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成体纤毛上皮细胞,曾被鉴定为具有视网膜修复潜力的视网膜干细胞,未能分化为新的杆状光感受器。

Adult ciliary epithelial cells, previously identified as retinal stem cells with potential for retinal repair, fail to differentiate into new rod photoreceptors.

机构信息

Developmental Biology Unit, Institute of Child Health, University College London, London, UK.

出版信息

Stem Cells. 2010 Jun;28(6):1048-59. doi: 10.1002/stem.423.

Abstract

The ciliary margin in lower vertebrates is a site of continual retinal neurogenesis and a stem cell niche. By contrast, the human eye ceases retinal neuron production before birth and loss of photoreceptors during life is permanent and a major cause of blindness. The discovery of a proliferative cell population in the ciliary epithelium (CE) of the adult mammalian eye, designated retinal stem cells, raised the possibility that these cells could help to restore sight by replacing lost photoreceptors. We previously demonstrated the feasibility of photoreceptor transplantation using cells from the developing retina. CE cells could provide a renewable source of photoreceptors for transplantation. Several laboratories reported that these cells generate new photoreceptors, whereas a recent report questioned the existence of retinal stem cells. We used Nrl.gfp transgenic mice that express green fluorescent protein in rod photoreceptors to assess definitively the ability of CE cells to generate new photoreceptors. We report that CE cells expanded in monolayer cultures, lose pigmentation, and express a subset of eye field and retinal progenitor cell markers. Simultaneously, they continue to express some markers characteristic of differentiated CE and typically lack a neuronal morphology. Previously reported photoreceptor differentiation conditions used for CE cells, as well as conditions used to differentiate embryonic retinal progenitor cells (RPCs) and embryonic stem cell-derived RPCs, do not effectively activate the Nrl-regulated photoreceptor differentiation program. Therefore, we conclude that CE cells lack potential for photoreceptor differentiation and would require reprogramming to be useful as a source of new photoreceptors.

摘要

在低等脊椎动物中,纤毛缘是视网膜神经发生和干细胞龛的部位。相比之下,人类眼睛在出生前就停止了视网膜神经元的产生,并且感光细胞的丧失是永久性的,是失明的主要原因。在成年哺乳动物眼睛的睫状上皮(CE)中发现了一个增殖细胞群,被指定为视网膜干细胞,这使得人们有可能通过替代丢失的感光细胞来恢复视力。我们之前已经证明了使用来自发育中的视网膜的细胞进行光感受器移植的可行性。CE 细胞可以为移植提供可再生的感光细胞来源。几个实验室报告称这些细胞产生新的感光细胞,而最近的一份报告对视网膜干细胞的存在提出了质疑。我们使用 Nrl.gfp 转基因小鼠,该小鼠在杆状光感受器中表达绿色荧光蛋白,以明确评估 CE 细胞产生新感光细胞的能力。我们报告说,CE 细胞在单层培养中扩增,失去色素沉着,并表达眼部和视网膜祖细胞标记物的一部分。同时,它们继续表达一些特征性分化 CE 的标记物,通常缺乏神经元形态。先前报道的用于 CE 细胞的光感受器分化条件,以及用于分化胚胎视网膜祖细胞(RPC)和胚胎干细胞衍生的 RPC 的条件,不能有效地激活 Nrl 调控的光感受器分化程序。因此,我们得出结论,CE 细胞缺乏光感受器分化的潜力,需要重新编程才能用作新感光细胞的来源。

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