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Antiarrhythmic drug effect analysis on a model of cardiac fiber

机译:心脏纤维模型的抗心律失常药物作用分析

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Pharmacological treatment of cardiac arrhythmias still arises serious questions concerning both efficiency and safety. CAST failure as well as classification based on functional characteristics revealed the arrhythmogenic potential of both class I and class III agents, but failed to identify proarrhythmic mechanisms. These study, presents results from a model of the ventricle using a modified Luo-Rudy phase I cellular formulation. The model was used for studying both pro- and antiarrhythmic mechanisms of class I drugs. "Monitoring" was performed at cellular and cardiac fiber level in normal conditions and after drug delivery. For each specific arrhythmogenic mechanism, vulnerable parameters were investigated in order to detect the appropriate agent and ifs delivering requirements. Simulations revealed the link between the cellular antiarrhythmic potential and a proarrhythmic effect at the multicellular level.
机译:心律失常的药理治疗仍然引起有关效率和安全性的严重问题。 CAST失败以及基于功能特征的分类揭示了I类和III类药物的致心律失常潜力,但未能确定心律失常的机制。这些研究提出了使用改良的Luo-Rudy I期细胞制剂的心室模型的结果。该模型用于研究I类药物的抗心律失常机制。在正常情况下以及给药后,在细胞和心脏纤维水平进行“监测”。对于每种特定的心律失常发生机制,都对易受伤害的参数进行了研究,以检测合适的药物以及是否满足输送要求。模拟揭示了细胞抗心律失常潜力与多细胞水平的心律失常作用之间的联系。

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