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迈向基于机制的体内药效学药物-药物相互作用分析

Towards a mechanism-based analysis of pharmacodynamic drug-drug interactions in vivo.

作者信息

Jonker Daniël M, Visser Sandra A G, van der Graaf Piet H, Voskuyl Rob A, Danhof Meindert

机构信息

Division of Pharmacology, Leiden/Amsterdam Center for Drug Research, Leiden University, P.O. Box 9502, 2300 RA, Leiden, The Netherlands.

出版信息

Pharmacol Ther. 2005 Apr;106(1):1-18. doi: 10.1016/j.pharmthera.2004.10.014. Epub 2004 Dec 23.

Abstract

The combination of drugs is a common practice for enhancing the efficiency of drug treatment, but selection of the optimal combination and the optimal doses remains a matter of trial and error. Prediction of synergistic, additive and antagonistic responses to drug combinations in vivo is therefore of considerable interest. The present review discusses the application of mathematical and statistical models to assess combined drug action by response surface modelling. The most commonly applied models are designed to distinguish between synergistic and additive responses on the basis of a single parameter to indicate whether a drug combination acts synergistic or not. It is, however, recognized that these relatively simple models often do not adequately describe complex drug interactions. This has led to the application of increasingly complex models with multiple drug interaction parameters that can describe a wide range of synergistic and antagonistic responses in a single-response surface. The capability to describe response surfaces with high resolution offers the opportunity to develop an understanding of the mechanisms that underlie the observed combined drug response. Operational models for drug interaction constitute a highly versatile framework for mechanism-based modelling by taking the signal transduction properties of the drug combination into account. On this basis, it is predicted that the occurrence of synergism is favoured by convergence of drug signals late in the signal transduction pathway as opposed to proximal convergence. Furthermore, a high efficiency of signal transduction poses in general a barrier to the occurrence of synergism. The in vivo application of operational models with advanced response surface modelling techniques will facilitate the rational development of synergistic drug combinations.

摘要

联合用药是提高药物治疗效果的常见做法,但选择最佳联合用药方案和最佳剂量仍然需要反复试验。因此,预测体内药物联合使用时的协同、相加和拮抗反应备受关注。本综述讨论了通过响应面建模应用数学和统计模型来评估联合用药作用。最常用的模型旨在基于单一参数区分协同和相加反应,以表明药物组合是否具有协同作用。然而,人们认识到这些相对简单的模型往往不能充分描述复杂的药物相互作用。这导致了应用越来越复杂的具有多个药物相互作用参数的模型,这些模型可以在单一响应面上描述广泛的协同和拮抗反应。以高分辨率描述响应面的能力为深入了解观察到的联合用药反应背后的机制提供了机会。药物相互作用的操作模型通过考虑药物组合的信号转导特性,构成了基于机制建模的高度通用框架。在此基础上,预测信号转导途径后期药物信号的汇聚有利于协同作用的发生,而不是近端汇聚。此外,一般来说,高效的信号转导对协同作用的发生构成障碍。将操作模型与先进的响应面建模技术应用于体内,将有助于合理开发协同药物组合。

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