Publication | Open Access
Androgens induce oxidative stress and radiation resistance in prostate cancer cells though NADPH oxidase
71
Citations
25
References
2009
Year
Nadph OxidaseProstate Cancer CellsRadiation BiologyReactive Oxygen SpeciesRedox BiologyOxidative StressRadiation MedicineCancer Cell BiologyRadiation OncologySteroid MetabolismBiochemistryMedicineReactive Oxygen SpeciePharmacologyCell BiologyEndocrine-related CancerReductive StressAndrogen Deprivation TherapyOncology
Androgen deprivation therapy (ADT) facilitates the response of prostate cancer (PC) to radiation. Androgens have been shown to induce elevated basal levels of reactive oxygen species (ROS) in PC, leading to adaptation to radiation-induced cytotoxic oxidative stress. Here, we show that androgens increase the expression of p22phox and gp91phox subunits of NADPH oxidase (NOX) and ROS production by NOX2 and NOX4 in PC. Pre-radiation treatment of 22Rv1 human PC cells with NOX inhibitors sensitize the cells to radiation similarly to ADT, suggesting that their future usage may spare the need for adjuvant ADT in PC patients undergoing radiation.
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