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Rab6A和Rab6A'小GTP酶在膜运输中发挥非重叠作用。

Rab6A and Rab6A' GTPases play non-overlapping roles in membrane trafficking.

作者信息

Del Nery Elaine, Miserey-Lenkei Stéphanie, Falguières Thomas, Nizak Clément, Johannes Ludger, Perez Franck, Goud Bruno

机构信息

Molecular Mechanisms of Intracellular Transport, UMR CNRS 144, Institut Curie, 26 rue d'Ulm, 75248 Paris Cedex 05, France.

出版信息

Traffic. 2006 Apr;7(4):394-407. doi: 10.1111/j.1600-0854.2006.00395.x.

Abstract

The closely related Rab6 isoforms, Rab6A and Rab6A', have been shown to regulate vesicular trafficking within the Golgi and post-Golgi compartments, but studies using dominant active or negative mutant suggested conflicting models. Here, we report that reduction in the expression of Rab6 isoform using specific small interfering RNA reveals noticeable differences in the Rab6A and Rab6A' biological functions. Surprisingly, Rab6A seems to be largely dispensable in membrane trafficking events, whereas knocking down the expression of Rab6A' hampers the intracellular transport of the retrograde cargo marker, the Shiga Toxin B-subunit along the endocytic pathway, and causes defects in Golgi- associated protein recycling through the endoplasmic reticulum. We also showed that Rab6A' is required for cell cycle progression through mitosis and identify Ile(62) as a key residue for uncoupling Rab6A' functions in mitosis and retrograde trafficking. Thus, our work shows that Rab6A and Rab6A' perform different functions within the cell and suggests a novel role for Rab6A' as the major Rab6 isoform regulating previously described Rab6-dependent transport pathways.

摘要

密切相关的Rab6亚型Rab6A和Rab6A'已被证明可调节高尔基体和高尔基体后区室中的囊泡运输,但使用显性激活或阴性突变体的研究提出了相互矛盾的模型。在此,我们报告,使用特异性小干扰RNA降低Rab6亚型的表达揭示了Rab6A和Rab6A'生物学功能上的显著差异。令人惊讶的是,Rab6A在膜运输事件中似乎基本 dispensable,而敲低Rab6A'的表达会阻碍逆行货物标记物志贺毒素B亚基沿内吞途径的细胞内运输,并导致通过内质网的高尔基体相关蛋白回收缺陷。我们还表明,Rab6A'是细胞周期通过有丝分裂进展所必需的,并确定Ile(62)是在有丝分裂和逆行运输中解开Rab6A'功能的关键残基。因此,我们的工作表明Rab6A和Rab6A'在细胞内执行不同的功能,并表明Rab6A'作为调节先前描述的Rab6依赖性运输途径的主要Rab6亚型具有新的作用。

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