UNITED STATES

SECURITIES AND EXCHANGE COMMISSION

WASHINGTON, D.C. 20549

 

FORM 8-K

 

CURRENT REPORT

Pursuant to Section 13 or 15(d) of the Securities Exchange Act of 1934

Date of Report (Date of earliest event reported): June 5, 2017

 

bluebird bio, Inc.

(Exact name of Registrant as Specified in Its Charter)

 

 

Registrant’s Telephone Number, Including Area Code: (339) 499-9300

Not Applicable

(Former Name or Former Address, if Changed Since Last Report)

 

Check the appropriate box below if the Form 8-K filing is intended to simultaneously satisfy the filing obligation of the registrant under any of the following provisions (see General Instructions A.2. below):

Indicate by check mark whether the registrant is an emerging growth company as defined in as defined in Rule 405 of the Securities Act of 1933 (§ 230.405 of this chapter) or Rule 12b-2 of the Securities Exchange Act of 1934 (§ 240.12b-2 of this chapter).

Emerging growth company ☐

If an emerging growth company, indicate by check mark if the registrant has elected not to use the extended transition period for complying with any new or revised financial accounting standards provided pursuant to Section 13(a) of the Exchange Act. ☐

 

 

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Item 7.01    Regulation FD Disclosure

 

On June 5, 2017, bluebird bio, Inc. (“bluebird”) will be conducting meetings with investors attending the American Society of Clinical Oncology Annual Meeting.  As part of these meetings, bluebird will deliver the slide presentation furnished to this report as Exhibit 99.1 and which is incorporated by reference herein.

 

See Item 8.01 below, which is incorporated by reference herein.

 

The information in Item 7.01 of this Report on Form 8-K and Exhibit 99.1 attached hereto is intended to be furnished and shall not be deemed “filed” for purposes of Section 18 of the Securities Exchange Act of 1934 (the “Exchange Act’) or otherwise subject to the liabilities of that section, nor shall it be deemed incorporated by reference in any filing under the Securities Act of 1933 or the Exchange Act, except as expressly set forth by specific reference in such filing.

 

Item 8.01   Other Events

 

On June 5, 2017, bluebird issued a press release announcing updated clinical data from its anti-BCMA CAR T cell therapy, being presented at the American Society of Clinical Oncology Annual Meeting on June 5, 2017.  The full text of bluebird’s press release regarding the announcement is filed as Exhibit 99.2 to this Current Report on Form 8-K and is incorporated herein by reference.

 

Item 9.01Financial Statements and Exhibits.

(d) Exhibits

 

 

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SIGNATURES

Pursuant to the requirements of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the undersigned hereunto duly authorized.

 

 

 

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EXHIBIT INDEX

 

 

 

bb2121 Investor & Analyst Event June 5, 2017 NASDAQ: BLUE Exhibit 99.1

These slides and the accompanying oral presentation contain forward-looking statements and information relating to bluebird bio, its product candidate bb2121 and oncology research and development plans. The use of words such as “may,” “might,” “will,” “should,” “expect,” “plan,” “anticipate,” “believe,” “estimate,” “project,” “intend,” “future,” “potential,” or “continue,” and other similar expressions are intended to identify forward-looking statements. For example, all statements we make regarding the initiation, timing, progress and results of our preclinical and clinical studies and our research and development programs, our ability to advance product candidates into, and successfully complete, clinical studies, and the timing or likelihood of regulatory filings and approvals are forward looking. All forward-looking statements are based on estimates and assumptions by our management that, although we believe to be reasonable, are inherently uncertain. All forward-looking statements are subject to risks and uncertainties that may cause actual results to differ materially from those that we expected. These statements are also subject to a number of material risks and uncertainties that are described in our most recent quarterly report on Form 10-Q, as well as our subsequent filings with the Securities and Exchange Commission. Any forward-looking statement speaks only as of the date on which it was made. We undertake no obligation to publicly update or revise any forward-looking statement, whether as a result of new information, future events or otherwise, except as required by law. Forward Looking Statements

