BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib

BACKGROUND: About 15% of Triple-Negative-Breast-Cancer (TNBC) present silencing of the BRCA1 promoter methylation and are assumed to be Homologous Recombination Deficient (HRD). BRCA1-methylated (BRCA1-Me) TNBC could, thus, be eligible to treatment based on PARP-inhibitors or Platinum salts. However...

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Autores principales: Velazquez, Carolina, Orhan, Esin, Tabet, Imene, Fenou, Lise, Orsetti, Béatrice, Adélaïde, José, Guille, Arnaud, Thézénas, Simon, Crapez, Evelyne, Colombo, Pierre-Emmanuel, Chaffanet, Max, Birnbaum, Daniel, Sardet, Claude, Jacot, William, Theillet, Charles
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10064050/
https://www.ncbi.nlm.nih.gov/pubmed/37007122
http://dx.doi.org/10.3389/fonc.2023.1125021
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author Velazquez, Carolina
Orhan, Esin
Tabet, Imene
Fenou, Lise
Orsetti, Béatrice
Adélaïde, José
Guille, Arnaud
Thézénas, Simon
Crapez, Evelyne
Colombo, Pierre-Emmanuel
Chaffanet, Max
Birnbaum, Daniel
Sardet, Claude
Jacot, William
Theillet, Charles
author_facet Velazquez, Carolina
Orhan, Esin
Tabet, Imene
Fenou, Lise
Orsetti, Béatrice
Adélaïde, José
Guille, Arnaud
Thézénas, Simon
Crapez, Evelyne
Colombo, Pierre-Emmanuel
Chaffanet, Max
Birnbaum, Daniel
Sardet, Claude
Jacot, William
Theillet, Charles
author_sort Velazquez, Carolina
collection PubMed
description BACKGROUND: About 15% of Triple-Negative-Breast-Cancer (TNBC) present silencing of the BRCA1 promoter methylation and are assumed to be Homologous Recombination Deficient (HRD). BRCA1-methylated (BRCA1-Me) TNBC could, thus, be eligible to treatment based on PARP-inhibitors or Platinum salts. However, their actual HRD status is discussed, as these tumors are suspected to develop resistance after chemotherapy exposure. METHODS: We interrogated the sensitivity to olaparib vs. carboplatin of 8 TNBC Patient-Derived Xenografts (PDX) models. Four PDX corresponded to BRCA1-Me, of which 3 were previously exposed to NeoAdjuvant-Chemotherapy (NACT). The remaining PDX models corresponded to two BRCA1-mutated (BRCA1-Mut) and two BRCA1-wild type PDX that were respectively included as positive and negative controls. The HRD status of our PDX models was assessed using both genomic signatures and the functional BRCA1 and RAD51 nuclear foci formation assay. To assess HR restoration associated with olaparib resistance, we studied pairs of BRCA1 deficient cell lines and their resistant subclones. RESULTS: The 3 BRCA1-Me PDX that had been exposed to NACT responded poorly to olaparib, likewise BRCA1-WT PDX. Contrastingly, 3 treatment-naïve BRCA1-deficient PDX (1 BRCA1-Me and 2 BRCA1-mutated) responded to olaparib. Noticeably, the three olaparib-responsive PDX scored negative for BRCA1- and RAD51-foci, whereas all non-responsive PDX models, including the 3 NACT-exposed BRCA1-Me PDX, scored positive for RAD51-foci. This suggested HRD in olaparib responsive PDX, while non-responsive models were HR proficient. These results were consistent with observations in cell lines showing a significant increase of RAD51-foci in olaparib-resistant subclones compared with sensitive parental cells, suggesting HR restoration in these models. CONCLUSION: Our results thus support the notion that the actual HRD status of BRCA1-Me TNBC, especially if previously exposed to chemotherapy, may be questioned and should be verified using the BRCA1- and RAD51-foci assay.
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spelling pubmed-100640502023-04-01 BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib Velazquez, Carolina Orhan, Esin Tabet, Imene Fenou, Lise Orsetti, Béatrice Adélaïde, José Guille, Arnaud Thézénas, Simon Crapez, Evelyne Colombo, Pierre-Emmanuel Chaffanet, Max Birnbaum, Daniel Sardet, Claude Jacot, William Theillet, Charles Front Oncol Oncology BACKGROUND: About 15% of Triple-Negative-Breast-Cancer (TNBC) present silencing of the BRCA1 promoter methylation and are assumed to be Homologous Recombination Deficient (HRD). BRCA1-methylated (BRCA1-Me) TNBC could, thus, be eligible to treatment based on PARP-inhibitors or Platinum salts. However, their actual HRD status is discussed, as these tumors are suspected to develop resistance after chemotherapy exposure. METHODS: We interrogated the sensitivity to olaparib vs. carboplatin of 8 TNBC Patient-Derived Xenografts (PDX) models. Four PDX corresponded to BRCA1-Me, of which 3 were previously exposed to NeoAdjuvant-Chemotherapy (NACT). The remaining PDX models corresponded to two BRCA1-mutated (BRCA1-Mut) and two BRCA1-wild type PDX that were respectively included as positive and negative controls. The HRD status of our PDX models was assessed using both genomic signatures and the functional BRCA1 and RAD51 nuclear foci formation assay. To assess HR restoration associated with olaparib resistance, we studied pairs of BRCA1 deficient cell lines and their resistant subclones. RESULTS: The 3 BRCA1-Me PDX that had been exposed to NACT responded poorly to olaparib, likewise BRCA1-WT PDX. Contrastingly, 3 treatment-naïve BRCA1-deficient PDX (1 BRCA1-Me and 2 BRCA1-mutated) responded to olaparib. Noticeably, the three olaparib-responsive PDX scored negative for BRCA1- and RAD51-foci, whereas all non-responsive PDX models, including the 3 NACT-exposed BRCA1-Me PDX, scored positive for RAD51-foci. This suggested HRD in olaparib responsive PDX, while non-responsive models were HR proficient. These results were consistent with observations in cell lines showing a significant increase of RAD51-foci in olaparib-resistant subclones compared with sensitive parental cells, suggesting HR restoration in these models. CONCLUSION: Our results thus support the notion that the actual HRD status of BRCA1-Me TNBC, especially if previously exposed to chemotherapy, may be questioned and should be verified using the BRCA1- and RAD51-foci assay. Frontiers Media S.A. 2023-03-17 /pmc/articles/PMC10064050/ /pubmed/37007122 http://dx.doi.org/10.3389/fonc.2023.1125021 Text en Copyright © 2023 Velazquez, Orhan, Tabet, Fenou, Orsetti, Adélaïde, Guille, Thézénas, Crapez, Colombo, Chaffanet, Birnbaum, Sardet, Jacot and Theillet https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Velazquez, Carolina
Orhan, Esin
Tabet, Imene
Fenou, Lise
Orsetti, Béatrice
Adélaïde, José
Guille, Arnaud
Thézénas, Simon
Crapez, Evelyne
Colombo, Pierre-Emmanuel
Chaffanet, Max
Birnbaum, Daniel
Sardet, Claude
Jacot, William
Theillet, Charles
BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title_full BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title_fullStr BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title_full_unstemmed BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title_short BRCA1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form RAD51 foci and respond poorly to olaparib
title_sort brca1-methylated triple negative breast cancers previously exposed to neoadjuvant chemotherapy form rad51 foci and respond poorly to olaparib
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10064050/
https://www.ncbi.nlm.nih.gov/pubmed/37007122
http://dx.doi.org/10.3389/fonc.2023.1125021
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