用于移植手术的诱导多能干细胞衍生角膜上皮:在日本进行的单臂、开放标签、首次人体介入研究

Takeshi Soma, Yoshinori Oie, Hiroshi Takayanagi, Shoko Matsubara, Tomomi Yamada, Masaki Nomura, Yu Yoshinaga, Kazuichi Maruyama, Atsushi Watanabe, Kayo Takashima, Zaixing Mao, Andrew J Quantock, Ryuhei Hayashi, Kohji Nishida
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引用次数: 0

摘要

背景角膜边缘的角膜上皮干细胞缺失对视力有严重影响,角膜边缘干细胞缺失症(LSCD)的病理表现难以治疗。据我们所知,我们在这里报告了世界上首次使用从人类诱导多能干细胞(iPSCs)中提取的角膜上皮细胞片治疗LSCD的情况。这些患者包括一名 44 岁的特发性 LSCD 女性患者(患者 1)、一名 66 岁的眼部粘膜丘疹病男性患者(患者 2)、一名 72 岁的特发性 LSCD 男性患者(患者 3)和一名 39 岁的中毒性表皮坏死女性患者(患者 4)。异体人类 iPSC 衍生的角膜上皮细胞片(iCEPSs)被移植到受影响的眼睛上。这是在两组HLA不匹配的手术中依次进行的,其中患者1和2接受了低剂量环孢素,而患者3和4则没有接受环孢素。主要结果是安全性,通过不良事件来确定。在为期 52 周的随访期间以及额外的 1 年安全监测期内,对这些不良事件进行了持续监测。此外,还记录了反映疗效的次要结果。该研究已在 UMIN(UMIN000036539)注册,并已完成。研究结果患者于 2019 年 6 月 17 日至 2020 年 11 月 16 日期间入组。在为期52周的随访期间,我们共发生了26起不良事件(包括18起轻度和1起中度治疗眼部事件,以及7起轻度非眼部事件),其中9起记录在为期1年的额外安全监测期内。在整个 2 年的观察期内,未发生肿瘤发生或临床排斥等严重不良事件。52 周时,次要疗效指标显示,所有接受治疗的眼睛的疾病阶段均有所改善,矫正远距离视力有所提高,角膜不透明有所减轻。角膜上皮缺损、主观症状、生活质量问卷评分和角膜新生血管大多有所改善或保持不变。总体而言,1 号和 2 号患者的疗效优于 3 号和 4 号患者。计划进行更大规模的临床试验,以进一步研究该手术的疗效。资金来源:日本医学研究开发机构、日本文部科学省、英国生物技术与生物科学研究委员会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Induced pluripotent stem-cell-derived corneal epithelium for transplant surgery: a single-arm, open-label, first-in-human interventional study in Japan

Background

The loss of corneal epithelial stem cells from the limbus at the edge of the cornea has severe consequences for vision, with the pathological manifestations of a limbal stem-cell deficiency (LSCD) difficult to treat. Here, to the best of our knowledge, we report the world's first use of corneal epithelial cell sheets derived from human induced pluripotent stem cells (iPSCs) to treat LSCD.

Methods

This non-randomised, single-arm, clinical study involved four eyes of four patients with LSCD at the Department of Ophthalmology, Osaka University Hospital. They comprised a woman aged 44 years with idiopathic LSCD (patient 1), a man aged 66 years with ocular mucous membrane pemphigoid (patient 2), a man aged 72 years with idiopathic LSCD (patient 3), and a woman aged 39 years with toxic epidermal necrosis (patient 4). Allogeneic human iPSC-derived corneal epithelial cell sheets (iCEPSs) were transplanted onto affected eyes. This was done sequentially in two sets of HLA-mismatched surgeries, with patients 1 and 2 receiving low-dose cyclosporin and patients 3 and 4 not. The primary outcome measure was safety, ascertained by adverse events. These were monitored continuously throughout the 52-week follow-up period, and during an additional 1-year safety monitoring period. Secondary outcomes, reflective of efficacy, were also recorded. This study is registered with UMIN, UMIN000036539 and is complete.

Findings

Patients were enrolled between June 17, 2019 and Nov 16, 2020. We had 26 adverse events during the 52-week follow-up period (consisting of 18 mild and one moderate event in treated eyes, and seven mild non-ocular events), with nine recorded in the additional 1-year safety monitoring period. No serious adverse events, such as tumourigenesis or clinical rejection, occurred during the whole 2-year observational period. At 52 weeks, secondary measures of efficacy showed that the disease stage had improved, corrected distance visual acuity was enhanced, and corneal opacification had diminished in all treated eyes. Corneal epithelial defects, subjective symptoms, quality-of-life questionnaire scores and corneal neovascularisation mostly improved or were unchanged. Overall, the beneficial efficacy outcomes achieved for patients 1 and 2 were better than those achieved for patients 3 and 4.

Interpretation

iCEPS transplantation for LSCD was found to be safe throughout the study period. A larger clinical trial is planned to further investigate the efficacy of the procedure.

Funding

The Japan Agency for Medical Research and Development, the Ministry of Education, Culture, Sports, Science, and Technology—Japan, and the UK Biotechnology and Biological Sciences Research Council.
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