AI Article Synopsis

  • Genetic mapping studies in mice and other model organisms aim to identify genes linked to complex traits but face limitations in resolution and polymorphisms using traditional methods.
  • Multiparent outbreeding populations, like Diversity Outbred (DO) mice, enhance genetic diversity and recombination but introduce new challenges in analysis, necessitating specialized software for accurate mapping.
  • A complete analytical pipeline, including methods for reconstructing founder haplotypes and adapting mapping for related animals, is provided through the R package DOQTL, with power analysis indicating different sample size requirements based on the effect size of the traits studied.

Article Abstract

Genetic mapping studies in the mouse and other model organisms are used to search for genes underlying complex phenotypes. Traditional genetic mapping studies that employ single-generation crosses have poor mapping resolution and limit discovery to loci that are polymorphic between the two parental strains. Multiparent outbreeding populations address these shortcomings by increasing the density of recombination events and introducing allelic variants from multiple founder strains. However, multiparent crosses present new analytical challenges and require specialized software to take full advantage of these benefits. Each animal in an outbreeding population is genetically unique and must be genotyped using a high-density marker set; regression models for mapping must accommodate multiple founder alleles, and complex breeding designs give rise to polygenic covariance among related animals that must be accounted for in mapping analysis. The Diversity Outbred (DO) mice combine the genetic diversity of eight founder strains in a multigenerational breeding design that has been maintained for >16 generations. The large population size and randomized mating ensure the long-term genetic stability of this population. We present a complete analytical pipeline for genetic mapping in DO mice, including algorithms for probabilistic reconstruction of founder haplotypes from genotyping array intensity data, and mapping methods that accommodate multiple founder haplotypes and account for relatedness among animals. Power analysis suggests that studies with as few as 200 DO mice can detect loci with large effects, but loci that account for <5% of trait variance may require a sample size of up to 1000 animals. The methods described here are implemented in the freely available R package DOQTL.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4169154PMC
http://dx.doi.org/10.1534/g3.114.013748DOI Listing

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