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脂-蛋白界面的结构、动力学与组成:自旋标记法的视角

Structure, dynamics and composition of the lipid-protein interface. Perspectives from spin-labelling.

作者信息

Marsh D, Horváth L I

机构信息

Max-Planck-Institut für biophysikalische Chemie, Abt. Spektroskopie, D-37070 Göttingen, Germany.

出版信息

Biochim Biophys Acta. 1998 Nov 10;1376(3):267-96. doi: 10.1016/s0304-4157(98)00009-4.

Abstract

Implications of the data on lipid-protein interactions involving integral proteins that are obtained from EPR spectroscopy with spin-labelled lipids in membranes are reviewed. The lipid stoichiometry, selectivity and exchange dynamics at the lipid-protein interface can be determined, in addition to information on the configuration and rotational dynamics of the protein-associated lipid chains. These parameters, particularly the stoichiometry and selectivity, are directly related to the intramembranous structure and degree of oligomerisation of the integral protein, and conversely may be used to study the state of assembly of such proteins in the membrane. Insertion of proteins into membranes can be studied by analogous methods. Comparison with the results obtained from integral proteins helps to define the extent of membrane penetration and degree of transmembrane crossing that are relevant to protein translocation mechanisms.

摘要

本文综述了通过电子顺磁共振波谱法(EPR)利用膜中自旋标记脂质获得的有关涉及整合蛋白的脂-蛋白相互作用的数据的意义。除了有关与蛋白相关的脂链的构型和旋转动力学的信息外,还可以确定脂-蛋白界面处的脂质化学计量、选择性和交换动力学。这些参数,特别是化学计量和选择性,与整合蛋白的膜内结构和寡聚化程度直接相关,反之,也可用于研究此类蛋白在膜中的组装状态。可以通过类似方法研究蛋白插入膜的过程。将这些结果与整合蛋白的结果进行比较,有助于确定与蛋白转运机制相关的膜穿透程度和跨膜穿越程度。

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