AAV mini-dystrophin gene therapy for Duchenne muscular dystrophy: a phase 1b trial

IF 58.7 1区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Nature Medicine Pub Date : 2025-06-27 DOI:10.1038/s41591-025-03750-3

Russell J. Butterfield, Perry B. Shieh, Huihua Li, Michael Binks, Tara G. McDonnell, Kelly A. Ryan, Marielle Delnomdedieu, Beth A. Belluscio, Srividya Neelakantan, Daniel I. Levy, Pamela F. Schwartz, Edward C. Smith

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Abstract

Gene therapy represents a promising approach for Duchenne muscular dystrophy (DMD), a rare X-linked genetic muscle disease. Fordadistrogene movaparvovec (PF-06939926) is an adeno-associated virus serotype 9 gene therapy containing a miniaturized dystrophin being developed for DMD, which aims to restore functional protein to muscle. We present 1-year data from ambulatory and nonambulatory participants in a phase 1b, multicenter, single-arm, open-label trial. Pediatric ambulatory male participants with a genetic DMD diagnosis and receiving stable glucocorticoids received a single intravenous low-dose (n = 3) or high-dose (n = 16) fordadistrogene movaparvovec. The primary endpoint was safety and tolerability at 1 year after dosing. In the ambulatory group, mean ± s.d. age at dosing was 8.6 ± 1.6 years. The most common treatment-emergent adverse events in the ambulatory group were vomiting (n = 15), nausea (n = 10), thrombocytopenia (n = 9), pyrexia (n = 9), decreased appetite (n = 8), fatigue (n = 7) and headache (n = 7). Three treatment-related serious adverse events occurred after dosing (dehydration, acute kidney injury, thrombocytopenia; all resolved within 15 days). In a small nonambulatory group (n = 3), mean ± s.d. age at dosing was 15.1 ± 1.0 years. The most common treatment-emergent adverse events were nausea (n = 3), vomiting (n = 3) and headache (n = 3); two severe treatment-related adverse events (hemolytic uremic syndrome and fatal cardiogenic shock) were observed. In the high-dose ambulatory group, the secondary endpoint of mini-dystrophin quantification showed robust expression. Mean (95% confidence interval) percent of mini-dystrophin-positive fibers for baseline, 2 months and 1 year were 0.1% (0.1–0.2), 20.3% (12.2–29.3) and 34.8% (21.1–49.8), respectively. At the 1-year time point of primary completion, fordadistrogene movaparvovec demonstrated an acceptable safety profile in the ambulatory population. Larger trials are needed to assess the efficacy of the gene therapy in DMD. ClinicalTrials.gov registration no. NCT03362502.

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AAV微型肌营养不良蛋白基因治疗杜氏肌营养不良症：1b期试验

杜氏肌营养不良症（DMD）是一种罕见的x连锁遗传性肌肉疾病，基因治疗是一种很有前途的方法。Fordadistrogene movaparvovec （PF-06939926）是一种腺相关病毒血清型9基因疗法，含有一种小型化的肌营养不良蛋白，旨在恢复肌肉的功能蛋白。我们提供了一项1b期、多中心、单臂、开放标签试验中门诊和非门诊参与者的1年数据。诊断为遗传性DMD并接受稳定糖皮质激素治疗的儿科门诊男性受试者接受单次低剂量（n = 3）或高剂量（n = 16）的莫帕洛韦静脉注射。主要终点是给药后1年的安全性和耐受性。门诊组平均±s.d。给药时年龄8.6±1.6岁。门诊组最常见的治疗不良事件为呕吐（n = 15）、恶心（n = 10）、血小板减少（n = 9）、发热（n = 9）、食欲下降（n = 8）、疲劳（n = 7）和头痛（n = 7）。给药后发生3个与治疗相关的严重不良事件(脱水、急性肾损伤、血小板减少；均在15天内解决)。在少数非卧床组（n = 3）中，平均±s.d。给药时年龄15.1±1.0岁。最常见的治疗不良事件是恶心（n = 3）、呕吐（n = 3）和头痛（n = 3）；观察到两个严重的治疗相关不良事件（溶血性尿毒症综合征和致死性心源性休克）。在高剂量门诊组中，mini-dystrophin定量的次要终点显示出强劲的表达。基线、2个月和1年微肌营养不良蛋白阳性纤维的平均（95%置信区间）百分比分别为0.1%（0.1-0.2）、20.3%（12.2-29.3）和34.8%（21.1-49.8）。在初步完成的1年时间点上，福达消孕莫帕洛韦在门诊人群中显示出可接受的安全性。需要更大规模的试验来评估基因疗法对DMD的疗效。ClinicalTrials.gov注册号：NCT03362502。

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来源期刊

Nature Medicine 医学-生化与分子生物学

CiteScore

100.90

自引率

0.70%

发文量

525

审稿时长

1 months

期刊介绍： Nature Medicine is a monthly journal publishing original peer-reviewed research in all areas of medicine. The publication focuses on originality, timeliness, interdisciplinary interest, and the impact on improving human health. In addition to research articles, Nature Medicine also publishes commissioned content such as News, Reviews, and Perspectives. This content aims to provide context for the latest advances in translational and clinical research, reaching a wide audience of M.D. and Ph.D. readers. All editorial decisions for the journal are made by a team of full-time professional editors. Nature Medicine consider all types of clinical research, including: -Case-reports and small case series -Clinical trials, whether phase 1, 2, 3 or 4 -Observational studies -Meta-analyses -Biomarker studies -Public and global health studies Nature Medicine is also committed to facilitating communication between translational and clinical researchers. As such, we consider “hybrid” studies with preclinical and translational findings reported alongside data from clinical studies.