输血依赖型非β0/β0基因型β-地中海贫血的基因治疗:Beti-cel 的首次实际应用经验。

IF 7.4 1区 医学 Q1 HEMATOLOGY
Adil Mirza, Mona-Lisa Ritsert, Gloria Tao, Himal Thakar, Stephan Lobitz, Sabine Heine, Leila Koscher, Matthias Dürken, Anita Schmitt, Michael Schmitt, Petra Pavel, Sascha Laier, Donate Jakoby, Johann Greil, Joachim B Kunz, Andreas Kulozik
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引用次数: 0

摘要

针对输血依赖型β地中海贫血的基因添加和编辑策略作为潜在的治愈性治疗方案,其疗效和安全性已得到研究证实。我们报告了 betibeglogene autotemcel(beti-cel;ZYNTEGLO™)在欧洲 2020 年 1 月至 2022 年 3 月有效许可期间的首次实际应用,用于年龄≥ 12 岁、无 β0/β0 基因型、无人类白细胞抗原(HLA)匹配的兄弟姐妹供体的患者。在 15 名经过筛选的患者中,有 4 人出于生育和安全考虑而选择放弃,2 人因明显的肝淤血而被排除,1 人因血液透析采集失败而被排除。8名患者在接受beti-cel治疗后接受了布舒芬骨髓溶解治疗,所有患者均在8至59天内实现了独立输血,治疗后血红蛋白水平在11.3至19.3 g/dL之间。没有出现死亡病例,但急性毒性与已知的丁胺苯磺吡啶影响相同。由于3名患者体内存在HLA抗体,治疗后的血小板管理面临挑战。截至第24个月的监测结果显示,3名女性患者和5名男性患者中的2名出现了垂体-性腺内分泌功能障碍。此外,我们还观察到了意想不到的治疗后遗症:1 名患者出现了多血症,但无法用已知的遗传或后天机制来解释;1 名患者在治疗后出现了抑郁和焦虑,无法重返工作岗位;1 名患者出现了疲劳,严重影响了生活质量和工作能力。这一实际经验证实了beti-cel的疗效和安全性,并提供了在实际治疗过程中观察到的不良反应信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Gene Therapy in Transfusion-Dependent Non-β0/β0 Genotype β-Thalassemia: First Real-World Experience of Beti-cel.

Gene addition and editing strategies for transfusion-dependent β-thalassemia have gained momentum as potentially curative treatment options, with studies showcasing their efficacy and safety. We report the first real-world application of betibeglogene autotemcel (beti-cel; ZYNTEGLO™) during its period of active license in Europe from January 2020 to March 2022 for patients aged ≥ 12 years without a β0/β0 genotype and without a human leukocyte antigen (HLA)-matched sibling donor, before beti-cel marketing authorization was withdrawn by its holder due to non-safety reasons. Among 15 screened patients, 4 opted out for fertility and safety concerns, 2 were excluded because of marked hepatic siderosis, and 1 had apheresis collection failure. Eight patients received beti-cel post busulfan myeloablative conditioning, all achieving transfusion independence within 8 to 59 days with posttreatment hemoglobin levels ranging from 11.3 to 19.3 g/dL. No deaths occurred, but acute toxicity mirrored busulfan's known effects. Posttreatment platelet management faced challenges due to HLA-antibodies in 3 patients. Monitoring up to Month 24 revealed pituitary-gonadal endocrine dysfunction in all 3 female and in 2 of 5 male patients. Additionally, we observed unexpected posttreatment sequelae: 1 patient developed polycythemia that could not be explained by known genetic or acquired mechanisms, 1 patient developed posttreatment depression and anxiety prohibiting her from returning to work, and 1 patient developed fatigue severely compromising both quality of life and work capacity. This real-world experience corroborates beti-cel's efficacy and safety and provides information on adverse events observed during real-world use of the therapy.

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来源期刊
Blood advances
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.
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