HMOX1 promoter polymorphism modulates the relationship between disease activity and joint damage in rheumatoid arthritis.
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Publication year
2008Author(s)
Number of pages
6 p.
Source
Arthritis and Rheumatism, 58, 11, (2008), pp. 3388-3393ISSN
Publication type
Article / Letter to editor
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Organization
Pharmacology-Toxicology
Human Genetics
Rheumatology
IMM - Institute for Molecules and Materials
Former Organization
Pharmacology/Toxicology
Journal title
Arthritis and Rheumatism
Volume
vol. 58
Issue
iss. 11
Page start
p. 3388
Page end
p. 3393
Subject
DCN 2: Functional Neurogenomics; EBP 1: Determinants in Health and Disease; EBP 2: Effective Hospital Care; IGMD 9: Renal disorder; N4i 1: Pathogenesis and modulation of inflammation; N4i 4: Auto-immunity, transplantation and immunotherapy; NCEBP 2: Evaluation of complex medical interventions; NCMLS 1: Infection and autoimmunity; NCMLS 2: Metabolism, transport and motion; NCMLS 5: Membrane transport and intracellular motility; Synthetic Organic Chemistry; UMCN 4.2: Chronic inflammation and autoimmunity; UMCN 5.1: Genetic defects of metabolism; UMCN 5.4: Renal disordersAbstract
OBJECTIVE: The guanine-thymidine (GT)n repeat in the HMOX1 promoter determines the level of induction of the heme-degrading enzyme heme oxygenase 1 (HO-1), which protects against inflammatory and oxidative stress. In individuals with short (GT)n repeats (where n < 25; SS genotype), higher levels of HO-1 activity are induced more rapidly than in those with long (GT)n repeats (where n > or = 25; LL genotype). Recently, it was demonstrated that HO-1 activity protects against the onset of rheumatoid arthritis (RA). The aim of this study was to determine whether the (GT)n-repeat length within the HMOX1 promoter region is associated with RA disease severity and radiographic joint damage. METHODS: A cohort of 325 well-characterized RA patients and 273 controls was investigated by DNA fragment-length analysis for the association of (GT)n repeats in the HMOX1 promoter region with RA disease susceptibility and severity. RESULTS: Although no significant differences in genotype or allele frequency were found between controls and RA patients, the odds ratios corresponded well to those in the previously described cohort. Among patients, those carrying the SS genotype had a more favorable radiographic outcome over 9 years than those carrying the LL genotype. This was unexpected since no differences in disease activity were found between the genotypes or alleles. CONCLUSION: Patients with the SS genotype have a better long-term radiographic outcome despite poor prognostic markers at baseline and despite disease activity at followup similar to that of patients with the LL genotype. This suggests that the HMOX1/HO-1 system is involved in the uncoupling of disease activity and joint damage and may provide a novel target for the treatment of RA.
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