The somatic mutation profiles of 2,433 breast cancers refine their genomic and transcriptomic landscapes

Author:

Pereira Bernard,Chin Suet-Feung,Rueda Oscar M.,Vollan Hans-Kristian Moen,Provenzano Elena,Bardwell Helen A.,Pugh Michelle,Jones Linda,Russell Roslin,Sammut Stephen-John,Tsui Dana W. Y.,Liu Bin,Dawson Sarah-Jane,Abraham Jean,Northen Helen,Peden John F.,Mukherjee Abhik,Turashvili Gulisa,Green Andrew R.,McKinney SteveORCID,Oloumi Arusha,Shah SohrabORCID,Rosenfeld Nitzan,Murphy Leigh,Bentley David R.,Ellis Ian O.,Purushotham Arnie,Pinder Sarah E.,Børresen-Dale Anne-Lise,Earl Helena M.,Pharoah Paul D.,Ross Mark T.,Aparicio Samuel,Caldas Carlos

Abstract

Abstract The genomic landscape of breast cancer is complex, and inter- and intra-tumour heterogeneity are important challenges in treating the disease. In this study, we sequence 173 genes in 2,433 primary breast tumours that have copy number aberration (CNA), gene expression and long-term clinical follow-up data. We identify 40 mutation-driver (Mut-driver) genes, and determine associations between mutations, driver CNA profiles, clinical-pathological parameters and survival. We assess the clonal states of Mut-driver mutations, and estimate levels of intra-tumour heterogeneity using mutant-allele fractions. Associations between PIK3CA mutations and reduced survival are identified in three subgroups of ER-positive cancer (defined by amplification of 17q23, 11q13–14 or 8q24). High levels of intra-tumour heterogeneity are in general associated with a worse outcome, but highly aggressive tumours with 11q13–14 amplification have low levels of intra-tumour heterogeneity. These results emphasize the importance of genome-based stratification of breast cancer, and have important implications for designing therapeutic strategies.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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