In Vitro Pharmacology of a Novel Non-Peptide Angiotensin II-Receptor Antagonist, E4177

抄録

E4177, 3-[(2''-carboxybiphenyl-4-yl)methyl]-2-cyclopropyl-7-methyl-3H-imidazo[4, 5-b]pyridine, was characterized by in vitro autoradiography and by examining functional antagonism upon angiotensin II (Ang II)-induced contraction of isolated vessels. In rat adrenal cortex and liver, E4177 competitively inhibited the specific binding of ¹²⁵I-[Sar¹, Ile⁸]Ang II, with IC₅₀ being (5.2±1.0)×10^-8M for the adrenal cortex and (1.2±0.3)×10^-7 M for the liver. These IC₅₀ values were similar to those for losartan, which showed an IC₅₀ of (6.0±0.9)×10^-8M for the adrenal cortex and (1.3±0.5)×10^-7M for the liver. In contrast, E4177 and losartan had little effect on the binding to rat adrenal medulla where AT₂-receptors predominate. These results indicate that E4177 is AT₁-specific as is losartan. E4177 and losartan competitively antagonized the Ang II-induced contraction of human and rabbit arterial strips without any agonistic action. The obtained IC₅₀ values indicated that E4177 was twice as potent as losartan in human arteries and three times more so in rabbit aortic strips. Responses to norepinephrine, serotonin, histamine or KCl were not affected by E4177. In addition, E4177 (10^-5M) had no effect on angiotensin-converting enzyme activity. These data indicate that E4177 is a potent AT₁ Ang II-receptor antagonist that may be clinically useful for the treatment of cardiovascular diseases such as hypertension.