N -phenacyl-cyclopropylamine hydrobromide (54761) was evaluated in vitro and in vivo as a monoamine oxidase (MAO) inhibitor in rats. In contrast to 51641, which has an o-chlorophenoxy group in place of the phenacyl group and which is a highly selective inhibitor of type A MAO, 54761 showed a slight preference as a type B MAO inhibitor, since it inhibited phenylethylamine oxidation at slightly lower concentrations than were required to inhibit serotonin oxidation in vitro by rat liver MAO. Twelve analogs of 54761 with various substituents on the phenyl ring were also studied, but none was substantially more selective than 54761 as a type B inhibitor and most were preferential type A inhibitors. When 51641 and 54761 were injected into rats and MAO activity was assayed in tissue homogenates, the oxidation of serotonin in brain, heart and liver was inhibited more by 51641 than by 54761. In contrast, the oxidation of phenylethylamine was inhibited more by 54761 than by 51641 in brain and liver. In heart, however, 51641 was a more effective inhibitor of phenylethylamine oxidation than was 54761, supporting earlier evidence that phenylethylamine is destroyed in heart mainly by type A MAO. The oxidation of exogenous [ 14 C]phenylethylamine was inhibited in vivo more effectively by 54761, whereas the oxidation of endogenous serotonin in brain was inhibited more by 51641. Although 54761 is not as selective an inhibitor of type B MAO as some other compounds such as deprenyl, it illustrates that a large range of selectivity in MAO inhibition can exist within the N -cyclopropylamine series. Further, selective type B inhibition could be achieved in vivo 24 hr after injection of 54761 by co-administration of harmaline. Harmaline selectively protected against the inactivation of type A MAO by 54761 but permitted the inactivation of type B MAO to occur.
