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简单生物膜中的纳米尺度复杂动力学。

Complex dynamics at the nanoscale in simple biomembranes.

机构信息

Department of Physics, Indian Institute of Science, Bangalore, 560 012, India.

Department of Chemical Engineering, Indian Institute of Science, Bangalore, 560 012, India.

出版信息

Sci Rep. 2017 Sep 11;7(1):11173. doi: 10.1038/s41598-017-11068-5.

Abstract

Nature is known to engineer complex compositional and dynamical platforms in biological membranes. Understanding this complex landscape requires techniques to simultaneously detect membrane re-organization and dynamics at the nanoscale. Using super-resolution stimulated emission depletion (STED) microscopy coupled with fluorescence correlation spectroscopy (FCS), we reveal direct experimental evidence of dynamic heterogeneity at the nanoscale in binary phospholipid-cholesterol bilayers. Domain formation on the length scale of ~200-600 nm due to local cholesterol compositional heterogeneity is found to be more prominent at high cholesterol content giving rise to distinct intra-domain lipid dynamics. STED-FCS reveals unique dynamical crossover phenomena at length scales of ~100-150 nm within each of these macroscopic regions. The extent of dynamic heterogeneity due to intra-domain hindered lipid diffusion as reflected from the crossover length scale, is driven by cholesterol packing and organization, uniquely influenced by phospholipid type. These results on simple binary model bilayer systems provide novel insights into pathways leading to the emergence of complex nanodomain substructures with implications for a wide variety of membrane mediated cellular events.

摘要

自然界被认为在生物膜中设计了复杂的组成和动态平台。要理解这个复杂的领域,需要技术来同时检测纳米尺度上的膜重组和动力学。我们使用超分辨率受激发射损耗(STED)显微镜结合荧光相关光谱(FCS),在二元磷脂-胆固醇双层中直接揭示了纳米尺度上动态异质性的实验证据。由于局部胆固醇组成异质性,在 ~200-600nm 的长度尺度上形成的域形成在高胆固醇含量下更为明显,导致了不同的域内脂质动力学。STED-FCS 在每个宏观区域的 ~100-150nm 的长度尺度上揭示了独特的动力学交叉现象。反映在交叉长度尺度上的域内受阻脂质扩散引起的动态异质性的程度,由胆固醇的堆积和组织驱动,受到磷脂类型的独特影响。这些关于简单二元模型双层系统的结果为导致出现具有广泛膜介导细胞事件影响的复杂纳米域亚结构的途径提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c5e/5593986/bf950bd0acc7/41598_2017_11068_Fig1_HTML.jpg

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