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本文引用的文献

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The biology of Gram-positive sortase enzymes.革兰氏阳性分选酶的生物学特性。
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2
Sortase B, a new class of sortase in Listeria monocytogenes.分选酶B,一种单核细胞增生李斯特菌中的新型分选酶。
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Differential roles of multiple signal peptidases in the virulence of Listeria monocytogenes.多种信号肽酶在单核细胞增生李斯特菌毒力中的不同作用
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An epizootic in Swiss mice caused by a group A Streptococcus, newly designated type 50.由新命名的50型A组链球菌引起的瑞士小鼠 epizootic(动物流行病,此处可意译为动物疫情) 。 (注:epizootic这个词在医学等领域有时用动物疫情来更符合语境意译,但严格按字面意思是动物流行病,这里按要求未加额外解释,直接保留原词)
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Inactivation of the srtA gene affects localization of surface proteins and decreases adhesion of Streptococcus pneumoniae to human pharyngeal cells in vitro.srtA基因的失活影响表面蛋白的定位,并降低肺炎链球菌在体外对人咽部细胞的粘附。
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Roles of sortase in surface expression of the major protein adhesin P1, saliva-induced aggregation and adherence, and cariogenicity of Streptococcus mutans.分选酶在变形链球菌主要蛋白黏附素P1的表面表达、唾液诱导的聚集与黏附以及致龋性中的作用。
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Virulence control in group A Streptococcus by a two-component gene regulatory system: global expression profiling and in vivo infection modeling.A组链球菌中由双组分基因调控系统进行的毒力控制:全基因组表达谱分析及体内感染建模
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Inactivation of the srtA gene in Listeria monocytogenes inhibits anchoring of surface proteins and affects virulence.单核细胞增生李斯特菌中srtA基因的失活会抑制表面蛋白的锚定并影响毒力。
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一种来自化脓性链球菌的新型分选酶SrtC2将含有QVPTGV基序的表面蛋白锚定到细胞壁上。

A novel sortase, SrtC2, from Streptococcus pyogenes anchors a surface protein containing a QVPTGV motif to the cell wall.

作者信息

Barnett Timothy C, Patel Aman R, Scott June R

机构信息

Department of Microbiology and Immunology, Emory University School of Medicine, Rollins Research Center, Atlanta, GA 30322, USA.

出版信息

J Bacteriol. 2004 Sep;186(17):5865-75. doi: 10.1128/JB.186.17.5865-5875.2004.

DOI:10.1128/JB.186.17.5865-5875.2004
PMID:15317792
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC516832/
Abstract

The important human pathogen Streptococcus pyogenes (group A streptococcus GAS), requires several surface proteins to interact with its human host. Many of these are covalently linked by a sortase enzyme to the cell wall via a C-terminal LPXTG motif. This motif is followed by a hydrophobic region and charged C terminus, which are thought to retard the protein in the cell membrane to facilitate recognition by the membrane-localized sortase. Previously, we identified two sortase enzymes in GAS. SrtA is found in all GAS strains and anchors most proteins containing LPXTG, while SrtB is present only in some strains and anchors a subset of LPXTG-containing proteins. We now report the presence of a third sortase in most strains of GAS, SrtC. We show that SrtC mediates attachment of a protein with a QVPTGV motif preceding a hydrophobic region and charged tail. We also demonstrate that the QVPTGV sequence is a substrate for anchoring of this protein by SrtC. Furthermore, replacing this motif with LPSTGE, found in the SrtA-anchored M protein of GAS, leads to SrtA-dependent secretion of the protein but does not lead to its anchoring by SrtA. We conclude that srtC encodes a novel sortase that anchors a protein containing a QVPTGV motif to the surface of GAS.

摘要

重要的人类病原体化脓性链球菌(A组链球菌,GAS)需要多种表面蛋白与人类宿主相互作用。其中许多蛋白通过分选酶经由C端LPXTG基序共价连接到细胞壁。该基序之后是一个疏水区和带电荷的C末端,据认为这会使蛋白质在细胞膜中滞留,以便被膜定位的分选酶识别。此前,我们在GAS中鉴定出两种分选酶。SrtA存在于所有GAS菌株中,可锚定大多数含有LPXTG的蛋白,而SrtB仅存在于某些菌株中,可锚定一部分含有LPXTG的蛋白。我们现在报告在大多数GAS菌株中存在第三种分选酶SrtC。我们表明,SrtC介导一种在疏水区和带电荷的尾部之前具有QVPTGV基序的蛋白的附着。我们还证明,QVPTGV序列是SrtC锚定该蛋白的底物。此外,用GAS的SrtA锚定的M蛋白中发现的LPSTGE取代该基序,会导致该蛋白依赖SrtA分泌,但不会导致其被SrtA锚定。我们得出结论,srtC编码一种新型分选酶,可将含有QVPTGV基序的蛋白锚定到GAS表面。