A meta-analysis of 87,040 individuals identifies 23 new susceptibility loci for prostate cancer

一项纳入 87,040 名受试者的荟萃分析发现了 23 个新的前列腺癌易感基因位点

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作者:Al Olama,Ali Amin,Kote-Jarai,Zsofia,Berndt,Sonja I,Conti,David V,Schumacher,Fredrick,Han,Ying,Benlloch,Sara,Hazelett,Dennis J,Wang,Zhaoming,Saunders,Ed,Leongamornlert,Daniel,Lindstrom,Sara,Jugurnauth-Little,Sara,Dadaev,Tokhir,Tymrakiewicz,Malgorzata,Stram,Daniel O,Rand,Kristin,Wan,Peggy,Stram,Alex,Sheng,Xin,Pooler,Loreall C,Park,Karen,Xia,Lucy,Tyrer,Jonathan,Kolonel,Laurence N,Le Marchand,Loic,Hoover,Robert N,Machiela,Mitchell J,Yeager,Merideth,Burdette,Laurie,Chung,Charles C,Hutchinson,Amy,Yu,Kai,Goh,Chee,Ahmed,Mahbubl,Govindasami,Koveela,Guy,Michelle,Tammela,Teuvo L J,Auvinen,Anssi,Wahlfors,Tiina,Schleutker,Johanna,Visakorpi,Tapio,Leinonen,Katri A,Xu,Jianfeng,Aly,Markus,Donovan,Jenny,Travis,Ruth C,Key,Tim J,Siddiq,Afshan,Canzian,Federico,Khaw,Kay-Tee,Takahashi,Atsushi,Kubo,Michiaki,Pharoah,Paul,Pashayan,Nora,Weischer,Maren,Nordestgaard,Borge G,Nielsen,Sune F,Klarskov,Peter,Røder,Martin Andreas,Iversen,Peter,Thibodeau,Stephen N,McDonnell,Shannon K,Schaid,Daniel J,Stanford,Janet L,Kolb,Suzanne,Holt,Sarah,Knudsen,Beatrice,Coll,Antonio Hurtado,Gapstur,Susan M,Diver,W Ryan,Stevens,Victoria L,Maier,Christiane,Luedeke,Manuel,Herkommer,Kathleen,Rinckleb,Antje E,Strom,Sara S,Pettaway,Curtis,Yeboah,Edward D,Tettey,Yao,Biritwum,Richard B,Adjei,Andrew A,Tay,Evelyn,Truelove,Ann,Niwa,Shelley,Chokkalingam,Anand P,Cannon-Albright,Lisa,Cybulski,Cezary,Wokołorczyk,Dominika,Kluźniak,Wojciech,Park,Jong,Sellers,Thomas,Lin,Hui-Yi,Isaacs,William B,Partin,Alan W,Brenner,Hermann,Dieffenbach,Aida Karina,Stegmaier,Christa,Chen,Constance,Giovannucci,Edward L,Ma,Jing,Stampfer,Meir,Penney,Kathryn L,Mucci,Lorelei,John,Esther M,Ingles,Sue A,Kittles,Rick A,Murphy,Adam B,Pandha,Hardev,Michael,Agnieszka,Kierzek,Andrzej M,Blot,William,Signorello,Lisa B,Zheng,Wei,Albanes,Demetrius,Virtamo,Jarmo,Weinstein,Stephanie,Nemesure,Barbara,Carpten,John,Leske,Cristina,Wu,Suh-Yuh,Hennis,Anselm,Kibel,Adam S,Rybicki,Benjamin A,Neslund-Dudas,Christine,Hsing,Ann W,Chu,Lisa,Goodman,Phyllis J,Klein,Eric A,Zheng,S Lilly,Batra,Jyotsna,Clements,Judith,Spurdle,Amanda,Teixeira,Manuel R,Paulo,Paula,Maia,Sofia,Slavov,Chavdar,Kaneva,Radka,Mitev,Vanio,Witte,John S,Casey,Graham,Gillanders,Elizabeth M,Seminara,Daniella,Riboli,Elio,Hamdy,Freddie C,Coetzee,Gerhard A,Li,Qiyuan,Freedman,Matthew L,Hunter,David J,Muir,Kenneth,Gronberg,Henrik,Neal,David E,Southey,Melissa,Giles,Graham G,Severi,Gianluca,Cook,Michael B,Nakagawa,Hidewaki,Wiklund,Fredrik,Kraft,Peter,Chanock,Stephen J,Henderson,Brian E,Easton,Douglas F,Eeles,Rosalind A,Haiman,Christopher A
期刊:Nature Genetics影响因子:29.000
时间:2014起止号:2014 Oct;46(10):1103-9
doi:10.1038/ng.3094研究方向: 肿瘤
疾病类型: 前列腺癌

Abstract

Genome-wide association studies (GWAS) have identified 76 variants associated with prostate cancer risk predominantly in populations of European ancestry. To identify additional susceptibility loci for this common cancer, we conducted a meta-analysis of > 10 million SNPs in 43,303 prostate cancer cases and 43,737 controls from studies in populations of European, African, Japanese and Latino ancestry. Twenty-three new susceptibility loci were identified at association P < 5 × 10(-8); 15 variants were identified among men of European ancestry, 7 were identified in multi-ancestry analyses and 1 was associated with early-onset prostate cancer. These 23 variants, in combination with known prostate cancer risk variants, explain 33% of the familial risk for this disease in European-ancestry populations. These findings provide new regions for investigation into the pathogenesis of prostate cancer and demonstrate the usefulness of combining ancestrally diverse populations to discover risk loci for disease.

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