DIPG-30. HIF2 OVEREXPRESSION DICTATES AGGRESSIVENESS ADDITIONALLY TO TP53 MUTATIONS IN H3.3K27M PEDIATRIC HIGH-GRADE GLIOMAS THROUGH RAS-MAPK AND WNT/BCATENIN PATHWAYS

Abstract Diffuse midline (DMG) and brainstem (DIPG) high-grade gliomas (HGG) bearing H3.3K27M driver mutation are aggressive and uncurable brain tumors. We evidenced by the past HIF-2a and its transcriptional gene, EPAS1, as a marker of resistance when targeting mTor/HIF-1a pathway. To understand HI...

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Published in:Neuro-oncology (Charlottesville, Va.) Va.), 2023-06, Vol.25 (Supplement_1), p.i19-i20
Main Authors: Fuchs, Quentin, Legras, Stephanie, Lhermitte, Benoit, Vauchelles, Romain, Cosset, Erika, Gorka, Lucas, Outilaft, Hassiba, Namer, Izzie Jacques, Guerin, Eric, Mura, Carole, Burckel, Hélène, Noel, Georges, Hibaoui, Youssef, Feki, Anis, Chammas, Agathe, Wolf, Thibaut, Coca, Andres Hugo, Foppolo, Sophie, Dontenwill, Monique, Entz-Werlé, Natacha
Format: Article
Language:English
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Final Category: Diffuse Intrinsic Pontine Glioma/Diffuse Midline Gliomas - DPIG
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Summary:Abstract Diffuse midline (DMG) and brainstem (DIPG) high-grade gliomas (HGG) bearing H3.3K27M driver mutation are aggressive and uncurable brain tumors. We evidenced by the past HIF-2a and its transcriptional gene, EPAS1, as a marker of resistance when targeting mTor/HIF-1a pathway. To understand HIF-2α potential role in chronically active hypoxic environment in DIPG/DMG, we investigate its status in a cohort of pediatric HGGs comprising notably H3.3K27M mutant tumors and in their paired in vitro derived models. Using concomitantly the low-input chromatin immunoprecipitation sequencing method CUT&RUN, RNAsequencing and metabolomics, we profiled the landscape of promoters and pathways regulated by HIF-2a in HGGs, where H3.3K27M and TP53 mutations are associated. Elucidation of HIF-2a downstream genes reveal statistically significant pathways linked to DIPGs (e.g., mTor and canonical Wnt pathways) and to DMGs (glutamatergic synapse and non-canoncial Wnt signaling). Finally, HIF-2a was evidenced as a new therapeutic target opening the path for its use concomitantly to irradiation.
ISSN:1522-8517
1523-5866
DOI:10.1093/neuonc/noad073.077