Transcriptional CDK inhibitors, CYC065 and THZ1 promote Bim-dependent apoptosis in primary and recurrent GBM through cell cycle arrest and Mcl-1 downregulation.
Adenosine
/ analogs & derivatives
Animals
Apoptosis
/ drug effects
Bcl-2-Like Protein 11
/ metabolism
Cell Cycle Checkpoints
/ drug effects
Cell Line, Tumor
Cell Proliferation
/ drug effects
Cell Survival
/ drug effects
Chick Embryo
Cyclin-Dependent Kinases
/ antagonists & inhibitors
Down-Regulation
/ drug effects
Gene Expression Regulation, Neoplastic
/ drug effects
Glioblastoma
/ genetics
Humans
Myeloid Cell Leukemia Sequence 1 Protein
/ genetics
Neoplasm Recurrence, Local
/ pathology
Neurons
/ drug effects
Phenylenediamines
/ pharmacology
Protein Kinase Inhibitors
/ pharmacology
Pyrimidines
/ pharmacology
RNA, Messenger
/ genetics
Spheroids, Cellular
/ drug effects
Transcription, Genetic
/ drug effects
Xenograft Model Antitumor Assays
Journal
Cell death & disease
ISSN: 2041-4889
Titre abrégé: Cell Death Dis
Pays: England
ID NLM: 101524092
Informations de publication
Date de publication:
03 08 2021
03 08 2021
Historique:
received:
22
03
2021
accepted:
19
07
2021
revised:
16
07
2021
entrez:
4
8
2021
pubmed:
5
8
2021
medline:
27
1
2022
Statut:
epublish
Résumé
Activation of cyclin-dependent kinases (CDKs) contributes to the uncontrolled proliferation of tumour cells. Genomic alterations that lead to the constitutive activation or overexpression of CDKs can support tumourigenesis including glioblastoma (GBM), the most common and aggressive primary brain tumour in adults. The incurability of GBM highlights the need to discover novel and more effective treatment options. Since CDKs 2, 7 and 9 were found to be overexpressed in GBM, we tested the therapeutic efficacy of two CDK inhibitors (CKIs) (CYC065 and THZ1) in a heterogeneous panel of GBM patient-derived cell lines (PDCLs) cultured as gliomaspheres, as preclinically relevant models. CYC065 and THZ1 treatments suppressed invasion and induced viability loss in the majority of gliomaspheres, irrespective of the mutational background of the GBM cases, but spared primary cortical neurons. Viability loss arose from G2/M cell cycle arrest following treatment and subsequent induction of apoptotic cell death. Treatment efficacies and treatment durations required to induce cell death were associated with proliferation velocities, and apoptosis induction correlated with complete abolishment of Mcl-1 expression, a cell cycle-regulated antiapoptotic Bcl-2 family member. GBM models generally appeared highly dependent on Mcl-1 expression for cell survival, as demonstrated by pharmacological Mcl-1 inhibition or depletion of Mcl-1 expression. Further analyses identified CKI-induced Mcl-1 loss as a prerequisite to establish conditions at which the BH3-only protein Bim can efficiently induce apoptosis, with cellular Bim amounts strongly correlating with treatment efficacy. CKIs reduced proliferation and promoted apoptosis also in chick embryo xenograft models of primary and recurrent GBM. Collectively, these studies highlight the potential of these novel CKIs to suppress growth and induce cell death of patient-derived GBM cultures in vitro and in vivo, warranting further clinical investigation.
Identifiants
pubmed: 34344865
doi: 10.1038/s41419-021-04050-7
pii: 10.1038/s41419-021-04050-7
pmc: PMC8333061
doi:
Substances chimiques
Bcl-2-Like Protein 11
0
CYC065
0
Myeloid Cell Leukemia Sequence 1 Protein
0
Phenylenediamines
0
Protein Kinase Inhibitors
0
Pyrimidines
0
RNA, Messenger
0
THZ1 compound
0
Cyclin-Dependent Kinases
EC 2.7.11.22
Adenosine
K72T3FS567
Types de publication
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
763Subventions
Organisme : EC | Horizon 2020 Framework Programme (EU Framework Programme for Research and Innovation H2020)
ID : 766069
Organisme : EC | Horizon 2020 Framework Programme (EU Framework Programme for Research and Innovation H2020)
ID : 766069
Organisme : EC | Horizon 2020 Framework Programme (EU Framework Programme for Research and Innovation H2020)
ID : 766069
Organisme : Science Foundation Ireland (SFI)
ID : 13/IA/1994
Organisme : Deutsche Forschungsgemeinschaft (German Research Foundation)
ID : MO3226 4/1
Informations de copyright
© 2021. The Author(s).
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