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. 2016 Jan 15;26(3):269–270. doi: 10.1038/cr.2016.7

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Copyright © 2016 Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences

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Mechanistic overview of proposed vitamin C toxicity in CRCs driven by KRAS and BRAF mutations. KRAS and BRAF mutations induce metabolic reprogramming by upregulating GLUT1, glucose uptake, and glycolytic flux. Upon vitamin C treatment and its extracellular oxidation, DHA (the oxidized form of vitamin C) is taken up through GLUT1 and is reduced back to vitamin C in the cells, depleting GSH and NADPH. Consequently, an increase in ROS leads to GAPDH oxidation, and with it, to a decrease in glycolytic flux. In parallel, ROS-mediated oxidative DNA damage induces PARP activation and subsequently, NAD⁺ levels fall and cause additional inhibition of GAPDH and glycolysis, resulting in energy crisis and cell death.