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Expansion of Biological Pathways Based on Evolutionary Inference

机译:基于进化推理的生物途径扩展

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The availability of diverse genomes makes it possible to predict gene function based on shared evolutionary history. This approach can be challenging, however, for pathways whose components do not exhibit a shared history but rather consist of distinct "evolutionary modules." We introduce a computational algorithm, clustering by inferred models of evolution (CLIME), which inputs a eukaryotic species tree, homology matrix, and pathway (gene set) of interest. CLIME partitions the gene set into disjoint evolutionary modules, simultaneously learning the number of modules and a tree-based evolutionary history that defines each module. CLIME then expands each module by scanning the genome for new components that likely arose under the inferred evolutionary model. Application of CLIME to ~1,000 annotated human pathways and to the proteomes of yeast, red algae, and malaria reveals unanticipated evolutionary modularity and coevolving components. CLIME is freely available and should become increasingly powerful with the growing wealth of eukaryotic genomes.
机译:多样的基因组的可用性使基于共同的进化史预测基因功能成为可能。但是,对于其组成部分没有共享历史而是由不同的“进化模块”组成的路径,此方法可能具有挑战性。我们介绍了一种计算算法,该算法通过推断的进化模型(CLIME)进行聚类,该算法输入了真核物种树,同源矩阵和感兴趣的途径(基因集)。 CLIME将基因集划分为不相交的进化模块,同时了解模块的数量和定义每个模块的基于树的进化历史。然后,CLIME通过扫描基因组以寻找在推测的进化模型下可能出现的新成分来扩展每个模块。将CLIME用于约1,000条带注释的人类途径以及酵母,红藻和疟疾蛋白质组的应用揭示了出乎意料的进化模块和共同进化的成分。 CLIME是免费提供的,并且随着越来越多的真核生物基因组的发展,其功能将越来越强大。

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