Scheer Nico, McLaughlin Lesley A, Rode Anja, Macleod A Kenneth, Henderson Colin J, Wolf C Roland
TaconicArtemis, Köln, Germany (N.S., A.R.); and Medical Research Institute, University of Dundee, Ninewells Hospital and Medical School, University of Dundee, Dundee, United Kingdom (L.A.M., A.K.M., C.J.H., C.R.W.).
Drug Metab Dispos. 2014 Jun;42(6):1022-30. doi: 10.1124/dmd.114.057885. Epub 2014 Mar 26.
In humans, 75% of all drugs are metabolized by the cytochrome P450-dependent monooxygenase system. Enzymes encoded by the CYP2C, CYP2D, and CYP3A gene clusters account for ∼80% of this activity. There are profound species differences in the multiplicity of cytochrome P450 enzymes, and the use of mouse models to predict pathways of drug metabolism is further complicated by overlapping substrate specificity between enzymes from different gene families. To establish the role of the hepatic and extrahepatic P450 system in drug and foreign chemical disposition, drug efficacy, and toxicity, we created a unique mouse model in which 30 cytochrome P450 genes from the Cyp2c, Cyp2d, and Cyp3a gene clusters have been deleted. Remarkably, despite a wide range of putative important endogenous functions, Cyp2c/2d/3a KO mice were viable and fertile, demonstrating that these genes have evolved primarily as detoxification enzymes. Although there was no overt phenotype, detailed examination showed Cyp2c/2d/3a KO mice had a smaller body size (15%) and larger livers (20%). Changes in hepatic morphology and a decreased blood glucose (30%) were also noted. A five-drug cocktail of cytochrome P450 isozyme probe substrates were used to evaluate changes in drug pharmacokinetics; marked changes were observed in either the pharmacokinetics or metabolites formed from Cyp2c, Cyp2d, and Cyp3a substrates, whereas the metabolism of the Cyp1a substrate caffeine was unchanged. Thus, Cyp2c/2d/3a KO mice provide a powerful model to study the in vivo role of the P450 system in drug metabolism and efficacy, as well as in chemical toxicity.
在人类中,所有药物的75%由细胞色素P450依赖性单加氧酶系统代谢。CYP2C、CYP2D和CYP3A基因簇编码的酶约占该活性的80%。细胞色素P450酶的多样性存在显著的物种差异,并且不同基因家族的酶之间底物特异性重叠使得利用小鼠模型预测药物代谢途径变得更加复杂。为了确定肝脏和肝外P450系统在药物和外来化学物质处置、药物疗效及毒性方面的作用,我们创建了一种独特的小鼠模型,其中来自Cyp2c、Cyp2d和Cyp3a基因簇的30个细胞色素P450基因已被删除。值得注意的是,尽管有一系列假定的重要内源性功能,Cyp2c/2d/3a基因敲除小鼠仍能存活且可育,这表明这些基因主要进化为解毒酶。虽然没有明显的表型,但详细检查显示Cyp2c/2d/3a基因敲除小鼠体型较小(15%)且肝脏较大(20%)。还注意到肝脏形态的变化以及血糖降低(30%)。使用细胞色素P450同工酶探针底物的五药混合物来评估药物药代动力学的变化;在Cyp2c、Cyp2d和Cyp3a底物的药代动力学或形成的代谢产物中观察到显著变化,而Cyp1a底物咖啡因的代谢未改变。因此,Cyp2c/2d/3a基因敲除小鼠为研究P450系统在药物代谢、疗效以及化学毒性方面的体内作用提供了一个有力的模型。
