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When testing for replication of results from a primary study with two-sided hypotheses in a follow-up study, we are usually interested in discovering the features with discoveries in the same direction in the two studies. The direction of testing in the follow-up study for each feature can therefore be decided by the primary study. We prove that in this case the methods suggested in Heller, Bogomolov, and Benjamini (2014) for control over false replicability claims are valid. Specifically, we prove that if we input into the procedures in Heller, Bogomolov, and Benjamini (2014) the one-sided p-values in the directions favoured by the primary study, then we achieve directional control over the desired error measure (family-wise error rate or false discovery rate).
For a multivariate linear model, Wilks likelihood ratio test (LRT) constitutes one of the cornerstone tools. However, the computation of its quantiles under the null or the alternative requires complex analytic approximations and more importantly, th
We are concerned with testing replicability hypotheses for many endpoints simultaneously. This constitutes a multiple test problem with composite null hypotheses. Traditional $p$-values, which are computed under least favourable parameter configurati
Small study effects occur when smaller studies show different, often larger, treatment effects than large ones, which may threaten the validity of systematic reviews and meta-analyses. The most well-known reasons for small study effects include publi
Given a family of null hypotheses $H_{1},ldots,H_{s}$, we are interested in the hypothesis $H_{s}^{gamma}$ that at most $gamma-1$ of these null hypotheses are false. Assuming that the corresponding $p$-values are independent, we are investigating com
HIV-1C is the most prevalent subtype of HIV-1 and accounts for over half of HIV-1 infections worldwide. Host genetic influence of HIV infection has been previously studied in HIV-1B, but little attention has been paid to the more prevalent subtype C.