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膜凝胶区域中形状和取向纹理的缓慢弛豫

Slow Relaxation of Shape and Orientational Texture in Membrane Gel Domains.

作者信息

Jeppesen Jonas Camillus, Solovyeva Vita, Brewer Jonathan R, Johannes Ludger, Hansen Per Lyngs, Simonsen Adam Cohen

机构信息

Institut Curie, UMR3666 CNRS, U1143 INSERM, 26 rue d'Ulm, 75248 Paris Cedex 05, France.

出版信息

Langmuir. 2015 Nov 24;31(46):12699-707. doi: 10.1021/acs.langmuir.5b03168. Epub 2015 Nov 11.

Abstract

Gel domains in lipid bilayers are structurally more complex than fluid domains. Growth dynamics can lead to noncircular domains with a heterogeneous orientational texture. Most model membrane studies involving gel domain morphology and lateral organization assume the domains to be static. Here we show that rosette shaped gel domains, with heterogeneous orientational texture and a central topological defect, after early stage growth, undergo slow relaxation. On a time scale of days to weeks domains converge to circular shapes and approach uniform texture. 1,2-Dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) enriched gel domains are grown by cooling 1,2-dioleoyl-sn-glycero-3-phosphocholine (DOPC):DPPC bilayers into the solid-liquid phase coexistence region and are visualized with fluorescence microscopy. The relaxation of individual domains is quantified through image analysis of time-lapse image series. We find a shape relaxation mechanism which is inconsistent with Ostwald ripening and coalescence as observed in membrane systems with coexisting liquid phases. Moreover, domain texture changes in parallel with the changes in domain shape, and selective melting and growth of particular subdomains cause the texture to become more uniform. We propose a relaxation mechanism based on relocation of lipids from high-energy lattice positions, through evaporation-condensation and edge diffusion, to low-energy positions. The relaxation process is modified significantly by binding Shiga toxin, a bacterial toxin from Shigella dysenteriae, to the membrane surface. Binding alters the equilibrium shape of the gel domains from circular to eroded rosettes with disjointed subdomains. This observation may be explained by edge diffusion while evaporation-condensation is restricted, and it provides further support for the proposed overall relaxation mechanism.

摘要

脂质双层中的凝胶结构域在结构上比流体结构域更复杂。生长动力学可导致具有异质取向纹理的非圆形结构域。大多数涉及凝胶结构域形态和横向组织的模型膜研究都假定这些结构域是静态的。在此我们表明,具有异质取向纹理和中心拓扑缺陷的玫瑰花结状凝胶结构域在早期生长后会经历缓慢弛豫。在数天至数周的时间尺度上,结构域会收敛为圆形并趋近均匀纹理。通过将1,2 - 二油酰 - sn - 甘油 - 3 - 磷酸胆碱(DOPC):1,2 - 二棕榈酰 - sn - 甘油 - 3 - 磷酸胆碱(DPPC)双层冷却至固 - 液相共存区域来生长富含DPPC的凝胶结构域,并用荧光显微镜进行观察。通过对延时图像序列进行图像分析来量化单个结构域的弛豫过程。我们发现一种形状弛豫机制,该机制与在具有共存液相的膜系统中观察到的奥斯特瓦尔德熟化和聚结现象不一致。此外,结构域纹理随结构域形状的变化而平行变化,特定子结构域的选择性熔化和生长导致纹理变得更加均匀。我们提出一种弛豫机制,该机制基于脂质从高能晶格位置通过蒸发 - 凝聚和边缘扩散重新定位到低能位置。通过将痢疾志贺氏菌的细菌毒素志贺毒素结合到膜表面,可显著改变弛豫过程。结合会使凝胶结构域的平衡形状从圆形变为具有不连续子结构域的侵蚀玫瑰花结状。这一观察结果可以通过边缘扩散来解释,而蒸发 - 凝聚受到限制,并且它为所提出的整体弛豫机制提供了进一步支持。

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