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基于模型的结核分枝杆菌和 HIV 合并感染患者异烟肼药代动力学和代谢变异性评估:对新型给药方案的启示。

Model-Based Assessment of Variability in Isoniazid Pharmacokinetics and Metabolism in Patients Co-Infected With Tuberculosis and HIV: Implications for a Novel Dosing Strategy.

机构信息

Unit for Pharmacokinetics and Drug Metabolism, Department of Pharmacology, Sahlgrenska Academy at University of Gothenburg, Gothenburg, Sweden.

Department of Pharmacy, School of Medicine and Pharmacy, University of Rwanda, Kigali, Rwanda.

出版信息

Clin Pharmacol Ther. 2020 Jul;108(1):73-80. doi: 10.1002/cpt.1806. Epub 2020 Mar 2.

DOI:10.1002/cpt.1806
PMID:32017035
Abstract

Tuberculosis is the most common cause of death in HIV-infected patients. Isoniazid is used as a first-line drug to treat tuberculosis infection. However, variability in isoniazid pharmacokinetics can result in hepatotoxicity or treatment failure. Determination of clinical factors affecting isoniazid pharmacokinetics and metabolic pathways in HIV co-infected patients is therefore critical. Plasma levels of isoniazid, acetyl-isoniazid, and isonicotinic acid from 63 patients co-infected with tuberculosis and HIV were analyzed by liquid chromatography with tandem mass spectrometry followed by nonlinear mixed-effects modeling. Patients were genotyped to determine acetylator status. Patients were either on concomitant efavirenz-based antiretroviral therapy or HIV treatment naïve. Clearances of isoniazid were 1.3-fold and 2.3-fold higher in intermediate and rapid acetylators, respectively, compared with slow acetylators. Patients on concomitant efavirenz-based antiretroviral therapy had 64% and 80% higher population predicted clearances of acetyl-isoniazid and isonicotinic acid, respectively, compared with patients who were HIV treatment naïve. Both sex and CD4 cell count affected the bioavailability of isoniazid. Variability in isoniazid exposure could be reduced by dose adaptions based on acetylator type and sex in addition to the currently used weight bands. A novel dosing strategy that has the potential to reduce isoniazid-related toxicity and treatment failure is presented.

摘要

结核病是 HIV 感染者中最常见的死亡原因。异烟肼被用作治疗结核病感染的一线药物。然而,异烟肼药代动力学的可变性可能导致肝毒性或治疗失败。因此,确定 HIV 合并感染患者影响异烟肼药代动力学和代谢途径的临床因素至关重要。通过液相色谱-串联质谱法对 63 例结核和 HIV 合并感染患者的血浆异烟肼、乙酰异烟肼和烟碱酸水平进行分析,并采用非线性混合效应模型进行分析。对患者进行基因分型以确定乙酰化状态。患者要么正在接受依非韦伦为基础的抗逆转录病毒治疗,要么是 HIV 初治。与慢乙酰化者相比,中速和快速乙酰化者的异烟肼清除率分别高出 1.3 倍和 2.3 倍。正在接受依非韦伦为基础的抗逆转录病毒治疗的患者,其乙酰异烟肼和烟碱酸的群体预测清除率分别比 HIV 初治患者高出 64%和 80%。性别和 CD4 细胞计数均影响异烟肼的生物利用度。除了目前使用的体重带外,根据乙酰化类型和性别进行剂量调整,可以降低异烟肼暴露的可变性。提出了一种新的给药策略,有可能降低异烟肼相关毒性和治疗失败的风险。

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