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异烟肼的临床药代动力学

Clinical pharmacokinetics of isoniazid.

作者信息

Weber W W, Hein D W

出版信息

Clin Pharmacokinet. 1979 Nov-Dec;4(6):401-22. doi: 10.2165/00003088-197904060-00001.

Abstract

The pharmacokinetics of isoniazid in man are described. Pronounced interindividual variation in circulating isoniazid concentration and clearance which occur after dosing with the drug are associated with hereditary differences in the acetylator status. The variations in rate of isoniazid inactivation and elimination in different (rapid and slow) acetylator phenotypes are primarily due to differences in the rate of acetylation of isoniazid by a genetically controlled polymorphic N-acetyltransferase in liver and small intestine. An appreciable 'first-pass' effect is observed following oral isoniazid administration, particularly in the rapid acetylator phenotype. Liver disease can cause a significant prolongation in the clearance of isoniazid; in the acutely ill patient, the prolongation correlates most closely with serum bilirubin elevation, although the degree of prolongation is less important than the intrinsic genetic difference between acetylator phenotypes. The effect of renal impairment on isoniazid excretion is relatively unimportant, even in slow acetylators. Methods for monitoring blood and urine concentrations of isoniazid and for acetylator phenotype determination which are convenient for the patient and clinician are available. Implications of phenotype differences in acetylator status for the optimal management of tuberculosis with isoniazid are considered. Attempts to devise new isoniazid formulations for this purpose are being evaluated.

摘要

本文描述了异烟肼在人体内的药代动力学。给药后,循环中异烟肼浓度和清除率存在明显的个体间差异,这与乙酰化状态的遗传差异有关。不同(快乙酰化和慢乙酰化)乙酰化表型中异烟肼失活和消除速率的差异,主要是由于肝脏和小肠中由基因控制的多态性N - 乙酰转移酶对异烟肼的乙酰化速率不同。口服异烟肼后可观察到明显的“首过”效应,在快乙酰化表型中尤为明显。肝脏疾病可导致异烟肼清除率显著延长;在急性病患者中,清除率延长与血清胆红素升高最密切相关,尽管延长程度不如乙酰化表型之间的内在遗传差异重要。肾功能损害对异烟肼排泄的影响相对较小,即使在慢乙酰化者中也是如此。已有方便患者和临床医生的监测异烟肼血药浓度和尿药浓度以及测定乙酰化表型的方法。文中还考虑了乙酰化状态的表型差异对异烟肼治疗结核病最佳方案的影响。目前正在评估为此目的设计新的异烟肼制剂的尝试。

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