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将链球菌补体抑制剂(SIC)的各种抑制作用归因于该分子内的区域。

Attribution of the various inhibitory actions of the streptococcal inhibitor of complement (SIC) to regions within the molecule.

作者信息

Binks Michael J, Fernie-King Barbara A, Seilly David J, Lachmann Peter J, Sriprakash Kadaba S

机构信息

Queensland Institute of Medical Research, Brisbane, Queensland, Australia.

出版信息

J Biol Chem. 2005 May 20;280(20):20120-5. doi: 10.1074/jbc.M414194200. Epub 2005 Mar 15.

Abstract

Some strains of Streptococcus pyogenes secrete a virulence factor called the streptococcal inhibitor of complement (SIC) function. SIC is a polyfunctional protein that interacts with a number of host proteins and peptides, especially with those that are involved in host defense systems. In addition to inhibiting the complement-mediated lysis of cells, SIC inhibits lysozyme, secretory leukocyte proteinase inhibitor, and beta-defensins. SIC also binds to proteins associated with the cytoskeleton and thereby may cause cytoskeletal derangement. The SIC molecule has three distinct structural domains constituting the N-proximal short repeat region (SRR), the central long repeat region (LRR), and the C-proximal proline-rich region (PRR). To map various functions to the structural domains, we have analyzed recombinant subclones expressing various parts of SIC and elastase-generated discrete fragments of SIC for binding to various ligands and for determining their biological properties. The results demonstrate the following. (a) SRR alone was sufficient to confer inhibition of complement function. (b) Anti-defensin and anti-lysozyme activities were mapped to the SRR plus LRR. (c) The LRR plus PRR harbored ezrin binding activity.

摘要

某些化脓性链球菌菌株分泌一种名为补体链球菌抑制剂(SIC)功能的毒力因子。SIC是一种多功能蛋白,它与许多宿主蛋白和肽相互作用,特别是与那些参与宿主防御系统的蛋白和肽。除了抑制补体介导的细胞裂解外,SIC还抑制溶菌酶、分泌型白细胞蛋白酶抑制剂和β-防御素。SIC还与细胞骨架相关蛋白结合,从而可能导致细胞骨架紊乱。SIC分子有三个不同的结构域,分别构成N近端短重复区域(SRR)、中央长重复区域(LRR)和C近端富含脯氨酸区域(PRR)。为了将各种功能定位到结构域,我们分析了表达SIC不同部分的重组亚克隆以及SIC经弹性蛋白酶产生的离散片段与各种配体的结合情况,并确定它们的生物学特性。结果表明如下:(a)单独的SRR足以赋予补体功能抑制作用。(b)抗防御素和抗溶菌酶活性定位到SRR加LRR。(c)LRR加PRR具有埃兹蛋白结合活性。

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