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蛋白质冠层对纳米颗粒-脂质膜结合的影响:结合强度与动力学

Effect of Protein Corona on Nanoparticle-Lipid Membrane Binding: The Binding Strength and Dynamics.

作者信息

Lee Hwankyu

机构信息

Department of Chemical Engineering, Dankook University, Yongin 16890, South Korea.

出版信息

Langmuir. 2021 Mar 30;37(12):3751-3760. doi: 10.1021/acs.langmuir.1c00249. Epub 2021 Mar 19.

Abstract

All-atom molecular dynamics simulations of the 10 nm-sized anionic polystyrene (PS) particle complexed with plasma proteins (human serum albumin, immunoglobulin gamma-1 chain-C, and apolipoprotein A-I) adsorbed onto lipid bilayers [asymmetrically composed of extracellular (zwitterionic) and cytosolic (anionic) leaflets] are performed. Free energies calculated from umbrella sampling simulations show that proteins on the particle more weakly bind to the zwitterionic leaflet than do bare particles, in agreement with experiments showing the suppression of the particle-bilayer binding by protein corona. Proteins on the particle interact more strongly with the anionic leaflet than with the zwitterionic leaflet because of charge interactions between cationic protein residues and anionic lipid headgroups, to an extent dependent on various plasma proteins. In particular, hydrogen bonds between proteins and zwitterionic leaflets restrict the motion of lipids and thus reduce the lateral dynamics of bilayers, while the tight binding between proteins and anionic leaflets disrupts the helical structure of proteins and disorders lipids, leading to an increase in the lateral dynamics of bilayers. These findings help explain the experimental observation regarding the fact that the bilayer dynamics decreases when interacting with protein corona and suggest that the effect of protein corona on the binding strength and bilayer dynamics depends on protein types and bilayer charges.

摘要

对吸附在脂质双层[由细胞外(两性离子)和胞质(阴离子)小叶不对称组成]上的与血浆蛋白(人血清白蛋白、免疫球蛋白γ-1链-C和载脂蛋白A-I)复合的10纳米大小的阴离子聚苯乙烯(PS)颗粒进行全原子分子动力学模拟。通过伞形采样模拟计算得到的自由能表明,颗粒上的蛋白质与两性离子小叶的结合比裸颗粒更弱,这与显示蛋白质冠抑制颗粒-双层结合的实验结果一致。由于阳离子蛋白质残基与阴离子脂质头基团之间的电荷相互作用,颗粒上的蛋白质与阴离子小叶的相互作用比与两性离子小叶的相互作用更强,其程度取决于各种血浆蛋白。特别是,蛋白质与两性离子小叶之间的氢键限制了脂质的运动,从而降低了双层的横向动力学,而蛋白质与阴离子小叶之间的紧密结合破坏了蛋白质的螺旋结构并扰乱了脂质,导致双层的横向动力学增加。这些发现有助于解释关于与蛋白质冠相互作用时双层动力学降低这一实验观察结果,并表明蛋白质冠对结合强度和双层动力学的影响取决于蛋白质类型和双层电荷。

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