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Alimera SciencesPROGENICS PHARMACEUTICALS INC FORM 10-K (Annual Report) Filed 03/09/17 for the Period Ending 12/31/16 Address Telephone CIK Symbol SIC Code Industry 777 OLD SAW MILL RIVER ROAD TARRYTOWN, NY 10591 9147892800 0000835887 PGNX 2834 - Pharmaceutical Preparations Biotechnology & Medical Research Sector Healthcare Fiscal Year 12/31 http://www.edgar-online.com © Copyright 2017, EDGAR Online, Inc. All Rights Reserved. Distribution and use of this document restricted under EDGAR Online, Inc. Terms of Use. Table of ContentsUNITED STATES SECURITIES AND EXCHANGE COMMISSION WASHINGTON, D.C. 20549 FORM 10-K (Mark One) ☒ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 For the fiscal year ended December 31, 2016 Or☐TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 For the transition period from ___________ to ___________ Commission File No. 000-23143 PROGENICS PHARMACEUTICALS, INC. (Exact name of registrant as specified in its charter) Delaware13-3379479(State or other jurisdiction of incorporation or organization)(I.R.S. Employer Identification Number) One World Trade Center, 47 Floor New York, NY 10007 (Address of principal executive offices, including zip code) Registrant’s telephone number, including area code: (646) 975-2500 Securities registered pursuant to Section 12(b) of the Act:Title of each className of each exchange on which registeredCommon Stock, par value $0.0013 per shareThe NASDAQ Stock Market LLC Securities registered pursuant to Section 12(g) of the Act:NoneIndicate by check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act. Yes ☐ No ☒ Indicate by check mark if the registrant is not required to file reports pursuant to Section 13 or Section 15(d) of the Act. Yes ☐ No ☒ Indicate by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during thepreceding 12 months (or for such shorter period that the registrant was required to file such reports) and (2) has been subject to such filing requirements for the past90 days. Yes ☒ No ☐ Indicate by check mark whether the registrant has submitted electronically and posted on its corporate Website, if any, every Interactive Data File required to besubmitted and posted pursuant to Rule 405 of Regulation S-T (§ 232.405 of this chapter) during the preceding 12 months (or for such shorter period that theregistrant was required to submit and post such files). Yes ☒ No ☐ Indicate by check mark if disclosure of delinquent filers pursuant to Item 405 of Regulation S-K is not contained herein, and will not be contained, to the best ofregistrant’s knowledge, in definitive proxy or information statements incorporated by reference in Part III of this Form 10-K or any amendment to this Form 10-K. ☒ Indicate by check mark whether the registrant is a large accelerated filer, an accelerated filer, a non-accelerated filer or a smaller reporting company. See definitionof “large accelerated filer,” “accelerated filer” and “smaller reporting company” in Rule 12b-2 of the Act: Large accelerated filer ☐Accelerated filer ☒Non-accelerated filer ☐ (Do not check if a smaller reporting company)Smaller reporting company ☐ Indicate by check mark whether the registrant is a shell company (as defined in Rule 12b-2 of the Exchange Act). Yes ☐ No ☒ The aggregate market value of the voting and non-voting stock held by non-affiliates of the registrant on June 30, 2016, based upon the closing price of theCommon Stock on The NASDAQ Stock Market LLC on that date of $4.22 per share, was $147,391,176 .Calculated by excluding all shares that may be deemed to be beneficially owned by executive officers, directors and five percent stockholders of theregistrant, without conceding that any such person is an “affiliate” of the registrant for purposes of the federal securities laws. As of March 6, 2017, a total of 70,190,099 shares of Common Stock, par value $.0013 per share, were outstanding. DOCUMENTS INCORPORATED BY REFERENCESpecified portions of the registrant’s definitive proxy statement to be filed in connection with solicitation of proxies for its 2017 Annual Meeting of Shareholdersth (1) (1)are hereby incorporated by reference into Part III of this Form 10-K where such portions are referenced. Table of Contents TABLE OF CONTENTS Page PART I1 Item 1. Business2 Item 1A. Risk Factors15 Item 1B. Unresolved Staff Comments32 Item 2. Properties32 Item 3. Legal Proceedings32 Item 4. Not Applicable33PART II33 Item 5. Market for Registrant’s Common Equity, Related Stockholder Matters and Issuer Purchases of Equity Securities33 Item 6. Selected Financial Data35 Item 7. Management’s Discussion and Analysis of Financial Condition and Results of Operations (MD&A)36 Item 7A. Quantitative and Qualitative Disclosures About Market Risk42 Item 8. Financial Statements and Supplementary Data42 Item 9. Changes in and Disagreements With Accountants on Accounting and Financial Disclosure42 Item 9A. Controls and Procedures43 Item 9B. Other Information44PART III45 Item 10. Directors, Executive Officers and Corporate Governance45 Item 11. Executive Compensation45 Item 12. Security Ownership of Certain Beneficial Owners and Management and Related Stockholder Matters45 Item 13. Certain Relationships and Related Transactions, and Director Independence45 Item 14. Principal Accounting Fees and Services45PART IV46 Item 15. Exhibits, Financial Statement Schedules46 INDEX TO CONSOLIDATED FINANCIAL STATEMENTSF-1 SIGNATURESS-1 EXHIBIT INDEXE-1 -i- Table of Contents PART I This document and other public statements we make may contain statements that do not relate strictly to historical fact, any of which may be forward-looking statements within the meaning of the U.S. Private Securities Litigation Reform Act of 1995. Statements contained in this communication that refer toProgenics’ estimated or anticipated future results or other non-historical facts are forward-looking statements that reflect Progenics’ current perception of existingtrends and information as of the date of this communication. Forward looking statements generally will be accompanied by words such as “anticipate,” “believe,”“plan,” “could,” “should,” “estimate,” “expect,” “forecast,” “outlook,” “guidance,” “intend,” “may,” “might,” “will,” “possible,” “potential,” “predict,”“project,” or other similar words, phrases or expressions. Such statements are predictions only, and are subject to risks and uncertainties that could cause actualevents or results to differ materially. Forward-looking statements involve known and unknown risks and uncertainties which may cause our actual results,performance or achievements to be materially different from those expressed or implied by forward-looking statements. While it is impossible to identify or predictall such matters, these differences between forward-looking statements and our actual results, performance or achievement may result from, among other things,the inherent uncertainty of the timing and success of, and expense associated with, research, development, regulatory approval and commercialization of ourproducts and product candidates, including the risks that clinical trials will not commence or proceed as planned; products which appear to be promising in earlytrials will not demonstrate efficacy or safety in larger-scale trials; clinical trial data on our products and product candidates will be unfavorable; our products willnot receive marketing approval from regulators or, if approved, do not gain sufficient market acceptance to justify development and commercialization costs; thesales of RELISTOR and other products by our partners and the revenue and income generated for us thereby may not meet expectations; competing productscurrently on the market or in development might reduce the commercial potential of our products; we, our collaborators or others might identify side effects afterthe product is on the market; or efficacy or safety concerns regarding marketed products, whether or not originating from subsequent testing or other activities byus, governmental regulators, other entities or organizations or otherwise, and whether or not scientifically justified, may lead to product recalls, withdrawals ofmarketing approval, reformulation of the product, additional pre-clinical testing or clinical trials, changes in labeling of the product, the need for additionalmarketing applications, declining sales, or other adverse events. We are also subject to risks and uncertainties associated with the actions of our corporate, academic and other collaborators and government regulatoryagencies, including risks from market forces and trends; potential product liability; intellectual property, litigation and other dispute resolution, environmental andother risks; the risk that we may not be able to obtain sufficient capital, recruit and retain employees, enter into favorable collaborations or transactions, or otherrelationships or that existing or future relationships or transactions may not proceed as planned; the risk that current and pending patent protection for ourproducts may be invalid, unenforceable or challenged, or fail to provide adequate market exclusivity, or that our rights to in-licensed intellectual property may beterminated for our failure to satisfy performance milestones; the risk of difficulties in, and regulatory compliance relating to, manufacturing products; and theuncertainty of our future profitability. Risks and uncertainties to which we are subject also include general economic conditions, including interest and currency exchange-rate fluctuations andthe availability of capital; changes in generally accepted accounting principles; the impact of legislation and regulatory compliance; the highly regulated nature ofour business, including government cost-containment initiatives and restrictions on third-party payments for our products; trade buying patterns; the competitiveclimate of our industry; and other factors set forth in this document and other reports filed with the U.S. Securities and Exchange Commission (“SEC”). Inparticular, we cannot assure you that RELISTOR will be commercially successful or be approved in the future in other formulations, indications or jurisdictions,that any of our other programs will result in a commercial product or that we will be able to successfully complete our integration of EXINI Diagnostics AB(“EXINI”) and to develop and commercialize its products. We do not have a policy of updating or revising forward-looking statements and, except as expressly required by law, we disclaim any intent or obligationto update or revise any statements as a result of new information or future events or developments. It should not be assumed that our silence over time means thatactual events are bearing out as expressed or implied in forward-looking statements. Available Information We file annual, quarterly and current reports, proxy statements and other documents with the SEC under the Securities Exchange Act of 1934. The SECmaintains an Internet website that contains reports, proxy and information statements and other information regarding issuers, including Progenics, which fileelectronically with the SEC. You may obtain documents that we file with the SEC at http://www.sec.gov , and read and copy them at the SEC’s Public ReferenceRoom at 100 F Street NE, Washington, DC 20549. You may obtain information on operation of the Public Reference Room by calling the SEC at 1-800-SEC-0330. We also make available free of charge our annual, quarterly and current reports and proxy materials on http://www.progenics.com . 1® Table of Contents Additional information concerning Progenics and its business may be available in press releases or other public announcements and quarterly and currentreports and documents filed with the SEC. Information on or accessed through our website is not included in Progenics’ SEC filings. In this document, RELISTOR , a registered trademark, refers to methylnaltrexone – the active ingredient of RELISTOR – as it has been and is beingdeveloped and commercialized by or in collaboration with Salix Pharmaceuticals, Inc., a subsidiary of Valeant Pharmaceuticals International, Inc. (“Valeant”),under a license agreement (the “RELISTOR License Agreement”). RELISTOR has received regulatory marketing approval for specific indications, and referencesto RELISTOR do not imply that any other form or possible use of the drug has received approval. RELISTOR’s approved U.S. label and full U.S. prescribinginformation is available at www.RELISTOR.com. Other approved labels for RELISTOR apply in ex-U.S. markets. AZEDRA is a trademark of our MolecularInsight Pharmaceuticals, Inc. (“Molecular Insight”) subsidiary. Item 1. Business Overview Progenics Pharmaceuticals, Inc. and its subsidiaries (collectively the “Company,” “Progenics”, “we”, or “us”) develop innovative medicines and othertechnologies to target and treat cancer. Our pipeline includes: (1) therapeutic agents designed to precisely target cancer (AZEDRA and 1095); (2) PSMA-targetedimaging agents for prostate cancer (1404 and PyL ); and (3) imaging analysis tools. Our first commercial product, RELISTOR (methylnaltrexone bromide) foropioid-induced constipation, is partnered with Valeant. Progenics Pharmaceuticals, Inc. was incorporated in the State of Delaware in 1986. Pipeline Our goal is to become a preeminent, patient-centric oncology company and we intend to make a difference in how patients with prostate cancer,pheochromocytoma and paraganglioma are diagnosed and treated. Our pipeline includes the following products and product candidates: Product / Candidate Description StatusUltra-Orphan Theranostic AZEDRA Treatment of malignant and/or recurrent pheochromocytoma andparaganglioma Completed dosing in registrational trial under aSpecial Protocol Assessment agreement with theU.S. Food and Drug Administration ("FDA"); anExpanded Access Program has been initiated Prostate CancerTheranostics 1404 Technetium-99m labeled PSMA targeted SPECT/CT imaging agent forprostate cancer Phase 3 trial in progressPyL Fluorinated PSMA-targeted PET/CT imaging agent for prostate cancer Phase 2/3 trial in progress1095 Iodine-131 labeled PSMA-targeted small molecule therapeutic fortreatment of metastatic prostate cancer Phase 1 trial initiated in first quarter of 2017PSMA TTC (TargetedThorium Conjugate)(antibody licensed to Bayer) Thorium-227 labeled PSMA-targeted antibody therapeutic fortreatment of metastatic prostate cancer Preclinical development in progressProstate cancer bone scanindexing products Software that quantifies the hotspots on bone scans and automaticallycalculates the bone scan index value EXINI bone BSI is currently sold in Europe andJapan; a web-based version is available withoutcharge to researchers in the U.S.; the product has a510(k) clearance form the FDA Opioid-Induced Constipation ("OIC") TreatmentRELISTOR-Subcutaneousinjection(licensed to Valeant) Treatment of OIC in adults with chronic non-cancer pain and treatmentof OIC in advanced-illness adult patients receiving palliative care whenlaxative therapy has not been sufficient Sold in the U.S., European Union, and CanadaRELISTOR-Oral Tablets(licensed to Valeant) Treatment of OIC in adults with chronic non-cancer pain Approved by the FDA on July 19, 2016; U.S.commercialization commenced in third quarter of2016 2® ® TM Table of Contents Our principal clinical-stage product candidates in oncology are: ●AZEDRA is a radiotherapeutic product candidate in development as a treatment for malignant and/or recurrent pheochromocytoma andparaganglioma, rare tumors found in the adrenal glands and outside of the adrenal glands, respectively. AZEDRA has been granted BreakthroughTherapy and Orphan Drug designations, as well as Fast Track status in the U.S. Under a SPA agreement with the FDA, a Phase 2 registrational trialhas been completed in patients with malignant and/or recurrent pheochromocytoma and paraganglioma; there is currently no FDA-approved therapyfor the treatment of these ultra-orphan diseases. ●1404 is a technetium-99m labeled small molecule which binds PSMA and is used as an imaging agent to diagnose and detect localized prostatecancer as well as soft tissue and bone metastases. We have completed a global multi-centered Phase 2 trial assessing the diagnostic accuracy of 1404imaging in men with high-risk prostate cancer and a multi-center, open-label Phase 3 trial is ongoing to determine the sensitivity and specificity of1404 to correctly identify whether or not patients have clinically significant prostate cancer (generally, Gleason score >3+4). ●PyL (also known as [18F]DCFPyL) is a clinical-stage, fluorinated PSMA-targeted Positron Emission Topography (PET) imaging agent for prostatecancer that was discovered and developed at the Center for Translational Molecular Imaging at the Johns Hopkins University School of Medicine. Aproof-of-concept study published in the April 2015 issue of the Journal of Molecular Imaging and Biology showed that the uptake of PyL is high insites of putative metastatic lesions and primary tumors, suggesting the potential for high sensitivity in detecting prostate cancer. A phase 2/3 trialcommenced in December 2016 to assess the diagnostic performance of PyL PET/CT imaging to detect prostate cancer in patients with recurrentand/or metastatic disease. ●1095 is a PSMA-targeted Iodine-131 labeled small molecule that is designed to deliver a dose of beta radiation directly to prostate cancer cells withminimal impact on the surrounding healthy tissues. In collaboration with Memorial Sloan-Kettering Cancer Center, an Investigational New Drug(“IND”) application has been filed in the U.S. and a Phase 1 trial has been initiated. ●PSMA TTC is a thorium-227 labeled PSMA-targeted antibody therapeutic. The PSMA TTC is designed to deliver a dose of alpha radiation directlyto prostate cancer cells with minimal impact on the surrounding healthy tissues. In April 2016, we granted Bayer exclusive worldwide rights todevelop and commercialize products using our PSMA antibody technology in combination with Bayer’s alpha-emitting radionuclides. ●Prostate cancer bone scan indexing products . Exini bone BSI quantifies the hotspots on bone scans of prostate cancer patients and automaticallycalculates the bone scan index value, representing the disease burden of prostate cancer shown on the bone scan. This quantifiable and reproduciblecalculation of the bone scan index value is intended to aid in the diagnosis and treatment of prostate cancer and may have utility in monitoring thecourse of the disease. The prognostic utility of the bone scan index value as a biomarker of prostate cancer is currently being investigated in severalclinical trials. EXINI bone BSI has been sold as standalone software to medical institutions in Europe and as a Japanese version to FUJIFILM RIPharma Co., Ltd. (“Fuji”) in Japan. A web based version of the product has a 510(k) clearance from the FDA and is currently being made availablewithout charge to prostate cancer researchers in the United States as we evaluate its potential. ●RELISTOR is a treatment for opioid induced constipation (“OIC”) that addresses its underlying mechanism of OIC and decreases the constipatingside effects induced by opioid pain medications such as morphine and codeine without diminishing their ability to relieve pain. RELISTOR Tablets(450 mg once daily) were approved in the U.S. for the treatment of OIC in patients with chronic non-cancer pain in July 2016 and launchedcommercially in September 2016. RELISTOR subcutaneous injection is approved and is being sold in the U.S., European Union (“E.U.”) andCanada. Under the RELISTOR License Agreement, Valeant is responsible for developing and commercializing RELISTOR. RELISTOR net sales (losses) and related royalty income (loss) during the years 2014 – 2016 are set forth below. Our recognition of royalty income(loss) for financial reporting purposes is explained in Management’s Discussion and Analysis of Financial Condition and Results of Operations(“MD&A”) and our consolidated financial statements included elsewhere in this document. 3Table of Contents First Second Third Fourth Full Quarter Quarter Quarter Quarter Year (in thousands) 2016 Net sales $16,600 $15,900 $22,100 $16,000 $70,600 Royalty income 2,189 2,380 3,319 2,407 10,295 2015 Net sales $900 $11,900 $8,000 $23,000 $43,800 Royalty income 140 1,773 1,208 3,452 6,573 2014 Net sales (losses) $4,800 $9,100 $10,800 $(4,400) $20,300 Royalty income (loss) 723 1,353 1,617 (657) 3,036 We continue to consider opportunities for strategic collaborations, out-licenses, and other arrangements with biopharmaceutical companies involvingproprietary research, development, clinical and commercialization programs, and may in the future also in-license or acquire additional oncology compoundsand/or programs. Clinical Trial Activities For purposes of this report, in general Phase 1 trials are initial evaluations of safety in humans which study mechanism of action and metabolism; Phase 2trials evaluate safety, dosing and activity or efficacy, and continue safety evaluation; and Phase 3 trials involve larger scale evaluations of safety, efficacy anddosing. Progenics’ practice is and has been to announce commencement and results of all of its significant clinical trials in press releases, medical and scientificmeetings and other venues. The following is a summary of current clinical trial activities involving our principal product candidates and RELISTOR. AZEDRA. In 2006, a Phase 1 trial was commenced with AZEDRA in 11 patients with malignant and/or recurrent pheochromocytoma/paraganglioma andmalignant carcinoid tumors to assess the safety, radiation dosimetry, and distribution metabolism of a single imaging dose of this compound. Following completionof this study, two dose-finding studies were conducted to determine a maximum tolerated therapeutic dose, and to assess safety, dosimetry and preliminary efficacyof AZEDRA in 21 patients with malignant and/or recurrent pheochromocytoma/paraganglioma and 15 with high-risk neuroblastoma, respectively. Subsequently, a Phase 2 trial of AZEDRA was commenced under a Special Protocol Assessment (“SPA”) agreement with the FDA regarding the designof this intended registrational Phase 2 trial to evaluate the efficacy and safety of the administration of two therapeutic doses of the compound in patients withmalignant and/or recurrent pheochromocytoma/paraganglioma. The primary efficacy endpoint of this U.S. study was to determine the clinical benefit of AZEDRAbased on the proportion of study participants with a reduction of all antihypertensive medication by at least 50% for at least six months. Of the 44 patients whoreceived any dose of AZEDRA, including an imaging dose, prior to the trial suspension in late 2010 by Molecular Insight due to lack of funding, 45.5% of patientsreported serious adverse events (“SAEs”), the most common of which were hematologic (11.4%) treatment-related events. Other commonly reported SAEsincluded constipation, dyspnea and myelodysplastic syndrome (each at 4.5%). One case of constipation (2.3%), one case of dyspnea (2.3%) and both cases ofmyelodysplastic syndrome (4.5%) were designated as treatment related. We resumed the Phase 2 trial in December 2014 with the goal of completing the study as specified under the SPA. In July 2015, the FDA designatedAZEDRA as a Breakthrough Therapy for the treatment of patients with iobenguane-avid malignant and/or recurrent pheochromocytoma and paraganglioma. InDecember 2015, we completed enrollment in the Phase 2 registrational trial. A total of 68 patients have been dosed in the study. We expect to report topline data inthe first quarter of 2017. 4Table of Contents 1404. We conducted five Phase 1 trials with 1404 in healthy volunteers as well as men with prostate cancer, to establish proof-of-concept and dosimetry,and to assess a simplified kit preparation as compared to multi-step preparation. We then conducted a Phase 2 trial in the U.S. and Europe to assess the safety andability of 1404 to detect prostate cancer within the prostate gland. Analysis of 1404 SPECT/CT images from this study showed that uptake of 1404 in the lobes ofthe prostate gland correlated significantly with Gleason score (p<0.0001). No deaths, SAEs, or adverse events (“AEs”) leading to discontinuations occurred duringthe study. Of the 105 subjects who received a 1404 injection, 4 subjects reported a total of 10 treatment-emergent adverse events (“TEAEs”) with 1 related to 1404(infusion site extravasation). No discernible trends in hematology, clinical chemistries, vital signs, or physical findings were observed during the study. Based on results from these studies, a multi-center, open-label phase 3 trial was initiated in December 2015 to evaluate the specificity of 1404 to detectclinically insignificant prostate cancer and sensitivity of to detect clinically significant disease in patients with low risk prostate cancer who are eligible or currentlyin active surveillance, but are planning to undergo radical prostatectomy (N=approximately 450 patients). In December 2016, an interim analysis of the ongoingPhase 3 trial was performed. An independent Data Monitoring Committee (“DMC”) completed review of the interim data and recommended that the trial continue.Separately, an agreement with FDA was reached to a modification in the Phase 3 trial’s protocol, allowing patients with very low risk prostate cancer to participatein the trial without having to undergo a radical prostatectomy. In these patients, the specificity and sensitivity of 1404, will be determined by comparison of theresults of the patient’s 1404 scan with the histopathology of tissue obtained from a biopsy of that patient, as opposed to the histopathology of tissue obtained from aradical prostatectomy, as continues to be the case with the other men in the trial. PyL. In July 2015, Progenics and the Johns Hopkins University entered into an exclusive worldwide licensing agreement for PyL, pursuant to which weobtained exclusive, worldwide (excluding Australia and New Zealand) rights to develop and commercialize PyL in PET imaging applications. PyL is a clinical-stage fluorinated PSMA-targeted PET imaging agent for prostate cancer. PyL has shown potential for use in identifying metastatic prostate cancer. Preclinical and clinical studies of PyL have been conducted by investigators in the U.S. and Europe, including the Johns Hopkins University. Preclinical invitro and in vivo studies have demonstrated that PyL binds to PSMA with high affinity and uptake of PyL is specific to prostate tumor tissues. A first-in-humanstudy conducted at the Johns Hopkins University using this tracer in patients with prostate cancer has shown that PET imaging with PyL is feasible and generallywell tolerated, with a dose of radiation typical for diagnostic radiotracers for PET. In that study, physiologic accumulation of PyL corresponded to the distributionof PSMA-expressing organs and excretion. Accumulation in primary tumor and metastatic lesions was very high which may permit the prospective detection ofresidual tumor following definitive local therapy (surgery or radiation) as well as regional or distant metastases with high sensitivity and specificity. In December 2016, we initiated a Phase 2/3 trial to assess the safety and efficacy of PyL in the detection of prostate cancer. In addition to our sponsoredstudies and clinical trial collaborations we anticipate that PyL’s potential activity will also be explored in investigator sponsored studies at various academicinstitutions. 1095. In February 2017, a Phase 1 clinical trial with 1095 had begun at Memorial Sloan-Kettering Cancer Center. This Phase 1 open-label, dose-escalationstudy plans to enroll approximately 30 patients with metastatic castration-resistant prostate cancer (“mCRPC”) who have demonstrated tumor avidity to 1095. Theprimary objectives of this study include determination of maximum tolerated dose, safety and tolerability, biodistribution, and efficacy. Findings from this trial areintended to guide the decision of an optimal dose for a Phase 2 trial. Business Acquisition In November 2015, we concluded a public tender offer (the “Offer”) conducted pursuant to Swedish law to acquire EXINI, which develops advancedimaging analysis tools. As of the end of the offer acceptance period on that date, the Offer had been accepted by shareholders representing a total of 17,794,850shares, corresponding to 96.81% of the total shares in EXINI. We commenced a judicial process in Sweden for acquiring the remaining shares and EXINI wasdelisted and ceased to be publicly traded effective as of the close of trading on December 4, 2015. On December 8, 2016, a Swedish arbitral tribunal awarded usadvanced title to the remaining shares of EXINI and, as of that date, EXINI became a wholly-owned subsidiary with 100% of the voting shares owned by us. 5Table of Contents Royalty Monetization On November 4, 2016, through a new wholly-owned subsidiary MNTX Royalties, we entered into a loan agreement (the “Royalty-Backed Loan”) with afund managed by HealthCare Royalty Partners III, L.P. (“HCRP”) pursuant to which HCRP agreed to make term loans in an aggregate principal amount of up to$100.0 million. We borrowed $50.0 million and can borrow an additional $50.0 million, subject to mutual agreement with HCRP, up to twelve months after theclosing date. MNTX Royalties was required to make up-front payments to HRCP at the funding of the Royalty-Backed Loan, in the amount of (i) a 1% fee and (ii)$500 thousand for the Lender’s expenses. Under the terms of the Royalty-Backed Loan, the lenders have no recourse to us or to any of our assets other than theright to receive royalty payments from the commercial sales of RELISTOR products owed under our agreement with Valeant. The RELISTOR royalty paymentswill be used to repay the principal and interest on the loan. The Royalty-Backed Loan bears interest at a per annum rate of 9.5%. Under the terms of the loan agreement, payments of interest and principal, if any, under the loan will be made on the last day of each calendar quarter outof RELISTOR royalty payments received since the immediately preceding payment date. On each payment date prior to March 31, 2018, RELISTOR royaltypayments received since the immediately preceding payment date will be applied solely to the payment of interest on the loan, with any royalties in excess of theinterest amount retained by us. Beginning on March 31, 2018, 50% of RELISTOR royalty payments received since the immediately preceding payment date inexcess of accrued interest on the loan will be used to repay the principal of the loan, with the balance retained by us. Starting on September 30, 2021, all of theRELISTOR royalties received since the immediately preceding payment date will be used to repay the interest and outstanding principal balance until the balance isfully repaid. The loan has a maturity date of June 30, 2025. Upon the occurrence of certain triggers in the loan agreement, or if HCRP so elects on or after January1, 2018, all of the RELISTOR royalty payments received after the immediately preceding payment date shall be applied to the payment of interest and repaymentof principal until the principal of the loan is fully repaid. In the event of such an election by HCRP, we have the right to repay the loan without any prepaymentpenalty. Research and Development Expenses Research and development is essential to our business. During each of the years ended December 31, 2016, 2015, and 2014, we incurred research anddevelopment costs of $37.6 million, $28.2 million, and $28.6 million, respectively. For additional information relating to our research and development expenses,see Management’s Discussion and Analysis of Financial Condition and Results of Operations – Results of Operations – Research and Development Expenses . 6Table of Contents License and Other Agreements Oncology In January 2013, we acquired Molecular Insight by purchasing all of its outstanding capital stock for 4,452,593 shares of our common stock in a privatetransaction. Under the agreement, we also agreed to pay to the former stockholders potential milestones, in cash or our stock at our option, of up to $23.0 millioncontingent upon achieving specified commercialization events and up to $70.0 million contingent upon achieving specified sales targets relating to the acquiredcompany’s products and the timing of these payments, if any is highly uncertain. In addition to utilizing our own proprietary technology, we have a number ofagreements with owners of intellectual property which we use or believe may be useful in the research, development and commercialization of product candidates,including: •A 2012 co-exclusive license agreement with the University of Zurich and the Paul Scherrer Institute for worldwide sublicensable rights to certainintellectual property related to production methodologies relevant to 1404. Under this agreement, we maintain related patent rights and are obligatedto pay low single-digit royalties on products using the licensed technology, license maintenance fees creditable against royalties, an annual fee for anoption to expand the license’s field of use, and clinical and regulatory milestone payments aggregating approximately $1.1 million. The agreementmay be terminated by the licensors upon certain material defaults by, and automatically terminates upon certain bankruptcy events relating toMolecular Insight, and may be terminated by us on prior written notice. •A 2012 out-license agreement with Fuji for the development and commercialization of 1404 in Japan. Under this agreement, we received upfrontand milestone payments, of $3.0 million and $1.0 million, respectively, and we have the right to receive additional potential future milestone androyalty payments. •A 2000 exclusive license agreement with The University of Western Ontario for worldwide sublicensable rights to certain intellectual propertyrelated to production methodologies relevant to AZEDRA. Under this agreement, we maintain related patent rights and are obligated to pay lowsingle-digit royalties on products using the licensed technology, minimum annual royalties creditable against royalties and clinical and regulatorymilestone payments aggregating approximately $0.3 million. The agreement, which either party may terminate upon certain bankruptcy events ormaterial defaults, continues through the last to expire of the related patent rights. In August 2015, we entered into an exclusive worldwide licensing agreement for PyL with Johns Hopkins University. PyL, when used in conjunction withhigh-resolution PET imaging, has shown potential for use in identifying prostate cancer and sites of distant metastasis. Progenics intends to focus the developmentof PyL with high resolution PET imaging to detect and localize recurrent disease in patients who have experienced a biochemical relapse. Under this agreement, weare obligated to pay milestone payments, low single-digit royalties, patent costs and minimum annual royalties which are creditable against royalties, aggregatingapproximately $2.8 million. In April 2016, we entered into an agreement with a Bayer subsidiary granting Bayer exclusive worldwide rights to develop and commercialize productsusing our PSMA antibody technology in combination with Bayer’s alpha-emitting radionuclides. Under this agreement, we received an upfront payment of $4.0million and two milestone payments totaling $3.0 million and we have the right to receive up to an additional $46.0 million in potential future developmentmilestones and up to $130.0 million in commercialization milestones as well as royalty payments. We have a collaboration agreement with Seattle Genetics, Inc. (“SGI”) under which SGI has granted us an exclusive worldwide license to its proprietaryantibody-drug conjugate technology. We have the right to use this technology, which is based in part on technology licensed by SGI from third parties, to linkchemotherapeutic agents to our monoclonal antibodies that target prostate specific membrane antigen utilizing technology licensed to us, through CytogenCorporation, from Sloan-Kettering Institute for Cancer Research. We are responsible for research, product development, manufacturing and commercialization ofall products, and are obligated to make maintenance and milestone payments and to pay royalties to SGI and its licensors, as applicable, on a percentage of netsales. The SGI agreement terminates at the later of (i) the tenth anniversary of the first commercial sale of each licensed product in each country or (ii) the latestdate of expiration of patents underlying the licensed products. We may terminate the agreement upon advance written notice; SGI may terminate if we fail to cure abreach of an SGI in-license after written notice; and either party may terminate after written notice upon an uncured breach or in the event of the other party’sbankruptcy. 7Table of Contents RELISTOR Under the RELISTOR License Agreement, Valeant is responsible for developing and commercializing RELISTOR worldwide, including completingclinical development necessary to support regulatory marketing approvals for potential new indications and formulations, and marketing and selling theproduct. Valeant is marketing RELISTOR directly through its specialty sales force in the U.S., and outside the U.S. directly through distribution and marketingpartners. Under our Agreement with Valeant, we recognized a development milestone of $40 million upon U.S. marketing approval for subcutaneous RELISTORin non-cancer pain patients in 2014, and a development milestone of $50 million for the U.S. marketing approval of an oral formulation of RELISTOR in July2016. We are also eligible to receive up to $200 million of commercialization milestone payments upon achievement of specified U.S. sales targets, including: ●$10 million based on the first achievement of combined U.S. net sales in excess of $100 million in any single calendar year;●$15 million based on the first achievement of combined U.S. net sales in excess of $150 million in any single calendar year;●$20 million based on the first achievement of combined U.S. net sales in excess of $200 million in any single calendar year;●$30 million based on the first achievement of combined U.S. net sales in excess of $300 million in any single calendar year;●$50 million based on the first achievement of combined U.S. net sales in excess of $750 million in any single calendar year; and●$75 million based on the first achievement of combined U.S. net sales in excess of $1 billion in any single calendar year. Each commercialization milestone payment is payable one time only, regardless of the number of times the condition is satisfied, and all six paymentscould be made within the same calendar year. We are also eligible to receive royalties from Valeant and its affiliates based on the following royalty scale: 15% onworldwide net sales up to $100 million, 17% on the next $400 million in worldwide net sales, and 19% on worldwide net sales over $500 million each calendaryear, and 60% of any upfront, milestone, reimbursement or other revenue (net of costs of goods sold, as defined, and territory-specific research and developmentexpense reimbursement) Valeant receives from sublicensees outside the U.S. The RELISTOR License Agreement may be terminated by either party upon an uncured material breach or specified bankruptcy events. In addition,Valeant may terminate the RELISTOR License Agreement for unresolved safety or efficacy issues or at its discretion upon specified prior notice at any time,subject to our one-time right to postpone such termination for a specified period of time if we have not successfully transitioned the development andcommercialization of the drug despite good faith and diligent efforts. See Risk Factors. We have licensed to Valeant our exclusive rights to develop and commercialize methylnaltrexone, the active ingredient of RELISTOR, which we in-licensed from the University of Chicago (“UC”). Our agreement with UC provides for an exclusive license to intellectual property in exchange for developmentand potential commercialization obligations, low single-digit royalties on commercial sales of resulting products and single-digit percentages of milestone andsublicensing revenues, and shared patent policing responsibilities. The UC agreement, as amended in connection with our RELISTOR collaborations, includingsubstantially all of our payment obligations thereunder, expires by its terms upon the expiration of the last to expire of the patents licensed thereunder, the last-to-expire of which expires in 2017. Valeant has also entered into license and distribution agreements to expand its sales channels outside of the U.S. for RELISTOR. In January 2016, Valeantentered into a distribution agreement with Swedish Orphan Biovitrum AB, also known as Sobi, for RELISTOR in Western Europe, Russia and Greece. In 2016, werecognized license revenue of $720 thousand for our share of the upfront payment Valeant received from Lupin Limited pursuant to a distribution agreement forRELISTOR in Canada. 