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Genome Analysis of Clostridium difficile PCR Ribotype 014 Lineage in Australian Pigs and Humans Reveals a Diverse Genetic Repertoire and Signatures of Long-Range Interspecies Transmission

机译:难辨梭状芽孢杆菌PCR Ribotype 014谱系在澳大利亚猪和人类中的基因组分析揭示了多样的遗传资源和远距离种间传播的特征。

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摘要

Clostridium difficile PCR ribotype (RT) 014 is well-established in both human and porcine populations in Australia, raising the possibility that C. difficile infection (CDI) may have a zoonotic or foodborne etiology. Here, whole genome sequencing and high-resolution core genome phylogenetics were performed on a contemporaneous collection of 40 Australian RT014 isolates of human and porcine origin. Phylogenies based on MLST (7 loci, STs 2, 13, and 49) and core orthologous genes (1260 loci) showed clustering of human and porcine strains indicative of very recent shared ancestry. Core genome single nucleotide variant (SNV) analysis found 42% of human strains showed a clonal relationship (separated by ≤2 SNVs in their core genome) with one or more porcine strains, consistent with recent inter-host transmission. Clones were spread over a vast geographic area with 50% of the human cases occurring without recent healthcare exposure. These findings suggest a persistent community reservoir with long-range dissemination, potentially due to agricultural recycling of piggery effluent. We also provide the first pan-genome analysis for this lineage, characterizing its resistome, prophage content, and in silico virulence potential. The RT014 is defined by a large “open” pan-genome (7587 genes) comprising a core genome of 2296 genes (30.3% of the total gene repertoire) and an accessory genome of 5291 genes. Antimicrobial resistance genotypes and phenotypes varied across host populations and ST lineages and were characterized by resistance to tetracycline [tetM, tetA(P), tetB(P) and tetW], clindamycin/erythromycin (ermB), and aminoglycosides (aph3-III-Sat4A-ant6-Ia). Resistance was mediated by clinically important mobile genetic elements, most notably Tn6194 (harboring ermB) and a novel variant of Tn5397 (harboring tetM). Numerous clinically important prophages (Siphoviridae and Myoviridae) were identified as well as an uncommon accessory gene regulator locus (agr3). Conservation in the pathogenicity locus and S-layer correlated with ST affiliation, further extending the concept of clonal C. difficile lineages. This study provides novel insights on the genetic variability and strain relatedness of C. difficile RT014, a lineage of emerging One Health importance. Ongoing molecular and genomic surveillance of strains in humans, animals, food, and the environment is imperative to identify opportunities to reduce the overall CDI burden.
机译:艰难梭菌PCR核糖型(RT)014在澳大利亚的人类和猪群中均已确立,这增加了艰难梭菌感染(CDI)可能具有人畜共患病或食源性病因的可能性。在这里,对人类和猪源性的40个澳大利亚RT014分离株的同期收集进行了全基因组测序和高分辨率核心基因组系统发育。基于MLST(7个基因座,STs 2、13和49)和核心直系同源基因(1260个基因座)的系统发育显示,人和猪株聚类,表明它们具有近来共有的血统。核心基因组单核苷酸变异(SNV)分析发现,有42%的人类病毒株与一种或多种猪毒株之间存在克隆关系(由其核心基因组中的≤2SNV分隔),与最近的宿主间传播一致。克隆散布在广阔的地理区域,其中有50%的人类病例是在近期没有医疗保健接触的情况下发生的。这些发现表明,可能是由于对猪场废水进行农业回收,造成了长期分布的社区水库。我们还为该谱系提供了第一个全基因组分析,以表征其抵抗力,噬菌体含量和计算机病毒毒力潜力。 RT014由大型“开放式”泛基因组(7587个基因)定义,该基因组包含2296个基因的核心基因组(占总基因组的30.3%)和5291个基因的辅助基因组。抗菌素耐药基因型和表型随宿主群体和ST谱系的不同而变化,其特征是对四环素[tetM,tetA(P),tetB(P)和tetW],克林霉素/红霉素(ermB)和氨基糖苷(aph3-III-Sat4A -ant6-Ia)。耐药性是由临床上重要的移动遗传因子介导的,其中最著名的是Tn6194(携带ermB)和Tn5397的新型变异体(携带tetM)。鉴定出许多临床上重要的原噬菌体(Siphoviridae和Myoviridae),以及罕见的辅助基因调节基因座(agr3)。致病性基因座和S层中的保守性与ST隶属关系有关,进一步扩展了艰难梭菌谱系的概念。这项研究提供了关于艰难梭菌RT014的遗传变异性和菌株相关性的新颖见解,这是新兴的“一生”重要性系列。必须对人类,动物,食物和环境中的菌株进行持续的分子和基因组监测,以发现减少总体CDI负担的机会。

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