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Background Rewiring of metabolism induced by oncogenic K-Ras in cancer cells involves both glucose and glutamine utilization sustaining enhanced, unrestricted growth. The development of effective anti-cancer treatments targeting metabolism may be facilitated by the identification and rational combinatorial targeting of metabolic pathways. Methods We performed mass spectrometric metabolomics analysis in vitro and in vivo experiments to evaluate the efficacy of drugs and identify metabolic connectivity. Results We show that K-Ras-mutant lung and colon cancer cells exhibit a distinct metabolic rewiring, the latter being more dependent on respiration. Combined treatment with the glutaminase inhibitor CB-839 and the PI3K/aldolase inhibitor NVP-BKM120 more consistently reduces cell growth of tumor xenografts. Maximal growth inhibition correlates with the disruption of redox homeostasis, involving loss of reduced glutathione regeneration, redox cofactors, and a decreased connectivity among metabolites primarily involved in nucleic acid metabolism. Conclusions Our findings open the way to develop metabolic connectivity profiling as a tool for a selective strategy of combined drug repositioning in precision oncology.

Disruption of redox homeostasis for combinatorial drug eefficacy in K-Ras tumors as revealed by metabolic connectivity proling / Gaglio, Daniela; Bonanomi, Marcella; Valtorta, Silvia; Bharat, Rohit; Ripamonti, Marilena; Conte, Federica; Fiscon, Giulia; Righi, Nicole; Napodano, Elisabetta; Papa, Federico; Raccagni, Isabella; Parker, Seth J.; Cifola, Ingrid; Camboni, Tania; Paci, Paola; Maria Colangelo, Anna; Vanoni, Marco; Metallo, Christian M.; Maria Moresco, Rosa; Alberghina, Lilia. - In: CANCER & METABOLISM. - ISSN 2049-3002. - 8:(2020), pp. 1-15. [10.1186/s40170-020-00227-4]

Disruption of redox homeostasis for combinatorial drug eefficacy in K-Ras tumors as revealed by metabolic connectivity proling

Giulia Fiscon;Paola Paci;
2020

Abstract

Background Rewiring of metabolism induced by oncogenic K-Ras in cancer cells involves both glucose and glutamine utilization sustaining enhanced, unrestricted growth. The development of effective anti-cancer treatments targeting metabolism may be facilitated by the identification and rational combinatorial targeting of metabolic pathways. Methods We performed mass spectrometric metabolomics analysis in vitro and in vivo experiments to evaluate the efficacy of drugs and identify metabolic connectivity. Results We show that K-Ras-mutant lung and colon cancer cells exhibit a distinct metabolic rewiring, the latter being more dependent on respiration. Combined treatment with the glutaminase inhibitor CB-839 and the PI3K/aldolase inhibitor NVP-BKM120 more consistently reduces cell growth of tumor xenografts. Maximal growth inhibition correlates with the disruption of redox homeostasis, involving loss of reduced glutathione regeneration, redox cofactors, and a decreased connectivity among metabolites primarily involved in nucleic acid metabolism. Conclusions Our findings open the way to develop metabolic connectivity profiling as a tool for a selective strategy of combined drug repositioning in precision oncology.
2020
Cancer Metabolism; Metabolic rewiring; Metabolic cancer therapy; Metabolic signature; Glycolysis; Glutamine; Combinatorial drug treatment; Precision oncology; Metabolic connectivity;
01 Pubblicazione su rivista::01a Articolo in rivista
Disruption of redox homeostasis for combinatorial drug eefficacy in K-Ras tumors as revealed by metabolic connectivity proling / Gaglio, Daniela; Bonanomi, Marcella; Valtorta, Silvia; Bharat, Rohit; Ripamonti, Marilena; Conte, Federica; Fiscon, Giulia; Righi, Nicole; Napodano, Elisabetta; Papa, Federico; Raccagni, Isabella; Parker, Seth J.; Cifola, Ingrid; Camboni, Tania; Paci, Paola; Maria Colangelo, Anna; Vanoni, Marco; Metallo, Christian M.; Maria Moresco, Rosa; Alberghina, Lilia. - In: CANCER & METABOLISM. - ISSN 2049-3002. - 8:(2020), pp. 1-15. [10.1186/s40170-020-00227-4]
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Note: https://cancerandmetabolism.biomedcentral.com/articles/10.1186/s40170-020-00227-4
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1570717
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