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2b型菌毛对无乳链球菌ST-17菌株所致侵袭性疾病的作用

Contribution of pilus type 2b to invasive disease caused by a Streptococcus agalactiae ST-17 strain.

作者信息

Lazzarin Maddalena, Mu Rong, Fabbrini Monica, Ghezzo Claudia, Rinaudo C Daniela, Doran Kelly S, Margarit Immaculada

机构信息

GSK S.r.l., Siena, Italy.

Department of Biology and Center for Microbial Sciences, San Diego State University, 5500 Campanile Dr., NLS 317, San Diego, CA, 92182, USA.

出版信息

BMC Microbiol. 2017 Jul 3;17(1):148. doi: 10.1186/s12866-017-1057-8.

Abstract

BACKGROUND

Group B Streptococcus (GBS) is a major cause of invasive disease especially in neonates. In GBS three structurally distinct pilus polymers have been identified as important virulence factors and promising vaccine candidates. The vast majority of Group B Streptococci belonging to the hypervirulent serotype III ST-17 lineage bear pilus types 1 and 2b. The purpose of this study was to investigate the relative contribution of these two pilus types to the pathogenesis of a ST-17 strain.

RESULTS

We performed in vivo and in vitro analysis of isogenic knockout mutants derived from the GBS COH1 ST-17 strain deprived of either pilus type 1 or 2b. We compared the two pilus mutants with the wild type strain in a mouse model of invasive disease, in vitro survival in macrophages, and adherence/invasion assays using human brain endothelial and lung epithelial cell lines. Significantly less of the pilus 2b mutant was recovered from the blood, lungs and brain tissue of infected mice compared to the wild-type and pilus 1 mutant strains. Further, while the pilus 2b mutant survived similarly in murine macrophages, it exhibited a lower capacity to adhere and invade human brain epithelial and lung endothelial cell lines.

CONCLUSIONS

The data suggest an important role of pilus 2b in mediating GBS infection and host cell interaction of strains belonging to the hypervirulent GBS ST-17 lineage.

摘要

背景

B族链球菌(GBS)是侵袭性疾病的主要病因,尤其是在新生儿中。在GBS中,已鉴定出三种结构不同的菌毛聚合物是重要的毒力因子和有前景的疫苗候选物。绝大多数属于高毒力血清型III ST-17谱系的B族链球菌携带1型和2b型菌毛。本研究的目的是调查这两种菌毛类型对ST-17菌株发病机制的相对贡献。

结果

我们对源自GBS COH1 ST-17菌株的同基因敲除突变体进行了体内和体外分析,这些突变体缺失了1型或2b型菌毛。我们在侵袭性疾病小鼠模型、巨噬细胞体外存活率以及使用人脑内皮细胞和肺上皮细胞系的黏附/侵袭试验中,将这两种菌毛突变体与野生型菌株进行了比较。与野生型和1型菌毛突变株相比,从感染小鼠的血液、肺和脑组织中回收的2b型菌毛突变体明显更少。此外,虽然2b型菌毛突变体在小鼠巨噬细胞中的存活情况相似,但它在黏附和侵袭人脑上皮细胞和肺内皮细胞系方面的能力较低。

结论

数据表明2b型菌毛在介导高毒力GBS ST-17谱系菌株的GBS感染和宿主细胞相互作用中起重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1b1/5496222/ba6dbdbf410b/12866_2017_1057_Fig1_HTML.jpg

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