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牛磺胆酸盐和类固醇葡萄糖醛酸苷:在离体灌注大鼠肝脏中对胆汁淤积的相互保护作用。

Taurocholate and steroid glucuronides: mutual protection against cholestasis in the isolated perfused rat liver.

作者信息

Durham S, Vore M

出版信息

J Pharmacol Exp Ther. 1986 May;237(2):490-5.

PMID:3701641
Abstract

Estradiol-17 beta-(beta-D-glucuronide) (E217G) was shown to be cholestatic in the isolated perfused female rat liver. Doses of 0.85, 1.3, 1.7 and 2.1 mumol decreased bile flow maximally at 15 to 30 min by 29, 37, 68 and 76% respectively. Approximately 95% of a dose of [3H]E217G was cleared from the perfusate in 30 min and was secreted in bile, with 93, 85, 71 and 55% of the dose appearing in bile within 120 min after doses of 0.85, 1.3, 1.7 and 2.1 mumol, respectively. Neither vehicle nor 1.7 mumol of estradiol-3-(beta-D-glucuronide) (E23G) significantly altered bile flow. Infusion of taurocholate at 40 and 60 mumol/hr, respectively, partially and completely protected against the cholestasis induced by 1.7 mumol of E217G. The log dose-response curve for E217G-induced cholestasis was much steeper and was shifted to the right in the presence of a 60 mumol/hr infusion of taurocholate. Infusion of taurocholate at 80 mumol/hr in the absence of E217G or E23G decreased bile flow by 79%. However, addition of 1.7 mumol of either E217G or E23G offered marked protection against taurocholate-induced cholestasis and increased bile acid secretion. Higher doses (3.4 mumol) of E217G or E23G further increased bile flow and bile acid secretion. A model system is presented to explain the mutual protection against cholestasis.

摘要

已证实,17β -雌二醇(β - D -葡萄糖醛酸苷)(E217G)在离体灌注的雌性大鼠肝脏中具有致胆汁淤积作用。剂量为0.85、1.3、1.7和2.1 μmol时,分别在15至30分钟内使胆汁流量最大程度减少29%、37%、68%和76%。一剂[3H]E217G中约95%在30分钟内从灌注液中清除并分泌到胆汁中,在给予0.85、1.3、1.7和2.1 μmol剂量后,分别有93%、85%、71%和55%的剂量在120分钟内出现在胆汁中。溶剂和1.7 μmol的3 -(β - D -葡萄糖醛酸苷)雌二醇(E23G)均未显著改变胆汁流量。分别以40和60 μmol/小时的速率输注牛磺胆酸盐,可部分和完全预防由1.7 μmol E217G诱导的胆汁淤积。E217G诱导胆汁淤积的对数剂量反应曲线更陡峭,并且在以60 μmol/小时的速率输注牛磺胆酸盐时向右移动。在不存在E217G或E23G的情况下,以80 μmol/小时的速率输注牛磺胆酸盐可使胆汁流量减少79%。然而,添加1.7 μmol的E217G或E23G均可显著预防牛磺胆酸盐诱导的胆汁淤积并增加胆汁酸分泌。更高剂量(3.4 μmol)的E217G或E23G可进一步增加胆汁流量和胆汁酸分泌。本文提出了一个模型系统来解释对胆汁淤积的相互保护作用。

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