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通过X射线、中子散射和分析超速离心法测定补体成分的溶液结构

Solution structures of complement components by X-ray and neutron scattering and analytical ultracentrifugation.

作者信息

Perkins S J, Gilbert H E, Aslam M, Hannan J, Holers V M, Goodship T H

机构信息

Department of Biochemistry and Molecular Biology, Darwin Building, University College London, Gower Street, UK.

出版信息

Biochem Soc Trans. 2002 Nov;30(Pt 6):996-1001. doi: 10.1042/bst0300996.

Abstract

The short consensus/complement repeat (SCR) domain (also known as the complement control protein domain) is the most abundant domain type in the complement system. Crystal and NMR structures for proteins that contain single and multiple SCR domains have now been published. These contain inter-SCR linkers of between three and eight residues, and the structures show much variability in inter-SCR orientations. X-ray and neutron scattering, combined with analytical ultracentrifugation and constrained modelling based on known subunit structures will yield a medium-resolution structure for the protein of interest. The fewer parameters that are associated with the structure of interest, the more defined the structure of interest becomes. These solution studies have been applied to several SCR-containing proteins in the complement system, most notably Factor H with 20 SCR domains, a complement receptor type 2 fragment with two SCR domains, and rat complement receptor-related protein (Crry) which contains five SCR domains. The results show great conformational variability in the inter-SCR orientation, and these will be reviewed. Even though the rotational orientation cannot be modelled, it is nonetheless possible to measure the degree of extension of the multi-SCR proteins and, from this, to obtain functionally useful results.

摘要

短共有序列/补体重复(SCR)结构域(也称为补体控制蛋白结构域)是补体系统中最为丰富的结构域类型。目前已发表了含有单个和多个SCR结构域的蛋白质的晶体结构和核磁共振结构。这些结构包含三到八个残基的SCR间连接子,并且结构显示出SCR间取向存在很大变异性。X射线和中子散射,结合分析超速离心以及基于已知亚基结构的约束建模,将为目标蛋白质生成中等分辨率的结构。与目标结构相关的参数越少,目标结构就越明确。这些溶液研究已应用于补体系统中几种含SCR的蛋白质,最显著的是具有20个SCR结构域的因子H、具有两个SCR结构域的2型补体受体片段以及含有五个SCR结构域的大鼠补体受体相关蛋白(Crry)。结果显示SCR间取向存在很大的构象变异性,本文将对此进行综述。尽管无法对旋转取向进行建模,但仍然可以测量多SCR蛋白的伸展程度,并由此获得功能上有用的结果。

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