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胆盐刺激的胆固醇酯酶增加了HepG2细胞对高密度脂蛋白相关胆固醇酯的摄取。

Bile salt stimulated cholesterol esterase increases uptake of high density lipoprotein-associated cholesteryl esters by HepG2 cells.

作者信息

Li F, Huang Y, Hui D Y

机构信息

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

出版信息

Biochemistry. 1996 May 28;35(21):6657-63. doi: 10.1021/bi952313q.

Abstract

Bile salt stimulated cholesterol esterase is predominantly synthesized in the pancreas. However, this enzyme is also synthesized by the liver and was found to be present in plasma. The physiologic role of the systemic cholesterol esterase has not been clearly defined. In the current study, the human hepatoma cell line HepG2 was used as a model to determine the role of cholesterol esterase on hepatic uptake of high density lipoprotein (HDL)-associated cholesteryl esters. The results showed that hepatic uptake of the cholesteryl esters analog [3H]cholesteryl ether on reconstituted HDL was inhibited by anti-cholesterol esterase antibodies. The HDL-associated cholesteryl ester transported to HepG2 cells was also increased 2-fold in the presence of taurocholate, an activator of the cholesterol esterase. These results suggest that liver-derived cholesterol esterase may play an important role in cellular uptake of cholesteryl esters from HDL. This hypothesis was supported by demonstrating the ability of exogenously added cholesterol esterase to further enhance hepatic uptake of HDL-associated cholesteryl esters. The results of the current study also showed that cholesterol esterase increased free-to-esterified cholesterol ratio in the lipoprotein. Thus, alteration of HDL structure and composition contributes to the cholesterol esterase-induced cellular uptake of HDL-associated cholesteryl esters. On the basis of these observations, we propose that liver-derived cholesterol esterase may play an important role in lipoprotein metabolism.

摘要

胆汁盐刺激的胆固醇酯酶主要在胰腺中合成。然而,这种酶也由肝脏合成,并在血浆中被发现。全身性胆固醇酯酶的生理作用尚未明确界定。在当前研究中,人类肝癌细胞系HepG2被用作模型,以确定胆固醇酯酶在肝脏摄取高密度脂蛋白(HDL)相关胆固醇酯中的作用。结果显示,抗胆固醇酯酶抗体抑制了重组HDL上胆固醇酯类似物[3H]胆固醇醚的肝脏摄取。在胆固醇酯酶激活剂牛磺胆酸盐存在的情况下,转运至HepG2细胞的HDL相关胆固醇酯也增加了2倍。这些结果表明,肝脏来源的胆固醇酯酶可能在细胞从HDL摄取胆固醇酯中起重要作用。通过证明外源性添加的胆固醇酯酶能够进一步增强肝脏对HDL相关胆固醇酯的摄取,这一假设得到了支持。当前研究结果还表明,胆固醇酯酶增加了脂蛋白中游离胆固醇与酯化胆固醇的比例。因此,HDL结构和组成的改变有助于胆固醇酯酶诱导的细胞摄取HDL相关胆固醇酯。基于这些观察结果,我们提出肝脏来源的胆固醇酯酶可能在脂蛋白代谢中起重要作用。

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