首页> 美国卫生研究院文献>AAPS PharmSci >In Vitro Evaluation of Reversible and Irreversible Cytochrome P450 Inhibition: Current Status on Methodologies and their Utility for Predicting Drug–Drug Interactions
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In Vitro Evaluation of Reversible and Irreversible Cytochrome P450 Inhibition: Current Status on Methodologies and their Utility for Predicting Drug–Drug Interactions

机译:可逆和不可逆细胞色素P450抑制的体外评估:方法学的现状及其在预测药物相互作用中的作用

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摘要

It is widely accepted that today’s practice of polypharmacy inevitably increases the incidence of drug–drug interactions (DDIs). Serious DDI is a major liability for any new chemical entity (NCE) entering the pharmaceutical market. As such, pharmaceutical companies employ various strategies to avoid problematic compounds for clinical development. A key cause for DDIs is the inhibition of cytochrome P450 enzymes (CYPs) that are responsible for metabolic clearance of many drugs. Screening for inhibition potency of CYPs by NCEs has therefore become a routine practice during the drug discovery stage. However, in order to make proper use of DDI data, an understanding of the strengths and weaknesses of the various experimental systems in current use is required. An illustrated review of experimental practices is presented with discussion of likely future developments. The combination of high quality in vitro data generation and the application of in vivo CYP inhibition modelling approaches should allow more informed decisions to be made in the search for drug molecules with acceptable DDI characteristics.
机译:人们普遍认为,当今的多药店做法不可避免地会增加药物与药物相互作用(DDI)的发生率。对于任何进入制药市场的新化学实体(NCE),严重的DDI都是主要责任。因此,制药公司采用各种策略来避免有问题的化合物用于临床开发。 DDI的主要原因是抑制细胞色素P450酶(CYP),而这些酶负责清除许多药物。因此,在药物发现阶段,通过NCE筛选CYP的抑制能力已成为常规操作。但是,为了正确使用DDI数据,需要了解当前使用的各种实验系统的优缺点。给出了对实验方法的图解说明,并讨论了可能的未来发展。高质量的体外数据生成和体内CYP抑制建模方法的应用相结合,应该可以在寻找具有可接受的DDI特征的药物分子时做出更明智的决定。

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