Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond

Radiotherapy is an essential component of multi-modality treatment of glioblastoma (GBM). However, treatment failure and recurrence are frequent and give rise to the dismal prognosis of this aggressive type of primary brain tumor. A high level of inherent treatment resistance is considered to be the...

Descripción completa

Detalles Bibliográficos
Autores principales: Orth, Michael, Albrecht, Valerie, Seidl, Karin, Kinzel, Linda, Unger, Kristian, Hess, Julia, Kreutzer, Lisa, Sun, Na, Stegen, Benjamin, Nieto, Alexander, Maas, Jessica, Winssinger, Nicolas, Friedl, Anna A., Walch, Axel K., Belka, Claus, Zitzelsberger, Horst, Niyazi, Maximilian, Lauber, Kirsten
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8011354/
https://www.ncbi.nlm.nih.gov/pubmed/33816244
http://dx.doi.org/10.3389/fonc.2021.612354
_version_ 1783673217553006592
author Orth, Michael
Albrecht, Valerie
Seidl, Karin
Kinzel, Linda
Unger, Kristian
Hess, Julia
Kreutzer, Lisa
Sun, Na
Stegen, Benjamin
Nieto, Alexander
Maas, Jessica
Winssinger, Nicolas
Friedl, Anna A.
Walch, Axel K.
Belka, Claus
Zitzelsberger, Horst
Niyazi, Maximilian
Lauber, Kirsten
author_facet Orth, Michael
Albrecht, Valerie
Seidl, Karin
Kinzel, Linda
Unger, Kristian
Hess, Julia
Kreutzer, Lisa
Sun, Na
Stegen, Benjamin
Nieto, Alexander
Maas, Jessica
Winssinger, Nicolas
Friedl, Anna A.
Walch, Axel K.
Belka, Claus
Zitzelsberger, Horst
Niyazi, Maximilian
Lauber, Kirsten
author_sort Orth, Michael
collection PubMed
description Radiotherapy is an essential component of multi-modality treatment of glioblastoma (GBM). However, treatment failure and recurrence are frequent and give rise to the dismal prognosis of this aggressive type of primary brain tumor. A high level of inherent treatment resistance is considered to be the major underlying reason, stemming from constantly activated DNA damage response (DDR) mechanisms as a consequence of oncogene overexpression, persistent replicative stress, and other so far unknown reasons. The molecular chaperone heat shock protein 90 (HSP90) plays an important role in the establishment and maintenance of treatment resistance, since it crucially assists the folding and stabilization of various DDR regulators. Accordingly, inhibition of HSP90 represents a multi-target strategy to interfere with DDR function and to sensitize cancer cells to radiotherapy. Using NW457, a pochoxime-based HSP90 inhibitor with favorable brain pharmacokinetic profile, we show here that HSP90 inhibition at low concentrations with per se limited cytotoxicity leads to downregulation of various DNA damage response factors on the protein level, distinct transcriptomic alterations, impaired DNA damage repair, and reduced clonogenic survival in response to ionizing irradiation in glioblastoma cells in vitro. In vivo, HSP90 inhibition by NW457 improved the therapeutic outcome of fractionated CBCT-based irradiation in an orthotopic, syngeneic GBM mouse model, both in terms of tumor progression and survival. Nevertheless, in view of the promising in vitro results the in vivo efficacy was not as strong as expected, although apart from the radiosensitizing effects HSP90 inhibition also reduced irradiation-induced GBM cell migration and tumor invasiveness. Hence, our findings identify the combination of HSP90 inhibition and radiotherapy in principle as a promising strategy for GBM treatment whose performance needs to be further optimized by improved inhibitor substances, better formulations and/or administration routes, and fine-tuned treatment sequences.
format Online
Article
Text
id pubmed-8011354
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-80113542021-04-01 Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond Orth, Michael Albrecht, Valerie Seidl, Karin Kinzel, Linda Unger, Kristian Hess, Julia Kreutzer, Lisa Sun, Na Stegen, Benjamin Nieto, Alexander Maas, Jessica Winssinger, Nicolas Friedl, Anna A. Walch, Axel K. Belka, Claus Zitzelsberger, Horst Niyazi, Maximilian Lauber, Kirsten Front Oncol Oncology Radiotherapy is an essential component of multi-modality treatment of glioblastoma (GBM). However, treatment failure and recurrence are frequent and give rise to the dismal prognosis of this aggressive type of primary brain tumor. A high level of inherent treatment resistance is considered to be the major