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低密度脂蛋白与糖胺聚糖相互作用的特异性。

Specificity of the low density lipoprotein-glycosaminoglycan interaction.

作者信息

Sambandam T, Baker J R, Christner J E, Ekborg S L

机构信息

Department of Biochemistry, University of Alabama, Birmingham 35294.

出版信息

Arterioscler Thromb. 1991 May-Jun;11(3):561-8. doi: 10.1161/01.atv.11.3.561.

DOI:10.1161/01.atv.11.3.561
PMID:2029496
Abstract

There is ample documentation of the binding of chondroitin sulfate/dermatan sulfate proteoglycans to low density lipoprotein (LDL) both in vivo and in vitro. The interaction of these two species may be an early and important step in atherogenesis. Therefore, there is interest in defining the features of both molecules that are critical for their interaction. We employed a recently described competitive microassay that measures initial binding of proteoglycan to immobilized LDL. We confirmed the work of others that it is the apolipoprotein B component and, at least in part, a heparin-binding domain of LDL that are responsible for binding chondroitin sulfate/dermatan sulfate proteoglycans. The principal thrust of our study was concerned with the effects of a glycosaminoglycan's degree of sulfation on the binding to LDL. Initial experiments comparing dermatan sulfate and chondroitin sulfate proteoglycans indicated that the former was more efficient at binding LDL than the latter and that oversulfation, rather than chain length or iduronate content, was the preeminent feature involved. Additional binding studies with dermatan sulfate, chemically sulfated chondroitin-4-sulfate, and naturally occurring oversulfated chondroitin sulfates indicated that the degree of sulfation, not the position of sulfation, determined affinity for LDL. These results suggest that studies should be undertaken to determine whether oversulfated segments of glycosaminoglycans are especially involved in associations with LDL, leading to lipid accumulation, in the artery wall.

摘要

体内和体外均有大量关于硫酸软骨素/硫酸皮肤素蛋白聚糖与低密度脂蛋白(LDL)结合的文献记载。这两种物质的相互作用可能是动脉粥样硬化形成早期的一个重要步骤。因此,人们有兴趣确定这两种分子相互作用的关键特征。我们采用了一种最近描述的竞争性微量测定法,该方法可测量蛋白聚糖与固定化LDL的初始结合。我们证实了其他人的研究结果,即载脂蛋白B成分以及至少部分LDL的肝素结合结构域负责与硫酸软骨素/硫酸皮肤素蛋白聚糖结合。我们研究的主要重点是糖胺聚糖的硫酸化程度对其与LDL结合的影响。比较硫酸皮肤素和硫酸软骨素蛋白聚糖的初步实验表明,前者比后者更有效地结合LDL,并且过度硫酸化而非链长或艾杜糖醛酸含量是主要涉及的特征。对硫酸皮肤素、化学硫酸化的硫酸软骨素-4-硫酸酯以及天然存在的过度硫酸化硫酸软骨素进行的额外结合研究表明,硫酸化程度而非硫酸化位置决定了对LDL的亲和力。这些结果表明,应该进行研究以确定糖胺聚糖的过度硫酸化片段是否特别参与与LDL的结合,从而导致动脉壁脂质积累。

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