Moracizine
Pharmacology
Moracizine, a
phenothiazine derivative, undergoes extensive first-pass metabolism and is also extensively metabolized after it has entered the circulation. It may have pharmacologically active metabolites. A clinical study has shown that moracizine is slightly less effective than
encainide or
flecainide in suppressing ventricular premature depolarizations. Compared with
disopyramide and
quinidine, moracizine was equally or more effective in suppressing premature ventricular contractions, couplets, and nonsustained ventricular tachycardia.
In the Cardiac Arrhythmia Suppression Trial (CAST), a large study testing the influence of antiarrhythmics on Mortality rate, showed a statistically non-significant increase of mortality from 5.4 to 7.2% under moracizine. This is in line with other class IC antiarrhythmics.
Synthesis
The reaction between N-phenyl-1,3-benzenediamine (1) and ethyl chloroformate (2) gives the
carbamate (3). Treatment with sulfur and iodine forms the phenothiazine derivative (4).
Amide formation with 3-chloropropionyl chloride (5) gives the penultimate intermediate (6).
Alkylation of
morpholine by nucleophilic substitution at the sidechain chlorine yields moricizine.
See also
