4.8 Article

GOT1 inhibition promotes pancreatic cancer cell death by ferroptosis

NATURE COMMUNICATIONS (2021)

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Journal

NATURE COMMUNICATIONS
Volume 12, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41467-021-24859-2

Keywords

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Categories

Multidisciplinary Sciences

Funding

  1. Department of Education GAANN fellowship through The University of Michigan Program in Chemical Biology
  2. Institutional National Research Service Award through NIDDK [T32-DK094775]
  3. Institutional National Research Service Award through NCI [T32-CA009676]
  4. NIH [K22CA237752, R01CA148828, R01CA245546, R01DK095201, 1R37CA237421, R01CA248160, R01CA244931]
  5. Cancer Prevention and Research Institute of Texas [RR190034]
  6. V Foundation for Cancer Research [V2020-006, V2016-009]
  7. NCI [R01-CA-198074, R01-CA-151588]
  8. ACS Research Scholar Grant
  9. Pancreatic Cancer Action Network/AACR [13-70-25-LYSS]
  10. Damon Runyon Cancer Research Foundation [DFS-09-14]
  11. Sidney Kimmel Foundation for Cancer Research [SKF-16-005]
  12. AACR [17-20-01-LYSS]
  13. Cancer Center Support Grant [P30 CA046592]
  14. Preclinical Imaging & Computational Analysis Shared Resource [P30CA046592]
  15. Charles Woodson Research Fund
  16. UM Pediatric Brain Tumor Initiative
  17. ACS Research Scholar Grant [RSG-18-186-01]
  18. [U01-CA-224145]
  19. [R01CA215607]
  20. [DK09715]
  21. [NCI-P30CA046592]

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Cancer metabolism is rewired to support cell survival, with targeting metabolic dependencies following GOT1 inhibition leading to ferroptosis, an iron-dependent form of cell death. The study identifies a biochemical connection between GOT1, iron regulation, and ferroptosis in pancreatic cancer cells.
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. The aspartate aminotransaminase GOT1 is important for maintaining redox balance. Here, the authors show that inhibition of GOT1 in pancreatic cancer cells leads to cell death via ferroptosis.

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