8Table of Contents Patents and Proprietary Technology Protection of our intellectual property rights is important to our business. We seek U.S. patent protection for many of our inventions, and generally filepatent applications in Canada, Japan, European countries that are party to the European Patent Convention, and other countries on a selective basis in order toprotect inventions we consider to be important to the development of business in those areas. Generally, patents issued in the U.S. are effective for either (i) 20years from the earliest asserted filing date, if the application was filed on or after June 8, 1995, or (ii) the longer of 17 years from the date of issue or 20 years fromthe earliest asserted filing date, if the application was filed prior to that date. In certain instances, the U.S. patent term can be extended up to a maximum of five years to recapture a portion of the term during which FDA regulatoryreview was being conducted. The duration of foreign patents varies in accordance with the provisions of applicable local law, although most countries provide forpatent terms of 20 years from the earliest asserted filing date and allow patent extensions similar to those permitted in the U.S. Patents may not enable us to preclude competitors from commercializing drugs in direct competition with our products, and consequently may not provideus with any meaningful competitive advantage. See Risk Factors. We also rely on trade secrets, proprietary know-how and continuing technological innovation todevelop and maintain a competitive position in our product areas. We require our employees, consultants and corporate partners who have access to our proprietaryinformation to sign confidentiality agreements. Information with respect to our current patent portfolio is set forth below. The original patents surrounding the AZEDRA program were licensed by Molecular Insight from the University of Western Ontario (“UWO”). The patentfamily directed to processes for making polymer precursors, as well as processes for making the final product, expire in 2018 in the U.S. and Canada. Otherlicensed patent families from UWO relate to alternative approaches for preparing AZEDRA, which if implemented, would expire in 2024 worldwide. Progenics haspending applications worldwide directed to manufacturing improvements and the resulting compositions which, if issued, would expire in 2035. Owned and in-licensed properties relating to 1404 have expiration ranges of 2020 to 2029; we view as most significant the composition-of-matter patenton the compound, as well as technetium-99 labeled forms, which expire in 2029 worldwide. Patent applications directed to methods of use are pending worldwide,which if issued would expire in 2034. The PyL patent family was licensed from Johns Hopkins University. Patent protection for the compound, radiolabeled forms of the compound, as well asmethods of use, expire in 2030 in the U.S. Corresponding patent family members are pending or issued worldwide, all expiring in 2029. Company-owned properties relating to 1095 have expiration ranges of 2027 to 2031 in the U.S. We view as most significant the composition-of-matterpatent on this compound, as well as radiolabeled forms, which expires in 2027 in the U.S., as well as Europe. Additional U.S. patents are directed to stablecompositions and radiolabeling processes which expire in 2030 and 2031, respectively. We own properties relating to automated detection of bone cancer metastases through our acquisition of EXINI. The patents on this technology expire in2028. The intellectual property directed to PSMA antibody-drug conjugate comprises co-owned and in-licensed properties. Composition-of-matter patents haveexpirations of 2022 and 2023 in the U.S and a pending U.S. application which would expire in 2026, if issued. A U.S. patent directed to methods of use expires in2031. Corresponding foreign counterparts to the U.S. composition-of-matter patents in Europe and certain other markets will expire 2022 and 2026, along with amethod of use patent which expires in 2029. We view all of these patents as significant. With regard to our RELISTOR-related intellectual property, the composition-of-matter patent for the active ingredient of RELISTOR, methylnaltrexone,was invented in the 1970’s and has expired. The University of Chicago, as well as us and our collaborators, have extended the methylnaltrexone patent estate withadditional patents and pending patent applications covering various inventions relating to the product. Valeant has listed in the FDA Orange Book six U.S. patentsrelating to subcutaneous RELISTOR, which have expiration dates ranging from 2017 to 2030, and six U.S. patents relating to RELISTOR tablet, which haveexpiration dates ranging from 2017 to 2031. Three Canadian patents (expiring in 2024 and 2027) have been listed with Health Canada relating to subcutaneousRELISTOR. 9Table of Contents We are aware of intellectual property rights held by third parties that relate to products or technologies we are developing. For example, we are aware ofothers investigating and developing technologies, imaging agents and drug candidates directed toward PSMA or related compounds as well as in the case ofmethylnaltrexone other peripheral opioid antagonists, and of patents and applications held or filed by others in those areas. The validity of issued patents,patentability of claimed inventions in pending applications and applicability of any of them to our programs are uncertain and subject to change, and patent rightsasserted against us could adversely affect our ability to commercialize or collaborate with others on specific products. Research, development, and commercialization of a biopharmaceutical product often require choosing between alternative development and optimizationroutes at various stages in the development process. Preferred routes depend upon current – and may be affected by subsequent – discoveries and test results andcannot be identified with certainty at the outset. There are numerous third-party patents in fields in which we work, and we may need to obtain license underpatents of others in order to pursue a preferred development route of one or more of our product candidates. The need to obtain a license would decrease theultimate value and profitability of an affected product. If we cannot negotiate such a license, we might have to pursue a less desirable development route orterminate the entire program altogether. Government Regulation We and our product candidates are subject to comprehensive regulation by the FDA and comparable authorities in other countries. Pharmaceuticalregulation currently is a topic of substantial interest in lawmaking and regulatory bodies in the U.S. and internationally, and numerous proposals exist for changesin FDA and non-U.S. regulation of pre-clinical and clinical testing, approval, safety, effectiveness, manufacturing, storage, recordkeeping, labeling, marketing,export, advertising, promotion and other aspects of biologics, small molecule drugs and medical devices, many of which, if adopted, could significantly alter ourbusiness and the current regulatory structure described below. See Risk Factors. FDA Regulation FDA approval, which involves review of scientific, clinical and commercial data, manufacturing processes and facilities, is required before a productcandidate may be marketed in the U.S. This process is costly, time consuming and subject to unanticipated delays, and a drug candidate may fail to progress at anypoint. None of our product candidates other than RELISTOR has received marketing approval from the FDA or any other regulatory authority. The processrequired by the FDA before product candidates may be approved for marketing in the U.S. generally involves: ●pre-clinical laboratory and animal tests; ●submission to and favorable review by the FDA of an investigational new drug application before clinical trials may begin; ●adequate and well-controlled human clinical trials to establish the safety and efficacy of the product for its intended indication (animal and othernonclinical studies also are typically conducted during each phase of human clinical trials); ●submission to the FDA of a marketing application; and ●FDA review of the marketing application in order to determine, among other things, whether the product is safe and effective for its intended uses. Pre-clinical tests include laboratory evaluation of product chemistry and animal studies to gain preliminary information about a compound’spharmacology and toxicology and to identify safety problems that would preclude testing in humans. Since product candidates must generally be manufacturedaccording to current Good Manufacturing Practices (“cGMP”), pre-clinical safety tests must be conducted by laboratories that comply with FDA good laboratorypractices regulations. Pre-clinical testing is preceded by initial research related to specific molecular targets, synthesis of new chemical entities, assay developmentand screening for identification and optimization of lead compound(s). Results of pre-clinical tests are submitted to the FDA as part of an IND which must become effective before clinical trials may commence. The INDsubmission must include, among other things, a description of the sponsor’s investigational plan; protocols for each planned study; chemistry, manufacturing andcontrol information; pharmacology and toxicology information and a summary of previous human experience with the investigational drug. Unless the FDA objectsto, makes comments or raises questions concerning an IND, it becomes effective 30 days following submission, and initial clinical studies may begin. Companiesoften obtain affirmative FDA approval, however, before beginning such studies. 10Table of Contents Clinical trials involve the administration of the investigational new drug to healthy volunteers or to individuals under the supervision of a qualifiedprincipal investigator. Clinical trials must be conducted in accordance with the FDA’s Good Clinical Practice requirements under protocols submitted to the FDAthat detail, among other things, the objectives of the study, parameters used to monitor safety and effectiveness criteria to be evaluated. Each clinical study must beconducted under the auspices of an Institutional Review Board, which considers, among other things, ethical factors, safety of human subjects, possible liability ofthe institution and informed consent disclosure which must be made to participants in the trial. Clinical trials are typically conducted in three sequential phases, which may overlap. During Phase 1, when the drug is initially administered to humansubjects, the product is tested for safety, dosage tolerance, absorption, metabolism, distribution and excretion. Phase 2 involves studies in a limited population toevaluate preliminarily the efficacy of the product for specific, targeted indications, determine dosage tolerance and optimal dosage and identify possible adverseeffects and safety risks. When a product candidate is found in Phase 2 evaluation to have an effect and an acceptable safety profile, Phase 3 trials are undertaken in order to furtherevaluate clinical efficacy and test for safety within an expanded population. Safety studies are conducted in accordance with the FDA’s International Conference onHarmonization Guidelines. Phase 2 results do not guarantee a similar outcome in Phase 3 trials. The FDA may suspend clinical trials at any point in this process ifit concludes that clinical subjects are being exposed to an unacceptable health risk. A New Drug Application (“NDA”) is an application to the FDA to market a new drug. A Biologic License Application (“BLA”) is an application tomarket a biological product. The new drug or biological product may not be marketed in the U.S. until the FDA has approved the NDA or issued a biologic license.The NDA must contain, among other things, information on chemistry, manufacturing and controls; non-clinical pharmacology and toxicology; humanpharmacokinetics and bioavailability; and clinical data. The BLA must contain, among other things, data derived from nonclinical laboratory and clinical studieswhich demonstrate that the product meets prescribed standards of safety, purity and potency, and a full description of manufacturing methods. Supplemental NDAs(“sNDAs”) are submitted to obtain regulatory approval for additional indications for a previously approved drug, and are reviewed by the FDA in a similar manner. The results of the pre-clinical studies and clinical studies, the chemistry and manufacturing data, and the proposed labeling, among other things, aresubmitted to the FDA in the form of an NDA or BLA. The FDA may refuse to accept the application for filing if certain administrative and content criteria are notsatisfied, and even after accepting the application for review, the FDA may require additional testing or information before approval of the application, in eithercase based upon changes in applicable law or FDA policy during the period of product development and FDA regulatory review. The applicant’s analysis of theresults of clinical studies is subject to review and interpretation by the FDA, which may differ from the applicant’s analysis, and in any event, the FDA must denyan NDA or BLA if applicable regulatory requirements are not ultimately satisfied. If regulatory approval of a product is granted, such approval may be madesubject to various conditions, including post-marketing testing and surveillance to monitor the safety of the product, or may entail limitations on the indicated usesfor which it may be marketed. Product approvals may also be withdrawn if compliance with regulatory standards is not maintained or if problems occur followinginitial marketing. Orphan Drug, Fast Track, and Breakthrough Therapy Designations Other FDA regulations and policies relating to drug approval have implications for certain of our current or future product candidates, particularlyAZEDRA. Designation as an Orphan Drug is available under U.S., E.U., and other laws for drug candidates intended to treat rare diseases or conditions, and whichif approved are granted a period of market exclusivity, subject to various conditions. Orphan Drug designation does not shorten or otherwise convey any advantagein the regulatory approval process. Under the Orphan Drug Act, the FDA may designate a product as an Orphan Drug if it is intended to treat a rare disease orcondition, generally defined as a patient population of fewer than 200,000 in the U.S.. AZEDRA is designated as an Orphan Drug. In the U.S., Orphan Drug designation entitles a party to certain financial incentives such as opportunities for grant funding towards clinical trial costs, taxadvantages and user-fee waivers. In addition, if a product receives the first FDA approval for the indication for which it has orphan designation, the product isentitled to Orphan Drug exclusivity, which means the FDA may not approve any other application to market the same drug for the same indication for a period ofseven years, except in limited circumstances, such as a showing of clinical superiority over the product with orphan exclusivity or where the manufacturer is unableto assure sufficient product quantity. 11Table of Contents In cases where the extent and scope of patent protection for a product is limited, the exclusivity period resulting from Orphan Drug designation may beimportant in helping products maintain a competitive position. Even if a product obtains Orphan Drug exclusivity, however, that exclusivity may not effectivelyprotect the product from competition because different drugs with different active moieties may be approved for the same condition. Even after an Orphan Drug isapproved, the FDA may subsequently approve the same drug with the same active moiety for the same condition if the FDA concludes that the later drug is safer,more effective or makes a major contribution to patient care. The FDA is also authorized to designate certain products for expedited review if they are intended to address an unmet medical need in the treatment of aserious or life-threatening disease or condition. These mechanisms for expedited review include fast track designation, breakthrough therapy designation andpriority review designation. AZEDRA has received both fast track and breakthrough therapy designations. The FDA may designate a product for fast track review if it is intended, whether alone or in combination with one or more other drugs, for the treatmentof a serious or life-threatening disease or condition, and it demonstrates the potential to address unmet medical needs for such a disease or condition. For fast trackproducts, sponsors may have greater interactions with the FDA and the FDA may initiate review of sections of a fast track product’s NDA before the application iscomplete. This rolling review may be available if the FDA determines, after preliminary evaluation of clinical data submitted by the sponsor, that a fast trackproduct may be effective. The sponsor must also provide, and the FDA must approve, a schedule for the submission of the remaining information and the sponsormust pay applicable user fees. However, the FDA’s time period goal for reviewing a fast track application does not begin until the last section of the NDA issubmitted. In addition, the fast track designation may be withdrawn by the FDA if the FDA believes that the designation is no longer supported by data emerging inthe clinical trial process. In 2012, as part of the Food and Drug Administration Safety and Improvement Act, a new regulatory scheme was established allowing expedited reviewof products designated as “breakthrough therapies.” A product may be designated as a breakthrough therapy if it is intended, either alone or in combination withone or more other drugs, to treat a serious or life-threatening disease or condition and preliminary clinical evidence indicates that the product may demonstratesubstantial improvement over existing therapies on one or more clinically significant endpoints, such as substantial treatment effects observed early in clinicaldevelopment. The FDA may take certain actions with respect to breakthrough therapies, including holding meetings with the sponsor throughout the developmentprocess; providing timely advice to the product sponsor regarding development and approval; involving more senior staff in the review process; assigning a cross-disciplinary project lead for the review team; and taking other steps to design the clinical trials in an efficient manner. Finally, the FDA may designate a product for priority review if it is a drug that treats a serious condition and, if approved, would provide a significantimprovement in safety or effectiveness. The FDA determines, on a case-by-case basis, whether the proposed drug represents a significant improvement whencompared with other available therapies. Significant improvement may be illustrated by evidence of increased effectiveness in the treatment of a condition,elimination or substantial reduction of a treatment-limiting drug reaction, documented enhancement of patient compliance that may lead to improvement in seriousoutcomes, and evidence of safety and effectiveness in a new subpopulation. A priority designation is intended to direct overall attention and resources to theevaluation of such applications, and to shorten the FDA’s goal for taking action on a marketing application from ten months to six months. Both before and after approval is obtained, a product, its manufacturer and the sponsor of the marketing application for the product are subject tocomprehensive regulatory oversight. Violations of existing or newly-adopted regulatory requirements at any stage, including the pre-clinical and clinical testingprocess, the approval process, or thereafter, may result in various adverse consequences, including FDA delay in approving or refusal to approve a product,withdrawal of an approved product from the market or the imposition of criminal penalties against the manufacturer or sponsor. Later discovery of previouslyunknown problems may result in restrictions on the product, manufacturer or sponsor, including withdrawal of the product from the market. Regulation Outside the U.S. Whether or not FDA approval has been obtained, approval of a pharmaceutical product by comparable government regulatory authorities abroad must beobtained prior to marketing the product there. The approval procedure varies from country to country, and the time required may be longer or shorter than thatrequired for FDA approval. The requirements for regulatory approval by governmental agencies in other countries prior to commercialization of products there canbe rigorous, costly and uncertain, and approvals may not be granted on a timely basis or at all. 12Table of Contents In E.U. countries, Canada, Australia, and Japan, regulatory requirements and approval processes are similar in principle to those in the U.S. Regulatoryapproval in Japan requires that clinical trials of new drugs be conducted in Japanese patients. Depending on the type of drug for which approval is sought, there arecurrently two potential tracks for marketing approval in E.U. countries: mutual recognition and the centralized procedure. These review mechanisms mayultimately lead to approval in all E.U. countries, but each method grants all participating countries some decision-making authority in product approval. Thecentralized procedure, which is mandatory for biotechnology derived products, results in a recommendation in all member states, while the E.U. mutual recognitionprocess involves country-by-country approval. In other countries, regulatory requirements may require additional pre-clinical or clinical testing regardless of whether FDA or European approval hasbeen obtained. This is the case in Japan, where trials are required to involve patient populations which we and our other collaborators have not examined in detail.If a product is manufactured in the U.S., it is also subject to FDA and other U.S. export provisions. In most countries outside the U.S., coverage, pricing andreimbursement approvals are also required, which may affect the profitability of the affected product. Other Regulation In addition to regulations enforced by the FDA, we are also subject to regulation under the U.S. Occupational Safety and Health Act, EnvironmentalProtection Act, Toxic Substances Control Act, Resource Conservation and Recovery Act, and various other current and potential future U.S. federal, state or localregulations. In addition, our research is dependent on maintenance of licenses from various authorities permitting the acquisition, use and storage of quantities ofradioactive isotopes that are critical for its manufacture and testing of research products. Biopharmaceutical research and development generally involves thecontrolled use of hazardous materials, chemicals, viruses, and various radioactive compounds. Even strict compliance with safety procedures for storing, handling,using and disposing of such materials prescribed by applicable regulations cannot completely eliminate the risk of accidental contaminations or injury from thesematerials, which may result in liability for resulting legal and regulatory violations as well as damages. Manufacturing Under the RELISTOR License Agreement, Valeant is responsible for the manufacture and supply, at its expense, of all active pharmaceutical ingredient(“API”) and finished and packaged products for its RELISTOR commercialization efforts, including contracting with contract manufacturing organizations(“CMOs”) for supply of RELISTOR API and subcutaneous and oral finished drug product. As to our other product candidates, the manufacture of biopharmaceuticals and radiopharmaceuticals is relatively complex and requires significant capitalexpenditures. As part of our ongoing efforts to manage our development costs and timely execute on our development plans, we rely on third parties for clinicalmanufacturing. We have engaged third-party CMOs to manufacture API and finished drug products for clinical trial supplies of AZEDRA, and are engaged in theprocess of putting in place sufficient manufacturing capacity to deliver commercial supplies in advance of the anticipated approval of AZEDRA. We have alsopartnered with third-parties to produce clinical trial supplies of 1404, PyL, and 1095, and may in the future undertake such efforts with respect to other assets andprograms. As a result, we depend significantly on the availability of high quality CMO services. If we are unable to arrange for satisfactory CMO services, wewould need to undertake such responsibilities on our own, resulting in our having to incur additional expenses and potentially delaying the development of ourproduct candidates. See Risk Factors . Commercial Organization We plan to commercialize AZEDRA in the U.S. ourselves, if regulatory approval is obtained, and to seek strategic partnerships to commercializeAZEDRA in other countries. We plan to begin building a small commercial organization for our U.S. efforts following receipt of the definitive data from the Phase2b registrational trial for AZEDRA, which is expected by the end of the first quarter of 2017. 13Table of Contents Competition Competition in the biopharmaceutical industry is intense and characterized by ongoing research and development and technological change. We facecompetition from many for-profit companies and major universities and research institutions in the U.S. and abroad. We face competition from companiesmarketing existing products or developing new products for diseases targeted by our technologies. Many of our competitors have substantially greater resources,experience in conducting pre-clinical studies and clinical trials and obtaining regulatory approvals for their products, operating experience, research anddevelopment and marketing capabilities and production capabilities than we do. Our products and product candidates under development may not competesuccessfully with existing products or products under development by other companies, universities and other institutions. Drug manufacturers that are first in themarket with a therapeutic for a specific indication generally obtain and maintain a significant competitive advantage over later entrants and therefore, the speedwith which industry participants move to develop products, complete clinical trials, approve processes and commercialize products is an important competitivefactor. RELISTOR was the first FDA-approved product for any indication involving OIC. We are, however, aware of other approved and marketed products, aswell as candidates in pre-clinical or clinical development, that target the side effects of opioid pain therapy. In September 2014, the FDA approved MOVANTIK (naloxegol), an oral peripheral mu-opioid receptor antagonist for patients with OIC developed by a Nektar Therapeutics-AstraZeneca PLC collaboration, whichalso has a related combination product in early stage development. MOVANTIK was made available to patients in 2015. In December 2014, AstraZeneca wasgranted a Marketing Authorization by the European Commission for MOVENTIG (naloxegol) for the treatment of OIC in adult patients who have had aninadequate response to laxative(s). Cubist Pharmaceuticals, a subsidiary of Merck & Co., Inc., markets ENTEREG (alvimopan) for the treatment of postoperativeileus, and has completed Phase 3 testing of a compound for OIC in chronic-pain patients. Sucampo Pharmaceuticals, Inc., in collaboration with TakedaPharmaceutical Company Limited, markets AMITIZA (lubiprostone), a selective chloride channel activator, for chronic idiopathic (non-opioid related)constipation, and in April 2013 received FDA approval of this drug for opioid-induced constipation. Shionogi & Co. filed an NDA with the FDA for Symproic®,another mu-opioid receptor antagonist, for patients with OIC. The target action date for Symproic under the Prescription Drug User Fee Act (“PDUFA”) is March23, 2017. In December 2016, Shionogi and Purdue Pharma L.P. announced the establishment of an alliance for the joint U.S. launch and commercialization ofSymproic. Theravance, Inc. has completed Phase 2 clinical testing of an oral peripheral mu-opioid antagonist. In Europe, Mundipharma International Limitedmarkets TARGIN (oxycodone/naloxone), a combination of an opioid and a systemic opioid antagonist. Other prescription, as well as over-the-counter (“OTC”),constipation products are also prescribed first line for OIC. As to our oncology pipeline, radiation and surgery are two traditional forms of treatment for prostate cancer. If the disease spreads, hormone (androgen)suppression therapy is often used to slow the cancer’s progression, but this form of treatment can eventually become ineffective. We are aware of severalcompetitors who are developing or have received approval for treatments for castration-resistant prostate cancer, including Johnson & Johnson subsidiary JanssenBiotech, Inc.’s ZYTIGA (abiraterone acetate), approved for use in combination with prednisone as a second-line (after chemotherapy with docetaxel) formetastatic castration-resistant prostate cancer treatment, and later for use with prednisone for metastatic castration-resistant disease before the use of chemotherapy;Medivation, Inc.’s XTANDI (enzalutamide), approved for patients with metastatic castration-resistant prostate cancer previously treated with docetaxel, and laterfor treatment of patients with metastatic castration-resistant prostate cancer before use of chemotherapy; and Bayer HealthCare Pharmaceuticals Inc.’sALPHARADIN (radium-223 dichloride) (marketed as XOFIGO ), approved for treatment of patients with castration-resistant prostate cancer, symptomaticbone metastases and no known visceral metastatic disease. Competitive products to our PSMA-targeted imaging agents include PROSTASCINT , which AytuBioscience Inc. acquired from Jazz Pharmaceuticals in 2015 and which is approved for detection of metastatic prostate cancer or relapsed or high-risk prostatecancer patients; and Blue Earth Diagnostic, Inc.’s Axumin (fluciclovine F 18), approved in 2016 as a diagnostic agent for injection that can be used to detectrecurring prostate cancer. There are currently no approved anticancer treatments in the U.S. for malignant and/or recurrent pheochromocytoma/paraganglioma. A significant amount of research in the biopharmaceutical field is carried out at academic and government institutions. An element of our research anddevelopment strategy has been to in-license technology and product candidates from academic and government institutions. These institutions are sensitive to thecommercial value of their findings and pursue patent protection and negotiate licensing arrangements to collect royalties for use of technology they develop. Theymay also market competitive commercial products on their own or in collaboration with competitors and compete with us in recruiting highly qualified scientificpersonnel, which may result in increased costs or decreased availability of technology or product candidates from these institutions to other industry participants. 14®® ® ® ® ® ® ® ® ® TM Table of Contents Competition with respect to our technologies and products is based on, among other things, product efficacy, safety, reliability, method of administration,availability, price and clinical benefit relative to cost; timing and scope of regulatory approval; sales, marketing and manufacturing capabilities; collaboratorcapabilities; insurance and other reimbursement coverage; and patent protection. Competitive position in our industry also depends on a participant’s ability toattract and retain qualified personnel, obtain patent protection or otherwise develop proprietary products or processes, and secure sufficient capital resources for thetypically substantial period between technological conception and commercial sales. Product Liability The testing, manufacturing and marketing of our product candidates and products involves an inherent risk of product liability attributable to unwantedand potentially serious health effects. To the extent we elect to test, manufacture or market product candidates and products independently, we bear the risk ofproduct liability directly. We maintain product liability insurance coverage in amounts and pursuant to terms and conditions customary for our industry, scale, andthe nature of our activities. Where local statutory requirements exceed the limits of our existing insurance or local policies of insurance are required, we maintainadditional clinical trial liability insurance to meet these requirements. This insurance is subject to deductibles and coverage limitations. The availability and cost ofmaintaining insurance may change over time. Human Resources At December 31, 2016, we had 58 full-time employees, 11 of whom hold Ph.D. degrees and 2 of whom hold M.D. degrees. At that date, 37 employeeswere engaged in research and development, medical, regulatory affairs, and manufacturing related activities and 21 were engaged in finance, legal, administration,sales, and business development. We consider our relations with our employees to be good. None of our employees is covered by a collective bargainingagreement. Item 1A. Risk Factors Product Development-related Risks Drug development is a long and inherently uncertain process with a high risk of failure at every stage of development. Drug development is a highly uncertain scientific and medical endeavor, and failure can unexpectedly occur at any stage of clinical development.Typically, there is a high rate of attrition for product candidates in preclinical and clinical trials due to scientific feasibility, safety, efficacy, changing standards ofmedical care and other variables. The risk of failure increases for our product candidates that are based on new technologies, as well as technologies with which wehave limited prior experience, such as those originally developed by Molecular Insight. Pre-clinical studies and clinical trials are long, expensive and highlyuncertain processes that can take many years. It will take us, or our collaborators, several years to complete clinical trials and the time required for completingtesting and obtaining approvals is uncertain. The start or end of a clinical trial is often delayed or halted due to changing regulatory requirements, manufacturingchallenges, required clinical trial administrative actions, slower than anticipated patient enrollment, changing standards of care, availability or prevalence of use ofa comparator drug or required prior therapy, clinical outcomes, or our and our partners’ financial constraints. The FDA and other U.S. and foreign regulatoryagencies have substantial discretion, at any phase of development, to terminate clinical trials, require additional clinical development or other testing, delay orwithhold registration and marketing approval and mandate product withdrawals, including recalls. Results attained in early human clinical trials may not beindicative of results in later clinical trials. In addition, many of our investigational or experimental drugs are at an early stage of development, and successfulcommercialization of early stage product candidates requires significant research, development, testing and approvals by regulators, and additional investment. Ourproducts in the research or pre-clinical development stage may not yield results that would permit or justify clinical testing. Our failure to demonstrate adequatelythe safety and efficacy of a product under development would delay or prevent marketing approval, which could adversely affect our operating results andcredibility. The failure of one or more of our product candidates could have a material adverse effect on our business, financial condition and results of operations. 15Table of Contents The future of our business and operations depends on the success of our RELISTOR collaborations and our oncology research and development andcommercialization programs. Our business and operations entail a variety of serious risks and uncertainties and are inherently risky. The research and development programs on whichwe focus involve novel approaches to human therapeutics. Our principal product candidates are in clinical development, and in some respects involve technologieswith which we have limited prior experience. We are subject to the risks of failure inherent in the development and commercialization of product candidates basedon new technologies. There is little precedent for the successful commercialization of products based on our technologies, and there are a number of technologicalchallenges that we must overcome to complete most of our development efforts. We may not be able successfully to develop further any of our product candidates.We and our RELISTOR and other collaborators must successfully complete clinical trials and obtain regulatory approvals for potential commercial products. Onceapproved, if at all, commercial product sales are subject to general and industry-specific local and international economic, regulatory, technological and policydevelopments and trends. Delays, higher costs or other weaknesses in manufacturing process capability of our CMOs could hinder the research, development andcommercialization of our product pipeline. The oncology space in which we operate presents numerous significant risks and uncertainties that may be expected toincrease to the extent it becomes more competitive or less favored in the commercial healthcare marketplace. The long-term success of our acquisitions of Molecular Insight and EXINI will be subject to all of the risks and uncertainties described in these riskfactors. In addition, the estimated fair values of Molecular Insight assets and liabilities reflected in our financial statements do not, given their uniqueness andattendant uncertainties, reflect actual transactions or quoted prices and may not correlate to any future values or results. Such information should not be interpretedor relied upon as indicative of any future value or results. Our failure to manage successfully any of our product candidates, technologies or programs could havean adverse impact on our business, and on the price of our stock. If we or our collaborators do not obtain regulatory approval for our product candidates on a timely basis, or at all, or if the terms of any approval imposesignificant restrictions or limitations on use, our business, results of operations and financial condition will be adversely affected. Setbacks in clinicaldevelopment programs could have a material adverse effect on our business. Regulatory approvals are necessary to market product candidates and require demonstration of a product’s safety and efficacy through extensive pre-clinical and clinical trials. We or our collaborators may not obtain regulatory approval for product candidates on a timely basis, or at all, and the terms of anyapproval (which in some countries includes pricing approval) may impose significant restrictions, limitations on use or other commercially unattractive conditions.The process of obtaining FDA and foreign regulatory approvals often takes many years and can vary substantially based upon the type, complexity and novelty ofthe products involved. We have had only limited experience in filing and pursuing applications and other submissions necessary to gain marketing approvals.Products under development may never obtain marketing approval from the FDA or other regulatory authorities necessary for commercialization. We, our collaborators or regulators may also amend, suspend or terminate clinical trials if we or they believe that the participating patients are beingexposed to unacceptable health risks, and after reviewing trial results, we or our collaborators may abandon projects which we previously believed to be promisingfor commercial or other reasons unrelated to patient risks. During this process, we may find, for example, that results of pre-clinical studies are inconclusive or notindicative of results in human clinical trials, clinical investigators or contract research organizations do not comply with protocols or applicable regulatoryrequirements, or that product candidates do not have the desired efficacy or have undesirable side effects or other characteristics that preclude marketing approvalor limit their potential commercial use if approved. In such circumstances, the entire development program for that product candidate could be adversely affected,resulting in delays in trials or regulatory filings for further marketing approval and a possible need to reconfigure our clinical trial programs to conduct additionaltrials or abandon the program involved. Conducting additional clinical trials or making significant revisions to a clinical development plan would lead to delays inregulatory filings. If clinical trials indicate, or regulatory bodies are concerned about, actual or possible serious problems with the safety or efficacy of a productcandidate, such as the concerns expressed during consideration of the oral RELISTOR development program, we or our collaborators may stop or significantlyslow development or commercialization of affected products. As a result of such concerns, the development programs for our product candidates may besignificantly delayed or terminated altogether. If the results of any of our future product candidate trials are not satisfactory or we or our collaborators encounter problems enrolling patients, clinical trialsupply issues, setbacks in developing drug formulations, including raw material-supply, manufacturing, stability or other difficulties, or issues complying withprotocols or applicable regulatory requirements, the entire development program for our product candidates could be adversely affected in a material manner. Suchscenarios could also befall our other clinical-stage product candidates. If any of our collaborators breach or terminate its agreement with us or otherwise fail toconduct successfully and in a timely manner the collaborative activities for which they are responsible, the preclinical or clinical development or commercializationof the affected product candidate or research program could be delayed or terminated. We generally do not control the amount and timing of resources that ourcollaborators devote to our programs or product candidates. We also do not know whether current or future collaboration partners, if any, might pursue alternativetechnologies or develop alternative products either on their own or in collaboration with others, including our competitors, as a means for developing treatments forthe diseases or conditions targeted by our collaborative arrangements. Setbacks of these types could have a material adverse effect on our business, results ofoperations and financial condition. 