Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities

Diffuse gliomas with K27M histone mutations (H3K27M glioma) are generally characterized by a fatal prognosis, particularly affecting the pediatric population. Based on the molecular heterogeneity observed in this tumor type, personalized treatment is considered to substantially improve therapeutic o...

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Autores principales: Gojo, Johannes, Pavelka, Zdenek, Zapletalova, Danica, Schmook, Maria T., Mayr, Lisa, Madlener, Sibylle, Kyr, Michal, Vejmelkova, Klara, Smrcka, Martin, Czech, Thomas, Dorfer, Christian, Skotakova, Jarmila, Azizi, Amedeo A., Chocholous, Monika, Reisinger, Dominik, Lastovicka, David, Valik, Dalibor, Haberler, Christine, Peyrl, Andreas, Noskova, Hana, Pál, Karol, Jezova, Marta, Veselska, Renata, Kozakova, Sarka, Slaby, Ondrej, Slavc, Irene, Sterba, Jaroslav
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6965319/
https://www.ncbi.nlm.nih.gov/pubmed/31998633
http://dx.doi.org/10.3389/fonc.2019.01436
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author Gojo, Johannes
Pavelka, Zdenek
Zapletalova, Danica
Schmook, Maria T.
Mayr, Lisa
Madlener, Sibylle
Kyr, Michal
Vejmelkova, Klara
Smrcka, Martin
Czech, Thomas
Dorfer, Christian
Skotakova, Jarmila
Azizi, Amedeo A.
Chocholous, Monika
Reisinger, Dominik
Lastovicka, David
Valik, Dalibor
Haberler, Christine
Peyrl, Andreas
Noskova, Hana
Pál, Karol
Jezova, Marta
Veselska, Renata
Kozakova, Sarka
Slaby, Ondrej
Slavc, Irene
Sterba, Jaroslav
author_facet Gojo, Johannes
Pavelka, Zdenek
Zapletalova, Danica
Schmook, Maria T.
Mayr, Lisa
Madlener, Sibylle
Kyr, Michal
Vejmelkova, Klara
Smrcka, Martin
Czech, Thomas
Dorfer, Christian
Skotakova, Jarmila
Azizi, Amedeo A.
Chocholous, Monika
Reisinger, Dominik
Lastovicka, David
Valik, Dalibor
Haberler, Christine
Peyrl, Andreas
Noskova, Hana
Pál, Karol
Jezova, Marta
Veselska, Renata
Kozakova, Sarka
Slaby, Ondrej
Slavc, Irene
Sterba, Jaroslav
author_sort Gojo, Johannes
collection PubMed
description Diffuse gliomas with K27M histone mutations (H3K27M glioma) are generally characterized by a fatal prognosis, particularly affecting the pediatric population. Based on the molecular heterogeneity observed in this tumor type, personalized treatment is considered to substantially improve therapeutic options. Therefore, clinical evidence for therapy, guided by comprehensive molecular profiling, is urgently required. In this study, we analyzed feasibility and clinical outcomes in a cohort of 12 H3K27M glioma cases treated at two centers. Patients were subjected to personalized treatment either at primary diagnosis or disease progression and received backbone therapy including focal irradiation. Molecular analyses included whole-exome sequencing of tumor and germline DNA, RNA-sequencing, and transcriptomic profiling. Patients were monitored with regular clinical as well as radiological follow-up. In one case, liquid biopsy of cerebrospinal fluid (CSF) was used. Analyses could be completed in 83% (10/12) and subsequent personalized treatment for one or more additional pharmacological therapies could be recommended in 90% (9/10). Personalized treatment included inhibition of the PI3K/AKT/mTOR pathway (3/9), MAPK signaling (2/9), immunotherapy (2/9), receptor tyrosine kinase inhibition (2/9), and retinoic receptor agonist (1/9). The overall response rate within the cohort was 78% (7/9) including one complete remission, three partial responses, and three stable diseases. Sustained responses lasting for 28 to 150 weeks were observed for cases with PIK3CA mutations treated with either miltefosine or everolimus and additional treatment with trametinib/dabrafenib in a case with BRAFV600E mutation. Immune checkpoint inhibitor treatment of a case with increased tumor mutational burden (TMB) resulted in complete remission lasting 40 weeks. Median time to progression was 29 weeks. Median overall survival (OS) in the personalized treatment cohort was 16.5 months. Last, we compared OS to a control cohort (n = 9) showing a median OS of 17.5 months. No significant difference between the cohorts could be detected, but long-term survivors (>2 years) were only present in the personalized treatment cohort. Taken together, we present the first evidence of clinical efficacy and an improved patient outcome through a personalized approach at least in selected cases of H3K27M glioma.
