Journal
CANCER RESEARCH
Volume 82, Issue 8, Pages 1646-1657Publisher
AMER ASSOC CANCER RESEARCH
DOI: 10.1158/0008-5472.CAN-21-2409
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Funding
- CERCA Program/Generalitat de Catalunya
- AstraZeneca
- Tesaro
- Catalan Agency AGAUR-FEDER [2017 SGR 540, 2019PROD00045]
- Instituto de Salud Carlos III (ISCIII), an initiative of the Spanish Ministry of Economy and Innovation - European Regional Development FEDER Funds [PI12/02606, PI17/01080, PI19/01303, PI20/00892, CP14/00228, CPII19/00033]
- Transcan-2 [AC15/00063]
- Spanish Association of Cancer Research (AECC) [LABAE16020PORTT]
- SPORE in Breast Cancer [NIH P50CA098131]
- La Caixa Foundation
- European Institute of Innovation and Technology/Horizon 2020 (CaixaImpulse) [LCF/TR/CC19/52470003]
- ESMO
- Roche
- Generalitat de Catalunya [PERIS SLT017/20/000081, PERIS SLT002/16/00477]
- AECC [INVES20095LLOP]
- La Caixa Foundation [100010434, LCF/BQ/DI19/11730051]
- Breast Cancer Research Foundation [BCRF-19-08]
- Instituto de Salud Carlos III project [AC15/00062]
- EC - FEDER, Instituto de Salud Carlos III [CB16/12/00449, PI19/01181]
- FERO Foundation
- ISCIII
- European Union's Horizon 2020 research and innovation programme under the Marie Skodowska-Curiegrant [837900]
- Cancer Research UK (CRUK) [C60100/A23916, C60100/A25274]
- National Institute of Health Research (NIHR) Cambridge Biomedical Research Centre grant [BRC-125-20014]
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PARP inhibitors are approved drugs for certain cancers such as ovarian, breast, prostate, and pancreatic cancers. This study validated a new test method for predicting patient response to PARPi and platinum-based therapies, showing higher accuracy compared to other detection methods. The results support further clinical assessment of this test in patient samples.
PARP inhibitors (PARPi) are approved drugs for platinum-sensitive, high-grade serous ovarian cancer (HGSOC) and for breast, prostate, and pancreatic cancers (PaC) harboring genetic alterations impairing homologous recombination repair (HRR). Detection of nuclear RAD51 foci in tumor cells is a marker of HRR functionality, and we previously established a test to detect RAD51 nuclear foci. Here, we aimed to validate the RAD51 score cut off and compare the performance of this test to other HRR deficiency (HRD) detection methods. Laboratory models from BRCA1/BRCA2-associated breast cancer, HGSOC, and PaC were developed and evaluated for their response to PARPi and cisplatin. HRD in these models and patient samples was evaluated by DNA sequencing of HRR genes, genomic HRD tests, and RAD51 foci detection. We established patient-derived xenograft models from breast cancer (n = 103), HGSOC (n = 4), and PaC (n = 2) that recapitulated patient HRD status and treatment response. The RAD51 test showed higher accuracy than HRR gene mutations and genomic HRD analysis for pre-dicting PARPi response (95%, 67%, and 71%, respectively). RAD51 detection captured dynamic changes in HRR status upon acquisition of PARPi resistance. The accuracy of the RAD51 test was similar to HRR gene mutations for predicting platinum response. The predefined RAD51 score cut off was validated, and the high predictive value of the RAD51 test in preclinical models was confirmed. These results collectively support pursuing clinical assessment of the RAD51 test in patient samples from randomized trials testing PARPi or platinum-based therapies. [GRAPHICS] .
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