Atherosclerotic Oxidized Lipids Affect Formation and Biophysical Properties of Supported Lipid Bilayers and Simulated Membranes.

IF 2.8 2区 化学 Q3 CHEMISTRY, PHYSICAL The Journal of Physical Chemistry B Pub Date : 2024-11-18 DOI:10.1021/acs.jpcb.4c05451
Dane E Santa, Turner P Brown, Wonpil Im, Nathan J Wittenberg
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Abstract

Oxidized lipids arising from oxidative stress are associated with many serious health conditions, including cardiovascular diseases. For example, KDdiA-PC and KOdiA-PC are two oxidized phosphatidylcholines (oxPC) directly linked to atherosclerosis, which precipitate heart failure, stroke, aneurysms, and chronic kidney disease. These oxPCs are well-characterized in small particles such as low-density lipoprotein, but how their presence affects the biophysical properties of larger bilayer membranes is unclear. It is also unclear how membrane mediators, such as cholesterol, affect lipid bilayers containing these oxPCs. Here, we characterize supported lipid bilayers (SLBs) containing POPC, KDdiA-PC, or KOdiA-PC, and cholesterol. We used a quartz crystal microbalance with dissipation monitoring (QCM-D), fluorescence microscopy, and all-atom molecular dynamics (MD) to examine the formation process, biophysical properties, and specific lipid conformations in simulated bilayers. Experimentally, we show that liposomes containing either oxPC form SLBs by rupturing on contact with SiO2 substrates, which differs from the typical adsorption-rupture pathway observed with nonoxidized liposomes. We also show that increasing the oxPC concentration in SLBs results in thinner bilayers that contain defects. Simulations reveal that the oxidized sn-2 tails of KDdiA-PC and KOdiA-PC bend out of the hydrophobic membrane core into the hydrophilic headgroup region and beyond. The altered conformations of these oxPC, which are affected by cholesterol content and protonation state of the oxidized functional groups, contribute to trends of decreasing membrane thickness and increasing membrane area with increasing oxPC concentration. This combined approach provides a comprehensive view of the biophysical properties of membranes containing KDdiA-PC and KOdiA-PC at the molecular level, which is crucial to understanding the role of lipid oxidation in cardiovascular disease and related immune responses.

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动脉粥样硬化氧化脂质影响支撑脂质双分子层和模拟膜的形成和生物物理性质
氧化应激引起的氧化脂质与包括心血管疾病在内的许多严重健康问题有关。例如,KDdiA-PC 和 KOdiA-PC 是与动脉粥样硬化直接相关的两种氧化磷脂酰胆碱(oxPC),它们会诱发心力衰竭、中风、动脉瘤和慢性肾病。这些氧化磷酸胆碱在低密度脂蛋白等小颗粒中的特性很好,但它们的存在如何影响较大双层膜的生物物理特性还不清楚。此外,胆固醇等膜介质如何影响含有这些氧化多糖的脂质双分子层也不清楚。在此,我们对含有 POPC、KDdiA-PC 或 KOdiA-PC 和胆固醇的支撑脂质双分子层 (SLB) 进行了表征。我们使用带耗散监测的石英晶体微天平(QCM-D)、荧光显微镜和全原子分子动力学(MD)来研究模拟双层膜的形成过程、生物物理特性和特定的脂质构象。实验结果表明,含有任一种 oxPC 的脂质体在与二氧化硅基质接触时会破裂,从而形成 SLB,这不同于在非氧化脂质体中观察到的典型吸附-破裂途径。我们还发现,SLBs 中 oxPC 浓度的增加会导致含有缺陷的双层膜变薄。模拟显示,KDdiA-PC 和 KOdiA-PC 的氧化 sn-2 尾端从疏水性膜核心弯曲到亲水性头基区甚至更远。这些氧化多氯联苯构象的改变受到胆固醇含量和氧化官能团质子化状态的影响,导致膜厚度随着氧化多氯联苯浓度的增加而减小,膜面积随着氧化多氯联苯浓度的增加而增大。这种综合方法在分子水平上全面揭示了含有 KDdiA-PC 和 KOdiA-PC 的膜的生物物理特性,这对于理解脂质氧化在心血管疾病和相关免疫反应中的作用至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
5.80
自引率
9.10%
发文量
965
审稿时长
1.6 months
期刊介绍: An essential criterion for acceptance of research articles in the journal is that they provide new physical insight. Please refer to the New Physical Insights virtual issue on what constitutes new physical insight. Manuscripts that are essentially reporting data or applications of data are, in general, not suitable for publication in JPC B.
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