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首页> 外文期刊>Brazilian Journal of Medical and Biological Research >Regulation of gap junctions by protein phosphorylation
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Regulation of gap junctions by protein phosphorylation

机译:通过蛋白质磷酸化调节间隙连接

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Gap junctions are constituted by intercellular channels and provide a pathway for transfer of ions and small molecules between adjacent cells of most tissues. The degree of intercellular coupling mediated by gap junctions depends on the number of gap junction channels and their activity may be a function of the state of phosphorylation of connexins, the structural subunit of gap junction channels. Protein phosphorylation has been proposed to control intercellular gap junctional communication at several steps from gene expression to protein degradation, including translational and post-translational modification of connexins (i.e., phosphorylation of the assembled channel acting as a gating mechanism) and assembly into and removal from the plasma membrane. Several connexins contain sites for phosphorylation for more than one protein kinase. These consensus sites vary between connexins and have been preferentially identified in the C-terminus. Changes in intercellular communication mediated by protein phosphorylation are believed to control various physiological tissue and cell functions as well as to be altered under pathological conditions.
机译:间隙连接由细胞间通道构成,并提供了在大多数组织的相邻细胞之间转移离子和小分子的途径。间隙连接介导的细胞间偶联程度取决于间隙连接通道的数量,它们的活性可能是连接蛋白磷酸化状态的函数,连接蛋白是间隙连接通道的结构亚基。已经提出蛋白质磷酸化可控制从基因表达到蛋白质降解的多个步骤的细胞间间隙连接通讯,包括连接蛋白的翻译和翻译后修饰(即,作为门控机制的组装通道的磷酸化)以及组装进去和从中去除质膜几种连接蛋白包含一个以上蛋白激酶的磷酸化位点。这些共有位点在连接蛋白之间有所不同,并已在C端得到了优先鉴定。据信由蛋白质磷酸化介导的细胞间通讯的变化控制了各种生理组织和细胞功能,并且在病理条件下发生了改变。

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