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European Heart Journal 1994 15(4):514-522;
Copyright © 1994 by the European Society of Cardiology.
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© 1994 The European Society of Cardiology

Effect of dofetilide on cardiac repolarization in patients with ventricular tachycardia A study using simultaneous monophasic action potential recordings from two sites in the right ventricle

S. YUAN, B. WOHLFART{dagger}, H. S. RASMUSSEN{ddagger}, S. OLSSON and C. BLOMSTRÖM-LUNDQVIST*

Departments of Cardiology University Hospital Lund, Sweden
{dagger}Clinical Physiology, University Hospital Lund, Sweden
{ddagger}Pfizer Central Research Kent, U.K.

Received 14 June 1993; revised 25 October 1993; .

Correspondence, Shiwen Yuan, M.D., Department of Cardiology, University Hospital of Lund, S-221 85 Lund, Sweden

Abstract

Monophasic action potentials (MAP) were simultaneously recorded from the right ventricular (RV) apex (RVA) and the outflow tract (RVOT) before and after an infusion of dofetilide in 10 patients with documented ventricular tachycardia. After the drug infusion, the MAP duration (MAPd), repolarization time, and corrected QT interval were significantly prolonged during sinus rhythm, R V pacing, and R V extra stimulation. The prolongation of MAPd at 90% repolarization during RV pacing at a cycle length of 500 ms was 31 ±6 ms (13%) and 26 ±7 ms (11%) at RVA and RVOT, respectively. The ventricular effective refractory period was significantly prolonged by 33 ±9 ms (13%) and 22 ±7 ms (9%) at driving cycle lengths 600 and 500 ms, respectively. The MAPd shortening with decreasing diastolic time intervals was significantly diminished by dofetilide in early extra beats during RV extra stimulation, suggesting a relatively more pronounced effect of this drug at the early diastolic phase. The dispersion of repolarization, defined as the difference in MAPd between R VA and R VOT, and the activation time were not significantly changed. In conclusion, acute administration of dofetilide in patients with ventricular tachycardia significantly prolonged the time intervals of ventricular repolarization and refractoriness in a parallel fashion, without affecting intraventricular conduction. The effect of dofetilide on MAPd prolongation appeared not to be reverse use-dependent in this study in humans. These results verify the selective class III antiarrhythmic property of dofetilide and warrant further studies in patients.

Key Words: Dofetilide • monophasic action potential • repolarization • dispersion • ventricular tachycardia


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