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首页> 外文期刊>Microbes and infection >Quantification of bacterial internalization by host cells using a beta-lactamase reporter strain: Neisseria gonorrhoeae invasion into cervical epithelial cells requires bacterial viability.
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Quantification of bacterial internalization by host cells using a beta-lactamase reporter strain: Neisseria gonorrhoeae invasion into cervical epithelial cells requires bacterial viability.

机译:使用β-内酰胺酶报道菌株对宿主细胞细菌内在化的定量:淋病奈瑟氏菌侵入宫颈上皮细胞需要细菌生存能力。

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Neisseria gonorrhoeae can invade into cervical epithelial cells to overcome this host defense barrier. We developed a beta-lactamase reporter system that allowed us to quantify at the single cell level if a host cell internalized a viable or nonviable microorganism. We autodisplayed beta-lactamase on the surface of FA1090 [FA1090Phi(bla-iga')] and demonstrated by confocal fluorescence microscopy and flow cytometry that FA1090Phi(bla-iga') cleaved the beta-lactamase substrate CCF2-AM loaded into host cells only when gonococci were internalized by these host cells. While FA1090Phi(bla-iga') adhered to almost all ME180 cells, viable N. gonorrhoeae were internalized by only a subset of cells during infection. Nonviable gonococci adhered to, but were not internalized by ME180 cells, and failed to recruit F-actin to sites of adherent bacteria. Overall, we show that epithelial cell invasion is a dynamic process that requires viable N. gonorrhoeae. We demonstrate the advantages of the beta-lactamase reporter system over the gentamicin protection assay in quantifying bacterial invasion. The reporter system that we have developed can be adapted to studying the internalization of any bacterial species into any host cell.
机译:淋病奈瑟氏球菌可侵入宫颈上皮细胞以克服宿主防御障碍。我们开发了一种β-内酰胺酶报告系统,可以使我们在宿主细胞内化活的或不活的微生物时在单细胞水平上进行定量。我们在FA1090 [FA1090Phi(bla-iga')]的表面上自动展示了β-内酰胺酶,并通过共聚焦荧光显微镜和流式细胞术证明了FA1090Phi(bla-iga')裂解了仅加载到宿主细胞中的β-内酰胺酶底物CCF2-AM当淋球菌被这些宿主细胞内化时。尽管FA1090Phi(bla-iga')几乎附着于所有ME180细胞,但在感染过程中,仅一部分细胞将淋病奈瑟氏球菌内在化。不能存活的淋球菌粘附但未被ME180细胞内在化,并且未能将F-肌动蛋白募集到粘附细菌的位点。总的来说,我们表明上皮细胞浸润是一个动态过程,需要淋病奈瑟氏球菌。我们证明了庆大霉素保护定量检测细菌入侵方面,β-内酰胺酶报告系统的优势。我们开发的报告系统可以适用于研究任何细菌物种进入任何宿主细胞的内在化。

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