Zeneca ZD7114 acts as an antagonist at β3‐adrenoceptors in rat isolated ileum

Abstract

The relaxant effects of Zeneca ZD7114, BRL37344 (putative β₃‐adrenoceptor agonists) and various phenylethylamine‐based agonists were studied in isolated ileum of the rat where tone was increased with carbachol (0.5 μm). Agonist‐induced relaxation was measured under equilibrium conditions with α‐, β₁‐ and β₂‐adrenoceptors inhibited. Relaxant responses were obtained to isoprenaline, noradrenaline, and BRL37344, although, the efficacy of this latter agent was significantly lower than that of isoprenaline. Salbutamol caused weak relaxation (K_B values of 5.7 with isoprenaline as the agonist and 5.5 with BRL37344 as the agonist. The non‐selective β‐adrenoceptor antagonist, (±)‐alprenolol (1–100 μm) caused competitive antagonism of the relaxant responses to isoprenaline (pA₂ value = 6.5). A similar pK_B value was obtained when BRL37344 was used as the agonist (6.4). Relaxant effects of isoprenaline and BRL37344 were also antagonized by ZD7114 (1–100 μm) yielding pA₂ and pK_B values of 6.3 and 6.7 respectively. The low potencies of (±)‐propranolol and (±)‐alprenolol as antagonists of the relaxant responses to isoprenaline and BRL37344 indicate that both the agonists and antagonists employed in the current study may interact with β₃‐adrenoceptors in the rat isolated ileum. Contrary to the previous findings in guinea‐pig ileum, where BRL37344 and ZD7114 were full agonists, in the current study, BRL37344 was a partial agonist and ZD7114 an antagonist at the β₃‐adrenoceptor in rat ileum.