The activation of ATP-sensitive potassium current [I/sub K(ATP)/] during metabolic impairment or by addition of potassium channel openers (KCOs), such as pinacidil, shortens the action potential duration (APD). This effect supports the hypothesis that KCOs are proarrhythmical agents. However, controversies on this purpose make necessary to study the problem further. In this work, we have formulated a mathematical model of the effects of pinacidil on I/sub K(ATP)/ based on experimental data in order to simulate these effects on a cell or a tissue. We have introduced our formulation in the ventricular cardiac action potential model described by Luo and Rudy [1994] (phase II) completed with the formulation of I/sub K(ATP)/ by Ferrero et al. [1996]. The results of our theoretical model are in accordance with the estimated experimental values, that show the shortening of APD after the addition of pinacidil, specially in pathological situations. This work is a first step towards further simulations on myocardial tissue, which could help to elucidate the problem of arrhythmogenesis under the action of pinacidil.
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机译:在代谢受损期间或通过添加钾通道开放剂(KCO)(例如吡那地尔)激活ATP敏感性钾电流[I / sub K(ATP)/],可缩短动作电位持续时间(APD)。这种效果支持了KCO是心律失常药物的假设。但是,为此目的的争议使得有必要进一步研究该问题。在这项工作中,我们基于实验数据制定了吡那地尔对I / sub K(ATP)/影响的数学模型,以便模拟这些对细胞或组织的影响。我们在Luo和Rudy [1994](第二阶段)描述的心室心脏动作电位模型中引入了我们的配方,并由Ferrero等人完成了I / sub K(ATP)/的配方。 [1996]。我们的理论模型的结果与估计的实验值一致,表明添加了吡那地尔后,APD缩短,特别是在病理情况下。这项工作是进一步模拟心肌组织的第一步,这可以帮助阐明在吡那地尔作用下心律不齐的问题。
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