shares could be sold to purchasers who might side with our Board of Directors in
opposing a takeover bid that the Board of Directors determines not to be in the best interests of our stockholders. It might also have the effect of
discouraging an attempt by another person or entity through the acquisition of a substantial number of shares of our Common Stock to acquire
control of us with a view to consummating a merger, sale of all or part of our assets, or a similar transaction, since the issuance of new shares could
be used to dilute the stock ownership of such person or entity.
Epic will have the ability to exert substantial influence over Elite.
Under the Epic Strategic Alliance Agreement, Elite agreed that it and its Board of Directors will take any and all action necessary so that (i) the size
of the Board of Directors will be set and remain at seven directors, (ii) three individuals designated by Epic (the “Epic Directors”) will be appointed
to the Board of Directors and (iii) the Epic Directors will be nominated at each annual or special meeting of stockholders at which an election of
directors is held or pursuant to any written consent of the stockholders; provided, however, that if at any time following the initial closing of the
Epic Strategic Alliance Agreement and ending on the later of (a) the date immediately following the first anniversary of the Initial Closing Date and
(b) the Third Closing Date, Epic owns less than (1) a number of shares of Series E Preferred Stock equal to ninety percent of the aggregate number of
shares of Series E Preferred Stock purchased by Epic or (2) following the conversion by Epic of the Series E Preferred Stock, a number of shares of
Common Stock equal to ninety percent of the number of shares of Common Stock so converted, neither Elite nor its Board of Directors will be
obligated to nominate Epic Directors or take any other action with respect to those actions described in (i), (ii) and/or (iii) above. No Epic Director
may be removed from office for cause unless such removal is directed or approved by (A) a majority of the independent members of the Board of
Directors and (B) all of the non-affected Epic Director(s). Any vacancies created by the resignation, removal or death of an Epic Director will be filled
by the appointment of an additional Epic Director. Any Epic Director may be removed from office upon the request of Epic, with or without cause.
Epic, by virtue of having the right to designate the three Epic Directors, will have the ability to exert substantial influence over the election of the
other members of Elite’s Board of Directors, the outcome of issues submitted to our stockholders for approval and the management and affairs of
Elite.
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�In addition, the Series E Certificate provides that on any matter presented to the holders of our Common Stock for their action or consideration at
any meeting of our stockholders (or by written consent of stockholders in lieu of meeting), Epic, as a holder of Series E Preferred Stock, will be
entitled to cast the number of votes equal to the number of shares of Common Stock into which the shares of Series E Preferred Stock held by Epic
are convertible as of the record date for determining the stockholders entitled to vote on such matter. Except as provided by law or by the other
provisions of the Series E Certificate, Epic will vote together with the holders of Common Stock, as a single class. In addition, pursuant to the Epic
Strategic Alliance Agreement and the Series E Certificate, Elite has agreed that, between the date of the initial closing under the Epic Strategic
Alliance Agreement and the date which is the earlier of (x) the date the Epic Directors constitute a majority of the Board of Directors and (y) ninety
days following the fifth anniversary of the Initial Closing Date, except as Epic otherwise agrees in writing, Elite may conduct its operations only in
the ordinary and usual course of business consistent with past practice. Further, pursuant to the Epic Strategic Alliance Agreement and the Series E
Certificate, Elite must obtain the prior written consent of Epic in order to take the actions specifically enumerated therein. Accordingly, as a result of
such concentration of ownership, Epic will have the ability to exert further influence over Elite and may have the effect of preventing a change of
control of Elite.
In addition, with respect to the products developed by Epic under the Epic Strategic Alliance Agreement, Elite may issue to Epic (a) warrants to
purchase up to an aggregate of 56,000,000 shares of its Common Stock upon the receipt by Elite from Epic of written notices of Epic’s receipt of an
acknowledgment from the FDA that the FDA accepted for filing an ANDA for certain controlled-release and immediate-release products developed by
Epic at the Facility and (b) up to an aggregate of 40,000,000 additional shares of its Common Stock following the receipt by Elite from Epic of
written notices of Epic’s receipt from the FDA of approval for certain controlledrelease and immediaterelease products developed by Epic at the
Facility. If Elite is required to issue such warrants and such additional shares of its Common Stock to Epic in accordance with the Epic Strategic
Alliance Agreement, Epic may beneficially own in excess of 50% of the issued and outstanding Common Stock or other voting securities of Elite.
Under the Epic Strategic Alliance Agreement, at such time as Epic owns more than 50% of the issued and outstanding Common Stock or other
voting securities of Elite, the number of Epic Directors that the Purchaser will be entitled to designate under the Alliance Agreement will be equal to
a majority of the Board of Directors.
Holders of our preferred stock may exercise their veto rights to make it more difficult for us to take an action or consummate a transaction
that may be deemed by the Board to be in our best interest or the best interest of the other stockholders.
The holders of Series B Preferred Stock, Series C Preferred Stock and Series E Preferred Stock have certain veto rights that may be exercised to
prevent us from taking an action or consummating a transaction that may be deemed by the Board to be in our best interest and the best interest of
the holders of our Common Stock if the holders of our preferred stock believe such action or transaction would be adverse to their own interests. If
the holders of our preferred stock exercise their veto rights to prevent us from taking any such action or consummating any such transaction, our
ability to achieve our strategic objectives may be hindered. The ability of holders of our preferred stock to affect our actions through use of their veto
rights might limit the price that certain investors would be willing to pay in the future for shares of our Common Stock.
In addition, pursuant to the Epic Strategic Alliance Agreement and the Series E Certificate, Elite has agreed that, between the date of the initial
closing under the Epic Strategic Alliance Agreement and the date which is the earlier of (x) the date the Epic Directors constitute a majority of the
Board of Directors and (y) ninety days following the fifth anniversary of the Initial Closing Date, except as Epic otherwise agrees in writing, Elite
may conduct its operations only in the ordinary and usual course of business consistent with past practice. Further, pursuant to the Epic Strategic
Alliance Agreement and the Series E Certificate, Elite must obtain the prior written consent of Epic in order to take certain actions specifically
enumerated therein. This right will terminate if Epic’s ownership percentage of the capital stock of Elite, on an asconverted basis, falls below 20%
of Elite’s capital stock, on an asconverted basis, as a result of transfers made by Epic.
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�Section 203 of the Delaware General Corporation Law may deter a third party from acquiring us.
Section 203 of the Delaware General Corporation Law prohibits a merger with a 15% shareholder within three years of the date such shareholder
acquired 15%, unless the merger meets one of several exceptions. The exceptions include, for example, approval by the holders of two-thirds of the
outstanding shares (not counting the 15% shareholder), or approval by the Board of Directors prior to the 15% shareholder acquiring its 15%
ownership. This provision makes it difficult for a potential acquirer to force a merger with or takeover of us, and could thus limit the price that
certain investors might be willing to pay in the future for shares of our Common Stock.
ITEM 1B.
UNRESOLVED STAFF COMMENTS.
Not applicable.
ITEM 2.
PROPERTIES.
We own a facility located at 165 Ludlow Avenue, Northvale, New Jersey (“165 Ludlow”) which contains approximately 15,000 square feet of floor
space. This real property and the improvements thereon are encumbered by a mortgage in favor of the New Jersey Economic Development Authority
( “NJEDA”) as security for a loan through taxexempt bonds from the NJEDA to Elite. The mortgage contains certain customary provisions
including, without limitation, the right of NJEDA to foreclose upon a default by Elite. The NJEDA has declared the payment of this bond to be in
default. Please see the discussion entitled “Liquidity and Capital Resources” in Item 7 – Management’s Discussion and Analysis of Financial
Condition and Results of Operations. We are currently using the Facility as a laboratory, manufacturing, storage and office space.
We entered into a lease for a portion of a onestory warehouse, located at 135 Ludlow Avenue, Northvale, New Jersey (“135 Ludlow”), consisting of
approximately 15,000 square feet of floor space. The lease term began on July 1, 2010. The lease includes an initial term of 5 years and 6 months
and we have the option to renew the lease for two additional terms, each of 5 years. The property related to this lease will be used for the storage of
pharmaceutical finished goods, raw materials, equipment and documents as well as engaging in manufacturing, packaging and distribution
activities. This property requires significant construction and qualification as a prerequisite to achieving suitability for such intended future
use. Approximately 3,500 square feet of this property was constructed and qualified as suitable for use for storage of pharmaceutical finished goods,
raw materials, equipment and documents and was placed into service on or before the expiration of the lease for the warehouse at 80 Oak Street, as
noted below. Construction and qualification as suitable for manufacturing, packaging and distribution operations are expected to be achieved within
two years from the beginning of the lease term. These are estimates based on current project plans, which are subject to change. There can be no
assurance that the construction and qualification will be accomplished during the estimated time frames, or that the property located at 135 Ludlow
Avenue, Northvale, New Jersey will ever achieve qualification for intended future utilization.
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�165 Ludlow and 135 Ludlow are hereinafter referred to as the “Facilities”.
During Fiscal 2011, on November 30, 2010, a lease which the Company entered into for a portion of a one-story warehouse, located at 80 Oak
Street, Norwood, New Jersey (“80 Oak”) consisting of approximately 3,500 square feet of floor space, and used for the storage of pharmaceutical
finished goods, raw materials, equipment and documents expired.
Properties used in our operation are considered suitable for the purposes for which they are used, at the time they are placed into service, and are
believed adequate to meet our needs for the reasonably foreseeable future.
ITEM 3.
LEGAL PROCEEDINGS.
In the ordinary course of business we may be subject to litigation from time to time. Except as follows, there is no past, pending or, to our
knowledge, threatened litigation or administrative action to which we are a party or of which our property is the subject (including litigation or
actions involving our officers, directors, affiliates, or other key personnel, or holders of record or beneficially of more than 5% of any class of our
voting securities, or any associate of any such party) which in our opinion has, or is expected to have, a material adverse effect upon our business,
prospects financial condition or operations.
Midsummer Investments, Ltd., et al. v. Elite Pharmaceuticals, Inc.
On or about September 22, 2009, Midsummer Investments, Ltd. (“Midsummer”) and Bushido Capital Master Fund, LP (“Bushido”, and together
with Midsummer, the “Plaintiffs”) filed a complaint against Elite Pharmaceuticals, Inc., a Delaware corporation (the “Company”), in the United
States District Court, Southern District of New York (Case No. 09 CIV 8074) (the “Action”). The Plaintiffs asserted claims for breach of contract
(injunctive relief and damages), anticipatory breach of contract (injunctive relief), conversion (injunctive relief and damages), and attorneys’ fees,
arising out of a Securities Purchase Agreement, dated September 15, 2008, by and among the Company and certain purchasers of the Company’s
securities (including the Plaintiffs) and the Certificate of Designation of Preferences, Rights and Limitations of Series D 8% Convertible Preferred
Stock, filed with the Secretary of State of the State of Delaware on September 15, 2009 (the “Series D Certificate”). Plaintiffs claimed that they were
entitled to a reduced conversion price for their Series D 8% Convertible Preferred Stock, par value US$0.01 per share (the “Series D Preferred
Stock”), as a result of the Strategic Alliance Agreement, dated March 18, 2009, as amended (the “Epic SAA”), by and among the Company, on the
one hand, and Epic Pharma, LLC (“Epic”) and Epic Investments, LLC (“Epic Investments”, and together with Epic, the “Epic Parties”). With
their complaint, the Plaintiffs concurrently filed a request for preliminary injunction. Pursuant to an order of the Court entered into on October 16,
2009, the Plaintiffs’ request for a preliminary injunction was denied. Thereafter, Plaintiffs filed an amended complaint (the “Complaint”), asserting
claims for breach of contract (injunctive relief and damages), anticipatory breach of contract (injunctive relief), conversion (damages) and attorneys’
fees, seeking compensatory damages of $7,455,363.00, delivery of 1,000,000 shares of the Company’s common stock, par value $0.001 per share
(the “Common Stock”), a declaration that all future conversions of the Series D Preferred Stock, held by Plaintiffs is at a conversion price of $0.05,
attorneys’ fees, interest and costs.
The Company disputed the claims in the Complaint, believing the lawsuit to be without merit, and vigorously defended against them. The
Company moved for summary judgment on the Complaint and the judge in the case did not issue an order on such motion. The Company
proceeded with extensive, timeconsuming and costly discovery. The court scheduled the trial to commence on June 28, 2010.
33
�In order to avoid the delays, expense and risks inherent in litigation, after extensive negotiations, the Company entered into (i) a Stipulation of
Settlement and Release, dated June 25, 2010 (the “Settlement Agreement”), with the Plaintiffs and the Epic Parties, (ii) an Amendment Agreement,
dated June 25, 2010 (the “Series D Amendment Agreement”), with the Plaintiffs and (iii) an Amendment Agreement, dated June 25, 2010 (the
“ Series E Amendment Agreement”) with the Epic Parties. As part of the Settlement Agreement, the Action will be dismissed with prejudice.
Series D Amendment Agreement
Pursuant to the Series D Amendment Agreement, the Company and Plaintiffs agreed to amend the Series D Certificate. The holders of at least
50.1%, in the aggregate, of the Company’s outstanding Series B Preferred 8% Convertible Preferred Stock, par value US$0.01 per share, Series C
8% Convertible Preferred Stock, par value US$0.01 per share, and Series D Preferred Stock, voting as one class, consented to the filing of the
Amended Certificate of Designations of the Series D 8% Convertible Preferred Stock (the “Amended Series D Certificate”) with the Secretary of State
of the State of Delaware. On June 29, 2010, pursuant to the authority of its Board of Directors, the Company filed with the Secretary of State of the
State of Delaware the Amended Series D Certificate.
Pursuant to the terms of the Amended Series D Certificate, the terms of the Series D Preferred Stock have been amended as follows:
∙
∙
Dividends: The Series D Preferred Stock will continue to accrue dividends at the rate of 8% per annum on their stated value of US$1,000
per share, payable quarterly on January 1, April 1, July 1 and October 1 and such rate shall not increase to 15% per annum as previously
provided prior to giving effect to the Series D Amendment Agreement. In addition to being payable in cash and shares of Common Stock,
as provided in the Series D Certificate, such dividends may also be paid in shares of Series D Preferred Stock (the “Dividend Payment
Preferred Stock”) or a combination of cash, Common Stock and Dividend Payment Preferred Stock. Dividend Payment Preferred Stock
will have the same rights, privileges and preferences as the Series D Preferred Stock, except that such Dividend Payment Preferred Stock
will not be entitled to, nor accrue, any dividends pursuant to the Amended Series D Certificate.
Conversion Price: The conversion price of the Series D Preferred Stock shall be reduced from US$0.20 per share to US$0.07 per share
(subject to adjustment as provided in the Amended Series D Certificate).
34
�∙
Automatic Monthly Conversion: On each Monthly Conversion Date (as defined below), a number of shares of Series D Preferred Stock
equal to each holder’s prorata portion (based on the shares of Series D Preferred Stock held by each Holder on June 25, 2010) of the
Monthly Conversion Amount (as defined below) will automatically convert into shares of Common Stock at the then-effective conversion
price (each such conversion, a “Monthly Conversion”). Notwithstanding the foregoing, the Company will not be permitted to effect a
Monthly Conversion on a Monthly Conversion Date unless (i) the Common Stock shall be listed or quoted for trading on a trading
market, (ii) there is a sufficient number of authorized shares of Common Stock for issuance of all Common Stock to be issued upon such
Monthly Conversion, (iii) as to any holder of Series D Preferred Stock, the issuance of the shares will not cause a breach of the beneficial
ownership limitations set forth in the Amended Series D Certificate, (iv) if requested by a holder of Series D Preferred Stock and a
customary Rule 144 representation letter relating to all shares of Common Stock to be issued upon each Monthly Conversion is provided
by such holder after request from the Company, the shares of Common Stock issued upon such Monthly Conversion are delivered
electronically through the Depository Trust Company or another established clearing corporation performing similar functions (“DTC”),
may be resold by such holder pursuant to an exemption under the Securities Act and are otherwise free of restrictive legends and trading
restrictions on such Holder, (v) there has been no public announcement of a pending or proposed Fundamental Transaction or Change of
Control Transaction (as such terms are defined in the Amended Series D Certificate) that has not been consummated, (vi) the applicable
holder of Series D Preferred Stock is not in possession of any information provided to such holder by the Company that constitutes
material non-public information, and (vii) the average VWAP (as defined in the Amended Series D Certificate) for the 20 trading days
immediately prior to the applicable Monthly Conversion Date equals or exceeds the then-effective conversion price of the Series D Preferred
Stock. Shares of the Series D Preferred Stock issued to the holders of Series D Preferred Stock as Dividend Payment Preferred Stock shall
be the last shares of Series D Preferred Stock to be subject to Monthly Conversion. As used herein, the following terms have the
following meanings: (i) “Monthly Conversion Date” means the first day of each month, commencing on August 1, 2010, and terminating
on the date the Series D Preferred Stock is no longer outstanding; (ii) “Monthly Conversion Amount” means an aggregate Stated Value of
Series D Preferred Stock among all Holders that is equal to 25% of aggregate dollar trading volume of the Common Stock during the 20
trading days immediately prior to the applicable Monthly Conversion Date (such 20 trading day period, the “Measurement Period”),
increasing to 35% of the aggregate dollar trading volume during the Measurement Period if the average VWAP during such Measurement
Period equals or exceeds $0.12 (subject to adjustment for forward and reverse stock splits and the like that occur after June 25, 2010) and
further increasing to 50% of the aggregate dollar trading volume during such Measurement Period if the average VWAP during such
Measurement Period equals or exceeds $0.16 (subject to adjustment for forward and reverse stock splits and the like that occur after June
25, 2010).
∙
Change of Control Transaction: Epic and its affiliates were expressly excluded from any event which would otherwise constitute a
“Change of Control Transaction” due to the acquisition in excess of 40% of the Company’s voting securities.
Pursuant to the Series D Amendment Agreement, the exercise price of the Warrants (the “Series D Warrants”) to purchase shares of Common Stock
issued to the holders of Series D Preferred Stock pursuant to the Securities Purchase Agreement, dated as of September 15, 2008, by and among the
Company and the purchasers of Series D Preferred Stock will be reduced from $0.25 per share to US$0.125. In addition, the exercise price of the
Series D Warrants may be reduced as follows:
(i)
(ii)
by 20%, if on September 15, 2011, the holder of such Warrant still beneficially owns more than 50% of the Series D
Preferred Stock beneficially owned by such holder as of June 25, 2010 (“Base Ownership”); and
by 20%, if (a) on September 15, 2011, such holder then beneficially owns more than 25% of the Base Ownership and 50%
or less of the Base Ownership and (b) on September 15, 2012, such holder then beneficially owns more than 25% of the Base
Ownership.
Notwithstanding the foregoing, (x) in no event will the exercise price of the Series D Warrants be reduced more than once as a result of the
amendments to such Series D Warrants, and (y) in the event that on September 15, 2011 or, if the condition of clause (ii)(a) above is met, on
September 15, 2012, the Holder beneficially owns 25% or less of the Base Ownership, then no adjustment shall occur pursuant to the Series D
Warrants, as amended by the Series D Amendment Agreement. Additionally, there will be no corresponding increase in the number of shares of
Common Stock issuable upon exercise of the Warrants solely as a result of the foregoing adjustments.
To the extent such issuance does not cause the breach of the beneficial ownership limitations set forth in the Amended Series D Certificate (any
excess shares will be issued to the affected holder of Series D Preferred Stock upon written notice from such holder when such holder’s beneficial
ownership is below 9.9% to the extent that such issuance does not cause such holder to exceed such amount), the Company agreed to issue certain
shares of Common Stock to the Plaintiffs and their respective affiliates in satisfaction of the Company’s obligation to pay certain previously accrued
but unpaid dividends through March 31, 2010 owing to the Plaintiffs and their respective affiliates.
35
�Series E Amendment Agreement
Pursuant to the Series E Amendment Agreement, the Company agreed to amend the Certificate of Designation of Preferences, Rights and Limitations
of the Series E Convertible Preferred Stock, filed with Secretary of State of the State of Delaware on June 3, 2009 (the “Series E Certificate”). The
Epic Parties, constituting all holders of Series E Preferred Stock, consented to the filing of the Amended Certificate of Designations of the Series E
Convertible Preferred Stock (the “Amended Series E Certificate”) with the Secretary of State of the State of Delaware. On June 29, 2010, pursuant to
the authority of its Board of Directors, Company filed with the Secretary of State of the State of Delaware the Amended Series E Certificate. Pursuant
to the terms of the Amended Series E Certificate, the conversion price of the Series E Preferred Stock will be adjusted downward to reflect, on a pro
rata basis, the reduction in the conversion price of the Series D Preferred Stock as the result of the Series D Amendment Agreement, to the extent
shares of Series D Preferred Stock are converted at the reduced conversion price set forth in the Amended Series D Certificate.
Pursuant to the Series E Amendment Agreement, the Epic SAA was amended so that the purchase of the 750 Additional Shares of Series E Preferred
Stock described therein for an aggregate purchase price of $750,000 would occur in 12 installments of 62.5 shares (for a purchase price of $62,500) (i)
on or prior to November 1, 2009 (which has been satisfied) and (ii) within 10 business days following the last day of each calendar quarter,
beginning with the first calendar quarter ending on September 30, 2010 and continuing for each of the 10 calendar quarters thereafter.
In addition, under the Series E Amendment Agreement, the third closing date is scheduled to occur on or before December 31, 2010, subject to
certain conditions set forth in the Epic SAA (as amended by the Series E Amendment Agreement).
Under each of the Series D Amendment Agreement and the Series E Amendment Agreement, the Company agreed that at its next meeting of
shareholders it will seek shareholder approval to amend its certificate of incorporation to increase the number of authorized but unissued shares of
Common Stock to at least 760,000,000.
Settlement Agreement
Pursuant to the Settlement Agreement, Elite and the Epic Parties, individually and on behalf of each of their respective officers, directors, agents,
representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns (the “Elite Releasors”) agreed to release and
discharge each of the Plaintiffs, BCMF Trustees LLC, an affiliate of Bushido (“BCMF”), their respective owners, officers, directors, investors,
agents, representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns (the “Plaintiffs’ Releasees”) from any
and all actions, causes of action, claims, liens, suits, debts, accounts, liabilities, expenses, attorneys’ fees, agreements, promises, charges,
complaints and demands (collectively, “Loses”) which the Elite Releasors have or may have against the Plaintiffs’ Releasees that could have been
asserted in the Action or any other court action, based upon any conduct up to and including the date of the Settlement Agreement. Notwithstanding
the foregoing, the Elite Releasors will not release any claim of breach of the terms of the Settlement Agreement, breach of the terms of the Series D
Amendment Agreement, or any cause of action arising from future conduct by the Plaintiffs’ Releasees.
Pursuant to the Settlement Agreement, the Plaintiffs and BCMF, individually and on behalf of each of their respective owners, officers, directors,
investors, agents, representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns (the “Plaintiffs’
Releasors”) agreed to release and discharge Elite and the Epic Parties and each of their respective officers, directors, agents, representatives,
successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns (the “Elite Releasees”), from any and all Losses which the
Plaintiffs’ Releasors have or may have against the Elite Releasees that could have been asserted in the Action or any other court action, based upon
any conduct up to and including the date of the Settlement Agreement. Notwithstanding the foregoing, the Plaintiffs’ Releasors did not release any
claim of breach of the terms of the Settlement Agreement, breach of the terms of the Series D Amendment Agreement or any cause of action arising
from future conduct by the Elite Releasees.
In addition, concurrently with the execution of the Settlement Agreement, legal counsel for both the Company and the Plaintiffs executed a
Stipulation of Discontinuance of the Action, which such counsel will file once all conditions precedent to the effectiveness of the Settlement
Agreement have been satisfied.
36
�The foregoing description of the Amended Series D Certificate, Amended Series E Certificate, Settlement Agreement, Series D Amendment
Agreement and Series E Amendment Agreement does not purport to be complete and is qualified in its entirety by reference to the complete text of
such documents which are filed herewith and incorporated herein by reference.
On July 1, 2010, the Company filed with the SEC a Current Report on Form 8-K announcing the settlement of the litigation with the Plaintiffs,
with such filing being incorporated by reference herein.
ThePharmaNetwork Inc. v. Elite Pharmaceuticals Inc.
On March 17, 2011, Elite Pharmaceuticals, Inc. (the “Company”) issued a press release announcing the settlement of a lawsuit filed in the Superior
Court of New Jersey, Chancery Division: Bergen County entitled ThePharmaNetwork, LLC v. Elite Pharmaceuticals, Inc. (Index No. C-272-10) (the
“Action”).
The Action was commenced on or about August 27, 2010 by ThePharmaNetwork, LLC (“TPN”). TPN alleged that the Company breached certain
obligations in connection with a Product Collaboration Agreement (the “Collaboration Agreement”), made as of November 10, 2006, pursuant to
which the Company and TPN agreed to collaborate in the development, commercialization, manufacturing and distribution of a generic
pharmaceutical product, which the parties subsequently agreed would be methadone hydrochloride in a 10 mg. tablet (the “Product”). In the lawsuit,
the Company asserted counterclaims against TPN arising out of the Collaboration Agreement, and sought damages of no less than $1,125,000 from
TPN. Both parties denied the other side’s allegations.
In order to fully and finally resolve the disputed claims arising in the Action, the Company and TPN have entered into a settlement agreement, dated
March 11, 2011 (the “Settlement Agreement”), pursuant to which the Action, including all of TPN’s claims and the Company’s counterclaims, will
be dismissed with prejudice.
Pursuant to the Settlement Agreement, the parties have agreed to terminate the Collaboration Agreement.
In addition, in consideration of the Company’s agreement to terminate the Collaboration Agreement and to relinquish to TPN all rights and interest
in the Abbreviated New Drug Application (“ANDA”) for the Product approved by the U.S. Food and Drug Administration (FDA), TPN made a
cash payment of $500,000 to Elite.
As part of the Settlement Agreement, TPN also acknowledges that the Company may develop a generic product containing methadone of any
strength (including the filing of an abbreviated new drug application relating to such product) and that nothing in the Settlement Agreement restricts
the Company from developing, commercializing, manufacturing and distributing any pharmaceutical product similar to, or which may compete with,
the Product or the ANDA filed in connection with the Product.
The Settlement Agreement also contained a mutual release pursuant to which the Company and TPN agreed to release and discharge each other and
their respective affiliates from all claims arising before the date of the Settlement Agreement.
