Mitochondrial protein synthesis quality control.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Lidiia Koludarova, Brendan J Battersby
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引用次数: 0

Abstract

Human mitochondrial DNA is one of the most simplified cellular genomes and facilitates compartmentalized gene expression. Within the organelle, there is no physical barrier to separate transcription and translation, nor is there evidence that quality control surveillance pathways are active to prevent translation on faulty mRNA transcripts. Mitochondrial ribosomes synthesize 13 hydrophobic proteins that require co-translational insertion into the inner membrane of the organelle. To maintain the integrity of the inner membrane, which is essential for organelle function, requires responsive quality control mechanisms to recognize aberrations in protein synthesis. In this review, we explore how defects in mitochondrial protein synthesis can arise due to the culmination of inherent mistakes that occur throughout the steps of gene expression. In turn, we examine the stepwise series of quality control processes that are needed to eliminate any mistakes that would perturb organelle homeostasis. We aim to provide an integrated view on the quality control mechanisms of mitochondrial protein synthesis and to identify promising avenues for future research.

线粒体蛋白质合成质量控制。
人类线粒体 DNA 是最简化的细胞基因组之一,有利于分区基因表达。在细胞器内,没有物理屏障将转录和翻译分开,也没有证据表明质量控制监控途径能够阻止错误的 mRNA 转录本进行翻译。线粒体核糖体合成 13 种疏水蛋白质,这些蛋白质需要通过共翻译插入细胞器的内膜。内膜对细胞器的功能至关重要,要保持内膜的完整性,就需要反应灵敏的质量控制机制来识别蛋白质合成中的异常。在这篇综述中,我们将探讨线粒体蛋白质合成缺陷是如何由基因表达整个步骤中发生的固有错误导致的。反过来,我们还研究了为消除任何可能扰乱细胞器平衡的错误所需的一系列逐步质量控制过程。我们旨在为线粒体蛋白质合成的质量控制机制提供一个综合视角,并为未来的研究确定有前途的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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