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胆固醇对盘状高密度脂蛋白热稳定性的影响。

Effects of cholesterol on thermal stability of discoidal high density lipoproteins.

机构信息

Department of Physiology and Biophysics, Boston University School of Medicine, Boston, MA 02118, USA.

出版信息

J Lipid Res. 2010 Feb;51(2):324-33. doi: 10.1194/jlr.M000117. Epub 2009 Aug 21.

DOI:10.1194/jlr.M000117
PMID:19700415
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2803234/
Abstract

Reverse cholesterol transport in plasma involves variations in HDL cholesterol concentration. To understand physicochemical and functional implications of such variations, we analyzed stability of reconstituted HDL containing human apolipoproteins (apoA-I, apoA-II, or apoC-I), phosphatidylcholines varying in chain length (12-18 carbons) and unsaturation (0 or 1), and 0-35 mol% cholesterol. Lipoprotein heat denaturation was monitored by circular dichroism for protein unfolding/dissociation and by light scattering for particle fusion. We found that cholesterol stabilizes relatively unstable complexes; for example, incorporation of 10-30 mol% cholesterol in apoC-I:dimyristoyl phosphatidylcholine complexes increased their kinetic stability by deltaDeltaG* congruent with 1 kcal/mol. In more stable complexes containing larger proteins and/or longer-chain lipids, incorporation of 10% cholesterol did not significantly alter the disk stability; however, 15% or more cholesterol destabilized the apoA-I-containing complexes and led to vesicle formation. Thus, cholesterol tends to stabilize less stable lipoproteins, apparently by enhancing favorable packing interactions, but in more stable lipoproteins, where such interactions are already highly optimized, the stabilizing effect of cholesterol decreases and, eventually, becomes destabilizing. These results help uncouple the functional roles of particle stability and chain fluidity and suggest that structural disorder in HDL surface, rather than chain fluidity, is an important physicochemical determinant of HDL function.

摘要

血浆中的胆固醇逆向转运涉及高密度脂蛋白胆固醇浓度的变化。为了理解这些变化的物理化学和功能意义,我们分析了含有人类载脂蛋白(载脂蛋白 A-I、载脂蛋白 A-II 或载脂蛋白 C-I)、不同链长(12-18 个碳)和不同不饱和度(0 或 1)的磷脂酰胆碱以及 0-35mol%胆固醇的重组高密度脂蛋白的稳定性。通过圆二色性监测脂蛋白的热变性来研究蛋白质的展开/解离,通过光散射监测粒子的融合。我们发现胆固醇稳定了相对不稳定的复合物;例如,在载脂蛋白 C-I:二肉豆蔻酰磷脂酰胆碱复合物中加入 10-30mol%胆固醇,使它们的动力学稳定性增加了约 1kcal/mol。在含有较大蛋白质和/或较长链脂质的更稳定的复合物中,加入 10%胆固醇不会显著改变盘状稳定性;然而,15%或更多的胆固醇会使载脂蛋白 A-I 含有复合物不稳定,并导致形成囊泡。因此,胆固醇似乎通过增强有利的包装相互作用来稳定不太稳定的脂蛋白,但在更稳定的脂蛋白中,这种相互作用已经高度优化,胆固醇的稳定作用降低,最终变得不稳定。这些结果有助于分离颗粒稳定性和链流动性的功能作用,并表明 HDL 表面的结构无序,而不是链流动性,是 HDL 功能的重要物理化学决定因素。

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