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Using Chimeric Mice with Humanized Livers to Predict Human Drug Metabolism and a Drug-Drug Interaction

机译:使用具有人源化肝脏的嵌合小鼠预测人的药物代谢和药物相互作用

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摘要

Interspecies differences in drug metabolism have made it difficult to use preclinical animal testing data to predict the drug metabolites or potential drug-drug interactions (DDIs) that will occur in humans. Although chimeric mice with humanized livers can produce known human metabolites for test substrates, we do not know whether chimeric mice can be used to prospectively predict human drug metabolism or a possible DDI. Therefore, we investigated whether they could provide a more predictive assessment for clemizole, a drug in clinical development for the treatment of hepatitis C virus (HCV) infection. Our results demonstrate, for the first time, that analyses performed in chimeric mice can correctly identify the predominant human drug metabolite before human testing. The differences in the rodent and human pathways for clemizole metabolism were of importance, because the predominant human metabolite was found to have synergistic anti-HCV activity. Moreover, studies in chimeric mice also correctly predicted that a DDI would occur in humans when clemizole was coadministered with a CYP3A4 inhibitor. These results demonstrate that using chimeric mice can improve the quality of preclinical drug assessment.
机译:物种间的新陈代谢差异使得难以使用临床前动物试验数据来预测将在人类中发生的药物代谢物或潜在的药物-药物相互作用(DDI)。尽管具有人源化肝脏的嵌合小鼠可以产生已知的人代谢产物作为测试底物,但我们不知道嵌合小鼠是否可用于前瞻性预测人的药物代谢或可能的DDI。因此,我们调查了他们是否可以对克列咪唑(一种用于治疗丙型肝炎病毒(HCV)感染的临床开发中的药物)提供更具预测性的评估。我们的结果首次证明在嵌合小鼠中进行的分析可以在进行人体测试之前正确地识别出主要的人类药物代谢产物。啮齿动物和人类克米唑代谢途径的差异是重要的,因为发现主要的人类代谢产物具有协同的抗HCV活性。此外,在嵌合小鼠中的研究还正确地预测了当克立咪唑与CYP3A4抑制剂共同给药时,DDI会在人体内发生。这些结果表明,使用嵌合小鼠可以提高临床前药物评估的质量。

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