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乙醇的首过代谢主要发生在胃部。

First-pass metabolism of ethanol is predominantly gastric.

作者信息

Lim R T, Gentry R T, Ito D, Yokoyama H, Baraona E, Lieber C S

机构信息

Alcohol Research and Treatment Center, Bronx Veterans Affairs Medical Center, NY 10468.

出版信息

Alcohol Clin Exp Res. 1993 Dec;17(6):1337-44. doi: 10.1111/j.1530-0277.1993.tb05250.x.

Abstract

Oral consumption of alcohol results in much lower blood alcohol concentrations (BACs) than does the same dose administered intravenously, suggesting significant first-pass metabolism (FPM). The questions remain, however, (1) whether this difference truly represents FPM or simply reflects slower absorption of alcohol, and (2) if there is FPM, is it mainly of gastric or hepatic origin. To study this, rats were given the same dose alcohol (1 g/kg) by either intragastric intubation or by intravenous, intraportal, and intraduodenal infusions at a rate that mimicked the loss of alcohol from the stomach. Higher BAC levels after intravenous than intragastric alcohol indicated true FPM. Higher levels after intraportal or intraduodenal infusions (in fact, comparable to those obtained with the intravenous route) demonstrated negligible FPM when the route of delivery bypassed the stomach, yet included the liver. Furthermore, rats that had developed portosystemic shunts after ligation of the portal ven exhibited blood alcohol curves and FPM equivalent to those of sham-operated controls, indicating that FPM is not dependent on first-pass flow through the liver, but reflects gastric metabolism. The absence of significant hepatic FPM is attributable to the saturation of hepatic alcohol dehydrogenase by recirculating alcohol, resulting in no appreciable increase in metabolism secondary to newly absorbed alcohol. Finally, the in vivo gastric metabolism of alcohol in pylorus-ligated rats was demonstrated by significantly lower BACs when alcohol was administered intragastrically than when an amount identical to that lost from the ligated stomach was given intraportally. Thus, the lower BACs with oral as opposed to intravenous alcohol are not simply a consequence of slow absorption, but result from FPM occurring predominantly in the stomach.

摘要

经口摄入酒精所导致的血液酒精浓度(BACs)远低于静脉注射相同剂量酒精所导致的浓度,这表明存在显著的首过代谢(FPM)。然而,问题仍然存在:(1)这种差异是真的代表首过代谢,还是仅仅反映了酒精吸收较慢;(2)如果存在首过代谢,其主要起源于胃还是肝脏。为了研究这一点,给大鼠经胃插管或通过静脉、门静脉和十二指肠输注给予相同剂量的酒精(1 g/kg),输注速率模拟酒精从胃中的损失情况。静脉注射酒精后比经胃给予酒精后的BAC水平更高,表明存在真正的首过代谢。当给药途径绕过胃但包括肝脏时,门静脉或十二指肠输注后更高的水平(实际上,与静脉途径获得的水平相当)表明首过代谢可忽略不计。此外,在门静脉结扎后形成门体分流的大鼠,其血液酒精曲线和首过代谢与假手术对照组相当,这表明首过代谢不依赖于通过肝脏的首过血流,而是反映了胃代谢。肝脏首过代谢不显著是由于再循环酒精使肝脏乙醇脱氢酶饱和,导致新吸收酒精继发的代谢没有明显增加。最后,幽门结扎大鼠经胃给予酒精时的BACs显著低于经门静脉给予与结扎胃中损失量相同的酒精时的BACs,这证明了酒精在体内的胃代谢。因此,与静脉注射酒精相比,口服酒精时较低的BACs不仅仅是吸收缓慢的结果,而是主要发生在胃中的首过代谢的结果。

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