Agenda Introduction bluebird Oncology Franchise CRB-401 Study Design and Clinical Overview CRB-401 Data Closing Q&A Manisha Pai, Nick Leschly Philip Gregory, D.Phil. M. Travis Quigley Jesus Berdeja, M.D. David Davidson, M.D. bluebird bio management Jesus Berdeja, M.D., principal investigator Michael Pehl, president, hematology & oncology, Celgene

Welcome Nick Leschly, chief bluebird

Our Vision: Make Hope a Reality TRUE BLUE BLUE MOJO OUR PATIENTS OUR PEOPLE

Advancing Multiple Programs in Parallel MM TDT SCD CALD

Our Strategic Intent Severe Genetic Diseases Hematopoietic Stem Cells (HSCs) Immunotherapy T Cells Late Stage (LentiGlobin, Lenti-D) Big Near Term Opportunities (SCD, Multiple Myeloma) Best Team (300+) Great Partners Truly Integrated Platform Transformative Product Focus “Tetris” R&D (Anti-Pure Play) Lentiviral Gene Delivery Pure, Potent, Reproducible, Scalable Global Manufacturing Platform Virus and Drug Product Genome Editing Platform MegaTALs

bluebird Oncology Franchise Philip Gregory, D.Phil., chief scientific officer

Pipeline COLLABORATORS

Good is Never Good Enough for Patients: bluebird Toolbox Strategy BCMA (bb2121) LentiGlobin v1.0 Transduction Durability BCMA & PI3Ki (bb21217) LentiGlobin & Enhancers v2.0 Novel areas; autoimmune In vivo gene editing Optimized severe genetic disease products New & enhanced oncology products vFuture BCMA & Solid Tumors LentiGlobin Product Engine MegaTAL Gene Editing LNPs Lentivirus mRNA

Building a Translational Oncology Products Company: The Right Approach for the Right Targets Targets Tools Partnerships Immuno-Oncology R&D Engine Oncology Pipeline Access to targets: both CARs and TCRs Optimization: gene editing; manufacturing enhancements; on/off switches; product and technology combinations Internal focus on bluebird strengths coupled with academic and industry collaborations to benefit from outside strengths Building a broad and diversified pipeline

Tumor Specific Antigens e.g. Intracellular Targets TCR technology provides T cell redirection to intracellular antigens not addressable by CARs Medigene partnership provides bluebird access to TCR therapeutic candidates against four targets Targets Personalized cancer treatment with TCRs Rapid, efficient and lean process for lead TCR candidates

Example 1: bb21217 – making younger T cells Example 2: megaTALs – driving site specific CAR insertion Tools Building on the T Cell Chassis with Manufacturing Improvements and Genome Editing

Building a Translational Oncology Products Company: The Right Approach for the Right Targets Access to targets: both CARs and TCRs Optimization: gene editing; manufacturing enhancements; on/off switches; product and technology combinations Internal focus on bluebird strengths coupled with academic and industry collaborations to benefit from outside strengths Building a broad and diversified pipeline Targets Tools Partnerships Immuno-Oncology R&D Engine Oncology Pipeline

CRB-401 Study Design and Clinical Overview M. Travis Quigley BCMA program leader & senior director, clinical development

Despite Progress in Multiple Myeloma, There Remains a Need for New Therapies Kenneth C. Anderson Clin Cancer Res 2016;22:5419-5427 “Despite the availability of these classes of drugs for the treatment of MM, a recent analysis of patients with relapsed and refractory MM (RRMM) who were double refractory to a PI and an IMiD or had relapsed after >3 prior lines of therapy, including the novel agents pomalidomide (third-generation IMiD) and carfilzomib (second-generation PI), showed a median overall survival (OS) of 8 months.” Usmani, Blood 2016 Improvement in overall survival from median of 3 to 8-10 years Proportion surviving Follow-up from diagnosis (years) Preclinical and clinical studies leading to FDA approvals in MM 2015 Daratumumab 2015 Elotuzumab 2006 Thalidomide 2005 2010 2015 2007 Doxil + BTZ 2003, 2005, 2008 Bortezomib (BTZ) 2012, 2015 Carfilzomib 2015 Panobinostat 2013, 2015 Pomalidomide 2015 Ixazomib Immunomodulatory agent Monoclonal antibody Proteasome inhibitor HDAC inhibitor 2006, 2014 Lenalidomide CCR Focus © 2016 American Association for Cancer Research