Please refer to the Current Report on Form 8-K filed with the SEC on March 17, 2011, such filing being herein incorporated by reference, for further
details on this settlement of litigation.
37
�ITEM 4.
REMOVED AND RESERVED.
PART II
ITEM 5.
MARKET FOR COMPANY’S COMMON EQUITY AND RELATED STOCKHOLDER MATTERS.
Market Information
Our Common Stock was traded on NYSE Amex (formerly, the American Stock Exchange) under the symbol “ELI” until May 21, 2009, at which
time Elite’s Common Stock began to be quoted on the OvertheCounter Bulletin Board (OTCBB) under the ticker symbol “ELTP”. The
following table shows, for the periods indicated, the high and low sales prices per share of our Common Stock as by OTC Bulletin Board.
Over-the-counter market quotations reflect inter-dealer prices, without retail mark-up, mark-down or commission and may not necessarily represent
actual transactions.
Quarter ended
High
Low
Common Stock
Fiscal Year ending March 31, 2011:
March 31, 2011
December 31, 2010
September 30, 2010
June 30, 2010
Fiscal Year ending March 31, 2010:
March 31, 2010
December 31, 2009
September 30, 2009
June 30, 2009
$
$
$
$
$
$
$
$
0.09 $
0.07 $
0.08 $
0.10 $
0.12 $
0.25 $
0.09 $
0.20 $
0.04
0.04
0.05
0.07
0.08
0.06
0.06
0.05
On June 24 2011, the last reported sale price of our Common Stock, as quoted by the OTC Bulletin Board, was $ 0.175 per share
Holders
As of June 30, 2011, there were approximately 188 holders of record of our Common Stock
Dividends
We have never paid cash dividends on our Common Stock. We currently anticipate that we will retain all available funds for use in the operation
and expansion of our business.
Recent Sales of Unregistered Securities
There were no sales of unregistered securities during the quarter ended March 31, 2011.
38
�Securities Authorized for Issuance under Equity Compensation Plans
The following table sets forth certain information regarding Elite’s equity compensation plans as of March 31, 2011.
Number of
securities to
be issued
upon exercise
of
outstanding
options,
warrants and
rights
(a)
Weighted-
average
exercise
price per
share 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))
(1)
3,057,000 $
—
1.51
—
4,622,500
—(2)
Plan Category
Equity compensation plans approved by security holders
Equity compensation plans not approved by security holders
Total
3,057,000 $
1.51
4,622,500
(1) Represents options issued under the 2004 Stock Option Plan
(2) Represents securities reserved and available for grant under the 2009 Equity Incentive Plan
2004 Stock Option Plan
Our 2004 Stock Option Plan (the “Stock Option Plan”) permits us to grant both incentive stock options (“Incentive Stock Options” or “ISOs”)
within the meaning of Section 422 of the Internal Revenue Code (the “Code”) to employees, and other options which do not qualify as Incentive
Stock Options (the “Non-Qualified Options”) to employees, officers, Directors of and consultants to Elite.
Unless earlier terminated by the Board of Directors, the Stock Option Plan (but not outstanding options issued thereunder) terminates on March 1,
2014, after which no further awards may be granted under the Stock Option Plan. The Stock Option Plan is administered by the Board of Directors.
Recipients of options under the Stock Option Plan (“Optionees”) are selected by the Board of Directors. The Board of Directors determines the terms
of each option grant including (1) the purchase price of shares subject to options, (2) the dates on which options become exercisable and (3) the
expiration date of each option (which may not exceed ten years from the date of grant). The minimum per share purchase price of options granted
under the Stock Option Plan for Incentive Stock Options is the fair market value (as defined in the Stock Option Plan) or for Nonqualified Options is
85% of fair market value of one share of the Common Stock on the date the option is granted.
39
�Optionees have no voting, dividend or other rights as stockholders with respect to shares of Common Stock covered by options prior to becoming
the holders of record of such shares. The purchase price upon the exercise of options may be paid in cash, by certified bank or cashier’s check, by
tendering stock held by the Optionee, as well as by cashless exercise either through the surrender of other shares subject to the option or through a
broker. The total number of shares of Common Stock available under the Stock Option Plan, and the number of shares and per share exercise price
under outstanding options will be appropriately adjusted in the event of any stock dividend, reorganization, merger or recapitalization or similar
corporate event. Subject to limitations set forth in the Stock Option Plan, the terms of option agreements will be determined by the Board of
Directors, and need not be uniform among Optionees.
The Board of Directors may at any time terminate the Stock Option Plan or from time to time make such modifications or amendments to the Stock
Option Plan as it may deem advisable and the Board of Directors may adjust, reduce, cancel and re-grant an unexercised option if the fair market
value declines below the exercise price except as may be required by any national stock exchange or national market association on which the
Common Stock is then listed. In no event may the Board of Directors, without the approval of stockholders, amend the Stock Option Plan to
increase the maximum number of shares of Common Stock for which options may be granted under the Stock Option Plan or change the class of
persons eligible to receive options under the Stock Option Plan.
2009 Equity Incentive Plan
Our Equity Incentive Plan was adopted by the Board on November 24, 2009, to provide incentives to attract, retain and motivate eligible persons
whose present and potential contributions are important to the success of the Company, and its Parent and Subsidiaries (if any), by offering them an
opportunity to participate in the Company’s future performance through awards of Options, the right to purchase Common Stock and Stock
Bonuses. An aggregate of 8,000,000 common shares are reserved for grant and issuance pursuant to the Equity Incentive Plan. The Equity Incentive
Plan is administered and interpreted by the Company’s Compensation Committee (the “Compensation Committee”). Under the Equity Incentive
Plan, the Company is permitted to grant both incentive stock options (“Incentive Stock Options” or “ISOs”) within the meaning of Section 422 of
the Internal Revenue Code (the “Code”) to employees, and other options which do not qualify as Incentive Stock Options (the “Non-Qualified
Options”) to employees, officers, Directors of and consultants to Elite. The per share purchase price of options granted under the Equity Incentive
Plan may not be less than the fair market value of the shares on the date of the grant, provided that the exercise price of any ISO granted to a ten
percent stockholder will not be less than 110% of the fair market value on the date of the grant. Recipients of ISO’s and NonQualified Options have
no voting, dividend or other rights as stockholders with respect to shares of Common Stock covered by options prior to becoming the holders of
record of such shares.
Under the Equity Incentive Plan, the Company is also permitted to offer stock awards (“Equity Incentive Plan Stock Awards”) to eligible
persons. The Equity Incentive Plan defines such stock awards as an offer by the Company to sell to an eligible person shares that may or may not be
subject to restrictions. The purchase of price of shares sold pursuant to an Equity Incentive Plan Stock Award may not be less than the fair market
value of the shares on the grant date, provided, however, that the number of shares issued for the payment of employee and officers’ salaries, or
directors’ fees will be computed using the average daily closing price, which is defined as the simple average of the closing price of each trading day
in the quarter or other applicable period for which payment is due.
40
�The Company is also permitted to award stock bonuses under the Equity Incentive Plan (“Equity Incentive Plan Stock Bonuses”), which defines
such stock bonuses as an award of shares for extraordinary services rendered to the Company.
ITEM 6
SELECTED FINANCIAL DATA
[Not applicable to smaller reporting companies]
ITEM 7.
MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATION
General
The following discussion and analysis should be read with the financial statements and accompanying notes, included elsewhere in this Annual
Report on Form 10K and the information described under the caption “Risk Factors” and “Special Note Regarding Forward Looking Statements”
above. The following discussion is intended to assist the reader in understanding and evaluating our financial position.
Overview
Elite is a specialty pharmaceutical company principally engaged in the development and manufacture of oral, controlled-release products, using
proprietary technology. Elite’s strategy includes improving offpatent drug products for life cycle management and developing generic versions of
controlledrelease drug products with high barriers to entry. Elite’s technology is applicable to develop delayed, sustained or targeted release pellets,
capsules, tablets, granules and powders.
Elite has one product, Phentermine 37.5mg tablets, currently being sold commercially. The Company also has a pipeline of additional generic drug
candidates under active development and the Company is developing ELI-216, an abuse resistant oxycodone product, and ELI-154, a once-a-day
oxycodone product. Elite’s facility in Northvale, New Jersey operates under Good Manufacturing Practice (“GMP”) and is a United States Drug
Enforcement Agency (“DEA”) registered facility for research, development and manufacturing.
During Fiscal 2011, the Company was also engaged in the commercial manufacture and sale of Lodrane 24® and Lodrane 24D®, with such products
constituting approximately 98% of the Company’s gross revenues. On March 3, 2011, the USFDA announced its intention to remove
approximately 500 cough/cold and allergy related products from the U.S. Market. This list included the Lodrane® Products. Shortly after this
announcement by the USFDA, the Company’s customer for the Lodrane® Products cancelled all outstanding orders, citing the USFDA’s directive
as the basis for such cancellations. Manufacturing by the Company of the Lodrane® Products has accordingly ceased.
While the announcement by the USFDA had a minimal effect on the Company’s results for Fiscal 2011, the Company’s inability to manufacture
the Lodrane Products®, has a material and adverse effect on its revenues for periods beginning subsequent to March 31, 2011.
41
�ECR (the owner and marketer of the Lodrane Products) has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products
and issued a press release on March 3, 2011 stating that they will continue to actively pursue approval for the Lodrane products. In addition, on
April 29, 2011, ECR filed a Petition for Review with the United States Court of Appeals for the District of Columbia, petitioning such court to
review and set aside the final order of the US-FDA with relation to the Lodrane Products.
Strategy
Elite is focusing its efforts on the following areas: (i) development of Elite’s pain management products, (ii) manufacturing of Phentermine and
Hydromorphone products; (iii) the development of the other products in Elite’s pipeline including development of the products pursuant to the Epic
Strategic Alliance Agreement and other partners; (iv) commercial exploitation of Elite’s products either by license and the collection of royalties, or
through the manufacture of Elite’s formulations, and (v) development of new products and the expansion of Elite’s licensing agreements with other
pharmaceutical companies, including co-development projects, joint ventures and other collaborations.
Elite is focusing on the development of various types of drug products, including branded drug products (which require new drug applications
( “NDA”) under Section 505(b)(1) or 505(b)(2) of the Drug Price Competition and Patent Term Restoration Act of 1984 as well as generic drug
products (which require abbreviated new drug applications (“ANDA”)).
Elite believes that its business strategy enables Elite to reduce Elite’s risk by having a diverse product portfolio that includes both branded and
generic products in various therapeutic categories and build collaborations and establish licensing agreements with companies with greater resources
thereby allowing Elite to share costs of development and to improve cash-flow.
Epic Strategic Alliance Agreement
On March 18, 2009, Elite and Epic Pharma, LLC and Epic Investments, LLC, a subsidiary of Epic Pharma, LLC (collectively “Epic”) entered into
the Epic Strategic Alliance Agreement (amended on April 30, 2009, June 1, 2009 and July 28, 2009), pursuant to which Elite commenced a
strategic relationship with Epic, a pharmaceutical company that operates a business synergistic to that of Elite in the research and development,
manufacturing, sales and marketing of oral immediate and controlled-release drug products.
Use of Facility and Joint Development of Drug Products
Pursuant to the Epic Strategic Alliance Agreement, on June 3, 2009 (the “Initial Closing Date”), Elite and Epic conducted the initial closing (the
“ Initial Closing”) of the transactions contemplated by the Epic Strategic Alliance Agreement, and Epic and its employees and consultants
commenced use of a portion of Elite’s facility located at 165 Ludlow Avenue, Northvale, New Jersey (the “Facility”), for the purpose of developing
new generic drug products, all at Epic’s sole cost and expense for a period of at least three years (the “Initial Term”), unless sooner terminated or
extended pursuant to the Epic Strategic Alliance Agreement or by mutual agreement of Elite and Epic (the Initial Term, as shortened or extended, the
“ Term”). In addition to the use of the Facility, Epic will use Elite’s machinery, equipment, systems, instruments and tools residing at the Facility
(collectively the “Personal Property”) in connection with its joint drug development project at the Facility. Under the Epic Strategic Alliance
Agreement, Epic has the right, exercisable in its sole discretion, to extend the Initial Term for two periods of one year each by giving written notice
to Elite of such extension within ninety days of the end of the Initial Term or any extension thereof. Any such extension will be on the same terms
and conditions contained in the Epic Strategic Alliance Agreement. Elite will be responsible for (and Epic will have no responsibility for) any
maintenance, services, repairs and replacements in, to or of the Facility and the Personal Property, unless any such maintenance, service, repair or
replacement is required as a result of the negligence or misconduct of Epic’s employees or representatives, in which case Epic will be responsible for
the costs and expenses associated therewith.
42
�During the Term, Epic will use and occupy a portion of the Facility and use the Personal Property for the purpose of developing (i) at least four
controlledrelease products (the “Identified CR Products”) and (ii) at least four immediaterelease products (the “Identified IR Products”), the
identity of each have been agreed upon by Epic and Elite. If, during the Term, Epic determines, in its reasonable business judgment, that the further
or continuing development of any Identified CR Product and/or Identified IR Product is no longer commercially feasible, Epic may, upon written
notice to Elite, eliminate from development under the Epic Strategic Alliance Agreement such Identified CR Product and/or Identified IR Product,
and replace such eliminated product with another controlled-release or immediate-release product, as applicable.
Pursuant to the Epic Strategic Alliance Agreement, Epic will also use a portion of the Facility and use the Personal Property for the purpose of
developing (x) additional controlledrelease products of Epic (the “Additional CR Products”), subject to the mutual agreement of Epic and Elite,
and/or (y) additional immediaterelease products of Epic (the “Additional IR Products”), subject to the mutual agreement of Elite and Epic (each
Identified CR Product, Identified IR Product, Additional CR Product and Additional IR Product, individually, a “Product,” and collectively, the
“ Products”). Under the Epic Strategic Alliance Agreement, Epic may not eliminate an Identified CR Product or an Identified IR Product unless it
replaces such Product with an Additional CR product or Additional IR Product, as the case may be. Subject to the mutual agreement of Elite and
Epic as to additional consideration and other terms, Epic may use and occupy the Facility for the development of other products (in addition to the
Products).
As additional consideration for Epic’s use and occupancy of a portion of the Facility and its use of the Personal Property during the Term and the
issuance and delivery by Elite to Epic of the Milestone Shares (as defined below) and Milestone Warrants (as defined below), for the period
beginning on the First Commercial Sale (as defined in the Epic Strategic Alliance Agreement) of each Product and continuing for a period of ten
years thereafter (measured independently for each Product), Epic will pay Elite a cash fee (the “Product Fee”) equal to fifteen percent of the Profit (as
defined in the Epic Strategic Alliance Agreement), if any, on each of the Products.
With respect to each Identified CR Product and Additional CR Product developed by Epic at the Facility: (i) Elite will issue and deliver to Epic a
seven-year warrant to purchase up to 10,000,000 shares of Common Stock, at an exercise price of $0.0625, following the receipt by Elite from Epic
of each written notice of Epic’s receipt of an acknowledgment from the FDA that the FDA accepted for filing an ANDA for such Identified CR
Products and/or Additional CR Products, up to a maximum of four such warrants for the right to purchase up to an aggregate of 40,000,000 shares of
Common Stock (such warrants, the “CR Related Warrants”), and (ii) Elite will issue and deliver to Epic 7,000,000 shares of Common Stock
following the receipt by Elite from Epic of each written notice of Epic’s receipt from the FDA of approval for such Identified CR Products and/or
Additional CR Products, up to a maximum of an aggregate of 28,000,000 shares of Common Stock (such shares, the “CR Related Shares”).
With respect to each Identified IR Product and Additional IR Product developed by Epic at the Facility, (i) Elite will issue and deliver to Epic a
seven year warrant to purchase up to 4,000,000 shares of Common Stock, at an exercise price of $0.0625, following the receipt by Elite from Epic of
each written notice of Epic’s receipt of an acknowledgment from the FDA that the FDA accepted for filing an ANDA for such Identified IR Products
and/or Additional IR Products, up to a maximum of four such warrants for the right to purchase up to an aggregate of 16,000,000 shares of Common
Stock (such warrants, together with the CR Related Warrants, the “Milestone Warrants”), and (ii) Elite will issue and deliver to Epic 3,000,000
shares of Common Stock following the receipt by Elite from Epic of each written notice of Epic’s receipt from the FDA of approval for such Identified
IR Products and/or Additional IR Products, up to a maximum of an aggregate of 12,000,000 shares of Common Stock (such shares, together with
the CR Related Shares, the “Milestone Shares”). The Milestone Warrants may only be exercised by payment of the applicable cash exercise
price. Elite will have no obligation to register with the United States Securities and Exchange Commission (the “SEC”) or any state securities
commission the resale of the Milestone Shares, Milestone Warrants or the shares of Common Stock issuable upon exercise of the Milestone
Warrants.
43
�Subject to the mutual agreement of Epic and Elite with respect to the selection of Additional CR Products and/or Additional IR Products pursuant to
the Epic Strategic Alliance Agreement, Epic will have the sole right to make all decisions regarding all aspects of the Products, including, but not be
limited to, (i) research and development, formulation, studies and validation of each Product, (ii) identifying, evaluating and obtaining ingredients for
each Product, (iii) preparing and filing the ANDA for each Product with the FDA and addressing and handling all regulatory inquiries, audits and
investigations pertaining to the ANDA, and (iv) the manufacture, marketing, supply and commercialization of each Product. In addition, Epic would
be the sole and exclusive owner of all right, title and interest in and to each of the Products.
Pursuant to the Epic Strategic Alliance Agreement, the use by each of Elite and Epic of the other party’s confidential and proprietary information is
restricted by customary confidentiality provisions. Elite and Epic also agreed in the Epic Strategic Alliance Agreement to indemnify and hold each
other harmless from certain losses under the Epic Strategic Alliance Agreement.
Under certain circumstances Epic will be entitled to terminate the Term early in the event that the Facility is totally damaged or destroyed such that
the Facility is rendered wholly untenable. In addition, subject to certain exceptions, either Elite or Epic may terminate the Term at any time if the
other party is in breach of any material obligations under Article V of the Epic Strategic Alliance Agreement and has not cured such breach within
sixty days after receipt of written notice requesting cure of such breach.
Elite may also terminate the Term by written notice to Epic if (i) all conditions precedent that Elite is obligated to satisfy pursuant to Article II of
the Epic Strategic Alliance Agreement on or prior to a Closing (as defined in the Epic Strategic Alliance Agreement) have been, or will have been,
satisfied by Elite in accordance with the terms thereof and (ii) Epic does not consummate such Closing in accordance with Article II.
Notwithstanding the foregoing, if Elite terminates the Epic Strategic Alliance Agreement as described in this paragraph, then any and all product fees
to which it would otherwise be entitled will remain the obligation of Epic and must be paid to Elite in accordance with the terms of Epic Strategic
Alliance Agreement.
Infusion of Additional Capital Necessary for Product Development
In order to provide Elite with the additional capital necessary for the product development and synergies presented by the strategic relationship with
Epic, Epic agreed to invest $3.75 million in Elite through the purchase of Elite’s Series E Preferred Stock and common stock warrants. At the
Initial Closing, which occurred on June 3, 2009, in order to fund the continued development of Elite’s drug products, Elite issued and sold to the
Epic, in a private placement, pursuant to an exemption from registration under Section 4(2) of the Securities Act, 1,000 shares of its Series E
Convertible Preferred Stock, par value $0.01 per share (the “Series E Preferred Stock”), at a price of $1,000 per share, each share convertible, at
$0.05 per share (the “Conversion Price”), into 20,000 shares of Common Stock, par value $0.001 per share (the “Common Stock”). The Conversion
Price is subject to adjustment for certain events, including, without limitation, dividends, stock splits, combinations and the like. The Conversion
Price is also subject to adjustment for (a) the sale of Common Stock or securities convertible into or exercisable for Common Stock, for which
Epic’s consent was not required under the Certificate of Designation of Preferences, Rights and Limitations of the Series E Convertible Preferred
Stock, at a price less than the then applicable Conversion Price, (b) the issuance of Common Stock in lieu of cash in satisfaction of Elite’s dividend
obligations on outstanding shares of its Series B 8% Convertible Preferred Stock, par value $0.01 per share, Series C 8% Convertible Preferred
Stock, par value $0.01 per share, and/or Series D 8% Convertible Preferred Stock, par value $0.01 per share (the “Series D Preferred Stock”), and (c)
the issuance of Common Stock as a result of any holder of Series D Preferred Stock exercising its right to require Elite to redeem all of such holder’s
shares of Series D Preferred Stock pursuant to the terms thereof. Epic also acquired a warrant to purchase 20,000,000 shares of Common Stock (the
"Initial Warrant"), exercisable on or prior to June 3, 2016, at a per share exercise price of $0.0625 (the “Exercise Price”), subject to adjustments for
certain events, including, but not limited to, dividends, stock splits, combinations and the like. The Exercise Price of the Initial Warrant will also
be subject to adjustment for the sale of Common Stock or securities convertible into Common Stock, for which Epic’s consent was not required
under the Epic Strategic Alliance Agreement, at a price less than the then applicable Exercise Price of the Initial Warrant. Epic paid an aggregate
purchase price of $1,000,000 for the shares of Series E Preferred Stock and the Initial Warrant issued and sold by Elite to the Epic at the Initial
Closing, of which $250,000 was received by Elite, in the form of a cash deposit, on April 30, 2009, pursuant to the First Amendment. The
remaining $750,000 of such aggregate purchase price was paid to Elite by Epic at the Initial Closing.
44
�On October 30, 2009, Elite completed the second closing of the Strategic Alliance Agreement with Epic. Epic paid to Elite a sum of $1,000,000 in
exchange for an additional 1,000 shares of Series E Preferred Stock, and a warrant to purchase an additional 40,000,000 shares of Common
Stock. The warrant is to be exercisable until the date that is the seventh anniversary of the Second Closing Date and is to have a per share exercise
price equal to $0.0625, subject to adjustments for certain events, including, without limitation, dividends, stock splits, combinations and the like.
On March 31, 2011, Elite completed the third closing of the Strategic Alliance Agreement with Epic Epic paid to Elite a sum of $1,000,000 in
exchange for an additional 1,000 shares of Series E Preferred Stock, and a warrant to purchase an additional 40,000,000 shares of Common
Stock. The warrant is to be exercisable until the date that is the seventh anniversary of the Second Closing Date and is to have a per share exercise
price equal to $0.0625, subject to adjustments for certain events, including, without limitation, dividends, stock splits, combinations and the like.
In addition, within ten business days following the last day of each calendar quarter, beginning with the first calendar quarter following the Initial
Closing Date and continuing for each of the eleven calendar quarters thereafter, Epic will pay to Elite a sum of $62,500, for an aggregate purchase
price over such period of $750,000, in exchange for an additional 62.5 shares of Series E Preferred Stock per quarter and 750 shares of Series E
Preferred Stock, in the aggregate, over such period, which such shares will be convertible into 1,250,000 shares of Common Stock per quarter and
15,000,000 shares of Common Stock, in the aggregate, over such period, subject to adjustment. Epic made the first payment for the quarter ending
September 30, 2009.
If Elite determines, in its reasonable judgment, that additional funding is required for the development of its pharmaceutical products, then, either (i)
Elite will issue, and Epic will purchase, such additional number of shares of Series E Preferred Stock or Common Stock from Elite, upon such terms
and conditions as may be agreed upon by Elite and Epic at the time of such determination; or (ii) on or after September 15, 2011, Epic will provide
a loan to Elite, in an aggregate principal amount not to exceed $1,000,000, which such loan will (A) have an interest rate equal to the then prime
interest rate as published in the Wall Street Journal on the date of such loan, (B) mature on the second anniversary of date of such loan, and (C) be
on such other terms and conditions which are customary and reasonable to loans of a similar nature and which are mutually agreed upon between
Epic and Elite.
45
�Elite believes, which as to such belief there can be no assurances, the completion of the transactions contemplated by the Epic Strategic Alliance
Agreement creates value for our stockholders by adding a new revenue source for Elite upon the commercialization of the Epic products developed at
our facility, providing an experienced partner to assist in the development, manufacture and licensing of our pharmaceutical products, and
contributing funding for the products. Importantly, Elite will continue the development of its pain products and, with the help of Epic, work towards
securing licensing arrangements for such pain products.
Board of Directors Composition and Voting Rights
As of the Initial Closing Date and at all times thereafter, except as otherwise set forth in the Epic Strategic Alliance Agreement, Elite and its Board
of Directors will take any and all action necessary so that (i) the size of the Board of Directors will be set and remain at seven directors, (ii) three
individuals designated by Epic (the “Epic Directors”) will be appointed to the Board of Directors and (iii) the Epic Directors will be nominated at
each annual or special meeting of stockholders at which an election of directors is held or pursuant to any written consent of the stockholders;
provided, however, that if at any time following the Lock-Up Period (as defined above) the Purchaser owns less than (i) a number of shares of Series
E Preferred Stock equal to ninety percent of the aggregate number of shares of Series E Preferred Stock purchased by the Purchaser at all of the then
applicable Closings or (ii) following the conversion by the Purchaser of the Series E Preferred Stock, a number of shares of Common Stock equal to
ninety percent of the number of shares of Common Stock so converted, neither Elite nor its Board of Directors will be obligated to nominate Epic
Directors or take any other action with respect to those actions described in (i), (ii) and/or (iii) above. No Epic Director may be removed from office
for cause unless such removal is directed or approved by (x) a majority of the independent members of the Board of Directors and (y) all of the
non-affected Epic Director (s). Any vacancies created by the resignation, removal or death of an Epic Director will be filled by the appointment of an
additional Epic Director. Any Epic Director may be removed from office upon the request of the Purchaser, with or without cause. At such time as the
Purchaser owns more than 50% of the issued and outstanding Common Stock or other voting securities of Elite, the number of Epic Directors that
the Purchaser will be entitled to designate under the Epic Strategic Alliance Agreement will be equal to a majority of the Board of Directors.
The Series E Certificate provides that on any matter presented to the holders of our Common Stock for their action or consideration at any meeting of
our stockholders (or by written consent of stockholders in lieu of meeting), Epic, as a holder of Series E Preferred Stock, will be entitled to cast the
number of votes equal to the number of shares of Common Stock into which the shares of Series E Preferred Stock held by Epic are convertible as of
the record date for determining the stockholders entitled to vote on such matter. Except as provided by law or by the other provisions of the Series E
Certificate, Epic will vote together with the holders of Common Stock, as a single class.
