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- W2801487934 abstract "The interplay between rewiring tumor metabolism and oncogenic driver mutations is only beginning to be appreciated. Metabolic deregulation has been described for decades as a bystander effect of genomic aberrations. However, for the biology of malignant cells, metabolic reprogramming is essential to tackle a harsh environment, including nutrient deprivation, ROS production and oxygen withdrawal. Besides the well-investigated glycolytic metabolism, it is emerging that several other metabolic fluxes are relevant for tumorigenesis in supporting redox balance, most notably PPP, folate and mitochondrial metabolism. The relationship between metabolic rewiring and mutant genes is still unclear and therefore we will discuss how metabolic needs and oncogene mutations influence each other to satisfy cancer cells’ demands. Mutations in oncogenes, i.e. PI3K/AKT/mTOR, RAS pathway and MYC, and tumor suppressors, i.e. p53 and LKB1, result in metabolic flexibility and may influence response to therapy. Since metabolic rewiring is shaped by oncogenic driver mutations, understanding how specific alterations in signaling pathways affect different metabolic fluxes will be instrumental for the development of novel targeted therapies. In the era of personalized medicine, the combination of driver mutations, metabolite levels and tissue of origin will pave the way to innovative therapeutic interventions." @default.
- W2801487934 created "2018-05-17" @default.
- W2801487934 creator A5018736882 @default.
- W2801487934 creator A5032548159 @default.
- W2801487934 creator A5064395568 @default.
- W2801487934 creator A5075168526 @default.
- W2801487934 date "2018-04-23" @default.
- W2801487934 modified "2023-10-15" @default.
- W2801487934 title "Signaling Pathways Regulating Redox Balance in Cancer Metabolism" @default.
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