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大鼠体内α-羟孕酮的代谢:通过肝脏混合功能氧化酶系统的降解速率限制麻醉效果的证据。

Metabolism of alphaxalone in the rat: evidence for the limitation of the anaesthetic effect by the rate of degradation through the hepatic mixed function oxygenase system.

作者信息

Sear J W, McGivan J D

出版信息

Br J Anaesth. 1981 Apr;53(4):417-24. doi: 10.1093/bja/53.4.417.

Abstract

The rates of degradation of the steroid anaesthetic alphaxalone (3 alpha-OH-5 alpha pregnane-11,20 dione) have been studied in vitro using isolated hepatocyte and microsome preparations. Evidence is presented that alphaxalone is metabolized rapidly by the hepatic mixed function oxygenase system. Induction of cytochrome P450 in vivo leads to an increase in the maximum rate of degradation of alphaxalone in both in vitro systems. Induction of cytochrome P450 caused a decrease in the duration of the anaesthetic affect in vivo of a limiting dose of Althesin (alphaxalone/alphadolone acetate). It is concluded that, under certain conditions, the duration of the anaesthetic effect of alphaxalone is determined by the rate of metabolism of this compound by the mixed function oxygenase system of the liver.

摘要

已使用分离的肝细胞和微粒体制剂在体外研究了甾体麻醉剂α-羟孕酮(3α-羟基-5α-孕烷-11,20-二酮)的降解速率。有证据表明,α-羟孕酮可被肝脏混合功能氧化酶系统快速代谢。体内细胞色素P450的诱导导致两种体外系统中α-羟孕酮的最大降解速率增加。细胞色素P450的诱导导致有限剂量的阿尔泰辛(α-羟孕酮/醋酸阿法多龙)在体内的麻醉作用持续时间缩短。得出的结论是,在某些条件下,α-羟孕酮的麻醉作用持续时间取决于该化合物被肝脏混合功能氧化酶系统代谢的速率。

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