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首页> 外文期刊>Journal of bacteriology >The N-Terminal Domain of Enterococcal Surface Protein, Esp, Is Sufficient for Esp-Mediated Biofilm Enhancement in Enterococcus faecalis
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The N-Terminal Domain of Enterococcal Surface Protein, Esp, Is Sufficient for Esp-Mediated Biofilm Enhancement in Enterococcus faecalis

机译:肠球菌表面蛋白,Esp的N末端域足以粪便肠球菌中Esp介导的生物膜增强。

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Enterococci have emerged as one of the leading causes of nosocomial bloodstream, surgical site, and urinary tract infections. More recently, enterococci have been associated with biofilms, which are bacterial communities attached to a surface and encased in an extracellular polymeric matrix. The enterococcal cell surface-associated protein, Esp, enhances biofilm formation by Enterococcus faecalis in a glucose-dependent manner. Mature Esp consists of a nonrepeat N-terminal domain and a central region made up of two types of tandem repeats followed by a C-terminal membrane-spanning and anchor domain. This study was undertaken to localize the specific domain(s) of Esp that plays a role in Esp-mediated biofilm enhancement. To achieve this objective, we constructed in-frame deletion mutants expressing truncated forms of Esp in an isogenic background. By comparing strains expressing the mutant forms of Esp to those expressing wild-type Esp, we found that the strain expressing Esp lacking the N-terminal domain formed biofilms that were quantitatively less in biovolume than the strain expressing wild-type Esp. Furthermore, an E. faecalis strain expressing only the N-terminal domain of Esp fused to a heterologous protein anchor formed biofilms that were quantitatively similar to those formed by a strain expressing full-length Esp. This suggested that the minimal region contributing to Esp-mediated biofilm enhancement in E. faecalis was confined to the nonrepeat N-terminal domain. Expression of full-length E. faecalis Esp in heterologous host systems of esp-deficient Lactococcus lactis and Enterococcus faecium did not enhance biofilm formation as was observed for E. faecalis. These results suggest that Esp may require interaction with an additional E. faecalis-specific factor(s) to result in biofilm enhancement.
机译:肠球菌已成为医院血流,手术部位和尿路感染的主要原因之一。最近,肠球菌与生物膜有关,生物膜是附着于表面并包裹在细胞外聚合物基质中的细菌群落。肠球菌细胞表面相关蛋白Esp以葡萄糖依赖性方式增强粪肠球菌的生物膜形成。成熟的Esp由一个非重复的N末端结构域和一个中央区域组成,该区域由两种类型的串联重复序列组成,随后是一个C末端跨膜结构和锚定结构域。进行这项研究以定位在Esp介导的生物膜增强中起作用的Esp的特定域。为了实现此目标,我们构建了在等基因背景中表达截短形式的Esp的框内缺失突变体。通过比较表达Esp突变形式的菌株与表达野生型Esp的菌株,我们发现缺乏N末端结构域的表达EsP的菌株形成的生物膜的生物量要比表达野生型Esp的菌株少。此外,还有一个 E。粪肠球菌仅表达Esp的N末端结构域,融合到异源蛋白质锚上,形成生物膜,其数量与表达全长Esp的菌株形成的膜相似。这表明在 E中有助于Esp介导的生物膜增强的最小区域。粪便仅限于非重复的N末端域。全长 E的表达。缺乏 esp 乳酸乳球菌粪肠球菌的异源宿主系统中的粪肠球菌没有增强生物膜的形成,如 em> E。粪便。这些结果表明,Esp可能需要与其他 E进行交互。粪便特异性因子导致生物膜增强。

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