AAV1-hOTOF gene therapy for autosomal recessive deafness 9: a single-arm trial

The Lancet Pub Date : 2024-01-24 DOI:10.1016/s0140-6736(23)02874-x

Jun Lv, Hui Wang, Xiaoting Cheng, Yuxin Chen, Daqi Wang, Longlong Zhang, Qi Cao, Honghai Tang, Shaowei Hu, Kaiyu Gao, Mengzhao Xun, Jinghan Wang, Zijing Wang, Biyun Zhu, Chong Cui, Ziwen Gao, Luo Guo, Sha Yu, Luoying Jiang, Yanbo Yin, Yilai Shu

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Abstract

Background

Autosomal recessive deafness 9, caused by mutations of the OTOF gene, is characterised by congenital or prelingual, severe-to-complete, bilateral hearing loss. However, no pharmacological treatment is currently available for congenital deafness. In this Article, we report the safety and efficacy of gene therapy with an adeno-associated virus (AAV) serotype 1 carrying a human OTOF transgene (AAV1-hOTOF) as a treatment for children with autosomal recessive deafness 9.

Methods

This single-arm, single-centre trial enrolled children (aged 1–18 years) with severe-to-complete hearing loss and confirmed mutations in both alleles of OTOF, and without bilateral cochlear implants. A single injection of AAV1-hOTOF was administered into the cochlea through the round window. The primary endpoint was dose-limiting toxicity at 6 weeks after injection. Auditory function and speech were assessed by appropriate auditory perception evaluation tools. All analyses were done according to the intention-to-treat principle. This trial is registered with Chinese Clinical Trial Registry, ChiCTR2200063181, and is ongoing.

Findings

Between Oct 19, 2022, and June 9, 2023, we screened 425 participants for eligibility and enrolled six children for AAV1-hOTOF gene therapy (one received a dose of 9 × 10¹¹ vector genomes [vg] and five received 1·5 × 10¹² vg). All participants completed follow-up visits up to week 26. No dose-limiting toxicity or serious adverse events occurred. In total, 48 adverse events were observed; 46 (96%) were grade 1–2 and two (4%) were grade 3 (decreased neutrophil count in one participant). Five children had hearing recovery, shown by a 40–57 dB reduction in the average auditory brainstem response (ABR) thresholds at 0·5–4·0 kHz. In the participant who received the 9 × 10¹¹ vg dose, the average ABR threshold was improved from greater than 95 dB at baseline to 68 dB at 4 weeks, 53 dB at 13 weeks, and 45 dB at 26 weeks. In those who received 1·5 × 10¹² AAV1-hOTOF, the average ABR thresholds changed from greater than 95 dB at baseline to 48 dB, 38 dB, 40 dB, and 55 dB in four children with hearing recovery at 26 weeks. Speech perception was improved in participants who had hearing recovery.

Interpretation

AAV1-hOTOF gene therapy is safe and efficacious as a novel treatment for children with autosomal recessive deafness 9.

Funding

National Natural Science Foundation of China, National Key R&D Program of China, Science and Technology Commission of Shanghai Municipality, and Shanghai Refreshgene Therapeutics.

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AAV1-HOTOF基因疗法治疗常染色体隐性耳聋9：单臂试验

背景常染色体隐性遗传性耳聋 9 由 OTOF 基因突变引起，其特征是先天性或舌前、严重至完全性双侧听力损失。然而，目前还没有治疗先天性耳聋的药物。在这篇文章中，我们报告了用携带人类 OTOF 转基因（AAV1-hOTOF）的腺相关病毒（AAV）血清型 1 进行基因治疗，治疗常染色体隐性耳聋患儿的安全性和有效性。试验通过圆窗将 AAV1-hOTOF 单次注入耳蜗。主要终点是注射后6周的剂量限制毒性。听觉功能和言语能力通过适当的听觉感知评估工具进行评估。所有分析均按照意向治疗原则进行。研究结果在2022年10月19日至2023年6月9日期间，我们筛选了425名符合条件的参与者，并招募了6名儿童接受AAV1-hOTOF基因治疗（1名接受了9×1011载体基因组[vg]的剂量，5名接受了1-5×1012 vg的剂量）。所有参与者均完成了第 26 周前的随访。没有发生剂量限制性毒性或严重不良事件。共观察到 48 例不良反应，其中 46 例（96%）为 1-2 级，2 例（4%）为 3 级（一名参与者中性粒细胞计数减少）。五名儿童的听力得到恢复，表现为 0-5-4-0 kHz 时平均听性脑干反应（ABR）阈值降低了 40-57 dB。在接受 9 × 1011 vg 剂量治疗的儿童中，ABR 平均阈值从基线时的大于 95 dB 降至 4 周时的 68 dB、13 周时的 53 dB 和 26 周时的 45 dB。在接受 1-5 × 1012 AAV1-hOTOF 治疗的儿童中，4 名儿童的平均 ABR阈值从基线时的大于 95 分贝降至 48 分贝、38 分贝、40 分贝和 55 分贝，26 周时听力恢复。AAV1-hOTOF基因疗法作为常染色体隐性耳聋患儿的一种新型治疗方法，安全有效。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Lancet

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