337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy

OBJECTIVES/GOALS: Treatment options for glioblastoma (GBM) are limited. Prognosis remains dismal, with an 18 month on average survival rate following diagnosis due to treatment resistance and disease recurrence. The goal of this project is to investigate hallmarks of cancer progression that contribu...

Descripción completa

Detalles Bibliográficos
Autores principales: Rowland, Emma, Walter, Thomas, Suter, Robert, Jermakowicz, Anna, Riggins, Rebecca, Ayad, Nagi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cambridge University Press 2023
Materias:
Precision Medicine/Health
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10129721/
http://dx.doi.org/10.1017/cts.2023.382
_version_ 1785030812652011520
author Rowland, Emma
Walter, Thomas
Suter, Robert
Jermakowicz, Anna
Riggins, Rebecca
Ayad, Nagi
author_facet Rowland, Emma
Walter, Thomas
Suter, Robert
Jermakowicz, Anna
Riggins, Rebecca
Ayad, Nagi
author_sort Rowland, Emma
collection PubMed
description OBJECTIVES/GOALS: Treatment options for glioblastoma (GBM) are limited. Prognosis remains dismal, with an 18 month on average survival rate following diagnosis due to treatment resistance and disease recurrence. The goal of this project is to investigate hallmarks of cancer progression that contribute to temozolomide (TMZ) resistance, a first tine treatment for GBM. METHODS/STUDY POPULATION: Two signaling pathways were investigated in TMZ-sensitive and -resistant GBM cell lines and in primary and recurrent patient-derived xenograft (PDX) tumor cells by genetically and pharmacologically inhibiting methionine adenosyltransferase 2A (MAT2A) and adenosylhomocysteinase (AHCY). Cell growth and survival were assessed by measuring protein expression of proliferation, oxidative stress and cell cycle arrest markers. EPIC array analysis and targeted bisulfite sequencing were conducted to identify changes in genome-wide and specific CpG island methylation. The Seahorse XF Analyzer measured mitochondrial respiratory capacity and oxidative metabolism. Induced pluripotent stem cell organoids were co-cultured with PDX tumor cells to determine if treatments mitigate tumor cell invasiveness. RESULTS/ANTICIPATED RESULTS: Compared to parental cells (PC), MAT2A gene expression was increased by 1.7-fold in acquired resistant and de novo resistant GBM cells (RC) [(transcript per million): PC, 7386 ± 0.012; RC, 12925 ± 0.023; n=2; p=2.10e-8]. Compared to TMZ-sensitive cells (TS), TMZ-resistant cells (TR) demonstrated a 56% increase in baseline oxygen consumption rate [(pmol/min): TS, 179 ± 6.7; TR, 279 ± 13; n=18; p=.0012] and 64% increase in maximal respiratory capacity [(pmol/min): TS, 403 ± 29; TR, 659 ± 35; n=6; p DISCUSSION/SIGNIFICANCE: MAT2A and AHCY contribute to TMZ resistance and recurrence by dysregulating methylation programs and upregulating antioxidant programs, respectively. These findings provide a foundation for developing novel combinatory therapeutic strategies and inform clinical studies intended to increase remission and reduce recurrence for GBM patients.
format Online
Article
Text
id pubmed-10129721
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Cambridge University Press
record_format MEDLINE/PubMed
spelling pubmed-101297212023-04-26 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy Rowland, Emma Walter, Thomas Suter, Robert Jermakowicz, Anna Riggins, Rebecca Ayad, Nagi J Clin Transl Sci Precision Medicine/Health OBJECTIVES/GOALS: Treatment options for glioblastoma (GBM) are limited. Prognosis remains dismal, with an 18 month on average survival rate following diagnosis due to treatment resistance and disease recurrence. The goal of this project is to investigate hallmarks of cancer progression that contribute to temozolomide (TMZ) resistance, a first tine treatment for GBM. METHODS/STUDY POPULATION: Two signaling pathways were investigated in TMZ-sensitive and -resistant GBM cell lines and in primary and recurrent patient-derived xenograft (PDX) tumor cells by genetically and pharmacologically inhibiting methionine adenosyltransferase 2A (MAT2A) and adenosylhomocysteinase (AHCY). Cell growth and survival were assessed by measuring protein expression of proliferation, oxidative stress and cell cycle arrest markers. EPIC array analysis and targeted bisulfite sequencing were conducted to identify changes in genome-wide and specific CpG island methylation. The Seahorse XF Analyzer measured mitochondrial respiratory capacity and oxidative metabolism. Induced pluripotent stem cell organoids were co-cultured with PDX tumor cells to determine if treatments mitigate tumor cell invasiveness. RESULTS/ANTICIPATED RESULTS: Compared to parental cells (PC), MAT2A gene expression was increased by 1.7-fold in acquired resistant and de novo resistant GBM cells (RC) [(transcript per million): PC, 7386 ± 0.012; RC, 12925 ± 0.023; n=2; p=2.10e-8]. Compared to TMZ-sensitive cells (TS), TMZ-resistant cells (TR) demonstrated a 56% increase in baseline oxygen consumption rate [(pmol/min): TS, 179 ± 6.7; TR, 279 ± 13; n=18; p=.0012] and 64% increase in maximal respiratory capacity [(pmol/min): TS, 403 ± 29; TR, 659 ± 35; n=6; p DISCUSSION/SIGNIFICANCE: MAT2A and AHCY contribute to TMZ resistance and recurrence by dysregulating methylation programs and upregulating antioxidant programs, respectively. These findings provide a foundation for developing novel combinatory therapeutic strategies and inform clinical studies intended to increase remission and reduce recurrence for GBM patients. Cambridge University Press 2023-04-24 /pmc/articles/PMC10129721/ http://dx.doi.org/10.1017/cts.2023.382 Text en © The Association for Clinical and Translational Science 2023 https://creativecommons.org/licenses/by-nc-nd/4.0/This is an Open Access article, distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives licence (https://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is unaltered and is properly cited. The written permission of Cambridge University Press must be obtained for commercial re-use or in order to create a derivative work.
spellingShingle Precision Medicine/Health
Rowland, Emma
Walter, Thomas
Suter, Robert
Jermakowicz, Anna
Riggins, Rebecca
Ayad, Nagi
337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title_full 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title_fullStr 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title_full_unstemmed 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title_short 337 Targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
title_sort 337 targeting metabolic and epigenetic programs to re-sensitize glioblastoma to chemotherapy
topic Precision Medicine/Health
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10129721/
http://dx.doi.org/10.1017/cts.2023.382
work_keys_str_mv AT rowlandemma 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy
AT walterthomas 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy
AT suterrobert 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy
AT jermakowiczanna 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy
AT rigginsrebecca 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy
AT ayadnagi 337targetingmetabolicandepigeneticprogramstoresensitizeglioblastomatochemotherapy

Ejemplares similares