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与IQGAP相关的蛋白DGAP1作为Rac1 GTP酶的效应器和螯合剂,介导向肌动蛋白细胞骨架的信号传导。

The IQGAP-related protein DGAP1 mediates signaling to the actin cytoskeleton as an effector and a sequestrator of Rac1 GTPases.

作者信息

Filić Vedrana, Marinović Maja, Faix Jan, Weber Igor

机构信息

Division of Molecular Biology, Ruđer Bošković Institute, Bijenička 54, 10000, Zagreb, Croatia.

出版信息

Cell Mol Life Sci. 2014 Aug;71(15):2775-85. doi: 10.1007/s00018-014-1606-3. Epub 2014 Mar 25.

Abstract

Proteins are typically categorized into protein families based on their domain organization. Yet, evolutionarily unrelated proteins can also be grouped together according to their common functional roles. Sequestering proteins constitute one such functional class, acting as macromolecular buffers and serving as an intracellular reservoir ready to release large quantities of bound proteins or other molecules upon appropriate stimulation. Another functional protein class comprises effector proteins, which constitute essential components of many intracellular signal transduction pathways. For instance, effectors of small GTP-hydrolases are activated upon binding a GTP-bound GTPase and thereupon participate in downstream interactions. Here we describe a member of the IQGAP family of scaffolding proteins, DGAP1 from Dictyostelium, which unifies the roles of an effector and a sequestrator in regard to the small GTPase Rac1. Unlike classical effectors, which bind their activators transiently leading to short-lived signaling complexes, interaction between DGAP1 and Rac1-GTP is stable and induces formation of a complex with actin-bundling proteins cortexillins at the back end of the cell. An oppositely localized Rac1 effector, the Scar/WAVE complex, promotes actin polymerization at the cell front. Competition between DGAP1 and Scar/WAVE for the common activator Rac1-GTP might provide the basis for the oscillatory re-polarization typically seen in randomly migrating Dictyostelium cells. We discuss the consequences of the dual roles exerted by DGAP1 and Rac1 in the regulation of cell motility and polarity, and propose that similar signaling mechanisms may be of general importance in regulating spatiotemporal dynamics of the actin cytoskeleton by small GTPases.

摘要

蛋白质通常根据其结构域组织被归类为蛋白质家族。然而,进化上不相关的蛋白质也可以根据它们共同的功能作用被归为一类。隔离蛋白就构成了这样一个功能类别,它们作为大分子缓冲物,充当细胞内储存库,准备在适当刺激下释放大量结合的蛋白质或其他分子。另一个功能蛋白类别包括效应蛋白,它们是许多细胞内信号转导途径的重要组成部分。例如,小GTP水解酶的效应器在结合GTP结合的GTP酶后被激活,随后参与下游相互作用。在这里,我们描述了一种支架蛋白IQGAP家族的成员,来自盘基网柄菌的DGAP1,它在小GTP酶Rac1方面兼具效应器和隔离物的作用。与经典效应器不同,经典效应器与它们的激活剂短暂结合导致形成短暂的信号复合物,而DGAP1与Rac1-GTP之间的相互作用是稳定的,并在细胞后端诱导与肌动蛋白束蛋白皮层蛋白形成复合物。一种定位相反的Rac1效应器,即Scar/WAVE复合物,促进细胞前端的肌动蛋白聚合。DGAP1和Scar/WAVE对共同激活剂Rac1-GTP的竞争可能为通常在随机迁移的盘基网柄菌细胞中看到的振荡性重新极化提供基础。我们讨论了DGAP1和Rac1在调节细胞运动性和极性中发挥的双重作用的后果,并提出类似的信号机制可能在通过小GTP酶调节肌动蛋白细胞骨架的时空动态方面具有普遍重要性。

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