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Large-scale SNP analysis reveals clustered and continuous patterns of human genetic variation

Authors :
Shriver Mark D
Mei Rui
Parra Esteban J
Sonpar Vibhor
Halder Indrani
Tishkoff Sarah A
Schurr Theodore G
Zhadanov Sergev I
Osipova Ludmila P
Brutsaert Tom D
Friedlaender Jonathan
Jorde Lynn B
Watkins W Scott
Bamshad Michael J
Gutierrez Gerardo
Loi Halina
Matsuzaki Hajime
Kittles Rick A
Argyropoulos George
Fernandez Jose R
Akey Joshua M
Jones Keith W
Source :
Human Genomics, Vol 2, Iss 2, Pp 81-89 (2005)
Publication Year :
2005
Publisher :
BMC, 2005.

Abstract

Abstract Understanding the distribution of human genetic variation is an important foundation for research into the genetics of common diseases. Some of the alleles that modify common disease risk are themselves likely to be common and, thus, amenable to identification using gene-association methods. A problem with this approach is that the large sample sizes required for sufficient statistical power to detect alleles with moderate effect make gene-association studies susceptible to false-positive findings as the result of population stratification 12. Such type I errors can be eliminated by using either family-based association tests or methods that sufficiently adjust for population stratification 345. These methods require the availability of genetic markers that can detect and, thus, control for sources of genetic stratification among populations. In an effort to investigate population stratification and identify appropriate marker panels, we have analysed 11,555 single nucleotide polymorphisms in 203 individuals from 12 diverse human populations. Individuals in each population cluster to the exclusion of individuals from other populations using two clustering methods. Higher-order branching and clustering of the populations are consistent with the geographic origins of populations and with previously published genetic analyses. These data provide a valuable resource for the definition of marker panels to detect and control for population stratification in population-based gene identification studies. Using three US resident populations (European-American, African-American and Puerto Rican), we demonstrate how such studies can proceed, quantifying proportional ancestry levels and detecting significant admixture structure in each of these populations.

Details

Language :
English
ISSN :
14797364
Volume :
2
Issue :
2
Database :
Directory of Open Access Journals
Journal :
Human Genomics
Publication Type :
Academic Journal
Accession number :
edsdoj.6b7917520ca4d44acec2e245416e58b
Document Type :
article
Full Text :
https://doi.org/10.1186/1479-7364-2-2-81