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Ethnic specificity of lupus-associated loci identified in a genome-wide association study in Korean women.

Authors
Lee, HS | Kim, T | Bang, SY | Na, YJ | Kim, I | Kim, K | Kim, JH | Chung, YJ | Shin, HD | Kang, YM | Shim, SC | Suh, CH  | Park, YB | Kim, JS | Kang, C | Bae, SC
Citation
Annals of the rheumatic diseases, 73(6). : 1240-1245, 2014
Journal Title
Annals of the rheumatic diseases
ISSN
0003-49671468-2060
Abstract
OBJECTIVES: To identify novel genetic candidates for systemic lupus erythematosus

(SLE) in the Korean population, and to validate the risk loci for SLE identified

in previous genome-wide association studies (GWAS). METHODS: We performed a GWAS

in 400 Korean female SLE patients and 445 controls. Selected single-nucleotide

polymorphisms (SNP) were then replicated in an independent cohort of 385 SLE

patients and 583 controls (replication cohort 1), and in a further 811 SLE

patients and 1502 controls (replication cohort 2). RESULTS: In the GWAS phase,

rs9275428 located near HLA-DQB1 showed the strongest association with SLE (OR

0.50, false discovery rate (FDR) p=3.07x10(-6)). Although no loci reached

genome-wide significance outside major histocompatibility complex (MHC),

C8orf13-BLK, STAT4, CSMD1, DIAPH3, GLDC and TNFSF4 showed FDR p < 0.05. Our

results suggest that STAT4, BLK, IRF5, PTTG1-miR-146a, UBE2L3 and TNFAIP3 are

shared susceptibility loci among Caucasians and Asians, while ETS1, IKZF1,

SLC15A4 are likely to be Asian-specific loci. In a combined analysis of 1596 SLE

patients and 2540 controls for selected 22 candidate SNP, STAT4 and BLK as

positive controls showed a strong association with SLE (FDR p=9.85x10(-13) and

2.28x10(-8), respectively). Of these, 16 candidates (PEX5L, TRAJ50, MYO18B, SOS1,

ARHGAP26, SMURF1, CADPS, HAND1, FAM78B, DIAPH3, TBL1XR1, CSMD1, ZBTB20, C3orf21,

HIPK1 and AP001042.1) showed only nominal significance (7.05x10(-4)
p
susceptibility for SLE between Caucasian and Asian ethnic groups. Although 16

putative novel loci for SLE have been suggested in the Korean population, further

research on a larger sample is required to discriminate truth from error.
MeSH

DOI
10.1136/annrheumdis-2012-202675
PMID
23740238
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Rheumatology
Ajou Authors
서, 창희
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