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A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains

The classic diallel takes a set of parents and produces offspring from all possible mating pairs. Phenotype values among the offspring can then be related back to their respective parentage. When the parents are diploid, sexed, and inbred, the diallel can characterize aggregate effects of genetic ba...

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Autores principales: Lenarcic, Alan B., Svenson, Karen L., Churchill, Gary A., Valdar, William
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Genetics Society of America 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3276624/
https://www.ncbi.nlm.nih.gov/pubmed/22345610
http://dx.doi.org/10.1534/genetics.111.132563
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author Lenarcic, Alan B.
Svenson, Karen L.
Churchill, Gary A.
Valdar, William
author_facet Lenarcic, Alan B.
Svenson, Karen L.
Churchill, Gary A.
Valdar, William
author_sort Lenarcic, Alan B.
collection PubMed
description The classic diallel takes a set of parents and produces offspring from all possible mating pairs. Phenotype values among the offspring can then be related back to their respective parentage. When the parents are diploid, sexed, and inbred, the diallel can characterize aggregate effects of genetic background on a phenotype, revealing effects of strain dosage, heterosis, parent of origin, epistasis, and sex-specific versions thereof. However, its analysis is traditionally intricate, unforgiving of unplanned missing information, and highly sensitive to imbalance, making the diallel unapproachable to many geneticists. Nonetheless, imbalanced and incomplete diallels arise frequently, albeit unintentionally, as by-products of larger-scale experiments that collect F(1) data, for example, pilot studies or multiparent breeding efforts such as the Collaborative Cross or the Arabidopsis MAGIC lines. We present a general Bayesian model for analyzing diallel data on dioecious diploid inbred strains that cleanly decomposes the observed patterns of variation into biologically intuitive components, simultaneously models and accommodates outliers, and provides shrinkage estimates of effects that automatically incorporate uncertainty due to imbalance, missing data, and small sample size. We further present a model selection procedure for weighing evidence for or against the inclusion of those components in a predictive model. We evaluate our method through simulation and apply it to incomplete diallel data on the founders and F(1)'s of the Collaborative Cross, robustly characterizing the genetic architecture of 48 phenotypes.
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spelling pubmed-32766242012-02-24 A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains Lenarcic, Alan B. Svenson, Karen L. Churchill, Gary A. Valdar, William Genetics Mouse Genetic Resources The classic diallel takes a set of parents and produces offspring from all possible mating pairs. Phenotype values among the offspring can then be related back to their respective parentage. When the parents are diploid, sexed, and inbred, the diallel can characterize aggregate effects of genetic background on a phenotype, revealing effects of strain dosage, heterosis, parent of origin, epistasis, and sex-specific versions thereof. However, its analysis is traditionally intricate, unforgiving of unplanned missing information, and highly sensitive to imbalance, making the diallel unapproachable to many geneticists. Nonetheless, imbalanced and incomplete diallels arise frequently, albeit unintentionally, as by-products of larger-scale experiments that collect F(1) data, for example, pilot studies or multiparent breeding efforts such as the Collaborative Cross or the Arabidopsis MAGIC lines. We present a general Bayesian model for analyzing diallel data on dioecious diploid inbred strains that cleanly decomposes the observed patterns of variation into biologically intuitive components, simultaneously models and accommodates outliers, and provides shrinkage estimates of effects that automatically incorporate uncertainty due to imbalance, missing data, and small sample size. We further present a model selection procedure for weighing evidence for or against the inclusion of those components in a predictive model. We evaluate our method through simulation and apply it to incomplete diallel data on the founders and F(1)'s of the Collaborative Cross, robustly characterizing the genetic architecture of 48 phenotypes. Genetics Society of America 2012-02 /pmc/articles/PMC3276624/ /pubmed/22345610 http://dx.doi.org/10.1534/genetics.111.132563 Text en Copyright © 2012 by the Genetics Society of America Available freely online through the author-supported open access option.
spellingShingle Mouse Genetic Resources
Lenarcic, Alan B.
Svenson, Karen L.
Churchill, Gary A.
Valdar, William
A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title_full A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title_fullStr A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title_full_unstemmed A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title_short A General Bayesian Approach to Analyzing Diallel Crosses of Inbred Strains
title_sort general bayesian approach to analyzing diallel crosses of inbred strains
topic Mouse Genetic Resources
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3276624/
https://www.ncbi.nlm.nih.gov/pubmed/22345610
http://dx.doi.org/10.1534/genetics.111.132563
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