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从细胞质的可及性对于ClpXP蛋白酶介导的ssrA标签依赖性整合膜蛋白降解至关重要。

Accessibility from the Cytoplasm Is Critical for ssrA Tag-Mediated Degradation of Integral Membrane Proteins by ClpXP Protease.

作者信息

Abeywansha Thilini, Chai Qian, Zhang Xinyi, Wang Zhaoshuai, Wei Yinan

机构信息

Department of Chemistry , University of Kentucky , Lexington , Kentucky 40506 , United States.

出版信息

Biochemistry. 2018 Sep 25;57(38):5602-5608. doi: 10.1021/acs.biochem.8b00641. Epub 2018 Sep 12.

DOI:10.1021/acs.biochem.8b00641
PMID:30169015
Abstract

The AAA+ protease ClpXP has long been established as the cellular rescue system that degrades ssrA-tagged proteins resulting from stalled ribosomes. Until recently, in all of these studies soluble proteins were used as model substrates, since the ClpXP complex and the related adapter SspB are all cytosolic proteins. In a previous study, we found that the introduction of an ssrA tag can facilitate complete degradation of a large and stable trimeric integral membrane protein AcrB, which is the first reported example of a membrane protein substrate. To investigate the mechanism of degradation of a membrane protein by a soluble protein complex, we experimented with the truncation of the C-terminal tail of AcrB. We found that the C-terminal tail is important for degradation, as systematic truncation of the tail diminished degradation. Thus, we hypothesize that membrane proteins need a cytosolic tail/domain for ClpXP-SspB to latch on to initiate degradation. To test this hypothesis, we introduced the ssrA tag at the C-terminal of several membrane proteins, including AqpZ, YiiP, YajR, as well as their truncation fragments, and examined their degradation. We found that the ssrA-facilitated degradation of membrane proteins by ClpXP-SspB depends on the presence of a CT tail or domain, which is critical for accessibility of the tag by ClpXP-SspB. When the ssrA tag is not well-exposed to the cytosol, FtsH can access and degrade the tagged protein, given that the substrate protein is metastable.

摘要

AAA+蛋白酶ClpXP长期以来一直被视为一种细胞救援系统,可降解因核糖体停滞产生的带有ssrA标签的蛋白质。直到最近,在所有这些研究中,由于ClpXP复合物和相关衔接蛋白SspB都是胞质蛋白,因此都使用可溶性蛋白作为模型底物。在之前的一项研究中,我们发现引入ssrA标签可以促进大型稳定三聚体整合膜蛋白AcrB的完全降解,这是首次报道的膜蛋白底物实例。为了研究可溶性蛋白复合物对膜蛋白的降解机制,我们对AcrB的C末端尾巴进行了截短实验。我们发现C末端尾巴对降解很重要,因为对其进行系统性截短会减少降解。因此,我们推测膜蛋白需要一个胞质尾巴/结构域,以便ClpXP-SspB附着从而启动降解。为了验证这一推测,我们在几种膜蛋白(包括AqpZ、YiiP、YajR)及其截短片段的C末端引入了ssrA标签,并检测它们的降解情况。我们发现,ClpXP-SspB通过ssrA促进的膜蛋白降解取决于CT尾巴或结构域的存在,这对于ClpXP-SspB接触标签至关重要。当ssrA标签不能很好地暴露于胞质溶胶时,鉴于底物蛋白是亚稳态的,FtsH可以接触并降解带标签的蛋白。

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