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Label-Free Characterization of Peptide-Lipid Interactions Using Immobilized Lipodisks

机译:使用固定化脂盘的肽-脂相互作用的无标签表征。

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摘要

Lipodisks, planar lipid bilayer structures stabilized by PEG-ylated lipids, were in the present study covalently bound and immobilized onto sensors for quartz crystal microbalance with dissipation monitoring (QCM-D) studies. It is shown that the modified sensors can be used to characterize the interaction of lipodisks with α-helical amphiphilic peptides with an accuracy similar to that obtained with well established fluorimetric approximations. The method presented has the great advantage that it can be used with peptides in their native form even if no fluorescent residues are present. The potential of the method is illustrated by determining the parameters describing the association of melittin, mastoparan X, and mastoparan with immobilized lipodisks. Both thermodynamic and kinetic analyses are possible. The presented method constitutes a useful tool for fundamental studies of peptide-membrane interactions and can also be applied to optimize the design of lipodisks, for example, for sustained release of antimicrobial peptides in therapeutic applications.
机译:在本研究中,通过聚乙二醇化的脂质稳定的平面脂质双层结构的脂膜共价结合并固定在传感器上,用于通过耗散监测(QCM-D)研究的石英晶体微天平。结果表明,改进的传感器可用于表征脂盘与α-螺旋两亲性肽的相互作用,其准确性与通过完善的荧光近似获得的准确度相似。提出的方法具有很大的优势,即使没有荧光残基,也可以与天然形式的肽一起使用。该方法的潜力通过确定描述蜂毒肽,马索帕兰X和马索帕兰与固定化脂盘的关联的参数来说明。热力学和动力学分析都是可能的。所提出的方法构成了用于肽-膜相互作用的基础研究的有用工具,并且还可以用于优化脂盘的设计,例如在治疗应用中持续释放抗微生物肽。

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