A new multimarker test for family-based association studies

## Abstract Genetic association is often determined in case‐control studies by the differential distribution of alleles or genotypes. Recent work has demonstrated that association can also be assessed by deviations from the expected distributions of alleles or genotypes. Specifically, multiple meth

## Abstract Family‐based study designs have an important role in the search for association between disease phenotypes and genetic markers. Unlike traditional case‐control methods, family‐based tests use within‐family data to avoid identification of spurious associations that may result from popula

In case-control genetic association studies, the robust procedure, Pearson's Chi-square test, is commonly used for testing association between disease status and genetic markers. However, this test does not take the possible trend of relative risks, which are due to genotype, into account. On the co

Linkage disequilibrium (LD) of genetic loci is routinely estimated and graphically illustrated in genetic association studies. It has been suggested that the information in LD is also useful for association mapping and genetic association can be detected by comparing LD patterns between cases and co

## Abstract We present a class of family‐based association tests (FBATs) for ordinal traits that adjust for the effects of covariates. For complex diseases, especially mental health conditions including nicotine dependence and substance use, the outcome variables are often recorded in an ordinal ra

## Abstract We address the analytical problem of evaluating the evidence for linkage at a test locus while taking into account the effect of a known linked disease locus. The method we propose is a multimarker regression approach that models the identity‐by‐descent states for affected sib‐pairs at