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CYP2D-related metabolism in animals of the Canoidea superfamily - species differences.

机译:CYP2D相关的CAM2D类动物中的代谢物种 - 物种差异。

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CYP2D-related drug metabolism in liver microsomes from animals of the Canoidea super family, i.e. mink (Mustela vison), bears (Ursus arctos), foxes (Vulpes vulpes) and dogs, were investigated. Propranolol, bunitrolol and imipramine, which are typically substrates of CYP2D subfamilies, were used in the experiment. All the animals of the Canoidea superfamily that were tested lacked the ability to catalyse 7-hydroxylation of propranolol, which is one of the major metabolic pathways in rats. Stereoselectivity of propranolol metabolism was towards (S)-propranolol in all the reactions of the animals tested with the exception of mink, which showed a selective tendency towards (R)-propranolol in N-dealkylation. As far as metabolic patterns of (R)- and (S)-propranolol are concerned, bears, foxes and dogs are alike, but minks are somewhat different. Liver microsomes from mink showed, among the animals of the Canoidea superfamily, the lowest propranolol hydroxylase activity at 4- and 5-positions and imipramine 2-hydroxylation and {N-}demethylation activities. We could not detect bunitrolol 4-hydroxylation in mink liver microsomes at the low substrate concentration used. We conclude that mink have the lowest activity of CYP2D-related xenobiotic metabolism among the Canoidea superfamily..
机译:研究了Cyp2D相关药物代谢来自动物超级家庭动物的肝微粒体,即Mink(Mustela Vison),熊(Ursus Arctos),狐狸(狐狸狐狸)和狗。在实验中使用了通常是Cyp2D亚壳的底物的普萘洛尔,Bunitrool和Inagramine。测试的所有动物的所有物质都缺乏催化普萘洛醇的7-羟基化的能力,这是大鼠的主要代谢途径之一。普萘洛尔代谢的立体选择性朝向(S) - 在用貂皮中检测的所有反应中的产丙醇,这表明在N-Deawhation中朝向(R) - 丙二醇醇的选择性趋势。至于(R)的代谢模式 - 和(s) - 普罗拉洛尔担心,熊,狐狸和狗都是相似的,但水貂有点不同。来自水貂的肝微粒体显示,在CAIoidea超家族的动物中,在4-和5-位和脂氧化的最低普萘洛醇羟化酶活性和脂氧化的2-羟基化和{N-}去甲基化活性。在所用的低底物浓度下,我们无法检测在水貂肝微粒体中的少硝基4-羟基化。我们得出结论,水貂在Cyp2D相关的外胚层代谢中具有最低的CYP2D相关的异教代谢。

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