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A Genomic Virulence Reference Map of Enterococcus faecalis Reveals an Important Contribution of Phage03-Like Elements in Nosocomial Genetic Lineages to Pathogenicity in a Caenorhabditis elegans Infection Model

机译:粪肠球菌的基因组毒力参考图揭示了秀丽隐杆线虫感染模型中医院遗传谱系中的噬菌体类似噬菌体元素对致病性的重要贡献。

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摘要

In the present study, the commensal and pathogenic host-microbe interaction of Enterococcus faecalis was explored using a Caenorhabditis elegans model system. The virulence of 28 E. faecalis isolates representing 24 multilocus sequence types (MLSTs), including human commensal and clinical isolates as well as isolates from animals and of insect origin, was investigated using C. elegans strain glp-4 (bn2ts); sek-1 (km4). This revealed that 6 E. faecalis isolates behaved in a commensal manner with no nematocidal effect, while the remaining strains showed a time to 50% lethality ranging from 47 to 120 h. Principal component analysis showed that the difference in nematocidal activity explained 94% of the variance in the data. Assessment of known virulence traits revealed that gelatinase and cytolysin production accounted for 40.8% and 36.5% of the observed pathogenicity, respectively. However, coproduction of gelatinase and cytolysin did not increase virulence additively, accounting for 50.6% of the pathogenicity and therefore indicating a significant (26.7%) saturation effect. We employed a comparative genomic analysis approach using the 28 isolates comprising a collection of 82,356 annotated coding sequences (CDS) to identify 2,325 patterns of presence or absence among the investigated strains. Univariate statistical analysis of variance (ANOVA) established that individual patterns positively correlated (n = 61) with virulence. The patterns were investigated to identify potential new virulence traits, among which we found five patterns consisting of the phage03-like gene clusters. Strains harboring phage03 showed, on average, 17% higher killing of C. elegans (P = 4.4e−6). The phage03 gene cluster was also present in gelatinase-and-cytolysin-negative strain E. faecalis JH2-2. Deletion of this phage element from the JH2-2 clinical strain rendered the mutant apathogenic in C. elegans, and a similar mutant of the nosocomial V583 isolate showed significantly attenuated virulence. Bioinformatics investigation indicated that, unlike other E. faecalis virulence traits, phage03-like elements were found at a higher frequency among nosocomial isolates. In conclusion, our report provides a valuable virulence map that explains enhancement in E. faecalis virulence and contributes to a deeper comprehension of the genetic mechanism leading to the transition from commensalism to a pathogenic lifestyle.
机译:在本研究中,使用秀丽隐杆线虫模型系统探索粪肠球菌的共生和病原宿主-微生物相互作用。使用秀丽隐杆线虫菌株glp-4(bn2ts)研究了代表24种多基因座序列类型(MLST)的28种粪肠球菌的毒性,其中包括人类共生和临床分离株以及来自动物和昆虫的分离株。 sek-1(km4)。这表明6种粪肠球菌的分离株表现出共生性,没有杀线虫作用,而其余菌株显示出47%至120h的致死率达50%。主成分分析表明,杀线虫活性的差异解释了数据差异的94%。对已知毒力特征的评估表明,明胶酶和溶细胞素的产生分别占观察到的致病性的40.8%和36.5%。然而,明胶酶和细胞溶素的共同生产并没有增加毒力,占致病性的50.6%,因此表明有明显的(26.7%)饱和作用。我们采用了包含28,356个带注释的编码序列(CDS)的28个分离株的比较基因组分析方法,以鉴定研究菌株之间存在或不存在的2,325种模式。单变量方差统计分析(ANOVA)确定,单个模式与毒力呈正相关(n = 61)。对这些模式进行了研究,以确定潜在的新毒力性状,其中我们发现了五个由噬菌体样基因簇组成的模式。携带噬菌体03的菌株对秀丽隐杆线虫的杀伤力平均提高了17%(P = 4.4e -6 )。噬菌体基因簇也存在于明胶酶和溶细胞素阴性菌株粪肠球菌JH2-2中。从JH2-2临床菌株中删除该噬菌体元件使该突变体在秀丽隐杆线虫中具有致病性,并且类似的医院V583分离株突变体显示出明显的减毒力。生物信息学调查表明,与其他粪肠球菌的毒性特征不同,在医院分离株中发现噬菌体样元件的频率更高。总之,我们的报告提供了有价值的毒力图,可以解释粪肠球菌的毒力增强,有助于更深入地了解导致从共生向病原性生活方式转变的遗传机制。

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