16Table of Contents We or our collaborators must design and conduct successful clinical trials for our product candidates to obtain regulatory approval. We rely on thirdparties for conduct of clinical trials, which reduces our control over them and may expose us to conflicts of interest. Clinical trial results may beunfavorable or inconclusive, and often take longer than expected. We have limited internal resources with conducting clinical trials, and we rely on or obtain the assistance of others to design, conduct, supervise, ormonitor some or all aspects of some of our clinical trials, including our ongoing Phase 3 trial of 1404, Phase 2/3 trial of PyL, and Phase 1 trial of 1095. We haveless control over the timing and other aspects of clinical trials for which we rely on third parties, such as CROs, clinical data management organizations, medicalinstitutions or clinical investigators, than if we conducted them entirely on our own. These third parties may also have relationships with other entities, some ofwhich may be our competitors. In all events, we are responsible for ensuring that each of our clinical trials is conducted in accordance with the generalinvestigational plan and protocols for the trial. The FDA requires us to comply with good clinical practices for conducting and recording and reporting the results ofclinical trials to assure that data and reported results are credible and accurate and that the rights, integrity and confidentiality of trial participants are protected. Ourreliance on third parties that we do not control does not relieve us of these responsibilities and requirements. To obtain regulatory approval of drug candidates, we must demonstrate through preclinical studies and clinical trials that they are safe and effective.Adverse or inconclusive clinical trial results concerning any of our drug candidates, or trials which regulators find deficient in scope, design or one or more othermaterial respects, could require additional trials, resulting in increased costs, significant delays in submissions of approval applications, approvals in narrowerindications than originally sought, or denials of approval, none of which we can predict. As a result, any projections that we publicly announce of commencementand duration of clinical trials are not certain. We have experienced clinical trial delays in the past as a result of slower than anticipated enrollment and such delaysmay recur. Delays can be caused by, among other things, deaths or other adverse medical events; regulatory or patent issues; interim or final results of ongoingclinical trials; failure to enroll clinical sites as expected; competition for enrollment from other clinical trials; scheduling conflicts with participating clinicians andinstitutions; disagreements, disputes or other matters arising from collaborations; our inability to obtain necessary funding; or manufacturing problems. Under our license agreement, Valeant generally has responsibility for conducting RELISTOR clinical trials, including all trials outside of the U.S. Inaddition, certain clinical trials for our product candidates may be conducted by government-sponsored agencies, and consequently will be dependent ongovernmental participation and funding. These arrangements expose us to the same considerations we face when contracting with third parties for our own trials. Even if our product candidates obtain marketing approval, our ability to generate revenue will be diminished if our products are not accepted in themarketplace, or if we or our collaboration partners select pricing strategies for our products that are less competitive than those of our competitors, orfail to obtain acceptable prices or an adequate level of reimbursement for products from third-party payers or government agencies. The commercial success of our products will depend upon their acceptance by the medical community and third-party payers as clinically useful, costeffective and safe. Market acceptance of approved products, such as RELISTOR for patients with advanced illnesses and for those with chronic, non-cancer pain, isaffected by a wide range of factors, including the timing of regulatory approvals, product launches and the presence of generic, over-the-counter or othercompetitors; the pricing of the product and relative prices of competing products; product development efforts for new indications; the availability ofreimbursement for the product; our ability to obtain sufficient commercial quantities of the product; success in arranging for necessary sublicense or distributionrelationships; and general and industry-specific local and international economic pressures. If health care providers believe that patients can be managed adequatelywith alternative, currently available therapies, they may not prescribe our products, especially if the alternative therapies are viewed as more effective, as having abetter safety or tolerability profile, as being more convenient to the patient or health care providers or as being less expensive. Third-party insurance coverage maynot be available to patients for any products we develop, alone or with collaborators. For pharmaceuticals administered in an institutional setting, the ability of theinstitution to be adequately reimbursed from government and health administration authorities, private health insurers and other third-party payers could also play asignificant role in demand for our products. Significant uncertainty exists as to the reimbursement status of newly-approved pharmaceuticals. Government andother third-party payers increasingly are attempting to contain healthcare costs by limiting both coverage and the level of reimbursement for new drugs and byrefusing, in some cases, to provide coverage for uses of approved products for indications for which the FDA has not granted labeling approval. In most foreignmarkets, pricing and profitability of prescription pharmaceuticals are subject to government control. In the U.S., we expect that there will continue to be a numberof federal and state proposals to implement similar government control and that the emphasis on managed care in the U.S. will continue to put pressure on thepricing of pharmaceutical products. Cost control initiatives could decrease the price that our collaborators receive for any products in the future and adversely affectthe ability of our collaborators to commercialize our products and our realization of royalties from commercialization. If any of our products do not achieve marketacceptance, we will likely lose our entire investment in that product. 17Table of Contents RELISTOR-related Risks We are dependent on Valeant to develop and commercialize RELISTOR, exposing us to significant risks. We rely on Valeant to complete development and obtain regulatory approvals for RELISTOR worldwide. At present, our revenue is almost exclusivelyderived from royalty and milestone payments from our RELISTOR collaboration with Valeant, which can result in significant fluctuation in our revenue fromperiod to period, and our past revenue is therefore not necessarily indicative of our future revenue. We are and will be dependent upon Valeant and any otherbusiness partners with which we may collaborate in the future to perform and fund development, including clinical testing of RELISTOR, making relatedregulatory filings and manufacturing and marketing products, including for new indications and in new formulations, in their respective territories. Revenue fromthe sale of RELISTOR depends entirely upon the efforts of Valeant and its sublicensees, which have significant discretion in determining the efforts and resourcesthey apply to sales of RELISTOR. Valeant may not be effective in obtaining approvals for new indications or formulations, marketing existing or future products orarranging for necessary sublicense or distribution relationships. Our business relationships with Valeant and other partners may not be scientifically, clinically orcommercially successful. For example, Valeant has a variety of marketed products and its own corporate objectives, which may not be consistent with our bestinterests, and may change its strategic focus or pursue alternative technologies in a manner that results in reduced or delayed revenue to us. Valeant may also havecommercial and financial interests that are not fully aligned with ours in a given territory or territories - which may make it more difficult for us to fully realize thevalue of RELISTOR, particularly in markets outside the U.S. We may have future disagreements with Valeant, which has significantly greater financial andmanagerial resources which it could draw upon in the event of a dispute. Such disagreements could lead to lengthy and expensive litigation or other dispute-resolution proceedings as well as extensive financial and operational consequences to us and have a material adverse effect on our business, results of operationsand financial condition. In addition, independent actions may be taken by Valeant concerning product development, marketing strategies, manufacturing and supplyissues, and rights relating to intellectual property. Under our agreements with Valeant relating to RELISTOR, we rely on Valeant to, among other things, effectively commercialize the product and managepricing, sales and marketing practices and inventory levels in the distribution channel. Assessing and reporting on these and other activities and metrics inconnection with RELISTOR has become increasingly difficult as a result of financial reporting and internal control issues that have surfaced both at Valeant and itspredecessor as our RELISTOR licensee, Salix. Our already limited visibility into the internal operations of Valeant and reliance on Valeant to accurately reportinformation concerning the commercialization of RELISTOR has been further obscured by certain recent events at Valeant. On February 22, 2016 Valeantannounced that it believed that approximately $58 million of net revenues previously recognized in the second half of 2014 should not have been recognized duringthat period, and that it expected to delay the filing of its Annual Report on Form 10-K. Both Valeant’s Form 10-K for 2015 and its Form 10-Q for the first quarterof 2016 were filed late, resulting in Valeant receiving notices of default from certain of its noteholders, in each instance. We remain exposed to Valeant’s credit riskand the possibility of default under the RELISTOR License Agreement in the event that Valeant were to terminate the agreement at its discretion or to becomeinsolvent or bankrupt. In the event of a Valeant bankruptcy, Valeant may be able to reject our agreements with it related to RELISTOR such that it would no longerbe obligated to commercialize the product or provide related services, or to assign those agreements without our consent to third parties with an unknown capacityto commercialize and market the product, which could expose us to greater counterparty risk of breaches under such agreements. Valeant further announced that itcontinued to work with its independent advisors in its ongoing assessment of the impact on financial reporting and internal controls of the accounting issues it haddiscovered Valeant commenced remediation efforts with respect to financial reporting and internal controls in the second quarter of 2016, and restated certainpreviously issued financial statements in its report on Form 10-Q for the same quarter. However, there is no assurance as to the adequacy of such efforts in avertingfuture losses incurred in connection with any failures of Valeant’s internal controls. Furthermore, prior to its acquisition by Valeant, Salix disclosed in January of2015, in connection with an internal review of issues related to its management’s prior characterizations of wholesaler inventory levels, that Salix’s previouslyissued audited consolidated financial statements for the year ended December 31, 2013 and the first nine months of 2014, and the disclosures and relatedcommunications for each of those periods, required correction of certain errors and should no longer be relied upon. Valeant continues its efforts to assess andmanage the potential ramifications relating to Salix's restatement of its historical financial results and Valeant’s internal control over financial reporting. 18Table of Contents The RELISTOR commercialization program continues to be subject to risk. Future developments in the commercialization of RELISTOR may result in Valeant or any other business partner with which we may collaborate in thefuture taking independent actions concerning product development, marketing strategies or other matters, including termination of its efforts to develop andcommercialize the drug. Although the FDA approved RELISTOR Tablets for the treatment of opioid-induced constipation in adults with chronic non-cancer pain and Valeantsubsequently announced the U.S. commercial launch of the product on September 6, 2016, there can be no assurances that we and our partners will be able tosuccessfully obtain approval to market oral RELISTOR outside the U.S. or for any other indications. In addition, our and our partners’ ability to optimallycommercialize either oral or subcutaneous RELISTOR in a given jurisdiction may be impacted by applicable labeling and other regulatory requirements. As notedin our risk factors on regulation and regulatory approvals, if clinical trials indicate, or regulatory bodies are concerned about, actual or possible serious problemswith the safety or efficacy of a product candidate, we or our collaborators may stop or significantly slow development or commercialization of affected products.As a result of such concerns, the development and/or commercialization programs for oral RELISTOR and our other products and product candidates may in thefuture be significantly delayed or terminated altogether. In such an event, we could be faced with either further developing and commercializing the drug on ourown or with one or more substitute collaborators, either of which paths would subject us to the development, commercialization, collaboration and/or financingrisks discussed in these risk factors. Any such significant action adverse to development and commercialization of RELISTOR could have a material adverseimpact on our business and on the price of our stock. Certain RELISTOR-related patents are subject to generic challenge. In October 2015 Progenics received notifications of Paragraph IV certifications with respect to certain patents for RELISTOR subcutaneous injection,which are listed in the FDA’s Approved Drug Products with Therapeutic Equivalence Evaluations, or the Orange Book. The certifications accompanied the filingby Actavis Inc. and Mylan Pharmaceuticals, Inc. of Abbreviated New Drug Applications (ANDAs) challenging such patents for RELISTOR subcutaneousinjection. Progenics and its licensee for RELISTOR, Valeant, have timely filed suit and commenced litigation against Actavis and Mylan. FDA approval of theANDA has been automatically stayed until the earlier of (i) 30 months from receipt of the notice or (ii) a District Court decision finding that the identified patentsare invalid, unenforceable or not infringed. In October 2016 Progenics received a notification of a Paragraph IV certification with respect to certain patents for RELISTOR Tablets, which are listedin the FDA's Approved Drug Products with Therapeutic Equivalence Evaluations, or the Orange Book. The certification accompanied the filing by Actavis LLC. ofan ANDA challenging such patents for RELISTOR Tablets. Progenics and its licensee for RELISTOR, Valeant, are assessing the notification and intend tovigorously enforce RELISTOR intellectual property rights. In addition to the above described ANDA notifications, in October 2015 Progenics also received notices of opposition to three European patents (EP1615646, EP 2368554 and EP 2368553) relating to methylnaltrexone. The oppositions were filed separately by each of Actavis Group PTC ehf and Fresenius KabiDeutschland GmbH. Although Progenics and Valeant are cooperating to defend against both the ANDA challenges and the European oppositions, and intend to vigorouslyenforce RELISTOR intellectual property rights, such litigation is inherently subject to significant risks and uncertainties, and there can be no assurance that theoutcome of these litigations will be favorable to Progenics or Valeant. An unfavorable outcome in these cases could result in the rapid genericization of RELISTORproducts, or could result in the shortening of available patent life. Any such outcome could have a material impact on our financial performance and stock price. Pursuant to the RELISTOR license agreement between Progenics and Valeant, Valeant has the first right to enforce the intellectual property rights at issueand is responsible for the costs of such enforcement. At the same time, supporting the conduct of the litigations in the U.S. and in Europe will continue to requiresignificant management focus and internal resources of Progenics. Operational and Regulatory Risks We are subject to extensive regulation, which can be costly and time consuming, may not lead to marketing approval for our product candidates, and cansubject us to unanticipated limitations, restrictions, delays and fines. Our business, products and product candidates are subject to comprehensive regulation by the FDA and comparable authorities in other countries, andinclude the recently enacted Sunshine Act under the Patient Protection and Affordable Care Act. These agencies and other entities regulate the pre-clinical andclinical testing, safety, effectiveness, approval, manufacture, labeling, marketing, export, storage, recordkeeping, advertising, promotion and other aspects of ourproducts and product candidates. We cannot guarantee that approvals of product candidates, processes or facilities will be granted on a timely basis, or at all. If weexperience delays or failures in obtaining approvals, commercialization of our product candidates will be slowed or stopped. 19Table of Contents Even if we obtain regulatory approval for a product candidate, the approval may include significant limitations on indicated uses for which the productcould be marketed or other significant marketing restrictions, such as a REMS. For example, while subcutaneous RELISTOR is approved for OIC both in patientswith advanced illness and for those with chronic, non-cancer pain, the oral formulation of and/or indication for RELISTOR is restricted to adult patients withchronic non-cancer pain. Approvals for product candidates other than RELISTOR, if approved at all, may also be limited or restricted. If we or our collaborators violate regulatory requirements at any stage, whether before or after marketing approval is obtained, we or they may besubject to forced removal of a product from the market, product seizure, civil and criminal penalties and other adverse consequences. Under our license agreement with Valeant, we are dependent on Valeant for compliance with these regulatory requirements as they apply to RELISTOR.Valeant’s subsidiary Salix disclosed that in February 2013 it received a subpoena from the U.S. Attorney’s Office for the Southern District of New York requestingdocuments regarding its sales and promotional practices for RELISTOR and certain of its other products, that it is continuing to respond to the subpoena andintends to cooperate fully with the subpoena and related government investigation, which has and will continue to increase its legal expenses and might requiremanagement time and attention Salix subsequently has become the subject of an SEC investigation and, beginning on November 7, 2014, the target of threeputative class action lawsuits filed by shareholders of Salix. Valeant has indicated that as of the filing of its report on Form 10-K for the year ended December 31,2016, it cannot predict the outcome or the duration of the SEC investigation or any other legal proceedings or any enforcement actions or other remedies that maybe imposed on Salix or Valeant arising out of the SEC investigation. Accordingly, no assurance can be given as to Valeant’s financial condition or results ofoperations, or ability to meet its royalty or milestone obligations to Progenics. Our products may face regulatory, legal or commercial challenges even after approval. Even if a product receives regulatory approval: ●It might not obtain labeling claims necessary to make the product commercially viable (in general, labeling claims define the medical conditions forwhich a drug product may be marketed, and are therefore very important to the commercial success of a product), or may be required to carryBoxed or other warnings that adversely affect its commercial success. ●Approval may be limited to uses of the product for treatment or prevention of diseases or conditions that are relatively less financiallyadvantageous to us than approval of greater or different scope or subject to an FDA-imposed REMS that imposes limits on the distribution or use ofthe product. ●Side effects (including different or aggravated effects such as SAEs encountered in our 1095 program) identified after the product is on the marketmight hurt sales or result in mandatory safety labeling changes, additional pre-clinical testing or clinical trials, imposition of a REMS, productrecalls or withdrawals from the market. ●Efficacy or safety concerns regarding a marketed product, or manufacturing or other problems, may lead to a recall, withdrawal of marketingapproval, reformulation of the product, additional pre-clinical testing or clinical trials, changes in labeling, imposition of a REMS, the need foradditional marketing applications, declining sales or other adverse events. These potential consequences may occur whether or not the concernsoriginate from subsequent testing or other activities by us, governmental regulators, other entities or organizations or otherwise, and whether or notthey are scientifically justified. If products lose previously received marketing and other approvals, our business, results of operations and financialcondition would be materially adversely affected. We or our collaborators will be subject to ongoing FDA obligations and continuous regulatory review, and might be required to undertake post-marketingtrials to verify the product’s efficacy or safety or other regulatory obligations. 20Table of Contents Our and/or our collaborators’ relationships with customers and third-party payers are or may become subject to applicable anti-kickback, fraud andabuse and other healthcare laws and regulations, which could expose us or them to criminal sanctions, civil penalties, program exclusion, contractualdamages, reputational harm and diminished profits and future earnings. Health care providers, physicians and third-party payers play a primary role in the recommendation and prescription of any product candidates for whichwe obtain marketing approval. Our or our collaborators' future arrangements with third-party payers and customers will or already do require us and them tocomply with broadly applicable fraud and abuse and other health care laws and regulations that may constrain the business or financial arrangements andrelationships through which we or our collaborators market, sell and distribute our products that obtain marketing approval. Efforts to ensure that businessarrangements comply with applicable health care laws and regulations involve substantial costs. It is possible that governmental authorities will conclude that ouror our collaborators' business practices may not comply with current or future statutes, regulations or case law involving applicable fraud and abuse or otherhealthcare laws and regulations. If such operations are found to be in violation of any of these laws or other applicable governmental regulations, we or thecollaborator may be subject to significant civil, criminal and administrative penalties, damages, fines, exclusion from government funded healthcare programs, suchas Medicare and Medicaid, and the curtailment or restructuring of related operations. If physicians or other providers or entities involved with our products arefound to be not in compliance with applicable laws, they may be subject to criminal, civil or administrative sanctions, including exclusions from governmentfunded healthcare programs, which may adversely affect us. If we or our collaborators are unable to obtain sufficient quantities of the raw and bulk materials needed to make our product candidates or RELISTOR,development of our product candidates or commercialization of our approved product could be slowed or stopped. Valeant may not be able to fulfill manufacturing obligations for RELISTOR, a key raw material for which grows in Tasmania, either on their own orthrough third-party suppliers. A delay or disruption of supplies of RELISTOR would have a material adverse effect on the RELISTOR franchise, and therefore onour business as a whole. Our existing arrangements with suppliers for our other product candidates may result in the supply of insufficient quantities of our productcandidates needed to accomplish our clinical development programs, and we may not have the right and in any event do not currently have the capability tomanufacture these products if our suppliers are unable or unwilling to do so. We currently arrange for supplies of critical raw materials used in production of ourproduct candidates from single sources. We do not have long-term contracts with any of these suppliers. Any delay or disruption in the availability of raw materialswould slow or stop product development and commercialization of the relevant product. Manufacturing resources could limit or adversely affect our ability to commercialize products. We or our collaborators may engage third parties to manufacture our approved product and product candidates. We or our collaborators may not be able toobtain adequate supplies from third-party manufacturers in a timely fashion for development or commercialization purposes, and commercial quantities of productsmay not be available from contract manufacturers at acceptable costs. Under our license agreement with Valeant, Valeant is responsible for obtaining supplies ofRELISTOR, including contracting with contract manufacturing organizations for supply of RELISTOR active pharmaceutical ingredient and subcutaneous and oralfinished drug product. These arrangements may not be on terms that are advantageous and, as a result of our royalty and other interests in RELISTOR’scommercial success, will subject us to risks that the counterparties may not perform optimally in terms of quality or reliability. In engaging third parties for theseactivities, we do not control many aspects of the manufacturing process, including compliance with current cGMP and other regulatory requirements. In order tocommercialize our product candidates successfully, we or our collaborators need to be able to manufacture or arrange for the manufacture of products incommercial quantities, in compliance with regulatory requirements, at acceptable costs and in a timely manner. Manufacture of our product candidates can becomplex, difficult to accomplish even in small quantities, difficult to scale-up for large-scale production and subject to delays, inefficiencies and low yields ofquality products. The cost of manufacturing some of our product candidates may make them prohibitively expensive. If adequate supplies of any of our productcandidates or related materials are not available on a timely basis or at all, our clinical trials could be seriously delayed, since these materials are time consuming tomanufacture and cannot be readily obtained from third-party sources. We continue to be dependent on a limited number of highly specialized manufacturing anddevelopment partners, including single source manufacturers for certain of our product candidates. If we were to lose one or more of these key relationships, itcould materially adversely affect our business. Establishing new manufacturing relationships, or creating our own manufacturing capability, would requiresignificant time, capital and management effort, and the transfer of product-related technology and know-how from one manufacturer to another is an inherentlycomplex and uncertain process. 21Table of Contents Failure of any manufacturer of RELISTOR or our various product candidates to comply with applicable regulatory requirements could subject us topenalties and have a material adverse effect on supplies of our product or products candidates. Third-party manufacturers are required to comply with cGMP or similar regulatory requirements outside of the U.S. If manufacturers of our product orproduct candidates cannot successfully manufacture material that conforms to the strict regulatory requirements of the FDA and any applicable foreign regulatoryauthority, they may not be able to supply us with our product or product candidates. If these facilities are not approved for commercial manufacture, we may needto find alternative manufacturing facilities, which could result in delays of several years in obtaining approval for a product candidate. We do not control themanufacturing operations and are completely dependent on our third-party manufacturing partners or contractors for compliance with the applicable regulatoryrequirements for the manufacture of RELISTOR and our product candidates. Manufacturers are subject to ongoing periodic unannounced inspections by the FDAand corresponding state and foreign agencies for compliance with cGMP and similar regulatory requirements. Failure of any manufacturer of RELISTOR or any ofour product candidates to comply with applicable cGMP or other regulatory requirements could result in sanctions being imposed on our collaborators or us,including fines, injunctions, civil penalties, delays, suspensions or withdrawals of approvals, operating restrictions, interruptions in supply and criminalprosecutions, any of which could significantly and adversely affect supplies of RELISTOR or such product candidate and have a material adverse impact on ourbusiness, financial condition and results of operations. The validity, enforceability and commercial value of our patents and other intellectual property rights are highly uncertain. We own or have direct or sub-licenses to a number of issued patents. We must obtain, maintain and enforce patent and other rights to protect ourintellectual property. The patent position of biotechnology and pharmaceutical firms is highly uncertain and involves many complex legal and technical issues.There are many laws, regulations and judicial decisions that dictate and otherwise influence the manner in which patent applications are filed and prosecuted and inwhich patents are granted and enforced, all of which are subject to change from time to time. There is no clear policy involving the breadth of claims allowed, orthe degree of protection afforded, under patents in this area. In addition, we are aware of others who have patent applications or patents containing claims similar toor overlapping those in our patents and patent applications. Accordingly, patent applications owned by or licensed to us may not result in patents being issued.Even if we own or license a relevant issued patent, we may not be able to preclude competitors from commercializing drugs that may compete directly with one ormore of our products or product candidates, in which event such rights may not provide us with any meaningful competitive advantage. In the absence or uponsuccessful challenge of patent protection, drugs may be subject to generic competition, which could adversely affect pricing and sales volumes of the affectedproducts. It is generally difficult to determine the relative strength or scope of a biotechnology or pharmaceutical patent position in absolute terms at any given time.The issuance of a patent is not conclusive as to its validity or enforceability, which can be challenged in litigation or via administrative proceedings. The licenseagreements from which we derive or out-license intellectual property provide for various royalty, milestone and other payment, commercialization, sublicensing,patent prosecution and enforcement, insurance, indemnification and other obligations and rights, and are subject to certain reservations of rights. While wegenerally have the right to defend and enforce patents licensed to or by us, either in the first instance or if the licensor or licensee chooses not to do so, we mustusually bear the cost of doing so. Under our license agreement with Valeant, Valeant generally has the first right to control the defense and enforcement of ourRELISTOR patents. We may incur substantial costs in seeking to uphold the validity of patents or to prevent infringement. If the outcome of a dispute or contest isadverse to us, third parties may be able to use our patented invention without payment to us. Third parties may also avoid our patents through design innovation. Patents have a limited life and expire by law. In addition to uncertainties as to scope, validity, enforceability and changes in law, patents by law have limited lives. Upon expiration of patent protection,our drug candidates and/or products may be subject to generic competition, which could adversely affect pricing and sales volumes of the affected products. The original patents surrounding the AZEDRA program were licensed by Molecular Insight from the University of Western Ontario (“UWO”). The patentfamily directed to processes for making polymer precursors, as well as processes for making the final product expire in 2018 in the U.S. and Canada. Other licensedpatent families from UWO relate to alternative approaches for preparing AZEDRA, which if implemented would expire in 2024, worldwide. Progenics has pendingapplications worldwide directed to manufacturing improvements and the resulting compositions which, if issued, would expire in 2035. Owned and in-licensed properties relating to the 1404 product candidate have expiration ranges of 2020 to 2029; we view as most significant thecomposition-of-matter patent on the compound, as well as technetium-99 labeled forms, which expires in 2029 worldwide. Patent applications directed to methodsof use are pending worldwide, which if issued would expire in 2034. 22Table of Contents Patent protection for the PyL compound, radiolabeled form of the compound, as well as methods of use expire in 2030 in the United States. Correspondingpatent family members are pending or issued worldwide, all with expirations of 2029. Company-owned properties relating to MIP-1095 have expiration ranges of 2027 to 2031 in the U.S. We view as most significant the composition-of-matter patent on this compound, as well as radiolabeled forms, which expires in 2027 in the U.S., as well as Europe. Additional U.S. patents are directed to stablecompositions and radiolabeling processes which expire in 2030 and 2031, respectively. We own properties relating to automated detection of bone cancer metastases through our acquisition of EXINI. The patents on this technology expire in2028. With respect to PSMA antibody-drug conjugate, currently issued composition-of-matter patents comprising co-owned and in-licensed properties haveexpiration ranges of 2022 to 2023 in the U.S. and a pending U.S. application which would expire in 2026, if issued. A U.S. patent directed to methods of useexpires in 2031. Corresponding foreign counterparts to the U.S. composition-of-matter patents will expire 2022 and 2026, along with a method of use patent whichexpires in 2029. We view all of these patents as significant. With regard to our RELISTOR-related intellectual property, the composition-of-matter patent for the active ingredient of RELISTOR, methylnaltrexone,was invented in the 1970’s and has expired. The University, as well as Progenics and its collaborators, have extended the methylnaltrexone patent estate withadditional patents and pending patent applications covering various inventions relating to the product. Valeant has listed in the FDA Orange Book six U.S. patentsrelating to subcutaneous RELISTOR, which have expiration dates ranging from 2017 to 2030. Six Orange Book listed U.S. patents relating to Relistor tablets, haveexpiration dates ranging from 2017 to 2031. Three Canadian patents (expiring 2024 and 2027) have been listed with Health Canada relating to subcutaneousRelistor..We depend on intellectual property licensed from third parties and unpatented technology, trade secrets and confidential information. If we lose any ofthese rights, including by failing to achi eve milestone requirements or to satisfy other conditions, or if they or data embodying or relevant to them arecompromised by disruptions or breaches of information or data security, our business, results of operations and financial condition could be harmed. Most of our product candidates, including RELISTOR, incorporate intellectual property licensed from third parties. For example, PyL utilizes technologylicensed to us from Johns Hopkins University. We could lose the right to patents and other intellectual property licensed to us if the related license agreement isterminated due to a breach by us or otherwise. Our ability, and that of our collaboration partners, to commercialize products incorporating licensed intellectualproperty would be impaired if the related license agreements were terminated. In addition, we are required to make substantial cash payments, achieve milestonesand satisfy other conditions, including filing for and obtaining marketing approvals and introducing products, to maintain rights under our intellectual propertylicenses. Due to the nature of these agreements and the uncertainties of research and development, we may not be able to achieve milestones or satisfy conditions towhich we have contractually committed, and as a result may be unable to maintain our rights under these licenses. If we do not comply with our licenseagreements, the licensors may terminate them, which could result in our losing our rights to, and therefore being unable to commercialize, related products. We also rely on unpatented technology, trade secrets and confidential information. Third parties may independently develop substantially equivalentinformation and techniques or otherwise gain access to our technology or disclose our technology, and we may be unable to effectively protect our rights inunpatented technology, trade secrets and confidential information. We require each of our employees, consultants and advisors to execute a confidentialityagreement at the commencement of an employment or consulting relationship with us. These agreements may, however, not provide effective protection in theevent of unauthorized use or disclosure of confidential information. Any loss of trade secret protection or other unpatented technology rights could harm ourbusiness, results of operations and financial condition. Progenics and other businesses and organizations worldwide, and in particular technology-intensive activities such as biotechnology research anddevelopment, are increasingly dependent on critical, complex and interdependent information technology systems, including Internet-based systems, to facilitate orperform basic research and development functions, business processes, internal and external communications, and other critical functions. Progenics relies on suchsystems for most aspects of its business. The size and complexity of computer, communications and other electronic networked data generation, storage andtransfer systems make them potentially vulnerable to breakdown, malicious intrusion, computer viruses and data security breaches by unauthorized third parties,employees or others. Such events may permit unauthorized persons to access, misappropriate and/or destroy sensitive data and result in the impairment ordisruption of important business processes, loss of trade secrets or other proprietary intellectual property or public exposure of personal information (includingsensitive personal information) of employees, business partners, clinical trial patients, customers and others. Any of the foregoing could have a material adverseeffect on our business, prospects, operating results and financial condition. 