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author Castroviejo‐Bermejo, Marta
Cruz, Cristina
Llop‐Guevara, Alba
Gutiérrez‐Enríquez, Sara
Ducy, Mandy
Ibrahim, Yasir Hussein
Gris‐Oliver, Albert
Pellegrino, Benedetta
Bruna, Alejandra
Guzmán, Marta
Rodríguez, Olga
Grueso, Judit
Bonache, Sandra
Moles‐Fernández, Alejandro
Villacampa, Guillermo
Viaplana, Cristina
Gómez, Patricia
Vidal, Marc
Peg, Vicente
Serres‐Créixams, Xavier
Dellaire, Graham
Simard, Jacques
Nuciforo, Paolo
Rubio, Isabel T
Dientsmann, Rodrigo
Barrett, J Carl
Caldas, Carlos
Baselga, José
Saura, Cristina
Cortés, Javier
Déas, Olivier
Jonkers, Jos
Masson, Jean‐Yves
Cairo, Stefano
Judde, Jean‐Gabriel
O'Connor, Mark J
Díez, Orland
Balmaña, Judith
Serra, Violeta
author_facet Castroviejo‐Bermejo, Marta
Cruz, Cristina
Llop‐Guevara, Alba
Gutiérrez‐Enríquez, Sara
Ducy, Mandy
Ibrahim, Yasir Hussein
Gris‐Oliver, Albert
Pellegrino, Benedetta
Bruna, Alejandra
Guzmán, Marta
Rodríguez, Olga
Grueso, Judit
Bonache, Sandra
Moles‐Fernández, Alejandro
Villacampa, Guillermo
Viaplana, Cristina
Gómez, Patricia
Vidal, Marc
Peg, Vicente
Serres‐Créixams, Xavier
Dellaire, Graham
Simard, Jacques
Nuciforo, Paolo
Rubio, Isabel T
Dientsmann, Rodrigo
Barrett, J Carl
Caldas, Carlos
Baselga, José
Saura, Cristina
Cortés, Javier
Déas, Olivier
Jonkers, Jos
Masson, Jean‐Yves
Cairo, Stefano
Judde, Jean‐Gabriel
O'Connor, Mark J
Díez, Orland
Balmaña, Judith
Serra, Violeta
author_sort Castroviejo‐Bermejo, Marta
collection PubMed
description Poly(ADP‐ribose) polymerase (PARP) inhibitors (PARPi) are effective in cancers with defective homologous recombination DNA repair (HRR), including BRCA1/2‐related cancers. A test to identify additional HRR‐deficient tumors will help to extend their use in new indications. We evaluated the activity of the PARPi olaparib in patient‐derived tumor xenografts (PDXs) from breast cancer (BC) patients and investigated mechanisms of sensitivity through exome sequencing, BRCA1 promoter methylation analysis, and immunostaining of HRR proteins, including RAD51 nuclear foci. In an independent BC PDX panel, the predictive capacity of the RAD51 score and the homologous recombination deficiency (HRD) score were compared. To examine the clinical feasibility of the RAD51 assay, we scored archival breast tumor samples, including PALB2‐related hereditary cancers. The RAD51 score was highly discriminative of PARPi sensitivity versus PARPi resistance in BC PDXs and outperformed the genomic test. In clinical samples, all PALB2‐related tumors were classified as HRR‐deficient by the RAD51 score. The functional biomarker RAD51 enables the identification of PARPi‐sensitive BC and broadens the population who may benefit from this therapy beyond BRCA1/2‐related cancers.
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spelling pubmed-62844402018-12-14 A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation Castroviejo‐Bermejo, Marta Cruz, Cristina Llop‐Guevara, Alba Gutiérrez‐Enríquez, Sara Ducy, Mandy Ibrahim, Yasir Hussein Gris‐Oliver, Albert Pellegrino, Benedetta Bruna, Alejandra Guzmán, Marta Rodríguez, Olga Grueso, Judit Bonache, Sandra Moles‐Fernández, Alejandro Villacampa, Guillermo Viaplana, Cristina Gómez, Patricia Vidal, Marc Peg, Vicente Serres‐Créixams, Xavier Dellaire, Graham Simard, Jacques Nuciforo, Paolo Rubio, Isabel T Dientsmann, Rodrigo Barrett, J Carl Caldas, Carlos Baselga, José Saura, Cristina Cortés, Javier Déas, Olivier Jonkers, Jos Masson, Jean‐Yves Cairo, Stefano Judde, Jean‐Gabriel O'Connor, Mark J Díez, Orland Balmaña, Judith Serra, Violeta EMBO Mol Med Research Articles Poly(ADP‐ribose) polymerase (PARP) inhibitors (PARPi) are effective in cancers with defective homologous recombination DNA repair (HRR), including BRCA1/2‐related cancers. A test to identify additional HRR‐deficient tumors will help to extend their use in new indications. We evaluated the activity of the PARPi olaparib in patient‐derived tumor xenografts (PDXs) from breast cancer (BC) patients and investigated mechanisms of sensitivity through exome sequencing, BRCA1 promoter methylation analysis, and immunostaining of HRR proteins, including RAD51 nuclear foci. In an independent BC PDX panel, the predictive capacity of the RAD51 score and the homologous recombination deficiency (HRD) score were compared. To examine the clinical feasibility of the RAD51 assay, we scored archival breast tumor samples, including PALB2‐related hereditary cancers. The RAD51 score was highly discriminative of PARPi sensitivity versus PARPi resistance in BC PDXs and outperformed the genomic test. In clinical samples, all PALB2‐related tumors were classified as HRR‐deficient by the RAD51 score. The functional biomarker RAD51 enables the identification of PARPi‐sensitive BC and broadens the population who may benefit from this therapy beyond BRCA1/2‐related cancers. John Wiley and Sons Inc. 2018-10-30 2018-12 /pmc/articles/PMC6284440/ /pubmed/30377213 http://dx.doi.org/10.15252/emmm.201809172 Text en © 2018 The Authors. Published under the terms of the CC BY 4.0 license This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Castroviejo‐Bermejo, Marta
Cruz, Cristina
Llop‐Guevara, Alba
Gutiérrez‐Enríquez, Sara
Ducy, Mandy
Ibrahim, Yasir Hussein
Gris‐Oliver, Albert
Pellegrino, Benedetta
Bruna, Alejandra
Guzmán, Marta
Rodríguez, Olga
Grueso, Judit
Bonache, Sandra
Moles‐Fernández, Alejandro
Villacampa, Guillermo
Viaplana, Cristina
Gómez, Patricia
Vidal, Marc
Peg, Vicente
Serres‐Créixams, Xavier
Dellaire, Graham
Simard, Jacques
Nuciforo, Paolo
Rubio, Isabel T
Dientsmann, Rodrigo
Barrett, J Carl
Caldas, Carlos
Baselga, José
Saura, Cristina
Cortés, Javier
Déas, Olivier
Jonkers, Jos
Masson, Jean‐Yves
Cairo, Stefano
Judde, Jean‐Gabriel
O'Connor, Mark J
Díez, Orland
Balmaña, Judith
Serra, Violeta
A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title_full A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title_fullStr A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title_full_unstemmed A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title_short A RAD51 assay feasible in routine tumor samples calls PARP inhibitor response beyond BRCA mutation
title_sort rad51 assay feasible in routine tumor samples calls parp inhibitor response beyond brca mutation
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6284440/
https://www.ncbi.nlm.nih.gov/pubmed/30377213
http://dx.doi.org/10.15252/emmm.201809172
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