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来自无β脂蛋白血症和正常新生儿血浆的含载脂蛋白E的高密度脂蛋白的受体结合活性。

Receptor binding activity of high-density lipoproteins containing apoprotein E from abetalipoproteinemic and normal neonate plasma.

作者信息

Innerarity T L, Bersot T P, Arnold K S, Weisgraber K H, Davis P A, Forte T M, Mahley R W

出版信息

Metabolism. 1984 Feb;33(2):186-95. doi: 10.1016/0026-0495(84)90133-1.

Abstract

The receptor binding properties of lipoproteins derived from neonates and abetalipoproteinemic patients were examined. Compared to normal adults, the neonate plasma contained reduced cholesterol levels, with only 40% of the total cholesterol transported in the low-density lipoproteins (LDL). When compared at equal cholesterol concentrations, however, the total neonate lipoproteins (d less than 1.21) were as effective as adult d less than 1.21 lipoproteins in stimulating cholesteryl ester formation in cultured human fibroblasts. Analysis of the neonate lipoproteins explained their enhanced ability to deliver cholesterol to the cells via LDL (apoprotein B,E) receptors: the neonate d = 1.02-1.063 fraction contained, in addition to LDL, alpha 2-migrating, apoprotein E-rich high-density lipoproteins (HDL1), which were isolated by Geon-Pevikon electrophoresis. In binding studies performed with human fibroblasts at 4 degrees C, the neonate HDL1 were 14-fold more effective than either neonate or adult human LDL in displacing 125I-LDL from apo-B,E receptors. The neonate HDL (d = 1.063-1.21) contained a subfraction rich in apo-E and apo(E-A-II), which was isolated by heparin-Sepharose chromatography. This fraction was also active in displacing 125I-LDL from the receptors on cultured fibroblasts. Apoprotein E-containing HDL subclasses, similar to those described in the blood of neonates, were present in the d less than 1.063 and d = 1.063-1.21 lipoprotein fractions of patients with abetalipoproteinemia. These HDL with apo-E were enriched in cholesterol and were as effective as normal LDL in competing with 125I-LDL for apo-B,E receptor-mediated binding, internalization, and degradation. When incubated with cultured human fibroblasts, the HDL with apo-E from the abetalipoproteinemic subjects increased the cholesteryl ester mass three- to fourfold. These studies suggest that neonates and abetalipoproteinemic subjects may depend (at least in part) upon lipoproteins containing apo-E to deliver cholesterol to various tissues via the LDL (apo-B,E) receptor.

摘要

对来自新生儿和无β脂蛋白血症患者的脂蛋白的受体结合特性进行了检测。与正常成年人相比,新生儿血浆中的胆固醇水平降低,低密度脂蛋白(LDL)中运输的总胆固醇仅占40%。然而,当在相等的胆固醇浓度下进行比较时,总的新生儿脂蛋白(密度小于1.21)在刺激培养的人成纤维细胞中胆固醇酯形成方面与成年人密度小于1.21的脂蛋白一样有效。对新生儿脂蛋白的分析解释了它们通过LDL(载脂蛋白B、E)受体向细胞递送胆固醇能力增强的原因:新生儿密度为1.02 - 1.063的部分,除了LDL外,还含有通过Geon - Pevikon电泳分离的α2迁移的、富含载脂蛋白E的高密度脂蛋白(HDL1)。在4℃下用人成纤维细胞进行的结合研究中,新生儿HDL1在从载脂蛋白B、E受体上置换125I - LDL方面比新生儿或成年人的LDL有效14倍。新生儿HDL(密度 = 1.063 - 1.21)含有一个富含载脂蛋白E和载脂蛋白(E - A - II)的亚组分,该亚组分通过肝素 - 琼脂糖层析分离。该组分在从培养的成纤维细胞上的受体置换125I - LDL方面也有活性。无β脂蛋白血症患者密度小于1. .063和密度 = 1.063 - 1.21的脂蛋白部分中存在与新生儿血液中描述的类似的含载脂蛋白E的HDL亚类。这些含载脂蛋白E的HDL富含胆固醇,在与125I - LDL竞争载脂蛋白B, E受体介导的结合、内化和降解方面与正常LDL一样有效。当与培养的人成纤维细胞一起孵育时,来自无β脂蛋白血症受试者的含载脂蛋白E的HDL使胆固醇酯质量增加三到四倍。这些研究表明,新生儿和无β脂蛋白血症受试者可能(至少部分地)依赖于含载脂蛋白E 的脂蛋白通过LDL(载脂蛋白B、E)受体将胆固醇递送至各种组织。

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