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人类流感 A 病毒的分子适应的基因组速率。

The genomic rate of molecular adaptation of the human influenza A virus.

机构信息

Department of Zoology, University of Oxford, Oxford, United Kingdom.

出版信息

Mol Biol Evol. 2011 Sep;28(9):2443-51. doi: 10.1093/molbev/msr044. Epub 2011 Mar 16.

Abstract

Quantifying adaptive evolution at the genomic scale is an essential yet challenging aspect of evolutionary biology. Here, we develop a method that extends and generalizes previous approaches to estimate the rate of genomic adaptation in rapidly evolving populations and apply it to a large data set of complete human influenza A virus genome sequences. In accord with previous studies, we observe particularly high rates of adaptive evolution in domain 1 of the viral hemagglutinin (HA1). However, our novel approach also reveals previously unseen adaptation in other viral genes. Notably, we find that the rate of adaptation (per codon per year) is higher in surface residues of the viral neuraminidase than in HA1, indicating strong antibody-mediated selection on the former. We also observed high rates of adaptive evolution in several nonstructural proteins, which may relate to viral evasion of T-cell and innate immune responses. Furthermore, our analysis provides strong quantitative support for the hypothesis that human H1N1 influenza experiences weaker antigenic selection than H3N2. As well as shedding new light on the dynamics and determinants of positive Darwinian selection in influenza viruses, the approach introduced here is applicable to other pathogens for which densely sampled genome sequences are available, and hence is ideally suited to the interpretation of next-generation genome sequencing data.

摘要

在基因组尺度上量化适应性进化是进化生物学中一个基本但具有挑战性的方面。在这里,我们开发了一种方法,扩展和推广了以前的方法来估计快速进化群体中基因组适应性的速度,并将其应用于大量完整的人类甲型流感病毒基因组序列数据集。与以前的研究一致,我们在病毒血凝素(HA1)的结构域 1 中观察到特别高的适应性进化率。然而,我们的新方法还揭示了其他以前未被发现的病毒基因的适应性。值得注意的是,我们发现病毒神经氨酸酶表面残基的适应速度(每个密码子每年)高于 HA1,表明前者受到强烈的抗体介导选择。我们还观察到几种非结构蛋白的适应性进化速度很高,这可能与病毒逃避 T 细胞和先天免疫反应有关。此外,我们的分析为以下假设提供了强有力的定量支持:人类 H1N1 流感经历的抗原选择比 H3N2 弱。除了为流感病毒中正向达尔文选择的动态和决定因素提供新的见解外,这里介绍的方法也适用于其他具有密集采样基因组序列的病原体,因此非常适合解释下一代基因组测序数据。

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