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高密度脂蛋白介导肝脏内皮细胞向实质细胞及胆汁进行体内逆向胆固醇转运的证据。

Evidence for reverse cholesterol transport in vivo from liver endothelial cells to parenchymal cells and bile by high-density lipoprotein.

作者信息

Bakkeren H F, Kuipers F, Vonk R J, Van Berkel T J

机构信息

Division of Biopharmaceutics, University of Leiden, Sylvius Laboratories, The Netherlands.

出版信息

Biochem J. 1990 Jun 15;268(3):685-91. doi: 10.1042/bj2680685.

Abstract

Acetylated low-density lipoprotein (acetyl-LDL), biologically labelled in the cholesterol moiety of cholesteryl oleate, was injected into control and oestrogen-treated rats. The serum clearance, the distribution among the various lipoproteins, the hepatic localization and the biliary secretion of the [3H]cholesterol moiety were determined at various times after injection. In order to monitor the intrahepatic metabolism of the cholesterol esters of acetyl-LDL in vivo, the liver was subdivided into parenchymal, endothelial and Kupffer cells by a low-temperature cell-isolation procedure. In both control and oestrogen-treated rats, acetyl-LDL is rapidly cleared from the circulation, mainly by the liver endothelial cells. Subsequently, the cholesterol esters are hydrolysed, and within 1 h after injection, about 60% of the cell- associated cholesterol is released. The [3H]cholesterol is mainly recovered in the high-density lipoprotein (HDL) range of the serum of control rats, while low levels of radioactivity are detected in serum of oestrogen-treated rats. In control rats cholesterol is transported from endothelial cells to parenchymal cells (reverse cholesterol transport), where it is converted into bile acids and secreted into bile. The data thus provide evidence that HDL can serve as acceptors for cholesterol from endothelial cells in vivo, whereby efficient delivery to the parenchymal cells and bile is assured. In oestrogen-treated rats the radioactivity from the endothelial cells is released with similar kinetics as in control rats. However, only a small percentage of radioactivity is found in the HDL fraction and an increased uptake of radioactivity in Kupffer cells is observed. The secretion of radioactivity into bile is greatly delayed in oestrogen-treated rats. It is concluded that, in the absence of extracellular lipoproteins, endothelial cells can still release cholesterol, although for efficient transport to liver parenchymal cells and bile, HDL is indispensable.

摘要

将胆固醇油酸酯的胆固醇部分进行生物标记的乙酰化低密度脂蛋白(acetyl-LDL)注射到对照大鼠和经雌激素处理的大鼠体内。在注射后的不同时间,测定了[3H]胆固醇部分的血清清除率、在各种脂蛋白中的分布、肝脏定位以及胆汁分泌情况。为了监测体内乙酰-LDL胆固醇酯的肝内代谢,通过低温细胞分离程序将肝脏细分为实质细胞、内皮细胞和库普弗细胞。在对照大鼠和经雌激素处理的大鼠中,乙酰-LDL均迅速从循环中清除,主要是被肝脏内皮细胞清除。随后,胆固醇酯被水解,注射后1小时内,约60%与细胞相关的胆固醇被释放。[3H]胆固醇主要在对照大鼠血清的高密度脂蛋白(HDL)范围内回收,而在经雌激素处理的大鼠血清中检测到的放射性水平较低。在对照大鼠中,胆固醇从内皮细胞转运到实质细胞(逆向胆固醇转运),在实质细胞中转化为胆汁酸并分泌到胆汁中。因此,这些数据提供了证据,表明HDL在体内可作为内皮细胞胆固醇的受体,从而确保有效地将胆固醇递送至实质细胞和胆汁。在经雌激素处理的大鼠中,内皮细胞的放射性以与对照大鼠相似的动力学释放。然而,在HDL组分中仅发现一小部分放射性,并且观察到库普弗细胞对放射性的摄取增加。在经雌激素处理的大鼠中,放射性分泌到胆汁中的过程大大延迟。得出的结论是,在没有细胞外脂蛋白的情况下,内皮细胞仍可释放胆固醇,尽管为了有效地将胆固醇转运至肝实质细胞和胆汁,HDL是必不可少的。

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