Identification of Secreted Phosphoprotein 1 Gene as a new Rheumatoid Arthritis Susceptibility Gene

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Gazal, Steven | Sacre, Karim | Allanore, Yannick | Teruel, Maria | Goodall, Alison, H | Tohma, Shigeto | Alfredsson, Lars | Okada, Yukinori | Xie, Gang | Constantin, Arnaud | Balsa, Alejandro | Kawasaki, Aya | Nicaise, Pascale | Amos, Christopher | Rodriguez-Rodriguez, Luis | Chioccia, Gilles | Boileau, Catherine | Zhang, Jinyi | Vittecoq, Olivier | Barnetche, Thomas | Gonzalez Gay, Miguel, A. | Furukawa, Hiroshi | Cantagrel, Alain | Le Loët, Xavier | Sumida, Takayuki | Hurtado-Nedelec, Margarita | Richez, Christophe | Chollet-Martin, Sylvie | Schaeverbeke, Thierry | Combe, Bernard | Khoryati, Liliane | Coustet, Baptiste | Siminovitch, Katherine | Plenge, Robert | Padyukov, Leonid | Martin, Javier | Tsuchiya, Naoyuki | Dieudé, Philippe

Edité par CCSD ; BMJ Publishing Group -

International audience. Objective To evaluate the contribution of the SPP1 rs11439060 and rs9138 polymorphisms, previously reported as autoimmune risk variants, in the RA genetic background according to anti-citrullinated protein antibodies (ACPAs) status of RA individuals. Methods We analyzed a total of 11,715 RA cases and 26,493 controls from 9 independent cohorts, all individuals were genotyped or had imputed genotypes for SPP1 rs11439060 and rs9138. The effect of the SPP1 rs11439060 and rs9138 risk-allele combination on OPN expression in macrophages and OPN serum levels was investigated. Results We provide evidence for a distinct contribution of SPP1 to RA susceptibility according to ACPA status: the combination of ≥ 3 SPP1 rs11439060 and rs9138 common alleles was associated mainly with ACPA negativity (P = 1.29x10-5, ORACPA-negative 1.257 1.135–1.394) and less with ACPA positivity (P = 0.0148, ORACPA-positive 1.072 1.014–1.134]). The odds ratios between these subgroups (i.e., ACPA-positive and -negative) significantly differed (P = 7.33x10-3). Expression quantitative trait locus analysis revealed an association of the SPP1 risk-allele combination with decreased SPP1 expression in peripheral macrophages from 599 individuals. To corroborate these findings, we found an association of the SPP1 risk-allele combination and low serum level of secreted OPN (P = 0.0157) as well as serum level of secreted OPN correlated positively with ACPA production (P = 0.005; r = 0.483). Conclusion We demonstrate a significant contribution of the combination of SPP1 rs11439060 and rs9138 frequent alleles to risk of RA, the magnitude of the association greater in patients negative for ACPAs.

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