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首页> 外文期刊>Xenobiotica: the fate of foreign compounds in biological systems >Comparison of the hepatic metabolism of triazolam in wild-type andCyp3a-knockout mice for understanding CYP3A-mediated metabolism inCYP3A-humanised mice in vivo
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Comparison of the hepatic metabolism of triazolam in wild-type andCyp3a-knockout mice for understanding CYP3A-mediated metabolism inCYP3A-humanised mice in vivo

机译:在野生型和诊断小鼠中进行三唑仑肝脏代谢的比较,以了解CYP3A介导的代谢INCYP3A-人育小鼠体内

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摘要

1. To investigate cytochrome P450 3A (CYP3A)-mediated metabolism in vivo, plasma concentrations of triazolam (TRZ) are often monitored as a CYP3A marker in CYP3A-humanised mice. However, it has not been determined whether plasma concentrations of TRZ after intravenous administration can reflect hepatic CYP3A activity in CYP3A-humanised mice. 2. Firstly, we investigated the pharmacokinetics of TRZ in wild-type and Cyp3a-knockout (Cyp3a-KO) mice. Plasma concentration profiles of TRZ and alpha-hydroxy (OH) TRZ were very similar in wild-type and Cyp3a-KO mice. On the other hand, AUC of 4-OH TRZ in Cyp3a-KO mice was significantly lower than that in wild-type mice. Pregnenolone 16 alpha-carbonitrile (PCN) decreased the areas under the plasma concentration-time curves (AUCs) of TRZ and alpha-OH TRZ in both groups. There was no significant effect of PCN on AUC of 4-OH TRZ in Cyp3a-KO mice. 3. Next, we verified that AUC of 4-OH TRZ in CYP3A-humanised mice was higher than that in Cyp3a-KO mice, although the difference was not significant. 4. In conclusion, plasma concentrations of 4-OH TRZ, but not those of TRZ and alpha-OH TRZ, might reflect hepatic CYP3A activity in mice in vivo. These results provide important insights for in vivo studies using a CYP3A-humanised model.
机译:1.研究细胞色素P450 3A(CYP3A)介导的体内代谢,经常监测三唑仑(TRZ)的血浆浓度作为CYP3A-人源化小鼠的CYP3A标志物。然而,尚未确定静脉内给药后TRZ的血浆浓度是否可以反映CYP3A-人源化小鼠的肝CYP3A活性。首先,我们研究了野生型和CYP3A敲除(CYP3A-KO)小鼠中TRZ的药代动力学。 TRZ和α-羟基(OH)TRZ的血浆浓度谱在野生型和CYP3A-KO小鼠中非常相似。另一方面,CYP3A-KO小鼠中4-OH TRZ的AUC显着低于野生型小鼠。孕烯醇龙16α-碳腈(PCN)在两组中降低TRZ和α-OH TRZ的血浆浓度 - 时间曲线(AUC)下的区域。 CYP3A-Ko小鼠AUC的4-OH TRZ对4-OH TRZ的显着影响。 3.接下来,我们核实CYP3A-人源化小鼠4-OH TRZ的AUC高于CYP3A-KO小鼠的4-OH TRZ,尽管差异并不重要。结果总之,4-OH TRZ的血浆浓度,但不是TRZ和α-OH TRZ的血浆浓度可能反映体内小鼠中的肝CYP3A活性。这些结果提供了使用CYP3A人化模型的体内研究的重要见解。

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