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A ketogenic diet sensitizes pancreatic cancer to glutamine metabolism inhibitors.

Cell reports. Medicine 2026 p. 102770 🔓 OA Diet and metabolism studies
OpenAlex 토픽 · Diet and metabolism studies Dietary Effects on Health Gut microbiota and health

Hajihassani O, Roichman A, Boyer JA, MacArthur M, Cordova R, Loftus A, Boutros CS, Hue JJ, Naji P, Tahhan S, Gallagher P, Beegan W, Shah D, Choi J, Manzoor N, Lei S, Kim C, Rathore M, Shah I, Lebo K, Cheng H, Mudigonda A, Hunter C, Zarei M, Alibeckoff S, Ji K, Graor H, Miyagi M, Vaziri-Gohar A, Brunengraber H, Wang R, Lund PJ, Rothermel LD, Rabinowitz JD, Winter JM

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Pancreatic cancer is the third leading cause of cancer-related death in the United States.

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APA Omid Hajihassani, Asael Roichman, et al. (2026). A ketogenic diet sensitizes pancreatic cancer to glutamine metabolism inhibitors.. Cell reports. Medicine, 102770. https://doi.org/10.1016/j.xcrm.2026.102770
MLA Omid Hajihassani, et al.. "A ketogenic diet sensitizes pancreatic cancer to glutamine metabolism inhibitors.." Cell reports. Medicine, 2026, pp. 102770.
PMID 42030935

Abstract

Pancreatic cancer is the third leading cause of cancer-related death in the United States. Current chemotherapy options provide limited benefits. Emerging evidence suggests that a ketogenic diet (KD) exerts anti-tumor effects by reprogramming tumor metabolism and revealing therapeutic vulnerabilities. Efforts to target glutamine metabolism-an essential pathway in many cancers-have shown promise in preclinical models, but clinical efficacy has remained limited. Here, we show that a KD increases tricarboxylic acid (TCA) cycle activity and elevates reliance on glutamine-related metabolites in murine pancreatic cancer models and in vitro under KD-mimicking conditions. This metabolic adaptation occurs in response to reduced glucose availability. We demonstrate that combining glutamine metabolism inhibitors, such as CB-839 or 6-diazo-5-oxo-L-norleucine (DON), with a KD leads to robust anti-tumor effects in preclinical models of pancreatic cancer. Thus, metabolic vulnerability induced by dietary intervention provides a rationale for combining glutamine-targeted therapies with a ketogenic diet in future clinical studies.

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