Geographic Differences in Genetic Susceptibility to IgA Nephropathy: GWAS Replication Study and Geospatial Risk Analysis

Lise Thibaudin,Antonio Amoroso,Marie Metzger,Simone Sanna‐Cherchi ,Kāri Stefánsson ,Guðmar Þorleifsson ,Juergen Floege ,Ali G Gharavi,Anne Boland,Holly J Snyder,Richard P Lifton,Patrik K E Magnusson ,Silvana Savoldi,Loreto Gesualdo,Bruce A Julian,Unnur Þorsteinsdóttir ,Kitty J Jager,Robert Wyatt ,Claudia Izzi,Judit Nagy,Hong Zhang,Murim Choi,Alexander Viktorin,Pasquale Zamboli,Francesco Scolari,Christoph Wanner,Mersedeh Rohanizadegan,Nan Chen,Hussein H Karnib,Dita Maixnerová ,Maddalena Gigante,Bénédicte Stengel ,Hitoshi Suzuki,Daniele Cusi,Jingyuan Xie,Kati Kristiansson,Ichiei Narita,Krzysztof Mucha,Jan Novák ,Ulf Panzer,F Berthoux ,Ping Hou,Markus Perola,Yifu Li,Vladimı́r Tesař ,Shin Goto,Frank Eitner,Krzysztof Kiryluk

doi:10.1371/journal.pgen.1002765

Abstract

IgA nephropathy (IgAN), major cause of kidney failure worldwide, is common in Asians, moderately prevalent in Europeans, and rare in Africans. It is not known if these differences represent variation in genes, environment, or ascertainment. In a recent GWAS, we localized five IgAN susceptibility loci on Chr.6p21 (HLA-DQB1/DRB1, PSMB9/TAP1, and DPA1/DPB2 loci), Chr.1q32 (CFHR3/R1 locus), and Chr.22q12 (HORMAD2 locus). These IgAN loci are associated with risk of other immune-mediated disorders such as type I diabetes, multiple sclerosis, or inflammatory bowel disease. We tested association of these loci in eight new independent cohorts of Asian, European, and African-American ancestry (N = 4,789), followed by meta-analysis with risk-score modeling in 12 cohorts (N = 10,755) and geospatial analysis in 85 world populations. Four susceptibility loci robustly replicated and all five loci were genome-wide significant in the combined cohort (P = 5×10−32–3×10−10), with heterogeneity detected only at the PSMB9/TAP1 locus (I2 = 0.60). Conditional analyses identified two new independent risk alleles within the HLA-DQB1/DRB1 locus, defining multiple risk and protective haplotypes within this interval. We also detected a significant genetic interaction, whereby the odds ratio for the HORMAD2 protective allele was reversed in homozygotes for a CFHR3/R1 deletion (P = 2.5×10−4). A seven–SNP genetic risk score, which explained 4.7% of overall IgAN risk, increased sharply with Eastward and Northward distance from Africa (r = 0.30, P = 3×10−128). This model paralleled the known East–West gradient in disease risk. Moreover, the prediction of a South–North axis was confirmed by registry data showing that the prevalence of IgAN–attributable kidney failure is increased in Northern Europe, similar to multiple sclerosis and type I diabetes. Variation at IgAN susceptibility loci correlates with differences in disease prevalence among world populations. These findings inform genetic, biological, and epidemiological investigations of IgAN and permit cross-comparison with other complex traits that share genetic risk loci and geographic patterns with IgAN.

Highlights

IgA nephropathy (IgAN) is a common kidney disease with a complex genetic determination
We genotyped the two top-scoring SNPs for the CFHR3/R1, TAP2/PSMB9, DPA1/DPB2, and HORMAD2 loci, but four SNPs were included for the DQB1/DRB1 locus to test for independent alleles at this interval by conditional analysis
We examined the largest IgAN case-control cohorts reported to date

Summary

Introduction

IgA nephropathy (IgAN) is a common kidney disease with a complex genetic determination. The disease has been detected among all ethnicities worldwide, but displays a striking geographic variation It is the most common cause of kidney failure in East Asian countries, has intermediate prevalence in European and US populations but is rarely reported in populations of African ancestry. Family members frequently have aberrant glycosylation of the hinge region of circulating IgA1, a defect with an estimated heritability of 40–50% [12,13]. These data suggest a strong genetic contribution to disease

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Conclusion