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A computational model predicts adjunctive pharmacotherapy for cardiac safety via selective inhibition of the late cardiac Na current

机译:一种计算模型通过选择性抑制晚期心脏钠电流来预测辅助药物治疗对心脏安全的作用

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摘要

BackgroundThe QT interval is a phase of the cardiac cycle that corresponds to action potential duration (APD) including cellular repolarization (T-wave). In both clinical and experimental settings, prolongation of the QT interval of the electrocardiogram (ECG) and related proarrhythmia have been so strongly associated that a prolonged QT interval is largely accepted as surrogate marker for proarrhythmia. Accordingly, drugs that prolong the QT interval are not considered for further preclinical development resulting in removal of many promising drugs from development. While reduction of drug interactions with hERG is an important goal, there are promising means to mitigate hERG block. Here, we examine one possibility and test the hypothesis that selective inhibition of the cardiac late Na current (INaL) by the novel compound GS-458967 can suppress proarrhythmic markers.
机译:背景QT间隔是心动周期的一个阶段,对应于包括细胞复极化(T波)的动作电位持续时间(APD)。在临床和实验环境中,心电图(ECG)的QT间隔延长和相关的心律失常都密切相关,以至于延长的QT间隔被广泛接受为心律失常的替代指标。因此,延长QT间隔的药物不被考虑用于进一步的临床前开发,从而导致从开发中去除了许多有希望的药物。虽然减少与hERG的药物相互作用是一个重要的目标,但仍有减轻hERG阻滞的有希望的手段。在这里,我们研究了一种可能性并检验了以下假设:新型化合物GS-458967对心脏晚期Na电流(INaL)的选择性抑制可以抑制心律失常标志物。

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