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短杆菌肽A及相关肽抗生素——离子通道模型

Alamethicin and related peptaibols--model ion channels.

作者信息

Sansom M S

机构信息

Laboratory of Molecular Biophysics, University of Oxford, UK.

出版信息

Eur Biophys J. 1993;22(2):105-24. doi: 10.1007/BF00196915.

Abstract

Peptaibols are considered as models of those ion channels which consist of a bundle of transbilayer helices surrounding a central pore. X-Ray diffraction and NMR studies have yielded high resolution structures for several peptaibols. In conjunction with other spectroscopic investigations and molecular dynamics simulations, these studies suggest that peptaibols form proline-kinked alpha-helices, and that there may be "hinge-bending" movement of the helix in the region of the central proline residue. The amphipathicity of peptaibol helices is analyzed in relation to their channel-forming properties. Studies of the interactions of peptaibols with lipid bilayers suggest that they are helical when in a membrane-like environment, and that the helix orientation relative to the bilayer is sensitive to the peptaibol:lipid ratio, and to the degree of hydration of the bilayer. Electrical studies reveal that many peptaibols form multiple-conductance level channels in a voltage-dependent fashion. Analysis of conductance levels provides support for the "barrel stave" model of channel formation, whereby different conductance levels correspond to different numbers of monomers in a helix bundle. Alternative models for voltage-activation are discussed, and the roles of molecular dipoles and of hinge-bending in this process are considered. Two molecular models for an N = 6 bundle of alamethicin helices are presented and their electrostatic properties analyzed. The relevance of studies of peptaibols to channel and transport proteins in general is considered.

摘要

短杆菌肽被视为由围绕中心孔的一束跨膜螺旋组成的离子通道模型。X射线衍射和核磁共振研究已得出几种短杆菌肽的高分辨率结构。结合其他光谱研究和分子动力学模拟,这些研究表明短杆菌肽形成脯氨酸扭结的α螺旋,并且在中心脯氨酸残基区域螺旋可能存在“铰链弯曲”运动。分析了短杆菌肽螺旋的两亲性与其通道形成特性的关系。对短杆菌肽与脂质双层相互作用的研究表明,它们在类似膜的环境中呈螺旋状,并且螺旋相对于双层的取向对短杆菌肽与脂质的比例以及双层的水合程度敏感。电学研究表明,许多短杆菌肽以电压依赖的方式形成多电导水平的通道。对电导水平的分析为通道形成的“桶板”模型提供了支持,即不同的电导水平对应于螺旋束中不同数量的单体。讨论了电压激活的替代模型,并考虑了分子偶极子和铰链弯曲在此过程中的作用。提出了一个由6个短杆菌酪肽螺旋组成的束的两种分子模型,并分析了它们的静电性质。总体上考虑了短杆菌肽研究与通道及转运蛋白的相关性。

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