23Table of Contents If we do not achieve milestones or satisfy conditions regarding some of our product candidates, we may not maintain our rights under related licenses. We are required to make substantial cash payments, achieve milestones and satisfy other conditions, including filing for and obtaining marketingapprovals and introducing products, to maintain rights under certain intellectual property licenses. Due to the nature of these agreements and the uncertainties ofresearch and development, we may not be able to achieve milestones or satisfy conditions to which we have contractually committed, and as a result may be unableto maintain our rights under these licenses. If we do not comply with our license agreements, the licensors may terminate them, which could result in our losing ourrights to, and therefore being unable to commercialize, related products. If we infringe third-party patent or other intellectual property rights, we may need to alter or terminate a product development program. There may be patent or other intellectual property rights belonging to others that require us to alter our products, pay licensing fees or cease certainactivities. If our products infringe patent or other intellectual property rights of others, the owners of those rights could bring legal actions against us claimingdamages and seeking to enjoin manufacturing and marketing of the affected products. If these legal actions are successful, in addition to any potential liability fordamages, we could be required to obtain a license in order to continue to manufacture or market the affected products. We may not prevail in any action broughtagainst us, and any license required under any rights that we infringe may not be available on acceptable terms or at all. We are aware of intellectual property rightsheld by third parties that relate to products or technologies we are developing. For example, we are aware of other groups investigating PSMA or relatedcompounds and monoclonal antibodies directed at PSMA, and methylnaltrexone and other peripheral opioid antagonists, and of patents held, and patentapplications filed, by these groups in those areas. While the validity of these issued patents, the patentability of these pending patent applications and theapplicability of any of them to our products and programs are uncertain, if asserted against us, any related patent or other intellectual property rights couldadversely affect our ability to commercialize our products. Research, development and commercialization of a biopharmaceutical product often require choosing between alternative development and optimizationroutes at various stages in the development process. Preferred routes may depend on subsequent discoveries and test results and cannot be predicted with certaintyat the outset. There are numerous third-party patents in our field, and we may need to obtain a license under a patent in order to pursue the preferred developmentroute of one or more of our products or product candidates. The need to obtain a license would decrease the ultimate profitability of the applicable product. If wecannot negotiate a license, we might have to pursue a less desirable development route or terminate the program altogether. We are dependent upon third parties for a variety of functions. These arrangements may not provide us with the benefits we expect. We rely on third parties to perform a variety of functions. We are party to numerous agreements which place substantial responsibility on clinical researchorganizations, consultants and other service providers for the development of our approved product and our product candidates. We also rely on medical andacademic institutions to perform aspects of our clinical trials of product candidates. In addition, an element of our research and development strategy has been to in-license technology and product candidates from academic and government institutions in order to minimize investments in early research. We have entered intoagreements under which we are now dependent on Valeant for the commercialization and development of RELISTOR. We may not be able to maintain our existingrelationships, or establish new ones for RELISTOR or other product candidates on beneficial terms. We may not be able to enter new arrangements without unduedelays or expenditures, and these arrangements may not allow us to compete successfully. Moreover, if third parties do not successfully carry out their contractualduties, meet expected deadlines or conduct clinical trials in accordance with regulatory requirements or applicable protocols, our product candidates may not beapproved for marketing and commercialization or such approval may be delayed. If that occurs, we or our collaborators will not be able, or may be delayed in ourefforts, to commercialize our product candidates. 24Table of Contents If we are unable to negotiate suitable collaboration agreements, our cash burn rate could increase and our rate of product development could decrease. Our ability to generate revenue in the near term depends on the timing of achievement, if any, of certain payment triggering events under our existingcollaboration agreements and our ability to enter into additional collaboration agreements with third parties. We may not be successful in negotiating additionalcollaboration arrangements with pharmaceutical and biotechnology companies to develop and commercialize product candidates and technologies. If we do notenter into new collaboration arrangements, we would have to devote more of our resources to clinical product development and product launch activities and toseeking additional sources of capital to fund those activities. If we were not successful in seeking such capital, our cash burn rate would increase or we would needto take steps to reduce our rate of product development. Our ability to enter into new collaborations may be dependent on many factors, such as the results ofclinical trials, competitive factors and the fit of our programs with the risk tolerance of a potential collaborator, including in relation to regulatory issues, the patentportfolio, the clinical pipeline, the stage of the available data, overall corporate goals, and financial position. If we are not able to generate revenue under ourcollaborations when and in accordance with our expectations or the expectations of industry analysts, this failure could harm our business and have an immediateadverse effect on the trading price of our common stock. We lack sales and marketing infrastructure and related staff, which will require significant investment to establish and in the meantime may make usdependent on third parties for their expertise in this area. We have no established sales, marketing or distribution infrastructure. If we receive marketing approval for a pharmaceutical product, significantinvestment, time and managerial resources would be required to build the commercial infrastructure required to market, sell and support it without a third-partypartner. Should we choose to commercialize a product directly, we may not be successful in developing an effective commercial infrastructure or in achievingsufficient market acceptance. Alternatively, we may choose to market and sell products through distribution, co-marketing, co-promotion or licensing arrangementswith third parties. We may also consider contracting with a third-party professional pharmaceutical detailing and sales organization to perform the marketingfunction for one or more products. To the extent that we enter into distribution, co-marketing, co-promotion, detailing or licensing arrangements for the marketingand sale of product candidates, any revenues we receive will depend primarily on the efforts of third parties. We will not control the amount and timing ofmarketing resources these third parties devote to our products. We are involved in various legal proceedings that are uncertain, costly and time-consuming and could have a material adverse impact on our business,financial condition and results of operations and could cause the market value of our common stock to decline . From time to time we are involved in legal proceedings and disputes and may be involved in litigation in the future. These proceedings are complex andextended and occupy the resources of our management and employees. These proceedings are also costly to prosecute and defend and may involve substantialawards or damages payable by us if not found in our favor. We may also be required to pay substantial amounts or grant certain rights on unfavorable terms inorder to settle such proceedings. Defending against or settling such claims and any unfavorable legal decisions, settlements or orders could have a material adverseeffect on our business, financial condition and results of operations and could cause the market value of our common stock to decline. For more informationregarding legal proceedings, see Item 3 and Note 10 in the notes to the consolidated financial statements in Item 15 of this Form 10-K. In particular, the pharmaceutical and medical device industries historically have generated substantial litigation concerning the manufacture, use and saleof products and we expect this litigation activity to continue. As a result, we expect that patents related to our products will be routinely challenged, and our patentsmay not be upheld. In order to protect or enforce patent rights, we may initiate litigation against third parties. If we are not successful in defending an attack on ourpatents and maintaining exclusive rights to market one or more of our products still under patent protection, we could lose a significant portion of sales in a veryshort period. We may also become subject to infringement claims by third parties and may have to defend against charges that we violated patents or theproprietary rights of third parties. If we infringe the intellectual property rights of others, we could lose our right to develop, manufacture or sell products, or couldbe required to pay monetary damages or royalties to license proprietary rights from third parties. In addition, in the U.S., it has become increasingly common for patent infringement actions to prompt claims that antitrust laws have been violated duringthe prosecution of the patent or during litigation involving the defense of that patent. Such claims by direct and indirect purchasers and other payers are typicallyfiled as class actions. The relief sought may include treble damages and restitution claims. Similarly, antitrust claims may be brought by government entities orprivate parties following settlement of patent litigation, alleging that such settlements are anti-competitive and in violation of antitrust laws. In the U.S. and Europe,regulatory authorities have continued to challenge as anti-competitive so-called “reverse payment” settlements between branded and generic drug manufacturers.We may also be subject to other antitrust litigation involving competition claims unrelated to patent infringement and prosecution. A successful antitrust claim by aprivate party or government entity against us could have a material adverse effect on our business, financial condition and results of operations and could cause themarket value of our common stock to decline. 25Table of Contents We are exposed to product liability claims, and in the future may not be able to obtain insurance against claims at a reasonable cost or at all. Our business exposes us to product liability risks, which are inherent in the testing, manufacturing, marketing and sale of pharmaceutical products. Wemay not be able to avoid product liability exposure. If a product liability claim is successfully brought against us, our financial position may be adversely affected.Under our license agreement with Valeant, we are responsible for product liability claims arising out of clinical trials that were conducted under our supervision.We are indemnified by Valeant under our license agreement with Valeant for product liability exposure arising from its supply, marketing and sales of RELISTOR,and maintain our own product liability insurance coverage in amounts and pursuant to terms and conditions customary for our industry, scale and the nature of ouractivities (subject to a deductible and an annual aggregate limitation), and other clinical trial or other insurance as required by contract and local laws. In October2009, we released our former collaborator, Wyeth Pharmaceuticals, from its indemnification responsibility for product liability exposure arising from its marketingand sales of RELISTOR. Product liability insurance for the biopharmaceutical industry is generally expensive, when available at all, and may not be available to usat a reasonable cost in the future. Our current insurance coverage and indemnification arrangements may not be adequate to cover claims brought against us, andare in any event subject to the insuring or indemnifying entity discharging its obligations to us. We and our CMOs handle hazardous materials and must comply with environmental laws and regulations, which can be expensive and restrict how we orour CMOs do business. If we or our CMOs are involved in a hazardous waste spill or other accident, we or our CMOs could be liable for damages,penalties or other forms of censure. Research and development work and manufacturing processes with our pipeline products involve the use of hazardous, controlled and/or radioactivematerials. We and our CMOs are subject to federal, state and local laws and regulations governing the use, manufacture, storage, handling and disposal of thesematerials. Despite procedures that we and our CMOs implement for handling and disposing of these materials, the risk of accidental contamination or injury cannotbe eliminated. In the event of a hazardous waste spill or other accident, we or our CMOs could be liable for damages, penalties or other forms of censure. Theremay be significant costs to comply with applicable environmental laws and regulations in the future, and such costs may be incurred by us directly or passedthrough to us by our CMOs. In the event of the damages, penalties, censures or higher costs outlined above, the efficiency and cost of our research, developmentand commercialization pipeline may be adversely impacted. If we lose key management and scientific personnel on whom we depend, our business could suffer. We are dependent upon our key management and scientific personnel, the loss of whom could require us to identify and engage qualified replacements,and could cause our management and operations to suffer in the interim. Competition for qualified employees among companies in the biopharmaceutical industryis intense. Future success in our industry depends in significant part on the ability to attract, retain and motivate highly skilled employees, which we may not besuccessful in doing. Health care reform measures could adversely affect our operating results and our ability to obtain marketing approval of and to commercialize ourproduct candidates. In the U.S. and some foreign jurisdictions, there have been a number of legislative and regulatory changes and proposed changes regarding the health caresystem that could prevent or delay marketing approval of our product candidates, restrict or regulate post-approval activities and affect our ability to profitably sellany product candidates for which we obtain marketing approval. Legislative and regulatory proposals have been made to expand post-approval requirements andrestrict sales and promotional activities for pharmaceutical products. In addition, increased scrutiny by the U.S. Congress of the FDA’s approval process maysignificantly delay or prevent marketing approval, as well as subject us to more stringent product labeling and post-marketing testing and other requirements. In theU.S., federal legislation has changed the way Medicare covers and pays for pharmaceutical products. Cost reduction initiatives and other provisions of legislationhave decreased coverage and reimbursement. Though such legislation applies only to drug benefits for Medicare beneficiaries, private payers often followMedicare coverage policy and payment limitations in setting their own reimbursement rates. More recent legislation is intended to broaden access to healthinsurance, further reduce or constrain the growth of healthcare spending, enhance remedies against fraud and abuse, add new transparency requirements for healthcare and health insurance industries, and impose new taxes and fees on the health industry and additional health policy reforms. New laws impose significantannual fees on companies that manufacture or import branded prescription drug products, and contain substantial new compliance provisions, which in each casemay affect our business practices with health care practitioners. Subject to federal and state agencies issuing regulations or guidance, it appears likely that new lawswill continue to pressure pharmaceutical pricing, especially under the Medicare program, and may also increase regulatory burdens and operating costs. We cannotbe sure whether additional legislative changes will be enacted, whether the FDA regulations, guidance or interpretations will be changed or what the impact of suchchanges on the marketing approvals of our product candidates, if any, may be. 26Table of Contents Our and/or our collaborators’ relationships with customers and third-party payers will be subject to applicable anti-kickback, fraud and abuse and otherhealthcare laws and regulations, which could expose us or them to criminal sanctions, civil penalties, program exclusion, contractual damages,reputational harm and diminished profits and future earnings. Health care providers, physicians and third-party payers play a primary role in the recommendation and prescription of any product candidates for whichwe obtain marketing approval. Our or our collaborators’ future arrangements with third-party payers and customers may expose us or them to broadly applicablefraud and abuse and other health care laws and regulations that may constrain the business or financial arrangements and relationships through which we or ourcollaborators market, sell and distribute our products that obtain marketing approval. Efforts to ensure that business arrangements comply with applicable healthcare laws and regulations involve substantial costs. It is possible that governmental authorities will conclude that our or our collaborators’ business practices maynot comply with current or future statutes, regulations or case law involving applicable fraud and abuse or other healthcare laws and regulations. If such operationsare found to be in violation of any of these laws or other applicable governmental regulations, we or the collaborator may be subject to significant civil, criminaland administrative penalties, damages, fines, exclusion from government funded healthcare programs, such as Medicare and Medicaid, and the curtailment orrestructuring of related operations. If physicians or other providers or entities involved with our products are found to be not in compliance with applicable laws,they may be subject to criminal, civil or administrative sanctions, including exclusions from government funded healthcare programs, which may adversely affectus. Our future depends on the proper management of our current and future business operations, including those of Molecular Insight and EXINI, and theirassociated expenses. Our business strategy requires us to manage our business to provide for the continued development and potential commercialization of our proprietary andpartnered product candidates. Our strategy also calls for us to undertake increased research and development activities and to manage an increasing number ofrelationships with partners and other third parties, while simultaneously managing the capital necessary to support this strategy. If we are unable to manageeffectively our current operations and any growth we may experience, our business, financial condition and results of operations may be adversely affected. If weare unable to effectively manage our expenses, we may find it necessary to reduce our personnel-related costs through reductions in our workforce, which couldharm our operations, employee morale and impair our ability to retain and recruit talent. Furthermore, if adequate funds are not available, we may be required toobtain funds through arrangements with partners or other sources that may require us to relinquish rights to certain of our technologies, products or future economicrights that we would not otherwise relinquish or require us to enter into other financing arrangements on unfavorable terms. Risks associated with our operations outside of the United States could adversely affect our business. Although we currently conduct nearly all of our business in the U.S., we are developing internationally and therefore have an increased exposure toforeign legal requirements, economic and political conditions and fluctuations in foreign currency exchange rates. We expect that we will continue to seek globalopportunities for our products and to develop our business outside the U.S. in the future. Such opportunities and development will inherently subject us to a numberof risks and uncertainties, including: ●changes in international regulatory and compliance requirements that could restrict our ability to develop, market and sell our products; ●political and economic instability; ●the impact of the vote by the United Kingdom decided by referendum to leave the European Union (commonly referred to as “Brexit”); ●diminished protection of intellectual property in some countries outside of the U.S.; ●trade protection measures and import or export licensing requirements; ●difficulty in staffing and managing international operations; ●differing labor regulations and business practices; ●potentially negative consequences from changes in or interpretations of tax laws; ●changes in international medical reimbursement policies and programs; ●financial risks such as longer payment cycles, difficulty collecting accounts receivable and exposure to fluctuations in foreign currency exchangerates; and ●regulatory and compliance risks that relate to maintaining accurate information and control over sales and distributors’ and service providers’activities that may fall within the purview of the FCPA or similar foreign laws such as the U.K. Bribery Act. 27Table of Contents Any of these factors may, individually or as a group, have a material adverse effect on our business and results of operations. These or other similar riskscould adversely affect our revenue and profitability. As we develop internationally, our exposure to these factors will increase. Reimbursement decisions by third-party payors may have an adverse effect on pricing and market acceptance of AZEDRA or any of our other drugcandidates. If there is not sufficient reimbursement for our future drugs, it is less likely that such drugs will be widely used. Reimbursement rates may vary according to the use of the drug and the clinical setting in which it is used, may be based on payments allowed for lower-cost products that are already reimbursed, may be incorporated into existing payments for other products or services, and may reflect budgetary constraints and/orimperfections in Medicare or Medicaid data used to calculate these rates. Net prices for drugs may be reduced by mandatory discounts or rebates required bygovernment health care programs. Such legislation, or similar regulatory changes or relaxation of laws that restrict imports of drugs from other countries, couldreduce the net price we receive for any future marketed drugs. As a result, our future drugs might not ultimately be considered cost-effective. We cannot be certain that reimbursement will be available for AZEDRA or any other drug candidates that we develop. Also, we cannot be certain thatreimbursement policies will not reduce the demand for, or the price paid for, any future drugs. If reimbursement is not available or is available on a limited basis,we may not be able to successfully commercialize AZEDRA or any other drug candidates that we develop. In general, other factors that could affect the demand for and sales and profitability of our future drugs include, but are not limited to: ●the timing of regulatory approval, if any, of competitive drugs; ●our or any other of our partners' pricing decisions, as applicable, including a decision to increase or decrease the price of a drug, and the pricingdecisions of our competitors; ●government and third-party payor reimbursement and coverage decisions that affect the utilization of our future drugs and competing drugs; ●negative safety or efficacy data from new clinical studies conducted either in the U.S. or internationally by any party could cause the sales of ourfuture drugs to decrease or a future drug to be recalled; ●the degree of patent protection afforded our future drugs by patents granted to or licensed by us and by the outcome of litigation involving our orany of our licensor's patents; ●the outcome of litigation involving patents of other companies concerning our future drugs or processes related to production and formulation ofthose drugs or uses of those drugs; ●the increasing use and development of alternate therapies; ●the rate of market penetration by competing drugs; and ●the termination of, or change in, existing arrangements with our partners. Any of these factors could have a material adverse effect on the sales of any drug candidates that we may commercialize in the future. Competitive Risks Competing products in development may adversely affect acceptance of our products. We are aware of a number of products and product candidates described in this Annual Report under Business – Competition which compete or maypotentially compete with RELISTOR. Any of these approved products or product candidates, or others which may be developed in the future, may achieve asignificant competitive advantage relative to RELISTOR, and, in any event, the existing or future marketing and sales capabilities of these competitors may impairValeant’s and/or other collaborators’ ability to compete effectively in the market. We are also aware of competitors, including those described under Business – Competition , which are developing alternative treatments for diseasetargets to which our research and development programs are directed, any of which – or others which may be developed in the future – may achieve a significantcompetitive advantage relative to any product we may develop. 28Table of Contents Marketplace acceptance depends in part on competition in our industry, which is intense, and competing products in development may adversely affectacceptance of our products. The extent to which any of our products achieves market acceptance will depend on competitive factors. Competition in the biopharmaceutical industry isintense and characterized by ongoing research and development and technological change. We face competition from many for-profit companies and majoruniversities and research institutions in the U.S. and abroad. We face competition from companies marketing existing products or developing new products fordiseases and conditions targeted by our technologies. We are aware of a number of products and product candidates, including those described in this AnnualReport under Business – Competition , which compete or may potentially compete with RELISTOR, PSMA-targeted imaging agents and therapeutics, or our otherproduct candidates. For instance, there are product candidates in pre-clinical or clinical development that target the side effects of opioid pain therapy, and amarketed product for the treatment of post-operative ileus could compete with RELISTOR. We are aware of several competitors, including those described underBusiness – Competition , which have received approval for or are developing alternative treatments or diagnostics for castration-resistant prostate cancer, some ofwhich are directed against PSMA. Any of these competing approved products or product candidates, or others which may be developed in the future, may achieve asignificant competitive advantage relative to RELISTOR, 1404, AZEDRA, PyL, 1095, or other product candidates. Competition with respect to our technologies and products is based on, among other things, product efficacy, safety, reliability, method of administration,availability, price and clinical benefit relative to cost; timing and scope of regulatory approval; sales, marketing and manufacturing capabilities; collaboratorcapabilities; insurance and other reimbursement coverage; and patent protection. Competitive disadvantages in any of these factors could materially harm ourbusiness and financial condition. Many of our competitors have substantially greater research and development capabilities and experience and greatermanufacturing, marketing, financial and managerial resources than we do. These competitors may develop products that are superior to those we are developingand render our products or technologies non-competitive or obsolete. Our products and product candidates under development may not compete successfully withexisting products or product candidates under development by other companies, universities and other institutions. Drug manufacturers that are first in the marketwith a therapeutic for a specific indication generally obtain and maintain a significant competitive advantage over later entrants and therefore, the speed with whichindustry participants move to develop products, complete clinical trials, approve processes and commercialize products is an important competitive factor. If ourproduct candidates receive marketing approval but cannot compete effectively in the marketplace, our operating results and financial position would suffer. Financial Risks We have outstanding debt - and failure by us or our royalty subsidiary to fulfill our obligations under the applicable loan agreements may cause therepayment obligations to accelerate. In November 2016, our subsidiary, MNTX Royalties, entered into a Royalty-Backed Loan with HCRP pursuant to which MNTX Royalties borrowed $50million and have the ability, subject to mutual agreement with HCRP, to borrow an additional $50 million up to twelve months after the initial closing date of theloan. The loan will be repaid from the royalty payments from the commercial sales of RELISTOR products owed under our agreement with Valeant. The obligations of MNTX Royalties under the loan agreement to repay the Royalty-Backed Loan may be accelerated upon the occurrence of certainevents of default, including but not limited to, if: ●MNTX Royalties fails to pay any principal or interest (except as permitted) within three Business days of when such payment is due and payable orotherwise made in accordance with the terms of the Royalty-Backed Loan; ●MNTX Royalties fails to pay when due any indebtedness of $15 thousand or more; ●any representation or warranty made by MNTX Royalties in the loan agreement or any other transaction document proves to be incorrect ormisleading in any material respect when made, and such failure is uncured on or before the 30 day following notice thereof; ●MNTX Royalties fails to perform or observe any covenant or agreement contained in the loan agreement or any other transaction document; 29th Table of Contents ●any uninsured judgment, decree, or order in an amount in excess of $25 thousand is rendered against MNTX Royalties and enforcement proceedingshave commenced upon such judgment, decree, or order or such judgment, decree, or order has not been stayed or bonded pending appeal, vacated, ordischarged, within 30 days from entry; ●any of a set of defined insolvency events occurs; ●we default under the agreement pursuant to which we contributed the royalty and related rights under the RELISTOR license to MNTX Royalties,and such default is continuing; ●any of the loan transaction documents cease to be in full force and effect or valid and enforceable; ●MNTX Royalties fails to perform or observe any covenant or agreement contained in any material contract and such failure is not cured or waivedwithin any applicable grace period; ●the agreement with Valeant is terminated or cancelled and is not replaced within 270 days after such termination or cancellation; and ●any security interest purported to be created by the loan agreement or the related security agreement ceases to be in full force and effect, or anyrights, powers, and privileges purported to be created and granted under the loan agreement or such security agreement ceases to be in full force andeffect. In connection with the Royalty-Backed Loan, MNTX Royalties granted a first priority lien and security interest (subject only to certain defined permittedliens) in all of its assets and all real, intangible and personal property, including all of its right, title, and interest in and to the royalty payments under our agreementwith Valeant. Under the terms of the loan agreement, HCRP has no recourse for non-payment of the Royalty-Backed Loan to Progenics Pharmaceuticals, Inc., or toany of our assets other than the RELISTOR royalty rights held by MNTX Royalties. However, Progenics Pharmaceuticals, Inc. does have certain obligations thatrun to the benefit of HCRP with respect to the representations, warranties and covenants it makes under the agreement pursuant to which we contributed the royaltyand related rights under the RELISTOR License to MNTX Royalties. A breach of these obligations could lead to recourse against Progenics Pharmaceuticals, Inc.with respect to any losses suffered by HCRP as a result of such breach. Our level of indebtedness could adversely affect our ability to raise additional capital to fund our operations, and limit our ability to react to changes inthe economy or our industry. As of December 31, 2016, our outstanding debt amounted to $49.5 million, which could increase by $50 million upon MNTX and HRCP’s mutualagreement, over the ensuing year. These levels could have adverse consequences for us, including: ●heightening our vulnerability to downturns in our business or our industry or the general economy and restricting us from making improvements oracquisitions, or exploring business opportunities; and ●limiting our ability to adjust to changing market conditions and placing us at a competitive disadvantage compared to our competitors who havegreater capital resources. Developing product candidates requires us to obtain additional financing from time to time. Our access to capital funding is uncertain. We incur significant costs to develop our product candidates. We do not have committed external sources of funding for these projects. We fund ouroperations to a significant extent from capital-raising. We may do so via equity securities issuances in public offerings, such as our first quarter 2014 $37.5 millionunderwritten public offering of 8.75 million shares of common stock, through our three-year facility with an investment bank pursuant to which we may sell fromtime to time up to $75.0 million of our stock in at-the-market transactions, or through further debt financing. We may also fund operations through collaboration,license, further royalty financings, private placement or other agreements with one or more pharmaceutical or other companies, or the receipt of milestone andother payments for out-licensed products. To the extent we raise additional capital by issuing equity securities, existing stockholders could experience substantialdilution, and if we issue securities other than common stock, new investors could have rights superior to existing stockholders. Any further debt financing that wemay obtain may involve operating covenants that restrict our business and significant repayment obligations. To the extent we raise additional funds through newcollaboration and licensing arrangements, we may be required to relinquish some rights to technologies or product candidates, or grant licenses on terms that arenot favorable to us. 30Table of Contents We cannot predict with certainty when we will need additional funds, how much we will need, the form a financing may take or whether additional fundswill be available at all. The variability of conditions in global financial and credit markets may exacerbate the difficulty of timing capital raising or other financing,as a result of which we may seek to consummate such transactions substantially in advance of immediate need. Our need for future funding will depend onnumerous factors, including the advancement of existing product development projects and the availability of new projects; the achievement of events, most ofwhich are out of our control and depend entirely on the efforts of others, triggering milestone payments to us; the progress and success of clinical trials and pre-clinical activities (including studies and manufacturing) involving product candidates, whether conducted by collaborators or us; the progress of research programscarried out by us; changes in the breadth of our research and development programs; the progress of research and development efforts of collaborators; our abilityto acquire or license necessary, useful or otherwise attractive technologies; competing technological and market developments; the costs and timing of obtaining,enforcing and defending patent and other intellectual property rights; the costs and timing of regulatory filings and approvals; our ability to manage Progenics’growth or contraction; and unforeseen litigation. These factors may be more important with respect to product candidates and programs that involve technologieswith which we have limited prior experience, such as those originally developed by Molecular Insight. Insufficient funds may require us to delay, scale back oreliminate some or all of our research and development or commercialization programs, cause us to lose rights under existing licenses or to relinquish greater or allrights to product candidates at an earlier stage of development or on less favorable terms than we would otherwise choose and may adversely affect our ability tooperate as a going concern. We may not be able at a given necessary time to obtain additional funding on acceptable terms, or at all. Our inability to raise additionalcapital on terms reasonably acceptable to us would seriously jeopardize our business. We have a history of operating losses. Progenics has incurred substantial losses throughout its history. A large portion of our revenue has historically consisted of upfront and milestone fromlicensing transactions. We have reported operating losses for 2015 and while we reported operating income for 2016 and 2014, as a result of milestone paymentsfrom Valeant, the timing and amount of any similar transactions in the future is highly unpredictable and uncertain. Without upfront or other such payments, weoperate at a loss, due in large part to the significant research and development expenditures required to identify and validate new product candidates and pursue ourdevelopment efforts. Moreover, we have derived no significant revenue from product sales and have only in the last several years derived revenue from royalties.We may not achieve significant product sales or royalty revenue for a number of years, if ever. We expect to incur net operating losses and negative cash flow fromoperations in the future, which could increase significantly if we expand our clinical trial programs and other product development efforts. Our ability to achieveand sustain profitability is dependent in part on obtaining regulatory approval for and then commercializing our product candidates, either alone or with others. Wemay not be able to develop and commercialize products beyond subcutaneous RELISTOR for OIC in patients with advanced illness and for those with chronic,non-cancer pain and RELISTOR Tablets for adult patients with chronic, non-cancer pain. Our operations may not be profitable even if any of our other productcandidates under development are commercialized. Our ability to use net operating losses to offset future taxable income is subject to certain limitations. We currently have significant net operating losses (“NOLs”) that may be used to offset future taxable income. The U.S. Internal Revenue Code limits theamount of taxable income that may be offset annually by NOL carryforwards after a change in control (generally greater than 50% change in ownership) of a losscorporation, and our use of NOL carryforwards may be further limited as a result of any future equity transactions that result in an additional change of control. Progenics’ stock price has a history of volatility and may be affected by selling pressure, including in the event of substantial sales of Progenics stock byformer Molecular Insight stockholders. You should consider an investment in Progenics stock as risky and invest only if you can withstand a significantloss. Our stock price has a history of significant volatility. It has varied between a high of $9.78 and a low of $3.61 in 2016 and between a high of $11.15 and alow of $4.86 in 2015. Factors that may have a significant impact on the market price of our common stock include the results of clinical trials and pre-clinicalstudies undertaken by us or others; delays, terminations or other changes in development programs; developments in marketing approval efforts; developments incollaborator or other business relationships, particularly regarding RELISTOR, AZEDRA or other significant products or programs; technological innovation orproduct announcements by us, our collaborators or our competitors; patent or other proprietary rights developments; governmental regulation; changes inreimbursement policies or health care legislation; safety and efficacy concerns about products developed by us, our collaborators or our competitors; our ability tofund ongoing operations; fluctuations in our operating results; general market conditions; and the reporting of or commentary on such matters by the press andothers. At times, our stock price has been volatile even in the absence of significant news or developments. The stock prices of biotechnology companies andsecurities markets generally have been subject to dramatic price swings in recent years, and financial and market conditions during that period have resulted inwidespread pressures on securities of issuers throughout the world economy. 