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蛋白酶体对外膜线粒体蛋白的降解作用。

Outer mitochondrial membrane protein degradation by the proteasome.

作者信息

Neutzner Albert, Youle Richard J, Karbowski Mariusz

机构信息

Biochemistry Section, SNB, NINDS, NIH, Bethesda, MD 20892, USA.

出版信息

Novartis Found Symp. 2007;287:4-14; discussion 14-20.

Abstract

Protein turnover is used for regulatory processes and to eliminate superfluous, denatured or chemically inactivated polypeptides. Mitochondrial proteins may be particularly susceptible to damage induced by reactive oxygen species and several pathways of mitochondrial proteolysis have been illuminated. However, in contrast to matrix and inner mitochondrial membrane protein degradation, little is known about the turnover of integral outer mitochondrial membrane (OMM) proteins or the mechanisms involved. We have found that pheromone treatment of Saccharomyces cerevisiae induces the proteasome-dependent elimination of the OMM spanning protein, Fzo1, from the mitochondria and that Fzo1 is ubiquitylated while still associated with the membrane. These characteristic processing steps are similar to those of the endoplasmic reticulum (ER)-associated degradation (ERAD) pathway suggesting the term OMMAD, outer mitochondrial membrane-associated degradation, to describe the process. ERAD is dependent upon ER membrane spanning RING domain E3 ubiquitin ligases suggesting that certain E3 ligases in the OMM may also regulate OMMAD. This led us to clone and characterize all 54 predicted human gene products that contain both RING domains and predicted membrane spanning domains. A surprising number of these localize to mitochondria where some may control OMMAD. Some of these mitochondrial RING domain proteins also regulate mitochondrial morphology, indicating a critical role of ubiquitin signalling in the maintenance of mitochondrial homeostasis.

摘要

蛋白质周转用于调节过程以及清除多余的、变性的或化学失活的多肽。线粒体蛋白质可能特别容易受到活性氧诱导的损伤,并且线粒体蛋白水解的几种途径已被阐明。然而,与线粒体基质和内膜蛋白降解不同,关于线粒体外膜(OMM)整合蛋白的周转或相关机制知之甚少。我们发现,用信息素处理酿酒酵母会诱导蛋白酶体依赖性地从线粒体中清除跨线粒体外膜的蛋白Fzo1,并且Fzo1在仍与膜结合时被泛素化。这些特征性加工步骤类似于内质网(ER)相关降解(ERAD)途径的步骤,因此我们提出了“线粒体外膜相关降解(OMMAD)”这一术语来描述该过程。ERAD依赖于内质网跨膜的RING结构域E3泛素连接酶,这表明线粒体外膜中的某些E3连接酶也可能调节OMMAD。这促使我们克隆并鉴定了所有54种预测的人类基因产物,它们都含有RING结构域和预测的跨膜结构域。其中数量惊人的蛋白定位于线粒体,其中一些可能控制OMMAD。这些线粒体RING结构域蛋白中的一些还调节线粒体形态,表明泛素信号在维持线粒体稳态中起关键作用。

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