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dc.contributor.author방소영-
dc.date.accessioned2018-03-23T08:45:05Z-
dc.date.available2018-03-23T08:45:05Z-
dc.date.issued2014-04-
dc.identifier.citationAmerican journal of human genetics , Vol.94 No.4 [2014] , 586-598en_US
dc.identifier.issn0002-9297-
dc.identifier.urihttps://linkinghub.elsevier.com/retrieve/pii/S0002929714001104-
dc.identifier.urihttp://hdl.handle.net/20.500.11754/51646-
dc.description.abstractEfforts to identify lupus-associated causal variants in the FAM167A/BLK locus on 8p21 are hampered by highly associated noncausal variants. In this report, we used a trans-population mapping and sequencing strategy to identify a common variant (rs922483) in the proximal BLK promoter and a tri-allelic variant (rs1382568) in the upstream alternative BLK promoter as putative causal variants for association with systemic lupus erythematosus. The risk allele (T) at rs922483 reduced proximal promoter activity and modulated alternative promoter usage. Allelic differences at rs1382568 resulted in altered promoter activity in B progenitor cell lines. Thus, our results demonstrated that both lupus-associated functional variants contribute to the autoimmune disease association by modulating transcription of BLK in B cells and thus potentially altering immune responses.en_US
dc.description.sponsorshipThe authors declare the following competing financial interests:H.S., T.W.B., and R.R.G. are full-time employees of Genentech.We thank all individuals who participated in this study and theresearch assistants, coordinators, and physicians who helped inthe recruitment of subjects. We thank Peter K. Gregersen forproviding genotyping controls and cases and controls from theABCoN and NYCP collections. We thank the members of theBIOLUPUS Network (see consortium section) for providing samplesused in this study. We thank Mary C. Comeau; MirandaC. Marion; Paula S. Ramos; Adam Adler; Stuart Glenn, and MaiLi Zhu for assistance in genotyping, quality-control analyses,and clinical-data management; J. Donald Capra for critical readingof the manuscript; Julie M. Robertson for scientific editing; and thestaff of the Oklahoma Rheumatic Disease Resources Cores Centerfor collecting and maintaining the samples. The content of thispublication is solely the responsibility of the authors and doesnot necessarily represent the official views of the NIH or any otherfunding organization. Specific NIH grant numbers and other fundinginformation can be found in the supplemental materials.en_US
dc.language.isoenen_US
dc.publisherElsevier Science B.V., Amsterdamen_US
dc.subject자연과학en_US
dc.subject유전학en_US
dc.subject생물학en_US
dc.titleTwo Functional Lupus-Associated BLK Promoter Variants Control Cell-Type- and Developmental-Stage-Specific Transcriptionen_US
dc.typeArticleen_US
dc.relation.no4-
dc.relation.volume94-
dc.identifier.doi10.1016/j.ajhg.2014.03.008-
dc.relation.page586-598-
dc.relation.journalAMERICAN JOURNAL OF HUMAN GENETICS-
dc.contributor.googleauthorGuthridge, J. M.-
dc.contributor.googleauthorLu, R.-
dc.contributor.googleauthorSun, H.-
dc.contributor.googleauthorSun, C.-
dc.contributor.googleauthorWiley, G. B.-
dc.contributor.googleauthorDominguez, N.-
dc.contributor.googleauthorMacwana, S. R.-
dc.contributor.googleauthorLessard, C. J.-
dc.contributor.googleauthorKim-Howard, X.-
dc.contributor.googleauthorCobb, B. L.-
dc.relation.code2014024671-
dc.sector.campusS-
dc.sector.daehakCOLLEGE OF MEDICINE[S]-
dc.sector.departmentDEPARTMENT OF MEDICINE-
dc.identifier.pidsybang-
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