Current U.S. Standard of Care in 3rd/4th Line Multiple Myeloma   Current U.S. Standards of Care Pomalyst and dex. (Pomalyst Product Monograph) Daratumamab (Lancet 2016, Lonial, S) N 452 106 Inclusion Criteria ≥2 prior therapies (including REVLIMID and bortezomib) Relapsed and refractory multiple myeloma Disease progression on or within 60 days of last therapy Previously treated with at least three lines of therapy (including proteasome inhibitors and immunomodulatory drugs), or were refractory to both proteasome inhibitors and immunomodulatory drugs Prior Tx 5 (2-14) 5 (2-14) CR Rate (%) <1% ~3% ORR (%) 23.5% 29% PFS (mos) 3.6 months 3.7 months The existing SOC outcomes for 3rd/4th line are limited in efficacy and durability leaving a need for new options for patients in need of better results Deep MRD negative responses are desirable in earlier lines of therapy and have demonstrated a benefit in long term outcomes

BCMA – A Promising Target in Multiple Myeloma Multiple myeloma cells expressing BCMA (brown color = BCMA protein) BCMA is member of the TNF receptor superfamily expressed nearly universally on multiple myeloma cells with expression largely restricted to plasma cells and some mature B cells Initial proof of anti-BCMA activity has been demonstrated using T cells transduced with a gamma-retroviral vector encoding an anti-BCMA CAR with a CD28 costimulatory domain, but significant cytokine release syndrome occurred in patients with high disease burden (Ali et al., Blood 2016) B-Cell Maturation Antigen (BCMA) Despite the availability of various approved therapies, including proteasome inhibitors, IMiDs and, more recently, anti-CD38 antibodies, multiple myeloma remains an incurable disease.

Introduction to bb2121 bb2121 is a second-generation CAR construct targeting BCMA, consisting of autologous T cells transduced with a lentiviral vector encoding a novel CAR incorporating an anti-BCMA scFv, a 4-1BB costimulatory motif to promote proliferation and persistence, and a CD3-zeta T cell activation domain Construct demonstrated potent preclinical in vivo activity with low tonic signaling bb2121: Anti-BCMA Chimeric Antigen Receptor T Cell Product Candidate

CRB-401 Phase 1 Study in Relapsed / Refractory Multiple Myeloma Objectives: Determine preliminary safety and efficacy and recommended phase 2 dose N = 50 patients, standard 3 + 3 dose escalation + expansion cohort Eligibility: Relapsed / refractory MM with ≥ 3 prior lines of therapy (including PI and IMiD), or double refractory Measurable disease ≥ 50% BCMA expression 9 U.S. Clinical Sites, 1 Centralized Manufacturing Site CRB-401 Open-label Phase 1 Clinical Study of bb2121

CRB-401 Data Jesus Berdeja, M.D. Sarah Cannon Research Institute & Tennessee Oncology

First-in-Human Multicenter Study of bb2121 anti-BCMA CAR T Cell Therapy for Relapsed/Refractory Multiple Myeloma: Updated Results Jesus G. Berdeja, MD1, Yi Lin, MD, PhD2, Noopur Raje, MD3, Nikhil Munshi, MD4, David Siegel, MD, PhD5, Michaela Liedtke, MD6, Sundar Jagannath, MD7, Marcela Maus, MD, PhD3, Ashley Turka8, Lyh Ping Lam8, Kristen Hege, MD9, Richard Morgan, PhD8, M. Travis Quigley8, and James N. Kochenderfer, MD10 1-Sarah Cannon Research Institute and Tennessee Oncology, Nashville, TN; 2-Mayo Clinic, Rochester, MN; 3-Massachusetts General Hospital Cancer Center, Boston, MA; 4-Dana Farber Cancer Institute, Boston, MA; 5-Hackensack University Medical Center, Hackensack, NJ; 6-Stanford University Medical Center, Palo Alto, CA; 7-Mt. Sinai Medical Center, New York, NY; 8-bluebird bio, Inc., Cambridge, MA; 9-Celgene, San Francisco, CA; 10-Experimental Transplantation and Immunology Branch, National Cancer Institute/National Institutes of Health, Bethesda, MD

