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Estimating the Distribution of Selection Coefficients from Phylogenetic Data Using Sitewise Mutation-Selection Models

机译:使用位点突变选择模型从系统发育数据中估算选择系数的分布

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摘要

Estimation of the distribution of selection coefficients of mutations is a long-standing issue in molecular evolution. In addition to population-based methods, the distribution can be estimated from DNA sequence data by phylogenetic-based models. Previous models have generally found unimodal distributions where the probability mass is concentrated between mildly deleterious and nearly neutral mutations. Here we use a sitewise mutation–selection phylogenetic model to estimate the distribution of selection coefficients among novel and fixed mutations (substitutions) in a data set of 244 mammalian mitochondrial genomes and a set of 401 PB2 proteins from influenza. We find a bimodal distribution of selection coefficients for novel mutations in both the mitochondrial data set and for the influenza protein evolving in its natural reservoir, birds. Most of the mutations are strongly deleterious with the rest of the probability mass concentrated around mildly deleterious to neutral mutations. The distribution of the coefficients among substitutions is unimodal and symmetrical around nearly neutral substitutions for both data sets at adaptive equilibrium. About 0.5% of the nonsynonymous mutations and 14% of the nonsynonymous substitutions in the mitochondrial proteins are advantageous, with 0.5% and 24% observed for the influenza protein. Following a host shift of influenza from birds to humans, however, we find among novel mutations in PB2 a trimodal distribution with a small mode of advantageous mutations.
机译:估计突变选择系数的分布是分子进化中一个长期存在的问题。除了基于人群的方法外,还可以通过基于系统发育的模型从DNA序列数据估算分布。先前的模型通常发现单峰分布,其中概率质量集中在轻度有害突变和近乎中性突变之间。在这里,我们使用定点突变选择系统发育模型来估计244个哺乳动物线粒体基因组数据和一组来自流感的401 PB2蛋白的新突变和固定突变(替代)之间的选择系数分布。我们发现线粒体数据集中的新型突变以及在其天然水库鸟类中进化的流感蛋白的选择系数的双峰分布。大多数突变是严重有害的,其余概率集中在轻度有害到中性突变附近。替换之间系数的分布是单峰的,并且在自适应平衡时,两个数据集的近似中性替换周围都是对称的。线粒体蛋白中约0.5%的非同义突变和14%的非同义取代是有利的,其中流感蛋白占0.5%和24%。但是,在将流感病毒从鸟类转移到人类之后,我们发现PB2中的新突变是具有小模式的有利突变的三峰分布。

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