Please use this identifier to cite or link to this item: https://hdl.handle.net/1959.11/22064
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dc.contributor.authorLee, Sang Hongen
dc.contributor.authorYang, Jen
dc.contributor.authorGoddard, M Een
dc.contributor.authorVisscher, P Men
dc.contributor.authorWray, N Ren
dc.date.accessioned2017-10-27T14:55:00Z-
dc.date.issued2012-
dc.identifier.citationBioinformatics, 28(19), p. 2540-2542en
dc.identifier.issn1367-4811en
dc.identifier.issn1367-4803en
dc.identifier.urihttps://hdl.handle.net/1959.11/22064-
dc.description.abstractGenetic correlations are the genome-wide aggregate effects of causal variants affecting multiple traits. Traditionally, genetic correlations between complex traits are estimated from pedigree studies, but such estimates can be confounded by shared environmental factors. Moreover, for diseases, low prevalence rates imply that even if the true genetic correlation between disorders was high, co-aggregation of disorders in families might not occur or could not be distinguished from chance. We have developed and implemented statistical methods based on linear mixed models to obtain unbiased estimates of the genetic correlation between pairs of quantitative traits or pairs of binary traits of complex diseases using population-based case-control studies with genome-wide single-nucleotide polymorphism data. The method is validated in a simulation study and applied to estimate genetic correlation between various diseases from Wellcome Trust Case Control Consortium data in a series of bivariate analyses. We estimate a significant positive genetic correlation between risk of Type 2 diabetes and hypertension of ~0.31 (SE 0.14, P = 0.024).en
dc.languageenen
dc.publisherOxford University Pressen
dc.relation.ispartofBioinformaticsen
dc.titleEstimation of pleiotropy between complex diseases using single-nucleotide polymorphism-derived genomic relationships and restricted maximum likelihooden
dc.typeJournal Articleen
dc.identifier.doi10.1093/bioinformatics/bts474en
dcterms.accessRightsGolden
dc.subject.keywordsGene Expression (incl. Microarray and other genome-wide approaches)en
local.contributor.firstnameSang Hongen
local.contributor.firstnameJen
local.contributor.firstnameM Een
local.contributor.firstnameP Men
local.contributor.firstnameN Ren
local.subject.for2008060405 Gene Expression (incl. Microarray and other genome-wide approaches)en
local.subject.seo2008920110 Inherited Diseases (incl. Gene Therapy)en
local.profile.schoolSchool of Environmental and Rural Scienceen
local.profile.emailslee38@une.edu.auen
local.output.categoryC1en
local.record.placeauen
local.record.institutionUniversity of New Englanden
local.identifier.epublicationsrecordune-20171024-181657en
local.publisher.placeUnited Kingdomen
local.format.startpage2540en
local.format.endpage2542en
local.peerreviewedYesen
local.identifier.volume28en
local.identifier.issue19en
local.access.fulltextYesen
local.contributor.lastnameLeeen
local.contributor.lastnameYangen
local.contributor.lastnameGoddarden
local.contributor.lastnameVisscheren
local.contributor.lastnameWrayen
dc.identifier.staffune-id:slee38en
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.identifier.unepublicationidune:22254en
local.identifier.handlehttps://hdl.handle.net/1959.11/22064en
dc.identifier.academiclevelAcademicen
local.title.maintitleEstimation of pleiotropy between complex diseases using single-nucleotide polymorphism-derived genomic relationships and restricted maximum likelihooden
local.output.categorydescriptionC1 Refereed Article in a Scholarly Journalen
local.search.authorLee, Sang Hongen
local.search.authorYang, Jen
local.search.authorGoddard, M Een
local.search.authorVisscher, P Men
local.search.authorWray, N Ren
local.uneassociationUnknownen
local.year.published2012en
local.subject.for2020310505 Gene expression (incl. microarray and other genome-wide approaches)en
local.subject.seo2020200101 Diagnosis of human diseases and conditionsen
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