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Siren Gold LimitedBIOCRYST PHARMACEUTICALS INC FORM 10-K (Annual Report) Filed 02/26/16 for the Period Ending 12/31/15 Address Telephone CIK Symbol SIC Code Industry 4505 EMPEROR BOULEVARD SUITE 200 DURHAM, NC 27703 919-859-1302 0000882796 BCRX 2836 - Biological Products, Except Diagnostic Substances Biotechnology & Drugs Sector Healthcare Fiscal Year 12/31 http://www.edgar-online.com © Copyright 2016, EDGAR Online, Inc. All Rights Reserved. Distribution and use of this document restricted under EDGAR Online, Inc. Terms of Use. UNITED STATESSECURITIES AND EXCHANGE COMMISSIONWashington, D.C. 20549________________________ Form 10-K________________________ ☒ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 For the fiscal year ended December 31, 2015 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 Number 000-23186 ________________________ BIOCRYST PHARMACEUTICALS, INC.(Exact name of registrant as specified in its charter)________________________ DELAWARE 62-1413174(State of other jurisdiction ofincorporation or organization) (I.R.S. employeridentification no.) 4505 Emperor Blvd., Suite 200, Durham, North Carolina 27703(Address of principal executive offices) (919) 859-1302(Registrant’s telephone number, including area code) Securities registered pursuant to Section 12(b) of the Act: Title of Each Class Name of Each Exchange on Which RegisteredCommon Stock, $.01 Par Value The NASDAQ Global Select Market Securities registered pursuant to Section 12(g) of the Act: Title of classNone________________________ Indicate by a check mark if the registrant is a well-known seasoned issuer, as defined in Rule 405 of the Securities Act. Yes ☐ No ☒ Indicate by a 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 a 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 a check mark whether the registrant submitted electronically and posted on its corporate Website, if any, every Interactive Data File required to be submitted andposted pursuant to Rule 405 of Regulation S-T (Section 232.405 of this chapter) during the preceding 12 months (or for such shorter period that the registrant was required tosubmit and post such files). Yes ☒ No ☐ Indicate by check mark if disclosure of delinquent filers pursuant to Item 405 of Regulation S-K (Section 229.405 of this chapter) is not contained herein, and will not becontained, to the best of registrant’s knowledge, in definitive proxy or information statements incorporated by reference in Part III of this Form 10-K or any amendment tothis 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 the definitions of“large accelerated filer,” “accelerated filer” and “smaller reporting company” in Rule 12b-2 of the Exchange Act. (Check one): Large accelerated filer ☒ Accelerated filer ☐ Non-accelerated filer ☐ (Do not check if a smaller reporting company) Smaller reporting company ☐ Indicate by a check mark whether the registrant is a shell company (as defined in Exchange Act Rule 12b-2). Yes ☐ No ☒. The Registrant estimates that the aggregate market value of the Common Stock on June 30, 2015 (based upon the closing price shown on the NASDAQ Global Select Marketon June 30, 2015) held by non-affiliates was $1,078,490,079. The number of shares of Common Stock, par value $.01, of the Registrant outstanding as of January 31, 2016 was 73,629,816 shares. DOCUMENTS INCORPORATED BY REFERENCE Portions of the Registrant’s definitive Proxy Statement to be filed in connection with the solicitation of proxies for its 2016 Annual Meeting of Stockholders are incorporatedby reference into Items 10, 11, 12, 13 and 14 under Part III hereof. TABLE OF CONTENTS PART I ITEM 1. BUSINESS4ITEM 1A. RISK FACTORS19ITEM 1B. UNRESOLVED STAFF COMMENTS36ITEM 2. PROPERTIES37ITEM 3. LEGAL PROCEEDINGS37ITEM 4. MINE SAFETY DISCLOSURES37 PART II ITEM 5. MARKET FOR REGISTRANT’S COMMON EQUITY, RELATED STOCKHOLDER MATTERS AND ISSUER PURCHASES OF EQUITY SECURITIES37ITEM 6. SELECTED FINANCIAL DATA39ITEM 7. MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS39ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK52ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA54ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE81ITEM 9A. CONTROLS AND PROCEDURES81ITEM 9B. OTHER INFORMATION81 PART III ITEM 10. DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE82ITEM 11. EXECUTIVE COMPENSATION82ITEM 12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS82ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS, AND DIRECTOR INDEPENDENCE82ITEM 14. PRINCIPAL ACCOUNTING FEES AND SERVICES82 PART IV ITEM 15. EXHIBITS, FINANCIAL STATEMENT SCHEDULES83SIGNATURES84INDEX TO EXHIBITS85EX-10.70 EX-10.71 EX-21 EX-23 EX-31.1 EX-31.2 EX-32.1 EX-32.2 EX-101 3 PART I ITEM 1. BUSINESS Forward-Looking Statements This report includes forward-looking statements within the meaning of Section 21E of the Securities Exchange Act of 1934, as amended, which are subject to the “safeharbor” created in Section 21E. In particular, statements about our expectations, beliefs, plans, objectives or assumptions of future events or performance are contained orincorporated by reference in this report. All statements other than statements of historical facts contained herein are forward-looking statements. We have based theseforward-looking statements on our current expectations about future events. While we believe these expectations are reasonable, forward-looking statements are inherentlysubject to risks and uncertainties, many of which are beyond our control. Our actual results may differ materially from those suggested by these forward-looking statementsfor various reasons, including those discussed in this report under the heading “Risk Factors.” Given these risks and uncertainties, you are cautioned not to place unduereliance on our forward-looking statements. The forward-looking statements included in this report are made only as of the date hereof. We do not undertake, and specificallydecline, any obligation to update any of these statements or to publicly announce the results of any revisions to any forward-looking statements to reflect future events ordevelopments. When used in the report, unless otherwise indicated, “we,” “our,” “us,” the “Company” and “BioCryst” refer to BioCryst Pharmaceuticals, Inc. Our Business We are a biotechnology company that designs, optimizes and develops novel small molecule drugs that block key enzymes involved in the pathogenesis of diseases. Wefocus on the treatment of rare diseases in which significant unmet medical needs exist and align with our capabilities and expertise. We integrate the disciplines of biology,crystallography, medicinal chemistry and computer modeling to discover and develop small molecule pharmaceuticals through the process known as structure-guided drugdesign. Structure-guided drug design is a drug discovery approach by which we design synthetic compounds from detailed structural knowledge of the active sites of enzymetargets associated with particular diseases. We use X-ray crystallography, computer modeling of molecular structures and advanced chemistry techniques to focus on thethree-dimensional molecular structure and active site characteristics of the enzymes that control cellular biology. Enzymes are proteins that act as catalysts for many vitalbiological reactions. Our goal generally is to design a compound that will fit in the active site of an enzyme and thereby prevent its catalytic activity. Molecules from ourdiscovery efforts which are commercially available or that are in development are summarized in the table below: Drug/Drug Candidate Drug Class Therapeutic Area(s) Phase RightsRAPIVAB ®(peramivir injection) Intravenous Neuraminidase Inhibitor Acute uncomplicated Influenza Approved(US) Seqirus (worldwide, exceptJapan, Taiwan, Korea andIsrael) BioCryst retainsU.S. stockpiling rights RAPIACTA ®(peramivir injection) Intravenous Neuraminidase Inhibitor Uncomplicated seasonal influenza Approved(Japan) Shionogi(Japan & Taiwan) PERAMIFLU ®(peramivir injection) Intravenous Neuraminidase Inhibitor Uncomplicated seasonal influenza Approved(Korea) Green Cross(Korea) Avoralstat (previously BCX4161) Oral Serine Protease Inhibitor Targeting Kallikrein Hereditary angioedema (“HAE”) Phase 2/3 BioCryst(worldwide) BCX7353 Oral Serine Protease Inhibitor Targeting Kallikrein(intended to be a once-daily treatment) HAEPhase 2 BioCryst(worldwide) Other 2 nd generation HAE compounds Oral Serine Protease Inhibitors Targeting Kallikrein HAE and other indications Preclinical BioCryst (worldwide) BCX4430 RNA dependent-RNA Polymerase Inhibitor Filoviruses, including Ebola andMarburg viruses Phase 1 BioCryst(worldwide) Forodesine Oral Purine Nucleoside Phosphorylase Inhibitor Oncology Preparing to file forregulatory approval Mundipharma(worldwide) 4 Business Strategy Our business strategy is to create shareholder value by focusing our discovery and development efforts on oral drugs for rare diseases for which a significant unmetmedical need exists. We select disease targets and product candidates in which a small molecule would offer a significant benefit over existing products or would be the firstto market. We strive to advance our product candidate portfolio from discovery to commercial markets efficiently by utilizing a small group of talented and highly-skilledemployees working in conjunction with strategic outsource partners. BioCryst is unique in its approach to treat orphan diseases with small molecules utilizing crystallographyand structure-guided drug design. The principal elements of our strategy are: • Focusing on High Value-Added Structure-Guided Drug Design Technologies. We utilize structure-guided drug design in order to most efficiently develop newtherapeutic candidates. Structure-guided drug design is a process by which we design a product candidate through detailed analysis of the enzyme target, whichthe product candidate must inhibit in order to stop the progression of the disease or disorder. We believe that structure-guided drug design is a powerful tool forthe efficient development of small-molecule product candidates that have the potential to be safe and effective. Our structure-guided drug design technologiestypically allow us to design and synthesize multiple product candidates that inhibit the same enzyme target, with the goal of establishing broad patent protectionand formulating compounds with competitive advantages. • Selecting Inhibitors that are Promising Product Candidates. We start by selecting disease targets with well-understood biology and characteristics that fit withour ability to utilize structure-guided drug design capabilities to build potent and specific enzyme inhibitors. Next, we narrow our selection of these productcandidates based on product characteristics, such as initial indications of safety and biologic activity on the target. • Developing our Product Candidates Efficiently. An important element of our business strategy is to efficiently progress our product candidates through thedevelopment process. In order to accomplish this, we strive for disease targets with a defined clinical and regulatory pathway for approval. In addition, wecontrol fixed costs and overhead by outsourcing with strategic partners and contractors or entering into license agreements with third parties, including the U.S.Government. We maintain a streamlined corporate infrastructure that focuses our expertise. By contracting with the U.S. Government and outsourcing certainaspects of our operations, we are able to control overhead costs and focus financial resources directly where they provide the most benefit and reduce ourbusiness risk. We are a Delaware corporation originally founded in 1986. Our corporate headquarters is located at 4505 Emperor Blvd., Suite 200, Durham, North Carolina 27703 andthe corporate telephone number is (919) 859-1302. For more information about us, please visit our website at www.biocryst.com. The information on our website is notincorporated into this Form 10-K. RAPIVAB (peramivir injection) Peramivir is an intravenous neuraminidase inhibitor approved in multiple countries for the treatment of patients with influenza, most recently in the United States asRAPIVAB ® . Influenza is a seasonal virus with the highest infection rates generally observed in colder months. Intravenous (“i.v.”) peramivir injection has also beenapproved in Japan (RAPIACTA ® ) and Korea (PERAMIFLU ® ). In the countries for which peramivir is commercially available, influenza occurs primarily during theSeptember to April timeframe. RAPIVAB was approved by the U.S. Food and Drug Administration (“FDA”) on December 19, 2014 for the treatment of acute uncomplicated influenza in patients 18years and older who have been symptomatic for no more than two days. In December 2013, we submitted a New Drug Application (“NDA”) which contained data from over2,700 subjects treated with peramivir in 27 clinical trials. We made RAPIVAB available for commercial sale through agreements with specialty distributorships during the2014-2015 influenza season. On June 17, 2015, we announced that BioCryst licensed RAPIVAB (peramivir injection) for the treatment of influenza to CSL Limited (“CSL“),a global biopharmaceutical company. RAPIVAB is being commercialized by a subsidiary of CSL called Seqirus UK Limited (“SUL”), which specializes in influenzaprevention through the supply of seasonal and pandemic influenza vaccine to global markets. Under the terms of the agreement, SUL obtained worldwide rights tocommercialize RAPIVAB, with the exception of Japan, Korea, Taiwan and Israel. BioCryst retained all rights to pursue pandemic stockpiling orders for RAPIVAB from theU.S. Government, while SUL is responsible for government stockpiling outside the U.S. With the out-license of RAPIVAB to SUL, a strategic and well-suitedcommercialization partner, our current goals for RAPIVAB are to: (1) obtain a stockpiling procurement contract with the U.S. Government to realize the strategic value of thisprogram; (2) fulfill our post-approval development requirements, including conducting a pediatric trial; and (3) submit a Marketing Authorization Application (“MAA”) andNew Drug Submission (“NDS”) in the European Union and Canada, respectively, to allow SUL the ability to commercialize the drug in those regions. 5 In January 2016, we filed a NDS with Health Canada for RAPIVAB as an i.v. treatment for acute, uncomplicated influenza. RAPIVAB was developed under a $234.8 million contract from the Biomedical Advanced Research and Development Authority within the United States Department ofHealth and Human Services (“BARDA/HHS”), which expired on June 30, 2014. See “Collaborations and In-License Relationships—BARDA/HHS” below for a furtherdiscussion of this development contract. In January 2010, our partner Shionogi & Co., Ltd. (“Shionogi”) received the first approval for peramivir injection and launched it in Japan under the commercial nameRAPIACTA. It was initially approved for the treatment of adults with uncomplicated seasonal influenza, as well as those at high-risk for complications associated withinfluenza. In October 2010, Shionogi received approval for an additional indication to treat children and infants with influenza in Japan. In August 2010, Green CrossCorporation (“Green Cross”) received marketing and manufacturing approval from the Korean Food & Drug Administration under the commercial name PERAMIFLU totreat patients with influenza A & B viruses, including pandemic H1N1 and avian influenza. In addition, we have a regional collaboration for the development andcommercialization of peramivir in Israel. Hereditary Angioedema Drug Candidates Avoralstat : Avoralstat is our most advanced hereditary angioedema (“HAE”) product candidate in a suite of molecules being developed as oral treatments for theprevention of HAE attacks. Avoralstat is positioned to be the first oral prophylactic kallikrein inhibitor for the prevention of HAE attacks. Avoralstat is a novel, selectiveinhibitor of plasma kallikrein in development as an orally-administered treatment for the prevention of attacks in patients with HAE. By inhibiting plasma kallikrein,avoralstat suppresses bradykinin production. Bradykinin is the mediator of acute swelling attacks in HAE patients. HAE is a rare, severely debilitating and potentially fatalgenetic condition that occurs in approximately 1 in 50,000 people. HAE symptoms include recurrent episodes of edema in various locations, including the hands, feet, face,genitalia and airway. Airway swelling is particularly dangerous and can lead to death by asphyxiation. In addition, patients often have bouts of excruciating abdominal pain,nausea and vomiting caused by swelling in the intestinal wall. In December 2014 and January 2015, respectively, the FDA granted avoralstat “Orphan Drug” designation and “Fast Track” designation for the treatment of HAE.Orphan drug designation is granted by the FDA Office of Orphan Products Development to novel drugs intended for the safe and effective treatment of a rare disease orcondition that affects fewer than 200,000 patients in the U.S. This designation provides certain incentives, including federal grants, tax credits, waiver of Prescription DrugUser Fee Act (“PDUFA”) filing fees, and a seven-year marketing exclusivity period against competition once the product candidate is approved. The Fast Track designationprocess of the FDA is designed to facilitate the development and expedite the review and approval of drugs intended to treat serious or life threatening conditions and thataddress unmet medical needs. A drug that receives Fast Track designation is usually eligible for more frequent written communication and meetings with the FDA to discussthe drug's development plan and the collection of appropriate data supporting drug approval. In addition, the Committee for Orphan Medicinal Products (“COMP”) of theEuropean Medicines Agency (“EMA”) issued a positive opinion on the application for orphan drug designation for avoralstat for the treatment of patients with HAE and theEuropean Commission recently affirmed this designation. Orphan drug designation by the EMA provides regulatory and financial incentives for companies to develop andmarket therapies that treat a life-threatening or chronically debilitating condition affecting no more than five in 10,000 persons in the European Union (“EU”). On December 18, 2014, we announced the dosing of the first patient in OPuS-2 ( O ral P rophylaxi S-2 ), a blinded, randomized, placebo-controlled clinical trial oforally-administered avoralstat in patients with HAE. OPuS-2 was a 12-week, three-arm, parallel cohort design trial to evaluate the efficacy and safety of two doses ofavoralstat, 300 mg and 500 mg, administered three-times daily compared with placebo. This trial was conducted in the U.S. and select European countries, and it enrolledapproximately 100 HAE patients. The primary goals of the trial were to characterize the efficacy of avoralstat in reducing the frequency of angioedema attacks, and toevaluate the safety and tolerability of 12 weeks of avoralstat treatment. The primary efficacy endpoint was angioedema attack frequency. 6 On February 8, 2016, we announced results from OPuS-2. In the OPuS-2 study, HAE patients with a historical attack frequency of greater than 0.45 attacks per weekwere randomized to treatment with either 500 mg or 300 mg of avoralstat, or placebo, administered three times daily for 12 weeks. Thirty-eight subjects received avoralstat500 mg, 36 subjects received avoralstat 300 mg, and 36 subjects received placebo. Treatment with 500 mg and 300 mg of avoralstat three times daily failed to demonstrate astatistically significantly lower mean attack rate versus placebo. The mean (standard deviation) attack rates per week were 0.63 (0.57) on avoralstat 500 mg and 0.71 (0.66) onavoralstat 300 mg, compared to 0.61 (0.41) on placebo. Statistically significant improvements in duration of attacks and in the Angioedema Quality of Life total score wereobserved comparing the 500 mg three times a day avoralstat arm to placebo. Following the analysis of OPuS-2 results, the decision was made to discontinue furtherdevelopment of softgel avoralstat formulation in order to focus development efforts on a novel solid dosage form of avoralstat to achieve meaningfully better drug exposure.We expect additional avoralstat results from a relative bioavailability study testing a novel solid dosage form of avoralstat by mid-year 2016. The primary goals of this studyare to achieve meaningfully better drug exposures and twice daily dosing. On May 27, 2014, we announced positive results from a Phase 2a proof of concept OPuS-1( O ral P rophylaxi S-1 ) clinical trial in patients with HAE. This clinical trialevaluated 400 mg of avoralstat administered three-times daily for 28 days in a randomized, placebo-controlled, two-period cross-over design. Twenty-four HAE patients whohad a high frequency of attacks (more than one per week) were enrolled. This study was designed to provide proof of concept for oral kallikrein inhibition as a treatmentstrategy for HAE. The primary goals of the trial were to estimate the degree of efficacy of avoralstat in reducing the frequency of angioedema attacks and to evaluate thesafety and tolerability of 28 days of avoralstat treatment. The OPuS-1 trial met its primary efficacy endpoint, several secondary endpoints as well as other objectivesestablished for the clinical trial. Each of the twenty-four patients dosed completed the trial. The primary efficacy endpoint for the trial was the mean angioedema attack rate.Treatment with avoralstat demonstrated a statistically significant mean attack rate reduction of 0.45 attacks per week versus placebo, p< 0.001. The mean attack rate per weekwas 0.82 on avoralstat treatment, compared to 1.27 on placebo. Oral administration of avoralstat was generally safe and well-tolerated, with an adverse event profile similar tothat observed for placebo. Patient dosing compliance in this trial was 98 percent. 2nd generation HAE compounds: The goal of our second generation HAE discovery program is to discover and develop oral molecules for the prevention of HAEattacks which have a superior selectivity and bioavailability profile while maintaining similar potency as compared to avoralstat. In December 2013, we announced theselection of two optimized plasma kallikrein inhibitors to advance into preclinical development as potential once-daily, oral prophylactic treatments for HAE. Based on earlypreclinical development studies, these structurally different molecules have a similar mechanism of action as avoralstat and have achieved the principal goal of improvedbioavailability. Both BCX7353 and the second compound had roughly five times better bioavailability than avoralstat. These compounds demonstrated sub-nanomolarpotency on the isolated enzyme and single digit nanomolar potency in suppressing kallikrein activity in an ex-vivo activated normal human plasma kallikrein inhibition(“aPKI”) assay. Plasma concentrations of each of the optimized compounds exceeded the aPKI assay EC80 concentration at 24 hours after a single oral dose of 10 mg/kg inrats, indicating potential for once-daily dosing. In January 2015, we selected BCX7353 to advance into Phase 1 development as a once-daily, oral prophylactic HAEtreatment. Given the other advanced second generation molecule’s inferior profile and similar molecular composition to BCX7353, we have chosen only to advanceBCX7353. In addition to BCX7353, we continue to work on and advance other second generation compounds that are at an earlier stage. These molecules are in preclinicaldevelopment and will be assessed for safety and efficacy in prophylactic HAE treatment as well as for other potential indications. We will provide additional information onthese molecules as we approach an Investigational New Drug (“IND”) filing or we obtain data suggesting efficacy and safety surrounding these molecules in potential HAEand other therapeutic indications. BCX7353 : BCX7353 is structurally different from avoralstat, but has a similar mechanism of action targeting plasma kallikrein. On May 13, 2015, we announced theinitiation of a Phase 1 clinical trial to evaluate the safety, pharmacokinetics and pharmacodynamics of orally-administered BCX7353 in healthy volunteers.On October 8, 2015, we announced that the randomized, placebo-controlled, Phase 1 clinical trial of orally-administered BCX7353 in healthy volunteers successfullymet all of its objectives.In this Phase 1 clinical trial BCX7353 dose levels included single doses of up to 1000mg, once-daily doses of up to 500 mg for seven days, and once-daily doses of 350mg for 14 days. Plasma levels increased in approximate proportion to dose, and drug exposure was not affected by dosing with food. The half-life of BCX7353 was estimatedat 50-60 hours. After daily dosing, blood levels met or exceeded a predicted target therapeutic range throughout the 24 hour dosing interval. Inhibition of the target enzyme,plasma kallikrein, was measured in a sensitive and specific bioassay. Daily dosing with BCX7353 strongly inhibited plasma kallikrein at all four dose levels; the degree ofinhibition was dose-related (p < 0.0001) and inhibition was sustained throughout the 24 hour dosing interval. This pharmacodynamic effect correlated strongly to the achieveddrug concentration (r = 0.91, p < 0.0001).Subsequently, cohorts of healthy Japanese volunteers were added to the study to support development of BCX7353 in Japan under the “Sakigake” accelerated R&Ddesignation. Following assessment of single oral doses of BCX7353 of 100mg (6 subjects) and 500 mg (6 subjects), 250 mg of BCX7353 was administered orally and dailyfor seven days to ten subjects. Compared to Western subjects administered the same dose level, plasma drug levels in Japanese subjects were moderately higher. Kallikreininhibition on day seven of daily dosing with 250 mg in Japanese subjects was similar to that seen at the 350 mg daily and 500 mg daily dose levels in Western subjects.The combined data from both Western and Japanese healthy volunteers indicates that oral BCX7353 has been generally safe and well tolerated in a total of 96 treatedhealthy volunteers, 46 with singles doses and 50 with multiple doses. No serious adverse events have been seen and no dose-limiting toxicity has been identified. There havebeen no clinically significant laboratory abnormalities, ECG changes, or vital sign changes observed.In single dose subjects, 89% (31 of 35) of adverse events (AEs) have been grade 1. The four grade 2 AEs observed were: nausea (1) and vomiting (1) occurring in onesubject: hay fever (1) and diarrhea (1 from Japanese cohort). 7 In multiple dose subjects, 90% (63 of 70) of adverse events (AEs) have been grade 1. The six grade 2 AEs observed were: upper abdominal pain (1, discontinued fromstudy); syncope (1) headache (1) diarrhea (1) and upper abdominal pain (1) occurring on one subject (discounted from study), and maculopapular rash. One grade 3 AE wasobserved, a cutaneous delayed-type hypersensitivity reaction. The two rash AE’s are described in more detail below.The incidence of drug-related skin rash across all multiple-dose cohorts was 4% (2 of 50 subjects). One Japanese subject dosed at 250 mg daily for seven daysdeveloped a grade 2 maculopapular skin rash following cessation of dosing, and one Western subject dosed at 500 mg daily for seven days developed a grade 3hypersensitivity reaction, described as a maculopapular skin rash, following cessation of dosing. Both AEs were assessed by the investigator as drug-related. The Japanesesubject received antihistamines and the Western subject received corticosteroids, and in both cases the rash resolved within a few days.The safety, tolerability, drug exposure and on-target plasma kallikrein inhibition results strongly support advancing the development program into a Phase 2 study inHAE patients. A Phase 2 trial (“APeX-1”) to evaluate the safety, tolerability, pharmacokinetics, pharmacodynamics and efficacy of BCX7353 as a preventative treatment toreduce the frequency of attacks in HAE patients is expected to begin in 2016. The design of the trial will be described when the APeX-1 protocol is approved by regulatoryauthorities and the clinical trial is initiated. On October 27, 2015 The Japanese Ministry of Health Labor & Welfare (“MHLW”) announced that BioCryst’s BCX7353 was one of six products designated underMLHW’s new Sakigake fast track review system. The Sakigake Designation System promotes R&D in Japan, aiming at early market availability for innovativepharmaceutical products. This designation provides for additional interactions with the regulatory agency in Japan from early development through filing, prioritizeddevelopment and review, and introduction of the product as soon as possible to address a serious unmet medical need. We expect the results of APeX-1 to help us and theMHLW to determine the regulatory pathway and timeline for BCX7353 in Japan. BCX4430 BCX4430 is a broad-spectrum antiviral (“BSAV”) research program and is currently being developed under contracts with the National Institute of Allergy andInfectious Diseases (“NIAID/HHS”) and the U.S. Department of Health and Human Services (“BARDA/HHS”). The objective of our BSAV program is to develop BCX4430as a broad-spectrum therapeutic for viruses that pose a threat to national health and security. The primary focus of the program is treatment of hemorrhagic fever viruses.NIAID/HHS funding has supported BCX4430’s development as a treatment for Marburg virus and Ebola virus. In March 2014, BCX4430 was featured in an online Naturepublication depicting successful efficacy results in animal models of infection with Marburg virus and Ebola virus. BCX4430 completely protected cynomolgus macaquesfrom Marburg virus infection when administered by intramuscular (“i.m.”) injection 48 hours post-infection. Post-exposure i.m. administration of BCX4430 also protectedrodents against Marburg virus and Ebola virus infections. In addition, BCX4430 was shown to be active in vitro against a broad range of other RNA viruses, including theemerging viral pathogen Middle East Respiratory Syndrome Coronavirus (“MERS-CoV”). The publication, which reported the protection of non-human primates fromfilovirus disease by BCX4430, describes efficacy results generated from an ongoing collaboration between scientists in the U.S. Army Medical Research Institute of InfectionDiseases (“USAMRIID”) and us. BCX4430 has been shown to be active against more than 20 RNA viruses in nine different families, including filoviruses, togaviruses,bunyaviruses, arenaviruses, paramyxoviruses, coronaviruses and flaviviruses. In tests conducted at USAMRIID, BCX4430 protected animals against parenteral exposures toMarburg, Ebola and Rift Valley Fever viruses and from exposures to aerosolized Marburg virus, an experimental condition designed to mimic an exposure scenario that couldresult during a bioterrorist attack. On December 23, 2014, we announced results from a successful proof-of-concept study of BCX4430 for the treatment of experimental Ebola virus infection in Rhesusmacaques, conducted at USAMRIID. The primary goal of the study was to assess the effect of BCX4430 treatment on survival through Day 41 in animals infected with Ebolavirus. Dosing of placebo or BCX4430 by i.m. injection was initiated 30-120 minutes after virus challenge and continued twice a day (“BID”) for 14 days. Animals were dosedwith either placebo, 16 mg/kg of BCX4430 BID or 25 mg/kg of BCX4430 BID. Survival at day 41 in the 16 mg/kg BID group of BCX4430 treated animals was 4 of 6(66.7%, p < 0.001 compared to 0% survival in controls) and 6 of 6 in the 25 mg/kg BID group (100%, p < 0.001 compared to controls). The overall survival rate for BCX4430treated animals at day 41 was 10 of 12 (83%, p < 0.001 compared to controls). Preliminary evaluation of the quantity of virus in the blood showed an approximate 3-logreduction in Ebola virus RNA copies/mL of plasma, compared with control animals. This Rhesus macaque study was conducted following the completion, in November 2014,of a dose-ranging study of BCX4430 for the experimental treatment of cynomolgus macaques infected with Ebola virus. The cynomolgus macaque study was designed toevaluate whether BCX4430 showed a meaningful benefit for survival in Ebola virus non-human primate (“NHP”) disease models and explore a dose range. In this studyBCX4430 demonstrated a statistically significant prolongation of survival for the animals at the highest dose regimen tested, but no animals survived beyond 21 days. On December 15, 2014, we announced the dosing of the first subject in a randomized, placebo-controlled Phase 1 clinical trial to evaluate i.m. administration ofBCX4430 in healthy volunteers. The main goals of this first-in-human study are to evaluate the safety, tolerability and pharmacokinetics of escalating doses of BCX4430administered via i.m. injection in healthy subjects. In part one of the study, subjects will receive a single dose of BCX4430; and then subjects will receive BCX4430 for sevendays in the second part of the study. Up to six single-dose cohorts and four multiple-dose cohorts will be evaluated, with a total of up to 88 volunteers participating. ThisPhase 1 study is expected to continue in 2016. ForodesineForodesine is a Purine Nucleoside Phosphorylase (“PNP”) inhibitor in development by Mundipharma as a treatment for cancer under a world-wide license agreement.PNP is a purine salvage pathway enzyme. High doses of PNP inhibitors could be useful in the treatment of hematological malignancies. Mundipharma has received orphandrug status for forodesine, and following successful completion of a Phase 2 pivotal study in recurrent/refractory peripheral T-cell lymphoma patients in Japan, is preparing tofile for regulatory approval. 8 On November 11, 2011, we entered into an Amended and Restated License and Development Agreement (the “Amended and Restated Agreement”) with Mundipharma,amending and restating the February 1, 2006 exclusive, royalty-bearing Development and License Agreement for the development and commercialization of forodesine foruse in the field of oncology. Under the terms of the Amended and Restated Agreement, Mundipharma obtained worldwide rights to forodesine, so Mundipharma controls theworldwide development and commercialization of forodesine and assumes all future development and commercialization costs. The Amended and Restated Agreement is amultiple element arrangement for accounting purposes in which we were required to deliver to Mundipharma both the worldwide rights to forodesine and the transfer ofproduct data and know-how to permit Mundipharma to develop and commercialize forodesine (the “Knowledge Transfer”). The world-wide license rights were granted toMundipharma upon execution of Amended and Restated Agreement and the Knowledge Transfer was completed in the first quarter of 2012. We have licensed the PNP technology from Albert Einstein College of Medicine of Yeshiva University (“AECOM”) and Industrial Research, Ltd. (“IRL”) and will owesublicense payments to AECOM/IRL based on the future milestone payments and royalties received by us from Mundipharma and any other partners for which we out-licenseour PNP inhibitors. On November 17, 2011, we amended our agreement with AECOM/IRL whereby AECOM/IRL agreed to accept a reduction of one-half of the percentageof Net Proceeds (as defined in the license agreement) received by us under our Amended and Restated Agreement with Mundipharma. This reduction does not apply toroyalty payments made as a result of sales of licensed products by our sub licensees. Collaborations and In-License Relationships U.S. Department of Health and Human Services (“BARDA/HHS”) . In January 2007, BARDA/HHS awarded us a $102.6 million, four-year contract for the advanceddevelopment of peramivir for the treatment of influenza. During 2009, peramivir clinical development shifted to focus on intravenous delivery and the treatment ofhospitalized patients. To support this focus, a September 2009 contract modification was awarded to extend the i.v. peramivir program and to increase funding by $77.2million. On February 24, 2011, we announced that BARDA/HHS had awarded us a $55.0 million contract modification, intended to fund completion of the Phase 3development of i.v. peramivir for the treatment of patients hospitalized with influenza. That contract modification brought the total contract award from BARDA/HHS to$234.8 million and provided funding to support the filing of an NDA to seek regulatory approval for i.v. peramivir in the U.S. In December 2013, we submitted an NDA filingfor i.v. peramivir to the FDA and the NDA was approved in December 2014. The BARDA/HHS contract expired on June 30, 2014 according to its terms. On March 31, 2015, we announced that BARDA/HHS awarded us a contract for the continued development of BCX4430 as a potential treatment for diseases caused byRNA pathogens, including filoviruses. This BARDA/HHS contract includes a base contract of $13.3 million to support BCX4430 drug manufacturing, as well as $22.9million in additional development options that can be exercised by the government, bringing the potential value of the contract to $36.2 million. As of December 31, 2015, atotal of $16.3 million has been awarded under exercised options within this contract. National Institute of Allergy and Infectious Diseases (“NIAID/HHS”) . In September 2013, NIAID/HHS contracted with us for the development of BCX4430 as atreatment for Marburg, and subsequently, Ebola virus disease. NIAID/HHS, part of the National Institutes of Health, made an initial award of $5.0 million to us. A total of$29.9 million of initial and option funding has been awarded under the NIAID/HHS contract to date and total funding under the contract could be up to $34.0 million, if allcontract options are exercised. The goals of this contract, including amendments, are to file IND applications for i.v. and i.m. BCX4430 for the treatment of Marburg virusdisease, to conduct an initial Phase 1 human clinical trial, as well as to study BCX4430 as a treatment for Ebola virus disease. The contracts with BARDA/HHS and NIAID/HHS are cost-plus-fixed-fee contracts. That is, we are entitled to receive reimbursement for all costs incurred inaccordance with the contracts provisions that are related to the development of peramivir and BCX4430 plus a fixed fee, or profit. BARDA/HHS and NIAID/HHS will makeperiodic assessments of progress and the continuation of the contract is based on our performance, the timeliness and quality of deliverables, and other factors. Thegovernment has rights under certain contract clauses to terminate these contracts. These contracts are terminable by the government at any time for breach or without cause. 9 Seqirus UK Limited . On June 16, 2015, we and SUL, a limited company organized under the laws of the United Kingdom and a subsidiary of CSL Limited, a companyorganized under the laws of Australia, entered into a License Agreement (the "SUL Agreement") granting SUL and its affiliates worldwide rights to develop, manufacture andcommercialize RAPIVAB (peramivir injection) for the treatment of influenza except for the rights to conduct such activities in Israel, Japan, Korea and Taiwan (the permittedgeographies together constituting the "Territory"). RAPIVAB is an intravenous treatment for acute uncomplicated influenza and is currently licensed for use in the UnitedStates, Japan and Korea. RAPIVAB is the first and only intravenous influenza treatment in the world and was approved by the U.S. Food and Drug Administration inDecember 2014 for the treatment of acute uncomplicated influenza in patients 18 years and older who have been symptomatic for no more than two days. We retain all rightsand associated economics to procure pandemic stockpiling orders for RAPIVAB from the U.S. Government, while SUL has the right to pursue government stockpilingoutside the U.S. Pursuant to the SUL Agreement, RAPIVAB will be commercialized by CSL's subsidiary, SUL, which specializes in influenza prevention through the supply of seasonaland pandemic vaccine to global markets. SUL will manufacture, commercialize and exercise decision-making authority with respect to the development andcommercialization of RAPIVAB within the Territory and be responsible for all related costs, including sales and promotion. We will exercise sole decision-making authoritywith regard to the development and commercialization of RAPIVAB outside of the Territory and are responsible for all associated costs. In December 2013, we submitted a NDA for RAPIVAB to the FDA. Under the terms of the SUL Agreement, we are responsible for fulfilling all post-marketingapproval commitments in connection with the FDA's approval of the NDA, and upon fulfillment will transfer ownership of and financial responsibility for the NDA to SUL.Pursuant to potential rights to sell RAPIVAB in Canada and the EU, we are also responsible for regulatory filings and interactions with the Health Canada and the EuropeanMedicines Agency until marketing approval for RAPIVAB is obtained and assigned to SUL. In accordance with the SUL Agreement, we and SUL formed a joint steeringcommittee, composed of an equal number of representatives from each party, to oversee, review and coordinate the conduct and progress of the commercialization ofRAPIVAB in the Territory and any additional development. Under the terms of the SUL Agreement, we received an upfront payment of $33.7 million, and may receive up to $12.0 million in additional milestone payments relatedto the successful achievement of regulatory milestones, including marketing approval (i) by the FDA for a pediatric indication, (ii) by the EMA for an adult indication in theEU and (iii) by Health Canada for an adult indication in Canada. We are also entitled under the SUL Agreement to receive tiered royalties at a percentage rate beginning inthe mid-teens contingent upon meeting minimum thresholds of net sales, as well as a low-thirties percentage of the gross profit from government stockpiling purchases madeoutside the U.S. Specifically, we receive tiered royalties at a percentage rate in the mid-teens to low-forties on net sales in the U.S. during a Contract Year (defined as July 1 -June 30) and tiered royalties at a percentage rate in the mid-teens to mid-twenties on net sales in the Territory, other than in the U.S., during a Calendar Year, each subject tocertain downward adjustments for circumstance or events impacting the overall market opportunity. SUL's royalty payment obligations commence on the date of the SULAgreement and expire, on a country-by-country basis, upon the later of (i) the expiration of legal exclusivity in such country and (ii) ten years from the date of the SULAgreement (the "Royalty Term"). We developed RAPIVAB under a license from UAB and will owe sublicense payments to them on any future milestone payments and/orroyalties received by us from SUL. The term of the SUL Agreement shall continue on a country-by-country basis until the expiration of the last-to-expire Royalty Term in any such country in the Territory.Either party may terminate the SUL Agreement in its entirety if the other party breaches a payment obligation, otherwise materially breaches the SUL Agreement, subject toapplicable cure periods, or if the other party suffers an insolvency event. We may also terminate the SUL Agreement if SUL or any of its affiliates seek to challenge thevalidity of our patents. Termination does not affect a party's rights which have accrued prior thereto, but there are no stated payments in connection with termination otherthan payments of obligations previously accrued. For all terminations exercised by us, the SUL Agreement provides for the termination of any sublicenses granted by SUL tothird parties, and in the case of termination by us for cause, the ceasing of SUL's activities with respect to RAPIVAB, the discontinued use of all of our intellectual propertyand the termination of licenses and rights previously granted to SUL. If requested by us, SUL shall also promptly sell to us all licensed product it then holds in stock,otherwise, SUL may continue to sell such licensed product for designated periods. Shionogi & Co., Ltd. (“Shionogi”) . On February 28, 2007, we entered into a License, Development and Commercialization Agreement (as amended, supplemented orotherwise modified, the “Shionogi Agreement”), an exclusive license agreement with Shionogi to develop and commercialize peramivir in Japan for the treatment of seasonaland potentially life-threatening human influenza. In October 2008, we and Shionogi amended the Shionogi Agreement to expand the territory covered by the agreement toinclude Taiwan. Under the terms of the Shionogi Agreement, Shionogi obtained rights to injectable formulations of peramivir in Japan in exchange for a $14.0 million upfrontpayment. The license provided for development milestone payments (up to $21.0 million), which have all been paid, and for commercial milestone payments (up to$95.0 million) in addition to double-digit (between 10% and 20%) royalty payments on product sales of peramivir. 10 Generally, all payments under the Shionogi Agreement are non-refundable and non-creditable, but they are subject to audit. Shionogi is responsible for all development,regulatory, and marketing costs in Japan. The term of the Shionogi Agreement is from February 28, 2007 until terminated. Either party may terminate in the event of anuncured breach. Shionogi has the right of termination without cause. In the event of termination, all license and rights granted to Shionogi shall terminate and shall revert backto us. We developed peramivir under a license from the University of Alabama Birmingham (“UAB”) and have paid sublicense payments to UAB on the upfront paymentsand will owe sublicense payments on any future event payments and/or royalties received by us from Shionogi. Shionogi Royalty Monetization and Non-Recourse Notes Payable . On March 9, 2011, we completed a $30.0 million financing transaction to monetize certain futureroyalty and milestone payments under the Shionogi Agreement, pursuant to which JPR Royalty Sub LLC (“Royalty Sub”) a wholly-owned subsidiary of BioCryst, issued thePhaRMA Notes discussed below. We received net proceeds of $22.7 million from this transaction. As part of the transaction, we entered into a purchase and sale agreement dated as of March 9, 2011 with Royalty Sub, whereby we transferred to Royalty Sub, amongother things, (i) its rights to receive certain royalty and milestone payments from Shionogi arising under the Shionogi Agreement, and (ii) the right to receive payments undera Japanese yen/US dollar foreign currency hedge arrangement (as further described below, the “Currency Hedge Agreement”) put into place by us in connection with thetransaction. Royalty payments will be paid by Shionogi in Japanese yen and milestone payments will be paid in U.S. dollars. Our collaboration with Shionogi was notimpacted by this transaction. On March 9, 2011, Royalty Sub completed a private placement to institutional investors of $30.0 million in aggregate principal amount of its PhaRMA Senior Secured14.0% Notes due 2020 (the “PhaRMA Notes”). The PhaRMA Notes were issued by Royalty Sub under an Indenture, dated as of March 9, 2011 (the “Indenture”), by andbetween Royalty Sub and U.S. Bank National Association, as Trustee. Principal and interest on the PhaRMA Notes issued are payable from, and are secured by, the rights toroyalty and milestone payments under the Shionogi Agreement transferred by us to Royalty Sub and payments, if any, made to Royalty Sub under the Currency HedgeAgreement. The PhaRMA Notes bear interest at 14% per annum, payable annually in arrears on September 1st of each year (the “Payment Date”). We remain entitled toreceive any royalties and milestone payments related to sales of peramivir by Shionogi following repayment by Royalty Sub of the PhaRMA Notes. Royalty Sub’s obligations to pay principal and interest on the PhaRMA Notes are obligations solely of Royalty Sub and are without recourse to any other person,including the Company, except to the extent of our pledge of its equity interests in Royalty Sub in support of the PhaRMA Notes. We may, but are not obligated to, makecapital contributions to a capital account that may be used to redeem, or on up to one occasion pay any interest shortfall on, the PhaRMA Notes. In September 2013, Royalty Sub paid $1.8 million of interest on the PhaRMA Notes from royalty payments received from RAPIACTA sales from the preceding fourcalendar quarters. This payment resulted in an obligation shortfall of approximately $2.4 million associated with accrued interest due September 3, 2013. As stipulated underthe PhaRMA Notes Indenture, if the amount available for payment on any Payment Date is insufficient to pay all of the interest due on a Payment Date, the shortfall ininterest will accrue interest at the interest rate applicable to the PhaRMA Notes compounded annually. Accordingly, commencing in September 2013, interest began to accrueat 14% per annum on the interest shortfall of $2.4 million. In March, June and August of 2014, Royalty Sub paid additional interest of $446,000, $1.9 million and $70,000,respectively, bringing the shortfall down to $222,000 as of September 30, 2014. Under the terms of the Indenture, Royalty Sub’s inability to pay the full amount of interestpayable in September 2013 by the next succeeding Payment Date for the PhaRMA Notes, which was September 1, 2014, constituted an event of default. Accordingly, wehave classified the PhaRMA Notes and related accrued interest as current liabilities on our balance sheet. As a result of the event of default under the PhaRMA Notes, theholders of the PhaRMA Notes may pursue acceleration of the PhaRMA Notes, may foreclose on the collateral securing the PhaRMA Notes and the equity interest in RoyaltySub and exercise other remedies available to them under the Indenture in respect of the PhaRMA Notes. In such event, we may not realize the benefit of future royaltypayments that might otherwise accrue to us following repayment of the PhaRMA Notes and we might otherwise be adversely affected. Due to the non-recourse nature of thePhaRMA Notes, in the event of any potential acceleration or foreclosure, we believe the primary impact to us would be the loss of future royalty payments from Shionogi andlegal costs associated with retiring the PhaRMA Notes. In addition, we may incur costs associated with liquidating the related Currency Hedge Agreement, which would nolonger be required in the event of foreclosure or if the PhaRMA Notes cease to be outstanding. As the PhaRMA Notes are the obligation of Royalty Sub, we do not currentlyexpect the event of default on the PhaRMA Notes to have a significant impact on our future results of operations or cash flows. As of December 31, 2015, the PhaRMA Notesremain in default. The Indenture does not contain any financial covenants. The Indenture includes customary representations and warranties of Royalty Sub, affirmative and negativecovenants of Royalty Sub, Events of Default and related remedies, and provisions regarding the duties of the Trustee, indemnification of the Trustee, and other matters typicalfor indentures used in structured financings of this type. The PhaRMA Notes are redeemable at the option of Royalty Sub at any time at a redemption price equal to 100% ofthe outstanding principal balance of the PhaRMA Notes being redeemed, plus accrued and unpaid interest through the redemption date on the PhaRMA Notes beingredeemed. 