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Experimental Evolution In Vivo To Identify Selective Pressures during Pneumococcal Colonization

机译:体内实验演化以鉴定肺炎球菌殖民过程中的选择性压力

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Experimental evolution is a powerful technique to understand how populations evolve from selective pressures imparted by the surrounding environment. With the advancement of whole-population genomic sequencing, it is possible to identify and track multiple contending genotypes associated with adaptations to specific selective pressures. This approach has been used repeatedly with model species in vitro , but only rarely in vivo . Herein we report results of replicate experimentally evolved populations of Streptococcus pneumoniae propagated by repeated murine nasal colonization with the aim of identifying gene products under strong selection as well as the population genetic dynamics of infection cycles. Frameshift mutations in one gene, dltB , responsible for incorporation of d -alanine into teichoic acids on the bacterial surface, evolved repeatedly and swept to high frequency. Targeted deletions of dltB produced a fitness advantage during initial nasal colonization coupled with a corresponding fitness disadvantage in the lungs during pulmonary infection. The underlying mechanism behind the fitness trade-off between these two niches was found to be enhanced adherence to respiratory cells balanced by increased sensitivity to host-derived antimicrobial peptides, a finding recapitulated in the murine model. Additional mutations that are predicted to affect trace metal transport, central metabolism, and regulation of biofilm production and competence were also selected. These data indicate that experimental evolution can be applied to murine models of pathogenesis to gain insight into organism-specific tissue tropisms. IMPORTANCE Evolution is a powerful force that can be experimentally harnessed to gain insight into how populations evolve in response to selective pressures. Herein we tested the applicability of experimental evolutionary approaches to gain insight into how the major human pathogen Streptococcus pneumoniae responds to repeated colonization events using a murine model. These studies revealed the population dynamics of repeated colonization events and demonstrated that in vivo experimental evolution resulted in highly reproducible trajectories that reflect the environmental niche encountered during nasal colonization. Mutations impacting the surface charge of the bacteria were repeatedly selected during colonization and provided a fitness benefit in this niche that was counterbalanced by a corresponding fitness defect during lung infection. These data indicate that experimental evolution can be applied to models of pathogenesis to gain insight into organism-specific tissue tropisms.
机译:实验进化是一种强大的技术,了解人口如何从周围环境赋予的选择性压力所发展。随着全群基因组测序的进步,可以识别和跟踪与适应性相关的多种竞争基因型,与特定的选择性压力相关。这种方法已经在体外反复使用模型物种,但仅限于体内。在此,我们报告了通过重复的小鼠鼻腔殖民化繁殖的肺炎链球菌的重复实验演化群体的结果,目的是在强烈的选择下鉴定基因产物以及感染循环的群体遗传动态。一种基因中的帧突变突变,​​DLTB,负责将D- alanine掺入细菌表面上的噻吩,反复演变并扫描到高频率。 DLTB的有针对性的缺失在初始鼻部定植期间在肺部感染期间与肺部相应的适应性缺点耦合的健身优势。在这两个核性之间的健身权衡背后的潜在机制被发现通过对宿主衍生的抗微生物肽的敏感性增加,增强对呼吸细胞的粘附性,其在鼠模型中综合的发现。还选择了预测痕量金属转运,中央代谢和对生物膜生产和能力调节的额外突变。这些数据表明,实验进化可以应用于病理发生的鼠模型,以获得对有机体特异性组织矫正性的洞察力。重要的演变是一种强大的力量,可以通过实验地利用,了解人口如何响应选择性压力而发展。在此,我们测试了实验进化方法的适用性,深入了解主要人体病原体链球菌肺炎线的敏感性如何使用鼠模型对重复的殖民化事件作出反应。这些研究揭示了重复定植事件的人口动态,并证明了在体内实验进化中产生高度可重复的轨迹,反映在鼻腔化期间遇到的环境利基。在定植期间反复选择影响细菌表面电荷的突变,并在该肺部中提供了在该肺部感染期间对应的适应性缺陷进行抗衡的适应性益处。这些数据表明,可以将实验进化应用于发病机制的模型,以获得对有机体特异性组织矫正性的洞察力。

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