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成年人类眼睛中具有干细胞特征的 Müller 胶质细胞和睫状上皮的神经发生和增殖能力的差异。

Differences between the neurogenic and proliferative abilities of Müller glia with stem cell characteristics and the ciliary epithelium from the adult human eye.

机构信息

Division of Ocular Biology and Therapeutics, UCL Institute of Ophthalmology and Moorfields Eye Hospital, 11 Bath Street, London EC1V 9EL, UK.

出版信息

Exp Eye Res. 2011 Dec;93(6):852-61. doi: 10.1016/j.exer.2011.09.015. Epub 2011 Oct 5.

Abstract

Much controversy has arisen on the nature and sources of stem cells in the adult human retina. Whilst ciliary epithelium has been thought to constitute a source of neural stem cells, a population of Müller glia in the neural retina has also been shown to exhibit neurogenic characteristics. This study aimed to compare the neurogenic and proliferative abilities between these two major cell populations. It also examined whether differences exist between the pigmented and non-pigmented ciliary epithelium (CE) from the adult human eye. On this basis, Müller glia with stem cell characteristics and pigmented and non-pigmented CE were isolated from human neural retina and ciliary epithelium respectively. Expression of glial, epithelial and neural progenitor markers was examined in these cells following culture under adherent and non-adherent conditions and treatments to induce neural differentiation. Unlike pigmented CE which did not proliferate, non-pigmented CE cells exhibited limited proliferation in vitro, unless epidermal growth factor (EGF) was present in the culture medium to prolong their survival. In contrast, Müller glial stem cells (MSC) cultured as adherent monolayers reached confluence within a few weeks and continued to proliferative indefinitely in the absence of EGF. Both MSC and non-pigmented CE expressed markers of neural progenitors, including SOX2, PAX6, CHX10 and NOTCH. Nestin, a neural stem cell marker, was only expressed by MSC. Non-pigmented CE displayed epithelial morphology, limited photoreceptor gene expression and stained strongly for pigmented epithelial markers upon culture with neural differentiation factors. In contrast, MSC adopted neural morphology and expressed markers of retinal ganglion cells and photoreceptors when cultured under similar conditions. This study provides the first demonstration that pigmented CE possess different proliferative abilities from non-pigmented CE. It also showed that although non-pigmented CE express genes of retinal progenitors, they do not differentiate into neurons in vitro, as that seen with Müller glia that proliferate indefinitely in vitro and that acquire markers of retinal neurons in culture under neural differentiation protocols. From these observations it is possible to suggest that Müller glia that express markers of neural progenitors and become spontaneously immortalized in vitro constitute a potential source of retinal neurons for transplantation studies and fulfil the characteristics of true stem cells due to their proliferative and neurogenic ability.

摘要

成人视网膜中干细胞的性质和来源存在很多争议。虽然睫状上皮被认为是神经干细胞的来源,但神经视网膜中的 Müller 胶质细胞也表现出神经发生的特征。本研究旨在比较这两种主要细胞群体的神经发生和增殖能力。它还检查了成人眼睛的色素和非色素睫状上皮 (CE) 之间是否存在差异。在此基础上,分别从人神经视网膜和睫状上皮中分离出具有干细胞特征的 Müller 胶质细胞和色素及非色素 CE。在贴壁和非贴壁培养条件以及诱导神经分化的处理下,检测这些细胞中神经胶质、上皮和神经祖细胞标记物的表达。与不增殖的色素 CE 不同,非色素 CE 细胞在体外增殖能力有限,除非培养基中存在表皮生长因子 (EGF) 以延长其存活。相比之下,作为贴壁单层培养的 Müller 胶质干细胞 (MSC) 在数周内达到汇合,并在没有 EGF 的情况下无限期增殖。MSC 和非色素 CE 均表达神经前体细胞标记物,包括 SOX2、PAX6、CHX10 和 NOTCH。神经干细胞标记物巢蛋白仅由 MSC 表达。非色素 CE 培养时有上皮形态,有限的光感受器基因表达,并在与神经分化因子一起培养时强烈染色色素上皮标记物。相比之下,MSC 在类似条件下培养时采用神经形态并表达视网膜节细胞和光感受器的标记物。本研究首次证明色素 CE 具有与非色素 CE 不同的增殖能力。它还表明,尽管非色素 CE 表达视网膜祖细胞的基因,但它们在体外不会分化为神经元,这与在体外无限增殖并在神经分化方案下培养时获得视网膜神经元标记物的 Müller 胶质细胞不同。从这些观察结果中可以推测,表达神经祖细胞标记物并在体外自发永生化的 Müller 胶质细胞构成了用于移植研究的视网膜神经元的潜在来源,并且由于其增殖和神经发生能力,符合真正干细胞的特征。

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