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胆固醇及胆固醇衍生物对膜结构的扰动取决于甾醇的取向。

Perturbations of membrane structure by cholesterol and cholesterol derivatives are determined by sterol orientation.

作者信息

Olsen Brett N, Schlesinger Paul H, Baker Nathan A

机构信息

Molecular Cell Biology Graduate Program, Center for Computational Biology, Washington University in St. Louis, 700 South Euclid Avenue, Campus Box 8036, St. Louis, Missouri 63110, USA.

出版信息

J Am Chem Soc. 2009 Apr 8;131(13):4854-65. doi: 10.1021/ja8095224.

Abstract

Cholesterol is essential for proper function and regulation of eukaryotic membranes, and significant amounts of metabolic energy are dedicated to controlling cellular cholesterol levels. Oxidation products of cholesterol, the oxysterols, are enzymatically produced molecules that play a major role in mediating cholesterol homeostasis through mechanisms which have not yet been fully elucidated. Certain oxysterols are known to have direct effects on membrane permeability and structure, effects that are strikingly different from that of cholesterol. We use molecular dynamics simulations of these oxysterols in 1-palmitoyl 2-oleoyl phosphatidylcholine (POPC) bilayers to explain the structural origins for the differing effects of cholesterol and 25-hydroxycholesterol on bilayer properties. In particular, we demonstrate that the source for these differing perturbations is the much wider range of molecular orientations accessible to 25-hydroxycholesterol when compared to cholesterol. This study shows that direct membrane perturbation by side-chain oxysterols is significant and suggests that these membrane perturbations may play a role in the oxysterol regulation of cholesterol homeostasis.

摘要

胆固醇对于真核细胞膜的正常功能和调节至关重要,大量的代谢能量用于控制细胞内胆固醇水平。胆固醇的氧化产物氧甾醇是通过尚未完全阐明的机制在介导胆固醇稳态中起主要作用的酶促产生的分子。已知某些氧甾醇对膜通透性和结构有直接影响,这些影响与胆固醇的影响显著不同。我们在1-棕榈酰-2-油酰磷脂酰胆碱(POPC)双层膜中对这些氧甾醇进行分子动力学模拟,以解释胆固醇和25-羟基胆固醇对双层膜性质不同影响的结构起源。特别是,我们证明,与胆固醇相比,25-羟基胆固醇可获得的分子取向范围要宽得多,这就是这些不同扰动的来源。这项研究表明,侧链氧甾醇对膜的直接扰动很显著,并表明这些膜扰动可能在氧甾醇对胆固醇稳态的调节中起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ed5/2675926/46a7c8fbadd7/nihms103677f1.jpg

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