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Pals1 是主要的调节因子,调节周围神经中上皮样极化和髓鞘延伸。

Pals1 is a major regulator of the epithelial-like polarization and the extension of the myelin sheath in peripheral nerves.

机构信息

Institute of Cell Biology, Department of Biology, Swiss Federal Institute of Technology Zürich, CH-8093 Zürich, Switzerland.

出版信息

J Neurosci. 2010 Mar 17;30(11):4120-31. doi: 10.1523/JNEUROSCI.5185-09.2010.

Abstract

Diameter, organization, and length of the myelin sheath are important determinants of the nerve conduction velocity, but the basic molecular mechanisms that control these parameters are only partially understood. Cell polarization is an essential feature of differentiated cells, and relies on a set of evolutionarily conserved cell polarity proteins. We investigated the molecular nature of myelin sheath polarization in connection with the functional role of the cell polarity protein pals1 (Protein Associated with Lin Seven 1) during peripheral nerve myelin sheath extension. We found that, in regard to epithelial polarity, the Schwann cell outer abaxonal domain represents a basolateral-like domain, while the inner adaxonal domain and Schmidt-Lanterman incisures form an apical-like domain. Silencing of pals1 in myelinating Schwann cells in vivo resulted in a severe reduction of myelin sheath thickness and length. Except for some infoldings, the structure of compact myelin was not fundamentally affected, but cells produced less myelin turns. In addition, pals1 is required for the normal polarized localization of the vesicular markers sec8 and syntaxin4, and for the distribution of E-cadherin and myelin proteins PMP22 and MAG at the plasma membrane. Our data show that the polarity protein pals1 plays an essential role in the radial and longitudinal extension of the myelin sheath, likely involving a functional role in membrane protein trafficking. We conclude that regulation of epithelial-like polarization is a critical determinant of myelin sheath structure and function.

摘要

髓鞘的直径、组织和长度是神经传导速度的重要决定因素,但控制这些参数的基本分子机制仅部分被理解。细胞极化是分化细胞的一个基本特征,依赖于一组进化上保守的细胞极性蛋白。我们研究了髓鞘极化的分子本质,以及细胞极性蛋白 pals1(与 Lin Seven 1 相关的蛋白)在周围神经髓鞘延伸过程中的功能作用。我们发现,就上皮细胞极性而言,施万细胞的外轴突背侧域代表基底外侧样域,而内轴突腹侧域和施密特-兰伯特切迹形成顶端样域。在体内沉默髓鞘形成施万细胞中的 pals1 导致髓鞘厚度和长度严重减少。除了一些内褶外,致密髓鞘的结构没有根本影响,但细胞产生的髓鞘匝数较少。此外,pals1 对于囊泡标记物 sec8 和 syntaxin4 的正常极化定位,以及 E-钙粘蛋白和髓鞘蛋白 PMP22 和 MAG 在质膜上的分布是必需的。我们的数据表明,极性蛋白 pals1 在髓鞘的径向和纵向延伸中发挥着重要作用,可能在膜蛋白运输中发挥功能作用。我们得出结论,上皮样极化的调节是髓鞘结构和功能的关键决定因素。

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