Cancer is a disease characterized by unrestrained cellular proliferation. In order to sustain growth, cancer cells undergo a complex metabolic rearrangement characterized by changes in metabolic pathways involved in energy production and biosynthetic processes. The relevance of the metabolic transformation of cancer cells has been recently included in the updated version of the review "Hallmarks of Cancer", where dysregulation of cellular metabolism was included as an emerging hallmark. While several lines of evidence suggest that metabolic rewiring is orchestrated by the concerted action of oncogenes and tumor suppressor genes, in some circumstances altered metabolism can play a primary role in oncogenesis. Recently, mutations of cytosolic and mitochondrial enzymes involved in key metabolic pathways have been associated with hereditary and sporadic forms of cancer. Together, these results demonstrate that aberrant metabolism, once seen just as an epiphenomenon of oncogenic reprogramming, plays a key role in oncogenesis with the power to control both genetic and epigenetic events in cells. In this review, we discuss the relationship between metabolism and cancer, as part of a larger effort to identify a broad-spectrum of therapeutic approaches. We focus on major alterations in nutrient metabolism and the emerging link between metabolism and epigenetics. Finally, we discuss potential strategies to manipulate metabolism in cancer and tradeoffs that should be considered. More research on the suite of metabolic alterations in cancer holds the potential to discover novel approaches to treat it.

Dysregulated metabolism contributes to oncogenesis / Hirschey M.D.; DeBerardinis R.J.; Diehl A.M.E.; Drew J.E.; Frezza C.; Green M.F.; Jones L.W.; Ko Y.H.; Le A.; Lea M.A.; Locasale J.W.; Longo V.D.; Lyssiotis C.A.; McDonnell E.; Mehrmohamadi M.; Michelotti G.; Muralidhar V.; Murphy M.P.; Pedersen P.L.; Poore B.; Raffaghello L.; Rathmell J.C.; Sivanand S.; Vander Heiden M.G.; Wellen K.E.; Amedei A.; Amin A.; Salman Ashraf S.; Azmi A.S.; Bhakta D.; Bisland A.; Boosani C.S.; Chen S.; Fujii H.; Georgakilas A.; Guha G.; Halicka D.; Helferich B.; Honoki K.; Keith W.N.; Mohammed S.; Niccolai E.; Nowsheen S.; Yang X.. - In: SEMINARS IN CANCER BIOLOGY. - ISSN 1044-579X. - ELETTRONICO. - 35:(2015), pp. S129-S150. [10.1016/j.semcancer.2015.10.002]

Dysregulated metabolism contributes to oncogenesis

Amedei A.;Niccolai E.;
2015

Abstract

Cancer is a disease characterized by unrestrained cellular proliferation. In order to sustain growth, cancer cells undergo a complex metabolic rearrangement characterized by changes in metabolic pathways involved in energy production and biosynthetic processes. The relevance of the metabolic transformation of cancer cells has been recently included in the updated version of the review "Hallmarks of Cancer", where dysregulation of cellular metabolism was included as an emerging hallmark. While several lines of evidence suggest that metabolic rewiring is orchestrated by the concerted action of oncogenes and tumor suppressor genes, in some circumstances altered metabolism can play a primary role in oncogenesis. Recently, mutations of cytosolic and mitochondrial enzymes involved in key metabolic pathways have been associated with hereditary and sporadic forms of cancer. Together, these results demonstrate that aberrant metabolism, once seen just as an epiphenomenon of oncogenic reprogramming, plays a key role in oncogenesis with the power to control both genetic and epigenetic events in cells. In this review, we discuss the relationship between metabolism and cancer, as part of a larger effort to identify a broad-spectrum of therapeutic approaches. We focus on major alterations in nutrient metabolism and the emerging link between metabolism and epigenetics. Finally, we discuss potential strategies to manipulate metabolism in cancer and tradeoffs that should be considered. More research on the suite of metabolic alterations in cancer holds the potential to discover novel approaches to treat it.
2015
35
S129
S150
Hirschey M.D.; DeBerardinis R.J.; Diehl A.M.E.; Drew J.E.; Frezza C.; Green M.F.; Jones L.W.; Ko Y.H.; Le A.; Lea M.A.; Locasale J.W.; Longo V.D.; Lys...espandi
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Utilizza questo identificatore per citare o creare un link a questa risorsa: https://hdl.handle.net/2158/1286725
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