严重肝硬化患者中吗啡的代谢及生物利用度
The metabolism and bioavailability of morphine in patients with severe liver cirrhosis.
作者信息
Hasselström J, Eriksson S, Persson A, Rane A, Svensson J O, Säwe J
机构信息
Department of Clinical Pharmacology, Karolinska Institute, Uppsala, Sweden.
出版信息
Br J Clin Pharmacol. 1990 Mar;29(3):289-97. doi: 10.1111/j.1365-2125.1990.tb03638.x.
Abstract
- The oral and intravenous kinetics of morphine were investigated in seven cirrhotic patients with a history of encephalopathy. The plasma concentrations of morphine and its metabolites morphine-3 (M3G) and morphine-6 (M6G) were measured by h.p.l.c. 2. The mean terminal elimination half-life of morphine was 4.2 h (95% CI 3.6-4.8) the mean volume of distribution was 4.1 l kg-1 (95% CI 2.9-5.4) and the mean plasma clearance was 11.4 ml min-1 kg-1 (95% CI 8.1-14.7). The mean oral bioavailability was 101% (95% CI 56-147). 3. The plasma clearance of morphine was significantly lower, its terminal elimination half-life longer and its oral bioavailability greater in the cirrhotic patients compared with patients with normal liver function. The metabolic ratio M3G/morphine was significantly lower in the cirrhotic patients than in control subjects after oral dosing, but did not differ after intravenous dosing. 4. The average urinary recoveries of morphine plus M3G and M6G were 49.9% after i.v. and 57.7% after oral administration. There were no statistically significant differences in the urinary recovery between the two routes of administration or between the cirrhotic patients and controls. 5. Specific changes in the EEG pattern could not be detected after intravenous dosage. 6. The metabolism of morphine is impaired significantly in patients with severe cirrhosis. Clinically important findings were a high oral bioavailability and a long elimination half-life. These findings call for cautious dosing of oral and intravenous morphine in patients with severe end stage liver disease.
摘要
- 对7名有脑病病史的肝硬化患者的吗啡口服及静脉动力学进行了研究。采用高效液相色谱法测定血浆中吗啡及其代谢产物吗啡-3(M3G)和吗啡-6(M6G)的浓度。2. 吗啡的平均终末消除半衰期为4.2小时(95%可信区间3.6 - 4.8),平均分布容积为4.1升/千克(95%可信区间2.9 - 5.4),平均血浆清除率为11.4毫升/分钟/千克(95%可信区间8.1 - 14.7)。平均口服生物利用度为101%(95%可信区间56 - 147)。3. 与肝功能正常的患者相比,肝硬化患者的吗啡血浆清除率显著降低,其终末消除半衰期更长,口服生物利用度更高。口服给药后,肝硬化患者的代谢比M3G/吗啡显著低于对照组,但静脉给药后无差异。4. 静脉注射后吗啡加M3G和M6G的平均尿回收率为49.9%,口服给药后为57.7%。两种给药途径之间或肝硬化患者与对照组之间的尿回收率无统计学显著差异。5. 静脉给药后未检测到脑电图模式的特异性变化。6. 严重肝硬化患者的吗啡代谢明显受损。临床上重要的发现是口服生物利用度高和消除半衰期长。这些发现要求对晚期肝病患者谨慎使用口服和静脉注射吗啡。
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