Literature DB >> 18814308

Power consequences of linkage disequilibrium variation between populations.

Yik Y Teo1, Kerrin S Small, Andrew E Fry, Yumeng Wu, Dominic P Kwiatkowski, Taane G Clark.   

Abstract

We quantify the degree to which LD differences exist in the human genome and investigates the consequences that variations in patterns of LD between populations can have on the power of case-control or family-trio association studies. Although only a small proportion of SNPs show significant LD differences (0.8-5%), these can introduce artificial signals of associations and reduce the power to detect true associations in case-control designs, even when meta-analytic approaches are used to account for stratification. We show that combining trios from different populations in the presence of significant LD differences can adversely affect power even though the number of trios has increased. Our results have implications on genetic studies conducted in populations with substantial population structure and show that the use of meta-analytic approaches or family-based designs to protect Type 1 error does not prevent loss of power due to differences in LD across populations.

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Mesh:

Year:  2009        PMID: 18814308      PMCID: PMC2997478          DOI: 10.1002/gepi.20366

Source DB:  PubMed          Journal:  Genet Epidemiol        ISSN: 0741-0395            Impact factor:   2.135


  42 in total

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10.  Classical sickle beta-globin haplotypes exhibit a high degree of long-range haplotype similarity in African and Afro-Caribbean populations.

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  16 in total

1.  Efficiency of trans-ethnic genome-wide meta-analysis and fine-mapping.

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2.  Genome-wide comparisons of variation in linkage disequilibrium.

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Review 3.  Genome-wide association studies in diverse populations.

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4.  A Bayesian approach using covariance of single nucleotide polymorphism data to detect differences in linkage disequilibrium patterns between groups of individuals.

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5.  Multiethnic genetic association studies improve power for locus discovery.

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6.  Singapore Genome Variation Project: a haplotype map of three Southeast Asian populations.

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7.  Genomewide association study of HLA alloimmunization in previously pregnant blood donors.

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8.  Host genetic and epigenetic factors in toxoplasmosis.

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9.  Candidate human genetic polymorphisms and severe malaria in a Tanzanian population.

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Review 10.  Methodological challenges of genome-wide association analysis in Africa.

Authors:  Yik-Ying Teo; Kerrin S Small; Dominic P Kwiatkowski
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