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Rab27 effector Slp2-a transports the apical signaling molecule podocalyxin to the apical surface of MDCK II cells and regulates claudin-2 expression

机译:Rab27效应子Slp2-a将顶信号分子podocalyxin转运至MDCK II细胞的顶表面并调节claudin-2的表达

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摘要

Most cells in tissues are polarized and usually have two distinct plasma membrane domains—an apical membrane and a basolateral membrane, which are the result of polarized trafficking of proteins and lipids. However, the mechanism underlying the cell polarization is not fully understood. In this study, we investigated the involvement of synaptotagmin- like protein 2-a (Slp2-a), an effector molecule for the small GTPase Rab27, in polarized trafficking by using Madin–Darby canine kidney II cells as a model of polarized cells. The results show that the level of Slp2-a expression in MDCK II cells increases greatly as the cells become polarized and that its expression is specifically localized at the apical membrane. The results also reveal that Slp2-a is required for targeting of the signaling molecule podocalyxin to the apical membrane in a Rab27A-dependent manner. In addition, ezrin, a downstream target of podocalyxin, and ERK1/2 are activated in Slp2-a–knockdown cells, and their activation results in a dramatic reduction in the amount of the tight junction protein claudin-2. Because both Slp2-a and claudin-2 are highly expressed in mouse renal proximal tubules, Slp2-a is likely to regulate claudin-2 expression through trafficking of podocalyxin to the apical surface in mouse renal tubule epithelial cells.
机译:组织中的大多数细胞是极化的,通常具有两个截然不同的质膜结构域—顶膜和基底外侧膜,这是蛋白质和脂质极化运输的结果。但是,细胞极化的机理尚不完全清楚。在这项研究中,我们通过使用Madin-Darby犬肾II细胞作为极化细胞模型,研究了突触结合蛋白样蛋白2-a(Slp2-a)(小GTPase Rab27的效应分子)在极化运输中的参与。结果表明,随着细胞极化,MDCK II细胞中Slp2-a的表达水平显着增加,并且其表达特异地位于顶膜。结果还表明,Slp2-a是通过Rab27A依赖性方式将信号分子足蛋白溶解素靶向顶膜所必需的。此外,在Slp2-a-knockdown细胞中激活了ezrin(podocalyxin的下游靶标)和ERK1 / 2,它们的激活导致紧密连接蛋白claudin-2的量大大减少。由于Slp2-a和claudin-2在小鼠肾近端小管中均高表达,因此Slp2-a可能通过将Podocalyxin转运至小鼠肾小管上皮细胞的顶端表面来调节claudin-2的表达。

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