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肝硬化会显著损害美西律的消除。

Cirrhosis of the liver markedly impairs the elimination of mexiletine.

作者信息

Pentikäinen P J, Hietakorpi S, Halinen M O, Lampinen L M

出版信息

Eur J Clin Pharmacol. 1986;30(1):83-8. doi: 10.1007/BF00614201.

Abstract

To study the effects of cirrhosis of the liver on the pharmacokinetics of mexiletine a single i.v. dose of 200 mg was administered to six cirrhotic patients and to six healthy controls. The distribution of mexiletine in both study groups was similar, as indicated by similar values of V1 and Vss, but it tended to occur more slowly in the cirrhotics. The plasma protein binding of mexiletine was unchanged in the patients with cirrhosis. The elimination of mexiletine was markedly retarded in the cirrhotics, as indicated by its lower total clearance (2.31 vs. 8.27 ml/kg/h,) lower total elimination rate constant (0.059 vs 0.353 h-1), and longer elimination half-life (28.7 vs 9.9 h). The antipyrine half-life was 38.3 h in the patients and 14.7 h in the controls. One healthy volunteer had a Morgagni-Stokes-Adams type of syncopal attack 5 min after administration of mexiletine due to disturbance of AV conduction induced by the drug. Thus, on a pharmacokinetic basis the loading dose of mexiletine need not be modified in cirrhotic patients, whereas the maintenance dosage should be reduced to one fourth - one third of the usual dose.

摘要

为研究肝硬化对美西律药代动力学的影响,对6例肝硬化患者和6例健康对照者静脉注射200mg单剂量美西律。两个研究组中美西律的分布相似,表现为V1和Vss值相近,但在肝硬化患者中其分布过程往往较慢。肝硬化患者中美西律的血浆蛋白结合率未发生改变。肝硬化患者中美西律的消除明显延迟,表现为其总清除率较低(2.31对8.27ml/kg/h)、总消除速率常数较低(0.059对0.353h-1)以及消除半衰期较长(28.7对9.9h)。患者中安替比林半衰期为38.3h,对照者中为14.7h。一名健康志愿者在注射美西律后5分钟因药物引起的房室传导紊乱发生了莫加尼-斯托克斯-亚当斯型晕厥发作。因此,基于药代动力学,肝硬化患者中美西律的负荷剂量无需调整,而维持剂量应减至常用剂量的四分之一至三分之一。

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