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甾醇结构特异性的意义。去氢胆甾醇无法在脂筏中替代胆固醇。

Significance of sterol structural specificity. Desmosterol cannot replace cholesterol in lipid rafts.

作者信息

Vainio Saara, Jansen Maurice, Koivusalo Mirkka, Róg Tomasz, Karttunen Mikko, Vattulainen Ilpo, Ikonen Elina

机构信息

Institute of Biomedicine/Anatomy, University of Helsinki, Helsinki FI-00014, Finland.

出版信息

J Biol Chem. 2006 Jan 6;281(1):348-55. doi: 10.1074/jbc.M509530200. Epub 2005 Oct 25.

Abstract

Desmosterol is an immediate precursor of cholesterol in the Bloch pathway of sterol synthesis and an abundant membrane lipid in specific cell types. The significance of the difference between the two sterols, an additional double bond at position C24 in the tail of desmosterol, is not known. Here, we provide evidence that the biophysical and functional characteristics of the two sterols differ and that this is because the double bond at C24 significantly weakens the sterol ordering potential. In model membranes, desmosterol was significantly weaker than cholesterol in promoting the formation or stability of ordered domains, and in mammalian cell membranes, desmosterol associated less avidly than cholesterol with detergent-resistant membranes. Atomic scale molecular dynamics simulations showed that the double bond gives rise to additional stress in the tail, creating a rigid structure between C24 and C27 and favoring tilting of desmosterol distinct from cholesterol. Functional effects of desmosterol in cell membranes were assessed upon acutely exchanging approximately 70% of cholesterol to desmosterol. This led to impaired raft-dependent signaling via the insulin receptor, whereas non-raft-dependent protein secretion was not affected. We suggest that the choice of cholesterol synthesis route may provide a physiological mechanism to modulate raft-dependent functions in cells.

摘要

在固醇合成的布洛赫途径中,羊毛甾醇是胆固醇的直接前体,并且在特定细胞类型中是一种丰富的膜脂。这两种固醇之间的差异,即羊毛甾醇尾部C24位存在一个额外的双键,其意义尚不清楚。在此,我们提供证据表明这两种固醇的生物物理和功能特性不同,这是因为C24位的双键显著削弱了固醇的有序化潜力。在模型膜中,羊毛甾醇在促进有序结构域的形成或稳定性方面明显弱于胆固醇,而在哺乳动物细胞膜中,羊毛甾醇与抗去污剂膜的结合不如胆固醇紧密。原子尺度的分子动力学模拟表明,该双键在尾部产生额外应力,在C24和C27之间形成刚性结构,并有利于羊毛甾醇呈现与胆固醇不同的倾斜状态。通过将约70%的胆固醇急性置换为羊毛甾醇,评估了羊毛甾醇在细胞膜中的功能效应。这导致通过胰岛素受体的脂筏依赖性信号传导受损,而非脂筏依赖性蛋白质分泌不受影响。我们认为,胆固醇合成途径的选择可能提供一种生理机制来调节细胞中的脂筏依赖性功能。

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