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人及大鼠肝脏、肺、肾和肠切片的药物代谢活性。

Drug-metabolizing activity of human and rat liver, lung, kidney and intestine slices.

作者信息

De Kanter R, De Jager M H, Draaisma A L, Jurva J U, Olinga P, Meijer D K F, Groothuis G M M

机构信息

Groningen University Institute for Drug Exploration, Department Pharmacokinetics & Drug Delivery, Ant. Deusinglaan 1, 9713 AV Groningen, The Netherlands.

出版信息

Xenobiotica. 2002 May;32(5):349-62. doi: 10.1080/00498250110112006.

Abstract
  1. Organ-specific biotransformation was studied in human and rat liver, lung, kidney and small intestine slices and compared on a protein basis, using four model substances. 2. Deethylation of lidocaine was highest in liver slices from both man and rat, followed by the small intestine. 3. Metabolism of testosterone was highest in liver slices, but a different overall metabolic pattern was found between the different organs. 4. Lung, kidney and intestine slices prepared from human and rat organs showed mainly an unknown metabolite of 7-ethoxycoumarin identified as 4-ethoxy-2-hydroxyphenyl propionic acid (EPPA). 5. The maximal metabolism of 7-ethoxycoumarin in slices was equal with in vivo V(max) in the rat. 6. Phase II metabolism of 7-hydroxycoumarin in kidney and intestinal slices was about 60% of the activity in liver slices. 7. In conclusion, organs other than the liver show a surprisingly high drug-metabolizing activity. Thus, the use of precision-cut slices of a combination of drug metabolizing organs in an in vitro test system from both animal and human origin is required for a proper systematic prediction of drug metabolism in man.
摘要
  1. 使用四种模型物质,在人及大鼠的肝、肺、肾和小肠切片中研究了器官特异性生物转化,并在蛋白质基础上进行了比较。2. 利多卡因的脱乙基作用在人和大鼠的肝切片中最高,其次是小肠。3. 睾酮的代谢在肝切片中最高,但不同器官之间发现了不同的总体代谢模式。4. 从人和大鼠器官制备的肺、肾和肠切片主要显示出7-乙氧基香豆素的一种未知代谢物,鉴定为4-乙氧基-2-羟基苯丙酸(EPPA)。5. 切片中7-乙氧基香豆素的最大代谢与大鼠体内的V(max)相等。6. 肾和肠切片中7-羟基香豆素的II相代谢约为肝切片中活性的60%。7. 总之,肝脏以外的器官显示出惊人的高药物代谢活性。因此,为了对人体药物代谢进行适当的系统预测,需要在来自动物和人类的体外测试系统中使用药物代谢器官组合的精密切片。

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