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地高辛毒苷的肝清除率:兔离体肝脏的药代动力学研究。蛋白结合的影响及与地高辛的比较。

Hepatic clearance of gitoxin: pharmacokinetic study on rabbit isolated liver. Influence of protein binding and comparison with digoxin.

作者信息

Pellegrin P, Lesne M

出版信息

Eur J Drug Metab Pharmacokinet. 1983;8(1):1-8. doi: 10.1007/BF03189574.

Abstract

Hepatic clearance of gitoxin has been studied in the rabbit and compared with that of digoxin using an isolated perfused liver technique. During 1.5 hour perfusions with a modified Krebs-Henseleit solution, gitoxin perfusate levels decreased biexponentially; the distribution and elimination half-lives were estimated to be 0.14 and 1.25 hour, Vd area to be 95.5 ml.g-1 and intrinsic metabolic clearance to be 1.98 ml.min-1.g-1. During 1.5 hour perfusions with modified Krebs-Henseleit solution containing 2.7% bovine serum albumin, gitoxin perfusate levels decreased monoexponentially. This is probably due to protein binding which moderates hepatic uptake so that distribution is not yet complete after 1.5 hour and it is therefore impossible to discriminate the two phases. This was confirmed by 5 hour perfusion experiments with an emulsion of perfluorocarbon in the modified Krebs-Henseleit solution also containing 2.7% bovine serum albumin, during which gitoxin levels decreased biexponentially. Distribution and elimination half-lives have been estimated to be 0.31 and 5.54 hours, Vd area to be 139 ml.g-1 and intrinsic metabolic clearance to be 1.36 ml.min-1.g-1. Gitoxin has been compared in these experimental conditions with digoxin, one of the most often used cardiotonic's. Distribution and elimination half-lives of digoxin were estimated to be 0.34 and 4.52 hours, Vd area to be 46.5 ml.g-1 and intrinsic metabolic clearance to be 0.17 ml.min-1.g-1. Other pharmacokinetic parameters (alpha, beta, V1, V2...) also have been calculated for these three types of perfusion experiments.

摘要

已在兔身上研究了吉妥辛的肝清除率,并使用离体灌注肝技术将其与地高辛的肝清除率进行了比较。在用改良的克雷布斯 - 亨泽莱特溶液进行1.5小时灌注期间,吉妥辛灌注液水平呈双指数下降;分布半衰期和消除半衰期估计分别为0.14小时和1.25小时,面积分布容积为95.5 ml·g⁻¹,内在代谢清除率为1.98 ml·min⁻¹·g⁻¹。在用含2.7%牛血清白蛋白的改良克雷布斯 - 亨泽莱特溶液进行1.5小时灌注期间,吉妥辛灌注液水平呈单指数下降。这可能是由于蛋白质结合减弱了肝脏摄取,以至于在1.5小时后分布尚未完成,因此无法区分两个阶段。在用同样含2.7%牛血清白蛋白的改良克雷布斯 - 亨泽莱特溶液中的全氟碳乳液进行5小时灌注实验时证实了这一点,在此期间吉妥辛水平呈双指数下降。分布半衰期和消除半衰期估计分别为0.31小时和5.54小时,面积分布容积为139 ml·g⁻¹,内在代谢清除率为1.36 ml·min⁻¹·g⁻¹。在这些实验条件下,已将吉妥辛与最常用的强心剂之一地高辛进行了比较。地高辛的分布半衰期和消除半衰期估计分别为0.34小时和4.52小时,面积分布容积为46.5 ml·g⁻¹,内在代谢清除率为0.17 ml·min⁻¹·g⁻¹。还针对这三种类型的灌注实验计算了其他药代动力学参数(α、β、V1、V2……)。

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