31Table of Contents Our stockholders may be diluted, and the price of our common stock may decrease, as a result of future issuances of securities, exercises of outstandingstock options, or sales of outstanding securities. We expect to issue additional common stock in public offerings, private placements and/or through our January 2017 sales agreement with an investmentbank, pursuant to which we may sell from time to time up to $75.0 million of our stock, and to issue options to purchase common stock for compensation purposes.We may issue preferred stock, restricted stock units or securities convertible into or exercisable or exchangeable for our common stock. All such issuances woulddilute existing investors and could lower the price of our common stock. Sales of substantial numbers of outstanding shares of common stock, such as sales byformer Molecular Insight stockholders of unregistered shares received in the acquisition, could also cause a decline in the market price of our stock. We requiresubstantial external funding to finance our research and development programs and may seek such funding through the issuance and sale of our common stock,which we have done in follow-on primary offerings in late 2012, mid-2013 and February 2014. We have a shelf registration statement which may be used to issueup to $250.0 million of common stock and other securities before any underwriter discounts, commissions and offering expenses. We also have in place registrationstatements covering shares issuable pursuant to our equity compensation plans, and sales of our securities under them could cause the market price of our stock todecline. Sales by existing stockholders or holders of options or other rights may adversely affect the market price of our common stock. Other Risks Our principal stockholders are able to exert significant influence over matters submitted to stockholders for approval. At December 31, 2016, our directors and executive officers together beneficially owned or controlled approximately 3.5% of our outstanding commonshares, including shares currently issuable upon option exercises, and our five largest other stockholders held approximately 47.7%. Should these parties choose toact alone or together, they could exert significant influence in determining the outcome of corporate actions requiring stockholder approval and otherwise controlour business. This control could, among other things, have the effect of delaying or preventing a change in control of the Company, adversely affecting our stockprice. Anti-takeover provisions may make removal of our Board and/or management more difficult, discouraging hostile bids for control that may be beneficialto our stockholders. Our Board is authorized, without further stockholder action, to issue from time to time shares of preferred stock in one or more designated series orclasses. The issuance of preferred stock, as well as provisions in some outstanding stock options that provide for acceleration of vesting upon a change of control,and Section 203 and other provisions of the Delaware General Corporation Law could make a takeover or the removal of our Board or management more difficult;discourage hostile bids for control in which stockholders may receive a premium for their shares; and otherwise dilute the rights of common stockholders anddepress the market price of our stock. Item 1B. Unresolved Staff Comments There were no unresolved SEC staff comments regarding our periodic or current reports under the Exchange Act as of December 31, 2016. Item 2. Properties At December 31, 2016, we occupied approximately 26,000 square feet of corporate office space located in New York City, pursuant to lease agreementsexpiring in September 2030 (subject to an early termination right) under which we pay rent and facilities charges including utilities, taxes, and operating expenses. Our EXINI subsidiary leases approximately 4,000 square feet of office space in Lund, Sweden. The lease term expires on December 31, 2018, with anoption to renew the term for an additional three years. Item 3. Legal Proceedings On January 4, 2017, we settled all claims against us under a federal action brought in 2010 by a former employee, where such former employee hadcomplained that we had violated the anti-retaliation provisions of the Federal Sarbanes-Oxley law by terminating him. In connection with this settlement, we andthe former employee exchanged mutual releases and we are to pay an aggregate sum of $4.0 million to the former employee and his attorneys, which is included inaccrued expenses on our consolidated balance sheet at December 31, 2016. We have $1.7 million held by the District Court in escrow and recorded as restrictedcash in other current assets on our consolidated balance sheet at December 31, 2016. 32Table of Contents On October 25, 2016, Progenics, Valeant, and Wyeth LLC (“Wyeth”, Valeant’s predecessor as licensee of RELISTOR) received a notification of aParagraph IV certification with respect to certain patents for RELISTOR Tablets. The certification accompanied the filing by Actavis LLC of an Abbreviated NewDrug Application (“ANDA”) challenging such patents for RELISTOR Tablets and seeking to obtain approval to market a generic version of RELISTOR tabletsbefore some or all of these patents expire. On October 28, 2015, Progenics, Valeant, and Wyeth received a second notification of a Paragraph IV certification with respect to the same patents forRELISTOR subcutaneous injection from Actavis LLC as a result of Actavis LLC’s filing of an ANDA with the FDA, also challenging these patents and seeking toobtain approval to market a generic version of RELISTOR subcutaneous injection before some or all of these patents expire. On October 7, 2015, Progenics, Valeant, and Wyeth received notification of a Paragraph IV certification for certain patents for RELISTOR(methylnaltrexone bromide) subcutaneous injection, which are listed in the FDA's Approved Drug Products with Therapeutic Equivalence Evaluations, or theOrange Book. The certification resulted from the filing by Mylan Pharmaceuticals, Inc. of an ANDA with the FDA, challenging such patents for RELISTORsubcutaneous injection and seeking to obtain approval to market a generic version of RELISTOR subcutaneous injection before some or all of these patents expire. In accordance with the Drug Price Competition and Patent Term Restoration Act (commonly referred to as the Hatch-Waxman Act), Progenics andValeant timely commenced litigation against each of these ANDA filers in order to obtain an automatic stay of FDA approval of the ANDA until the earlier of (i)30 months from receipt of the notice or (ii) a District Court decision finding that the identified patents are invalid, unenforceable or not infringed. In addition to the above described ANDA notifications, in October 2015 Progenics received notices of opposition to three European patents relating tomethylnaltrexone. The oppositions were filed separately by each of Actavis Group PTC ehf. and Fresenius Kabi Deutschland GmbH. Each of the above-described proceedings is in its early stages and Progenics and Valeant continue to cooperate closely to vigorously defend and enforceRELISTOR intellectual property rights. Pursuant to the RELISTOR License Agreement between Progenics and Valeant, Valeant has the first right to enforce theintellectual property rights at issue and is responsible for the costs of such enforcement. We are or may be from time to time involved in various other disputes, governmental and/or regulatory inspections, inquires, investigations andproceedings that could result in litigation, and other litigation matters that arise from time to time. The process of resolving matters through litigation or othermeans is inherently uncertain and it is possible that an unfavorable resolution of these matters will adversely affect us, our results of operations, financial condition,and cash flows. Item 4. Not Applicable PART II Item 5. Market for Registrant’s Common Equity, Related Stockholder Matters and Issuer Purchases of Equity Securities Price Range of Common Stock Our common stock is quoted on The NASDAQ Stock Market LLC under the symbol PGNX. The following table sets forth, for the periods indicated, thehigh and low sales price per share of the common stock, as reported on NASDAQ. High Low 2016 Fourth quarter $9.78 $4.84 Third quarter 7.09 4.19 Second quarter 5.75 4.00 First quarter 6.13 3.61 2015 Fourth quarter $8.37 $5.20 Third quarter 11.15 5.38 Second quarter 9.27 4.86 First quarter 7.84 5.35 33Table of Contents On March 6, 2017, the last sale price for our common stock, as reported by The NASDAQ Stock Market LLC, was $10.99. There were approximately 68holders of record of our common stock as of that date. Comparative Stock Performance Graph The graph below compares, for the past five years, the cumulative stockholder return on our common stock with the cumulative stockholder return of (i)the NASDAQ U.S. Benchmark (TR) Index and (ii) the ICB: 4577 Pharmaceuticals (Subsector) Index, assuming an investment in each of $100 on December 30,2011. 34Table of Contents Dividends We have never paid any dividends, and we currently anticipate that all earnings, if any, will be retained for development of our business and no dividendswill be declared in the foreseeable future. Item 6. Selected Financial Data The selected historical consolidated statement of operations data presented below for the years ended December 31, 2016, 2015, and 2014 and thehistorical consolidated balance sheet data as of December 31, 2016 and 2015 have been derived from our audited consolidated financial statements, which areincluded elsewhere in this Annual Report on Form 10-K. The historical consolidated statement of operations data presented below for the year ended December 31,2013 and 2012 and the historical consolidated balance sheet data as of December 31, 2014, 2013, and 2012 have been derived from our audited consolidatedfinancial statements that do not appear in this report. The data set forth below should be read in conjunction with Management’s Discussion and Analysis ofFinancial Condition and Results of Operations and the consolidated financial statements and related notes included elsewhere herein. The selected historicalfinancial information in this section is not intended to replace our financial statements and the related notes thereto. Years Ended December 31, 2016 2015 2014 2013 2012 (In thousands, except per share data) Consolidated Statements of Operations Data: Revenue: Royalty income $10,295 $6,608 $3,101 $5,923 $4,963 License revenue 59,081 1,955 41,196 1,595 8,525 Research grants - - - 275 488 Other revenue 53 113 80 69 72 Total revenue 69,429 8,676 44,377 7,862 14,048 Expenses: Research and development 37,569 28,196 28,592 34,582 33,001 General and administrative 23,356 18,184 15,489 15,541 16,538 Intangible impairment charges - - 2,676 919 - Change in contingent consideration liability (4,600) 1,600 1,500 (200) - Total operating expenses 56,325 47,980 48,257 50,842 49,539 Other operating income - - 7,250 - - Operating income (loss) 13,104 (39,304) 3,370 (42,980) (35,491) Other income (expense): Interest (expense) income, net (493) 52 51 46 60 Other expense, net (34) - - - - Total other (expense) income (527) 52 51 46 60 Income (loss) before income tax (expense) benefit 12,577 (39,252) 3,421 (42,934) (35,431)Income tax (expense) benefit (1,844) 133 989 362 - Net income (loss) 10,733 (39,119) 4,410 (42,572) (35,431)Net loss attributable to noncontrolling interests (73) (7) - - - Net income (loss) attributable to Progenics $10,806 $(39,112) $4,410 $(42,572) $(35,431) Per share amount on net income (loss) attributable to Progenics: Basic $0.15 $(0.56) $0.06 $(0.76) $(1.02)Diluted $0.15 $(0.56) $0.06 $(0.76) $(1.02) December 31, 2016 2015 2014 2013 2012 (In thousands) Consolidated Balance Sheets Data: Cash and cash equivalents $138,909 $74,103 $119,302 $65,860 $58,838 Auction rate securities - - - 2,208 3,240 Working capital 131,744 73,556 115,241 64,055 58,805 Total assets 198,986 131,251 161,037 114,541 76,308 Other liabilities - long term 77,867 30,861 29,443 28,935 1,078 Total stockholders' equity 104,762 90,661 124,909 78,979 66,568 35Table of Contents Item 7. Management’s Discussion and Analysis of Financial Condition and Results of Operations ( “ MD&A ” ) Overview We develop innovative medicines and other technologies to target and treat cancer. Our pipeline includes: (1) therapeutic agents designed to preciselytarget cancer (AZEDRA and 1095); (2) PSMA-targeted imaging agents for prostate cancer (1404 and PyL); and (3) imaging analysis tools. Our first commercialproduct, RELISTOR (methylnaltrexone bromide) for opioid-induced constipation, is partnered with Valeant. We have licensed RELISTOR to Valeant, and have partnered other internally-developed or acquired compounds and technologies with third parties. Wecontinue to consider opportunities for strategic collaborations, out-licenses and other arrangements with biopharmaceutical companies involving proprietaryresearch, development and clinical programs, and may in the future also in-license or acquire additional oncology compounds and/or programs. EXINI Acquisition Update On November 12, 2015, we acquired 92.45% of the outstanding shares of EXINI, a Lund, Sweden based leader in the development of advanced imaginganalysis tools and solutions for medical decision support. EXINI's operations are included in our consolidated financial statements beginning November 12, 2015,the date we acquired control. Through the end of the extended acceptance period of November 27, 2015, we acquired additional outstanding shares, bringing ourownership to 96.81%. We commenced a judicial process in Sweden for acquiring the remaining shares and EXINI was delisted and ceased to be publicly tradedeffective as of the close of trading on December 4, 2015. On December 8, 2016, a Swedish arbitral tribunal awarded us advanced title to the remaining shares ofEXINI and, as of that date, EXINI became a wholly-owned subsidiary with 100% of the voting shares owned by us. A portion of EXINI’s results of operations from November 12, 2015 through December 31, 2015 and from January 1, 2016 through December 8, 2016 hasbeen allocated to the noncontrolling interests in EXINI for 2015 and 2016, respectively. License Agreement In April 2016, we entered into an agreement with a Bayer subsidiary granting Bayer exclusive worldwide rights to develop and commercialize productsusing our PSMA antibody technology in combination with Bayer's alpha-emitting radionuclides. Royalty Monetization On November 4, 2016, through a new wholly-owned subsidiary MNTX Royalties, we entered into a loan agreement (the “Royalty-Backed Loan”) with afund managed by HealthCare Royalty Partners III, L.P. (“HCRP”) pursuant to which HCRP agreed to make term loans in an aggregate principal amount of up to$100.0 million. We borrowed $50.0 million and can borrow an additional $50.0 million, subject to mutual agreement with HCRP, up to twelve months after theclosing date. (see Note 9. Long-Term Debt, Net for additional information) Liquidity and Capital Resources Our current principal sources of revenue from operations are royalty, development and commercial milestones, and sublicense revenue-sharing payments.Royalty and further milestone payments from RELISTOR depend on success in development and commercialization, which is dependent on many factors, such asValeant’s efforts, decisions by the FDA and other regulatory bodies, competition from drugs for the same or similar indications, and the outcome of clinical andother testing of RELISTOR. Under the agreement with Bayer, we received in the second quarter of 2016 a $4.0 million upfront payment and a $1.0 millionpayment related to the achievement of a preclinical development milestone. In addition, in the fourth quarter of 2016, we recognized $2.0 million as licenserevenue from Bayer related to the achievement of a second preclinical development milestone. In 2015, we received a $1.5 million milestone payment as a result ofCytoDyn’s dosing of the first patient in its Phase 3 clinical trial for PRO 140. In 2014, we Progenics and Ono Pharmaceutical Co., Ltd. (“Ono”), our formerlicensee of RELISTOR in Japan, settled all claims between them relating to an arbitration commenced by us in 2013, the parties’ October 2008 License Agreement,and the former licensee’s development and commercialization of the drug. In connection therewith, the parties exchanged mutual releases and the former licenseepaid us $7.25 million, which is reflected as other operating income in our consolidated statement of operations in 2014. 36Table of Contents We fund our operations to a significant extent from capital-raising. In 2014, we completed an underwritten public offering of 8.75 million shares ofcommon stock at a public offering price of $4.60 per share, resulting in net proceeds of approximately $37.5 million. In 2016, we entered into the Royalty-BackedLoan resulting in net proceeds of approximately $48.7 million. If we do not realize sufficient royalty or milestone revenue from RELISTOR, or are unable to enter into favorable collaboration, license, asset sale,additional capital raising, or other financing transactions, we will have to reduce, delay, or eliminate spending on certain programs, and/or take other economicmeasures. Results of Operations The following table is an overview of our results of operations (in thousands, except percentages): 2016 2015 2014 2016 vs. 2015 2015 vs. 2014 Total revenue $69,429 $8,676 $44,377 700% (80%)Operating expenses $56,325 $47,980 $48,257 17% (1%)Operating income (loss) $13,104 $(39,304) $3,370 (133%) (1266%)Net income (loss) $10,733 $(39,119) $4,410 (127%) (987%)Net income (loss) attributable to Progenics $10,806 $(39,112) $4,410 (128%) (987%) Revenue Our sources of revenue during the years indicated below include royalties and license fees from Valeant, Bayer and other licensees and, to a small extent,sale of research reagents. The following table is a summary of our worldwide revenue (in thousands, except percentages): Source 2016 2015 2014 2016 vs. 2015 2015 vs. 2014 Royalty income $10,295 $6,608 $3,101 56% 113%License revenue 59,081 1,955 41,196 2922% (95%)Other revenue 53 113 80 (53%) 41%Total revenue $69,429 $8,676 $44,377 700% (80%) Royalty income. We recognized royalty income primarily based on the below net sales of RELISTOR as reported to us by Valeant (in thousands). 2016 2015 2014 2016 vs. 2015 2015 vs. 2014 U.S. $66,900 $40,700 $16,200 64% 151%Outside U.S. 3,700 3,100 4,100 19% (24%)Worldwide net sales of RELISTOR $70,600 $43,800 $20,300 61% 116% The increase in worldwide net sales of RELISTOR of $26.8 million in 2016 compared to 2015 was primarily attributable to higher unit sales. Sales ofRELISTOR tablets were launched in September 2016. The increase in worldwide net sales of RELISTOR of $23.5 million in 2015 compared to 2014 was primarilyattributable to higher unit sales of RELISTOR subcutaneous injection. In 2014, RELISTOR subcutaneous injection was approved for treatment of OIC in non-cancer pain patients. License revenue. The increase in license revenue of $57.1 million in 2016 compared to 2015 was attributable to a $50.0 million milestone paymentreceived under the RELISTOR License Agreement and $7.0 million for upfront and milestone payments under the Bayer license agreement. The decrease in licenserevenue of $39.2 million in 2015 compared to 2014 was primarily attributable to a $40.0 million milestone payment received from Valeant in 2014 for the approvalof RELISTOR subcutaneous injection for treatment of OIC in non-cancer pain patients. 37Table of Contents Operating Expenses The following table is a summary of our operating expenses (in thousands, except percentages): Operating Expenses 2016 2015 2014 2016 vs. 2015 2015 vs. 2014 Research and development $37,569 $28,196 $28,592 33% (1%)General and administrative 23,356 18,184 15,489 28% 17%Intangible impairment charges - - 2,676 N/A (100%)Change in contingent consideration liability (4,600) 1,600 1,500 (388%) 7%Total operating expenses $56,325 $47,980 $48,257 17% (1%) Research and Development (“R&D”) R&D expenses increased by $9.4 million, or 33%, in 2016 compared to 2015 and decreased by $0.4 million, or 1%, in 2015 compared to 2014. Theincrease in 2016 was primarily attributable to higher clinical trial expenses related to the start of the Phase 3 trial for 1404 and the Phase 2/3 trial for PyL inaddition to higher contract manufacturing expenses for the planned Phase 1 trial of 1095 and the Phase 2 registrational trial for AZEDRA. The decrease in 2015was primarily attributable to lower personnel related expenses (salaries, benefits, and stock-based compensation), partially offset by higher contract manufacturingexpenses for AZEDRA. General and Administrative (“G&A”) G&A expenses increased by $5.2 million, or 28%, in 2016 compared to 2015 and $2.7 million, or 17%, in 2015 compared to 2014. The increase in 2016was primarily attributable to higher depreciation expense as a result of a reduction in the remaining useful lives of the leasehold improvements at our formerlocation in Tarrytown, New York, higher compensation costs related to increases in headcount, and higher market research expenses. The increase in 2015 wasprimarily attributable to an accrual for compensation related to litigation with a former employee and personnel related expenses (salaries, benefits, and stock-basedcompensation). Intangible Impairment Charges There were no intangible impairment charges recognized in 2016 and 2015. The 2014 charge of $2.7 million was due to impairments of our indefinite-and finite-lived intangibles based on our annual review of the intangible assets. Change in Contingent Consideration Liability The decrease in the contingent consideration liability of $4.6 million in 2016 resulted primarily from a change in the discount rates and sales projectionsused in calculating the contingent consideration liability for the potential sales-based milestone payments to former Molecular Insight stockholders under theacquisition agreement. The increase in the contingent consideration liability of $1.6 million in 2015 resulted primarily from a decrease in the discount period. Other Income (Expense) The following table is a summary of our other income (expense) (in thousands, except percentages): Other Income (Expense) 2016 2015 2014 2016 vs. 2015 2015 vs. 2014 Interest (expense) income, net (493) 52 51 (1048%) 2%Other expense, net (34) - - N/A N/A Other (expense) income $(527) $52 $51 (1113%) 2% Other income (expense) decreased by $579 thousand, or 1113%, in 2016 compared to 2015 and increased by $1 thousand, or 2%, in 2015 compared to2014. The decrease in 2016 was primarily attributable to interest expense on the Royalty-Backed Loan, partially offset by an increase in interest income due tohigher average cash balances during the current year and higher average interest rates earned by our money market funds. The change in 2015 was essentially flatwith 2014. 38Table of Contents Income Taxes The following table is a summary of our income tax (provision) benefit and effective tax rate (in thousands, except percentages): 2016 2015 2014 Income tax (provision) benefit $(1,844) $133 $989 Effective tax rate 14.7% 0.3% -28.8% The income tax provision increased by $2.0 million in 2016 compared to 2015 as a result of an increase in the effective tax rate. The effective tax rate for2016 was 14.7%. Our effective tax rate was impacted by our relocation to New York City, which has its own local tax rate and adds to the overall tax rate used forcalculating the income tax provision. The income tax benefit decreased by $0.8 million in 2015 compared to 2014 as a result of the change in the temporarydifference between carrying amounts of in-process research and development assets for financial reporting purposes and the amounts used for income tax purposes.The effective tax rate for 2015 was 0.3% Net Income (Loss) Our net income was $10.8 million in 2016 compared to a net loss of $39.1 million in 2015 and net income of $4.4 million in 2014. The milestonepayments received from the Valeant license agreement of $50.0 million and $40.0 million in 2016 and 2014, respectively, were the primary drivers for realizing netincome in those years. Liquidity and Capital Resources The following table is a summary of selected financial data (in thousands): 2016 2015 2014 Cash and cash equivalents $138,909 $74,103 $119,302 Accounts receivable, net $4,864 $3,543 $109 Total assets $198,986 $131,251 $161,037 Working capital $131,744 $73,556 $115,241 We have to-date funded operations principally through proceeds received from private placements of equity securities, public offerings of common stock,monetization of royalties, up-front payments, development milestones, royalties from license agreements, and proceeds from the exercise of outstanding stockoptions. At December 31, 2016, we had $138.9 million in cash and cash equivalents, an increase of $64.8 million from $74.1 million at December 31, 2015. Webelieve our existing balances of cash and cash equivalents will be sufficient to satisfy our working capital needs, capital asset purchases, outstanding commitments,and other liquidity requirements associated with our existing operations over the next twelve (12) months. If we do not realize sufficient royalties or milestone payments from Valeant, Bayer, or other licensees, or raise additional capital, we will have to reduce,delay, or eliminate spending on certain programs, and/or take other economic measures. During the first quarter of 2017, we established a $250.0 million replacement shelf registration statement. Cash Flows The following table is a summary of our cash flow activities (in thousands): 2016 2015 2014 Net cash provided by (used in) operating activities $19,209 $(40,137) $13,726 Net cash (used in) provided by investing activities $(3,939) $(6,524) $1,829 Net cash provided by financing activities $49,622 $1,445 $37,887 Operating Activities Net cash provided by operating activities during 2016 and 2014 was primarily attributable to the milestone payments received from Valeant for theRELISTOR approvals ($50.0 million in 2016 and $40.0 million in 2014), partially offset by operating expenses, net of non-cash items. Net cash used by operatingactivities during 2015 was primarily attributable to funding operating expenses, net of non-cash items. 39Table of Contents Investing Activities Net cash used in investing activities was primarily related to capital expenditures in 2016 and the acquisition of EXINI in 2015, partially offset byproceeds from the sale of fixed assets. During 2014, net cash provided by investing activities included $2.4 million in proceeds from redemption of auction ratesecurities. Financing Activities Net cash provided by financing activities during 2016, 2015, and 2014 was attributable to proceeds from the exercise of stock options, in addition to thenet proceeds from the royalty monetization in 2016 and from the issuance of common stock from an underwritten public offering in 2014. Contractual Obligations Our funding requirements for the next 12 months and beyond will include required payments under operating leases and fixed payments under licenseagreements. The following table summarizes our contractual obligations as of December 31, 2016 for future payments under these agreements: Payments Due by Period Total Less than oneyear 1 to 3 years 3 to 5 years Greater than 5years Operating leases $29.9 $1.8 $3.7 $3.7 $20.7 Fixed payments under license agreements 1.2 0.2 0.4 0.1 0.5 Total $31.1 $2.0 $4.1 $3.8 $21.2 (1)Does not include milestone or contractual payment obligations contingent upon the achievement of certain milestones or events if the amount and timing of such obligations areunknown or uncertain. We may be required to pay additional amounts up to approximately: (i) $90.6 million in contingent milestone payments under our license agreements; (ii)$93.0 million in payments to the former stockholders of Molecular Insight, contingent upon achieving specified commercialization events or sales targets; and (iii) $77.2 million infuture principal and interest, based upon estimated sales projections, under the Royalty-Backed Loan. We periodically assess the scientific progress and merits of each of our programs to determine if continued research and development is commercially andeconomically viable. Certain of our programs have been terminated due to the lack of scientific progress and prospects for ultimate commercialization. Because ofthe uncertainties associated with research and development in these programs, the duration and completion costs of our research and development projects aredifficult to estimate and are subject to considerable variation. Our inability to complete research and development projects in a timely manner or failure to enterinto collaborative agreements could significantly increase capital requirements and adversely affect our liquidity. Our cash requirements may vary materially from those now planned because of results of research and development and product testing, changes inexisting relationships or new relationships with licensees, licensors or other collaborators, changes in the focus and direction of our research and developmentprograms, competitive and technological advances, the cost of filing, prosecuting, defending and enforcing patent claims, the regulatory approval process,manufacturing and marketing and other costs associated with the commercialization of products following receipt of regulatory approvals and other factors. The above discussion contains forward-looking statements based on our current operating plan and the assumptions on which it relies. There could bedeviations from that plan that would consume our assets earlier than planned. Off-Balance Sheet Arrangements and Guarantees We have no obligations under off-balance sheet arrangements and do not guarantee the obligations of any other unconsolidated entity. Critical Accounting Policies We prepare our financial statements in conformity with accounting principles generally accepted in the U.S. Our significant accounting policies aredisclosed in Note 2 to our financial statements included in this Report. The selection and application of these accounting principles and methods requires us tomake estimates and assumptions that affect the reported amounts of assets, liabilities, revenues and expenses, as well as certain financial statement disclosures. Weevaluate these estimates on an ongoing basis. We base these estimates on historical experience and on various other assumptions that we believe reasonable underthe circumstances. The results of these evaluations form the basis for making judgments about the carrying values of assets and liabilities that are not otherwisereadily apparent. While we believe that the estimates and assumptions we use in preparing the financial statements are appropriate, they are subject to a number offactors and uncertainties regarding their ultimate outcome and, therefore, actual results could differ from these estimates. 40(1)Table of Contents The critical accounting policies we use and the estimates we make are described below. These are policies and estimates that we believe are the mostimportant in portraying our financial condition and results of operations, and that require our most difficult, subjective or complex judgments, often as a result ofthe need to make estimates about the effect of matters that are inherently uncertain. We have discussed the development, selection and disclosure of these criticalaccounting policies and estimates with the Audit Committee of our Board of Directors. Revenue Recognition. We recognize revenue from all sources based on the provisions of the SEC’s Staff Accounting Bulletin (“SAB”) No. 104 (“SAB104”) and the Financial Accounting Standards Board (“FASB”) Accounting Standards Codification (“ASC”) 605 (Topic 605, Revenue Recognition ). ASC 605 specifies how to separate deliverables in multiple-deliverable arrangements, and how to measure and allocate arrangement consideration to oneor more units of accounting, and provides that the delivered item(s) are separate units of accounting, if (i) the delivered item(s) have value to a collaborator on astand-alone basis, and (ii), if the arrangement includes a general right of return relative to the delivered item, delivery or performance of the undelivered item(s) isconsidered probable and substantially in our control. Royalty revenue or loss is recognized based upon net sales of related licensed products, and is recognized in the period the sales (losses) occur, providedthat the royalty amounts are fixed or determinable, collection of the related receivable is reasonably assured and we have no remaining performance obligationsunder the arrangement providing for the royalty. Royalty loss is recognized based upon reported sales deductions in excess of gross sales resulting in net losses andare recognized in the period net losses occur. Royalty loss is classified in royalty income in the consolidated statements of operations and the related accruedroyalty loss liability is classified in accounts payable and accrued expenses in the consolidated balance sheets. Share-Based Payment Arrangements. Our share-based compensation of employees includes non-qualified stock options and restricted stock, which arecompensatory under ASC 718 (Topic 718, Compensation – Stock Compensation ). We account for share-based compensation to non-employees, including non-qualified stock options and restricted stock, in accordance with ASC 505 (Topic 505, Equity ). The fair value of each non-qualified stock option award is estimated on the date of grant using the Black-Scholes option pricing model. The modelrequires input assumptions with respect to (i) expected volatility of our common stock, which is based upon the daily quoted market prices on The NASDAQ StockMarket LLC over a period equal to the expected term, (ii) the period of time over which employees, officers, directors and non-employee consultants are expectedto hold their options prior to exercise, (iii) expected dividend yield (zero in our case due to never having paid dividends and not expecting to pay dividends in thefuture), and (iv) risk-free interest rates for periods within the expected term of the options, which are based on the U.S. Treasury yield curve in effect at the time ofgrant. Historical volatilities are based upon daily quoted market prices of our common stock on The NASDAQ Stock Market LLC over a period equal to theexpected term of the related equity instruments. We rely only on historical volatility since we believe it is generally viewed as providing the most reliableindication of future volatility. In estimating expected future volatility, we assume it will be consistent with historical; we calculate historical volatility using asimple average calculation; we use available historical data for the length of the option’s expected term, and we consistently use a sufficient number of priceobservations. Since our stock options are not traded on a public market, we do not use implied volatility. The expected term of options granted represents the period of time that options granted are expected to be outstanding based upon historical data related toexercise and post-termination cancellation activity. The expected term of stock options granted to our Chief Executive Officer (“CEO”) and non-employeedirectors, consultants and officers are calculated separately from stock options granted to other employees. We apply a forfeiture rate to the number of unvested awards in each reporting period in order to estimate the number of awards that are expected to vest.Estimated forfeiture rates are based upon historical data on vesting behavior of employees. We adjust the total amount of compensation cost recognized for eachaward, in the period in which each award vests, to reflect the actual forfeitures related to that award. Changes in our estimated forfeiture rate will result in changesin the rate at which compensation cost for an award is recognized over its vesting period. 