A multimetric approach to analysis of genome-wide association by single markers and composite likelihood.

Gibson, J; Tapper, W; Cox, D; Zhang, W; Pfeufer, A; Gieger, C; Wichmann, HE; Kääb, S; Collins, AR; Meitinger, T; Morton, N

doi:10.1073/pnas.0711903105

journal article

Dokumenttyp:: Journal Article; Research Support, N.I.H., Extramural; Article
Autor(en):: Gibson, J; Tapper, W; Cox, D; Zhang, W; Pfeufer, A; Gieger, C; Wichmann, HE; Kääb, S; Collins, AR; Meitinger, T; Morton, N
Titel:: A multimetric approach to analysis of genome-wide association by single markers and composite likelihood.
Abstract:: Two case/control studies with different phenotypes, marker densities, and microarrays were examined for the most significant single markers in defined regions. They show a pronounced bias toward exaggerated significance that increases with the number of observed markers and would increase further with imputed markers. This bias is eliminated by Bonferroni adjustment, thereby allowing combination by principal component analysis with a Malecot model composite likelihood evaluated by a permutation procedure to allow for multiple dependent markers. This intermediate value identifies the only demonstrated causal locus as most significant even in the preliminary analysis and clearly recognizes the strongest candidate in the other sample. Because the three metrics (most significant single marker, composite likelihood, and their principal component) are correlated, choice of the n smallest P values by each test gives <3n regions for follow-up in the next stage. In this way, methods with different response to marker selection and density are given approximately equal weight and economically compared, without expressing an untested prejudice or sacrificing the most significant results for any of them. Large numbers of cases, controls, and markers are by themselves insufficient to control type 1 and 2 errors, and so efficient use of multiple metrics with Bonferroni adjustment promises to be valuable in identifying causal variants and optimal design simultaneously.
Zeitschriftentitel:: Proc Natl Acad Sci U S A
Jahr:: 2008
Band / Volume:: 105
Heft / Issue:: 7
Seitenangaben Beitrag:: 2592-7
Sprache:: eng
Volltext / DOI:: doi:10.1073/pnas.0711903105
PubMed:: http://view.ncbi.nlm.nih.gov/pubmed/18268331
Print-ISSN:: 0027-8424
TUM Einrichtung:: Institut für Humangenetik
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