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哺乳动物端脑的细胞命运特化

Cell fate specification in the mammalian telencephalon.

作者信息

Guillemot François

机构信息

National Institute for Medical Research, Mill Hill, London NW74LL, UK.

出版信息

Prog Neurobiol. 2007 Sep;83(1):37-52. doi: 10.1016/j.pneurobio.2007.02.009. Epub 2007 Mar 7.

Abstract

A fundamental feature of neural development in vertebrates is that different cell types are generated in a precise temporal sequence, first neurons, followed by oligodendrocytes and astrocytes. The mechanisms underlying these remarkable changes in progenitor fate during development are not well understood, but are thought to include both changes in the intrinsic properties of neural progenitors and changes in their signaling environment. I discuss the mechanisms that control the specification of neuronal, astroglial and oligodendroglial fates, focusing on the mammalian telencephalon, one of the most extensively used models to study neural specification mechanisms in vertebrates. I first consider the multiple extracellular signals that have been implicated in neural fate specification. Their roles are often complex, with the same signals having different effects at different developmental stages, and different signaling pathways interacting extensively. The selection of a particular cell fate ultimately results from the integration of multiple signals. Signaling pathways regulate cell fates by modulating the expression and activity of numerous transcription factors in neural stem cells. I discuss how transcription factors also act in a combinatorial manner to determine progenitor fates, with individual factors promoting the generation of one or two cell types and repressing alternative fate(s). Finally, I discuss the many levels of regulation involved in preventing premature astrocyte differentiation during neurogenesis, and later on in controlling the transition from neurogenesis to gliogenesis.

摘要

脊椎动物神经发育的一个基本特征是,不同类型的细胞按照精确的时间顺序产生,首先是神经元,随后是少突胶质细胞和星形胶质细胞。发育过程中祖细胞命运发生这些显著变化的潜在机制尚未完全了解,但据认为包括神经祖细胞内在特性的变化及其信号环境的变化。我将讨论控制神经元、星形胶质细胞和少突胶质细胞命运特化的机制,重点是哺乳动物端脑,这是研究脊椎动物神经特化机制最广泛使用的模型之一。我首先考虑与神经命运特化有关的多种细胞外信号。它们的作用通常很复杂,相同的信号在不同的发育阶段有不同的影响,而且不同的信号通路广泛相互作用。特定细胞命运的选择最终源于多种信号的整合。信号通路通过调节神经干细胞中众多转录因子的表达和活性来调节细胞命运。我将讨论转录因子如何也以组合方式起作用来决定祖细胞命运,单个因子促进一种或两种细胞类型的产生并抑制其他命运。最后,我将讨论在神经发生过程中防止星形胶质细胞过早分化以及随后控制从神经发生向胶质发生转变所涉及的多个调控层面。

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