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Comparative genomics of Clostridium bolteae and Clostridium clostridioforme reveals species-specific genomic properties and numerous putative antibiotic resistance determinants

机译:梭状芽胞杆菌和梭状梭菌的比较基因组学揭示了物种特异性的基因组特性和许多推定的抗生素抗性决定子

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Background Clostridium bolteae and Clostridium clostridioforme , previously included in the complex C. clostridioforme in the group Clostridium XIVa, remain difficult to distinguish by phenotypic methods. These bacteria, prevailing in the human intestinal microbiota, are opportunistic pathogens with various drug susceptibility patterns. In order to better characterize the two species and to obtain information on their antibiotic resistance genes, we analyzed the genomes of six strains of C. bolteae and six strains of C. clostridioforme, isolated from human infection. Results The genome length of C. bolteae varied from 6159 to 6398?kb, and 5719 to 6059 CDSs were detected. The genomes of C. clostridioforme were smaller, between 5467 and 5927?kb, and contained 5231 to 5916 CDSs. The two species display different metabolic pathways. The genomes of C. bolteae contained lactose operons involving PTS system and complex regulation, which contribute to phenotypic differentiation from C. clostridioforme . The Acetyl-CoA pathway, similar to that of Faecalibacterium prausnitzii , a major butyrate producer in the human gut, was only found in C. clostridioforme. The two species have also developed diverse flagella mobility systems contributing to gut colonization. Their genomes harboured many CDSs involved in resistance to beta-lactams, glycopeptides, macrolides, chloramphenicol, lincosamides, rifampin, linezolid, bacitracin, aminoglycosides and tetracyclines. Overall antimicrobial resistance genes were similar within a species, but strain-specific resistance genes were found. We discovered a new group of genes coding for rifampin resistance in C. bolteae. C. bolteae 90B3 was resistant to phenicols and linezolide in producing a 23S rRNA methyltransferase. C. clostridioforme 90A8 contained the VanB-type Tn 1549 operon conferring vancomycin resistance. We also detected numerous genes encoding proteins related to efflux pump systems. Conclusion Genomic comparison of C. bolteae and C. clostridiofrome revealed functional differences in butyrate pathways and in flagellar systems, which play a critical role within human microbiota. Most of the resistance genes detected in both species were previously characterized in other bacterial species. A few of them were related to antibiotics inactive against Clostridium spp. Some were part of mobile genetic elements suggesting that these commensals of the human microbiota act as reservoir of antimicrobial resistances.
机译:背景先前包含在梭状芽胞杆菌XIVa组中的复杂梭状芽孢杆菌中的螺栓梭状芽胞杆菌和梭状梭状芽孢杆菌,仍然很难通过表型方法进行区分。这些细菌在人类肠道菌群中占主导地位,是具有各种药物敏感性模式的机会性病原体。为了更好地表征这两个物种并获得有关其抗生素抗性基因的信息,我们分析了从人类感染中分离出来的六株克氏假单胞菌和六株梭状芽孢杆菌的基因组。结果检测到的C.boleae基因组长度为6159〜6398?kb,CDS为5719〜6059。梭状梭状芽孢杆菌的基因组较小,在5467和5927?kb之间,并包含5231至5916个CDS。这两个物种显示不同的代谢途径。螺栓隐球菌的基因组包含涉及PTS系统和复杂调控的乳糖操纵子,这有助于从梭状芽胞杆菌的表型分化。乙酰辅酶A途径类似于人肠道中主要的丁酸酯生产者普氏杆菌(Faecalibacterium prausnitzii),仅在梭状芽胞杆菌中发现。这两个物种还开发了有助于鞭毛定殖的多种鞭毛迁移系统。他们的基因组中有许多CDS,它们对β-内酰胺,糖肽,大环内酯,氯霉素,林可酰胺,利福平,利奈唑胺,杆菌肽,氨基糖苷和四环素具有抗性。在一个物种中,总体抗药性耐药基因相似,但是发现了菌株特异性抗药性基因。我们发现了一组新的基因,用于编码C. bolteae中的利福平抗性。 C.bolteae 90B3在产生23S rRNA甲基转移酶时对苯甲酚和利奈唑胺具有抗性。梭状芽胞杆菌90A8含有赋予万古霉素抗性的VanB型Tn 1549操纵子。我们还检测了许多编码与外排泵系统有关的蛋白质的基因。结论C. bolteae和C. clostridiofrome的基因组比较显示,丁酸酯途径和鞭毛系统具有功能差异,这在人类微生物群中起关键作用。在这两个物种中检测到的大多数抗性基因以前都是在其他细菌物种中鉴定的。其中一些与对梭菌属无活性的抗生素有关。一些是移动遗传元件的一部分,表明人类微生物群的这些共鸣可作为抗药性的储藏库。

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