11 Foreign Currency Hedge . In connection with the issuance by Royalty Sub of the PhaRMA Notes, we entered into a Currency Hedge Agreement to hedge certain risksassociated with changes in the value of the Japanese yen relative to the U.S. dollar. Under the Currency Hedge Agreement, we have the right to purchase dollars and sell yenat a rate of 100 yen per dollar for which we may be required to pay a premium in each year from 2016 through 2020. A payment of $2.0 million will be required if, on May 18of the relevant year, the U.S. dollar is worth 100 yen or less, as determined in accordance with the Currency Hedge Agreement. The Currency Hedge Agreement does not qualify for hedge accounting treatment; therefore, mark-to-market adjustments are recognized in our Consolidated Statementof Comprehensive Loss. Cumulative mark-to-market adjustments resulted in a loss of $0.6 million and gains of $5.5 million and $5.3 million for the twelve months endedDecember 30, 2015, 2014 and 2013, respectively. In addition, a realized currency exchange gain of $1.6 million was recognized in 2015 related to the exercise of a U.S.dollar/Japanese yen currency option under our foreign currency hedge. Thus, a resulting $1.1 million net gain is recognized on our foreign currency derivative for 2015.Weare also required to post collateral in connection with the mark-to-market adjustments based on defined thresholds. As of December 31, 2015, no collateral was posted underthe Currency Hedge Agreement. We will not be required at any time to post collateral exceeding the maximum premium payments remaining payable under the CurrencyHedge Agreement. The maximum amount of hedge collateral we would be required to post is $9.8 million. We are required to maintain a foreign currency hedge at 100 yenper dollar under the agreements governing the PhaRMA Notes. Green Cross . In June 2006, we entered into an agreement with Green Cross to develop and commercialize peramivir in Korea. Under the terms of the agreement, GreenCross is responsible for all development, regulatory, and commercialization costs in Korea. We received a one-time license fee of $250,000. The license provides that we willshare in profits resulting from the sale of peramivir in Korea, including the sale of peramivir to the Korean government for stockpiling purposes. Furthermore, Green Crosswill pay us a premium over its cost to supply peramivir for development and any future marketing of peramivir products in Korea. Both parties have the right to terminate inthe event of an uncured material breach. In the event of termination, all rights, data, materials, products and other information would be transferred to us. In August 2010, we announced that Green Cross had received marketing and manufacturing approval from the Korean Food & Drug Administration for i.v. peramivir,under the commercial name PERAMIFLU ® . PERAMIFLU is intended to treat patients with influenza A & B viruses, including pandemic H1N1 and avian influenza. GreenCross received the indication of single dose administration of 300 mg i.v. peramivir. Since PERAMIFLU’s approval, Green Cross has been in pricing discussions with theKorean National Health Insurance Corporation and has yet to agree to a formulary price. PERAMIFLU’s distribution to date has been limited to a case-by-case basis andsignificant sales have not occurred. Other Peramivir Collaborations . In addition to our collaborations with Shionogi and Green Cross, in March 2011 we entered into an arrangement with NeopharmScientific Limited, granting certain commercial and distribution rights for peramivir in Israel. Mundipharma . In February 2006, we entered into an exclusive, royalty bearing right and license agreement with Mundipharma for the development andcommercialization of forodesine, a PNP inhibitor, for use in oncology (the “Original Agreement”). Under the terms of the Original Agreement, Mundipharma obtained rightsto forodesine in markets across Europe, Asia, and Australasia in exchange for a $10.0 million up-front payment. In addition, Mundipharma contributed $10.0 million of thedocumented out-of-pocket development costs incurred by us in respect of the current and planned trials as of the effective date of the agreement, and Mundipharma wouldconduct additional clinical trials at their own cost up to a maximum of $15.0 million. The Original Agreement provided for the possibility of future event payments totaling$155.0 million for achieving specified development, regulatory and commercial events (including certain sales level amounts following a product’s launch) for certainindications. In addition, the Original Agreement provided that we would receive royalties (ranging from single digits to mid teens) based on a percentage of net product sales,which varies depending upon when certain indications receive NDA approval in a major market country and can vary by country depending on the patent coverage or sales ofgeneric compounds in a particular country. Generally, all payments under the Original Agreement were nonrefundable and non-creditable, but they are subject to audit. Welicensed forodesine and other PNP inhibitors from AECOM/IRL and will owe sublicense payments to AECOM/IRL on all milestone payments and royalties received by usfrom Mundipharma. On November 11, 2011, we entered into the Amended and Restated Agreement with Mundipharma. Under the terms of this Amended and Restated Agreement,Mundipharma obtained worldwide rights to forodesine in the field of oncology. Mundipharma will control the development and commercialization of forodesine and assumeall future development and commercialization costs. The Amended and Restated Agreement provides for the possibility of future event payments totaling $15.0 million forachieving specified regulatory events for certain indications. In addition, the Amended and Restated Agreement provides that we will receive tiered royalties ranging frommid- to high-single digit percentages of net product sales in each country where forodesine is sold by Mundipharma. These royalties are subject to downward adjustmentsbased on the then-existing patent coverage and/or the availability of generic compounds in each country. Generally, all payments under the Amended and Restated Agreementare nonrefundable and non-creditable, but they are subject to audit. 12 Mundipharma will also have a right of exclusive negotiations with us for a limited period of time if they initiate negotiations for a specified backup PNP inhibitor.Otherwise, they will be able to participate in the same negotiations process we enter into with another company for the backup PNP inhibitor. The Amended and RestatedAgreement will continue for the commercial life of the licensed products, but may be terminated by either party following an uncured material breach by the other party or inthe event the pre-existing third party license with AECOM/IRL expires. It may be terminated by Mundipharma upon 60 days written notice without cause or under certainother conditions as specified in the Amended and Restated Agreement. If Mundipharma terminates the Amended and Restated Agreement, Mundipharma would no longerhave any rights in forodesine and the rights would revert back to us; provided, however, that in the event the we determine to subsequently use the data developed under theAmended and Restated Agreement for development and commercialization of forodesine in the field of oncology, then we would have to pay Mundipharma 150% of the costof such data for such use. Albert Einstein College of Medicine of Yeshiva University and Industrial Research, Ltd. (“AECOM” and “IRL” respectively) . In June 2000, we licensed a series ofpotent inhibitors of PNP from AECOM and IRL, (collectively, the “Licensors”). The lead product candidate from this collaboration is forodesine. We have obtainedworldwide exclusive rights to develop and ultimately distribute it, or any other, product candidates that might arise from research on these inhibitors. We have the option toexpand our license agreement with the Licensors to include other inventions in the field made by the investigators or employees of the Licensors. We agreed to usecommercially reasonable efforts to develop these drugs. In addition, we have agreed to pay certain milestone payments for each licensed product (which range in theaggregate from $1.4 million to almost $4.0 million per indication) for future development of these inhibitors, single digit royalties on net sales of any resulting product madeby us, and to share approximately one quarter of future payments received from other third-party partners, if any. In addition, we have agreed to pay annual license fees,which can range from $150,000 to $500,000, that are creditable against actual royalties and other payments due to the Licensors. This agreement may be terminated by us atany time by giving 60 days advance notice or in the event of material uncured breach by the Licensors. In May 2010, we amended the license agreement through which we obtained worldwide exclusive rights to develop and ultimately distribute any product candidates thatmight arise from research on a series of PNP inhibitors, including forodesine. Under the terms of the amendment, the Licensors agreed to accept a reduction of one-half in thepercentage of future payments received from third-party sub licensees of the licensed PNP inhibitors that must be paid to the Licensors. This reduction does not apply to(i) any milestone payments we may receive in the future under our license agreement with Mundipharma and (ii) royalties received from its sub licensees in connection withthe sale of licensed products, for which the original payment rate will remain in effect. The rate of royalty payments to the Licensors based on net sales of any resultingproduct made by us remains unchanged. At our sole option and subject to certain agreed upon conditions, any future non-royalty payments due to be paid by us to theLicensors under the license agreement may be made either in cash, in shares of our common stock, or in a combination of cash and shares. On November 17, 2011, we further amended our agreements with the Licensors whereby the Licensors agreed to accept a reduction of one-half in the percentage of NetProceeds (as defined in the license agreement) received by us under our Amended and Restated Agreement with Mundipharma that will be paid to AECOM/IRL. On June 19, 2012, we further amended our agreements with the Licensors whereby the parties clarified the definition of the field with respect to PNP inhibition and theLicensors agreed to grant an exclusive worldwide license of BCX4430 to us for any antiviral use. The University of Alabama at Birmingham (“UAB”) . We currently have agreements with UAB for influenza neuraminidase and complement inhibitors. Under theterms of these agreements, UAB performed specific research for us in return for research payments and license fees. UAB has granted us certain rights to any discoveries inthese areas resulting from research developed by UAB or jointly developed with us. We have agreed to pay single digit royalties on sales of any resulting product and to sharein future payments received from other third-party partners. We have completed the research under the UAB agreements. These two agreements have initial 25-year terms, areautomatically renewable for five-year terms throughout the life of the last patent and are terminable by us upon three months’ notice and by UAB under certain circumstances.Upon termination both parties shall cease using the other parties’ proprietary and confidential information and materials, the parties shall jointly own joint inventions andUAB shall resume full ownership of all UAB licensed products. There is currently no activity between us and UAB on these agreements, but when we license this technology,such as in the case of the Shionogi and Green Cross agreements, or commercialize products related to these programs, we will owe sublicense fees or royalties on amounts itreceives. 13 Government Contracts U.S. Department of Health and Human Services (“BARDA/HHS”) . In January 2007, BARDA/HHS awarded us a $102.6 million four-year contract for the advanceddevelopment of peramivir for the treatment of influenza. During 2009, peramivir clinical development shifted to focus on intravenous delivery and the treatment ofhospitalized patients. To support this focus, a September 2009 contract modification was awarded to extend the i.v. peramivir program and to increase funding by $77.2million. On February 24, 2011, we announced that BARDA/HHS had awarded us a $55.0 million contract modification, intended to fund completion of the Phase 3development of i.v. peramivir for the treatment of patients hospitalized with influenza. That contract modification brought the total contract award from BARDA/HHS to$234.8 million and provided funding to support the filing of an NDA to seek regulatory approval for i.v. peramivir in the U.S. In December 2013, we submitted an NDA filingfor i.v. peramivir to the FDA and the NDA was approved in December 2014. The BARDA/HHS contract expired on June 30, 2014 according to its terms. Under the defined scope of work in the contract with BARDA/HHS for the development of peramivir, a process was undertaken to validate a U.S.-based manufacturerand the related method for producing commercial batches of peramivir active pharmaceutical ingredient (“API”). As a required outcome of this validation process, largequantities of peramivir API were produced. In accordance with our accounting practices, we recorded all costs associated with this validation process as research anddevelopment expenses in our Consolidated Statements of Comprehensive Loss. Simultaneously, revenue from the BARDA/HHS contract was also recorded in ourConsolidated Statements of Comprehensive Loss in 2009. BARDA/HHS subsequently reimbursed us for these costs and upon reimbursement from BARDA/HHS, theassociated peramivir API became property of the U.S. Government. Under the terms of the contract, if we determine the amount of peramivir API produced under the contract is in excess of what is necessary to complete the contract, wecan acquire any excess peramivir API at cost to use for our own purposes. We believe that as a result of the manufacturing campaign described above, more peramivir APIhas been produced than what was required to support U.S. regulatory approval. If we use any excess API for our other contracts or activities, we will need to reconcile throughan appropriate acquisition process with BARDA/HHS and to determine the appropriate acquisition process remuneration for this API. On March 31, 2015, we announced that BARDA/HHS awarded us a contract for the continued development of BCX4430 as a potential treatment for diseases causedby RNA pathogens, including filoviruses. This BARDA/HHS contract includes a base contract of $13.3 million to support BCX4430 drug manufacturing, as well as $22.9million in additional development options that can be exercised by the government, bringing the potential value of the contract to $36.2 million. As of December 31, 2015, atotal of $16.3 million has been awarded under exercised options within this contract. National Institute of Allergy and Infectious Diseases (“NIAID/HHS”) . In September 2013, NIAID/HHS contracted with us for the development of BCX4430 as atreatment for Marburg virus disease. NIAID/HHS, part of the National Institutes of Health, made an initial award of $5.0 million to the Company. The total funding under thiscontract as of December 31, 2015 could be up to $34.0 million, if all contract options are exercised by NIAID/HHS, over a five year period. The goals of this contract,including amendments, are to file IND applications for i.v. and i.m. BCX4430 for the treatment of Marburg virus disease, to study BCX4430 as a treatment for Ebola virusdisease and to conduct an initial Phase 1 human clinical trial. As of December 31, 2015, a total of $29.9 million has been awarded under exercised options within this contract.BCX4430 is the lead compound in our BSAV research program. The contracts with BARDA/HHS and NIAID/HHS are cost-plus-fixed-fee contracts. That is, we are entitled to receive reimbursement for all costs incurred inaccordance with the contracts provisions that are related to the development of BCX4430 plus a fixed fee, or profit. BARDA/HHS and NIAID/HHS will make periodicassessments of progress and the continuation of the contract is based on our performance, the timeliness and quality of deliverables, and other factors. The government hasrights under certain contract clauses to terminate these contracts. These contracts are terminable by the government at any time for breach or without cause. Patents and Proprietary Information Our success will depend in part on our ability to obtain and enforce patent protection for our products, methods, processes and other proprietary technologies, preserveour trade secrets, and operate without infringing on the proprietary rights of other parties, both in the United States and in other countries. We own or have rights to certainproprietary information, proprietary technology, issued and allowed patents and patent applications which relate to compounds we are developing. We actively seek, whenappropriate, protection for our products, proprietary technology and proprietary information by means of U.S. and foreign patents, trademarks and contractual arrangements.In addition, we rely upon trade secrets and contractual arrangements to protect certain of our proprietary information, proprietary technology and products. 14 The patent positions of companies like ours are generally uncertain and involve complex legal and factual questions. Our ability to maintain and solidify our proprietaryposition for our technology will depend on our success in obtaining effective patent claims and enforcing those claims once granted. We do not know whether any of ourpatent applications or those patent applications that we license will result in the issuance of any patents. Our issued patents and those that may issue in the future, or thoselicensed to us, may be challenged, invalidated, rendered unenforceable or circumvented, which could limit our ability to stop competitors from marketing related products orthe length of term of patent protection that we may have for our products. In addition, the rights granted under any issued patents may not provide us with competitiveadvantages against competitors with similar compounds or technology. Furthermore, our competitors may independently develop similar technologies or duplicate anytechnology developed by us in a manner that does not infringe our patents or other intellectual property. Because of the extensive time required for development, testing andregulatory review of a potential product, it is possible that, before any of our product candidates or those developed by our partners can be commercialized, any related patentmay expire or remain in force for only a short period following commercialization, thereby reducing any advantage of the patent. As of December 31, 2015, we have been issued approximately 13 U.S. patents that expire between 2017 and 2030 and that relate to our HAE program compounds,neuraminidase inhibitor compounds and PNP compounds. We have licensed a number of compounds protected by certain composition of matter patents from AECOM andIRL, plus additional manufacturing patents, totaling 14 additional U.S. patents that expire between 2017 and 2029. Additionally, we have approximately 12 PatentCooperation Treaty or U.S. patent applications pending related to HAE program compounds, neuraminidase inhibitor compounds, BSAV and PNP compounds. Our pendingapplications may not result in issued patents, our patents may not cover the products of interest or may not be enforceable in all, or any jurisdictions and our patents may notprovide us with sufficient protection against competitive products or otherwise be commercially viable. After expiration of composition of matter patents for our products andproduct candidates, we may rely on data exclusivity, or in some cases, method of use patents. The enforceability of these patents varies from jurisdiction to jurisdiction andmay not be allowed or enforceable in some territories where we may seek approval. We may not have the funds to continue patent prosecution or to defend all of our existingpatents in our current patent estate and may selectively abandon patents or patent families worldwide or in certain territories. Our success is also dependent upon the skills, knowledge and experience of our scientific and technical personnel, none of which is patentable. To help protect ourrights, we require all employees, consultants, advisors and partners to enter into confidentiality agreements, which prohibit the disclosure of confidential information toanyone outside of BioCryst and, where possible, require disclosure and assignment to us of their ideas, developments, discoveries and inventions. These agreements may notprovide adequate protection for our trade secrets, know-how or other proprietary information in the event of any unauthorized use or disclosure or the lawful development byothers of such information. Competition The pharmaceutical and biotechnology industries are intensely competitive. Many companies, including biotechnology, chemical and pharmaceutical companies, areactively engaged in activities similar to ours, including research and development of drugs for the treatment of rare medical conditions. Many of these companies havesubstantially greater financial and other resources, larger research and development staffs, and more extensive marketing and manufacturing organizations than we do. Inaddition, some of them have considerable experience in preclinical testing, clinical trials and other regulatory approval procedures. In addition, there are also academicinstitutions, governmental agencies and other research organizations that are conducting research in areas in which we are working. We expect to encounter significantcompetition for any of the pharmaceutical products we plan to develop. Companies that successfully complete clinical trials, obtain required regulatory approvals andcommence commercial sales of their products may achieve a significant competitive advantage. Antivirals : The pharmaceutical market for products that prevent or treat influenza is very competitive. Key competitive factors for RAPIVAB (peramivir injection)include, among others, efficacy, ease of use, safety, price and cost-effectiveness, storage and handling requirements and reimbursement. A number of neuraminidase inhibitorsare currently available in the U.S. and/or other counties, including Japan, for the prevention or treatment of influenza, including seasonal flu vaccines and F. Hoffmann-LaRoche Ltd.’s (“Roche”) TAMIFLU ® , GlaxoSmithKline plc’s (“GSK”) RELENZA ® and Daiichi Sankyo Co., Ltd.’s INAVIR ® . In addition, FUJIFILM Corporation’sfavipiravir, a polymerase inhibitor, is approved in Japan. Roche’s neuraminidase inhibitor is also approved for prophylaxis of influenza, and both Roche and GSK have i.v.formulations in clinical trial development. In January 2011, GSK announced initiation of a multi-country Phase 3 study of i.v. zanamivir (the same active ingredient as in RELENZA) in hospitalized patients withinfluenza. The GSK study was completed during the 2014-2015 flu season. In addition to these companies with neuraminidase inhibitors, there are other companies workingto develop additional antiviral drugs to be used against various strains of influenza. Currently, there are a number of other companies developing potential new influenzatherapies. Various government entities throughout the world are offering incentives, grants and contracts to encourage additional investment into preventative and therapeuticagents against influenza, which may have the effect of further increasing the number of our competitors and/or providing advantages to certain competitors. BCX4430 is a product candidate in our BSAV research program and is currently being developed under a contract with NIAID/HHS. The objective of our BSAVprogram is to develop BCX4430 as a broad-spectrum therapeutic for viruses that pose a threat to national health and security. The U.S. Government is investing in a numberof programs intended to address gaps in its medical countermeasure plan. Due to the Ebola outbreak in West Africa in 2014, investment in medical countermeasures hasincreased worldwide. Therapeutic products with potentially promising data to treat Ebola include FUJIFILM Corporation’s favipiravir (polymerase inhibitor), TekmiraPharmaceuticals Corporation’s TKM-Ebola (RNAi interference based) and Mapp Biopharmaceutical, Inc.’s ZMapp (antibody-based). Both TKM-Ebola and ZMapp havebeen used in Ebola patients. Gilead Sciences, Inc announced in October 2015 that it had provided the investigational compound, GS-5734, to two patients with Ebola forcompassionate use. 15 HAE : HAE is an autosomal dominant disease characterized by painful, unpredictable, recurrent attacks of inflammation affecting the hands, feet, face, abdomen,urogenital tract, and the larynx. The inflammation can be disfiguring, debilitating, or in the case of laryngeal attacks, life-threatening. Prevalence for HAE is uncertain but isestimated to be approximately 1 case per 50,000 persons without known differences among ethnic groups and is caused by deficient (Type I) or dysfunctional (Type II) levelsof C1-Inhibitor (“C1-INH”), a naturally occurring molecule that is known to inhibit kallikrein, bradykinin, and other serine proteases in the blood. If left untreated, HAE canresult in a mortality rate as high as 40% primarily due to upper airway obstruction. There are a number of licensed and developmental therapies for HAE, including thefollowing: ·C1-INH therapy is available as an acute therapy (Berinert ® ) and as a prophylactic therapy (Cinryze ® ). These therapies are available intravenously andwork by replacing the missing or malfunctioning C1-INH protein in patients. ·Kallikrein Inhibition - Kalbitor ® (ecallantide) is a specific recombinant plasma kallikrein inhibitor that halts the production of bradykinin and can be dosedsubcutaneously in an inpatient setting. ·Bradykinin receptor antagonist - Firazyr ® (icatibant) is a competitive antagonist of the bradykinin B2 receptor. Firazyr is approved for the treatment ofacute attacks and is administered by subcutaneous administration. ·Other medications - Prophylactic administration of synthetic attenuated androgens (generically available as danazol or stanozolol) has been utilized toreduce the frequency or severity of attacks. However, long-term use of danazol or stanozolol may result in virilization and arterial hypertension. Six-monthliver function tests, annual lipid profiles, and biennial hepatic ultrasound are recommended because these medications increase production of C1-INH in theliver. In addition to avoralstat, BCX7353 and our other second generation compounds, there are a number of other HAE therapies in development. These include aprophylactic plasma derived C1-INH delivered by subcutaneous injection in Phase 3 (CSL Behring); DX-2930/SHP643, a monoclonal antibody administered by subcutaneousinjection for prophylactic treatment of HAE in Phase 3 (Shire PLC); ISIS-PKK, a RNA-targeted antisense drug to inhibit prekallikrein for prophylactic treatment of HAE inPhase 1 (ISIS Pharmaceuticals, Inc.); and two potential oral kallikrein inhibitors being developed by KalVista and Global Blood Therapeutics, respectively. In order to compete successfully in these and other therapeutic areas, we must develop proprietary positions in patented drugs for therapeutic markets that have not beensatisfactorily addressed by conventional research strategies and, in the process, expand our expertise in structure-based drug design. Our product candidates, even ifsuccessfully tested and developed, may not be adopted by physicians over other products and may not offer economically feasible alternatives to other therapies. Research and Development We initiated our research and development activities in 1986. We have assembled a scientific research staff with expertise in a broad base of advanced researchtechnologies including protein biochemistry, X-ray crystallography, chemistry and pharmacology. Our research facilities, located in Birmingham, Alabama, include proteinbiochemistry and organic synthesis laboratories, testing facilities, X-ray crystallography, computer and graphics equipment and facilities to make product candidates on asmall scale for early stage clinical trials. During the years ended December 31, 2015, 2014 and 2013, our research and development expenses were $72.8 million, $51.8million and $41.9 million, respectively. Compliance We conduct our business in an ethical, fair, honest and lawful manner. We act responsibly, respectfully and with integrity in our relationships with patients, health careprofessionals, collaborators, governments, regulatory entities, stockholders, suppliers and vendors. In order to ensure compliance with applicable laws and regulations, our Chief Financial Officer, General Counsel and Vice President of Human Resources overseecompliance training, education, auditing and monitoring; enforce disciplinary guidelines for any infractions of our corporate polices; implement new policies and procedures;respond to any detected issues; and undertake corrective action procedures. Our controls address compliance with laws and regulations that govern public pharmaceuticalcompanies including, but not limited to, the following: federal and state law, such as the Sarbanes-Oxley Act of 2002 and the U.S. Foreign Corrupt Practices Act of 1977;NASDAQ listing requirements; the regulations of the Financial Industry Regulatory Authority; the Securities and Exchange Commission (“SEC”); the FDA; and the UnitedStates Department of Health and Human Services. Our standard operating procedures are designed to provide a framework for corporate governance in accordance withethical standards and best legal practices. 16 Government Regulation The FDA regulates the pharmaceutical and biotechnology industries in the U.S., and our product candidates are subject to extensive and rigorous domestic governmentregulations prior to commercialization. The FDA regulates, among other things, the development, testing, manufacture, safety, efficacy, record-keeping, labeling, storage,approval, advertising, promotion, sale and distribution of pharmaceutical products. In foreign countries, our products are also subject to extensive regulation by foreigngovernments. These government regulations will be a significant factor in the production and marketing of any pharmaceutical products that we develop. Failure to complywith applicable FDA and other regulatory requirements at any stage during the regulatory process may subject us to sanctions, including: • delays; • warning letters; • fines; • product recalls or seizures; • injunctions; • penalties; • refusal of the FDA to review pending market approval applications or supplements to approval applications; • total or partial suspension of production; • civil penalties; • withdrawals of previously approved marketing applications; and • criminal prosecutions. The regulatory review and approval process is lengthy, expensive and uncertain. Before obtaining regulatory approvals for the commercial sale of any products, we orour partners must demonstrate that our product candidates are safe and effective for use in humans. The approval process takes many years, substantial expenses may beincurred and significant time may be devoted to clinical development. Before testing potential product candidates in humans, we carry out laboratory and animal studies to determine safety and biological activity. After completingpreclinical trials, we must file an IND, including a proposal to begin clinical trials, with the FDA. Thirty days after filing an IND, a Phase 1 human clinical trial can start,unless the FDA places a hold on the trial. Clinical trials to support a NDA are typically conducted in three sequential phases, but the phases may overlap. Phase 1—During Phase 1, the initial introduction of the drug into healthy volunteers, the drug is tested to assess metabolism, pharmacokinetics and pharmacologicalactions and safety, including side effects associated with increasing doses. Phase 2—Phase 2 usually involves trials in a limited patient population to: (1) assess the efficacy of the drug in specific, targeted indications; (2) assess dosage toleranceand optimal dosage; and (3) identify possible adverse effects and safety risks. Phase 3 (pivotal) —If a compound is found to be potentially effective and to have an acceptable safety profile in Phase 2 evaluations, Phase 3 clinical trials, also calledpivotal studies, major studies or advanced clinical trials, are undertaken to further demonstrate clinical efficacy and to further test for safety within an expanded patientpopulation at geographically dispersed clinical trial sites. In general, the FDA requires that at least two adequate and well-controlled Phase 3 clinical trials be conducted. Initiation and completion of the clinical trial phases are dependent on several factors including things that are beyond our control. For example, the clinical trials cannotbegin at a particular site until that site receives approval from its Institutional Review Board (“IRB”), which reviews the protocol and related documents. This process can takefrom several weeks to several months. In addition, clinical trials are dependent on patient enrollment, but the rate at which patients enroll in the study depends on: • willingness of investigators to participate in a study; 17 • ability of clinical sites to obtain approval from their IRB; • the availability of the required number of eligible subjects to be enrolled in a given trial; • the availability of existing or other experimental drugs for the disease we intend to treat; • the willingness of patients to participate; and • the patients meeting the eligibility criteria. Delays in planned patient enrollment may result in increased expense and longer development timelines. After successful completion of the required clinical testing, generally an NDA is submitted. Upon receipt of the NDA, the FDA will review the application forcompleteness. Within 60 days, the FDA will determine if the application is sufficiently complete to warrant full review and will consider the application “filed” at that time.Also upon receipt of the application, the FDA will assign a review priority to the application. Priority review applications are usually reviewed within 8 months; standardreview applications are usually reviewed within 12 months. The FDA will usually refer NDAs for new molecular entities to an appropriate advisory committee for review andevaluation in regards to providing a recommendation as to whether the application should be approved. The FDA is not bound to follow the recommendation of an advisorycommittee. Following the review of the application, which may include requests for additional information from the sponsor and results from inspections of manufacturing andclinical sites, the FDA will issue an “action letter” on the application. The action letter will either be an “approval letter,” in which case the product may be lawfully marketedin the United States, or a “complete response letter.” A complete response letter will state that the FDA cannot approve the NDA in its present form and, usually, will describeall of the specific deficiencies that the FDA has identified in the application. The complete response letter, when possible, will include the FDA’s recommended actions toplace the application in a condition for approval. Deficiencies can be minor (e.g., labeling changes) or major (e.g., requiring additional clinical trials). A complete responseletter may also be issued before the FDA conducts the required facility inspection and/or reviews labeling, leaving the possibility that additional deficiencies in the originalNDA could be subsequently cited. An applicant receiving a complete response letter is permitted to resubmit the NDA addressing the identified deficiencies (in which case anew two or six month review cycle will begin), or withdraw the NDA. The FDA may consider a failure to take action within one year of a complete response letter to be arequest to withdraw, unless the applicant has requested an extension of time in which to resubmit. If the FDA approves an NDA, the marketing of the product will be limitedto the particular disease states and conditions of use that are described in the product label. We and all of our contract manufacturers are also required to comply with the applicable FDA current Good Manufacturing Practice, or cGMP, regulations duringclinical development and to ensure that the product can be consistently manufactured to meet the specifications submitted in an NDA. The cGMP regulations includerequirements relating to product quality as well as the corresponding maintenance of records and documentation. Manufacturing facilities must be approved by the FDAbefore they can be used to manufacture our products. Based on an inspection, the FDA determines whether manufacturing facilities are in compliance with applicableregulations. Manufacturing facilities in non-United States countries that are utilized to manufacture drugs for distribution into the United States are also subject to inspectionby the FDA. Additionally, failure to comply with local regulatory requirements could affect production and availability of product in relevant markets. Human Resources As of January 31, 2016, we had approximately 70 employees, of whom approximately 50 were engaged in the research and development function of our operations. Ourresearch and development staff, 24 of whom hold Ph.D. or M.D. degrees, have diversified experience in biochemistry, pharmacology, X-ray crystallography, synthetic organicchemistry, computational chemistry, medicinal chemistry, clinical development and regulatory affairs. Our employees are not represented by any collective bargaining agreements, and we have never experienced a work stoppage. Employees are required to executeconfidentiality and assignment of intellectual property agreements. We consider our relations with our employees to be satisfactory. Available Information We have available a website on the Internet. Our address is www.biocryst.com. We make available, free of charge, at our website our Annual Reports on Form 10-K,Quarterly Reports on Form 10-Q, Current Reports on Form 8-K, and amendments to those reports filed or furnished pursuant to Section 13(a) or 15(d) of the Exchange Act assoon as reasonably practicable after we electronically file such material with, or furnish it to, the SEC. We also make available at our website copies of our audit committeecharter, compensation committee charter, corporate governance and nominating committee charter and our code of business conduct, which applies to all our employees aswell as the members of our Board of Directors. Any amendment to, or waiver from, our code of business conduct will be posted on our website. 18 Financial Information For information related to our revenues, profits, net loss and total assets, in addition to other financial information, please refer to the Financial Statements and Notes toFinancial Statements contained in this Annual Report. Financial information about revenues derived from foreign countries is included in Note 1 to the Financial Statementscontained in this Annual Report. ITEM 1A. RISK FACTORS An investment in our stock involves risks. You should carefully read this entire report and consider the following uncertainties and risks, which may adversely affect ourbusiness, financial condition or results of operations, along with all of the other information included in our other filings with the Securities and Exchange Commission,before deciding to buy our common stock. Risks Relating to Our Business We have incurred losses since our inception, expect to continue to incur such losses, and may never be profitable. Since our inception, we have not achieved sustained profitability. We expect to incur additional losses for the foreseeable future, and our losses could increase as ourresearch and development efforts progress. We expect that such losses will fluctuate from quarter to quarter and losses and fluctuations may be substantial. To become profitable, we, or our collaborative partners, must successfully manufacture and develop product candidates, receive regulatory approval, and successfullycommercialize and/or enter into profitable agreements with other parties. It could be several years, if ever, before we receive significant revenue from any current or futurelicense agreements or revenues directly from product sales. Because of the numerous risks and uncertainties associated with developing our product candidates and their potential for commercialization, we are unable to predictthe extent of any future losses. Even if we do achieve profitability, we may not be able to sustain or increase profitability on a quarterly or annual basis. If we are unable toachieve and sustain profitability, the market value of our common stock will likely decline. Our success depends upon our ability to advance our products through the various stages of development, especially through the clinical trial process. To receive the regulatory approvals necessary for the sale of our product candidates, we or our partners must demonstrate through preclinical studies and clinical trialsthat each product candidate is safe and effective. The development process and related regulatory process are complex and uncertain. Because of the cost and duration ofclinical trials, we may decide to discontinue development of product candidates that are unlikely to show good results in the clinical trials, unlikely to help advance a productto the point of a meaningful collaboration, or unlikely to have reasonable commercial potential. We may suffer significant setbacks in pivotal pre-clinical studies and clinicaltrials (e.g. BCX4430, avoralstat, BCX7353 and our other rare disease product candidates), even after earlier clinical trials show promising results. The development of ourproduct candidates, including our clinical trials, may not be adequately designed or executed, which could affect the potential outcome and analysis of study results. Any ofour product candidates may produce undesirable side effects in humans. The pre-clinical and clinical data from our product candidates could cause us or regulatory authoritiesto interrupt, delay, modify or halt preclinical or clinical trials of a product candidate. Undesirable or inconclusive data or side effects in humans could also result in the FDAor foreign regulatory authorities refusing to approve the product candidate for any targeted indications. In addition, the FDA or other regulatory agencies may determine thatstudy data from our product candidates necessitates additional studies or study designs which differ from our planned development strategy, and regulatory agencies may alsorequire patient monitoring and testing or may implement restrictions or other conditions on our development activities, any of which could materially impact the cost andtiming of our planned development strategy. We, our partners, the FDA or foreign regulatory authorities may suspend or terminate clinical trials at any time if we or theybelieve the trial participants face unacceptable health risks. Clinical trials may fail to demonstrate that our product candidates are safe or effective and have acceptablecommercial viability. Regulatory authorities may interrupt, delay or halt clinical trials for a product candidate for any number of reasons. Our ability to successfully complete clinical trials is dependent upon many factors, including but not limited to: •our ability to find suitable clinical sites and investigators to enroll patients;19 •the ability to maintain contact with patients to provide complete data after treatment; •our product candidates may not prove to be either safe or effective; •clinical protocols or study procedures may not be adequately designed or followed by the investigators; •formulation improvements may not work as expected, which could negatively impact commercial demand for our product candidates; •manufacturing or quality control problems could affect the supply of product candidates for our trials; and •delays or changes in our planned development strategy, the regulations or guidelines, or other unexpected conditions or requirements by governmental agencies. Clinical trials are lengthy and expensive. We or our partners incur substantial expense for, and devote significant time to, preclinical testing and clinical trials, yet wecannot be certain that the tests and trials will ever result in the commercial sale of a product. For example, clinical trials require adequate supplies of drug and sufficientpatient enrollment. Lack of adequate drug supply or delays in patient enrollment can result in increased costs and longer development times. Even if we or our partnerssuccessfully complete clinical trials for our product candidates, we or our partners might not file the required regulatory submissions in a timely manner and may not receiveregulatory approval for the product candidates. We focus on rare diseases, which may create additional risks and challenges. Because we focus on developing drugs as treatments for rare diseases, we may seek orphan drug, breakthrough therapy or fast track designations for our productcandidates in the United States or the equivalent designations elsewhere in the world. Often, regulatory agencies have broad discretion in determining whether or not to grantsuch designations. We cannot guarantee that we will be able to receive orphan drug status from the FDA or equivalent regulatory designations elsewhere. We also cannotguarantee that we will obtain breakthrough therapy or fast track designation, which may provide certain potential benefits such as more frequent meetings with the FDA todiscuss the development plan, intensive guidance on an efficient drug development program, and potential eligibility for rolling review or priority review. Even if we aresuccessful in obtaining any such designation by the FDA or other regulatory agency for our product candidates, such designations may not lead to faster development orregulatory review or approval, and it does not increase the likelihood that our product candidates will receive marketing approval. We may not be able to obtain or maintainsuch designations for our product candidates, and our competitors may obtain these designations for their product candidates, which could impact our ability to develop andcommercialize our product candidates or compete with such competitors, which may adversely impact our business, financial condition or results of operations. We have received orphan and fast track designations for avoralstat in the United States. Despite this designation; we may not experience a faster development, reviewor approval process compared to the conventional FDA procedures. The FDA may withdraw fast track designation if it believes the designation is no longer supported by datafrom our clinical development program. Although we have also received Sakigake designation for BCX7353 in Japan, we may not experience a faster development, review orapproval process compared to the conventional process. Our clinical trials may not adequately show that our product candidates are safe or effective. Progression of our product candidates through the clinical development process is dependent upon our trials indicating our product