In addition, pursuant to the Epic Strategic Alliance Agreement and the Series E Certificate, Elite has agreed that, between the date of the initial
closing under the Epic Strategic Alliance Agreement and the date which is the earlier of (x) the date the Epic Directors constitute a majority of the
Board of Directors and (y) ninety days following the fifth anniversary of the Initial Closing Date, except as Epic otherwise agrees in writing, Elite
may conduct its operations only in the ordinary and usual course of business consistent with past practice. Further, pursuant to the Epic Strategic
Alliance Agreement and the Series E Certificate, Elite must obtain the prior written consent of Epic in order to take the actions specifically
enumerated therein.
For information regarding composition of the Board and voting rights in connection with the Epic Strategic Alliance Agreement, refer to the “Risk
Factors” under Item 1A, of this Annual Report on Form 10K and our Current Reports on Form 8K, filed with the SEC on March 23, 2009, May
6, 2009 and June 5, 2009, which are incorporated herein by reference.
46
�Novel Labs Investment
At the end of 2006, Elite entered into a joint venture with VGS Pharma, LLC (“VGS”) and created Novel Laboratories, Inc. (“Novel”), a
privately-held company specializing in pharmaceutical research, development, manufacturing, licensing, acquisition and marketing of specialty
generic pharmaceuticals. Novel's business strategy is to focus on its core strength in identifying and timely executing niche business opportunities in
the generic pharmaceutical area. Elite’s ownership interest in Novel’s Class A Voting Common Stock of Novel is approximately 10% of the
outstanding shares of Class A Voting Common Stock of Novel. As of October 1, 2007, Elite deconsolidated its financial statements from Novel and
the investment in Novel is accounted for under the cost method of accounting.
Since its inception, Novel has filed at least 11 Abbreviated New Drug Applications with the US Food and Drug Administration. The first ANDA
approval for Novel was received in Dec 2008 and at least three additional ANDA approvals were received in 2009. Four of the Novel ANDAs have
been granted first-to-file status.
In addition, Novel has acquired three ANDAs to supplement its own inhouse product development and marketing strategy. Novel has publicly said
that it has identified over 50 drug products which are in various stages of development that it plans to commercialize in the coming years.
We also know from public information that Perrigo Company acquired rights in 2010 for an undisclosed amount to an additional Novel ANDA
approved in 2010 for the product HalfLytely®. Novel believes this is a first to file ANDA. Perrigo expects to be in a position to launch a generic
version of this product later this year and they expect to have 180 days of generic exclusivity. Novel will manufacture the product exclusively for
Perrigo. Annual sales for the branded product was approximately $80 million according to Wolters Kluwer.
In accordance with GAAP, the Company records an impairment write-down to such investments when the cost of the investment exceeds its fair
value and when the decline in value is determined to be other-than temporary. Indicators of an other-than-temporary decline in value include, without
limitation, the following:
∙
A significant deterioration in the earnings performance, credit rating, asset quality, or business prospects of the investee
∙
A significant adverse change in the regulatory, economic, or technological environment of the investee
∙
A significant adverse change in the general market condition of either the geographic area or the industry in which the investee operates
∙∙ A bona fide offer to purchase (whether solicited or unsolicited), an offer by the investee to sell, or a completed auction process for the same
∙
or similar security for an amount less than the cost of the investment
Factors that raise significant concerns about the investee's ability to continue as a going concern, such as negative cash flows from
operations, working capital deficiencies, or noncompliance with statutory capital requirements or debt covenants.
A review and assessment of all documents available, public announcements by Novel and communications with the management of Novel does not
indicate the existence of impairment indicators. Accordingly, the Company determined that no impairment is required in the valuation of its
investment in Novel as of March 31, 2011. The valuation of the Company’s investment in Novel remains at $3,329,322, an amount equal to the
valuation as of March 31, 2010 with no impairment write downs.
47
�Elite’s Purchase of a Generic Hydromorphone HCl Product
On May 18, 2010, Elite executed an asset purchase agreement with Mikah Pharma LLC (“Mikah”) (the “Hydromorphone Agreement”). Pursuant to
the Hydromorphone Agreement, the Company acquired from Mikah an Abbreviated New Drug Application for Hydromorphone Hydrochloride
Tablets USP, 8 mg, for aggregate consideration of $225,000, comprised of an initial payment of $150,000, which was made on May 18, 2010. A
second payment of $75,000 was due to be paid to Mikah on June 15, 2010, with the Company having the option to make this payment in cash or
by issuing to Mikah 937,500 shares of the Company’s common stock. The Company elected and did issue 937,500 shares of Common Stock
during the quarter ended December 31, 2010, in full payment of the $75,000 due to Mikah pursuant to the asset purchase agreement dated May 18,
2010. A current report on form 8K was filed on May 24, 2010 in relation to this announcement, such filing being incorporated herein by this
reference.
For further details on the Hydromorphone Agreement, please refer to Exhibit 10.4 to the Quarterly Report on Form 10-Q, filed with the SEC on
November 15, 2010, and incorporated herein by reference.
On May 31, 2011, the Company received a letter from the US Food and Drug Administration (FDA) responding to a Changes Being Effected in 30
Days (“CBE 30”) supplement filed by the Company with the agency to change the manufacturing and packaging location of the Hydromorphone
Hydrochloride Tablets USP, 8 mg ANDA purchased from Mikah Pharma. The letter from the FDA informed the Company that the agency has
reclassified the application as a prior approval supplemental application which will delay the commercialization. A current report on form 8K was
filed on June 6, 2011 in relation to this announcement, such filing being incorporated herein by this reference.
As a result of the delay in commercialization resulting from the reclassification of the Company’s application, the Company recorded an impairment
of the ANDA asset acquired from Mikah Pharma pursuant to the Hydromorphone Agreement in an amount equal to the entire purchase price of the
acquisition.
This product is included in the license and manufacturing agreements executed with Precision Dose Inc (“Precision Dose”) and its wholly owned
subsidiary, TAGI Pharma Inc (“TAGI”) and dated September 10, 2010. A current report on form 8K was filed on September 16, 2010, in relation
to the signing of this agreement, such filing being herein incorporated by reference.
Elite’s Purchase of a Generic Naltrexone Product
On August 27, 2010, Elite executed an asset purchase with Mikah (the “Naltrexone Agreement”). Pursuant to the Naltrexone Agreement, Elite
acquired from Mikah the Abbreviated New Drug Application number 75-274 (Naltrexone Hydrochloride Tablets USP, 50 mg), and all amendments
thereto (the “ANDA”), that have to date been filed with the FDA seeking authorization and approval to manufacture, package, ship and sell the
products described in the ANDA within the United States and its territories (including Puerto Rico) for aggregate consideration of $200,000. In lieu
of cash, Mikah agreed to accept from Elite product development services to be performed by Elite. A current report on form 8K was filed on August
27, 2010 in relation to this announcement, such filing being incorporated herein by this reference. Please also refer to exhibit 10.5 of the Quarterly
Report on Form 10-Q filed with SEC on November 15, 2010, such filing being incorporated herein by this reference.
48
�The transfer of production of Naltrexone Hydrochloride Tablets USP, 50mg (“Naltrexone 50mg Tablets”) from Mikah to the Facility is currently in
progress. Such transfer of production, however, will include the filing of a CBE 30 supplement which is similar in relevant aspects to the CBE 30
supplement filed for the site transfer of the manufacture of Hydromorphone 8mg. It is possible that FDA’s response to a CBE 30 supplement filed for
transfer of the manufacturing site of Naltrexone 50mg, may be similar to its response to the CBE 30 supplement filed for the transfer of the
manufacturing site of Hydromorphone 8mg. Accordingly, Elite has recorded an impairment, equal to the full historical cost of the Naltrexone 50mg
ANDA.
Elite’s Purchase of a Generic Phentermine Product
On September 10, 2010, Elite, together with its subsidiary, Elite Laboratories, Inc., executed a Purchase Agreement (the “Phentermine Purchase
Agreement”) with Epic Pharma LLC (the “Seller”) for the purpose of acquiring from the seller an Abbreviated New Drug Application for a generic
phentermine product (the “Phentermine ANDA”), with such being filed with, but not yet approved by the FDA at the time the Phentermine
Purchase Agreement was executed. On February 4, 2011, the Company announced the approval by the FDA of the Phentermine ANDA. As per the
terms and conditions of the Phentermine Purchase Agreement, the acquisition of the Phentermine ANDA will close on the later of 60 days from the
date of the Purchase Agreement or upon receipt of FDA approval of the Phentermine ANDA. Upon the closing, Elite will pay a portion of the
purchase price. The remainder of the purchase price will be paid in quarterly installments over a period of three years, beginning at the end of the
first full quarter following the closing. Current reports on form 8K were filed on September 10, 2010 and February 4, 2011 in relation to the
Phentermine Purchase Agreement and the Phentermine ANDA, with such filings being incorporated herein by this reference. Please also refer to
exhibit 10.7 of the Quarterly Report on Form 10-Q filed with SEC on November 15, 2010, such filing being incorporated herein by this reference.
This product is being marketed and distributed by Precision Dose Inc (“Precision Dose”) and its wholly owned subsidiary, TAGI Pharma Inc.
(“TAGI”) pursuant license and manufacturing agreements dated September 10, 2010. A current report on form 8K was filed on September 16, 2010
in relation to signing of this agreement, such filing being incorporated herein by this reference
Licensing Agreement with Precision Dose Inc.
On September 10, 2010, Elite Pharmaceuticals Inc. (“Elite”) executed a License Agreement with Precision Dose, Inc. (“Precision Dose”) to market
and sell four Elite generic products, consisting of Hydromorphone, Naltrexone, Phentermine 37.5mg tablets (“Phentermine 37.5mg”) and one
additional generic products for which an ANDA has been filed but not yet approved by the FDA., through its wholly-owned subsidiary, TAGI
Pharma, Inc. in the United States, Puerto Rico and Canada. Precision Dose will have the exclusive right to market the products in the United States
and Puerto Rico and a nonexclusive right to market the products in Canada. Pursuant to the License Agreement, Elite will receive a license fee and
milestone payments. The license fee will be computed as a percentage of the gross profit, as defined in the License Agreement, earned by Precision
Dose as a result of sales of the products. The license fee is payable monthly for the term of the License Agreement. The milestone payments will be
paid in 6 installments. The first installment was paid upon execution of the License Agreement. The remaining installments are to be paid upon
FDA approval and initial shipment of the products to Precision Dose. The term of the License Agreement is 15 years and may be extended for 3
successive terms, each of 5 years. A current report on form 8K was filed on September 10, 2010 in relation to this announcement, such filing being
incorporated herein by this reference. Please also refer to exhibits 10.8 and 10.9 of the Quarterly Report on Form 10Q filed with SEC on November
15, 2010, such filings being incorporated herein by this reference.
49
�Manufacturing and Supply Agreement with Mikah Pharma LLC
On June 1, 2011, Elite Pharmaceuticals Inc. (“Elite”) executed a Manufacturing and Supply Agreement (the “Agreement”) with Mikah Pharma, LLC
(“Mikah”) to undertake and perform certain services relating to two generic products: Isradipine Capsules USP, 2.5 mg and 5 mg and
Phendimetrazine Tartrate Tablets USP, 35 mg (the “Products”), including (a) developing and preparing the documentation required for the transfer of
the manufacturing process to Elite’s facility and the appropriate regulatory filing for the ANDA, and (b) manufacturing finished dosage forms
appropriate for commercial sale, marketing and distribution in the United States of America, its territories, possessions, and commonwealths in
accordance with the requirements of this Agreement; Elite shall perform, at its sole cost and expense, all Technology Transfer, validation and
qualification services (including: equipment, methods and facility qualification), validation and stability services required by Applicable Laws to
commence manufacturing the Products for commercial sale by Mikah or its designees in accordance with the terms of this Agreement. During the
term of this Agreement and subject to the provisions herein, Mikah shall purchase from Elite and Elite agrees to manufacture and supply solely and
exclusively to Mikah, such Product as Mikah may order from time to time pursuant to this Agreement. Mikah will compensate Elite at an agreed
upon transfer price for the manufacturing and packaging of the Products. For the Isradipine product, Elite will also receive a 10% royalty on net
profits of the finished Product. The payment is to be calculated and paid quarterly. Elite will also receive a onetime milestone payment for each
Product for the work associated with the Technology transfer. The milestone payment shall be made upon the successful manufacturing and testing of
the exhibit batch.
The Manufacturing and Supply Agreement has a term of five (5) years and shall automatically renew for additional periods of one (1) year unless
Mikah provides written notice of termination to Elite at least six (6) months prior to the expiration of the Term or any Renewal Term.
A current report on Form 8K was filed on June 6, 2011, with such filing being herein incorporated by reference. Please also refer to exhibit 10.70 to
this annual report on Form 10-K.
Critical Accounting Policies and Estimates
Management’s discussion addresses our Consolidated Financial Statements, which have been prepared in accordance with accounting principles
generally accepted in the United States of America. The preparation of these financial statements requires management to make estimates and
assumptions that affect the reported amounts of assets and liabilities, the disclosure of contingent assets and liabilities at the date of financial
statements and the reported amounts of revenues and expenses during the reporting period. On an ongoing basis, management evaluates its estimates
and judgment, including those related to bad debts, intangible assets, income taxes, workers compensation, and contingencies and litigation.
Management bases its estimates and judgments on historical experience and on various other factors that are believed to be reasonable under the
circumstances, the results of which form the basis for making judgments about the carrying values of assets and liabilities that are not readily
apparent from other sources. Actual results may differ from these estimates under different assumptions or conditions.
50
�Management believes the following critical accounting policies, among others, affect its more significant judgments and estimates used in the
preparation of its Consolidated Financial Statements. Our most critical accounting policies include the recognition of revenue upon completion of
certain phases of projects under research and development contracts. We also assess a need for an allowance to reduce our deferred tax assets to the
amount that we believe is more likely than not to be realized. We assess the recoverability of inventory, long-lived assets and intangible assets
whenever events or changes in circumstances indicate that the carrying value of the asset may not be recoverable. We assess our exposure to current
commitments and contingencies. It should be noted that actual results may differ from these estimates under different assumptions or conditions.
Liquidity and Capital Resources
As of March 31, 2011, our principal source of liquidity was approximately $1.8 million of cash and cash equivalents. Our strategic alliance with
Epic may also generate (i) an additional $0.6875 million in cash proceeds to us through Epic’s purchase of additional shares of Series E Preferred
Stock over the course of additional closings pursuant to the terms and conditions of the Epic Strategic Alliance Agreement and (ii) profit sharing in
the revenue from commercialized products which were developed at Elite’s Facility pursuant to the Epic Strategic Alliance Agreement. However, no
assurance can be given that we will consummate such additional closings of the transactions contemplated by, or successfully commercialize the
products developed under, the Epic Strategic Alliance Agreement. If adequate funds are not available to us as we need them, it would raise
substantial doubt about our ability to continue as a going concern.
From time to time we will consider potential strategic transactions including acquisitions, strategic alliances, joint ventures and licensing
arrangements with other pharmaceutical companies. There can be no assurance that any such transaction will be available or consummated in the
future.
For the year ended March 31, 2011, operating activities provided the Company with $1.5 million in cash, with an additional $1.0 million in cash
being provided by net financing activities. The cash provided by net financing activities was primarily from $1.0625 million in gross proceeds
realized from the issuance of Series E Preferred Stock pursuant to the Epic Strategic Alliance Agreement. The Company expended $1.4 million in
investing activities, with such amount mostly consisting of $0.9 million in costs incurred for intellectual property assets, $0.3 million in leasehold
improvements and $0.2 million for the purchase of manufacturing equipment. Cash and cash equivalents at March 31, 2011 were $1.8 million, an
increase of $1.2 million from the $0.6 million of cash and cash equivalents on hand at March 31, 2010.
The Company’s working capital at March 31, 2011 was negative $1.5 million, compared with a working capital at March 31, 2010 of negative $2.3
million.
On March 31, 2011, we consummated the Third Closing of the transactions contemplated by the Epic Strategic Alliance Agreement and received
from Epic cash payments of $1,000,000 in exchange for 1,000 shares of our Series E Preferred Stock. These funds provide us with the additional
capital necessary for the development of both the product and the business synergies contemplated by the Epic Strategic Alliance Agreement.
On September 29, 2010, the Company issued 62.5 shares of Series E Preferred Stock, in exchange for $62,500 which was received from Epic on
November 12, 2009. The Epic Strategic Alliance Agreement also contemplates an additional 11 payments of $62,500, over the next three years,
which could generate an additional $687,500 in cash proceeds through Epic’s purchase of additional shares of Series E Preferred Stock.
51
�The Company had outstanding, as of March 31, 2011, bonds in the aggregate principal amount of $3,385,000 consisting of $3,140,000 of 6.5% tax
exempt bonds with an outside maturity of September 1, 2030 and $245,000 of 9.0% bonds with an outside maturity of September 1, 2012 (together,
the “NJEDA Bonds”). The NJEDA Bonds are secured by a first lien on the Facility in Northvale, New Jersey. Pursuant to the terms of the NJEDA
Bonds, a restricted cash account has been established for the payment of bond principal and interest, in the event that the Company does not make
such payments when due. Bond proceeds were utilized for the redemption of previously issued tax exempt bonds issued by the Authority in
September 1999 and to refinance equipment financing, as well as provide approximately $1,000,000 of capital for the purchase of additional
equipment for the manufacture and development at the Facility of pharmaceutical products and the maintenance of a $388,990 debt service reserve (the
“Debt Service Reserve Fund”) to be held in the restricted cash account established with the Trustee for the NJEDA Bonds. All proceeds from the
NJEDA Bonds, other than the amount used to establish the Debt Service Reserve Fund, were expended within the year ended March 31, 2007.
The NJEDA Bonds require the Company to make an annual principal payment on September 1st of varying amounts as specified in the loan
documents and semi-annual interest payments on March 1st and September 1st, equal to interest due on the outstanding principal at the applicable
rate for the semi-annual period just ended.
The principal payment due on September 1, 2009, totaling $210,000, the interest payment due on September 1, 2009, totaling and interest
payments due on March 1, 2010, September 1, 2010 and March 1, 2011 totaling $113,075 each, were all paid from the Debt Service Reserve Fund,
due to the Company not having sufficient available funds to make such payments when due.
The Company did not have sufficient funds available to make the principal payments due on September 1, 2010, totaling $200,000, and requested
the Trustee to withdraw the funds from the debt services reserve held in the restricted cash account and to utilize such funds to make the principal
payment due. The Company’s request was denied by the Trustee. Accordingly, the principal payment due on September 1, 2010 was not paid.
Non-payment of the amounts when due, even if such payment is made from the Debt Service Reserve Fund, constitute an Event of Default under the
NJEDA Bonds and the loan document executed with NJEDA Bonds. Pursuant to the terms of the NJEDA Bonds, the Company is required to
replenish any amounts withdrawn from the Debt Service Reserve Fund and used to make principal or interest payments in six monthly installments,
each being equal to one-sixth of the amount withdrawn and with the first installment due on the 15th of the month in which the withdrawal from
Debt Service Reserve Fund occurred and the remaining five monthly payments being due on the 15th of the five immediately subsequent months.
The Company has, to date, made all payments required in relation to the withdrawals made from the debt service reserve on September 1, 2009
March 1, 2010 and September 1, 2010. The Company is required to make two additional payments of $19,529 each, on July 15, 2011 and August
15, 2011, in order to fully replenish the March 1, 2011 withdrawal from the debt service reserve.
The Company has received Notice of Default from the Trustee of the NJEDA Bonds in relation to the withdrawals from the Debt Service Reserve
Fund and nonpayment of the Company’s obligation when due. The Company has requested a postponement of principal payments due on
September 1st of 2010, 2011 and 2012, with an aggregate of all such postponed principal payments being added to the principal payments due on
September 1, 2013. Resolution of the Company’s default under the NJEDA Bonds and our request for postponement of principal payments will
have a significant effect on our ability to operate in the future.
Until the event of default is waived or rescinded, the Company has classified the entire principal due, an amount aggregating $3.385 million, as a
current liability.
The Trustee’s remedies on default include declaring the NJEDA Bonds due and payable and exercising rights against the collateral provided to
secure the NJEDA Bonds.
52
�Results of Operations:
Year Ended March 31, 2011 as compared to the Year Ended March 31, 2010
Elite’s revenues for the year ended March 31, 2011 were $4,265,963, an increase of $921,664 over revenues for the prior year, and consisted of
$3,086,183 in manufacturing fees, $831,538 in royalty fees and $348,242 in contract lab service fees. Revenues for the year ended March 31, 2010
consisted of $2,575,942 in manufacturing fees, $763,928 in royalty fees and $4,429 in contract lab service fees. Manufacturing fees increased by
approximately 20% and royalties increased by approximately 9% due to growth of product sales.
Research and development costs for the year ended March 31, 2011 were $1,385,211, an increase of $590,778, or approximately 74%, from $794,433
of such costs for the prior year. Increases in research and development costs were mainly attributable to charges recorded as a result of the FDA’s
reclassification of the Company’s application for transferring of the site of manufacture of Hydromorphone 8mg, costs related to the transfer of
production of new products acquired by the Company during the year and an increase in research and development activities. Research and
development costs are expected to increase, in future periods, once Phase III and other clinical trials for ELI-216 are initiated.
General and administrative expenses for the year ended March 31, 2011, were $876,012, a decrease of $965,413, or approximately 52% from
$1,841,425 of general and administrative expenses for the prior year. The decrease was primarily attributable to decreases in salaries and fringe
benefits from Elite’s force reduction and management’s continued cost reduction efforts.
Non-cash compensation satisfied by the issuance of stock options and warrants decreased $82,987 to $42,017 for the year ended March 31, 2011 from
$125,004 for the year ended March 31, 2010. Decreases were the result of previously issued options becoming vested and forfeitures as a result of the
reduction in workforce.
Depreciation and amortization decreased by $40,592, or approximately 19%, from $213,955 for the prior year to $173,363. While depreciation
expense for the year ended March 31, 2011 decreased from the prior year, please note that during the year ended March 31, 2011, we acquired
equipment costing approximately $180k and invested approximately $340k in leasehold improvements. Neither the equipment nor the leasehold
improvements were placed in service during the year ended March 31, 2011, but we anticipate both to be placed in service during the year
immediately subsequent to March 31, 2011. Accordingly, depreciation expenses in future years are expected to increase. Other income (expenses) for
the year ended March 31, 2011 were $(13,125,979) compared to (expenses) of $(6,120,553) for the year ended March 31, 2010. The decrease in other
income (expenses) was due to derivative expenses related to changes in the fair value of our preferred shares and outstanding warrants of $(11,714,372
), derivative interest expense of $(1,259,480 ) and discount in Series E issuance attributable to beneficial conversion features of ($292,213 ),
impairment of intangible assets of ($440,000), offset by sales of New Jersey Net Operating Losses of $311,835 and proceeds received pursuant to the
settlement of litigation with The Pharma Network totaling $500,000.
As a result of the foregoing, Elite’s net loss for the year ended March 31, 2011 was $13,582,159 compared to a net loss of $8,056,874 for the year
ended March 31, 2010.
53
�Material Changes in Financial Condition
Our working capital (total current assets less total current liabilities), increased to a working capital deficiency of $1,521,959 as of March 31, 2011
from a working capital deficiency of $2,274,572 as of March 31, 2010, primarily due to net proceeds received as a result of our private placement of
Series E Convertible Preferred Stock, and by net cash provided by operations.
We experienced positive cash flows from operations of $1,552,815 for the year ended March 31, 2011, primarily due to our net loss of $13,582,159,
offset by non-cash expenses totaling $14,474,751, included in the net loss, combined with a decrease in inventory of $754,931.
On November 15, 2004 and on December 18, 2006, Elite’s partner, ECR, launched Lodrane 24® and Lodrane 24D®, respectively. Under its
agreement with ECR, Elite manufactured, through April 2011, commercial batches of Lodrane 24® and Lodrane 24D® in exchange for
manufacturing margins and royalties on product revenues. Manufacturing revenues and royalty income earned for the year ended March 31, 2011 was
$3,086,183 and $831,538, respectively. In addition, the Company earned $348,242 from contract lab services related to the Lodrane
Products. Gross revenues earned in relation to the Lodrane Products equaled 98% of the Company’s revenues for the year ended March 31, 2011.
On March 3, 2011, the USFDA announced its intention to remove approximately 500 cough/cold and allergy related products from the U.S.
market, with Lodrane 24® and Lodrane 24D® being included in such list. According to the press release issued by the USFDA, manufacturers
must stop manufacturing the affected products within 90 days of March 3, 2011 and distribution of the affected products must stop within 180 days of
March 3, 2011. Elite’s customer for Lodrane 24® and Lodrane 24D® cancelled all outstanding orders, other than those orders for which
manufacturing had commenced, citing the announcement by the USFDA and advising that existing stocks of Lodrane 24® and Lodrane 24D® were
sufficient and that additional quantities could not be sold prior to the 180 day distribution deadline announced by the US-FDA.
While the timing of the announcement by the USFDA resulted in such having a minimal effect on the Company’s results for the year ended March
31, 2011, the Company’s inability to manufacture Lodrane 24® and Lodrane 24D® has a material and adverse effect on its revenues for period
beginning after March 31, 2011.
Please refer to the Current Report on Form 8-K filed with the SEC on March 4, 2011, such filing being herein incorporated by reference, for further
details.
ECR (the owner and marketer of the Lodrane Products) has initiated a formal approval process with the FDA in 2010 regarding the Lodrane Products
and issued a press release on March 3, 2011 stating that they will continue to actively pursue approval for the Lodrane products. In addition, on
April 29, 2011, ECR filed a Petition for Review with the United States Court of Appeals for the District of Columbia, petitioning such court to
review and set aside the final order of the US-FDA with relation to the Lodrane Products.
Off-balance sheet arrangements
None.
ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK
Not applicable to smaller reporting companies
54
�ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA
Attached hereto and filed as a part of this Annual Report on Form 10-K are our Consolidated Financial Statements, beginning on page F-1.
ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL
DISCLOSURE
None
ITEM 9A. CONTROLS AND PROCEDURES
Evaluation of Disclosure Controls and Procedures
Under the supervision and with the participation of our management, including the Chief Executive and Chief Financial Officers, we evaluated the
effectiveness of the design and operation of our disclosure controls and procedures (as defined in Rule 13a-15(e) and 15d-15(e) under the Securities
Exchange Act of 1934 (the “Exchange Act”) as of the end of the period covered by this Annual Report on Form 10K. Based upon that evaluation,
our Chief Executive and Chief Financial Officers concluded that our disclosure controls and procedures as of the end of the period covered by this
report were not effective so that that the information required to be disclosed by us in reports filed under the Exchange Act is (i) recorded, processed,
summarized and reported within the time periods specified in the SEC’s rules and forms and (ii) accumulated and communicated to our management
to allow for timely decisions regarding disclosure. A controls system cannot provide absolute assurance, however, that the objectives of the controls
system are met, and no evaluation of controls can provide absolute assurance that all control issues and instances of fraud, if any, within a company
have been detected.
Management has determined that, as of March 31, 2011, there were material weaknesses in both the design and effectiveness of our internal control
over financial reporting. A material weakness is a deficiency, or a combination of deficiencies, in internal control over financial reporting such that
there is a reasonable possibility that a material misstatement of our annual or interim financial statements will not be prevented or detected on a
timely basis.
The deficiencies in our internal controls over financial reporting and disclosure controls and procedures are related to the lack of segregation of duties
due to the size of our accounting department, which replaced an outside accounting firm and non-employee Chief Financial Officer on July 1, 2009,
and limited enterprise resource planning systems. When our financial position improves, we intend to hire additional personnel and implement
enterprise resource planning systems required to remedy such deficiencies.
55
�Management's Annual Report on Internal Control over Financial Reporting
Our management is responsible for establishing and maintaining adequate internal control over financial reporting. Our internal control over financial
reporting has been 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 in the United States of America (“GAAP”).
Our internal control over financial reporting includes policies and procedures that pertain to the maintenance of records that, in reasonable detail,
accurately and fairly reflect transactions and dispositions of our assets; provide reasonable assurance that transactions are recorded as necessary to
permit preparation of financial statements in accordance with accounting principles generally accepted in the United States of America, that receipts
and expenditures are being made only in accordance with authorization of our management and directors; and provide reasonable assurance regarding
prevention or timely detection of unauthorized acquisition, use or disposition of our assets that could have a material effect on our financial
statements.
Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements or fraudulent actions. Therefore,
even those systems determined to be effective can provide only reasonable assurance with respect to financial statement preparation and presentation.
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.
This annual report does not include an attestation report of our registered public accounting firm regarding internal control over financial reporting.
Management's report was not subject to attestation by our registered public accounting firm pursuant to temporary rules of the SEC that permit us to
provide only management's report in this annual report.
Our management assessed the effectiveness of our internal control over financial reporting as of March 31, 2011. In making this assessment,
management used the criteria set forth by the Committee of Sponsoring Organizations of the Treadway Commission in Internal Control—Integrated
Framework. Based on that assessment under those criteria, management has determined that, at March 31, 2011, there were material weaknesses in
both the design and effectiveness of our internal control over financial reporting. A material weakness is a deficiency, or a combination of
deficiencies, in internal control over financial reporting such that there is a reasonable possibility that a material misstatement of our annual or
interim financial statements will not be prevented or detected on a timely basis.
The deficiencies in our internal controls over financial reporting and disclosure controls and procedures are related to the lack of segregation of duties
due to the size of our accounting department, which replaced an outside accounting firm and non-employee Chief Financial Officer on July 1, 2009,
and limited enterprise resource planning systems. When our financial position improves, we intend to hire additional personnel and implement
enterprise resource planning systems required to remedy such deficiencies.
Changes in Internal Control over Financial Reporting
There have been no changes in our internal control over financial reporting (as such term is defined in Rules 13a15(f) and 15d15(f) under the
Exchange Act) during the fourth quarter of fiscal year 2010 that have materially affected, or are reasonably likely to materially affect, our internal
control over financial reporting.
56
�ITEM 9B. OTHER INFORMATION
PART III
ITEM 10. DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE
Directors
The information concerning our directors required under this Item is incorporated herein by reference from our proxy statement, which will be filed
with the Securities and Exchange Commission, relating to our 2011 Annual Meeting of Stockholders (2011 Proxy Statement).
Executive Officers
The information concerning Elite’s executive officers is incorporated herein by reference from our 2011 Proxy Statement,
Code of Ethics
At the first meeting of the Board of Directors following the annual meeting of stockholders held on June 22, 2004, the Board of Directors adopted a
Code of Business Conduct and Ethics that is applicable to the Company’s directors, officers and employees. A copy of the Code of Business
Conduct and Ethics is available on our website at www.elitepharma.com, under Investor Relations.
Audit Committee
The information concerning our Audit Committee is incorporated herein by reference from our 2011 Proxy Statement.
Audit Committee Financial Experts
The information concerning our Audit Committee Financial Experts is incorporated herein by reference from our 2011 Proxy Statement.
ITEM 11. EXECUTIVE COMPENSATION
The information required under this Item is incorporated herein by reference from our 2011 Proxy Statement.
ITEM 12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED
STOCKHOLDER MATTERS
Information required by this item is incorporated by reference from the discussion under the headings Equity Compensation Plan Information in our
2011 Proxy Statement.
ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS AND DIRECTOR INDEPENDENCE
The information required under this Item is incorporated herein by reference from our 2011 Proxy Statement.
ITEM 14. PRINCIPAL ACCOUNTING FEES AND SERVICES
Information about the fees for 2010 and 2009 for professional services rendered by our independent registered public accounting firm is incorporated
herein by reference from our 2011 Proxy Statement. Our Audit Committee’s policy on preapproval of audit and permissible nonaudit services of our
independent registered public accounting firm is incorporated by reference from our 2011 Proxy Statement.
57
�ITEM 15. EXHIBITS, FINANCIAL STATEMENTS AND SCHEDULES.
(a)
The following are filed as part of this Annual Report on Form 10-K
PART IV
(1)
(2)
The financial statements and schedules required to be filed by Item 8 of this Annual Report on Form 10-K and listed in the Index
to Consolidated Financial Statements.
The Exhibits required by Item 601 of Regulation SK and listed below in the “Index to Exhibits required by Item 601 of
Regulation SK.”
(b)
(c)
The Exhibits are filed with or incorporated by reference in this Annual Report on Form 10-K
None
Index to Exhibits required by Item 601 of Regulation S-K.
Exhibit
No.
3.1(a)
3.1(b)
3.1(c)
3.1(d)
Description
Certificate of Incorporation of the Company, together with all other amendments thereto, as filed with the Secretary of State of the
State of Delaware, incorporated by reference to (a) Exhibit 4.1 to the Registration Statement on Form S-4 (Reg. No. 333-101686),
filed with the SEC on December 6, 2002 (the “Form S4”), (b) Exhibit 3.1 to the Company’s Current Report on Form 8K dated
July 28, 2004 and filed with the SEC on July 29, 2004, (c) Exhibit 3.1 to the Company’s Current Report on Form 8K dated
June 26, 2008 and filed with the SEC on July 2, 2008, and (d) Exhibit 3.1 to the Company’s Current Report on Form 8K dated
December 19, 2008 and filed with the SEC on December 23, 2008.
Certificate of Designations, Preferences and Rights of Series A Preferred Stock, as filed with the Secretary of the State of Delaware,
incorporated by reference to Exhibit 4.5 to the Current Report on Form 8-K dated October 6, 2004, and filed with the SEC on
October 12, 2004.
Certificate of Retirement with the Secretary of the State of the Delaware to retire 516,558 shares of the Series A Preferred Stock, as
filed with the Secretary of State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K dated
March 10, 2006, and filed with the SEC on March 14, 2006.
Certificate of Designations, Preferences and Rights of Series B 8% Convertible Preferred Stock, as filed with the Secretary of the
State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K dated March 15, 2006, and filed
with the SEC on March 16, 2006.
58
�3.1(e)
3.1(f)
3.1(g)
3.1(h)
3.1(i)
3.1(j)
3.1(k)
3.1(l)
Amended Certificate of Designations of Preferences, Rights and Limitations of Series B 8% Convertible Preferred Stock, as filed
with the Secretary of State of the State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K
dated April 24, 2007, and filed with the SEC on April 25, 2007.
Certificate of Designations, Preferences and Rights of Series C 8% Convertible Preferred Stock, as filed with the Secretary of the
State of Delaware, incorporated by reference to Exhibit 3.2 to the Current Report on Form 8-K dated April 24, 2007, and filed with
the SEC on April 25, 2007.
Amended Certificate of Designations, Preferences and Rights of Series C 8% Convertible Preferred Stock, as filed with the Secretary
of the State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K dated April 24, 2007, and
filed with the SEC on April 25, 2007
Amended Certificate of Designations of Preferences, Rights and Limitations of Series B 8% Convertible Preferred Stock, as filed
with the Secretary of State of the State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K
dated September 15, 2008, and filed with the SEC on September 16, 2008.
Amended Certificate of Designations, Preferences and Rights of Series C 8% Convertible Preferred Stock, as filed with the Secretary
of the State of Delaware, incorporated by reference to Exhibit 3.2 to the Current Report on Form 8-K dated September 15, 2008,
and filed with the SEC on September 16, 2008.
Amended Certificate of Designations of Preferences, Rights and Limitations of Series D 8% Convertible Preferred Stock, as filed
with the Secretary of State of the State of Delaware, incorporated by reference to Exhibit 3.3 to the Current Report on Form 8-K
dated September 15, 2008, and filed with the SEC on September 16, 2008.
Certificate of Designation of Preferences, Rights and Limitations of Series E Convertible Preferred Stock, as filed with the Secretary
of State of the State of Delaware, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K dated June 1, 2009,
and filed with the SEC on June 5, 2009.
Amended Certificate of Designations of the Series D 8% Convertible Preferred Stock as filed with the Secretary of State of the State
of Delaware on June 29, 2010, incorporated by reference to Exhibit 3.1 to the Current Report on Form 8-K, dated June 24, 2010
and filed with the SEC on July 1, 2010
3.1(m)
Amended Certificate of Designations of the Series E Convertible Preferred Stock as filed with the Secretary of State of the State of
Delaware on June 29, 2010, incorporated by reference to Exhibit 3.2 to the Current Report on Form 8-K, dated June 24, 2010 and
filed with the SEC on July 1, 2010
3.2
ByLaws of the Company, as amended, incorporated by reference to Exhibit 3.2 to the Company’s Registration Statement on Form
SB2 (Reg. No. 33390633) made effective on February 28, 2000 (the “Form SB2”).
4.1
Form of specimen certificate for Common Stock of the Company, incorporated by reference to Exhibit 4.1 to the Form SB-2.
59
�4.2
Form of specimen certificate for Series A 8% Convertible Preferred Stock of the Company, incorporated by reference to Exhibit 4.5
to the Current Report on Form 8-K, dated October 6, 2004, and filed with the SEC on October 12, 2004.
4.3
Form of specimen certificate for Series B 8% Convertible Preferred Stock of the Company, incorporated by reference to Exhibit 4.1
to the Current Report on Form 8-K, dated March 15, 2006 and filed with the SEC on March 16, 2006.
4.4
Form of specimen certificate for Series C 8% Convertible Preferred Stock of the Company, incorporated by reference to Exhibit 4.1
to the Current Report on Form 8-K, dated April 24, 2007 and filed with the SEC on April 25, 2007.
4.5
Warrant to purchase 100,000 shares of Common Stock issued to DH Blair Investment Banking Corp., incorporated by reference to
Exhibit 10.2 to the Quarterly Report on Form 10-Q for the period ended September 30, 2004.
4.6
Warrant to purchase 50,000 shares of Common Stock issued to Jason Lyons incorporated by reference to Exhibit 10.3 to the
Quarterly Report on Form 10-Q for the period ended June 30, 2004.
4.7
Form of Warrant to purchase shares of Common Stock issued to designees of lender with respect to financing of an equipment loan
incorporated by reference to Exhibit 10.2 to the Quarterly Report on Form 10-Q for the period ended June 30, 2004.
4.8
4.9
4.10
4.11
4.12
Form of Short Term Warrant to purchase shares of Common Stock issued to purchasers in the private placement which initially
closed on October 6, 2004 (the “Series A Financing”), incorporated by reference to Exhibit 4.6 to the Current Report on Form
8-K, dated October 6, 2004, and filed with the SEC on October 12, 2004.
Form of Long Term Warrant to purchase shares of Common Stock issued to purchasers in the Series A Financing, incorporated by
reference to Exhibit 4.7 to the Current Report on Form 8-K, dated October 6, 2004, and filed with the SEC on October 12, 2004.
Form of Warrant to purchase shares of Common Stock issued to the Placement Agent, in connection with the Series A Financing,
incorporated by reference to Exhibit 4.8 to the Current Report on Form 8-K, dated October 6, 2004, and filed with the SEC on
October 12, 2004.
Form of Replacement Warrant to purchase shares of Common Stock in connection with the offer to holders of Warrants in the
Series A Financing (the “Warrant Exchange”), incorporated by reference as Exhibit 4.1 to the Current Report on Form 8K, dated
December 14, 2005, and filed with the SEC on December 20, 2005.
Form of Warrant to purchase shares of Common Stock to the Placement Agent, in connection with the Warrant Exchange,
incorporated by reference as Exhibit 4.2 to the Current Report on Form 8-K, dated December 14, 2005, and filed with the SEC on
December 20, 2005.
60
�4.13
Form of Warrant to purchase shares of Common Stock issued to purchasers in the private placement which closed on March 15,
2006 (the “Series B Financing”), incorporated by reference to Exhibit 4.2 to the Current Report on Form 8K, dated March 15,
2006 and filed with the SEC on March 16, 2006.
4.14
Form of Warrant to purchase shares of Common Stock issued to purchasers in the Series B Financing, incorporated by reference to
Exhibit 4.3 to the Current Report on Form 8-K, dated March 15, 2006 and filed with the SEC on March 16, 2006.
4.15
Form of Warrant to purchase shares of Common Stock issued to the Placement Agent, in connection with the Series B Financing,
incorporated by reference to Exhibit 4.4 to the Current Report on Form 8-K, dated March 15, 2006 and filed with the SEC on
March 16, 2006.
4.16
Form of Warrant to purchase 600,000 shares of Common Stock issued to Indigo Ventures, LLC, incorporated by reference to
Exhibit 4.1 to the Current Report on Form 8-K, dated July 12, 2006 and filed with the SEC on July 18, 2006.
4.17
Form of Warrant to purchase up to 478,698 shares of Common Stock issued to VGS PHARMA, LLC, incorporated by reference
as Exhibit 3(a) to the Current Report on Form 8-K, dated December 6, 2006 and filed with the SEC on December 12, 2006.
4.18
4.19
Form of Non-Qualified Stock Option Agreement for 1,750,000 shares of Common Stock granted to Veerappan Subramanian,
incorporated by reference as Exhibit 3(b) to the Current Report on Form 8-K, dated December 6, 2006 and filed with the SEC on
December 12, 2006.
Form of Warrant to purchase shares of Common Stock issued to purchasers in the private placement which closed on April 24,
2007 (the “Series C Financing”), incorporated by reference to Exhibit 4.2 to the Current Report on Form 8K, dated April 24,
2007 and filed with the SEC on April 25, 2007.
4.20
Form of Warrant to purchase shares of Common Stock issued to the placement agent in the Series C Financing, incorporated by
reference to Exhibit 4.3 to the Current Report on Form 8-K, dated April 24, 2007 and filed with the SEC on April 25, 2007.
4.21
Form of specimen certificate for Series D 8% Convertible Preferred Stock of the Company, incorporated by reference to Exhibit 4.1
to the Current Report on Form 8-K, dated September 15, 2008 and filed with the SEC on September 16, 2008.
4.22
4.23
Form of Warrant to purchase shares of Common Stock issued to purchasers in the private placement which closed on September
15, 2008 (the “Series D Financing”), incorporated by reference to Exhibit 4.2 to the Current Report on Form 8K, dated
September 15, 2008 and filed with the SEC on September 16, 2008.
Form of Warrant to purchase shares of Common Stock issued to the placement agent in the Series D Financing, incorporated by
reference to Exhibit 4.3 to the Current Report on Form 8-K, dated September 15, 2008 and filed with the SEC on September 16,
2008.
61
�4.24
Form of specimen certificate for Series E Convertible Preferred Stock of the Company, incorporated by reference to Exhibit 4.1 to
the Current Report on Form 8-K, dated June 1, 2009, and filed with the SEC on June 5, 2009.
4.25
Warrant to purchase shares of Common Stock issued to Epic Investments, LLC in the initial closing of the Strategic Alliance
Agreement, dated as of March 18, 2009, by and among the Company, Epic Pharma, LLC and Epic Investments, LLC,
incorporated by reference to Exhibit 4.2 to the Current Report on Form 8-K, dated June 1, 2009, and filed with the SEC on June
5, 2009.
10.1
2004 Employee Stock Option Plan approved by stockholders on June 22, 2004, incorporated by reference to Exhibit A to the
Proxy Statement filed on Schedule 14A with respect to the Annual Meeting of Stockholders held on June 22, 2004.
10.2
Form of Confidentiality Agreement (corporate), incorporated by reference to Exhibit 10.7 to the Form SB-2.
10.3
Form of Confidentiality Agreement (employee), incorporated by reference to Exhibit 10.8 to the Form SB-2.
10.4
Amended and Restated Employment Agreement dated as of September 2, 2005 between Bernard Berk and the Company,
incorporated by reference to Exhibit 10.1 to Current Report on Form 8-K, dated September 2, 2005, and filed with the SEC on
September 9, 2005.
10.5
Option Agreement between Bernard Berk and the Company dated as of July 23, 2003 incorporated by reference to Exhibit 10.7 to
the Quarterly Report on Form 10Q for three months ended June 30, 2003 (the “June 30, 2003 10Q Report”).
10.6
Option Agreement between Bernard Berk and the Company dated as of July 23, 2003, incorporated by reference to Exhibit 10.8 to
the June 30, 2003 10Q Report.
10.7
10.8
10.9
Amendment, dated as of September 2, 2005, by and between, the Company and Bernard Berk, to the Stock Option Agreement,
dated as of July 23, 2003, incorporated by reference to Exhibit 10.2 to Current Report on Form 8-K, dated September 2, 2005, and
filed with the SEC on September 9, 2005.
Stock Option Agreement, dated as of September 2, 2005, by and between the Company and Bernard Berk, incorporated by
reference to Exhibit 10.3 to Current Report on Form 8-K, dated September 2, 2005, and filed with the SEC on September 9, 2005.
Stock Option Agreement, dated as of September 2, 2005, by and between the Company and Bernard Berk, incorporated by
reference to Exhibit 10.4 to Current Report on Form 8-K, dated September 2, 2005, and filed with the SEC on September 9, 2005.
10.10
Engagement letter dated February 26, 1998, between Gittelman & Co. P.C. and the Company incorporated by reference to Exhibit
10.10 to the Form 10-K for the period ended March 31, 2004 filed with the SEC on June 29, 2004.
62
�10.11
10.12
10.13
Product Development and Commercialization Agreement, dated as of June 21, 2005, between the Company and
IntelliPharmaceutics, Corp., incorporated by reference as Exhibit 10.1 to the Current Report on Form 8-K, dated June 21, 2005
and originally filed with the SEC on June 27, 2005, as amended on the Current Report on Form 8-K/A filed September 7, 2005,
as further amended by the Current Report on Form 8-K/A filed December 7, 2005 (Confidential Treatment granted with respect to
portions of the Agreement).
Agreement, dated December 12, 2005, by and among the Company, Elite Labs, and IntelliPharmaCeutics Corp., incorporated by
reference as Exhibit 10.1 to the Current Report on Form 8-K, dated December 12, 2005, and originally filed with the SEC on
December 16, 2005, as amended by the Current Report on Form 8-K/A filed March 7, 2006 (Confidential Treatment granted with
respect to portions of the Agreement).
Loan Agreement, dated as of August 15, 2005, between New Jersey Economic Development Authority (“NJEDA”) and the
Company, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated August 31, 2005 and filed with the
SEC on September 6, 2005.
10.14
Series A Note in the aggregate principal amount of $3,660,000.00 payable to the order of the NJEDA, incorporated by reference to
Exhibit 10.2 to the Current Report on Form 8-K, dated August 31, 2005 and filed with the SEC on September 6, 2005.
10.15
Series B Note in the aggregate principal amount of $495,000.00 payable to the order of the NJEDA, incorporated by reference to
Exhibit 10.3 to the Current Report on Form 8-K, dated August 31, 2005 and filed with the SEC on September 6, 2005.
10.16
Mortgage from the Company to the NJEDA, incorporated by reference to Exhibit 10.4 to the Current Report on Form 8-K, dated
August 31, 2005 and filed with the SEC on September 6, 2005.
10.17
Indenture between NJEDA and the Bank of New York as Trustee, dated as of August 15, 2005, incorporated by reference to Exhibit
10.5 to the Current Report on Form 8-K, dated August 31, 2005 and filed with the SEC on September 6, 2005.
10.18
Form of Warrant Exercise Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit 10.1
to the Current Report on Form 8-K, dated December 14, 2005 and filed with the SEC on December 20, 2005.
10.19
Form of Registration Rights Agreement, between the Registrant and signatories thereto, incorporated by reference to Exhibit 10.2
to the Current Report on Form 8-K, dated December 14, 2005 and filed with the SEC on December 20, 2005.
10.20
Form of Securities Purchase Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit
10.1 to the Current Report on Form 8-K, dated March 15, 2006 and filed with the SEC on March 16, 2006.
10.21
Form of Registration Rights Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit
10.2 to the Current Report on Form 8-K, dated March 15, 2006 and filed with the SEC on March 16, 2006.
63
�10.22
Form of Placement Agent Agreement, between the Registrant and Indigo Securities, LLC, incorporated by reference as Exhibit
10.3 to the Current Report on Form 8-K, dated March 15, 2006, and filed with the SEC on March 16, 2006.
10.23
Financial Advisory Agreement between the Registrant and Indigo Ventures LLC, incorporated by reference as Exhibit 10.1 to
the Current Report on Form 8-K dated July 12, 2006 and filed with the SEC on July 18, 2006.
10.24
Seconded Amended and Restated Employment Agreement between the Registrant and Bernard Berk, incorporated by reference
as Exhibit 10.1 to the Quarterly Report on Form 10-Q for the quarter ended September 30, 2006 and filed with the SEC on
November 14, 2006.
10.25
Employment Agreement between the Registrant and Charan Behl, incorporated by reference as Exhibit 10.2 to the Quarterly Report
on Form 10-Q for the quarter ended September 30, 2006 and filed with the SEC on November 14, 2006.
10.26
Employment Agreement between the Registrant and Chris Dick, incorporated by reference as Exhibit 10.3 to the Quarterly Report
on Form 10-Q for the quarter ended September 30, 2006 and filed with the SEC on November 14, 2006.
10.27
10.28
Product Collaboration Agreement between the Registrant and ThePharmaNetwork LLC, incorporated by reference as Exhibit 10.1
to the Current Report on Form 8-K, dated November 10, 2006 and filed with the SEC on November 15, 2006. (Confidential
Treatment granted with respect to portions of the Agreement).
Strategic Alliance Agreement among the Registrant, VGS Pharma (“VGS”) and Veerappan S. Subramanian (“VS”), incorporated
by reference as Exhibit 10(a) to the Current Report on Form 8-K, dated December 6, 2006 and filed with the SEC on December 12,
2006.
10.29
Advisory Agreement, between the Registrant and VS, incorporated by reference as Exhibit 10(b) to the Current Report on Form
8-K, dated December 6, 2006 and filed with the SEC on December 12, 2006.
10.30
Registration Rights Agreement between the Registrant, VGS and VS, incorporated by reference as Exhibit 10(c) to the Current
Report on Form 8-K, dated December 6, 2006 and filed with the SEC on December 12, 2006.
10.31
Employment Agreement between Novel Laboratories Inc. (“Novel”) and VS, incorporated by reference as Exhibit 10(d) to the
Current Report on Form 8-K, dated December 6, 2006 and filed with the SEC on December 12, 2006.
10.32
Stockholders’ Agreement between Registrant, VGS, VS and Novel, incorporated by reference as Exhibit 10(e) to the Current
Report on Form 8-K, dated December 6, 2006 and filed with the SEC on December 12, 2006.
64
�10.33
Amended and Restated Employment Agreement, between the Registrant and Charan Behl, incorporated by reference as Exhibit
10.1 to the Current Report on Form 8-K, dated February 9, 2007 and filed with the SEC on February 14, 2007.
10.34
Form of Securities Purchase Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit
10.1 to the Current Report on Form 8-K, dated April 24, 2007 and filed with the SEC on April 25, 2007.
10.35
Form of Registration Rights Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit
10.2 to the Current Report on Form 8-K, dated April 24, 2007 and filed with the SEC on April 25, 2007.
10.36
Form of Placement Agent Agreement, between the Company and Oppenheimer & Company, Inc., incorporated by reference as
Exhibit 10.3 to the Current Report on Form 8-K, dated April 24, 2007 and filed with the SEC on April 25, 2007.
10.37
Form of Securities Purchase Agreement, between the Registrant and the signatories thereto, incorporated by reference to Exhibit
10.1 to the Current Report on Form 8-K, dated July 17, 2007 and filed with the SEC on July 23, 2007.
10.38
10.39
10.40
Form of Registration Rights Agreement, between the Registrant and the signatories thereto, incorporated by reference as Exhibit
10.2 to the Current Report on Form 8-K, dated July 17, 2007 and filed with the SEC on July 23, 2007.
Consulting Agreement, dated as of July 27, 2007, between the Registrant and Willstar Consultants, Inc., incorporated by reference
as Exhibit 10.1 to the Quarterly Report on Form 10-Q for the period ending September 30, 2007 and filed with the SEC on
November 14, 2007.
Consulting Agreement, dated as of September 4, 2007, between the Registrant, Bridge Ventures, Inc. and Saggi Capital, Inc.,
incorporated by reference as Exhibit 10.2 to the Quarterly Report on Form 10-Q for the period ending September 30, 2007 and filed
with the SEC on November 14, 2007.
10.41
Employment Agreement, dated as of January 3, 2008, by and between the Registrant and Dr. Stuart Apfel, incorporated by
reference as Exhibit 10.1 to the Current Report on Form 8-K dated January 3, 2008 and filed with the SEC on January 9, 2008.
10.42
Form of Securities Purchase Agreement, between the Company and the signatories thereto, incorporated by reference to Exhibit
10.1 to the Current Report on Form 8-K, dated September 15, 2008 and filed with the SEC on September 16, 2008.
