Antiarrhythmic vs. pro-arrhythmic effects depending on the intensity of adrenergic stimulation in a canine anthopleurin-A model of type-3 long QT syndrome

doi:10.1093/europace/eun002

Europace 2008 10(2):249-255; doi:10.1093/europace/eun002

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EXPERIMENTAL STUDIES

Antiarrhythmic vs. pro-arrhythmic effects depending on the intensity of adrenergic stimulation in a canine anthopleurin-A model of type-3 long QT syndrome

Masaomi Chinushi¹^,*, Daisuke Izumi², Kenichi Iijima², Shizue Ahara¹, Satoru Komura², Hiroshi Furushima², Yukio Hosaka² and Yoshifusa Aizawa²

¹ School of Health Science, Niigata University School of Medicine, 2-746 Asahimachi, Nigata 951-8518, Japan; ² First Department of Internal Medicine, Niigata University School of Medicine, Nigata, Japan

Aims: The effects of adrenergic activity and beta-blockade were studiedin a canine experimental model of type-3 long QT syndrome (LQT3)induced by application of anthopleurin-A.

Methods and results: Boluses of epinephrine at 0.5 and/or 1.0 µg/kg were administeredbefore and after propranolol, 0.3 mg/kg, and the distributionof the ventricular repolarization and the development of polymorphicventricular tachyarrhythmia (VA) were assessed. Using needleelectrodes, transmural unipolar electrograms were recorded acrossthe left ventricle (LV) and right ventricle (RV). Activation-recoveryinterval (ARI) was measured in each electrogram to estimatelocal repolarization during RV pacing at the cycle length of750 ms after the creation of complete atrioventricular block.Before propranolol, epinephrine, 0.5 µg/kg, did not induceVA in any experiment. However, a dose of 1.0 µg/kg inducedpolymorphic VA following multiple premature ventricular complex(PVC) in four of six experiments. Epinephrine, 0.5 µg/kg,shortened ARI at all sites and lessened LV transmural ARI dispersion.Neither ARI nor its dispersion could be determined after 1.0µg/kg of epinephrine because of the induction of PVC,polymorphic VA, or both. Propranolol (i) prevented epinephrine-inducedPVC and polymorphic VA in all experiments, (ii) slightly prolongedARI at all sites, along with a decrease in LV transmural ARIdispersion, and (iii) reversed the epinephrine-induced shorteningof ARI.

Conclusion: In this LQT3 model, an increase in adrenergic activity by epinephrinehad dose-dependent, opposite effects on ventricular electricalstability. Since beta-adrenergic blockade suppressed epinephrine-inducedPVC and polymorphic VA, it might be considered for supplementaltherapy to suppress VA in patients presenting with LQT3.

Key Words: Type-3 long QT syndrome, Adrenergic activity, Beta-adrenergic blockade

^* Corresponding author. Tel: +81 25 227 2185; fax: +81 25 227 0774.E-mail address: masaomi{at}clg.niigata-u.ac.jp

Manuscript submitted 12 September 2007. Accepted after revision 28 December 2007.

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