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A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations

BACKGROUND: For children with cancer, the clinical integration of precision medicine to enable predictive biomarker–based therapeutic stratification is urgently needed. METHODS: We have developed a hybrid-capture next-generation sequencing (NGS) panel, specifically designed to detect genetic alterat...

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Autores principales: George, Sally L., Izquierdo, Elisa, Campbell, James, Koutroumanidou, Eleni, Proszek, Paula, Jamal, Sabri, Hughes, Deborah, Yuan, Lina, Marshall, Lynley V., Carceller, Fernando, Chisholm, Julia C., Vaidya, Sucheta, Mandeville, Henry, Angelini, Paola, Wasti, Ajla, Bexelius, Tomas, Thway, Khin, Gatz, Susanne A., Clarke, Matthew, Al-Lazikani, Bissan, Barone, Giuseppe, Anderson, John, Tweddle, Deborah A., Gonzalez, David, Walker, Brian A., Barton, Jack, Depani, Sarita, Eze, Jessica, Ahmed, Saira W., Moreno, Lucas, Pearson, Andrew, Shipley, Janet, Jones, Chris, Hargrave, Darren, Jacques, Thomas S., Hubank, Michael, Chesler, Louis
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science Ltd 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6839402/
https://www.ncbi.nlm.nih.gov/pubmed/31543384
http://dx.doi.org/10.1016/j.ejca.2019.07.027
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author George, Sally L.
Izquierdo, Elisa
Campbell, James
Koutroumanidou, Eleni
Proszek, Paula
Jamal, Sabri
Hughes, Deborah
Yuan, Lina
Marshall, Lynley V.
Carceller, Fernando
Chisholm, Julia C.
Vaidya, Sucheta
Mandeville, Henry
Angelini, Paola
Wasti, Ajla
Bexelius, Tomas
Thway, Khin
Gatz, Susanne A.
Clarke, Matthew
Al-Lazikani, Bissan
Barone, Giuseppe
Anderson, John
Tweddle, Deborah A.
Gonzalez, David
Walker, Brian A.
Barton, Jack
Depani, Sarita
Eze, Jessica
Ahmed, Saira W.
Moreno, Lucas
Pearson, Andrew
Shipley, Janet
Jones, Chris
Hargrave, Darren
Jacques, Thomas S.
Hubank, Michael
Chesler, Louis
author_facet George, Sally L.
Izquierdo, Elisa
Campbell, James
Koutroumanidou, Eleni
Proszek, Paula
Jamal, Sabri
Hughes, Deborah
Yuan, Lina
Marshall, Lynley V.
Carceller, Fernando
Chisholm, Julia C.
Vaidya, Sucheta
Mandeville, Henry
Angelini, Paola
Wasti, Ajla
Bexelius, Tomas
Thway, Khin
Gatz, Susanne A.
Clarke, Matthew
Al-Lazikani, Bissan
Barone, Giuseppe
Anderson, John
Tweddle, Deborah A.
Gonzalez, David
Walker, Brian A.
Barton, Jack
Depani, Sarita
Eze, Jessica
Ahmed, Saira W.
Moreno, Lucas
Pearson, Andrew
Shipley, Janet
Jones, Chris
Hargrave, Darren
Jacques, Thomas S.
Hubank, Michael
Chesler, Louis
author_sort George, Sally L.
collection PubMed
description BACKGROUND: For children with cancer, the clinical integration of precision medicine to enable predictive biomarker–based therapeutic stratification is urgently needed. METHODS: We have developed a hybrid-capture next-generation sequencing (NGS) panel, specifically designed to detect genetic alterations in paediatric solid tumours, which gives reliable results from as little as 50 ng of DNA extracted from formalin-fixed paraffin-embedded (FFPE) tissue. In this study, we offered an NGS panel, with clinical reporting via a molecular tumour board for children with solid tumours. Furthermore, for a cohort of 12 patients, we used a circulating tumour DNA (ctDNA)–specific panel to sequence ctDNA from matched plasma samples and compared plasma and tumour findings. RESULTS: A total of 255 samples were submitted from 223 patients for the NGS panel. Using FFPE tissue, 82% of all submitted samples passed quality control for clinical reporting. At least one genetic alteration was detected in 70% of sequenced samples. The overall detection rate of clinically actionable alterations, defined by modified OncoKB criteria, for all sequenced samples was 51%. A total of 8 patients were sequenced at different stages of treatment. In 6 of these, there were differences in the genetic alterations detected between time points. Sequencing of matched ctDNA in a cohort of extracranial paediatric solid tumours also identified a high detection rate of somatic alterations in plasma. CONCLUSION: We demonstrate that tailored clinical molecular profiling of both tumour DNA and plasma-derived ctDNA is feasible for children with solid tumours. Furthermore, we show that a targeted NGS panel–based approach can identify actionable genetic alterations in a high proportion of patients.