candidates have adequate safety andefficacy in the patients being treated by achieving pre-determined safety and efficacy endpoints according to the clinical trial protocols. Failure to achieve any of theseendpoints in any of our programs, including avoralstat, BCX7353 and our other rare disease product candidates, could result in delays in our trials or require the performanceof additional unplanned trials. This could result in delays in the development of our product candidates and could result in significant unexpected costs or the termination ofprograms. If our development collaborations with third parties, such as our development partners and contract research organizations, fail, the development of our productcandidates will be delayed or stopped. We rely heavily upon third parties for many important stages of our product candidate development, including but not limited to: •discovery of compounds that cause or enable biological reactions necessary for the progression of the disease or disorder, called enzyme targets;20 •licensing or designing of enzyme inhibitors for development as product candidates; •execution of certain preclinical studies and late-stage development for our compounds and product candidates; •management of our clinical trials, including medical monitoring and data management; •execution of additional toxicology studies that may be required to obtain approval for our product candidates; •formulation improvement strategies and methods, including those for avoralstat; and •manufacturing the starting materials and drug substance required to formulate our products and the product candidates to be used in our clinical trials, toxicologystudies and any potential commercial product. Our failure to engage in successful collaborations at any one of these stages would greatly impact our business. If we do not license enzyme targets or inhibitors fromacademic institutions or from other biotechnology companies on acceptable terms, our drug development efforts would suffer. Similarly, if the contract research organizationsthat conduct our initial or late-stage clinical trials, conduct our toxicology studies, manufacture our starting materials, drug substance and product candidates or manage ourregulatory function breached their obligations to us or perform their services inconsistent with industry standards and not in accordance with the required regulations, thiswould delay or prevent both the development of our product candidates and the availability of any potential commercial product. If we lose our relationship with any one or more of these parties, we could experience a significant delay in both identifying another comparable provider and thencontracting for its services. We may be unable to retain an alternative provider on reasonable terms, if at all. Even if we locate an alternative provider, it is likely that thisprovider may need additional time to respond to our needs and may not provide the same type or level of service as the original provider. In addition, any provider that weretain will be subject to applicable FDA current Good Laboratory Practices (“cGLP”), current Good Manufacturing Practices (“cGMP”) and current Good Clinical Practices(“cGCP”), and comparable foreign standards. We do not have control over compliance with these regulations by these providers. Consequently, if these practices andstandards are not adhered to by these providers, the development and commercialization of our product candidates could be delayed. If any of the foregoing risks are realized,our business, financial condition and results of operations could be materially adversely affected. Because we have limited manufacturing experience, we depend on third-party manufacturers to manufacture our product, product candidates and the materials forour product candidates. Often, especially early in the development and commercialization process, we have only one source for manufacturing. If we cannot rely onexisting third-party manufacturers, we will be required to incur significant costs and potential delays in finding new third-party manufacturers. We have limited manufacturing experience and only a small scale manufacturing facility. We currently rely upon a very limited number of third-party manufacturers tomanufacture the materials required for our product, product candidates and most of the preclinical and clinical quantities of our product candidates. We depend on these third-party manufacturers to perform their obligations in a timely manner and in accordance with applicable governmental regulations. Our third-party manufacturers, which maybe the only manufacturer we have engaged for a particular product, may encounter difficulties with meeting our requirements including but not limited to problems involving: •inconsistent production yields; •product liability claims or recalls of commercial product; •difficulties in scaling production to commercial and validation sizes; •interruption of the delivery of materials required for the manufacturing process; •scheduling of plant time with other vendors or unexpected equipment failure; •potential catastrophes that could strike their facilities or have an effect on infrastructure; •potential impurities in our drug substance or products that could affect availability of product for our clinical trials or future commercialization;21 •poor quality control and assurance or inadequate process controls; and •lack of compliance or cooperation with regulations and specifications or requests set forth by the FDA or other foreign regulatory agencies, particularly associatedwith RAPIVAB and planned studies for avoralstat, BCX7353 and BCX4430. These contract manufacturers may not be able to manufacture the materials required for our product candidates at a cost or in quantities necessary to make themcommercially viable. We also have no control over whether third-party manufacturers breach their agreements with us or whether they may terminate or decline to renewagreements with us. To date, our third-party manufacturers have met our manufacturing requirements, but they may not continue to do so. Furthermore, changes in themanufacturing process or procedure, including a change in the location where the drug is manufactured or a change of a third-party manufacturer, may require prior reviewand approval in accordance with the FDA’s cGMP and comparable foreign requirements. This review may be costly and time-consuming and could delay or prevent thelaunch of a product. The FDA or similar foreign regulatory agencies may at any time implement new standards, or change their interpretation and enforcement of existingstandards for manufacture, packaging or testing of products. If we or our contract manufacturers are unable to comply, we or they may be subject to regulatory action, civilactions or penalties any of which could be costly to the Company and could result in a delay or shortage of product. If we are unable to maintain current manufacturing or other contract relationships, or enter into new agreements with additional manufacturers on commerciallyreasonable terms, or if there is poor manufacturing performance or failure to comply with any regulatory agency on the part of any of our third-party manufacturers, we maynot be able to complete development of, seek timely approval of, or market, our product candidates. Our raw materials, drug substances, and product candidates are manufactured by a limited group of suppliers, including some at a single facility. If any of thesesuppliers were unable to produce these items, this could significantly impact our supply of product candidate material for further preclinical testing and clinical trials. We face intense competition, and if we are unable to compete effectively, the demand for our products, if any, may be reduced. The biotechnology and pharmaceutical industries are highly competitive and subject to rapid and substantial technological change. There are many companies seekingto develop products for the same indications that we currently target. Our competitors in the United States and elsewhere are numerous and include, among others, majormultinational pharmaceutical and chemical companies and specialized biotechnology firms. Most of these competitors have greater resources than we do, including greaterfinancial resources, larger research and development staffs and more experienced marketing and manufacturing organizations. In addition, most of our competitors havegreater experience than we do in conducting clinical trials and obtaining FDA and other regulatory approvals. Accordingly, our competitors may succeed in obtaining FDA orother regulatory approvals of product candidates more rapidly than we do. Companies that complete clinical trials, obtain required regulatory approvals, and commencecommercial sale of their drugs before we do may achieve a significant competitive advantage, including patent and FDA exclusivity rights that would delay our ability tomarket products. We face, and will continue to face, competition in the licensing of potential product candidates for desirable disease targets licensing of desirable productcandidates, and development and marketing of our product candidates from academic institutions, government agencies, research institutions and biotechnology andpharmaceutical companies. Competition may also arise from, among other things: •other drug development technologies; •methods of preventing or reducing the incidence of disease, including vaccines; and •new small molecule or other classes of therapeutic agents. Developments by others may render our product candidates or technologies obsolete or noncompetitive. We and our partners are performing research on or developing products for the treatment of several disorders including HAE and recurrent/refractory peripheral T-celllymphoma, as well as broad spectrum antivirals that may be developed as medical countermeasures. We expect to encounter significant competition for any of thepharmaceutical products we plan to develop. Companies that complete clinical trials, obtain required funding or government support, obtain required regulatory approvals andcommence commercial sales or stockpiling orders of their products before their competitors may achieve a significant competitive advantage. Such is the case with Eisai Co.Ltd.’s TARGRETIN ® for cutaneous T-lymphoma; the current neuraminidase inhibitors marketed by GSK and Roche for influenza; CINRYZE ® , KALBITOR ® andFIRAZYR ® , marketed by Shire Pharmaceuticals, Inc. for HAE; and BERINERT ® , marketed by CSL for HAE. Therapeutic products with potentially promising data totreat Ebola include Mapp Biopharmaceutical, Inc.’s ZMapp (antibody-based) and Gilead Sciences, Inc.’s product currently under development (small molecule), both ofwhich have been used in Ebola infected patients. Further, several pharmaceutical and biotechnology firms, including major pharmaceutical companies and specializedstructure-based drug design companies, have announced efforts in the field of structure-based drug design and molecules in development in the fields of HAE and in othertherapeutic areas where we have discovery and development efforts ongoing. If one or more of our competitors’ products or programs are successful, the market for ourproducts may be reduced or eliminated. 22 Compared to us, many of our competitors and potential competitors have substantially greater: •capital resources; •research and development resources, including personnel and technology; •regulatory experience; •preclinical study and clinical testing experience; •manufacturing and marketing experience; and •production facilities. Any of these competitive factors could impede our funding efforts, render technology and product candidates noncompetitive or eliminate or reduce demand for ourproduct candidates. We face risks related to our government-funded programs; if BARDA/HHS or NIAID/HHS were to eliminate, reduce or delay funding from our contracts, thiswould have a significant negative impact on the programs associated with such funding and could have a significant negative impact on our revenues and cashflows. Our projections of revenues and incoming cash flows are substantially dependent upon BARDA/HHS and NIAID/HHS reimbursement for the costs related to ourBCX4430 program. If BARDA/HHS or NIAID/HHS were to eliminate, reduce or delay the funding for these programs or disallow some of our incurred costs, we would haveto obtain additional funding for continued development or regulatory registration for these product candidates or significantly reduce or stop the development effort. In contracting with BARDA/HHS and NIAID/HHS, we are subject to various U.S. Government contract requirements, including general clauses for a cost-reimbursement research and development contract, which may limit our reimbursement or if we are found to be in violation could result in contract termination. If the U.S.Government terminates any of its contracts with us for its convenience, or if we default by failing to perform in accordance with the contract schedule and terms, significantnegative impact on our cash flows and operations could result. Our government contracts with BARDA/HHS and NIAID/HHS have special contracting requirements, which create additional risks of reduction or loss of funding. We have completed work under a contract with BARDA/HHS for the development of our neuraminidase inhibitor, peramivir. We also have entered into contracts withBARDA/HHS and NIAID/HHS for the development of BCX4430 as a treatment for diseases caused by RNA pathogens, including Marburg virus disease and Ebola virusdisease. In contracting with these government agencies, we are subject to various U.S. Government contract requirements, including general clauses for a cost-reimbursementresearch and development contract, which may limit our reimbursement or, if we are found to be in violation, could result in contract termination. U.S. Government contracts typically contain a number of extraordinary provisions that would not typically be found in commercial contracts and which may create adisadvantage and additional risks to us as compared to competitors that do not rely on U.S. Government contracts. These risks include the ability of the U.S. Government tounilaterally: •terminate or reduce the scope of our contract with or without cause; •interpret relevant regulations (federal acquisition regulation clauses); •require performance under circumstances which may not be favorable to us; •require an in process review where the U.S. Government will review the project and its options under the contract;23 •control the timing and amount funding, which impacts the development progress of our programs; and •audit and object to our contract-related costs and fees, including allocated indirect costs. Our government contracts with BARDA/HHS and NIAID/HHS have termination and audit provisions which create additional risks to us. The U.S. Government may terminate its contracts with us either for its convenience or if we default by failing to perform in accordance with the contract schedule andterms. Termination for convenience provisions generally enable us to recover only our costs incurred or committed, and settlement expenses and profit on the work completedprior to termination. Termination does not permit these recoveries under default provisions. In the event of termination or upon expiration of a contract, the U.S. Governmentmay dispute wind-down and termination costs and may question prior expenses under the contract and deny payment of those expenses. Should we choose to challenge theU.S. Government for denying certain payments under a contract, such a challenge could subject us to substantial additional expenses which we may or may not recover.Further, if the U.S. Government terminates its contracts with us for its convenience, or if we default by failing to perform in accordance with the contract schedule and terms,significant negative impact on our cash flows and operations could result. As a U.S. Government contractor, we are required to comply with applicable laws, regulations and standards relating to our accounting practices and are subject toperiodic audits and reviews. As part of any such audit or review, the U.S. Government may review the adequacy of, and our compliance with, our internal control systems andpolicies, including those relating to our purchasing, property, estimating, compensation and management information systems. Audits conducted by the U.S. Government forthe completed BARDA/HHS contract have been performed and concluded through fiscal 2009; all subsequent fiscal years are still open and auditable. Audits under the activeBARDA/HHS and NIAID/HHS contracts may occur at the election of the U.S. Government and have been concluded through fiscal 2013. Based on the results of its audits,the U.S. Government may adjust our contract-related costs and fees, including allocated indirect costs. This adjustment could impact the amount of revenues reported on ahistoric basis and could impact our cash flows under the contracts prospectively. In addition, in the event BARDA/HHS or NIAID/HHS determines that certain costs and feeswere unallowable or determines that the allocated indirect cost rate was higher than the actual indirect cost rate, BARDA/HHS or NIAID/HHS would be entitled to recoup anyoverpayment from us as a result. In addition, if an audit or review uncovers any improper or illegal activity, we may be subject to civil and criminal penalties andadministrative sanctions, including termination of our contracts, forfeiture of profits, suspension of payments, fines and suspension or prohibition from doing business withthe U.S. Government. We could also suffer serious harm to our reputation if allegations of impropriety were made against us. In addition, under U.S. Government purchasingregulations, some of our costs may not be reimbursable or allowed under our contracts. Further, as a U.S. Government contractor, we are subject to an increased risk ofinvestigations, criminal prosecution, civil fraud, whistleblower lawsuits and other legal actions and liabilities as compared to private sector commercial companies. If we fail to reach milestones or to make annual minimum payments or otherwise breach our obligations under our license agreements, our licensors may terminateour agreements with them and seek additional remedies. If we are unable or fail to meet payment obligations, performance milestones relating to the timing of regulatory filings, product supply obligations, post approvalcommitments for RAPIVAB, or development and commercial diligence obligations; are unable or fail to make milestone payments or material data use payments inaccordance with applicable provisions; or fail to pay the minimum annual payments under our respective licenses, our licensors may terminate the applicable license or seekother available remedies. As a result, our development of the respective product candidate or commercialization of the product would cease. If we fail to obtain additional financing or acceptable partnership arrangements, we may be unable to complete the development and commercialization of ourproduct candidates or continue operations. As our programs advance, our costs are likely to increase. Our current and planned discovery activities, pre-clinical and clinical trials, the related development,manufacturing, regulatory approval process requirements, and the additional personnel resources and testing required for supporting the development of our productcandidates will consume significant capital resources. Our expenses, revenues and cash utilization rate could vary significantly depending on many factors, including: ourability to raise additional capital; the development progress of our collaborative agreements for our product candidates; the amount of funding we receive from NIAID/HHSand BARDA/HHS for BCX4430 or from other new partnerships with third parties for the development of our product candidates, including avoralstat, BCX7353 and ourother rare disease product candidates; the commercial success of peramivir achieved by our partners; the amount or profitability of any orders for RAPIVAB or BCX4430 byany government agency or other party; the progress and results of our current and proposed clinical trials for our most advanced product candidates, including avoralstat,BCX7353 and our other rare disease product candidates; the progress made in the manufacture of our lead products and the progression of our other programs. 24 We expect that we will be required to raise additional capital to complete the development and commercialization of our current product candidates and we may seek toraise capital at any time. Additional funding, whether through additional sales of securities or collaborative arrangements with partners, including governmental agencies ingeneral and from any BARDA/HHS or NIAID/HHS contract specifically, may not be available when needed or on terms acceptable to us. The issuance of preferred orcommon stock or convertible securities, with terms and prices significantly more favorable than those of the currently outstanding common stock, could have the effect ofdiluting or adversely affecting the holdings or rights of our existing stockholders. In addition, collaborative arrangements may require us to transfer certain material rights tosuch corporate partners. Insufficient funds or lack of an acceptable partnership may require us to delay, scale-back or eliminate certain of our research and developmentprograms. In order to continue future operations and continue our drug development programs, we will be required to raise additional capital. In addition to seeking strategicpartnerships, transactions and government funding, we may decide to access the equity or debt markets or seek other sources to meet liquidity needs. Our ability to raiseadditional capital may be limited and may greatly depend upon the success of ongoing development related to our current drug development programs, including postapproval studies for RAPIVAB, the progress, timeline and ultimate outcome of the avoralstat development program (including, but not limited to, formulation trials, phase 3trials, long-term human safety studies, and the timing of carcinogenicity studies), the progress of BCX7353 and our other rare disease product candidates, funding for andcontinued successful development of BCX4430, and the progress of our early discovery programs. In addition, constriction and volatility in the equity and debt markets mayrestrict our future flexibility to raise capital when such needs arise. Furthermore, we have exposure to many different industries, financing partners and counterparties,including commercial banks, investment banks and partners (which include investors, licensing partners, and the U.S. Government) which may be unstable or may becomeunstable in the current economic and political environment. Any such instability may impact these parties’ ability to fulfill contractual obligations to us or they might limit orplace burdensome conditions upon future transactions with us. Also, it is possible that suppliers may be negatively impacted. Any such unfavorable outcomes in our currentprograms or unfavorable economic conditions could place severe downward pressure on the price of our common stock and may decrease opportunities to raise capital in thecapital or credit markets, and further could reduce the return available on invested corporate cash, which, if severe and sustained, could have a material and adverse impact onour results of operations and cash flows and limit our ability to continue development of our product candidates. If we fail to successfully commercialize or establish collaborative relationships to commercialize certain of our product candidates, or if any partner terminates orfails to perform its obligations under agreements with us, potential revenues from commercialization of our product candidates could be reduced, delayed oreliminated. Our business strategy is to increase the asset value of our product candidate portfolio. We believe this is best achieved by retaining full product rights or throughcollaborative arrangements with third parties as appropriate. As needed, potential third-party relationships could include preclinical development, clinical development,regulatory approval, marketing, sales and distribution of our product candidates. Currently, we have established collaborative relationships with Mundipharma for the development and commercialization of forodesine and with each of Shionogi andGreen Cross for the development and commercialization of peramivir, in Japan, Taiwan and South Korea. Most recently we have established a collaborative relationship withSeqirus UK Limited for RAPIVAB in the United States and countries other than Israel, Japan, Korea and Taiwan. The process of establishing and implementing collaborativerelationships is difficult, time-consuming and involves significant uncertainty, including: •our partners may seek to renegotiate or terminate their relationships with us due to unsatisfactory clinical results, including post approval clinical commitments, achange in business strategy, a change of control or other reasons; •our contracts for collaborative arrangements may expire; •our partners may choose to pursue alternative technologies, including those of our competitors; •we may have disputes with a partner that could lead to litigation or arbitration; •we do not have day to day control over the activities of our partners and have limited control over their decisions; •our ability to generate future event payments and royalties from our partners depends upon their abilities to establish the safety and efficacy of our productcandidates, obtain regulatory approvals and achieve market acceptance of products developed from our product candidates;25 •we or our partners may fail to properly initiate, maintain or defend our intellectual property rights, where applicable, or a party may utilize our proprietaryinformation in such a way as to invite litigation that could jeopardize or potentially invalidate our proprietary information or expose us to potential liability; •we or our partners may not devote sufficient capital or resources towards our product candidates; and •we or our partners may not comply with applicable government regulatory requirements. If we or our partners fail to fulfill our responsibilities in a timely manner, or at all, our commercialization efforts related to that collaboration could be reduced, delayedor terminated, or it may be necessary for us to assume responsibility for activities that would otherwise have been the responsibility of our partner. If we are unable toestablish and maintain collaborative relationships on acceptable terms, we may have to delay or discontinue further development of one or more of our product candidates,undertake commercialization activities at our own expense or find alternative sources of funding. Any delay in the development or commercialization of our productcandidates would severely affect our business, because if our product candidates do not progress through the development process or reach the market in a timely manner, orat all, we may not receive additional future event payments and may never receive milestone, product sales or royalty payments. We do not have a great deal of experience in commercializing our products or technologies, and our future revenue generation is uncertain. We do not have a great deal of experience in commercializing our products or technologies. We currently have limited marketing and commercial capability, no director third-party sales force and limited distribution capabilities. We may be unable to establish or sufficiently increase these capabilities for products we currently, or plan to,commercialize. In addition, our revenue from collaborative agreements may be dependent upon the status of our preclinical and clinical programs. If we fail to advance theseprograms to the point of being able to enter into successful collaborations, we will not receive any potential future event or other collaborative payments. Our ability to receive revenue from products we commercialize presents several risks, including: •we or our collaborators may fail to successfully complete clinical trials, or satisfy post-marketing commitments, sufficient to obtain and keep FDA marketingapproval; •many competitors are more experienced and have significantly more resources, and their products could reach the market faster, be more cost effective or have abetter efficacy or tolerability profile than our product candidates; •we may fail to employ a comprehensive and effective intellectual property strategy, which could result in decreased commercial value of our Company and ourproducts; •we may fail to employ a comprehensive and effective regulatory strategy, which could result in a delay or failure in commercialization of our products; •our ability to successfully commercialize our products is affected by the competitive landscape, which cannot be fully known at this time; •reimbursement is constantly changing, which could greatly affect usage of our products; and •future revenue from product sales would depend on our ability to successfully complete clinical studies, obtain regulatory approvals, and manufacture, market andcommercialize our approved drugs. Commercialization of RAPIVAB by our partners is subject to the potential commercialization risks described herein and numerous additional risks. Any potentialrevenue benefits to us in the form of milestone payments, royalties or other consideration are highly speculative. Commercialization success of RAPIVAB is uncertain and is subject to all the risks and uncertainties disclosed in our other risk factors relating to drug developmentand commercialization. In addition, commercialization of RAPIVAB is subject to further risks and may be negatively impacted by a number of factors, including, but notlimited to, the following: •RAPIVAB may not prove to be adequately safe and effective for market approval in markets other than the United States;26 •necessary funding for post-marketing commitments and further development of RAPIVAB may not be available timely, at all, or in sufficient amounts; •flu prevention or pandemic treatment concerns may not materialize at all, or in the near future; •advances in flu vaccines or other antivirals, including competitive i.v. antivirals, could substantially replace potential demand for RAPIVAB; •a limited number of governmental entities are expected to be the primary potential stockpiling customers for RAPIVAB and if we are not successful at marketingRAPIVAB to these entities for any reason, we will not receive substantial revenues from stockpiling orders; •government and third party payors may not provide sufficient coverage or reimbursement which would negatively impact the demand for RAPIVAB; •we may not be able to supply commercial material to our partners and our partners may not be able to maintain or establish sufficient and acceptable commercialmanufacturing, either directly or through third-party manufacturers; •the commercial demand and acceptance for RAPIVAB by healthcare providers and by patients may not be sufficient to result in substantial revenues of RAPIVAB toour partners and may result in little to no milestones or royalties to us; •effectiveness of marketing efforts for RAPIVAB by our partners; •market satisfaction with existing alternative therapies; •perceived efficacy relative to other available therapies; •disease prevalence; •cost of treatment; •pricing and availability of alternative products; •marketing and sales activities of competitors; •shifts in the medical community to new treatment paradigms or standards of care; and •relative convenience and ease of administration. We are subject to various federal and state laws related to RAPIVAB and other products under development and, if we or our partners do not comply with theseregulations, we could face substantial penalties. Our or our partners activities related to RAPIVAB, or any of our other products under development and following their regulatory approval, are subject to regulatoryand law enforcement authorities in addition to the FDA, including the Federal Trade Commission, the Department of Justice, and state and local governments. In the case ofour collaboration with SUL, although SUL is responsible for RAPIVAB marketing and commercialization efforts, we continue to carry certain risks associated withRAPIVAB because we hold the RAPIVAB NDA. For example, we are responsible for reporting adverse drug experiences, we have responsibility for certain post-approvalstudies, we may have responsibilities and costs related to a recall or withdrawal of RAPIVAB from sale, we may incur liability associated with RAPIVAB manufacturingcontracted by us or in support of any of our partners, we are required to maintain records and provide data and reports to regulatory agencies related to RAPIVAB (e.g. riskevaluation and mitigation strategies, track and trace requirements, adverse events), and we may incur certain promotional regulatory and government pricing risks, all ofwhich could have a material adverse impact on our operations and financial condition. In addition, we are now subject to the federal physician sunshine act and certain similarlegislation in various states. We are subject to various federal and state laws pertaining to health care “fraud and abuse,” including both federal and state anti-kickback laws.Although we seek to comply with these statutes, it is possible that our practices, or those of our distributors, might be challenged under anti-kickback or similar laws.Violations of the physician sunshine act and similar state legislation or the fraud and abuse laws may be punishable by civil or criminal sanctions, including fines and civilmonetary penalties, and future exclusion from participation in government healthcare programs. 27 We have a number of outstanding post-marketing commitments to the FDA that we retain, despite our partnership with SUL, which we may not complete successfullyor on time for any number of reasons, including but not limited to lack of funds to complete the studies and insufficient interest by appropriate sites, investigators or studysubjects. For example, as a condition of the approval of RAPIVAB, we are required to complete a pediatric patient study of RAPIVAB and to submit the final results of thisclinical trial to the FDA. Depending on the outcome of this clinical trial, we may be unable to expand the indication for RAPIVAB or we may be required to include specificwarnings or limitations on dosing this product, which could negatively impact sales of RAPIVAB and negatively impact our relationship with our partner. We may be subjectto penalties if we fail to comply with post-approval legal and regulatory requirements and our products could be subject to continual recordkeeping and reportingrequirements, review and periodic inspections by the FDA and other regulatory bodies. Regulatory approval of a product may be subject to limitations on the indicated usesfor which the product may be marketed or to the other restrictive conditions of approval that limit our ability to promote, sell or distribute a product. Furthermore, theapproval of RAPIVAB and any other future product candidates may be subject to requirements for costly post-marketing testing and surveillance to monitor its safety orefficacy. Advertising and promotion are subject to stringent FDA rules and oversight and as the holder of the NDA we may be held responsible for any advertising andpromotion conducted by our partner that is not in compliance with the rules and regulations. In particular, the claims in all promotional materials and activities must beconsistent with the FDA approvals for approved products, and must be appropriately substantiated and fairly balanced with information on the safety risks and limitations ofthe products. Adverse event information concerning approved products must be reviewed and as the NDA holder of RAPIVAB we are required to make expedited andperiodic adverse event reports to the FDA and other regulatory authorities. In addition, the research, manufacturing, distribution, sale and promotion of products are potentially subject to regulation by various federal, state and local authoritiesin addition to the FDA, including the Centers for Medicare and Medicaid Services, other divisions of the U.S. Department of Health and Human Services, the U.S.Department of Justice and individual U.S. Attorney offices within the Department of Justice, and state and local governments. Until we can successfully transfer the pricingresponsibilities to our partner, we remain responsible for pricing and rebate programs. Pricing and rebate programs must comply with the Medicaid rebate requirements of theOmnibus Budget Reconciliation Act of 1990, as amended, and the Veterans Health Care Act of 1992, as amended. If products are made available to authorized users of theFederal Supply Schedule of the General Services Administration, additional laws and requirements apply. All of these activities are also potentially subject to federal and stateconsumer protection and unfair competition laws. If our operations with respect to RAPIVAB or our other products that are subject to healthcare laws and regulations are found to be in violation of any of the healthcarefraud and abuse laws described above or any other governmental regulations that apply to us, we may be subject to penalties, including civil and criminal penalties, damages,fines and the curtailment or restructuring of our operations. Any penalties, damages, fines, curtailment or restructuring of our operations could adversely affect our ability tooperate our business and our financial results. Although compliance programs can mitigate the risk of investigation and prosecution for violations of these laws, the riskscannot be entirely eliminated. Any action against us for violation of these laws, even if we successfully defend against it, could cause us to incur significant legal expensesand divert our management's attention from the operation of our business. Moreover, achieving and sustaining compliance with all applicable federal and state fraud and abuselaws may be costly. We and our partners may be subject to new legislation, regulatory proposals and healthcare payor initiatives that may increase our costs of compliance and adverselyaffect our or our partners ability to market our products, including RAPIVAB, obtain collaborators and raise capital. The Patient Protection and Affordable Care Act, or PPACA, made extensive changes to the delivery of health care in the U.S. The PPACA includes numerousprovisions that affect pharmaceutical companies, some of which became effective immediately and others of which will be taking effect over the next several years. Forexample, the PPACA seeks to expand health care coverage to the uninsured through private health insurance reforms and an expansion of Medicaid. The PPACA will alsoimpose substantial costs on pharmaceutical manufacturers, such as an increase in liability for rebates paid to Medicaid, new drug discounts that must be offered to certainenrollees in the Medicare prescription drug benefit, an annual fee imposed on all manufacturers of brand prescription drugs in the U.S., and an expansion of an existingprogram requiring pharmaceutical discounts to certain types of hospitals and federally subsidized clinics. The PPACA also contains cost containment measures that couldreduce reimbursement levels for health care items and services generally, including pharmaceuticals. It also will require reporting and public disclosure of payments and othertransfers of value provided by pharmaceutical companies to physicians and teaching hospitals. We cannot predict what effect the PPACA or other healthcare reform initiativesthat may be adopted in the future will have on our business. Further, it remains unclear whether there will be any changes made to provisions of the PPACA or other healthcare laws through acts of Congress in the future. The continuing efforts of the government, insurance companies, managed care organizations and other payors of health careservices to contain or reduce costs of health care could result in decreased net revenues from our pharmaceutical products and decrease potential returns from ourdevelopment efforts. In addition, pharmaceutical and device manufacturers will also be required to report and disclose investment interests held by physicians and theirimmediate family members during the preceding calendar year. Failure to submit required information may result in civil monetary penalties for payments, transfers of valueor ownership or investment interests not reported in an annual submission. Compliance with the PPACA and state laws with similar provisions is difficult and timeconsuming, and companies that do not comply with these state laws face civil penalties. Because of the breadth of these laws and the narrowness of the safe harbors, it ispossible that some of our business activities could be subject to challenge under one or more of such laws. Such a challenge could have a material adverse effect on ourbusiness, financial condition, results of operations and growth prospects. 28 In addition, there have been a number of other legislative and regulatory proposals aimed at changing the pharmaceutical industry. In particular, legislation has beenenacted in certain states and proposed at a federal level that requires development of an electronic pedigree to track and trace each prescription drug at the saleable unit levelthrough the distribution system. Compliance with these electronic pedigree requirements may increase our operational expenses and impose significant administrativeburdens. In addition, our compliance may be deemed insufficient and we could face a material adverse effect on our business, financial condition, results of operations andgrowth prospects. As a result of these and other new proposals, we may determine to change our current manner of operation, provide additional benefits or change ourcontract arrangements, any of which could have a material adverse effect on our business, financial condition and results of operations. Managed care organizations are increasingly challenging the prices charged for medical products and services and, in some cases, imposing restrictions on the coverageof particular drugs. Many managed care organizations negotiate the price of medical services and products and develop formularies which establish pricing andreimbursement levels. Exclusion of a product from a formulary can lead to its sharply reduced usage in the managed care organization’s patient population. The process forobtaining coverage can be lengthy and costly, and we expect that it could take several months before a particular payor initially reviews our product and makes a decisionwith respect to coverage. For example, third-party payors may require cost-benefit analysis data from us in order to demonstrate the cost-effectiveness of RAPIVAB or anyother product we might bring to market. For any individual third-party payor, we may not be able to provide data sufficient to gain reimbursement on a similar or preferredbasis to competitive products, or at all which may have a material adverse effect on our business, financial condition and results of operations. There are risks related to the potential government use or sale of peramivir (RAPIVAB). United States Government use or sale of RAPIVAB in emergency situations, or otherwise, may result in the use of RAPIVAB outside of its approved use. To theextent that RAPIVAB is used as a treatment for influenza by the U.S. Government or peramivir by any other government entity, there can be no assurance that it will prove tobe generally safe, well-tolerated and effective. Such government use of peramivir may create certain liabilities for us or our partners in the case of government use outside ofthe U.S. There is no assurance that we or our manufacturers will be able to fully meet the demand for peramivir in the event of additional orders. Further, we may not achievea favorable price for additional orders of RAPIVAB in the U.S. or peramivir in any other country. Our competitors may develop products that could compete with or replaceperamivir. We may face competition in markets where we have no existing intellectual property protection or are unable to successfully enforce our intellectual propertyrights. There is no assurance that the non-U.S. partnerships that we have entered into for peramivir will result in any order for peramivir in those countries. There is noassurance that peramivir will be approved for any use or will achieve market approval in additional countries. In the event that any emergency use or market approval isgranted, there is no assurance that any government order or commercialization of peramivir in any countries will be substantial or will be profitable to us. In addition, the saleof peramivir, emergency use or other use of peramivir in any country may create certain liabilities for us and our partners. If we or our partners do not obtain and maintain governmental approvals for our product candidates under development, we or our partners will not be able to sellthese potential products, which would significantly harm our business because we will receive no revenue. We or our partners must obtain regulatory approval before marketing or selling our future product candidates. If we or our partners are unable to receive regulatoryapproval and do not market or sell our future product candidates, we will never receive any revenue from such product sales. In the United States, we or our partners mustobtain FDA approval for product candidates that we intend to commercialize. The process of preparing for and obtaining FDA approval may be lengthy and expensive, andapproval is never certain. Products distributed abroad are also subject to foreign government regulation and export laws of the United States. Because of the risks anduncertainties in biopharmaceutical development, our product candidates could take a significantly longer time to gain regulatory approval than we expect or may never gainapproval. If the FDA delays regulatory approval of our product candidates, our management’s credibility, our value and our operating results may suffer. Even if the FDA orforeign regulatory agencies approve a product candidate, the approval may limit the indicated uses for a product candidate and/or may require post-approval studies. 29 The FDA regulates, among other things, the record keeping and storage of data pertaining to potential pharmaceutical products. We currently store most of ourpreclinical research data, our clinical data and our manufacturing data at our facility. While we do store duplicate copies of most of our clinical data offsite and a significantportion of our data is included in regular backups of our systems, we could lose important data if our facility incurs damage, or if our vendor data systems fail, suffer damageor are destroyed. If we receive approval to market our potential products, whether in the United States or internationally, we will continue to be subject to extensive regulatoryrequirements. These requirements are wide ranging and govern, among other things: •adverse drug experience reporting regulations; •product promotion; •product manufacturing, including good manufacturing practice requirements; and •product changes or modifications. Our failure to comply with existing or future regulatory requirements, or our loss of, or changes to, previously obtained approvals, could have a material adverse effecton our business because we will not receive product or royalty revenues if we or our partners do not receive approval of our products for marketing. Royalties and milestone payments from Shionogi under our license agreement with Shionogi (the “Shionogi Agreement”) will be required to be used by Royalty Subto service its obligations under its PhaRMA Notes, and generally will not be available to us for other purposes until Royalty Sub has repaid in full its obligationsunder the PhaRMA Notes. In March 2011, our wholly-owned subsidiary Royalty Sub issued $30.0 million in aggregate principal amount of PhaRMA Notes. The PhaRMA Notes are securedprincipally by (i) certain royalty and milestone payments under the Shionogi Agreement, pursuant to which Shionogi licensed from us the rights to market peramivir in Japanand, if approved for commercial sale, Taiwan, (ii) rights to certain payments under a Japanese yen/U.S. dollar foreign currency hedge arrangement put into place by us inconnection with the issuance of the PhaRMA Notes and (iii) the pledge by us of our equity interest in Royalty Sub. Payments from Shionogi to us under the ShionogiAgreement will generally not be available to us for other purposes until Royalty Sub has repaid in full its obligations under the PhaRMA Notes. Accordingly, these funds willbe required to be dedicated to Royalty Sub’s debt service and not available to us for product development or other purposes. As of September 1, 2014, the payments fromShionogi were insufficient for Royalty Sub to service its obligations under the PhaRMA Notes, resulting in an event of default with respect to the PhaRMA Notes. As a resultof this event of default, the holders of the PhaRMA Notes may be able to pursue acceleration of the PhaRMA Notes and foreclose on the collateral securing the PhaRMANotes and our equity interest in Royalty Sub and may exercise other remedies available to them under the indenture or other documents related to the PhaRMA Notes. In suchevent, we may not realize the benefit of future royalty payments that might otherwise accrue to us following repayment of the PhaRMA Notes, we may incur legal costs andwe might otherwise be adversely affected. Because an event of default has occurred under the PhaRMA Notes, the holders of the PhaRMA Notes may be able to pursue acceleration of the PhaRMA Notes andforeclose on the collateral securing the PhaRMA Notes and our equity interest in Royalty Sub, in which case we may not realize the benefit of future royaltypayments that might otherwise accrue to us following repayment of the PhaRMA Notes and we could otherwise be adversely affected. Royalty Sub’s ability to service its payment obligations in respect of the PhaRMA Notes, and our ability to benefit from our equity interest in Royalty Sub, is subject tonumerous risks. Royalty Sub’s ability to service the PhaRMA Notes may be adversely affected by, among other things, changes in or any termination of our relationship withShionogi, reimbursement, regulatory, manufacturing and/or intellectual property issues, product returns, product recalls, product liability claims and allegations of safetyissues, as well as other factors. As Royalty Sub has been unable to service its obligations under the PhaRMA Notes and an event of default has occurred under the PhaRMANotes, the holders of the PhaRMA Notes may be able to pursue acceleration of the PhaRMA Notes and foreclose on the collateral securing the PhaRMA Notes and our equityinterest in Royalty Sub and may exercise other remedies available to them under the indenture or other documents related to the PhaRMA Notes. In such event, we may notrealize the benefit of future royalty payments that might otherwise accrue to us following repayment of the PhaRMA Notes, we may incur legal costs and we might otherwisebe adversely affected. 