The posterior probability of linkage allowing for linkage disequilibrium and a new estimate of disequilibrium between a trait and a marker

被引:26
|
作者
Yang, XQ
Huang, J
Logue, MW
Vieland, VJ
机构
[1] Univ Iowa, Ctr Stat Genet Res, Iowa City, IA 52242 USA
[2] Univ Iowa, Dept Biostat, Iowa City, IA 52242 USA
[3] Univ Iowa, Dept Stat & Actuarial Sci, Iowa City, IA 52242 USA
[4] Univ Iowa, Dept Psychiat, Iowa City, IA 52242 USA
[5] Univ Iowa, Dept Publ Hlth Genet, Iowa City, IA 52242 USA
关键词
trait-marker linkage disequilibrium; disequilibrium estimation; posterior probability of linkage; Bayesian linkage analysis;
D O I
10.1159/000086699
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
The posterior probability of linkage (PPL) statistic has been developed as a method for the rigorous accumulation of evidence for or against linkage allowing for both intra- and inter-sample heterogeneity. To date, the method has assumed linkage equilibrium between alleles at the trait locus and the marker locus. We now generalize the PPL to allow for linkage disequilibrium (ILD), by incorporating variable phase probabilities into the underlying linkage likelihood. This enables us to recover the marginal posterior density of the recombination fraction, integrating out nuisance parameters of the trait model, including the locus heterogeneity (admixture) parameter, as well as a vector of LID parameters. The marginal posterior density can then be updated across data subsets or new data as they become available, while allowing parameters of the trait model to vary between data sets. The method applies immediately to general pedigree structures and to markers with multiple alleles. In the case of SNPs, the likelihood is parameterized in terms of the standard single LD parameter D'; and it therefore affords a mechanism for estimation of D' between the marker and the trait, again, without fixing the parameters of the trait model and allowing for updating across data sets. It is even possible to allow for a different associated allele in different populations, while accumulating information regarding the strength of LD. While a computationally efficient implementation for multi-allelic markers is still in progress, we have implemented a version of this new LD-PPL for SNPs and evaluated its performance in nuclear families. Our simulations show that LD-PPLs tend to be larger than PPLs (stronger evidence in favor of linkage/LD) with increased LD level, under a variety of generating models; while in the absence of linkage and LD, LD-PPLs tend to be smaller than PPLs (stronger evidence against linkage). The estimate of D' also behaves well even in relatively small, heterogeneous samples.
引用
收藏
页码:210 / 219
页数:10
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