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Modeling early retinal development with human embryonic and induced pluripotent stem cells

机译:用人类胚胎干细胞和诱导性多能干细胞模拟早期视网膜发育

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摘要

Human pluripotent stem cells have the potential to provide comprehensive model systems for the earliest stages of human ontogenesis. To serve in this capacity, these cells must undergo a targeted, stepwise differentiation process that follows a normal developmental timeline. Here we demonstrate the ability of both human embryonic stem cells (hESCs) and induced pluripotent stem (iPS) cells to meet these requirements for human retinogenesis. Upon differentiation, hESCs initially yielded a highly enriched population of early eye field cells. Thereafter, a subset of cells acquired features of advancing retinal differentiation in a sequence and time course that mimicked in vivo human retinal development. Application of this culture method to a human iPS cell line also generated retina-specific cell types at comparable times in vitro. Lastly, altering endogenous signaling during differentiation affected lineage-specific gene expression in a manner consistent with established mechanisms of early neural and retinal cell fate determination. These findings should aid in the investigation of the molecular events governing retinal specification from human pluripotent stem cells.
机译:人多能干细胞有潜力为人类本体发育的最早阶段提供全面的模型系统。为了以这种能力发挥作用,这些细胞必须经历遵循正常发育时间表的靶向,逐步分化过程。在这里,我们证明了人类胚胎干细胞(hESCs)和诱导性多能干(iPS)细胞都能满足人类视网膜发生的这些要求。分化后,hESC最初产生了高度富集的早期眼场细胞。此后,一部分细胞以模仿体内人视网膜发育的序列和时间过程获得了促进视网膜分化的特征。将该培养方法应用于人iPS细胞系,在体外可比较的时间也产生了视网膜特异性细胞类型。最后,在分化过程中改变内源性信号以与早期神经和视网膜细胞命运确定的既定机制一致的方式影响谱系特异性基因表达。这些发现应有助于调查人类多能干细胞控制视网膜规格的分子事件。

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