Limits of fine-mapping a quantitative trait

## Abstract When a novel genetic trait arises in a population, it introduces a signal in the haplotype distribution of that population. Through recombination that signal's history becomes differentiated from the DNA distant to it, but remains similar to the DNA close by. Fine‐scale mapping techniqu

We discuss analyses of Genetic Analysis Workshop 14 data from the Collaborative Study on the Genetics of Alcoholism (COGA) as well as from a simulated complex disease, Kofendrerd personality disorder (KPD), with both genetic and phenotypic heterogeneity. Both data sets included numerous related phen

Sib pairs were selectively sampled for extreme concordance or discordance for the quantitative trait Q1, a simulated phenotype (GAW10). Two selective sampling criteria were used (SC1 and SC2), and results for these were compared to linkage analyses using all pairs (ALL). In total 773 sib pairs were

## Abstract In this paper, bivariate/multivariate variance component models are proposed for high‐resolution combined linkage and association mapping of quantitative trait loci (QTL), based on combinations of pedigree and population data. Suppose that a quantitative trait locus is located in a chro

## Abstract Fulker and Cardon's interval mapping extension of Haseman and Elston's sib‐pair linkage method was used to map loci affecting the quantitative phenotypes presented as part of Problem 2, both adjusted and not adjusted for covariates: Q1 was adjusted for age and the environmental factor (