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时相分析血管内皮屏障的破坏

Time-resolved analysis of invading the endothelial barrier.

机构信息

Department of Medical Microbiology, University of Groningen, University Medical Center Groningen , Groningen, The Netherlands.

Department of Nanomedicine and Drug Targeting, Groningen Research Institute of Pharmacy, University of Groningen , Groningen, The Netherlands.

出版信息

Virulence. 2020 Dec;11(1):1623-1639. doi: 10.1080/21505594.2020.1844418.

Abstract

is a leading cause of infections world-wide. Once this pathogen has reached the bloodstream, it can invade different parts of the human body by crossing the endothelial barrier. Infected endothelial cells may be lysed by bacterial products, but the bacteria may also persist intracellularly, where they are difficult to eradicate with antibiotics and cause relapses of infection. Our present study was aimed at investigating the fate of methicillin resistant (MRSA) isolates of the USA300 lineage with different epidemiological origin inside endothelial cells. To this end, we established two infection models based on primary human umbilical vein endothelial cells (HUVEC), which mimic conditions of the endothelium when infection occurs. For comparison, the laboratory strain HG001 was used. As shown by flow cytometry and fluorescence- or electron microscopy, differentiation of HUVEC into a cell barrier with cell-cell junctions sets limits to the rates of bacterial internalization, the numbers of internalized bacteria, the percentage of infected cells, and long-term intracellular bacterial survival. Clear strain-specific differences were observed with the HG001 strain infecting the highest numbers of HUVEC and displaying the longest intracellular persistence, whereas the MRSA strains reproduced faster intracellularly. Nonetheless, all internalized bacteria remained confined in membrane-enclosed LAMP-1-positive lysosomal or vacuolar compartments. Once internalized, the bacteria had a higher propensity to persist within the differentiated endothelial cell barrier, probably because internalization of lower numbers of bacteria was less toxic. Altogether, our findings imply that intact endothelial barriers are more likely to sustain persistent intracellular infection.

摘要

是全球范围内感染的主要原因。一旦这种病原体进入血液,它就可以穿过内皮屏障侵入人体的不同部位。受感染的内皮细胞可能会被细菌产物溶解,但细菌也可能在细胞内持续存在,在那里它们很难被抗生素根除,并导致感染复发。我们目前的研究旨在调查具有不同流行病学起源的 USA300 谱系耐甲氧西林金黄色葡萄球菌(MRSA)分离株在血管内皮细胞内的命运。为此,我们建立了两种基于原代人脐静脉内皮细胞(HUVEC)的感染模型,模拟了感染发生时内皮的条件。为了比较,使用了实验室菌株 HG001。如流式细胞术、荧光或电子显微镜所示,HUVEC 分化为具有细胞-细胞连接的细胞屏障,限制了细菌内化的速度、内化细菌的数量、感染细胞的百分比和长期的细胞内细菌存活。HG001 菌株感染 HUVEC 的数量最多,细胞内存活时间最长,表现出明显的菌株特异性差异,而 MRSA 菌株在细胞内的繁殖速度更快。尽管如此,所有内化的细菌仍然局限在膜封闭的 LAMP-1 阳性溶酶体或空泡腔内。一旦内化,细菌在分化的内皮细胞屏障内持续存在的可能性更高,可能是因为内化的细菌数量较少毒性较低。总之,我们的发现表明完整的内皮屏障更有可能维持持续的细胞内感染。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6b22/7714425/b6783743a0d5/KVIR_A_1844418_F0001_OC.jpg

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