CRB-401 Open-label Phase 1 Clinical Study of bb2121 Study Status CRB-401 is a phase 1 dose-escalation and dose response study in relapsed / refractory MM Objectives: Determine preliminary safety and efficacy and recommended phase 2 dose 50 patients planned, standard 3 + 3 dose escalation followed by expansion cohort Key eligibility criteria Relapsed / refractory MM with ≥ 3 prior lines of therapy (including PI and IMiD), or double refractory Measurable disease ≥ 50% BCMA expression by IHC Adequate bone marrow (ANC ≥1,000, platelet count ≥50,000), adequate renal and hepatic function 3 + 3 Dose Escalation of CAR + T Cells Consented N=35 Cells Collected N=24 Dosed N=21 Clinical deterioration prior to infusion N=3  1 Month Response Evaluation N=18 * bb2121 Successfully manufactured for all patients collected

Baseline Demographics, Clinical Characteristics and Treatment History 21 patients have received bb2121 as of the data cut-off of May 4, 2017. Median follow-up is 15.4 weeks (range 1.4 to 54.4). 1 ECOG: Eastern Cooperative Oncology Group Performance Score 2 ISS: International Staging System 3 SCT: Stem Cell Transplant Parameter Statistic N=21 Dosed Patients Age years Median (range) 58 (37-74) Male gender N (%) 13 (62%) Time since diagnosis (years) Median (range) 5 (1-16) ECOG1 = 0 N (%) 10 (48%) ISS2 Stage I II III N (%) 6 (29%) 11 (52%) 4 (19%) High-risk cytogenetics (del17p, t(4;14), t(14;16), 1q, del 13)    N (%) 14 (67%) Demographics and Clinical Characteristics Parameter Statistic N=21 Dosed Patients Prior lines of therapy Median (range) 7 (3-14) Prior autologous SCT3 N (%) 21 (100%) Prior Therapies Exposed Refractory Bortezomib 100% 67% Carfilzomib 91% 57% Lenalidomide 100% 86% Pomalidomide 91% 71% Daratumumab 71% 48% Cumulative Exposure Exposed Refractory Bort / Len 100% 67% Bort / Len / Car 91% 48% Bort / Len / Pom 91% 57% Bort / Len / Car / Pom 86% 43% Bort / Len / Car / Pom / Dara 71% 29% MM Treatment History

No dose-limiting toxicities (DLTs) observed as of data cut-off Cytopenias related to Cy/Flu lymphodepletion 1 unrelated death due to cardio pulmonary arrest in a patient with an extensive cardiac history, the event occurred over 4 months after bb2121 infusion. The patient had achieved a stringent CR at 1 month and remained in remission at time of event 11 patients experienced 1 or more SAEs. SAEs occurring in more than 1 patient were CRS* Grade 1-2 that required hospitalization per protocol (N=4) and pyrexia (N=2) bb2121 Generally Well Tolerated *CRS uniformly graded according to Lee et al., Blood 2014;124:188-195 Treatment-Emergent Adverse Events in >2 Patients (N=21 Patients Dosed)

Cytokine Release Syndrome Readily Manageable 15/21 (71%) with cytokine release syndrome (CRS)   2 patients with Grade 3 CRS that resolved in 24 hours 4 patients received tocilizumab, 1 (Grade 2 CRS) with steroids CRS grade does not appear related to tumor burden CRS-related symptoms mostly Grade 1-2 No Grade 3/4 neurotoxicity Reported CRS-Related Symptoms In 15/21 treated patients with CRS *In anti-BCMA and anti-CD19 CAR T studies. Ali et al., Blood 2016 128: 1688. Maude et al., NEJM 2014 Peak Cytokine Levels Levels reported in patients with severe CRS*

All Patients in Active Dose Cohorts Achieved an Objective Response, Duration up to 54 Weeks * High tumor burden (>50% bone marrow involvement) Includes unscheduled assessments.

