AMPK/mTOR-driven autophagy & Nrf2/HO-1 cascade modulation by amentoflavone ameliorates indomethacin-induced ‎gastric ‎ulcer

Gastric ulcer (GU) is a worldwide gastrointestinal disorder associated with ‎NSAID use. Recently, ‎amentoflavone proved to be a potent autophagy modulator, ‎antioxidant, anti-inflammatory, and ‎anti-apoptotic agent. Eight-week-old male ‎Wistar rats received amentoflavone orally for ‎‎14 days at 25, 50, or ‎‎100 mg/kg/day. On day 14 of treatment, GU was induced by a single ‎oral ‎instillation of 100 mg/kg indomethacin, one hour after the last treatment. ‎Amentoflavone ‎dose-dependently alleviated indomethacin-induced GU, as demonstrated ‎by repression of gastric mucosa ‎pathological manifestations (ulcer index, ‎ulcer surface area, histopathological deviations, and score) ‎and increased ‎ulcer inhibition percentage. These protective effects were due to the enhancement of gastric ‎mucosa ‎autophagy, as demonstrated by increased levels of beclin-1, MAP1LC3B, and CTSD, and reduced expression of p62 (SQSTM1). In addition, amentoflavone modulated the AMPK/mTOR ‎pathway by increasing ‎p-AMPK and reducing mTORC1 levels. Moreover, it ‎hindered the redox aberrations by reducing ‎MDA level and enhancing SOD ‎activity, GSH level, and Nrf2/HO-1 cascade. Furthermore, a decrease in caspase-3 levels, Bax/Bcl-2 ratio and an increase in Bcl-2 expression suggest inhibition of the apoptotic process. Additionally, amentoflavone suppressed gastric mucosal inflammation by decreasing IL-‎‎1β, TNF-α, IFN-γ ‎levels, IL-4, IL-6 mRNA expressions and MPO activity, and increasing IL-10 mRNA expresion. Therefore, amentoflavone could consider a ‎promising natural agent protecting ‎against indomethacin-induced GU‎.‎‎