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Dealing with hERG liabilities early: diverse approaches to an important goal in drug development

机译:尽早处理hERG债务:实现药物开发重要目标的多种方法

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摘要

In drug development, early recognition of a potential for blocking the human ether-a-go-go related gene (hERG) channels is perhaps the best way to avoid later disappointment when QT interval prolongation shows up in clinical trials. Knowledge of the hERG blocking liability offers the chance to modify the molecule to reduce, or even eliminate, this unwanted activity and lack of success in such modification is a good reason to stop further development of the molecule. In this issue of the BJP, different methods for early detection of hERG channel blocking liability are discussed by Pollard et al. One attractive approach is widespread screening of molecules at a very early stage of research to detect compounds with this liability and thereby eliminate them. There are now several methodologies available that offer hERG channel testing on a high-throughput format but entail a diverse selection of direct and indirect readouts of hERG channel blocking activity and all are subject to practical limitations that also need to be considered prior to investing in a particular experimental approach. The approach selected, if any, should reflect the resources and expertise available. In any case, it is essential to be aware of the experimental limitations and potential inaccuracies that are inherent to each approach.This article is a commentary on Pollard et al., pp. 12–21 of this issue and is part of a themed section on QT safety. To view this issue visit
机译:在药物开发中,当QT间隔延长在临床试验中显示出来时,尽早识别潜在的阻断人类以太相关基因(hERG)通道的可能是避免以后失望的最好方法。对hERG阻断责任的了解为修饰分子以减少甚至消除这种不想要的活性提供了机会,并且在这种修饰中缺乏成功是阻止分子进一步发展的良好理由。在本期BJP中,Pollard等人讨论了用于早期检测hERG通道阻滞性的不同方法。一种有吸引力的方法是在研究的早期阶段广泛筛选分子,以检测具有这种责任的化合物,从而消除它们。现在,有几种方法可以以高通量格式提供hERG通道测试,但需要选择直接和间接读出hERG通道阻滞活性的多种方法,所有这些方法都有实际的局限性,因此在投资于eERG之前必须考虑这些限制。特殊的实验方法。选择的方法(如果有)应反映可用的资源和专业知识。无论如何,必须意识到每种方法固有的实验局限性和潜在的不准确性。本文是对Pollard等人的评论,第12至21页,是主题部分的一部分。关于QT安全性。要查看此问题,请访问

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