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E(z),一种用于评估氨基酸侧链插入膜中能量的深度依赖势:推导及其在确定跨膜和界面螺旋方向上的应用

E(z), a depth-dependent potential for assessing the energies of insertion of amino acid side-chains into membranes: derivation and applications to determining the orientation of transmembrane and interfacial helices.

作者信息

Senes Alessandro, Chadi Deborah C, Law Peter B, Walters Robin F S, Nanda Vikas, Degrado William F

机构信息

Deparment of Biochemistry and Molecular Biophysics, School of Medicine, University of Pennsylvania, Philadelphia, PA 19104-6059, USA.

出版信息

J Mol Biol. 2007 Feb 16;366(2):436-48. doi: 10.1016/j.jmb.2006.09.020. Epub 2006 Sep 12.

Abstract

We have developed an empirical residue-based potential (E(z) potential) for protein insertion in lipid membranes. Propensities for occurrence as a function of depth in the bilayer were calculated for the individual amino acid types from their distribution in known structures of helical membrane proteins. The propensities were then fit to continuous curves and converted to a potential using a reverse-Boltzman relationship. The E(z) potential demonstrated a good correlation with experimental data such as amino acid transfer free energy scales (water to membrane center and water to interface), and it incorporates transmembrane helices of varying composition in the membrane with trends similar to those obtained with translocon-mediated insertion experiments. The potential has a variety of applications in the analysis of natural membrane proteins as well as in the design of new ones. It can help in calculating the propensity of single helices to insert in the bilayer and estimate their tilt angle with respect to the bilayer normal. It can be utilized to discriminate amphiphilic helices that assume a parallel orientation at the membrane interface, such as those of membrane-active peptides. In membrane protein design applications, the potential allows an environment-dependent selection of amino acid identities.

摘要

我们开发了一种基于经验残基的蛋白质插入脂质膜的势能(E(z)势能)。根据螺旋膜蛋白已知结构中各氨基酸类型的分布,计算了它们在双层膜中随深度出现的倾向。然后将这些倾向拟合为连续曲线,并使用反向玻尔兹曼关系转换为势能。E(z)势能与诸如氨基酸转移自由能标度(从水到膜中心以及从水到界面)等实验数据显示出良好的相关性,并且它纳入了膜中不同组成的跨膜螺旋,其趋势与通过转运体介导的插入实验获得的趋势相似。该势能在天然膜蛋白分析以及新膜蛋白设计中具有多种应用。它有助于计算单个螺旋插入双层膜的倾向,并估计它们相对于双层膜法线的倾斜角度。它可用于区分在膜界面处呈平行取向的两亲性螺旋,例如膜活性肽的螺旋。在膜蛋白设计应用中,该势能允许根据环境选择氨基酸类型。

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