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Reactive Oxygen Species-Dependent Innate Immune Mechanisms Control Methicillin-Resistant Staphylococcus aureus Virulence in the Drosophila Larval Model

机译:反应性氧物种依赖性先天免疫机制对照甲氧西蛋白抗性<命名含量含量型=“属型”> <斜视>果蝇的葡萄球菌毒力幼虫模型

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ABSTRACT Antibiotic-resistant Staphylococcus aureus strains constitute a major public health concern worldwide and are responsible for both health care- and community-associated infections. Here, we establish a robust and easy-to-implement model of oral S. aureus infection using Drosophila melanogaster larvae that allowed us to follow the fate of S. aureus at the whole-organism level as well as the host immune responses. Our study demonstrates that S. aureus infection triggers H _(2)O _(2) production by the host via the Duox enzyme, thereby promoting antimicrobial peptide production through activation of the Toll pathway. Staphylococcal catalase mediates H _(2)O _(2) neutralization, which not only promotes S. aureus survival but also minimizes the host antimicrobial response, hence reducing bacterial clearance in vivo . We show that while catalase expression is regulated in vitro by the accessory gene regulatory system (Agr) and the general stress response regulator sigma B (SigB), it no longer depends on these two master regulators in vivo . Finally, we confirm the versatility of this model by demonstrating the colonization and host stimulation capabilities of S. aureus strains belonging to different sequence types (CC8 and CC5) as well as of two other bacterial pathogens, Salmonella enterica serovar Typhimurium and Shigella flexneri . Thus, the Drosophila larva can be a general model to follow in vivo the innate host immune responses triggered during infection by human pathogens.
机译:摘要抗生素抗金黄色葡萄球菌菌株构成全球主要的公共卫生问题,负责医疗保健和社区相关的感染。在这里,我们建立了使用果蝇马拉替洛斯克幼虫的稳健且易于实现的口腔桂葡萄球菌感染模型,使我们能够在全生物水平以及宿主免疫应答中遵循S.UUREUS的命运。我们的研究表明,S.UUREUS感染通过DUOX酶通过宿主触发H _(2)O _(2),从而通过激活Toll途径来促进抗微生物肽产生。葡萄球菌过氧化氢酶介导H _(2)o _(2)中和,这不仅促进了金黄色葡萄球菌存活,而且最小化了宿主抗微生物反应,因此降低了体内细菌间隙。我们表明,在辅助基因调节系统(AGR)和一般应激反应调节器Sigma B(Sigb)中对过氧化氢酶表达进行调节,而不再取决于这两种母稳调节剂在体内。最后,我们通过证明属于不同序列类型(CC8和CC5)的殖民化和宿主刺激能力以及另外两种细菌病原体,沙门氏菌肠道毛孢菌和Shigella Flexeri,确认了该模型的多功能性。因此,果蝇幼虫可以是遵循体内的一般模型,在人类病原体感染期间触发的先天宿主免疫应答。

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