Retinoschisin gene therapy in photoreceptors, Müller glia or all retinal cells in the Rs1h−/− mouse

生物 视网膜 视网膜劈裂 视网膜 分泌物 穆勒胶质细胞 细胞生物学 病毒载体 遗传增强 感光细胞 基因 视网膜脱离 遗传学 神经科学 干细胞 内分泌学 生物化学 祖细胞 重组DNA
作者
Leah C. Byrne,Bilge Esin Öztürk,Trevor Lee,Cécile Fortuny,Meike Visel,Deniz Dalkara,David V. Schaffer,John G. Flannery
出处
期刊:Gene Therapy [Springer Nature]
卷期号:21 (6): 585-592 被引量:73
标识
DOI:10.1038/gt.2014.31
摘要

X-linked retinoschisis, a disease characterized by splitting of the retina, is caused by mutations in the retinoschisin gene, which encodes a putative secreted cell adhesion protein. Currently, there is no effective treatment for retinoschisis, though viral vector-mediated gene replacement therapies offer promise. We used intravitreal delivery of three different AAV vectors to target delivery of the RS1 gene to Müller glia, photoreceptors or multiple cell types throughout the retina. Müller glia radially span the entire retina, are accessible from the vitreous, and remain intact throughout progression of the disease. However, photoreceptors, not glia, normally secrete retinoschisin. We compared the efficacy of rescue mediated by retinoschisin secretion from these specific subtypes of retinal cells in the Rs1h−/− mouse model of retinoschisis. Our results indicate that all three vectors deliver the RS1 gene, and that several cell types can secrete retinoschisin, leading to transport of the protein across the retina. The greatest long-term rescue was observed when photoreceptors produce retinoschisin. Similar rescue was observed with photoreceptor-specific or generalized expression, although photoreceptor secretion may contribute to rescue in the latter case. These results collectively point to the importance of cell targeting and appropriate vector choice in the success of retinal gene therapies.

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