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Cited 13 time in webofscience Cited 14 time in scopus
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p53-dependent glutamine usage determines susceptibility to oxidative stress in radioresistant head and neck cancer cells

Authors
Chang, Hyo WonLee, MyungJinLee, Yoon SunKim, Song HeeLee, Jong CheolPark, Jung JeNam, Hae YunKim, Mi RaHan, Myung WoulKim, Seong WhoKim, Sang Yoon
Issue Date
Jan-2021
Publisher
Elsevier BV
Keywords
p53; Glutamine; Glycolytic shift; Radioresistant cancer cells; Reactive oxygen species
Citation
Cellular Signalling, v.77
Indexed
SCIE
SCOPUS
Journal Title
Cellular Signalling
Volume
77
URI
https://scholarworks.gnu.ac.kr/handle/sw.gnu/4325
DOI
10.1016/j.cellsig.2020.109820
ISSN
0898-6568
1873-3913
Abstract
The manner in which p53 maintains redox homeostasis and the means by which two key metabolic elements, glucose and glutamine, contribute to p53-dependent redox stability remain unclear. To elucidate the manner in which p53 deals with glucose-deprived, reactive oxygen species (ROS)-prone conditions in this regard, two isogenic cancer subclones (HN3R-A and HN3R-B) bearing distinct p53 mutations as an in vitro model of intratumoral p53 heterogeneity were identified. Following cumulative irradiation, the subclones showed a similar metabolic shift to aerobic glycolysis and increasing NADPH biogenesis for cellular defense against oxidative damage irrespective of p53 status. The radioresistant cancer cells became more sensitive to glycolysis-targeting drugs. However, in glucose-deprived and ROS-prone conditions, HN3R-B, the subclone with the original p53 increased the utilization of glutamine by GLS2, thereby maintaining redox homeostasis and ATP. Conversely, HN3R-A, the p53-deficient radioresistant subclone displayed an impairment in glutamine usage and high susceptibility to metabolic stresses as well as ROS-inducing agents despite the increased ROS scavenging system. Collectively, our findings suggest that p53 governs the alternative utilization of metabolic ingredients, such as glucose and glutamine, in ROS-prone conditions. Thus, p53 status may be an important biomarker for selecting cancer treatment strategies, including metabolic drugs and ROS-inducing agents, for recurrent cancers after radiotherapy.
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