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ccdA 抗毒素的高突变敏感性与密码子优化有关。

The High Mutational Sensitivity of ccdA Antitoxin Is Linked to Codon Optimality.

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bangalore 560012, India.

Institute of Bioinformatics, Bangalore 560100, India.

出版信息

Mol Biol Evol. 2022 Oct 7;39(10). doi: 10.1093/molbev/msac187.

Abstract

Deep mutational scanning studies suggest that synonymous mutations are typically silent and that most exposed, nonactive-site residues are tolerant to mutations. Here, we show that the ccdA antitoxin component of the Escherichia coli ccdAB toxin-antitoxin system is unusually sensitive to mutations when studied in the operonic context. A large fraction (∼80%) of single-codon mutations, including many synonymous mutations in the ccdA gene shows inactive phenotype, but they retain native-like binding affinity towards cognate toxin, CcdB. Therefore, the observed phenotypic effects are largely not due to alterations in protein structure/stability, consistent with a large region of CcdA being intrinsically disordered. E. coli codon preference and strength of ribosome-binding associated with translation of downstream ccdB gene are found to be major contributors of the observed ccdA mutant phenotypes. In select cases, proteomics studies reveal altered ratios of CcdA:CcdB protein levels in vivo, suggesting that the ccdA mutations likely alter relative translation efficiencies of the two genes in the operon. We extend these results by studying single-site synonymous mutations that lead to loss of function phenotypes in the relBE operon upon introduction of rarer codons. Thus, in their operonic context, genes are likely to be more sensitive to both synonymous and nonsynonymous point mutations than inferred previously.

摘要

深度突变扫描研究表明,同义突变通常是沉默的,大多数暴露的非活性部位残基对突变具有耐受性。在这里,我们表明,大肠杆菌 ccdAB 毒素-抗毒素系统的 ccdA 抗毒素成分在操纵子背景下研究时,对突变异常敏感。很大一部分(约 80%)单密码子突变,包括 ccdA 基因中的许多同义突变,表现出无活性表型,但它们对同源毒素 CcdB 保留了天然样结合亲和力。因此,观察到的表型效应主要不是由于蛋白质结构/稳定性的改变,这与 CcdA 的一大区域呈固有无序状态一致。大肠杆菌密码子偏好和与下游 ccdB 基因翻译相关的核糖体结合强度被发现是观察到的 ccdA 突变表型的主要贡献者。在某些情况下,蛋白质组学研究揭示了体内 CcdA:CcdB 蛋白水平的比例发生改变,表明 ccdA 突变可能改变操纵子中两个基因的相对翻译效率。我们通过研究在引入稀有密码子时导致 relBE 操纵子丧失功能表型的单个同义突变来扩展这些结果。因此,在它们的操纵子背景下,基因可能比以前推断的更敏感于同义和非同义点突变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b6bc/9555053/71fbf8a595b7/msac187f1.jpg

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