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Year

  • 2013 (1)

Author

  • Angeles-Han, Sheila (1)
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  • Secondary Appointment: Department of Pediatrics
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Article

Susceptibility to childhood onset rheumatoid arthritis: Investigation of a weighted genetic risk score that integrates cumulative effects of variants at five genetic loci

by Sampath Prahalad; Karen N Conneely; Yunxuan Jiang; Marc Sudman; Carol A. Wallace; Milton R Brown; Lori A. Ponder; Mina Rohani-Pichavant; Michael Zwick; David J Cutler; Sheila Angeles-Han; Larry B Vogler; Christine Kennedy; Kelly A. Rouster Stevens; Carol A. Wise; Marilynn Punaro; Ann M. Reed; Elizabeth D. Mellins; John F. Bohnsack; David N. Glass; Susan D. Thompson

2013

Subjects
  • Health Sciences, General
  • Health Sciences, Human Development
  • Biology, Genetics
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Abstract:Close

Objectives Children with rheumatoid-factor or anti-citrullinated peptide antibody positive juvenile idiopathic arthritis represent the childhood onset of RA (CORA). To test the hypothesis that adult-onset RA-associated variants are also associated with CORA, we investigated RA-associated variants at five loci in our CORA cohort. We also assessed the cumulative association of these variants in the susceptibility to CORA using a weighted genetic risk score (wGRS). Methods 155 children with CORA and 684 healthy controls were genotyped for five variants in PTPN22, TRAF1/C5, STAT4, and TNFAIP3 loci. High-resolution HLA-DRB1 genotypes were available for 149 cases and 373 controls. We tested each locus for association with CORA via logistic regression. We also computed a wGRS for each subject, with weights based on the natural log of the published odds ratios for the alleles investigated, and used logistic regression to test the wGRS for association with CORA. Results CORA was associated with TNFAIP3-rs10499194 [OR 0.60 (95%CI 0.44–0.83)], PTPN22-rs2476601 [OR 1.61 (1.11–2.31)], and STAT4-rs7574865 [OR 1.41 (1.06–1.87)] variants. The wGRS was significantly different between cases and controls (P<2×10−16). Individuals in the third to fifth quintiles of wGRS had a significantly increased disease risk compared to the baseline. Higher wGRS associated with increased risk of CORA, especially among males. Conclusions TNFAIP3, STAT4 and PTPN22 variants are associated with CORA in a similar magnitude and direction as in RA, suggesting that adult-onset RA and CORA share common genetic risk factors. Utilizing a wGRS, we have demonstrated the cumulative association of RA-associated variants in the susceptibility to CORA.
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