Glutamine is one of the most abundant circulating amino acids that is critical for many fundamental functions in cancer cells, including synthesis of metabolites that maintain mitochondrial metabolism, protein synthesis, acting as a carbon source or as the primary nitrogen donor for multiple essential biosynthetic pathways, and in the activation of cell signaling. Here we have identified significant differences in glutamine in human plasma from pancreatic cancer patients that were also observed in tumor interstitial fluid from pancreatic cancer xenografts that induced cachexia. These results suggest that agents with glutaminolytic activity may be useful in treating cachexia.
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