A high-resolution HLA and SNP haplotype map for disease association studies in the extended human MHC

被引:0
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作者
Paul I W de Bakker
Gil McVean
Pardis C Sabeti
Marcos M Miretti
Todd Green
Jonathan Marchini
Xiayi Ke
Alienke J Monsuur
Pamela Whittaker
Marcos Delgado
Jonathan Morrison
Angela Richardson
Emily C Walsh
Xiaojiang Gao
Luana Galver
John Hart
David A Hafler
Margaret Pericak-Vance
John A Todd
Mark J Daly
John Trowsdale
Cisca Wijmenga
Tim J Vyse
Stephan Beck
Sarah Shaw Murray
Mary Carrington
Simon Gregory
Panos Deloukas
John D Rioux
机构
[1] Program in Medical and Population Genetics,Department of Statistics
[2] Broad Institute of Harvard and MIT,Department of Medical Genetics
[3] Seven Cambridge Center,Department of Medicine
[4] Center for Human Genetic Research,undefined
[5] Massachusetts General Hospital,undefined
[6] University of Oxford,undefined
[7] Wellcome Trust Sanger Institute,undefined
[8] Wellcome Trust Centre for Human Genetics,undefined
[9] University of Oxford,undefined
[10] Complex Genetics Section,undefined
[11] University Medical Center,undefined
[12] Laboratory of Genomic Diversity,undefined
[13] SAIC-Frederick,undefined
[14] Inc. and National Cancer Institute–Frederick,undefined
[15] Illumina,undefined
[16] Inc.,undefined
[17] Center for Human Genetics,undefined
[18] Duke University Medical Center,undefined
[19] Center for Neurologic Diseases Brigham and Women's Hospital and Harvard Medical School,undefined
[20] Juvenile Diabetes Research Foundation/Wellcome Trust Diabetes and Inflammation Laboratory,undefined
[21] Cambridge Institute for Medical Research,undefined
[22] University of Cambridge,undefined
[23] Cambridge Institute for Medical Research,undefined
[24] Addensbrookes Hospital,undefined
[25] Imperial College of London,undefined
[26] Université de Montréal,undefined
[27] Montréal Heart Institute,undefined
来源
Nature Genetics | 2006年 / 38卷
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摘要
The proteins encoded by the classical HLA class I and class II genes in the major histocompatibility complex (MHC) are highly polymorphic and are essential in self versus non-self immune recognition. HLA variation is a crucial determinant of transplant rejection and susceptibility to a large number of infectious and autoimmune diseases1. Yet identification of causal variants is problematic owing to linkage disequilibrium that extends across multiple HLA and non-HLA genes in the MHC2,3. We therefore set out to characterize the linkage disequilibrium patterns between the highly polymorphic HLA genes and background variation by typing the classical HLA genes and >7,500 common SNPs and deletion-insertion polymorphisms across four population samples. The analysis provides informative tag SNPs that capture much of the common variation in the MHC region and that could be used in disease association studies, and it provides new insight into the evolutionary dynamics and ancestral origins of the HLA loci and their haplotypes.
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页码:1166 / 1172
页数:6
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