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aurein 2.3的功能由倾斜取向的α-螺旋结构支持。

Aurein 2.3 functionality is supported by oblique orientated α-helical formation.

作者信息

Mura Manuela, Dennison Sarah R, Zvelindovsky Andrei V, Phoenix David A

机构信息

Computational Physics Group and Institute for nanotechnology and Bioengineering, University of Central Lancashire, Preston PR1 2HE, UK.

出版信息

Biochim Biophys Acta. 2013 Feb;1828(2):586-94. doi: 10.1016/j.bbamem.2012.08.019. Epub 2012 Aug 31.

Abstract

In this study, an amphibian antimicrobial peptide, aurein 2.3, was predicted to use oblique orientated α-helix formation in its mechanism of membrane destabilisation. Molecular dynamic (MD) simulations and circular dichroism (CD) experimental data suggested that aurein 2.3 exists in solution as unstructured monomers and folds to form predominantly α-helical structures in the presence of a dimyristoylphosphatidylcholine membrane. MD showed that the peptide was highly surface active, which supported monolayer data where the peptide induced surface pressure changes>34 mNm(-1). In the presence of a lipid membrane MD simulations suggested that under hydrophobic mismatch the peptide is seen to insert via oblique orientation with a phenylalanine residue (PHE3) playing a key role in the membrane interaction. There is evidence of snorkelling leucine residues leading to further membrane disruption and supporting the high level of lysis observed using calcein release assays (76%). Simulations performed at higher peptide/lipid ratio show peptide cooperativity is key to increased efficiency leading to pore-formation.

摘要

在本研究中,一种两栖抗菌肽aurein 2.3被预测在其膜去稳定化机制中采用倾斜取向的α-螺旋形成方式。分子动力学(MD)模拟和圆二色性(CD)实验数据表明,aurein 2.3在溶液中以无结构的单体形式存在,在二肉豆蔻酰磷脂酰胆碱膜存在的情况下折叠形成主要为α-螺旋的结构。MD显示该肽具有高表面活性,这支持了单层数据,即该肽诱导表面压力变化>34 mN/m(-1)。在脂质膜存在的情况下,MD模拟表明,在疏水不匹配的情况下,该肽通过倾斜取向插入,其中一个苯丙氨酸残基(PHE3)在膜相互作用中起关键作用。有证据表明亮氨酸残基的“ snorkelling”导致进一步的膜破坏,并支持使用钙黄绿素释放测定法观察到的高水平裂解(76%)。在更高的肽/脂质比下进行的模拟表明,肽的协同作用是提高导致孔形成效率的关键。

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