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连接蛋白蛋白质-蛋白质相互作用的多样性:新出现的作用

Diversity in protein-protein interactions of connexins: emerging roles.

作者信息

Hervé Jean-Claude, Bourmeyster Nicolas, Sarrouilhe Denis

机构信息

UMR CNRS no. 6558, Faculté de Sciences Fondamentales et Appliquées, Université de Poitiers, Pôle Biologie-Santé, 86022 Poitiers Cedex, France.

出版信息

Biochim Biophys Acta. 2004 Mar 23;1662(1-2):22-41. doi: 10.1016/j.bbamem.2003.10.022.

Abstract

Gap junctions, specialised membrane structures that mediate cell-to-cell communication in almost all tissues, are composed of channel-forming integral membrane proteins termed connexins. The activity of these intercellular channels is closely regulated, particularly by intramolecular modifications as phosphorylations of proteins by protein kinases, which appear to regulate the gap junction at several levels, including assembly of channels in the plasma membrane, connexin turnover as well as directly affecting the opening and closure ("gating") of channels. The regulation of membrane channels by protein phosphorylation/dephosphorylation processes commonly requires the formation of a multiprotein complex, where pore-forming subunits bind to auxiliary proteins (e.g. scaffolding proteins, catalytic and regulatory subunits), that play essential roles in channel localisation and activity, linking signalling enzymes, substrates and effectors into a structure frequently anchored to the cytoskeleton. The present review summarises the up-to-date progress regarding the proteins capable of interacting or at least of co-localising with connexins and their functional importance.

摘要

间隙连接是一种特殊的膜结构,几乎在所有组织中介导细胞间通讯,由称为连接蛋白的形成通道的整合膜蛋白组成。这些细胞间通道的活性受到密切调控,特别是通过分子内修饰,如蛋白激酶对蛋白质的磷酸化,这似乎在多个水平上调节间隙连接,包括质膜中通道的组装、连接蛋白的周转以及直接影响通道的开放和关闭(“门控”)。蛋白质磷酸化/去磷酸化过程对膜通道的调节通常需要形成多蛋白复合物,其中形成孔的亚基与辅助蛋白(如支架蛋白、催化和调节亚基)结合,这些辅助蛋白在通道定位和活性中起重要作用,将信号酶、底物和效应器连接成一个经常锚定在细胞骨架上的结构。本综述总结了关于能够与连接蛋白相互作用或至少共定位的蛋白质及其功能重要性的最新进展。

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