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The role of genetic breast cancer susceptibility variants as prognostic factors
Authors:Fasching Peter A  Pharoah Paul D P  Cox Angela  Nevanlinna Heli  Bojesen Stig E  Karn Thomas  Broeks Annegien  van Leeuwen Flora E  van't Veer Laura J  Udo Renate  Dunning Alison M  Greco Dario  Aittomäki Kristiina  Blomqvist Carl  Shah Mitul  Nordestgaard Børge G  Flyger Henrik  Hopper John L  Southey Melissa C  Apicella Carmel  Garcia-Closas Montserrat  Sherman Mark  Lissowska Jolanta  Seynaeve Caroline  Huijts Petra E A  Tollenaar Rob A E M  Ziogas Argyrios  Ekici Arif B  Rauh Claudia  Mannermaa Arto  Kataja Vesa  Kosma Veli-Matti  Hartikainen Jaana M  Andrulis Irene L  Ozcelik Hilmi  Mulligan Anna-Marie  Glendon Gord
Affiliation:University Breast Center, Department of Gynecology and Obstetrics, University Hospital Erlangen, Comprehensive Cancer Center Erlangen Nuremberg, Friedrich-Alexander University Erlangen-Nuremberg, Erlangen, Germany. peter.fasching@uk-erlangen.de
Abstract:
Recent genome-wide association studies identified 11 single nucleotide polymorphisms (SNPs) associated with breast cancer (BC) risk. We investigated these and 62 other SNPs for their prognostic relevance. Confirmed BC risk SNPs rs17468277 (CASP8), rs1982073 (TGFB1), rs2981582 (FGFR2), rs13281615 (8q24), rs3817198 (LSP1), rs889312 (MAP3K1), rs3803662 (TOX3), rs13387042 (2q35), rs4973768 (SLC4A7), rs6504950 (COX11) and rs10941679 (5p12) were genotyped for 25 853 BC patients with the available follow-up; 62 other SNPs, which have been suggested as BC risk SNPs by a GWAS or as candidate SNPs from individual studies, were genotyped for replication purposes in subsets of these patients. Cox proportional hazard models were used to test the association of these SNPs with overall survival (OS) and BC-specific survival (BCS). For the confirmed loci, we performed an accessory analysis of publicly available gene expression data and the prognosis in a different patient group. One of the 11 SNPs, rs3803662 (TOX3) and none of the 62 candidate/GWAS SNPs were associated with OS and/or BCS at P<0.01. The genotypic-specific survival for rs3803662 suggested a recessive mode of action [hazard ratio (HR) of rare homozygous carriers=1.21; 95% CI: 1.09-1.35, P=0.0002 and HR=1.29; 95% CI: 1.12-1.47, P=0.0003 for OS and BCS, respectively]. This association was seen similarly in all analyzed tumor subgroups defined by nodal status, tumor size, grade and estrogen receptor. Breast tumor expression of these genes was not associated with prognosis. With the exception of rs3803662 (TOX3), there was no evidence that any of the SNPs associated with BC susceptibility were associated with the BC survival. Survival may be influenced by a distinct set of germline variants from those influencing susceptibility.
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