Prolonged Hyporesponsiveness of Vascular Smooth Muscle Contraction after Halothane Anesthesia in Rabbits

Abstract

Halothane diminishes smooth muscle contractility in vascular tissue. In order to further characterize this phenomenon we undertook a series of in vivo and ex vivo experiments. Pressor dose-response curves to the selective α₁-adrenergic agonist, phenyleyhrine, were constructed in groups of rabbits before, during and 2 hr after halothane anesthesia and the dose of phenylephrine that induced a 25 torr increase in mean arterial pressure (ED₂₅) was derived by polynomial regression analysis. ED₂₅ torr increased significantly during halothane anesthesia, and rabbits remained in this insensitive state when the ED₂₅ was assessed 2 hr after anesthesia. The halothane-induced loss of responsiveness was corroborated by ex vivo experiments utilizing aortic rings from halothane-anesthetized rabbits. The maximal contraction to norepinephrine (NE) urns significantly lower in halothane-treated aortic rings and only slowly returned to normal by 4 hr. The EC₅₀ (the dose causing a 50% maximal contraction) for NE was significantly greater in aortic rings from halothane-anesthetized rabbits. This loss of sensitivity, reflected by the higher EC₅₀ was not restored by 4 hr of ex vivo incubation in a halothane-free medium. We conclude that halothane induces loss of sensitivity to adrenergic agonists that persists for several hours after termination of the halothane anesthetic.