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Curvature, order, and dynamics of lipid hexagonal phases studied by deuterium NMR spectroscopy.通过氘核磁共振光谱研究脂质六方相的曲率、有序性和动力学。
Biochemistry. 1993 May 25;32(20):5394-410. doi: 10.1021/bi00071a015.
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A molecular model for lipid-protein interaction in membranes: the role of hydrophobic mismatch.膜中脂类-蛋白质相互作用的分子模型:疏水错配的作用。
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A general method for the preparation of mixed micelles of hydrophobic peptides and sodium dodecyl sulphate.
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Three-dimensional crystals of a membrane protein complex. The photosynthetic reaction centre from Rhodopseudomonas viridis.一种膜蛋白复合物的三维晶体。来自绿脓杆菌的光合反应中心。
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Mixtures of gramicidin and lysophosphatidylcholine form lamellar structures.
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Rhodopsin. Purification and recombination with phospholipids assayed by the metarhodopsin I leads to metarhodopsin II transition.视紫红质。通过视紫红质I测定的纯化及与磷脂的重组导致视紫红质I向视紫红质II的转变。
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Acyl chain orientational order in the hexagonal HII phase of phospholipid-water dispersions.磷脂 - 水分散体系六方HII相中的酰基链取向有序性。
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A model for gramicidin A'-phospholipid interactions in bilayers.双层膜中短杆菌肽A'-磷脂相互作用的模型。
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9
The membrane as an environment of minimal interconversion. A circular dichroism study on the solvent dependence of the conformational behavior of gramicidin in diacylphosphatidylcholine model membranes.作为最小互变环境的膜。关于短杆菌肽在二酰基磷脂酰胆碱模型膜中构象行为的溶剂依赖性的圆二色性研究。
Biochemistry. 1988 Jun 28;27(13):4848-55. doi: 10.1021/bi00413a040.
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1H-NMR study of gramicidin A transmembrane ion channel. Head-to-head right-handed, single-stranded helices.短杆菌肽A跨膜离子通道的1H-NMR研究。头对头右手单链螺旋。
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通过2H核磁共振光谱研究N,N-二甲基十二烷基氧化胺/短杆菌肽D/水体系中的相平衡和分子堆积。

Phase equilibria and molecular packing in the N,N-dimethyldodecylamine oxide/gramicidin D/water system studied by 2H nuclear magnetic resonance spectroscopy.

作者信息

Orädd G, Lindblom G, Arvidson G, Gunnarsson K

机构信息

Department of Physical Chemistry, University of Umeä, Sweden.

出版信息

Biophys J. 1995 Feb;68(2):547-57. doi: 10.1016/S0006-3495(95)80216-X.

DOI:10.1016/S0006-3495(95)80216-X
PMID:7535115
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1281719/
Abstract

A partial phase diagram of the system N,N-dimethyldodecylamine oxide (DDAO)/water/gramicidin D was determined by 2H-NMR. Both 2H2O and perdeuterated DDAO (DDAO-d31) were studied by solid state NMR techniques. Addition of gramicidin D to the micellar (L1), normal hexagonal (HI) and cubic (I) phases of DDAO induces phase separations, giving two-phase regions, which all contain a lamellar (L alpha) phase. The L alpha phase containing gramicidin is characterized by larger order parameters for DDAO-d31 compared with the corresponding order parameters in the L alpha and HI phases of DDAO-d31/H2O. The L alpha phase may stay in equilibrium with any other phase in the phase diagram. The DDAO exchange between the coexisting phases is slow on the NMR timescale, which is why the recorded NMR spectrum consists of superimposed spectra from the different phases occurring in the sample. Gramicidin D can be solubilized in appreciable quantities only in the lamellar phase of DDAO-d31. Increasing amounts of gramicidin in the liquid crystalline phases result in a continuous increase in the molecular ordering up to about 5 mol% gramicidin, where a plateau is reached. This is consistent with a recent theoretical model describing the influence on the ordering of lipids by a membrane protein with larger hydrophobic thickness than the lipid bilayer. The solvent used for dissolving gramicidin at the incorporation of the peptide in the lipid aggregates has no effect on the 2H-NMR lineshapes of DDAO-d31. It is concluded that gramicidin is solubilized in the L alpha phase and that it always adopts the channel conformation independent of a particular solvent. The channel conformation is also supported by CD studies. In some of the samples, macroscopic orientation of the lipid aggregates is observed. It is concluded that DDAO-d31 in the binary system favors an orientation with the long axis of the hydrocarbon chain perpendicular to the magnetic field, whereas when gramicidin D is present the hydrocarbon chain orients parallel to the magnetic field. This is explained by the fact that gramicidin aligns with its helical axis parallel to the magnetic field, thereby forcing also the DDAO-d31 molecules to obtain such an orientation.

摘要

通过2H-NMR确定了N,N-二甲基十二烷基氧化胺(DDAO)/水/短杆菌肽D体系的部分相图。采用固态NMR技术研究了2H2O和全氘代DDAO(DDAO-d31)。向DDAO的胶束相(L1)、正六边形相(HI)和立方相(I)中添加短杆菌肽D会引起相分离,形成两相区,所有两相区均包含层状相(Lα)。与DDAO-d31/H2O的Lα相和HI相中的相应序参相比,含有短杆菌肽的Lα相的DDAO-d31序参更大。Lα相可与相图中的任何其他相保持平衡。在NMR时间尺度上,共存相之间的DDAO交换很慢,这就是记录的NMR谱由样品中不同相的叠加谱组成的原因。短杆菌肽D仅能大量溶解于DDAO-d31的层状相中。液晶相中短杆菌肽含量的增加导致分子有序度持续增加,直至约5 mol%的短杆菌肽时达到平稳状态。这与最近一个理论模型一致,该模型描述了一种疏水厚度大于脂质双层的膜蛋白对脂质有序性的影响。在将肽掺入脂质聚集体时用于溶解短杆菌肽的溶剂对DDAO-d31的2H-NMR线形没有影响。得出的结论是,短杆菌肽溶解于Lα相中,并且它总是采用通道构象,与特定溶剂无关。圆二色性研究也支持通道构象。在一些样品中,观察到了脂质聚集体的宏观取向。得出的结论是,二元体系中的DDAO-d31倾向于烃链长轴垂直于磁场的取向,而当存在短杆菌肽D时,烃链平行于磁场取向。这是因为短杆菌肽的螺旋轴与磁场平行排列,从而也迫使DDAO-d31分子获得这样的取向。