Genetic association study of NF-κB genes in UK caucasian adult and juvenile onset idiopathic inflammatory myopathy

Hector Chinoy, Charles K C Li, Hazel Platt, Noreen Fertig, Hemlata Varsani, Harsha Gunawardena, Zoe Betteridge, Chester V. Oddis, Neil J. Mchugh, Lucy R. Wedderburn, William E R Ollier, Robert G. Cooper

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    Abstract

    Objective: Treatment-resistant muscle wasting is an increasingly recognized problem in idiopathic inflammatory myopathy (IIM). TNF-α is thought to induce muscle catabolism via activation of nuclear factor-kappa B (NF-κB). Several genes share homology with the NF-κB family of proteins. This study investigated the role of NF-κB-related genes in disease susceptibility in UK Caucasian IIM. Methods: Data from 362 IIM cases [274 adults, 49 (±14.0) years, 72% female; 88 juveniles, 6 (±3.6) years, 73% female) were compared with 307 randomly selected Caucasian controls. DNA was genotyped for 63 single nucleotide polymorphisms (SNPs) from NF-κB-related genes. Data were stratified by IIM subgroup/serotype. Results: A significant allele association was observed in the overall IIM group vs controls for the IKBL-62T allele (rs2071592, odds ratio 1.5, 95% CI 1.21, 1.89, corrected P = 0.0086), which strengthened after stratification by anti-Jo-1 or -PM-Scl antibodies. Genotype analysis revealed an increase for the AT genotype in cases under a dominant model. No other SNP was associated in the overall IIM group. Strong pairwise linkage disequilibrium was noted between IKBL-62T, TNF-308A and HLA-B*08 (D' = 1). Using multivariate regression, the IKBL-62T IIM association was lost after adjustment for TNF-308A or HLA-B*08. Conclusion: An association was noted between IKBL-62T and IIM, with increased risk noted in anti-Jo-1- and -PM-Scl antibody-positive patients. However, the IKBL-62T association is dependent on TNF-308A and HLA-B*08, due to strong shared linkage disequilibrium between these alleles. After adjustment of the 8.1 HLA haplotype, NF-κB genes therefore do not independently confer susceptibility in IIM. © The Author(s) 2011. Published by Oxford University Press on behalf of The British Society for Rheumatology.
    Original languageEnglish
    Article numberker379
    Pages (from-to)794-799
    Number of pages5
    JournalRheumatology
    Volume51
    Issue number5
    DOIs
    Publication statusPublished - May 2012

    Keywords

    • Autoantibodies
    • Dermatomyositis
    • Immunogenetics
    • NF-κB
    • Polymyositis
    • Single nucleotide polymorphisms
    • TNF

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