Journal
CANCER RESEARCH
Volume 79, Issue 16, Pages 4258-4270Publisher
AMER ASSOC CANCER RESEARCH
DOI: 10.1158/0008-5472.CAN-18-3835
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Funding
- Spanish Ministerio de Ciencia, Innovacion y Universidades, Agencia Estatal de Investigacion (AEI) [SAF2008-01975, SAF2011-22893, SAF2014-55997-R, SAF2017-86117-R]
- ISCIII [PIE13/00022, CP14/0028]
- European Regional Development Fund. ERDF, a way to build Europe
- Susan Komen Foundation [CCR13262449]
- ERC [LS4-682935]
- MICINN
- FI programme of the Secretariat for Universities and Research of the Department of Business and Knowledge of the Government of Catalonia
- European Social Fund (ESF) ESF, Investing in your future
- GHD-pink research support via the FERO Foundation
- Breast Cancer Research Foundation [BCRF-17-008]
- Instituto de Salud Carlos III [PI16/00253, CB16/12/00449, PI13/01718]
- AECC grant [AIOC15152806CRUZ]
- Spanish Ministry of Economy and Competitivity MINECO [SAF2017-87811R]
- FIS [PI12-02606]
- Cancer Research UK
- Breast Cancer Research Foundation
- Susan G. Komen Foundation
- V Foundation
- NIH/NCI [U54CA224076]
- BCM Breast Cancer SPORE [P50 CA186784]
- BCM Cancer Center grant [P30 CA125123]
- Cancer Prevention & Research Institutes of Texas [CPRIT RR160027]
- StandUp To Cancer-American Association for Cancer Research Dream Team Translational Cancer Research Grant [SU2C-AACR-DT0209]
- Mary Kay Ash Foundation
- Ovarian Cancer Research Foundation
- Breast Cancer Alliance
- NIH [RO1 1R01CA226776-01]
- Merck Co.
- [PI15/00854]
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Taxanes are the mainstay of treatment in triple-negative breast cancer (TNBC), with de novo and acquired resistance limiting patient's survival. To investigate the genetic basis of docetaxel resistance in TNBC, exome sequencing was performed on matched TNBC patient-derived xenografts (PDX) sensitive to docetaxel and their counterparts that developed resistance in vivo upon continuous drug exposure. Most mutations, small insertions/deletions, and copy number alterations detected in the initial TNBC human metastatic samples were maintained after serial passages in mice and emergence of resistance. We identified a chromosomal amplification of chr12p in a human BRCA1-mutated metastatic sample and the derived chemoresistant PDX, but not in the matched docetaxel-sensitive PDX tumor. Chr12p amplification was validated in a second pair of docetaxel-sensitive/resistant BRCA1-mutated PDXs and after short-term docetaxel treatment in several TNBC/BRCA1-mutated PDXs and cell lines, as well as during metastatic recurrence in a patient with BRCA1-mutated breast cancer who had progressed on docetaxel treatment. Analysis of clinical data indicates an association between chr12p amplification and patients with TNBC/basal-like breast cancer, a BRCA1 mutational signature, and poor survival after chemotherapy. Detection of chr12p amplification in a cohort of TNBC PDX models was associated with an improved response to carboplatin. Our findings reveal tumor clonal dynamics during chemotherapy treatments and suggest that a preexisting population harboring chr12p amplification is associated with the emergence of docetaxel resistance and carboplatin responsiveness in TNBC/BRCA1-mutated tumors. Significance: Chr12p copy number gains indicate rapid emergence of resistance to docetaxel and increased sensitivity to carboplatin, therefore sequential docetaxel/carboplatin treatment could improve survival in TNBC/BRCA1 patients.
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