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The role of bacterial size shape and surface in macrophage engulfment of uropathogenic E. coli cells

机译:细菌大小、形状和表面在尿路致病性大肠杆菌细胞巨噬细胞吞噬中的作用

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摘要

Uropathogenic Escherichia coli (UPEC) can undergo extensive filamentation in the host during acute urinary tract infections (UTIs). It has been hypothesised that this morphological plasticity allows bacteria to avoid host immune responses such as macrophage engulfment. However, it is still unclear what properties of filaments are important in macrophage-bacteria interactions. The aim of this work was to investigate the contribution of bacterial biophysical parameters, such as cell size and shape, and physiological parameters, such as cell surface and the environment, to macrophage engulfment efficiency. Viable, reversible filaments of known lengths and volumes were produced in the UPEC strain UTI89 using a variety of methods, including exposure to cell-wall targeting antibiotics, genetic manipulation and isolation from an in vitro human bladder cell model. Quantification of the engulfment ability of macrophages using gentamicin-protection assays and fluorescence microscopy demonstrated that the ability of filaments to avoid macrophage engulfment is dependent on a combination of size (length and volume), shape, cell surface and external environmental factors. UTI89 filamentation and macrophage engulfment efficiency were also found to occur independently of the SOS-inducible filamentation genes, sulA and ymfM in both in vivo and in vitro models of infection. Compared to filaments formed via antibiotic inhibition of division, the infection-derived filaments were preferentially targeted by macrophages. With several strains of UPEC now resistant to current antibiotics, our work identifies the importance of bacterial physiological and morphological states during infection.
机译:尿路致病性大肠杆菌 (UPEC) 在急性尿路感染 (UTI) 期间可在宿主体内发生广泛的丝状形成。据推测,这种形态可塑性使细菌能够避免宿主免疫反应,例如巨噬细胞吞噬。然而,目前尚不清楚细丝的哪些特性在巨噬细胞-细菌相互作用中很重要。这项工作的目的是研究细菌生物物理参数(如细胞大小和形状)和生理参数(如细胞表面和环境)对巨噬细胞吞噬效率的影响。使用多种方法在 UPEC 菌株 UTI89 中产生已知长度和体积的活的可逆细丝,包括暴露于细胞壁靶向抗生素、遗传操作和从体外人膀胱细胞模型中分离。使用庆大霉素保护测定和荧光显微镜对巨噬细胞吞噬能力的定量表明,细丝避免巨噬细胞吞噬的能力取决于大小(长度和体积)、形状、细胞表面和外部环境因素的组合。在体内和体外感染模型中,还发现 UTI89 细丝化和巨噬细胞吞噬效率独立于 SOS 诱导的细丝基因 sulA 和 ymfM 发生。与通过抗生素抑制分裂形成的细丝相比,感染衍生的细丝优先成为巨噬细胞的靶点。由于几种 UPEC 菌株现在对当前的抗生素具有耐药性,我们的工作确定了感染期间细菌生理和形态状态的重要性。
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