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Screening system for drug-induced arrhythmogenic risk combining a patch clamp and heart simulator

机译:膜片钳和心脏模拟器相结合的药物致心律失常风险筛查系统

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摘要

To save time and cost for drug discovery, a paradigm shift in cardiotoxicity testing is required. We introduce a novel screening system for drug-induced arrhythmogenic risk that combines in vitro pharmacological assays and a multiscale heart simulator. For 12 drugs reported to have varying cardiotoxicity risks, dose-inhibition curves were determined for six ion channels using automated patch clamp systems. By manipulating the channel models implemented in a heart simulator consisting of more than 20 million myocyte models, we simulated a standard electrocardiogram (ECG) under various doses of drugs. When the drug concentrations were increased from therapeutic levels, each drug induced a concentration-dependent characteristic type of ventricular arrhythmia, whereas no arrhythmias were observed at any dose with drugs known to be safe. We have shown that our system combining in vitro and in silico technologies can predict drug-induced arrhythmogenic risk reliably and efficiently.
机译:为了节省药物发现的时间和成本,需要进行心脏毒性测试的范例转换。我们介绍了一种针对药物诱发的心律失常风险的新型筛查系统,该系统结合了体外药理测定和多尺度心脏模拟器。对于据报道具有不同心脏毒性风险的12种药物,使用自动膜片钳系统确定了六个离子通道的剂量抑制曲线。通过操纵在包含超过2000万个心肌细胞模型的心脏模拟器中实现的通道模型,我们在各种剂量的药物下模拟了标准心电图(ECG)。当药物浓度从治疗水平升高时,每种药物都会引起浓度依赖性的室性心律失常特征类型,而已知任何安全剂量的药物在任何剂量下均未观察到心律失常。我们已经表明,将体外和计算机技术相结合的系统可以可靠,有效地预测药物引起的心律失常风险。

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