10.43
10.44
Form of Placement Agent Agreement, between the Company, ROTH Capital Partners, LLC and Boenning & Scattergood, Inc.,
incorporated by reference to Exhibit 10.3 to the Current Report on Form 8-K, dated September 15, 2008 and filed with the SEC on
September 16, 2008.
Separation Agreement and General Release of Claims, dated as of October 20, 2008, by and between the Company and Stuart
Apfel, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated October 15, 2008 and filed with the
SEC on October 21, 2008.
65
�10.45
10.46
Consulting Agreement, dated as of October 20, 2008, by and between the Company and Parallex Clinical Research, incorporated
by reference to Exhibit 10.2 to the Current Report on Form 8-K, dated October 15, 2008 and filed with the SEC on October 21,
2008.
Separation Agreement and General Release of Claims, dated as of November 3, 2008, by and between the Company and Charan
Behl, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated October 28, 2008 and filed with the
SEC on November 3, 2008.
10.47
Consulting Agreement, dated as of November 3, 2008, by and between the Company and Charan Behl, incorporated by reference to
Exhibit 10.2 to the Current Report on Form 8-K, dated October 28, 2008 and filed with the SEC on November 3, 2008.
10.48
10.49
10.50
10.51
10.52
10.53
Separation Agreement and General Release of Claims, dated as of November 5, 2008, by and between the Company and Bernard J.
Berk, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated November 6, 2008 and filed with the
SEC on November 6, 2008.
Amendment to Employment Agreement, dated as of November 10, 2008, by and between the Company and Chris Dick,
incorporated by reference to Exhibit 10.1 to the Quarterly Report on Form 10-Q for the period ended September 30, 2008 and filed
with the SEC on November 14, 2008.
Compensation Agreement, dated as of December 1, 2008, by and between the Company and Jerry I. Treppel, incorporated by
reference to Exhibit 10.1 to the Current Report on Form 8-K, dated December 1, 2008 and filed with the SEC on December 4,
2008.
Strategic Alliance Agreement, dated as of March 18, 2009, by and among the Company, Epic Pharma, LLC and Epic Investments,
LLC, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated March 18, 2009 and filed with the SEC
on March 23, 2009.
Amendment to Strategic Alliance Agreement, dated as of April 30, 2009, by and among the Company, Epic Pharma, LLC and
Epic Investments, LLC, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated April 30, 2009 and
filed with the SEC on May 6, 2009.
Second Amendment to Strategic Alliance Agreement, dated as of June 1, 2009, by and among the Company, Epic Pharma, LLC
and Epic Investments, LLC, incorporated by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated June 1, 2009, and
filed with the SEC on June 5, 2009.
10.54
Employment Agreement, dated as of July 1, 2009, by and between the Company and Carter J. Ward, incorporated by reference to
Exhibit 10.1 to the Current Report on Form 8-K dated July 1, 2009 and filed with the SEC on July 8, 2009.
10.55
Third Amendment to Strategic Alliance Agreement, dated as of Aug 18, 2009, by and among the Company, Epic Pharma LLC
and Epic Investments, LLC, incorporated by reference to Exhibit 10.3 to the Quarterly Report on Form 10-Q, for the period ending
June 30, 2009 and filed with the SEC on August 19, 2009.
66
�10.56
10.57
10.58
10.59
Employment Agreement, dated as of November 13, 2009, by and between the Company and Chris Dick, , incorporated by
reference to Exhibit 10.1 to the Quarterly Report on Form 10-Q, for the period ending September 30, 2009 and filed with the SEC
on November 16, 2009.
Employment Agreement, dated as of November 13, 2009, by and between the Company and Carter J. Ward, incorporated by
reference to Exhibit 10.2 to the Quarterly Report on Form 10-Q, for the period ending September 30, 2009 and filed with the SEC
on November 16, 2009.
Elite Pharmaceuticals Inc. 2009 Equity Incentive Plan, as adopted November 24, 2009, incorporated by reference to Exhibit 10.1
to the Registration Statement Under the Securities Act of 1933 on Form S-8, dated December 18, 2009 and filed with the SEC on
December 22, 2009.
Stipulation of Settlement and Release, dated as of June 25, 2010, by and among the Company, Midsummer Investment, Ltd.,
Bushido Capital Master Fund, LP, BCMF Trustees, LLC, Epic Pharma, LLC and Epic Investments, LLC, incorporated by
reference to Exhibit 10.1 to the Current Report on Form 8-K, dated June 25, 2010 and filed with the SEC on July 1, 2010
10.60
Amendment Agreement, dated as of June 25, 2010, by and among the Company, and the investors signatory thereto, incorporated
by reference to Exhibit 10.2 to the Current Report on Form 8-K, dated June 25, 2010 and filed with the SEC on July 1, 2010
10.61
10.62
10.63
10.64
Amendment Agreement, dated as of June 2010, by and among the Company, Epic Pharma, LLC and Epic Investments, LLC,
incorporated by reference to Exhibit 10.3 to the Current Report on Form 8-K, dated June 25, 2010 and filed with the SEC on July
1, 2010
Asset Purchase Agreement dated as of May 18, 2010, by and among Mikah Pharma LLC and the Company, incorporated by
reference to Exhibit 10.4 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed with the SEC
on November 15, 2010.
Asset Purchase Agreement, dated as of August 27, 2010, by and among Mikah Pharma LLC and the Company, incorporated by
reference to Exhibit 10.5 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed with the SEC
on November 15, 2010. Confidential portions of this exhibit have been redacted and filed separately with the Commission
pursuant to a confidential treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended. A
description of this Asset Purchase Agreement is incorporated by reference to Item 2.01 of the Current Report on Form 8-K, dated
August 27, 2010 and filed with SEC on September 1, 2010
Master Development and License Agreement, dated as of August 27, 2010, by and among Mikah Pharma LLC and the Company
incorporated by reference to Exhibit 10.6 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed
with the SEC on November 15, 2010. Confidential portions of this exhibit have been redacted and filed separately with the
Commission pursuant to a confidential treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as
amended. A description of this Asset Purchase Agreement is incorporated by reference to Item 1.01 of the Current Report on Form
8-K, dated August 27, 2010 and filed with SEC on September 1, 2010
67
�10.65
10.66
10.67
Purchase Agreement, dated as of September 10, 2010, by and among Epic Pharma LLC and the Company, incorporated by
reference to Exhibit 10.7 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed with the SEC
on November 15, 2010. Confidential portions of this exhibit have been redacted and filed separately with the Commission pursuant
to a confidential treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended. A
description of this Asset Purchase Agreement is incorporated by reference to Item 2.01 of the Current Report on Form 8-K, dated
September 10, 2010 and filed with SEC on September 16, 2010
License Agreement, dated as of September 10, 2010, by and among Precision Dose Inc. and the Company, incorporated by
reference to Exhibit 10.8 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed with the SEC
on November 15, 2010. Confidential portions of this exhibit have been redacted and filed separately with the Commission pursuant
to a confidential treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended. A
description of this Asset Purchase Agreement is incorporated by reference to Item 1.01 of the Current Report on Form 8-K, dated
September 10, 2010 and filed with SEC on September 16, 2010
Manufacturing and Supply Agreement, dated as of September 10, 2010, by and among Precision Dose Inc. and the Company,
incorporated by reference to Exhibit 10.9 to the Quarterly Report on Form 10-Q, for the period ended September 30, 2010 and filed
with the SEC on November 15, 2010. Confidential portions of this exhibit have been redacted and filed separately with the
Commission pursuant to a confidential treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as
amended. A description of this Asset Purchase Agreement is incorporated by reference to Item 1.01 of the Current Report on Form
8-K, dated September 10, 2010 and filed with SEC on September 16, 2010
10.68
Product Development Agreement between the Company and Hi-Tech Pharmacal Co., Inc. dated as of January 4, 2011, incorporated
by reference to Exhibit 10.1 to the Current Report on Form 8-K, dated January 4, 2011 and filed with the SEC on January 10,
2011. Confidential portions of this exhibit have been redacted and filed separately with the Commission pursuant to a confidential
treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended.
10.69
Settlement Agreement between the Company and ThePharmaNetwork, LLC, dated as of March 11, 2011, incorporated by reference
to Exhibit 10.1 to the Current Report on Form 8-K, dated March 11, 2011 and filed with the SEC on March 17, 2011.
10.70
10.71
Manufacturing and Supply Agreement between the Company and Mikah Pharma LLC, dated as of June 1, 2011. Confidential
portions of this exhibit have been redacted and filed separately with the Commission pursuant to a confidential treatment request in
accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended.
Manufacturing and Supply Agreement between the Company and ThePharmaNetwork LLC, dated as of June 23,
2011. Confidential portions of this exhibit have been redacted and filed separately with the Commission pursuant to a confidential
treatment request in accordance with Rule 24b-2 of the Securities Exchange Act of 1934, as amended.
68
�21
Subsidiaries of the Company.*
31.1*
Certification of Chief Executive Officer pursuant to Section 302 of the Sarbanes-Oxley Act of 2002*
31.2*
Certification of Chief Financial Officer pursuant to Section 302 of the Sarbanes-Oxley Act of 2002*
32.1**
Certification of Chief Executive Officer pursuant to Section 906 of the Sarbanes-Oxley Act of 2002.*
32.2**
Certification of Chief Financial Officer pursuant to Section 906 of the Sarbanes-Oxley Act of 2002.*
* Filed herewith.
** As contemplated by SEC Release No. 33-8212, these exhibits are furnished with this Annual Report on Form 10-K and are not deemed filed with
the Securities and Exchange Commission and are not incorporated by reference in any filing of Elite Pharmaceuticals, Inc. under the Securities Act or
the Securities Exchange Act, whether made before or after the date hereof and irrespective of any general incorporation language in any such filings.
69
�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.
ELITE PHARMACEUTICALS, INC.
SIGNATURES
By:
/s/ Jerry Treppel
Jerry Treppel
Chief Executive Officer
Dated: June 29, 2011
By:
/s/ Carter J. Ward
Carter J. Ward
Chief Financial Officer
Dated: June 29, 2011
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.
Signature
Title
/s/ Jerry Treppel
/s/ Chris Dick
Chairman, Chief Executive Officer
President, Chief Operating Officer, Director
/s/ Carter J. Ward
Chief Financial Officer, Treasurer, Secretary
/s/ Barry Dash
/s/ Jeenarine Narine
/s/ Ashok Nigalaye
/s/ Ram Potti
/s/ Jeffrey Whitnell
Director
Director
Director
Director
Director
70
Date
June 29, 2011
June 29, 2011
June 29, 2011
June 29, 2011
June 29, 2011
June 29, 2011
June 29, 2011
June 29, 2011
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED FINANCIAL STATEMENTS
FOR THE YEARS ENDED MARCH 31, 2011 AND 2010
CONTENTS
REPORTS OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM
CONSOLIDATED BALANCE SHEETS
CONSOLIDATED STATEMENTS OF OPERATIONS
CONSOLIDATED STATEMENTS OF STOCKHOLDERS (DEFICIT) EQUITY
CONSOLIDATED STATEMENTS OF CASH FLOWS
NOTES TO CONSOLIDATED FINANCIAL STATEMENTS
F-1
PAGE
F - 2
F - 3
F - 6
F - 7
F 10
F - 12
�Report of Independent Registered Public Accounting Firm
To The Board of Directors and
Shareholders of Elite Pharmaceuticals, Inc. & Subsidiaries
We have audited the accompanying consolidated balance sheets of Elite Pharmaceuticals, Inc. and Subsidiaries (“the Company”) as of March 31,
2011 and 2010 and the related consolidated statements of operations, stockholders' deficit and cash flows for each of the years in the two-year period
ended March 31, 2011. The Company’s management is responsible for these consolidated financial statements. Our responsibility is to express an
opinion on these consolidated financial statements 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. The Company is not required to have, nor were we engaged to perform, an audit of its internal control over financial reporting. Our
audit included consideration of internal control over financial reporting as a basis for designing audit procedures that are appropriate in the
circumstances, but not for the purpose of expressing an opinion on the effectiveness of the Company’s internal control over financial
reporting. Accordingly, we express no such opinion. An audit also 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 Elite
Pharmaceuticals, Inc. and Subsidiaries as of March 31, 2011 and 2010 and the results of their operations and their cash flows for each of the years in
the two year period ended March 31, 2011 in conformity with accounting principles generally accepted in the United States of America.
The accompanying consolidated financial statements have been prepared assuming that Elite Pharmaceuticals, Inc. and Subsidiaries will continue as
a going concern. As shown in the consolidated financial statements, the Company has experienced significant losses resulting in a working capital
deficiency and shareholders’ deficit. These conditions raise substantial doubt about its ability to continue as a going concern. Management’s plans
in regard to these matters are more fully described in Note 2. The consolidated financial statements do not include any adjustments that might result
from the outcome of these uncertainties.
/s/Demetrius & Company, L.L.C.
Wayne, New Jersey 07470
June 29, 2011
F-2
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED BALANCE SHEETS
MARCH 31, 2011 and 2010
ASSETS
CURRENT ASSETS
Cash and cash equivalents
Accounts receivable (net of allowance for doubtful accounts of -0-)
Inventories (net of reserve of $1,047,456 and $494,425, respectively)
Prepaid expenses and other current assets
2011
2010
$
1,825,858 $
571,667
616,362
133,472
578,187
404,961
1,371,292
131,507
Total Current Assets
3,147,359
2,485,947
PROPERTY AND EQUIPMENT - net of accumulated depreciation of $4,189,618 and $3,840,279, respectively
4,118,274
4,095,814
INTANGIBLE ASSETS – net of accumulated amortization of $0 and $76,434, respectively
597,556
96,407
OTHER ASSETS
Investment in Novel Laboratories, Inc.
Security deposits
Restricted cash – debt service for EDA bonds
EDA bond offering costs, net of accumulated amortization of $78,898 and $64,767, respectively
Total Other Assets
TOTAL ASSETS
3,329,322
28,377
291,420
275,554
3,329,322
14,652
294,836
289,685
3,924,673
3,928,495
$ 11,787,862 $ 10,606,663
The accompanying notes are an integral part of the consolidated financial statements
F-3
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED BALANCE SHEETS
MARCH 31, 2011 and 2010
LIABILITIES AND STOCKHOLDERS’ DEFICIT
CURRENT LIABILITIES
EDA bonds payable
Short term loans and current portion of long-term debt
Accounts payable and accrued expenses
Customer Deposits
Deferred revenues – current
Preferred share derivative interest payable
2011
2010
$
$
3,385,000
13,105
935,797
39,400
13,333
282,680
3,385,000
82,302
986,777
—
—
306,440
Total Current Liabilities
4,669,315
4,760,519
LONG TERM LIABILITIES
Deferred revenues
Long term debt, less current portion
Other long term liabilities
Derivative liability – preferred shares
Derivative liability – warrants
Total Long Term Liabilities
TOTAL LIABILITIES
STOCKHOLDERS’ DEFICIT
Common stock – par value $0.001, Authorized 355,516,558 shares Issued and outstanding – 180,545,657
shares and 83,950,168 shares, respectively
Additional paid-in-capital
Accumulated deficit
Treasury stock at cost (100,000 common shares)
178,890
6,717
68,746
—
19,823
14,192,329
10,543,145
7,924,763
8,499,423
24,989,827
16,444,009
29,659,142
21,204,528
180,546
83,950
97,116,044
90,903,896
(114,861,029) (101,278,870)
(306,841)
(306,841)
TOTAL STOCKHOLDERS’ DEFICIT
(17,871,280)
(10,597,865)
TOTAL LIABILITIES AND STOCKHOLDERS’ DEFICIT
$ 11,787,862
$ 10,606,663
The accompanying notes are an integral part of the consolidated financial statements
F-4
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENTS OF OPERATIONS
REVENUES
Manufacturing Fees
Royalties
Lab Fee Revenues
COSTS OF REVENUES
Total Revenues
Gross Profit
OPERATING EXPENSES
Research and Development
General and Administrative
Non-cash compensation through issuance of stock options
Depreciation and Amortization
Total Operating Expenses
(LOSS) FROM OPERATIONS
OTHER INCOME / (EXPENSES)
Interest expense, net
Change in fair value of warrant derivatives
Change in fair value of preferred share derivatives
Interest expense attributable to preferred share derivatives
Discount in Series E issuance attributable to beneficial conversion features
Proceeds from litigation settlement
Total Other Income / (Expense)
(LOSS) BEFORE PROVISION FOR INCOME TAXES
CREDIT FOR INCOME TAXES
NET (LOSS) ATTRIBUTABLE TO COMMON SHAREHOLDERS
Years Ended
March 31,
2011
2010
$
$
3,086,183
831,538
348,242
2,575,942
763,928
4,429
4,265,963
2,675,118
3,344,299
2,305,763
1,590,845
1,038,536
1,385,211
876,014
42,016
173,364
794,433
1,841,425
125,004
213,995
2,476,605
2,974,857
(885,760)
(1,936,321)
(231,745)
(1,297,998)
(10,416,376)
(1,259,480)
(292,213)
500,000
(12,997,812)
(260,337)
(3,792,130)
(283,920)
(1,271,254)
(512,912)
—
(6,120,553)
(13,883,570)
301,413
$ (13,582,159) $
(8,056,874)
—
(8,056,874)
BASIC AND DILUTED LOSS PER COMMON SHARE
$
(0.14) $
(0.11)
WEIGHTED AVERAGE NUMBER OF COMMON SHARES OUTSTANDING
100,020,520
75,581,345
The accompanying notes are an integral part of the consolidated financial statements
F-5
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENT OF CHANGES IN STOCKHOLDERS (DEFICIT) EQUITY
FOR THE YEAR ENDED MARCH 31, 2010
(page 1 of 2)
Balance at March 31, 2009
1,046
$
11
13,705
$
137
9,154
$
91
Series B
Preferred Stock
Series C
Preferred Stock
Series D
Preferred Stock
Shares
Amount
Shares
Amount
Shares
Amount
Common Stock
Shares
60,839,374
Amount
$
608,394
Cumulative effect of reclassification of preferred
stock and warrants
Proceeds received in exchange for beneficial
conversion features embedded in Series E
Preferred Shares
Conversion of Series B, Series C and Series D
Preferred Shares into Common Shares
Costs associated with raising capital
Non-cash compensation through the issuance of
stock options and warrants
Net income for the year ended March 31, 2010
Dividends
Common shares issued in lieu of cash in payment
of preferred share derivative interest expense
Reduction in par value
Common shares issued in lieu of cash in payment
of legal and consulting expenses
Write-off of subscription receivable from defunct
company
(11)
(137)
(91)
(150)
(8,287)
(146)
5,383,010
53,830
3,914,944
39,149
12,699,749
93,504
(712,040)
1,113,091
1,113
Balance at March 31, 2010
896
—
5,418
—
9,008
—
83,950,168
$
83,950
The accompanying notes are an integral part of the consolidated financial statements
F-6
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENT OF CHANGES IN STOCKHOLDERS (DEFICIT) EQUITY
FOR THE YEAR ENDED MARCH 31, 2010
(page 2 of 2)
Balance at March 31, 2009
Additional
Subscription
Receivable
$
(75,000)
Paid-In
Capital
$ 95,718,082
Treasury Stock
Shares
Amount
(100,000)
$
(306,841)
Accumulated
Deficit
$ (90,001,793)
Stockholders
(Deficit) Equity
5,943,081
$
Cumulative effect of reclassification of preferred stock and warrants
(7,144,131)
(3,220,203)
(10,364,573)
Proceeds received in exchange for beneficial conversion features embedded
in Series E Preferred Shares
512,912
Conversion of Series B, Series C and Series D Preferred Shares into Common
Shares
(150)
14,000
Costs associated with raising capital
Non-cash compensation through the issuance of stock options and warrants
Net income for the year ended March 31, 2010
Dividends
Common shares issued in lieu of cash in payment of preferred share
derivative interest expense
Reduction in par value
Common shares issued in lieu of cash in payment of legal and consulting
expenses
(183,456)
125,004
319,472
805,882
712,040
99,091
512,912
67,830
(183,456)
125,004
(8,056,874)
(8,056,874)
358,621
899,386
100,204
Write-off of subscription receivable from defunct company
75,000
(75,000)
Balance at March 31, 2010
—
$ 90,903,896
(100,000)
$
(306,841)
$ (101,278,870)
$
(10,597,865)
The accompanying notes are an integral part of the consolidated financial statements
F-7
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENT OF CHANGES IN STOCKHOLDERS (DEFICIT) EQUITY
FOR THE YEAR ENDED MARCH 31, 2011
Common Stock
Paid-In
Treasury Stock
Accumulated
Stockholders’
Additional
Balance at Mar 31, 2010
Net Income
Shares
83,950,168
Amount
$
83,950
Capital
$ 90,903,896
Shares
Amount
100,000
$
(306,841)
Deficit
$ (101,278,870)
Deficit
$ (10,597,865)
(13,582,159)
(12,747,581)
Common shares issued in lieu of cash in payment of preferred
share derivative interest expense
21,241,590
21,242
1,261,999
Common shares issued pursuant to the conversion of Series D
Convertible Preferred Derivatives
70,649,154
70,649
4,394,935
Non-cash compensation through the issuance of stock options
42,017
Common shares issued pursuant to ANDA purchase agreement
dated 5/18/2010
937,500
938
74,062
Common shares issued in lieu of cash in payment of consulting
expenses
343,425
343
13,394
Common shares issued in payment of Director’s Fees
2,493,589
2,494
97,249
Common shares issued in payment of employee salaries
930,231
930
36,280
Proceeds received in exchange for beneficial conversion
features embedded in Series E Preferred Shares
292,213
1,283,240
4,465,584
42,017
75,000
13,737
99,743
37,210
292,213
Balance at Mar 31, 2011
180,545,657
$
180,546
$ 97,116,044
100,000
$
(306,841)
$ (114,861,029)
$ (17,871,280)
The accompanying notes are an integral part of the consolidated financial statements
F-8
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENTS OF CASH FLOWS
(page 1 of 2)
CASH FLOWS FROM OPERATING ACTIVITIES
Loss from continuing operations
Adjustments to reconcile net loss to cash used in operating activities:
Depreciation and amortization
Inventory adjustment
Change in fair value of warrant derivative liability
Change in fair value of preferred shares derivative liability
Discount in Series E issuance attributable to embedded beneficial ownership feature
Preferred shares derivative interest satisfied by the issuance of common stock
Legal and consulting expenses satisfied by the issuance of common stock
Salaries and Directors Fees satisfied by the issuance of common stock
Non-cash compensation satisfied by the issuance of common stock, options and warrants
Non-cash rent expense
Impairment of Intangible Assets
Non-cash lease accretion
Changes in assets and liabilities:
Accounts and interest receivable
Inventories
Prepaid expenses and other current assets
Security deposit
Accounts payable, accrued expenses and other current liabilities
NET CASH PROVIDED BY (USED IN) OPERATING ACTIVITIES
CASH FLOWS FROM INVESTING ACTIVITIES
Purchases of property and equipment
Cost of leasehold improvements
Proceeds from sale of retired equipment
Costs incurred for intellectual property assets
Withdrawals from restricted cash, net
NET CASH (USED IN ) INVESTING ACTIVITIES
CASH FLOWS FROM FINANCING ACTIVITIES
Other loan payments
NJEDA bond principal payments
Proceeds from issuance of Series E Convertible Preferred Stock and Warrants
NET CASH PROVIDED BY FINANCING ACTIVITIES
NET CHANGE IN CASH AND CASH EQUIVALENTS
Years Ended March 31,
2010
2011
$ (13,582,159) $
(8,056,874)
483,473
—
1,297,997
10,416,375
292,213
1,283,240
13,737
136,953
42,017
48,064
440,000
20,682
508,610
311,986
3,792,130
283,920
512,912
964,814
100,204
—
125,004
—
—
—
(166,706)
754,931
(1,962)
(13,725)
87,686
1,552,815
(395,245)
20,488
16,659
12,909
437,734
(1,364,748)
(178,169)
(343,631)
30,000
(866,150)
3,416
—
—
—
(96,404)
32,599
(1,354,533)
(63,805)
(13,106)
—
1,062,500
(65,839)
(210,000)
2,000,000
1,049,394
1,724,161
1,247,676
295,609
CASH AND CASH EQUIVALENTS – beginning of period
CASH AND CASH EQUIVALENTS – end of period
$
Schedule continues on next page The accompanying notes are an integral part of the consolidated financial statements
$
578,187
1,825,858
282,578
578,187
F-9
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
CONSOLIDATED STATEMENTS OF CASH FLOWS
(page 2 of 2)
SUPPLEMENTAL DISCLOSURES OF CASH FLOW INFORMATION
Cash paid for interest
Cash paid for income taxes
SCHEDULE OF NON-CASH INVESTING AND FINANCING ACTIVITIES
Cumulative effect of reclassification of Preferred Stock and Warrants as Derivative Liabilities
Reduction in par value of common stock from $0.01 per share to $0.001 per share
Common stock issued for purchase of intangible assets
The accompanying notes are an integral part of the consolidated financial statements
F-10
Years Ended March 31,
2010
2011
226,150
7,822
$
262,685
—
10,364,573
712,954
75,000
�ELITE PHARMACEUTICALS, INC. AND SUBSIDIARIES
NOTES TO CONSOLIDATED FINANCIAL STATEMENTS
MARCH 31, 2011 AND 2010
NOTE 1
SUMMARY OF SIGNIFICANT ACCOUNTING POLICIES
BASIS OF PRESENTATION
The accompanying audited financial statements have been prepared in accordance with accounting principles generally accepted in
the United States of America (“GAAP”)
PRINCIPLES OF CONSOLIDATION
The consolidated financial statements include the accounts of Elite Pharmaceuticals, Inc. and its consolidated subsidiaries,
(collectively the “Company”) including its whollyowned subsidiaries, Elite Laboratories, Inc. (“Elite Labs”) and Elite Research,
Inc. (“ERI”) for the years ended March 31, 2011 (“Fiscal Year 2011”) and 2010 (“Fiscal Year 2010”). Our Company consolidates
all entities that we control by ownership of a majority voting interest. As of March 31, 2011, the financial statements of all
wholly-owned entities are consolidated and all significant intercompany accounts are eliminated upon consolidation.
