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首页> 外文期刊>Biophysical Chemistry: An International Journal Devoted to the Physical Chemistry of Biological Phenomena >Membrane morphology effects in quartz crystal microbalance characterization of antimicrobial peptide activity
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Membrane morphology effects in quartz crystal microbalance characterization of antimicrobial peptide activity

机译:石英晶体微稳定表征抗微生物肽活性的膜形态作用

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摘要

The mechanism of action of membrane disrupting antimicrobial peptides (AMPs) and the basis of their specificity and selectivity to pathogens are often studied by using biomimetic model membranes. It is often assumed that all model membrane morphologies, e.g. liposomes, supported bilayers, tethered bilayers etc. are equivalent. In this work the validity of this assumption was assessed. Melittin was used as the reference AMP as it can disrupt both bacterial and mammalian-mimetic membranes. Quartz crystal microbalance (QCM) viscoelastic fingerprints show characteristic differences between the three model morphologies: single bilayer membranes, multilamellar membrane stacks and unilamellar liposomes. In the second and third case, initial trends show material removal instead of material addition as in the single bilayer case, consistent with dissolution of some bilayers, and bursting liposomes, respectively. The latter is accompanied by a characteristic drop in the dissipation signal as the liposomes collapse. The results also highlight an important limitation of the QCM method, the need for a well established reference system for qualitative analysis of the viscoelastic fingerprints, and thus the importance of using the right model system, i.e. single bilayer membrane, for studies of the mechanism of action of AMPs.
机译:通过使用仿生模型膜来研究膜破坏抗微生物肽(AMPS)的作用机理及其对病原体的特异性和选择性的基础。通常假设所有模型膜形态,例如,脂质体,负载的双层,束缚双层等是等同的。在这项工作中,评估了这种假设的有效性。 Melittin用作参考放大器,因为它可以破坏细菌和哺乳动物模拟膜。石英晶体微稳态(QCM)粘弹性指纹显示三种模型形态学之间的特征差异:单双层膜,多层膜堆叠和Unilamellar脂质体之间。在第二和第三案例中,初始趋势显示出材料去除而不是单层壳体中的材料除外,与一些双层的溶解相一致,并分别筛选脂质体。后者伴随着脂质体塌陷的耗散信号中的特征下降。结果还突出了QCM方法的一个重要限制,需要采用良好的参考系统进行粘弹性指纹的定性分析,因此使用右模型系统的重要性,即单层膜,用于研究机制的研究AMPS的行动。

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