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Membrane Topology of a 14-mer Model Amphipathic Peptide:A Solid-State NMR Spectroscopy Study

机译:14-mer模型两亲性肽的膜拓扑:固态NMR光谱研究

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We have investigated the interaction between a synthetic amphipathic 14-mer peptide and model membranes by solid-state NMR.The 14-mer peptide is composed of leucines and phenylalanines modified by the addition of crown ethers and forms a helical amphipathic structure in solution and bound to lipid membranes.To shed light on its membrane topology,31P,2H,15N solid-state NMR experiments have been performed on the 14-mer peptide in interaction with mechanically oriented bilayers of dilauroylphosphatidylcholine (DLPC),dimyristoylphosphatidylcholine (DMPC),and dipalmitoylphos-phatidylcholine (DPPC).The 31P,2H,and 15N NMR results indicate that the 14-mer peptide remains at the surface of the DLPC,DMPC,and DPPC bilayers stacked between glass plates and perturbs the lipid orientation relative to the magnetic field direction.Its membrane topology is similar in DLPC and DMPC bilayers,whereas the peptide seems to be more deeply inserted in DPPC bilayers,as revealed by the greater orientational and motional disorder of the DPPC lipid headgroup and acyl chains.15N{31P} rotational echo double resonance experiments have also been used to measure the intermolecular dipole-dipole interaction between the 14-mer peptide and the phospholipid headgroup of DMPC multilamellar vesicles,and the results indicate that the 14-mer peptide is in contact with the polar region of the DMPC lipids.On the basis of these studies,the mechanism of membrane perturbation of the 14-mer peptide is associated to the induction of a positive curvature strain induced by the peptide lying on the bilayer surface and seems to be independent of the bilayer hydrophobic thickness.
机译:我们已经通过固态NMR研究了合成的两亲性14-mer肽与模型膜之间的相互作用.14-mer肽由亮氨酸和苯丙氨酸组成,它们通过添加冠醚而修饰,并在溶液中形成螺旋状两亲结构并结合为了阐明其膜拓扑结构,已对14-mer肽与机械定位的二月桂酰磷脂酰胆碱(DLPC),二肉豆蔻酰基磷脂酰胆碱(DMPC)和二棕榈酰磷进行了机械相互作用的双层分子进行了31P,2H,15N固态NMR实验31P,2H和15N NMR结果表明14-mer肽保留在DLPC,DMPC和DPPC双层堆叠在玻璃板之间的表面上,并且扰乱了脂质相对于磁场方向的方向它的膜拓扑在DLPC和DMPC双层中相似,而该肽似乎更深地插入DPPC双层中,如更大的方向性和15N {31P}旋转回波双共振实验还用于测量14-mer肽与DMPC多层囊泡的磷脂头基之间的分子间偶极-偶极相互作用,并测定结果这表明14-mer肽与DMPC脂质的极性区域接触。在这些研究的基础上,14-mer肽的膜微扰机制与诱导由DMPC脂质诱导的正曲率应变有关。肽位于双层表面上,似乎与双层疏水厚度无关。

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