Clinical Response: Time to Response and MRD Efficacy Parameter % (95% CI) ORR all doses 89% (65-99) ORR (> 50 x 106 CAR+ cells) 100% (78.2-100) ≥VGPR (> 50 x 106 CAR+ cells) 73% CR rate (> 50 x 106 CAR+ cells) 27% Median (range) Time to First Response (days) 31 (15-92) Time to Best Response (days) 59.5 (15-186) Duration of Response (days, as of data cut-off) 134+ (7-361) Patient ID Month 1 Month 3 Month 6 4 Negative 10-5 Negative 10-4 (10-5 undetermined) (10-6 undetermined) Negative 10-4 & 10-5 Positive 10-6 6 Negative 10-5 failed QC N/A 8 N/A Negative 10-4 and 10-5 (10-6 undetermined) N/A 9 Negative 10-4 & 10-5 (10-6 undetermined) Negative at 10-4 & 10-5 (10-6 undetermined) N/A *Pt 5 and Pt 7 had no clone identified at baseline; Pt 10 Month 1 failed QC † MRD assessed using next-gen sequencing immunoSEQ, Adaptive, Inc. Durable responses in all evaluable subjects at doses > 50 x 106 CAR+ cells 4 of 4 evaluable patients are MRD negative at 10-5 sensitivity level Assessment of Minimal Residual Disease (MRD)† ORR: overall response rate among patients evaluable for clinical response Response Rates and Timing Pt 9 M1 (PR) M3 (PR) Baseline Pt 12 Baseline D14 M3 (sCR) Pt 6 D14 Baseline M9 (VGPR) Clearance of Myeloma in the Bone Marrow by IHC (CD138+ cells) as Early as Day 14

Tumor Response Kinetics: Rapid Clearance of PET Uptake, sBCMA and sFLC; Slower Clearance of M-protein PET imaging Pt 8 dFLC (% change from baseline)* Serum M-protein (% change from baseline) Serum BCMA (% change from baseline)

Persistence of CAR T Cells in Peripheral Blood up to 24 Weeks

Summary bb2121 has induced durable and deepening responses in a heavily pre-treated population with relapsed/refractory multiple myeloma, including: 100% ORR, 73% VGPR or better, 27% CR (at doses > 50 x 106) MRD negative results in all evaluable patients (N=4) No disease progression in patients treated with doses > 50 x 106, with 1 patient past 1 year and 8 patients past 6 months To date, the safety profile of bb2121 has been manageable through doses as high as 800 x 106 The 2 reported events of grade 3 CRS resolved within 24 hours No grade 3/4 neurotoxicity reported These results will inform identification of the dose(s) to bring forward into the expansion phase of the study in future development

Closing David Davidson, M.D., chief medical officer

Key Takeaways As of May 4 Data Cut-off No DLTs; toxicity readily manageable, CRS largely grade 1/2, two Grade 3 CRS resolved within 24 hours with tocilizumab Safety Profile Responses Durability 100% response rate in active dose cohorts (above 50x106) 27% complete response rate 73% VGPR or better All patients tested for MRD status (N=4) were found to be MRD-negative No patients with clinical progression in active dose cohorts (above 50x106) Heavily pre-treated; all had prior auto transplant, median of 7 prior lines of therapy Patient Population

Q&A

Q&A Nick Leschly, chief bluebird David Davidson, M.D., chief medical officer Philip Gregory, D.Phil., chief scientific officer M. Travis Quigley, BCMA program leader & senior director, clinical development Jesus Berdeja, M.D., Sarah Cannon Research Institute & Tennessee Oncology Michael Pehl, president, hematology & oncology, Celgene

  

 

Exhibit 99.2

 

bluebird bio and Celgene Corporation Announce Updated Clinical Results from Ongoing First-in-Human Multicenter Study of bb2121 Anti-BCMA CAR T Cell Therapy in Relapsed/Refractory Multiple Myeloma at American Society of Clinical Oncology (ASCO) Annual Meeting

