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肝硬化患者中镇痛药的生物利用度提高且清除率降低。

Enhanced bioavailability and decreased clearance of analgesics in patients with cirrhosis.

作者信息

Neal E A, Meffin P J, Gregory P B, Blaschke T F

出版信息

Gastroenterology. 1979 Jul;77(1):96-102.

PMID:447033
Abstract

The effect of moderate cirrhosis on the bioavailability and systemic clearance of three model analgesic compounds (pethidine, pentazocine, and salicylamide) with substantial first-pass metabolism was examined in 8 cirrhotic subjects and 4 agematched healthy controls. There was a 46% decrease in the clearance of pentazocine and a 278% increase in bioavailability. The corresponding figures for pethidine were 36% and 81%. The area under the plasma curve after oral salicylamide was increased by 551% in cirrhotic subjects compared with controls. This study demonstrated that drugs with the highest hepatic clearance will have the largest relative increases in bioavailability in cirrhotic patients due to portosystemic shunting. The decrease in clearance and increase in bioavailability will have multiplicative, rather than simply additive, effects on total area under the curve and, if related, pharmacologic response.

摘要

在8名肝硬化患者和4名年龄匹配的健康对照者中,研究了中度肝硬化对三种具有显著首过代谢的模型镇痛化合物(哌替啶、喷他佐辛和水杨酰胺)生物利用度和全身清除率的影响。喷他佐辛的清除率降低了46%,生物利用度增加了278%。哌替啶的相应数字分别为36%和81%。与对照组相比,肝硬化患者口服水杨酰胺后的血浆曲线下面积增加了551%。这项研究表明,由于门体分流,肝清除率最高的药物在肝硬化患者中的生物利用度相对增加幅度最大。清除率的降低和生物利用度的增加对曲线下总面积以及(如有关的话)药理反应将产生相乘而非简单相加的效应。

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