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口服乙酰水杨酸可诱导大鼠胆汁中胆固醇的分泌。

Oral acetylsalicylic acid induces biliary cholesterol secretion in the rat.

作者信息

Prigge W F, Gebhard R L

机构信息

Department of Medicine, VA Medical Center, Minneapolis, Minnesota 55417, USA.

出版信息

Lipids. 1997 Jul;32(7):753-8. doi: 10.1007/s11745-997-0096-y.

Abstract

Several agents can alter biliary cholesterol secretion, critical for cholesterol excretion and gallstone formation. Although salicylate effects on bile formation and gallstones have been studied, biliary lipid secretion has not been measured during oral aspirin treatment. We examined whether oral acetylsalicylic acid affects bile lipid secretion. Three groups of young rats were fed chow for 3 wk. Two of the groups then received aspirin at either 1.67 or 3.33 g/kg diet for 4 d. Serum, hepatic, and bile lipids were measured, as were enzymes of cholesterol synthesis and esterification. With oral aspirin, bile cholesterol secretion increased by 42% and hepatic cholesteryl ester content decreased by 40%. Serum cholesterol and hepatic free cholesterol did not change. To evaluate mechanisms of the cholesterol hypersecretion, hypothyroid animals fed low-fat or fish oil diets and repleted with triiodothyronine were also studied. Aspirin stimulated cholesterol secretion to a degree similar to triiodothyronine. An additive response was seen in fish oil-fed rats. Aspirin did not appear to have a primary action on 3-hydroxy-3-methylglutaryl-CoA reductase or acyl CoA:cholesterol acyltransferase activities, and had no direct effect on esterification of cholesterol by isolated hepatocytes. Aspirin may directly increase cholesterol transport into bile or have cell membrane effects which alter cholesterol transport. It remains to be determined whether the observed alterations in bile cholesterol secretion are specific to the rat or also apply to humans.

摘要

几种药物可改变胆汁胆固醇分泌,这对胆固醇排泄和胆结石形成至关重要。尽管已对水杨酸盐对胆汁形成和胆结石的影响进行了研究,但在口服阿司匹林治疗期间尚未测定胆汁脂质分泌情况。我们研究了口服乙酰水杨酸是否会影响胆汁脂质分泌。三组幼鼠喂食普通饲料3周。然后其中两组以1.67或3.33 g/kg饲料的剂量接受阿司匹林治疗4天。测定血清、肝脏和胆汁中的脂质,以及胆固醇合成和酯化的酶。口服阿司匹林后,胆汁胆固醇分泌增加了42%,肝脏胆固醇酯含量降低了40%。血清胆固醇和肝脏游离胆固醇没有变化。为了评估胆固醇分泌过多的机制,还研究了喂食低脂或鱼油饮食并补充三碘甲状腺原氨酸的甲状腺功能减退动物。阿司匹林刺激胆固醇分泌的程度与三碘甲状腺原氨酸相似。在喂食鱼油的大鼠中观察到了相加反应。阿司匹林似乎对3-羟基-3-甲基戊二酰辅酶A还原酶或酰基辅酶A:胆固醇酰基转移酶活性没有主要作用,并且对分离的肝细胞中胆固醇的酯化没有直接影响。阿司匹林可能直接增加胆固醇向胆汁中的转运,或者具有改变胆固醇转运的细胞膜效应。观察到的胆汁胆固醇分泌变化是否仅针对大鼠,还是也适用于人类,仍有待确定。

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