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Influence of Membrane-Fusogen Distance on the Secondary Structure of Fusogenic Coiled Coil Peptides

机译:膜致致致致致纺织卷线肽二次结构的影响

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Liposomal membrane fusion is an important tool to study complex biological fusion mechanisms. We use lipidated derivatives of the specific heterodimeric coiled coil pair E: (EIAALEK)(3) and K: (KIAALKE)(3) to study and control the fusion of liposomes. In this model system, peptides are tethered to their liposomes via a poly(ethylene glycol) (PEG) spacer and a lipid anchor. The efficiency of the fusion mechanism and function of the peptides is highly affected by the PEG-spacer length and the lipid anchor type. Here, the influence of membrane-fusogen distance on the peptide-membrane interactions and the peptide secondary structures is studied with Langmuir film balance and infrared reflection absorption spectroscopy. We found that the introduction of a spacer to monolayer-tethered peptide E changes its conformation from solvated random coils to homo-oligomers. In contrast, the described peptide-monolayer interaction of peptide K is not affected by the PEG-spacer length. Furthermore, the coexistence of different conformations when both lipopeptides E and K are present at the membrane surface is demonstrated empirically, which has many implications for the design of effective fusogenic recognition units and the field of artificial membrane fusion.
机译:脂质体膜融合是研究复杂生物融合机制的重要工具。我们使用特定的异二聚体卷绕线圈对e:(Eiaalek)(3)和K:(kiaalke)(3)来研究和控制脂质体融合的脂质衍生物。在该模型系统中,肽通过聚(乙二醇)(PEG)间隔物和脂质锚来将其拴在其脂质体上。熔融机理和肽的功能的效率受到PEG - 间隔长度和脂质锚固型的高度影响。这里,用朗米尔薄膜平衡和红外反射吸收光谱研究了膜 - 致密孔对肽 - 膜相互作用和肽二次结构的影响。我们发现将间隔物引入单层拴肽E将其与溶剂化的无规卷材的构象变化为同种寡聚体。相反,所述肽K的所述肽 - 单层相互作用不受PEG - 间隔物长度的影响。此外,脂肪肽E和K在膜表面存在时不同构象的共存,其经验上证明了对有效沉重识别单元和人工膜融合领域的设计具有许多影响。

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