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一种用于临床前测试的多功能激光诱导猪眼外视网膜和脉络膜变性模型。

A versatile laser-induced porcine model of outer retinal and choroidal degeneration for preclinical testing.

机构信息

National Eye Institute (NEI), NIH, Bethesda, Maryland, USA.

McPherson Eye Research Institute and Waisman Center, and.

出版信息

JCI Insight. 2023 Jun 8;8(11):e157654. doi: 10.1172/jci.insight.157654.

Abstract

Over 30 million people worldwide suffer from untreatable vision loss and blindness associated with childhood-onset and age-related eye diseases caused by photoreceptor (PR), retinal pigment epithelium (RPE), and choriocapillaris (CC) degeneration. Recent work suggests that RPE-based cell therapy may slow down vision loss in late stages of age-related macular degeneration (AMD), a polygenic disease induced by RPE atrophy. However, accelerated development of effective cell therapies is hampered by the lack of large-animal models that allow testing safety and efficacy of clinical doses covering the human macula (20 mm2). We developed a versatile pig model to mimic different types and stages of retinal degeneration. Using an adjustable power micropulse laser, we generated varying degrees of RPE, PR, and CC damage and confirmed the damage by longitudinal analysis of clinically relevant outcomes, including analyses by adaptive optics and optical coherence tomography/angiography, along with automated image analysis. By imparting a tunable yet targeted damage to the porcine CC and visual streak - with a structure similar to the human macula - this model is optimal for testing cell and gene therapies for outer retinal diseases including AMD, retinitis pigmentosa, Stargardt, and choroideremia. The amenability of this model to clinically relevant imaging outcomes will facilitate faster translation to patients.

摘要

全世界有超过 3000 万人患有无法治愈的视力丧失和失明,这些疾病与儿童期和老年相关的眼部疾病有关,这些疾病是由光感受器 (PR)、视网膜色素上皮 (RPE) 和脉络膜毛细血管 (CC) 变性引起的。最近的研究表明,基于 RPE 的细胞疗法可能会减缓老年黄斑变性 (AMD) 的晚期视力丧失,AMD 是一种多基因疾病,由 RPE 萎缩引起。然而,由于缺乏能够测试覆盖人类黄斑(20mm²)的临床剂量的安全性和有效性的大型动物模型,有效的细胞疗法的快速发展受到了阻碍。我们开发了一种多功能猪模型来模拟不同类型和阶段的视网膜变性。我们使用可调功率微脉冲激光产生不同程度的 RPE、PR 和 CC 损伤,并通过对包括自适应光学和光相干断层扫描/血管造影在内的临床相关结果进行纵向分析,以及自动图像分析,来确认损伤。通过对猪的 CC 和视觉纹状体施加可调节但靶向的损伤——其结构类似于人类黄斑——该模型是测试包括 AMD、色素性视网膜炎、Stargardt 病和脉络膜黑变病等外视网膜疾病的细胞和基因疗法的最佳选择。该模型对临床相关成像结果的适应性将促进更快地转化为患者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a70/10393234/ed53c0bd7c8a/jciinsight-8-157654-g175.jpg

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