摘要
用麻醉犬研究美托洛尔(Met)光学异构体药动学—药效学结合模型。结果表明,ig(+)Met或(-)Met后,其药动学符合二室模型,药动学参数Vd/F,CLs/F和AUC在两种Met之间有显著性差异。(+)Met和(-)Met的效应和血药浓度关系呈逆时针滞后环。引入效应室理论后,药效和效应室浓度之间的关系符合SigmoidEmax模型。应用CAPP软件进行模型拟合,血药浓度的预测值和药效的预测值皆与其实测值较为接近。(+)Met抑制Vmax,dp/dtmax及HR效应的Ce50分别是(-)Met的37,68,63倍,证实(-)Met对犬心脏的抑制作用强于(+)Met。
The PK PD model of (+) Met and (-) Met was studied in anesthetized dogs. The plasma drug concentration time profiles were most adequately described by two compartment model. Significant differences of V d/ F , CL s/ F and AUC between (+) Met and (-) Met were observed. The peak times of plasma (+) Met and (-) Met concentration in dogs were 24±5 and 30±5 min, respectively. But the peak times of drug inhibitory effects on V max , d p /d t max , LVSP, SBP and HR were about 90~120 min, showing the hysteresis loops. When using the effect compartment model, the counterclock wise hysteresis collapsed and the relationships between the effects and concentration in effect compartment were fit by using Sigmoid E max model. The C e 50 values of inhibitory effects on V max , d p /d t max and HR of (+) Met were 250±80, 450±210, 520±210 μg·L -1 and those of (-) Met were 70±30, 70±40 and 82±27 μg·L -1 , respectively. Significant differences of C e 50 of (+) Met and (-) Met were found. The values of C e 50+ / C e 50- were 3 7, 6 8 and 6 3, indicating that the inhibitory effects on V max , d p /d t max and HR of (-) Met were stronger than those of (+) Met in dogs.
出处
《药学学报》
CAS
CSCD
北大核心
1997年第6期411-415,共5页
Acta Pharmaceutica Sinica
基金
国家自然科学基金
