Circulation, Vol 68, 385-391, Copyright © 1983 by American Heart Association
HJ Duff, AK Dawson, DM Roden, JA Oates, RF Smith and RL Woosley
Differences between the electrophysiologic actions of the antiarrhythmic
agent encainide have been reported after short-term intravenous and oral
administration. Only prolongation of the HV interval and QRS duration have
been described immediately after short- term intravenous administration of
encainide in dogs and man. However, during oral therapy or more prolonged
infusions, prolongation of the AH interval and atrial and ventricular
effective refractory periods have also occurred. In most patients receiving
encainide therapy, metabolites (O-demethyl encainide and
3-methoxy-O-demethyl encainide) accumulate during prolonged therapy to
concentrations greater than those of the parent drug. We compared the
electrophysiologic action of O-demethyl encainide with that of saline in
anesthetized dogs to determine if this metabolite has pharmacologic
activity and whether its electrophysiologic effects could account for the
disparities noted between effects of intravenous and oral encainide
therapy. An initial pharmacokinetic evaluation allowed design of a series
of loading and maintenance infusions that produced plasma concentrations
similar to those seen during encainide therapy in man (concentration after
first maintenance dose, 149 +/- 27 ng/ml [+/- SE] and after second
maintenance dose, 230 +/- 45 ng/ml). Significant increases in atrial
effective refractory period and ventricular refractoriness, and
prolongation of AH interval and HV conduction time were observed. These
effects are similar to those reported after prolonged oral encainide
therapy but are substantially different from those seen after short- term
infusions of encainide. These findings indicate that the difference between
the electrophysiologic actions of intravenous and oral encainide may be due
to pharmacologic effects of at least one encainide metabolite, O-demethyl
encainide.
ARTICLES
Electrophysiologic actions of O-demethyl encainide: an active metabolite
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