Using the realized relationship matrix to disentangle confounding factors for the estimation of genetic variance components of complex traits 英文参考文献.docVIP
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Using the realized relationship matrix to disentangle confounding factors for the estimation of genetic variance components of complex traits 英文参考文献
Lee et al. Genetics Selection Evolution 2010, 42:22
/content/42/1/22
Genetics
Selection
Evolution
RESEARCH
Open Access
Using the realized relationship matrix to Research
disentangle confounding factors for the estimation
of genetic variance components of complex traits
Sang Hong Lee*1, Michael E Goddard2,3, Peter M Visscher1 and Julius HJ van der Werf4
Abstract
Background: In the analysis of complex traits, genetic effects can be confounded with non-genetic effects, especially
when using full-sib families. Dominance and epistatic effects are typically confounded with additive genetic and non-
genetic effects. This confounding may cause the estimated genetic variance components to be inaccurate and biased.
Methods: In this study, we constructed genetic covariance structures from whole-genome marker data, and thus used
realized relationship matrices to estimate variance components in a heterogenous population of ~ 2200 mice for
which four complex traits were investigated. These mice were genotyped for more than 10,000 single nucleotide
polymorphisms (SNP) and the variances due to family, cage and genetic effects were estimated by models based on
pedigree information only, aggregate SNP information, and model selection for specific SNP effects.
Results and conclusions: We show that the use of genome-wide SNP information can disentangle confounding
factors to estimate genetic variances by separating genetic and non-genetic effects. The estimated variance
components using realized relationship were more accurate and less biased, compared to those based on pedigree
information only. Models that allow the selection of individual SNP in addition to fitting a relationship matrix are more
efficient for traits with a significant dominance variance.
Background
otide polymorphisms (SNP) across the whole genome,
and genome-wide association studies have been per-
formed in a number of species [12,13]. It is expected that
SNP and causal genes will be
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