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首页> 外文期刊>The American Journal of Human Genetics >Estimating odds ratios in genome scans: an approximate conditional likelihood approach.
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Estimating odds ratios in genome scans: an approximate conditional likelihood approach.

机译:估计基因组扫描中的比值比:一种近似的条件似然方法。

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摘要

In modern whole-genome scans, the use of stringent thresholds to control the genome-wide testing error distorts the estimation process, producing estimated effect sizes that may be on average far greater in magnitude than the true effect sizes. We introduce a method, based on the estimate of genetic effect and its standard error as reported by standard statistical software, to correct for this bias in case-control association studies. Our approach is widely applicable, is far easier to implement than competing approaches, and may often be applied to published studies without access to the original data. We evaluate the performance of our approach via extensive simulations for a range of genetic models, minor allele frequencies, and genetic effect sizes. Compared to the naive estimation procedure, our approach reduces the bias and the mean squared error, especially for modest effect sizes. We also develop a principled method to construct confidence intervals for the genetic effect that acknowledges the conditioning on statistical significance. Our approach is described in the specific context of odds ratios and logistic modeling but is more widely applicable. Application to recently published data sets demonstrates the relevance of our approach to modern genome scans.
机译:在现代的全基因组扫描中,使用严格的阈值来控制全基因组测试误差会扭曲估计过程,从而产生估计的效应大小,其平均大小可能远大于真实的效应大小。我们基于遗传效应的估计及其标准统计软件所报告的标准误差,引入一种方法来纠正病例对照研究中的这种偏见。我们的方法具有广泛的适用性,比竞争性方法容易实施,并且可能经常应用于已发布的研究而无需访问原始数据。我们通过对一系列遗传模型,次要等位基因频率和遗传效应大小的广泛模拟来评估我们方法的性能。与幼稚的估计程序相比,我们的方法减少了偏差和均方误差,尤其是对于中等效应大小。我们还开发了一种有原则的方法来构造对遗传效应的置信区间,该可信区间承认统计意义上的条件。我们的方法是在比值比和逻辑模型的特定上下文中描述的,但适用范围更广。在最近发布的数据集上的应用证明了我们的方法与现代基因组扫描的相关性。

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