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Intracellular trafficking pathways of Cx43 gap junction channels

机译:CX43间隙连接通道的细胞内运输途径

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摘要

Abstract Gap Junction (GJ) channels, including the most common Connexin 43 (Cx43), have fundamental roles in excitable tissues by facilitating rapid transmission of action potentials between adjacent cells. For instance, synchronization during each heartbeat is regulated by these ion channels at the cardiomyocyte cell-cell border. Cx43 protein has a short half-life, and rapid synthesis and timely delivery of those proteins to particular subdomains are crucial for the cellular organization of gap junctions and maintenance of intracellular coupling. Impairment in gap junction trafficking contributes to dangerous complications in diseased hearts such as the arrhythmias of sudden cardiac death. Of recent interest are the protein-protein interactions with the Cx43 carboxy-terminus. These interactions have significant impact on the full length Cx43 lifecycle and also contribute to trafficking of Cx43 as well as possibly other functions. We are learning that many of the known non-canonical roles of Cx43 can be attributed to the recently identified six endogenous Cx43 truncated isoforms which are produced by internal translation. In general, alternative translation is a new leading edge for proteome expansion and therapeutic drug development. This review highlights recent mechanisms identified in the trafficking of gap junction channels, involvement of other proteins contributing to the delivery of channels to the cell-cell border, and understanding of possible roles of the newly discovered alternatively translated isoforms in Cx43 biology. This article is part of a Special Issue entitled: Gap Junction Proteins edited by Jean Claude Herve. Graphical abstract Display Omitted Highlights ? Gap junction channels are essential aspects of cardiomyocyte coupling which provide synchronous cardiac contraction. ? The trafficking of gap junction channels through Targeted Delivery is important for maintenance of cardiac synchrony. ? Seven different protein-isoforms of Cx43 are produced from the same GJA1 mRNA molecule by means of alternative translation. ? 20kDa alternatively translated isoform of Cx43 is a protein-chaperone to autoregulate trafficking of the full length protein.
机译:摘要间隙结(GJ)通道,包括最常见的Connexin 43(CX43),通过促进相邻细胞之间的动作电位快速传输,具有激发组织的基本作用。例如,每心跳期间的同步由心肌细胞细胞 - 细胞边界处的这些离子通道调节。 CX43蛋白质的半衰期短,并且对这些蛋白质的快速合成和及时递送给特定亚域是对细胞组织间隙结和细胞内偶联的维持至关重要。差距交叉口贩运的减值导致患病心脏的危险并发症,如突然心死的心律失常。最近的兴趣是与CX43羧基末端的蛋白质 - 蛋白质相互作用。这些相互作用对全长CX43生命周期产生了重大影响,也有助于贩运CX43以及可能的其他功能。我们正在学习CX43的许多已知的非规范作用可以归因于最近鉴定的六个内源CX43截短的同种型,其通过内部翻译产生。通常,替代翻译是蛋白质组扩张和治疗药物开发的新领先优势。该综述突出了跨空白结渠道贩运中确定的最新机制,涉及促进往复到细胞 - 细胞边界的渠道的其他蛋白质,以及对CX43生物学中新发现的可选择的同种型的可能作用的理解。本文是题为的特殊问题的一部分:Jean Claude Herve编辑的Gap Junction蛋白。图形抽象显示省略了亮点?间隙结沟道是心肌细胞偶联的重要方面,其提供同步心脏收缩。还通过目标交付贩运间隙结渠道对于维持心脏同步来说是重要的。还通过替代翻译,由相同的GJA1 mRNA分子产生七种不同的CX43蛋白质 - 同种型。还20KDA可选地翻译CX43的同种型是一种蛋白质伴侣,用于自动调用全长蛋白的运输。

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