Immunogenetic risk and protective factors for juvenile dermatomyositis in Caucasians

Objective To define the relative importance (RI) of class II major histocompatibility complex (MHC) alleles and peptide binding motifs as risk or protective factors for juvenile dermatomyositis (DM), and to compare these with HLA associations in adult DM. Methods DRB1 and DQA1 typing was performed i...

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Bibliographic Details
Published in:Arthritis and rheumatism 2006-12, Vol.54 (12), p.3979-3987
Main Authors: Mamyrova, Gulnara, O'Hanlon, Terrance P., Monroe, Jason B., Carrick, Danielle Mercatante, Malley, James D., Adams, Sharon, Reed, Ann M., Shamim, Ejaz A., James‐Newton, Laura, Miller, Frederick W., Rider, Lisa G.
Format: Article
Language:English
Subjects:
Adolescent
Adult
Binding Sites
Biological and medical sciences
Dermatomyositis - diagnosis
Dermatomyositis - genetics
Dermatomyositis - immunology
European Continental Ancestry Group - genetics
Genetic Predisposition to Disease
Histocompatibility Testing
HLA-DQ alpha-Chains
HLA-DQ Antigens - genetics
HLA-DQ Antigens - immunology
HLA-DR Antigens - genetics
HLA-DR Antigens - immunology
HLA-DRB1 Chains
Humans
Medical sciences
Odds Ratio
Risk Factors
Sarcoidosis. Granulomatous diseases of unproved etiology. Connective tissue diseases. Elastic tissue diseases. Vasculitis
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Summary:Objective To define the relative importance (RI) of class II major histocompatibility complex (MHC) alleles and peptide binding motifs as risk or protective factors for juvenile dermatomyositis (DM), and to compare these with HLA associations in adult DM. Methods DRB1 and DQA1 typing was performed in 142 Caucasian patients with juvenile DM, and the results were compared with HLA typing data from 193 patients with adult DM and 797 race‐matched controls. Random Forests classification and multiple logistic regression were used to assess the RI of the HLA associations. Results The HLA–DRB1*0301 allele was a primary risk factor (odds ratio [OR] 3.9), while DQA1*0301 (OR 2.8), DQA1*0501 (OR 2.1), and homozygosity for DQA1*0501 (OR 3.2) were additional risk factors for juvenile DM. These risk factors were not present in patients with adult DM without defined autoantibodies. DQA1 alleles *0201 (OR 0.37), *0101 (OR 0.38), and *0102 (OR 0.51) were identified as novel protective factors for juvenile DM, the latter 2 also being protective factors in adult DM. The peptide binding motif DRB1 9EYSTS13 was a risk factor, and DQA1 motifs F25, S26, and 45(V/A)W(R/K)47 were protective. Random Forests classification analysis revealed that among the identified risk factors for juvenile DM, DRB1*0301 had a higher RI (100%) than DQA1*0301 (RI 57%), DQA1*0501 (RI 42%), or the peptide binding motifs. In a logistic regression model, DRB1*0301 and DQA1*0201 were the strongest risk and protective factors, respectively, for juvenile DM. Conclusion DRB1*0301 is ranked higher in RI than DQA1*0501 as a risk factor for juvenile DM. DQA1*0301 is a newly identified HLA risk factor for juvenile DM, while 3 of the DQA1 alleles studied are newly identified protective factors for juvenile DM.
ISSN:0004-3591
1529-0131
DOI:10.1002/art.22216