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Quantifying Dominance And Deleterious Effect Onhuman Disease Genes

机译:量化对人类疾病基因的主导作用和有害作用

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Human genes responsible for inherited diseases are important for the understanding of human disease. We investigated the degree of polymorphism and divergence in the human disease genes to elucidate the effect of natural selection on human disease genes. In particular, the effect of disease dominance was incorporated into the analysis. Both dominant disease genes (DDG) and recessive disease genes (RDG) had a higher mutation rate per site and encoded longer proteins than the nondisease genes, which exposed the disease genes to a faster flux of new mutations. Using an unbiased polymorphism dataset, we found that, proportionally, RDG harbor more nonsynonymous polymorphisms compared with DDG. We estimated the selection intensity on the disease genes using polymorphism and divergence data and determined whether the different patterns of polymorphism and divergence between DDG and RDG could be explained by the difference in only dominance. Even after the dominance effect was considered, the selection intensity on RDG was significantly different from DDG, suggesting that the deleterious effect of the dominant and recessive disease mutations are fundamentally different.
机译:负责遗传疾病的人类基因对于理解人类疾病很重要。我们调查了人类疾病基因的多态性和差异程度,以阐明自然选择对人类疾病基因的影响。特别是,将疾病优势的影响纳入了分析。与非疾病基因相比,优势疾病基因(DDG)和隐性疾病基因(RDG)的每个位点均具有较高的突变率,并且编码的蛋白质更长,从而使疾病基因面临更快的新突变通量。使用无偏多态性数据集,我们发现与DDG相比,RDG具有更多的非同义多态性。我们使用多态性和差异数据估计了疾病基因的选择强度,并确定了DDG和RDG之间多态性和差异的不同模式是否可以由仅优势性的差异来解释。即使考虑了优势作用,RDG的选择强度也与DDG显着不同,这表明显性和隐性疾病突变的有害作用根本不同。

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