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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Cholesterol attenuates the interaction of the antimicrobial peptide gramicidin S with phospholipid bilayer membranes
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Cholesterol attenuates the interaction of the antimicrobial peptide gramicidin S with phospholipid bilayer membranes

机译:胆固醇减弱了抗菌肽短杆菌肽S与磷脂双层膜的相互作用

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摘要

We have investigated the effect of the presence of 25 mol percent cholesterol on the interactions of the antimicrobial peptide gramicidin S (GS) with phosphatidylcholine and phosphatidylethanolamine model membrane systems using a variety of methods. Our circular dichroism spectroscopic measurements indicate that the incorporation of cholesterol into egg phosphatidylcholine vesicles has no significant effect on the conformation of the GS molecule but that this peptide resides in a range of intermediate polarity as compared to aqueous solution or an organic solvent. Our Fourier transform infrared spectroscopic measurements confirm these findings and demonstrate that in both cholesterol-containing and cholesterol-free dimyristoylphosphatidylcholine liquid-crystalline bilayers, GS is located in a region of intermediate polarity at the polarnonpolar interfacial region of the lipid bilayer. However, GS appears to be located in a more polar environment nearer the bilayer surface when cholesterol is present. Our ~(31)P-nuclear magnetic resonance studies demonstrate that the presence of cholesterol markedly reduces the tendency of GS to induce the formation of inverted nonlamellar phases in model membranes composed of an unsaturated phosphatidylethanolamine. Finally, fluorescence dye leakage experiments indicate that cholesterol inhibits the GS-induced permeabilization of phosphatidylcholine vesicles. Thus in all respects the presence of cholesterol attenuates but does not abolish the interactions of GS with, and the characteristic effects of GS on, phospholipid bilayers. These findings may explain why it is more potent at disrupting cholesterol-free bacterial than cholesterol-containing eukaryotic membranes while nevertheless disrupting the integrity of the latter at higher peptide concentrations. This additional example of the lipid specificity of GS may aid in the rational design of GS analogs with increased antibacterial but reduced hemolytic activities.
机译:我们已使用多种方法研究了25摩尔%胆固醇的存在对抗菌肽短杆菌肽S(GS)与磷脂酰胆碱和磷脂酰乙醇胺模型膜系统相互作用的影响。我们的圆二色性光谱测量结果表明,将胆固醇掺入卵磷脂酰胆碱囊泡中对GS分子的构象没有显着影响,但与水溶液或有机溶剂相比,该肽存在于中间极性范围内。我们的傅里叶变换红外光谱测量结果证实了这些发现,并证明在含胆固醇和不含胆固醇的二肉豆蔻酰基磷脂酰胆碱液晶双层膜中,GS位于脂质双层的非极性界面区域的中间极性区域。但是,当存在胆固醇时,GS似乎位于更靠近双层表面的极性更大的环境中。我们的〜(31)P-核磁共振研究表明,胆固醇的存在显着降低了GS诱导由不饱和磷脂酰乙醇胺组成的模型膜中形成反相非层状相的趋势。最后,荧光染料泄漏实验表明胆固醇抑制了GS诱导的磷脂酰胆碱囊泡的透化作用。因此,在所有方面,胆固醇的存在都会减弱但不会消除GS与磷脂双层的相互作用以及GS对磷脂双层的特征性作用。这些发现可能解释了为什么它在破坏不含胆固醇的细菌方面比含胆固醇的真核膜更有效,而在更高的肽浓度下却破坏了后者的完整性。 GS的脂质特异性的这个另外的例子可以帮助具有增加的抗菌但降低的溶血活性的GS类似物的合理设计。

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