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Association of tumor necrosis factor α polymorphism, but not the shared epitope, with increased radiographic progression in a seropositive rheumatoid arthritis inception cohort

✍ Scribed by Dinesh Khanna; Hui Wu; Grace Park; Vivian Gersuk; Richard H. Gold; Gerald T. Nepom; Weng Kee Wong; John T. Sharp; Elaine F. Reed; Harold E. Paulus; Betty P. Tsao; Western Consortium of Practicing Rheumatologists

Publisher
John Wiley and Sons
Year
2006
Tongue
English
Weight
143 KB
Volume
54
Category
Article
ISSN
0004-3591

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✦ Synopsis

Abstract

Objective

To determine whether the tumor necrosis factor α (TNFA) –308 guanine‐to‐adenosine polymorphism and/or the shared epitope (SE) is associated with radiographic damage in patients with early rheumatoid arthritis (RA).

Methods

The cohort consisted of 189 patients with early seropositive RA (median 5.6 months since symptom onset) who had active disease, no previous disease‐modifying antirheumatic drug treatment, and ≥2 sets of scored radiographs of the hands/wrists and forefeet. TNFA –308 polymorphism was analyzed by polymerase chain reaction pyrosequencing. The SE was defined as presence of any 1 of the following HLA–DRB1 alleles: *0101, *0102, *0401, *0404, *0405, *0408, *0410, *1001, *1402, or *1406. Radiographic progression was assessed by the total Sharp score.

Results

Using a weighted least‐squares regression analysis, patients with the –308 TNFA AA plus AG genotypes (n = 49) had significantly higher rates of progression in erosion scores (median 0.84 versus 0.48 units/year), joint space narrowing (JSN) scores (0.42 versus 0.04), and total Sharp scores (1.70 versus 0.61) compared with patients with the TNFA GG genotype (n = 140). Presence of the SE (n = 137) was associated with significantly lower progression rates (per year) for total Sharp scores (median 0.9 versus 1.25 units/year) and JSN scores (0.04 versus 0.41), but not for erosion scores (0.50 versus 0.61) compared with patients without the SE (n = 52). In a least‐squares multiple linear regression model, the presence of the AA plus AG genotypes was associated with a significantly higher progression rate after adjusting for the presence of the SE, interaction between the SE and the AA plus AG genotypes, baseline log C‐reactive protein level, Health Assessment Questionnaire Disability Index, total Sharp score, swollen joint count, and presence of osteophytes (osteoarthritis). There was a strong linkage disequilibrium between DRB1*0301 and TNFA polymorphism (D′ = 0.84, r^2^ = 0.45, P < 0.001).

Conclusion

This study showed an association between the TNFA –308 polymorphism and progression of radiographic damage in patients with early seropositive RA. This association appeared to be independent of the SE, but might be dependent on other genetic variants in linkage disequilibrium with the –308 TNFA A allele and DRB1*0301. Further studies should be conducted to validate these results in both longitudinal observational cohorts and randomized clinical trials.

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Increased radiographic damage scores at
Increased radiographic damage scores at the onset of seropositive rheumatoid arthritis in older patients are associated with osteoarthritis of the hands, but not with more rapid progression of damage
✍ Dinesh Khanna; Veena K. Ranganath; John FitzGerald; Grace S. Park; Roy D. Altman 📂 Article 📅 2005 🏛 John Wiley and Sons 🌐 English ⚖ 124 KB 👁 1 views

## Abstract ## Objective To investigate the impact of patient age at symptom onset on radiographic joint damage at study entry, and on subsequent progression of damage in a cohort of patients with early seropositive rheumatoid arthritis (RA). ## Methods We studied 186 patients with RA of <15 mon