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The Molecular Structure of Human Red Blood Cell Membranes from Highly Oriented Solid Supported Multi-Lamellar Membranes

机译:高度定向固相支持的多层膜的人红细胞膜的分子结构

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摘要

We prepared highly oriented, multi-lamellar stacks of human red blood cell (RBC) membranes applied on silicon wafers. RBC ghosts were prepared by hemolysis and applied onto functionalized silicon chips and annealed into multi-lamellar RBC membranes. High resolution X-ray diffraction was used to determine the molecular structure of the stacked membranes. We present direct experimental evidence that these RBC membranes consist of nanometer sized domains of integral coiled-coil peptides, as well as liquid ordered (lo) and liquid disordered (ld) lipids. Lamellar spacings, membrane and hydration water layer thicknesses, areas per lipid tail and domain sizes were determined. The common drug aspirin was added to the RBC membranes and found to interact with RBC membranes and preferably partition in the head group region of the lo domain leading to a fluidification of the membranes, i.e., a thinning of the bilayers and an increase in lipid tail spacing. Our results further support current models of RBC membranes as patchy structures and provide unprecedented structural details of the molecular organization in the different domains.
机译:我们准备了高度定向的多层堆叠的人类红细胞(RBC)膜,该膜应用在硅晶圆上。通过溶血制备RBC鬼影,并将其施加到功能化的硅芯片上,并退火成多层RBC膜。高分辨率X射线衍射用于确定堆叠膜的分子结构。我们提供了直接的实验证据,这些RBC膜由完整的卷曲螺旋肽的纳米尺寸域以及液体有序(lo)和液体无序(ld)脂质组成。确定层间距,膜和水合水层的厚度,每个脂质尾部的面积和区域大小。将常见药物阿司匹林添加到RBC膜中,发现与RBC膜相互作用,并优选在lo结构域的头基区域分配,从而导致膜的流化,即双层变薄和脂质尾巴增加间距。我们的结果进一步支持了当前的RBC膜的斑片结构模型,并提供了不同域中分子组织的前所未有的结构细节。

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