α- and β-Naphthoflavone synergistically attenuate H2O2-induced neuron SH-SY5Y cell damage

Previous studies have demonstrated an association between neurological diseases and oxidative stress (OS). Naphthoflavone is a synthetic derivative of naturally occurring Flavonoids that serves an important role in the treatment and prevention of OS-related diseases. The current study was designed to apply α- and β-Naphthoflavone individually and in combination to counteract the detrimental effects of OS on neurons in vitro. Neuronal SH-SY5Y cells were subjected to 20 µM H₂O₂, followed by exposure to 20 µM α-Naphthoflavone and/or 10 µM β-Naphthoflavone. Results indicated that α- and β-Naphthoflavone effectively antagonized the apoptosis-promoting effect of H₂O₂ on neuronal SH-SY5Y cells, and that β-Naphthoflavone significantly (P<0.05) reversed H₂O₂-inhibited cell viability. Notably, co-treatment of α- and β-Naphthoflavone reversed the H₂O₂-induced Apoptosis rate elevation and cell viability reduction. Further analysis demonstrated that H₂O₂ inhibited the activities of antioxidant enzymes including catalase, superoxide dismutase and Glutathione Peroxidase, but this was reversed by the co-treatment with α- and β-Naphthoflavone and selectively enhanced by the treatment with α- or β-Naphthoflavone. H₂O₂-stimulated p38 mitogen-activated protein kinase activation was repressed following treatment with α- and/or β-Naphthoflavone, along with a decreased expression of the apoptosis-related factors and inhibited Caspase-3 activation. In conclusion, co-treatment with α- and β-Naphthoflavone minimized H₂O₂-led neuron damage compared with treatment with α- or β-Naphthoflavone, suggesting a synergetic effect between α- and β-Naphthoflavone. This indicates that utilizing α- and β-Naphthoflavone together in the clinical setting may provide a novel therapeutic for Neurological Disease.