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Streptococcus pneumoniae TIGR4 Phase-Locked Opacity Variants Differ in Virulence Phenotypes

机译:肺炎链球菌TIGR4锁相不透明变体的毒力表型不同。

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Streptococcus pneumoniae (pneumococcus) is a leading human pathogen that can cause serious localized and invasive diseases. Pneumococci can undergo a spontaneous and reversible phase variation that is reflected in colony opacity and which allows the population to adapt to different host environments. Generally, transparent variants are adapted for nasopharyngeal colonization, whereas opaque variants are associated with invasive disease. In recent work, colony phase variation was shown to occur by means of recombination events to generate multiple alleles of the hsdS targeting domain of a DNA methylase complex, which mediates epigenetic changes in gene expression. A panel of isogenic strains were created in the well-studied S.?pneumoniae TIGR4 background that are “locked” in the transparent ( n = 4) or opaque ( n = 2) colony phenotype. The strains had significant differences in colony size which were stable over multiple passages in vitro and in vivo . While there were no significant differences in adherence for the phase-locked mutant strains to immortalized epithelial cells, biofilm formation and viability were reduced for the opaque variants in static assays. Nasopharyngeal colonization was stable for all strains, but the mortality rates differed between them. Transcript profiling by transcriptome sequencing (RNA-seq) analyses revealed that the expression levels of certain virulence factors were increased in a phase-specific manner. As epigenetic regulation of phase variation (often referred to as "phasevarion") is emerging as a common theme for mucosal pathogens, these results serve as a model for future studies of host-pathogen interactions. IMPORTANCE A growing number of bacterial species undergo epigenetic phase variation due to variable expression or specificity of DNA-modifying enzymes. For pneumococci, this phase variation has long been appreciated as being revealed by changes in colony opacity, which are reflected in changes in expression or accessibility of factors on the bacterial surface. Recent work showed that recombination-generated variation in alleles of the HsdS DNA methylase specificity subunit mediated pneumococcal phase variation. We generated phase-locked populations of S.?pneumoniae TIGR4 expressing a single nonvariant hsdS allele and observed significant differences in gene expression and virulence. These results highlight the importance of focused pathogenesis studies within specific phase types. Moreover, the generation of single-allele hsdS constructs will greatly facilitate such studies.
机译:肺炎链球菌(肺炎球菌)是一种主要的人类病原体,可引起严重的局部和侵入性疾病。肺炎球菌可经历自发和可逆的相变,反映在菌落的不透明性中,使种群能够适应不同的宿主环境。通常,透明变体适合鼻咽定植,而不透明变体与侵袭性疾病有关。在最近的工作中,显示出通过重组事件发生菌落相变化,以产生DNA甲基化酶复合物的hsdS靶向结构域的多个等位基因,其介导基因表达的表观遗传学变化。在经过充分研究的肺炎链球菌TIGR4背景中创建了一组等基因菌株,这些菌株“锁定”在透明(n = 4)或不透明(n = 2)菌落表型中。该菌株具有明显的菌落大小差异,在体外和体内多次传代时都稳定。虽然锁相突变菌株对永生化的上皮细胞的依从性没有显着差异,但在静态测定中不透明变体的生物膜形成和活力降低了。鼻咽部定植在所有菌株中均稳定,但死亡率之间存在差异。通过转录组测序(RNA-seq)分析的转录谱分析显示,某些毒力因子的表达水平以阶段特异性方式增加。由于相变的表观遗传学调控(通常称为“相变”)正在成为粘膜病原体的共同主题,这些结果可作为今后研究宿主-病原体相互作用的模型。重要由于DNA修饰酶的可变表达或特异性,越来越多的细菌种类经历了表观遗传的相变。对于肺炎球菌而言,长期以来人们一直认为这种相变是通过菌落不透明度的变化来揭示的,这反映在细菌表面因子表达或可及性的变化中。最近的工作表明,HsdS DNA甲基化酶特异性亚基的等位基因重组产生的变异介导了肺炎球菌的相变。我们生成了表达单个非hsdS等位基因的肺炎链球菌TIGR4的锁相种群,并观察到了基因表达和毒力的显着差异。这些结果突出了在特定阶段类型内进行重点发病机制研究的重要性。此外,单等位基因hsdS构建体的产生将大大促进此类研究。

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