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通过光感受器移植逆转终末期视网膜变性并恢复视觉功能。

Reversal of end-stage retinal degeneration and restoration of visual function by photoreceptor transplantation.

机构信息

Nuffield Laboratory of Ophthalmology, Nuffield Department of Clinical Neurosciences, University of Oxford, Oxford OX3 9DU, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2013 Jan 15;110(3):1101-6. doi: 10.1073/pnas.1119416110. Epub 2013 Jan 3.

Abstract

One strategy to restore vision in retinitis pigmentosa and age-related macular degeneration is cell replacement. Typically, patients lose vision when the outer retinal photoreceptor layer is lost, and so the therapeutic goal would be to restore vision at this stage of disease. It is not currently known if a degenerate retina lacking the outer nuclear layer of photoreceptor cells would allow the survival, maturation, and reconnection of replacement photoreceptors, as prior studies used hosts with a preexisting outer nuclear layer at the time of treatment. Here, using a murine model of severe human retinitis pigmentosa at a stage when no host rod cells remain, we show that transplanted rod precursors can reform an anatomically distinct and appropriately polarized outer nuclear layer. A trilaminar organization was returned to rd1 hosts that had only two retinal layers before treatment. The newly introduced precursors were able to resume their developmental program in the degenerate host niche to become mature rods with light-sensitive outer segments, reconnecting with host neurons downstream. Visual function, assayed in the same animals before and after transplantation, was restored in animals with zero rod function at baseline. These observations suggest that a cell therapy approach may reconstitute a light-sensitive cell layer de novo and hence repair a structurally damaged visual circuit. Rather than placing discrete photoreceptors among preexisting host outer retinal cells, total photoreceptor layer reconstruction may provide a clinically relevant model to investigate cell-based strategies for retinal repair.

摘要

一种恢复色素性视网膜炎和年龄相关性黄斑变性视力的策略是细胞替代。通常,当外视网膜光感受器层丢失时,患者会失去视力,因此治疗目标将是在疾病的这个阶段恢复视力。目前还不知道是否缺乏光感受器细胞的外核层的变性视网膜是否允许替代光感受器的存活、成熟和重新连接,因为之前的研究在治疗时使用了预先存在外核层的宿主。在这里,我们使用一种严重的人类色素性视网膜炎的小鼠模型,在没有宿主杆细胞的阶段,我们表明移植的杆前体细胞可以重新形成解剖上不同且适当极化的外核层。在治疗前只有两层视网膜的 rd1 宿主中,出现了三层结构。新引入的前体细胞能够在退化的宿主龛位中恢复其发育程序,成为具有光敏感外节的成熟杆状细胞,并与下游的宿主神经元重新连接。在移植前后对同一动物进行的视觉功能检测显示,在基线时没有杆状细胞功能的动物的视觉功能得到了恢复。这些观察结果表明,细胞治疗方法可能会从头重新构成一个光敏感的细胞层,从而修复结构受损的视觉回路。与将离散的光感受器放置在预先存在的宿主外视网膜细胞之间不同,总光感受器层重建可能为研究基于细胞的视网膜修复策略提供一个临床相关的模型。

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