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多极阶段与神经元迁移紊乱。

The multipolar stage and disruptions in neuronal migration.

作者信息

LoTurco Joseph J, Bai Jilin

机构信息

Department of Physiology and Neurobiology, 75 North Eagleville Road U-3156, University of Connecticut, Storrs, CT 06269, USA.

Department of Physiology and Neurobiology, 75 North Eagleville Road U-3156, University of Connecticut, Storrs, CT 06269, USA.

出版信息

Trends Neurosci. 2006 Jul;29(7):407-413. doi: 10.1016/j.tins.2006.05.006. Epub 2006 May 19.

Abstract

The genetic basis is now known for several disorders of neuronal migration in the developing cerebral cortex. Identification of the cellular processes mediated by the implicated genes is revealing crucial stages of neuronal migration and has the potential to reveal common cellular causes of neuronal migration disorders. We hypothesize that a newly recognized morphological stage of neuronal migration, the multipolar stage, is vulnerable and is disrupted in several disorders of neocortical development. The multipolar stage occurs as bipolar progenitor cells become radially migrating neurons. Several studies using in utero electroporation and RNAi have revealed that transition out of the multipolar stage depends on the function of filamin A, LIS1 and DCX. Mutations in the genes encoding these proteins in humans cause distinct neuronal migration disorders, including periventricular nodular heterotopia, subcortical band heterotopia and lissencephaly. The multipolar stage therefore seems to be a critical point of migration control and a vulnerable target for disruption of neocortical development. This review is part of the INMED/TINS special issue "Nature and nurture in brain development and neurological disorders", based on presentations at the annual INMED/TINS symposium (http://inmednet.com/).

摘要

目前已知发育中的大脑皮质中几种神经元迁移障碍的遗传基础。对相关基因介导的细胞过程的鉴定,正在揭示神经元迁移的关键阶段,并有可能揭示神经元迁移障碍的常见细胞病因。我们推测,一种新认识到的神经元迁移形态学阶段——多极阶段,是脆弱的,并且在几种新皮质发育障碍中会受到破坏。多极阶段发生在双极祖细胞转变为径向迁移神经元之时。几项利用子宫内电穿孔和RNA干扰技术的研究表明,从多极阶段过渡出来取决于细丝蛋白A、LIS1和双皮质素(DCX)的功能。人类中编码这些蛋白质的基因突变会导致不同的神经元迁移障碍,包括室管膜下结节性异位、皮质下带状异位和无脑回畸形。因此,多极阶段似乎是迁移控制的关键点,也是新皮质发育受破坏的脆弱靶点。本综述是INMED/TINS特刊“大脑发育和神经疾病中的先天与后天”的一部分,基于在年度INMED/TINS研讨会上的发言(http://inmednet.com/)。

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