TY - JOUR
T1 - Genetic determinants and an epistasis of LILRA3 and HLA-B*52 in Takayasu arteritis
AU - Terao, Chikashi
AU - Yoshifuji, Hajime
AU - Matsumura, Takayoshi
AU - Naruse, Taeko K.
AU - Ishii, Tomonori
AU - Nakaoka, Yoshikazu
AU - Kirino, Yohei
AU - Matsuo, Keitaro
AU - Origuchi, Tomoki
AU - Shimizu, Masakazu
AU - Maejima, Yasuhiro
AU - Amiya, Eisuke
AU - Tamura, Natsuko
AU - Kawaguchi, Takahisa
AU - Takahashi, Meiko
AU - Setoh, Kazuya
AU - Ohmura, Koichiro
AU - Watanabe, Ryu
AU - Horita, Tetsuya
AU - Atsumi, Tatsuya
AU - Matsukura, Mitsuru
AU - Miyata, Tetsuro
AU - Kochi, Yuta
AU - Suda, Toshio
AU - Tanemoto, Kazuo
AU - Meguro, Akira
AU - Okada, Yukinori
AU - Ogimoto, Akiyoshi
AU - Yamamoto, Motohisa
AU - Takahashi, Hiroki
AU - Nakayamada, Shingo
AU - Saito, Kazuyoshi
AU - Kuwana, Masataka
AU - Mizuki, Nobuhisa
AU - Tabara, Yasuharu
AU - Ueda, Atsuhisa
AU - Komuro, Issei
AU - Kimura, Akinori
AU - Isobe, Mitsuaki
AU - Mimori, Tsuneyo
AU - Matsuda, Fumihiko
N1 - Publisher Copyright:
© 2018 National Academy of Sciences. All rights reserved.
PY - 2018/12/18
Y1 - 2018/12/18
N2 - Takayasu arteritis (TAK) is a systemic vasculitis with severe complications that affects the aorta and its large branches. HLA-B*52 is an established susceptibility locus to TAK. To date, there are still only a limited number of reports concerning non-HLA susceptibility loci to TAK. We conducted a genome-wide association study (GWAS) and a follow-up study in a total of 633 TAK cases and 5,928 controls. A total of 510,879 SNPs were genotyped, and 5,875,450 SNPs were imputed together with HLA-B*52. Functional annotation of significant loci, enhancer enrichment, and pathway analyses were conducted. We identified four unreported significant loci, namely rs2322599, rs103294, rs17133698, and rs1713450, in PTK2B, LILRA3/LILRB2, DUSP22, and KLHL33, respectively. Two additional significant loci unreported in non-European GWAS were identified, namely HSPA6/FCGR3A and chr21q.22. We found that a single variant associated with the expression of MICB, a ligand for natural killer (NK) cell receptor, could explain the entire association with the HLA-B region. Rs2322599 is strongly associated with the expression of PTK2B. Rs103294 risk allele in LILRA3/LILRB2 is known to be a tagging SNP for the deletion of LILRA3, a soluble receptor of HLA class I molecules. We found a significant epistasis effect between HLA-B*52 and rs103294 (P = 1.2 × 10 −3 ). Enhancer enrichment analysis and pathway analysis suggested the involvement of NK cells (P = 8.8 × 10 −5 , enhancer enrichment). In conclusion, four unreported TAK susceptibility loci and an epistasis effect between LILRA3 and HLA-B*52 were identified. HLA and non-HLA regions suggested a critical role for NK cells in TAK.
AB - Takayasu arteritis (TAK) is a systemic vasculitis with severe complications that affects the aorta and its large branches. HLA-B*52 is an established susceptibility locus to TAK. To date, there are still only a limited number of reports concerning non-HLA susceptibility loci to TAK. We conducted a genome-wide association study (GWAS) and a follow-up study in a total of 633 TAK cases and 5,928 controls. A total of 510,879 SNPs were genotyped, and 5,875,450 SNPs were imputed together with HLA-B*52. Functional annotation of significant loci, enhancer enrichment, and pathway analyses were conducted. We identified four unreported significant loci, namely rs2322599, rs103294, rs17133698, and rs1713450, in PTK2B, LILRA3/LILRB2, DUSP22, and KLHL33, respectively. Two additional significant loci unreported in non-European GWAS were identified, namely HSPA6/FCGR3A and chr21q.22. We found that a single variant associated with the expression of MICB, a ligand for natural killer (NK) cell receptor, could explain the entire association with the HLA-B region. Rs2322599 is strongly associated with the expression of PTK2B. Rs103294 risk allele in LILRA3/LILRB2 is known to be a tagging SNP for the deletion of LILRA3, a soluble receptor of HLA class I molecules. We found a significant epistasis effect between HLA-B*52 and rs103294 (P = 1.2 × 10 −3 ). Enhancer enrichment analysis and pathway analysis suggested the involvement of NK cells (P = 8.8 × 10 −5 , enhancer enrichment). In conclusion, four unreported TAK susceptibility loci and an epistasis effect between LILRA3 and HLA-B*52 were identified. HLA and non-HLA regions suggested a critical role for NK cells in TAK.
KW - Autoimmunity
KW - Epistasis
KW - Genome-wide association study
KW - HLA
KW - Takayasu arteritis
UR - http://www.scopus.com/inward/record.url?scp=85058703530&partnerID=8YFLogxK
U2 - 10.1073/pnas.1808850115
DO - 10.1073/pnas.1808850115
M3 - Article
C2 - 30498034
AN - SCOPUS:85058703530
SN - 0027-8424
VL - 115
SP - 13045
EP - 13050
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 51
ER -