Department of Microbiology, Schulich School of Medicine and Dentistry, Siebens Drake Research Institute and Centre for Human Immunology, University of Western Ontario, London ON, Canada. martin.mcgavin@ schulich.uwo.ca
Front Cell Infect Microbiol. 2012 Apr 9;2:48. doi: 10.3389/fcimb.2012.00048. eCollection 2012.
Staphylococcus aureus clonal complex CC30 has caused infectious epidemics for more than 60 years, and, therefore, provides a model system to evaluate how evolution has influenced the disease potential of closely related strains. In previous multiple genome comparisons, phylogenetic analyses established three major branches that evolved from a common ancestor. Clade 1, comprised of historic pandemic phage type 80/81 methicillin susceptible S. aureus (MSSA), and Clade 2 comprised of contemporary community acquired methicillin resistant S. aureus (CA-MRSA) were hyper-virulent in murine infection models. Conversely, Clade 3 strains comprised of contemporary hospital associated MRSA (HA-MRSA) and clinical MSSA exhibited attenuated virulence, due to common single nucleotide polymorphisms (SNP's) that abrogate production of α-hemolysin Hla, and interfere with signaling of the accessory gene regulator agr. We have now completed additional in silico genome comparisons of 15 additional CC30 genomes in the public domain, to assess the hypothesis that Clade 3 has evolved to favor niche adaptation. In addition to SNP's that influence agr and hla, other common traits of Clade 3 include tryptophan auxotrophy due to a di-nucleotide deletion within trpD, a premature stop codon within isdH encoding an immunogenic cell surface protein involved in iron acquisition, loss of a genomic toxin-antitoxin (TA) addiction module, acquisition of S. aureus pathogenicity islands SaPI4, and SaPI2 encoding toxic shock syndrome toxin tst, and increased copy number of insertion sequence ISSau2, which appears to target transcription terminators. Compared to other Clade 3 MSSA, S. aureus MN8, which is associated with Staphylococcal toxic shock syndrome, exhibited a unique ISSau2 insertion, and enhanced production of toxic shock syndrome toxin encoded by SaPI2. Cumulatively, our data support the notion that Clade 3 strains are following an evolutionary blueprint toward niche-adaptation.
金黄色葡萄球菌克隆复合体 CC30 已经引起了超过 60 年的传染病流行,因此为评估进化如何影响密切相关菌株的疾病潜力提供了一个模型系统。在之前的多次全基因组比较中,系统发育分析确立了从共同祖先进化而来的三个主要分支。第 1 组,由历史上的流行噬菌体 80/81 型甲氧西林敏感金黄色葡萄球菌(MSSA)组成,以及第 2 组,由当代社区获得性耐甲氧西林金黄色葡萄球菌(CA-MRSA)组成,在小鼠感染模型中具有高度毒性。相反,由当代医院相关耐甲氧西林金黄色葡萄球菌(HA-MRSA)和临床 MSSA 组成的第 3 组菌株由于常见的单核苷酸多态性(SNP)而导致α-溶血素 Hla 的产生缺失,并干扰辅助基因调节剂 agr 的信号转导,表现出减弱的毒力。我们现在已经完成了在公共领域中另外 15 个 CC30 基因组的额外的计算机基因组比较,以评估以下假设:第 3 组已经进化以有利于生态位适应。除了影响 agr 和 hla 的 SNP 之外,第 3 组的其他常见特征还包括色氨酸营养缺陷,这是由于 trpD 内的二核苷酸缺失引起的;isdH 编码的免疫原性细胞表面蛋白参与铁摄取的提前终止密码子;基因组毒素-抗毒素(TA)成瘾模块的缺失;获得金黄色葡萄球菌致病性岛 SaPI4 和编码中毒性休克综合征毒素 tst 的 SaPI2;以及插入序列 ISSau2 的拷贝数增加,这似乎针对转录终止子。与其他第 3 组 MSSA 相比,与葡萄球菌中毒性休克综合征相关的金黄色葡萄球菌 MN8 表现出独特的 ISSau2 插入,并增强了 SaPI2 编码的中毒性休克综合征毒素的产生。总之,我们的数据支持以下观点:第 3 组菌株正在遵循生态位适应的进化蓝图。
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