30 We may be required to pay significant premiums under the foreign currency hedge arrangement entered into by us in connection with the issuance of the PhaRMANotes. In addition, because our potential obligations under the foreign currency hedge are marked to market, we may experience additional quarterly volatility inour operating results and cash flows attributable to the foreign currency hedge arrangement. In connection with the issuance by Royalty Sub of the PhaRMA Notes, we entered into a foreign currency hedge arrangement to hedge certain risks associated withchanges in the value of the Japanese yen relative to the U.S. dollar. Under the foreign currency hedge agreement, we may be required to pay an annual premium in the amountof $2.0 million in each May continuing through May 2020. Such payment will be required if, in May of the relevant year, the spot rate of exchange for Japanese yen-U.S.dollars (determined in accordance with the foreign currency hedge arrangement) is such that the U.S. dollar is worth 100 yen or less. We will be required to mark-to-marketour potential obligations under the currency hedge and post cash collateral, which may cause us to experience additional quarterly volatility in our operating results and cashflows as a result. Additionally, we may be required to pay significant premiums or a termination fee under the foreign currency hedge agreement entered into by us inconnection with the issuance of the PhaRMA Notes. We are required to maintain a foreign currency hedge at 100 yen per dollar under the agreements governing the PhaRMANotes. If we fail to adequately protect or enforce our intellectual property rights or secure rights to patents of others, the value of those rights would diminish. Our success will depend in part on our ability and the abilities of our partners to obtain, protect and enforce viable intellectual property rights including but not limitedto trade name, trademark and patent protection for our Company and its products, methods, processes and other technologies we may license or develop, to preserve our tradesecrets, and to operate without infringing the proprietary rights of third parties both domestically and abroad. The patent position of biotechnology and pharmaceuticalcompanies is generally highly uncertain, involves complex legal and factual questions and has recently been the subject of much litigation. Neither the United States Patentand Trademark Office (“USPTO”), the Patent Cooperation Treaty offices, nor the courts of the United States and other jurisdictions have consistent policies nor predictablerulings regarding the breadth of claims allowed or the degree of protection afforded under many biotechnology and pharmaceutical patents. Further, we may not haveworldwide patent protection for all of our product candidates and our intellectual property rights may not be legally protected or enforceable in all countries throughout theworld. In some jurisdictions, some of our product candidates in certain programs, including our HAE program, may have short or no composition of matter patent life and wemay therefore rely on orphan drug exclusivity or data exclusivity. There can be no assurance that we will obtain orphan drug exclusivity or data exclusivity in everyjurisdiction. Further, in some jurisdictions, we may rely on formulation patents or method of use patents. Both the ability to achieve issuance and the enforcement offormulation and method of use patents can be highly uncertain and can vary from jurisdiction to jurisdiction, and such patents may therefore not adequately preventcompetitors and potential infringers in some jurisdictions. The validity, scope, enforceability and commercial value of the rights protected by such patents, therefore, is highlyuncertain. We also rely on trade secrets to protect technology in cases when we believe patent protection is not appropriate or obtainable. However, trade secrets are difficult toprotect. If we cannot maintain the confidentiality of our technology and other confidential information in connection with our collaborators and advisors, our ability to receivepatent protection or protect our proprietary information may be imperiled. We may be involved in lawsuits to protect or enforce our patents, the patents of our partners or our other intellectual property rights, which could be expensive, timeconsuming and unsuccessful . Competitors may infringe or otherwise violate our patents, the patents of our licensors or our other intellectual property rights. To counter infringement or unauthorizeduse, we may be required to file legal claims, which can be expensive and time-consuming and unsuccessful. An adverse result in any litigation or defense proceeding couldput one or more of our patents at risk. Our success depends in part on avoiding the infringement of other parties’ patents and other intellectual property rights as well asavoiding the breach of any licenses relating to our technologies and products. In the United States, patent applications filed in recent years are confidential for 18 months,while older applications are not published until the patent issues. As a result, avoiding patent infringement may be difficult and we may inadvertently infringe third-partypatents or proprietary rights. These third parties could bring claims against us, our partners or our licensors that even if resolved in our favor, could cause us to incursubstantial expenses and, if resolved against us, could additionally cause us to pay substantial damages. Further, if a patent infringement suit were brought against us, ourpartners or our licensors, we or they could be forced to stop or delay research, development, manufacturing or sales of any infringing product in the country or countriescovered by the patent we infringe, unless we can obtain a license from the patent holder. Such a license may not be available on acceptable terms, or at all, particularly if thethird party is developing or marketing a product competitive with the infringing product. Even if we, our partners or our licensors were able to obtain a license, the rights maybe nonexclusive, which would give our competitors access to the same intellectual property. 31 If we or our partners are unable or fail to adequately initiate, protect, defend or enforce our intellectual property rights in any area of commercial interest or in any partof the world where we wish to seek regulatory approval for our products, methods, processes and other technologies, the value of the product candidates to produce revenuewould diminish. Additionally, if our products, methods, processes, and other technologies or our commercial use of such products, processes, and other technologies,including but not limited to any trade name, trademark or commercial strategy infringe the proprietary rights of other parties, we could incur substantial costs. The USPTOand the patent offices of other jurisdictions have issued to us a number of patents for our various inventions and we have in-licensed several patents from various institutions.We have filed additional patent applications and provisional patent applications with the USPTO. We have filed a number of corresponding foreign patent applications andintend to file additional foreign and U.S. patent applications, as appropriate. We have also filed certain trademark and trade name applications worldwide. We cannot assureyou as to: •the degree and range of protection any patents will afford against competitors with similar products; •if and when patents will issue; •if patents do issue we cannot be sure that we will be able to adequately defend such patents and whether or not we will be able to adequately enforce such patents; or •whether or not others will obtain patents claiming aspects similar to those covered by our patent applications. If the USPTO or other foreign patent office upholds patents issued to others or if the USPTO grants patent applications filed by others, we may have to: •obtain licenses or redesign our products or processes to avoid infringement; •stop using the subject matter claimed in those patents; or •pay damages. We may initiate, or others may bring against us, litigation or administrative proceedings related to intellectual property rights, including proceedings before the USPTOor other foreign patent office. Any judgment adverse to us in any litigation or other proceeding arising in connection with a patent or patent application could materially andadversely affect our business, financial condition and results of operations. In addition, the costs of any such proceeding may be substantial whether or not we are successful. Our success is also dependent upon the skills, knowledge and experience, none of which is patentable, of our scientific and technical personnel. To help protect ourrights, we require all employees, consultants, advisors and partners to enter into confidentiality agreements that prohibit the disclosure of confidential information to anyoneoutside of our company and require disclosure and assignment to us of their ideas, developments, discoveries and inventions. These agreements may not provide adequateprotection for our trade secrets, know-how or other proprietary information in the event of any unauthorized use or disclosure or the lawful development by others of suchinformation, and if any of our proprietary information is disclosed, our business will suffer because our revenues depend upon our ability to license or commercialize ourproduct candidates and any such events would significantly impair the value of such product candidates. We face an inherent risk of liability in the event that the use or misuse of our products results in personal injury or death and our product liability insurancecoverage may be insufficient. If the use or misuse of peramivir or any other regulatory body-approved products we or a partner may sell in the future harms people, we may be subject to costly anddamaging product liability claims brought against us by consumers, healthcare providers, pharmaceutical companies, third-party payors or others. The use of our productcandidates in clinical trials, including post marketing clinical studies, could also expose us to product liability claims. We cannot predict all of the possible harms or sideeffects that may result from the use of our products or the testing of product candidates and, therefore, the amount of insurance coverage we currently may not be adequate tocover all liabilities or defense costs we might incur. A product liability claim or series of claims brought against us could give rise to a substantial liability that could exceedour resources. Even if claims are not successful, the costs of defending such claims and potential adverse publicity could be harmful to our business. We face an inherent risk of product liability exposure related to the testing of our product candidates in human clinical trials and will face even greater risks upon anycommercialization by us of our product candidates. We have product liability insurance covering our commercial sale of RAPIVAB and our clinical trials. Clinical trial andproduct liability insurance is becoming increasingly expensive. As a result, we may be unable to obtain sufficient insurance or increase our existing coverage at a reasonablecost to protect us against losses that could have a material adverse effect on our business. An individual may bring a product liability claim against us if one of our products orproduct candidates causes, or is claimed to have caused, an injury or is found to be unsuitable for consumer use. Any product liability claim brought against us, with orwithout merit, could result in: 32 •liabilities that substantially exceed our product liability insurance, which we would then be required to pay from other sources, if available; •an increase of our product liability insurance rates or the inability to maintain insurance coverage in the future on acceptable terms, or at all; •withdrawal of clinical trial volunteers or patients; •damage to our reputation and the reputation of our products, resulting in lower sales; •regulatory investigations that could require costly recalls or product modifications; •litigation costs; and •the diversion of management’s attention from managing our business. Insurance coverage is increasingly more costly and difficult to obtain or maintain. While we currently have insurance for our business, property, directors and officers, and our products insurance is increasingly more costly and narrower in scope, andwe may be required to assume more risk in the future. If we are subject to claims or suffer a loss or damage in excess of our insurance coverage, we will be required to bearany loss in excess of our insurance limits. If we are subject to claims or suffer a loss or damage that is outside of our insurance coverage, we may incur significant uninsuredcosts associated with loss or damage that could have an adverse effect on our operations and financial position. Furthermore, any claims made on our insurance policies mayimpact our ability to obtain or maintain insurance coverage at reasonable costs or at all. If our facility incurs damage or power is lost for a significant length of time, or if we incur significant cost overruns or delays in the construction of our newresearch facility in Birmingham, Alabama, our business will suffer. We store clinical and stability samples at our facility that could be damaged if our facility incurs physical damage or in the event of an extended power failure. Wehave backup power systems in addition to backup generators to maintain power to all critical functions, but any loss of these samples could result in significant delays in ourdrug development process. In addition, we store most of our preclinical and clinical data at our facilities. Duplicate copies of most critical data are secured off-site. Any significant degradation orfailure of our computer systems could cause us to inaccurately calculate or lose our data. Loss of data could result in significant delays in our drug development process andany system failure could harm our business and operations. We also face the risk that the costs and time required in connection with the construction of our new research facility in Birmingham, Alabama could exceed ourcurrent expectations. If there is a significant cost overrun or significant delay in the completion of the construction, our business, financial condition, and results of operationscould be adversely affected. A significant disruption in our information technology systems or a cyber-security breach could adversely affect our business. We are increasingly dependent on information technology systems to operate our business. Like other companies in our industry, our networks and infrastructure maybe vulnerable to cyber-attacks or intrusions, including by computer hackers, foreign governments, foreign companies or competitors, or may be breached by employee error,malfeasance or other disruption. A breakdown, invasion, corruption, destruction or interruption of critical information technology systems could negatively impactoperations. If our systems are damaged, fail to function properly or otherwise become unavailable, we may incur substantial costs to repair or replace them, and we mayexperience loss of critical data and interruptions or delays in our ability to perform critical functions, which could adversely affect our business, financial condition or resultsof operations. Any compromise of our data security could also result in a violation of applicable privacy and other laws, significant legal and financial exposure, damage toour reputation, loss or misuse of the information and a loss of confidence in our data security measures, which could harm our business. There can be no assurance that ourefforts to protect our data and information technology systems will prevent breakdowns or breaches in our systems, or those of third parties with which we do business, andany such events could adversely affect our business. 33 If we fail to retain our existing key personnel or fail to attract and retain additional key personnel, the development of our product candidates and commercializationof our products and the related expansion of our business will be delayed or stopped. We are highly dependent upon our senior management and scientific team, the unexpected loss of whose services might impede the achievement of our developmentand commercial objectives. Competition for key personnel with the experience that we require is intense and is expected to continue to increase. Our inability to attract andretain the required number of skilled and experienced management, commercial, operational and scientific personnel will harm our business because we rely upon thesepersonnel for many critical functions of our business. If because of our use of hazardous materials, we violate any environmental controls or regulations that apply to such materials, we may incur substantial costs andexpenses in our remediation efforts. Our research and development involves the controlled use of hazardous materials, chemicals and various radioactive compounds. We are subject to federal, state andlocal laws and regulations governing the use, storage, handling and disposal of these materials and some waste products. Accidental contamination or injury from thesematerials could occur. In the event of an accident, we could be liable for any damages that result and any liabilities could exceed our resources. Compliance withenvironmental laws and regulations or a violation of such environmental laws and regulations could require us to incur substantial unexpected costs, which would materiallyand adversely affect our results of operations. Risks relating to investing in our common stock Our existing principal stockholders hold a substantial amount of our common stock and may be able to influence significant corporate decisions, which may conflictwith the interest of other stockholders. Several of our stockholders own greater than 5% of our outstanding common stock. Our top ten stockholders own more than 50% of BioCryst and can individually, andas a group, influence our operations based upon their concentrated ownership. These stockholders, if they act together, may be able to influence the outcome of mattersrequiring approval of the stockholders, including the election of our directors and other corporate actions. Our stock price has been, and is likely to continue to be, highly volatile, which could result in the value of an investment in our common stock to declinesignificantly. The market prices for securities of biotechnology companies in general have been highly volatile and may continue to be highly volatile in the future. Moreover, ourstock price has fluctuated frequently, and these fluctuations are often not related to our financial results. For the twelve months ended December 31, 2015, the 52-week rangeof the market price of our stock was from $7.85 to $16.83 per share. The following factors, in addition to other risk factors described in this section, may have a significantimpact on the market price of our common stock: •announcements of technological innovations or new products by us or our competitors; •developments or disputes concerning patents or proprietary rights; •additional dilution through sales of our common stock or other derivative securities; •status of new or existing licensing or collaborative agreements and government contracts; •announcements relating to the status of our programs; •developments and announcements regarding new and virulent strains of influenza; •we or our partners achieving or failing to achieve development milestones; •publicity regarding actual or potential medical results relating to products under development by us or our competitors; •publicity regarding certain public health concerns for which we are or may be developing treatments; •regulatory developments in both the United States and foreign countries; •public concern as to the safety of pharmaceutical products; •actual or anticipated fluctuations in our operating results;34 •changes in financial estimates or recommendations by securities analysts; •changes in the structure of healthcare payment systems, including developments in price control legislation; •announcements by us or our competitors of significant acquisitions, strategic partnerships, joint ventures or capital commitments; •additions or departures of key personnel or members of our board of directors; •purchases or sales of substantial amounts of our stock by existing stockholders, including officers or directors; •economic and other external factors or other disasters or crises; and •period-to-period fluctuations in our financial results. Future sales and issuances of securities may dilute the ownership interests of our current stockholders and cause our stock price to decline. Future sales of our common stock by current stockholders into the public market could cause the market price of our stock to fall. As of January 31, 2016, there were73,629,816 shares of our common stock outstanding. We may from time to time issue securities in relation to a license arrangement, collaboration, merger or acquisition. Wemay also sell, for our own account, shares of common stock or other equity securities, from time to time at prices and on terms to be determined at the time of sale. As of January 31, 2016, there were 11,022,560 stock options and restricted stock units outstanding, 96,588 shares available for issuance under our Amended andRestated Stock Incentive Plan, and 497,204 shares available for issuance under our Employee Stock Purchase Plan. In addition, we could also make equity compensationgrants outside of our Stock Incentive Plan. The shares underlying existing stock options, restricted stock units and possible future stock options, stock appreciation rights andstock awards have been registered pursuant to registration statements on Form S-8. If some or all of such shares are sold or otherwise issued into the public market over a short period of time, our current stockholders’ ownership interests may bediluted and the value of all publicly traded shares is likely to decline, as the market may not be able to absorb those shares at then-current market prices. Additionally, suchsales and issuances may make it more difficult for us to sell equity securities or equity-related securities in the future at a time and price that our management deemsacceptable, or at all. We have anti-takeover provisions in our corporate charter documents that may result in outcomes with which you do not agree. Our board of directors has the authority to issue up to 4,800,000 shares of undesignated preferred stock and to determine the rights, preferences, privileges andrestrictions of those shares without further vote or action by our stockholders. The rights of the holders of any preferred stock that may be issued in the future may adverselyaffect the rights of the holders of common stock. The issuance of preferred stock could make it more difficult for third parties to acquire a majority of our outstanding votingstock. In addition, our certificate of incorporation provides for staggered terms for the members of the board of directors and supermajority approval of the removal of anymember of the board of directors and prevents our stockholders from acting by written consent. Our certificate also requires supermajority approval of any amendment ofthese provisions. These provisions and other provisions of our by-laws and of Delaware law applicable to us could delay or make more difficult a merger, tender offer orproxy contest involving us. We have never paid dividends on our common stock and do not anticipate doing so in the foreseeable future. We have never paid cash dividends on our stock. We currently intend to retain all future earnings, if any, for use in the operation of our business. Accordingly, we donot anticipate paying cash dividends on our common stock in the foreseeable future. Information Regarding Forward-Looking Statements This filing contains forward-looking statements within the meaning of Section 21E of the Securities Exchange Act of 1934, as amended, which are subject to the “safeharbor” created in Section 21E. All statements other than statements of historical facts contained in this filing are forward-looking statements. These forward-lookingstatements can generally be identified by the use of words such as “may,” “will,” “intends,” “plans,” “believes,” “anticipates,” “expects,” “estimates,” “predicts,” “potential,”the negative of these words or similar expressions. Statements that describe our future plans, strategies, intentions, expectations, objectives, goals or prospects are alsoforward-looking statements. Discussions containing these forward-looking statements are principally contained in “Business,” “Risk Factors” and “Management’s Discussionand Analysis of Financial Condition and Results of Operations,” as well as any amendments we make to those sections in filings with the SEC. These forward-lookingstatements include, but are not limited to, statements about: 35 •the initiation, timing, progress and results of our preclinical testing, clinical trials, and to the extent applicable, post-marketing commitments, for our HAE productcandidates, RAPIVAB, BCX4430, and our other research and development efforts; •the further preclinical development, clinical development, commercialization, or post marketing studies by either us or partners of our product candidates andproducts, including our HAE program, RAPIVAB, BCX4430, and early stage discovery programs; •the potential funding from our contracts with NIAID/HHS and BARDA/HHS for the development of BCX4430; •the potential for government stockpiling orders of RAPIVAB, additional regulatory approvals of RAPIVAB or milestones royalties or profit from commercial salesof RAPIVAB by us or our partners; •the potential use of RAPIVAB as a treatment for H1N1, H5N1, and H7N9 or other strains of influenza; •the implementation of our business model, strategic plans for our business, products, product candidates and technology; •our ability to establish and maintain collaborations or out-license rights to our drug candidates; •plans, programs, progress and potential success of our collaborations, including Seqirus UK Limited (“SUL”) for RAPIVAB, Mundipharma for forodesine andShionogi and Green Cross for peramivir in their territories; •Royalty Sub’s ability to service its payment obligations in respect of the PhaRMA Notes, and our ability to benefit from our equity interest in Royalty Sub; •the foreign currency hedge agreement entered into by us in connection with the issuance by Royalty Sub of the PhaRMA Notes; •the scope of protection we are able to establish and maintain for intellectual property rights covering our products, product candidates and technology; •our ability to operate our business without infringing the intellectual property rights of others; •estimates of our expenses, revenues, capital requirements, annual cash utilization and our needs for additional financing; •the timing or likelihood of regulatory filings or regulatory agreements, deferrals, and approvals; •our ability to raise additional capital to fund our operations; •our financial performance; and •competitive companies, technologies and our industry. These statements relate to future events or to our future financial performance and involve known and unknown risks, uncertainties and other important factors that maycause our actual results, performance or achievements to be materially different from any future results, performance or achievements expressed or implied by these forward-looking statements. Factors that may cause actual results to differ materially from current expectations include, among other things, those listed under “Risk Factors.” Anyforward-looking statement reflects our current views with respect to future events and is subject to these and other risks, uncertainties and assumptions relating to ouroperations, results of operations, industry and future growth. Except as required by law, we assume no obligation to update or revise these forward-looking statements for anyreason, even if new information becomes available in the future.ITEM 1B.UNRESOLVED STAFF COMMENTS None. 36 ITEM 2.PROPERTIES We lease property in both Durham, North Carolina and Birmingham, Alabama. Our headquarters, including our clinical and regulatory operations, are based in Durham,while our principal research facility is located in Birmingham. We currently lease approximately 15,000 square feet in Durham through June 30, 2020 and leaseapproximately 35,000 square feet in Birmingham through June 30, 2016. We have recently leased an additional approximate 32,000 square foot facility in Birminghamthrough 2027 to house our new research facility. In October of 2015, we began construction of leasehold improvements on our new research facility and expect to move intothe new facility in the third quarter of 2016. We believe that our facilities are adequate for our current operations. ITEM 3.LEGAL PROCEEDINGS None. ITEM 4.MINE SAFETY DISCLOSURES Not applicable. PART II ITEM 5.MARKET FOR REGISTRANT’S COMMON EQUITY, RELATED STOCKHOLDER MATTERS AND ISSUER PURCHASES OF EQUITYSECURITIES Market Information Our common stock trades on the NASDAQ Global Select Market under the symbol BCRX. The following table sets forth the low and high sales prices of our commonstock as reported by the NASDAQ Global Select Market for each quarter in 2015 and 2014: 2015 2014 Low High Low HighFirst quarter $7.85 $12.71 $7.46 $13.33 Second quarter $8.50 $16.43 $7.29 $12.86 Third quarter $10.26 $16.83 $9.78 $14.62 Fourth quarter $8.01 $12.88 $9.02 $13.28 The last sale price of the common stock on January 29, 2016 as reported by the NASDAQ Global Select Market was $6.97 per share. Holders As of January 31, 2016, there were approximately 187 holders of record of our common stock Dividends We have never paid cash dividends and do not anticipate paying cash dividends in the foreseeable future. 37 Stock Performance Graph This performance graph is not “soliciting material,” is not deemed filed with the SEC and is not to be incorporated by reference in any filing by us under the SecuritiesAct or the Exchange Act, whether made before or after the date hereof and irrespective of any general incorporation language in any such filing. The stock price performanceshown on the graph is not necessarily indicative of future price performance. PERFORMANCE GRAPH FOR BIOCRYSTIndexed Comparison Since 2010 Beginning Investment 12/31/10 Investment at 12/31/11 Investment at 12/31/12 Investment at 12/31/13 Investment at 12/31/14 Investment at 12/31/15BioCryst Pharmaceuticals, Inc. $100.00 $47.78 $27.47 $147.00 $235.20 $199.61 NASDAQ Stock Market (U.S.) 100.00 100.31 116.79 155.90 175.33 176.17 NASDAQ Pharmaceutical Stocks 100.00 117.48 134.31 182.23 221.99 234.05 The above graph measures the change in a $100 investment in our common stock based on its closing price of $5.17 on December 31, 2010 and its year-end closingprice thereafter. Our relative performance is then compared with the CRSP Total Return Indexes for the NASDAQ Stock Market (U.S.) and NASDAQ Pharmaceutical Stocks. Recent Sales of Unregistered Securities: None. Issuer Purchases of Equity Securities There were no repurchases of our common stock or shares surrendered to satisfy tax obligations during the fourth quarter of 2015. 38 ITEM 6.SELECTED FINANCIAL DATA The selected Statement of Operations Data and Balance Sheet data with respect to the years ended December 31, 2015, 2014, 2013, 2012, and 2011 set forth below arederived from our consolidated financial statements. The selected financial data set forth below should be read in conjunction with “Management’s Discussion and Analysis ofFinancial Condition and Results of Operations” contained in Item 7 below and our consolidated financial statements and the notes thereto appended to this annual report. Years Ended December 31, 2015 2014 2013 2012 2011 (In thousands, except per share amounts)Statement of Operations Data: Total revenues $48,257 $13,608 $17,331 $26,293 $19,643 Cost of product sold 1,368 1 — — — Research and development expenses 72,758 51,796 41,943 49,160 55,538 General and administrative expenses 13,047 7,461 6,007 9,130 13,692 Royalty expense 528 121 98 132 — Restructuring costs — — — 1,759 — Loss from operations (39,444) (45,771) (30,717) (33,888) (49,587)Net loss (43,019) (45,189) (30,108) (39,081) (56,948)Basic and diluted net loss per share $(0.59) $(0.68) $(0.55) $(0.79) $(1.26)Weighted average shares outstanding 72,901 66,773 55,216 49,474 45,144 As of December 31, 2015 2014 2013 2012 2011 (In thousands)Balance Sheet Data: Cash, cash equivalents and investments $100,858 $114,038 $40,788 $37,058 $57,725 Receivables 6,243 9,490 2,115 4,562 5,831 Inventory 1,612 683 — — 263 Total assets 124,555 136,874 48,866 57,439 82,208 Long-term deferred revenue 9,674 3,552 4,736 5,920 7,103 Non-recourse notes payable 30,000 30,000 30,000 30,000 30,000 Accumulated deficit (510,917) (467,898) (422,709) (392,601) (353,520)Total stockholders’ equity (deficit) 47,724 75,635 (1,126) (454) 14,806 ITEM 7.MANAGEMENT’S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS This Annual Report on Form 10-K contains certain statements of a forward-looking nature relating to future events or the future financial performance of BioCryst.Such statements are only predictions and the actual events or results may differ materially from the results discussed in the forward-looking statements. Factors that couldcause or contribute to such differences include those discussed below and elsewhere in this report, as well as those discussed in other filings made by BioCryst with theSecurities and Exchange Commission. The following Management’s Discussion and Analysis (“MD&A”) is intended to help the reader understand our results of operations and financial condition. MD&A isprovided as a supplement to, and should be read in conjunction with, our audited financial statements and the accompanying notes to the financial statements and otherdisclosures included in this Annual Report on Form 10-K (including the disclosures under “Item 1A. Risk Factors”). Cautionary Statement The discussion herein contains forward-looking statements within the meaning of Section 21E of the Securities Exchange Act of 1934, as amended, which are subject tothe “safe harbor” created in Section 21E. Forward looking statements regarding our financial condition and our results of operations that are based upon our consolidatedfinancial statements, which have been prepared in accordance with accounting principles generally accepted within the United States (“U.S. GAAP”), as well as projectionsfor the future. The preparation of these financial statements requires our management to make estimates and judgments that affect the reported amounts of assets, liabilities,revenues and expenses, and related disclosure of contingent assets and liabilities. We evaluate our estimates on an ongoing basis. Our estimates are based on historicalexperience and on various other assumptions that are believed to be reasonable under the circumstances. The results of our estimates form the basis for making judgmentsabout the carrying values of assets and liabilities that are not readily apparent from other sources. 39 We operate in a highly competitive environment that involves a number of risks, some of which are beyond our control. We are subject to risks common tobiotechnology and biopharmaceutical companies, including risks inherent in our drug discovery, drug development and commercialization efforts, clinical trials, uncertaintyof regulatory actions and marketing approvals, reliance on collaborative partners, enforcement of patent and proprietary rights, the need for future capital, competitionassociated with products, potential competition associated with our product candidates and retention of key employees. In order for any of our product candidates to becommercialized, it will be necessary for us, or our collaborative partners, to conduct clinical trials, demonstrate efficacy and safety of the product candidate to the satisfactionof regulatory authorities, obtain marketing approval, enter into manufacturing, distribution and marketing arrangements, and obtain market acceptance and adequatereimbursement from government and private insurers. We cannot provide assurance that we will generate significant revenues or achieve and sustain profitability in thefuture. In addition, we can provide no assurance that we will have sufficient funding to meet our future capital requirements. Statements contained in Management’sDiscussion and Analysis of Financial Condition and Results of Operations and elsewhere in this report which are not historical facts are, or may constitute, forward-lookingstatements. Forward-looking statements involve known and unknown risks that could cause our actual results to differ materially from expected results. The most significantknown risks are discussed in the section entitled “Risk Factors.” Although we believe the expectations reflected in the forward-looking statements are reasonable, we cannotguarantee future results, levels of activity, performance or achievements. We caution you not to place undue reliance on any forward-looking statements. Our revenues are difficult to predict and depend on numerous factors, including the prevalence and severity of influenza in regions for which peramivir has receivedregulatory approval, seasonality of influenza, ongoing discussions with government agencies regarding future RAPIVAB and/or BCX4430 development and stockpilingprocurement, as well as entering into, or modifying, licensing agreements for our product candidates. Furthermore, revenues related to our collaborative developmentactivities are dependent upon the progress toward and the achievement of developmental milestones by us or our collaborative partners. Our operating expenses are also difficult to predict and depend on several factors, including research and development expenses (and whether these expenses arereimbursable under government contracts), drug manufacturing, and clinical research activities, the ongoing requirements of our development programs, and the availabilityof capital and direction from regulatory agencies, which are difficult to predict. Management may be able to control the timing and level of research and development andgeneral and administrative expenses, but many of these expenditures will occur irrespective of our actions due to contractually committed activities and/or payments. As a result of these factors, we believe that period to period comparisons are not necessarily meaningful and you should not rely on them as an indication of futureperformance. Due to all of the foregoing factors, it is possible that our operating results will be below the expectations of market analysts and investors. In such event, theprevailing market price of our common stock could be materially adversely affected. Overview We are a biotechnology company that designs, optimizes and develops novel small molecule drugs that block key enzymes involved in the pathogenesis of diseases. Wefocus on the treatment of rare diseases in which significant unmet medical needs exist and align with our capabilities and expertise. We integrate the disciplines of biology,crystallography, medicinal chemistry and computer modeling to discover and develop small molecule pharmaceuticals through the process known as structure-guided drugdesign. Critical Accounting Policies and Estimates The accompanying discussion and analysis of our financial condition and results of operations are based upon our consolidated financial statements and the relateddisclosures, which have been prepared in accordance with U.S. GAAP. The preparation of these consolidated financial statements requires us to make estimates andjudgments that affect the reported amounts of assets, liabilities, revenues, expenses and related disclosure of contingent assets and liabilities. We evaluate our estimates,judgments and the policies underlying these estimates on a periodic basis, as situations change, and regularly discuss financial events, policies, and issues with members ofour audit committee and our independent registered public accounting firm. We routinely evaluate our estimates and policies regarding revenue recognition, administration,inventory and manufacturing, taxes, stock-based compensation, research and development, consulting and other expenses and any associated liabilities. 40 Recent Corporate Highlights RAPIVAB (peramivir injection) RAPIVAB was approved by the FDA on December 19, 2014 for the treatment of acute uncomplicated influenza in adult patients who have been symptomatic for nomore than two days. We have elected the “Sell-Through” revenue recognition methodology and recognized approximately $0.6 million of RAPIVAB product sales in 2015.With the approval, commercial availability and out-licensing collaboration of RAPIVAB, we have moved our focus to: (1) obtaining a stockpiling procurement contract withthe U.S. Government to realize the strategic value of this program; (2) fulfilling our post-approval development requirements, including conducting a pediatric trial; and (3)submitting a MAA and a NDS in the European Union and Canada, respectively, to allow SUL (defined below) the ability to commercialize the drug in those regions. On June 16, 2015, we and Seqirus UK Limited, a limited company organized under the laws of the UK ("SUL") and a subsidiary of CSL, entered into a LicenseAgreement (the "SUL Agreement") granting SUL and its affiliates worldwide rights to develop, manufacture and commercialize RAPIVAB (peramivir injection) for thetreatment of influenza except for the rights to conduct such activities in Israel, Japan, Korea and Taiwan (the permitted geographies together constituting the "Territory").RAPIVAB is an intravenous treatment for acute uncomplicated influenza and is currently licensed for use in the United States, Japan and Korea. RAPIVAB is the first andonly intravenous influenza treatment in the world. We retain all rights and associated economics to procure pandemic stockpiling orders for RAPIVAB from the U.S.government, while SUL has the right to pursue government stockpiling outside the U.S. Pursuant to the SUL Agreement, RAPIVAB will be commercialized by CSL's subsidiary, SUL, which specializes in influenza prevention through the supply ofseasonal and pandemic vaccine to global markets. SUL will manufacture, commercialize and exercise decision-making authority with respect to the development andcommercialization of RAPIVAB within the Territory and be responsible for all related costs, including sales and promotion. We will exercise sole decision-making authoritywith regard to the development and commercialization of RAPIVAB outside of the Territory and are responsible for all associated costs. Under the terms of the SUL Agreement, we are responsible for fulfilling all post-marketing approval commitments in connection with the FDA's approval of the NDA,and upon fulfillment we will transfer ownership of and financial responsibility for the NDA to SUL. Pursuant to potential rights to sell RAPIVAB in Canada and the EuropeanUnion (“EU”), we are also responsible for regulatory filings and interactions with the Health Products and Food Branch of Health Canada ("Health Canada") and theEuropean Medicines Agency ("EMA") until marketing approval for RAPIVAB is obtained and assigned to SUL. In accordance with the SUL Agreement, we and SUL formeda joint steering committee, composed of an equal number of representatives from each party, to oversee, review and coordinate the conduct and progress of thecommercialization of RAPIVAB in the Territory and any additional development. Under the terms of the SUL Agreement, we received an upfront payment of $33.7 million, and we may receive up to $12.0 million in additional milestone paymentsrelated to the successful achievement of regulatory milestones, including marketing approval (i) by the FDA for a pediatric indication, (ii) by the EMA for an adult indicationin the EU and (iii) by Health Canada for an adult indication in Canada. We are also entitled under the SUL Agreement to receive tiered royalties at a percentage ratebeginning in the mid-teens contingent upon meeting minimum thresholds of net sales, as well as a low-thirties percentage of the gross profit from government stockpilingpurchases made outside the U.S. Specifically, we receive tiered royalties at a percentage rate in the mid-teens to low-forties on net sales in the U.S. during a Contract Year(defined as July 1 – June 30) and tiered royalties at a percentage rate in the mid-teens to mid-twenties on net sales in the Territory, other than in the U.S., during a ContractYear, each subject to certain downward adjustments for circumstance or events impacting the overall market opportunity. SUL's royalty payment obligations commence onthe date of the SUL Agreement and expire, on a country-by-country basis, upon the later of (i) the expiration of legal exclusivity in such country and (ii) ten years from thedate of the SUL Agreement (the "Royalty Term"). 