41Table of Contents Changes in the assumptions used to compute the fair value of the option awards are likely to affect their fair value and the amount of compensationexpense recognized in future periods. A higher volatility, longer expected term and higher risk-free rate increases the resulting compensation expense recognized infuture periods. Conversely, a lower volatility, shorter expected term and lower risk-free rate decreases such expense recognized in future periods. Clinical Trial and Other Research and Develo pment Expenses . Clinical trial expenses, which are included in research and development expenses,represent obligations resulting from contracts with various clinical investigators and clinical research organizations in connection with conducting clinical trials forour product candidates. Such costs are expensed as incurred, and are generally based on the total number of patients in the trial, the rate at which the patients enterthe trial and the period over which the clinical investigators and clinical research organizations provide services. We believe that this method best aligns the effortsexpended on a clinical trial with the expenses we record. We adjust our rate of clinical expense recognition if actual results differ from our estimates. In addition toclinical trial expenses, we estimate the amounts of other research and development expenses, for which invoices have not been received at the end of a period,based upon communication with third parties that have provided services or goods during the period. Such estimates are subject to change as additional informationbecomes available. In–Process Research and Development, Intangible Assets-Technology , and Goodwill. In connection with the acquisitions of Molecular Insight andEXINI, we have established a policy for accounting for intangible assets, under which in-process research and development (“IPR&D”), intangible assets-technology and goodwill are initially measured at fair value and capitalized as intangible assets. Impairment tests for goodwill and IPR&D, which are indefinite-lived intangibles, are performed annually in the fourth quarter, unless impairment indicators require an earlier evaluation. Finite-lived intangible assets, includingintangible assets-technology, are evaluated only when impairment indicators are present. IPR&D will be amortized upon and subject to commercialization of theunderlying candidates and intangible assets-technology is amortized over the relevant estimated useful life. Contingent Consideration Liability. The estimated fair value of the contingent consideration liability, initially measured and recorded on the acquisitiondate, is considered to be a Level 3 instrument and is reviewed quarterly, or whenever events or circumstances occur that indicate a change in fair value. Thecontingent consideration liability is recorded at fair value at the end of each period. Legal Proceedings. From time to time, we may be a party to legal proceedings in the course of our business. The outcome of any such proceedings,regardless of the merits, is inherently uncertain. The assessment of whether a loss is probable or reasonably possible, and whether the loss or a range of loss isestimable, often involves a series of complex judgments about future events. The Company records accruals for contingencies to the extent that the occurrence ofthe contingency is probable and the amount of liability is reasonably estimable. If the reasonable estimate of liability is within a range of amounts and some amountwithin the range appears to be a better estimate than any other, then the Company records that amount as an accrual. If no amount within the range is a reasonableestimate, then the Company records the lowest amount as an accrual. Loss contingencies that are assessed as remote are not reported in the financial statements, orin the notes to the consolidated financial statements. Item 7A. Quantitative and Qualitative Disclosures About Market Risk Our primary investment objective is to preserve principal. Our money market funds have interest rates that are variable and totaled $137.3 million atDecember 31, 2016. As a result, we do not believe that these investment balances have a material exposure to interest-rate risk. The majority of our business is conducted in U.S. dollars. However, we do conduct certain transactions in other currencies, including Euros, BritishPounds, Swiss Francs, and Swedish Krona. Historically, fluctuations in foreign currency exchange rates have not materially affected our consolidated results ofoperations and during the years ended December 31, 2016, 2015, and 2014, our consolidated results of operations were not materially affected by fluctuations inforeign currency exchange rates. Item 8. Financial Statements and Supplementary Data See page F-1, Index to Consolidated Financial Statements. Item 9. Changes in and Disagreements With Accountants on Accounting and Financial Disclosure None. 42Table of Contents Item 9A. Controls and Procedures Evaluation of Disclosure Controls and Procedures We maintain disclosure controls and procedures that are designed to ensure that information required to be disclosed in our Exchange Act reports isrecorded, processed, summarized and reported within the timelines specified in the SEC’s rules and forms, and that such information is accumulated andcommunicated to our management, including our CEO and Chief Financial Officer (“CFO”), as appropriate, to allow timely decisions regarding requireddisclosure. In designing and evaluating the disclosure controls and procedures, management recognized that any controls and procedures, no matter how welldesigned and operated, can only provide reasonable assurance of achieving the desired control objectives, and in reaching a reasonable level of assurance,management necessarily was required to apply its judgment in evaluating the cost-benefit relationship of possible controls and procedures. We have a DisclosureCommittee consisting of members of our senior management which monitors and implements our policy of disclosing material information concerning theCompany in accordance with applicable law. As required by SEC Rule 13a-15(e), we carried out an evaluation, under the supervision and with the participation of our management, including our CEOand CFO, of the effectiveness of the design and operation of our disclosure controls and procedures as of the end of the period covered by this report. Based on theforegoing, our CEO and CFO concluded that our current disclosure controls and procedures, as designed and implemented, were effective at the reasonableassurance level. 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 the Exchange Act Rules 13a-15(f) and 15d-15(f)during our fiscal quarter ended December 31, 2016 that have materially affected, or are reasonably likely to materially affect, our internal control over financialreporting. Management’s Report on Internal Control Over Financial Reporting Internal control over financial reporting is a process designed by, or under the supervision of, our CEO and CFO and effected by our Board, managementand other personnel to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposesin accordance with generally accepted accounting principles. Our management is responsible for establishing and maintaining adequate internal control overfinancial reporting which includes policies and procedures that: ●Pertain to the maintenance of records that in reasonable detail accurately and fairly reflect the transactions and dispositions of assets; ●Provide reasonable assurance that transactions are recorded as necessary to permit preparation of financial statements in accordance with generallyaccepted accounting principles, and that receipts and expenditures are being made only in accordance with authorization of management anddirectors; and ●Provide reasonable assurance regarding prevention or timely detection of unauthorized acquisition, use or disposition of assets that could have amaterial effect on the financial statements. Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Projections of any evaluation ofeffectiveness to future periods are subject to the risk that controls may become inadequate because of changes in conditions, or that the degree of compliance withthe policies or procedures may deteriorate. Management has used the framework set forth in the report entitled Internal Control – Integrated Framework issued by the Committee of SponsoringOrganizations of the Treadway Commission (2013 framework), known as COSO, to evaluate the effectiveness of our internal control over financial reporting.Management has concluded that our internal control over financial reporting was effective as of December 31, 2016. The effectiveness of our internal control over financial reporting has been audited by Ernst & Young LLP, an independent registered public accountingfirm, as of December 31, 2016 as stated in their report which is provided below. 43Table of Contents Report of Independent Registered Public Accounting Firm The Board of Directors and Stockholders of Progenics Pharmaceuticals, Inc. We have audited Progenics Pharmaceuticals, Inc.’s internal control over financial reporting as of December 31, 2016, based on criteria established in InternalControl—Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (2013 framework) (the COSO criteria).Progenics Pharmaceuticals, Inc.’s management is responsible for maintaining effective internal control over financial reporting, and for its assessment of theeffectiveness of internal control over financial reporting included in the accompanying Management’s Report on Internal Control Over Financial Reporting. Ourresponsibility is to express an opinion on the Company’s internal control over financial reporting based on our audit. We conducted our audit in accordance with the standards of the Public Company Accounting Oversight Board (United States). Those standards require that we planand perform the audit to obtain reasonable assurance about whether effective internal control over financial reporting was maintained in all material respects. Ouraudit included obtaining an understanding of internal control over financial reporting, assessing the risk that a material weakness exists, testing and evaluating thedesign and operating effectiveness of internal control based on the assessed risk, and performing such other procedures as we considered necessary in thecircumstances. We believe that our audit provides a reasonable basis for our opinion. A company’s internal control over financial reporting is a process designed to provide reasonable assurance regarding the reliability of financial reporting and thepreparation of financial statements for external purposes in accordance with generally accepted accounting principles. A company’s internal control over financialreporting includes those policies and procedures that (1) pertain to the maintenance of records that, in reasonable detail, accurately and fairly reflect the transactionsand dispositions of the assets of the company; (2) provide reasonable assurance that transactions are recorded as necessary to permit preparation of financialstatements in accordance with generally accepted accounting principles, and that receipts and expenditures of the company are being made only in accordance withauthorizations of management and directors of the company; and (3) provide reasonable assurance regarding prevention or timely detection of unauthorizedacquisition, use, or disposition of the company’s assets that could have a material effect on the financial statements. Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Also, projections of any evaluation ofeffectiveness to future periods are subject to the risk that controls may become inadequate because of changes in conditions, or that the degree of compliance withthe policies or procedures may deteriorate. In our opinion, Progenics Pharmaceuticals, Inc. maintained, in all material respects, effective internal control over financial reporting as of December 31, 2016,based on the COSO criteria . We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), the consolidated balance sheet ofProgenics Pharmaceuticals, Inc. as of December 31, 2016 and 2015 and the related consolidated statements of operation, comprehensive (loss) income,stockholders’ equity, and cash flows for each of the three years in the period ended December 31, 2016 of Progenics Pharmaceuticals, Inc. and our report datedMarch 9, 2017 expressed an unqualified opinion thereon. /s/ Ernst & Young LLP Hartford, ConnecticutMarch 9, 2017 Item 9B. Other Information None. 44Table of Contents PART III The information required by the Form 10-K Items listed in the following table will be included under the respective headings specified for such Items inour definitive proxy statement for our 2017 Annual Meeting of Stockholders to be filed with the SEC no later than 120 days after December 31, 2016, which proxystatement is incorporated herein by reference: Item of Form 10-KLocation in 201 7 Proxy Statement Item 10. Directors, Executive Officers and Corporate GovernanceElection of Directors.Executive and Other Officers.Corporate Governance.Code of Bus iness Ethics and Conduct.*Section 16(a) Beneficial Ownership Reporting and Compliance.* The full text of our Code of Business Ethics and Conduct is available on ourwebsite ( www.progenics.com ). Item 11. Executive CompensationExecutive Compensation .Compensation Committee Report.Compensation Committee Interlocks and Insider Participation. Item 12. Security Ownership of Certain Beneficial Owners and Managementand Related Stockholder MattersEquity Compensation Plan Information.Security Ownership of Certain Beneficial Owners and Management . Item 13. Certain Relationships and Related Transactions, and DirectorIndependenceCertain Relationships and Related Transactions.Affirmative Determinations Regarding Director Independence and OtherMatters. Item 14. Principal Accounting Fees and ServicesFees Billed for Services Rendered by our Independent Registered PublicAccounting Firm.Pre-approval of Audit and Non-Audit Services by the Audit Committee. 45Table of Contents PART IV Item 15. Exhibits, Financial Statement Schedules The following documents or the portions thereof indicated are filed as a part of this Annual Report. (a)Documents filed as part of this Annual Report: (1)Consolidated Financial Statements of Progenics Pharmaceuticals, Inc.: Report of Independent Registered Public Accounting Firm Consolidated Balance Sheets at December 31, 2016 and 2015 Consolidated Statements of Operations for the years ended December 31, 2016, 2015 and 2014 Consolidated Statements of Comprehensive Income (Loss) for the years ended December 31, 2016, 2015 and 2014 Consolidated Statements of Stockholders’ Equity for the years ended December 31, 2016, 2015 and 2014 Consolidated Statements of Cash Flows for the years ended December 31, 2016, 2015 and 2014 Notes to Consolidated Financial Statements (2)Financial Statement Schedules Schedule II – Valuation and Qualifying Accounts Financial statement schedules referred to in Item 12-01 of Regulation S-X and not listed above are inapplicable and therefore have beenomitted. (3)Item 601 Exhibits Exhibits required to be filed by Item 601 of Regulation S-K are listed in the Exhibit Index immediately following the signature page of thisReport and incorporated herein by reference. 46Table of Contents PROGENICS PHARMACEUTICALS, INC.INDEX TO CONSOLIDATED FINANCIAL STATEMENTS PageReport of Independent Registered Public Accounting FirmF-2Financial Statements: Consolidated Balance Sheets at December 31, 2016 and 2015F-3Consolidated Statements of Operations for the years ended December 31, 2016, 2015, and 2014F-4Consolidated Statements of Comprehensive Income (Loss) for the years ended December 31, 2016, 2015, and 2014F-5Consolidated Statements of Stockholders’ Equity for the years ended December 31, 2016, 2015, and 2014F-6Consolidated Statements of Cash Flows for the years ended December 31, 2016, 2015, and 2014F-7Notes to Consolidated Financial StatementsF-8 F-1Table of Contents Report of Independent Registered Public Accounting Firm The Board of Directors and Stockholders of Progenics Pharmaceuticals, Inc. We have audited the accompanying consolidated balance sheets of Progenics Pharmaceuticals, Inc. as of December 31, 2016 and 2015 and the related consolidatedstatements of operations, comprehensive income (loss), stockholders' equity, and cash flows for each of the three years in the period ended December 31, 2016. Ouraudits also included the financial statement schedule listed in the Index at Item 15(a). These financial statements and schedule are the responsibility of theCompany's management. Our responsibility is to express an opinion on these financial statements and schedule 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 weplan and perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. An audit includes examining, ona test basis, evidence supporting the amounts and disclosures in the financial statements. An audit also includes assessing the accounting principles used andsignificant estimates made by management, as well as evaluating the overall financial statement presentation. We believe that our audits provide a reasonable basisfor our opinion. In our opinion, the financial statements referred to above present fairly, in all material respects, the consolidated financial position of Progenics Pharmaceuticals,Inc. at December 31, 2016 and 2015 and the consolidated results of its operations and its cash flows for each of the three years in the period ended December 31,2016, in conformity with U.S. generally accepted accounting principles. Also, in our opinion, the related financial statement schedule, when considered in relationto the basic financial statements taken as a whole, presents fairly in all material respects information set forth therein. We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), Progenics Pharmaceuticals, Inc.'sinternal control over financial reporting as of December 31, 2016, based on criteria established in Internal Control-Integrated Framework issued by the Committeeof Sponsoring Organizations of the Treadway Commission (2013 framework) and our report dated March 9, 2017 expressed an unqualified opinion thereon. /s/ Ernst & Young LLPHartford, ConnecticutMarch 9, 2017 F-2Table of Contents PROGENICS PHARMACEUTICALS, INC. CONSOLIDATED BALANCE SHEETS(In thousands, except per share data) December 31, 2016 2015 ASSETS Current assets: Cash and cash equivalents $138,909 $74,103 Accounts receivable, net 4,864 3,543 Other current assets 4,328 5,639 Total current assets 148,101 83,285 Property and equipment, net 4,760 2,407 Intangible assets, net 30,581 30,793 Goodwill 13,074 13,074 Other assets 2,470 1,692 Total assets $198,986 $131,251 LIABILITIES AND STOCKHOLDERS' EQUITY Current liabilities: Accounts payable $567 $332 Accrued expenses 15,764 9,212 Other current liabilities 26 185 Total current liabilities 16,357 9,729 Contingent consideration liability 14,200 18,800 Deferred tax liability 13,010 11,199 Long-term debt, net 49,453 - Other liabilities 1,204 862 Total liabilities 94,224 40,590 Commitments and Contingencies Stockholders’ equity: Preferred stock, $0.001 par value Authorized - 20,000 shares; issued and outstanding - none - - Common stock, $0.0013 par value Authorized - 160,000 shares; issued - 70,390 shares in 2016 and 70,146shares in 2015 92 91 Additional paid-in capital 598,069 594,511 Treasury stock at cost, 200 shares of common stock (2,741) (2,741)Accumulated other comprehensive loss (85) (26)Accumulated deficit (490,573) (501,379)Total Progenics stockholders' equity 104,762 90,456 Noncontrolling interests - 205 Total stockholders’ equity 104,762 90,661 Total liabilities and stockholders’ equity $198,986 $131,251 The accompanying notes are an integral part of the financial statements. F-3Table of Contents PROGENICS PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF OPERATIONS( In thousands, except per share data) Years Ended December 31, 2016 2015 2014 Revenue: Royalty income $10,295 $6,608 $3,101 License revenue 59,081 1,955 41,196 Other revenue 53 113 80 Total revenue 69,429 8,676 44,377 Operating expenses: Research and development 37,569 28,196 28,592 General and administrative 23,356 18,184 15,489 Intangible impairment charges - - 2,676 Change in contingent consideration liability (4,600) 1,600 1,500 Total operating expenses 56,325 47,980 48,257 Other operating income - - 7,250 Operating income (loss) 13,104 (39,304) 3,370 Other income (expense): Interest (expense) income, net (493) 52 51 Other expense, net (34) - - Total other (expense) income (527) 52 51 Income (loss) before income tax (expense) benefit 12,577 (39,252) 3,421 Income tax (expense) benefit (1,844) 133 989 Net income (loss) 10,733 (39,119) 4,410 Net loss attributable to noncontrolling interests (73) (7) - Net income (loss) attributable to Progenics $10,806 $(39,112) $4,410 Net income (loss) per share attributable to Progenics - basic $0.15 $(0.56) $0.06 Weighted-average shares - basic 70,003 69,716 68,185 Net income (loss) per share attributable to Progenics - diluted $0.15 $(0.56) $0.06 Weighted-average shares - diluted 70,155 69,716 68,243 The accompanying notes are an integral part of the financial statements. F-4Table of Contents PROGENICS PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF COMPREHENSIVE INCOME (LOSS)(In thousands) Years Ended December 31, 2016 2015 2014 Net income (loss) $10,733 $(39,119) $4,410 Other comprehensive (loss) income: Foreign currency translation adjustments (62) (26) - Net change in unrealized loss on auction rate securities - - 192 Total other comprehensive (loss) income (62) (26) 192 Comprehensive income (loss) 10,671 (39,145) 4,602 Comprehensive loss attributable to noncontrolling interests (73) (7) - Comprehensive income (loss) attributable to Progenics $10,744 $(39,138) $4,602 The accompanying notes are an integral part of the financial statements. F-5Table of Contents PROGENICS PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF STOCKHOLDERS’ EQUITY(In thousands) Accumulated Common Stock Additional Other Treasury Stock Total Number Paid-in Accumulated Comprehensive Number Noncontrolling Stockholders’ of Shares ParValue Capital Deficit Loss of Shares Cost Interests Equity Balance at December 31,2013 61,025 $79 $548,510 $(466,677) $(192) (200) $(2,741) $- $78,979 Net income - - - 4,410 - - - - 4,410 Other comprehensiveincome - - - - 192 - - - 192 Stock-basedcompensation expense - - 3,523 - - - - - 3,523 Sale of common stock inpublic offering, net ofunderwriting discountsandcommissions($2,415)and offering expenses($376) 8,750 12 37,447 - - - - - 37,459 Acquisition ofsubsidiary escrow sharesreturned (19) - (82) - - - - - (82)Exercise of stockoptions 77 - 428 - - - - - 428 Balance at December 31,2014 69,833 $91 $589,826 $(462,267) $- (200) $(2,741) $- $124,909 Net loss - - - (39,112) - - - (7) (39,119)Acquisition ofsubsidiary - - - - - - - 504 504 Purchase ofnoncontrolling interests - - - - - - - (292) (292)Other comprehensiveloss - - - - (26) - - - (26)Stock-basedcompensation expense - - 2,948 - - - - - 2,948 Exercise of stockoptions 313 - 1,737 - - - - - 1,737 Balance at December 31,2015 70,146 $91 $594,511 $(501,379) $(26) (200) $(2,741) $205 $90,661 Net income (loss) - - - 10,806 - - - (73) 10,733 Purchase ofnoncontrolling interests - - (239) - - - - (129) (368)Foreign currencytranslation adjustment - - - - (59) - - (3) (62)Stock-basedcompensation expense - - 2,457 - - - - - 2,457 Exercise of stockoptions 244 1 1,340 - - - - - 1,341 Balance at December 31,2016 70,390 $92 $598,069 $(490,573) $(85) (200) $(2,741) $- $104,762 The accompanying notes are an integral part of the financial statements. F-6Table of Contents PROGENICS PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF CASH FLOWS( In thousands) Years Ended December 31, 2016 2015 2014 Cash flows from operating activities: Net income (loss) $10,733 $(39,119) $4,410 Adjustments to reconcile net income (loss) to net cash provided by (used in) operatingactivities: Depreciation and amortization 2,078 565 545 Stock-based compensation expense 2,457 2,948 3,523 Gain on sale of fixed assets (296) (2) (110)Intangible impairment charge - - 2,676 Paid in-kind interest 765 - - Non-cash interest expense 38 - - Deferred income tax 1,811 (133) (989)Change in fair value of contingent consideration liability (4,600) 1,600 1,500 Acqusition of subsidiary escrow shares returned - - (82)Changes in assets and liabilities: Accounts receivable (1,322) (3,415) 2,770 Other current assets 1,314 (3,058) (572)Other assets (778) (1,535) - Accounts payable 243 (202) (435)Accrued expenses 6,581 2,354 493 Deferred tax and other current liabilities (158) (60) - Other liabilities 343 (80) (3)Net cash provided by (used in) operating activities 19,209 (40,137) 13,726 Cash flows from investing activities: Acquisition of subsidiary, net of cash acquired - (6,202) - Purchases of property and equipment (4,286) (370) (714)Proceeds from sale of fixed assets 347 48 143 Proceeds from redemption of auction rate securities - - 2,400 Net cash (used in) provided by investing activities (3,939) (6,524) 1,829 Cash flows from financing activities: Net proceeds from issuance of long-term debt 48,650 - - Net proceeds from public offering of common stock - - 37,459 Proceeds from exercise of stock options 1,340 1,737 428 Purchase of noncontrolling interests (368) (292) - Net cash provided by financing activities 49,622 1,445 37,887 Effect of currency rate changes on cash and cash equivalents (86) 17 - Net increase (decrease) in cash and cash equivalents 64,806 (45,199) 53,442 Cash and cash equivalents at beginning of period 74,103 119,302 65,860 Cash and cash equivalents at end of period $138,909 $74,103 $119,302 The accompanying notes are an integral part of the financial statements. F-7Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) 1. Organization and Business Business Progenics Pharmaceuticals, Inc. and its subsidiaries (“the Company,” “Progenics,” “we” or “us”) develop innovative medicines and other technologies totarget and treat cancer. Our pipeline includes: 1) therapeutic agents designed to precisely target cancer (AZEDRA and 1095), 2) PSMA-targeted imaging agentsfor prostate cancer (1404 and PyL ), and 3) imaging analysis tools. In February 2011, we licensed our first commercial drug, RELISTOR (methylnaltrexone bromide) subcutaneous injection for the treatment of opioidinduced constipation (“OIC”), to Salix Pharmaceuticals, Inc. (a wholly-owned subsidiary of Valeant Pharmaceuticals International, Inc. (“Valeant”)). In September2014 RELISTOR received an expanded approval from the U.S. Food and Drug Administration ("FDA") for the treatment of OIC in patients taking opioids forchronic non-cancer pain. On July 19, 2016, the FDA approved RELISTOR Tablets for the treatment of OIC in adults with chronic non-cancer pain, for which wereceived a $50.0 million development milestone payment from Valeant in the third quarter of 2016. We have partnered other internally-developed or acquiredcompounds and technologies with third parties. We continue to consider opportunities for strategic collaborations, out-licenses and other arrangements withbiopharmaceutical companies involving proprietary research, development and clinical programs, and may in the future also in-license or acquire additionaloncology compounds and/or programs. Our current principal sources of revenue from operations are royalty, development and commercial milestones, and sublicense revenue-sharing paymentsfrom Valeant relating to RELISTOR. Royalty and further milestone payments from RELISTOR depend on success in development and commercialization, whichis dependent on many factors, such as Valeant’s efforts, decisions by the FDA and other regulatory bodies, competition from drugs for the same or similarindications, and the outcome of clinical and other testing of RELISTOR. We commenced principal operations in 1988, became publicly traded in 1997, and throughout have been engaged primarily in research and developmentefforts, establishing corporate collaborations and related activities. Certain of our intellectual property rights are held by wholly owned subsidiaries. All of our U.S.operations are presently conducted at our headquarters in New York, and EXINI’s operations are conducted at our facility in Lund, Sweden. We operate under asingle research and development segment. Liquidity At December 31, 2016, we had $138.9 million in cash and cash equivalents, an increase of $64.8 million from $74.1 million at December 31, 2015. Weexpect that this amount will be sufficient to fund operations as currently anticipated beyond one year from the filing date of this Form 10-K. We have historicallyfunded our operations to a significant extent from capital-raising and we expect to require additional funding in the future, the availability of which is neverguaranteed and may be uncertain. During 2014, we raised $37.5 million in an underwritten public offering of 8.75 million shares of common stock at a publicoffering price of $4.60 per share. During 2016, we raised net proceeds of $48.7 million through a royalty monetization transaction (See Note 9. Long-Term Debt,Net for additional information). We expect that we may continue to incur operating losses for the foreseeable future. 2. Summary of Significant Accounting Policies Basis of Presentation The consolidated financial statements have been prepared on the basis of accounting principles generally accepted in the U.S. (“GAAP”). The preparationof financial statements in conformity with GAAP requires management to make estimates and assumptions that affect the amounts reported in the financialstatements and the accompanying notes. On an ongoing basis, we evaluate our estimates, including but not limited to those related to collectability of receivables,intangible assets and contingencies. As additional information becomes available or actual amounts become determinable, the recorded estimates are revised andreflected in the operating results. Actual results could differ from those estimates. Certain expense amounts have been combined in prior periods’ financialstatements to conform to the current year presentation. F-8® TM ® Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Principles of Consolidation The condensed consolidated financial statements include the accounts of Progenics as well as its wholly-owned and controlled subsidiaries. All materialintercompany transactions and balances have been eliminated in consolidation. Foreign Currency Translation Each of our international subsidiaries generally considers their respective local currency to be their functional currency. Assets and liabilities of theseinternational subsidiaries are translated into U.S. dollars at quarter-end exchange rates and revenues and expenses are translated at average exchange rates duringthe quarter and year-to-date period. Foreign currency translation adjustments for the reported periods are included in accumulated other comprehensive loss(“AOCL”) in our condensed consolidated statements of comprehensive income (loss), and the cumulative effect is included in the stockholders' equity section ofour condensed consolidated balance sheets. Realized gains and losses denominated in foreign currencies are recorded in operating expenses in our condensedconsolidated statements of operations and were not material to our consolidated results of operations for the three years ended December 31, 2016. Use of Estimates The preparation of consolidated financial statements in conformity with GAAP requires management to make estimates and assumptions that affect theamounts reported in the consolidated financial statements and accompanying notes. Actual results may differ from those estimates. Revenue Recognition We recognize revenue from all sources based on the provisions of the U.S. Securities and Exchange Commission (“SEC”) Staff Accounting Bulletin(“SAB”) No. 104 (“SAB 104”) and the Financial Accounting Standards Board (“FASB”) Accounting Standards Codification (“ASC”) 605 (Topic 605, RevenueRecognition ). Under ASC 605, delivered items are separate units of accounting, provided (i) the delivered items have value to a collaborator on a stand-alone basis,and (ii) if the arrangement includes a general right of return relative to the delivered item, delivery or performance of the undelivered items is considered probableand substantially in our control. A separate update to ASC 605 provides guidance on the criteria that should be met when determining whether the milestonemethod of revenue recognition is appropriate. If we are involved in a steering or other committee as part of a multiple-deliverable arrangement, we assess whether our involvement constitutes aperformance obligation or a right to participate. For those committees that are deemed obligations, we will evaluate our participation along with other obligations inthe arrangement and will attribute revenue to our participation through the period of our committee responsibilities. We recognize revenue for payments that arecontingent upon performance solely by our collaborator immediately upon the achievement of the defined event if we have no related performance obligations.Reimbursement of costs is recognized as revenue provided the provisions of ASC 605 are met, the amounts are determinable and collection of the relatedreceivable is reasonably assured. Amounts received prior to satisfying the above revenue recognition criteria are recorded as deferred revenue. Amounts not expected to be recognizedwithin one year of the balance sheet date are classified as long-term. Royalty revenue is recognized in the period the sales occur, provided the royalty amounts are fixed or determinable, collection of the related receivable isreasonably assured and we have no remaining performance obligations under the arrangement providing for the royalty. Royalty loss is recognized based uponreported sales deductions in excess of gross sales resulting in net sales (losses) and is recognized in the period net sales (losses) occur. Royalty loss is classified inroyalty income in the consolidated statements of operations and the related accrued royalty loss liability is classified in accounts payable and accrued expenses inthe consolidated balance sheets. During the past three years, we also recognized revenue from sales of research reagents. F-9Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Under the agreement with Bayer, we are entitled to receive an upfront payment of $4.0 million and up to $49.0 million in potential clinical and regulatorydevelopment milestones. We are also entitled to single digit royalties on net sales, and potential net sales milestone payments up to an aggregate total of $130.0million. In 2016, we recognized license revenue of $7.0 million, of which $4.0 million related to the upfront payment and $3.0 million related to the achievement ofa preclinical development milestones. During 2015, we recognized $1.5 million milestone revenue under our agreement with CytoDyn Inc. as a result of CytoDyn’s dosing of the first patient inits Phase 3 clinical trial of PRO 140. We are eligible for future milestone and royalty payments. During 2014, we recognized $40.0 million milestone revenue from Valeant upon U.S. marketing approval for subcutaneous RELISTOR in non-cancerpain patients and $1.0 million milestone revenue from FUJIFILM RI Pharma Co., Ltd. (“Fuji”) upon execution of the first contract by Fuji with an investigationsite for a Phase 1 trial of 1404 in Japan. In 2014, Valeant entered into an agreement with Lupin Limited for distribution of RELISTOR in Canada. During the second quarter of 2016, werecognized license revenue of $720 thousand for our share of the upfront payment Valeant received from Lupin pursuant to the distribution agreement. Research and Development Expenses Research and development expenses include costs directly attributable to the conduct of research and development programs, including the cost ofsalaries, payroll taxes, employee benefits, materials, supplies, maintenance of research equipment, costs related to research collaboration and licensing agreements,the purchase of in-process research and development, the cost of services provided by outside contractors, including services related to our clinical trials, the fullcost of manufacturing drug for use in research, pre-clinical development and clinical trials. All costs associated with research and development are expensed asincurred. At each period end, we evaluate the accrued expense balance related to these activities based upon information received from the suppliers and estimatedprogress towards completion of the research or development objectives to ensure that the balance is reasonably stated. Such estimates are subject to change asadditional information becomes available. Patents As a result of research and development efforts conducted by us, we have applied, or are applying, for a number of patents to protect proprietaryinventions. All costs associated with patents are expensed as incurred. Net Income (Loss) Per Share We prepare earnings per share (EPS) data in accordance with ASC 260 (Topic 260, Earnings Per Share ). Basic net income (loss) per share amounts havebeen computed by dividing net income (loss) attributable to Progenics by the weighted-average number of common shares outstanding during the period. For 2015,we reported net losses and, therefore, potential common shares, amounts of unrecognized compensation expense and windfall tax benefits have been excluded fromdiluted net loss per share since they would be anti-dilutive. For 2016 and 2014, we reported net income, and the computation of diluted earnings per share is basedupon the weighted-average number of our common shares and dilutive effect, determined using the treasury stock method, of potential common shares outstandingincluding amounts of unrecognized compensation expense. Shares to be issued upon the assumed conversion of the contingent consideration liability are excludedfrom the diluted earnings per share calculation, if performance conditions have not been met. Concentrations of Credit Risk Financial instruments which potentially subject Progenics to concentrations of risk consist principally of cash, cash equivalents and receivables. We investour excess cash in money market funds, which are classified as cash and cash equivalents. We have established guidelines that relate to credit quality,diversification and maturity and that limit exposure to any one issue of securities. We hold no collateral for these financial instruments. F-10Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Cash and Cash Equivalents We consider all highly liquid investments which have maturities of three months or less, when acquired, to be cash equivalents. The carrying amountreported in the balance sheet for cash and cash equivalents approximates its fair value. Cash and cash equivalents subject us to concentrations of credit risk. AtDecember 31, 2016 and 2015, we had invested approximately $137.3 million and $68.1 million, respectively, in cash equivalents in the form of money marketfunds with one major investment company and held approximately $1.6 million and $6.0 million, respectively, in three commercial banks. Accounts Receivable We estimate the level of accounts receivable which ultimately will be uncollectable based on a review of specific receivable balances, industry experienceand the current economic environment. We reserve for affected accounts receivable an allowance for doubtful accounts, which at December 31, 2015 and 2014 was$10 thousand. During 2016, we wrote-off the uncollectable accounts receivable balance of $10 thousand against the allowance for doubtful accounts. At December31, 2016, we had no allowance for doubtful accounts. In-Process Research and Development, Other Identified Intangible Assets and Goodwill The fair values of in-process research and development (“IPR&D”) and other identified intangible assets acquired in business combinations arecapitalized. The Company utilizes the “income method”, which applies a probability weighting that considers the risk of development and commercialization to theestimated future net cash flows that are derived from projected sales revenues and estimated costs or “replacement costs”, whichever is greater. These projectionsare based on factors such as relevant market size, patent protection, historical pricing of similar products and expected industry trends. The estimated future netcash flows are then discounted to the present value using an appropriate discount rate. This analysis is performed for each IPR&D project and other identifiedintangible assets independently. IPR&D assets are treated as indefinite-lived intangible assets until completion or abandonment of the projects, at which time theassets are amortized over the remaining useful life or written off, as appropriate. Other identified intangible assets are amortized over the relevant estimated usefullife. The IPR&D assets are tested at least annually or when a triggering event occurs that could indicate a potential impairment and any impairment loss isrecognized in our consolidated statements of operations. Goodwill represents excess consideration in a business combination over the fair value of identifiable net assets acquired. Goodwill is not amortized, butis subject to impairment testing at least annually or when a triggering event occurs that could indicate a potential impairment. The Company determines whethergoodwill may be impaired by comparing the fair value of the reporting unit (the Company has determined that it has only one reporting unit for this purpose),calculated as the product of shares outstanding and the share price as of the end of a period, to its carrying value (for this purpose, the Company’s totalstockholders’ equity). No goodwill impairment has been recognized as of December 31, 2016 or 2015. Fair Value Measurements In accordance with ASC 820 (Topic 820, Fair Value Measurements and Disclosures ), we use a three-level hierarchy for fair value measurements ofcertain assets and liabilities for financial reporting purposes that distinguishes between market participant assumptions developed from market data obtained fromoutside sources (observable inputs) and our own assumptions about market participant assumptions developed from the best information available to us in thecircumstances (unobservable inputs). We assign hierarchy levels to our contingent consideration liability arising from the Molecular Insight Pharmaceuticals, Inc.