LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults

OBJECTIVE: Gliomas in adolescents and young adults (AYA) are commonly treated with a standard chemo-radiation approach based on data from adults. The clinical impact of paediatric-type alterations in these tumours is unknown. METHODS: We compiled a multi-institutional cohort of patients diagnosed wi...

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Autores principales: Bennett, Julie, Nobre, Liana, Sheth, Javal, Ryall, Scott, Fang, Karen, Johnson, Monique, Negm, Logine, Chung, Jiil, Komosa, Martin, Nunes, Nuno M, Fat, Mary Jane Lim, Perry, James, Sahgal, Arjun, Detsky, Jay, Bouffet, Eric, Naz-Hazrati, Lili, Dirks, Peter, Ertl-Wagner, Birgit, Kongkham, Paul, Zadeh, Gelareh, Mason, Warren, Climans, Seth, Cusimano, Michael, Das, Sunit, Gao, Andrew, Tsang, Derek, Nguyen, Lananh, Laperriere, Normand, Keith, Julia, Munoz, David, Tabori, Uri, Hawkins, Cynthia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Low Grade Glioma
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165411/
http://dx.doi.org/10.1093/neuonc/noac079.353
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author Bennett, Julie
Nobre, Liana
Sheth, Javal
Ryall, Scott
Fang, Karen
Johnson, Monique
Negm, Logine
Chung, Jiil
Komosa, Martin
Nunes, Nuno M
Fat, Mary Jane Lim
Perry, James
Sahgal, Arjun
Detsky, Jay
Bouffet, Eric
Naz-Hazrati, Lili
Dirks, Peter
Ertl-Wagner, Birgit
Kongkham, Paul
Zadeh, Gelareh
Mason, Warren
Climans, Seth
Cusimano, Michael
Das, Sunit
Gao, Andrew
Tsang, Derek
Nguyen, Lananh
Laperriere, Normand
Keith, Julia
Munoz, David
Tabori, Uri
Hawkins, Cynthia
author_facet Bennett, Julie
Nobre, Liana
Sheth, Javal
Ryall, Scott
Fang, Karen
Johnson, Monique
Negm, Logine
Chung, Jiil
Komosa, Martin
Nunes, Nuno M
Fat, Mary Jane Lim
Perry, James
Sahgal, Arjun
Detsky, Jay
Bouffet, Eric
Naz-Hazrati, Lili
Dirks, Peter
Ertl-Wagner, Birgit
Kongkham, Paul
Zadeh, Gelareh
Mason, Warren
Climans, Seth
Cusimano, Michael
Das, Sunit
Gao, Andrew
Tsang, Derek
Nguyen, Lananh
Laperriere, Normand
Keith, Julia
Munoz, David
Tabori, Uri
Hawkins, Cynthia
author_sort Bennett, Julie
collection PubMed
description OBJECTIVE: Gliomas in adolescents and young adults (AYA) are commonly treated with a standard chemo-radiation approach based on data from adults. The clinical impact of paediatric-type alterations in these tumours is unknown. METHODS: We compiled a multi-institutional cohort of patients diagnosed with glioma between 15-39.9 years over 20 years. Complete molecular analysis, therapeutic data and outcome was collected. For specific alterations, analysis included patients aged 0-39.9 years. RESULTS: A total of 1900 patients with 876 AYA gliomas were included. Ongoing analysis reveals genetic alterations in 95% of available tumours. IDH-mutant tumours account for only 53%, while paediatric-type mutations were found in 35% of AYA tumours with IDH-WT GBM accounting for the remaining 12%. The most common paediatric alterations in AYAs included BRAF p.V600E (11%) and FGFR alterations (6%) while BRAF fusions, H3 p.K27M and H3.3 p.G34R were rarely observed (4%, 4% and 1% respectively). BRAF fused tumours with non-canonical binding partners were enriched in AYAs. Analysis of BRAF-V600E gliomas between ages 0-40 revealed increased tendency for malignant tumours in patients >20 years suggesting malignant transformation possibly due to higher rate of secondary hits including TP53, CDKN2A and ATRX mutations. This resulted in worse overall-survival for AYA patients with BRAF-V600E glioma when compared to children under 20 years (p=0.0032). Ten-year OS of 100%, 90% and 95% was seen for BRAF fused, BRAF-V600E and FGFR-altered AYA low grade glioma respectively, compared to 14% and 25% for BRAF-V600E and FGFR-altered high grade glioma. In contrast, continuous decline was observed in the IDH-mutant gliomas with 10-year OS of 50% which declined to 29% at 15 years. CONCLUSIONS: Gliomas in AYA are enriched for paediatric-type alterations with distinct molecularly-based outcomes. As these tumours carry different outcomes than childhood glioma and may respond to targeted inhibitors, AYA gliomas would benefit from comprehensive diagnostic and therapeutic approaches.