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spelling pubmed-68394022019-11-12 A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations George, Sally L. Izquierdo, Elisa Campbell, James Koutroumanidou, Eleni Proszek, Paula Jamal, Sabri Hughes, Deborah Yuan, Lina Marshall, Lynley V. Carceller, Fernando Chisholm, Julia C. Vaidya, Sucheta Mandeville, Henry Angelini, Paola Wasti, Ajla Bexelius, Tomas Thway, Khin Gatz, Susanne A. Clarke, Matthew Al-Lazikani, Bissan Barone, Giuseppe Anderson, John Tweddle, Deborah A. Gonzalez, David Walker, Brian A. Barton, Jack Depani, Sarita Eze, Jessica Ahmed, Saira W. Moreno, Lucas Pearson, Andrew Shipley, Janet Jones, Chris Hargrave, Darren Jacques, Thomas S. Hubank, Michael Chesler, Louis Eur J Cancer Article BACKGROUND: For children with cancer, the clinical integration of precision medicine to enable predictive biomarker–based therapeutic stratification is urgently needed. METHODS: We have developed a hybrid-capture next-generation sequencing (NGS) panel, specifically designed to detect genetic alterations in paediatric solid tumours, which gives reliable results from as little as 50 ng of DNA extracted from formalin-fixed paraffin-embedded (FFPE) tissue. In this study, we offered an NGS panel, with clinical reporting via a molecular tumour board for children with solid tumours. Furthermore, for a cohort of 12 patients, we used a circulating tumour DNA (ctDNA)–specific panel to sequence ctDNA from matched plasma samples and compared plasma and tumour findings. RESULTS: A total of 255 samples were submitted from 223 patients for the NGS panel. Using FFPE tissue, 82% of all submitted samples passed quality control for clinical reporting. At least one genetic alteration was detected in 70% of sequenced samples. The overall detection rate of clinically actionable alterations, defined by modified OncoKB criteria, for all sequenced samples was 51%. A total of 8 patients were sequenced at different stages of treatment. In 6 of these, there were differences in the genetic alterations detected between time points. Sequencing of matched ctDNA in a cohort of extracranial paediatric solid tumours also identified a high detection rate of somatic alterations in plasma. CONCLUSION: We demonstrate that tailored clinical molecular profiling of both tumour DNA and plasma-derived ctDNA is feasible for children with solid tumours. Furthermore, we show that a targeted NGS panel–based approach can identify actionable genetic alterations in a high proportion of patients. Elsevier Science Ltd 2019-11 /pmc/articles/PMC6839402/ /pubmed/31543384 http://dx.doi.org/10.1016/j.ejca.2019.07.027 Text en Crown Copyright © 2019 Published by Elsevier Ltd. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
George, Sally L.
Izquierdo, Elisa
Campbell, James
Koutroumanidou, Eleni
Proszek, Paula
Jamal, Sabri
Hughes, Deborah
Yuan, Lina
Marshall, Lynley V.
Carceller, Fernando
Chisholm, Julia C.
Vaidya, Sucheta
Mandeville, Henry
Angelini, Paola
Wasti, Ajla
Bexelius, Tomas
Thway, Khin
Gatz, Susanne A.
Clarke, Matthew
Al-Lazikani, Bissan
Barone, Giuseppe
Anderson, John
Tweddle, Deborah A.
Gonzalez, David
Walker, Brian A.
Barton, Jack
Depani, Sarita
Eze, Jessica
Ahmed, Saira W.
Moreno, Lucas
Pearson, Andrew
Shipley, Janet
Jones, Chris
Hargrave, Darren
Jacques, Thomas S.
Hubank, Michael
Chesler, Louis
A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title_full A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title_fullStr A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title_full_unstemmed A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title_short A tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
title_sort tailored molecular profiling programme for children with cancer to identify clinically actionable genetic alterations
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6839402/
https://www.ncbi.nlm.nih.gov/pubmed/31543384
http://dx.doi.org/10.1016/j.ejca.2019.07.027
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