Leavis Helen L, Willems Rob J L, van Wamel Willem J B, Schuren Frank H, Caspers Martien P M, Bonten Marc J M
Eijkman-Winkler Institute for Medical Microbiology, Infectious Diseases and Inflammation, University Medical Center Utrecht, Utrecht, The Netherlands.
PLoS Pathog. 2007 Jan;3(1):e7. doi: 10.1371/journal.ppat.0030007.
Enterococcus faecium, an ubiquous colonizer of humans and animals, has evolved in the last 15 years from an avirulent commensal to the third most frequently isolated nosocomial pathogen among intensive care unit patients in the United States. E. faecium combines multidrug resistance with the potential of horizontal resistance gene transfer to even more pathogenic bacteria. Little is known about the evolution and virulence of E. faecium, and genomic studies are hampered by the absence of a completely annotated genome sequence. To further unravel its evolution, we used a mixed whole-genome microarray and hybridized 97 E. faecium isolates from different backgrounds (hospital outbreaks (n = 18), documented infections (n = 34) and asymptomatic carriage of hospitalized patients (n = 15), and healthy persons (n = 15) and animals (n = 21)). Supported by Bayesian posterior probabilities (PP = 1.0), a specific clade containing all outbreak-associated strains and 63% of clinical isolates was identified. Sequencing of 146 of 437 clade-specific inserts revealed mobile elements (n = 74), including insertion sequence (IS) elements (n = 42), phage genes (n = 6) and plasmid sequences (n = 26), hypothetical (n = 58) and membrane proteins (n = 10), and antibiotic resistance (n = 9) and regulatory genes (n = 11), mainly located on two contigs of the unfinished E. faecium DO genome. Split decomposition analysis, varying guanine cytosine content, and aberrant codon adaptation indices all supported acquisition of these genes through horizontal gene transfer with IS16 as the predicted most prominent insert (98% sensitive, 100% specific). These findings suggest that acquisition of IS elements has facilitated niche adaptation of a distinct E. faecium subpopulation by increasing its genome plasticity. Increased genome plasticity was supported by higher diversity indices (ratio of average genetic similarities of pulsed-field gel electrophoresis and multi locus sequence typing) for clade-specific isolates. Interestingly, the previously described multi locus sequence typing-based clonal complex 17 largely overlapped with this clade. The present data imply that the global emergence of E. faecium, as observed since 1990, represents the evolution of a subspecies with a presumably better adaptation than other E. faecium isolates to the constraints of a hospital environment.
屎肠球菌是人和动物中普遍存在的定植菌,在过去15年里,它已从一种无毒共生菌演变为美国重症监护病房患者中第三常见的医院病原体。屎肠球菌兼具多重耐药性,还具有将水平抗性基因转移至更多病原菌的潜力。人们对屎肠球菌的进化和毒力知之甚少,由于缺乏完整注释的基因组序列,基因组研究受到了阻碍。为了进一步揭示其进化过程,我们使用了混合全基因组微阵列,对97株来自不同背景的屎肠球菌分离株进行杂交(医院暴发菌株(n = 18)、确诊感染菌株(n = 34)、住院患者无症状携带菌株(n = 15)、健康人菌株(n = 15)以及动物菌株(n = 21))。在贝叶斯后验概率(PP = 1.0)的支持下,鉴定出一个特定分支,其中包含所有与暴发相关的菌株以及63%的临床分离株。对437个分支特异性插入片段中的146个进行测序,发现了移动元件(n = 74),包括插入序列(IS)元件(n = 42)、噬菌体基因(n = 6)和质粒序列(n = 26)、假设蛋白(n = 58)和膜蛋白(n = 10),以及抗生素抗性基因(n = 9)和调控基因(n = 11),这些元件主要位于未完成的屎肠球菌DO基因组的两条重叠群上。分裂分解分析、鸟嘌呤胞嘧啶含量变化以及异常密码子适应指数均支持这些基因是通过以IS16为预测最突出插入片段的水平基因转移获得的(敏感性98%,特异性100%)。这些发现表明,IS元件的获得通过增加其基因组可塑性促进了一个独特屎肠球菌亚群对生态位的适应。分支特异性分离株更高的多样性指数(脉冲场凝胶电泳和多位点序列分型的平均遗传相似性之比)支持了基因组可塑性的增加。有趣的是,先前描述的基于多位点序列分型的克隆复合体17与该分支在很大程度上重叠。目前的数据表明,自1990年以来观察到的屎肠球菌在全球范围内的出现代表了一个亚种的进化,该亚种可能比其他屎肠球菌分离株更能适应医院环境的限制。
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