41 HAE Program Avoralstat On December 18, 2014, we announced the dosing of the first patient in OPuS-2 ( O ral P rophylaxi S-2 ), a blinded, randomized, placebo-controlled clinical trial oforally-administered avoralstat in patients with hereditary angioedema (“HAE”). OPuS-2 was a 12-week, three-arm, parallel cohort design trial to evaluate the efficacy andsafety of two doses of avoralstat, 300 mg and 500 mg, administered three-times daily compared with placebo. This trial was conducted in the U.S. and select Europeancountries. The primary efficacy endpoint for the trial was the mean angioedema attack rate for each avoralstat dose group compared to placebo. On February 8, 2016, weannounced results from OPuS-2. In the OPuS-2 study, HAE patients with a historical attack frequency of greater than 0.45 attacks per week were randomized to treatmentwith either 500 mg or 300 mg of avoralstat, or placebo, administered three times daily for 12 weeks. Thirty-eight subjects received avoralstat 500 mg, 36 subjects receivedavoralstat 300 mg, and 36 subjects received placebo. Treatment with 500 mg and 300 mg of avoralstat three times daily failed to demonstrate a statistically significantly lowermean attack rate versus placebo. The mean (standard deviation) attack rates per week were 0.63 (0.57) on avoralstat 500mg and 0.71 (0.66) on avoralstat 300mg, compared to0.61 (0.41) on placebo. Statistically significant improvements in duration of attacks and in the Angioedema Quality of Life total score were observed comparing the 500 mgthree times a day avoralstat arm to placebo. Following the analysis of OPuS-2 results, the decision was made to discontinue further development of softgel avoralstatformulation in order to focus development efforts on a novel solid dosage form of avoralstat to achieve meaningfully better drug exposure. We expect additional avoralstatresults from a relative bioavailability study testing a novel solid dosage form of avoralstat by mid-year 2016. The primary goals of this study are to achieve meaningfullybetter drug exposures and twice daily dosing. BCX7353 and other 2nd generation HAE compounds In January 2015, we selected BCX7353 to advance into Phase 1 development as a once-daily, oral prophylactic HAE treatment. BCX7353 is structurally different fromavoralstat, but has a similar mechanism of action targeting plasma kallikrein. On May 13, 2015, we announced the initiation of a Phase 1 clinical trial to evaluate the safety,pharmacokinetics and pharmacodynamics of orally-administered BCX7353 in healthy volunteers. On October 8, 2015, we announced that the randomized, placebo-controlled, Phase 1 clinical trial of orally-administered BCX7353 in healthy volunteers successfullymet all of its objectives.In this Phase 1 clinical trial BCX7353 dose levels included single doses of up to 1000mg, once-daily doses of up to 500 mg for seven days, and once-daily doses of 350mg for 14 days. Plasma levels increased in approximate proportion to dose, and drug exposure was not affected by dosing with food. The half-life of BCX7353 was estimatedat 50-60 hours. After daily dosing, blood levels met or exceeded a predicted target therapeutic range throughout the 24 hour dosing interval. Inhibition of the target enzyme,plasma kallikrein, was measured in a sensitive and specific bioassay. Daily dosing with BCX7353 strongly inhibited plasma kallikrein at all four dose levels; the degree ofinhibition was dose-related (p < 0.0001) and inhibition was sustained throughout the 24 hour dosing interval. This pharmacodynamic effect correlated strongly to the achieveddrug concentration (r = 0.91, p < 0.0001).Subsequently, cohorts of healthy Japanese volunteers were added to the study to support development of BCX7353 in Japan under the “Sakigake” accelerated R&Ddesignation. Following assessment of single oral doses of BCX7353 of 100mg (6 subjects) and 500 mg (6 subjects), 250 mg of BCX7353 was administered orally and dailyfor seven days to ten subjects. Compared to Western subjects administered the same dose level, plasma drug levels in Japanese subjects were moderately higher. Kallikreininhibition on day seven of daily dosing with 250 mg in Japanese subjects was similar to that seen at the 350 mg daily and 500 mg daily dose levels in Western subjects.The combined data from both Western and Japanese healthy volunteers indicates that oral BCX7353 has been generally safe and well tolerated in a total of 96 treatedhealthy volunteers, 46 with singles doses and 50 with multiple doses. No serious adverse events have been seen and no dose-limiting toxicity has been identified. There havebeen no clinically significant laboratory abnormalities, ECG changes, or vital sign changes observed.In single dose subjects, 89% (31 of 35) of adverse events (AEs) have been grade 1. The four grade 2 AEs observed were: nausea (1) and vomiting (1) occurring in onesubject: hay fever (1) and diarrhea (1 from Japanese cohort).In multiple dose subjects, 90% (63 of 70) of adverse events (AEs) have been grade 1. The six grade 2 AEs observed were; upper abdominal pain (1, discontinued fromstudy); syncope (1) headache (1) diarrhea (1) and upper abdominal pain (1) occurring on one subject (discounted from study), and maculopapular rash. One grade 3 AE wasobserved, a cutaneous delayed-type hypersensitivity reaction. The two rash AE’s are described in more detail below.The incidence of drug-related skin rash across all multiple-dose cohorts was 4% (2 of 50 subjects). One Japanese subject dosed at 250 mg daily for seven daysdeveloped a grade 2 maculopapular skin rash following cessation of dosing, and one Western subject dosed at 500 mg daily for seven days developed a grade 3hypersensitivity reaction, described as a maculopapular skin rash, following cessation of dosing. Both AEs were assessed by the investigator as drug-related. The Japanesesubject received antihistamines and the Western subject received corticosteroids, and in both cases the rash resolved within a few days. 42 The safety, tolerability, drug exposure and on-target plasma kallikrein inhibition results strongly support advancing the development program into a Phase 2 study inHAE patients. A Phase 2 trial (“APeX-1”) to evaluate the safety, tolerability, pharmacokinetics, pharmacodynamics and efficacy of BCX7353 as a preventative treatment toreduce the frequency of attacks in HAE patients is expected to begin in 2016. The design of the trial will be described when the APeX-1 protocol is approved by regulatoryauthorities and the clinical trial is initiated. On October 27, 2015 the Japanese Ministry of Health Labor & Welfare (“MHLW”) announced that BioCryst’s BCX7353 was one of six products designated underMHLW’s new Sakigake fast track review system. The Sakigake Designation System promotes R&D in Japan, aiming at early practical application for innovativepharmaceutical products. This designation provides for additional interactions with the regulatory agency in Japan from early development through filing, and prioritizeddevelopment and review, with the aim of introduction of the product as soon as possible to address a serious unmet medical need. We expect the results of APeX-1 to help usand the MHLW to determine the regulatory pathway and timeline for BCX7353 in Japan. Other 2 nd generation HAE compounds In addition to BCX7353, we have succeeded in inventing several uniquely different plasma kallikrein inhibitor molecules from distinct structural classes. Accordingly,we have selected additional drug candidates that have suitable pharmacologic properties to advance into preclinical development. The development of these candidates forHAE or in other therapeutic areas is ongoing and additional disclosure on these compounds will occur as we near IND filings of these compounds. BCX4430 On December 15, 2014, we announced the dosing of the first subject in a randomized, placebo-controlled Phase 1 clinical trial to evaluate i.m. administration ofBCX4430 in healthy volunteers. The main goals of this first-in-human study are to evaluate the safety, tolerability and pharmacokinetics of escalating doses of BCX4430administered via i.m. injection in healthy subjects. This Phase 1 study is expected to continue in 2016. On December 23, 2014, we announced results from a successful proof-of-concept study of BCX4430 for the treatment of experimental Ebola virus infection in Rhesusmacaques, conducted at USAMRIID. The primary goal of the study was to assess the effect of BCX4430 treatment on survival through Day 41 in animals infected with Ebolavirus. Dosing of placebo or BCX4430 by i.m. injection was initiated 30-120 minutes after virus challenge and continued twice a day for 14 days. The overall survival rate forBCX4430 treated animals at day 41 was 10 of 12 (83%, p < 0.001 compared to controls). Preliminary evaluation of the quantity of virus in the blood showed an approximate3-log reduction in Ebola virus RNA copies/mL of plasma, compared with control animals. This Rhesus macaques study was conducted following the completion, inNovember 2014, of a dose-ranging study of BCX4430 for the treatment of cynomolgus macaques infected with Ebola virus. The cynomolgus macaques study was designed toevaluate whether BCX4430 showed a meaningful benefit for survival in Ebola virus NHP disease models. In this study, BCX4430 demonstrated a statistically significantprolongation of survival for the animals at the highest dose regimen tested, but no animals survived beyond 21 days. Results of Operations Year Ended December 31, 2015 Compared to 2014 Total 2015 revenues increased to $48.3 million as compared to 2014 revenues of $13.6 million. The increase in 2015 was primarily due to recognizing revenueassociated with the SUL out-licensing transaction, RAPIVAB product revenue and increased collaboration revenue associated with BCX4430 development. The 2015 revenueconsisted of $5.7 million of RAPIVAB product revenue and $21.8 million of collaborative revenue related to the SUL Agreement, $2.4 million of royalty revenue from SUL,Shionogi and Green Cross associated with sales of peramivir in the United States, Japan and Korea, $16.3 million of reimbursement of collaborative expenses fromBARDA/HHS and NIAID/HHS related to the development of peramivir and BCX4430, and $1.4 million associated with collaborative revenue amortization from othercorporate partnerships. In addition, we recorded approximately $618,000 of RAPIVAB revenue under the “Sell-Through” revenue recognition methodology, but goingforward will recognize all future commercial RAPIVAB sales as royalty revenue under one of our partnership arrangements. RAPIVAB was available for commercial sale onDecember 26, 2014. The 2014 revenue consisted of $3.0 million of royalty revenue from Shionogi and Green Cross associated with sales of peramivir in Japan and Korea,$9.4 million of reimbursement of collaborative expenses from BARDA/HHS related to the development of peramivir, $1.2 million associated with collaborative revenueamortization from other corporate partnerships and $33,000 of RAPIVAB revenue. With the expiration of BARDA/HHS peramivir contract, unless we enter into newgovernment contracts, all significant and future reimbursement of collaborative expenses will be under the NIAID/HHS and BARDA/HHS BCX4430 development contracts.Our RAPIVAB product revenue will be difficult to predict because of volatility in prevalence, timing and severity of influenza season to season. Research and Development (“R&D”) expenses increased to $72.8 million in 2015 from $51.8 million in 2014. 2015 R&D expenses, compared with 2014, reflectincreased spending on our HAE programs and slightly higher spending on our RAPIVAB program. In addition, our 2014 equity compensation expense allocated to R&Dincreased due to the vesting of two underlying milestones under previously issued performance-based stock options for the successful outcome of OPuS-1 and RAPIVABapproval in the U.S. The following table summarizes our R&D expenses for the periods indicated (amounts are in thousands). 2015 2014 2013R&D expenses by program: Avoralstat $27,769 $19,005 $15,442 BCX7353 11,819 — — Other 2nd generation HAE compounds 9,320 11,681 — BCX4430 12,400 13,060 3,318 Peramivir 3,690 2,898 13,627 Other research, preclinical and development costs 7,760 5,152 9,556 Total R&D expenses $72,758 $51,796 $41,943 43 R&D expenses include all direct and indirect expenses and are allocated to specific programs at the point of development of a lead product candidate. Direct expensesare charged directly to the program to which they relate and indirect expenses are allocated based upon internal direct labor hours dedicated to each respective program. Directexpenses consist of compensation for R&D personnel and costs of outside parties to conduct laboratory studies, develop manufacturing processes, manufacture the productcandidates, conduct and manage clinical trials, as well as other costs related to our clinical and preclinical studies. Indirect R&D expenses consist of lab supplies and services,facility expenses, depreciation of development equipment and other overhead of our research and development efforts. R&D expenses vary according to the number ofprograms in clinical development and the stage of development of our clinical programs. Later stage clinical programs tend to cost more than earlier stage programs due to thelonger length of time of the clinical trials and the higher number of patients enrolled in these clinical trials. Selling, General and administrative (“SG&A”) expenses increased to $13.0 million in 2015 compared to $7.5 million in 2014. The increase of $5.5 million is primarilyassociated with increased marketing and medical affairs activities associated with our HAE programs, as well as unrestricted grants awarded to the U.S. and internationalHAE patient advocacy groups. Interest expense, related to the non-recourse notes issued in conjunction with the peramivir royalty monetization transaction in March 2011, increased slightly to $5.2million in 2015 as compared to $5.0 million in 2014. In addition, a mark to market loss of $0.6 million was recognized in 2015 related to the foreign currency hedge enteredinto in conjunction with the royalty monetization transaction, compared to a mark to market gain of $5.5 million in 2014, both resulting from changes in the U.S.dollar/Japanese yen exchange rate during the respective years. In addition, a realized currency exchange gain of $1.6 million was recognized in 2015 related to the exercise ofa U.S. dollar/Japanese yen currency option under our foreign currency hedge. Thus, a resulting $1.1 million net gain is recognized on our foreign currency derivative for 2015.We entered into a foreign currency hedge agreement to hedge changes in the value of the Japanese yen relative to the U.S. dollar. The currency hedge does not qualify forhedge accounting treatment and therefore mark to market adjustments are recognized in our Consolidated Statements of Comprehensive Loss. Although we cannot predict thefuture yen/dollar exchange rate, the applicable foreign currency rates moved such that we currently have no collateral posted; however, it is possible that collateral will berequired in 2016 or the future. We are unable to predict future changes in the yen/dollar exchange rate or increases/decreases in our hedge loss associated with the currencyhedge agreement. Year Ended December 31, 2014 Compared to 2013 Total 2014 revenues decreased to $13.6 million as compared to 2013 revenues of $17.3 million. The 2014 revenue consisted of $3.0 million of royalty revenue fromShionogi and Green Cross associated with sales of peramivir in Japan and Korea, $9.4 million of reimbursement of collaborative expenses from BARDA/HHS andNIAID/HHS related to the development of peramivir and BCX4430, and $1.2 million associated with collaborative revenue amortization from other corporate partnerships. Inaddition, we recorded approximately $33,000 of RAPIVAB revenue under the “Sell-Through” revenue recognition methodology. RAPIVAB was available for commercialsale on December 26, 2014. The decrease in total revenues was primarily the result of the June 2014 BARDA/HHS peramivir contract expiration associated with completionof development activities under this contract. The 2013 revenue consisted of $2.6 million of royalty revenue from Shionogi and Green Cross associated with sales ofperamivir in Japan and Korea, $13.5 million of reimbursement of collaborative expenses from BARDA/HHS related to the development of peramivir and $1.2 millionassociated with collaborative revenue amortization from other corporate partnerships. With the expiration of BARDA/HHS peramivir contract, unless we enter into newgovernment contracts, all significant and future reimbursement of collaborative expenses will be under the NIAID/HHS BCX4430 development contract. In addition, weexpect RAPIVAB product sales to increase in future years when the product is available prior to the beginning of the influenza season and for a longer period of time within afiscal year. However, our RAPIVAB product revenue will be difficult to predict because of volatility in prevalence, timing and severity of influenza season to season in theUnited States and because we will not incur substantial commercialization expenses to promote it. R&D expenses increased to $51.8 million in 2014 from $41.9 million in 2013. 2014 R&D expenses, compared with 2013, reflect increased spending on our HAE andBCX4430 programs which were partially offset by the wind-down of peramivir development activities and the expiration of the BARDA/HHS development contract. Inaddition, our 2014 equity compensation expense allocated to R&D increased due to the vesting of two underlying milestones under previously issued performance-basedstock options for the successful outcome of OPuS-1 and RAPIVAB approval in the U.S. In 2013, we recognized approximately $5.0 million of R&D costs related to a write-off of deferred collaboration costs associated with our PNP licensing agreement with AECOM/IRL. This write-off, and related R&D expenses, was allocated to the ulodesineprogram and represents the majority of 2013 ulodesine expense represented in the table below. 44 SG&A expenses increased to $7.5 million in 2014 compared to $6.0 million in 2013. The increase of $1.5 million is primarily due to RAPIVAB distribution expensesand unrestricted grants awarded to U.S. and international HAE patient advocacy groups. We expect our future SG&A expenses to increase due to increases in administrativeexpenses associated with corporate growth in preparation for future NDA and other regulatory filings and for product commercialization. Interest expense, related to the non-recourse notes issued in conjunction with the peramivir royalty monetization transaction in March 2011, increased slightly to $5.0million in 2014 as compared to $4.8 million in 2013. In addition, a mark to market gain of $5.5 million was recognized in 2014 related to the foreign currency hedge enteredinto in conjunction with the royalty monetization transaction, compared to a mark to market gain of $5.3 million in 2013, both resulting from changes in the U.S.dollar/Japanese yen exchange rate during the respective years. Liquidity and Capital Resources Cash expenditures have exceeded revenues since our inception and we expect our 2016 operating expenses to exceed our 2016 revenues. Our operations have principallybeen funded through public offerings and private placements of equity securities; cash from collaborative and other research and development agreements, including U.S.Government contracts for peramivir and BCX4430; and to a lesser extent, the PhaRMA Notes financing. To date, we have been awarded a BARDA/HHS peramivirdevelopment contract totaling $234.8 million, which expired on June 30, 2014, a NIAID/HHS BCX4430 development contract totaling $34.0 million, which is ongoing, and aBARDA/HHS BCX4430 development contract totaling $36.2 million, which is also ongoing. The total amount of NIAID/HHS and BARDA/HHS funding obligated underawarded options in the active contracts is $29.9 million and $16.3 million, respectively. Most recently, we completed a successful public offering in June 2014 of 11.5 millionshares of common stock at a price of $10.00 per share, which provided net proceeds to us of approximately $107.8 million. This financing and the recently completed SULout-licensing transaction provides us liquidity through mid-2017. We may issue securities through private placement transactions or registered public offerings pursuant to aregistration statement filed with the SEC. In addition to the above, we have received funding from other sources, including other collaborative and other research anddevelopment agreements; government grants; equipment lease financing; facility leases; research grants; and interest income on our investments. As of December 31, 2015, we had net working capital of $1.5 million, a decrease of approximately $30.6 million from $32.1 million at December 31, 2014. Thedecrease in working capital was principally due to our normal operating expenses associated with the development of our product candidates and the reclassification of ournon-recourse notes payable to current liabilities. Our principal sources of liquidity at December 31, 2015 were approximately $28.9 million in cash and cash equivalents;approximately $70.3 million in investments considered available-for-sale, and approximately $5.5 million in U.S. Government receivables. We anticipate our cash andinvestments will fund our operations through mid-2017. We intend to contain costs and cash flow requirements by closely managing our third party costs and headcount, leasing scientific equipment and facilities, contractingwith other parties to conduct certain research and development projects and using consultants. We expect to incur additional expenses, potentially resulting in significantlosses, as we continue to pursue our research and development activities and begin to build a commercial infrastructure. We may incur additional expenses related to thefiling, prosecution, maintenance, defense and enforcement of patent and other intellectual property claims and additional regulatory costs as our clinical programs advancethrough later stages of development. The objective of our investment policy is to ensure the safety and preservation of invested funds, as well as maintaining liquiditysufficient to meet cash flow requirements. We place our excess cash with high credit quality financial institutions, commercial companies, and government agencies in orderto limit the amount of our credit exposure. We have not realized any significant losses on our investments. We extended or executed additional lease obligations in 2015 for our Birmingham, Alabama operations which increased the obligations by $5.6 million and extendedthe new obligations out to 2027. These operating lease obligations encompass future rental obligations of our Birmingham operating facilities. We plan to finance our needs principally from the following: • lease or loan financing and future public or private equity financing; • our existing capital resources and interest earned on that capital; • payments under existing and executing new contracts with the U.S. Government; and • payments under collaborative and licensing agreements with corporate partners. 45 As our programs continue to advance, our costs will increase. Our current and planned clinical trials, plus the related development, manufacturing, regulatory approvalprocess requirements and additional personnel resources and testing required for the continuing development of our product candidates will consume significant capitalresources and will increase our expenses. Our expenses, revenues and cash utilization rate could vary significantly depending on many factors, including our ability to raiseadditional capital, the development progress of our collaborative agreements for our product candidates, the amount and timing of funding we receive from existing U.S.Government contracts for BCX4430, the amount of funding or assistance, if any, we receive from new U.S. Government contracts or other new partnerships with third partiesfor the development and or commercialization of our product candidates, the progress and results of our current and proposed clinical trials for our most advanced productcandidates, the progress made in the manufacturing of our lead product candidates and the progression of our other programs. With the funds available at December 31, 2015, we believe these resources will be sufficient to fund our operations through mid-2017. Our future liquidity needs, andability to address those needs, will largely be determined by the success of our product candidates and key development and regulatory events in the future. In order tocontinue our operations substantially beyond mid-2017, we will need to: (1) successfully secure or increase U.S. Government funding of our programs, including procurementcontracts; (2) out-license rights to certain of our products or product candidates, pursuant to which we would receive cash milestones; (3) raise additional capital throughequity or debt financings or from other sources; (4) obtain additional product candidate regulatory approvals, which would generate revenue and cash flow; (5) reducespending on one or more research and development programs; and/or (6) restructure operations. We may issue securities through private placement transactions or registeredpublic offerings pursuant to a registration statement filed with the SEC. Our long-term capital requirements and the adequacy of our available funds will depend upon many factors, including: • our ability to perform under our government contracts and receive reimbursement, and receive stockpiling procurement contracts; • the magnitude of work under our government contracts; • the progress and magnitude of our research, drug discovery and development programs; • changes in existing collaborative relationships or government contracts; • our ability to establish additional collaborative relationships with academic institutions, biotechnology or pharmaceutical companies and governmental agenciesor other third parties; • the extent to which our partners, including governmental agencies, will share in the costs associated with the development of our programs or run thedevelopment programs themselves; • our ability to negotiate favorable development and marketing strategic alliances for certain product candidates or a decision to build or expand internaldevelopment and commercial capabilities; • successful commercialization of marketed products by either us or a partner; • the scope and results of preclinical studies and clinical trials to identify and develop product candidates; • our ability to engage sites and enroll subjects in our clinical trials; • the scope of manufacturing of our product candidates to support our preclinical research and clinical trials; • increases in personnel and related costs to support the development and commercialization of our product candidates; • the scope of manufacturing of our drug substance and product candidates required for future NDA filings; • competitive and technological advances; • the time and costs involved in obtaining regulatory approvals; • post-approval commitments for RAPIVAB and other products that receive regulatory approval; and • the costs involved in all aspects of intellectual property strategy and protection including the costs involved in preparing, filing, prosecuting, maintaining,defending and enforcing patent claims. 46 We expect that we will be required to raise additional capital to complete the development and commercialization of our current product candidates and we may seek toraise capital in the future. Additional funding, whether through additional sales of equity or debt securities, collaborative or other arrangements with corporate partners orfrom other sources, including governmental agencies in general and existing government contracts specifically, may not be available when needed or on terms acceptable tous. The issuance of preferred or common stock or convertible securities, with terms and prices significantly more favorable than those of the currently outstanding commonstock, could have the effect of diluting or adversely affecting the holdings or rights of our existing stockholders. In addition, collaborative arrangements may require us totransfer certain material rights to such corporate partners. Insufficient funds may require us to delay, scale back or eliminate certain of our research and developmentprograms. Our future working capital requirements, including the need for additional working capital, will be largely determined by the advancement of our portfolio ofproduct candidates as well as rate of reimbursement by U.S. Government agencies of our BCX4430 expenses and any future decisions regarding the future of the RAPIVABand BCX4430 programs, including those relating to stockpiling procurement. More specifically, our working capital requirements will be dependent on the number,magnitude, scope and timing of our development programs; regulatory approval of our product candidates; obtaining funding from collaborative partners; the cost, timing andoutcome of regulatory reviews, regulatory investigations, and changes in regulatory requirements; the costs of obtaining patent protection for our product candidates; thetiming and terms of business development activities; the rate of technological advances relevant to our operations; the efficiency of manufacturing processes developed on ourbehalf by third parties; and the level of required administrative support for our daily operations. Financial Outlook for 2016 Based upon our development plans, expected operations and our awarded government contracts, we expect 2016 operating cash usage to be in the range of $55 to $75million, and expect our total 2016 operating expenses to be in the range of $78 to $98 million. Our operating expense range excludes equity-based compensation expense dueto the difficulty in accurately projecting this expense as it is significantly impacted by the volatility and price of the Company’s stock, as well as vesting of the Company’soutstanding performance-based stock options. Our operating cash forecast excludes any impact of our royalty monetization, hedge collateral posted or returned, and any othernon-routine cash outflows or inflows. Our ability to remain within our operating expense and operating cash target ranges is subject to multiple factors, includingunanticipated or additional general development and administrative costs and other factors described under the Risk Factors located elsewhere in this report. Off-Balance Sheet Arrangements As of December 31, 2015, we are not involved in any unconsolidated entities or off–balance sheet arrangements. Contractual Obligations In the table below, we set forth our enforceable and legally binding obligations and future commitments and obligations related to all contracts that we are likely tocontinue regardless of the fact that they are cancelable as of December 31, 2015. Some of the amounts we include in this table are based on management’s estimates andassumptions about these obligations, including their duration, the possibility of renewal, anticipated actions by third parties, and other factors. Because these estimates andassumptions are necessarily subjective, the obligations we will actually pay in future periods may vary from those reflected in the table. Payments Due by Period (In thousands)Contractual Obligations Total Less Than 1 Year 1-3 Years 3-5 Years More Than 5 YearsOperating lease obligations $6,908 $651 $1,741 $1,471 $3,045 Purchase obligations(1) 34,137 34,137 — — — Contingent license obligations 2,000 225 450 425 900 Non-recourse notes payable(2) 57,396 10,946 8,400 38,050 — Total $100,441 $45,959 $10,591 $39,946 $3,945 (1)Purchase obligations include commitments related to clinical development, manufacturing and research operations and other purchase commitments.(2)Assumes the PhaRMA Notes will be repaid at maturity and the related interest costs will accrue and be paid annually through maturity. This assumption is based onthe unpredictable nature of the royalty payments from Shionogi, which are designated for both principal and interest payments on the PhaRMA Notes. 47 Under the Currency Hedge Agreement, we have the right to purchase dollars and sell yen at a rate of 100 yen per dollar for which we may be required to pay a premiumin each year from 2016 through 2020. A payment of $2.0 million will be required if, during the relevant year, the dollar is worth 100 yen or less. As of December 31, 2015,we have no hedge collateral posted against the Currency Hedge Agreement. Because the posting of additional collateral and payment of annual premiums is contingent on thevalue of the yen relative to the dollar and other factors, such payments have been excluded from the foregoing table. In addition to the above, we have committed to make potential future “sublicense” payments to third-parties as part of in-licensing and development programs. Paymentsunder these agreements generally become due and payable only upon achievement of certain developmental, regulatory and/or commercial milestones. Because theachievement of these milestones is neither probable nor reasonably estimable, such contingencies have not been recorded on our balance sheet. Critical Accounting Policies We have established various accounting policies that govern the application of U.S. GAAP, which were utilized in the preparation of our consolidated financialstatements. Certain accounting policies involve significant judgments and assumptions by management that have a material impact on the carrying value of certain assets andliabilities. Management considers such accounting policies to be critical accounting policies. The judgments and assumptions used by management are based on historicalexperience and other factors, which are believed to be reasonable under the circumstances. Because of the nature of the judgments and assumptions made by management,actual results could differ from these judgments and estimates, which could have a material impact on the carrying values of assets and liabilities and the results of operations. While our significant accounting policies are more fully described in Note 1 to our consolidated financial statements included in this Annual Report on Form 10-K forthe year ended December 31, 2015, we believe that the following accounting policies are the most critical to aid you in fully understanding and evaluating our reportedfinancial results and affect the more significant judgments and estimates that we use in the preparation of our financial statements. Inventory Our inventories consist of RAPIVAB finished goods and work in process, which are valued at the lower of cost or market using the first-in, first-out (i.e., FIFO) method.Cost includes materials, labor, overhead, shipping and handling costs. Our inventories are subject to expiration dating. We regularly evaluate the carrying value of ourinventories and provide valuation reserves for any estimated obsolete, short-dated or unmarketable inventories. In addition, we may experience spoilage of our raw materialsand supplies. Our determination that a valuation reserve might be required, in addition to the quantification of such reserve, requires us to utilize significant judgment. Inconnection with the FDA approval of RAPIVAB in December 2014, we began capitalizing costs associated with the production of RAPIVAB commercial inventories. Accrued Expenses We enter into contractual agreements with third-party vendors who provide research and development, manufacturing, and other services in the ordinary course ofbusiness. Some of these contracts are subject to milestone-based invoicing and services are completed over an extended period of time. We record liabilities under thesecontractual commitments when an obligation has been incurred. This accrual process involves reviewing open contracts and purchase orders, communicating with ourapplicable personnel to identify services that have been performed and estimating the level of service performed and the associated cost when we have not yet been invoicedor otherwise notified of actual cost. The majority of our service providers invoice us monthly in arrears for services performed. We make estimates of our accrued expenses asof each balance sheet date based on the facts and circumstances known to us. We periodically confirm the accuracy of our estimates with the service providers and makeadjustments if necessary. Examples of estimated accrued expenses include: • fees paid to Clinical Research Organizations (“CROs”) in connection with preclinical and toxicology studies and clinical trials; • fees paid to investigative sites in connection with clinical trials; • fees paid to contract manufacturers in connection with the production of our raw materials, drug substance and product candidates; and • professional fees. 48 We base our expenses related to clinical trials on our estimates of the services received and efforts expended pursuant to contracts with multiple research institutions andCROs that conduct and manage clinical trials on our behalf. The financial terms of these agreements are subject to negotiation, vary from contract to contract and may resultin uneven payment flows. Payments under some of these contracts depend on factors such as the successful enrollment of patients and the completion of clinical trialmilestones. In accruing service fees, we estimate the time period over which services will be performed and the level of effort expended in each period. If the actual timing ofthe performance of services or the level of effort varies from our estimate, we will adjust the accrual accordingly. If we do not identify costs that we have begun to incur or ifwe underestimate or overestimate the level of these costs, our actual expenses could differ from our estimates. Revenue Recognition We recognize revenues from collaborative and other research and development arrangements and product sales. Revenue is realized or realizable and earned when all ofthe following criteria are met: (i) persuasive evidence of an arrangement exists; (ii) delivery has occurred or services have been rendered; (iii) the seller’s price to the buyer isfixed or determinable; and (iv) collectability is reasonably assured. Collaborative and Other Research and Development Arrangements and Royalties Revenue from license fees, royalty payments, event payments, and research and development fees are recognized as revenue when the earnings process is complete andwe have no further continuing performance obligations or we have completed the performance obligations under the terms of the agreement. Fees received under licensingagreements that are related to future performance are deferred and recognized over an estimated period determined by management based on the terms of the agreement andthe products licensed. In the event a license agreement contains multiple deliverables, we evaluate whether the deliverables are separate or combined units of accounting.Revisions to revenue or profit estimates as a result of changes in the estimated revenue period are recognized prospectively. Under certain of our license agreements, we receive royalty payments based upon our licensees’ net sales of covered products. We recognize royalty revenues when wecan reliably estimate such amounts and collectability is reasonably assured. Royalty revenue paid by Shionogi on their product sales is subject to returns. For arrangements that involve the delivery of more than one element, each product, service and/or right to use assets is evaluated to determine whether it qualifies as aseparate unit of accounting. This determination is based on whether the deliverable has “stand-alone value” to the customer. The consideration that is fixed or determinable isthen allocated to each separate unit of accounting based on the relative selling price of each deliverable. The estimated selling price of each deliverable is determined using thefollowing hierarchy of values: (i) vendor-specific objective evidence of fair value, (ii) third-party evidence of selling price (“TPE”) and (iii) best estimate of selling price(“BESP”). The BESP reflects our best estimate of what the selling price would be if the deliverable was regularly sold by us on a stand-alone basis. In most cases we expect touse TPE or BESP for allocating consideration to each deliverable. The consideration allocated to each unit of accounting is recognized as the related goods or services aredelivered, limited to the consideration that is not contingent upon future deliverables. Analyzing the arrangement to identify deliverables requires the use of judgment, andeach deliverable may be an obligation to deliver services, a right or license to use an asset, or another performance obligation. In June 2015, we entered into a License Agreement (the "SUL Agreement") granting SUL and its affiliates worldwide rights, excluding Israel, Japan, Korea andTaiwan, to develop, manufacture and commercialize RAPIVAB. The SUL Agreement provides for various types of payments, including a non-refundable upfront fee,milestone payments, and future royalties. Analysis of the SUL Agreement identified three deliverables: (i) license rights, (ii) inventory and (iii) regulatory support to obtainCanadian and EU marketing approvals. We received an upfront payment of $33.7 million from SUL of which $7.0 million was determined to be contingent upon EUmarketing approval and will be deferred until that time. Approximately $21.8 million of the upfront payment was allocated to the license rights and recognized as revenue inthe second quarter. Approximately $3.7 million of the upfront payment was allocated to the sale of inventory and was recognized in the third quarter when the inventorytransfer was completed. Approximately $1.2 million of the revenue from the SUL Agreement will be recognized ratably over the expected period of involvement in theseregulatory support activities. Milestone payments are recognized as licensing revenue upon the achievement of specified milestones if (i) the milestone is substantive in nature and the achievementof the milestone was not reasonably assured at the inception of the SUL Agreement; and (ii) the fees are non-refundable. Any milestone payments received prior to satisfyingthese revenue recognition criteria are recorded as deferred revenue. Under the terms of the SUL Agreement, we may receive up to $12.0 million in additional payments related to the successful achievement of regulatory milestones,including marketing approval (i) by the FDA for a pediatric indication, (ii) by the EMA for an adult indication in the EU and (iii) by Health Canada for an adult indication inCanada. We evaluated each event based payment under the provisions of ASU 2010-17, Milestone Method of Revenue Recognition , and determined that each event basedpayment met the criteria to be considered substantive and represents a milestone under the milestone method of accounting. No event based payments were achieved duringthe periods presented. 49 Reimbursements received for direct out-of-pocket expenses related to research and development costs are recorded as revenue in the income statement rather than as areduction in expenses. Under our contracts with BARDA/HHS and NIAID/HHS, revenue is recognized as reimbursable direct and indirect costs are incurred. Product Sales We recognize revenue for sales of RAPIVAB when title and substantially all the risks and rewards of ownership have transferred to the customer, which generallyoccurs on the date of shipment from our specialty distributors, utilizing the Sell-Through revenue recognition methodology. Product sales are recognized when there ispersuasive evidence that an arrangement exists, title has passed, the price was fixed and determinable, and collectability is reasonably assured. Product sales are recognizednet of estimated allowances, discounts, sales returns, chargebacks and rebates. In the United States, prior to completion of the SUL transaction, we sold RAPIVAB tospecialty distributors, who, in turn, sell to physician offices, hospitals and federal, state and commercial health care organizations. Sales deductions consist of statutory rebates to state Medicaid, Medicare and other government agencies and sales discounts (including trade discounts and distributionservice fees). These deductions are recorded as reductions to revenue from RAPIVAB in the same period as the related sales with estimates of future utilization derived fromhistorical experience adjusted to reflect known changes in the factors that impact such reserves. We utilize data from external sources to help estimate gross-to-net sales adjustments as they relate to the recognition of revenue for RAPIVAB sold. External sourceddata includes, but is not limited to, information obtained from specialty distributors with respect to their inventory levels and sell-through to customers, and information fromthird-party suppliers of market research data to the pharmaceutical industry. We have categorized and described more fully the following significant sales deductions, all of which involve estimates and judgments, which we consider to be criticalaccounting estimates, and requires us to use information from external sources. Rebates and Chargebacks Statutory rebates to state Medicaid agencies and Medicare are based on statutory discounts to RAPIVAB’s selling price. As it can take up to nine months or more forinformation to be received on actual usage of RAPIVAB in Medicaid and other governmental programs, we maintain reserves for amounts payable under these programsrelating to RAPIVAB sales. Chargebacks claimed by specialty distributors are based on the differentials between product acquisition prices paid by the specialty distributors and lower governmentcontract pricing paid by eligible customers covered under federally qualified programs. The amount of the reserve for rebates and chargebacks is based on multiple qualitative and quantitative factors, including the historical and projected utilization levels,historical payment experience, changes in statutory laws and interpretations as well as contractual terms, product pricing (both normal selling prices and statutory ornegotiated prices), changes in prescription demand patterns and utilization of our product through public benefit plans, and the levels of RAPIVAB inventory in thedistribution channel. We acquire prescription utilization data from third-party suppliers of market research data to the pharmaceutical industry. We update our estimates andassumptions each period and record any necessary adjustments to reserves. Settlements of rebates and chargebacks typically occur within nine months from point of sale. Tothe extent actual rebates and chargebacks differ from our estimates, additional reserves may be required or reserves may need to be reversed, either of which would impactcurrent period product revenue. Discounts and Sales Incentives Discounts and other sales incentives primarily consist of Inventory Management Agreement (“IMA”) Fees. Per contractual agreements with our specialty distributors,we provide an IMA fee based on a percentage of their purchases of RAPIVAB. The IMA fee rates are set forth in our individual contracts. We track sales to our specialtydistributors each period and accrue a liability relating to the unpaid portion of these fees by applying contractual rates to such sales. Product Returns We do not record a product return allowance as we do not offer the ability to return goods once a bona fide shipment has been accepted by a specialty distributor. 50 Research and Development Expenses Our research and development costs are charged to expense when incurred. Advance payments for goods or services that will be used or rendered for future research anddevelopment activities are deferred and capitalized. Such amounts are recognized as expense when the related goods are delivered or the related services are performed.Research and development expenses include, among other items, personnel costs, including salaries and benefits, manufacturing costs, clinical, regulatory, and toxicologyservices performed by CROs, materials and supplies, and overhead allocations consisting of various administrative and facilities related costs. Most of our manufacturing andclinical and preclinical studies are performed by third-party CROs. Costs for studies performed by CROs are accrued by us over the service periods specified in the contractsand estimates are adjusted, if required, based upon our on-going review of the level of services actually performed. Additionally, we have license agreements with third parties, such as AECOM, IRL, and UAB, which require fees related to sublicense agreements or maintenance fees.We expense sublicense payments as incurred unless they are related to revenues that have been deferred, in which case the expenses are deferred and recognized over therelated revenue recognition period. We expense maintenance payments as incurred. Deferred collaboration expenses represent sub-license payments paid to our academic partners upon receipt of consideration from various commercial partners, andother consideration to our academic partners for modification to existing license agreements. These deferred expenses would not have been incurred without receipt of suchpayments or modifications from our commercial partners and are being expensed in proportion to the related revenue being recognized. We believe that this accountingtreatment appropriately matches expenses with the associated revenue. We group our R&D expenses into two major categories: direct external expenses and indirect expenses. Direct expenses consist of compensation for R&D personnel andcosts of outside parties to conduct laboratory studies, develop manufacturing processes and manufacture the product candidate, conduct and manage clinical trials, as well asother costs related to our clinical and preclinical studies. These costs are accumulated and tracked by program. Indirect expenses consist of lab supplies and services, facilityexpenses, depreciation of development equipment and other overhead of our research and development efforts. These costs apply to work on our clinical and preclinicalcandidates as well as our discovery research efforts. Stock-Based Compensation All share-based payments, including grants of stock option awards and restricted stock unit awards, are recognized in our Consolidated Statements of ComprehensiveLoss based on their fair values. Stock-based compensation cost is estimated at the grant date based on the fair value of the award and is recognized as expense on a straight-line basis over the requisite service period of the award. Determining the appropriate fair value model and the related assumptions for the model requires judgment, includingestimating the life of an award, the stock price volatility, and the expected term. We utilize the Black-Scholes option-pricing model to value our awards and recognizecompensation expense on a straight-line basis over the vesting periods. The estimation of share-based payment awards that will ultimately vest requires judgment, and to theextent actual results or updated estimates differ from our current estimates, such amounts will be recorded as a cumulative adjustment in the period estimates are revised. Inaddition, we have outstanding performance-based stock options for which no compensation expense is recognized until “performance” has occurred. Significant managementjudgment is also required in determining estimates of future stock price volatility and forfeitures to be used in the valuation of the options. Actual results, and future changesin estimates, may differ substantially from our current estimates. Foreign Currency Hedge In connection with our issuance of the PhaRMA Notes, we entered into a foreign Currency Hedge Agreement to hedge certain risks associated with changes in the valueof the Japanese yen relative to the U.S. dollar. Under the Currency Hedge Agreement, we have the right to purchase dollars and sell yen at a rate of 100 yen per dollar forwhich we may be required to pay a premium in each year from 2016 through 2020, provided the Currency Hedge Agreement remains in effect. A payment of $2.0 million willbe required if, on May 18 of the relevant year, the U.S. dollar is worth 100 yen or less as determined in accordance with the Currency Hedge Agreement. In conjunction withestablishing the Currency Hedge Agreement, we will be required to post collateral to the counterparty, which may cause us to experience additional quarterly volatility in ourfinancial results. We will not be required at any time to post collateral exceeding the maximum premium payments remaining payable under the Currency Hedge Agreement.In establishing the hedge, we provided initial funds of approximately $2.0 million to support our potential hedge obligations. As of December 31, 2015, the maximum amountof hedge collateral we may be required to post is $9.8 million. The Currency Hedge Agreement does not qualify for hedge accounting treatment and therefore mark to market adjustments will be recognized in our ConsolidatedStatements of Comprehensive Loss. Mark to market adjustments are determined by quoted prices in markets that are not actively traded and for which significant inputs areobservable directly or indirectly, representing the Level 2 in the fair value hierarchy as defined by generally accepted accounting principles (“U.S. GAAP”). The Company isalso required to post collateral in connection with the mark to market adjustments based on defined thresholds. As of December 31, 2015, no collateral was posted under theagreement. 