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Liver glycogen phosphorylase is upregulated in glioblastoma and provides a metabolic vulnerability to high dose radiation
- Source :
- Cell death & disease, 13(6):573. Nature Publishing Group
- Publication Year :
- 2023
- Publisher :
- Springer Nature, 2023.
-
Abstract
- Channelling of glucose via glycogen, known as the glycogen shunt, may play an important role in the metabolism of brain tumours, especially in hypoxic conditions. We aimed to dissect the role of glycogen degradation in glioblastoma (GBM) response to ionising radiation (IR). Knockdown of the glycogen phosphorylase liver isoform (PYGL), but not the brain isoform (PYGB), decreased clonogenic growth and survival of GBM cell lines and sensitised them to IR doses of 10–12 Gy. Two to five days after IR exposure of PYGL knockdown GBM cells, mitotic catastrophy and a giant multinucleated cell morphology with senescence-like phenotype developed. The basal levels of the lysosomal enzyme alpha-acid glucosidase (GAA), essential for autolysosomal glycogen degradation, and the lipidated forms of gamma-aminobutyric acid receptor-associated protein-like (GABARAPL1 and GABARAPL2) increased in shPYGL U87MG cells, suggesting a compensatory mechanism of glycogen degradation. In response to IR, dysregulation of autophagy was shown by accumulation of the p62 and the lipidated form of GABARAPL1 and GABARAPL2 in shPYGL U87MG cells. IR increased the mitochondrial mass and the colocalisation of mitochondria with lysosomes in shPYGL cells, thereby indicating reduced mitophagy. These changes coincided with increased phosphorylation of AMP-activated protein kinase and acetyl-CoA carboxylase 2, slower ATP generation in response to glucose loading and progressive loss of oxidative phosphorylation. The resulting metabolic deficiencies affected the availability of ATP required for mitosis, resulting in the mitotic catastrophy observed in shPYGL cells following IR. PYGL mRNA and protein levels were higher in human GBM than in normal human brain tissues and high PYGL mRNA expression in GBM correlated with poor patient survival. In conclusion, we show a major new role for glycogen metabolism in GBM cancer. Inhibition of glycogen degradation sensitises GBM cells to high-dose IR indicating that PYGL is a potential novel target for the treatment of GBMs.
- Subjects :
- Liver/metabolism
Cancer Research
DATA SCIENCE
Immunology
Messenger
MATHEMATICAL MODELLING OF BIOLOGICAL SYSTEMS
Glycogen/metabolism
METABOLISM
GBM
Cellular and Molecular Neuroscience
Adenosine Triphosphate
Humans
Protein Isoforms
Glycogen Phosphorylase/genetics
RNA, Messenger
HEALTH RESEARCH
BIOINFORMATICS
Glycogen Phosphorylase
Cell Biology
BIOMEDICAL RESEARCH
CANCER
Glucose/pharmacology
Glioblastoma/genetics
MEDICAL INFORMATICS
COMPUTATIONAL BIOLOGY, DATA SCIENCE, MATHEMATICAL MODELLING OF BIOLOGICAL SYSTEMS, BIOINFORMATICS, GENOMICS, BIOMEDICAL RESEARCH, HEALTH RESEARCH, MEDICAL INFORMATICS, METABOLISM, CANCER, GBM
Glucose
Liver
RNA
Glioblastoma
GENOMICS
COMPUTATIONAL BIOLOGY
Glycogen
Subjects
Details
- Language :
- English
- ISSN :
- 20414889
- Database :
- OpenAIRE
- Journal :
- Cell death & disease, 13(6):573. Nature Publishing Group
- Accession number :
- edsair.doi.dedup.....a06de15fcf3391c2662033fa4d150bd3