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通过 ABC-F 蛋白 EttA 调节核糖体暂停实现全球调控。

Global regulation via modulation of ribosome pausing by the ABC-F protein EttA.

机构信息

Expression Génétique Microbienne, CNRS, Université Paris Cité, Institut de Biologie Physico-Chimique, Paris, France.

Biomarqueurs et nouvelles cibles thérapeutiques en oncologie, INSERM U981, Université Paris Saclay, Institut de Cancérologie Gustave Roussy, Villejuif Cedex, France.

出版信息

Nat Commun. 2024 Jul 26;15(1):6314. doi: 10.1038/s41467-024-50627-z.

Abstract

Having multiple rounds of translation of the same mRNA creates dynamic complexities along with opportunities for regulation related to ribosome pausing and stalling at specific sequences. Yet, mechanisms controlling these critical processes and the principles guiding their evolution remain poorly understood. Through genetic, genomic, physiological, and biochemical approaches, we demonstrate that regulating ribosome pausing at specific amino acid sequences can produce ~2-fold changes in protein expression levels which strongly influence cell growth and therefore evolutionary fitness. We demonstrate, both in vivo and in vitro, that the ABC-F protein EttA directly controls the translation of mRNAs coding for a subset of enzymes in the tricarboxylic acid (TCA) cycle and its glyoxylate shunt, which modulates growth in some chemical environments. EttA also modulates expression of specific proteins involved in metabolically related physiological and stress-response pathways. These regulatory activities are mediated by EttA rescuing ribosomes paused at specific patterns of negatively charged residues within the first 30 amino acids of nascent proteins. We thus establish a unique global regulatory paradigm based on sequence-specific modulation of translational pausing.

摘要

将同一段 mRNA 进行多次翻译会产生动态复杂性,并为核糖体在特定序列上暂停和停滞相关的调控提供机会。然而,控制这些关键过程的机制以及指导它们进化的原则仍知之甚少。通过遗传、基因组、生理和生化方法,我们证明了在特定氨基酸序列上调节核糖体暂停可以产生约 2 倍的蛋白质表达水平变化,这强烈影响细胞生长,从而影响进化适应性。我们在体内和体外都证明,ABC-F 蛋白 EttA 直接控制编码三羧酸 (TCA) 循环及其乙醛酸支路中一组酶的 mRNA 的翻译,这调节了一些化学环境中的生长。EttA 还调节与代谢相关的生理和应激反应途径中特定蛋白质的表达。这些调节活动是通过 EttA 拯救在新生蛋白质的前 30 个氨基酸内的特定负电荷残基模式下暂停的核糖体来介导的。因此,我们建立了一个基于翻译暂停的序列特异性调节的独特的全局调控范例。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b776/11282234/7269922f8e90/41467_2024_50627_Fig1_HTML.jpg

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