Cellular and ionic mechanisms underlying the effects of cilostazol, milrinone, and isoproterenol to suppress arrhythmogenesis in an experimental model of early repolarization syndrome

Bence Patocskai; Hector Barajas-Martinez; Dan Hu; Zsolt Gurabi; István Koncz; Charles Antzelevitch

doi:10.1016/j.hrthm.2016.01.024

Cellular and ionic mechanisms underlying the effects of cilostazol, milrinone, and isoproterenol to suppress arrhythmogenesis in an experimental model of early repolarization syndrome

Heart Rhythm. 2016 Jun;13(6):1326-34. doi: 10.1016/j.hrthm.2016.01.024. Epub 2016 Jan 25.

Authors

Bence Patocskai¹, Hector Barajas-Martinez², Dan Hu², Zsolt Gurabi¹, István Koncz¹, Charles Antzelevitch³

Affiliations

¹ Masonic Medical Research Laboratory, Utica, New York; Department of Pharmacology and Pharmacotherapy, University of Szeged, Szeged, Hungary.
² Masonic Medical Research Laboratory, Utica, New York.
³ Lankenau Institute for Medical Research, Wynnewood, Pennsylvania. Electronic address: barajash@mmrl.edu.

Abstract

Background: Early repolarization syndrome (ERS) is associated with polymorphic ventricular tachycardia (PVT) and ventricular fibrillation, leading to sudden cardiac death.

Objective: The present study tests the hypothesis that the transient outward potassium current (Ito)-blocking effect of phosphodiesterase-3 (PDE-3) inhibitors plays a role in reversing repolarization heterogeneities responsible for arrhythmogenesis in experimental models of ERS.

Methods: Transmembrane action potentials (APs) were simultaneously recorded from epicardial and endocardial regions of coronary-perfused canine left ventricular (LV) wedge preparations, together with a transmural pseudo-electrocardiogram. The Ito agonist NS5806 (7-15 μM) and L-type calcium current (ICa) blocker verapamil (2-3 μM) were used to induce an early repolarization pattern and PVT.

Results: After stable induction of arrhythmogenesis, the PDE-3 inhibitors cilostazol and milrinone or isoproterenol were added to the coronary perfusate. All were effective in restoring the AP dome in the LV epicardium, thus abolishing the repolarization defects responsible for phase 2 reentry and PVT. Arrhythmic activity was suppressed in 7 of 8 preparations by cilostazol (10 μM), 6 of 7 by milrinone (2.5 μM), and 7 of 8 by isoproterenol (0.1-1 μM). Using voltage clamp techniques applied to LV epicardial myocytes, both cilostazol (10 μM) and milrinone (2.5 μM) were found to reduce Ito by 44.4% and 40.4%, respectively, in addition to their known effects to augment ICa.

Conclusion: Our findings suggest that PDE-3 inhibitors exert an ameliorative effect in the setting of ERS by producing an inward shift in the balance of current during the early phases of the epicardial AP via inhibition of Ito as well as augmentation of ICa, thus reversing the repolarization defects underlying the development of phase 2 reentry and ventricular tachycardia/ventricular fibrillation.

Keywords: Early repolarization; Electrophysiology; Pharmacology; Phosphodiesterase-3 inhibitors; Sudden cardiac death; Transient outward potassium current; Ventricular fibrillation.

MeSH terms

Action Potentials
Animals
Cardiac Electrophysiology / methods
Cardiovascular Agents / pharmacology
Cilostazol
Death, Sudden, Cardiac / etiology
Death, Sudden, Cardiac / prevention & control
Disease Models, Animal
Dogs
Electrocardiography / drug effects
Ion Channels / metabolism
Isoproterenol / pharmacology*
Milrinone / pharmacology*
Tachycardia, Ventricular* / drug therapy
Tachycardia, Ventricular* / physiopathology
Tetrazoles / pharmacology*
Ventricular Fibrillation* / drug therapy
Ventricular Fibrillation* / physiopathology

Substances

Cardiovascular Agents
Ion Channels
Tetrazoles
Milrinone
Isoproterenol
Cilostazol

Grants and funding

R01 HL047678/HL/NHLBI NIH HHS/United States