(“Molecular Insight”) acquisition based on our assessment of the transparency and reliability of the inputs used in the valuation. ASC 820 defines the threehierarchy levels as: ●Level 1 - Valuations based on unadjusted quoted market prices in active markets for identical securities. ●Level 2 - Valuations based on observable inputs other than Level 1 prices, such as quoted prices for similar assets at the measurement date, quoted pricesin markets that are not active or other inputs that are observable, either directly or indirectly. ●Level 3 - Valuations based on unobservable inputs that are significant to the overall fair value measurement, which as noted above involve managementjudgment. F-11Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Recurring Fair Value Measurements We believe the carrying amounts of our cash equivalents, accounts receivable, other current assets, other assets, accounts payable, and accrued expensesapproximated their fair values as of December 31, 2016 and 2015. The fair value of the contingent consideration liability represents future potential milestone payments related to the Molecular Insight acquisition. The fairvalue of the contingent consideration liability is categorized as a Level 3 instrument, as displayed in Note 4. We record the contingent consideration liability at fairvalue with changes in estimated fair values recorded in the consolidated statements of operations. We reassess the fair value of the contingent consideration at eachreporting period. The contingent consideration liability results from probability adjusted discounted cash flows and Monte Carlo simulation models which includeestimates of milestone payments to former Molecular Insight stockholders under the acquisition agreement. Nonrecurring Fair Value Measurements Our non-financial assets, such as intangible assets and property and equipment, are measured and recorded at fair value on the acquisition date, and ifindicators of impairment exist, we assess recoverability by measuring the amount of any impairment by comparing the carrying value of the asset to its then-currentestimated fair value (for intangible assets) or to market prices for similar assets (for property and equipment). If the carrying value is not recoverable we record animpairment charge in our consolidated statements of operations. No impairments occurred for the year ended December 31, 2016. We reassessed the value of theindefinite lived intangible assets and recorded a non-cash charge to earnings of $2.7 million in 2014. This impairment was the result of changes in the Level 3assumptions as follows: the timing of beginning cash inflows from 2021 to 2024 and a decrease in discount rate from 20% to 13.5% for the 1095 intangible asset,in addition to the third quarter 2014 impairments of the ONALTA indefinite-lived and finite-lived intangible assets, resulting from decreased probabilities ofsuccess. Other current assets are comprised of prepaid expenses, interest, amount held in escrow for former employee litigation, which is restricted, and otherreceivables of $4.3 million and $5.6 million at December 31, 2016 and 2015, respectively, which are expected to be settled within one year. Restricted cash,included in other assets, of $2.0 million and $1.7 million at December 31, 2016 and 2015, respectively, represents collateral for letters of credit securing leaseobligations and advanced title to remaining shares held by noncontrolling interests. We believe the carrying value of these assets approximates fair value and areconsidered Level 1 assets. Fixed Assets Leasehold improvements, furniture and fixtures, and equipment are stated at cost. Furniture, fixtures and equipment are depreciated on a straight-line basisover their estimated useful lives. Leasehold improvements are amortized on a straight-line basis over the life of the lease or of the improvement, whichever isshorter. Costs of construction of long-lived assets are capitalized but are not depreciated until the assets are placed in service. Expenditures for maintenance and repairs which do not materially extend the useful lives of the assets are charged to expense as incurred. The cost andaccumulated depreciation of assets retired or sold are removed from the respective accounts and any gain or loss is recognized in operations. The estimated usefullives of fixed assets are as follows: Computer equipment (years) 3 Machinery and equipment (years) 5-7 Furniture and fixtures (years) 5 Leasehold improvements Earlier of life ofimprovement or lease F-12TM Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Deferred L ease L iability and Incentive Our lease agreements include fixed escalations of minimum annual lease payments and we recognize rental expense on a straight-line basis over the leaseterms and record the difference between rent expense and current rental payments as deferred lease liability. Deferred lease incentive includes a constructionallowance from our landlord which is amortized as a reduction to rental expense on a straight-line basis over the lease term. As of December 31, 2016 and 2015,our consolidated balance sheets include the following: 2016 2015 Other current liabilities: Deferred lease incentive $26 $115 Other liabilities: Deferred lease liability $876 $402 Deferred lease incentive $328 $460 Income Taxes We account for income taxes in accordance with the provisions of ASC 740 (Topic 740, Income Taxes ), which requires that we recognize deferred taxliabilities and assets for the expected future tax consequences of events that have been included in the financial statements or tax returns. Under this method,deferred tax assets and liabilities are determined on the basis of the difference between the tax basis of assets and liabilities and their respective financial reportingamounts (temporary differences) at enacted tax rates in effect for the years in which the temporary differences are expected to reverse. A valuation allowance isestablished for deferred tax assets for which realization is uncertain. In accordance with ASC 718 (Topic 718, Compensation – Stock Compensation ) and ASC 505 (Topic 505, Equity ), we have made a policy decisionrelated to intra-period tax allocation, to account for utilization of windfall tax benefits based on provisions in the tax law that identify the sequence in whichamounts of tax benefits are used for tax purposes (i.e., tax law ordering). Uncertain tax positions are accounted for in accordance with ASC 740, which prescribes a comprehensive model for the manner in which a companyshould recognize, measure, present and disclose in its financial statements all material uncertain tax positions that we have taken or expect to take on a tax return.ASC 740 applies to income taxes and is not intended to be applied by analogy to other taxes, such as sales taxes, value-add taxes, or property taxes. We review ournexus in various tax jurisdictions and our tax positions related to all open tax years for events that could change the status of our ASC 740 liability, if any, orrequire an additional liability to be recorded. Such events may be the resolution of issues raised by a taxing authority, expiration of the statute of limitations for aprior open tax year or new transactions for which a tax position may be deemed to be uncertain. Those positions, for which management's assessment is that there ismore than a 50% probability of sustaining the position upon challenge by a taxing authority based upon its technical merits, are subjected to the measurementcriteria of ASC 740. We record the largest amount of tax benefit that is greater than 50% likely of being realized upon ultimate settlement with a taxing authorityhaving full knowledge of all relevant information. Any ASC 740 liabilities for which we expect to make cash payments within the next twelve months areclassified as "short term." In the event that we conclude that we are subject to interest and/or penalties arising from uncertain tax positions, we will record interestand penalties as a component of income taxes (see Note 13. Income Taxes for additional information). Risks and Uncertainties We have to date relied principally on external funding, license agreements with Valeant, Bayer and others, out-licensing and asset sale arrangements,royalty and product revenue to finance our operations. There can be no assurance that our research and development will be successfully completed, that anyproducts developed will obtain necessary marketing approval by regulatory authorities or that any approved products will be commercially viable. In addition, weoperate in an environment of rapid change in technology, and we are dependent upon satisfactory relationships with our partners and the continued services of ourcurrent employees, consultants and subcontractors. We are also dependent upon Valeant and Fuji fulfilling their manufacturing obligations, either on their own orthrough third-party suppliers. For 2016, 2015, and 2014, the primary sources of our revenues were royalty and milestone payments. There can be no assurance thatsuch revenues will continue. Substantially all of our accounts receivable at December 31, 2016 and 2015 were from the above-named sources. F-13Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Comprehensive Income (Loss) Comprehensive income (loss) represents the change in net assets of a business enterprise during a period from transactions and other events andcircumstances from non-owner sources. Our comprehensive income (loss) includes net income (loss) adjusted for the changes in foreign currency translationadjustment and net change in unrealized loss on auction rate securities. The disclosures required by ASC 220 (Topic 220, Comprehensive Income ) for 2016, 2015,and 2014 have been included in the consolidated statements of comprehensive income (loss). There was no income tax expense/benefit allocated to any componentof other comprehensive income (loss) (see Note 10. Stockholders’ Equity for additional information). Legal Proceedings From time to time, we may be a party to legal proceedings in the course of our business. The outcome of any such proceedings, regardless of the merits, isinherently uncertain. The assessment of whether a loss is probable or reasonably possible, and whether the loss or a range of loss is estimable, often involves aseries of complex judgments about future events. The Company records accruals for contingencies to the extent that the occurrence of the contingency is probableand the amount of liability is reasonably estimable. If the reasonable estimate of liability is within a range of amounts and some amount within the range appears tobe a better estimate than any other, then the Company records that amount as an accrual. If no amount within the range is a reasonable estimate, then the Companyrecords the lowest amount within the range as an accrual. Loss contingencies that are assessed as remote are not reported in the financial statements, or in the notesto the consolidated financial statements. Impact of Recently Issued and Adopted Accounting Standards Recently Adopted In September 2015, the FASB issued ASU No. 2015-16 (“ASU 2015-16”), Business Combinations (Topic 805): Simplifying the Accounting forMeasurement-Period Adjustments . The standard requires the acquirer in a business combination to recognize in the reporting period in which adjustment amountsare determined any adjustments to provisional amounts that are identified during the measurement period, calculated as if the accounting had been completed at theacquisition date. We adopted this standard during the quarter ended March 31, 2016. The adoption had no impact on our consolidated results of operations,financial condition, or cash flows as presented. However, the future impact of ASU 2015-16 will be dependent on future acquisitions, if any. In August 2014, the FASB issued ASU No. 2014-15, Disclosure of Uncertainties about an Entity’s Ability to Continue as a Going Concern . This ASUexplicitly requires management to assess an entity’s ability to continue as a going concern, and to provide related footnote disclosure in certain circumstances. Weadopted this standard as of December 31, 2016. The adoption of this ASU had no material impact on our consolidated financial statements and consolidated notesto these statements. Not Yet Adopted In January 2017, the FASB issued ASU 2017-04 (“ASU 2017-04”), Intangibles - Goodwill and Other (Topic 350): Simplifying the Test for GoodwillImpairment . The update simplifies how an entity is required to test goodwill for impairment by eliminating Step 2 from the goodwill impairment test. Step 2measures a goodwill impairment loss by comparing the implied fair value of a reporting unit’s goodwill with the carrying amount. ASU 2017-04 will be effectivefor the annual or any interim goodwill impairment tests in fiscal years beginning after December 15, 2019. Early adoption is permitted for interim or annualgoodwill impairment tests performed on testing dates after January 1, 2017. We do not expect the adoption of the new standard to have a material impact on ourconsolidated financial statements. In November 2016, the FASB issued ASU No. 2016-18 (“ASU 2016-18”), Statement of Cash Flows (Topic 230) – Restricted Cash. For entities that haverestricted cash and are required to present a statement of cash flows, ASU 2016-18 changes the cash flow presentation for restricted cash. ASU 2016-18 will beeffective for annual reporting periods beginning after December 15, 2017, and interim periods within those annual periods. We do not expect the adoption of thisnew standard to have a material impact on our consolidated financial statements or statement of cash flows. F-14Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) In August 2016, the FASB issued ASU No. 2016-15 (“ASU 2016-15”), Statement of Cash Flows (Topic 230): Classification of Certain Cash Receipts andCash Payments . The standard provides guidance on eight (8) cash flow issues: (1) debt prepayment or debt extinguishment costs; (2) settlement of zero-couponbonds; (3) contingent consideration payments after a business combination; (4) proceeds from the settlement of insurance claims; (5) proceeds from the settlementof corporate-owned life insurance policies; (6) distributions received from equity method investees; (7) beneficial interests in securitization transactions; and (8)separately identifiable cash flows and application of the predominance principle. ASU 2016-15 addresses how certain cash receipts and cash payments arepresented and classified in the statement of cash flows. ASU 2016-15 is effective for fiscal years, and interim periods within those years, beginning after December15, 2017 with early adoption permitted. We do not expect the adoption of this new standard to have a material impact on our consolidated financial statements. In March 2016, the FASB issued ASU No. 2016-09, Compensation – Stock Compensation (Topic 718) ("ASU 2016-09"). The standard simplifies severalaspects of accounting for stock-based payment transactions, including the accounting for income taxes, forfeitures, statutory tax withholding requirements, as wellas classification in the statement of cash flows. ASU 2016-09 is effective for reporting periods beginning after December 15, 2016; however, early adoption ispermitted. We are currently evaluating the impact of this new standard on our consolidated financial statements. In February 2016, the FASB issued ASU No. 2016-02, Leases (Topic 842) ("ASU 2016-02") . The standard requires lessees to recognize leases on theirbalance sheets, and leaves lessor accounting largely unchanged. Additionally, ASU 2016-02 requires a modified retrospective approach for all leases existing at, orentered into after, the date of initial application, with an option to elect to use certain transition relief. ASU 2016-02 is effective for fiscal years, and interim periodswithin those fiscal years, beginning after December 15, 2018. Early application is permitted for all entities. We are currently evaluating the impact of this newstandard on our consolidated financial statements. In January 2016, the FASB issued ASU No. 2016-01, Recognition and Measurement of Financial Assets and Financial Liabilities ("ASU 2016-01"). Thestandard requires equity investments (except those accounted for under the equity method of accounting or those that result in consolidation of the investee) to bemeasured at fair value with changes in fair value recognized in net income, and separate presentation of financial assets and financial liabilities by measurementcategory and form of financial asset. Additionally, ASU 2016-01 eliminates the requirement to disclose the methods and significant assumptions used to estimatethe fair value that is required to be disclosed for financial instruments on the balance sheet. ASU 2016-01 is effective for fiscal years, and interim periods withinthose fiscal years, beginning after December 15, 2017. Other than an amendment relating to presenting in comprehensive income the portion of the total change inthe fair value of a liability resulting from a change in instrument-specific credit risk (if the entity has elected to measure the liability at fair value), early adoption isnot permitted. We are currently evaluating the impact of this standard on our consolidated financial statements. In May 2014, the FASB issued ASU No. 2014-09, Revenue from Contracts with Customers (Topic 606) ("ASU 2014-09"). The standard provides a singlemodel for revenue arising from contracts with customers and supersedes current revenue recognition guidance. This ASU provides that an entity should recognizerevenue to depict transfers of promised goods or services to customers in amounts reflecting the consideration to which the entity expects to be entitled in thetransaction by: (1) identifying the contract; (2) identifying the contract's performance obligations; (3) determining the transaction price; (4) allocating thetransaction price to the performance obligations; and (5) recognizing revenue when or as the entity satisfies the performance obligations. The guidance permitscompanies to apply the requirements either retrospectively to all prior periods presented or in the year of adoption through a cumulative adjustment. ASU 2014-09is effective for fiscal years, and interim periods within those fiscal years, beginning after December 15, 2017. Early adoption is permitted for annual reportingperiods beginning after December 15, 2016 and interim periods therein. In 2016, the FASB issued several amendments to the standard, including principal versusagent considerations when another party is involved in providing goods or services to a customer and the process of identifying performance obligations. We are inthe process of evaluating our significant revenue contracts and the review of our current accounting policies and practices to identify potential differences thatwould result from applying the requirements of the new standard to our revenue contracts and the impact it may have on our consolidated financial statements anddisclosures. In addition, we are in the process of identifying the appropriate changes to business processes, systems, and controls to support recognition anddisclosure under the new standard. We expect to adopt the new revenue standard in the first quarter of 2018 applying the modified retrospective transition method. F-15Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) 3. Acquisitions, Goodwill, and Acquired Intangible Assets Acquisition of EXINI Diagnostics AB On November 12, 2015, we acquired 92.45% of the outstanding shares of EXINI, a Lund, Sweden based leader in the development of advanced imaginganalysis tools and solutions for medical decision support. EXINI's operations are included in our consolidated financial statements beginning November 12, 2015,the date we acquired control. Through the end of the extended acceptance period of November 27, 2015, we acquired additional outstanding shares, bringing ourownership to 96.81%. We commenced a judicial process in Sweden for acquiring the remaining shares and EXINI was delisted and ceased to be publicly tradedeffective as of the close of trading on December 4, 2015. On December 8, 2016, a Swedish arbitral tribunal awarded us advanced title to the remaining shares ofEXINI and, as of that date, EXINI became a wholly-owned subsidiary with 100% of the voting shares owned by us. Goodwill and Acquired Intangible Assets In connection with the 2015 acquisition of EXINI and the 2013 acquisition of Molecular Insight, intangible assets and goodwill were initially measured atthe acquisition date at estimated fair value and capitalized. Third and fourth quarter 2014 reviews of our intangible assets resulted in $2.7 million impairments of the indefinite-lived balance and a $16 thousandimpairment of the finite-lived balance, with the corresponding impairment charges recorded in our consolidated statements of operations. The following table summarizes the activity related to goodwill and intangible assets: Other Intangible Goodwill IPR&D Assets Balance at January 1, 2015 $7,702 $28,700 $- Increase related to EXINI acquisition 5,372 - 2,120 Amortization expense - - (27)Impairment - - - Balance at December 31, 2015 13,074 28,700 2,093 Amortization expense - - (212)Balance at December 31, 2016 $13,074 $28,700 $1,881 The following table reflects the components of the finite-lived intangible assets as of December 31, 2016: Gross Amount AccumulatedAmortization Net CarryingValue Finite lived intangible assets $2,120 $239 $1,881 Total $2,120 $239 $1,881 The weighted-average remaining life of the finite-lived intangible assets was approximately nine years at December 31, 2016. Amortization expense was calculated on a straight-line basis over the estimated useful life of the asset and was $212 thousand and $27 thousand for theyear ended December 31, 2016 and 2015, respectively. Assuming no changes in the gross carrying amount of finite lived intangible assets, the future annualamortization expense related to finite lived intangible assets is expected to be $212 thousand in each of the next five years (2017 through 2021) . F-16Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) 4. Fair Value Measurements We record the contingent consideration liability resulting from the Molecular Insight acquisition at fair value in accordance with ASC 820-10-50. The following tables present our money market funds, included in cash and cash equivalents, and contingent consideration liability measured at fair valueon a recurring basis as of the dates indicated, classified by valuation hierarchy: Fair Value Measurements at December 31, 2016 Quoted Prices in Significant Other Significant Balance at Active Marketsfor Observable Unobservable December 31, Identical Assets Inputs Inputs 2016 (Level 1) (Level 2) (Level 3) Assets: Money market funds $137,340 $137,340 $- $- Total assets $137,340 $137,340 $- $- Liabilities: Contingent consideration liability $14,200 $- $- $14,200 Total liabilities $14,200 $- $- $14,200 Fair Value Measurements at December 31, 2015 Quoted Prices in Significant Other Significant Balance at Active Marketsfor Observable Unobservable December 31, Identical Assets Inputs Inputs 2015 (Level 1) (Level 2) (Level 3) Assets: Money market funds $68,140 $68,140 $- $- Total assets $68,140 $68,140 $- $- Liabilities: Contingent consideration liability $18,800 $- $- $18,800 Total liabilities $18,800 $- $- $18,800 Under the terms of the terms of the acquisition agreement, we agreed to pay to the former stockholders potential milestones, in cash or our common stockat our option, of up to $23.0 million contingent upon achieving specified commercialization events and up to $70.0 million contingent upon achieving specifiedsales targets relating to Molecular Insight’s products. We consider this contingent liability a Level 3 instrument (one with significant unobservable inputs) in thefair value hierarchy. The estimated fair value of the contingent consideration liability of $14.2 million as of December 31, 2016, represents future potentialmilestone payments to former Molecular Insight stockholders. The estimated fair value was determined based on probability adjusted discounted cash flow andMonte Carlo simulation models that included significant estimates and assumptions pertaining to commercialization events and sales targets. The most significantunobservable inputs were the probabilities of achieving regulatory approval of the development projects and subsequent commercial success, and discount rates. Significant changes in any of the probabilities of success would result in a significantly higher or lower fair value measurement. Significant changes in theprobabilities as to the periods in which milestones will be achieved would result in a significantly lower or higher fair value measurement. We record thecontingent consideration liability at fair value with changes in estimated fair values recorded in change in contingent consideration liability in our consolidatedstatements of operations. F-17Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) The following tables present quantitative information pertaining to the December 31, 2016 and 2015 fair value measurements of the Level 3 inputs. The2016 decrease in the contingent consideration liability of $4.6 million resulted primarily from a decrease in the projected sales and an increase in the discount rateused to calculate the present value of the potential sales-based milestone payments to former Molecular Insight stockholders under the acquisition agreement. Fair Value at December 31, Range 2016 Valuation Technique Unobservable Input (Weighted-Average) Contingent ConsiderationLiability: AZEDRA commercialization $3,800 Probability adjusted Probability of success 54% discounted cash flow model Period of expected milestone achievement 2018 Discount rate 10% 1404 commercialization 4,700 Probability adjusted Probability of success 59% discounted cash flow model Period of expected milestone achievement 2019 Discount rate 10% 1095 commercialization 400 Probability adjusted Probability of success 16% discounted cash flow model Period of expected milestone achievement 2024 Discount rate 10% Net sales targets 5,300 Monte-Carlo simulation Probability of success 16%-59% Discount rate 10% Total $14,200 Fair Value at December 31, Range 2015 Valuation Technique Unobservable Input (Weighted-Average) Contingent ConsiderationLiability: AZEDRA commercialization $2,500 Probability adjusted Probability of success 40% discounted cash flow model Period of expected milestone achievement Discount rate 10% 1404 commercialization 4,200 Probability adjusted Probability of success 59% discounted cash flow model Period of expected milestone achievement 2019 Discount rate 10% 1095 commercialization 500 Probability adjusted Probability of success 19% discounted cash flow model Period of expected milestone achievement 2023 Discount rate 10% Net sales targets 11,600 Monte-Carlo simulation Probability of success 19%-59%(37%) Discount rate 12%/4% Total $18,800 (1) The contingent consideration liability related to the net sales targets was derived from a model under a risk neutral framework resulting in the application of 12% and 4% discount rates toestimated cash flows. For those financial instruments with significant Level 3 inputs, the following table summarizes the activities for the periods indicated: Liability - Contingent Consideration Fair Value Measurements Using Significant Unobservable Inputs (Level 3) 2016 2015 Balance at beginning of period $18,800 $17,200 Fair value change included in net income (loss) (4,600) 1,600 Balance at end of period $14,200 $18,800 Changes in unrealized gains or losses for the period included in earnings (orchanges in net assets) for liabilities held at the end of the reporting period $(4,600) $1,600 F-18(1)Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) 5 . Accounts Receivable Our accounts receivable represent amounts due to us from collaborators, royalties, and sales of research reagents, and consisted of the following atDecember 31, 2016 and 2015: 2016 2015 Royalties $2,407 $3,463 Collaborators 2,000 63 Other 457 27 Accounts receivable, gross 4,864 3,553 Less - Allowance for doubtful accounts - (10)Accounts receivable, net $4,864 $3,543 6. Fixed Assets Fixed assets as of December 31, 2016 and 2015 consisted of the following: 2016 2015 Machinery and equipment $1,493 $5,706 Leasehold improvements 1,640 5,027 Computer equipment 695 1,727 Furniture and fixtures 877 131 Construction in progress 893 87 Property and equipment, gross 5,598 12,678 Less - accumulated depreciation (838) (10,271)Property and equipment, net $4,760 $2,407 At December 31, 2016 and 2015, $1.6 million and $1.5 million, respectively, of net leasehold improvements, were being amortized over periods of 13.8years and 6.4 – 10.8 years, under leases with terms through September 30, 2030 and December 31, 2020, respectively. We recorded depreciation expense of $1.9million, $0.5 million, and $0.5 million during 2016, 2015, and 2014, respectively. 7. Accrued Expenses The carrying value of our accrued expenses approximates fair value as it represents amounts that will be satisfied within one year. Accrued expensesconsisted of the following at December 31, 2016 and 2015: 2016 2015 Loss contingency for litigation $4,000 $2,516 Accrued legal and professional fees 1,123 1,089 Accrued consulting and clinical trial costs 6,933 2,844 Accrued payroll and related costs 1,957 1,961 Other 1,751 802 Accrued expenses $15,764 $9,212 8. Commitments and Contingencies a. Operating Leases At December 31, 2016, we leased corporate office space in New York City, pursuant to a lease agreement expiring in September 2030 (subject to an earlytermination right), and additional office space in Lund, Sweden, which expires in December 2018. Rental payments are recognized as rent expense on a straight-line basis over the term of the lease. In addition to rents due under these agreements, we areobligated to pay additional facilities charges, including utilities, taxes and operating expenses. F-19Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) As of December 31, 2016, future minimum annual payments under all operating lease agreements are as follows: Years ending Minimum Annual December 31, Payments 2017 $1,835 2018 1,868 2019 1,818 2020 1,852 2021 1,886 Thereafter 20,682 Total $29,941 Rental expense totaled approximately $1.2 million, $1.9 million, and $1.9 million for 2016, 2015, and 2014, respectively. For 2016, rent expense exceededamounts paid by $210 thousand and for 2015 and 2014, amounts paid exceeded rent expense by $49 thousand and $3 thousand, respectively. Additional facilitycharges, including utilities, taxes, and operating expenses, for 2016, 2015, and 2014 were approximately $1.1 million, $2.5 million, and $2.1 million, respectively. b. Licensing, Service and Supply Agreements We have entered into intellectual property-based license and service agreements in connection with product development programs, and have incurredmilestone, license and sublicense fees and supply costs, included in research and development expenses, totaling approximately $324 thousand, $388 thousand, and$498 thousand during the 2016, 2015, and 2014, respectively. Paid frominception/acquisitiontoDecember 31, 2016 FutureCommitments TermsSeattle Genetics, Inc. $4,701 $13,700 Milestone and periodic maintenance payments to use ADCtechnology to link chemotherapeutic agents to monoclonalantibodies that target prostate specific membrane antigen.ADC technology is based in part on technology licensedby SGI from third parties. Amgen Fremont, Inc. (formerlyAbgenix) $1,350 $5,750 Milestones and royalties to use XenoMouse technologyfor generating fully human antibodies to PSMA LLC’sPSM A antigen. Former member of PSMA LLC $391 $52,188 Annual minimum royalty payments and milestones to usetechnology related to PSMA. University of Zurich and the PaulScherrer Institute $335 $1,005 Annual maintenance and license fee payments, milestonesand royalties in respect of licensed technology related to1404. University of Western Ontario $38 $275 Annual minimum royalty, administration and milestonepayments in respect of licensed technology related toAZEDRA. Johns Hopkins UniversityTechnology $150 $2,760 Annual minimum royalty payments and milestones to usetechnology related to PyL. Selexis Commercial LicenseAgreement $59 $1,802 Milestones and royalties to use Selexis technology relatedto PSMA Antibodies.Amounts based on known contractual obligations as specified in the respective license agreements, which are dependent on the achievement or occurrence of future milestones orevents and exclude amounts for royalties which are dependent on future sales and are unknown. In addition, we are planning to out-license or terminate non-germane licenses and service agreements, as to which we have paid $301 thousand throughDecember 31, 2016, and have future commitments of $14.3 million, subject to occurrence of future milestones or events. F-20(1)® (1) Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) c. Consulting Agreements As part of our research and development efforts, we have from time to time entered into consulting agreements with external scientific specialists. Theseagreements contain various terms and provisions, including fees to be paid by us and royalties, in the event of future sales, and milestone payments, uponachievement of defined events, payable by us. Certain of these scientists are advisors to us, and some have purchased our common stock or received stock optionswhich are subject to vesting provisions. We have recognized expenses with regard to the consulting agreements of $164 thousand, $54 thousand, and $67 thousandfor 2016, 2015, and 2014, respectively. d. Legal Proceedings On January 4, 2017, we settled all claims against us under a federal action brought in 2010 by a former employee, where such former employee hadcomplained that we had violated the anti-retaliation provisions of the Federal Sarbanes-Oxley law by terminating him. In connection with this settlement, we andthe former employee exchanged mutual releases and we are to pay an aggregate sum of $4.0 million to the former employee and his attorneys, which is included inaccrued expenses on our consolidated balance sheet at December 31, 2016. We have $1.7 million held by the District Court in escrow and recorded as restrictedcash in other current assets on our consolidated balance sheet at December 31, 2016. On October 7, 2015 Progenics, Valeant and Wyeth LLC (Valeant’s predecessor as licensee of RELISTOR) received notification of a Paragraph IVcertification for certain patents for RELISTOR (methylnaltrexone bromide) subcutaneous injection, which are listed in the FDA's Approved Drug Products withTherapeutic Equivalence Evaluations, or the Orange Book. The certification resulted from the filing by Mylan Pharmaceuticals, Inc. of an Abbreviated New DrugApplication (“ANDA”) with the FDA, challenging such patents for RELISTOR subcutaneous injection and seeking to obtain approval to market a generic versionof RELISTOR subcutaneous injection before some or all of these patents expire. On October 28, 2015, Progenics, Valeant and Wyeth LLC received a second notification of a Paragraph IV certification with respect to the same patentsfor RELISTOR subcutaneous injection from Actavis LLC as a result of Actavis LLC’s filing of an ANDA with the FDA, also challenging these patents and seekingto obtain approval to market a generic version of RELISTOR subcutaneous injection before some or all of these patents expire. In October 2016, Progenics, Valeant, and Wyeth LLC received a notification of a Paragraph IV certification with respect to certain patents for RELISTORTablets. The certification accompanied the filing by Actavis LLC of an ANDA challenging such patents for RELISTOR Tablets and seeking to obtain approval tomarket a generic version of RELISTOR tablets before some or all of these patents expire. In accordance with the Drug Price Competition and Patent Term Restoration Act (commonly referred to as the Hatch-Waxman Act), Progenics andValeant timely commenced litigation against each of these ANDA filers in order to obtain an automatic stay of FDA approval of the ANDA until the earlier of (i)30 months from receipt of the notice or (ii) a District Court decision finding that the identified patents are invalid, unenforceable or not infringed. In addition to the above described ANDA notifications, in October 2015 Progenics received notices of opposition to three European patents relating tomethylnaltrexone. The oppositions were filed separately by each of Actavis Group PTC ehf. and Fresenius Kabi Deutschland GmbH. Each of the above-described proceedings is in its early stages and Progenics and Valeant continue to cooperate closely to vigorously defend and enforceRELISTOR intellectual property rights. Pursuant to the RELISTOR license agreement between Progenics and Valeant, Valeant has the first right to enforce theintellectual property rights at issue and is responsible for the costs of such enforcement. We are or may be from time to time involved in various other disputes, governmental and/or regulatory inspections, inquires, investigations andproceedings that could result in litigation, and other litigation matters that arise from time to time. The process of resolving matters through litigation or othermeans is inherently uncertain and it is possible that an unfavorable resolution of these matters will adversely affect us, our results of operations, financial condition,and cash flows. In the third quarter of 2014, Progenics and Ono, its former licensee of RELISTOR in Japan, settled all claims between them relating to an arbitrationcommenced by Progenics in 2013, the parties’ October 2008 License Agreement and the former licensee’s development and commercialization of the drug. Inconnection therewith, the parties exchanged mutual releases and the former licensee paid us $7.25 million, which was recorded as other operating income. F-21® Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) 9. Non-Recourse Long-Term Debt, Net On November 4, 2016, through a new wholly-owned subsidiary MNTX Royalties Sub LLC (“MNTX Royalties”), we entered into a loan agreement (the“Royalty-Backed Loan”) with a fund managed by HealthCare Royalty Partners III, L.P. (“HCRP”) pursuant to which HCRP agreed to make term loans in anaggregate principal amount of up to $100.0 million. We borrowed $50.0 million and can borrow an additional $50.0 million, subject to mutual agreement withHCRP, up to twelve months after the closing date. Under the terms of the Royalty-Backed Loan, the lenders have no recourse to us or to any of our assets otherthan the right to receive royalty payments from the commercial sales of RELISTOR products owed under our agreement with Valeant. The RELISTOR royaltypayments will be used to repay the principal and interest on the loan. The Royalty-Backed Loan bears interest at a per annum rate of 9.5%. Under the terms of the loan agreement, payments of interest and principal, if any, under the loan will be made on the last day of each calendar quarter outof RELISTOR royalty payments received since the immediately preceding payment date. On each payment date prior to March 31, 2018, RELISTOR royaltypayments received since the immediately preceding payment date will be applied solely to the payment of interest on the loan, with any royalties in excess of theinterest amount retained by us. Beginning on March 31, 2018, 50 percent of RELISTOR royalty payments received since the immediately preceding payment datein excess of accrued interest on the loan will be used to repay the principal of the loan, with the balance retained by us. Starting on September 30, 2021, all of theRELISTOR royalties received since the immediately preceding payment date will be used to repay the interest and outstanding principal balance until the balance isfully repaid. The loan has a maturity date of June 30, 2025. Upon the occurrence of certain triggers in the loan agreement, or if HCRP so elects on or after January1, 2018, all of the RELISTOR royalty payments received after the immediately preceding payment date shall be applied to the payment of interest and repaymentof principal until the principal of the loan is fully repaid. In the event of such an election by HCRP, we have the right to repay the loan without any prepaymentpenalty. In connection with the Royalty-Backed Loan, the debt issuance costs have been recorded as a debt discount in our consolidated balance sheets and arebeing amortized and recorded as interest expense throughout the life of the loan using the effective interest method. The Loan Agreement contains customary defined events of default, upon which any outstanding principal and unpaid interest shall be immediately dueand payable. These include: failure to pay any principal or interest when due; any uncured breach of a representation, warranty or covenant; any uncured failure toperform or observe covenants; any uncured cross default under a material contract; any uncured breach of our representations, warranties or covenants under acontribution and servicing agreement with MNTX Royalties; any termination of the RELISTOR license agreement; certain bankruptcy or insolvency events; andthe occurrence of a material adverse effect. As of December 31, 2016, we were in compliance with all material covenants under the Royalty-Backed Loan and there was no material adverse changein our business, operations, or financial conditions, as defined in the loan agreement. Future principal, based upon estimated sales projections, under the Royalty-Backed Loan as of December 31, 2016, are as follows: 2017 $-- 2018 2,626 2019 3,678 2020 4,795 2021 8,068 Thereafter 31,598 Total payments $50,765 F-22Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Interest expense, including amortization of debt discount, related to the Royalty-Backed Loan for the year ended December 31, 2016 was approximately$0.8 million. Accrued interest, which was accreted as part of principal at December 31, 2016, was $0.7 million. 