Abstract
We previously established an 80 kb haplotype upstream of TNFSF4 as a susceptibility locus in the autoimmune disease SLE. SLE-associated alleles at this locus are associated with inflammatory disorders, including atherosclerosis and ischaemic stroke. In Europeans, the TNFSF4 causal variants have remained elusive due to strong linkage disequilibrium exhibited by alleles spanning the region. Using a trans-ancestral approach to fine-map the locus, utilising 17,900 SLE and control subjects including Amerindian/Hispanics (1348 cases, 717 controls), African-Americans (AA) (1529, 2048) and better powered cohorts of Europeans and East Asians, we find strong association of risk alleles in all ethnicities; the AA association replicates in African-American Gullah (152,122). The best evidence of association comes from two adjacent markers: rs2205960-T (P = 1.71×10−34, OR = 1.43[1.26–1.60]) and rs1234317-T (P = 1.16×10−28, OR = 1.38[1.24–1.54]). Inference of fine-scale recombination rates for all populations tested finds the 80 kb risk and non-risk haplotypes in all except African-Americans. In this population the decay of recombination equates to an 11 kb risk haplotype, anchored in the 5′ region proximal to TNFSF4 and tagged by rs2205960-T after 1000 Genomes phase 1 (v3) imputation. Conditional regression analyses delineate the 5′ risk signal to rs2205960-T and the independent non-risk signal to rs1234314-C. Our case-only and SLE-control cohorts demonstrate robust association of rs2205960-T with autoantibody production. The rs2205960-T is predicted to form part of a decameric motif which binds NF-κBp65 with increased affinity compared to rs2205960-G. ChIP-seq data also indicate NF-κB interaction with the DNA sequence at this position in LCL cells. Our research suggests association of rs2205960-T with SLE across multiple groups and an independent non-risk signal at rs1234314-C. rs2205960-T is associated with autoantibody production and lymphopenia. Our data confirm a global signal at TNFSF4 and a role for the expressed product at multiple stages of lymphocyte dysregulation during SLE pathogenesis. We confirm the validity of trans-ancestral mapping in a complex trait.
Highlights
Tumour Necrosis Factor Superfamily (TNFS) members control wide-ranging facets of immunity when they interact with their complimentary TNF Receptors [1]
We have previously shown single nucleotide polymorphisms (SNPs) in the 59 tumour-necrosis family superfamily member 4 (TNFSF4) region to be associated with lupus in European families and a case-control cohort [4]
A major obstacle in pinpointing the marker(s) at TNFSF4 which best explain the risk of systemic lupus erythematosus (SLE) has been the strong correlation between adjacent markers across the TNFSF4 region in this population
Summary
Tumour Necrosis Factor Superfamily (TNFS) members control wide-ranging facets of immunity when they interact with their complimentary TNF Receptors [1]. Several lines of evidence published over the last 15 years suggest the TNFSF4–TNFRSF4 interaction is required for the induction of anti-tumour immunity, allergy and autoimmunity [3,4,5,6] and inhibits generation of adaptive T regulatory (TR1) cells [7]. The outcome is not limited to human disease; blockade of the TNFSF4-TNFRS4 interaction has ameliorative effects in animal models of T cell pathologies [8] including allergic and autoimmune manifestations [9]. Genetic variation at TNFSF4 has been associated with the autoimmune disease systemic lupus erythematosus (SLE), and other inflammatory conditions including atherosclerosis and ischaemic stroke. Multiple SLE riskassociated TNFSF4 variants are associated with systemic sclerosis [16], primary Sjogren’s syndrome [17] and myocardial infarction [18,19]
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