Acceleration of functional reentry by rapid pacing in anisotropic cardiac monolayers: Formation of multi-wave functional reentries

doi:10.1016/j.cardiores.2005.09.014

Cardiovascular Research 2006 69(2):381-390; doi:10.1016/j.cardiores.2005.09.014

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Acceleration of functional reentry by rapid pacing in anisotropic cardiac monolayers: Formation of multi-wave functional reentries

Nenad Bursac^b^,* and Leslie Tung^a

^aDepartment of Biomedical Engineering, Johns Hopkins University, Baltimore, MD, 21205, USA
^bDepartment of Biomedical Engineering, Duke University, 3000 Science Drive, Durham, NC, 27708, USA

^* Corresponding author. Tel.: +1 919 660 5510; fax: +1 919 684 4488. Email address: nbursac{at}duke.edu

Objective: Attempts to cardiovert tachycardia by rapid pointpacing can sometimes result in transient or stable increaseof the heart rate (acceleration), changed ECG morphology, and/orfibrillation. The goal of this study was to investigate theeffect of rapid pacing on the dynamics of functional reentryin monolayer cultures of cardiac cells.

Methods: Fully confluent, uniformly anisotropic monolayers ofneonatal rat ventricular myocytes were prepared using methodsof microabrasion. Cells were paced by a point electrode at restand during functional reentry, and membrane voltages were opticallymapped.

Results: Point pacing readily induced single loop anisotropicfunctional reentry with monomorphic optical pseudo-ECG (pECG)and average rotation period of 193 ± 52 ms (n=71 monolayers).Attempts to cardiovert reentry by rapid pacing at rates 10–50%faster than the reentry rate were successful in 57/71 monolayers.In 14/71 monolayers, the number of rotating waves was stablyincreased by 1 to 4, yielding a 10–70% acceleration ofpECG rate and change to a different monomorphic or polymorphicpECG. The resulting multi-wave functional reentries were classifiedbased on the number and direction of their rotating waves. Thehigher the number of waves in the multi-wave reentry, the moreaccelerated was the rate of cell firing in the monolayer. Importantly,stable acceleration was only inducible in monolayers with relativelydeep and broad conduction velocity restitution relationships.Reapplication of point pacing further accelerated, decelerated,or eventually terminated the reentrant activity.

Conclusions: These results suggest that stable multiplicationof rotating waves in conjunction with a deep and broad conductionvelocity restitution relationship is a possible mechanism forstable acceleration of functional reentry by rapid pacing.

KEYWORDS Cardiac electrophysiology; Optical mapping; Cell culture; Functional reentry; Rate acceleration

Time for primary review 21 days

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