Microsatellite typing for DRB1 alleles: application to the analysis of HLA associations with rheumatoid arthritis

被引:0
|
作者
H-S Lee
W Li
A Lee
P Rodine
R R Graham
W A Ortmann
F Batliwalla
K W Lee
S C Bae
T W Behrens
P K Gregersen
机构
[1] Feinstein Institute for Medical Research,Department of Medicine, Division of Rheumatic and Autoimmune Diseases
[2] North Shore LIJ Health System,undefined
[3] University of Minnesota Medical School,undefined
[4] Program in Medical and Population Genetics,undefined
[5] Broad Institute of Harvard and the Massachusetts Institute of Technology,undefined
[6] The Center for Human Genetics Research and Molecular Biology,undefined
[7] Massachusetts General Hospital,undefined
[8] Hallym Institution for Genome Application,undefined
[9] Hallym University Sacred Heart Hospital,undefined
[10] Hanyang University College of Medicine,undefined
[11] Hospital for Rheumatic Diseases,undefined
来源
Genes & Immunity | 2006年 / 7卷
关键词
microsatellite typing; HLA-DRBI; rheumatoid arthritis;
D O I
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中图分类号
学科分类号
摘要
The current methods for molecular typing of HLA-DR alleles incur a substantial financial burden when performing large population studies. In the current study, we aimed to provide much less expensive typing approach with high predictability for DRB1 genotype. We have used a panel of three microsatellite markers in the class II region (D6S2666, D6S2665 and D6S2446) for genotyping and haplotype reconstruction in a total of 1687 Caucasian (1313 RA patients and 374 controls) and 1364 Korean individuals (744 RA patients and 620 controls), all of whom were previously genotyped for DRB1. We found that a total of 88.4 and 87.4% of all observed three-marker haplotypes could determine the DR type with a positive predictive value >0.8 with high sensitivity and specificity. There was a high degree of haplotype conservation when comparing Caucasian and Asian populations. Interestingly, we found that the majority of DRB1*09 and DRB1*10 alleles share a common three-marker haplotype in both Caucasian and Asian populations. This is unexpected, since these two alleles are found on very different haplotype families. In addition, these two alleles are both associated with rheumatoid arthritis, making the elucidation of these haplotype relationships potentially important for understanding disease susceptibility.
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页码:533 / 543
页数:10
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