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Local false discovery rate and minimum total error rate approaches to identifying interesting chromosomal regions

机译:局部错误发现率和最小总错误率的方法来识别有趣的染色体区域

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摘要

The simultaneous testing of a large number of hypotheses in a genome scan, using individual thresholds for significance, inherently leads to inflated genome-wide false positive rates. There exist various approaches to approximating the correct genomewide p-values under various assumptions, either by way of asymptotics or simulations. We explore a philosophically different criterion, recently proposed in the literature, which controls the false discovery rate. The test statistics are assumed to arise from a mixture of distributions under the null and non-null hypotheses. We fit the mixture distribution using both a nonparametric approach and commingling analysis, and then apply the local false discovery rate to select cut-off points for regions to be declared interesting. Another criterion, the minimum total error, is also explored. Both criteria seem to be sensible alternatives to controlling the classical type I and type II error rates.
机译:使用重要性的单个阈值在基因组扫描中同时测试大量假设,必然会导致全基因组范围内的假阳性率升高。在各种假设下,有多种方法可以通过渐近或模拟来逼近正确的全基因组p值。我们探索了最近在文献中提出的控制错误发现率的哲学上不同的标准。假定检验统计量是根据零假设和非零假设下的分布混合得出的。我们使用非参数方法和混合分析来拟合混合物的分布,然后应用局部错误发现率来为要声明为感兴趣的区域选择截止点。还探讨了另一个准则,即最小总误差。这两个标准似乎都是控制经典I型和II型错误率的明智选择。

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