Spiral- and scroll-wave dynamics in mathematical models for canine and human ventricular tissue with varying Potassium and Calcium currents


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We conduct a systematic,direct-numerical-simulation study,in mathematical models for ventricular tissue,of the dependence of spiral-and scroll-wave dynamics on $G_{Kr}$, the maximal conductance of the delayed rectifier Potassium current($I_{Kr}$) channel,and the parameter $gamma_{Cao}$,which determines the magnitude and shape of the current $I_{CaL}$ for the L-type calcium-current channel,in both square and anatomically realistic,whole-ventricle simulation domains using canine and human models. We use ventricular geometry with fiber-orientation details and employ a physiologically realistic model for a canine ventricular myocyte. We restrict ourselves to an HRD-model parameter regime, which does not produce spiral- and scroll-wave instabilities because of other,well-studied causes like a very sharp action-potential-duration-restitution (APDR) curve or early after depolarizations(EADs) at the single-cell level. We find that spiral- or scroll-wave dynamics are affected predominantly by a simultaneous change in $I_{CaL}$ and $I_{Kr}$,rather than by a change in any one of these currents;other currents do not have such a large effect on these wave dynamics in this parameter regime of the HRD model.We obtain stability diagrams in the $G_{Kr} -gamma_{Cao}$ plane.In the 3D domain,the geometry of the domain supports the confinement of the scroll waves and makes them more stable compared to their spiral-wave counterparts in 2D domain. We have also carried out a comparison of our HRD results with their counterparts for the human-ventricular TP06 model and have found important differences. In both these models,to make a transition,(from broken-wave to stable-scroll states or vice versa) we must simultaneously increase $I_{Kr}$ and decrease $I_{CaL}$;a modification of only one of these currents is not enough to effect this transition.

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