通过两种特异性酶免疫测定法测定依那普利和依那普利拉后，健康志愿者中马来酸依那普利的药代动力学和药效学特征。

Pharmacokinetics and pharmacodynamics profiles of enalapril maleate in healthy volunteers following determination of enalapril and enalaprilat by two specific enzyme immunoassays.

作者信息

Arafat T, Awad R, Hamad M, Azzam R, Al-Nasan A, Jehanli A, Matalka K

机构信息

Faculty of Pharmacy and Medical Technology, University of Petra, Amman, Jordan.

出版信息

J Clin Pharm Ther. 2005 Aug;30(4):319-28. doi: 10.1111/j.1365-2710.2005.00646.x.

DOI:10.1111/j.1365-2710.2005.00646.x

PMID:15985045

Abstract

BACKGROUND AND OBJECTIVES

Most of the pharmacokinetic (PK) parameters for enalapril and enalaprilat were established following determination of the drug and its metabolite, using angiotensin converting enzyme (ACE) inhibition assays. In these methods, enalapril has to be hydrolysed to enalaprilat first and then assayed. The purpose of this study was to re-estimate the PK parameters of enalapril and enalaprilat in healthy volunteers using two specific enzyme immunoassays for enalapril and enalaprilat.

METHODS

The rate and extent of absorption of enalapril and enalaprilat from a 10-mg dose of two enalapril maleate commercial brands (Renetic and Enalapril) were estimated using a two-way-cross over design with 1-week washout period. Blood pressure was also measured at specified time intervals and correlated to enalaprilat plasma concentrations.

RESULTS

For enalapril, the AUC(o-->infinity) values (Mean+/-SD) were 450.0+/-199.5 and 479.6+/-215.6 ng h/mL, Cmax values were 313.5+/-139.6 and 310.1+/-186.6 ng/mL, Tmax values were 1.06+/-0.30 h and 1.13+/-0.22 h, and t1/2 ranged between 0.3 to 6.1 h (1.6+/-1.5) and 0.40 to 5.05 h (1.3+/-1.0), for the two brands. For enalaprilat, the AUC(o-->infinity) values were 266.9+/-122.7 and 255.9+/-121.8 ng h/ml, Cmax values were 54.8+/-29.5 and 57.2+/-29.0 ng/mL, Tmax values were 4.6+/-1.6 h and 4.3+/-1.45 h, and t1/2 ranged between 1.1 to 10.5 h (4.5+/-2.9) and 0.6 to 9.4 h (3.5+/-2.5) for the two brands.

CONCLUSIONS

Cmax values for enalapril are about 10 times those published in the literature and the rate and extent of absorption of the two brands of enalapril and their deesterification to enalaprilat following the administration of either brand were bioequivalent. Secondly, enalaprilat concentrations at 12-24 h following a single oral dose of enalapril in healthy volunteers were lower than those reported in the literature. The values reported here correlated with the return of blood pressure to predose level. Thirdly, enzyme immunoassays for enalapril and enalaprilat are better than ACE inhibition assays and can be used in bioequivalence assessment of enalapril and enalaprilat and for therapeutic drug monitoring in a clinical laboratory setting.

摘要

背景与目的

依那普利和依那普利拉的大多数药代动力学（PK）参数是在使用血管紧张素转换酶（ACE）抑制试验测定药物及其代谢物之后确定的。在这些方法中，依那普利必须先水解为依那普利拉，然后进行测定。本研究的目的是使用两种针对依那普利和依那普利拉的特异性酶免疫测定法，重新估算健康志愿者中依那普利和依那普利拉的PK参数。

方法

采用两交叉设计，洗脱期为1周，估算了两种马来酸依那普利商业品牌（Renetic和Enalapril）10mg剂量中依那普利和依那普利拉的吸收速率和程度。还在特定时间间隔测量血压，并将其与依那普利拉血浆浓度相关联。

结果

对于依那普利，两个品牌的AUC（o→∞）值（均值±标准差）分别为450.0±199.5和479.6±215.6 ng·h/mL，Cmax值分别为313.5±139.6和310.1±186.6 ng/mL，Tmax值分别为1.06±0.30 h和1.13±0.22 h，t1/2范围在0.3至6.1 h（1.6±1.5）和0.40至5.05 h（1.3±1.0）之间。对于依那普利拉，两个品牌的AUC（o→∞）值分别为266.9±122.7和255.9±121.8 ng·h/ml，Cmax值分别为54.8±29.5和57.2±29.0 ng/mL，Tmax值分别为4.6±1.6 h和4.3±1.45 h，t1/2范围在1.1至10.5 h（4.5±2.9）和0.6至9.4 h（3.5±2.5）之间。

结论

依那普利的Cmax值约为文献报道值的10倍，两种品牌的依那普利及其给药后去酯化为依那普利拉的吸收速率和程度具有生物等效性。其次，健康志愿者单次口服依那普利后12 - 24小时的依那普利拉浓度低于文献报道值。此处报告的值与血压恢复到给药前水平相关。第三，依那普利和依那普利拉的酶免疫测定法优于ACE抑制试验，可用于依那普利和依那普利拉的生物等效性评估以及临床实验室环境中的治疗药物监测。