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Viewing cancer genes from co-evolving gene modules

机译:从共同进化的基因模块中查看癌症基因

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Motivation: Studying the evolutionary conservation of cancer genes can improve our understanding of the genetic basis of human cancers. Functionally related proteins encoded by genes tend to interact with each other in a modular fashion, which may affect both the mode and tempo of their evolution.Results: In the human PPI network, we searched for subnetworks within each of which all proteins have evolved at similar rates since the human and mouse split. Identified at a given co-evolving level, the subnetworks with non-randomly large sizes were defined as co-evolving modules. We showed that proteins within modules tend to be conserved, evolutionarily old and enriched with housekeeping genes, while proteins outside modules tend to be less-conserved, evolutionarily younger and enriched with genes expressed in specific tissues. Viewing cancer genes from co-evolving modules showed that the overall conservation of cancer genes should be mainly attributed to the cancer proteins enriched in the conserved modules. Functional analysis further suggested that cancer proteins within and outside modules might play different roles in carcinogenesis, providing a new hint for studying the mechanism of cancer.
机译:动机:研究癌症基因的进化保守性可以改善我们对人类癌症遗传基础的了解。由基因编码的功能相关蛋白倾向于以模块化的方式相互影响,这可能会影响其进化的方式和速度。结果:在人类PPI网络中,我们搜索了每个蛋白都在其中进化的子网络。自从人类和老鼠分裂以来的比率相似。在给定的共同发展水平上,具有非随机大尺寸的子网被定义为共同发展模块。我们发现模块内的蛋白质趋于保守,进化变老并富含管家基因,而模块外的蛋白质趋向于保守性较差,进化上更年轻且富含特定组织中表达的基因。从共同进化的模块中查看癌症基因表明,癌症基因的总体保守性应主要归因于在保守模块中富集的癌症蛋白。功能分析进一步表明,模块内部和外部的癌症蛋白可能在致癌过程中发挥不同的作用,为研究癌症的机制提供了新的提示。

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