51 Tax We account for uncertain tax positions in accordance with U.S. GAAP. Significant management judgment is required in determining our provision for income taxes,deferred tax assets and liabilities and any valuation allowance recorded against net deferred tax assets. We have recorded a valuation allowance against all potential tax assets,due to uncertainties in our ability to utilize deferred tax assets, primarily consisting of certain net operating losses carried forward, before they expire. The valuation allowanceis based on estimates of taxable income in each of the jurisdictions in which we operate and the period over which our deferred tax assets will be recoverable. Impact of Inflation We do not believe that our operating results have been materially impacted by inflation during the past three years. However, we cannot be assured that our operatingresults will not be adversely affected by inflation in the future. We will continually seek to mitigate the adverse effects of inflation on the services that we use throughimproved operating efficiencies and cost containment initiatives. Recent Accounting Pronouncements Note 11 to the Consolidated Financial Statements included in Item 8 of this Annual Report on Form 10-K discusses accounting pronouncements recently issued orproposed but not yet required to be adopted. ITEM 7A.QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK. Interest Rate Risk We are subject to interest rate risk on our investment portfolio and borrowings under our PhaRMA Notes. We invest in marketable securities in accordance with our investment policy. The primary objectives of our investment policy are to preserve capital, maintain properliquidity to meet operating needs and maximize yields. Our investment policy specifies credit quality standards for our investments and limits the amount of credit exposure toany single issue, issuer or type of investment. We place our excess cash with high credit quality financial institutions, commercial companies, and government agencies inorder to limit the amount of credit exposure. Some of the securities we invest in may have market risk. This means that a change in prevailing interest rates may cause theprincipal amount of the investment to fluctuate. Our investment exposure to market risk for changes in interest rates relates to the increase or decrease in the amount of interest income we can earn on our portfolio,changes in the market value due to changes in interest rates and other market factors as well as the increase or decrease in any realized gains and losses. Our investmentportfolio includes only marketable securities and instruments with active secondary or resale markets to help ensure portfolio liquidity. A hypothetical 100 basis point drop ininterest rates along the entire interest rate yield curve would not significantly affect the fair value of our interest sensitive financial instruments. We generally have the abilityto hold our fixed-income investments to maturity and therefore do not expect that our operating results, financial position or cash flows will be materially impacted due to asudden change in interest rates. However, our future investment income may fall short of expectations due to changes in interest rates, or we may suffer losses in principal ifforced to sell securities which have declined in market value due to changes in interest rates or other factors, such as changes in credit risk related to the securities’ issuers. Tominimize this risk, we schedule our investments to have maturities that coincide with our expected cash flow needs, thus avoiding the need to redeem an investment prior toits maturity date. Accordingly, we do not believe that we have material exposure to interest rate risk arising from our investments. Generally, our investments are notcollateralized. We have not realized any significant losses from our investments. We do not use interest rate derivative instruments to manage exposure to interest rate changes. We ensure the safety and preservation of invested principal funds bylimiting default risk, market risk and reinvestment risk. We reduce default risk by investing in investment grade securities. 52 Foreign Currency Risk The majority of our transactions occur in U.S. dollars and we do not have operating subsidiaries or investments in foreign countries. Therefore, we are not subject tosignificant foreign currency exchange risk in our normal operations. In connection with the issuance by Royalty Sub of the PhaRMA Notes, we entered into a Currency Hedge Agreement to hedge certain risks associated with changes inthe value of the Japanese yen relative to the U.S. dollar. Under the Currency Hedge Agreement, we are required to post collateral based on our potential obligations under theCurrency Hedge Agreement as determined by periodic mark-to-market adjustments. Provided the Currency Hedge Agreement remains in effect, we may be required to pay anannual premium in the amount of $2.0 million from May 2016 through May 2020. Such payment will be required if, in May of the relevant year, the spot rate of exchange forJapanese yen-U.S. dollars (determined in accordance with the Currency Hedge Agreement) is such that the U.S. dollar is worth 100 yen or less. 53 ITEM 8.FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA BIOCRYST PHARMACEUTICALS, INC. CONSOLIDATED BALANCE SHEETS(In thousands, except per share amounts) December 31, 2015 2014ASSETS Cash and cash equivalents $28,899 $54,540 Restricted cash 1,612 150 Investments 22,664 18,232 Receivables from collaborations 6,243 3,849 Receivables from product sales — 5,641 Inventory 1,612 683 Prepaid expenses and other current assets 4,870 6,172 Deferred collaboration expense 90 76 Total current assets 65,990 89,343 Investments 47,683 41,116 Property and equipment, net 5,149 207 Deferred collaboration expense 265 177 Other assets 5,468 6,031 Total assets $124,555 $136,874 LIABILITIES AND STOCKHOLDERS’ EQUITY Accounts payable $9,307 $2,849 Accrued expenses 16,237 11,329 Interest payable 6,746 6,029 Deferred collaboration revenue 2,163 1,481 Deferred product sales revenue — 5,605 Non-recourse notes payable 30,000 30,000 Total current liabilities 64,453 57,293 Deferred collaboration revenue 9,674 3,552 Deferred rent 329 394 Lease financing obligation 2,375 — Stockholders’ equity: Preferred stock, $0.001 par value; shares authorized — 5,000; no shares outstanding — — Common stock, $0.01 par value; shares authorized — 200,000; shares issued and outstanding — 73,355 in 2015 and 71,955 in2014 734 720 Additional paid-in capital 558,113 542,943 Accumulated other comprehensive loss (206) (130)Accumulated deficit (510,917) (467,898)Total stockholders’ equity 47,724 75,635 Total liabilities and stockholders’ equity $124,555 $136,874 See accompanying notes to consolidated financial statements. 54 BIOCRYST PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF COMPREHENSIVE LOSS(In thousands, except per share amounts) Year Ended December 31, 2015 2014 2013Revenues Product sales, net $6,291 $33 $— Royalty revenue 2,386 3,025 2,562 Collaborative and other research and development 39,580 10,550 14,769 Total revenues 48,257 13,608 17,331 Expenses Cost of products sold 1,368 1 — Research and development 72,758 51,796 41,943 Selling, general and administrative 13,047 7,461 6,007 Royalty 528 121 98 Total operating expenses 87,701 59,379 48,048 Loss from operations (39,444) (45,771) (30,717)Interest and other income 535 93 93 Interest expense (5,200) (4,998) (4,778)Gain on foreign currency derivative 1,090 5,487 5,294 Net loss $(43,019) $(45,189) $(30,108)Basic and diluted net loss per common share $(0.59) $(0.68) $(0.55)Weighted average shares outstanding 72,901 66,773 55,216 Unrealized loss on available for sale investments $(76) $(134) $(23)Comprehensive loss $(43,095) $(45,323) $(30,131) See accompanying notes to consolidated financial statements. 55 BIOCRYST PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF CASH FLOWS(In thousands, except per share amounts) Year Ended December 31, 2015 2014 2013Operating activities: Net loss $(43,019) $(45,189) $(30,108)Adjustments to reconcile net loss to net cash used in operating activities: Depreciation, amortization, and impairment 180 177 304 Loss (gain) on disposal of property and equipment — 27 (47)Stock-based compensation expense 9,705 10,177 4,368 Amortization of debt issuance costs 439 439 439 Change in fair value of foreign currency derivative 564 (5,487) (5,294)Changes in operating assets and liabilities: Receivables 3,247 (7,375) 2,447 Inventory (929) (683) — Prepaid expenses and other assets 1,207 (1,943) (620)Deferred collaboration expense (102) 59 5,133 Accounts payable and accrued expenses 14,393 6,818 (2,049)Deferred revenue 1,199 4,429 (1,103)Net cash used in operating activities: (13,116) (38,551) (26,530)Investing activities: Acquisition of property and equipment (5,122) (106) (30)Proceeds from sale of property and equipment — — 50 Change in restricted cash (1,462) 1 157 Purchases of investments (53,830) (73,875) (23,974)Sales and maturities of investments 42,410 34,000 20,330 Net cash used in investing activities: (18,004) (39,980) (3,467)Financing activities: Sale of common stock, net — 106,600 23,633 Exercise of stock options 5,124 4,997 1,333 Employee stock purchase plan sales 355 310 124 Receipt of foreign currency derivative collateral — — 5,180 Net cash provided by financing activities: 5,479 111,907 30,270 (Decrease) increase in cash and cash equivalents (25,641) 33,376 273 Cash and cash equivalents at beginning of year 54,540 21,164 20,891 Cash and cash equivalents at end of year $28,899 $54,540 $21,164 See accompanying notes to consolidated financial statements. 56 BIOCRYST PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF STOCKHOLDERS’ EQUITY (DEFICIT)(In thousands, except per share amounts) Common Stock Additional Paid-In Capital Accumulated Other Comprehensive (Loss) Income Accumulated Deficit Total Stockholders’ Equity (Deficit)Balance at Decembe r 31, 2012 $509 $391,611 $27 $(392,601) $(454)Net loss — — — (30,108) (30,108)Other comprehensive loss — — (23) — (23)Exercise of stock options, 563 shares, net 6 1,327 — — 1,333 Employee stock purchase plan sales, 89 shares, net 1 123 — — 124 Issuance of common stock, 7,547 shares, net 75 23,559 — — 23,634 Stock-based compensation expense — 4,368 — — 4,368 Balance at December 31, 2013 591 420,988 4 (422,709) (1,126) Net loss — — — (45,189) (45,189)Other comprehensive loss — — (134) — (134)Exercise of stock options, 1,314 shares, net 13 4,984 — — 4,997 Employee stock purchase plan sales, 49 shares, net 1 309 — — 310 Issuance of common stock, 11,500 shares, net 115 106,485 — — 106,600 Stock-based compensation expense — 10,177 — — 10,177 Balance at December 31, 2014 720 542,943 (130) (467,898) 75,635 Net loss — — — (43,019) (43,019)Other comprehensive loss — — (76) — (76)Exercise of stock options, 1,359 shares, net 14 5,110 — — 5,124 Employee stock purchase plan sales, 41 shares, net — 355 — — 355 Stock-based compensation expense — 9,705 — — 9,705 Balance at December 31, 2015 $734 $558,113 $(206) $(510,917) $47,724 See accompanying notes to consolidated financial statements. 57 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Note 1 — Significant Accounting Policies and Concentrations of Risk The Company BioCryst Pharmaceuticals, Inc. (the “Company”) is a biotechnology company that designs, optimizes and develops novel small molecule drugs that block key enzymesinvolved in the pathogenesis of diseases. The Company focuses on the treatment of rare diseases in which significant unmet medical needs exist and align with its capabilitiesand expertise. The Company was incorporated in Delaware in 1986 and its headquarters is located in Durham, North Carolina. The Company integrates the disciplines ofbiology, crystallography, medicinal chemistry and computer modeling to discover and develop small molecule pharmaceuticals through the process known as structure-guideddrug design. BioCryst has incurred losses and negative cash flows from operations since inception. Based on its current operating plans, the Company expects it has sufficient liquidity, with its existing cash, restricted cash and investments of $100,858, to continue itsplanned operations through mid-2017. The Company’s liquidity needs, and ability to address those needs, will largely be determined by the success of its product candidatesand key development and regulatory events in the future. In order to continue its operations substantially beyond mid-2017 it will need to: (1) successfully secure or increaseU.S. Government funding of its programs, including procurement contracts; (2) out-license rights to certain of its products or product candidates, pursuant to which theCompany would receive cash milestones; (3) raise additional capital through equity or debt financings or from other sources; (4) obtain additional product candidateregulatory approvals, which would generate revenue and cash flow; (5) reduce spending on one or more research and development programs; and/or (6) restructure operations.The Company may issue securities through private placement transactions or registered public offerings pursuant to a registration statement filed with the SEC. Additionally,the Company retains the ability to offer for sale approximately $10,000 of securities, including common stock, preferred stock, depositary shares, stock purchase contracts,warrants and units from its effective shelf S-3 registration statement, which it filed with the Securities and Exchange Commission (“SEC”) on November 6, 2013. TheCompany will continue to incur operating losses and negative cash flows until revenues reach a level sufficient to support ongoing operations. Basis of Presentation Beginning in March 2011, the consolidated financial statements include the accounts of the Company and its wholly-owned subsidiary, JPR Royalty Sub LLC (“RoyaltySub”). Royalty Sub was formed in connection with a $30,000 financing transaction the Company completed on March 9, 2011. See Note 3, Royalty Monetization, for afurther description of this transaction. All intercompany transactions and balances have been eliminated. The Company’s consolidated financial statements have been prepared in accordance with accounting principles generally accepted in the United States (“U.S. GAAP”).Such consolidated financial statements reflect all adjustments that are, in management’s opinion, necessary to present fairly, in all material respects, the Company’sconsolidated financial position, results of operations, and cash flows. There were no adjustments other than normal recurring adjustments. Reclassifications Long term deferred rent as of December 31, 2014 has been reclassified to conform to the 2015 presentation. Cash and Cash Equivalents The Company generally considers cash equivalents to be all cash held in commercial checking accounts, certificates of deposit, money market accounts or investmentsin debt instruments with maturities of three months or less at the time of purchase. The carrying value of cash and cash equivalents approximates fair value due to the short-term nature of these items. Restricted Cash Restricted cash as of December 31, 2015 reflects $150 the Company is required to maintain in an interest bearing certificate of deposit to serve as collateral for acorporate credit card program, $59 in royalty revenue paid by Shionogi & Co., Ltd. (“Shionogi”) designated for interest on the PhaRMA Notes (defined in Note 3) and $1,403the Company is required to maintain as collateral for a letter of credit associated with the lease execution and build-out of its new Birmingham research facilities. 58 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Investments The Company invests in high credit quality investments in accordance with its investment policy, which is designed to minimize the possibility of loss. The objective ofthe Company’s investment policy is to ensure the safety and preservation of invested funds, as well as maintaining liquidity sufficient to meet cash flow requirements. TheCompany places its excess cash with high credit quality financial institutions, commercial companies, and government agencies in order to limit the amount of its creditexposure. In accordance with its policy, the Company is able to invest in marketable debt securities that may consist of U.S. Government and government agency securities,money market and mutual fund investments, municipal and corporate notes and bonds, commercial paper and asset or mortgage-backed securities, among others. TheCompany’s investment policy requires it to purchase high-quality marketable securities with a maximum individual maturity of three years and requires an average portfoliomaturity of no more than 18 months. Some of the securities the Company invests in may have market risk. This means that a change in prevailing interest rates may cause theprincipal amount of the investment to fluctuate. To minimize this risk, the Company schedules its investments with maturities that coincide with expected cash flow needs,thus avoiding the need to redeem an investment prior to its maturity date. Accordingly, the Company does not believe it has a material exposure to interest rate risk arisingfrom its investments. Generally, the Company’s investments are not collateralized. The Company has not realized any significant losses from its investments. The Company classifies all of its investments as available-for-sale. Unrealized gains and losses on investments are recognized in comprehensive loss, unless anunrealized loss is considered to be other than temporary, in which case the unrealized loss is charged to operations. The Company periodically reviews its investments forother than temporary declines in fair value below cost basis and whenever events or changes in circumstances indicate that the carrying amount of an asset may not berecoverable. The Company believes the individual unrealized losses represent temporary declines primarily resulting from interest rate changes. Realized gains and losses arereflected in interest and other income in the Consolidated Statements of Comprehensive Loss and are determined using the specific identification method with transactionsrecorded on a settlement date basis. Investments with original maturities at date of purchase beyond three months and which mature at or less than 12 months from the balancesheet date are classified as current. Investments with a maturity beyond 12 months from the balance sheet date are classified as long-term. At December 31, 2015, theCompany believes that the costs of its investments are recoverable in all material respects. The following tables summarize the fair value of the Company’s investments by type. The estimated fair value of the Company’s fixed income investments areclassified as Level 2 in the fair value hierarchy as defined in U.S. GAAP. These valuations are based on observable direct and indirect inputs, primarily quoted prices ofsimilar, but not identical, instruments in active markets or quoted prices for identical or similar instruments in markets that are not active. These fair values are obtained fromindependent pricing services which utilize Level 2 inputs. December 31, 2015 Amortized Cost Accrued Interest Gross Unrealized Gains Gross Unrealized Losses Estimated Fair ValueObligations of U.S. Government and its agencies $26,557 $88 $— $(99) $26,546 Corporate debt securities 21,820 184 — (41) 21,963 Certificates of deposit 21,884 21 5 (72) 21,838 Total investments $70,261 $293 $5 $(212) $70,347 December 31, 2014 Amortized Cost Accrued Interest Gross Unrealized Gains Gross Unrealized Losses Estimated Fair ValueObligations of U.S. Government and its agencies $20,307 $22 $— $(23) $20,306 Corporate debt securities 27,152 151 5 (47) 27,261 Commercial paper 11,838 6 — (63) 11,781 Total investments $59,297 $179 $5 $(133) $59,348 The following table summarizes the scheduled maturity for the Company’s investments at December 31, 2015 and 2014. 2015 2014Maturing in one year or less $22,664 $18,232 Maturing after one year through two years 28,395 25,459 Maturing after two years 19,288 15,657 Total investments $70,347 $59,348 59 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Receivable from Collaborations Receivables from collaborations are recorded for amounts due to the Company related to reimbursable research and development costs from the U.S. Department ofHealth and Human Services, royalty receivables from Shionogi and Seqirus UK Limited (“SUL”), and product sales to SUL. These receivables are evaluated to determine ifany reserve or allowance should be established at each reporting date. At December 31, 2015 and 2014, the Company had the following receivables. December 31, 2015 Billed Unbilled TotalU.S. Department of Health and Human Services $— $5,536 $5,536 Shionogi & Co. Ltd. 469 — 469 Seqirus UK Limited 210 28 238 Total receivables $679 $5,564 $6,243 December 31, 2014 Billed Unbilled TotalU.S. Department of Health and Human Services $— $2,778 $2,778 Shionogi & Co. Ltd. 1,071 — 1,071 Total receivables $1,071 $2,778 $3,849 Monthly invoices are submitted to the U.S. Department of Health and Human Services related to reimbursable research and development costs. The Company is alsoentitled to monthly reimbursement of indirect costs based on rates stipulated in the underlying contract. The Company’s calculations of its indirect cost rates are subject toaudit by the U.S. Government. Receivables from Product Sales Receivables from product sales are recorded for amounts due to the Company related to sales of RAPIVAB. These receivables are evaluated to determine if any reserveor allowance should be established at each reporting date. Inventory At December 31, 2015 and 2014, the Company’s inventory consisted of RAPIVAB finished goods inventory and work in process. Inventory is stated at the lower ofcost, determined under the first-in, first-out (“FIFO”) method, or market. The Company expenses costs related to the production of inventories as research and developmentexpenses in the period incurred until such time it is believed that future economic benefit is expected to be recognized, which generally is reliant upon receipt of regulatoryapproval. Upon regulatory approval, the Company will capitalize subsequent costs related to the production of inventories. During 2014, in connection with the FDA approval of RAPIVAB, the Company began capitalizing costs associated with the production of RAPIVAB inventories. The Company’s inventory consisted of the following: As of December 31, 2015 2014Work in process $1,612 $267 Finished goods — 416 Net inventories $1,612 $683 60 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Property and Equipment Property and equipment are recorded at cost. Depreciation is computed using the straight-line method over the estimated useful lives of the assets. Computer equipmentis depreciated over a life of three years. Laboratory equipment, office equipment, and software are depreciated over a life of five years. Furniture and fixtures are depreciatedover a life of seven years. Leasehold improvements are amortized over their estimated useful lives or the remaining lease term, whichever is less. Property consists of a leasedbuilding which did not meet the sale-leaseback criteria and is recorded at its fair value, less depreciation. The building is being depreciated over a period of ten years equal tothe term of the related lease In accordance with U.S. GAAP, the Company periodically reviews its property and equipment for impairment when events or changes in circumstances indicate that thecarrying amount of such assets may not be recoverable. Determination of recoverability is based on an estimate of undiscounted future cash flows resulting from the use of theasset and its eventual disposition. In the event that such cash flows are not expected to be sufficient to recover the carrying amount of the assets, the assets are written down totheir estimated fair values. Property and equipment to be disposed of are reported at the lower of carrying amount or fair value less cost to sell. Patents and Licenses The Company seeks patent protection on all internally developed processes and products. All patent related costs are expensed to selling, general and administrativeexpenses when incurred as recoverability of such expenditures is uncertain. Accrued Expenses The Company generally enters into contractual agreements with third-party vendors who provide research and development, manufacturing, and other services in theordinary course of business. Some of these contracts are subject to milestone-based invoicing and services are completed over an extended period of time. The Companyrecords liabilities under these contractual commitments when it determines an obligation has been incurred, regardless of the timing of the invoice. This process involvesreviewing open contracts and purchase orders, communicating with applicable Company personnel to identify services that have been performed on its behalf and estimatingthe level of service performed and the associated cost incurred for the service when the Company has not yet been invoiced or otherwise notified of actual cost. The majorityof service providers invoice the Company monthly in arrears for services performed. The Company makes estimates of accrued expenses as of each balance sheet date in itsfinancial statements based on the facts and circumstances. The Company periodically confirms the accuracy of its estimates with the service providers and makes adjustmentsif necessary. Examples of estimated accrued expenses include: • fees paid to Clinical Research Organizations (“CROs”) in connection with preclinical and toxicology studies and clinical trials; • fees paid to investigative sites in connection with clinical trials; • fees paid to contract manufacturers in connection with the production of our raw materials, drug substance and drug products; and • professional fees. The Company bases its expenses related to clinical trials on its estimates of the services received and efforts expended pursuant to contracts with multiple researchinstitutions and CROs that conduct and manage clinical trials on the Company’s behalf. The financial terms of these agreements are subject to negotiation, vary from contractto contract and may result in uneven payment flows. Payments under some of these contracts depend on factors such as the successful enrollment of patients and thecompletion of clinical trial milestones. In accruing service fees, the Company estimates the time period over which services will be performed and the level of effort expendedin each period. If the actual timing of the performance of services or the level of effort varies from the estimate, the Company will adjust the accrual accordingly. 61 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Accrued expenses were comprised of the following: December 31, 2015 2014Compensation and benefits $424 $2,105 Development costs 10,398 4,232 Inventory 549 397 Professional fees 242 238 Duties and taxes 102 75 Other 4,522 4,282 Total accrued expenses $16,237 $11,329 As of December 31, 2015 and 2014, the carrying value of accrued expenses approximates their fair value due to their short-term settlement. Income Taxes The liability method is used in the Company’s accounting for income taxes. Under this method, deferred tax assets and liabilities are determined based on differencesbetween financial reporting and tax bases of assets and liabilities and are measured using the enacted tax rates and laws that are expected to be in effect when the differencesare expected to reverse. Accumulated Other Comprehensive Loss Accumulated other comprehensive loss is comprised of unrealized gains and losses on available-for-sale investments and is disclosed as a separate component ofstockholders’ equity. Amounts reclassified from accumulated other comprehensive loss are recorded as interest and other income on the Consolidated Statements ofComprehensive Loss. During 2015, realized gains of $13 were reclassified out of accumulated other comprehensive loss. No reclassifications out of accumulated othercomprehensive loss were recorded during 2014. Revenue Recognition The Company recognizes revenues from collaborative and other research and development arrangements, royalties and product sales when realized or realizable andearned. Revenue is realized or realizable and earned when all of the following criteria are met: (i) persuasive evidence of an arrangement exists; (ii) delivery has occurred orservices have been rendered; (iii) the seller’s price to the buyer is fixed or determinable; and (iv) collectability is reasonably assured. Collaborative and Other Research and Development Arrangements and Royalties Revenue from license fees, royalty payments, event payments, and research and development fees are recognized as revenue when the earnings process is complete andthe Company has no further continuing performance obligations or the Company has completed the performance obligations under the terms of the agreement. Fees receivedunder licensing agreements that are related to future performance are deferred and recognized over an estimated period determined by management based on the terms of theagreement and the products licensed. Revisions to revenue or profit estimates as a result of changes in the estimated revenue period are recognized prospectively. Under certain of the Company’s license agreements, the Company receives royalty payments based upon its licensees’ net sales of covered products. The Companyrecognizes royalty revenues when it can reliably estimate such amounts and collectability is reasonably assured. For arrangements that involve the delivery of more than one element, each product, service and/or right to use assets is evaluated to determine whether it qualifies as aseparate unit of accounting. This determination is based on whether the deliverable has “stand-alone value” to the customer. The consideration that is fixed or determinable isthen allocated to each separate unit of accounting based on the relative selling price of each deliverable. The estimated selling price of each deliverable is determined using thefollowing hierarchy of values: (i) vendor-specific objective evidence of fair value, (ii) third-party evidence of selling price (“TPE”) and (iii) best estimate of selling price(“BESP”). The BESP reflects our best estimate of what the selling price would be if the deliverable was regularly sold by the Company on a stand-alone basis. In most casesthe Company expects to use TPE or BESP for allocating consideration to each deliverable. The consideration allocated to each unit of accounting is recognized as the relatedgoods or services are delivered, limited to the consideration that is not contingent upon future deliverables. Analyzing the arrangement to identify deliverables requires the useof judgment, and each deliverable may be an obligation to deliver services, a right or license to use an asset, or another performance obligation. 62 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) In June 2015, the Company entered into a License Agreement (the “SUL Agreement”) granting Seqirus UK Limited (“SUL”) and its affiliates worldwide rights,excluding Israel, Japan, Korea and Taiwan, to develop, manufacture and commercialize RAPIVAB. The SUL Agreement provides for various types of payments, including anon-refundable upfront fee, milestone payments, and future royalties. Analysis of the SUL Agreement identified three deliverables: (i) license rights, (ii) inventory and (iii)regulatory support to obtain Canadian and European Union (“EU”) marketing approvals. The Company received an upfront payment of $33,740 from SUL, of which $7,000was determined to be contingent upon EU marketing approval and will be deferred until that time. Approximately $21,777 of the upfront payment was allocated to the licenserights and recognized as revenue in the second quarter. Approximately $3,740 of the upfront payment was allocated to the pending sale of inventory and was recognizedduring the third quarter, when the inventory transfer was completed. Approximately $1,223 of the revenue from the SUL Agreement will be recognized over the expectedperiod of involvement in these regulatory support activities. Milestone payments are recognized as licensing revenue upon the achievement of specified milestones if (i) the milestone is substantive in nature and the achievementof the milestone was not reasonably assured at the inception of the agreement; and (ii) the fees are non-refundable. Any milestone payments received prior to satisfying theserevenue recognition criteria are recorded as deferred revenue. Under the terms of the SUL Agreement, the Company may receive up to $12,000 in additional payments related to the successful achievement of regulatorymilestones, including marketing approval (i) by the FDA for a pediatric indication, (ii) by the EMA for an adult indication in the EU and (iii) by Health Products and FoodBranch of Health Canada (“Health Canada”) for an adult indication in Canada. The Company evaluated each event based payment under the provisions of ASU 2010-17,Milestone Method of Revenue Recognition , and determined that each event based payment met the criteria to be considered substantive and represents a milestone under themilestone method of accounting. No event based payments were achieved during the periods presented. Reimbursements received for direct out-of-pocket expenses related to research and development costs are recorded as revenue in the Consolidated Statements ofComprehensive Loss rather than as a reduction in expenses. Under the Company’s contracts with the Biomedical Advanced Research and Development Authority within theUnited States Department of Health and Human Services (”BARDA/HHS”) and the National Institute of Allergy and Infectious Diseases (“NIAID/HHS”), revenue isrecognized as reimbursable direct and indirect costs are incurred. Product Sales The Company recognizes revenue for sales of RAPIVAB when title and substantially all the risks and rewards of ownership have transferred to the customer, whichgenerally occurs on the date of shipment from our specialty distributors, utilizing the Sell-Through revenue recognition methodology. Product sales are recognized when thereis persuasive evidence that an arrangement exists, title has passed, the price is fixed and determinable, and collectability is reasonably assured. Product sales are recognizednet of estimated allowances, discounts, sales returns, chargebacks and rebates. In the United States, and prior to the SUL Agreement, the Company sold RAPIVAB tospecialty distributors, who in turn, sell to physician offices, hospitals and federal, state and commercial health care organizations. With the completion of the SUL worldwidelicense of RAPIVAB, SUL will be primarily responsible for sales of RAPIVAB, other than U.S. Government stockpiling sales, and the Company’s commercial sales will beminimal. Sales deductions consist of statutory rebates to state Medicaid, Medicare and other government agencies and sales discounts (including trade discounts and distributionservice fees). These deductions are recorded as reductions from revenue from RAPIVAB in the same period as the related sales with estimates of future utilization derivedfrom historical experience adjusted to reflect known changes in the factors that impact such reserves. The Company utilizes data from external sources to help it estimate gross-to-net sales adjustments as they relate to the recognition of revenue for RAPIVAB sold.Externally sourced data includes, but is not limited to, information obtained from specialty distributors with respect to their inventory levels and their sell-through tocustomers, as well as information from third-party suppliers of market research data to the pharmaceutical industry. The Company accounts for these sales deductions in accordance with authoritative guidance on revenue recognition when consideration is given by a vendor to acustomer. The Company has categorized and described more fully the following significant sales deductions, all of which involve estimates and judgments, which the Companyconsiders to be critical accounting estimates, and require it to use information from external sources. 63 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Rebates and Chargebacks Statutory rebates to state Medicaid agencies and Medicare are based on statutory discounts to RAPIVAB’s selling price. As it can take up to nine months or more forinformation to be received on actual usage of RAPIVAB in Medicaid and other governmental programs, the Company maintains reserves for amounts payable under theseprograms relating to RAPIVAB sales. Chargebacks claimed by specialty distributors are based on the differentials between product acquisition prices paid by the specialty distributors and lower governmentcontract pricing paid by eligible customers covered under federally qualified programs. The amount of the reserve for rebates and chargebacks is based on multiple qualitative and quantitative factors, including the historical and projected utilization levels,historical payment experience, changes in statutory laws and interpretations as well as contractual terms, product pricing (both normal selling prices and statutory ornegotiated prices), changes in prescription demand patterns and utilization of the Company’s product through public benefit plans, and the levels of RAPIVAB inventory inthe distribution channel. The Company acquires prescription utilization data from third-party suppliers of market research data to the pharmaceutical industry. The Companyupdates its estimates and assumptions each period and records any necessary adjustments to its reserves. Settlements of rebates and chargebacks typically occur within ninemonths from point of sale. To the extent actual rebates and chargebacks differ from the Company’s estimates, additional reserves may be required or reserves may need to bereversed, either of which would impact current period product revenue. Discounts and Sales Incentives Discounts and other sales incentives primarily consist of Inventory Management Agreement (“IMA”) Fees. Per contractual agreements with the Company’s specialtydistributors, the Company provides an IMA fee based on a percentage of their purchases of RAPIVAB. The IMA fee rates are set forth in individual contracts. The Companytracks sales to these distributors each period and accrues a liability relating to the unpaid portion of these fees by applying the contractual rates to such product sales. Product Returns The Company does not record a product return allowance as it does not offer the ability to return goods once a bonafide shipment has been accepted by a specialtydistributor. The Company recorded the following revenues for the years ended December 31: 2015 2014 2013Product sales, net $6,291 $33 $— Royalty revenue 2,386 3,025 2,562 Collaborative and other research and development revenues: U.S. Department of Health and Human Services 16,337 9,366 13,585 Green Cross Corporation 132 — — Shionogi (Japan) 1,184 1,184 1,184 Seqirus UK Limited 21,927 — — Total collaborative and other research and development revenues 39,580 10,550 14,769 Total revenues $48,257 $13,608 $17,331 Advertising The Company engages in very limited distribution and direct-response advertising when promoting RAPIVAB. Advertising and promotional costs are expensed as thecosts are incurred. Advertising and product promotion expenses were $103 and $290 for the years ended December 31, 2015 and 2014, respectively. Research and Development Expenses The Company’s research and development costs are charged to expense when incurred. Research and development expenses include all direct and indirectdevelopment costs related to the development of the Company’s portfolio of product candidates. Advance payments for goods or services that will be used or rendered forfuture research and development activities are deferred and capitalized. Such amounts are recognized as expense when the related goods are delivered or the related servicesare performed. Research and development expenses include, among other items, personnel costs, including salaries and benefits, manufacturing costs, clinical, regulatory, andtoxicology services performed by CROs, materials and supplies, and overhead allocations consisting of various administrative and facilities related costs. Most of theCompany’s manufacturing and clinical and preclinical studies are performed by third-party CROs. Costs for studies performed by CROs are accrued by the Company over theservice periods specified in the contracts and estimates are adjusted, if required, based upon the Company’s on-going review of the level of services actually performed. 64 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Additionally, the Company has license agreements with third parties, such as Albert Einstein College of Medicine of Yeshiva University (“AECOM”), IndustrialResearch, Ltd. (“IRL”), and the University of Alabama at Birmingham (“UAB”), which require fees related to sublicense agreements or maintenance fees. The Companyexpenses sublicense payments as incurred unless they are related to revenues that have been deferred, in which case the expenses are deferred and recognized over the relatedrevenue recognition period. The Company expenses maintenance payments as incurred. Deferred collaboration expenses represent sub-license payments, paid to the Company’s academic partners upon receipt of consideration from various commercialpartners, and other consideration paid to our academic partners for modification to existing license agreements. These deferred expenses would not have been incurredwithout receipt of such payments or modifications from the Company’s commercial partners and are being expensed in proportion to the related revenue being recognized.The Company believes that this accounting treatment appropriately matches expenses with the associated revenue. Stock-Based Compensation All share-based payments, including grants of stock option awards and restricted stock unit awards, are recognized in the Company’s Consolidated Statements ofComprehensive Loss based on their fair values. The fair value of stock option awards is estimated using the Black-Scholes option pricing model. The fair value of restrictedstock unit awards is based on the grant date closing price of the common stock. Stock-based compensation cost is recognized as expense on a straight-line basis over therequisite service period of the award. In addition, we have outstanding performance-based stock options for which no compensation expense is recognized until“performance” has occurred. Interest Expense and Deferred Financing Costs Interest expense for the years ended December 31, 2015, 2014 and 2013 was $5,200, $4,998 and $4,778, respectively, and relates to the issuance of the PhaRMA Notes.Costs directly associated with the issuance of the PhaRMA Notes have been capitalized and are included in other non-current assets on the Consolidated Balance Sheets.These costs are being amortized to interest expense over the term of the PhaRMA Notes using the effective interest rate method. Amortization of deferred financing costsincluded in interest expense was $439 for each of the years ended December 31, 2015, 2014 and 2013. Currency Hedge Agreement In connection with the issuance by Royalty Sub of the PhaRMA Notes, the Company entered into a Currency Hedge Agreement to hedge certain risks associated withchanges in the value of the Japanese yen relative to the U.S. dollar. The Currency Hedge Agreement does not qualify for hedge accounting treatment; therefore mark tomarket adjustments are recognized in the Company’s Consolidated Statements of Comprehensive Loss. Cumulative mark to market adjustments for the years endedDecember 31, 2015, 2014 and 2013 resulted in a loss of $564 and gains of $5,487 and $5,294, respectively. Mark to market adjustments are determined by a third partypricing model which uses quoted prices in markets that are not actively traded and for which significant inputs are observable directly or indirectly, representing Level 2 in thefair value hierarchy as defined by U.S. GAAP. In addition, a realized currency exchange gain of $1,654 was recognized in 2015 related to the exercise of a U.S.dollar/Japanese yen currency option under our foreign currency hedge. The Company is also required to post collateral in connection with the mark to market adjustmentsbased on defined thresholds. As of December 31, 2015 and December 31, 2014, no hedge collateral was posted under the agreement. Net Loss Per Share Net loss per share is based upon the weighted average number of common shares outstanding during the period. Diluted loss per share is equivalent to basic net loss pershare for all periods presented herein because common equivalent shares from unexercised stock options, outstanding warrants, and common shares expected to be issuedunder the Company’s employee stock purchase plan were anti-dilutive. The calculation of diluted earnings per share for the years ended December 31, 2015, 2014, and 2013does not include 3,524, 3,991 and 1,430 respectively, of potential common shares as their impact would be anti-dilutive. Use of Estimates The preparation of financial statements in conformity with U.S. GAAP requires the Company to make estimates and assumptions that affect the amounts reported in thefinancial statements. Actual results could differ from those estimates. 