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通过核糖体质量控制和无义衰变进行蛋白质稳态调节。

Proteostasis regulation through ribosome quality control and no-go-decay.

机构信息

Department of Biochemistry, McGill University, Montreal, Canada.

出版信息

Wiley Interdiscip Rev RNA. 2023 Nov-Dec;14(6):e1809. doi: 10.1002/wrna.1809. Epub 2023 Jul 24.

DOI:10.1002/wrna.1809
PMID:37488089
Abstract

Cell functionality relies on the existing pool of proteins and their folding into functional conformations. This is achieved through the regulation of protein synthesis, which requires error-free mRNAs and ribosomes. Ribosomes are quality control hubs for mRNAs and proteins. Problems during translation elongation slow down the decoding rate, leading to ribosome halting and the eventual collision with the next ribosome. Collided ribosomes form a specific disome structure recognized and solved by ribosome quality control (RQC) mechanisms. RQC pathways orchestrate the degradation of the problematic mRNA by no-go decay and the truncated nascent peptide, the repression of translation initiation, and the recycling of the stalled ribosomes. All these events maintain protein homeostasis and return valuable ribosomes to translation. As such, cell homeostasis and function are maintained at the mRNA level by preventing the production of aberrant or unnecessary proteins. It is becoming evident that the crosstalk between RQC and the protein homeostasis network is vital for cell function, as the absence of RQC components leads to the activation of stress response and neurodegenerative diseases. Here, we review the molecular events of RQC discovered through well-designed stalling reporters. Given the impact of RQC in proteostasis, we discuss the relevance of identifying endogenous mRNA regulated by RQC and their preservation in stress conditions. This article is categorized under: RNA Turnover and Surveillance > Turnover/Surveillance Mechanisms Translation > Regulation.

摘要

细胞功能依赖于现有的蛋白质库及其折叠成功能构象。这是通过蛋白质合成的调节来实现的,蛋白质合成需要无错误的 mRNA 和核糖体。核糖体是 mRNA 和蛋白质的质量控制中心。翻译延伸过程中的问题会降低解码速度,导致核糖体停顿,并最终与下一个核糖体发生碰撞。碰撞的核糖体形成一种特殊的二联体结构,被核糖体质量控制(RQC)机制识别和解决。RQC 途径通过无意义衰变和截断新生肽来协调有问题的 mRNA 的降解、翻译起始的抑制以及stalled ribosomes 的回收。所有这些事件都维持了蛋白质的内稳,使有价值的核糖体重新参与翻译。因此,通过防止产生异常或不必要的蛋白质,细胞内稳和功能在 mRNA 水平上得以维持。现在越来越明显的是,RQC 与蛋白质稳态网络之间的串扰对于细胞功能至关重要,因为缺乏 RQC 成分会导致应激反应和神经退行性疾病的激活。在这里,我们通过精心设计的stalling 报告者来回顾 RQC 的分子事件。鉴于 RQC 在蛋白质稳态中的影响,我们讨论了识别受 RQC 调节的内源性 mRNA 及其在应激条件下保存的相关性。本文属于:RNA 周转和监控 > 周转/监控机制 翻译 > 调控。

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