Large-scale genome-wide association study in a Japanese population identifies novel susceptibility loci across different diseases

一项针对日本人群的大规模全基因组关联研究发现了多种疾病的新易感基因位点

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作者:Ishigaki,Kazuyoshi,Akiyama,Masato,Kanai,Masahiro,Takahashi,Atsushi,Kawakami,Eiryo,Sugishita,Hiroki,Sakaue,Saori,Matoba,Nana,Low,Siew-Kee,Okada,Yukinori,Terao,Chikashi,Amariuta,Tiffany,Gazal,Steven,Kochi,Yuta,Horikoshi,Momoko,Suzuki,Ken,Ito,Kaoru,Koyama,Satoshi,Ozaki,Kouichi,Niida,Shumpei,Sakata,Yasushi,Sakata,Yasuhiko,Kohno,Takashi,Shiraishi,Kouya,Momozawa,Yukihide,Hirata,Makoto,Matsuda,Koichi,Ikeda,Masashi,Iwata,Nakao,Ikegawa,Shiro,Kou,Ikuyo,Tanaka,Toshihiro,Nakagawa,Hidewaki,Suzuki,Akari,Hirota,Tomomitsu,Tamari,Mayumi,Chayama,Kazuaki,Miki,Daiki,Mori,Masaki,Nagayama,Satoshi,Daigo,Yataro,Miki,Yoshio,Katagiri,Toyomasa,Ogawa,Osamu,Obara,Wataru,Ito,Hidemi,Yoshida,Teruhiko,Imoto,Issei,Takahashi,Takashi,Tanikawa,Chizu,Suzuki,Takao,Sinozaki,Nobuaki,Minami,Shiro,Yamaguchi,Hiroki,Asai,Satoshi,Takahashi,Yasuo,Yamaji,Ken,Takahashi,Kazuhisa,Fujioka,Tomoaki,Takata,Ryo,Yanai,Hideki,Masumoto,Akihide,Koretsune,Yukihiro,Kutsumi,Hiromu,Higashiyama,Masahiko,Murayama,Shigeo,Minegishi,Naoko,Suzuki,Kichiya,Tanno,Kozo,Shimizu,Atsushi,Yamaji,Taiki,Iwasaki,Motoki,Sawada,Norie,Uemura,Hirokazu,Tanaka,Keitaro,Naito,Mariko,Sasaki,Makoto,Wakai,Kenji,Tsugane,Shoichiro,Yamamoto,Masayuki,Yamamoto,Kazuhiko,Murakami,Yoshinori,Nakamura,Yusuke,Raychaudhuri,Soumya,Inazawa,Johji,Yamauchi,Toshimasa,Kadowaki,Takashi,Kubo,Michiaki,Kamatani,Yoichiro
期刊:Nature Genetics影响因子:29.000
时间:2020起止号:2020 Jul;52(7):669-679
doi:10.1038/s41588-020-0640-3

Abstract

The overwhelming majority of participants in current genetic studies are of European ancestry. To elucidate disease biology in the East Asian population, we conducted a genome-wide association study (GWAS) with 212,453 Japanese individuals across 42 diseases. We detected 320 independent signals in 276 loci for 27 diseases, with 25 novel loci (P < 9.58 × 10(-9)). East Asian-specific missense variants were identified as candidate causal variants for three novel loci, and we successfully replicated two of them by analyzing independent Japanese cohorts; p.R220W of ATG16L2 (associated with coronary artery disease) and p.V326A of POT1 (associated with lung cancer). We further investigated enrichment of heritability within 2,868 annotations of genome-wide transcription factor occupancy, and identified 378 significant enrichments across nine diseases (false discovery rate < 0.05) (for example, NKX3-1 for prostate cancer). This large-scale GWAS in a Japanese population provides insights into the etiology of complex diseases and highlights the importance of performing GWAS in non-European populations.

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