Literature DB >> 15088268

Design and analysis of admixture mapping studies.

C J Hoggart1, M D Shriver, R A Kittles, D G Clayton, P M McKeigue.   

Abstract

Admixture between populations originating on different continents can be exploited to detect disease susceptibility loci at which risk alleles are distributed differentially between these populations. We first examine the statistical power and mapping resolution of this approach in the limiting situation in which gamete admixture and locus ancestry are measured without uncertainty. We show that, for a rare disease, the most efficient design is to study affected individuals only. In a typical African American population (two-way admixture proportions 0.8/0.2, ancestry crossover rate 2 per 100 cM), a study of 800 affected individuals has 90% power to detect at P values <10(-5) a locus that generates a risk ratio of 2 between populations, with an expected mapping resolution (size of 95% confidence region for the position of the locus) of 4 cM. In practice, to infer locus ancestry from marker data requires Bayesian computationally intensive methods, as implemented in the program ADMIXMAP. Affected-only study designs require strong prior information on the frequencies of each allele given locus ancestry. We show how data from unadmixed and admixed populations can be combined to estimate these ancestry-specific allele frequencies within the admixed population under study, allowing for variation between allele frequencies in unadmixed and admixed populations. Using simulated data based on the genetic structure of the African American population, we show that 60% of information can be extracted in a test for linkage using markers with an ancestry information content of 36% at 3-cM spacing. As in classic linkage studies, the most efficient strategy is to use markers at a moderate density for an initial genome search and then to saturate regions of putative linkage with additional markers, to extract nearly all information about locus ancestry.

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Year:  2004        PMID: 15088268      PMCID: PMC1181989          DOI: 10.1086/420855

Source DB:  PubMed          Journal:  Am J Hum Genet        ISSN: 0002-9297            Impact factor:   11.025


  22 in total

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4.  Bayesian mapping of multiple quantitative trait loci from incomplete outbred offspring data.

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Review 6.  Analysis of multilocus models of association.

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Review 8.  Gene mapping in the 20th and 21st centuries: statistical methods, data analysis, and experimental design.

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9.  Skin pigmentation, biogeographical ancestry and admixture mapping.

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10.  Relation of risk of systemic lupus erythematosus to west African admixture in a Caribbean population.

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  170 in total

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2.  Statistical tests for admixture mapping with case-control and cases-only data.

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Journal:  Am J Hum Genet       Date:  2004-09-22       Impact factor: 11.025

Review 3.  Prospects for admixture mapping of complex traits.

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6.  Fast and accurate inference of local ancestry in Latino populations.

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Journal:  Bioinformatics       Date:  2012-04-11       Impact factor: 6.937

7.  Admixture mapping of lung cancer in 1812 African-Americans.

Authors:  Ann G Schwartz; Angela S Wenzlaff; Cathryn H Bock; Julie J Ruterbusch; Wei Chen; Michele L Cote; Amanda S Artis; Alison L Van Dyke; Susan J Land; Curtis C Harris; Sharon R Pine; Margaret R Spitz; Christopher I Amos; Albert M Levin; Paul M McKeigue
Journal:  Carcinogenesis       Date:  2010-11-29       Impact factor: 4.944

8.  Adjustment for local ancestry in genetic association analysis of admixed populations.

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10.  Assessing the relative ages of admixture in the bovine hybrid zones of Africa and the Near East using X chromosome haplotype mosaicism.

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