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首页> 外文期刊>MBio >The Emergence of Successful Streptococcus pyogenes Lineages through Convergent Pathways of Capsule Loss and Recombination Directing High Toxin Expression
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The Emergence of Successful Streptococcus pyogenes Lineages through Convergent Pathways of Capsule Loss and Recombination Directing High Toxin Expression

机译:成功的化脓性链球菌谱系通过胶囊丢失和重组指导高毒素表达的收敛途径出现

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Gene transfer and homologous recombination in Streptococcus pyogenes has the potential to trigger the emergence of pandemic lineages, as exemplified by lineages of emm 1 and emm 89 that emerged in the 1980s and 2000s, respectively. Although near-identical replacement gene transfer events in the nga (NADase) and slo (streptolysin O) loci conferring high expression of these toxins underpinned the success of these lineages, extension to other emm genotype lineages is unreported. The emergent emm 89 lineage was characterized by five regions of homologous recombination additional to nga-slo , including complete loss of the hyaluronic acid capsule synthesis locus hasABC , a genetic trait replicated in two other leading emm types and recapitulated by other emm types by inactivating mutations. We hypothesized that other leading genotypes may have undergone similar recombination events. We analyzed a longitudinal data set of genomes from 344 clinical invasive disease isolates representative of locations across England, dating from 2001 to 2011, and an international collection of S. pyogenes genomes representing 54 different genotypes and found frequent evidence of recombination events at the nga - slo locus predicted to confer higher toxin genotype. We identified multiple associations between recombination at this locus and inactivating mutations within hasAB , suggesting convergent evolutionary pathways in successful genotypes. This included common genotypes emm 28 and emm 87. The combination of no or low capsule and high expression of nga and slo may underpin the success of many emergent S. pyogenes lineages of different genotypes, triggering new pandemics, and could change the way S. pyogenes causes disease.
机译:化脓性链球菌中的基因转移和同源重组有可能触发大流行谱系的出现,例如分别在1980年代和2000年代出现的emm 1和emm 89世系就是例证。尽管赋予这些毒素高表达的Nga(NADase)和slo(链球菌溶血素O)位点的近乎相同的替代基因转移事件巩固了这些谱系的成功,但尚未报道将其延伸至其他emm基因型谱系。出现的emm 89谱系的特征是nga-slo以外的五个同源重组区域,包括透明质酸胶囊合成位点hasABC的完全丧失,透明质酸胶囊合成基因hasABC的遗传特性在其他两个领先的emm类型中复制,并通过失活突变被其他emm类型概括。 。我们假设其他先导基因型可能经历了类似的重组事件。我们分析了2001年至2011年代表英格兰各地的344个临床侵袭性疾病分离株的基因组纵向数据集,以及代表54种不同基因型的化脓性链球菌基因组的国际收集,并发现了在nga发生重组事件的频繁证据-单个位点预计将赋予更高的毒素基因型。我们确定了在该基因座的重组与hasAB内的失活突变之间的多种关联,表明成功基因型的趋同进化途径。其中包括常见的基因型emm 28和emm87。无或低荚膜以及nga和slo的高表达可能结合了许多不同基因型的新兴化脓性链球菌谱系的成功,引发了新的大流行,并可能改变S的流行方式。化脓性疾病引起疾病。

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