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The newt reprograms mature RPE cells into a unique multipotent state for retinal regeneration

机译:t将成熟的RPE细胞重新编程为独特的多能状态以实现视网膜再生

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摘要

The reprogramming of retinal pigment epithelium (RPE) cells in the adult newt immediately after retinal injury is an area of active research for the study of retinal disorders and regeneration. We demonstrate here that unlike embryonic/larval retinal regeneration, adult newt RPE cells are not directly reprogrammed into retinal stem/progenitor cells; instead, they are programmed into a unique state of multipotency that is similar to the early optic vesicle (embryo) but preserves certain adult characteristics. These cells then differentiate into two populations from which the prospective-neural retina and -RPE layers are formed with the correct polarity. Furthermore, our findings provide insight into the similarity between these unique multipotent cells in newts and those implicated in retinal disorders, such as proliferative vitreoretinopathy, in humans. These findings provide a foundation for biomedical approaches that aim to induce retinal self-regeneration for the treatment of RPE-mediated retinal disorders.
机译:视网膜损伤后成年new的视网膜色素上皮(RPE)细胞重编程是研究视网膜疾病和再生的活跃研究领域。我们在这里证明,与胚胎/幼虫的视网膜再生不同,成年new RPE细胞不会直接重编程为视网膜干/祖细胞。取而代之的是,它们被编程为一种独特的多能状态,该状态类似于早期的视神经泡(胚胎),但保留了某些成人特征。然后,这些细胞分化为两个种群,由此形成具有正确极性的前瞻性神经视网膜和-RPE层。此外,我们的发现提供了对new中这些独特的多能细胞与人类中涉及视网膜疾病(如增生性玻璃体视网膜病变)的细胞之间相似性的见识。这些发现为旨在诱导视网膜自我再生以治疗RPE介导的视网膜疾病的生物医学方法提供了基础。

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