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一个调控视网膜神经节细胞特化的bHLH转录网络。

A bHLH transcriptional network regulating the specification of retinal ganglion cells.

作者信息

Matter-Sadzinski Lidia, Puzianowska-Kuznicka Monika, Hernandez Julio, Ballivet Marc, Matter Jean-Marc

机构信息

University of Lausanne, Eye Hospital Jules Gonin and Institute for Research in Ophthalmology, 15 avenue de France, 1004 Lausanne, Switzerland.

出版信息

Development. 2005 Sep;132(17):3907-21. doi: 10.1242/dev.01960. Epub 2005 Aug 3.

Abstract

In the developing retina, the production of ganglion cells is dependent on the proneural proteins NGN2 and ATH5, whose activities define stages along the pathway converting progenitors into newborn neurons. Crossregulatory interactions between NGN2, ATH5 and HES1 maintain the uncommitted status of ATH5-expressing cells during progenitor patterning, and later on regulate the transition from competence to cell fate commitment. Prior to exiting the cell cycle, a subset of progenitors is selected from the pool of ATH5-expressing cells to go through a crucial step in the acquisition of a definitive retinal ganglion cell fate. The selected cells are those in which the upregulation of NGN2, the downregulation of HES1 and the autostimulation of ATH5 are coordinated with the progression of progenitors through the last cell cycle. This coordinated pattern initiates the transcription of ganglion cell-specific traits and determines the size of the ganglion cell population.

摘要

在发育中的视网膜中,神经节细胞的产生依赖于神经前体蛋白NGN2和ATH5,它们的活性定义了祖细胞转化为新生神经元过程中的各个阶段。NGN2、ATH5和HES1之间的交叉调节相互作用在祖细胞模式形成过程中维持表达ATH5细胞的未分化状态,随后调节从感受态到细胞命运决定的转变。在退出细胞周期之前,从表达ATH5的细胞池中选择一部分祖细胞,使其经历获得确定的视网膜神经节细胞命运的关键步骤。所选细胞是那些NGN2上调、HES1下调以及ATH5自激活与祖细胞通过最后一个细胞周期的进程相协调的细胞。这种协调模式启动神经节细胞特异性特征的转录,并决定神经节细胞群体的大小。

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