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TRIad: foundation for proarrhythmia (triangulation, reverse use dependence and instability)

机译:三合一:预审血症基础(三角测量,反向使用依赖性和不稳定性)

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There exist both safe and dangerous prolongations of the QT interval. Proarrhythmia can be induced by triangulation of the cardiac action potential, reverse use dependence and instability, a set of three features termed TRIad. TRIad leads to dispersion (spatial, transmural and temporal), stalling of fast repolarization or even early after-depolarization (EAD). EAD can progress to Torsade de Pointes (TdP) especially in the presence of prolonged APD; as the QT interval shortens (e.g. by reverse use-dependence), the cardiac wavelength shortens and TdP can progress to ventricular fibrillation (VF). In the absence of TRIad and QT prolongation, chemicals exhibit on average neither pro- nor anti-arrhythmia. However, QT prolongation in the absence of TRIad becomes antiarrhythmic. Furthermore, this desirable effect increases as TRIad components are replaced by squaring of the action potential, use-dependent prolongation of APD and stabilization of the action potential. It is concluded that proarrhythmic characteristics of drugs can readily be recognized and that hope exists for an effective and safe class III antiarrhythmic agent after all.
机译:QT间隔存在安全且危险的延长。逆血可以通过心动动作潜力的三角测量来诱导,反向使用依赖性和不稳定,一套三种特征称为三合一。三合会导致分散(空间,透气和时间),停止快速复极性甚至甚至早期去极化(EAD)。 EAD可以进展到扭转DE指向(TDP),特别是在延长APD的存在下;随着Qt间隔缩短(例如通过反向使用依赖性),心脏波长缩短和TDP可以进入心室纤维化(VF)。在没有TRIAD和QT延长的情况下,化学品平均既不是或抗心律失常。然而,在没有三合会的情况下QT延长变为抗心律失常。此外,随着Triad组分通过平衡Action电位的平衡,APD的使用依赖性延长和动作电位的稳定而替换,该期望的效果增加。得出结论,可以容易地认识到药物的预训练特征,并希望毕竟存在有效和安全的III类抗真瘤剂。

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