Association analysis of the interleukin 17A gene in Caucasian rheumatoid arthritis patients from Norway and New Zealand

doi:10.1093/rheumatology/ken512

Rheumatology Advance Access originally published online on February 10, 2009
Rheumatology 2009 48(4):367-370; doi:10.1093/rheumatology/ken512

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Association analysis of the interleukin 17A gene in Caucasian rheumatoid arthritis patients from Norway and New Zealand

Gry B. N. Nordang¹, Marte K. Viken¹, Jade E. Hollis-Moffatt², Tony R. Merriman², Øystein T. Førre³, Knut Helgetveit⁴, Tore K. Kvien⁵^,6 and Benedicte A. Lie¹

¹Institute of Immunology, Rikshospitalet University Hospital, Oslo, Norway, ²Department of Biochemistry, University of Otago, Dunedin, New Zealand, ³Department of Rheumatology, Rikshospitalet University Hospital, Oslo, ⁴Martina Hansens Hospital, Sandvika, ⁵Department of Rheumatology, Diakonhjemmet Hospital, Oslo and ⁶Faculty of Medicine, University of Oslo, Oslo, Norway.

Correspondence to: Gry B. N. Nordang, Institute of Immunology, Rikshospitalet University Hospital, 0027 Oslo, Norway. E-mail: gry.namlos.nordang{at}rr-research.no

Abstract

Objective. Elevated levels of IL-17A have been detected in theinflamed synovium of RA patients, and murine arthritis modelsdeficient in IL17A have shown reduced inflammation. Our aimwas to investigate IL17A as a candidate gene for RA, and toassess correlations between risk variants and disease phenotypes.

Methods. Five single nucleotide polymorphisms (SNPs) were selectedto tag the genetic variability of the IL17A region and weregenotyped by TaqMan technology on 950 RA cases and 933 randomcontrols from Norway. Associations to progression of radiographicdamage and presence of autoantibodies were examined in a 10-yrfollow-up cohort of early RA. In addition, 580 RA patients and504 controls from New Zealand were used as a replication dataset.

Results. A weak association between RA and the promoter SNPrs2275913 [odds ratio (OR) = 1.17; 95% CI 1.02, 1.34; P = 0.02]was found in the Norwegian population. The association was alsoevident at the genotype level where it indicated a recessivemodel. The allelic association was not replicated in the RAcohort from New Zealand (OR = 0.96; 95% CI 0.81, 1.16; P = 0.69).However, combined analysis suggested a weak recessive association(OR = 1.19; 95% CI 1.02, 1.37; P = 0.02). No significant associationswere observed with radiographic progression, anti-cyclic citrullinatedpeptide or IgM-RF.

Conclusions. Modest evidence of an association with IL17A inNorwegian RA patients was observed. Although, our findings werenot replicated in an independent RA material from New Zealand,a significant common risk estimate indicated that IL17A warrantsfurther investigation in RA.

KEY WORDS: RA, IL17A, Genetic predisposition

Submitted 20 August 2008; revised version accepted 19 December 2008.
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