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肌动蛋白丝末端的调节因子概览。

Regulators of actin filament barbed ends at a glance.

作者信息

Shekhar Shashank, Pernier Julien, Carlier Marie-France

机构信息

Cytoskeleton Dynamics and Cell Motility, I2BC, CNRS, Gif-sur-Yvette 91198, France.

Cytoskeleton Dynamics and Cell Motility, I2BC, CNRS, Gif-sur-Yvette 91198, France

出版信息

J Cell Sci. 2016 Mar 15;129(6):1085-91. doi: 10.1242/jcs.179994. Epub 2016 Mar 3.

DOI:10.1242/jcs.179994
PMID:26940918
Abstract

Cells respond to external stimuli by rapidly remodeling their actin cytoskeleton. At the heart of this function lies the intricately controlled regulation of individual filaments. The barbed end of an actin filament is the hotspot for the majority of the biochemical reactions that control filament assembly. Assays performed in bulk solution and with single filaments have enabled characterization of a plethora of barbed-end-regulating proteins. Interestingly, many of these regulators work in tandem with other proteins, which increase or decrease their affinity for the barbed end in a spatially and temporally controlled manner, often through simultaneous binding of two regulators at the barbed ends, in addition to standard mutually exclusive binding schemes. In this Cell Science at a Glance and the accompanying poster, we discuss key barbed-end-interacting proteins and the kinetic mechanisms by which they regulate actin filament assembly. We take F-actin capping protein, gelsolin, profilin and barbed-end-tracking polymerases, including formins and WH2-domain-containing proteins, as examples, and illustrate how their activity and competition for the barbed end regulate filament dynamics.

摘要

细胞通过快速重塑其肌动蛋白细胞骨架来响应外部刺激。这一功能的核心在于对单个肌动蛋白丝的复杂调控。肌动蛋白丝的尖端是控制丝组装的大多数生化反应的热点区域。在体溶液和单丝上进行的实验已能够对大量尖端调控蛋白进行表征。有趣的是,许多这些调控蛋白与其他蛋白质协同工作,这些蛋白质通常通过在尖端同时结合两种调控蛋白,以空间和时间可控的方式增加或降低它们对尖端的亲和力,这是除了标准的互斥结合模式之外的情况。在本“细胞科学一览”及随附的海报中,我们讨论了关键的尖端相互作用蛋白以及它们调控肌动蛋白丝组装的动力学机制。我们以F-肌动蛋白封端蛋白、凝溶胶蛋白、丝切蛋白以及尖端追踪聚合酶(包括formin和含WH2结构域的蛋白)为例,说明它们的活性以及对尖端的竞争如何调控丝的动态变化。

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