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spelling pubmed-69653192020-01-29 Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities Gojo, Johannes Pavelka, Zdenek Zapletalova, Danica Schmook, Maria T. Mayr, Lisa Madlener, Sibylle Kyr, Michal Vejmelkova, Klara Smrcka, Martin Czech, Thomas Dorfer, Christian Skotakova, Jarmila Azizi, Amedeo A. Chocholous, Monika Reisinger, Dominik Lastovicka, David Valik, Dalibor Haberler, Christine Peyrl, Andreas Noskova, Hana Pál, Karol Jezova, Marta Veselska, Renata Kozakova, Sarka Slaby, Ondrej Slavc, Irene Sterba, Jaroslav Front Oncol Oncology Diffuse gliomas with K27M histone mutations (H3K27M glioma) are generally characterized by a fatal prognosis, particularly affecting the pediatric population. Based on the molecular heterogeneity observed in this tumor type, personalized treatment is considered to substantially improve therapeutic options. Therefore, clinical evidence for therapy, guided by comprehensive molecular profiling, is urgently required. In this study, we analyzed feasibility and clinical outcomes in a cohort of 12 H3K27M glioma cases treated at two centers. Patients were subjected to personalized treatment either at primary diagnosis or disease progression and received backbone therapy including focal irradiation. Molecular analyses included whole-exome sequencing of tumor and germline DNA, RNA-sequencing, and transcriptomic profiling. Patients were monitored with regular clinical as well as radiological follow-up. In one case, liquid biopsy of cerebrospinal fluid (CSF) was used. Analyses could be completed in 83% (10/12) and subsequent personalized treatment for one or more additional pharmacological therapies could be recommended in 90% (9/10). Personalized treatment included inhibition of the PI3K/AKT/mTOR pathway (3/9), MAPK signaling (2/9), immunotherapy (2/9), receptor tyrosine kinase inhibition (2/9), and retinoic receptor agonist (1/9). The overall response rate within the cohort was 78% (7/9) including one complete remission, three partial responses, and three stable diseases. Sustained responses lasting for 28 to 150 weeks were observed for cases with PIK3CA mutations treated with either miltefosine or everolimus and additional treatment with trametinib/dabrafenib in a case with BRAFV600E mutation. Immune checkpoint inhibitor treatment of a case with increased tumor mutational burden (TMB) resulted in complete remission lasting 40 weeks. Median time to progression was 29 weeks. Median overall survival (OS) in the personalized treatment cohort was 16.5 months. Last, we compared OS to a control cohort (n = 9) showing a median OS of 17.5 months. No significant difference between the cohorts could be detected, but long-term survivors (>2 years) were only present in the personalized treatment cohort. Taken together, we present the first evidence of clinical efficacy and an improved patient outcome through a personalized approach at least in selected cases of H3K27M glioma. Frontiers Media S.A. 2020-01-10 /pmc/articles/PMC6965319/ /pubmed/31998633 http://dx.doi.org/10.3389/fonc.2019.01436 Text en Copyright © 2020 Gojo, Pavelka, Zapletalova, Schmook, Mayr, Madlener, Kyr, Vejmelkova, Smrcka, Czech, Dorfer, Skotakova, Azizi, Chocholous, Reisinger, Lastovicka, Valik, Haberler, Peyrl, Noskova, Pál, Jezova, Veselska, Kozakova, Slaby, Slavc and Sterba. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Gojo, Johannes
Pavelka, Zdenek
Zapletalova, Danica
Schmook, Maria T.
Mayr, Lisa
Madlener, Sibylle
Kyr, Michal
Vejmelkova, Klara
Smrcka, Martin
Czech, Thomas
Dorfer, Christian
Skotakova, Jarmila
Azizi, Amedeo A.
Chocholous, Monika
Reisinger, Dominik
Lastovicka, David
Valik, Dalibor
Haberler, Christine
Peyrl, Andreas
Noskova, Hana
Pál, Karol
Jezova, Marta
Veselska, Renata
Kozakova, Sarka
Slaby, Ondrej
Slavc, Irene
Sterba, Jaroslav
Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title_full Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title_fullStr Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title_full_unstemmed Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title_short Personalized Treatment of H3K27M-Mutant Pediatric Diffuse Gliomas Provides Improved Therapeutic Opportunities
title_sort personalized treatment of h3k27m-mutant pediatric diffuse gliomas provides improved therapeutic opportunities
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6965319/
https://www.ncbi.nlm.nih.gov/pubmed/31998633
http://dx.doi.org/10.3389/fonc.2019.01436
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