奈非那韦的单剂量和多剂量药代动力学以及慢性肝病的人类免疫缺陷病毒感染患者的CYP2C19活性
Single and multiple dose pharmacokinetics of nelfinavir and CYP2C19 activity in human immunodeficiency virus-infected patients with chronic liver disease.
作者信息
Khaliq Y, Gallicano K, Seguin I, Fyke K, Carignan G, Bulman D, Badley A, Cameron D W
机构信息
Clinical Investigation Unit, Ottawa Hospital Research Institute, Ontario, Canada.
出版信息
Br J Clin Pharmacol. 2000 Aug;50(2):108-15. doi: 10.1046/j.1365-2125.2000.00238.x.
AIMS
To evaluate the single-dose and multiple-dose pharmacokinetics of nelfinavir and its active M8 metabolite in eight HIV-seropositive patients with liver disease, and to examine the relationship between CYP2C19 activity (genotype and plasma M8/nelfinavir metabolic ratio) and the severity of liver disease in these patients.
METHODS
Nelfinavir was given as a single dose (500 or 750 mg) to patients beginning therapy and twice (500, 750 or 1000 mg) or three times (250 or 750 mg) daily during chronic therapy. Single-dose pharmacokinetic values were used to predict multiple-dose regimens. Peak and total plasma exposures between 2-4 microg ml-1 and 45-75 microg ml-1 h, respectively, and predose levels > 0.7 microg ml-1 were targeted for multidose nelfinavir. Genotype was determined by analysis for CYP2C191, CYP2C192, and CYP2C19*3. Individuals were grouped according to their genotype, molar M8/nelfinavir AUC ratio (low: < 0.1, intermediate: 0.1-0.3, high > 0.3), and Child-Pugh classification for severity of liver disease.
RESULTS
Nelfinavir pharmacokinetics were characterized by wide interindividual variability, low clearance (181-496 ml min-1 70 kg-1, n = 7), and prolonged half-life (5-20 h, n = 7). M8/nelfinavir AUC ratio increased 58% (n = 4) and alpha 1-acid glycoprotein levels decreased up to 39% (n = 5) from single to multiple dosing. CYP2C19 activity was low (metabolic AUC ratio < 0.1) in four patients with moderate to severe liver disease even though they were genetically extensive CYP2C19 metabolizers (*1/*1 or *1/*2). Three patients required lower daily doses than the standard regimen of 750 mg every 8 h to achieve target concentrations and maintain virologic suppression at < 50 RNA copies ml-1 (up to 20 months).
CONCLUSIONS
Acquired CYP2C19 deficiency from moderate or severe liver disease resulted in decreased M8 formation. Long-term HIV suppression is possible using low nelfinavir doses in patients with liver disease.
目的
评估奈非那韦及其活性代谢产物M8在8例HIV血清反应阳性的肝病患者中的单剂量和多剂量药代动力学,并研究这些患者中CYP2C19活性(基因型和血浆M8/奈非那韦代谢比)与肝病严重程度之间的关系。
方法
开始治疗时给予患者单剂量奈非那韦(500或750mg),慢性治疗期间每日两次(500、750或1000mg)或每日三次(250或750mg)。单剂量药代动力学值用于预测多剂量方案。多剂量奈非那韦的目标是分别使2 - 4μg/ml和45 - 75μg/ml·h之间的血浆峰浓度和总暴露量,以及给药前水平>0.7μg/ml。通过分析CYP2C191、CYP2C192和CYP2C19*3来确定基因型。个体根据其基因型、M8/奈非那韦AUC摩尔比(低:<0.1,中:0.1 - 0.3,高>0.3)以及肝病严重程度的Child - Pugh分类进行分组。
结果
奈非那韦药代动力学的特征是个体间差异大、清除率低(181 - 496ml·min⁻¹·70kg⁻¹,n = 7)和半衰期延长(5 - 20h,n = 7)。从单剂量给药到多剂量给药,M8/奈非那韦AUC比增加了58%(n = 4),α1 - 酸性糖蛋白水平下降了39%(n = 5)。4例中度至重度肝病患者的CYP2C19活性较低(代谢AUC比<0.1),尽管他们在基因上是CYP2C19广泛代谢者(*1/1或1/*2)。3例患者需要的每日剂量低于每8小时750mg的标准方案,以达到目标浓度并将病毒载量维持在<50 RNA拷贝/ml(长达20个月)。
结论
中度或重度肝病导致的获得性CYP2C19缺乏导致M8生成减少。对于肝病患者,使用低剂量奈非那韦有可能实现长期的HIV抑制。
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