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肺炎链球菌的体外生物膜形成及胆碱结合蛋白-DNA复合物的形成

In vitro biofilm development of Streptococcus pneumoniae and formation of choline-binding protein-DNA complexes.

作者信息

Domenech Mirian, Ruiz Susana, Moscoso Miriam, García Ernesto

机构信息

Departamento de Microbiología Molecular y Biología de las Infecciones, Centro de Investigaciones Biológicas (CIB-CSIC), Madrid, 28040, Spain.

CIBER de Enfermedades Respiratorias (CIBERES), Madrid, Spain.

出版信息

Environ Microbiol Rep. 2015 Oct;7(5):715-27. doi: 10.1111/1758-2229.12295. Epub 2015 Jun 18.

DOI:10.1111/1758-2229.12295
PMID:25950767
Abstract

Extracellular deoxyribonucleic acid (eDNA) is an essential component of bacterial biofilm matrices, and is required in their formation and maintenance. Extracellular DNA binds to exopolysaccharides or extracellular proteins, affording biofilms greater structural integrity. Recently, we reported evidence of intercellular eDNA-LytC complexes in pneumococcal biofilms. The LytC lysozyme is a member of the choline-binding family of proteins (CBPs) located on the pneumococcal surface. The present work shows that other CBPs, i.e. LytA, LytB, Pce, PspC and CbpF, which have a pI between 5 and 6, can bind DNA in vitro. This process requires the presence of divalent cations other than Mg(2+). This DNA binding capacity of CBPs appears to be independent of their enzymatic activity and, at least in the case of LytA, does not require the choline-binding domain characteristic of CBPs. Positively charged, surface-exposed, 25 amino acid-long peptides derived from the catalytic domain of LytB, were also found capable of DNA binding through electrostatic interactions. Confocal laser scanning microcopy revealed the existence of cell-associated LytB-eDNA complexes in Streptococcus pneumoniae biofilms. These and other findings suggest that these surface-located proteins of S. pneumoniae could play roles of varying importance in the colonization and/or invasion of human host where different environmental conditions exist.

摘要

细胞外脱氧核糖核酸(eDNA)是细菌生物膜基质的重要组成部分,在生物膜的形成和维持过程中不可或缺。细胞外DNA与胞外多糖或胞外蛋白结合,赋予生物膜更高的结构完整性。最近,我们报道了肺炎球菌生物膜中存在细胞间eDNA-LytC复合物的证据。LytC溶菌酶是位于肺炎球菌表面的胆碱结合蛋白家族(CBPs)的成员。目前的研究表明,其他pI在5至6之间的CBPs,即LytA、LytB、Pce、PspC和CbpF,在体外能够结合DNA。这一过程需要除Mg(2+)之外的二价阳离子存在。CBPs的这种DNA结合能力似乎与其酶活性无关,至少就LytA而言,不需要CBPs特有的胆碱结合结构域。从LytB催化结构域衍生的带正电荷、暴露于表面的25个氨基酸长的肽段,也被发现能够通过静电相互作用结合DNA。共聚焦激光扫描显微镜显示肺炎链球菌生物膜中存在细胞相关的LytB-eDNA复合物。这些以及其他发现表明,肺炎链球菌这些位于表面的蛋白可能在存在不同环境条件的人类宿主的定植和/或入侵过程中发挥不同程度的重要作用。

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