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Characterization of cytochrome P450-mediated drug metabolism in cats

机译:猫中细胞色素P450介导的药物代谢的表征

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In this study we examined activities of cytochrome P450 (CYP)1A, 2C, 2D and 3A using hepatic microsomes from five male and five female cats. CYP1A, 2C, 2D and 3A activities were referred by ethoxyresorufin O-deethylation (EROD), tolbutamide hydroxylation (TBH), bufuralol 1'-hydroxylation (BLH) and midazolam 1'- and 4-hydroxylation respectively. The anti-rat CYP1A2 and CYP3A2 serum significantly inhibited EROD and midazolam 1'- and 4-hydroxylation, suggesting that EROD and midazolam 1'- and 4-hydroxylation were catalysed by CYP1A and 3A in cats respectively. Quinidine inhibited BLH in cats microsomes at quite low concentrations, suggesting that BLH was catalysed by CYP2D in cats. Tolbutamide hydroxylation activities were negligible in hepatic microsomes from both male and female cats, suggesting CYP2C activities of cats are extremely low. This suggests that CYP2C substrates should be carefully administered to cats. Although there is no sexual difference in CYP1A activities, there are differences in CYP2D and 3A activities of cats. CYP2D activities were higher (3-fold), but CYP3A activities were lower (one-fifth) in female cats. These results might suggest that CYP2D and 3A substrates should be prescribed for male and female cats using different dosage regimen.
机译:在这项研究中,我们使用来自五只雄性和五只雌性猫的肝微粒体检查了细胞色素P450(CYP)1A,2C,2D和3A的活性。 CYP1A,2C,2D和3A的活性分别通过乙氧基间苯二酚的O-脱乙基化(EROD),甲苯磺丁酰胺羟化(TBH),布法洛尔1'-羟基化(BLH)和咪达唑仑1'-和4-羟基化来表示。抗大鼠CYP1A2和CYP3A2血清显着抑制EROD和咪达唑仑1'-和4-羟基化,表明EROD和咪达唑仑1'-和4-羟基化分别由猫中的CYP1A和3A催化。奎尼丁在猫微粒体中以极低的浓度抑制BLH,这表明CYP2D在猫中催化BLH。在雄性和雌性猫的肝微粒体中,甲苯磺丁酰胺的羟化活性微不足道,表明猫的CYP2C活性极低。这表明CYP2C底物应谨慎用于猫。尽管CYP1A活性没有性别差异,但猫的CYP2D和3A活性也存在差异。在雌性猫中,CYP2D活性较高(3倍),但CYP3A活性较低(五分之一)。这些结果可能提示应使用不同的剂量方案为雄性和雌性猫开具CYP2D和3A底物。

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