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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Membrane perturbation by the antimicrobial peptide PMAP-23: a fluorescence and molecular dynamics study.
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Membrane perturbation by the antimicrobial peptide PMAP-23: a fluorescence and molecular dynamics study.

机译:抗菌肽PMAP-23对膜的扰动:荧光和分子动力学研究。

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摘要

Several bioactive peptides exert their biological function by interacting with cellular membranes. Structural data on their location inside lipid bilayers are thus essential for a detailed understanding of their mechanism of action. We propose here a combined approach in which fluorescence spectroscopy and molecular dynamics (MD) simulations were applied to investigate the mechanism of membrane perturbation by the antimicrobial peptide PMAP-23. Fluorescence spectra, depth-dependent quenching experiments, and peptide-translocation assays were employed to determine the location of the peptide inside the membrane. MD simulations were performed starting from a random mixture of water, lipids and peptide, and following the spontaneous self-assembly of the bilayer. Both experimental and theoretical data indicated a peptide location just below the polar headgroups of the membrane, with an orientation essentially parallel to the bilayer plane. These findings, together with experimental results on peptide-induced leakage from large and giant vesicles, lipid flip-flop and peptide exchange between vesicles, support a mechanism of action consistent with the "carpet" model. Furthermore, the atomic detail provided by the simulations suggested the occurrence of an additional, more specific and novel mechanism of bilayer destabilization by PMAP-23, involving the unusual insertion of charged side chains into the hydrophobic core of the membrane.
机译:几种生物活性肽通过与细胞膜相互作用而发挥其生物学功能。因此,有关它们在脂质双层中的位置的结构数据对于详细了解其作用机理至关重要。我们在这里提出一种组合的方法,其中荧光光谱和分子动力学(MD)模拟被应用于研究抗菌肽PMAP-23对膜扰动的机制。荧光光谱,深度依赖性猝灭实验和肽易位测定法用于确定肽在膜内的位置。 MD模拟是从水,脂质和肽的随机混合物开始,并在双层的自发自组装之后进行的。实验和理论数据均表明肽的位置恰好在膜的极性头基下方,其取向基本平行于双层平面。这些发现以及关于肽诱导的大泡和大泡泄漏,脂质翻转和小泡之间的肽交换的实验结果,支持了与“地毯”模型一致的作用机理。此外,模拟提供的原子细节表明,发生了PMAP-23双层失稳的另一种更具体新颖的机制,其中涉及带电侧链异常插入膜的疏水核中。

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