NATURE OF BUSINESS
Elite Pharmaceuticals, Inc. was incorporated on October 1, 1997 under the laws of the State of Delaware, and its wholly-owned
subsidiary Elite Laboratories, Inc. was incorporated on August 23, 1990 under the laws of the State of Delaware. Elite Labs
engages primarily in researching, developing and licensing proprietary controlled-release drug delivery systems and products. The
Company is also equipped to manufacture controlled-release products on a contract basis for third parties and itself if and when the
products are approved; however the Company has concentrated on developing orally administered controlled-release products.
These products include drugs that cover therapeutic areas for pain, allergy and infection. The Company also engages in research and
development activities for the purpose of obtaining Food and Drug Administration approval, and, thereafter, commercially
exploiting generic and new controlled-release pharmaceutical products. The Company also engages in contract research and
development on behalf of other pharmaceutical companies.
CASH AND CASH EQUIVALENTS
The Company considers all highly liquid investments with an original maturity of three months or less to be cash equivalents.
Cash and cash equivalents consist of cash on deposit with banks and money market instruments. The Company places its cash and
cash equivalents with high-quality, U.S. financial institutions and, to date has not experienced losses on any of its balances.
INVENTORIES
Inventories are stated at the lower of cost (first-in, first-out basis) or market (net realizable value).
F-11
�LONG-LIVED ASSETS
The Company periodically evaluates the fair value of long-lived assets, which include property and equipment and intangibles,
whenever events or changes in circumstances indicate that its carrying amounts may not be recoverable. Such conditions may
include an economic downturn or a change in the assessment of future operations. A charge for impairment is recognized whenever
the carrying amount of a long-lived asset exceeds its fair value. Management has determined that no impairment of long-lived
assets has occurred.
Property and equipment are stated at cost. Depreciation is provided on the straight-line method based on the estimated useful lives
of the respective assets which range from five to forty years. Major repairs or improvements are capitalized. Minor replacements and
maintenance and repairs which do not improve or extend asset lives are expensed currently.
Upon retirement or other disposition of assets, the cost and related accumulated depreciation are removed from the accounts and the
resulting gain or loss, if any, is recognized in income.
Costs incurred to acquire intangible assets such as for the application of patents and trademarks are capitalized and amortized on the
straight-line method, based on their estimated useful lives ranging from five to fifteen years, commencing upon approval of the
patent and trademarks. Such costs are charged to expense if the patent or trademark is unsuccessful.
RESEARCH AND DEVELOPMENT
Research and development expenditures are charged to expense as incurred.
CONCENTRATION OF CREDIT RISK
The Company maintains cash balances, which, at times, may exceed the amounts insured by the Federal Deposit Insurance Corp.
Uninsured balances at March 31, 2011 are $1,575,858. Management does not believe that there is any significant risk of losses.
The Company in the normal course of business extends credit to its customers based on contract terms and performs ongoing credit
evaluations. An allowance for doubtful accounts due to uncertainty of collection is established based on historical collection
experience. Amounts are written off when payment is not received after exhaustive collection efforts. During Fiscal 2010 and Fiscal
2011 the Company generated all its revenues from two companies. The termination of the contracts with either of such two
companies will result in the loss of a significant amount of revenues currently being earned.
USE OF ESTIMATES
The preparation of financial statements in conformity with GAAP requires management to make estimates and assumptions that
affect the reported amounts of assets and liabilities and disclosure of contingent assets and liabilities at the date of the financial
statements and the reported amounts of revenues and expenses during the reporting period. Actual results could differ from those
estimates. Significant estimates made by management include, but are not limited to, the recognition of revenue, the amount of the
allowance for doubtful accounts receivable and the fair value of intangible assets, stock-based awards and derivatives.
INCOME TAXES
The Company uses the liability method for reporting income taxes, under which current and deferred tax liabilities and assets are
recorded in accordance with enacted tax laws and rates. Deferred income taxes reflect the net tax effects of temporary differences
between the carrying amounts of assets and liabilities for financial reporting purposes and the amounts used for income tax
purposes. Under the liability method, the amounts of deferred tax liabilities and assets at the end of each period are determined
using the tax rate expected to be in effect when taxes are actually paid or recovered. Further tax benefits are recognized when it is
more likely than not, that such benefits will be realized. Valuation allowances are provided to reduce deferred tax assets to the
amount considered likely to be realized.
F-12
�GAAP prescribes a recognition threshold and measurement attribute for how a company should recognize, measure, present, and
disclose in its financial statements uncertain tax positions that the company has taken or expects to take on a tax return. GAAP
requires that the financial statements reflect expected future tax consequences of such positions presuming the taxing authorities’
full knowledge of the position and all relevant facts, but without considering time values. No adjustments related to uncertain tax
positions were recognized during the years ended March 31, 2011 and March 31, 2010.
The Company recognizes interest and penalties related to uncertain tax positions as a reduction of the income tax benefit. No
interest and penalties related to uncertain tax positions were accrued as of March 31, 2011 and March 31, 2010.
The Company operates in multiple tax jurisdictions within the United States of America. Although we do not believe that we are
currently under examination in any of our major tax jurisdictions, we remain subject to examination in all of our tax jurisdiction
until the applicable statutes of limitation expire. As of March 31, 2011, a summary of the tax years that remain subject to
examination in our major tax jurisdictions are: United States – Federal and State – 2005 and forward. The Company does not
expect to have a material change to unrecognized tax positions within the next twelve months.
EARNINGS PER COMMON SHARE
Basic earnings per common share is calculated by dividing net earnings by the weighted average number of shares outstanding
during each period presented. Diluted earnings per share are calculated by dividing earnings by the weighted average number of
shares and common stock equivalents. The Company’s common stock equivalents consist of options, warrants and convertible
securities.
REVENUE RECOGNITION
Revenues earned under manufacturing agreements with other pharmaceutical companies are recognized on the date of shipment of
the product, when title for the goods is transferred, and for which the price is agreed to and it has been determined that
collectability is reasonably assured.
Revenues derived from royalties are recognized when such are reasonably estimable and collectible. Revenues from royalties which
cannot be reasonably estimated are recognized when the payment is received.
Revenues derived from providing research and development services under contracts with other pharmaceutical companies are
recognized when earned. These contracts provide for non-refundable upfront and milestone payments. Because no discrete earnings
event has occurred when the upfront payment is received, that amount is deferred until the achievement of a defined milestone. Each
nonrefundable milestone payment is recognized as revenue when the performance criteria for that milestone have been met. Under
each contract, the milestones are defined, substantive effort is required to achieve the milestone, the amount of the non-refundable
milestone payment is reasonable, commensurate with the effort expended, and achievement of the milestone is reasonably assured.
F-13
�Revenues earned by licensing certain pharmaceutical products developed by the Company are recognized at the beginning of a
license term when the Company’s customer has legal right to the use of the product. Revenues are recognized on licensing income
on a straight line basis over the life of the licensing agreement.
TREASURY STOCK
The Company records common shares purchased and held in treasury at cost.
FAIR VALUE OF FINANCIAL INSTRUMENTS
The carrying amounts of current assets and liabilities approximate fair value due to the short-term nature of these instruments. The
carrying amounts of noncurrent assets are reasonable estimates of their fair values based on management’s evaluation of future cash
flows. The long-term liabilities are carried at amounts that approximate fair value based on borrowing rates available to the
Company for obligations with similar terms, degrees of risk and remaining maturities.
STOCK-BASED COMPENSATION
The Company accounts for all stock-based payments and awards under the fair value based method. Stock-based payments to
non-employees are measured at the fair value of the consideration received, or the fair value of the equity instruments issued, or
liabilities incurred, whichever is more reliably measurable. The fair value of stock-based payments to non-employees is periodically
re-measured until the counterparty performance is complete, and any change therein is recognized over the vesting period of the
award and in the same manner as if the Company had paid cash instead of paying with or using equity based instruments on an
accelerated basis. The cost of the stock-based payments to nonemployees that are fully vested and non-forfeitable as at the grant date
is measured and recognized at that date, unless there is a contractual term for services in which case such compensation would be
amortized over the contractual term.
The Company accounts for the granting of share purchase options to employees using the fair value method whereby all awards to
employees will be recorded at fair value on the date of the grant. Share based awards granted to employees with a performance
condition are measured based on the probable outcome of that performance condition during the requisite service period. Such an
award with a performance condition is accrued if it is probable that a performance condition will be achieved. Compensation costs
for stock-based payments to employees that do not include performance conditions are recognized on a straight-line basis. The fair
value of all share purchase options is expensed over their vesting period with a corresponding increase to additional capital surplus.
Upon exercise of share purchase options, the consideration paid by the option holder, together with the amount previously
recognized in additional capital surplus, is recorded as an increase to share capital
F-14
�The Company uses the Black-Scholes option valuation model to calculate the fair value of share purchase options at the date of the
grant. Option pricing models require the input of highly subjective assumptions, including the expected price volatility. Changes
in these assumptions can materially affect the fair value estimate.
The compensation expense recognized for the years ended March 31, 2011 and 2010 was $42,016 and $125,004, respectively.
RECENTLY ISSUED ACCOUNTING PRONOUNCEMENTS
From time to time, new accounting pronouncements are issued by the Financial Accounting Standards Board, or FASB, or other
standard setting bodies that are adopted by us as of the specified effective date. Unless otherwise discussed, we believe that the
impact of recently issued standards that are not yet effective will not have a material impact on our consolidated financial position
or results of operations upon adoption.
In October 2009, the Financial Accounting Standards Board (“FASB”) issued ASU 200913, Multiple Deliverable Revenue
Arrangements. ASU 2009-13 provides principles and application guidance on whether multiple deliverables exist, how the
arrangement should be separated, and the consideration allocated. This standard shall be applied prospectively for revenue
arrangements entered into or materially modified in fiscal years beginning on or after June 15, 2010, with earlier application
permitted. Alternatively, an entity may elect to adopt this standard on a retrospective basis. Adoption of this standard is not
expected to have a material impact on the financial statements.
In March 2010, the FASB ratified Emerging Issues Task Force (EITF) Issue No. 089, “Milestone Method of Revenue
Recognition” (Issue 089). The Accounting Standards Update resulting from Issue 089 amends ASC 60528.1. The Task Force
concluded that the milestone method is a valid application of the proportional performance model when applied to research or
development arrangements. Accordingly, the consensus states that an entity can make an accounting policy election to recognize a
payment that is contingent upon the achievement of a substantive milestone in its entirety in the period in which the milestone is
achieved. The milestone method is not required and is not the only acceptable method of revenue recognition for milestone
payments. The guidance in Issue 08-9 is effective for fiscal years, and interim periods within those years, beginning on or after June
15, 2010, and may be applied: prospectively to milestones achieved after the adoption date, or retrospectively for all periods
presented. Adoption of this standard is not expected to have a material impact on the financial statements.
NOTE 2
MANAGEMENT’S LIQUIDITY PLANS
The Company reported net losses of $13,582,159 and $8,056,874 for the fiscal years ended March 31, 2011 and 2010, respectively.
At March 31, 2011, the Company had a working capital deficiency of approximately $1.5 million and an accumulated deficit of
approximately $114.9 million, consolidated assets of approximately $11.8 million, and negative stockholders’ equity of
approximately $17.9 million. The Company has not generated any significant profits to date. During the fiscal year ended March
31, 2011, the Company raised $1,062,500 of net proceeds from the sale of Series E Preferred Stock, and issued Series E Preferred
Stock with a face value of $1,062,500, with the payment for such Series E Preferred Stock being received during Fiscal 2010.
F-15
�The Company’s strategy is to continue to be engaged in the development and manufacturing of oral controlledrelease products. It
will continue to develop generic versions of controlled-release drug products with high barriers to entry and assist partner
companies in the life cycle management of products to improve off-patent drug products. The Company has two products currently
being sold commercially; a generic product recently purchased and being transferred to Elite but not yet being sold; an approval for
a generic product not yet being sold; and a pipeline of products under development.
As of March 31, 2011, the Company’s principal source of liquidity was approximately $1.8 million of cash and cash equivalents
The Company may also receive funds through the exercise of outstanding stock options and warrants and $0.6875 million from the
issuance of the Company’s Series E Convertible Preferred Stock pursuant to the Strategic Alliance Agreement with Epic
Pharma. However, there can be no assurance of the exercise of any outstanding options or warrants, the performance of Epic
Pharma under the Strategic Alliance Agreement, or that any cash received from such sources will be material to contribute sufficient
amounts to continue operating activities.
As a result there is no assurance that the Company’s business strategy will be successfully implemented, and with the Company’s
existing working capital levels, there can be no assurance that the Company will continue as a going concern.
NOTE 3
INVENTORIES
Inventories are recorded at the lower of cost or market. Inventories at March 31, 2011 and 2010 consist of the following:
Finished Goods
Raw Materials
Less: Inventory Valuation Reserve
2011
2010
$ 156,399 $ 164,529
1,507,419 1,701,188
1,663,818 1,865,717
(
1,047,456)
(494,425)
$ 616,362 $1,371,292
The Inventory Valuation Reserve as of March 31, 2011, consists of raw materials with an aggregate cost of $918,355 having no
commercial value due to the FDA’s decision to remove Lodrane from the market and the FDA’s recent reclassification of the
Company’s application to transfer the manufacturing site of Hydromorphone to its facilities from CBE30 to Prior Approval, as
well as $35,762 in expired raw materials which have not yet been destroyed and $93,339 in mark-to-market adjustments required
to fairly state the Company’s raw materials inventory at the lower of cost or market, with current replacement cost being the
standard upon which the market value is determined.
Please refer to the Current Reports on Form 8K filed with the SEC on March 4, 2011 and June 6, 2011 for details on the FDA’s
decision to remove Lodrane from the market and the FDA’s reclassification of the Company’s application for transfer of
manufacturing site, respectively, with such filings being herein incorporated by reference.
F-16
�The Inventory Valuation Reserve as of March 31, 2010, consisted of $494,425 in mark-to-market adjustments required to fairly
state the Company’s raw materials inventory at the lower of cost or market, with current replacement cost being the standard upon
which the market value is determined.
NOTE 4 PROPERTY AND EQUIPMENT
Property and equipment at March 31, 2011 and 2010 consists of the following:
Laboratory manufacturing, and warehouse equipment
Office equipment
Furniture and fixtures
Transportation equipment
Land, building and improvements
Equipment under capital lease
Less: Accumulated depreciation and amortization
2011
5,117,709 $
56,961
62,406
66,855
2,835,783
168,179
8,307,893
(4,189,619)
4,118,274 $
2010
5,089,540
56,961
62,406
66,855
2,492,152
168,179
7,936,093
(3,840,279)
4,095,814
$
$
Depreciation and amortization expense amounted to $483,473 and $508,610 for the years ended March 31, 2011 and 2010,
respectively.
NOTE 5
INTANGIBLE ASSETS
Costs to acquire intangible assets, such as asset purchases of Abbreviated New Drug Applications (“ANDA’s”) which are approved
by the FDA or costs incurred in the application of patents are capitalized and amortized on the straight-line method, based on their
estimated useful lives ranging from five to fifteen years, commencing upon approval of the patent or site transfers required for
commercialization of an acquired ANDA. Such costs are charged to expense if the patent application or ANDA site transfer is
unsuccessful.
As of March 31, 2011 and 2010, the following costs were recorded as intangible assets on the Company’s balance sheet:
F-17
�Intangible assets at beginning of fiscal year
Patent application costs
Trademarks
ANDA acquisitions
Less: Accumulated Amortization
Net Intangible Assets at beginning of fiscal year
Intangible asset costs capitalized during the fiscal year
Patent application costs
Trademarks
ANDA acquisition costs
Total cost of intangible assets capitalized
Amortization of intangible assets during fiscal year
Patent application costs
Trademarks
ANDA acquisition costs
Total amortization of intangible assets
Impairment of intangible assets during the fiscal year
Patent application costs
Trademarks
ANDA acquisition costs
Accumulated amortization of impaired assets
Net impairment of intangible assets
Intangible assets at end of fiscal year
Patent application costs
Trademarks
ANDA acquisition costs
Less: Accumulated Amortization
Net Intangible Assets
2011
2010
172,841
—
—
(76,434)
96,407
151,300
8,120
—
(131,677)
27,743
51,152
—
890,000
941,152
—
—
—
—
76,434
—
(440,000)
(76,434)
(440,000)
147,556
—
450,000
—
597,556
$
$
96,404
—
96,404
6,990
540
—
7,530
74,863
8,120
—
(62,773)
20,210
172,841
—
—
(76,434)
96,407
The costs incurred in patent applications totaling $51,152 and $96,404 for the 2011 and 2010 fiscal years, were all related to our
abuse resistant and extended release opioid product lines. The Company is continuing its efforts to achieve approval of such
patents. Additional costs incurred in relation to such patent applications will be capitalized as intangible assets, with amortization
of such costs to commence upon approval of the patents.
The ANDA acquisition costs of $890,000 incurred during the 2011 fiscal year, are related to our acquisition of the ANDA’s for
Hydromorphone 8mg, Naltrexone 50mg and Phentermine 37.5mg tablets. For further details on these acquisitions, please refer to
the current reports on Form 8-K filed with the SEC on May 24, 2010 for the Hydromorphone ANDA acquisition and September 1,
2010 for the Naltrexone and Phentermine ANDA acquisitions, such filings being herein incorporated by this reference. In addition,
please refer to exhibits 10.4, 10.5 and 10.7 of the quarterly report on Form 10-Q filed with the SEC on November 15, 2010 for the
purchase agreements for Hydromorphone, Naltrexone, and Phentermine, respectively, such filings being herein incorporated by this
reference.
The Company has successfully transferred production of the Phentermine 37.5mg product to its facilities and has commenced
commercial production of this product. Please refer to the current report on form 8K, filed with the SEC on April 7, 2011, such
filing being herein incorporated by reference.
F-18
�On May 31, 2011, the Company received a letter from the FDA responding to a Changes Being Effected in 30 Days (“CBE 30”)
supplement filed by the Company with the agency to change the manufacturing and packaging location of the Hydromorphone
Hydrochloride Tablets USP, 8mg ANDA purchased from Mikah Pharma. The letter from the FDA informed the Company that the
agency has reclassified the application as a prior approval supplemental application which will delay the commercialization of the
product. The delay imposed by such reclassification is a significant detrimental factor to the value of the Hydromorphone
AND. In accordance with GAAP, the Company recorded an impairment equal to the full historical cost.
The Company has also recorded an impairment equal to the full historical cost of the Naltrexone 50mg ANDA, as the reason given
by the FDA for the reclassification of the Company’s application filed with the FDA for Hydromorphone may also apply to a
similar application filed by the Company with the FDA for the transfer of manufacturing and packaging for Naltrexone 50mg.
NOTE 6
INVESTMENT IN NOVEL LABORATORIES INC.
At the end of 2006, Elite entered into a joint venture with VGS Pharma, LLC (“VGS”) and created Novel Laboratories, Inc.
( “Novel”), a privatelyheld company specializing in pharmaceutical research, development, manufacturing, licensing, acquisition
and marketing of specialty generic pharmaceuticals. Novel's business strategy is to focus on its core strength in identifying and
timely executing niche business opportunities in the generic pharmaceutical area. Elite’s ownership interest in Novel’s Class A
Voting Common Stock of Novel is approximately 10% of the outstanding shares of Class A Voting Common Stock of Novel. As
of October 1, 2007, Elite deconsolidated its financial statements from Novel and the investment in Novel is accounted for under the
cost method of accounting.
Since its inception, Novel has filed at least 11 Abbreviated New Drug Applications with the US Food and Drug
Administration. The first ANDA approval for Novel was received in Dec 2008 and at least three additional ANDA approvals were
received in 2009. Four of the Novel ANDAs have been granted firsttofile status.
In addition, Novel has acquired three ANDAs to supplement its own inhouse product development and marketing strategy. Novel
has publicly said that it has identified over 50 drug products which are in various stages of development that it plans to
commercialize in the coming years.
We also know from public information that Perrigo Company acquired rights in 2010 for an undisclosed amount to an additional
Novel ANDA approved in 2010 for the product HalfLytely®. Novel believes this is a first to file ANDA. Perrigo expects to be in
a position to launch a generic version of this product later this year and they expect to have 180 days of generic exclusivity. Novel
will manufacture the product exclusively for Perrigo. Annual sales for the branded product were approximately $80 million
according to Wolters Kluwer.
In accordance with GAAP, the company records an impairment write-down to such investments when the cost of the investment
exceeds its fair value and when the decline in value is determined to be other-than temporary. Indicators of an other-than-temporary
decline in value include, without limitation, the following:
F-19
�∙
∙
∙
∙
∙
A significant deterioration in the earnings performance, credit rating, asset quality, or business prospects of the investee
A significant adverse change in the regulatory, economic, or technological environment of the investee
A significant adverse change in the general market condition of either the geographic area or the industry in which the
investee operates
A bona fide offer to purchase (whether solicited or unsolicited), an offer by the investee to sell, or a completed auction
process for the same or similar security for an amount less than the cost of the investment
Factors that raise significant concerns about the investee's ability to continue as a going concern, such as negative cash
flows from operations, working capital deficiencies, or noncompliance with statutory capital requirements or debt
covenants.
A review and assessment of all documents available, public announcements by Novel and communications with the management of
Novel does not indicate the existence of impairment indicators. Accordingly, the Company determined that no impairment is
required in the valuation of its investment in Novel as of March 31, 2011. The valuation of the Company’s investment in Novel
remains at $3,329,322, an amount equal to the valuation as of March 31, 2010 with no impairment write downs.
NOTE 7 NJEDA BONDS
On September 2, 1999, the Company completed the issuance of tax exempt bonds by the New Jersey Economic Development
Authority (“NJEDA” or the “Authority”). The aggregate proceeds from the issuance of the fifteen year term bonds were
$3,000,000. Interest on the bonds accrues at 7.75% per annum. A portion of the proceeds were used by the Company to refinance
its land and building, and the remaining proceeds were intended to be used for the purchase of manufacturing equipment and
building improvements.
On August 31, 2005, the Company successfully completed a refinancing of a prior 1999 bond issue through the issuance of new
taxexempt bonds (the “Bonds”). The refinancing involved borrowing $4,155,000, evidenced by a 6.5% Series A Note in the
principal amount of $3,660,000 maturing on September 1, 2030 and a 9% Series B Note in the principal amount of $495,000
maturing on September 1, 2012. The net proceeds, after payment of issuance costs, were used (i) to redeem the outstanding
tax-exempt Bonds originally issued by the Authority on September 2, 1999, (ii) refinance other equipment financing and (iii) for
the purchase of certain equipment to be used in the manufacture of pharmaceutical products.
Interest is payable semiannually on March 1 and September 1 of each year. The Bonds are collateralized by a first lien on the
Company’s facility and equipment acquired with the proceeds of the original and refinanced Bonds. The related Indenture requires
the maintenance of a $415,500 Debt Service Reserve Fund consisting of $366,000 from the Series A Notes proceeds and $49,500
from the Series B Notes proceeds. The Debt Service Reserve is maintained in restricted cash accounts that are classified in Other
Assets. $1,274,311 of the proceeds had been deposited in a short-term restricted cash account to fund the purchase of manufacturing
equipment and development of the Company’s facility. As of September 30, 2010, all of these proceeds were utilized to upgrade
the Company’s manufacturing facilities and for the purchase of manufacturing and laboratory equipment.
F-20
�Bond issue costs of $354,000 were paid from the bond proceeds and are being amortized over the life of the bonds. Amortization of
bond issuance costs amounted to $3,533 and $10,598 for the three and nine months ended December 31, 2010, respectively.
The NJEDA Bonds require the Company to make an annual principal payment on September 1st of varying amounts as specified in
the loan documents and semi-annual interest payments on March 1st and September 1st, equal to interest due on the outstanding
principal at the applicable rate for the semi-annual period just ended.
The interest payment of $120,775 due on September 1, 2009, and three separate interest payments of $113,075 due on March 31,
2010, September 1, 2010 and March 1, 2011, respectively, were paid from the debt service reserve held in the restricted cash
account, due to the Company not having sufficient funds to make such payments when due.
The principal payment due on September 1, 2009, totaling $210,000 was paid from the debt service reserve held in the restricted
cash account, due to the Company not having sufficient funds to make the payment when due.
The Company did not have sufficient funds available to make the principal payments due on September 1, 2010 totaling $225,000
(the “2010 Principal Payment”), and requested the Trustee to withdraw the funds from debt service reserve held in the restricted
cash account and to utilize such funds to make the principal payment due. The Company’s request was denied by the
Trustee. Accordingly, the principal payment due on September 1, 2010, totaling $200,000 was not made.
Pursuant to the terms of the NJEDA Bonds, the Company is required to replenish any amounts withdrawn from the debt service
reserve and used to make principal or interest payments in six monthly installments, each being equal to one-sixth of the amount
withdrawn and with the first installment due on the 15th of the month in which the withdrawal from debt service reserve occurred
and the remaining five monthly payments being due on the 15th of the five immediately subsequent months. The Company has, to
date, made all payments required in relation to the withdrawals made from the debt service reserve on September 1, 2009, March 1,
2010, September 1, 2010 and March 1, 2011. The Company is required to make two additional monthly payments of $19,529
during the period June 29, 2011 through August, 2011, in order to fully replenish the March 1, 2011 withdrawal from the debt
service reserve.
The Company does not expect to have sufficient available funds to make the interest payment of $113,075 due on September 1,
2011 as well as principal payments totaling $245,000 due on September 1, 2011 (the “2011 Principal Payment”). Please note that
the 2011 Principal Payment is in addition to the 2010 Principal Payment, which has not yet been paid.
The Company has received Notice of Default from the Trustee of the NJEDA Bonds in relation to the withdrawals from the debt
service reserve, and has requested a postponement of principal payments due on September 1st of 2010, 2011 and 2012, with an
aggregate of all such postponed principal payments being added to the principal payments due on September 1, 2013. Resolution
of the Company’s default under the NJED Bonds and our request for postponement of principal payments will have a significant
effect on our ability to operate in the future.
F-21
�Due to issuance of a Notice of Default being received from the Trustee of the NJEDA Bonds, and until the event of default is
waived or rescinded, the Company has classified the entire principal due, an amount aggregating $3.385 million, as a current
liability.
