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CD2AP Links Cortactin and Capping Protein at the Cell Periphery To Facilitate Formation of Lamellipodia

机译:CD2AP链接Cortactin和在细胞外围的封顶蛋白,以促进Lamellipodia的形成

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摘要

Understanding the physiology of complex relationships between components of signaling pathways and the actin cytoskeleton is an important challenge. CD2AP is a membrane scaffold protein implicated in a variety of physiological and disease processes. The physiological function of CD2AP is unclear, but its biochemical interactions suggest that it has a role in dynamic actin assembly. Here, we report that CD2AP functions to facilitate the recruitment of actin capping protein (CP) to the Src kinase substrate, cortactin, at the cell periphery, and that this is necessary for formation of the short branched filaments that characterize lamellipodium formation and are required for cell migration. Superresolution fluorescence microscopy demonstrated that the efficient colocalization of CP and cortactin at the cell periphery required CD2AP. As both cortactin and CP function to enhance branched actin filament formation, CD2AP functions synergistically to enhance the function of both proteins. Our data demonstrate how the interplay between specialized actin regulatory molecules shapes the actin cytoskeleton.
机译:理解信号传导途径的成分与肌动蛋白细胞骨架之间复杂关系的生理学是一项重要的挑战。 CD2AP是一种涉及多种生理和疾病过程的膜支架蛋白。 CD2AP的生理功能尚不清楚,但其生化相互作用表明它在动态肌动蛋白装配中具有作用。在这里,我们报告CD2AP的功能是促进细胞周围的Src激酶底物cortactin的肌动蛋白加帽蛋白(CP)的募集,这对于形成表征lamellipodium形成的短分支细丝是必需的,并且是必需的用于细胞迁移。超分辨率荧光显微镜显示,CP和cortactin在细胞外围的有效共定位需要CD2AP。由于cortactin和CP均具有增强分支肌动蛋白丝形成的功能,因此CD2AP具有协同增效作用,从而增强两种蛋白的功能。我们的数据证明了专门的肌动蛋白调节分子之间的相互作用如何塑造肌动蛋白的细胞骨架。

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