Long-Term Safety and Efficacy of Factor IX Gene Therapy in Hemophilia B

Amit Nathwani; Ulreke M. Reiss; Edward G. D. Tuddenham; Cecilia Rosales; Pratima Chowdary; Jenny McIntosh; Marco Della Peruta; Elsa Lhériteau; Nishal Patel; Deepak B. Thimiri Govinda Raj; Anne Riddell; Jun Pie; Savita Rangarajan; David Bevan; Michael Recht; Yu‐Min Shen; Kathleen G. Halka; Etiena Basner‐Tschakarjan; Federico Mingozzi; Katherine A. High; James A. Allay; Mark A. Kay; Catherine Y. Ng; Junfang Zhou; Maria Cancio; Christopher L. Morton; John T. Gray; Deo Kumar Srivastava; Arthur W. Nienhuis; Andrew M. Davidoff

doi:10.1056/nejmoa1407309

Long-Term Safety and Efficacy of Factor IX Gene Therapy in Hemophilia B

Amit Nathwani(The Royal Free Hospital), Ulreke M. Reiss, Edward G. D. Tuddenham(University College London), Cecilia Rosales(University College London), Pratima Chowdary(University College London), Jenny McIntosh(London Cancer), Marco Della Peruta(University College London), Elsa Lhériteau(Cancer Institute (WIA)), Nishal Patel(London Cancer), Deepak B. Thimiri Govinda Raj(University College London), Anne Riddell(The Royal Free Hospital), Jun Pie(University College London), Savita Rangarajan(Basingstoke and North Hampshire Hospital), David Bevan(St. Thomas Hospital), Michael Recht(Oregon Health & Science University), Yu‐Min Shen(The University of Texas Southwestern Medical Center), Kathleen G. Halka(Baylor Scott & White Health), Etiena Basner‐Tschakarjan(Children's Hospital of Philadelphia), Federico Mingozzi(Children's Hospital of Philadelphia), Katherine A. High(Children's Hospital of Philadelphia), James A. Allay(St. Jude Children's Research Hospital), Mark A. Kay(Stanford University), Catherine Y. Ng, Junfang Zhou, Maria Cancio, Christopher L. Morton, John T. Gray, Deo Kumar Srivastava, Arthur W. Nienhuis, Andrew M. Davidoff

New England Journal of Medicine

November 20, 2014

10.1056/nejmoa1407309

Cited by 1,248Open Access

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Abstract

BACKGROUND: In patients with severe hemophilia B, gene therapy that is mediated by a novel self-complementary adeno-associated virus serotype 8 (AAV8) vector has been shown to raise factor IX levels for periods of up to 16 months. We wanted to determine the durability of transgene expression, the vector dose-response relationship, and the level of persistent or late toxicity. METHODS: We evaluated the stability of transgene expression and long-term safety in 10 patients with severe hemophilia B: 6 patients who had been enrolled in an initial phase 1 dose-escalation trial, with 2 patients each receiving a low, intermediate, or high dose, and 4 additional patients who received the high dose (2×10(12) vector genomes per kilogram of body weight). The patients subsequently underwent extensive clinical and laboratory monitoring. RESULTS: A single intravenous infusion of vector in all 10 patients with severe hemophilia B resulted in a dose-dependent increase in circulating factor IX to a level that was 1 to 6% of the normal value over a median period of 3.2 years, with observation ongoing. In the high-dose group, a consistent increase in the factor IX level to a mean (±SD) of 5.1±1.7% was observed in all 6 patients, which resulted in a reduction of more than 90% in both bleeding episodes and the use of prophylactic factor IX concentrate. A transient increase in the mean alanine aminotransferase level to 86 IU per liter (range, 36 to 202) occurred between week 7 and week 10 in 4 of the 6 patients in the high-dose group but resolved over a median of 5 days (range, 2 to 35) after prednisolone treatment. CONCLUSIONS: In 10 patients with severe hemophilia B, the infusion of a single dose of AAV8 vector resulted in long-term therapeutic factor IX expression associated with clinical improvement. With a follow-up period of up to 3 years, no late toxic effects from the therapy were reported. (Funded by the National Heart, Lung, and Blood Institute and others; ClinicalTrials.gov number, NCT00979238.).

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