Approximate analytical solutions for excitation and propagation in cardiac tissue

D'Artagnan Greene and Yohannes Shiferaw
Phys. Rev. E 91, 042719 – Published 30 April 2015

Abstract

It is well known that a variety of cardiac arrhythmias are initiated by a focal excitation in heart tissue. At the single cell level these currents are typically induced by intracellular processes such as spontaneous calcium release (SCR). However, it is not understood how the size and morphology of these focal excitations are related to the electrophysiological properties of cardiac cells. In this paper a detailed physiologically based ionic model is analyzed by projecting the excitation dynamics to a reduced one-dimensional parameter space. Based on this analysis we show that the inward current required for an excitation to occur is largely dictated by the voltage dependence of the inward rectifier potassium current (IK1), and is insensitive to the detailed properties of the sodium current. We derive an analytical expression relating the size of a stimulus and the critical current required to induce a propagating action potential (AP), and argue that this relationship determines the necessary number of cells that must undergo SCR in order to induce ectopic activity in cardiac tissue. Finally, we show that, once a focal excitation begins to propagate, its propagation characteristics, such as the conduction velocity and the critical radius for propagation, are largely determined by the sodium and gap junction currents with a substantially lesser effect due to repolarizing potassium currents. These results reveal the relationship between ion channel properties and important tissue scale processes such as excitation and propagation.

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  • Received 2 January 2015

DOI:https://doi.org/10.1103/PhysRevE.91.042719

©2015 American Physical Society

Authors & Affiliations

D'Artagnan Greene and Yohannes Shiferaw

  • Department of Physics and Astronomy, California State University, Northridge, California 91330, USA

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Issue

Vol. 91, Iss. 4 — April 2015

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