Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial

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

doi:10.1038/s41591-018-0009-7

Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial

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. HoadleyJyoti 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

^*Corresponding author for this work

Division of Cancer Sciences (L5)

Research output: Contribution to journal › Article › peer-review

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.

Original language	English
Pages (from-to)	628-637
Number of pages	10
Journal	Nature Medicine
Volume	24
Issue number	5
Early online date	30 Apr 2018
DOIs	https://doi.org/10.1038/s41591-018-0009-7
Publication status	Published - 2018

Research Beacons, Institutes and Platforms

Manchester Cancer Research Centre

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1038/s41591-018-0009-7

Cite this

Tutt, A., Tovey, H., Cheang, M. C. U., Kernaghan, S., Kilburn, L., Gazinska, P., Owen, J., Abraham, J., Barrett, S., Barrett-Lee, P., Brown, R., Chan, S., Dowsett, M., Flanagan, J. M., Fox, L., Grigoriadis, A., Gutin, A., Harper-Wynne, C., Hatton, M. Q., ... Bliss, J. M. (2018). Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial. Nature Medicine, 24(5), 628-637. https://doi.org/10.1038/s41591-018-0009-7

@article{8912937272c64628a25a6e84332de448,

title = "Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial",

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.",

author = "Andrew Tutt and Holly Tovey and Cheang, {Maggie Chon U.} and Sarah Kernaghan and Lucy Kilburn and Patrycja Gazinska and Julie Owen and Jacinta Abraham and Sophie Barrett and Peter Barrett-Lee and Robert Brown and Stephen Chan and Mitchell Dowsett and Flanagan, {James M.} and Lisa Fox and Anita Grigoriadis and Alexander Gutin and Catherine Harper-Wynne and Hatton, {Matthew Q.} and Hoadley, {Katherine A.} and Jyoti Parikh and Peter Parker and Perou, {Charles M.} and Rebecca Roylance and Vandna Shah and Adam Shaw and Smith, {Ian E.} and Timms, {Kirsten M.} and Wardley, {Andrew M.} and Gregory Wilson and Cheryl Gillett and Lanchbury, {Jerry S.} and Alan Ashworth and Nazneen Rahman and Mark Harries and Paul Ellis and Pinder, {Sarah E.} and Bliss, {Judith M.}",

year = "2018",

doi = "10.1038/s41591-018-0009-7",

language = "English",

volume = "24",

pages = "628--637",

journal = "Nature Medicine",

issn = "1078-8956",

publisher = "Nature Research",

number = "5",

}

Tutt, A, Tovey, H, Cheang, MCU, Kernaghan, S, Kilburn, L, Gazinska, P, Owen, J, Abraham, J, Barrett, S, Barrett-Lee, P, Brown, R, Chan, S, Dowsett, M, Flanagan, JM, Fox, L, Grigoriadis, A, Gutin, A, Harper-Wynne, C, Hatton, MQ, Hoadley, KA, Parikh, J, Parker, P, Perou, CM, Roylance, R, Shah, V, Shaw, A, Smith, IE, Timms, KM, Wardley, AM, Wilson, G, Gillett, C, Lanchbury, JS, Ashworth, A, Rahman, N, Harries, M, Ellis, P, Pinder, SE & Bliss, JM 2018, 'Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial', Nature Medicine, vol. 24, no. 5, pp. 628-637. https://doi.org/10.1038/s41591-018-0009-7

TY - JOUR

T1 - Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups

T2 - The TNT Trial

AU - Tutt, Andrew

AU - Tovey, Holly

AU - Cheang, Maggie Chon U.

AU - Kernaghan, Sarah

AU - Kilburn, Lucy

AU - Gazinska, Patrycja

AU - Owen, Julie

AU - Abraham, Jacinta

AU - Barrett, Sophie

AU - Barrett-Lee, Peter

AU - Brown, Robert

AU - Chan, Stephen

AU - Dowsett, Mitchell

AU - Flanagan, James M.

AU - Fox, Lisa

AU - Grigoriadis, Anita

AU - Gutin, Alexander

AU - Harper-Wynne, Catherine

AU - Hatton, Matthew Q.

AU - Hoadley, Katherine A.

AU - Parikh, Jyoti

AU - Parker, Peter

AU - Perou, Charles M.

AU - Roylance, Rebecca

AU - Shah, Vandna

AU - Shaw, Adam

AU - Smith, Ian E.

AU - Timms, Kirsten M.

AU - Wardley, Andrew M.

AU - Wilson, Gregory

AU - Gillett, Cheryl

AU - Lanchbury, Jerry S.

AU - Ashworth, Alan

AU - Rahman, Nazneen

AU - Harries, Mark

AU - Ellis, Paul

AU - Pinder, Sarah E.

AU - Bliss, Judith M.

PY - 2018

Y1 - 2018

N2 - 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.

AB - 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.

UR - http://www.scopus.com/inward/record.url?scp=85046110400&partnerID=8YFLogxK

U2 - 10.1038/s41591-018-0009-7

DO - 10.1038/s41591-018-0009-7

M3 - Article

AN - SCOPUS:85046110400

SN - 1078-8956

VL - 24

SP - 628

EP - 637

JO - Nature Medicine

JF - Nature Medicine

IS - 5

ER -

Carboplatin in BRCA1/2-mutated and triple-negative breast cancer BRCAness subgroups: The TNT Trial

Abstract

Research Beacons, Institutes and Platforms

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this