Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients

INTRODUCTION: With the emergence of targeted therapies, there is a need to accurately identify more tumor biomarkers. The EXOMA trial was designed to offer tumor and germline exome sequencing (ES) to patients with solid malignant tumors and facing therapeutic failure. As hereditary cancer predisposi...

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Autores principales: Mazel, Benoit, Bertolone, Geoffrey, Baurand, Amandine, Cosset, Elodie, Sawka, Caroline, Robert, Marion, Gautier, Elodie, Lançon, Allan, Réda, Manon, Favier, Laure, Dérangère, Valentin, Richard, Corentin, Binquet, Christine, Boidot, Romain, Goussot, Vincent, Albuisson, Juliette, Ghiringhelli, François, Faivre, Laurence, Nambot, Sophie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2023
Materias:
RESEARCH ARTICLES
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10557826/
https://www.ncbi.nlm.nih.gov/pubmed/37694493
http://dx.doi.org/10.1002/cam4.6498
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author Mazel, Benoit
Bertolone, Geoffrey
Baurand, Amandine
Cosset, Elodie
Sawka, Caroline
Robert, Marion
Gautier, Elodie
Lançon, Allan
Réda, Manon
Favier, Laure
Dérangère, Valentin
Richard, Corentin
Binquet, Christine
Boidot, Romain
Goussot, Vincent
Albuisson, Juliette
Ghiringhelli, François
Faivre, Laurence
Nambot, Sophie
author_facet Mazel, Benoit
Bertolone, Geoffrey
Baurand, Amandine
Cosset, Elodie
Sawka, Caroline
Robert, Marion
Gautier, Elodie
Lançon, Allan
Réda, Manon
Favier, Laure
Dérangère, Valentin
Richard, Corentin
Binquet, Christine
Boidot, Romain
Goussot, Vincent
Albuisson, Juliette
Ghiringhelli, François
Faivre, Laurence
Nambot, Sophie
author_sort Mazel, Benoit
collection PubMed
description INTRODUCTION: With the emergence of targeted therapies, there is a need to accurately identify more tumor biomarkers. The EXOMA trial was designed to offer tumor and germline exome sequencing (ES) to patients with solid malignant tumors and facing therapeutic failure. As hereditary cancer predispositions could be identified, with genetic counseling and health management implications, a genetic consultation was systematically established. This design needs to be discussed as genetic human resources are limited and indication of theranostic tests will increase. METHODS: Genetic counseling was conducted within 15 days following inclusion in the study for patients recruited between December 2015 and July 2019. In silico analyses from theranostic ES were limited to 317 genes involved in oncogenesis, from both tumor and blood DNA. RESULTS: Six hundred and sixty six patients had a genetic consultation before ES. In 65/666 patients, 66 germline pathogenic or likely pathogenic (P/LP) variants were identified in 16 actionable genes and seven non‐actionable genes according to French guidelines. 24/65 patients had previously received genetic analysis for diagnostic purposes, and for 17 of them, a P/LP variant had already been identified. Among the 48/65 remaining cases for which the EXOMA protocol revealed a previously unknown P/LP variant, only 19 met the criteria for genetic testing for inherited cancer risk after familial survey. These criteria had not been identified by the oncologist in 10 cases. In 21/65 cases, the variant was considered incidental. DISCUSSION: In 7.4% of patients, an undiagnosed hereditary genetic predisposition was identified, whether or not related to the clinical presentation, and germline analysis impacted oncological management for only 6.3% of the cohort. This low percentage should be weighed against the burden of systematic genetic consultation and urgent circuits. Information or training tools to form oncologists to the prescription of germline genetic analyses should be explored, as well as information supports and patient preferences.
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spelling pubmed-105578262023-10-07 Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients Mazel, Benoit Bertolone, Geoffrey Baurand, Amandine Cosset, Elodie Sawka, Caroline Robert, Marion Gautier, Elodie Lançon, Allan Réda, Manon Favier, Laure Dérangère, Valentin Richard, Corentin Binquet, Christine Boidot, Romain Goussot, Vincent Albuisson, Juliette Ghiringhelli, François Faivre, Laurence Nambot, Sophie Cancer Med RESEARCH ARTICLES INTRODUCTION: With the emergence of targeted therapies, there is a need to accurately identify more tumor biomarkers. The EXOMA trial was designed to offer tumor and germline exome sequencing (ES) to patients with solid malignant tumors and facing therapeutic failure. As hereditary cancer predispositions could be identified, with genetic counseling and health management implications, a genetic consultation was systematically established. This design needs to be discussed as genetic human resources are limited and indication of theranostic tests will increase. METHODS: Genetic counseling was conducted within 15 days following inclusion in the study for patients recruited between December 2015 and July 2019. In silico analyses from theranostic ES were limited to 317 genes involved in oncogenesis, from both tumor and blood DNA. RESULTS: Six hundred and sixty six patients had a genetic consultation before ES. In 65/666 patients, 66 germline pathogenic or likely pathogenic (P/LP) variants were identified in 16 actionable genes and seven non‐actionable genes according to French guidelines. 24/65 patients had previously received genetic analysis for diagnostic purposes, and for 17 of them, a P/LP variant had already been identified. Among the 48/65 remaining cases for which the EXOMA protocol revealed a previously unknown P/LP variant, only 19 met the criteria for genetic testing for inherited cancer risk after familial survey. These criteria had not been identified by the oncologist in 10 cases. In 21/65 cases, the variant was considered incidental. DISCUSSION: In 7.4% of patients, an undiagnosed hereditary genetic predisposition was identified, whether or not related to the clinical presentation, and germline analysis impacted oncological management for only 6.3% of the cohort. This low percentage should be weighed against the burden of systematic genetic consultation and urgent circuits. Information or training tools to form oncologists to the prescription of germline genetic analyses should be explored, as well as information supports and patient preferences. John Wiley and Sons Inc. 2023-09-11 /pmc/articles/PMC10557826/ /pubmed/37694493 http://dx.doi.org/10.1002/cam4.6498 Text en © 2023 The Authors. Cancer Medicine published by John Wiley & Sons Ltd. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://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
Mazel, Benoit
Bertolone, Geoffrey
Baurand, Amandine
Cosset, Elodie
Sawka, Caroline
Robert, Marion
Gautier, Elodie
Lançon, Allan
Réda, Manon
Favier, Laure
Dérangère, Valentin
Richard, Corentin
Binquet, Christine
Boidot, Romain
Goussot, Vincent
Albuisson, Juliette
Ghiringhelli, François
Faivre, Laurence
Nambot, Sophie
Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title_full Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title_fullStr Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title_full_unstemmed Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title_short Advancing precision oncology through systematic germline and tumor genetic analysis: The oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
title_sort advancing precision oncology through systematic germline and tumor genetic analysis: the oncogenetic point of view on findings from a prospective multicenter clinical trial of 666 patients
topic RESEARCH ARTICLES
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10557826/
https://www.ncbi.nlm.nih.gov/pubmed/37694493
http://dx.doi.org/10.1002/cam4.6498
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