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病毒多样性与抗体选择之间的失同步限制了流感病毒的进化。

Asynchrony between virus diversity and antibody selection limits influenza virus evolution.

机构信息

Department of Ecology & Evolutionary Biology, Princeton University, Princeton, United States.

Department of Human Genetics, Wellcome Trust Sanger Institute, Cambridge, United Kingdom.

出版信息

Elife. 2020 Nov 11;9:e62105. doi: 10.7554/eLife.62105.

Abstract

Seasonal influenza viruses create a persistent global disease burden by evolving to escape immunity induced by prior infections and vaccinations. New antigenic variants have a substantial selective advantage at the population level, but these variants are rarely selected within-host, even in previously immune individuals. Using a mathematical model, we show that the temporal asynchrony between within-host virus exponential growth and antibody-mediated selection could limit within-host antigenic evolution. If selection for new antigenic variants acts principally at the point of initial virus inoculation, where small virus populations encounter well-matched mucosal antibodies in previously-infected individuals, there can exist protection against reinfection that does not regularly produce observable new antigenic variants within individual infected hosts. Our results provide a theoretical explanation for how virus antigenic evolution can be highly selective at the global level but nearly neutral within-host. They also suggest new avenues for improving influenza control.

摘要

季节性流感病毒通过进化逃避先前感染和疫苗接种所诱导的免疫,从而造成持续的全球疾病负担。新的抗原变体在人群水平上具有很大的选择优势,但这些变体在宿主内很少被选择,即使是在以前免疫的个体中也是如此。我们使用数学模型表明,宿主内病毒指数增长与抗体介导的选择之间的时间不同步可能会限制宿主内的抗原进化。如果针对新抗原变体的选择主要发生在病毒初次接种的时刻,即小病毒种群在先前感染的个体中遇到匹配良好的黏膜抗体的时刻,那么就有可能存在针对再感染的保护,而在个体感染宿主内不会经常产生可观察到的新抗原变体。我们的研究结果为病毒抗原进化如何在全球范围内具有高度选择性而在宿主内几乎呈中性提供了理论解释。它们还为改善流感控制提供了新的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a93c/7748417/178a73fbb95a/elife-62105-fig1.jpg

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