首页> 外文期刊>Frontiers in Microbiology >Prophage Excision in Streptococcus pneumoniae Serotype 19A ST320 Promote Colonization: Insight Into Its Evolution From the Ancestral Clone Taiwan 19F-14 (ST236)
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Prophage Excision in Streptococcus pneumoniae Serotype 19A ST320 Promote Colonization: Insight Into Its Evolution From the Ancestral Clone Taiwan 19F-14 (ST236)

机译:19A ST320型肺炎链球菌的噬菌体切除促进定植:从祖先克隆台湾19F-14看其进化

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Streptococcus pneumoniae 19A ST320, a multidrug-resistant strain with high disease severity that notoriously spread before the use of expanded pneumococcal conjugate vaccines, was derived from a capsular switching event between an international strain Taiwan 19F-14 (ST236) and a serotype 19A strain. However, the molecular mechanisms underlying the adaptive evolution of 19F ST236 to 19A ST320 are unknown. In this study, we compared 19A ST320 to its ancestral clone, 19F ST236, in terms of adherence to respiratory epithelial cells, whole transcriptome, and ability to colonize a young mouse model. Serotype 19A ST320 showed five-fold higher adherence to A549 cells than serotype 19F ST236. High-throughput mRNA sequencing identified a prophage region located between dnaN and ychF in both strains; however, the genes in this region were expressed at significantly higher levels in 19A ST320 than in 19F ST236. Analysis by polymerase chain reaction (PCR) showed that the prophage is able to spontaneously excise from the chromosome and form a circular episome in 19A ST320, but not in 19F ST236. Deletion of the integrase in the prophage of 19A ST320 decreased spontaneous excision and cell adherence, which were restored by complementation. Competition experiments in mice showed that the integrase mutant was six-fold less competitive than the 19A ST320 parent (competitive index [CI]: 0.16; p = 0.02). The 19A ST320 prophage-deleted strain did not change cell adherence capacity, whereas prophage integration strains ( integrase mutant and 19F) had decreased expression of the down-stream ychF gene compared to that of 19A ST320. Further deletion of ychF significantly reduced cell adherence. In conclusions, these findings suggest that spontaneous prophage induction confers a competitive advantage to virulent pneumococci.
机译:肺炎链球菌19A ST320是一种具有高度疾病严重性的多药耐药菌株,在使用扩大的肺炎球菌结合疫苗之前就已经广为传播,它源自国际菌株台湾19F-14(ST236)与血清型19A菌株之间的荚膜转换事件。但是,从19F ST236到19A ST320适应性进化的分子机制尚不清楚。在这项研究中,我们比较了19A ST320和它的祖先克隆19F ST236,它们对呼吸道上皮细胞的粘附,完整的转录组以及对年轻小鼠模型的定殖能力。血清型19A ST320对A549细胞的粘附性比血清型19F ST236高五倍。高通量mRNA测序鉴定了两个菌株中位于dnaN和ychF之间的噬菌体区域。然而,该区域的基因在19A ST320中的表达水平明显高于19F ST236。通过聚合酶链反应(PCR)的分析表明,噬菌体能够自发地从染色体上切除,并在19A ST320中形成环状附加体,而在19F ST236中则不能。 19A ST320噬菌体中整合酶的缺失减少了自发切除和细胞粘附,并通过互补得以恢复。小鼠的竞争实验表明,整合酶突变体的竞争性比19A ST320亲本低六倍(竞争指数[CI]:0.16; p = 0.02)。与19A ST320相比,删除了19A ST320噬菌体的菌株并未改变细胞的粘附能力,而噬菌体整合菌株(整合酶突变体和19F)却降低了下游ychF基因的表达。 ychF的进一步删除显着降低了细胞粘附。总而言之,这些发现表明自发的预言诱导赋予了毒性肺炎球菌竞争优势。

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