Abstract
Genome-wide association studies and meta-analysis indicate that several genes/loci are consistently associated with rheumatoid arthritis (RA) in European and Asian populations. To evaluate the transferability status of these findings to an ethnically diverse north Indian population, we performed a replication analysis. We investigated the association of 47 single-nucleotide polymorphisms (SNPs) at 43 of these genes/loci with RA in a north Indian cohort comprising 983 RA cases and 1007 age and gender matched controls. Genotyping was done using Infinium human 660w-quad. Association analysis by chi-square test implemented in plink was carried out in two steps. Firstly, association of the index or surrogate SNP (r2>0.8, calculated from reference GIH Hap-Map population) was tested. In the second step, evidence for allelic/locus heterogeneity at aforementioned genes/loci was assessed for by testing additional flanking SNPs in linkage equilibrium with index/surrogate marker.Of the 44 European specific index SNPs, neither index nor surrogate SNPs were present for nine SNPs in the genotyping array. Of the remaining 35, associations were replicated at seven genes namely PTPN22 (rs1217407, p = 3×10−3); IL2–21 (rs13119723, p = 0.008); HLA-DRB1 (rs660895, p = 2.56×10−5; rs6457617, p = 1.6×10−09; rs13192471, p = 6.7×10−16); TNFA1P3 (rs9321637, p = 0.03); CCL21 (rs13293020, p = 0.01); IL2RA (rs2104286, p = 1.9×10−4) and ZEB1 (rs2793108, p = 0.006). Of the three Asian specific loci tested, rs2977227 in PADI4 showed modest association (p<0.02). Further, of the 140 SNPs (in LE with index/surrogate variant) tested, association was observed at 11 additional genes: PTPRC, AFF3, CD28, CTLA4, PXK, ANKRD55, TAGAP, CCR6, BLK, CD40 and IL2RB. This study indicates limited replication of European and Asian index SNPs and apparent allelic heterogeneity in RA etiology among north Indians warranting independent GWAS in this population. However, replicated associations of HLA-DRB1, PTPN22 (which confer ∼50% of the heritable risk to RA) and IL2RA suggest that cross-ethnicity fine mapping of such loci is apposite for identification of causal variants.
Highlights
Genome wide association studies (GWAS) have enumerated several new genes/loci for common-complex diseases
21 out of the 44 European specific index singlenucleotide polymorphisms (SNPs) were present in the SNP array used in this study
Of the remaining 23 SNPs, surrogates were identified for 14 index variants but none for nine SNPs [Table S1]
Summary
Genome wide association studies (GWAS) have enumerated several new genes/loci for common-complex diseases. Recent GWAS in rheumatoid arthritis (RA; MIM180300) have unraveled disease susceptibility loci of small to moderate effect size Most of these genes/loci have risk alleles of known immune function [1] justifying their involvement in RA which is a complex autoimmune disorder characterized by chronic inflammation of the synovial joints followed by progressive articular damage and major functional disability [2]. In addition to HLA, GWAS carried out in European populations have identified a total of 24 susceptibility genes/loci (having 26 risk alleles) almost consistently associated with RA. SNPs at Asian specific RA loci i.e., PADI4, SLC22A4, and FCRL3 [9] showed either modest or no association in the meta-analysis [5] and other association studies reported in European populations [10,11,12] These findings point towards genetic heterogeneity in RA susceptibility across different ethnic groups
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