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合成苯甲脒类凝血酶抑制剂在兔和大鼠体内的胆汁排泄

Biliary excretion of synthetic benzamidine-type thrombin inhibitors in rabbits and rats.

作者信息

Hauptmann J, Kaiser B, Paintz M, Markwardt F

机构信息

Institute of Pharmacology and Toxicology, Medical Academy Erfurt, GDR.

出版信息

Biomed Biochim Acta. 1987;46(6):445-53.

PMID:3675563
Abstract

In rabbits and rats the excretion via the bile of the highly effective and selective synthetic thrombin inhibitor N alpha-(2-naphthylsulfonylglycyl)-4-amidinophenylalanine piperidide was studied after various routes of administration and varying doses. The concentration in the bile was determined using a biological method, the reliability of which was checked by HPLC-determinations. The compound was excreted in the bile in biologically active unchanged form. Cumulative biliary excretion of the synthetic thrombin inhibitor in rabbits amounted to a high percentage of the administered dose after low doses given either systemically or intraportally. In rats the excretion rates during and after intravenous infusion reached a maximum indicating saturation kinetics. Hepatic uptake and biliary excretion of the highly basic benzamidine derivative essentially contribute to its short plasma half-life.

摘要

在兔子和大鼠中,研究了高效选择性合成凝血酶抑制剂Nα-(2-萘磺酰甘氨酰)-4-脒基苯丙氨酸哌啶经不同给药途径和不同剂量给药后通过胆汁的排泄情况。使用生物方法测定胆汁中的浓度,并通过高效液相色谱法测定来检验其可靠性。该化合物以生物活性未改变的形式经胆汁排泄。在经全身或门静脉给予低剂量后,兔子体内合成凝血酶抑制剂的累积胆汁排泄量占给药剂量的比例很高。在大鼠中,静脉输注期间和之后的排泄率达到最大值,表明存在饱和动力学。高度碱性的苯甲脒衍生物的肝脏摄取和胆汁排泄在很大程度上导致了其较短的血浆半衰期。

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