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Shiga toxin 2 translocation across intestinal epithelium is linked to virulence of Shiga toxin-producing Escherichia coli in humans

机译:志贺毒素2跨肠上皮易位与人类产生志贺毒素的大肠杆菌的毒力有关

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摘要

Shiga toxin-producing Escherichia coli (STEC) are characterized by the release of potent Shiga toxins (Stx), which are associated with severe intestinal and renal disease. Although all STEC strains produce Stx, only a few serotypes cause infection in humans. To determine which virulence traits in vitro are linked to human disease in vivo, 13 Stx2a-producing STEC strains of seropathotype (SPT) A or B (associated with severe human intestinal disease and outbreaks) and 6 strains of SPT D or E (rarely or not linked to human disease) were evaluated in a microaerobic human colonic epithelial infection model. All SPT strains demonstrated similar growth, colonization of polarized T84 colon carcinoma cells and Stx release into the medium. In contrast, Stx translocation across the T84 cell monolayer was significantly lower in SPT group DE compared to SPT group AB strains. Further experiments showed that Stx penetration occurred via a transcellular pathway and was independent of bacterial type III secretion and attaching and effacing lesion formation. These results suggest that the extent of Stx transcytosis across the gut epithelium may represent an important indicator of STEC pathogenicity for humans.
机译:产生志贺毒素的大肠埃希菌(STEC)的特征是释放出了严重的志贺毒素(Stx),这与严重的肠道和肾脏疾病有关。尽管所有STEC菌株均产生Stx,但只有少数血清型会引起人类感染。为了确定体外哪些毒力特性与体内人类疾病相关,我们选择了13种产生Stx2a的血清型(SPT)A或B的STEC菌株(与严重的人类肠道疾病和暴发相关),以及6种SPT D或E的菌株(罕见或(与人类疾病无关)在有氧人类结肠上皮感染模型中进行了评估。所有SPT菌株均表现出相似的生长,极化的T84结肠癌细胞的定殖和Stx释放到培养基中。相反,与SPT组AB株相比,SPT组DE中跨T84细胞单层的Stx转运明显更低。进一步的实验表明,Stx的渗透是通过跨细胞途径发生的,并且与细菌III型分泌以及附着和消失的病变形成无关。这些结果表明跨肠上皮的Stx胞吞作用的程度可能代表了人类STEC致病性的重要指标。

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