Bond financing consisting of the following, as of March 31,
Refinanced NJEDA Bonds
Current portion
2011
2010
$
3,385,000
$
3,385,000
(3,385,000)
(3,385,000
Long term portion, net of current maturities
$
—
$
—
Maturities of Bonds for the next five years are as follows:
YEAR ENDING MARCH 31,
2012
2013
2014
2015
2016
Thereafter
NOTE 8 LOANS PAYABLE AND LONG TERM DEBT
Loans payable and long term debt consisted of the following:
AMOUNT
470,000
$
260,000
185,000
195,000
210,000
2,065,000
3,385,000
$
March 31, 2011
March 31, 2010
Current
Long-
Term
Current
Long-
Term
Note payable to First Niagara Bank in 60
monthly installments of $1,180, including
interest at the rate of 9.00% per annum;
Final payment in September 2012 ; Secured
by vehicle purchased with proceeds of loan $
Short term loan to finance commercial
insurance policy
Short term loan to finance directors &
officers insurance policy
13,105
$
6,717
$
11,793
$
19,823
9,701
60,808
TOTAL
$
13,105
$
6,717
$
82,302
$
19,823
F-22
�NOTE 9 LEASES OF RENTAL PROPERTIES
The following leases for rental properties were operative during the year ended March 31, 2011:
Effective Date
Termination Date
Lease term
80 Oak Street
Unit 102
August 1, 2009
135 Ludlow Ave
(see note 10)
July 1, 2010
November 30, 2010 December 31, 2015
Month-to-month 5 years with 2 tenant
renewal options for 5
years each
Rent expense for the 2011 Fiscal Year
$
29,102 $
67,753
Minimum 5 Year Lease Payments*
Fiscal year ended March 31, 2012
Fiscal year ended March 31, 2013
Fiscal year ended March 31, 2014
Fiscal year ended March 31, 2015
Fiscal year ended March 31, 2016
—
—
—
—
—
— $
79,248
81,228
83,259
85,344
87,363
416,442
* Minimum lease payments are exclusive of additional expenses related to certain expenses incurred in the operation and
maintenance of the premises, including, without limitation, real estate taxes and common area charges which may be due under the
terms and conditions of the lease, but which are not quantifiable at the time of filing of this annual report on Form 10-K
The real estate leases are recorded as operating leases.
The lease for 80 Oak Street was a month-to-month lease, and accordingly the rent expense was equal to rent payments made during
Fiscal Year 2011.
Rent expense related to the operating lease at 135 Ludlow was recorded using the straight line method and summarized as follows:
F-23
�Summary of Rent Expense – 135 Ludlow Avenue
Rent Expense
Actual lease payments
Increase in deferred rent liability
Balance of deferred rent liability
NOTE 10 LEASE OF 135 LUDLOW AVENUE
Fiscal Year
Ended
March 31, 2011
67,753
19,689
48,064
48,064
The Company entered into a lease for a portion of a one-story warehouse, located at 135 Ludlow Avenue, Northvale, New Jersey,
consisting of approximately 15,000 square feet of floor space. The lease term began on July 1, 2010 and is classified as an
operating lease.
The lease includes an initial term of 5 years and 6 months and the Company has the option to renew the lease for two additional 5
year terms. The property related to this lease will be used for the storage of pharmaceutical finished goods, raw materials,
equipment and documents as well as pharmaceutical manufacturing, packaging and distribution activities.
This property requires significant leasehold improvements and qualification as a prerequisite to achieving suitability for such
intended future use.
Leasehold improvements and qualification as suitable for manufacturing, packaging and distribution operations are expected to be
achieved within two years from the beginning of the lease term. These are estimates based on current project plans, which are
subject to change. There can be no assurance that the construction and qualification will be accomplished during the estimated time
frames, or that the property located at 135 Ludlow Avenue, Northvale, New Jersey will ever achieve qualification for intended future
utilization.
Please refer to Note 9 of these financial statements for details on minimum lease payments, rent expense and deferred rent liabilities.
NOTE 11 LEASE TERMINATION COSTS - 135 LUDLOW AVENUE
The lease for the property located at 135 Ludlow Avenue, Northvale NJ, includes a requirement that, at termination, the Company
return the property to its condition at the inception of the lease, with normal wear and tear excepted. Such requirement accordingly
represents an unconditional obligation associated with the retirement of a long-lived asset and subject to ASC 410 of the
Codification. The Company estimates such costs would amount to $50,000, at lease termination, and pursuant to ASC 410 has
recorded a liability and offsetting asset equal to the present value, at lease inception, of such obligation. This liability is accreted
over the term of the lease (including extensions), using the interest method.
F-24
�NOTE 12 DEFERRED REVENUES
Deferred revenues in the aggregate amount of $192,222, consisting of a current component of $13,333 and a long term component
of $178,890 represents the unamortized amount of a $200,000 advance payment received for a licensing agreement with a fifteen
year term beginning in September 2010 and ending in August 2025. The advance payment was recorded as deferred revenue when
received and is earned, on a straight line basis over the fifteen year life of the license. The current component is equal to the
amount of revenue to be earned during the 12 month period immediately subsequent to the balance date and the long term
component is equal to the amount of revenue to be earned thereafter.
NOTE 13 PREFERRED SHARE DERIVATIVE INTEREST PAYABLE
Preferred share derivative interest payable as of March 31, 2011 consisted of $282,680 in derivative interest accrued as of March 31,
2011. The full amount of derivative interest payable as of March 31, 2011 was paid via the issuance of 4,775,017 shares of
Common Stock, in lieu of cash, in April 2011.
Preferred share derivative interest payable as of March 31, 2010 consisted of $306,440 in derivative interest accrued as of March 31,
2010. The full amount of derivative interest payable as of March 31, 2011 was paid via the issuance of 3,402,813 shares of
Common Stock, in lieu of cash, in April 2010.
NOTE 14 DERIVATIVE LIABILITIES – PREFERRED SHARES
Accounting Standard Codification “ASC” 815 – Derivatives and Hedging, which provides guidance on determining what types of
instruments or embedded features in an instrument issued by a reporting entity can be considered indexed to its own stock for the
purpose of evaluating the first criteria of the scope exception in the pronouncement on accounting for derivatives. These
requirements can affect the accounting for warrants and convertible preferred instruments issued by the Company. As the
conversion features within, and the detachable warrants issued with the Company’s Series B, Series C, Series D and Series E
Preferred Stock, do not have fixed settlement provisions because their conversion and exercise prices may be lowered if the
Company issues securities at lower prices in the future, we have concluded that the instruments are not indexed to the Company’s
stock and are to be treated as derivative liabilities.
Preferred Stock Derivative Liabilities – Fiscal Year 2011
Series B
Series D
Series C
Series E
Total
Preferred shares
Outstanding as of March
31, 2011
Underlying common
shares into which
Preferred may convert
Closing price on
valuation date
Preferred stock
derivative liability at
March 31, 2011
896
5,418
4,063
3,062.5
13,439.5
730,274
4,280,842
58,042,861
118,898,957 181,952,934
$
0.078 $
0.078 $
0.078 $
0.078 $
0.078
$
56,961 $
333,906 $
4,527,343 $
9,274,119 $
14,192,329
Change in preferred stock derivative liability for the 2011 Fiscal Year
$
10,416,376
F-25
�The change of $10,416,375 in value of the preferred stock derivative liability occurring during the 2011 Fiscal Year is included in
the amount reported in the “Other Income/(Expense)” section of the statement of operations. Increases in value are reported as
other expenses and decreases in value are reported as other income.
Preferred shares
Outstanding as of March
31, 2010
Underlying common
shares into which
Preferred may convert
Closing price on
valuation date
Preferred stock
derivative liability at
March 31, 2010
Preferred Stock Derivative Liabilities – Fiscal Year 2010
Series B
Series C
Series D
Series E
Total
896
5,418
9,008
2,000
17,322
574,076
3,365,217
45,037,200
44,256,006 93,232,499
$
0.085 $
0.085 $
0.085 $
0.085 $
0.085
$
48,797 $
286,043 $
3,828,162 $
3,761,761 $
7,924,763
Change in preferred stock derivative liability for the 2010 Fiscal Year
$
283,920
The change of $283,920 in value of the preferred stock derivative liability occurring during the 2011 Fiscal Year is included in the
amount reported in the “Other Income/(Expense)” section of the statement of operations. Increases in value are reported as other
expenses and decreases in value are reported as other income.
NOTE 15 DERIVATIVE LIABILITIES - WARRANTS
To date, the Company has authorized the issuance of Common Stock Purchase Warrants, with terms of five to seven years, to
various corporations and individuals, in connection with the sale of securities, loan agreements and consulting
agreements. Exercise prices range from $0.0625 to $3.25 per warrant. The warrants expire at various times through March 31,
2018.
F-26
�A summary of warrant activity for the fiscal years indicated below is as follows:
Fiscal Year 2011
Fiscal Year 2010
Balance at beginning of year
125,299,740
$
0.25
Weighted
Average
Exercise
Price
Warrant
Shares
Warrant
Shares
39,667,853
$
Warrants issued
40,000,000
$
0.06
80,000,000
$
Exchange warrants issued
—
—
5,806,887
$
Warrant exercises, forfeited or expired
9,974,692
$
0.69
175,000
$
Ending Balance
155,325,048
$
0.15
125,299,740
$
Weighted
Average
Exercise
Price
0.63
0.06
0.25
2.82
0.25
Accounting Standard Codification “ASC” 815 – Derivatives and Hedging, which provides guidance on determining what types of
instruments or embedded features in an instrument issued by a reporting entity can be considered indexed to its own stock for the
purpose of evaluating the first criteria of the scope exception in the pronouncement on accounting for derivatives. These
requirements can affect the accounting for warrants and convertible preferred instruments issued by the Company. As the
conversion features within, and the detachable warrants issued with the Company’s Series B, Series C, Series D and Series E
Preferred Stock, do not have fixed settlement provisions because their conversion and exercise prices may be lowered if the
Company issues securities at lower prices in the future, we have concluded that the instruments are not indexed to the Company’s
stock and are to be treated as derivative liabilities.
The portion of derivative liabilities related to outstanding warrants was valued using the Black-Scholes option valuation model
and the following assumptions on the following dates:
RiskFree interest rate
Expected volatility
Expected life (in years)
Expected dividend yield
Number of warrants
March 31
2011
.09% 2.9%
138% - 194%
0.3 – 7.0
—
155,325,048
March 31
2010
2.4% 3.3%
126% - 214%
0.5 – 6.6
—
125,299,740
Fair value – Warrant Derivative Liability
$
10,543,145
$
8,499,423
Change in warrant derivative liability for the twelve months ended $
1,297,998
$
3,792,130
F-27
�The risk free interest rate was based on rates established by the US Treasury Department. The expected volatility was based on the
historical volatility of the Company’s share price for periods equal to the expected life of the outstanding warrants at each valuation
date. The expected dividend rate was based on the fact that the Company has not historically paid dividends on common stock
and does not expect to pay dividends on common stock in the future.
The changes of $1,297,998 and $ 3,792,130 in value of the warrant derivative liability occurring during the years ended March 31,
2011 and 2010, respectively, are included in the amounts reported in the “Other Income/(Expense)” section of the statement of
operations. Increases in value are reported as other expenses and decreases in value are reported as other income.
NOTE 16 BENEFICAL CONVERSION FEATURES OF SERIES E PREFERRED SHARES
The Series E Preferred shares include an option, exercisable from the issuance date, to convert to common shares at prices which
were less than the market price of the Company’s Common Stock on the date such Series E Preferred shares were issued. The
difference between the share price and option price represents a beneficial conversion feature existing on the issue date.
In accordance with GAAP, the beneficial conversion feature was valued separately and allocated to additional paid in capital. The
valuations were calculated using the relative fair value method allocating the proceeds from each issuance of the Series E Preferred
shares to the conversion option and detachable warrants, if such warrants were included with an issuance.
The beneficial conversion option is then required to be recognized as a discount and amortized over a period that begins on the date
of issuance and ends on the earliest conversion date. As the conversion options were exercisable on their issue date, the full value
assigned to the conversion option was immediately amortized and charged to interest expense.
During Fiscal Year 2011, the Company had two separate issuances of Series E Preferred Stock, consisting of 62.5 shares issued in
September 2010 and 1,000 shares issued in March 2011.
The valuation of the beneficial conversion features, and detachable warrants, were applicable, for each issuance of Series E Preferred
Stock occurring during Fiscal Year 2011 is summarized as follows:
F-28
�Allocation of proceeds to conversion option
Proceeds from issuance of Series E shares
Value of detachable warrants – March 2011 only (see BlackScholes
calculation below)
Total of proceeds plus warrants
Allocation % attributable to Series E shares (quotient of proceeds divided
by proceeds plus warrant value)
Proceeds allocated to conversion option
Proceeds allocated to warrants
Gross value of beneficial conversion option
Share price on date of issuance
Conversion option price
Beneficial conversion feature per share
Common shares on conversion
Gross value of beneficial conversion feature
Beneficial Conversion Feature Recorded (lesser of gross value or
proceeds allocated)
Sept 2010
Issuance
March 2011
Issuance
$
62,500
$
1,000,000
-0-
62,500
2,951,297
3,951,297
100%
25.3%
62,500
—
$
$
253,081
746,919
0.0600
0.0369
0.0231
1,693,870
39,132
$
$
$
$
0.0780
0.0258
0.0522
38,824,149
2,028,284
39,132
$
253,081
$
$
$
$
$
$
The warrants issued with the Series E Preferred shares were valued using the Black-Scholes option valuation model, with the
following assumptions:
Risk-free interest rate
Expected volatility
Expected life (in years)
Number of warrants
Fair value
March 2011
Issuance
2.90%
138.4%
7
40 million
2,951,297
$
During Fiscal Year 2010, the Company had two separate issuances of Series E Preferred Stock, consisting of 1,000 shares issued in
June 2009 and 1,000 shares issued in October 2009.
The valuation of the beneficial conversion features, and detachable warrants, were applicable, for each issuance of Series E Preferred
Stock occurring during Fiscal Year 2010 is summarized as follows:
Allocation of proceeds to conversion option
Proceeds from issuance of Series E shares
Value of detachable warrants – (see BlackScholes calculation below)
Total of proceeds plus warrants
Allocation % attributable to Series E shares (quotient of proceeds
divided by proceeds plus warrant value)
Proceeds allocated to conversion option
Proceeds allocated to warrants
Gross value of beneficial conversion option
Share price on date of issuance
Conversion option price
Beneficial conversion feature per share
Common shares on conversion
Gross value of beneficial conversion feature
June 2009
Issuance
October 2009
Issuance
$
1,000,000
2,869,361
3,869,361
1,000,000
2,931,983
3,931,983
25.9%
25.4%
258,700
741,300
$
$
254,212
745,788
0.0800
0.0500
0.0300
20,000,000
600,000
$
$
$
$
0.08
0.05
0.03
20,000,000
715,282
$
$
$
$
$
$
Beneficial Conversion Feature Recorded (lesser of gross value or
proceeds allocated)
$
600,000
$
254,212
F-29
�The warrants issued with the Series E Preferred shares were valued using the Black-Scholes option valuation model, with the
following assumptions:
Risk-free interest rate
Expected volatility
Expected life (in years)
Number of warrants
Fair value
NOTE 17 COMMON STOCK
June 2009
Issuance
October 2009
Issuance
2.31%
115.2%
7
40 million
2,869,361
$
2.21%
123.3%
7
40 million
2,931,983
During Fiscal Year 2011, the Company issued a total of 96,595,489 shares of Common Stock, with such issuances of Common
Stock being summarized as follows:
Description
Shares
Of
Common Stock
Common Shares issued in lieu of cash payment in payment of preferred share derivative
interest expenses totaling $1,283,240
21,241,590
Common Shares issued pursuant to the conversion of Series D Convertible Preferred Share
derivatives, with such derivative liabilities totaling $4,465,584 at the time of their
conversion.
Common Shares issued in payment of $75,000 due and payable pursuant to the Asset
Purchase Agreement dated 5/18/2010.
Common Shares issued in lieu of cash in payment of consulting expenses totaling
$13,737.
Common Shares issued in payment of Director’s fees totaling $99,743
Common shares issued in payment of employee salaries totaling $37,210
Total Common Shares issued during Fiscal Year 2011
Common Shares outstanding at March 31, 2010
Common Shares outstanding at March 31, 2011
F-30
70,649,154
937,500
343,425
2,493,589
930,231
96,595,489
83,950,168
180,545,657
�NOTE 18 PER SHARE INFORMATION
Basic earnings per share of common stock (“Basic EPS”) is computed by dividing the net income(loss) by the weightedaverage
number of shares of common stock outstanding. Diluted earnings per share of common stock (“Diluted EPS”) is computed by
dividing the net income(loss) by the weighted-average number of shares of common stock and dilutive common stock equivalents
and convertible securities then outstanding. GAAP requires the presentation of both Basic EPS and Diluted EPS, if such Diluted
EPS is not antidilutive, on the face of the Company’s Consolidated Statements of Operations. As the Company had a net loss for
Fiscal Year 2011 and Fiscal Year 2010, Diluted EPS is not presented as the effect of the Company’s common stock equivalents and
convertible securities is anti-dilutive.
Basic EPS is calculated as follows:
Fiscal Year
2011
Fiscal Year
2010
Numerator
Net (Loss) attributable to common shareholders
$
(13,582,159) $
(8,056,874)
Denominator
Weighted average shares of common stock outstanding
100,020,520
75,581,345
Net (Loss) per Share – Basic and Diluted
$
(0.14) $
(0.11)
Potentially dilutive securities excluded from the calculation of diluted loss per share
( in accordance with GAAP)
Stock Options
Convertible Preferred Stock
Warrants
3,057,000
3,287,000
180,881,120
94,370,379
155,325,048
125,469,740
F-31
�NOTE 19 STOCK-BASED COMPENSATION
Part or all of the compensation paid by the Company to its Directors and employees consists of the issuance of Common Stock or
via the granting of options to purchase Common Stock
Stock-based Director Compensation
The Company’s Director compensation policy instituted in October 2009 includes provisions that Director’s fees are to be paid via
the issuance of shares of the Company’s Common Stock, in lieu of cash, with the valuation of such shares being calculated on a
quarterly basis and equal to the average closing price of the Company’s common stock for the quarter just ended.
During Fiscal Year 2011, the Company issued 2,493,589 shares of Common Stock to its Directors in payment of Director’s fees in
the aggregate amount of $99,743 and related to the period beginning on October 1, 2009 and ending on December 31,
2010. Please note that the shares issued during Fiscal Year 2011, include those shares owed and not yet issued at the end of Fiscal
Year 2010.
As of March 31, 2011, the Company owes its Directors a total of 592,996 shares of Common Stock in payment of Directors Fees
totaling $32,500 for the three months ended March 31, 2011. The Company anticipates that these shares of Common Stock will
be issued during the fiscal year ended March 31, 2012.
Stock-based Employee Compensation
Employment contracts with the Company’s President, Chief Financial Officer and certain other employees includes provisions for a
portion of each employees salaries to be paid via the issuance of shares of the Company’s Common, in lieu of cash, with the
valuation of such shares being calculated on a quarterly basis and equal to the average closing price of the Company’s common
stock for the quarter just ended.
During Fiscal Year 2011, the Company issued a total of 930,231 shares of Common Stock to its President, Chief Financial Officer
and certain other employees in payment of salaries in the aggregate amount of $37,210 and related to the period beginning on
October 1, 2009 and ending on December 31, 2010. Please note that the shares issued during Fiscal Year 2011, include those
shares owed and not yet issued at the end of Fiscal Year 2010.
As of March 31, 2011, the Company owes its President, Chief Financial Officer and certain other employees a total of 273,690
shares of Common Stock in payment of salaries totaling $15,000 for the three months ended March 31, 2011, with such amount
being recorded in accrued expenses. The Company anticipates that these shares of Common Stock will be issued during the fiscal
year ended March 31, 2012.
Stock option based Employee Compensation
During the years ended March 31, 2011 and 2010, the Company issued zero and 1,000,000, respectively, options to purchase
Common Stock to employees. The options issued during Fiscal 2010 have an exercise price of $0.10, vest over a three year
period which commences one year from the date of grant and expire ten years from the date of grant. The fair value of the options
granted during Fiscal Year 2010 was $93,452, computed using the BlackScholes options pricing model on the grant date. Such
fair value is being amortized by the Company, on a straight line basis, over the vesting period, and recorded on the Company’s
Statement of Income as “Noncash compensation through the issuance of stock options”.
F-32
�In addition to the stock options granted in Fiscal 2010, the amount recorded on the Company’s Statement of Income as noncash
compensation through the issuance of stock options includes amortization of the fair value of stock options granted prior to Fiscal
Year 2010. The fair value of these options, totaling $196,983 on the date of such grants, was fully amortized by the end of Fiscal
Year 2011.
Stock option based employee compensation is summarized as follows:
Fiscal Year
2011
Fiscal Year
2010
Non-cash compensation expense related to stock options granted prior to
Fiscal Year 2010
$
17,056
$
118,514
Non-cash compensation expense related to stock options granted during
Fiscal Year 2010
24,960
6,490
Total non-cash compensation through the issuance of stock options
$
42,016
$
125,004
NOTE 20 STOCK OPTION PLANS
Under its 2004 Stock Option Plan and prior options plans, the Company may grant stock options to officers, selected employees,
as well as members of the Board of Directors and advisory board members. All options have generally been granted at a price
equal to or greater than the fair market value of the Company’s Common Stock at the date of the grant. Generally, options are
granted with a vesting period of up to three years and expire ten years from the date of grant.
Transactions under the plans for years indicated were as follows:
Fiscal Year 2011
Fiscal Year 2010
Weighted
Average
Exercise
Price
Options
Options
Outstanding at beginning of year
3,287,000 $
1.41
2,554,900 $
Weighted
Average
Exercise
Price
1.87
0.10
—
—
—
1,000,000 $
—
230,000 $
0.10
(267,900) $
0.87
Options Granted
Options Exercised
Options Expired
Options Vested
Outstanding at end of year
3,057,000 $
1.51
3,287,000 $
1.41
F-33
�The following table summarizes information about stock options outstanding at March 31, 2011:
Options
Range
Outstanding
$ 0.01 – 1.00
1.01 – 2.00
2.01 – 3.00
968,000
99,000
1,990,000
Weighted
Average
Remaining
Contractual
Life
(Years)
Weighted
Average
Exercise
Price
Options
Exercisable
Weighted
Average
Exercise
Price
8.58 $
6.82 $
6.06 $
0.09
1.08
2.22
444,667 $
95,999 $
1,490,000 $
0.08
1.08
2.22
1.69
$ 0.01 – 3.00
6.88 $
1.51
$
There are 6,520,100 options available for future grant under our Stock Option Plan.
NOTE 21 INCOME TAXES
The components of the credit for income taxes are as follows:
Federal:
Current
Deferred
State
Current
Deferred
Sale of New Jersey Net Operating Losses
Net Credit for Income Taxes
Year Ended March 31,
2010
2011
$
$
$
$
$
—
—
(10,422) $
—
311,835
$
301, 413
$
—
—
—
—
—
—
The Major components of deferred tax assets and liabilities at March 31, 2011 and 2010 are as follows:
Federal
Net Operating Loss Carry forward
Less: Deferred Tax Liability
Subtotal
Valuation Allowance
State
Net Operating Loss Carryforwards
Less: Deferred Tax Liability
Subtotal
Valuation Allowance
F-34
March 31,
2011
2010
(305,716)
$ 17,789,382 $ 17,604,348
—
17,483,666 17,604,348
(17,483,666) (17,604,348)
—
— $
$
2,223,278
(68,786)
2,154,492
(2,154,492)
— $
2,481,065
—
2,481,065
(2,481,065)
—
$
�At March 31, 2011 and 2010, a 100% valuation allowance is provided, as it is uncertain if the deferred tax assets will provide any
future benefits because of the uncertainty about the Company’s ability to generate the future taxable income necessary to use the net
operating loss carryforwards.
NOTE 22 REMOVAL OF LODRANE PRODUCTS FROM THE US MARKET
On March 3, 2011, the U.S. Food and Drug Administration (“USFDA”) announced its intention to remove approximately 500
cough/cold and allergy related products from the U.S. market. The Company manufactured two of the drugs impacted by the
USFDA’s action. The affected products are:
Product
Lodrane® 24 Capsules
Lodrane® 24D Capsules
Active Ingredient , Strength
Brompheniramine maleate, 12mg
Brompheniramine maleate, 12mg/pseudoephedrine HCl, 90mg
According to the press release issued by the US-FDA, manufacturers must stop manufacturing the affected products within 90 days
after March 3, 2011 and distribution of the effected products must stop within 180 days after March 3, 2011.
For the year ended March 31, 2011, gross revenues earned by the Company from the Lodrane® products equaled $4.2 million, or
approximately 97% of the Company’s total income for the year.
Shortly after the announcement by the USFDA, the Company’s customer for the Lodrane® products cancelled all outstanding
orders, other than those for which manufacturing had already begun, advising the Company that existing stocks of Lodrane® were
sufficient and that additional quantities could not be sold prior to the 180 day deadline announced by the US-FDA.
The last shipment of Lodrane® products was made by the Company in April 2011 and manufacturing of Lodrane® has ceased.
While the timing of the announcement by the USFDA resulted in such having a minimal effect on the Company’s operations for
the 2011 Fiscal Year, the Company’s inability to manufacture Lodrane® has a material and adverse effect on its revenues for periods
beginning after March 31, 2011.
Please refer to the Current Report on Form 8-K filed with the SEC on March 4, 2011, such filing being herein incorporated by
reference, for further details on this announcement.
F-35
�NOTE 23 MAJOR CUSTOMERS
One customer accounted for approximately 97 percent and 100 percent of revenues for the years ended March 31, 2011 and 2010,
respectively.
Please note that this major customer was the purchaser of the Lodrane® products, which have been discontinued pursuant to an
announcement by the US-FDA.
Shortly after the announcement by the US-FDA, this customer cancelled all outstanding orders, other than those for which
manufacturing had already begun, advising the Company that existing stocks of Lodrane® were sufficient and that additional
quantities could not be sold prior to the 180 day deadline announced by the US-FDA.
The last shipment of Lodrane® products was made by the Company in April 2011 and manufacturing of Lodrane® has ceased.
While the timing of the announcement by the USFDA resulted in such having a minimal effect on the Company’s operations for
the 2011 Fiscal Year, the Company’s inability to manufacture Lodrane® has a material and adverse effect on its revenues for periods
beginning after March 31, 2011.
Please refer to Note 22 to these financial statements and the Current Report on Form 8-K filed with the SEC on March 4, 2011,
such filing being herein incorporated by reference, for further details on this announcement.
