Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families

The introduction of multigene panel testing for hereditary breast/ovarian cancer screening has greatly improved efficiency, speed, and costs. However, its clinical utility is still debated, mostly due to the lack of conclusive evidences on the impact of newly discovered genetic variants on cancer ri...

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Autores principales: Coppa, Anna, Nicolussi, Arianna, D'Inzeo, Sonia, Capalbo, Carlo, Belardinilli, Francesca, Colicchia, Valeria, Petroni, Marialaura, Zani, Massimo, Ferraro, Sergio, Rinaldi, Christian, Buffone, Amelia, Bartolazzi, Armando, Screpanti, Isabella, Ottini, Laura, Giannini, Giuseppe
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Clinical Cancer Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5773970/
https://www.ncbi.nlm.nih.gov/pubmed/29271107
http://dx.doi.org/10.1002/cam4.1251
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author Coppa, Anna
Nicolussi, Arianna
D'Inzeo, Sonia
Capalbo, Carlo
Belardinilli, Francesca
Colicchia, Valeria
Petroni, Marialaura
Zani, Massimo
Ferraro, Sergio
Rinaldi, Christian
Buffone, Amelia
Bartolazzi, Armando
Screpanti, Isabella
Ottini, Laura
Giannini, Giuseppe
author_facet Coppa, Anna
Nicolussi, Arianna
D'Inzeo, Sonia
Capalbo, Carlo
Belardinilli, Francesca
Colicchia, Valeria
Petroni, Marialaura
Zani, Massimo
Ferraro, Sergio
Rinaldi, Christian
Buffone, Amelia
Bartolazzi, Armando
Screpanti, Isabella
Ottini, Laura
Giannini, Giuseppe
author_sort Coppa, Anna
collection PubMed
description The introduction of multigene panel testing for hereditary breast/ovarian cancer screening has greatly improved efficiency, speed, and costs. However, its clinical utility is still debated, mostly due to the lack of conclusive evidences on the impact of newly discovered genetic variants on cancer risk and lack of evidence‐based guidelines for the clinical management of their carriers. In this pilot study, we aimed to test whether a systematic and multiparametric characterization of newly discovered mutations could enhance the clinical utility of multigene panel sequencing. Out of a pool of 367 breast/ovarian cancer families Sanger‐sequenced for BRCA1 and BRCA2 gene mutations, we selected a cohort of 20 BRCA1/2‐negative families to be subjected to the BROCA‐Cancer Risk Panel massive parallel sequencing. As a strategy for the systematic characterization of newly discovered genetic variants, we collected blood and cancer tissue samples and established lymphoblastoid cell lines from all available individuals in these families, to perform segregation analysis, loss‐of‐heterozygosity and further molecular studies. We identified loss‐of‐function mutations in 6 out 20 high‐risk families, 5 of which occurred on BRCA1,CHEK2 and ATM and are esteemed to be risk‐relevant. In contrast, a novel RAD50 truncating mutation is most likely unrelated to breast cancer. Our data suggest that integrating multigene panel testing with a pre‐organized, multiparametric characterization of newly discovered genetic variants improves the identification of risk‐relevant alleles impacting on the clinical management of their carriers.
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spelling pubmed-57739702018-02-07 Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families Coppa, Anna Nicolussi, Arianna D'Inzeo, Sonia Capalbo, Carlo Belardinilli, Francesca Colicchia, Valeria Petroni, Marialaura Zani, Massimo Ferraro, Sergio Rinaldi, Christian Buffone, Amelia Bartolazzi, Armando Screpanti, Isabella Ottini, Laura Giannini, Giuseppe Cancer Med Clinical Cancer Research The introduction of multigene panel testing for hereditary breast/ovarian cancer screening has greatly improved efficiency, speed, and costs. However, its clinical utility is still debated, mostly due to the lack of conclusive evidences on the impact of newly discovered genetic variants on cancer risk and lack of evidence‐based guidelines for the clinical management of their carriers. In this pilot study, we aimed to test whether a systematic and multiparametric characterization of newly discovered mutations could enhance the clinical utility of multigene panel sequencing. Out of a pool of 367 breast/ovarian cancer families Sanger‐sequenced for BRCA1 and BRCA2 gene mutations, we selected a cohort of 20 BRCA1/2‐negative families to be subjected to the BROCA‐Cancer Risk Panel massive parallel sequencing. As a strategy for the systematic characterization of newly discovered genetic variants, we collected blood and cancer tissue samples and established lymphoblastoid cell lines from all available individuals in these families, to perform segregation analysis, loss‐of‐heterozygosity and further molecular studies. We identified loss‐of‐function mutations in 6 out 20 high‐risk families, 5 of which occurred on BRCA1,CHEK2 and ATM and are esteemed to be risk‐relevant. In contrast, a novel RAD50 truncating mutation is most likely unrelated to breast cancer. Our data suggest that integrating multigene panel testing with a pre‐organized, multiparametric characterization of newly discovered genetic variants improves the identification of risk‐relevant alleles impacting on the clinical management of their carriers. John Wiley and Sons Inc. 2017-12-22 /pmc/articles/PMC5773970/ /pubmed/29271107 http://dx.doi.org/10.1002/cam4.1251 Text en © 2017 The Authors. Cancer Medicine published by John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (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 Clinical Cancer Research
Coppa, Anna
Nicolussi, Arianna
D'Inzeo, Sonia
Capalbo, Carlo
Belardinilli, Francesca
Colicchia, Valeria
Petroni, Marialaura
Zani, Massimo
Ferraro, Sergio
Rinaldi, Christian
Buffone, Amelia
Bartolazzi, Armando
Screpanti, Isabella
Ottini, Laura
Giannini, Giuseppe
Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title_full Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title_fullStr Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title_full_unstemmed Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title_short Optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
title_sort optimizing the identification of risk‐relevant mutations by multigene panel testing in selected hereditary breast/ovarian cancer families
topic Clinical Cancer Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5773970/
https://www.ncbi.nlm.nih.gov/pubmed/29271107
http://dx.doi.org/10.1002/cam4.1251
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