AI Article Synopsis
- Cancer cells adapt their metabolism for survival under stress, and targeting these adaptations is a key research focus.
- The study examines how the inhibition of a specific enzyme, GOT1, in pancreatic cancer affects the cells' metabolic dependencies and redox balance.
- Findings show that blocking GOT1 leads to vulnerabilities in antioxidant functions and triggers ferroptosis, a type of cell death linked to iron and oxidative stress, highlighting a connection between GOT1, iron regulation, and cell death mechanisms.
Article Abstract
Cancer metabolism is rewired to support cell survival in response to intrinsic and environmental stressors. Identification of strategies to target these adaptions is an area of active research. We previously described a cytosolic aspartate aminotransaminase (GOT1)-driven pathway in pancreatic cancer used to maintain redox balance. Here, we sought to identify metabolic dependencies following GOT1 inhibition to exploit this feature of pancreatic cancer and to provide additional insight into regulation of redox metabolism. Using pharmacological methods, we identify cysteine, glutathione, and lipid antioxidant function as metabolic vulnerabilities following GOT1 withdrawal. We demonstrate that targeting any of these pathways triggers ferroptosis, an oxidative, iron-dependent form of cell death, in GOT1 knockdown cells. Mechanistically, we reveal that GOT1 inhibition represses mitochondrial metabolism and promotes a catabolic state. Consequently, we find that this enhances labile iron availability through autophagy, which potentiates the activity of ferroptotic stimuli. Overall, our study identifies a biochemical connection between GOT1, iron regulation, and ferroptosis.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8357841 | PMC |
| http://dx.doi.org/10.1038/s41467-021-24859-2 | DOI Listing |
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