65 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Significant Customers and Other Risks Significant Customers Prior to the SUL Agreement, the Company relied primarily on three specialty distributors to purchase and supply the majority of RAPIVAB. These threepharmaceutical specialty distributors accounted for greater than 90% of all RAPIVAB product sales to date and accounted for predominantly all of the Company’soutstanding receivables from product sales. The loss of one or more of these specialty distributors as a customer could negatively impact the commercialization of RAPIVAB.However, the Company will utilize these specialty distributors on a limited basis subsequent to the SUL collaboration as SUL, and other peramivir collaboration partners, willbe responsible for commercial sales on a worldwide basis. In addition, in connection with the SUL collaboration, all peramivir sales (i.e., RAPIVAB, RAPIACTA, andPERAMIFLU) will be made by the Company’s partners and the Company will be reliant on these partners to generate sales and remit cash to satisfy receivables. The Company’s primary source of revenue that has an underlying cash flow stream is the reimbursement of RAPIVAB and BCX4430 development expenses earnedunder cost-plus-fixed-fee contracts with BARDA/HHS and NIAID/HHS, respectively. The Company relies on BARDA/HHS and NIAID/HHS to reimburse predominantly allof the development costs for its RAPIVAB and BCX4430 programs. Accordingly, reimbursement of these expenses represents a significant portion of the Company’scollaborative and other research and development revenues. The completion (as with the June 30, 2014 BARDA/HHS peramivir development contract) or termination of theNIAID/HHS and BARDA/HHS BCX4430 contracts could negatively impact the Company’s future Consolidated Statements of Comprehensive Loss and Cash Flows. Inaddition, the Company also recognizes royalty revenue from the net sales of RAPIACTA by Shionogi; however, the underlying cash flow from these royalty payments goesdirectly to pay the interest, and then the principal, on the Company’s non-recourse notes payable. Payment of the interest and the ultimate repayment of principal of thesenotes will be entirely funded by future royalty payments derived from net sales of RAPIACTA. Further, the Company’s drug development activities are performed by alimited group of third party vendors. If any of these vendors were unable to perform their services, this could significantly impact the Company’s ability to complete its drugdevelopment activities. Risks from Third Party Manufacturing and Distribution Concentration The Company relies on single source manufacturers for active pharmaceutical ingredient and finished drug product manufacturing of RAPIVAB, as well as for its otherproduct candidates in development. Delays in the manufacture or distribution of any product could adversely impact the commercial revenue and future procurementstockpiling of RAPIVAB. Credit Risk Cash equivalents and investments are financial instruments which potentially subject the Company to concentration of risk to the extent recorded on the ConsolidatedBalance Sheets. The Company deposits excess cash with major financial institutions in the United States. Balances may exceed the amount of insurance provided on suchdeposits. The Company believes it has established guidelines for investment of its excess cash relative to diversification and maturities that maintain safety and liquidity. Tominimize the exposure due to adverse shifts in interest rates, the Company maintains a portfolio of investments with an average maturity of approximately 18 months or less.Other than product sale and collaborative partner receivables discussed above, the majority of the Company’s receivables from collaborations are due from the U.S.Government, for which there is no assumed credit risk. Note 2 — Property and Equipment Property and equipment consisted of the following at December 31: 2015 2014Furniture and fixtures $718 $542 Office equipment 1,122 1,115 Software 1,427 1,423 Laboratory equipment 6,004 5,786 Leased equipment 63 63 Leasehold improvements 5,610 5,303 Construction in progress 2,821 — Building 1,589 — 19,354 14,232 Less accumulated depreciation and amortization (14,205) (14,025)Property and equipment, net $5,149 $207 66 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Depreciation and amortization expense for the years ended December 31, 2015, 2014 and 2013 was $180, $177 and $304, respectively. Note 3— Royalty Monetization Overview On March 9, 2011, the Company completed a $30,000 financing transaction to monetize certain future royalty and milestone payments under the Shionogi Agreement,pursuant to which Shionogi licensed from the Company the rights to market RAPIACTA in Japan and, if approved for commercial sale, Taiwan. The Company received netproceeds of $22,691 from the transaction after transaction costs of $4,309 and the establishment of a $3,000 interest reserve account by Royalty Sub, available to help coverinterest shortfalls in the future. All of the interest reserve account has been fully utilized with the September 2012 interest payment. As part of the transaction, the Company entered into a purchase and sale agreement dated as of March 9, 2011 with Royalty Sub, whereby the Company transferred toRoyalty Sub, among other things, (i) its rights to receive certain royalty and milestone payments from Shionogi arising under the Shionogi Agreement, and (ii) the right toreceive payments under a Japanese yen/US dollar foreign currency hedge arrangement (as further described below, the “Currency Hedge Agreement”) put into place by theCompany in connection with the transaction. Royalty payments will be paid by Shionogi in Japanese yen and milestone payments will paid in U.S. dollars. The Company’scollaboration with Shionogi was not impacted as a result of this transaction. Non-Recourse Notes Payable On March 9, 2011, Royalty Sub completed a private placement to institutional investors of $30,000 in aggregate principal amount of its PhaRMA Senior Secured14.0% Notes due 2020 (the “PhaRMA Notes”). The PhaRMA Notes were issued by Royalty Sub under an Indenture, dated as of March 9, 2011 (the “Indenture”), by andbetween Royalty Sub and U.S. Bank National Association, as Trustee. Principal and interest on the PhaRMA Notes issued are payable from, and are secured by, the rights toroyalty and milestone payments under the Shionogi Agreement transferred by the Company to Royalty Sub and payments, if any, made to Royalty Sub under the CurrencyHedge Agreement. The PhaRMA Notes bear interest at 14% per annum, payable annually in arrears on September 1st of each year. The Company remains entitled to receiveany royalties and milestone payments related to sales of peramivir by Shionogi following repayment of the PhaRMA Notes. Royalty Sub’s obligations to pay principal and interest on the PhaRMA Notes are obligations solely of Royalty Sub and are without recourse to any other person,including the Company, except to the extent of the Company’s pledge of its equity interests in Royalty Sub in support of the PhaRMA Notes. The Company may, but is notobligated to, make capital contributions to a capital account that may be used to redeem, or on up to one occasion pay any interest shortfall on, the PhaRMA Notes. In September 2013, Royalty Sub paid $1,844 of interest on the PhaRMA Notes from royalty payments received from RAPIACTA ® sales from the preceding fourcalendar quarters. This payment resulted in an obligation shortfall of approximately $2,356 associated with accrued interest due September 3, 2013. As stipulated under thePhaRMA Notes Indenture, if the amount available for payment on any Payment Date is insufficient to pay all of the interest due on a Payment Date, the shortfall in interestwill accrue interest at the interest rate applicable to the PhaRMA Notes compounded annually. Accordingly, commencing in September 2013, the Company began accruinginterest at 14% per annum on the interest shortfall of $2,356. In March, June and August of 2014, Royalty Sub paid additional interest of $446, $1,882 and $70, respectively,bringing the 2013 shortfall down to $222 as of September 30, 2014. Under the terms of the Indenture, Royalty Sub’s inability to pay the full amount of interest payable inSeptember 2013 by the next succeeding Payment Date for the PhaRMA Notes, which was September 1, 2014, constituted an event of default. Accordingly, the PhaRMANotes and related accrued interest have been classified as current liabilities on the December 31, 2014 balance sheet. As a result of the event of default under the PhaRMANotes, the holders of the PhaRMA Notes may pursue acceleration of the PhaRMA Notes, may foreclose on the collateral securing the PhaRMA Notes and the equity interestin Royalty Sub and exercise other remedies available to them under the Indenture in respect of the PhaRMA Notes. In such event, the Company may not realize the benefit offuture royalty payments that might otherwise accrue to it following repayment of the PhaRMA Notes and it might otherwise be adversely affected. Due to the non-recoursenature of the PhaRMA Notes, in the event of any potential acceleration or foreclosure, the primary impact to the Company would be the loss of future royalty payments fromShionogi and legal costs associated with retiring the PhaRMA Notes. In addition, the Company may incur costs associated with liquidating the related Currency HedgeAgreement, which would no longer be required in the event of foreclosure, or if the PhaRMA Notes cease to be outstanding. As the PhaRMA Notes are the obligation ofRoyalty Sub and non-recourse to the Company, the event of default of the PhaRMA Notes is not expected to have a significant impact on the Company’s future results ofoperations or cash flows. As of December 31, 2015, the PhaRMA Notes remain in default. 67 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) The Indenture does not contain any financial covenants. The Indenture includes customary representations and warranties of Royalty Sub, affirmative and negativecovenants of Royalty Sub, Events of Default and related remedies, and provisions regarding the duties of the Trustee, indemnification of the Trustee, and other matters typicalfor indentures used in structured financings of this type. As of December 31, 2015, the aggregate fair value of the PhaRMA Notes was estimated to be approximately 50% of its carrying value of $30,000. The estimated fairvalue of the PhaRMA Notes is classified as Level 2 in the fair value hierarchy as defined in U.S. GAAP. The PhaRMA Notes are redeemable at the option of Royalty Sub at any time at a redemption price equal to the outstanding principal balance of the PhaRMA Notesbeing redeemed plus accrued and unpaid interest through the redemption date on the PhaRMA Notes being redeemed. Foreign Currency Hedge In connection with the issuance by Royalty Sub of the PhaRMA Notes, the Company entered into a Currency Hedge Agreement to hedge certain risks associated withchanges in the value of the Japanese yen relative to the U.S. dollar. Under the Currency Hedge Agreement, the Company has the right to purchase dollars and sell yen at a rateof 100 yen per dollar for which the Company may be required to pay a premium in each year from 2016 through 2020, provided the Currency Hedge Agreement remains ineffect. A payment of $1,950 will be required if, on May 18 of the relevant year, the U.S. dollar is worth 100 yen or less as determined in accordance with the Currency HedgeAgreement. The Currency Hedge Agreement does not qualify for hedge accounting treatment; therefore mark to market adjustments are recognized in the Company’s ConsolidatedStatement of Comprehensive Loss. Cumulative mark to market adjustments in 2015, 2014 and 2013 resulted in a loss of $564 and gains of $5,487 and $5,294 respectively. Inaddition, a realized currency exchange gain of $1,654 was recognized in 2015 related to the exercise of a U.S. dollar/Japanese yen currency option under our foreign currencyhedge. The Company is also required to post collateral in connection with the mark to market adjustments based on defined thresholds. As of December 31, 2015 and 2014,no collateral was posted under the Currency Hedge Agreement. The Company will not be required at any time to post collateral exceeding the maximum premium paymentsremaining payable under the Currency Hedge Agreement. As of December 31, 2015, the maximum amount of hedge collateral the Company may be required to post is$9,750. Note 4 — Lease Obligations and Other Contingencies The Company has the following minimum payments under operating lease obligations that existed at December 31, 2015: 2016 $651 2017 871 2018 870 2019 820 2020 651 Thereafter 3,045 Total minimum payments $6,908 The obligations in the preceding table are primarily related to the Company’s leases for buildings in Birmingham, Alabama and Durham, North Carolina. The lease forthe Company’s headquarters in Durham, North Carolina expires June 30, 2020. The lease for the existing facility in Birmingham, Alabama currently expires on June 30, 2016;however, in 2015, the Company leased an additional approximate 32,000 square feet in Birmingham to house its new research facility. The Company began construction onleasehold improvements for its new research facility in 2015 and this lease obligates the Company for $4,839 of lease payments into 2027. Rent expense for operating leaseswas $664, $633, and $526 in 2015, 2014, and 2013, respectively.Lease Financing ObligationBased on the terms of the lease agreement for the new research facility in Birmingham, Alabama, the Company had construction period risks during the constructionperiod and the Company was deemed the owner of the building (for accounting purposes only) during the construction period. Accordingly, the Company recorded an asset of$1,589, representing the Company’s leased portion of the building and recorded a corresponding liability. Upon completion of leasehold improvement construction, theCompany will not meet the sale-leaseback criteria for de-recognition of the building asset and liability. Therefore, the lease is accounted for as a financing obligation. Theasset will be depreciated over the expected duration of the lease, and rental payments will be treated as principal and interest payments on the lease financing obligationliability. The underlying accounting for this transaction has no impact on cash flows associated with the underlying lease and or construction in process. 68 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) At December 31, 2015, the lease financing obligation balance was $2,375 and was recorded as a long term liability on the consolidated balance sheets. The remainingfuture minimum payments under the lease financing obligation are $4,839. Note 5 — Stockholders’ Equity Sales of Common Stock On March 3, 2015, the Company filed a $150,000 shelf registration statement on Form S-3 with the SEC. This shelf registration statement became effective upon filingand allows the Company to sell securities, including common stock, preferred stock, depository shares, stock purchase contracts, warrants and units, from time to time atprices and on terms to be determined at the time of sale. The Company intends to file a post-effective amendment to this registration statement, which will allow for its use bythe Company when declared effective by the SEC’s staff. On November 6, 2013, the Company filed a $125,000 shelf registration statement on Form S-3 with the SEC. This shelf registration statement was declared effective inNovember 2013 and allows us to sell securities, including common stock, preferred stock, depository shares, stock purchase contracts, warrants and units, from time to time atprices and on terms to be determined at the time of sale. On June 3, 2014, the Company issued 11,500 shares of common stock for gross proceeds of $115,000 under this$125,000 shelf registration statement. Net proceeds were approximately $107,800 after deducting underwriting discounts and offering expenses. The Company has $10,000remaining under this shelf registration statement In August 2013, the Company completed a public offering of 4,600 shares of its common stock at a price of $4.40 per share, which included the underwriters’ over-allotment allocation of an additional 600 shares. Net proceeds were approximately $18,500 after deducting underwriting discounts and offering expenses. Shares of commonstock in this offering were sold under the $70,000 shelf registration statement declared effective in July 2011. In June 2011, the Company entered into an At Market Issuance Sales Agreement (the “ATM Agreement”) with McNicoll, Lewis & Vlak (“MLV”) pursuant to whichthe Company was able to sell $70,000 in shares of its common stock at current market prices under a Form S-3 registration statement with MLV acting as the sales agent.During 2012, the Company sold an aggregate of 4,516 shares of common stock at an average per share price of $4.08 pursuant to the ATM Agreement for net proceeds of$17,805. During 2013, the Company sold an aggregate of 2,883 shares of common stock at an average per share price of $1.85 pursuant to the Agreement for net proceeds of$5,218. Note 6 — Stock-Based Compensation Stock Incentive Plan As of December 31, 2015, the Company had two stock-based employee compensation plans, the Stock Incentive Plan (“Incentive Plan”) and the Employee StockPurchase Plan (“ESPP”), both which were amended and restated in March 2014 and approved by the Company’s stockholders in May 2014. Stock-based compensationexpense of $9,705 ($9,485 of expense related to the Incentive Plan, $220 of expense related to the ESPP) was recognized during 2015, while $10,177 ($9,963 of expenserelated to the Incentive Plan, $214 of expense related to the ESPP) was recognized during 2014, and $4,368 ($4,253 of expense related to the Incentive Plan, $115 of expenserelated to the ESPP) was recognized during 2013. The Company accounts for stock-based compensation in accordance with FASB authoritative guidance regarding share-based payments. Total stock-basedcompensation was allocated as follows: Year Ended December 31, 2015 2014 2013Research and development $7,580 $8,906 $3,664 General and administrative 2,125 1,271 704 Total stock-based compensation expense $9,705 $10,177 $4,368 69 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) The Company grants stock option awards and restricted stock unit awards to its employees, directors, and consultants under the Incentive Plan. Under the IncentivePlan, stock option awards are granted with an exercise price equal to the market price of the Company’s stock at the date of grant. Commencing March 1, 2011, stock optionawards granted to employees generally vest 25% each year until fully vested after four years. In January 2013, the Company made retention grants of stock option awards andrestricted stock units. These awards vest 50% each year until fully vested after two years. In August 2013 and December 2014, the Company issued 1,032 and 1,250performance-based stock options, respectively. These awards vest upon successful completion of specific development milestones. As of December 31, 2015, 75% of theAugust 2013 grants have vested based upon achievement of three milestones: (1) successful completion of the OPuS-1 clinical trial, for which vesting occurred in the secondquarter of 2014, (2) FDA approval of RAPIVAB for which vesting occurred in the fourth quarter of 2014, and (3) initiation of a Phase 1 clinical trial to evaluate the safety,pharmacokinetics and pharmacodynamics of orally-administered BCX7353 in healthy volunteers, for which vesting occurred in the second quarter of 2015. Thus, as ofDecember 31, 2015, 25% of the August 2013 performance-based grants and 100% of the December 2014 performance-based grants remain unvested and no compensationexpense has been recognized for these portions of the previously issued performance-based grants. Stock option awards granted to non-employee directors of the Companygenerally vest monthly over one year. All stock option awards have contractual terms of 5 to 10 years. The vesting exercise provisions of all awards granted under theIncentive Plan are subject to acceleration in the event of certain stockholder-approved transactions, or upon the occurrence of a change in control as defined in the IncentivePlan. Related activity under the Incentive Plan is as follows: Awards Available Options Outstanding Weighted Average Exercise PriceBalance at December 31, 2012 2,815 8,073 $6.09 Restricted stock awards granted (310) — — Restricted stock awards cancelled 53 — — Stock option awards granted (3,277) 3,277 3.05 Stock option awards exercised — (563) 2.37 Stock option awards cancelled 1,801 (1,801) 7.22 Balance at December 31, 2013 1,082 8,986 4.99 Plan amendment 3,750 — — Restricted stock awards granted (593) — — Restricted stock awards cancelled — — — Stock option awards granted (1,965) 1,965 10.99 Stock option awards exercised — (1,258) 4.78 Stock option awards cancelled 88 (88) 8.83 Balance at December 31, 2014 2,362 9,605 6.21 Restricted stock awards granted (163) — — Restricted stock awards cancelled 1 — — Stock option awards granted (2,217) 2,217 11.52 Stock option awards exercised — (1,118) 4.36 Stock option awards cancelled 33 (33) 9.87 Balance at December 31, 2015 16 10,671 $7.50 For stock option awards granted under the Incentive Plan during 2015, 2014 and 2013, the fair value was estimated on the date of grant using a Black-Scholes optionpricing model and the assumptions noted in the table below. The weighted average grant date fair value of these awards granted during 2015, 2014 and 2013 was $7.72, $8.02,and $1.28, respectively. The fair value of the stock option awards is amortized to expense over the vesting periods using a straight-line expense attribution method. Thefollowing explanations describe the assumptions used by the Company to value the stock option awards granted during 2015, 2014, and 2013. The expected life is based onthe average of the assumption that all outstanding stock option awards will be exercised at full vesting and the assumption that all outstanding stock option awards will beexercised at the midpoint of the current date (if already vested) or at full vesting (if not yet vested) and the full contractual term. The expected volatility represents thevolatility over the most recent period corresponding with the expected life. The Company has assumed no expected dividend yield, as dividends have never been paid tostockholders and will not be for the foreseeable future. The weighted average risk-free interest rate is the implied yield currently available on zero-coupon government issueswith a remaining term equal to the expected term. 70 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Weighted Average Assumptions for Stock Option Awards Granted under the Incentive Plan 2015 2014 2013Expected Life 5.5 5.5 4.7 Expected Volatility 81% 87% 84%Expected Dividend Yield 0.0% 0.0% 0.0%Risk-Free Interest Rate 1.6% 1.6% 0.7% The total intrinsic value of stock option awards exercised under the Incentive Plan was $10,117 during 2015, $8,522 during 2014, $738 and during 2013. The intrinsicvalue represents the total proceeds (fair market value at the date of exercise, less the exercise price, times the number of stock option awards exercised) received by allindividuals who exercised stock option awards during the period. The following table summarizes, at December 31, 2015, by price range: (1) for stock option awards outstanding under the Incentive Plan, the number of stock optionawards outstanding, their weighted average remaining life and their weighted average exercise price; and (2) for stock option awards exercisable under the Plan, the numberof stock option awards exercisable and their weighted average exercise price: Outstanding ExercisableRange Number Weighted Average Remaining Life Weighted Average Exercise Price Number Weighted Average Exercise Price$0to3 1,826 6.4 $1.51 1,322 $1.55 3to6 2,792 6.1 4.63 2,329 4.53 6to9 1,153 4.5 7.10 1,070 7.13 9to12 3,728 8.1 11.07 714 11.45 12to15 1,077 6.4 12.44 374 12.65 15to18 95 9.5 15.39 — — $0to18 10,671 6.7 $7.50 5,809 $5.70 The weighted average remaining contractual life of stock option awards exercisable under the Incentive Plan at December 31, 2015 was 5.0 years. The aggregate intrinsic value of stock option awards outstanding and exercisable under the Incentive Plan at December 31, 2015 was $28,511. The aggregate intrinsicvalue represents the value (the period’s closing market price, less the exercise price, times the number of in-the-money stock option awards) that would have been received byall stock option award holders under the Incentive Plan had they exercised their stock option awards at the end of the year. The total fair value of the stock option awards vested under the Incentive Plan was $4,492 during 2015, $2,844 during 2014, and $3,483 during 2013. As of December 31, 2015, the number of stock option awards vested and expected to vest under the Incentive Plan is 9,633. The weighted average exercise price ofthese stock option awards is $7.51 and their weighted average remaining contractual life is 6.6 years. 71 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) The following table summarizes the changes in the number and weighted-average grant-date fair value of non-vested stock option awards during 2015: Non-Vested Stock Option Awards Weighted Average Grant-Date Fair ValueBalance December 31, 2014 4,385 $4.27 Stock option awards granted 2,217 7.72 Stock option awards vested (1,711) 2.63 Stock option awards forfeited (28) 6.39 Balance December 31, 2015 4,863 $6.40 As of December 31, 2015, there was approximately $18,607 of total unrecognized compensation cost related to non-vested employee stock option awards and restrictedstock units granted by the Company. That cost is expected to be recognized as follows: $7,023 in 2016, $6,010 in 2017, $3,891 in 2018, and $1,683 in 2019. Employee Stock Purchase Plan The Company has reserved a total of 1,475 shares of common stock to be purchased under the ESPP, of which 497 shares remain available for purchase at December 31,2015. Eligible employees may authorize up to 15% of their salary to purchase common stock at the lower of 85% of the beginning or 85% of the ending price during six-month purchase intervals. No more than 3 shares may be purchased by any one employee at the six-month purchase dates and no employee may purchase stock having a fairmarket value at the commencement date of $25 or more in any one calendar year. There were 41, 49 and 89 shares of common stock purchased under the ESPP in 2015, 2014, and 2013, respectively, at a weighted average price per share of $8.65,$6.29, and $1.39, respectively. Expense of $220, $214, and $115, related to the ESPP was recognized during 2015, 2014, and 2013, respectively. Compensation expense forshares purchased under the ESPP related to the purchase discount and the “look-back” option were determined using a Black-Scholes option pricing model. The weightedaverage grant date fair values of shares granted under the ESPP during 2015, 2014, and 2013, were $4.93, $4.41, and $1.27, respectively. Note 7 — Income Taxes The Company has incurred net losses since inception and, consequently, has not recorded any U.S. Federal and state income tax expense or benefit. The differencesbetween the Company’s effective tax rate and the statutory tax rate in 2015, 2014, and 2013 are as follows: 2015 2014 2013Income tax benefit at federal statutory rate (35%) $(15,057) $(15,816) $(10,538)State and local income taxes net of federal tax benefit (819) (1,286) (839)Permanent items 560 258 738 Rate change 1,012 22 1,892 Expiration of attribute carryforwards 330 373 242 Research and development tax credits (10,454) (748) (1,206)Orphan drug credit 4,307 — — Other (218) (115) 1,144 Change in valuation allowance 20,339 17,312 8,567 Income tax expense $— $— $— The Company recognizes the impact of a tax position in its financial statements if it is more likely than not that the position will be sustained on audit based on thetechnical merits of the position. The Company has concluded that it has an uncertain tax position pertaining to its research and development and orphan drug creditcarryforwards. The Company has established these credits based on information and calculations it believes are appropriate and the best estimate of the underlying credit. Anychanges to the Company’s unrecognized tax benefits are offset by an adjustment to the valuation allowance and there would be no impact on the Company’s financialstatements. The Company does not expect its unrecognized tax benefits to change significantly over the next 12 months. 72 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) A reconciliation of the beginning and ending amount of unrecognized tax benefits is as follows: 2015 2014Balance at January 1, $472 $284 Additions to current period tax positions 2,616 176 Additions to prior period tax positions — 12 Reductions to prior period tax provisions (3) — Balance at December 31, $3,085 $472 The Company’s ability to utilize the net operating loss and tax credit carryforwards in the future may be subject to substantial restrictions in the event of past or futureownership changes as defined in Section 382 of the Internal Revenue Code of 1986, as amended and similar state tax law. Significant components of the Company’s deferred tax assets and liabilities are as follows: 2015 2014Deferred tax assets: Net federal and state operating losses $142,836 $135,922 Research and development credits 48,551 38,096 Fixed assets 1,054 1,073 Deferred revenue 4,240 3,798 Stock-based compensation 8,605 7,086 Other 2,590 1,178 Total deferred tax assets 207,876 187,153 Deferred tax liabilities: Foreign currency derivative (2,668) (2,285)Total deferred tax liabilities (2,668) (2,285) Valuation allowance (205,208) (184,868)Net deferred tax assets $— $— The majority of the Company’s deferred tax assets relate to net operating loss and research and development carryforwards that can only be realized if the Company isprofitable in future periods. It is uncertain whether the Company will realize any tax benefit related to these carryforwards. Accordingly, the Company has provided a fullvaluation allowance against the net deferred tax assets due to uncertainties as to their ultimate realization. The valuation allowance will remain at the full amount of thedeferred tax assets until it is more likely than not that the related tax benefits will be realized. The Company’s valuation allowance increased by $20,339 in 2015, $17,312 in2014, and $8,567 in 2013. As of December 31, 2015, the Company had federal operating loss carryforwards of $386,219, state operating loss carryforwards of $373,454, and research anddevelopment and orphan drug credit carryforwards of $48,551, which will expire at various dates from 2016 through 2035. The federal losses begin to expire in 2018, the statelosses begin to expire in 2016 and the research and development contracts begin to expire in 2018. The Company’s federal and state operating loss carryforwards include $15,655 of excess tax benefits related to a deduction from the exercise of stock options. The taxbenefit of these deductions has not been recognized in deferred tax assets. If utilized, the benefits from these deductions will be recorded as adjustments to additional paid-incapital. Tax years 2012-2014 remain open to examination by the major taxing jurisdictions to which the Company is subject. Additionally, years prior to 2012 are also open toexamination to the extent of loss and credit carryforwards from those years. The Company recognizes interest and penalties accrued related to unrecognized tax benefits ascomponents of its income tax provision. However, there were no provisions or accruals for interest and penalties in 2015, 2014, and 2013. 73 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) Note 8 — Employee 401(k) Plan In January 1991, the Company adopted an employee retirement plan (“401(k) Plan”) under Section 401(k) of the Internal Revenue Code covering all employees.Employee contributions may be made to the 401(k) Plan up to limits established by the Internal Revenue Service. Company matching contributions may be made at thediscretion of the Board of Directors. The Company made matching contributions of $366, $361, and $313, in 2015, 2014, and 2013, respectively. Note 9 — Collaborative and Other Research and Development Contracts U.S. Department of Health and Human Services (“BARDA/HHS”). In January 2007, the U.S. Department of Health and Human Services (“BARDA/HHS”) awarded theCompany a $102,661, four-year contract for the advanced development of peramivir for the treatment of influenza. During 2009, peramivir clinical development shifted tofocus on intravenous delivery and the treatment of hospitalized patients. To support this focus, a September 2009 contract modification was awarded to extend the i.v.peramivir program and to increase funding by $77,191. On February 24, 2011, the Company announced that BARDA/HHS had awarded it a $55,000 contract modification,intended to fund completion of the Phase 3 development of i.v. peramivir for the treatment of patients hospitalized with influenza. That contract modification brought the totalcontract award from BARDA/HHS to $234,852 and provided funding to support the filing of a NDA to seek regulatory approval for i.v. peramivir in the U.S. In December2013, BioCryst submitted an NDA filing for i.v. peramivir to the FDA and the NDA was approved in December 2014. The BARDA/HHS contract expired on June 30, 2014. On March 31, 2015, the Company announced that the Biomedical Research and Development Authority within the U.S. Department of Health and Human Services’Office of the Assistant Secretary for Preparedness and Response awarded BioCryst a contract for the continued development of BCX4430 as a potential treatment for diseasescaused by RNA pathogens, including filoviruses. This BARDA/HHS contract includes a base contract of $13,314 to support BCX4430 drug manufacturing, as well as$22,855 in additional development options that can be exercised by the government, bringing the potential value of the contract to $36,169. As of September 30, 2015, a totalof $16,300 has been awarded under exercised options within this contract. National Institute of Allergy and Infectious Diseases (“NIAID/HHS”). In September 2013, NIAID/HHS contracted with the Company for the development of BCX4430as a treatment for Marburg virus disease. NIAID/HHS, part of the National Institutes of Health, made an initial award of $5,000 to the Company. The total funding under thiscontract as of December 31, 2015 could be up to $34,002, if all contract options are exercised by NIAID/HHS, over a five year period. The goals of this contract, includingamendments, are to file IND applications for intravenous and intramuscular BCX4430 for the treatment of Marburg virus disease, to study BCX4430 as a treatment for Ebolavirus disease and to conduct an initial Phase 1 human clinical trial. As of December 31, 2015, a total of $29,875 has been awarded under exercised options within thiscontract. BCX4430 is the lead compound in the Company’s BSAV research program. The contracts with BARDA/HHS and NIAID/HHS are cost-plus-fixed-fee contracts. That is, the Company is entitled to receive reimbursement for all costs incurred inaccordance with the contracts provisions that are related to the development of peramivir and BCX4430 plus a fixed fee, or profit. BARDA/HHS and NIAID/HHS will makeperiodic assessments of progress and the continuation of the contract is based on the Company’s performance, the timeliness and quality of deliverables, and other factors.The government has rights under certain contract clauses to terminate these contracts. These contracts are terminable by the government at any time for breach or withoutcause. Seqirus UK Limited (“SUL”). On June 16, 2015, the Company and Seqirus UK Limited ("SUL"), a limited company organized under the laws of the United Kingdomand a subsidiary of CSL Limited, a company organized under the laws of Australia, entered into a License Agreement (the "SUL Agreement") granting SUL and its affiliatesworldwide rights to develop, manufacture and commercialize RAPIVAB (peramivir injection) for the treatment of influenza except for the rights to conduct such activities inIsrael, Japan, Korea and Taiwan (the permitted geographies together constituting the "Territory"). RAPIVAB is an intravenous treatment for acute uncomplicated influenzaand is currently licensed for use in the United States, Japan and Korea. RAPIVAB is the first and only intravenous influenza treatment in the world and was approved by theU.S. Food and Drug Administration in December 2014 for the treatment of acute uncomplicated influenza in patients 18 years and older who have been symptomatic for nomore than two days. The Company retains all rights and associated economics to procure pandemic stockpiling orders for RAPIVAB from the U.S. Government, while SULhas the right to pursue government stockpiling outside the U.S. Pursuant to the SUL Agreement, RAPIVAB will be commercialized by CSL's subsidiary, SUL, which specializes in influenza prevention through the supply ofseasonal and pandemic vaccine to global markets. SUL will manufacture, commercialize and exercise decision-making authority with respect to the development andcommercialization of RAPIVAB within the Territory and be responsible for all related costs, including sales and promotion. 74 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) In December 2013, the Company submitted a New Drug Application ("NDA") for RAPIVAB to the FDA. Under the terms of the SUL Agreement, the Company isresponsible for fulfilling all post-marketing approval commitments in connection with the FDA's approval of the NDA, and upon fulfillment will transfer ownership of andfinancial responsibility for the NDA to SUL. Pursuant to potential rights to sell RAPIVAB in Canada and the EU, the Company is also responsible for regulatory filings andinteractions with the Health Canada and the European Medicines Agency ("EMA") until marketing approval for RAPIVAB is obtained and assigned to SUL. In accordancewith the SUL Agreement, the Company and SUL formed a joint steering committee, composed of an equal number of representatives from each party, to oversee, review andcoordinate the conduct and progress of the commercialization of RAPIVAB in the Territory and any additional development. Under the terms of the SUL Agreement, the Company received an upfront payment of $33,740, and may receive up to $12,000 in additional milestone payments relatedto the successful achievement of regulatory milestones, including marketing approval (i) by the FDA for a pediatric indication, (ii) by the EMA for an adult indication in theEU and (iii) by Health Canada for an adult indication in Canada. The Company is also entitled under the SUL Agreement to receive tiered royalties at a percentage ratebeginning in the mid-teens contingent upon meeting minimum thresholds of net sales, as well as a low-thirties percentage of the gross profit from government stockpilingpurchases made outside the U.S. Specifically, the Company receives tiered royalties at a percentage rate in the mid-teens to low-forties on net sales in the U.S. during aContract Year (defined as July 1 - June 30) and tiered royalties at a percentage rate in the mid-teens to mid-twenties on net sales in the Territory, other than in the U.S., duringa Calendar Year, each subject to certain downward adjustments for circumstance or events impacting the overall market opportunity. SUL's royalty payment obligationscommence on the date of the SUL Agreement and expire, on a country-by-country basis, upon the later of (i) the expiration of legal exclusivity in such country and (ii) tenyears from the date of the SUL Agreement (the "Royalty Term"). The Company developed RAPIVAB under a license from UAB and will owe sublicense payments to themon any future milestone payments and/or royalties received by the Company from SUL. Shionogi & Co., Ltd. (“Shionogi”). In February 2007, the Company entered into an exclusive license agreement with Shionogi to develop and commercialize peramivirin Japan for the treatment of seasonal and potentially life-threatening human influenza. Under the terms of the agreement, Shionogi obtained rights to injectable formulationsof peramivir in Japan. The Company developed peramivir under a license from UAB and will owe sublicense payments to them on any future milestone payments and/orroyalties received by the Company from Shionogi. In October 2008, the Company and Shionogi amended the license agreement to expand the territory covered by theagreement to include Taiwan. Shionogi has commercially launched peramivir under the commercial name RAPIACTA in Japan. Shionogi submitted an NDA to the TaiwanFDA in late 2013. Green Cross Corporation (“Green Cross”). In June 2006, the Company entered into an agreement with Green Cross to develop and commercialize peramivir in Korea.Under the terms of the agreement, Green Cross will be responsible for all development, regulatory, and commercialization costs in Korea. The Company received a one-timelicense fee of $250. The license also provides that the Company will share in profits resulting from the sale of peramivir in Korea, including the sale of peramivir to theKorean government for stockpiling purposes. Furthermore, Green Cross will pay the Company a premium over its cost to supply peramivir for development and any futuremarketing of peramivir products in Korea. Mundipharma International Holdings Limited (“Mundipharma”). In February 2006, the Company entered into an exclusive, royalty bearing right and license agreementwith Mundipharma for the development and commercialization of forodesine, a Purine Nucleoside Phosphorylase (“PNP”) inhibitor, for use in oncology (the “OriginalAgreement”). Under the terms of the Original Agreement, Mundipharma obtained rights to forodesine in markets across Europe, Asia, and Australasia in exchange for a$10,000 up-front payment. 75 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) The Company deferred revenue recognition of the $10,000 up-front payment that was received from Mundipharma in February 2006 because the Company wasinvolved in the continued development of forodesine. Amortization of this revenue commenced in February 2006 and was initially scheduled to end in October 2017, which isthe date of expiration for the last-to-expire patent covered by the agreement. The Company also deferred revenue recognition of a $5,000 payment received fromMundipharma in connection with the initiation of a clinical trial in 2007. Amortization of this deferred revenue commenced in 2007 and was initially scheduled to end inOctober 2017. Under its agreement with AECOM/IRL, the Company paid sublicense payments related to these upfront cash payments received from Mundipharma. Expenserecognition of these sublicense payments was deferred and recognized under the same term as the related deferred revenue. On November 11, 2011, the Company entered into the Amended and Restated License and Development Agreement (the “Amended and Restated Agreement”) withMundipharma, amending and restating the Original Agreement. Under the terms of the Amended and Restated Agreement, Mundipharma obtained worldwide rights toforodesine. Commencing on November 11, 2011, Mundipharma controls the development and commercialization of forodesine and assumes all future development andcommercialization costs. The Amended and Restated Agreement provides for the possibility of future event payments totaling $15,000 for achieving specified regulatoryevents for certain indications and tiered royalties ranging from mid to high single-digit percentages of net product sales in each country where forodesine is sold byMundipharma. These royalties are subject to downward adjustments based on the then-existing patent coverage and/or the availability of generic compounds in each country. The Amended and Restated Agreement is a multiple element arrangement for accounting purposes, in which the Company is required to deliver to Mundipharma boththe worldwide rights to forodesine in the field of oncology and the transfer of product data and know-how to permit Mundipharma to develop and commercialize forodesine(the “Knowledge Transfer”). The Company accounted for these elements as a combined unit of accounting as they do not have stand-alone value to Mundipharma. Theworldwide license rights were granted to Mundipharma on November 11, 2011 and the Knowledge Transfer was completed during the first quarter of 2012. Albert Einstein College of Medicine of Yeshiva University and Industrial Research, Ltd. (“AECOM” and “IRL” respectively). In June 2000, the Company licensed aseries of potent inhibitors of PNP from AECOM and IRL, (collectively, the “Licensors”). The lead product candidates from this collaboration are forodesine and ulodesine.The Company has obtained worldwide exclusive rights to develop and ultimately distribute these, or any other, product candidates that might arise from research on theseinhibitors. The Company has the option to expand the Agreement to include other inventions in the field made by the investigators or employees of the Licensors. TheCompany agreed to use commercially reasonable efforts to develop these drugs. In addition, the Company has agreed to pay certain milestone payments for each licensedproduct (which range in the aggregate from $1,400 to almost $4,000 per indication) for future development of these inhibitors, single digit royalties on net sales of anyresulting product made by the Company, and to share approximately one quarter of future payments received from other third-party partners, if any. In addition, the Companyhas agreed to pay annual license fees, which can range from $150 to $500, that are creditable against actual royalties and other payments due to the Licensors. This agreementmay be terminated by the Company at any time by giving 60 days advance notice or in the event of material uncured breach by the Licensors. In May 2010, the Company amended the licensee agreement through which the Company obtained worldwide exclusive rights to develop and ultimately distribute anyproduct candidates that might arise from research on a series of PNP inhibitors, including forodesine and ulodesine. Under the terms of the amendment, the Licensors agreedto accept a reduction of one-half in the percentage of future payments received from third-party sub licensees of the licensed PNP inhibitors that must be paid to the Licensors.This reduction does not apply to (i) any milestone payments the Company may receive in the future under its license agreement dated February 1, 2006 with Mundipharmaand (ii) royalties received from its sub licensees in connection with the sale of licensed products, for which the original payment rate will remain in effect. The rate of royaltypayments to the Licensors based on net sales of any resulting product made by the Company remains unchanged. In consideration for these modifications in 2010, the Company issued to the Licensors shares of its common stock with an aggregate value of $5,911 and paid theLicensors $90 in cash. Additionally, at the Company’s sole option and subject to certain agreed upon conditions, any future non-royalty payments due to be paid by it to theLicensors under the license agreement may be made either in cash, in shares of its common stock, or in a combination of cash and shares. On November 17, 2011, the Company further amended its agreements with the Licensors whereby the Licensors agreed to accept a reduction of one-half in thepercentage of Net Proceeds (as defined) received by the Company under its Amended and Restated Agreement with Mundipharma that will be paid to AECOM/IRL. On June 19, 2012, the Company further amended its agreements with AECOM/IRL whereby the parties clarified the definition of the field with respect to PNPinhibition and AECOM/IRL agreed to exclusive worldwide license of BCX4430 to BioCryst for any antiviral use. 76 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) At its sole option and subject to certain agreed upon conditions, any future non-royalty payments due to be paid by the Company to AECOM/IRL under the licenseagreement may be made either in cash, in shares of the Company’s common stock, or in a combination of cash and shares. On January 6, 2014, the Carbohydrate Chemistry Research Team from Callaghan Innovation Research Limited, formerly Industrial Research Limited, transferred toVictoria University of Wellington (“VUW”) to establish the Ferrier Research Institute. The intellectual property rights relating to this research team, and the contracts relatingto that intellectual property were transferred to a wholly owned subsidiary of VUW, including the contracts to which BioCryst is a party. The parties executed novationagreements in order to effectuate the transfer. Except for a substitution of parties, the terms and conditions of the contracts are substantially the same The University of Alabama at Birmingham (“UAB”). The Company currently has agreements with UAB for influenza neuraminidase and complement inhibitors. Underthe terms of these agreements, UAB performed specific research for the Company in return for research payments and license fees. UAB has granted the Company certainrights to any discoveries in these areas resulting from research developed by UAB or jointly developed with the Company. The Company has agreed to pay single digitroyalties on sales of any resulting product and to share in future payments received from other third-party partners. The Company has completed the research under the UABagreements. These two agreements have initial 25-year terms, are automatically renewable for five-year terms throughout the life of the last patent and are terminable by theCompany upon three months’ notice and by UAB under certain circumstances. Upon termination both parties shall cease using the other parties’ proprietary and confidentialinformation and materials, the parties shall jointly own joint inventions and UAB shall resume full ownership of all UAB licensed products. There is currently no activitybetween the Company and UAB on these agreements, but when the Company licenses this technology, such as in the case of the Shionogi, Green Cross and SUL agreements,or commercializes products related to these programs, the Company will owe sublicense fees or royalties on amounts it receives. Note 10 — Quarterly Financial Information (Unaudited) First Second Third Fourth2015 Quarters Revenues $6,826 $25,842 $10,987 $4,602 Net (Loss) Income (15,164) 4,901 (14,621) (18,135)Basic net (loss) income per share (0.21) 0.07 (0.20) (0.25)Diluted net (loss) income per share (0.21) 0.06 (0.20) (0.25)2014 Quarters Revenues $3,458 $1,466 $3,238 $5,446 Net Loss (10,137) (14,649) (8,731) (11,672)Basic and diluted net loss per share (0.17) (0.23) (0.12) (0.16) Note 11 — Recent Accounting Pronouncements In November 2015, the Financial Accounting Standards Board (“FASB”) issued Accounting Standards Update (“ASU”) No. 2015-17, Balance Sheet Classification ofDeferred Taxes , requiring all deferred tax assets and liabilities, and any related valuation allowance, to be classified as noncurrent on the balance sheet. The classificationchange for all deferred taxes as noncurrent simplifies entities’ processes as it eliminates the need to separately identify the net current and net noncurrent deferred tax asset orliability in each jurisdiction and allocate valuation allowances. We elected to prospectively adopt the accounting standard in the beginning of our fourth quarter of fiscal 2015.Adoption of this standard had no impact on the Company’s consolidated financial statements. In April 2015, the FASB issued ASU No.2015-03, Simplifying the Presentation of Debt Issuance Costs . This standard amends existing guidance to require thepresentation of debt issuance costs in the balance sheet as a deduction from the carrying amount of the related debt liability instead of a deferred charge. It is effective forannual reporting periods beginning after December 15, 2015. Early adoption is permitted. The Company does not expect this standard will have a material impact on itsconsolidated financial statements. 