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使用静脉注射和口服咪达唑仑时CYP3A活性的性别差异。

Sex differences in CYP3A activity using intravenous and oral midazolam.

作者信息

Chen Maylee, Ma Lei, Drusano George L, Bertino Joseph S, Nafziger Anne N

机构信息

Ordway Research Institute Drug Development Center, Albany, NY 12206-1066, USA.

出版信息

Clin Pharmacol Ther. 2006 Nov;80(5):531-8. doi: 10.1016/j.clpt.2006.08.014.

Abstract

BACKGROUND

Studies examining sex differences in CYP3A activity have produced conflicting results. Our objective is to investigate whether sex differences exist in CYP3A activity as assessed by intravenous (IV) or oral midazolam pharmacokinetic analysis in healthy volunteers.

METHODS

Data from 13 previous studies were used. A single dose of IV midazolam (0.025 mg/kg) was administered to 66 white adults (37 women and 29 men; mean age, 36.3+/-7.7 years). A single dose of oral midazolam, 0.075 mg/kg (5 studies), 0.15 mg/kg (1 study), or 5 mg (1 study), was administered to 72 adults (71 white and 1 Asian; 37 women and 35 men; mean age, 38.3+/-8.9 years). Pharmacokinetic parameters were determined via population methods by use of a nonparametric adaptive grid program and a 2-compartment IV and 1-compartment oral absorption model. The maximum a posteriori probability Bayesian method was used to estimate each subject's pharmacokinetic parameters. Monte Carlo simulation was performed to determine the probability distribution of the area under the concentration-time curves (AUCs).

RESULTS

Women exhibited 11% higher mean weight-corrected total body midazolam clearance and 28% higher oral clearance compared with men (P<or=.01). The median AUC of IV midazolam was 0.05 mg.h/L (range, 0.02-0.14 mg.h/L) in women and 0.06 mg.h/L (range, 0.02-0.14 mg.h/L) in men. The median AUC of oral midazolam was 0.11 mg.h/L (range, 0.02-0.60 mg.h/L) in women and 0.12 mg.h/L (range, 0.04-0.45 mg.h/L) in men.

CONCLUSIONS

Although women showed significantly greater hepatic and intestinal CYP3A activity, only a minor sex difference in AUC was noted. Therefore the observed disparity may be of negligible clinical importance.

摘要

背景

关于细胞色素P450 3A(CYP3A)活性性别差异的研究结果相互矛盾。我们的目的是通过对健康志愿者静脉注射(IV)或口服咪达唑仑的药代动力学分析,研究CYP3A活性是否存在性别差异。

方法

使用之前13项研究的数据。对66名白人成年人(37名女性和29名男性;平均年龄36.3±7.7岁)静脉注射单剂量咪达唑仑(0.025mg/kg)。对72名成年人(71名白人、1名亚洲人;37名女性和35名男性;平均年龄38.3±8.9岁)口服单剂量咪达唑仑,剂量分别为0.075mg/kg(5项研究)、0.15mg/kg(1项研究)或5mg(1项研究)。通过群体方法,使用非参数自适应网格程序以及二室静脉注射和一室口服吸收模型确定药代动力学参数。采用最大后验概率贝叶斯方法估计每个受试者的药代动力学参数。进行蒙特卡洛模拟以确定浓度-时间曲线下面积(AUC)的概率分布。

结果

与男性相比,女性体重校正后的咪达唑仑总体清除率平均高11%,口服清除率高28%(P≤0.01)。女性静脉注射咪达唑仑的AUC中位数为0.05mg·h/L(范围0.02 - 0.14mg·h/L),男性为0.06mg·h/L(范围0.02 - 0.14mg·h/L)。女性口服咪达唑仑的AUC中位数为0.11mg·h/L(范围0.02 - 0.60mg·h/L),男性为0.12mg·h/L(范围0.04 - 0.45mg·h/L)。

结论

虽然女性的肝脏和肠道CYP3A活性明显更高,但仅观察到AUC存在微小的性别差异。因此,观察到的差异在临床上可能无足轻重。

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