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内质网蛋白 Ema19 促进未导入的线粒体前体蛋白的降解。

The ER protein Ema19 facilitates the degradation of nonimported mitochondrial precursor proteins.

机构信息

Cell Biology, University of Kaiserslautern, 67663 Kaiserslautern, Germany.

Department of Molecular Genetics, Weizmann Institute of Science, Rehovot 7610001, Israel.

出版信息

Mol Biol Cell. 2021 Apr 15;32(8):664-674. doi: 10.1091/mbc.E20-11-0748. Epub 2021 Feb 17.

Abstract

For the biogenesis of mitochondria, hundreds of proteins need to be targeted from the cytosol into the various compartments of this organelle. The intramitochondrial targeting routes these proteins take to reach their respective location in the organelle are well understood. However, the early targeting processes, from cytosolic ribosomes to the membrane of the organelle, are still largely unknown. In this study, we present evidence that an integral membrane protein of the endoplasmic reticulum (ER), Ema19, plays a role in this process. Mutants lacking Ema19 show an increased stability of mitochondrial precursor proteins, indicating that Ema19 promotes the proteolytic degradation of nonproductive precursors. The deletion of Ema19 improves the growth of respiration-deficient cells, suggesting that Ema19-mediated degradation can compete with productive protein import into mitochondria. Ema19 is the yeast representative of a conserved protein family. The human Ema19 homologue is known as sigma 2 receptor or TMEM97. Though its molecular function is not known, previous studies suggested a role of the sigma 2 receptor as a quality control factor in the ER, compatible with our observations about Ema19. More globally, our data provide an additional demonstration of the important role of the ER in mitochondrial protein targeting.

摘要

对于线粒体的生物发生,数百种蛋白质需要从细胞质靶向到细胞器的各个隔室。这些蛋白质进入细胞器时所采取的内部靶向途径已得到很好的理解。然而,从细胞质核糖体到细胞器膜的早期靶向过程在很大程度上仍然未知。在这项研究中,我们提供了证据表明内质网(ER)的一种完整膜蛋白 Ema19 在这个过程中发挥作用。缺乏 Ema19 的突变体显示线粒体前体蛋白稳定性增加,表明 Ema19 促进非生产性前体的蛋白水解降解。Ema19 的缺失改善了呼吸缺陷细胞的生长,表明 Ema19 介导的降解可以与有生产力的蛋白质导入线粒体竞争。Ema19 是酵母中保守蛋白家族的代表。人类 Ema19 同源物被称为 sigma 2 受体或 TMEM97。尽管其分子功能尚不清楚,但先前的研究表明 sigma 2 受体作为 ER 中的质量控制因素的作用与其在 Ema19 中的观察结果一致。更广泛地说,我们的数据提供了 ER 在靶向线粒体蛋白质中的重要作用的另一个例证。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2305/8108515/c28ffba856ea/mbc-32-664-g001.jpg

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