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跨膜结构域对于Sbh1p的功能、其与Sec61复合体的结合以及与Rtn1p的相互作用而言是足够的。

The transmembrane domain is sufficient for Sbh1p function, its association with the Sec61 complex, and interaction with Rtn1p.

作者信息

Feng Dejiang, Zhao Xueqiang, Soromani Christina, Toikkanen Jaana, Römisch Karin, Vembar Shruthi S, Brodsky Jeffrey L, Keränen Sirkka, Jäntti Jussi

机构信息

VTT Biotechnology, FI-02044 VTT, Espoo, Finland.

出版信息

J Biol Chem. 2007 Oct 19;282(42):30618-28. doi: 10.1074/jbc.M701840200. Epub 2007 Aug 14.

Abstract

The Sec61 protein translocation complex in the endoplasmic reticulum (ER) membrane is composed of three subunits. The alpha-subunit, called Sec61p in yeast, is a multispanning membrane protein that forms the protein conducting channel. The functions of the smaller, carboxyl-terminally tail-anchored beta subunit Sbh1p, its close homologue Sbh2p, and the gamma subunit Sss1p are not well understood. Here we show that co-translational protein translocation into the ER is reduced in sbh1Delta sbh2Delta cells, whereas there is a limited reduction of post-translational translocation and no effect on export of a mutant form of alpha-factor precursor for ER-associated degradation in the cytosol. The translocation defect and the temperature-sensitive growth phenotype of sbh1Delta sbh2Delta cells were rescued by expression of the transmembrane domain of Sbh1p alone, and the Sbh1p transmembrane domain was sufficient for coimmunoprecipitation with Sec61p and Sss1p. Furthermore, we show that Sbh1p co-precipitates with the ER transmembrane protein Rtn1p. Sbh1p-Rtn1p complexes do not appear to contain Sss1p and Sec61p. Our results define the transmembrane domain as the minimal functional domain of the Sec61beta homologue Sbh1p in ER translocation, identify a novel interaction partner for Shb1p, and imply that Sbh1p has additional functions that are not directly linked to protein translocation in association with the Sec61 complex.

摘要

内质网(ER)膜中的Sec61蛋白易位复合体由三个亚基组成。α亚基在酵母中称为Sec61p,是一种多次跨膜蛋白,形成蛋白质传导通道。较小的、羧基末端尾锚定的β亚基Sbh1p、其紧密同源物Sbh2p和γ亚基Sss1p的功能尚不清楚。在这里,我们表明,在sbh1Δsbh2Δ细胞中,共翻译的蛋白质向内质网的易位减少,而翻译后易位仅有有限的减少,并且对细胞质中用于内质网相关降解的α因子前体突变形式的输出没有影响。单独表达Sbh1p的跨膜结构域可挽救sbh1Δsbh2Δ细胞的易位缺陷和温度敏感生长表型,并且Sbh1p跨膜结构域足以与Sec61p和Sss1p进行共免疫沉淀。此外,我们表明Sbh1p与内质网跨膜蛋白Rtn1p共沉淀。Sbh1p-Rtn1p复合物似乎不包含Sss1p和Sec61p。我们的结果将跨膜结构域定义为内质网易位中Sec61β同源物Sbh1p的最小功能结构域,确定了Shb1p的一个新的相互作用伙伴,并暗示Sbh1p具有与Sec61复合物相关的、不直接与蛋白质易位相关的其他功能。

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