新型广谱抗真菌药静脉注射伏立康唑的药代动力学及安全性
The pharmacokinetics and safety of intravenous voriconazole - a novel wide-spectrum antifungal agent.
作者信息
Purkins Lynn, Wood Nolan, Greenhalgh Katie, Eve Malcolm D, Oliver Stuart D, 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):2-9. doi: 10.1046/j.1365-2125.2003.01992.x.
AIMS
Voriconazole is a new triazole with broad-spectrum antifungal activity against clinically significant and emerging pathogens. These studies evaluated the pharmacokinetics and safety of intravenous voriconazole in healthy male volunteers.
METHODS
Two single-blind, placebo-controlled studies were conducted. In Study A, 12 subjects were randomized to voriconazole (3 mg kg-1) or placebo, administered once daily on days 1 and 12, and every 12 h on days 3-11. In Study B, 18 subjects were randomized to voriconazole or placebo, with voriconazole being administered as a loading dose at 6 mg kg-1 twice on day 1, then at 3 mg kg-1 twice daily on days 2-9, and once at 3 mg kg-1 on day 10.
RESULTS
In both studies, the plasma concentrations of voriconazole increased rapidly following the initiation of dosing. Minimum observed plasma concentration (Cmin) values at steady state were above the in vitro minimum inhibitory concentrations (MICs) for most fungal pathogens (Cmin > 0.8 micro g ml-1). The use of a loading dose in Study B resulted in a shorter time to steady-state Cmin values than was observed in Study A. Values of the final day plasma pharmacokinetic parameters in Studies A and B were similar: maximum observed plasma concentration (Cmax) 3621 and 3063 ng ml-1; areas under the plasma concentration-time curve from time zero to the end of the dosing interval (AUCtau) 16 535 and 13 245 ng.h ml-1, and terminal elimination phase half-lives (t1/2) 6.5 and 6.7 h, respectively. On multiple dosing, voriconazole accumulated (AUCtau accumulation ratio 2.53-3.17, Study A) at a level that was not predictable from single-dose data. The mean concentration-time profiles for voriconazole in saliva were similar to those in plasma. Multiple doses of voriconazole were well tolerated and no subject discontinued from either study. Seven cases of possibly drug-related visual disturbance were reported in three subjects (Study B).
CONCLUSIONS
Administration of a loading dose of 6 mg kg-1 i.v. voriconazole on the first day of treatment followed by 3 mg kg-1 i.v. twice daily achieves steady state by the third day of dosing. This dosage regimen results in plasma levels of the drug that rapidly exceed the minimum inhibitory concentrations (MICs) against important fungal pathogens, including Aspergillus spp.
目的
伏立康唑是一种新型三唑类药物,对临床上重要的和新出现的病原体具有广谱抗真菌活性。这些研究评估了静脉注射伏立康唑在健康男性志愿者中的药代动力学和安全性。
方法
进行了两项单盲、安慰剂对照研究。在研究A中,12名受试者被随机分为伏立康唑组(3mg/kg)或安慰剂组,在第1天和第12天每日给药1次,在第3 - 11天每12小时给药1次。在研究B中,18名受试者被随机分为伏立康唑组或安慰剂组,伏立康唑在第1天以6mg/kg的负荷剂量静脉注射两次,然后在第2 - 9天每日两次以3mg/kg静脉注射,在第10天以3mg/kg静脉注射1次。
结果
在两项研究中,给药开始后伏立康唑的血浆浓度迅速升高。稳态时观察到的最低血浆浓度(Cmin)值高于大多数真菌病原体的体外最低抑菌浓度(MICs)(Cmin > 0.8μg/ml)。研究B中使用负荷剂量导致达到稳态Cmin值的时间比研究A中观察到的时间短。研究A和B中最后一天血浆药代动力学参数的值相似:观察到的最大血浆浓度(Cmax)分别为3621和3063ng/ml;从给药间隔开始到结束的血浆浓度 - 时间曲线下面积(AUCtau)分别为16535和13245ng·h/ml,以及终末消除相半衰期(t1/2)分别为6.5和6.7小时。多次给药时,伏立康唑会蓄积(AUCtau蓄积比2.53 - 3.17,研究A),其蓄积水平无法从单剂量数据预测。伏立康唑在唾液中的平均浓度 - 时间曲线与血浆中的相似。多次剂量的伏立康唑耐受性良好,两项研究中均无受试者退出。在3名受试者中报告了7例可能与药物相关的视觉障碍(研究B)。
结论
在治疗的第一天静脉注射6mg/kg的伏立康唑负荷剂量,随后每日两次静脉注射3mg/kg,在给药第三天达到稳态。这种给药方案导致药物的血浆水平迅速超过针对重要真菌病原体(包括曲霉菌属)的最低抑菌浓度(MICs)。
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