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Divergent in vitro/in vivo responses to drug treatments of highly aggressive NIH-Ras cancer cells: a PET imaging and metabolomics-mass-spectrometry study.

Articolo
Data di Pubblicazione:
2016
Abstract:
Oncogenic K-ras is capable to control tumor growth and progression by rewiring cancer metabolism. In vitro NIH-Ras cells convert glucose to lactate and use glutamine to sustain anabolic processes, but their in vivo environmental adaptation and multiple metabolic pathways activation ability is poorly understood. Here, we show that NIH-Ras cancer cells and tumors are able to coordinate nutrient utilization to support aggressive cell proliferation and survival. Using PET imaging and metabolomics-mass spectrometry, we identified the activation of multiple metabolic pathways such as: glycolysis, autophagy recycling mechanism, glutamine and serine/glycine metabolism, both under physiological and under stress conditions. Finally, differential responses between in vitro and in vivo systems emphasize the advantageous and uncontrolled nature of the in vivo environment, which has a pivotal role in controlling the responses to therapy.
Tipologia CRIS:
01.01 Articolo in rivista
Keywords:
Tumor; metabolic rewiring; PET-imaging; metabolomics-mass-spectrometry; oncogenic-K-ras
Elenco autori:
DI GRIGOLI, Giuseppe; Gilardi, MARIA CARLA; Belloli, Sara; DI CAMPLI, Antonella; Luini, Alberto; Gaglio, Daniela; Valtorta, Silvia; Ripamonti, Marilena
Autori di Ateneo:
BELLOLI SARA
GAGLIO DANIELA
LUINI ALBERTO
RIPAMONTI MARILENA
VALTORTA SILVIA
Link alla scheda completa:
https://iris.cnr.it/handle/20.500.14243/317584
Pubblicato in:
ONCOTARGET
Journal
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