复极化的双重药理学挑战为药物安全性研究开辟了新途径。
Double pharmacological challenge on repolarization opens new avenues for drug safety research.
作者信息
Thomsen M B
机构信息
Department of Pharmacology, College of Physicians and Surgeons, Columbia University, 630 W. 168th Street, NY 10032, USA.
出版信息
Br J Pharmacol. 2007 Aug;151(7):909-11. doi: 10.1038/sj.bjp.0707299. Epub 2007 Jun 4.
Abstract
The pharmaceutical industry is testing new potential drugs for their propensity to prolong human cardiac repolarization, and regards this as a sign of proarrhythmic risk. Many studies have dethroned the common perception that prolonged repolarization is a reliable surrogate marker for torsades de pointes (TdP) arrhythmia. Both the pharmaceutical industry and the regulatory bodies are neglecting the available proarrhythmia models. In vitro studies have suggested that combined pharmacological hits on repolarization will produce a superior substrate for in vivo proarrhythmia, compared to the single-drug assessment. By using consecutive pharmacological challenges, a simple model is proposed, in which combinatorial pharmacology is employed to provoke TdP in the conscious dog. The pharmaceutical industry interested in evaluating the proarrhythmic potential of their present and future drugs now has a simple means of doing so.
摘要
制药行业正在测试新的潜在药物延长人类心脏复极的倾向,并将此视为致心律失常风险的一个迹象。许多研究已推翻了长期以来的一种普遍观念,即复极延长是尖端扭转型室速(TdP)心律失常的可靠替代标志物。制药行业和监管机构都在忽视现有的致心律失常模型。体外研究表明,与单一药物评估相比,对复极进行联合药理学干预会为体内致心律失常产生更优的底物。通过连续进行药理学挑战,提出了一个简单的模型,其中采用组合药理学在清醒犬中诱发TdP。现在,有意评估其现有和未来药物致心律失常潜力的制药行业有了一种简单的方法来做到这一点。
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