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哌替啶在人体中的胃和胆汁排泄。

Gastric and biliary excretion of meperidine in man.

作者信息

Dunkerley R, Johnson R, Schenker S, Wilkinson G R

出版信息

Clin Pharmacol Ther. 1976 Nov;20(5):546-51. doi: 10.1002/cpt1976205546.

Abstract

The role and importance of enterogastric secretion in the disposition and elimination of the weak base, meperidine (pKa 8.63), was studied after intravenous administration (50 mg) of the drug to 6 normal volunteers. Continuous collection of the gastric fluid over a 4-hr period demonstrated the establishment of high gastric fluid/plasma concentration ratios for meperidine (mean about 50, range, 10 to 200). However, the total amount of drug recovered, even after correction for incomplete collection, was only a small percentage of the administered dose. Under basal conditions a mean +/- SE of 1.9 +/- 0.3 mg, equivalent to 3.7% of the administered dose, was found in the total gastric aspirate. Stimulation of gastric secretion by subcutaneous injection of betazole (1.5 mg/kg) increased this recovery to 3.6 +/- 0.3 mg (7.2%) primarily due to the increase in gastric volumen output. Aspiration of the gastric fluid in either the basal or stimulated situation had no observable effect upon the plasma concentration/time profile of meperidine whether assessed by the terminal half-life, t 1/2 beta, or the plasma clearance; control values were 3.8 +/- hr and 1,190 +/- 130 ml/min, respectively. In 2 subjects "bile fluid" was also collected for 2.5 hr and found to contain less than 0.2% of the administered dose. Enterosystemic recycling is therefore of minor importance in the disposition and elimination of meperidine in man.

摘要

在给6名正常志愿者静脉注射(50毫克)哌替啶(pKa 8.63)后,研究了肠胃分泌在这种弱碱药物的处置和消除过程中的作用及重要性。在4小时内持续收集胃液,结果显示哌替啶的胃液/血浆浓度比很高(平均约为50,范围为10至200)。然而,即使校正了收集不完全的情况,回收的药物总量也仅占给药剂量的一小部分。在基础条件下,在总的胃液抽吸物中发现平均±标准误为1.9±0.3毫克,相当于给药剂量的3.7%。皮下注射倍他唑(1.5毫克/千克)刺激胃液分泌后,回收量增加到3.6±0.3毫克(7.2%),这主要是由于胃液分泌量增加所致。无论是在基础状态还是刺激状态下抽吸胃液,对哌替啶的血浆浓度/时间曲线均未观察到明显影响,无论通过终末半衰期t 1/2β还是血浆清除率来评估;对照值分别为3.8±小时和1190±130毫升/分钟。在2名受试者中,还收集了2.5小时的“胆汁液”,发现其中含有的药物不到给药剂量的0.2%。因此,肠肝循环在人体哌替啶的处置和消除过程中不太重要。

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