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2
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Adv Mater. 2011 May 24;23(20):2348-52. doi: 10.1002/adma.201003604. Epub 2011 Mar 1.
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Lipid rafts as a membrane-organizing principle.脂筏作为一种膜组织原则。
Science. 2010 Jan 1;327(5961):46-50. doi: 10.1126/science.1174621.
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Overcoming rapid inactivation of lung surfactant: analogies between competitive adsorption and colloid stability.克服肺表面活性剂的快速失活:竞争性吸附与胶体稳定性之间的类比
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Role of cholesterol in the biophysical dysfunction of surfactant in ventilator-induced lung injury.胆固醇在呼吸机相关性肺损伤中表面活性剂生物物理功能障碍中的作用。
Am J Physiol Lung Cell Mol Physiol. 2010 Jan;298(1):L117-25. doi: 10.1152/ajplung.00218.2009. Epub 2009 Nov 6.
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胆固醇纳米域对单层形态和动力学的影响。

Effect of cholesterol nanodomains on monolayer morphology and dynamics.

机构信息

Department of Chemical Engineering, University of California, Santa Barbara, CA 93106, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Aug 13;110(33):E3054-60. doi: 10.1073/pnas.1303304110. Epub 2013 Jul 30.

DOI:10.1073/pnas.1303304110
PMID:23901107
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3746890/
Abstract

At low mole fractions, cholesterol segregates into 10- to 100-nm-diameter nanodomains dispersed throughout primarily dipalmitoylphosphatidylcholine (DPPC) domains in mixed DPPC:cholesterol monolayers. The nanodomains consist of 6:1 DPPC:cholesterol "complexes" that decorate and lengthen DPPC domain boundaries, consistent with a reduced line tension, λ. The surface viscosity of the monolayer, ηs, decreases exponentially with the area fraction of the nanodomains at fixed surface pressure over the 0.1- to 10-Hz range of frequencies common to respiration. At fixed cholesterol fraction, the surface viscosity increases exponentially with surface pressure in similar ways for all cholesterol fractions. This increase can be explained with a free-area model that relates ηs to the pure DPPC monolayer compressibility and collapse pressure. The elastic modulus, G', initially decreases with cholesterol fraction, consistent with the decrease in λ expected from the line-active nanodomains, in analogy to 3D emulsions. However, increasing cholesterol further causes a sharp increase in G' between 4 and 5 mol% cholesterol owing to an evolution in the domain morphology, so that the monolayer is elastic rather than viscous over 0.1-10 Hz. Understanding the effects of small mole fractions of cholesterol should help resolve the controversial role cholesterol plays in human lung surfactants and may give clues as to how cholesterol influences raft formation in cell membranes.

摘要

在低摩尔分数下,胆固醇会分离成 10 到 100nm 直径的纳米域,分散在主要的二棕榈酰磷脂酰胆碱(DPPC)域中,存在于 DPPC:胆固醇混合单层中。纳米域由 DPPC:胆固醇“复合物”组成,这些复合物修饰并延长 DPPC 域边界,与线张力 λ 降低一致。在呼吸过程中常见的 0.1 到 10Hz 频率范围内,在固定表面压力下,单层的表面粘度 ηs 随纳米域的面积分数呈指数下降。在固定胆固醇分数下,表面粘度以类似的方式随表面压力呈指数增加,所有胆固醇分数都是如此。这种增加可以用一个自由面积模型来解释,该模型将 ηs 与纯 DPPC 单层压缩性和崩溃压力联系起来。弹性模量 G'最初随胆固醇分数的增加而降低,这与线活性纳米域导致的 λ 降低一致,类似于 3D 乳液。然而,进一步增加胆固醇会导致 G'在 4 到 5mol%胆固醇之间急剧增加,这是由于域形态的演变,使得单层在 0.1 到 10Hz 之间具有弹性而不是粘性。了解胆固醇的小摩尔分数的影响应该有助于解决胆固醇在人类肺表面活性剂中争议性的作用,并可能为胆固醇如何影响细胞膜中筏形成提供线索。