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Evolutionary population genetics of promoters: Predicting binding sites and functional phylogenies

机译:启动子的进化种群遗传学:预测结合位点和功能系统发育。

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We study the evolution of transcription factor-binding sites in prokaryotes, using an empirically grounded model with point mutations and genetic drift. Selection acts on the site sequence via its binding affinity to the corresponding transcription factor. Calibrating the model with populations of functional binding sites, we verify this form of selection and show that typical sites are under substantial selection pressure for functionality: for cAMP response protein sites in Escherichia coli, the product of fitness difference and effective population size takes values 2NΔF of order 10. We apply this model to cross-species comparisons of binding sites in bacteria and obtain a prediction method for binding sites that uses evolutionary information in a quantitative way. At the same time, this method predicts the functional histories of orthologous sites in a phylogeny, evaluating the likelihood for conservation or loss or gain of function during evolution. We have performed, as an example, a cross-species analysis of E. coli. Salmonella typhi-murium, and Yersinia pseudotuberculosis. Detailed lists of predicted sites and their functional phylogenies are available.
机译:我们使用点突变和遗传漂移的经验基础模型研究原核生物中转录因子结合位点的进化。选择通过其对相应转录因子的结合亲和力作用于位点序列。使用功能性结合位点群体对模型进行校准,我们验证了这种选择形式,并表明典型位点在功能选择压力方面处于很大压力:对于大肠杆菌中的cAMP反应蛋白位点,适应性差异和有效群体大小的乘积取值为2NΔF阶10。我们将此模型应用于细菌中结合位点的种间比较,并获得结合位点的预测方法,该方法以定量方式使用进化信息。同时,该方法可预测系统发育中直系同源位点的功能历史,评估进化过程中保守或功能丧失或获得功能的可能性。例如,我们已经对大肠杆菌进行了跨物种分析。鼠伤寒沙门氏菌和假结核耶尔森氏菌。提供了预测位点及其功能系统发育的详细列表。

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