Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway

Introduction: Glioblastoma (GBM) is invariably resistant to temozolomide (TMZ) chemotherapy. Inhibiting the proteasomal pathway is an emerging strategy to accumulate damaged proteins and inhibit their lysosomal degradation. We hypothesized that pre-treatment of glioblastoma with bortezomib (BTZ) mig...

Descripción completa

Detalles Bibliográficos
Autores principales: Rahman, Mohummad Aminur, Engelsen, Agnete S. T., Sarowar, Shahin, Bindesbøll, Christian, Birkeland, Even, Goplen, Dorota, Lotsberg, Maria L., Knappskog, Stian, Simonsen, Anne, Chekenya, Martha
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9814514/
https://www.ncbi.nlm.nih.gov/pubmed/36619857
http://dx.doi.org/10.3389/fcell.2022.1022191
_version_ 1784864151476109312
author Rahman, Mohummad Aminur
Engelsen, Agnete S. T.
Sarowar, Shahin
Bindesbøll, Christian
Birkeland, Even
Goplen, Dorota
Lotsberg, Maria L.
Knappskog, Stian
Simonsen, Anne
Chekenya, Martha
author_facet Rahman, Mohummad Aminur
Engelsen, Agnete S. T.
Sarowar, Shahin
Bindesbøll, Christian
Birkeland, Even
Goplen, Dorota
Lotsberg, Maria L.
Knappskog, Stian
Simonsen, Anne
Chekenya, Martha
author_sort Rahman, Mohummad Aminur
collection PubMed
description Introduction: Glioblastoma (GBM) is invariably resistant to temozolomide (TMZ) chemotherapy. Inhibiting the proteasomal pathway is an emerging strategy to accumulate damaged proteins and inhibit their lysosomal degradation. We hypothesized that pre-treatment of glioblastoma with bortezomib (BTZ) might sensitize glioblastoma to temozolomide by abolishing autophagy survival signals to augment DNA damage and apoptosis. Methods: P3 patient-derived glioblastoma cells, as well as the tumour cell lines U87, HF66, A172, and T98G were investigated for clonogenic survival after single or combined treatment with temozolomide and bortezomib in vitro. We investigated the requirement of functional autophagy machinery by utilizing pharmacological inhibitors or CRISPR-Cas9 knockout (KO) of autophagy-related genes -5 and -7 (ATG5 and ATG7) in glioblastoma cells and monitored changes in autophagic flux after temozolomide and/or bortezomib treatments. P3 wild-type and P3 ATG5−/− (ATG5 KO) cells were implanted orthotopically into NOD-SCID mice to assess the efficacy of bortezomib and temozolomide combination therapy with and without functional autophagy machinery. Results: The chemo-resistant glioblastoma cells increased autophagic flux during temozolomide treatment as indicated by increased degradation of long-lived proteins, diminished expression of autophagy markers LC3A/B-II and p62 (SQSTM1), increased co-localisation of LC3A/B-II with STX17, augmented and no induction of apoptosis. In contrast, bortezomib treatment abrogated autophagic flux indicated by the accumulation of LC3A/B-II and p62 (SQSTM1) positive autophagosomes that did not fuse with lysosomes and thus reduced the degradation of long-lived proteins. Bortezomib synergistically enhanced temozolomide efficacy by attenuating cell proliferation, increased DNA double-strand breaks, and apoptosis in an autophagy-dependent manner. Abolishing autophagy in ATG5 KOs reversed the bortezomib-induced toxicity, rescued glioblastoma cell death and reduced animal survival. Discussion: We conclude that bortezomib abrogates temozolomide induced autophagy flux through an ATG5 dependent pathway.
format Online
Article
Text
id pubmed-9814514
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-98145142023-01-06 Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway Rahman, Mohummad Aminur Engelsen, Agnete S. T. Sarowar, Shahin Bindesbøll, Christian Birkeland, Even Goplen, Dorota Lotsberg, Maria L. Knappskog, Stian Simonsen, Anne Chekenya, Martha Front Cell Dev Biol Cell and Developmental Biology Introduction: Glioblastoma (GBM) is invariably resistant to temozolomide (TMZ) chemotherapy. Inhibiting the proteasomal pathway is an emerging strategy to accumulate damaged proteins and inhibit their lysosomal degradation. We hypothesized that pre-treatment of glioblastoma with bortezomib (BTZ) might sensitize glioblastoma to temozolomide by abolishing autophagy survival signals to augment DNA damage and apoptosis. Methods: P3 patient-derived glioblastoma cells, as well as the tumour cell lines U87, HF66, A172, and T98G were investigated for clonogenic survival after single or combined treatment with temozolomide and bortezomib in vitro. We investigated the requirement of functional autophagy machinery by utilizing pharmacological inhibitors or CRISPR-Cas9 knockout (KO) of autophagy-related genes -5 and -7 (ATG5 and ATG7) in glioblastoma cells and monitored changes in autophagic flux after temozolomide and/or bortezomib treatments. P3 wild-type and P3 ATG5−/− (ATG5 KO) cells were implanted orthotopically into NOD-SCID mice to assess the efficacy of bortezomib and temozolomide combination therapy with and without functional autophagy machinery. Results: The chemo-resistant glioblastoma cells increased autophagic flux during temozolomide treatment as indicated by increased degradation of long-lived proteins, diminished expression of autophagy markers LC3A/B-II and p62 (SQSTM1), increased co-localisation of LC3A/B-II with STX17, augmented and no induction of apoptosis. In contrast, bortezomib treatment abrogated autophagic flux indicated by the accumulation of LC3A/B-II and p62 (SQSTM1) positive autophagosomes that did not fuse with lysosomes and thus reduced the degradation of long-lived proteins. Bortezomib synergistically enhanced temozolomide efficacy by attenuating cell proliferation, increased DNA double-strand breaks, and apoptosis in an autophagy-dependent manner. Abolishing autophagy in ATG5 KOs reversed the bortezomib-induced toxicity, rescued glioblastoma cell death and reduced animal survival. Discussion: We conclude that bortezomib abrogates temozolomide induced autophagy flux through an ATG5 dependent pathway. Frontiers Media S.A. 2022-12-22 /pmc/articles/PMC9814514/ /pubmed/36619857 http://dx.doi.org/10.3389/fcell.2022.1022191 Text en Copyright © 2022 Rahman, Engelsen, Sarowar, Bindesbøll, Birkeland, Goplen, Lotsberg, Knappskog, Simonsen and Chekenya. https://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 Cell and Developmental Biology
Rahman, Mohummad Aminur
Engelsen, Agnete S. T.
Sarowar, Shahin
Bindesbøll, Christian
Birkeland, Even
Goplen, Dorota
Lotsberg, Maria L.
Knappskog, Stian
Simonsen, Anne
Chekenya, Martha
Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title_full Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title_fullStr Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title_full_unstemmed Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title_short Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway
title_sort bortezomib abrogates temozolomide-induced autophagic flux through an atg5 dependent pathway
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9814514/
https://www.ncbi.nlm.nih.gov/pubmed/36619857
http://dx.doi.org/10.3389/fcell.2022.1022191
work_keys_str_mv AT rahmanmohummadaminur bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT engelsenagnetest bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT sarowarshahin bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT bindesbøllchristian bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT birkelandeven bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT goplendorota bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT lotsbergmarial bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT knappskogstian bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT simonsenanne bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway
AT chekenyamartha bortezomibabrogatestemozolomideinducedautophagicfluxthroughanatg5dependentpathway

Ejemplares similares