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Regulating the actin cytoskeleton during vesicular transport [Review]

机译:在水泡运输过程中调节肌动蛋白的细胞骨架[综述]

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Although the actin cytoskeleton is widely believed to play an important role in intracellular protein transport this role is poorly understood. Recently, progress has been made toward identifying specific actin-binding proteins and signaling molecules involved in regulating actin structures that function in the secretory pathway. Studies on coat protomer I (COPI)mediated transport at the Golgi apparatus and on clathrin-mediated endocytosis have been particularly informative in identifying such mechanisms. Important similarities between actin regulation at the Golgi and at the plasma membrane have been uncovered. The studies reveal that ADP-ribosylation factor and vesicle coat proteins are able to act through the Rho-family GTP-binding proteins, Cdc42 and Rac, and several specific actin-binding proteins to direct actin assembly through the Arp2/3 complex. Efficient function of the secretory pathway is likely to require precise temporal regulation among transport-vesicle assembly, vesicle scission, and the targeting machinery. It is proposed that numerous actin regulatory mechanisms and the connections between actin signaling and vesicle-coat formation are employed to provide such temporal regulation.
机译:尽管普遍认为肌动蛋白的细胞骨架在细胞内蛋白运输中起重要作用,但对此作用知之甚少。最近,在鉴定特定的肌动蛋白结合蛋白和信号分子参与调节在分泌途径中起作用的肌动蛋白结构方面取得了进展。在高尔基体中对外套前体I(COPI)介导的转运以及网格蛋白介导的内吞作用的研究在确定此类机制方面特别有用。高尔基体和质膜的肌动蛋白调节之间的重要相似性尚未发现。研究表明,ADP-核糖基化因子和囊泡外壳蛋白能够通过Rho家族的GTP结合蛋白,Cdc42和Rac以及几种特定的肌动蛋白结合蛋白起作用,从而指导肌动蛋白通过Arp2 / 3复合体组装。分泌途径的有效功能可能需要在运输-囊泡组装,囊泡分裂和靶向机制之间进行精确的时间调节。提出了多种肌动蛋白调节机制以及肌动蛋白信号传导和囊泡包衣形成之间的联系来提供这种时间调节。

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