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Bayesian Selection of Nucleotide Substitution Models and Their Site Assignments

机译:核苷酸取代模型的贝叶斯选择及其位点分配

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Probabilistic inference of a phylogenetic tree from molecular sequence data is predicated on a substitution model describing the relative rates of change between character states along the tree for each site in the multiple sequence alignment. Commonly, one assumes that the substitution model is homogeneous across sites within large partitions of the alignment, assigns these partitions a priori, and then fixes their underlying substitution model to the best-fitting model from a hierarchy of named models. Here, we introduce an automatic model selection and model averaging approach within a Bayesian framework that simultaneously estimates the number of partitions, the assignment of sites to partitions, the substitution model for each partition, and the uncertainty in these selections. This new approach is implemented as an add-on to the BEAST 2 software platform. We find that this approach dramatically improves the fit of the nucleotide substitution model compared with existing approaches, and we show, using a number of example data sets, that as many as nine partitions are required to explain the heterogeneity in nucleotide substitution process across sites in a single gene analysis. In some instances, this improved modeling of the substitution process can have a measurable effect on downstream inference, including the estimated phylogeny, relative divergence times, and effective population size histories.
机译:从分子序列数据对系统发生树的概率推断是基于替代模型,该模型描述了多序列比对中每个位点沿树的字符状态之间的相对变化率。通常,人们假定替换模型在路线的较大分区内的各个站点之间是同质的,先对这些分区进行分配,然后从命名模型的层次结构中将其基础替换模型固定为最适合的模型。在这里,我们介绍一种在贝叶斯框架内的自动模型选择和模型平均方法,该方法同时估算分区的数量,分区的站点分配,每个分区的替换模型以及这些选择的不确定性。这种新方法是BEAST 2软件平台的一个附加组件。我们发现,与现有方法相比,该方法显着改善了核苷酸取代模型的拟合度,并且我们使用大量示例数据集显示,需要多达9个分区来解释核苷酸置换过程中跨位点的异质性。单基因分析。在某些情况下,这种替代过程的改进模型可以对下游推断产生可测量的影响,包括估计的系统发育,相对发散时间和有效种群规模历史。

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