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Sources of variation in false discovery rate estimation include sample size correlation and inherent differences between groups

机译:错误发现率估计的变化源包括样本大小相关性以及组之间的固有差异

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摘要

BackgroundHigh-throughtput technologies enable the testing of tens of thousands of measurements simultaneously. Identification of genes that are differentially expressed or associated with clinical outcomes invokes the multiple testing problem. False Discovery Rate (FDR) control is a statistical method used to correct for multiple comparisons for independent or weakly dependent test statistics. Although FDR control is frequently applied to microarray data analysis, gene expression is usually correlated, which might lead to inaccurate estimates. In this paper, we evaluate the accuracy of FDR estimation.
机译:背景技术高通量技术可以同时测试数以万计的测量结果。鉴定差异表达或与临床结果相关的基因会引发多重检测问题。错误发现率(FDR)控制是一种统计方法,用于校正独立或弱相关测试统计数据的多次比较。尽管FDR控制经常用于微阵列数据分析,但是基因表达通常是相关的,这可能导致估算不准确。在本文中,我们评估了FDR估计的准确性。

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