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脂质控制的肽拓扑结构和双层相互作用:协同增强 PGLa 和 Magainin 2 抗菌活性的结构见解。

Lipid-controlled peptide topology and interactions in bilayers: structural insights into the synergistic enhancement of the antimicrobial activities of PGLa and magainin 2.

机构信息

Université de Strasbourg/Centre National de la Recherche Scientifique, Institut de Chimie, Strasbourg, France.

出版信息

Biophys J. 2011 Mar 16;100(6):1473-80. doi: 10.1016/j.bpj.2011.01.070.

Abstract

To gain further insight into the antimicrobial activities of cationic linear peptides, we investigated the topology of each of two peptides, PGLa and magainin 2, in oriented phospholipid bilayers in the presence and absence of the other peptide and as a function of the membrane lipid composition. Whereas proton-decoupled (15)N solid-state NMR spectroscopy indicates that magainin 2 exhibits stable in-plane alignments under all conditions investigated, PGLa adopts a number of different membrane topologies with considerable variations in tilt angle. Hydrophobic thickness is an important parameter that modulates the alignment of PGLa. In equimolar mixtures of PGLa and magainin 2, the former adopts transmembrane orientations in dimyristoyl-, but not 1-palmitoyl-2-oleoyl-, phospholipid bilayers, whereas magainin 2 remains associated with the surface in all cases. These results have important consequences for the mechanistic models explaining synergistic activities of the peptide mixtures and will be discussed. The ensemble of data suggests that the thinning of the dimyristoyl membranes caused by magainin 2 tips the topological equilibrium of PGLa toward a membrane-inserted configuration. Therefore, lipid-mediated interactions play a fundamental role in determining the topology of membrane peptides and proteins and thereby, possibly, in regulating their activities as well.

摘要

为了更深入地了解阳离子线性肽的抗菌活性,我们研究了两种肽,PGLa 和 Magainin 2,在存在和不存在另一种肽的情况下以及作为膜脂质组成的函数,在定向磷脂双层中的拓扑结构。虽然质子去耦(15)N 固态 NMR 光谱表明 Magainin 2 在所有研究条件下均表现出稳定的平面排列,但 PGLa 采用了多种不同的膜拓扑结构,其倾斜角度有很大差异。疏水性厚度是调节 PGLa 排列的重要参数。在 PGLa 和 Magainin 2 的等摩尔混合物中,前者在二肉豆蔻酰磷脂双层中采用跨膜取向,但在 1-棕榈酰-2-油酰磷脂双层中不采用,而 Magainin 2 在所有情况下都与表面结合。这些结果对解释肽混合物协同作用的机制模型有重要影响,将进行讨论。综合数据表明,Magainin 2 引起的二肉豆蔻酰膜变薄促使 PGLa 的拓扑平衡向插入膜的构型倾斜。因此,脂质介导的相互作用在确定膜肽和蛋白质的拓扑结构方面起着重要作用,并且可能在调节它们的活性方面也起着重要作用。

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