| Literature DB >> 28123851 |
Vassiliki Kotoula1, Florentia Fostira2, Kyriaki Papadopoulou3, Paraskevi Apostolou2, Eleftheria Tsolaki3, Georgios Lazaridis4, Kyriaki Manoussou5, Flora Zagouri6, Dimitrios Pectasides7, Ioannis Vlachos8, Ioannis Tikas3, Sotiris Lakis3, Irene Konstantopoulou2, George Pentheroudakis9, Helen Gogas10, Pavlos Papakostas11, Christos Christodoulou12, Dimitrios Bafaloukos13, Evangelia Razis14, Vasilios Karavasilis4, Christina Bamias15, Drakoulis Yannoukakos2, George Fountzilas16.
Abstract
The preservation of pathogenic BRCA1/2 germline mutations in tumor tissues is usually not questioned, while it remains unknown whether these interact with somatic genotypes for patient outcome. Herein we compared germline and tumor genotypes in operable triple-negative breast cancer (TNBC) and evaluated their combined effects on prognosis. We analyzed baseline germline and primary tumor genotype data obtained by Sanger and Next Generation Sequencing in 194 TNBC patients. We also performed multiple tests interrogating the preservation of germline mutations in matched tumors and breast tissue from carriers with available material. Patients had been treated within clinical trials with adjuvant anthracyclines-taxanes based chemotherapy. We identified 50 (26%) germline mutation carriers (78% in BRCA1) and 136 (71%) tumors with somatic mutations (83% in TP53). Tumor mutation patterns differed between carriers and non-carriers (P<0.001); PIK3CA mutations were exclusively present in non-carriers (P=0.007). Germline BRCA1/2 mutations were not detected in matched tumors and breast tissues from 14 out of 33 (42%) evaluable carriers. Microsatellite markers revealed tumor loss of the germline mutant allele in one case only. Tumors that had lost the germline mutation demonstrated a higher incidence of somatic TP53 mutations as compared to tumors with preserved germline mutations (P=0.036). Germline mutation status significantly interacted with tumor TP53 mutations for patient disease-free survival (interaction P=0.026): In non-carriers, tumor TP53 mutations did not affect outcome; In carriers, those with mutated TP53 tumors experienced more relapses compared to those with wild-type TP53 tumors (36% vs. 9% relapse rate, respectively). In conclusion, we show that loss of germline BRCA1/2 mutations is not a rare event in TNBC. This finding, the observed differences in tumor genotypes with respect to germline status and the prognostic interaction between germline BRCA1-related and tumor TP53 mutation status prompt for combined germline and tumor genotyping for the classification of TNBC, particularly in the context of clinical trials evaluating synthetic lethality drugs.Entities:
Keywords: BRCA1; BRCA2; TNBC; TP53; adjuvant chemotherapy; germline; haploinsufficiency; mutant-LOH; mutation reversion; somatic
Year: 2017 PMID: 28123851 PMCID: PMC5250684
Source DB: PubMed Journal: Am J Cancer Res ISSN: 2156-6976 Impact factor: 6.166