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首页> 美国卫生研究院文献>Springer Open Choice >Physiologically Based Pharmacokinetic Modelling of Cytochrome P450 2C9-Related Tolbutamide Drug Interactions with Sulfaphenazole and Tasisulam
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Physiologically Based Pharmacokinetic Modelling of Cytochrome P450 2C9-Related Tolbutamide Drug Interactions with Sulfaphenazole and Tasisulam

机译:细胞色素P450 2C9相关的甲苯磺丁酰胺药物与磺胺苯并噻唑仑相互作用的生理基础药代动力学模型

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Background and ObjectivesCytochrome P450 2C9 (CYP2C9) is involved in the biotransformation of many commonly used drugs, and significant drug interactions have been reported for CYP2C9 substrates. Previously published physiologically based pharmacokinetic (PBPK) models of tolbutamide are based on an assumption that its metabolic clearance is exclusively through CYP2C9; however, many studies indicate that CYP2C9 metabolism is only responsible for 80–90% of the total clearance. Therefore, these models are not useful for predicting the magnitude of CYP2C9 drug–drug interactions (DDIs). This paper describes the development and verification of SimCYP®-based PBPK models that accurately describe the human pharmacokinetics of tolbutamide when dosed alone or in combination with the CYP2C9 inhibitors sulfaphenazole and tasisulam.
机译:背景与目的细胞色素P450 2C9(CYP2C9)参与了许多常用药物的生物转化,并且据报道CYP2C9底物具有显着的药物相互作用。先前发表的甲苯磺丁酰胺基于生理的药代动力学(PBPK)模型基于以下假设:其代谢清除率仅通过CYP2C9;但是,许多研究表明,CYP2C9代谢仅占总清除率的80–90%。因此,这些模型对于预测CYP2C9药物-药物相互作用(DDI)的程度没有用。本文描述了基于SimCYP ®的PBPK模型的开发和验证,该模型准确描述了单独或与CYP2C9抑制剂磺胺苯并噻唑和他克苏仑合用时甲苯磺丁胺的人药代动力学。

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