77 BIOCRYST PHARMACEUTICALS, INC. NOTES TO CONSOLIDATED FINANCIAL STATEMENTS(In thousands, except per share amounts) In August 2014, the FASB issued ASU No. 2014-15 – Presentation of Financial Statements - Going Concern (Subtopic 205-40): Disclosure of Uncertainties about anEntity’s Ability to Continue as a Going Concern, which defines management’s responsibility to evaluate, at each annual and interim reporting period, whether there areconditions or events that raise substantial doubt about an entity’s ability to continue as a going concern within one year after the date the financial statements are issued and toprovide related footnote disclosures in certain circumstances. In connection with each annual and interim period, management must assess if there is substantial doubt aboutthe company’s ability to continue as a going concern within one year after the issuance date. Disclosures are required if conditions give rise to substantial doubt. Thisstandard is effective for all companies in the first annual period ending after December 15, 2016, and interim periods thereafter, with early adoption permitted. The Companyis currently evaluating the impact this standard will have on its financial statements and disclosures. In May 2014, the FASB issued ASU 2014-09 – Revenue from Contracts with Customers , which provides a single, comprehensive revenue recognition model for allcontracts with customers. The core principal of this ASU is that an entity should recognize revenue when it transfers promised goods or services to customers in an amountthat reflects the consideration to which the entity expects to be entitled in exchange for those goods or services. This ASU also requires additional disclosure about the nature,amount, timing and uncertainty of revenue and cash flows arising from customer contracts, including significant judgments and changes in judgments and assets recognizedfrom costs incurred to obtain or fulfill a contract. In July 2015, the FASB finalized a one year delay in the effective date of this standard, which will now be effective January1, 2018; however, early adoption is permitted any time after the original effective date, January 1, 2017. Companies can transition to the new standard under the fullretrospective method or the modified retrospective method. The Company is currently evaluating the impact this standard will have on its consolidated financial statements. 78 Report of Independent Registered Public Accounting Firm The Board of Directors and StockholdersBioCryst Pharmaceuticals, Inc. We have audited the consolidated balance sheets of BioCryst Pharmaceuticals, Inc. as of December 31, 2015 and 2014, and the related consolidated statements ofcomprehensive loss, stockholders’ equity and cash flows for each of the three years in the period ended December 31, 2015. These financial statements are the responsibilityof the Company’s management. Our responsibility is to express an opinion on these financial statements based on our audits. We conducted our audits in accordance with the standards of the Public Company Accounting Oversight Board (United States). Those standards require that we planand perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. An audit includes examining, on a test basis,evidence supporting the amounts and disclosures in the financial statements. An audit also includes assessing the accounting principles used and significant estimates made bymanagement, as well as evaluating the overall financial statement presentation. We believe that our audits provide a reasonable basis for our opinion. In our opinion, the financial statements referred to above present fairly, in all material respects, the consolidated financial position of BioCryst Pharmaceuticals, Inc. atDecember 31, 2015 and 2014, and the consolidated results of its operations and its cash flows for each of the three years in the period ended December 31, 2015, inconformity with U.S. generally accepted accounting principles. We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), BioCryst Pharmaceuticals, Inc.’s internalcontrol over financial reporting as of December 31, 2015, based on criteria established in Internal Control-Integrated Framework issued by the Committee of SponsoringOrganizations of the Treadway Commission (2013 Framework) and our report dated February 26, 2016 expressed an unqualified opinion thereon. /s/ Ernst & Young LLP Raleigh, North Carolina February 26, 2016 79 Report of Independent Registered Public Accounting Firm The Board of Directors and StockholdersBioCryst Pharmaceuticals, Inc. We have audited BioCryst Pharmaceuticals, Inc.’s internal control over financial reporting as of December 31, 2015, based on criteria established in Internal Control-Integrated Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission (2013 Framework) (the COSO criteria). BioCrystPharmaceuticals, Inc.’s management is responsible for maintaining effective internal control over financial reporting, and for its assessment of the effectiveness of internalcontrol over financial reporting included in the accompanying Management’s Report on Internal Control Over Financial Reporting. Our responsibility is to express an opinionon 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 plan andperform the audit to obtain reasonable assurance about whether effective internal control over financial reporting was maintained in all material respects. Our audit includedobtaining an understanding of internal control over financial reporting, assessing the risk that a material weakness exists, testing and evaluating the design and operatingeffectiveness of internal control based on the assessed risk, and performing such other procedures as we considered necessary in the circumstances. We believe that our auditprovides 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 financial reportingincludes those policies and procedures that (1) pertain to the maintenance of records that, in reasonable detail, accurately and fairly reflect the transactions and dispositions ofthe assets of the company; (2) provide reasonable assurance that transactions are recorded as necessary to permit preparation of financial statements in accordance withgenerally accepted accounting principles, and that receipts and expenditures of the company are being made only in accordance with authorizations of management anddirectors of the company; and (3) provide reasonable assurance regarding prevention or timely detection of unauthorized acquisition, use, or disposition of the company’sassets that could have a material effect on the financial statements. Because of its inherent limitations, internal control over financial reporting may not prevent or detect misstatements. Also, projections of any evaluation of effectivenessto future periods are subject to the risk that controls may become inadequate because of changes in conditions, or that the degree of compliance with the policies or proceduresmay deteriorate. In our opinion, BioCryst Pharmaceuticals, Inc. maintained, in all material respects, effective internal control over financial reporting as of December 31, 2015, based onthe COSO criteria. We also have audited, in accordance with the standards of the Public Company Accounting Oversight Board (United States), the consolidated balance sheets of BioCrystPharmaceuticals, Inc. as of December 31, 2015 and 2014, and the related consolidated statements of comprehensive loss, stockholders’ equity, and cash flows for each of thethree years in the period ended December 31, 2015 of BioCryst Pharmaceuticals, Inc. and our report dated February 26, 2016 expressed an unqualified opinion thereon. /s/ Ernst & Young LLP Raleigh, North Carolina February 26, 2016 80 ITEM 9.CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE None.ITEM 9A.CONTROLS AND PROCEDURES Evaluation of Disclosure Controls and Procedures We maintain a set of disclosure controls and procedures that are designed to ensure that information relating to BioCryst Pharmaceuticals, Inc. required to be disclosedin our periodic filings under the Securities Exchange Act of 1934, as amended (the “Exchange Act”), is recorded, processed, summarized and reported in a timely mannerunder the Exchange Act of 1934. We carried out an evaluation as required by paragraph (b) of Rule 13a-15 or Rule 15d-15 under the Exchange Act, under the supervision andwith the participation of management, including our Chief Executive Officer and Chief Financial Officer, of the effectiveness of the design and operation of our disclosurecontrols and procedures (as defined in Rule 13a-15(e) or Rule 15d-15 under the Exchange Act). Based upon that evaluation, the Chief Executive Officer and Chief FinancialOfficer concluded that, as of December 31, 2014, our disclosure controls and procedures are effective. We believe that our disclosure controls and procedures will ensure thatinformation required to be disclosed in the reports filed or submitted by us under the Exchange Act is recorded, processed, summarized and reported within the time periodsspecified in the rules and forms of the Securities and Exchange Commission, and include controls and procedures designed to ensure that information required to be disclosedby us in such reports is accumulated and communicated to our management, including our Chairman and Chief Executive Officer and Chief Financial Officer, as appropriateto allow timely decisions regarding required disclosure. Management’s Report on Internal Control Over Financial Reporting Management of BioCryst Pharmaceuticals, Inc. is responsible for establishing and maintaining adequate internal control over financial reporting and for the assessmentof the effectiveness of internal control over financial reporting. As defined by the Securities and Exchange Commission, internal control over financial reporting is a processdesigned by, or under the supervision of our principal executive and principal financial officers and effected by our Board of Directors, management and other personnel, toprovide reasonable assurance regarding the reliability of financial reporting and the preparation of the financial statements in accordance with U.S. GAAP. Our internal control over financial reporting is supported by written policies and procedures that (1) pertain to the maintenance of records that, in reasonable detail,accurately and fairly reflect our transactions and dispositions of our assets; (2) provide reasonable assurance that transactions are recorded as necessary to permit preparationof the financial statements in accordance with U.S. GAAP, and that our receipts and expenditures are being made only in accordance with authorizations of our managementand directors; and (3) provide reasonable assurance regarding prevention or timely detection of unauthorized acquisition, use or disposition of our 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. Also, projections of any evaluation of effectivenessto future periods are subject to the risk that controls may become inadequate because of changes in conditions, or that the degree of compliance with the policies or proceduresmay deteriorate. In connection with the preparation of our annual financial statements, management has undertaken an assessment of the effectiveness of our internal control overfinancial reporting as of December 31, 2015, based on criteria established in Internal Control — Integrated Framework issued by the Committee of Sponsoring Organizationsof the Treadway Commission (2013 Framework) (the COSO Framework). Management’s assessment included an evaluation of the design of our internal control overfinancial reporting and testing of the operational effectiveness of those controls. Based on this assessment, management has concluded that as of December 31, 2015, our internal control over financial reporting was effective. Management believesour internal control over financial reporting will provide reasonable assurance regarding the reliability of financial reporting and the preparation of financial statements forexternal purposes in accordance with U.S. GAAP. Ernst & Young LLP, the independent registered public accounting firm that audited our financial statements included in this report, has issued an attestation report onthe Company’s internal control over financial reporting, a copy of which appears on page 80 of this annual report. Changes in Internal Control over Financial Reporting There have been no changes in our internal control over financial reporting that occurred during the quarter ended December 31, 2015 that have materially affected, orare reasonably likely to materially affect, our internal control over financial reporting. ITEM 9B.OTHER INFORMATION None. 81 PART III ITEM 10.DIRECTORS, EXECUTIVE OFFICERS AND CORPORATE GOVERNANCE The information required by this item is set forth under the captions “Items to be Voted on — 1. Election of Directors,” “Executive Officers,” “Section 16(a) BeneficialOwnership Reporting Compliance” and “Corporate Governance” in our definitive Proxy Statement for the 2016 Annual Meeting of Stockholders and incorporated herein byreference. ITEM 11.EXECUTIVE COMPENSATION The information required by this item is set forth under the captions “Compensation Discussion and Analysis,” “Summary Compensation Table,” “Grants of Plan-Based Awards in 2015,” “Outstanding Equity Awards at December 31, 2015,” “2015 Option Exercises and Stock Vested,” “Potential Payments Upon Termination orChange in Control,” “2015 Director Compensation,” “Compensation Committee Interlocks and Insider Participation” and “Compensation Committee Report” in ourdefinitive Proxy Statement for the 2016 Annual Meeting of Stockholders and incorporated herein by reference. ITEM 12.SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT AND RELATED STOCKHOLDER MATTERS The information required by this item is set forth under the captions “Equity Compensation Plan Information” and “ Security Ownership of Certain Beneficial Ownersand Management” in our definitive Proxy Statement for the 2016 Annual Meeting of Stockholders and incorporated herein by reference. ITEM 13.CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS, AND DIRECTOR INDEPENDENCE The information required by this item is set forth under the captions “Certain Relationships and Related Transactions” and “ Corporate Governance” in our definitiveProxy Statement for the 2016 Annual Meeting of Stockholders and incorporated herein by reference. ITEM 14.PRINCIPAL ACCOUNTING FEES AND SERVICES The information required by this item is set forth under the caption “2. Ratification of Appointment of Independent Registered Public Accountants” in our definitiveProxy Statement for the 2016 Annual Meeting of Stockholders and incorporated herein by reference. 82 PART IV ITEM 15.EXHIBITS, FINANCIAL STATEMENT SCHEDULES (a) Financial Statements The following financial statements appear in Item 8 of this Form 10-K: Page in Form 10-KConsolidated Balance Sheets at December 31, 2015 and 2014 54 Consolidated Statements of Comprehensive Loss for the years ended December 31, 2015, 2014 and 2013 55 Consolidated Statements of Cash Flows for the years ended December 31, 2015, 2014 and 2013 56 Consolidated Statements of Stockholders’ Equity for the years ended December 31, 2015, 2014 and 2013 57 Notes to Consolidated Financial Statements 58 Report of Independent Registered Public Accounting Firm on Consolidated Financial Statements 79 Report of Independent Registered Public Accounting Firm on Internal Control 80 No financial statement schedules are included because the information is either provided in the consolidated financial statements or is not required under the relatedinstructions or is inapplicable and such schedules therefore have been omitted. (b) Exhibits. See Index of Exhibits. 83 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 its behalf by theundersigned, thereunto duly authorized on February 26, 2016. BIOCRYST PHARMACEUTICALS, INC. By:/s/ Jon P. Stonehouse Jon P. Stonehouse Chief Executive Officer Pursuant to the requirements of the Securities Exchange Act of 1934, this report has been signed below by the following persons on behalf of the registrant and in thecapacities indicated on February 26, 2016: Signature Title(s) /s/ Jon P. Stonehouse President, Chief Executive Officer and Director(Jon P. Stonehouse) (Principal Executive Officer) /s/ Thomas R. Staab II Senior Vice President, Chief Financial Officer and Treasurer(Thomas R. Staab II) (Principal Financial Officer and Principal Accounting Officer) /s/ George B. Abercrombie Director(George B. Abercrombie) /s/ Fred E. Cohen Director(Fred E. Cohen, M.D., D. Phil) /s/ Stanley C. Erck Director(Stanley C. Erck) /s/ Nancy Hutson Director(Nancy Hutson, Ph.D.) /s/ Robert A. Ingram Director(Robert A. Ingram) /s/ Kenneth B. Lee, Jr. Director(Kenneth B. Lee, Jr.) /s/ Sanj K. Patel Director(Sanj K. Patel) /s/ Charles A. Sanders Director(Charles A. Sanders, M.D.) 84 INDEX TO EXHIBITS Number Description 3.1 Third Restated Certificate of Incorporation of Registrant. Incorporated by reference to Exhibit 3.1 to the Company’s Form 8-K filed December 22, 2006. 3.2 Certificate of Amendment to the Third Restated Certificate of Incorporation of Registrant. Incorporated by reference to Exhibit 3.1 to the Company’s Form8-K filed July 24, 2007. 3.3 Certificate of Amendment to the Third Restated Certificate of Incorporation of Registrant. Incorporated by reference to Exhibit 3.1 to the Company’s Form8-K filed May 8, 2014. 3.4 Certificate of Increase of Authorized Number of Shares of Series B Junior Participating Preferred Stock. Incorporated by reference to Exhibit 3.1 to theCompany’s Form 8-K filed November 4, 2008. 3.5 Certificate of Increase of Authorized Number of Shares of Series B Junior Participating Preferred Stock. Incorporated by reference to Exhibit 3.2 to theCompany’s Form 8-K filed May 8, 2014. 3.6 Amended and Restated Bylaws of Registrant effective October 29, 2008. Incorporated by reference to Exhibit 3.2 to the Company’s Form 8-K filedNovember 4, 2008. 4.1 Indenture, dated as of March 9, 2011 by and between JPR Royalty Sub LLC and U.S. Bank National Association, as trustee. Incorporated by reference toExhibit 4.3 of the Company’s Form 10-Q filed May 6, 2011. 10.1& Amended and Restated Stock Incentive Plan dated March 29, 2012. Incorporated by reference to Exhibit 10.1 of the Company’s Form 8-K, filed May 25,2012. 10.2& Amended and Restated Stock Incentive Plan dated March 8, 2014. Incorporated by reference to Exhibit 10.1 to the Company’s Form 8-K filed May 5, 2014. 10.3& Amended and Restated Employee Stock Purchase Plan dated March 29, 2012. Incorporated by reference to the Company’s Form 8-K, filed May 25, 2012. 10.4& Amended and Restated Employee Stock Purchase Plan dated March 8, 2014. Incorporated by reference to Exhibit 10.2 to the Company’s Form 8-K filedMay 5, 2014. 10.5 Form of Notice of Grant of Non-Employee Director Automatic Stock Option and Stock Option Agreement. Incorporated by reference to Exhibit 10.4 of theCompany’s Form 10-K filed March 4, 2008. 10.6& Form of Notice of Grant of Stock Option and Stock Option Agreement. Incorporated by reference to Exhibit 10.5 of the Company’s Form 10-K filed March4, 2008. 10.7& Form of Notice of Grant of Stock Option and Stock Option Agreement. Incorporated by reference to Exhibit 10.7 of the Company’s Form 10-K filed March2, 2015. 10.8& Form of Notice of Grant of Restricted Stock Unit Award and Restricted Stock Unit Agreement. Incorporated by reference to Exhibit 10.8 of the Company’sForm 10-K filed March 2, 2015. 10.9& Annual Incentive Plan. Incorporated by reference to Exhibit 10.1 of the Company’s Form 8-K filed March 12, 2012. 10.10& Executive Relocation Policy. Incorporated by reference to Exhibit 10.2 of the Company’s Form 10-K filed March 4, 2008. 10.11& Amended and Restated Employment Letter Agreement dated February 14, 2007, by and between the Company and Jon P. Stonehouse. Incorporated byreference to Exhibit 10.12 to the Company’s Form 10-K for the year ended December 31, 2006, filed March 14, 2007. 10.12& Employment Letter Agreement between BioCryst Pharmaceuticals, Inc. and Thomas R. Staab II, dated May 23, 2011. Incorporated by reference to Exhibit10.1 of the Company’s Form 8-K filed May 25, 2011. 85 10.13& Employment Letter Agreement between BioCryst Pharmaceuticals, Inc. and William P. Sheridan dated June 12, 2008. Incorporated by reference to Exhibit10.27 of the Company’s Form 10-Q filed August 8, 2008. 10.14& Employment Letter Agreement between BioCryst Pharmaceuticals, Inc. and Yarlagadda S. Babu dated April 27, 2012. 10.15& Employment Letter Agreement between BioCryst Pharmaceuticals, Inc. and Alane P. Barnes dated August 8, 2013. 10.16& Employment Letter Agreement between BioCryst Pharmaceuticals, Inc. and Lynne Powell dated December 30, 2015. Incorporated by reference to Exhibit10.16 of the Company’s Form 10-K filed March 2, 2015. 10.17# Agreement dated January 3, 2007, between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services, as amended by Amendmentnumber 1 dated January 3, 2007 and Amendment number 2 dated May 11, 2007. Incorporated by reference to Exhibit 10.3 to the Company’s Form 10-Q filedAugust 9, 2007. (Portions omitted pursuant to request for confidential treatment.) 10.18 Amendment #3 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services, dated October 2, 2007.Incorporated by reference to Exhibit 10.6 of the Company’s Form 10-K filed March 4, 2008. 10.19 Amendment #4 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated April 3, 2008. Incorporatedby reference to Exhibit 10.29 of the Company’s Form 10-Q filed August 8, 2008. 10.20 Amendment #5 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated July 2, 2008. Incorporatedby reference to Exhibit 10.30 of the Company’s Form 10-Q filed August 8, 2008. 10.21 Amendment #6 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated August 18, 2008.Incorporated by reference to Exhibit 10.1 of the Company’s Form 8-K filed November 7, 2008. 10.22 Amendment #7 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated November 17, 2008.Incorporated by reference to Exhibit 10.12 of the Company’s Form 10-K filed March 6, 2009. 10.23 Amendment #8 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated March 13, 2009.Incorporated by reference to Exhibit 10.13 of the Company’s Form 10-K filed March 9, 2010. 10.24 Amendment #9 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Department of Health and Human Services dated September 18, 2009.Incorporated by reference to Exhibit 10.1 of the Company’s Form 10-Q filed November 6, 2009. 10.25 Amendment #10 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated October 15, 2009. Incorporated byreference to Exhibit 10.2 of the Company’s Form 10-Q filed November 6, 2009. 10.26 Amendment #11 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated February 23, 2011. Incorporated byreference to Exhibit 10.25 of the Company’s Form 10-K filed March 15, 2011. 10.27 Stop-Work Order from U.S. Department of Health and Human Services, dated March 26, 2013, relating to Agreement dated January 3, 2007 between theCompany and the U.S. Department of Health and Human Services. Incorporated by reference to Exhibit 10.1 of the Company’s Form 10-Q filed May 9, 2013. 10.28 Amendment #13 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated February 15, 2012. 10.29 Amendment #14 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated June 4, 2013. Incorporated by referenceto Exhibit 10.1 of the Company’s Form 10-Q filed June 5, 2013. 10.30# Amendment #15 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated September 5, 2013. Incorporated byreference to Exhibit 10.1 of the Company’s Form 10-Q filed November 8, 2013. (Portions omitted pursuant to request for confidential treatment.) 10.31 Amendment #16 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated December 17, 2013. Incorporated byreference to Exhibit 10.1 of the Company’s Form 8-K filed December 23, 2013. 10.32 Amendment #17 to the Agreement between the Company and the U.S. Department of Health & Human Services, dated February 21, 2014. Incorporated byreference to Exhibit 10.1 of the Company’s Form 8-K filed February 26, 2014. 86 10.33 Order for Supplies or Services from the U.S. Department of Health & Human Services, dated November 4, 2009. Incorporated by reference to Exhibit 10.16 ofthe Company’s Form 10-K filed March 9, 2010. 10.34 Amendment #18 to the Agreement between BioCryst Pharmaceuticals, Inc. and the U.S. Department of Health and Human Services, dated March 28, 2014.Incorporated by reference to Exhibit 10.1 to the Company’s Form 8-K filed April 3, 2014. 10.35 Amendment #19 to the Agreement between BioCryst Pharmaceuticals, Inc. and the U.S. Department of Health and Human Services, dated April 29, 2014.Incorporated by reference to Exhibit 10.1 to the Company’s Form 8-K filed May 2, 2014. 10.36 Amendment #20 to the Agreement to the Agreement between BioCryst Pharmaceuticals, Inc. and the U.S. Department of Health and Human Services, datedMay 30, 2014. . Incorporated by reference to Exhibit 10.1 to the Company’s Form 8-K filed June 5, 2014. 10.37# License, Development and Commercialization Agreement dated as of February 28, 2007, by and between the Company and Shionogi & Co., Ltd. Incorporatedby reference to Exhibit 10.4 to the Company’s Form 10-Q filed May 10, 2007. (Portions omitted pursuant to request for confidential treatment.) 10.38# First Amendment to License, Development and Commercialization Agreement, effective as of September 30, 2008, between the Company and Shionogi & Co.,Ltd. Incorporated by reference to Exhibit 10.19 to the Company’s Form 10-K filed March 6, 2009. (Portions omitted pursuant to request for confidentialtreatment.) 10.39 Riverchase Business Park Warehouse Lease dated July 12, 2000 between RBP, LLC an Alabama Limited Liability Company and the Registrant foroffice/warehouse space. Incorporated by reference to Exhibit 10.8 to the Company’s Form 10-Q for the second quarter ending June 30, 2000 filed August 8,2000. 10.40 Third Amendment to Lease Agreement dated August 7, 2007, by and between Riverchase Capital LLC, a Florida limited liability company, Stow Riverchase,LLC, a Florida limited liability company, as successor landlord to RBP, LLC and the Company. Incorporated by reference to Exhibit 10.4 of the Company’sForm 10-Q filed August 9, 2007. 10.41 Fourth Amendment to the Lease Agreement dated February 1, 2012, by and between Riverchase Capital LLC, a Florida limited liability company, StowRiverchase, LLC, a Florida limited liability company, as successor landlord to RBP, LLC and the Company. Incorporated by reference to Exhibit 10.27 of theCompany’s Form 10-K filed March 11, 2013. 10.42 Fifth Amendment to Lease Agreement dated January 15, 2015, by and between Riverchase Capital LLC, a Florida limited liability company, Stow Riverchase,LLC, a Florida limited liability company, as successor landlord to RBP, LLC and the Company. Incorporated by reference to Exhibit 10.42 of the Company’sForm 10-K filed March 2, 2015. 10.43 Stock and Warrant Purchase Agreement dated as of August 6, 2007, by and among BioCryst Pharmaceuticals, Inc. and each of the Investors identified on thesignature pages thereto. Incorporated by reference to Exhibit 4.1 of the Company’s Form 8-K filed August 7, 2007. 10.44 Stock Purchase Agreement, dated as of February 17, 2005, by and among BioCryst Pharmaceuticals, Inc., Baker Bros. Investments, L.P., Baker Biotech Fund II,L.P., Baker Bros. Investments II, L.P., Baker Biotech Fund II (Z), L.P., Baker/Tisch Investments, L.P., Baker Biotech Fund III, L.P., Baker Biotech Fund I,L.P., Baker Biotech Fund III (Z), L.P. and 14159, L.P. Incorporated by reference to Exhibit 4.1 to the Company’s Form 8-K filed February 17, 2005. 10.45# Development and License Agreement dated as of February 1, 2006, by and between BioCryst Pharmaceuticals, Inc. and Mundipharma International HoldingsLimited. Incorporated by reference to Exhibit 10.2 to the Company’s Form 8-K/A filed May 2, 2006. (Portions omitted pursuant to request for confidentialtreatment.) 10.46# Amended and Restated Development and License Agreement, dated as of November 11, 2011, by and between BioCryst Pharmaceuticals, Inc. andMundipharma International Corporation Limited. Incorporated by reference to Exhibit 10.32 to the Company’s Form 10-K filed March 6, 2012. (Portionsomitted pursuant to request for confidential treatment.) 10.47# License Agreement dated as of June 27, 2000, by and among Albert Einstein College of Medicine, Industrial Research, Ltd. and BioCryst Pharmaceuticals, Inc.,as amended by the First Amendment Agreement dated as of July 26, 2002 and the Second Amendment Agreement dated as of April 15, 2005. Incorporated byreference to Exhibit 10.1 to the Company’s Form 8-K filed November 30, 2005. (Portions omitted pursuant to request for confidential treatment.) 87 10.48# Third Amendment Agreement by and among Albert Einstein College of Medicine, Industrial Research, Ltd. and BioCryst Pharmaceuticals, Inc., dated as ofDecember 11, 2009. Incorporated by reference to Exhibit 10.33 to the Company’s Form 10-K filed March 9, 2010. (Portions omitted pursuant to request forconfidential treatment.) 10.49# Fourth Amendment Agreement by and among Albert Einstein College of Medicine, Industrial Research, Ltd. and BioCryst Pharmaceuticals, Inc., dated as of May5, 2010. Incorporated by reference to Exhibit 10.1 to the Company’s Form 10-Q filed August 6, 2010. (Portions omitted pursuant to request for confidentialtreatment.) 10.50# Fifth Amendment Agreement by and among Albert Einstein College of Medicine, Industrial Research, Ltd. and BioCryst Pharmaceuticals, Inc., dated as ofNovember 17, 2011. Incorporated by reference to Exhibit 10.36 to the Company’s Form 10-K filed March 6, 2012. (Portions omitted pursuant to request forconfidential treatment.) 10.51# Sixth Amendment Agreement by and among Albert Einstein College of Medicine, Industrial Research, Ltd. and BioCryst Pharmaceuticals, Inc., dated as of June19, 2012. Incorporated by reference to Exhibit 10.1 to the Company’s Form 10-Q filed August 8, 2012. (Portions omitted pursuant to request for confidentialtreatment.) 10.52 Novation Agreement among Albert Einstein College of Medicine of Yeshiva University, BioCryst Pharmaceuticals, Inc., Mundipharma International CorporationLimited, Callaghan Innovation Research Limited, and Victoria Link Limited, dated May 18, 2015. Incorporated by reference to Exhibit 10.6 to the Company’sForm 10-Q filed August 7, 2015. 10.53 Novation Agreement among Albert Einstein College of Medicine of Yeshiva University, BioCryst Pharmaceuticals, Inc., Callaghan Innovation Research Limited,and Victoria Link Limited, dated June 24, 2015. Incorporated by reference to Exhibit 10.7 to the Company’s Form 10-Q filed August 7, 2015. 10.54 Purchase and Sale Agreement, dated as of March 9, 2011 between BioCryst Pharmaceuticals, Inc. and JPR Royalty Sub LLC. Incorporated by reference toExhibit 10.1 of the Company’s Form 10-Q filed May 6, 2011. 10.55 Pledge and Security Agreement, dated as of March 9, 2011 between BioCryst Pharmaceuticals, Inc. and U.S. Bank National Association, as trustee. Incorporatedby reference to Exhibit 10.2 of the Company’s Form 10-Q filed May 6, 2011. 10.56 Confirmation of terms and conditions of ISDA Master Agreement, dated as of March 7, 2011, between Morgan Stanley Capital Services Inc. and BioCrystPharmaceuticals, Inc. dated as of March 9, 2011. Incorporated by reference to Exhibit 10.3 of the Company’s Form 10-Q filed May 6, 2011. 10.57# Agreement, dated as of September 12, 2013, between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases. Incorporatedby reference to Exhibit 10.2 of the Company’s Form 10-Q filed November 8, 2013. (Portions omitted pursuant to request for confidential treatment.) 10.58# Amendment #1 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated December 26,2013. Incorporated by reference to Exhibit 10.51 to the Company’s Form 10-K filed on March 10, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.59# Amendment #2 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated January 24,2014. Incorporated by reference to Exhibit 10.52 to the Company’s Form 10-K filed on March 10, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.60# Amendment #3 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated June 17, 2014.Incorporated by reference to Exhibit 10.5 to the Company’s Form 10-Q filed on August 8, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.61# Amendment #4 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated June 17, 2014.Incorporated by reference to Exhibit 10.6 to the Company’s Form 10-Q filed on August 8, 2014. (Portions omitted pursuant to request for confidential treatment.) 10.61# Amendment #5 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated August 11, 2014.Incorporated by reference to Exhibit 10.1 to the Company’s Form 10-Q filed on November 7, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.62# Amendment #6 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated August 27,2014. Incorporated by reference to Exhibit 10.2 to the Company’s Form 10-Q filed on November 7, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 88 10.63# Amendment #8 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated September 17,2014. Incorporated by reference to Exhibit 10.3 to the Company’s Form 10-Q filed on November 7, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.64# Amendment #9 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated October 29,2014. Incorporated by reference to Exhibit 10.4 to the Company’s Form 10-Q filed on November 7, 2014. (Portions omitted pursuant to request for confidentialtreatment.) 10.65# Amendment #10 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated February 13,2015. Incorporated by reference to Exhibit 10.2 to the Company’s Form 10-Q filed on August 7, 2015. (Portions omitted pursuant to request for confidentialtreatment.) 10.66# Amendment #11 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated March 19,2015. Incorporated by reference to Exhibit 10.3 to the Company’s Form 10-Q filed on August 7, 2015. (Portions omitted pursuant to request for confidentialtreatment.) 10.67# Amendment #12 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated June 12,2015. Incorporated by reference to Exhibit 10.4 to the Company’s Form 10-Q filed on August 7, 2015. (Portions omitted pursuant to request for confidentialtreatment.) 10.68# Amendment #13 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated June 17,2015. Incorporated by reference to Exhibit 10.5 to the Company’s Form 10-Q filed on August 7, 2015. (Portions omitted pursuant to request for confidentialtreatment.) 10.69# Amendment #14 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated September 16,2015. Incorporated by reference to Exhibit 10.3 to the Company’s Form 10-Q filed on November 6, 2015. (Portions omitted pursuant to request for confidentialtreatment.) (10.70) Amendment #15 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated November 16,2015. (10.71)† Amendment #16 to the Agreement between BioCryst Pharmaceuticals, Inc. and the National Institute of Allergy and Infectious Diseases, dated December 18,2015. (Portions omitted pursuant to request for confidential treatment.) 10.72# Agreement between BioCryst Pharmaceuticals, Inc. and the Biomedical Advanced Research and Development Authority within the U.S. Department of Healthand Human Services' Office of the Assistant Secretary for Preparedness and Response, dated March 27, 2015. Incorporated by reference to Exhibit 10.2 to theCompany’s Form 10-Q filed on May 8, 2015. (Portions omitted pursuant to request for confidential treatment.) 10.73# Amendment #1 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Biomedical Advanced Research and Development Authority within the U.S.Department of Health and Human Services’ Office of the Assistant Secretary for Preparedness and Response, dated June 2, 2015. Incorporated by reference toExhibit 10.1 to the Company’s Form 10-Q filed on August 7, 2015. (Portions omitted pursuant to request for confidential treatment.) 10.74# Amendment #2 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Biomedical Advanced Research and Development Authority within the U.S.Department of Health and Human Services’ Office of the Assistant Secretary for Preparedness and Response, dated July 8, 2015. Incorporated by reference toExhibit 10.1 to the Company’s Form 10-Q filed on November 6, 2015. (Portions omitted pursuant to request for confidential treatment.) 10.75# Amendment #3 to the Agreement between BioCryst Pharmaceuticals, Inc. and the Biomedical Advanced Research and Development Authority within the U.S.Department of Health and Human Services’ Office of the Assistant Secretary for Preparedness and Response, dated August 25, 2015. Incorporated by referenceto Exhibit 10.2 to the Company’s Form 10-Q filed on November 6, 2015. (Portions omitted pursuant to request for confidential treatment.) 10.76# License Agreement by and between BioCryst Pharmaceuticals, Inc. and Seqirus UK Limited, dated as of June 16, 2015. Incorporated by reference to Exhibit 10.8to the Company’s Form 10-Q filed on May 8, 2015. (Portions omitted pursuant to request for confidential treatment.) 89 (21) Subsidiaries of the Registrant. (23) Consent of Ernst & Young, LLP, Independent Registered Public Accounting Firm. (31.1) Certification of the Chief Executive Officer Pursuant to Section 302 of the Sarbanes-Oxley Act of 2002. (31.2) Certification of the Chief Financial Officer Pursuant to Section 302 of the Sarbanes-Oxley Act of 2002. (32.1) Certification pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of the Sarbanes-Oxley Act of 2002. (32.2) Certification pursuant to 18 U.S.C. Section 1350, as adopted pursuant to Section 906 of the Sarbanes-Oxley Act of 2002. (101) Financial statements from the Annual Report on Form 10-K of BioCryst Pharmaceuticals, Inc. for the year ended December 31, 2015, formatted in XBRL: (i)Consolidated Balance Sheets, (ii) Consolidated Statements of Comprehensive Loss, (iii) Consolidated Statements of Cash Flows, (iv) Consolidated Statementsof Stockholders’ Equity and (v) Notes to Consolidated Financial Statements. † Confidential treatment requested.# Confidential treatment granted.& Management contracts.( ) Filed herewith. 90 Exhibit 10.70 EXHIBIT 10.71 Exhibit 21Subsidiaries of the Registrant Subsidiary Jurisdiction of Incorporation JPR Royalty Sub LLC Delaware BioCryst UK Limited United Kingdom Exhibit 23 Consent of Independent Registered Public Accounting Firm We consent to the incorporation by reference in the following Registration Statements: • Registration Statements (Form S-8 Nos. 333-120345, 333-39484 and 333-30751) pertaining to the BioCryst Pharmaceuticals, Inc. 1991 Stock Option Plan, asamended and restated as of March 8, 2004; • Registration Statement (Form S-8 No. 333-90582) pertaining to the BioCryst Pharmaceuticals, Inc. Employee Stock Purchase Plan; • Registration Statement (Form S-8 No. 333-136703) pertaining to the BioCryst Pharmaceuticals, Inc. Stock Incentive Plan, which amended and restated theBioCryst Pharmaceuticals, Inc. 1991 Stock Option Plan as of May 17, 2006; • Registration Statement (Form S-3 No. 333-145638) pertaining to the registration of up to 8,140,000 shares of common stock; • Registration Statement (Form S-8 No. 333-145627) pertaining to the BioCryst Pharmaceuticals, Inc. Stock Incentive Plan as amended and restated effectiveMarch 2007 and Employment Letter Agreement dated April 2, 2007 between BioCryst Pharmaceuticals, Inc. and David McCullough; • Registration Statement (Form S-3 No. 333-153084) for the registration of 3,335,408 shares of BioCryst Pharmaceuticals, Inc. common stock and 3,159,895warrants to purchase common stock of BioCryst Pharmaceuticals, Inc.; • Registration Statement (Form S-8 No. 333-152570) pertaining to the BioCryst Pharmaceutical, Inc. Stock Incentive Plan, as amended and restated effectiveFebruary 28, 2008 and the BioCryst Pharmaceuticals, Inc. Employee Stock Purchase Plan, as amended and restated effective February 28, 2008; • Registration Statement (Form S-8 No. 333-167830) pertaining to the BioCryst Pharmaceuticals, Inc. Stock Incentive Plan, as amended and restated effectiveMarch 31, 2010 and the BioCryst Pharmaceuticals, Inc. Employee Stock Purchase Plan, as amended and restated effective March 31, 2010; • Registration Statement (Form S-8 No. 333-176096) pertaining to the BioCryst Pharmaceutical, Inc. Stock Incentive Plan, as amended and restated effectiveFebruary 17, 2011; • Registration Statement (Form S-3 No. 333-192117) for the registration of up to $125 million of BioCryst Pharmaceuticals, Inc. common stock, preferred stock,depository shares, stock purchase contracts, warrants or units; • Registration Statement (Form S-8 No. 333-187193) pertaining to the BioCryst Pharmaceuticals, Inc. Stock Incentive Plan and Employee Stock Purchase Plan,each as amended and restated effective March 29, 2012; • Registration Statement (Form S-8 No. 333-195869) pertaining to the BioCryst Pharmaceuticals, Inc. Stock Incentive Plan and Employee Stock Purchase Plan,each as amended and restated effective March 8, 2014; • Registration Statement (Form S-8 No. 333-202466) for the registration of up to $150 million of BioCryst Pharmaceuticals, Inc. common stock, preferred stock,depositary shares, stock purchase contracts, warrants or units; of our reports dated February 26, 2016 with respect to the consolidated financial statements of BioCryst Pharmaceuticals, Inc. and the effectiveness of internal control overfinancial reporting of BioCryst Pharmaceuticals, Inc. included in this Annual Report (Form 10-K) of BioCryst Pharmaceuticals, Inc. for the year ended December 31, 2015. /s/ Ernst & Young LLP Raleigh, North Carolina February 26, 2016 Exhibit 31.1CERTIFICATIONSI, Jon P. Stonehouse, certify that:1. I have reviewed this annual report on Form 10-K of BioCryst 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 the statements made,in light of the circumstances under which such statements were made, not misleading with respect to the period covered by this report;3. Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects the financialcondition, 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(s) and I are responsible for establishing and maintaining disclosure controls and procedures (as defined in Exchange ActRules 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 thatmaterial information relating to the registrant, including its consolidated subsidiaries, is made known to us by others within those entities, particularly during the periodin which this report is being prepared;b) designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under our supervision, to providereasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposes in accordance with generallyaccepted accounting principles;c) evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our conclusions about the effectiveness of thedisclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; andd) disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during the registrant’s most recent fiscal quarter (theregistrant’s fourth fiscal quarter in the case of an annual report) that has materially affected, or is reasonably likely to materially affect, the registrant’s internal controlover financial reporting; and5. The registrant’s other certifying officer(s) and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to the registrant’sauditors and the audit committee of the registrant’s board of directors (or persons performing the equivalent functions):a) all significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which are reasonably likely toadversely affect the registrant’s ability to record, process, summarize and report financial information; andb) any fraud, whether or not material, that involves management or other employees who have a significant role in the registrant’s internal control over financialreporting. /s/ Jon P. Stonehouse Jon P. Stonehouse Chief Executive OfficerDate: February 26, 2016Exhibit 31.2CERTIFICATIONSI, Thomas R. Staab II, certify that:1. I have reviewed this annual report on Form 10-K of BioCryst 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 the statements made,in light of the circumstances under which such statements were made, not misleading with respect to the period covered by this report;3. Based on my knowledge, the financial statements, and other financial information included in this report, fairly present in all material respects the financialcondition, 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(s) and I are responsible for establishing and maintaining disclosure controls and procedures (as defined in Exchange ActRules 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 thatmaterial information relating to the registrant, including its consolidated subsidiaries, is made known to us by others within those entities, particularly during the periodin which this report is being prepared;b. designed such internal control over financial reporting, or caused such internal control over financial reporting to be designed under our supervision, to providereasonable assurance regarding the reliability of financial reporting and the preparation of financial statements for external purposes in accordance with generallyaccepted accounting principles;c. evaluated the effectiveness of the registrant’s disclosure controls and procedures and presented in this report our conclusions about the effectiveness of thedisclosure controls and procedures, as of the end of the period covered by this report based on such evaluation; andd. disclosed in this report any change in the registrant’s internal control over financial reporting that occurred during the registrant’s most recent fiscal quarter (theregistrant’s fourth fiscal quarter in the case of an annual report) that has materially affected, or is reasonably likely to materially affect, the registrant’s internal controlover financial reporting; and5. The registrant’s other certifying officer(s) and I have disclosed, based on our most recent evaluation of internal control over financial reporting, to the registrant’sauditors and the audit committee of the registrant’s board of directors (or persons performing the equivalent functions):a. all significant deficiencies and material weaknesses in the design or operation of internal control over financial reporting which are reasonably likely toadversely affect the registrant’s ability to record, process, summarize and report financial information; andb. any fraud, whether or not material, that involves management or other employees who have a significant role in the registrant’s internal control over financialreporting. /s/ Thomas R. Staab II Thomas R. Staab II Chief Financial Officer and Treasurer (Principal Financial Officer)Date: February 26, 2016 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 In connection with the Annual Report of BioCryst Pharmaceuticals, Inc. (the “Company”) on Form 10-K for the period ending December 31, 2015 as filed with theSecurities and Exchange Commission on the date hereof (the “Report”), I, Jon P. Stonehouse, Chief Executive Officer of the Company, certify, pursuant to 18 U.S.C. § 1350,as adopted pursuant to § 906 of the Sarbanes-Oxley Act of 2002, that, to the best of my knowledge: (1) The Report fully complies with the requirements of section 13(a) or 15(d) of the Securities Exchange Act of 1934; and (2) The information contained in the Report fairly presents, in all material respects, the financial condition and results of operations of the Company. /s/ Jon P. Stonehouse Jon P. StonehouseChief Executive Officer February 26, 2016 This certification is furnished with this Report on Form 10-K pursuant to Section 906 of the Sarbanes-Oxley Act of 2002 and shall not, except to the extent required bysuch Act, be deemed filed by the Company for purposes of Section 18 of the Securities Exchange Act of 1934, as amended (the “Exchange Act”). Such certification will notbe deemed to be incorporated by reference into any filing under the Securities Act of 1933, as amended, or the Exchange Act, except to the extent that the Companyspecifically incorporates it by reference. 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 In connection with the Annual Report of BioCryst Pharmaceuticals, Inc. (the “Company”) on Form 10-K for the period ending December 31, 2015 as filed with theSecurities and Exchange Commission on the date hereof (the “Report”), I, Thomas R. Staab, II, Chief Financial Officer of the Company, certify, pursuant to 18 U.S.C. § 1350,as adopted pursuant to § 906 of the Sarbanes-Oxley Act of 2002, that, to the best of my knowledge: (1) The Report fully complies with the requirements of section 13(a) or 15(d) of the Securities Exchange Act of 1934; and (2) The information contained in the Report fairly presents, in all material respects, the financial condition and results of operations of the Company. /s/ Thomas R. Staab II Thomas R. Staab II Chief Financial Officer and Treasurer (Principal Financial Officer) February 26, 2016 This certification is furnished with this Report on Form 10-K pursuant to Section 906 of the Sarbanes-Oxley Act of 2002 and shall not, except to the extent required bysuch Act, be deemed filed by the Company for purposes of Section 18 of the Securities Exchange Act of 1934, as amended (the “Exchange Act”). Such certification will notbe deemed to be incorporated by reference into any filing under the Securities Act of 1933, as amended, or the Exchange Act, except to the extent that the Companyspecifically incorporates it by reference.
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