首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Toroidal pores formed by antimicrobial peptides show significant disorder.
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Toroidal pores formed by antimicrobial peptides show significant disorder.

机译:由抗菌肽形成的环形孔显示出明显的紊乱。

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摘要

A large variety of antimicrobial peptides have been shown to act, at least in vitro, by poration of the lipid membrane. The nanometre size of these pores, however, complicates their structural characterization by experimental techniques. Here we use molecular dynamics simulations, to study the interaction of a specific class of antimicrobial peptides, melittin, with a dipalmitoylphosphatidylcholine bilayer in atomic detail. We show that transmembrane pores spontaneously form above a critical peptide to lipid ratio. The lipid molecules bend inwards to form a toroidally shaped pore but with only one or two peptides lining the pore. This is in strong contrast to the traditional models of toroidal pores in which the peptides are assumed to adopt a transmembrane orientation. We find that peptide aggregation, either prior or after binding to the membrane surface, is a prerequisite to pore formation. The presence of a stable helical secondary structure of the peptide, however is not. Furthermore, results obtained with modified peptides point to the importance of electrostatic interactions in the poration process. Removing the charges of the basic amino-acid residues of melittin prevents pore formation. It was also found that in the absence of counter ions pores not only form more rapidly but lead to membrane rupture. The rupture process occurs via a novel recursive poration pathway, which we coin the Droste mechanism.
机译:已经显示出各种各样的抗微生物肽至少在体外通过脂质膜的渗透起作用。然而,这些孔的纳米尺寸通过实验技术使它们的结构表征复杂化。在这里,我们使用分子动力学模拟,详细研究了特定类别的抗菌肽,蜂毒肽与二棕榈酰磷脂酰胆碱双层的相互作用。我们显示跨膜孔自发形成以上关键的肽与脂质的比率。脂质分子向内弯曲以形成环形孔,但只有一个或两个肽排在孔中。这与传统的环形孔模型形成鲜明对比,在传统的环形孔模型中,假定肽采用跨膜取向。我们发现,在与膜表面结合之前或之后的肽聚集是孔形成的先决条件。但是,该肽没有稳定的螺旋二级结构。此外,用修饰的肽获得的结果指出了在渗透过程中静电相互作用的重要性。除去蜂毒素的碱性氨基酸残基的电荷可防止孔形成。还发现在不存在抗衡离子的情况下,孔不仅形成得更快,而且导致膜破裂。破裂过程通过新颖的递归渗透途径发生,我们称之为Droste机制。

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