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Comparative Genomic Analysis Identifies Divergent Genomic Features of Pathogenic Enterococcus cecorum Including a Type IC CRISPR-Cas System a Capsule Locus an epa-Like Locus and Putative Host Tissue Binding Proteins

机译:比较基因组分析确定了致病性肠球菌的不同基因组特征包括类型IC CRISPR-Cas系统胶囊基因座epa样基因座和推定的宿主组织结合蛋白

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摘要

Enterococcus cecorum (EC) is the dominant enteric commensal of adult chickens and contributes to the gut consortia of many avian and mammalian species. While EC infection is an uncommon zoonosis, like other enterococcal species it can cause life-threating nosocomial infection in people. In contrast to other enterococci which are considered opportunistic pathogens, emerging pathogenic strains of EC cause outbreaks of musculoskeletal disease in broiler chickens. Typical morbidity and mortality is comparable to other important infectious diseases of poultry. In molecular epidemiologic studies, pathogenic EC strains were found to be genetically clonal. These findings suggested acquisition of specific virulence determinants by pathogenic EC. To identify divergent genomic features and acquired virulence determinants in pathogenic EC; comparative genomic analysis was performed on genomes of 3 pathogenic and 3 commensal strains of EC. Pathogenic isolates had smaller genomes with a higher GC content, and they demonstrated large regions of synteny compared to commensal isolates. A molecular phylogenetic analysis demonstrated sequence divergence in pathogenic EC genomes. At a threshold of 98% identity, 414 predicted proteins were identified that were highly conserved in pathogenic EC but not in commensal EC. Among these, divergent CRISPR-cas defense loci were observed. In commensal EC, the type IIA arrangement typical for enterococci was present; however, pathogenic EC had a type IC locus, which is novel in enterococci but commonly observed in streptococci. Potential mediators of virulence identified in this analysis included a polysaccharide capsular locus similar to that recently described for E. faecium, an epa-like locus, and cell wall associated proteins which may bind host extracellular matrix. This analysis identified specific genomic regions, coding sequences, and predicted proteins which may be related to the divergent evolution and increased virulence of emerging pathogenic strains of EC.
机译:盲肠肠球菌(EC)是成年鸡的主要肠道共生体,对许多禽类和哺乳动物的肠道菌群都有贡献。尽管EC感染是一种罕见的人畜共患病,但与其他肠球菌一样,它可以引起威胁生命的医院感染。与被认为是机会性病原体的其他肠球菌相反,新兴的EC致病菌引起肉鸡爆发肌肉骨骼疾病。典型的发病率和死亡率与家禽的其他重要传染病相当。在分子流行病学研究中,发现致病性EC菌株具有基因克隆性。这些发现表明,致病性EC获得了特定的毒力决定因素。鉴定致病性EC中不同的基因组特征和获得性毒力决定因素;对3种致病性和3种共生性乳杆菌的基因组进行了比较基因组分析。致病分离株的基因组较小,GC含量较高,与普通分离株相比,它们具有较大的同义区域。分子系统发育分析表明,致病性EC基因组中的序列差异。在98%的同一性阈值下,鉴定出414种预测蛋白在致病性EC中高度保守,而在共生EC中则高度保守。其中,观察到不同的CRISPR-cas防御基因座。在普通型EC中,存在典型的肠球菌IIA型排列。然而,致病性EC具有IC型基因座,这种基因在肠球菌中很新颖,但在链球菌中很常见。在此分析中确定的潜在毒力介质包括与荚膜肠球菌最近描述的多糖荚膜基因座,epa样基因座以及可结合宿主细胞外基质的细胞壁相关蛋白。该分析鉴定了特定的基因组区域,编码序列和预测的蛋白质,这些蛋白质可能与新兴的EC致病菌株的发散进化和增加的毒力有关。

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