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体内局部基因治疗隐性营养不良型大疱性表皮松解症:一项 1 期和 2 期临床试验。

In vivo topical gene therapy for recessive dystrophic epidermolysis bullosa: a phase 1 and 2 trial.

机构信息

Program in Epithelial Biology and Department of Dermatology, Stanford University School of Medicine, Stanford, CA, USA.

Krystal Biotech, Pittsburgh, PA, USA.

出版信息

Nat Med. 2022 Apr;28(4):780-788. doi: 10.1038/s41591-022-01737-y. Epub 2022 Mar 28.

DOI:10.1038/s41591-022-01737-y
PMID:35347281
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9018416/
Abstract

Recessive dystrophic epidermolysis bullosa (RDEB) is a lifelong genodermatosis associated with blistering, wounding, and scarring caused by mutations in COL7A1, the gene encoding the anchoring fibril component, collagen VII (C7). Here, we evaluated beremagene geperpavec (B-VEC), an engineered, non-replicating COL7A1 containing herpes simplex virus type 1 (HSV-1) vector, to treat RDEB skin. B-VEC restored C7 expression in RDEB keratinocytes, fibroblasts, RDEB mice and human RDEB xenografts. Subsequently, a randomized, placebo-controlled, phase 1 and 2 clinical trial (NCT03536143) evaluated matched wounds from nine RDEB patients receiving topical B-VEC or placebo repeatedly over 12 weeks. No grade 2 or above B-VEC-related adverse events or vector shedding or tissue-bound skin immunoreactants were noted. HSV-1 and C7 antibodies sometimes presented at baseline or increased after B-VEC treatment without an apparent impact on safety or efficacy. Primary and secondary objectives of C7 expression, anchoring fibril assembly, wound surface area reduction, duration of wound closure, and time to wound closure following B-VEC treatment were met. A patient-reported pain-severity secondary outcome was not assessed given the small proportion of wounds treated. A global assessment secondary endpoint was not pursued due to redundancy with regard to other endpoints. These studies show that B-VEC is an easily administered, safely tolerated, topical molecular corrective therapy promoting wound healing in patients with RDEB.

摘要

隐性营养不良型大疱性表皮松解症(RDEB)是一种终生遗传性皮肤病,与 COL7A1 基因突变有关,COL7A1 基因编码锚定纤维成分 VII 型胶原(C7)。在这里,我们评估了 beceragene geperpavec(B-VEC),这是一种工程化的、非复制的含有单纯疱疹病毒 1 型(HSV-1)载体的 COL7A1 基因,用于治疗 RDEB 皮肤。B-VEC 恢复了 RDEB 角质形成细胞、成纤维细胞、RDEB 小鼠和人 RDEB 异种移植物中的 C7 表达。随后,一项随机、安慰剂对照、1 期和 2 期临床试验(NCT03536143)评估了 9 名 RDEB 患者接受局部 B-VEC 或安慰剂治疗 12 周后匹配的伤口。未观察到 2 级或以上与 B-VEC 相关的不良事件、载体脱落或组织结合的皮肤免疫反应物。HSV-1 和 C7 抗体有时在基线时出现或在 B-VEC 治疗后增加,但对安全性或疗效没有明显影响。C7 表达、锚定纤维组装、伤口表面积减少、伤口闭合持续时间和 B-VEC 治疗后伤口闭合时间的主要和次要目标都得到了满足。由于治疗的伤口比例较小,未评估 B-VEC 治疗后患者报告的疼痛严重程度次要结局。由于其他终点与次要终点存在冗余,因此未追求全球评估终点。这些研究表明,B-VEC 是一种易于管理、安全耐受的局部分子矫正治疗方法,可促进 RDEB 患者的伤口愈合。

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