10 . Stockholders’ Equity Common Stock and Preferred Stock We are authorized to issue 160 million shares of our common stock, par value $.0013, and 20 million shares of preferred stock, par value $.001. TheBoard of Directors (the “Board”) has the authority to issue common and preferred shares, in series, with rights and privileges as determined by the Board. Shelf Registration During the first quarter of 2017, we established a $250.0 million replacement shelf registration statement. Under a previously established $150.0 millionreplacement shelf registration statement, in February 2014, we completed an underwritten public offering of 8.75 million shares of common stock at a publicoffering price of $4.60 per share, resulting in net proceeds of approximately $37.5 million. All sales of shares have been and will continue to be made pursuant toan effective shelf registration statement on Form S-3 filed with the U.S. Securities and Exchange Commission. Accumulated Other Comprehensive Loss (“AOCL”) The following table summarizes the components of AOCL at December 31, 2016: Foreign CurrencyTranslation AOCL Balance at January 1, 2016 $(26) $(26)Foreign currency translation adjustment (59) (59)Balance at December 31, 2016 $(85) $(85) We did not have any reclassifications out of AOCL to losses during 2016. 11. Stock-Based Compensation Equity Incentive Plans We adopted the following stockholder-approved equity incentive plans: ● The 1996 Amended Stock Incentive Plan (the "1996 Plan") authorized the issuance of up to 5,000,000 shares of our common stock covering severaldifferent types of awards, including stock options, restricted shares, stock appreciation rights, performance shares, and phantom stock. The 1996 Plan wasterminated in 2006. Options granted before termination of the 1996 Plan will continue to remain outstanding until exercised, cancelled, or expired. ● The 2005 Stock Incentive Plan (the "2005 Plan"), pursuant to which we are authorized to issue up to 11,450,000 shares of common stock coveringseveral different types of awards, including stock options, restricted shares, stock appreciation rights, performance shares, and phantom stock. The 2005Plan will terminate on March 25, 2024. The stock option plans provide that options may be granted at an exercise price of 100% of fair market value of our common stock on the date of grant,may be exercised in full or in installments, at the discretion of the Board or its Compensation Committee, and must be exercised within ten years from date of grant.Stock options generally vest pro rata over three to five years. We recognize stock-based compensation expense on a straight-line basis over the requisite service(vesting) period based on fair values. We use historical data to estimate expected employee behaviors related to option exercises and forfeitures and included theseexpected forfeitures as a part of the estimate of stock-based compensation expense as of the grant date. We adjust the total amount of stock-based compensationexpense recognized for each award, in the period in which each award vests, to reflect the actual forfeitures related to that award. Changes in our estimatedforfeiture rate will result in changes in the rate at which compensation cost for an award is recognized over its vesting period. F-23Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) Stock Options The following table summarizes stock options activity for the year ended December 31, 2016: Weighted Weighted Average Number Average Remaining of Shares Exercise Price Contractual Life Outstanding at January 1, 2016 5,134 $9.05 5.69 Granted 1,229 $4.77 Exercised (244) $5.50 Cancelled (926) $6.86 Expired (306) $24.88 Outstanding at December 31, 2016 4,887 $7.57 5.81 Exercisable at December 31, 2016 3,517 $8.46 4.65 Vested and expected to vest at December 31, 2016 4,668 $7.67 5.66 The weighted average fair value of options granted during 2016, 2015, and 2014 was $3.24, $5.02, and $3.41 per share, respectively. The total intrinsic value (the excess of the market price over the exercise price) was approximately $12.1 million for stock options outstanding, $7.5million for stock options exercisable, and $11.4 million for stock options vested and expected to vest, as of December 31, 2016. The total intrinsic value for stockoptions exercised during 2016, 2015, and 2014 was $476 thousand, $465 thousand, and $102 thousand, respectively. We typically do not expect to realize any tax benefits from our stock option activity or the recognition of stock-based compensation expense, because wecurrently have net operating losses and have a full valuation allowance against our deferred tax assets. Accordingly, no amounts related to windfall tax benefitshave been reported in cash flows from operations or cash flows from financing activities for 2016, 2015 or 2014. Stock-Based Compensa tion Expense We account for stock-based awards issued to employees in accordance with the provisions of ASC 718 (Topic 718, Compensation – Stock Compensation). We recognize stock-based compensation expense on a straight-line basis over the service period of the award, which is generally three to five years. Stock-basedawards issued to consultants are accounted for in accordance with the provisions of ASC 718 and ASC 505-50 (Subtopic 50 "Equity-Based Payments to Non-Employees" of Topic 505, Equity ). Options granted to consultants are periodically revalued as the options vest, and are recognized as an expense over the relatedperiod of service or the vesting period, whichever is longer. Under the provisions of ASC 718, members of the Board are considered employees for calculation ofstock-based compensation expense. We estimated the fair value of the stock options granted on the date of grant using a Black-Scholes valuation model that used the weighted averageassumptions noted in the following table. The risk-free interest rate assumption we use is based upon U.S. Treasury interest rates appropriate for the expected lifeof the awards. The expected life (estimated period of time that we expect employees, directors, and consultants to hold their stock options) was estimated based onhistorical rates for three group classifications, (i) employees, (ii) outside directors and officers, and (iii) consultants. Expected volatility was based on historicalvolatility of our stock price for a period equal to the stock option's expected life and calculated on a daily basis. The expected dividend rate is zero since we do notcurrently pay cash dividends on our common stock and do not anticipate doing so in the foreseeable future. F-24Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) The following table presents assumptions used in computing the fair value of option grants during 2016, 2015, and 2014: 2016 2015 2014 Risk-free interest rate 1.53% 2.00% 2.13%Expected life (in years) 6.77 6.97 6.84 Expected volatility 74% 81% 82%Expected dividend yield -- -- -- Stock-based compensation expense for the three years ended December 31, 2016 was recorded in our consolidated statement of operations as follows: 2016 2015 2014 Research and development expenses $843 $1,099 $1,843 General and administrative expenses 1,614 1,849 1,680 Total stock-based compensation expense $2,457 $2,948 $3,523 At December 31, 2016, unrecognized stock-based compensation expense related to stock options was approximately $2.8 million and is expected to berecognized over a weighted average period of approximately 2.6 years. 12. Employee Savings Plan The terms of the amended and restated Progenics Pharmaceuticals 401(k) Plan (the “401(k) Plan”), among other things, allow eligible employees toparticipate in the Amended Plan by electing to contribute to the 401(k) Plan a percentage of their compensation to be set aside to pay their future retirementbenefits. We matched 50% of employee contributions equal to 1% - 10% of compensation during the two years ended December 31, 2016 and 50% of employeecontributions equal to 5% - 8% of compensation during the year ended December 31, 2014, made by eligible employees to the 401(k) Plan (the “MatchingContribution”). In addition, we may also make a discretionary contribution each year on behalf of all participants who are non-highly compensated employees. Wemade Matching Contributions of approximately $281 thousand, $327 thousand, and $276 thousand to the 401(k) Plan for 2016, 2015, and 2014, respectively. Nodiscretionary contributions were made during those years. 13. Income Taxes We account for income taxes using the liability method in accordance with ASC 740 (Topic 740, Income Taxes ). Deferred income taxes reflect the net taxeffects of temporary differences between the carrying amounts of assets and liabilities for financial reporting purposes and the amounts used for income taxpurposes. In 2016, we recorded an income tax provision of $1.8 million primarily due to an adjustment to our deferred tax liability for higher effective tax rate,resulting from relocation of our headquarters to New York City. We recorded an income tax benefit of $133 thousand and $989 thousand in 2015 and 2014,respectively, resulting from the change in the temporary difference between carrying amounts of in-process research and development assets for financial reportingpurposes and the amounts used for income tax purposes. We have completed calculations through June 30, 2016, under Internal Revenue Code Section 382, theresults of which indicate that past ownership changes will limit annual utilization of net operating losses (“NOLs”) in the future. Ownership changes subsequent toJune 30, 2016, may further limit the future utilization of net operating loss and tax credit carry-forwards as defined by the Federal and state tax codes. F-25Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) The components of the provision for (benefit from) income taxes during 2016, 2015, and 2014 consisted of the following: 2016 2015 2014 Current taxes: United States $11 $- $- Foreign - - - State 22 - - Total current taxes $33 $- $- Deferred taxes: United States $- $- $- Foreign - - - State 1,811 (133) (989)Total deferred taxes $1,811 $(133) $(989) Provision for (benefit from) income taxes $1,844 $(133) $(989) Deferred tax assets and liabilities as of December 31, 2016 and 2015, consisted of the following: 2016 2015 Deferred tax assets: Depreciation and amortization $788 $2,215 Research & Experimental and Orphan Drug tax credit carry-forwards 27,361 19,284 NYS investment tax credit carry-forwards 933 1,087 AMT credit carry-forwards 221 211 Net operation loss carry-forwards 227,171 226,639 Capitalized research and development expenditures 11,915 15,149 Stock compensation 12,343 12,250 Other items 4,513 2,562 Total gross deferred tax assets 285,245 279,397 Less valuation allowance (285,245) (279,397)Deferred tax assets - - Deferred tax liability (13,010) (11,199)Net deferred tax liability $(13,010) $(11,199) We maintain a full valuation allowance on deferred tax assets considering our history of taxable losses and the uncertainty regarding our ability togenerate sufficient taxable income in the future to utilize these deferred tax assets. For 2015 and 2014, we incurred net losses for tax purposes. We recognized a fulltax valuation against deferred tax assets at December 31, 2016 and 2015. In 2016 and 2015, we recognized deferred income tax liabilities of $13.0 million and$11.2 million, respectively, to reflect the net tax effects of temporary differences between the carrying amounts of in process research and development assets forfinancial reporting purposes and the amounts used for income tax purposes. The following is a reconciliation of income taxes computed at the Federal statutory income tax rate to the actual effective income tax provision during2016, 2015, and 2014: 2016 2015 2014 U.S. Federal statutory rate 34.0% 34.0% 34.0%State income taxes, net of Federal benefit 10.8% 4.8% 8.0%Foreign rate differential 2.6% (0.1%) 0.0%Research and experimental and Orphan Drug tax credit (63.0%) 1.7% (16.0%)Effect of federal and state tax rate changes (43.0%) (4.8%) 1.6%Permanent differences 0.1% (1.4%) 15.1%Stock option shortfalls 22.3% (6.1%) 38.1%Change in valuation allowance 50.9% (27.8%) (109.6%)Income tax expense/benefit 14.7% 0.3% (28.8%) As of December 31, 2016, we had available, for tax return purposes, unused Federal NOLs of approximately $599.7 million, which will expire in variousyears from 2018 to 2035, $18.7 million of which were generated from deductions post January 1, 2006 that, when realized, will reduce taxes payable and willincrease paid-in-capital and are not reflected in our deferred tax assets above. Additionally, $11.2 million of the valuation allowance relates to NOLs attributable toexcess tax deductions for equity compensation pre January 1, 2006. When realized this will also be reflected as an increase to paid-in-capital. Also, we hadavailable, for tax return purposes, unused state NOLs of approximately $554.0 million, which will expire in various years from 2030 to 2035. F-26Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) We have reviewed our nexus in various tax jurisdictions and our tax positions related to all open tax years for events that could change the status of ourtax liability under ASC 740, if any, or require an additional liability to be recorded. We have not, as of yet, conducted a study of our research and experimental(“R&E”) credit carry-forwards. Such a study might result in an adjustment to our R&E credit carry-forwards, but until a study is completed and any adjustment isknown, no amounts are being presented as an uncertain tax position under ASC 740-10 except for uncertain tax positions acquired in connection with the MolecularInsight acquisition. A full valuation allowance has been provided against our R&E credits and, if an adjustment is required, this adjustment would be offset by anadjustment to the valuation allowance. Thus, there would be no impact to the statements of operations and comprehensive loss if an adjustment was required. As of December 31, 2016, we are subject to Federal, foreign, and state income tax. Open tax years relate to years in which unused net operating losseswere generated or, if used, for which the statute of limitation for examination by taxing authorities has not expired. Our open tax years extend back to 1997. Noamounts of interest or penalties were recognized in our consolidated statements of operations or consolidated balance sheets as of and for the years endedDecember 31, 2016, 2015, and 2014. Our R&E tax credit carry-forwards of approximately $28 million at December 31, 2016 expire in various years from 2018 to 2036. As of December 31, 2016 and 2015, we have not recognized any liability for uncertain tax positions, because of our full valuation allowance. We willrecognize interest and penalties related to these positions, should such costs be assessed. The recognition of unrecognized tax benefits would not affect our effectivetax rate because the tax benefit would be offset by an increase in our valuation allowance. The following is a tabular reconciliation of the total amounts of unrecognized tax benefits for the years ended December 31, 2016 and 2015. 2016 2015 Beginning uncertain tax benefits $2,661 $2,661 Current year - increases - - Current year - decreases - - Settlements - - Expired statuses - - Ending uncertain tax benefits $2,661 $2,661 14 . Net Income (Loss) Per Share Our basic net income (loss) per share attributable to Progenics amounts have been computed by dividing net income (loss) attributable to Progenics by theweighted-average number of common shares outstanding during the period. For 2016 and 2014, we reported net income, and the computation of diluted earningsper share is based upon the weighted-average number of our common shares and dilutive effect of stock options (determined using the treasury stock method). For2015 we reported net losses and, accordingly, potential common shares were not included since such inclusion would have been anti-dilutive. As a result, basic anddiluted EPS are the same for the 2015. In applying the treasury stock method for the calculation of diluted EPS, amounts of unrecognized compensation expense and windfall tax benefits arerequired to be included in the assumed proceeds in the denominator of the diluted EPS calculation unless they are anti-dilutive. We have made an accounting policydecision to calculate windfall tax benefits/shortfalls, for purposes of diluted EPS calculation, excluding the impact of deferred tax assets. This policy decision willapply when we have net income and windfall tax benefits/shortfalls are realizable. F-27Table of Contents PROGENICS PHARMACEUTICALS, INC . NOTES TO CONSOLIDATED FINANCIAL STATEMENTS — continued(amounts in thousands, except per share amounts or as otherwise noted) The calculations of net income (loss) per share, basic and diluted, are as follows: Net income (loss) Weighted-average attributable shares to Progenics outstanding Per share (Numerator) (Denominator) amount 2016 Basic $10,806 70,003 $0.15 Dilutive effect of stock options - 152 Diluted $10,806 70,155 $0.15 2015 Basic and diluted $(39,112) 69,716 $(0.56) 2014 Basic $4,410 68,185 $0.06 Dilutive effect of stock options - 58 Diluted $4,410 68,243 $0.06 The following table summarizes anti-dilutive common shares or common shares where performance conditions have not been met, that were excludedfrom the calculation of the diluted net income (loss) per share: 2016 2015 2014 Stock options 3,577 6,381 5,036 Contingent consideration liability 1,644 2,827 3,457 Total securities excluded 5,221 9,208 8,493 1 5 . Unaudited Quarterly Results (unaudited) Summarized quarterly financial data during 2016 and 2015 are as follows: 2016 Quarter Ended March 31 June 30 September 30 December 31 Revenues $2,450 $8,476 $53,850 $4,653 Net (loss) income $(12,673) $(5,657) $36,282 $(7,219)Net loss attributable to noncontrolling interests $(18) $(19) $(21) $(15)Net (loss) income attributable to Progenics $(12,655) $(5,638) $36,303 $(7,204)Net (loss) income per share attributable to Progenics - basic $(0.18) $(0.08) $0.52 $(0.10)Net (loss) income per share attributable to Progenics - diluted $(0.18) $(0.08) $0.52 $(0.10) 2015 Quarter Ended March 31 June 30 September 30 December 31 Revenues $248 $1,937 $1,396 $5,095 Net loss $(10,254) $(11,697) $(10,014) $(7,154)Net loss attributable to noncontrolling interests $- $- $- $(7)Net loss attributable to Progenics $(10,254) $(11,697) $(10,014) $(7,147)Net loss per share attributable to Progenics - basic $(0.15) $(0.17) $(0.14) $(0.10)Net loss per share attributable to Progenics - diluted $(0.15) $(0.17) $(0.14) $(0.10) Revenues in the second and fourth quarters of 2016 included $5.0 million and $2.0 million license revenue from Bayer, respectively, and revenues in the third quarter of 2016included $50.0 million milestone payment received from Valeant. Revenues in the fourth quarter of 2015 included $1.5 million milestone payment received from CytoDyn. F-28(1)(2)(1) (2) Table of Contents SCHEDULE II – VALUATION AND QUALIFYING ACCOUNTS Allowance for Doubtful Accounts Year ended December 31, BeginningBalance Additions Chargedto General andAdministrativeExpenses DeductionsAccounts WrittenOffDuring Period EndingBalance (in thousands) 2016 $10 $- $(10) $- 2015 $10 $- $- $10 2014 $7 $3 $- $10 F-29Table of Contents SIGNATURES 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 itsbehalf by the undersigned, thereunto duly authorized. PROGENICS PHARMACEUTICALS, INC. By:/s/ MARK R. BAKER Mark R. Baker Chief Executive Officer and Director(Principal Executive Officer) Date: March 9, 2017 Pursuant to the requirements of the Securities Exchange Act of 1934, this report has been signed below by the following persons on behalf of theregistrant in the capacities and on the dates indicated. Signature CapacityDate /s/ PETER J. CROWLEY ChairmanMarch 9, 2017Peter J. Crowley /s/ MARK R. BAKER Chief Executive Officer and DirectorMarch 9, 2017Mark R. Baker (Principal Executive Officer) /s/ BRADLEY CAMPBELL DirectorMarch 9, 2017Bradley Campbell /s/ KAREN J. FERRANTE DirectorMarch 9, 2017Karen J. Ferrante, M.D. /s/ MICHAEL D. KISHBAUCH DirectorMarch 9, 2017Michael D. Kishbauch /s/ DAVID A. SCHEINBERG DirectorMarch 9, 2017David A. Scheinberg, M.D., Ph.D. /s/ NICOLE S. WILLIAMS DirectorMarch 9, 2017Nicole S. Williams /s/ PATRICK FABBIO Senior Vice President and Chief Financial OfficerMarch 9, 2017Patrick Fabbio (Principal Financial and Accounting Officer) S-1Table of Contents EXHIBIT INDEX Exhibit Number * Description3.1(1) Amended and Restated Certificate of Incorporation of the Registrant.3.2(2) Amended and Restated By-laws of the Registrant.4.1(3) Specimen Certificate for Common Stock, $0.0013 par value per share, of the Registrant.10.5(4) ‡ Amended and Restated 1996 Stock Incentive Plan10.6.3(5) ‡ Amended 2005 Stock Incentive Plan10.6.4(6) ‡ Form of Non-Qualified Stock Option Award Agreement10.6.5(6) ‡ Form of Restricted Stock Award Agreement 10.7(7) ‡ Form of Indemnification Agreement10.21.1(9) Amended and Restated Agreement of Lease, dated October 28, 2009, between BMR-Landmark at Eastview LLC and the Registrant.10.25(10) † Option and License Agreement, dated May 8, 1985, by and between the University of Chicago and UR Labs, Inc., as amended by (i) Amendmentto Option and License Agreement, dated September 17, 1987, by and between the University of Chicago and UR Labs, Inc. and (ii) SecondAmendment to Option and License Agreement, dated March 3, 1989, by and among the University of Chicago, ARCH Development Corporationand UR Labs, Inc.10.26(11) Membership Interest Purchase Agreement, dated April 20, 2006, between the Registrant Inc. and Cytogen Corporation.10.27(11) † Amended and Restated PSMA/PSMP License Agreement, dated April 20, 2006, by and among the Registrant, Cytogen Corporation and PSMADevelopment Company LLC.10.34(12) † Collaboration Agreement, effective June 14, 2005, by and between Seattle Genetics, Inc. and PSMA Development Company, LLC.10.37(13) † License Agreement dated as of February 3, 2011, by and between Salix Pharmaceuticals, Inc., the Registrant, Progenics Pharmaceuticals Nevada,Inc. and Excelsior Life Sciences Ireland Limited. 10.37.1(13) † 2010 Agreement Related to Progenics’ MNTX In-License, dated February 3, 2011, by and among the University of Chicago, acting on behalf ofitself and ARCH Development Corporation, the Registrant, Progenics Pharmaceuticals Nevada, Inc. and Salix Pharmaceuticals, Inc.10.38(14) † Stock Purchase and Sale Agreement, dated January 16, 2013, by and between Molecular Insight Pharmaceuticals, Inc., its Stockholders, theRegistrant, and Highland Capital Management, L.P., as Stockholders Representative.10.39(14) † License Agreement, dated September 1, 2012, by and between FUJIFILM RI Pharma Co., Ltd. and Molecular Insight Pharmaceuticals, Inc.10.40(15) † License Agreement, dated May 4, 2012, between Molecular Insight Pharmaceuticals, Inc., the University of Zurich and the Paul ScherrerInstitute.10.41(16) License Agreement, dated as of December 15, 2000, between Molecular Insight Pharmaceuticals, Inc. and The Board of Governors of theUniversity of Western Ontario.10.43(17) Controlled Equity Offering Sales Agreement dated as of January 23, 2014, by and between the Registrant and Cantor Fitzgerald & Co.10.45(12) † Collaboration Agreement, effective February 21, 2001, by and between Abgenix, Inc. and PSMA Development Company, LLC.10.46 (18) † Lease, dated December 31, 2015, between Progenics Pharmaceuticals, Inc. and WTC TOWER 1 LLC.10.47(23 ) † License Agreement, dated as of 30 July, 2015 between the Registrant and The Johns Hopkins University.10.48(23) Employment Offer Letter Agreement between the Registrant and Sheldon Hirt.10.49(23) Employment Offer Letter Agreement between the Registrant and Patrick Fabbio.10.50(19) Exclusive License Agreement, dated as of April 28, 2016, between PSMA Development Company LLC and Bayer AS.10.51(20) Assignment and Assumption Agreement, dated as of May 6, 2016, between Progenics Pharmaceuticals, Inc., BMR-Landmark at Eastview LLCand Regeneron Pharmaceuticals, Inc.10.52(21) Loan Agreement, dated as of November 4, 2016, between Progenics Pharmaceuticals, Inc. through its wholly-owned subsidiary MNTX RoyaltiesSub LLC, and Healthcare Royalty Partners.10.53(22) Controlled Equity Offering Sales Agreement, dated January 6, 2017, between Progenics Pharmaceuticals, Inc. and Cantor Fitzgerald & Co.21.1 Subsidiaries of the Registrant.23.1 Consent of Ernst & Young LLP.31.1 Certification of Mark R. Baker, Chief Executive Officer of the Registrant pursuant to 13a-14(a) and Rule 15d-14(a) under the SecuritiesExchange Act of 1934, as amended.31.2 Certification of Patrick Fabbio, Senior Vice President and Chief Financial Officer of the Registrant pursuant to 13a-14(a) and Rule 15d-14(a)under the Securities Exchange Act of 1934, as amended. E-1SM SM Table of Contents 32.1 Certification of Mark R. Baker, Chief Executive Officer of the Registrant pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906of the Sarbanes-Oxley Act of 2002.32.2 Certification of Patrick Fabbio, Senior Vice President and Chief Financial Officer of the Registrant pursuant to 18 U.S.C. Section 1350, asadopted pursuant to Section 906 of the Sarbanes-Oxley Act of 2002.101 Interactive Data File101.INS XBRL Instance Document101.SCH XBRL Taxonomy Extension Schema101.CAL XBRL Taxonomy Extension Calculation Linkbase101.LAB XBRL Taxonomy Extension Label Linkbase101.PRE XBRL Taxonomy Extension Presentation Linkbase101.DEF XBRL Taxonomy Extension Definition Document * Exhibits footnoted as previously filed have been filed as an exhibit to the document of the Registrant or other registrant referenced in the footnote below,and are incorporated by reference herein. (1) Previously filed in Current Report on Form 8-K filed on June 13, 2013.(2) Previously filed in Current Report on Form 8-K filed on January 30, 2017.(3) Previously filed in Registration Statement on Form S-1, Commission File No. 333-13627.(4) Previously filed in Registration Statement on Form S-8, Commission File No. 333-120508.(5) Previously filed in Current Report on Form 8-K filed on June 18, 2014.(6) Previously filed in Current Report on Form 8-K filed on July 8, 2008.(7) Previously filed in Quarterly Report on Form 10-Q for the quarter ended March 31, 2007.(9) Previously filed in Current Report on Form 8-K filed on November 28, 2012.(10) Previously filed in Annual Report on Form 10-K for the year ended December 31, 2005.(11) Previously filed in Quarterly Report on Form 10-Q for the quarter ended June 30, 2006(12) Previously filed in Amendment No. 2 to Annual Report on Form 10-K/A for the year ended December 31, 2009.(13) Previously filed in Quarterly Report on Form 10-Q for the quarter ended March 31, 2011.(14) Previously filed in Quarterly Report on Form 10-Q for the quarter ended March 31, 2013.(15) Previously filed in Annual Report on Form 10-K for the year ended December 31, 2013.(16) Previously filed in Registration Statement on Form S-1, Commission File No. 333-129570 filed by Molecular Insight Pharmaceuticals, Inc.(17) Previously filed in Registration Statement on Form S-3, Commission File No. 333-193521.(18) Previously filed in Current Report on Form 8-K filed on January 5, 2016.(19) Previously filed in Current Report on Form 8-K filed on May 4, 2016.(20) Previously filed in Current Report on Form 8-K filed on May 10, 2016.(21) Previously filed in Current Report on Form 8-K filed on November 7, 2016.(22) Previously filed in Current Report on Form 8-K filed on January 6, 2017.(23) Previously filed in Annual Report on Form 10-K for the year ended December 31, 2015. † Confidential treatment granted as to certain portions omitted and filed separately with the Commission.‡ Management contract or compensatory plan or arrangement. E-2Exhibit 21.1 Progenics Pharmaceuticals, Inc.Subsidiaries N ame J urisdiction of Incorporation Excelsior Life Sciences Ireland Limited IrelandMolecular Insight Pharmaceuticals, Inc. DelawareMolecular Insight Limited* England and WalesProgenics Life Sciences Limited England and WalesProgenics Pharmaceuticals Nevada, Inc. NevadaPSMA Development Company LLC DelawareEXINI Diagnostics AB SwedenMNTX Royalties Sub LLC Delaware * Subsidiary of Molecular Insight Pharmaceuticals, Inc. Exhibit 23.1 Consent of Independent Registered Public Accounting Firm We consent to the incorporation by reference in the following Registration Statements: (1)Registration Statement (Form S-3 Nos. 333-193521 and 333-215454) of Progenics Pharmaceuticals, Inc., (2)Registration Statements (Form S-8 Nos. 333-197071, 333-183511, 333-176204, 333-160389, 333-143670, and 333-124910) pertaining to the 2005Stock Incentive Plan of Progenics Pharmaceuticals, Inc., and (3)Registration Statements (Form S-8 Nos. 333-120508 and 333-52277) pertaining to the Amended and Restated 1996 Stock Incentive Plan of ProgenicsPharmaceuticals, Inc.; of our reports dated March 9, 2017, with respect to the consolidated financial statements and schedules of Progenics Pharmaceuticals, Inc. and the effectiveness ofinternal control over financial reporting of Progenics Pharmaceuticals, Inc. included in this Annual Report (Form 10-K) of Progenics Pharmaceuticals, Inc. for theyear ended December 31, 2016. /s/ Ernst & Young LLP Hartford, Connecticut March 9, 2017Exhibit 31.1 CERTIFICATION PURSUANT TO RULE 13a-14(a) AND RULE 15d-14(a) UNDER THE SECURITIES EXCHANGE ACT OF 1934, AS AMENDED I, Mark R. Baker, certify that: 1.I have reviewed this annual report on Form 10-K of Progenics Pharmaceuticals, Inc.; 2.Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact necessary to make thestatements made, in light of the circumstances under which such statements were made, not misleading with respect to the period covered by thisreport; 3.Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects thefinancial condition, results of operations and cash flows of the registrant as of, and for, the periods presented in this report; 4.The registrant’s other certifying officer and I are responsible for establishing and maintaining disclosure controls and procedures (as defined inExchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the registrant and have: a)designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be designed under our supervision,to ensure that material information relating to the registrant is made known to us by others within the registrant, particularly during theperiod in which this report is being prepared; b)designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under oursupervision, to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements forexternal purposes in accordance with generally accepted accounting principles; c)evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our conclusions about theeffectiveness of the disclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; and d)disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during the registrant’s mostrecent fiscal quarter (the registrant’s fourth fiscal quarter in the case of an annual report) that has materially affected, or is reasonably likelyto materially affect, the registrant’s internal control over financial reporting; and 5.The registrant’s other certifying officer and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to theregistrant’s independent registered public accounting firm and the audit committee of the registrant’s board of directors (or persons performing theequivalent function): a)all significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which arereasonably likely to adversely affect the registrant’s ability to record, process, summarize and report financial information; and b)any fraud, whether or not material, that involves management or other employees who have a significant role in the registrant’s internalcontrol over financial reporting. /s/ Mark R. BakerDate: March 9, 2017Mark R. Baker Chief Executive Officer(Principal Executive Officer) Exhibit 31.2 CERTIFICATION PURSUANT TO RULE 13a-14(a) AND RULE 15d-14(a) UNDER THE SECURITIES EXCHANGE ACT OF 1934, AS AMENDED I, Patrick Fabbio, certify that: 1.I have reviewed this annual report on Form 10-K of Progenics Pharmaceuticals, Inc.; 2.Based on my knowledge, this report does not contain any untrue statement of a material fact or omit to state a material fact necessary to make thestatements made, in light of the circumstances under which such statements were made, not misleading with respect to the period covered by thisreport; 3.Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects thefinancial condition, results of operations and cash flows of the registrant as of, and for, the periods presented in this report; 4.The registrant’s other certifying officer and I are responsible for establishing and maintaining disclosure controls and procedures (as defined inExchange Act Rules 13a-15(e) and 15d-15(e)) and internal control over financial reporting (as defined in Exchange Act Rules 13a-15(f) and 15d-15(f)) for the registrant and have: a)designed such disclosure controls and procedures, or caused such disclosure controls and procedures to be designed under our supervision,to ensure that material information relating to the registrant is made known to us by others within the registrant, particularly during theperiod in which this report is being prepared; b)designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under oursupervision, to provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements forexternal purposes in accordance with generally accepted accounting principles; c)evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our conclusions about theeffectiveness of the disclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; and d)disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during the registrant’s mostrecent fiscal quarter (the registrant’s fourth fiscal quarter in the case of an annual report) that has materially affected, or is reasonably likelyto materially affect, the registrant’s internal control over financial reporting; and 5.The registrant’s other certifying officer and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to theregistrant’s independent registered public accounting firm and the audit committee of the registrant’s board of directors (or persons performing theequivalent function): a)all significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which arereasonably likely to adversely affect the registrant’s ability to record, process, summarize and report financial information; and b)any fraud, whether or not material, that involves management or other employees who have a significant role in the registrant’s internalcontrol over financial reporting. /s/ Patrick FabbioDate: March 9, 2017Patrick Fabbio Chief Financial Officer (Principal Financial and Accounting Officer) Exhibit 32.1 CERTIFICATION PURSUANT TO 18 U.S.C. SECTION 1350, AS ADOPTED PURSUANT TO SECTION 906 OF THE SARBANES-OXLEY ACT OF 2002 The undersigned Chief Executive Officer of Progenics Pharmaceuticals, Inc. (the “Company”) does hereby certify as follows: This annual report on Form 10-K of the Company for the period ended December 31, 2016 and filed with the Securities and Exchange Commission on thedate hereof (the “Report”) fully complies with the requirements of Section 13(a) or 15(d) of the Securities Exchange Act of 1934 and the information contained inthe Report fairly presents, in all material respects, the financial condition and results of operations of the Company. /s/ Mark R. BakerDate: March 9, 2017Mark R. Baker Chief Executive Officer(Principal Executive Officer) A signed original of this written statement required by Section 906, or other document authenticating, acknowledging, or otherwise adopting the signaturethat appears in typed form within the electronic version of this written statement required by Section 906, has been provided to Progenics Pharmaceuticals, Inc. andwill be retained by Progenics Pharmaceuticals, Inc. and furnished to the Securities and Exchange Commission or its staff upon request. Exhibit 32.2 CERTIFICATION PURSUANT TO 18 U.S.C. SECTION 1350, AS ADOPTED PURSUANT TO SECTION 906 OF THE SARBANES-OXLEY ACT OF 2002 The undersigned Chief Financial Officer of Progenics Pharmaceuticals, Inc. (the “Company”) does hereby certify as follows: This annual report on Form 10-K of the Company for the period ended December 31, 2016 and filed with the Securities and Exchange Commission on thedate hereof (the “Report”) fully complies with the requirements of Section 13(a) or 15(d) of the Securities Exchange Act of 1934 and the information contained inthe Report fairly presents, in all material respects, the financial condition and results of operations of the Company. /s/ Patrick FabbioDate: March 9, 2017Patrick Fabbio Chief Financial Officer (Principal Financial and Accounting Officer) A signed original of this written statement required by Section 906, or other document authenticating, acknowledging, or otherwise adopting the signaturethat appears in typed form within the electronic version of this written statement required by Section 906, has been provided to Progenics Pharmaceuticals, Inc. andwill be retained by Progenics Pharmaceuticals, Inc. and furnished to the Securities and Exchange Commission or its staff upon request.
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