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神经元-胶质细胞在发育和成年肠神经系统中的相互作用。

Neuron-Glia Interaction in the Developing and Adult Enteric Nervous System.

机构信息

Institute of Anatomy, Medical Faculty Carl Gustav Carus, TechnischeUniversität Dresden School of Medicine, 01307 Dresden, Germany.

出版信息

Cells. 2020 Dec 31;10(1):47. doi: 10.3390/cells10010047.

Abstract

The enteric nervous system (ENS) constitutes the largest part of the peripheral nervous system. In recent years, ENS development and its neurogenetic capacity in homeostasis and allostasishave gained increasing attention. Developmentally, the neural precursors of the ENS are mainly derived from vagal and sacral neural crest cell portions. Furthermore, Schwann cell precursors, as well as endodermal pancreatic progenitors, participate in ENS formation. Neural precursorsenherite three subpopulations: a bipotent neuron-glia, a neuronal-fated and a glial-fated subpopulation. Typically, enteric neural precursors migrate along the entire bowel to the anal end, chemoattracted by glial cell-derived neurotrophic factor (GDNF) and endothelin 3 (EDN3) molecules. During migration, a fraction undergoes differentiation into neurons and glial cells. Differentiation is regulated by bone morphogenetic proteins (BMP), Hedgehog and Notch signalling. The fully formed adult ENS may react to injury and damage with neurogenesis and gliogenesis. Nevertheless, the origin of differentiating cells is currently under debate. Putative candidates are an embryonic-like enteric neural progenitor population, Schwann cell precursors and transdifferentiating glial cells. These cells can be isolated and propagated in culture as adult ENS progenitors and may be used for cell transplantation therapies for treating enteric aganglionosis in Chagas and Hirschsprung's diseases.

摘要

肠神经系统(ENS)构成了外周神经系统的最大部分。近年来,ENS 的发展及其在体内平衡和适应中的神经遗传能力引起了越来越多的关注。在发育过程中,ENS 的神经前体细胞主要来自迷走神经和骶神经嵴细胞部分。此外,施万细胞前体细胞以及内胚层胰腺祖细胞参与 ENS 的形成。神经前体细胞继承了三个亚群:一个双能神经元-胶质细胞、一个神经元命运和一个胶质命运亚群。通常,肠神经前体细胞沿着整个肠道迁移到肛门末端,被胶质细胞衍生的神经营养因子(GDNF)和内皮素 3(EDN3)分子趋化。在迁移过程中,一部分分化为神经元和神经胶质细胞。分化受骨形态发生蛋白(BMP)、Hedgehog 和 Notch 信号的调节。完全形成的成年 ENS 可能会对损伤和损伤做出反应,产生神经发生和神经胶质发生。然而,分化细胞的来源目前仍存在争议。潜在的候选者是类似胚胎的肠神经前体细胞群、施万细胞前体细胞和转分化的神经胶质细胞。这些细胞可以在体外作为成年 ENS 祖细胞进行分离和培养,并可能用于细胞移植治疗恰加斯病和先天性巨结肠的肠无神经节症。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5fa/7823798/38eccc8349dc/cells-10-00047-g001.jpg

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