食物对多剂量口服伏立康唑药代动力学的影响。
Effect of food on the pharmacokinetics of multiple-dose oral voriconazole.
作者信息
Purkins Lynn, Wood Nolan, Kleinermans Diane, Greenhalgh Katie, Nichols Don
机构信息
Pfizer Global Research and Development, Sandwich, Kent CT13 9NJ, UK.
出版信息
Br J Clin Pharmacol. 2003 Dec;56 Suppl 1(Suppl 1):17-23. doi: 10.1046/j.1365-2125.2003.01994.x.
AIMS
Voriconazole is a new triazole antifungal agent with activity against a range of clinically important and emerging pathogens. This study determined the effect of food on the pharmacokinetics of voriconazole in healthy volunteers.
METHODS
This was an open, randomized, two-way crossover, multiple-dose study in male volunteers. Twelve subjects received voriconazole 200 mg twice daily for 6.5 days. Each dose was administered either with food or in the fasted state, i.e. not within 2 h of food. Treatment periods were separated by a minimum 7-day washout period. Plasma samples were taken for the estimation of voriconazole plasma concentrations on days 1 and 7. Safety and toleration were assessed by monitoring of both laboratory safety tests and adverse events.
RESULTS
Administering voriconazole with food significantly decreased both day 7 AUCtau and Cmax by approximately 35% (9598-7520 ng.h ml-1; P = 0.003) and 22% (2038-1332 ng ml-1; P = 0.008), respectively. Administering voriconazole with food statistically significantly delayed absorption, evident from tmax values; the mean difference for tmax on day 7 was 1.1 h. The terminal phase rate constant was unchanged by administering voriconazole with food. The fasted terminal phase half-life was 7.3 h compared with 6.6 h for the fed state. Visual inspection of Cmin values suggests that steady state was achieved after 5 days in both dietary states. Voriconazole accumulation, as assessed by ratios of Cmax and AUCtau on days 1 and 7, was statistically significantly greater when administered with food (Cmax, P = 0.010, AUCtau, P = 0.006). Mean Cmax accumulation in the fasted state was 2.1-fold compared with 3.5-fold in the fed state. AUCtau accumulation in the fasted state was 3.1-fold compared with 4.2-fold in the fed state. There were no discontinuations due to adverse events or laboratory abnormalities. Treatment-related mild-to-moderate visual disturbances were experienced by six out of 12 subjects.
CONCLUSIONS
The bioavailability of twice-daily 200 mg voriconazole is reduced by approximately 22% as measured by AUCtau after multiple dosing when taken with food, compared with fasting.
目的
伏立康唑是一种新型三唑类抗真菌药物,对一系列临床上重要的和新出现的病原体具有活性。本研究确定了食物对伏立康唑在健康志愿者体内药代动力学的影响。
方法
这是一项针对男性志愿者的开放、随机、双向交叉、多剂量研究。12名受试者每天两次服用200mg伏立康唑,共6.5天。每次给药要么与食物同服,要么处于禁食状态,即不在进食后2小时内。治疗期之间至少有7天的洗脱期。在第1天和第7天采集血浆样本以估计伏立康唑的血浆浓度。通过监测实验室安全测试和不良事件来评估安全性和耐受性。
结果
与食物同服伏立康唑显著降低了第7天的AUCtau和Cmax,分别约降低了35%(从9598降至7520 ng·h/ml;P = 0.003)和22%(从2038降至1332 ng/ml;P = 0.008)。从tmax值可明显看出,与食物同服伏立康唑在统计学上显著延迟了吸收;第7天tmax的平均差异为1.1小时。与食物同服伏立康唑对终末相速率常数无影响。禁食状态下的终末相半衰期为7.3小时,而进食状态下为6.6小时。通过观察Cmin值表明,在两种饮食状态下5天后均达到稳态。根据第1天和第7天的Cmax和AUCtau比值评估,与食物同服伏立康唑时的蓄积在统计学上显著更高(Cmax,P = 0.010;AUCtau,P = 0.006)。禁食状态下的平均Cmax蓄积为2.1倍,而进食状态下为3.5倍。禁食状态下的AUCtau蓄积为3.1倍,而进食状态下为4.2倍。没有因不良事件或实验室异常而停药的情况。12名受试者中有6名经历了与治疗相关的轻度至中度视觉障碍。
结论
与禁食相比,多次给药后,以AUCtau衡量,每天两次服用200mg伏立康唑时,与食物同服其生物利用度降低约22%。
Zotero 插件