Receptor Interactions of Abbott-81988, A Highly Potent, Non-Peptide Angiotensin-II Antagonist Selective for Type-1 Receptors

Abstract

Abbott-81988 (A-81988) was selected from a series of related compounds as a highly potent and selective antagonist of angiotensin receptors. In the rabbit aorta, A-81988 exhibited a _pA₂ of 10.12 (± 0.08) vs. angiotensin-II, for type 1 receptors (AT₁), and the antagonism appeared competitive. These results agreed with radioligand assays in which A-81988 inhibited the binding of [¹²⁵l]-Sar¹ –lle⁸—Angiotensin-II to rat liver membranes with a _pK_I of 9.12 (± 0.63). A-81988 was selective for AT₁ receptors based on its lack of activity at other sites, such as aortic α 1 receptors. Moreover, A-81988 lacked affinity for AT₂ receptors of bovine cerebellar membranes or for α or β adrenergic receptors in binding assays. A-81988 lowered blood pressure significantly in vivo in renal artery-ligated rats at doses of 0.3 mg/kg administered either i.v. or p.o. The compound was rapidly and almost completely absorbed from the duodenum of anesthetized rats and demonstrated very low first-pass metabolism in the rat liver. These properties of selectivity toward and potency for antagonizing AT₁ receptors, activity in lowering blood pressure in experimental animals, and favorable pharmacokinetic properties indicate that A-81988 should be a useful antihypertensive agent in man.