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全基因组剖析导致严重侵袭性疾病流行的一组 A 链球菌强毒、新近出现克隆。

Full-genome dissection of an epidemic of severe invasive disease caused by a hypervirulent, recently emerged clone of group A Streptococcus.

机构信息

Department of Pathology and Genomic Medicine, Center for Molecular and Translational Human Infectious Diseases Research, The Methodist Hospital System, Houston, Texas 77030, USA.

出版信息

Am J Pathol. 2012 Apr;180(4):1522-34. doi: 10.1016/j.ajpath.2011.12.037. Epub 2012 Feb 11.

DOI:10.1016/j.ajpath.2011.12.037
PMID:22330677
Abstract

Group A Streptococcus (GAS) causes an exceptionally broad range of infections in humans, from relatively mild pharyngitis and skin infections to life-threatening necrotizing fasciitis and toxic shock syndrome. An epidemic of severe invasive human infections caused by type emm59 GAS, heretofore an exceedingly rare cause of disease, spread west to east across Canada over a 3-year period (2006 to 2008). By sequencing the genomes of 601 epidemic, historic, and other emm59 organisms, we discovered that a recently emerged, genetically distinct emm59 clone is responsible for the Canadian epidemic. Using near-real-time genome sequencing, we were able to show spread of the Canadian epidemic clone into the United States. The extensive genome data permitted us to identify patterns of geographic dissemination as well as links between emm59 subclonal lineages that cause infections. Mouse and nonhuman primate models of infection demonstrated that the emerged clone is unusually virulent. Transmission of epidemic emm59 strains may have occurred primarily by skin contact, as suggested by an experimental model of skin transmission. In addition, the emm59 strains had a significantly impaired ability to persist in human saliva and to colonize the oropharynx of mice, and seldom caused human pharyngitis. Our study contributes new information to the rapidly emerging field of molecular pathogenomics of bacterial epidemics and illustrates how full-genome data can be used to precisely illuminate the landscape of strain dissemination during a bacterial epidemic.

摘要

A 组链球菌(GAS)可导致人类发生范围非常广泛的感染,从相对轻微的咽炎和皮肤感染到威胁生命的坏死性筋膜炎和中毒性休克综合征。在 3 年期间(2006 年至 2008 年),一种由emm59 型 GAS 引起的、以往极其罕见的严重侵袭性人类感染的流行疫情,在加拿大自西向东蔓延。通过对 601 株流行疫情株、历史株和其他 emm59 菌株的基因组进行测序,我们发现,最近出现的、遗传上截然不同的 emm59 克隆株是导致加拿大疫情的原因。通过使用近乎实时的基因组测序,我们能够显示加拿大流行克隆株在美国的传播。广泛的基因组数据使我们能够确定地理传播模式以及引起感染的 emm59 亚克隆谱系之间的联系。感染的小鼠和非人类灵长类动物模型表明,这种新出现的克隆株具有异常高的毒力。传播流行的 emm59 菌株可能主要通过皮肤接触进行,这与皮肤传播的实验模型一致。此外,emm59 菌株在人类唾液中持续存在和在小鼠口咽部定植的能力显著受损,很少引起人类咽炎。我们的研究为细菌流行疫情的分子病原体基因组学这一快速发展的领域提供了新的信息,并说明了如何利用全基因组数据来精确阐明细菌流行疫情期间菌株传播的格局。

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