Pharmacologic properties of FPL 55712 administered by aerosol

Abstract

FPL 55712 was investigated by the aerosol route of administration for efficacy at protecting against leukotriene-induced bronchoconstrictions in guinea pigs and for mediator release inhibitory activity in passively sensitized rats. In the studies to investigate leukotriene antagonism; anesthetized, spontaneously breathing guinea pigs were pretreated with propranolol and were exposed via tracheal cannula to aerosols generated by a Monaghan nebulizer. Subsequently, the animals were artificially ventilated and challenged with LTD₄ or LTE₄ (25 μg/kg, i.v.). FPL 55712 produced a concentration-dependent inhibition of LTD₄ and LTE₄-induced bronchoconstriction (IC₅₀'s 0.5% and 0.8%, respectively). Although the biologic half-life of FPL 55712, administered intravenously, was very short (1.7 minutes against LTD₄ and 1.2 minutes against LTE₄) after aerosol administration the biological half-life was surprisingly long (120 minutes against LTD₄ and 90 minutes against LTE₄). Aerosolized FPL 55712 also possessed weak antiallergic activity in comparison to disodium cromoglycate when measured as an inhibitor of IgE-mediated anaphylactic bronchoconstriction in rats (IC₅₀'s of 2.0% and 0.01%, respectively). Thus, these studies demonstrate that, when administered by aerosol, FPL 55712 is effective at protecting against leukotriene-induced bronchoconstrictions, exhibits a long duration of action and also possesses weak antiallergic activity.