EFFICACY AND SAFETY OF MORICIZINE IN PATIENTS WITH CONGESTIVE HEART-FAILURE - A SUMMARY OF THE EXPERIENCE IN THE UNITED-STATES

Patients with ventricular premature beats (VPBs) and congestive heart failure (CHF) have an increased risk of sudden death, yet suppression of arrhythmia in this population is frequently complicated by proarrhythmia and by the negative inotropic effects of antiarrhythmic drugs. The purpose of this study was to evaluate the safety and efficacy of moricizine in patients with clinical CHF. The New Drug Application data base submitted to the Food and Drug Administration was analyzed. A total of 908 patients were treated with moricizine for ventricular arrhythmias; CHF developed in 49 of them (5.4%). Of the 908 patients, 374 had a history of CHF, 326 of whom tolerated moricizine for a mean of 97±217 days. New-onset CHF occurred only once (1/546=0.2%). Recurrence of exacerbation of clinical CHF during treatment with moricizine occurred in 48 of 374 patients (12.8%), 28 of whom continued to take moricizine with alteration in CHF therapy. The mean left ventricular ejection fraction (LVEF) of those patients in whom CHF developed was 26%. It is important to note that patients with a history of CHF were as likely to have suppression of VPBs (defined as ≥75% reduction) as those without a history of CHF. In fact, suppression of arrhythmia was achieved as often in patients with LVEF <30% as in those with more preserved LVEF. Of the 374 patients with a history of CHF, 15 (4%) had a proarrhythmic event within 14 days of therapy. The incidence of sudden cardiac death in this group was 0.8%. These proarrhythmia rates compare favorably with those of other antiarrhythmic drugs. In conclusion, moricizine has a good safety profile and appears to be well tolerated in patients with mild CHF, in whom suppression of VPBs is often achieved. © 1990 Mosby-Year Book, Inc.