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Function of human pluripotent stem cell-derived photoreceptor progenitors in blind mice

机译:人多能干细胞源性光感受器祖细胞在盲小鼠中的功能

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Photoreceptor degeneration due to retinitis pigmentosa (RP) is a primary cause of inherited retinal blindness. Photoreceptor cell-replacement may hold the potential for repair in a completely degenerate retina by reinstating light sensitive cells to form connections that relay information to downstream retinal layers. This study assessed the therapeutic potential of photoreceptor progenitors derived from human embryonic and induced pluripotent stem cells (ESCs and iPSCs) using a protocol that is suitable for future clinical trials. ESCs and iPSCs were cultured in four specific stages under defined conditions, resulting in generation of a near-homogeneous population of photoreceptor-like progenitors. Following transplantation into mice with end-stage retinal degeneration, these cells differentiated into photoreceptors and formed a cell layer connected with host retinal neurons. Visual function was partially restored in treated animals, as evidenced by two visual behavioral tests. Furthermore, the magnitude of functional improvement was positively correlated with the number of engrafted cells. Similar efficacy was observed using either ESCs or iPSCs as source material. These data validate the potential of human pluripotent stem cells for photoreceptor replacement therapies aimed at photoreceptor regeneration in retinal disease.
机译:色素性视网膜炎(RP)引起的感光细胞变性是遗传性视网膜失明的主要原因。通过恢复光敏细胞以形成将信息中继到下游视网膜层的连接,感光细胞的置换可以保持在完全退化的视网膜中修复的潜力。这项研究使用适合未来临床试验的方案评估了源自人类胚胎和诱导多能干细胞(ESC和iPSC)的光感受器祖细胞的治疗潜力。 ESC和iPSC在确定的条件下分四个特定阶段进行培养,从而产生了近乎均匀的感光受体样祖细胞群。移植到视网膜末期变性小鼠后,这些细胞分化为感光细胞,并形成与宿主视网膜神经元连接的细胞层。两次视觉行为测试证明,治疗动物的视觉功能已部分恢复。此外,功能改善的程度与移植细胞的数量呈正相关。使用ESC或iPSC作为源材料,观察到相似的功效。这些数据验证了人类多能干细胞在视网膜疾病中针对光感受器再生的光感受器替代疗法的潜力。

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