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Experimental genital tract infection demonstrates Neisseria gonorrhoeae MtrCDE efflux pump is not required for in vivo human infection and identifies gonococcal colonization bottleneck

机译:实验性生殖道感染表明淋病奈瑟菌 MtrCDE 外排泵不是体内人类感染所必需的并确定了淋球菌定植瓶颈

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摘要

The MtrCDE efflux pump of Neisseria gonorrhoeae exports a wide range of antimicrobial compounds that the gonococcus encounters at mucosal surfaces during colonization and infection and is a known gonococcal virulence factor. Here, we evaluate the role of this efflux pump system in strain FA1090 during in vivo human male urethral infection with N. gonorrhoeae using a controlled human infection model. With the strategy of competitive infections initiated with mixtures of wild-type FA1090 and an isogenic mutant FA1090 strain that does not contain a functional MtrCDE pump, we found that the presence of the efflux pump is not required for an infection to be established in the human male urethra. This finding contrasts with previous studies of in vivo infection in the lower genital tract of female mice, which demonstrated that mutant gonococci of a different strain (FA19) lacking a functional MtrCDE pump had a significantly reduced fitness compared to their wild-type parental FA19 strain. To determine if these conflicting results are due to strain or human vs. mouse differences, we conducted a series of systematic competitive infections in female mice with the same FA1090 strains as in humans, and with FA19 strains, including mutants that do not assemble a functional MtrCDE efflux pump. Our results indicate the fitness advantage provided by the MtrCDE efflux pump during infection of mice is strain dependent. Owing to the equal fitness of the two FA1090 strains in men, our experiments also demonstrated the presence of a colonization bottleneck of N. gonorrhoeae in the human male urethra, which may open a new area of inquiry into N. gonorrhoeae infection dynamics and control.TRIAL REGISTRATION. Clinicaltrials.gov NCT03840811.
机译:淋病奈瑟菌的 MtrCDE 外排泵输出淋球菌在定植和感染过程中在粘膜表面遇到的各种抗菌化合物,是一种已知的淋球菌毒力因子。在这里,我们使用受控的人类感染模型评估了这种外排泵系统在体内人类男性尿道感染淋病奈瑟菌期间菌株 FA1090 中的作用。通过野生型 FA1090 和不包含功能性 MtrCDE 泵的同基因突变体 FA1090 菌株的混合物启动竞争性感染的策略,我们发现外排泵的存在不是在人类男性尿道中建立感染所必需的。这一发现与先前对雌性小鼠下生殖道体内感染的研究形成鲜明对比,后者表明,缺乏功能性 MtrCDE 泵的不同菌株 (FA19) 的突变淋球菌与其野生型亲本 FA19 菌株相比,适应性显着降低。为了确定这些相互矛盾的结果是由于菌株还是人类与小鼠的差异,我们在雌性小鼠中进行了一系列系统性的竞争性感染,这些小鼠具有与人类相同的 FA1090 菌株和 FA19 菌株,包括不组装功能性 MtrCDE 外排泵的突变体。我们的结果表明,MtrCDE 外排泵在小鼠感染期间提供的适应性优势是依赖于菌株的。由于两种 FA1090 菌株在男性中的适应性相等,我们的实验还证明了淋病奈瑟菌在人类男性尿道中存在定植瓶颈,这可能为淋病奈瑟菌感染动力学和控制开辟新的研究领域。试用注册。Clinicaltrials.gov NCT03840811。

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