首页> 外文期刊>The Journal of Infectious Diseases >Penicillin-binding protein 7/8 contributes to the survival of Acinetobacter baumannii in vitro and in vivo.
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Penicillin-binding protein 7/8 contributes to the survival of Acinetobacter baumannii in vitro and in vivo.

机译:青霉素结合蛋白7/8有助于鲍曼不动杆菌在体外和体内的存活。

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BACKGROUND: Acinetobacter baumannii is a bacterial pathogen of increasing medical importance. Little is known about genes important for its survival in vivo. METHODS AND RESULTS: Screening of random transposon mutants of the model pathogen AB307-0294 identified the mutant AB307.27. AB307.27 contained its transposon insertion in pbpG, which encodes the putative low-molecular-mass penicillin-binding protein 7/8 (PBP-7/8). AB307.27 was significantly killed in ascites (P<.001), but its growth in Luria-Bertani broth was similar to that of its parent, AB307-0294 (P=.13). The survival of AB307.27 was significantly decreased in a rat soft-tissue infection model (P<.001) and a rat pneumonia model (P=.002), compared with AB307-0294. AB307.27 was significantly killed in 90% human serum in vitro, compared with AB307-0294 (P<.001). Electron microscopy demonstrated more coccobacillary forms of AB307.27, compared with AB307-0294, suggesting a possible modulation in the peptidoglycan, which may affect susceptibility to host defense factors. CONCLUSIONS: These findings demonstrate that PBP-7/8 contributes to the pathogenesis of A. baumannii. PBP-7/8 either directly or indirectly contributes to the resistance of AB307-0294 to complement-mediated bactericidal activity. An understanding of how PBP-7/8 contributes to serum resistance will lend insight into the role of this low-molecular-mass PBP whose function is poorly understood.
机译:背景:鲍曼不动杆菌是一种具有越来越重要的医学意义的细菌病原体。对其在体内存活重要的基因知之甚少。方法和结果:对模型病原体AB307-0294的随机转座子突变体进行筛选,鉴定出突变体AB307.27。 AB307.27将其转座子插入pbpG,该pbpG编码假定的低分子质量青霉素结合蛋白7/8(PBP-7 / 8)。 AB307.27在腹水中被杀死(P <.001),但在Luria-Bertani肉汤中的生长与其母本AB307-0294相似(P = .13)。与AB307-0294相比,在大鼠软组织感染模型(P <.001)和大鼠肺炎模型(P = .002)中,AB307.27的存活率显着降低。与AB307-0294相比,AB307.27在体外90%的人血清中被杀死(P <.001)。电子显微镜显示,与AB307-0294相比,AB307.27的球菌形式更多,这表明肽聚糖可能存在调节作用,这可能会影响宿主防御因子的敏感性。结论:这些发现表明PBP-7 / 8有助于鲍曼不动杆菌的发病机理。 PBP-7 / 8直接或间接有助于AB307-0294对补体介导的杀菌活性的抗性。了解PBP-7 / 8如何促进血清抗药性将有助于深入了解这种功能未知的低分子PBP的作用。

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