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载脂蛋白A-I在盘状和球状重组高密度脂蛋白颗粒中的电荷与结构稳定性

The charge and structural stability of apolipoprotein A-I in discoidal and spherical recombinant high density lipoprotein particles.

作者信息

Sparks D L, Lund-Katz S, Phillips M C

机构信息

Department of Biochemistry, Medical College of Pennsylvania, Philadelphia 19129.

出版信息

J Biol Chem. 1992 Dec 25;267(36):25839-47.

PMID:1464598
Abstract

The details of how high density lipoprotein (HDL) microstructure affects the conformation and net charge of apolipoprotein (apo) A-I in various classes of HDL particles have been investigated in homogeneous recombinant HDL (rHDL) particles containing apoA-I, palmitoyl-oleoyl phosphatidylcholine (POPC) and cholesteryl oleate. Isothermal denaturation with guanidine HCl was used to monitor alpha-helix structural stability, whereas electrokinetic analyses and circular dichroism were used to determine particle charge and apoA-I secondary structure, respectively. Electrokinetic analyses show that at pH 8.6 apoA-I has a net negative charge on discoidal (POPC.apoA-I) particles (-5.2 electronic units/mol of apoA-I) which is significantly greater than that of apoA-I either free in solution or on spherical (POPC.cholesteryl oleate.apoA-I) rHDL (approximately -3.5 electronic units). Raising the POPC content (32-128 mol/ml of apoA-I) of discoidal particles 1) increases the particle major diameter from 9.3 to 12.1 nm, 2) increases the alpha-helix content from 62 to 77%, and 3) stabilizes the helical segments by increasing the free energy of unfolding (delta GD degree) from 1.4 to 3.0 kcal/mol of apoA-I. Raising the POPC content (28-58 mol/mol of apoA-I) of spherical particles 1) increases the particle diameter from 7.4 to 12.6 nm, 2) increases the percent alpha-helix from 62 to 69%, and 3) has no significant effect on delta GD degree (2.2 kcal/mol of apoA-I). This study shows that different HDL subspecies maintain particular apoA-I conformations that confer unique charge and structural characteristics on the particles. It is likely that the charge and conformation of apoA-I are critical molecular properties that modulate the metabolism of HDL particles and influence their role in cholesterol transport.

摘要

在含有载脂蛋白A-I(apoA-I)、棕榈酰油酰磷脂酰胆碱(POPC)和油酸胆固醇酯的均一重组高密度脂蛋白(rHDL)颗粒中,研究了高密度脂蛋白(HDL)微观结构如何影响各类HDL颗粒中载脂蛋白(apo)A-I的构象和净电荷的细节。用盐酸胍进行等温变性以监测α-螺旋结构稳定性,而电动分析和圆二色性分别用于测定颗粒电荷和apoA-I二级结构。电动分析表明,在pH 8.6时,盘状(POPC.apoA-I)颗粒上的apoA-I带净负电荷(-5.2电子单位/摩尔apoA-I),这明显大于溶液中游离的apoA-I或球状(POPC.油酸胆固醇酯.apoA-I)rHDL上的apoA-I净负电荷(约-3.5电子单位)。提高盘状颗粒的POPC含量(32 - 128摩尔/毫升apoA-I):1)使颗粒的长径从9.3纳米增加到12.1纳米;2)使α-螺旋含量从62%增加到77%;3)通过将解折叠自由能(ΔGD°)从1.4千卡/摩尔apoA-I增加到3.0千卡/摩尔apoA-I来稳定螺旋片段。提高球状颗粒的POPC含量(28 - 58摩尔/摩尔apoA-I):1)使颗粒直径从7.4纳米增加到12.6纳米;2)使α-螺旋百分比从62%增加到69%;3)对ΔGD°(2.2千卡/摩尔apoA-I)没有显著影响。这项研究表明,不同的HDL亚类维持特定的apoA-I构象,这些构象赋予颗粒独特的电荷和结构特征。apoA-I的电荷和构象很可能是调节HDL颗粒代谢并影响其在胆固醇转运中作用的关键分子特性。

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