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Contributions of EspA Filaments and Curli Fimbriae in Cellular Adherence and Biofilm Formation of Enterohemorrhagic Escherichia coli O157:H7

机译:EspA细丝和卷曲菌毛对肠出血性大肠杆菌O157:H7的细胞粘附和生物膜形成的贡献

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摘要

In Escherichia coli O157:H7 (O157), the filamentous structure of the type III secretion system is produced from the polymerization of the EspA protein. EspA filaments are essential for O157 adherence to epithelial cells. In previous studies, we demonstrated that O157 hha deletion mutants showed increased adherence to HEp-2 cells and produced abundant biofilms. Transcriptional analysis revealed increased expression of espA as well as the csgA gene, which encodes curli fimbriae that are essential for biofilm formation. In the present study, we constructed hha espA, hha csgA, and hha csgA espA deletion mutants to determine the relative importance of EspA and CsgA in O157 adherence to HEp-2 cells and biofilm formation. In vitro adherence assays, conducted at 37°C in a tissue culture medium containing 0.1% glucose, showed that HEp-2 cell adherence required EspA because hha espA and hha csgA espA mutants adhered to HEp-2 cells at higher levels only when complemented with an espA-expressing plasmid. Biofilm assays performed at 28°C in a medium lacking glucose showed dependency of biofilm formation on CsgA; however EspA was not produced under these conditions. Despite production of detectable levels of EspA at 37°C in media supplemented with 0.1% glucose, the biofilm formation occurred independent of EspA. These results indicate dependency of O157 adherence to epithelial cells on EspA filaments, while CsgA promoted biofilm formation under conditions mimicking those found in the environment (low temperature with nutrient limitations) and in the digestive tract of an host animal (higher temperature and low levels of glucose).
机译:在大肠杆菌O157:H7(O157)中,III型分泌系统的丝状结构是由EspA蛋白的聚合产生的。 EspA细丝对于O157粘附于上皮细胞至关重要。在以前的研究中,我们证明了O157 hha缺失突变体显示出对HEp-2细胞的粘附增加并产生了丰富的生物膜。转录分析显示espA和csgA基因表达增加,该基因编码生物膜形成必不可少的卷曲菌毛。在本研究中,我们构建了hha espA,hs csgA和hs csgA espA缺失突变体,以确定EspA和CsgA在O157粘附于HEp-2细胞和生物膜形成中的相对重要性。在37°C的含0.1%葡萄糖的组织培养基中进行的体外粘附试验表明,HEp-2细胞的粘附需要EspA,因为hha espA和hs csgA espA突变体仅在与Hep-2互补时才以较高水平粘附表达espA的质粒。在缺乏葡萄糖的培养基中于28°C进行的生物膜测定表明,生物膜形成对CsgA的依赖性。但是,在这些条件下并未产生EspA。尽管在补充0.1%葡萄糖的培养基中在37°C产生可检测水平的EspA,但生物膜的形成与EspA无关。这些结果表明,O157粘附在EspA细丝上对上皮细胞的依赖性,而CsgA在模拟环境(低温,营养有限)和宿主动物消化道(高温和低水平的肠胃道)中发现的条件下促进生物膜形成。葡萄糖)。

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