Asynchronous development of electrical remodeling and cardiac hypertrophy in the complete AV block dog

doi:10.1016/S0008-6363(03)00430-9

Cardiovascular Research 2003 59(2):351-359; doi:10.1016/S0008-6363(03)00430-9
© 2003 by European Society of Cardiology

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Asynchronous development of electrical remodeling and cardiac hypertrophy in the complete AV block dog

Marieke Schoenmakers, Christian Ramakers, Jurren M. van Opstal, Jet D.M. Leunissen, Camila Londoño and Marc A. Vos^*

Department of Cardiology, Cardiovascular Research Institute Maastricht, PO Box 5800, 6202 AZ Maastricht, The Netherlands

^* Corresponding author. Tel.: +31-43-387-5097; fax: +31-43-387-5104. New address: Department of Medical Physiology, UMCU, Universiteitsweg 100, 3584 CG Utrecht, The Netherlands. Tel.: +31-30-2538900; fax: +31-30-2539036. m.vos{at}cardio.azm.nl m.a.vos{at}med.uu.nl

Objective: Left ventricular hypertrophy has been associatedwith the prolongation of QT-time, and an increased risk of ventriculararrhythmias. The renin angiotensin system has been implicatedin the development of ventricular hypertrophy. At 5 weeks completeAV block (CAVB) in the dog, there is: (1) biventricular hypertrophyassociated with a transient activation of components of therenin angiotensin system, (2) increased APD, more pronouncedin the left than in the right ventricle leading to spatial dispersionof repolarization, and (3) enhanced susceptibility to drug-inducedtorsade de pointes arrhythmias. To investigate whether theseremodeling processes develop in parallel, time dependency wasassessed in absence or presence of the AT1 receptor-blockerIrbesartan. Methods and results: Dogs in sinus rhythm, 2 and5 weeks CAVB were compared to dogs chronically treated withIrbesartan (30 mg/kg BID). Endocardial monophasic APD of leftand right ventricle was measured and susceptibility to torsadede pointes was tested by infusing Dofetilide (0.025 mg/kg/5').Hypertrophy was determined by relating heart-to-body weightat sacrifice. Left ventricular APD had increased more than rightventricular APD at 2 and 5 weeks CAVB, leading to an increasein spatial dispersion. At that time torsade de pointes wereevocable in the majority of the dogs. Hypertrophy had only developedcompletely at 5 weeks CAVB. Irbesartan had no effect on electricaland structural parameters or on arrhythmogenicity. Conclusions:In the CAVB dog ventricular hypertrophy is not a prerequisitefor electrical remodeling or drug-induced torsade de pointes,and the AT1-receptor has no dominant role in the completionof these remodeling processes.

KEYWORDS Repolarization; Ventricular arrhythmias; Renin angiotensin system

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