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筏介导的顶端驻留蛋白运输在极化肝细胞的直接和转胞吞途径中均有发生:不同脂质微区的作用

Raft-mediated trafficking of apical resident proteins occurs in both direct and transcytotic pathways in polarized hepatic cells: role of distinct lipid microdomains.

作者信息

Slimane Tounsia Aït, Trugnan Germain, Van IJzendoorn Sven C D, Hoekstra Dick

机构信息

Department of Membrane Cell Biology, University of Groningen, The Netherlands.

出版信息

Mol Biol Cell. 2003 Feb;14(2):611-24. doi: 10.1091/mbc.e02-08-0528.

Abstract

In polarized hepatic cells, pathways and molecular principles mediating the flow of resident apical bile canalicular proteins have not yet been resolved. Herein, we have investigated apical trafficking of a glycosylphosphatidylinositol-linked and two single transmembrane domain proteins on the one hand, and two polytopic proteins on the other in polarized HepG2 cells. We demonstrate that the former arrive at the bile canalicular membrane via the indirect transcytotic pathway, whereas the polytopic proteins reach the apical membrane directly, after Golgi exit. Most importantly, cholesterol-based lipid microdomains ("rafts") are operating in either pathway, and protein sorting into such domains occurs in the biosynthetic pathway, largely in the Golgi. Interestingly, rafts involved in the direct pathway are Lubrol WX insoluble but Triton X-100 soluble, whereas rafts in the indirect pathway are both Lubrol WX and Triton X-100 insoluble. Moreover, whereas cholesterol depletion alters raft-detergent insolubility in the indirect pathway without affecting apical sorting, protein missorting occurs in the direct pathway without affecting raft insolubility. The data implicate cholesterol as a traffic direction-determining parameter in the direct apical pathway. Furthermore, raft-cargo likely distinguishing single vs. multispanning membrane anchors, rather than rafts per se (co)determine the sorting pathway.

摘要

在极化的肝细胞中,介导驻留的顶端胆小管蛋白流动的途径和分子原理尚未明确。在此,我们一方面研究了糖基磷脂酰肌醇连接蛋白和两种单跨膜结构域蛋白的顶端转运,另一方面研究了极化的HepG2细胞中两种多跨膜结构域蛋白的顶端转运。我们证明,前者通过间接转胞吞途径到达胆小管膜,而多跨膜结构域蛋白在高尔基体出芽后直接到达顶端膜。最重要的是,基于胆固醇的脂质微区(“脂筏”)在这两种途径中都发挥作用,并且蛋白分选进入这些微区发生在生物合成途径中,主要是在高尔基体中。有趣的是,参与直接途径的脂筏不溶于月桂醇聚醚硫酸酯钠(Lubrol WX)但可溶于曲拉通X-100(Triton X-100),而间接途径中的脂筏既不溶于Lubrol WX也不溶于Triton X-100。此外,虽然胆固醇耗竭改变了间接途径中脂筏-去污剂不溶性但不影响顶端分选,但在直接途径中发生了蛋白错分选而不影响脂筏不溶性。这些数据表明胆固醇是直接顶端途径中决定运输方向的参数。此外,脂筏-货物可能区分单跨膜与多跨膜膜锚定,而不是脂筏本身(共同)决定分选途径。

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