Identification of new overlapping and disease-specific genetic risk factors for rheumatoid arthritis and radiographic axial spondyloarthritis: a meta-analysis of three large European populations and functional characterization
Cabrera-Serrano A, Carretero-Fernández M, Pérez-Rojo B, Ter Horst R, Cañadas-Garre M, Canhão H, Quartuccio L, Sorensen S, Glintborg B, Filipescu I, Pérez-Pampin E, Conesa-Zamora P, Swierkot J, den Broeder A, de Vita S, Brix Petersen E, Li Y, Coenen M, Bogunia-Kubik K, Andersen V, Fonseca J, Lund Hetland M, López Nevot M, López-Medina C, Reyes-Zurita F, Netea M, Escudero A, Cáliz R, Collantes-Estévez E, Sánchez-Maldonado J, Sainz J
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Frontiers in Immunology: Volume 17, Page 1637735
Abstract
INTRODUCTION: This study conducted a meta-analysis across three large European cohorts (UKBB, FinnGen, and REPAIR), including 12,660 rheumatoid arthritis (RA) cases, 2,446 radiographic axial spondyloarthritis (r-axSpA) cases, and over 530,000 shared controls. METHODS: Ten independent SNPs in CARMIL1, GRM4, ITPR3, PRSS16, ZNF322, HTT, IKZF1, MANEA, and MGAM2 were analyzed, and functional characterization was performed through cytokine and protein assessments as well as eQTL analyses. RESULTS: Ten independent SNPs were significantly associated with both RA and r-axSpA. Risk alleles included HTT (rs363075A), IKZF1 (rs12718261A), MANEA (rs72920280T), and MGAM2 (rs73158426G), while CARMIL1 (rs72831267C), GRM4 (rs2495964G), ITPR3 (rs77601296A), ITPR3 (rs9469540T), PRSS16 (rs72843633T), and ZNF322 (rs6901425G) had protective effects. Functional analysis showed that GRM4 (rs2495964G) was linked to decreased CCL25 levels (p = 0.00030), and ITPR3 (rs9469540T) to reduced IL10 production after LPS stimulation (p = 1.3×10(-4)). The ZNF322rs6901425G allele was associated with reduced TNFB and increased TGM2 levels (p = 9.60×10(-4) and p = 3.00×(10-4)), both involved in immune signaling and tissue remodeling. Disease-specific associations were found in BTN2A1, BTN3A2, and H2BC11. The BTN2A1 (rs1977199A) allele was protective in RA (OR = 0.93) but increased r-axSpA risk (OR = 1.23), and was associated with reduced IL22 (p = 0.00016) and elevated HO-1 in obese individuals (p = 6.73×10(-6)). In contrast, BTN3A2 (rs9393716G) and H2BC11 (rs66462181C) increased RA risk but were protective in r-axSpA, linked to decreased HO-1 and IL6 (p = 2.43×10(-5), 3.287times;10(-4), 1.18×10(-4)). These SNPs also acted as eQTLs for immune-related genes such as BTN3A2, HMGN4, and TRIM38. DISCUSSION: Our findings highlight novel shared and disease-specific variants and key immunoregulatory mediators-IL10, IL22, IL6, CCL25, and HO-1-offering insights for disease stratification and therapeutic targeting.
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