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Multiple testing corrections for imputed SNPs.

机译:推算的SNP的多次测试更正。

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摘要

Multiple testing corrections are an active research topic in genetic association studies, especially for genome-wide association studies (GWAS), where tests of association with traits are conducted at millions of imputed SNPs with estimated allelic dosages now. Failure to address multiple comparisons appropriately can introduce excess false-positive results and make subsequent studies following up those results inefficient. Permutation tests are considered the gold standard in multiple testing adjustment; however, this procedure is computationally demanding, especially for GWAS. Notably, the permutation thresholds for the huge number of estimated allelic dosages in real data sets have not been reported. Although many researchers have recently developed algorithms to rapidly approximate the permutation thresholds with accuracy similar to the permutation test, these methods have not been verified with estimated allelic dosages. In this study, we compare recently published multiple testing correction methods using 2.5M estimated allelic dosages. We also derive permutation significance levels based on 10,000 GWAS results under the null hypothesis of no association. Our results show that the simpleM method works well with estimated allelic dosages and gives the closest approximation to the permutation threshold while requiring the least computation time.
机译:多重测试校正是遗传关联研究中一个活跃的研究主题,尤其是对于全基因组关联研究(GWAS),其中与性状关联的测试目前在数百万个估算的等位基因剂量的SNP上进行。未能正确处理多个比较会引入过多的假阳性结果,并使后续研究无效。置换测试在多次测试调整中被视为黄金标准;但是,此过程对计算要求很高,尤其是对于GWAS。值得注意的是,尚未报道真实数据集中大量估计的等位基因剂量的置换阈值。尽管最近有许多研究人员开发了算法来以近似于置换测试的准确性快速逼近置换阈值,但是尚未用估计的等位基因剂量验证这些方法。在这项研究中,我们比较了最近发表的使用2.5M估计的等位基因剂量的多种测试校正方法。我们还根据无关联的零假设下的10,000个GWAS结果得出置换显着性水平。我们的结果表明,simpleM方法在估计等位基因剂量时效果很好,并且在需要最少计算时间的情况下,可以最接近置换阈值。

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