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首页> 外文期刊>Biophysical Journal >Interfacial tension and surface pressure of high density lipoprotein, low density lipoprotein, and related lipid droplets
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Interfacial tension and surface pressure of high density lipoprotein, low density lipoprotein, and related lipid droplets

机译:高密度脂蛋白,低密度脂蛋白及相关脂滴的界面张力和表面压力

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摘要

Lipid droplets play a central role in energy storage and metabolism on a cellular scale. Their core is comprised of hydrophobic lipids covered by a surface region consisting of amphiphilic lipids and proteins. For example, high and low density lipoproteins (HDL and LDL, respectively) are essentially lipid droplets surrounded by specific proteins, their main function being to transport cholesterol. Interfacial tension and surface pressure of these particles are of great interest because they are related to the shape and the stability of the droplets and to protein adsorption at the interface. Here we use coarse-grained molecular-dynamics simulations to consider a number of related issues by calculating the interfacial tension in protein-free lipid droplets, and in HDL and LDL particles mimicking physiological conditions. First, our results suggest that the curvature dependence of interfacial tension becomes significant for particles with a radius of ~5 nm, when the area per molecule in the surface region is 1.4 nm 2. Further, interfacial tensions in the used HDL and LDL models are essentially unaffected by single apo-proteins at the surface. Finally, interfacial tensions of lipoproteins are higher than in thermodynamically stable droplets, suggesting that HDL and LDL are kinetically trapped into a metastable state.
机译:脂质液滴在细胞规模的能量存储和代谢中起着核心作用。它们的核心由被两亲脂质和蛋白质组成的表面区域覆盖的疏水脂质组成。例如,高密度和低密度脂蛋白(分别为HDL和LDL)本质上是被特定蛋白质包围的脂滴,其主要功能是转运胆固醇。这些颗粒的界面张力和表面压力非常令人关注,因为它们与液滴的形状和稳定性以及界面处的蛋白质吸附有关。在这里,我们通过计算无蛋白质脂质液滴以及模拟生理条件的HDL和LDL颗粒的界面张力,使用粗粒度分子动力学模拟来考虑许多相关问题。首先,我们的结果表明,当表面区域中每个分子的面积小于1.4 nm时,对于半径约为5 nm的粒子,界面张力的曲率依赖性变得显着2。此外,使用的HDL和LDL模型中的界面张力基本上不受表面单个脱辅基蛋白的影响。最后,脂蛋白的界面张力高于热力学稳定的液滴,这表明HDL和LDL在动力学上陷入了亚稳态。

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