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Rab GTPase Rab8作为纤毛发生和免疫突触组装的共同调节因子:从保守途径到多样的细胞结构

The Rab GTPase Rab8 as a shared regulator of ciliogenesis and immune synapse assembly: From a conserved pathway to diverse cellular structures.

作者信息

Patrussi Laura, Baldari Cosima T

机构信息

a Department of Life Sciences , University of Siena , Siena , Italy.

出版信息

Small GTPases. 2016;7(1):16-20. doi: 10.1080/21541248.2015.1111852. Epub 2015 Nov 20.

Abstract

Rab GTPases, which form the largest branch of the Ras GTPase superfamily, regulate almost every step of vesicle-mediated trafficking. Among them, Rab8 is an essential participant in primary cilium formation. In a report recently published in the Journal of Cell Science, Finetti and colleagues identify Rab8 as a novel player in vesicular traffic in the non-ciliated T lymphocytes, which contributes to the assembly of the specialized signaling platform known as the immune synapse. By interacting with the v-SNARE VAMP-3, Rab8 is indeed responsible for the final docking/fusion step in T cell receptor (TCR) recycling to the immune synapse. A second important take-home message which comes to light from this work is that VAMP-3 also interacts with Rab8 at the base of the cilium in NIH-3T3 cells, where it regulates ciliary growth and targeting of Smoothened at the plasma membrane. Hence the data presented in this report, in addition to identifying Rab8 as a novel player in vesicular traffic to the immune synapse, reveal how both ciliated and non-ciliated cells take advantage of a conserved pathway to build highly specific cellular structures.

摘要

Rab GTP酶是Ras GTP酶超家族中最大的一个分支,几乎调控着囊泡介导运输的每一个步骤。其中,Rab8是初级纤毛形成过程中的重要参与者。在最近发表于《细胞科学杂志》的一篇报告中,菲内蒂及其同事发现Rab8是非纤毛T淋巴细胞囊泡运输中的一个新角色,它有助于被称为免疫突触的特殊信号平台的组装。通过与v-SNARE蛋白VAMP-3相互作用,Rab8确实负责T细胞受体(TCR)循环利用至免疫突触的最终对接/融合步骤。这项研究揭示的另一个重要信息是,在NIH-3T3细胞中,VAMP-3也在纤毛基部与Rab8相互作用,在那里它调节纤毛生长以及平滑受体在质膜上的定位。因此,本报告中呈现的数据,除了将Rab8鉴定为免疫突触囊泡运输中的一个新角色外,还揭示了纤毛细胞和非纤毛细胞如何利用一条保守途径构建高度特异性的细胞结构。

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