Completion of phase 2b trial of etranacogene dezaparvovec gene therapy in patients with hemophilia B over 5 years.

IF 7.1 1区医学 Q1 HEMATOLOGY Blood advances Pub Date : 2025-07-22 DOI:10.1182/bloodadvances.2024015291

Annette von Drygalski, Esteban Gomez, Adam Giermasz, Giancarlo Castaman, Nigel S Key, Susan U Lattimore, Frank W G Leebeek, Wolfgang A Miesbach, Michael Recht, Paul E Monahan, Sandra Le Quellec, Steven W Pipe

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Abstract

Abstract: Etranacogene dezaparvovec (CSL222, formerly AMT-061) is a recombinant adeno-associated virus serotype 5 (AAV5) vector containing the highly active factor IX (FIX) Padua variant controlled by a liver-specific promoter. This phase 2b, open-label, single-dose, single-arm, multicenter trial evaluated the efficacy and safety of etranacogene dezaparvovec. Three adult participants with severe or moderately severe hemophilia B (FIX ≤2%) and AAV5-neutralizing antibodies received a single IV dose (2 × 1013 genome copies per kg) of etranacogene dezaparvovec. The primary end point of FIX activity ≥5 IU/dL at 6 weeks was met (mean, 30.6 IU/dL). Secondary end points included bleed frequency, FIX concentrate use, and adverse events. Here, we report the end-of-study 5-year outcomes. After administration, mean (range) FIX activity increased to 40.8 IU/dL (31.3-50.2) at year 1 and was maintained at 45.7 IU/dL (39.0-51.2) at year 5. Mean annualized bleeding rate (all bleeds) was 0.14 for the cumulative follow-up period years 0 to 5. Two participants had 5 bleed-free years after treatment. Per protocol, 1 participant received episodic FIX replacement therapy after treatment for elective surgeries, 2 bleeding episodes, and 2 single self-administered infusions for unreported reasons. All participants discontinued and remained free of FIX prophylaxis. During the 5-year study period, there were no clinically significant elevations in liver enzymes, requirement for steroids, FIX inhibitor development, thrombotic complications, or late-emergent safety events in any participant. Five years after administration, etranacogene dezaparvovec was effective in adults with hemophilia B with a favorable safety profile. Participants are eligible to participate in an extension study (ClinicalTrials.gov identifier: NCT05962398) for 10-year additional follow-up. This trial was registered at www.clinicaltrials.gov as #NCT03489291.

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完成etranacogene dezaparvovec基因治疗5年以上B型血友病患者的2b期试验。

Etranacogene dezaparvovec（CSL222，原名 AMT-061）是一种重组腺相关病毒血清型 5（AAV5）载体，含有由肝脏特异性启动子控制的高活性因子 IX（FIX）帕多瓦变体。这项 2b 期、开放标签、单剂量、单臂、多中心试验评估了 etranacogene dezaparvovec 的疗效和安全性。所有参与者（n=3）均为成年人，患有重度或中度血友病 B（FIX ≤2%）和 AAV5 中和抗体。参与者接受了单剂量（2×1013 基因组拷贝/公斤）的 etranacogene dezaparvovec 静脉注射。6周时FIX活性≥5 IU/dL的主要终点达到（平均30.6IU/dL）。次要终点包括出血频率、FIX浓缩液的使用和不良事件。我们在此报告研究结束后的 5 年结果。给药后，第 1 年的平均 FIX 活性（范围）增至 40.8 IU/dL (31.3-50.2)，第 5 年维持在 45.7 IU/dL (39.0-51.2)。在第 0-5 年的累计随访期间，平均 ABR（所有出血）为 0.14。两名参与者在治疗后 5 年无出血。根据方案，一名参与者在治疗后因择期手术、两次出血和两次未报告原因的单次自我输注而接受了偶发性 FIX 替代治疗。所有参与者都停止了 FIX 预防治疗，并一直未再使用。在为期 5 年的研究期间，没有任何参与者出现肝酶临床显著升高、需要使用类固醇、出现 FIX 抑制剂、血栓并发症或后期突发安全事件。用药五年后，etranacogene dezaparvovec 对成年 B 型血友病患者有效，且安全性良好。参与者有资格参加一项延长10年随访的扩展研究（NCT05962398）。ClinicalTrials.gov Identifier：NCT03489291。

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来源期刊

Blood advances Medicine-Hematology

CiteScore

12.70

自引率

2.70%

发文量

840

期刊介绍： Blood Advances, a semimonthly medical journal published by the American Society of Hematology, marks the first addition to the Blood family in 70 years. This peer-reviewed, online-only, open-access journal was launched under the leadership of founding editor-in-chief Robert Negrin, MD, from Stanford University Medical Center in Stanford, CA, with its inaugural issue released on November 29, 2016. Blood Advances serves as an international platform for original articles detailing basic laboratory, translational, and clinical investigations in hematology. The journal comprehensively covers all aspects of hematology, including disorders of leukocytes (both benign and malignant), erythrocytes, platelets, hemostatic mechanisms, vascular biology, immunology, and hematologic oncology. Each article undergoes a rigorous peer-review process, with selection based on the originality of the findings, the high quality of the work presented, and the clarity of the presentation.