Carboplatin in BRCA1/2-mutated and Triple-negative Breast Cancer BRCAness Subgroups: the TNT Trial

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2018 May 2

PMID 29713086

Citations 396

Authors

Andrew Tutt

Holly Tovey

Maggie Chon U Cheang

Sarah Kernaghan

Lucy Kilburn

Patrycja Gazinska

Julie Owen

Jacinta Abraham

Sophie Barrett

Peter Barrett-Lee

Robert Brown

Stephen Chan

Mitchell Dowsett

James M Flanagan

Lisa Fox

Anita Grigoriadis

Alexander Gutin

Catherine Harper-Wynne

Matthew Q Hatton

Katherine A Hoadley

Jyoti Parikh

Peter Parker

Charles M Perou

Rebecca Roylance

Vandna Shah

Adam Shaw

Ian E Smith

Kirsten M Timms

Andrew M Wardley

Gregory Wilson

Cheryl Gillett

Jerry S Lanchbury

Alan Ashworth

Nazneen Rahman

Mark Harries

Paul Ellis

Sarah E Pinder

Judith M Bliss

Affiliations

Soon will be listed here.

Abstract

Germline mutations in BRCA1/2 predispose individuals to breast cancer (termed germline-mutated BRCA1/2 breast cancer, gBRCA-BC) by impairing homologous recombination (HR) and causing genomic instability. HR also repairs DNA lesions caused by platinum agents and PARP inhibitors. Triple-negative breast cancers (TNBCs) harbor subpopulations with BRCA1/2 mutations, hypothesized to be especially platinum-sensitive. Cancers in putative 'BRCAness' subgroups-tumors with BRCA1 methylation; low levels of BRCA1 mRNA (BRCA1 mRNA-low); or mutational signatures for HR deficiency and those with basal phenotypes-may also be sensitive to platinum. We assessed the efficacy of carboplatin and another mechanistically distinct therapy, docetaxel, in a phase 3 trial in subjects with unselected advanced TNBC. A prespecified protocol enabled biomarker-treatment interaction analyses in gBRCA-BC and BRCAness subgroups. The primary endpoint was objective response rate (ORR). In the unselected population (376 subjects; 188 carboplatin, 188 docetaxel), carboplatin was not more active than docetaxel (ORR, 31.4% versus 34.0%, respectively; P = 0.66). In contrast, in subjects with gBRCA-BC, carboplatin had double the ORR of docetaxel (68% versus 33%, respectively; biomarker, treatment interaction P = 0.01). Such benefit was not observed for subjects with BRCA1 methylation, BRCA1 mRNA-low tumors or a high score in a Myriad HRD assay. Significant interaction between treatment and the basal-like subtype was driven by high docetaxel response in the nonbasal subgroup. We conclude that patients with advanced TNBC benefit from characterization of BRCA1/2 mutations, but not BRCA1 methylation or Myriad HRD analyses, to inform choices on platinum-based chemotherapy. Additionally, gene expression analysis of basal-like cancers may also influence treatment selection.

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