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Comparing GWAS Results of Complex Traits Using Full Genetic Model and Additive Models for Revealing Genetic Architecture

机译:使用全遗传模型和附加模型对复杂性状的GWAS结果进行比较,揭示遗传建筑

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Most of the genome-wide association studies (GWASs) for human complex diseases have ignored dominance, epistasis and ethnic interactions. We conducted comparative GWASs for total cholesterol using full model and additive models, which illustrate the impacts of the ignoring genetic variants on analysis results and demonstrate how genetic effects of multiple loci could differ across different ethnic groups. There were 15 quantitative trait loci with 13 individual loci and 3 pairs of epistasis loci identified by full model, whereas only 14 loci (9 common loci and 5 different loci) identified by multi-loci additive model. Again, 4 full model detected loci were not detected using multi-loci additive model. PLINK-analysis identified two loci and GCTA-analysis detected only one locus with genome-wide significance. Full model identified three previously reported genes as well as several new genes. Bioinformatics analysis showed some new genes are related with cholesterol related chemicals and/or diseases. Analyses of cholesterol data and simulation studies revealed that the full model performs were better than the additive-model performs in terms of detecting power and unbiased estimations of genetic variants of complex traits.
机译:人类复杂疾病的大多数基因组协会研究(GWASS)忽略了统治,外观和族裔互动。我们使用全模型和添加剂模型对总胆固醇进行了比较GWAS,这阐述了忽略遗传变异对分析结果的影响,并证明了多个基因座的遗传效应在不同的族群中可能会有所不同。有15个定量特质基因座,具有13个单独的基因座和3对全部模型的11对外置基因座,而多基因座添加剂模型仅识别的14个基因座(9个公共基因座和5个不同的基因座)。同样,使用多基因座添加剂模型未检测到4个全模型检测到的基因座。 plink分析确定了两个基因座和GCTA分析,仅检测到一个基因组显着性的基因座。全模型确定了三个先前报告的基因以及几种新基因。生物信息学分析显示一些新的基因与胆固醇相关的化学品和/或疾病有关。胆固醇数据和仿真研究的分析表明,在检测复合状性状的遗传变异遗传变异估计方面,完全模型表现优于添加剂模型。

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