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Circulation. 1999;100:2010-2017

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(Circulation. 1999;100:2010-2017.)
© 1999 American Heart Association, Inc.

Basic Science Reports

Electrophysiological and Antiarrhythmic Effects of the Atrial Selective 5-HT4 Receptor Antagonist RS-100302 in Experimental Atrial Flutter and Fibrillation

Marc M. Rahme, PhD; Bruno Cotter, MD; Elisabeth Leistad, MD; Manish K. Wadhwa, MD; Rajendra Mohabir, PhD; Anthony P. D. W. Ford, PhD; Richard M. Eglen, PhD; Gregory K. Feld, MD

From the Cardiac Electrophysiology Program, Division of Cardiology, Department of Medicine, University of California, San Diego (M.M.R., B.C., E.L., M.K.W., G.K.F.); Genentech, Inc, South San Francisco (R.M.); and Roche Bioscience, Inc, Palo Alto (A.P.D.W.F., R.M.E.), Calif.

Correspondence to Gregory K. Feld, MD, 200 W Arbor Dr, No. 8411, San Diego, CA 92103. E-mail gfeld{at}ucsd.edu

Background—Stimulation of 5-HT4 receptors increases atrial chronotropic and inotropic responses. Whether other electrophysiological effects are produced is unknown. In humans and swine, 5-HT4 receptors are present only in atrium. Therefore, the effects of a novel 5-HT4 receptor antagonist, RS-100302, and the partial agonist cisapride on atrial flutter and fibrillation induced in swine were studied to delineate the role of the 5-HT4 receptor in modulating atrial electrophysiological properties and the antiarrhythmic potential of RS-100302.

Methods and Results—In 17 anesthetized, open-chest, juvenile pigs, atrial flutter or fibrillation was induced by rapid right atrial pacing with or without a right atrial free wall crush injury, respectively. Atrial effective refractory period (ERP), conduction velocity, wavelength, and dispersion of refractoriness were determined during programmed stimulation via a 56-electrode mapping plaque sutured to the right atrial free wall. Ventricular electrophysiological parameters were also measured. All electrophysiological parameters were measured at baseline and after infusion of RS-100302 and cisapride. In the atrium, RS-100302 prolonged mean ERP (115±8 versus 146±7 ms, P<0.01) and wavelength (8.3±0.9 versus 9.9±0.8 cm, P<0.01), reduced dispersion of ERP (15±5 versus 8±1 ms, P<0.01), and minimally slowed conduction velocity (72±4 versus 67±5 cm/s, P<0.01). These effects were all partially reversed by cisapride. RS-100302 produced no ventricular electrophysiological effects. RS-100302 terminated atrial flutter in 6 of 8 animals and atrial fibrillation in 8 of 9 animals and prevented reinduction of sustained tachycardia in all animals.

Conclusions—The electrophysiological profile of RS-100302 suggests that it may have atrial antiarrhythmic potential without producing ventricular proarrhythmic effects.


Key Words: fibrillation • atrial flutter • serotonin • electrophysiology




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