NOTE 24 SETTLEMENT OF MIDSUMMER INVESTMENTS, Ltd. Et al v. Elite Pharmaceuticals Inc.
Midsummer Investments, Ltd., et al. v. Elite Pharmaceuticals, Inc. – On or about September 22, 2009, Midsummer Investments,
Ltd. (“Midsummer”) and Bushido Capital Master Fund, LP (“Bushido”, and together with Midsummer, the “Plaintiffs”) filed a
complaint against Elite Pharmaceuticals, Inc., a Delaware corporation (the “Company”), in the United States District Court,
Southern District of New York (Case No. 09 CIV 8074) (the “Action”). The Plaintiffs asserted claims for breach of contract
(injunctive relief and damages), anticipatory breach of contract (injunctive relief), conversion (injunctive relief and damages), and
attorneys’ fees, arising out of a Securities Purchase Agreement, dated September 15, 2008, by and among the Company and certain
purchasers of the Company’s securities (including the Plaintiffs) and the Certificate of Designation of Preferences, Rights and
Limitations of Series D 8% Convertible Preferred Stock, filed with the Secretary of State of the State of Delaware on September 15,
2009 (the “Series D Certificate”). Plaintiffs claimed that they were entitled to a reduced conversion price for their Series D 8%
Convertible Preferred Stock, par value US$0.01 per share (the “Series D Preferred Stock”), as a result of the Strategic Alliance
Agreement, dated March 18, 2009, as amended (the “Epic SAA”), by and among the Company, on the one hand, and Epic
Pharma, LLC (“Epic”) and Epic Investments, LLC (“Epic Investments”, and together with Epic, the “Epic Parties”). With their
complaint, the Plaintiffs concurrently filed a request for preliminary injunction. Pursuant to an order of the Court entered into on
October 16, 2009, the Plaintiffs’ request for a preliminary injunction was denied. Thereafter, Plaintiffs filed an amended complaint
(the “Complaint”), asserting claims for breach of contract (injunctive relief and damages), anticipatory breach of contract (injunctive
relief), conversion (damages) and attorneys’ fees, seeking compensatory damages of $7,455,363.00, delivery of 1,000,000 shares of
the Company’s common stock, par value $0.001 per share (the “Common Stock”), a declaration that all future conversions of the
Series D Preferred Stock, held by Plaintiffs is at a conversion price of $0.05, attorneys’ fees, interest and costs.
F-36
�The Company disputed the claims in the Complaint, believing the lawsuit to be without merit, and vigorously defended against
them. The Company moved for summary judgment on the Complaint and the judge in the case did not issue an order on such
motion. The Company proceeded with extensive, timeconsuming and costly discovery. The court scheduled the trial to
commence on June 28, 2010.
In order to avoid the delays, expense and risks inherent in litigation, after extensive negotiations, the Company entered into (i) a
Stipulation of Settlement and Release, dated June 25, 2010 (the “Settlement Agreement”), with the Plaintiffs and the Epic Parties,
(ii) an Amendment Agreement, dated June 25, 2010 (the “Series D Amendment Agreement”), with the Plaintiffs and (iii) an
Amendment Agreement, dated June 25, 2010 (the “Series E Amendment Agreement”) with the Epic Parties. As part of the
Settlement Agreement, the Action will be dismissed with prejudice.
Series D Amendment Agreement
Pursuant to the Series D Amendment Agreement, the Company and Plaintiffs agreed to amend the Series D Certificate. The
holders of at least 50.1%, in the aggregate, of the Company’s outstanding Series B Preferred 8% Convertible Preferred Stock, par
value US$0.01 per share, Series C 8% Convertible Preferred Stock, par value US$0.01 per share, and Series D Preferred Stock,
voting as one class, consented to the filing of the Amended Certificate of Designations of the Series D 8% Convertible Preferred
Stock (the “Amended Series D Certificate”) with the Secretary of State of the State of Delaware. On June 29, 2010, pursuant to the
authority of its Board of Directors, the Company filed with the Secretary of State of the State of Delaware the Amended Series D
Certificate.
Pursuant to the terms of the Amended Series D Certificate, the terms of the Series D Preferred Stock have been amended as follows:
∙
∙
Dividends: The Series D Preferred Stock will continue to accrue dividends at the rate of 8% per annum on their stated value of
US$1,000 per share, payable quarterly on January 1, April 1, July 1 and October 1 and such rate shall not increase to 15% per
annum as previously provided prior to giving effect to the Series D Amendment Agreement. In addition to being payable in cash
and shares of Common Stock, as provided in the Series D Certificate, such dividends may also be paid in shares of Series D
Preferred Stock (the “Dividend Payment Preferred Stock”) or a combination of cash, Common Stock and Dividend Payment
Preferred Stock. Dividend Payment Preferred Stock will have the same rights, privileges and preferences as the Series D Preferred
Stock, except that such Dividend Payment Preferred Stock will not be entitled to, nor accrue, any dividends pursuant to the
Amended Series D Certificate.
Conversion Price: The conversion price of the Series D Preferred Stock shall be reduced from US$0.20 per share to US$0.07 per
share (subject to adjustment as provided in the Amended Series D Certificate).
F-37
�∙
Automatic Monthly Conversion: On each Monthly Conversion Date (as defined below), a number of shares of Series D Preferred
Stock equal to each holder’s prorata portion (based on the shares of Series D Preferred Stock held by each Holder on June 25, 2010)
of the Monthly Conversion Amount (as defined below) will automatically convert into shares of Common Stock at the then-effective
conversion price (each such conversion, a “Monthly Conversion”). Notwithstanding the foregoing, the Company will not be
permitted to effect a Monthly Conversion on a Monthly Conversion Date unless (i) the Common Stock shall be listed or quoted for
trading on a trading market, (ii) there is a sufficient number of authorized shares of Common Stock for issuance of all Common
Stock to be issued upon such Monthly Conversion, (iii) as to any holder of Series D Preferred Stock, the issuance of the shares will
not cause a breach of the beneficial ownership limitations set forth in the Amended Series D Certificate, (iv) if requested by a holder
of Series D Preferred Stock and a customary Rule 144 representation letter relating to all shares of Common Stock to be issued upon
each Monthly Conversion is provided by such holder after request from the Company, the shares of Common Stock issued upon
such Monthly Conversion are delivered electronically through the Depository Trust Company or another established clearing
corporation performing similar functions (“DTC”), may be resold by such holder pursuant to an exemption under the Securities Act
and are otherwise free of restrictive legends and trading restrictions on such Holder, (v) there has been no public announcement of a
pending or proposed Fundamental Transaction or Change of Control Transaction (as such terms are defined in the Amended Series
D Certificate) that has not been consummated, (vi) the applicable holder of Series D Preferred Stock is not in possession of any
information provided to such holder by the Company that constitutes material non-public information, and (vii) the average VWAP
(as defined in the Amended Series D Certificate) for the 20 trading days immediately prior to the applicable Monthly Conversion
Date equals or exceeds the theneffective conversion price of the Series D Preferred Stock. Shares of the Series D Preferred Stock
issued to the holders of Series D Preferred Stock as Dividend Payment Preferred Stock shall be the last shares of Series D Preferred
Stock to be subject to Monthly Conversion. As used herein, the following terms have the following meanings: (i) “Monthly
Conversion Date” means the first day of each month, commencing on August 1, 2010, and terminating on the date the Series D
Preferred Stock is no longer outstanding; (ii) “Monthly Conversion Amount” means an aggregate Stated Value of Series D Preferred
Stock among all Holders that is equal to 25% of aggregate dollar trading volume of the Common Stock during the 20 trading days
immediately prior to the applicable Monthly Conversion Date (such 20 trading day period, the “Measurement Period”), increasing
to 35% of the aggregate dollar trading volume during the Measurement Period if the average VWAP during such Measurement
Period equals or exceeds $0.12 (subject to adjustment for forward and reverse stock splits and the like that occur after June 25, 2010)
and further increasing to 50% of the aggregate dollar trading volume during such Measurement Period if the average VWAP during
such Measurement Period equals or exceeds $0.16 (subject to adjustment for forward and reverse stock splits and the like that occur
after June 25, 2010).
∙
Change of Control Transaction: Epic and its affiliates were expressly excluded from any event which would otherwise constitute a
“Change of Control Transaction” due to the acquisition in excess of 40% of the Company’s voting securities.
Pursuant to the Series D Amendment Agreement, the exercise price of the Warrants (the “Series D Warrants”) to purchase shares of
Common Stock issued to the holders of Series D Preferred Stock pursuant to the Securities Purchase Agreement, dated as of
September 15, 2008, by and among the Company and the purchasers of Series D Preferred Stock will be reduced from $0.25 per
share to US$0.125. In addition, the exercise price of the Series D Warrants may be reduced as follows:
(i)
(ii)
by 20%, if on September 15, 2011, the holder of such Warrant still beneficially owns more than 50% of the Series D Preferred
Stock beneficially owned by such holder as of June 25, 2010 (“Base Ownership”); and
by 20%, if (a) on September 15, 2011, such holder then beneficially owns more than 25% of the Base Ownership and 50% or less
of the Base Ownership and (b) on September 15, 2012, such holder then beneficially owns more than 25% of the Base Ownership.
Notwithstanding the foregoing, (x) in no event will the exercise price of the Series D Warrants be reduced more than once as a
result of the amendments to such Series D Warrants, and (y) in the event that on September 15, 2011 or, if the condition of clause
(ii)(a) above is met, on September 15, 2012, the Holder beneficially owns 25% or less of the Base Ownership, then no adjustment
shall occur pursuant to the Series D Warrants, as amended by the Series D Amendment Agreement. Additionally, there will be no
corresponding increase in the number of shares of Common Stock issuable upon exercise of the Warrants solely as a result of the
foregoing adjustments.
F-38
�To the extent such issuance does not cause the breach of the beneficial ownership limitations set forth in the Amended Series D
Certificate (any excess shares will be issued to the affected holder of Series D Preferred Stock upon written notice from such holder
when such holder’s beneficial ownership is below 9.9% to the extent that such issuance does not cause such holder to exceed such
amount), the Company agreed to issue certain shares of Common Stock to the Plaintiffs and their respective affiliates in satisfaction
of the Company’s obligation to pay certain previously accrued but unpaid dividends through March 31, 2010 owing to the
Plaintiffs and their respective affiliates.
Series E Amendment Agreement
Pursuant to the Series E Amendment Agreement, the Company agreed to amend the Certificate of Designation of Preferences,
Rights and Limitations of the Series E Convertible Preferred Stock, filed with Secretary of State of the State of Delaware on June 3,
2009 (the “Series E Certificate”). The Epic Parties, constituting all holders of Series E Preferred Stock, consented to the filing of
the Amended Certificate of Designations of the Series E Convertible Preferred Stock (the “Amended Series E Certificate”) with the
Secretary of State of the State of Delaware. On June 29, 2010, pursuant to the authority of its Board of Directors, Company filed
with the Secretary of State of the State of Delaware the Amended Series E Certificate. Pursuant to the terms of the Amended Series
E Certificate, the conversion price of the Series E Preferred Stock will be adjusted downward to reflect, on a pro rata basis, the
reduction in the conversion price of the Series D Preferred Stock as the result of the Series D Amendment Agreement, to the extent
shares of Series D Preferred Stock are converted at the reduced conversion price set forth in the Amended Series D Certificate.
Pursuant to the Series E Amendment Agreement, the Epic SAA was amended so that the purchase of the 750 Additional Shares of
Series E Preferred Stock described therein for an aggregate purchase price of $750,000 would occur in 12 installments of 62.5 shares
(for a purchase price of $62,500) (i) on or prior to November 1, 2009 (which has been satisfied) and (ii) within 10 business days
following the last day of each calendar quarter, beginning with the first calendar quarter ending on September 30, 2010 and
continuing for each of the 10 calendar quarters thereafter.
In addition, under the Series E Amendment Agreement, the third closing date is scheduled to occur on or before December 31,
2010, subject to certain conditions set forth in the Epic SAA (as amended by the Series E Amendment Agreement).
Under each of the Series D Amendment Agreement and the Series E Amendment Agreement, the Company agreed that at its next
meeting of shareholders it will seek shareholder approval to amend its certificate of incorporation to increase the number of
authorized but unissued shares of Common Stock to at least 760,000,000.
Settlement Agreement
Pursuant to the Settlement Agreement, Elite and the Epic Parties, individually and on behalf of each of their respective officers,
directors, agents, representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns (the
“ Elite Releasors”) agreed to release and discharge each of the Plaintiffs, BCMF Trustees LLC, an affiliate of Bushido (“BCMF”),
their respective owners, officers, directors, investors, agents, representatives, successors, affiliated entities, subsidiaries, heirs,
employees, administrators and assigns (the “Plaintiffs’ Releases”) from any and all actions, causes of action, claims, liens, suits,
debts, accounts, liabilities, expenses, attorneys’ fees, agreements, promises, charges, complaints and demands (collectively,
“ Loses”) which the Elite Releasors have or may have against the Plaintiffs’ Releasees that could have been asserted in the Action
or any other court action, based upon any conduct up to and including the date of the Settlement Agreement. Notwithstanding the
foregoing, the Elite Releasors will not release any claim of breach of the terms of the Settlement Agreement, breach of the terms of
the Series D Amendment Agreement, or any cause of action arising from future conduct by the Plaintiffs’ Releases.
F-39
�Pursuant to the Settlement Agreement, the Plaintiffs and BCMF, individually and on behalf of each of their respective owners,
officers, directors, investors, agents, representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators
and assigns (the “Plaintiffs’ Releasors”) agreed to release and discharge Elite and the Epic Parties and each of their respective
officers, directors, agents, representatives, successors, affiliated entities, subsidiaries, heirs, employees, administrators and assigns
(the “Elite Releasees”), from any and all Losses which the Plaintiffs’ Releasors have or may have against the Elite Releasees that
could have been asserted in the Action or any other court action, based upon any conduct up to and including the date of the
Settlement Agreement. Notwithstanding the foregoing, the Plaintiffs’ Releasors did not release any claim of breach of the terms of
the Settlement Agreement, breach of the terms of the Series D Amendment Agreement or any cause of action arising from future
conduct by the Elite Releasees.
In addition, concurrently with the execution of the Settlement Agreement, legal counsel for both the Company and the Plaintiffs
executed a Stipulation of Discontinuance of the Action, which such counsel will file once all conditions precedent to the
effectiveness of the Settlement Agreement have been satisfied.
The foregoing description of the Amended Series D Certificate, Amended Series E Certificate, Settlement Agreement, Series D
Amendment Agreement and Series E Amendment Agreement does not purport to be complete and is qualified in its entirety by
reference to the complete text of such documents which are filed herewith and incorporated herein by reference.
On July 1, 2010, the Company filed with the SEC a Current Report on Form 8-K announcing the settlement of the litigation with
the Plaintiffs, with such filing being incorporated by reference herein.
NOTE 25 SETTLEMENT OF ThePharmaNetwork Inc. v. Elite Pharmaceuticals Inc.
On March 17, 2011, Elite Pharmaceuticals, Inc. (the “Company”) issued a press release announcing the settlement of a lawsuit
filed in the Superior Court of New Jersey, Chancery Division: Bergen County entitled ThePharmaNetwork, LLC v. Elite
Pharmaceuticals, Inc. (Index No. C27210) (the “Action”).
The Action was commenced on or about August 27, 2010 by ThePharmaNetwork, LLC (“TPN”). TPN alleged that the Company
breached certain obligations in connection with a Product Collaboration Agreement (the “Collaboration Agreement”), made as of
November 10, 2006, pursuant to which the Company and TPN agreed to collaborate in the development, commercialization,
manufacturing and distribution of a generic pharmaceutical product, which the parties subsequently agreed would be methadone
hydrochloride in a 10 mg. tablet (the “Product”). In the lawsuit, the Company asserted counterclaims against TPN arising out of
the Collaboration Agreement, and sought damages of no less than $1,125,000 from TPN. Both parties denied the other side’s
allegations.
F-40
�In order to fully and finally resolve the disputed claims arising in the Action, the Company and TPN have entered into a
settlement agreement, dated March 11, 2011 (the “Settlement Agreement”), pursuant to which the Action, including all of TPN’s
claims and the Company’s counterclaims, will be dismissed with prejudice.
Pursuant to the Settlement Agreement, the parties have agreed to terminate the Collaboration Agreement.
In addition, in consideration of the Company’s agreement to terminate the Collaboration Agreement and to relinquish to TPN all
rights and interest in the Abbreviated New Drug Application (“ANDA”) for the Product approved by the U.S. Food and Drug
Administration (FDA), TPN made a cash payment of $500,000 to Elite.
As part of the Settlement Agreement, TPN also acknowledges that the Company may develop a generic product containing
methadone of any strength (including the filing of an abbreviated new drug application relating to such product) and that nothing in
the Settlement Agreement restricts the Company from developing, commercializing, manufacturing and distributing any
pharmaceutical product similar to, or which may compete with, the Product or the ANDA filed in connection with the Product.
The Settlement Agreement also contained a mutual release pursuant to which the Company and TPN agreed to release and
discharge each other and their respective affiliates from all claims arising before the date of the Settlement Agreement.
Please refer to the Current Report on Form 8-K filed with the SEC on March 17, 2011, such filing being herein incorporated by
reference, for further details on this settlement of litigation.
NOTE 26 TRANSACTIONS WITH RELATED PARTIES
Transactions with Epic Pharma LLC and Epic Investments LLC
On March 18, 2009, the Company entered into the Epic Strategic Alliance Agreement with Epic Pharma, LLC and Epic
Investments, LLC, a subsidiary controlled by Epic Pharma LLC, as disclosed in this Annual Report Form 10-K under Item 7 of
Part II of this Annual Report on Form 10K, under the heading “Epic Strategic Alliance Agreement,” Item 9B and Item 10, under
the heading “Directors and Executive Officers,” and in our Current Reports on Form 8K, filed with the SEC on March 23, 2009,
May 6, 2009 and June 5, 2009, which disclosures are incorporated herein by reference. Ashok G. Nigalaye, Jeenarine Narine and
Ram Potti, each were elected as members of our Board of Directors, effective June 24, 2009, as the three directors that Epic is
entitled to designate for appointment to the Board pursuant to the terms of the Epic Strategic Alliance Agreement. Messrs.
Nigalaye, Narine and Potti are also officers of Epic Pharma, LLC, in the following capacities:
∙ Mr. Nigalaye, Chairman and Chief Executive Officer of Epic Pharma, LLC;
∙ Mr. Narine, President and Chief Operating Officer of Epic Pharma, LLC;
∙ Mr. Potti, Vice President of Epic Pharma, LLC.
F-41
�As part of the operation of the strategic alliance, the Company and Epic identified areas of synergy, including, without limitation,
raw materials used by both entities, and various regulatory and operational resources existing at Epic that could be utilized by the
Company.
With regards to synergies related to raw materials usage, the strategic alliance allowed the Company to purchase such raw materials
from Epic, at the Epic acquisition cost, without markup. In all cases, the acquisition cost of Epic was lower than those costs
available to the Company, mainly as a result of efficiencies of scale generated by significantly larger volumes purchased by Epic
during the course of their normal operations. During the fiscal year ended 3/31/2011, an aggregate amount of $232,305 in such
materials was purchased from Epic Pharma LLC. All purchases were at Epic Pharma’s acquisition cost, without markup and
evidenced by supporting documents of Epic Pharma LLC’s acquisition cost.
With regards to synergies related to regulatory and operational resources, the strategic alliance allowed the Company to utilize
Epic’s substantial resources and technical competencies on an “as needed” basis at a cost equal to Epic’s actual cost for only the
resources utilized by the Company. Without such access to Epic’s resources, the Company would have to invest significant
amounts in human resources and fixed assets as well as incur substantial costs with third party providers to provide the same
resources provided by Epic and necessary for the operations of the Company. During the fiscal year ended 3/31/2011, an aggregate
amount of $73,440 was paid to Epic as reimbursement for costs associated with facility maintenance, engineering and regulatory
resources utilized by the Company as well as $140,000 in manufacturing equipment.
The Company also purchased an ANDA for Phentermine 37.5mg tablets from Epic Pharma LLC for a cost of $450,000. Please
refer to Exhibit 10.7 of the Quarterly Report on Form 10-Q filed with SEC on November 15, 2010 for further details on this
ANDA purchase.
Total purchases from Epic by the Company during the fiscal year ended March 31, 2011 were $895,745.
During the fiscal year ended March 31, 2011, the Company also performed method development services for Epic Pharma LLC, for
which it was paid $25,000, sold retired equipment to Epic for $30,000 and sold excess raw materials to Epic for a total of $2,903.
NOTE 27 CONVERSIONS OF PREFERRED STOCK DERIVATIVES TO COMMON STOCK
The Amended Certificate of Designations of the Series D 8% Convertible Preferred Stock of Elite Pharmaceuticals (the “Series D
Preferred Derivatives”), includes provisions entitling the holders of Series D Preferred Derivatives to convert shares of the Series D
Preferred Derivatives into shares of Common Stock. The Series D Preferred Derivatives are classified as a liability to the
Company, and the liability represented by those shares of Series D Preferred Derivatives being converted must be valued at the
time of such conversion, with increases/(decreases) in the value of preferred share derivative liabilities being appropriately recorded
and reflected in the Other Income section of the Company’s Statement of Operations. The amount of equity recorded as a result of
the conversion of Series D Preferred Derivatives is equal to the value of such Series D Preferred Derivatives being converted, at the
time of the conversion, with such amount also representing the decrease in the Preferred Share Derivative Liability on the
Company’s Balance Sheet.
F-42
�Conversions of Series D Preferred Derivatives during the year ended March 31, 2011 are summarized as follows:
# of Series D Preferred Derivative shares converted
4,945
# of Common Shares issued pursuant to conversions of Series D Preferred
Derivatives
70,649,154
Value of Series D Preferred Derivative shares at time of conversion (represents
decrease in derivative liability resulting from conversions)
$
4,465,584
Change in value of preferred share derivative liability recorded at time of conversion
1,639,618
Par value of Common Shares issued
Additional paid in capital recorded as a result of the conversions
70,649
4,394,935
NOTE 28 SUBSEQUENT EVENTS
The Company has evaluated subsequent events from the balance sheet date through June 29, 2011, the date the accompanying
financial statements were issued. The following are material subsequent events:
Common shares issued in lieu of cash in payment of derivative interest expense
Derivative interest expense related to the Preferred Share derivatives due and payable as of March 31, 2011 were paid during April
2011 through the issuance of 7,775,017 shares of common stock.
Conversion of Series D Convertible Preferred Stock to Common Stock
On May 24, 2011 the Company issued a press release announcing that all of the outstanding shares of its Series D 8% Convertible
Preferred Stock (the “Series D”) has been converted into the Company’s common stock, pursuant to the Amended Certificate of
Designations of the Series D 8% Convertible Preferred Stock as filed with the Secretary of State of the State of Delaware on June
29, 2010. The Series D conversion thereby eliminates the Company’s obligations to pay $720,000 in annual dividends and
eliminates the administrative costs associated therewith.
A Current Report on Form 8-K was filed with the SEC on May 24, 2011, such filing being herein incorporated by this reference.
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�Reclassification of Supplement filed with the FDA
On May 31, 2011, the Company received a letter from the US Food and Drug Administration (FDA) responding to a Changes
Being Effected in 30 Days (“CBE 30”) supplement filed by the Company with the agency to change the manufacturing and
packaging location of the Hydromorphone Hydrochloride Tablets USP, 8 mg ANDA purchased from Mikah Pharma. The letter
from the FDA informed the Company that the agency has reclassified the application as a prior approval supplemental application
which will significantly delay the commercialization.
The reclassification of the Company’s application as a prior approval supplemental application is expected to have a material and
detrimental effect on the Company’s future operations as well as its ability to operate in the future.
A Current Report on Form 8-K was filed with the SEC on June 7, 2011, such filing being herein incorporated by this reference.
Manufacturing and Supply Agreement with Mikah Pharma
On June 1, 2011, Elite Pharmaceuticals Inc. (“Elite”) executed a Manufacturing and Supply Agreement (the “Agreement”) with
Mikah Pharma, LLC (“Mikah”) to undertake and perform certain services relating to two generic products: Isradipine Capsules
USP, 2.5 mg and 5 mg and Phendimetrazine Tartrate Tablets USP, 35 mg (the “Products”), including (a) developing and
preparing the documentation required for the transfer of the manufacturing process to Elite’s facility and the appropriate regulatory
filing for the ANDA, and (b) manufacturing finished dosage forms appropriate for commercial sale, marketing and distribution in
the United States of America, its territories, possessions, and commonwealths in accordance with the requirements of this
Agreement; Elite shall perform, at its sole cost and expense, all Technology Transfer, validation and qualification services
(including: equipment, methods and facility qualification), validation and stability services required by Applicable Laws to
commence manufacturing the Products for commercial sale by Mikah or its designees in accordance with the terms of this
Agreement. During the term of this Agreement and subject to the provisions herein, Mikah shall purchase from Elite and Elite
agrees to manufacture and supply solely and exclusively to Mikah, such Product as Mikah may order from time to time pursuant to
this Agreement. Mikah will compensate Elite at an agreed upon transfer price for the manufacturing and packaging of the Products.
For the Isradipine product, Elite will also receive a 10% royalty on net profits of the finished Product. The payment is to be
calculated and paid quarterly. Elite will also receive a onetime milestone payment for each Product for the work associated with the
Technology transfer. The milestone payment shall be made upon the successful manufacturing and testing of the exhibit batch.
The Manufacturing and Supply Agreement has a term of five (5) years and shall automatically renew for additional periods of one
(1) year unless Mikah provides written notice of termination to Elite at least six (6) months prior to the expiration of the Term or
any Renewal Term.
A Current Report on Form 8-K was filed with the SEC on June 7, 2011, such filing being herein incorporated by this reference.
Manufacturing and Supply Agreement with ThePharmaNetwork
On June 29, 2011 the Company announced that it has entered into a commercial Manufacturing and Supply Agreement with
ThePharmaNetwork, LLC, and its wholly owned subsidiary, Ascend Laboratories, LLC (together "TPN"). Under the terms of the
agreement, Elite will perform manufacturing and packaging for TPN’s Methadone Hydrochloride, 10 mg tablets.
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�Elite will be compensated at an agreed upon price for the manufacturing and packaging of the products.
A Current Report on Form 8K was filed with the SEC on June 29, 2011, such filing being herein incorporated by this reference.
Please also refer to exhibit 10.71 to this annual report on Form 10-K.
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