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spelling pubmed-91654112022-06-06 LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults Bennett, Julie Nobre, Liana Sheth, Javal Ryall, Scott Fang, Karen Johnson, Monique Negm, Logine Chung, Jiil Komosa, Martin Nunes, Nuno M Fat, Mary Jane Lim Perry, James Sahgal, Arjun Detsky, Jay Bouffet, Eric Naz-Hazrati, Lili Dirks, Peter Ertl-Wagner, Birgit Kongkham, Paul Zadeh, Gelareh Mason, Warren Climans, Seth Cusimano, Michael Das, Sunit Gao, Andrew Tsang, Derek Nguyen, Lananh Laperriere, Normand Keith, Julia Munoz, David Tabori, Uri Hawkins, Cynthia Neuro Oncol Low Grade Glioma OBJECTIVE: Gliomas in adolescents and young adults (AYA) are commonly treated with a standard chemo-radiation approach based on data from adults. The clinical impact of paediatric-type alterations in these tumours is unknown. METHODS: We compiled a multi-institutional cohort of patients diagnosed with glioma between 15-39.9 years over 20 years. Complete molecular analysis, therapeutic data and outcome was collected. For specific alterations, analysis included patients aged 0-39.9 years. RESULTS: A total of 1900 patients with 876 AYA gliomas were included. Ongoing analysis reveals genetic alterations in 95% of available tumours. IDH-mutant tumours account for only 53%, while paediatric-type mutations were found in 35% of AYA tumours with IDH-WT GBM accounting for the remaining 12%. The most common paediatric alterations in AYAs included BRAF p.V600E (11%) and FGFR alterations (6%) while BRAF fusions, H3 p.K27M and H3.3 p.G34R were rarely observed (4%, 4% and 1% respectively). BRAF fused tumours with non-canonical binding partners were enriched in AYAs. Analysis of BRAF-V600E gliomas between ages 0-40 revealed increased tendency for malignant tumours in patients >20 years suggesting malignant transformation possibly due to higher rate of secondary hits including TP53, CDKN2A and ATRX mutations. This resulted in worse overall-survival for AYA patients with BRAF-V600E glioma when compared to children under 20 years (p=0.0032). Ten-year OS of 100%, 90% and 95% was seen for BRAF fused, BRAF-V600E and FGFR-altered AYA low grade glioma respectively, compared to 14% and 25% for BRAF-V600E and FGFR-altered high grade glioma. In contrast, continuous decline was observed in the IDH-mutant gliomas with 10-year OS of 50% which declined to 29% at 15 years. CONCLUSIONS: Gliomas in AYA are enriched for paediatric-type alterations with distinct molecularly-based outcomes. As these tumours carry different outcomes than childhood glioma and may respond to targeted inhibitors, AYA gliomas would benefit from comprehensive diagnostic and therapeutic approaches. Oxford University Press 2022-06-03 /pmc/articles/PMC9165411/ http://dx.doi.org/10.1093/neuonc/noac079.353 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Low Grade Glioma
Bennett, Julie
Nobre, Liana
Sheth, Javal
Ryall, Scott
Fang, Karen
Johnson, Monique
Negm, Logine
Chung, Jiil
Komosa, Martin
Nunes, Nuno M
Fat, Mary Jane Lim
Perry, James
Sahgal, Arjun
Detsky, Jay
Bouffet, Eric
Naz-Hazrati, Lili
Dirks, Peter
Ertl-Wagner, Birgit
Kongkham, Paul
Zadeh, Gelareh
Mason, Warren
Climans, Seth
Cusimano, Michael
Das, Sunit
Gao, Andrew
Tsang, Derek
Nguyen, Lananh
Laperriere, Normand
Keith, Julia
Munoz, David
Tabori, Uri
Hawkins, Cynthia
LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title_full LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title_fullStr LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title_full_unstemmed LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title_short LGG-41. The clinical and molecular landscape of gliomas in adolescents and young adults
title_sort lgg-41. the clinical and molecular landscape of gliomas in adolescents and young adults
topic Low Grade Glioma
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165411/
http://dx.doi.org/10.1093/neuonc/noac079.353
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