 

 

CAMBRIDGE, Mass. and Summit, N.J., June 5, 2017 – bluebird bio, Inc. (NASDAQ: BLUE), and Celgene Corporation (NASDAQ: CELG) today announced that updated results from the ongoing CRB-401 Phase 1 clinical study of bb2121, an investigational anti-BCMA CAR T cell therapy, in 18 patients with relapsed/refractory multiple myeloma will be presented at the American Society of Clinical Oncology (ASCO) Annual Meeting in Chicago, Illinois. The objective of this Phase 1 dose-escalation study is to evaluate safety and efficacy of bb2121 and determine a recommended Phase 2 dose. bluebird bio and Celgene are jointly developing bb2121.

 

“It is impressive to see objective responses in all patients treated at dose levels of 150 x 10⁶ CAR+ T cells or higher in such a heavily pretreated population, including those with high tumor burden.  We are encouraged by the duration and depth of responses, and pleased that the safety profile remains readily manageable,” said David Davidson, M.D., chief medical officer, bluebird bio. “Although these data are still early, it is encouraging that no patient in the active dose cohorts has had myeloma progression. In light of these results, we look forward to initiating the expansion phase of the CRB-401 study in the coming months.”

 

“The heavily pretreated, relapsed/refractory patients in this study have few effective treatment options, highlighting the importance of this interim data. All patients previously underwent autologous HSCT, and received a median of 7 lines of prior therapy,” said Michael Pehl, President, Hematology and Oncology for Celgene. “The

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consistency, depth and durability of these patients’ responses coupled with a manageable safety profile is very exciting, and we believe will provide hope for patients in this setting. Efforts are underway to advance the development of bb2121 for patients with relapsed/refractory multiple myeloma.”

 

First-in-Human Multicenter Study of bb2121 anti-BCMA CAR T Cell Therapy for Relapsed/Refractory Multiple Myeloma: Updated Results. (Abstract #3010)

 

Presenter: Jesus G. Berdeja, M.D., Sarah Cannon Research Institute and Tennessee Oncology, Nashville, TN

Date: Monday, June 5, 2017, 4:45-6:00 pm CT (poster discussion); 8:00-11:30 am CT

Location: Hall D1

Session Title: Poster Discussion Session: Developmental Therapeutics—Immunotherapy

The open-label Phase 1 CRB-401 study (NCT02658929) is investigating the administration of bb2121 anti-BCMA CAR T cells in patients with relapsed and/or refractory multiple myeloma. The primary endpoint of the study is incidence of adverse events (AEs) and abnormal laboratory test results, including dose-limiting toxicities (DLTs). The study also seeks to assess disease-specific response criteria including: complete response (CR), very good partial response (VGPR), and partial response (PR) according to the International Myeloma Working Group (IMWG) Uniform Response Criteria for Multiple Myeloma. The study also seeks to determine the recommended dose for further clinical trials.

Patients on study were heavily pre-treated, with a median of seven prior therapies (range: 3 - 14):

As of the May 4, 2017 data cut-off, 21 patients had been enrolled and dosed in four dose cohorts: 50 x 10⁶, 150 x 10⁶, 450 x 10⁶ and 800 x 10⁶ CAR+ T cells. All 21 dosed patients were evaluable for safety, and 18 patients have undergone their first multiple myeloma tumor restaging and were evaluable for efficacy. This study has enrolled patients at seven sites in the U.S., with an anticipated total enrollment of up to 50 patients.

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Patients received a conditioning regimen of cyclophosphamide and fludarabine, followed by an infusion of bb2121 anti-BCMA CAR T cells. The CAR T cells were produced from each patient’s own blood cells, which were modified using a lentiviral vector encoding the anti-BCMA CAR.

bb2121 is an investigational compound that is not approved for any use in any country.