underlying reason, stemming from constantly activated DNA damage response (DDR) mechanisms as a consequence of oncogene overexpression, persistent replicative stress, and other so far unknown reasons. The molecular chaperone heat shock protein 90 (HSP90) plays an important role in the establishment and maintenance of treatment resistance, since it crucially assists the folding and stabilization of various DDR regulators. Accordingly, inhibition of HSP90 represents a multi-target strategy to interfere with DDR function and to sensitize cancer cells to radiotherapy. Using NW457, a pochoxime-based HSP90 inhibitor with favorable brain pharmacokinetic profile, we show here that HSP90 inhibition at low concentrations with per se limited cytotoxicity leads to downregulation of various DNA damage response factors on the protein level, distinct transcriptomic alterations, impaired DNA damage repair, and reduced clonogenic survival in response to ionizing irradiation in glioblastoma cells in vitro. In vivo, HSP90 inhibition by NW457 improved the therapeutic outcome of fractionated CBCT-based irradiation in an orthotopic, syngeneic GBM mouse model, both in terms of tumor progression and survival. Nevertheless, in view of the promising in vitro results the in vivo efficacy was not as strong as expected, although apart from the radiosensitizing effects HSP90 inhibition also reduced irradiation-induced GBM cell migration and tumor invasiveness. Hence, our findings identify the combination of HSP90 inhibition and radiotherapy in principle as a promising strategy for GBM treatment whose performance needs to be further optimized by improved inhibitor substances, better formulations and/or administration routes, and fine-tuned treatment sequences. Frontiers Media S.A. 2021-03-17 /pmc/articles/PMC8011354/ /pubmed/33816244 http://dx.doi.org/10.3389/fonc.2021.612354 Text en Copyright © 2021 Orth, Albrecht, Seidl, Kinzel, Unger, Hess, Kreutzer, Sun, Stegen, Nieto, Maas, Winssinger, Friedl, Walch, Belka, Zitzelsberger, Niyazi and Lauber 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
Orth, Michael
Albrecht, Valerie
Seidl, Karin
Kinzel, Linda
Unger, Kristian
Hess, Julia
Kreutzer, Lisa
Sun, Na
Stegen, Benjamin
Nieto, Alexander
Maas, Jessica
Winssinger, Nicolas
Friedl, Anna A.
Walch, Axel K.
Belka, Claus
Zitzelsberger, Horst
Niyazi, Maximilian
Lauber, Kirsten
Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title_full Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title_fullStr Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title_full_unstemmed Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title_short Inhibition of HSP90 as a Strategy to Radiosensitize Glioblastoma: Targeting the DNA Damage Response and Beyond
title_sort inhibition of hsp90 as a strategy to radiosensitize glioblastoma: targeting the dna damage response and beyond
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8011354/
https://www.ncbi.nlm.nih.gov/pubmed/33816244
http://dx.doi.org/10.3389/fonc.2021.612354
work_keys_str_mv AT orthmichael inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT albrechtvalerie inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT seidlkarin inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT kinzellinda inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT ungerkristian inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT hessjulia inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT kreutzerlisa inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT sunna inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT stegenbenjamin inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT nietoalexander inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT maasjessica inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT winssingernicolas inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT friedlannaa inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT walchaxelk inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT belkaclaus inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT zitzelsbergerhorst inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT niyazimaximilian inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond
AT lauberkirsten inhibitionofhsp90asastrategytoradiosensitizeglioblastomatargetingthednadamageresponseandbeyond

Ejemplares similares