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A general pharmacodynamic interaction model identifies perpetrators and victims in drug interactions

机译:一个通用的药效相互作用模型可以识别药物相互作用中的犯罪者和受害者

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Assessment of pharmacodynamic (PD) drug interactions is a cornerstone of the development of combination drug therapies. To guide this venture, we derive a general pharmacodynamic interaction (GPDI) model for ≥2 interacting drugs that is compatible with common additivity criteria. We propose a PD interaction to be quantifiable as multidirectional shifts in drug efficacy or potency and explicate the drugs’ role as victim, perpetrator or even both at the same time. We evaluate the GPDI model against conventional approaches in a data set of 200 combination experiments in Saccharomyces cerevisiae: 22% interact additively, a minority of the interactions (11%) are bidirectional antagonistic or synergistic, whereas the majority (67%) are monodirectional, i.e., asymmetric with distinct perpetrators and victims, which is not classifiable by conventional methods. The GPDI model excellently reflects the observed interaction data, and hence represents an attractive approach for quantitative assessment of novel combination therapies along the drug development process.
机译:药效学(PD)药物相互作用的评估是联合药物疗法发展的基石。为了指导这项事业,我们针对≥2种相互作用的药物推导出了通用药效学相互作用(GPDI)模型,该模型与常见的加性标准兼容。我们认为,PD相互作用可量化为药物功效或效能的多向转移,并同时阐明药物作为受害者,作案者或什至两者的作用。我们在酿酒酵母(Saccharomyces cerevisiae)的200个组合实验的数据集中评估了GPDI模型与传统方法的对比:22%的相互作用是加性相互作用,少数相互作用(11%)是双向拮抗或协同作用,而大多数(67%)是单向相互作用,即不对称,有不同的犯罪者和受害者,这是传统方法无法分类的。 GPDI模型可以很好地反映观察到的相互作用数据,因此代表了一种在药物开发过程中定量评估新型联合疗法的有吸引力的方法。

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