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Thermodynamic Profiling of Peptide Membrane Interactions by Isothermal Titration Calorimetry: A Search for Pores and Micelles

机译:通过等温滴定量热法对肽膜相互作用的热力学分析:毛孔和胶束的搜索。

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摘要

Antimicrobial peptides are known to interact strongly with negatively charged lipid membranes, initially by peripheral insertion of the peptide into the bilayer, which for some antimicrobial peptides will be followed by pore formation, and successive solubilization of the membranes resulting in mixed peptide-lipid micelles. We have investigated the mode of action of the antimicrobial peptide mastoparan-X using isothermal titration calorimetry (ITC) and cryo-transmission electron microscopy (cryo-TEM). The results show that mastoparan-X induces a range of structural transitions of POPC/POPG (3:1) lipid membranes at different peptide/lipid ratios. It has been established that ITC can be used as a fast method for localizing membrane transitions and when combined with DLS and cryo-TEM can elucidate structural changes, including the threshold for pore formation and micellation. Cryo-TEM was employed to confirm the structural changes associated with the thermodynamic transitions found by ITC. The pore-formation process has furthermore been investigated in detail and the thermodynamic parameters of pore formation have been characterized using a system-specific temperature where the enthalpy of peptide partitioning becomes zero (Tzero). This allows for an exclusive study of the pore-formation process. The use of ITC to find Tzero allows for characterization of the thermodynamic parameters of secondary processes on lipid membranes.
机译:已知抗菌肽会与带负电荷的脂质膜发生强烈相互作用,首先是将肽外围插入双层中,对于某些抗菌肽,随后将形成孔,随后膜被溶解,从而形成混合的肽-脂质胶束。我们已经使用等温滴定热法(ITC)和低温透射电子显微镜(cryo-TEM)研究了抗微生物肽马多巴兰-X的作用方式。结果表明,在不同的肽/脂质比率下,mastopanran-X诱导了一系列POPC / POPG(3:1)脂质膜的结构转变。已经确定,ITC可以用作定位膜过渡的快速方法,当与DLS和cryo-TEM结合使用时,ITC可以阐明结构变化,包括孔形成和胶束形成的阈值。使用低温TEM来确认与ITC发现的热力学转变相关的结构变化。进一步详细地研究了孔形成过程,并使用系统特定温度表征了孔形成的热力学参数,其中肽分配的焓为零(Tzero)。这允许对孔形成过程进行专门研究。使用ITC查找Tzero可以表征脂质膜上次级过程的热力学参数。

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