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冠状病毒基因组和宿主适应的多种途径。

Variable routes to genomic and host adaptation among coronaviruses.

机构信息

British Columbia Centre for Excellence in HIV/AIDS, Vancouver, BC, Canada.

Bioinformatics Programme, University of British Columbia, Vancouver, BC, Canada.

出版信息

J Evol Biol. 2021 Jun;34(6):924-936. doi: 10.1111/jeb.13771. Epub 2021 Mar 10.

Abstract

Natural selection operating on the genomes of viral pathogens in different host species strongly contributes to adaptation facilitating host colonization. Here, we analyse, quantify and compare viral adaptation in genomic sequence data derived from seven zoonotic events in the Coronaviridae family among primary, intermediate and human hosts. Rates of nonsynonymous (d ) and synonymous (d ) changes on specific amino acid positions were quantified for each open reading frame (ORF). Purifying selection accounted for 77% of all sites under selection. Diversifying selection was most frequently observed in viruses infecting the primary hosts of each virus and predominantly occurred in the orf1ab genomic region. Within all four intermediate hosts, diversifying selection on the spike gene was observed either solitarily or in combination with orf1ab and other genes. Consistent with previous evidence, pervasive diversifying selection on coronavirus spike genes corroborates the role this protein plays in host cellular entry, adaptation to new hosts and evasion of host cellular immune responses. Structural modelling of spike proteins identified a significantly higher proportion of sites for SARS-CoV-2 under positive selection in close proximity to sites of glycosylation relative to the other coronaviruses. Among human coronaviruses, there was a significant inverse correlation between the number of sites under positive selection and the estimated years since the virus was introduced into the human population. Abundant diversifying selection observed in SARS-CoV-2 suggests the virus remains in the adaptive phase of the host switch, typical of recent host switches. A mechanistic understanding of where, when and how genomic adaptation occurs in coronaviruses following a host shift is crucial for vaccine design, public health responses and predicting future pandemics.

摘要

自然选择作用于不同宿主物种中病毒病原体的基因组,强烈促进了适应宿主定殖的过程。在这里,我们分析、量化并比较了冠状病毒科中 7 种人畜共患病例的基因组序列数据中的病毒适应性。针对每个开放阅读框(ORF),对特定氨基酸位置的非同义(dN)和同义(dS)变化率进行了量化。选择压力下的所有位点中,有 77%受到了纯化选择的影响。在感染每种病毒的原始宿主的病毒中,最频繁观察到的是多样化选择,且主要发生在 orf1ab 基因组区域。在所有 4 个中间宿主中,刺突基因的多样化选择要么是孤立的,要么与 orf1ab 和其他基因一起发生。与之前的证据一致,冠状病毒刺突基因的广泛多样化选择证实了该蛋白在宿主细胞进入、适应新宿主和逃避宿主细胞免疫反应中的作用。刺突蛋白的结构建模确定了 SARS-CoV-2 中有显著更高比例的正选择位点,这些位点与糖基化位点接近,而其他冠状病毒则没有。在人类冠状病毒中,正选择位点的数量与病毒引入人类种群的估计年份之间存在显著的负相关关系。在 SARS-CoV-2 中观察到丰富的多样化选择表明,该病毒仍处于宿主转换的适应阶段,这是近期宿主转换的典型特征。深入了解冠状病毒在宿主转换后何时、何地以及如何发生基因组适应性,对于疫苗设计、公共卫生应对和预测未来的大流行至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/33a1/8251820/0fd2344c70b9/JEB-34-924-g005.jpg

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