AI Article Synopsis

  • Cancers share common hallmarks, especially in their metabolism, which significantly impacts tumor behavior and treatment responses.
  • Researchers analyzed metabolic patterns in 10,915 patients from 34 cancer types to understand how different metabolic modes relate to patient outcomes.
  • Their findings suggest certain metabolic pathways are useful indicators of prognosis and highlight the potential for repurposing therapies across different cancer types based on metabolic modeling.

Article Abstract

Despite the high variability in cancer biology, cancers nevertheless exhibit cohesive hallmarks across multiple cancer types, notably dysregulated metabolism. Metabolism plays a central role in cancer biology, and shifts in metabolic pathways have been linked to tumor aggressiveness and likelihood of response to therapy. We therefore sought to interrogate metabolism across cancer types and understand how intrinsic modes of metabolism vary within and across indications and how they relate to patient prognosis. We used context specific genome-scale metabolic modeling to simulate metabolism across 10,915 patients from 34 cancer types from The Cancer Genome Atlas and the MMRF-COMMPASS study. We found that cancer metabolism clustered into modes characterized by differential glycolysis, oxidative phosphorylation, and growth rate. We also found that the simulated activities of metabolic pathways are intrinsically prognostic across cancer types, especially tumor growth rate, fatty acid biosynthesis, folate metabolism, oxidative phosphorylation, steroid metabolism, and glutathione metabolism. This work shows the prognostic power of individual patient metabolic modeling across multiple cancer types. Additionally, it shows that analyzing large-scale models of cancer metabolism with survival information provides unique insights into underlying relationships across cancer types and suggests how therapies designed for one cancer type may be repurposed for use in others.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11240338PMC
http://dx.doi.org/10.3390/cancers16132302DOI Listing

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