The roles of prostaglandin E receptor subtypes in the cytoprotective action of prostaglandin E2 in rat stomach

Abstract

Aim: To investigate the EP receptor subtype involved in the gastroprotective action of prostaglandin (PG) E₂ using various EP receptor agonists in rats, and using knockout mice lacking EP₁ or EP₃ receptors. Methods: Male SD rats and C57BL/6 mice were used after an 18‐h fast. Gastric lesions were induced by oral administration of HCl/ethanol (150 m m HCl in 60% ethanol). Rats were given various EP agonists i.v. 10 min before HCl/ethanol: PGE₂, sulprostone (EP₁/EP₃ agonist), butaprost (EP₂ agonist), 17‐phenyl‐ω‐trinorPGE₂ (17‐phenylPGE₂: EP₁ agonist), ONO‐NT012 (EP₃ agonist) and 11‐deoxyPGE₁ (EP₃/EP₄ agonist). In a separate study, the effect of PGE₂ on HCl/ethanol lesions was examined in EP₁‐ and EP₃‐receptor knockout mice. Results: Gastric lesions induced by HCl/ethanol were dose dependently prevented by PGE₂; this effect was mimicked by sulprostone and 17‐phenylPGE₂ and was significantly antagonized by ONO‐AE‐829, an EP₁ antagonist. Neither butaprost, ONO‐NT012 nor 11‐deoxyPGE₁ exhibited any protective activity against HCl/ethanol‐induced gastric lesions. PGE₂ caused an inhibition of gastric motility as well as an increase of mucosal blood flow and mucus secretion, the effects being mimicked by prostanoids activating EP₁ receptors, EP₂/EP₃/EP₄ receptors and EP₄ receptors, respectively. On the other hand, although HCl/ethanol caused similar damage in both wild‐type mice and knockout mice lacking EP₁ or EP₃ receptors, the cytoprotective action of PGE₂ observed in wild‐type and EP₃‐receptor knockout mice totally disappeared in mice lacking EP₁ receptors. Conclusion: The gastric cytoprotective action of PGE₂ is mediated by activation of EP₁ receptors. This effect may be functionally associated with inhibition of gastric motility but not with increased mucosal blood flow or mucus secretion.