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人类诱导多能干细胞协调的眼部发育和角膜功能的恢复。

Co-ordinated ocular development from human iPS cells and recovery of corneal function.

机构信息

Department of Stem Cells and Applied Medicine, Osaka University Graduate School of Medicine, Suita, Osaka 565-0871, Japan.

Department of Ophthalmology, Osaka University Graduate School of Medicine, Suita, Osaka 565-0871, Japan.

出版信息

Nature. 2016 Mar 17;531(7594):376-80. doi: 10.1038/nature17000. Epub 2016 Mar 9.

DOI:10.1038/nature17000
PMID:26958835
Abstract

The eye is a complex organ with highly specialized constituent tissues derived from different primordial cell lineages. The retina, for example, develops from neuroectoderm via the optic vesicle, the corneal epithelium is descended from surface ectoderm, while the iris and collagen-rich stroma of the cornea have a neural crest origin. Recent work with pluripotent stem cells in culture has revealed a previously under-appreciated level of intrinsic cellular self-organization, with a focus on the retina and retinal cells. Moreover, we and others have demonstrated the in vitro induction of a corneal epithelial cell phenotype from pluripotent stem cells. These studies, however, have a single, tissue-specific focus and fail to reflect the complexity of whole eye development. Here we demonstrate the generation from human induced pluripotent stem cells of a self-formed ectodermal autonomous multi-zone (SEAM) of ocular cells. In some respects the concentric SEAM mimics whole-eye development because cell location within different zones is indicative of lineage, spanning the ocular surface ectoderm, lens, neuro-retina, and retinal pigment epithelium. It thus represents a promising resource for new and ongoing studies of ocular morphogenesis. The approach also has translational potential and to illustrate this we show that cells isolated from the ocular surface ectodermal zone of the SEAM can be sorted and expanded ex vivo to form a corneal epithelium that recovers function in an experimentally induced animal model of corneal blindness.

摘要

眼睛是一个复杂的器官,具有高度专业化的组成组织,这些组织来源于不同的原始细胞谱系。例如,视网膜由神经外胚层通过视泡发育而来,角膜上皮来自表面外胚层,而虹膜和富含胶原的角膜基质则起源于神经嵴。最近,在培养的多能干细胞中进行的研究揭示了以前被低估的内在细胞自我组织水平,重点是视网膜和视网膜细胞。此外,我们和其他人已经证明了从多能干细胞体外诱导角膜上皮细胞表型。然而,这些研究只有一个组织特异性的焦点,未能反映整个眼睛发育的复杂性。在这里,我们从人诱导多能干细胞中生成了一个自我形成的外胚层自主多区(SEAM)的眼部细胞。在某些方面,同心的 SEAM 模拟了整个眼睛的发育,因为不同区域内的细胞位置表明了谱系,跨越了眼表面外胚层、晶状体、神经视网膜和视网膜色素上皮。因此,它代表了眼部形态发生的新的和正在进行的研究的有前途的资源。该方法也具有转化潜力,为了说明这一点,我们展示了可以从 SEAM 的眼表面外胚层区分离和体外扩增细胞,以形成角膜上皮,在角膜盲的动物模型中恢复功能。

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IGF-1 Signaling Plays an Important Role in the Formation of Three-Dimensional Laminated Neural Retina and Other Ocular Structures From Human Embryonic Stem Cells.胰岛素样生长因子-1信号通路在人胚胎干细胞形成三维层状神经视网膜及其他眼部结构过程中发挥重要作用。
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