Rheumatoid arthritis risk allele <i>PTPRC</i> is also associated with response to anti–tumor necrosis factor α therapy

Jing Cui; Saedís Saevarsdóttir; Brian Thomson; Leonid Padyukov; Annette H M van der Helm–van Mil; Joanne Nititham; Laura B. Hughes; Niek de Vries; Soumya Raychaudhuri; Lars Alfredsson; Johan Askling; Sara Wedrén; Bo Ding; Candace Guiducci; Gertjan Wolbink; J. Bart A. Crusius; Irene van der Horst‐Bruinsma; Marieke M. J. Herenius; Michael E. Weinblatt; Nancy A. Shadick; Jane Worthington; Franak Batliwalla; Marlena Kern; Ann W Morgan; Anthony G. Wilson; John D. Isaacs; Kimme L Hyrich; Michael F. Seldin; Larry W. Moreland; Timothy W. Behrens; Cornelia F Allaart; Lindsey A. Criswell; T. Huizinga; Paul P. Tak; S. Louis Bridges; René E. M. Toes; Anne Barton; Lars Klareskog; Peter K. Gregersen; Elizabeth W. Karlson; Robert M. Plenge

doi:10.1002/art.27457

Rheumatoid arthritis risk allele <i>PTPRC</i> is also associated with response to anti–tumor necrosis factor α therapy

Jing Cui(Brigham and Women's Hospital), Saedís Saevarsdóttir(Karolinska University Hospital), Brian Thomson(Broad Institute), Leonid Padyukov(Karolinska University Hospital), Annette H M van der Helm–van Mil(Leiden University Medical Center), Joanne Nititham(University of California, San Francisco), Laura B. Hughes(University of Alabama at Birmingham), Niek de Vries(Amsterdam UMC Location University of Amsterdam), Soumya Raychaudhuri(Broad Institute), Lars Alfredsson(Karolinska Institutet), Johan Askling(Karolinska University Hospital), Sara Wedrén(Karolinska Institutet), Bo Ding(Karolinska Institutet), Candace Guiducci(Broad Institute), Gertjan Wolbink(Amsterdam UMC Location University of Amsterdam), J. Bart A. Crusius(Amsterdam UMC Location Vrije Universiteit Amsterdam), Irene van der Horst‐Bruinsma(Amsterdam UMC Location Vrije Universiteit Amsterdam), Marieke M. J. Herenius(Amsterdam UMC Location University of Amsterdam), Michael E. Weinblatt(Brigham and Women's Hospital), Nancy A. Shadick(Brigham and Women's Hospital), Jane Worthington(University of Manchester), Franak Batliwalla(Northwell Health), Marlena Kern(Northwell Health), Ann W Morgan(University of Leeds), Anthony G. Wilson(University of Sheffield), John D. Isaacs(Newcastle University), Kimme L Hyrich(University of Manchester), Michael F. Seldin(University of California, Davis), Larry W. Moreland(University of Pittsburgh Medical Center), Timothy W. Behrens, Cornelia F Allaart(Leiden University Medical Center), Lindsey A. Criswell(University of California, San Francisco), T. Huizinga(Leiden University Medical Center), Paul P. Tak(Amsterdam UMC Location University of Amsterdam), S. Louis Bridges(University of Alabama at Birmingham), René E. M. Toes(Leiden University Medical Center), Anne Barton(University of Manchester), Lars Klareskog(Karolinska University Hospital), Peter K. Gregersen(Northwell Health), Elizabeth W. Karlson(Brigham and Women's Hospital), Robert M. Plenge(Broad Institute)

Arthritis & Rheumatism

March 22, 2010

10.1002/art.27457

Cited by 125Open Access

Full Text

Abstract

OBJECTIVE: Anti-tumor necrosis factor alpha (anti-TNF) therapy is a mainstay of treatment in rheumatoid arthritis (RA). The aim of the present study was to test established RA genetic risk factors to determine whether the same alleles also influence the response to anti-TNF therapy. METHODS: A total of 1,283 RA patients receiving etanercept, infliximab, or adalimumab therapy were studied from among an international collaborative consortium of 9 different RA cohorts. The primary end point compared RA patients with a good treatment response according to the European League Against Rheumatism (EULAR) response criteria (n = 505) with RA patients considered to be nonresponders (n = 316). The secondary end point was the change from baseline in the level of disease activity according to the Disease Activity Score in 28 joints (triangle upDAS28). Clinical factors such as age, sex, and concomitant medications were tested as possible correlates of treatment response. Thirty-one single-nucleotide polymorphisms (SNPs) associated with the risk of RA were genotyped and tested for any association with treatment response, using univariate and multivariate logistic regression models. RESULTS: Of the 31 RA-associated risk alleles, a SNP at the PTPRC (also known as CD45) gene locus (rs10919563) was associated with the primary end point, a EULAR good response versus no response (odds ratio [OR] 0.55, P = 0.0001 in the multivariate model). Similar results were obtained using the secondary end point, the triangle upDAS28 (P = 0.0002). There was suggestive evidence of a stronger association in autoantibody-positive patients with RA (OR 0.55, 95% confidence interval [95% CI] 0.39-0.76) as compared with autoantibody-negative patients (OR 0.90, 95% CI 0.41-1.99). CONCLUSION: Statistically significant associations were observed between the response to anti-TNF therapy and an RA risk allele at the PTPRC gene locus. Additional studies will be required to replicate this finding in additional patient collections.

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