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静脉注射硝酸异山梨酯的药代动力学

Pharmacokinetics of intravenous isosorbide-dinitrate.

作者信息

Platzer R, Reutemann G, Galeazzi R L

出版信息

J Pharmacokinet Biopharm. 1982 Dec;10(6):575-86. doi: 10.1007/BF01062541.

DOI:10.1007/BF01062541
PMID:7182455
Abstract

The kinetics of isosorbide dinitrate (ISDN) after i.v. administration and the absolute availability of an oral slow release preparation (SR) were studied in young healthy volunteers. ISDN and the 2- and 5-mononitrates of isosorbide (2-MN, 5-MN) were determined by GLC. After i.v. administration plasma levels of ISDN declined biexponentially and could be adequately described by an open two compartment body model. Distribution half-life was extremely rapid (2-5 min). Terminal disappearance had a half-life of 67 (62-75) min (mean, range). Total plasma clearance was 1.6 (1.2-2.2) litres X min-1, thus approaching liver blood flow. Nevertheless, absolute systemic availability (F) or oral ISDN amounted to 22% (16-29%). Assuming that oral ISDN is completely absorbed and blood levels do not exceed serum levels, an upper limit of hepatic clearance (liver blood flow 1.5 litres X min-1 X (1-F/100)) can be estimated, which is significantly smaller (p less than 0.05) than the measured clearance. This finding is best interpreted by assuming that ISDN is partly eliminated by extrahepatic routes, which is further substantiated by a different pattern of metabolites after i.v. and oral dosing. Whereas after i.v. administration more 2-MN is produced, 5-MN is the main metabolite after oral ISDN. Since the glutathione-S-transferases are found in the cytosol of most cells, it seems likely that other organs than the liver contribute to the metabolism of ISDN.

摘要

在年轻健康志愿者中研究了静脉注射硝酸异山梨酯(ISDN)后的动力学以及口服缓释制剂(SR)的绝对生物利用度。通过气相色谱法测定ISDN及其异山梨醇的2-和5-单硝酸盐(2-MN,5-MN)。静脉注射后,ISDN的血浆水平呈双指数下降,可用开放二室模型充分描述。分布半衰期极快(2-5分钟)。终末消除半衰期为67(62-75)分钟(平均值,范围)。总血浆清除率为1.6(1.2-2.2)升×分钟⁻¹,接近肝血流量。然而,口服ISDN的绝对全身生物利用度(F)为22%(16-29%)。假设口服ISDN完全吸收且血药水平不超过血清水平,可估算肝清除率上限(肝血流量1.5升×分钟⁻¹×(1-F/100)),该值明显小于实测清除率(p<0.05)。这一发现最好解释为ISDN部分通过肝外途径消除,静脉注射和口服给药后代谢产物模式不同进一步证实了这一点。静脉注射后产生更多的2-MN,而口服ISDN后5-MN是主要代谢产物。由于谷胱甘肽-S-转移酶存在于大多数细胞的胞质溶胶中,除肝脏外的其他器官似乎也参与了ISDN的代谢。

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本文引用的文献

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Pharmacokinetics of isosorbide dinitrate and its mononitrate metabolites after intravenous infusion.静脉输注后硝酸异山梨酯及其单硝酸代谢产物的药代动力学
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