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一种小的Rab GTP酶在非极化细胞的细胞质小泡中分布,但在极化上皮细胞中与紧密连接标记物ZO-1共定位。

A small rab GTPase is distributed in cytoplasmic vesicles in non polarized cells but colocalizes with the tight junction marker ZO-1 in polarized epithelial cells.

作者信息

Zahraoui A, Joberty G, Arpin M, Fontaine J J, Hellio R, Tavitian A, Louvard D

机构信息

Institut National de la Sante et de la Recherche Medicale U. 248, Faculté de médecine Lariboisière Saint Louis, Paris, France.

出版信息

J Cell Biol. 1994 Jan;124(1-2):101-15. doi: 10.1083/jcb.124.1.101.

Abstract

Small rab/Ypt1/Sec4 GTPase family have been involved in the regulation of membrane traffic along the biosynthetic and endocytic pathways in eucaryotic cells. Polarized epithelial cells have morphologically and functionally distinct apical and basolateral surfaces separated by tight junctions. The establishment and maintenance of these structures require delivery of membrane proteins and lipids to these domains. In this work, we have isolated a cDNA clone from a human intestinal cDNA library encoding a small GTPase, rab13, closely related to the yeast Sec4 protein. Confocal microscopy analysis on polarized Caco-2 cells shows that rab13 protein colocalized with the tight junction marker ZO-1. Cryostat sections of tissues confirm that rab13 localized to the junctional complex region of a variety of epithelia, including intestine, kidney, liver, and of endothelial cells. This localization requires assembly and integrity of the tight junctions. Disruption of tight junctions by incubation in low Ca2+ media induces the redistribution of rab13. In cells devoid of tight junctions, rab13 was found associated with vesicles dispersed throughout the cytoplasm. Cell-cell contacts initiated by E-cadherin in transfected L cells do not recruit rab13 to the resulting adherens-like junction complexes. The participation of rab13 in polarized transport, in the assembly and/or the activity of tight junctions is discussed.

摘要

小GTP酶家族rab/Ypt1/Sec4参与了真核细胞中沿生物合成和内吞途径的膜运输调控。极化上皮细胞具有形态和功能上不同的顶端和基底外侧表面,由紧密连接分隔。这些结构的建立和维持需要将膜蛋白和脂质运输到这些区域。在这项研究中,我们从人肠道cDNA文库中分离出一个编码小GTP酶rab13的cDNA克隆,它与酵母Sec4蛋白密切相关。对极化的Caco-2细胞进行共聚焦显微镜分析表明,rab13蛋白与紧密连接标记物ZO-1共定位。组织冰冻切片证实rab13定位于包括肠道、肾脏、肝脏和内皮细胞在内的多种上皮细胞的连接复合体区域。这种定位需要紧密连接的组装和完整性。在低钙培养基中孵育破坏紧密连接会诱导rab13的重新分布。在没有紧密连接的细胞中,发现rab13与分散在整个细胞质中的囊泡相关。转染的L细胞中由E-钙黏蛋白引发的细胞间接触不会将rab13招募到形成的黏附样连接复合体中。本文讨论了rab13在极化运输、紧密连接的组装和/或活性中的作用。

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