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胆固醇酯酶(胆汁盐刺激脂肪酶)基因敲除小鼠的膳食游离胆固醇和酯化胆固醇吸收情况

Dietary free and esterified cholesterol absorption in cholesterol esterase (bile salt-stimulated lipase) gene-targeted mice.

作者信息

Howles P N, Carter C P, Hui D Y

机构信息

Department of Pathology and Laboratory Medicine, University of Cincinnati College of Medicine, Cincinnati, Ohio 45267-0529, USA.

出版信息

J Biol Chem. 1996 Mar 22;271(12):7196-202. doi: 10.1074/jbc.271.12.7196.

Abstract

The involvement of pancreatic cholesterol esterase (bile salt-stimulated lipase) in cholesterol absorption through the intestine has been controversial. We have addressed this issue by using homologous recombination in embryonic stem cells to produce mice lacking a functional cholesterol esterase gene. Cholesterol esterase knockout mice and their wild type counterparts were fed a bolus dose of [3H]cholesterol and a trace amount of [beta-14C]sitosterol by gavage. The ratio of the two radiolabels excreted in the feces over a 24-h period was found to be similar in the control and cholesterol esterase-null mice. Similar results were observed when the radiolabeled sterols were supplied in an emulsion with phospholipid and triolein or in lipid vesicles with phosphatidylcholine. Cholesterol absorption results were similar between the control and cholesterol esterase-null mice regardless of whether the animals were fed a low fat diet or a high fat/high cholesterol diet. The rate of [3H]cholesterol appearance in the serum of the gene-targeted mice paralleled that observed in control animals. In contrast to these results, when experiments were performed with [3H]cholesteryl oleate instead of [3H]cholesterol, a higher amount of the 3H radiolabel was found excreted in feces and dramatically less of the radiolabel was detected in the serum of the cholesterol esterase-null mice in comparison with that detected in control animals. Serum cholesterol levels were not significantly different between control and cholesterol esterase-null mice fed either control or an atherogenic diet. These results indicate that cholesterol esterase is responsible for mediating intestinal absorption of cholesteryl esters but does not play a primary role in free cholesterol absorption.

摘要

胰腺胆固醇酯酶(胆汁盐刺激脂肪酶)在肠道胆固醇吸收过程中的作用一直存在争议。我们通过在胚胎干细胞中进行同源重组来培育缺乏功能性胆固醇酯酶基因的小鼠,从而解决了这个问题。给胆固醇酯酶基因敲除小鼠及其野生型对照小鼠经口灌胃给予大剂量的[3H]胆固醇和微量的[β-14C]谷甾醇。结果发现,在24小时内,对照小鼠和胆固醇酯酶基因缺失小鼠粪便中排出的两种放射性标记物的比例相似。当放射性标记的甾醇与磷脂和三油酸甘油酯制成乳剂或与磷脂酰胆碱制成脂质体提供时,也观察到了类似的结果。无论给动物喂食低脂饮食还是高脂/高胆固醇饮食,对照小鼠和胆固醇酯酶基因缺失小鼠的胆固醇吸收结果都相似。基因靶向小鼠血清中[3H]胆固醇的出现速率与对照动物中观察到的速率平行。与这些结果相反,当用[3H]油酸胆固醇代替[3H]胆固醇进行实验时,与对照动物相比,在胆固醇酯酶基因缺失小鼠的粪便中发现排出的3H放射性标记物更多,而在血清中检测到的放射性标记物显著减少。喂食对照饮食或致动脉粥样硬化饮食的对照小鼠和胆固醇酯酶基因缺失小鼠的血清胆固醇水平没有显著差异。这些结果表明,胆固醇酯酶负责介导胆固醇酯的肠道吸收,但在游离胆固醇吸收中不发挥主要作用。

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