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β-溶血性咽峡炎链球菌 sag 操纵子同源物中编码的新型双链球菌溶血素 S 样肽。

Novel twin streptolysin S-like peptides encoded in the sag operon homologue of beta-hemolytic Streptococcus anginosus.

机构信息

Department of Biological Science and Technology, Life System, Institute of Technology and Science, The University of Tokushima Graduate School, Minamijosanjima-cho, Tokushima, Japan.

出版信息

J Bacteriol. 2013 Mar;195(5):1090-9. doi: 10.1128/JB.01344-12. Epub 2013 Jan 4.

DOI:10.1128/JB.01344-12
PMID:23292771
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3571330/
Abstract

Streptococcus anginosus is a member of the anginosus group streptococci, which form part of the normal human oral flora. In contrast to the pyogenic group streptococci, our knowledge of the virulence factors of the anginosus group streptococci, including S. anginosus, is not sufficient to allow a clear understanding of the basis of their pathogenicity. Generally, hemolysins are thought to be important virulence factors in streptococcal infections. In the present study, a sag operon homologue was shown to be responsible for beta-hemolysis in S. anginosus strains by random gene knockout. Interestingly, contrary to pyogenic group streptococci, beta-hemolytic S. anginosus was shown to have two tandem sagA homologues, encoding streptolysin S (SLS)-like peptides, in the sag operon homologue. Gene deletion and complementation experiments revealed that both genes were functional, and these SLS-like peptides were essential for beta-hemolysis in beta-hemolytic S. anginosus. Furthermore, the amino acid sequence of these SLS-like peptides differed from that of the typical SLS of S. pyogenes, especially in their propeptide domain, and an amino acid residue indicated to be important for the cytolytic activity of SLS in S. pyogenes was deleted in both S. anginosus homologues. These data suggest that SLS-like peptides encoded by two sagA homologues in beta-hemolytic S. anginosus may be potential virulence factors with a different structure essential for hemolytic activity and/or the maturation process compared to the typical SLS present in pyogenic group streptococci.

摘要

咽峡炎链球菌是酿脓链球菌群的一员,属于人类口腔正常菌群。与化脓性链球菌群不同,我们对酿脓链球菌群包括咽峡炎链球菌在内的毒力因子的了解还不足以清楚地了解其致病基础。通常认为,溶血素是链球菌感染的重要毒力因子。在本研究中,通过随机基因敲除显示 sag 操纵子同源物负责咽峡炎链球菌菌株的β-溶血。有趣的是,与化脓性链球菌群相反,β-溶血的咽峡炎链球菌在 sag 操纵子同源物中显示出两个串联的 sagA 同源物,编码链球菌溶血素 S(SLS)样肽。基因缺失和互补实验表明这两个基因都是功能性的,这些 SLS 样肽对于β-溶血的咽峡炎链球菌的β-溶血是必不可少的。此外,这些 SLS 样肽的氨基酸序列与化脓性链球菌的典型 SLS 不同,特别是在它们的前肽结构域中,并且在化脓性链球菌中对 SLS 细胞溶解活性很重要的一个氨基酸残基在两个咽峡炎链球菌同源物中被删除。这些数据表明,β-溶血的咽峡炎链球菌中由两个 sagA 同源物编码的 SLS 样肽可能是潜在的毒力因子,与化脓性链球菌群中存在的典型 SLS 相比,其结构不同,对于溶血活性和/或成熟过程是必不可少的。

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