 

Results, as of May 4, 2017 Data Cut-off:

 

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Webcast Information
bluebird bio will host a live webcast at 6:30 p.m. CT (7:30 p.m. ET) today, June 5, 2017. The live webcast can be accessed under "Calendar of Events" in the Investors and Media section of the company's website at www.bluebirdbio.com.

About bluebird bio, Inc.

With its lentiviral-based gene therapies, T cell immunotherapy expertise and gene editing capabilities, bluebird bio has built an integrated product platform with broad potential application to severe genetic diseases and cancer. bluebird bio’s gene therapy clinical programs include its Lenti-D™ product candidate, currently in a Phase 2/3 study, called the Starbeam Study, for the treatment of cerebral adrenoleukodystrophy, and its LentiGlobin™ product candidate, currently in four clinical studies for the treatment of transfusion-dependent β-thalassemia, and severe sickle cell disease. bluebird bio’s oncology pipeline is built upon the company’s leadership in lentiviral gene delivery and T cell engineering, with a focus on developing novel T cell-based immunotherapies, including chimeric antigen receptor (CAR T) and T cell receptor (TCR) therapies. bluebird bio’s lead oncology program, bb2121, is an anti-BCMA CAR T program partnered with Celgene. bb2121 is currently being studied in a Phase 1 trial for the treatment of relapsed/refractory multiple myeloma.

 

bluebird bio also has discovery research programs utilizing megaTAL/homing endonuclease gene editing technologies with the potential for use across the company’s pipeline.

 

bluebird bio has operations in Cambridge, Massachusetts, Seattle, Washington and Europe.

 

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About Celgene

Celgene Corporation, headquartered in Summit, New Jersey, is an integrated global biopharmaceutical company engaged primarily in the discovery, development and commercialization of innovative therapies for the treatment of cancer and inflammatory diseases through next-generation solutions in protein homeostasis, immuno-oncology, epigenetics, immunology and neuro-inflammation. For more information, please visit www.celgene.com. Follow Celgene on Social Media: @Celgene, Pinterest, LinkedIn, Facebook and YouTube.

 

About the bluebird bio-Celgene Collaboration

In March 2013, bluebird bio and Celgene entered into a collaboration to develop chimeric antigen receptor (CAR) T cell therapies to target and destroy cancer cells. In June 2015, the collaboration was amended and restated to focus on developing product candidates targeting B-cell maturation antigen (BCMA). bluebird bio and Celgene are working together on the initial, lead anti-BCMA product candidate (bb2121), and are developing next-generation anti-BCMA product candidates, including bb21217.

 

Forward-Looking Statements

This press release contains forward-looking statements, which are generally statements that are not historical facts, including statements regarding the potential of the bb2121 product candidate to treat relapsed/refractory multiple myeloma and future clinical development plans of the Company and Celgene. Forward-looking statements can be identified by the words "expects," "anticipates," "believes," "intends," "estimates," "plans," "will," “outlook” and similar expressions. Forward-looking statements are based on management’s current plans, estimates, assumptions and projections, and speak only as of the date they are made. Neither Celgene nor bluebird bio undertake any obligation to update any forward-looking statement in light of new information or future events, except as otherwise required by law. Forward-looking statements involve inherent risks and uncertainties, most of which are difficult to predict and are generally beyond each company’s control. These risks and uncertainties include, but are not limited to, the risk that the bb2121 product candidate will not be successfully developed, approved or commercialized in relapsed/refractory multiple myeloma, or the risk that the bb2121 product candidate will be safe and efficacious in other disease settings. Actual results or outcomes may differ materially from those implied by the forward-looking statements as a result of the impact of a number of factors, many of which are discussed in more detail in the section entitled “Risk Factors”  of the Annual Report on Form 10-K and other reports of each company filed with the Securities and Exchange Commission.

 

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For bluebird:

Investors:

Manisha Pai, 617-245-2107

mpai@bluebirdbio.com

 

Media:

Elizabeth Pingpank, 617-914-8736

epingpank@bluebirdbio.com

 

For Celgene:

Investors:

Patrick Flanigan, 908-673-9969

pflanigan@celgene.com

 

Media:

Greg Geissman, 908-673-9854

ggeissman@celgene.com