Genome-wide association studies identify four ER negative-specific breast cancer risk loci.

Garcia Closas M; Couch FJ; Lindstrom S; Michailidou K; Schmidt MK; Brook MN; Orr N; Rhie SK; Riboli E; Feigelson HS; Le Marchand L; Buring JE; Eccles D; Miron P; Fasching PA; Brauch H; Chang Claude J; Carpenter J; Godwin AK; Nevanlinna H; Giles GG; Cox A; Hopper JL; Bolla MK; Wang Q; Dennis J; Dicks E; Howat WJ; Schoof N; Bojesen SE; Lambrechts D; Broeks A; Andrulis IL; Guénel P; Burwinkel B; Sawyer EJ; Hollestelle A; Fletcher O; Winqvist R; Brenner H; Mannermaa A; Hamann U; Meindl A; Lindblom A; Zheng W; Devillee P; Goldberg MS; Lubinski J; Kristensen V; Swerdlow A; Anton Culver H; Dörk T; Muir K; Matsuo K; Wu AH; Radice P; Teo SH; Shu XO; Blot W; Kang D; Hartman M; Sangrajrang S; Shen CY; Southey MC; Park DJ; Hammet F; Stone J; Veer LJ; Rutgers EJ; Lophatananon A; Stewart Brown S; Siriwanarangsan P; Peto J; Schrauder MG; Ekici AB; Beckmann MW; Dos Santos Silva I; Johnson N; Warren H; Tomlinson I; Kerin MJ; Miller N; Marme F; Schneeweiss A; Sohn C; Truong T; Laurent Puig P; Kerbrat P; Nordestgaard BG; Nielsen SF; Flyger H; Milne RL; Perez JI; Menéndez P; Müller H; Arndt V; Stegmaier C; Lichtner P; Lochmann M; Justenhoven C; Ko YD; Gene ENvironmental Interaction; breast CAncer Network; Muranen TA; Aittomäki K; Blomqvist C; Greco D; Heikkinen T; Ito H; Iwata H; Yatabe Y; Antonenkova NN; Margolin S; Kataja V; Kosma VM; Hartikainen JM; Balleine R; kConFab Investigators; Tseng CC; Berg DV; Stram DO; Neven P; Dieudonné AS; Leunen K; Rudolph A; Nickels S; Flesch Janys D; Peterlongo P; Peissel B; Bernard L; Olson JE; Wang X; Stevens K; Severi G; BAGLIETTO, LAURA; McLean C; Coetzee GA; Feng Y; Henderson BE; Schumacher F; Bogdanova NV; Labrèche F; Dumont M; Yip CH; Taib NA; Cheng CY; Shrubsole M; Long J; Pylkäs K; Jukkola Vuorinen A; Kauppila S; Knight JA; Glendon G; Mulligan AM; Tollenaar RA; Seynaeve CM; Kriege M; Hooning MJ; van den Ouweland AM; van Deurzen CH; Lu W; Gao YT; Cai H; Balasubramanian SP; Cross SS; Reed MW; Signorello L; Cai Q; Shah M; Miao H; Chan CW; Chia KS; Jakubowska A; Jaworska K; Durda K; Hsiung CN; Wu PE; Yu JC; Ashworth A; Jones M; Tessier DC; González Neira A; Pita G; Alonso MR; Vincent D; Bacot F; Ambrosone CB; Bandera EV; John EM; Chen GK; Hu JJ; Rodriguez Gil JL; Bernstein L; Press MF; Ziegler RG; Millikan RM; Deming Halverson SL; Nyante S; Ingles SA; Waisfisz Q; Tsimiklis H; Makalic E; Schmidt D; Bui M; Gibson L; Müller Myhsok B; Schmutzler RK; Hein R; Dahmen N; Beckmann L; Aaltonen K; Czene K; Irwanto A; Liu J; Turnbull C; Familial Breast Cancer Study; Rahman N; Meijers Heijboer H; Uitterlinden AG; Rivadeneira F; Australian Breast Cancer Tissue Bank Investigators; Olswold C; Slager S; Pilarski R; Ademuyiwa F; Konstantopoulou I; Martin NG; Montgomery GW; Slamon DJ; Rauh C; Lux MP; Jud SM; Bruning T; Weaver J; Sharma P; Pathak H; Tapper W; Gerty S; Durcan L; Trichopoulos D; Tumino R; Peeters PH; Kaaks R; CAMPA, DANIELE; Canzian F; Weiderpass E; Johansson M; Khaw KT; Travis R; Clavel Chapelon F; Kolonel LN; Chen C; Beck A; Hankinson SE; Berg CD; Hoover RN; Lissowska J; Figueroa JD; Chasman DI; Gaudet MM; Diver WR; Willett WC; Hunter DJ; Simard J; Benitez J; Dunning AM; Sherman ME; Chenevix Trench G; Chanock SJ; Hall P; Pharoah PD; Vachon C; Easton DF; Haiman CA; Kraft P.

doi:10.1038/ng.2561

Estrogen receptor (ER)-negative tumors represent 20-30% of all breast cancers, with a higher proportion occurring in younger women and women of African ancestry. The etiology and clinical behavior of ER-negative tumors are different from those of tumors expressing ER (ER positive), including differences in genetic predisposition. To identify susceptibility loci specific to ER-negative disease, we combined in a meta-analysis 3 genome-wide association studies of 4,193 ER-negative breast cancer cases and 35,194 controls with a series of 40 follow-up studies (6,514 cases and 41,455 controls), genotyped using a custom Illumina array, iCOGS, developed by the Collaborative Oncological Gene-environment Study (COGS). SNPs at four loci, 1q32.1 (MDM4, P = 2.1 × 10-12 and LGR6, P = 1.4 × 10-8), 2p24.1 (P = 4.6 × 10-8) and 16q12.2 (FTO, P = 4.0 × 10-8), were associated with ER-negative but not ER-positive breast cancer (P > 0.05). These findings provide further evidence for distinct etiological pathways associated with invasive ER-positive and ER-negative breast cancers.