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正常及胆红素结合功能受损大鼠的胆红素排泄:苯巴比妥的作用

Bilirubin excretion in rats with normal and impaired bilirubin conjugation: effect of phenobarbital.

作者信息

Robinson S H, Yannoni C, Nagasawa S

出版信息

J Clin Invest. 1971 Dec;50(12):2606-13. doi: 10.1172/JCI106761.

Abstract

The effect of phenobarbital on bilirubin excretion was studied in rats with different capacities for bilirubin conjugation. Drug treatment induced substantial increases in bilirubin UDP-glucuronyl transferase activity in the liver of both normal and heterozygous Gunn rats, but not homozygous Gunn rats in which enzyme activity is completely absent. However, enhancement of bilirubin excretion in vivo was observed only in heterozygous Gunn rats. In these animals the maximum capacity to excrete bilirubin into bile (T(max)), like the activity of the conjugating enzyme, was half normal; phenobarbital caused an increase in T(max) to levels characteristic of normal animals, with a twofold rise in the excretion of conjugated pigment. This appeared to be largely unrelated to enhancement of bile flow, and there was no stimulation of alternate pathways of bilirubin excretion. Conjugated bilirubin was consistently recovered from the plasma and urine of both untreated normal and heterozygous Gunn rats infused with unconjugated pigment. The quantities thus recovered comprised a similar fraction of the total pigment conjugated in both types of animal. Moreover, there were linear correlations between T(max) and both the rate of bile flow and the activity of the conjugating enzyme over the range of values represented by control rats of both types. These findings suggest that the process by which conjugated bilirubin is secreted into the bile is closely related to conjugation and limits the final excretory rate at different levels of pigment excretion. The phenobarbital effect uniquely observed in heterozygous Gunn rats appears to be mediated primarily by enhancement of the limited capacity for bilirubin conjugation with an associated rise in functional secretory capacity.

摘要

在具有不同胆红素结合能力的大鼠中研究了苯巴比妥对胆红素排泄的影响。药物治疗使正常大鼠和杂合子Gunn大鼠肝脏中的胆红素UDP - 葡萄糖醛酸基转移酶活性大幅增加,但对于纯合子Gunn大鼠则无此作用,因为该酶在纯合子Gunn大鼠中完全缺失。然而,仅在杂合子Gunn大鼠中观察到体内胆红素排泄增强。在这些动物中,胆红素向胆汁中排泄的最大能力(T(max))与结合酶的活性一样,只有正常水平的一半;苯巴比妥使T(max)增加到正常动物的特征水平,结合色素的排泄增加了两倍。这似乎在很大程度上与胆汁流量的增加无关,并且没有刺激胆红素排泄的替代途径。在输注未结合色素的未治疗正常大鼠和杂合子Gunn大鼠的血浆和尿液中均持续回收了结合胆红素。在这两种类型的动物中,回收的量占总结合色素的比例相似。此外,在两种类型对照大鼠所代表的值范围内,T(max)与胆汁流速和结合酶活性之间存在线性相关性。这些发现表明,结合胆红素分泌到胆汁中的过程与结合密切相关,并在不同色素排泄水平限制了最终排泄率。在杂合子Gunn大鼠中独特观察到的苯巴比妥效应似乎主要是通过增强有限的胆红素结合能力以及相关的功能性分泌能力增加来介导的。

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