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拟南芥 II 型formin 蛋白 AtFH19 能起始肌动蛋白组装,结合于肌动蛋白丝的加帽端,并拮抗 AtFH1 对肌动蛋白动力学的影响。

An Arabidopsis class II formin, AtFH19, nucleates actin assembly, binds to the barbed end of actin filaments, and antagonizes the effect of AtFH1 on actin dynamics.

机构信息

Key Laboratory of Plant Molecular Physiology, Institute of Botany, the Chinese Academy of Sciences, Beijing 100093, China.

出版信息

J Integr Plant Biol. 2012 Oct;54(10):800-13. doi: 10.1111/j.1744-7909.2012.01160.x.

Abstract

Formin is a major protein responsible for regulating the nucleation of actin filaments, and as such, it permits the cell to control where and when to assemble actin arrays. It is encoded by a multigene family comprising 21 members in Arabidopsis thaliana. The Arabidopsis formins can be separated into two phylogenetically-distinct classes: there are 11 class I formins and 10 class II formins. Significant questions remain unanswered regarding the molecular mechanism of actin nucleation and elongation stimulated by each formin isovariant, and how the different isovariants coordinate to regulate actin dynamics in cells. Here, we characterize a class II formin, AtFH19, biochemically. We found that AtFH19 retains all general properties of the formin family, including nucleation and barbed end capping activity. It can also generate actin filaments from a pool of actin monomers bound to profilin. However, both the nucleation and barbed end capping activities of AtFH19 are less efficient compared to those of another well-characterized formin, AtFH1. Interestingly, AtFH19 FH1FH2 competes with AtFH1 FH1FH2 in binding actin filament barbed ends, and inhibits the effect of AtFH1 FH1FH2 on actin. We thus propose a mechanism in which two quantitatively different formins coordinate to regulate actin dynamics by competing for actin filament barbed ends.

摘要

formin 是一种主要的蛋白质,负责调节肌动蛋白丝的成核,因此,它允许细胞控制何时何地组装肌动蛋白阵列。它由一个多基因家族编码,在拟南芥中包含 21 个成员。拟南芥formin 可分为两个系统发育上不同的类:有 11 个类 I formin 和 10 个类 II formin。关于每个 formin 同工型刺激的肌动蛋白成核和延伸的分子机制,以及不同同工型如何协调调节细胞中的肌动蛋白动力学,仍存在许多悬而未决的问题。在这里,我们对一种类 II formin,AtFH19,进行了生化表征。我们发现 AtFH19 保留了 formin 家族的所有一般特性,包括成核和带刺末端封闭活性。它还可以从与丝状肌动蛋白结合的肌动蛋白单体池中生成肌动蛋白丝。然而,与另一种经过充分研究的 formin(AtFH1)相比,AtFH19 的成核和带刺末端封闭活性效率较低。有趣的是,AtFH19 FH1FH2 与 AtFH1 FH1FH2 竞争结合肌动蛋白丝的带刺末端,并抑制 AtFH1 FH1FH2 对肌动蛋白的影响。因此,我们提出了一种机制,其中两种数量不同的 formin 通过竞争肌动蛋白丝的带刺末端来协调调节肌动蛋白动力学。

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