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表皮生长因子受体过表达诱导的视网膜细胞命运变化。

Changes in retinal cell fate induced by overexpression of EGF receptor.

作者信息

Lillien L

机构信息

Department of Anatomy and Neurobiology, Medical College of Pennsylvania, Philadelphia 19072, USA.

出版信息

Nature. 1995 Sep 14;377(6545):158-62. doi: 10.1038/377158a0.

Abstract

The differentiation of multipotential progenitor cells in the vertebrate retina into photoreceptors, neurons and glial cells is regulated in part by cell-cell signalling. Transforming growth factor (TGF)-alpha is one of the extracellular signals implicated in the control of several aspects of retinal development, including proliferation and cell fate. The way cells interpret pleiotropic signals such as TGF-alpha is influenced by the level of expression of epidermal growth factor receptor (EGF-R) in some cell lines. To address the influence of receptor level on responses of retinal progenitor cells to TGF-alpha, additional copies of EGF-Rs were introduced in vitro and in vivo with a retrovirus. Normally in vitro, low concentrations of TGF-alpha stimulated proliferation whereas high concentrations biased choice of cell fate, inhibiting differentiation into rod photoreceptors while promoting differentiation into Müller glial cells. We report here that introduction of extra EGF-Rs into progenitor cells in vitro reduced the concentration of TGF-alpha required for changes in rod and Müller cell differentiation but did not enhance proliferation. Introduction of extra EGF-Rs in vivo increased the proportion of clones that contained Müller glial cells, suggesting that receptor level is normally limiting. These findings demonstrate that responsiveness to extracellular signals during development can be modulated by the introduction of additional receptors, and suggest that the level of expression of receptors for these signals contributes to the regulation of cell fate.

摘要

脊椎动物视网膜中多能祖细胞向光感受器、神经元和神经胶质细胞的分化部分受细胞间信号传导调控。转化生长因子(TGF)-α是参与视网膜发育多个方面控制的细胞外信号之一,包括增殖和细胞命运。在某些细胞系中,细胞解读诸如TGF-α这类多效信号的方式受表皮生长因子受体(EGF-R)表达水平的影响。为了研究受体水平对视网膜祖细胞对TGF-α反应的影响,利用逆转录病毒在体外和体内导入额外的EGF-R拷贝。通常在体外,低浓度的TGF-α刺激增殖,而高浓度则偏向细胞命运选择,抑制向视杆光感受器的分化,同时促进向米勒神经胶质细胞的分化。我们在此报告,在体外向祖细胞中导入额外的EGF-R可降低视杆细胞和米勒细胞分化变化所需的TGF-α浓度,但不会增强增殖。在体内导入额外的EGF-R增加了含有米勒神经胶质细胞的克隆比例,表明受体水平通常是受限的。这些发现表明,发育过程中对细胞外信号的反应性可通过导入额外受体来调节,并表明这些信号受体的表达水平有助于细胞命运的调控。

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