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Complete genome assembly and characterization of an outbreak strain of the causative agent of swine erysipelas – Erysipelothrix rhusiopathiae SY1027

机译:完整的基因组组装和猪丹毒引起病原体暴发性菌株Erysipelothrix rhusiopathiae SY1027的鉴定

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Background Erysipelothrix rhusiopathiae is the causative agent of animal erysipelas and, to a fewer occurrences, human erysipeloid. It is ubiquitous in nature and commensal in diverse species of animals, wild or domestic, from mammals and birds to reptiles and fish. Mechanisms of its virulence and pathogenicity are poorly understood. Results Making use of the complete genome sequencing of E. rhusiopathiae strain SY1027 and comparative genome analysis between the three highly pathogenic strains (SY1027, Fujisawa and ATCC19414), the genomic structure and putative functional elements, such as pathogenicity island (PAI)-like regions, potential virulence factors and horizontal transferring genes of the bacteria are identified. Strain SY1027 genome is 1,752,910 base pairs long, just 30 kilobases smaller than strain Fujisawa, with the same GC level of 36.36%. It contains 1,845 open reading frames (ORF) predicted by GLIMMER 3.02, of which 1,775 were annotated by PGAAP, 1,757 (~95.23%) were annotated by NCBI nr blast, 1,209 by COG database and 1,076 by KEGG database. 37 potential virulence factors were annotated in strain SY1027 by VFDB, while 19 (~51.35%) of them are common in the 2 strains, 7 of which are potentially related to antibiotic resistance and highly conserved (~98-100% match identity (ID)) amongst the three strains of E. rhusiopathiae and modestly homologous to other gastrointestinal tract-inhabiting Firmicutes (~40% match ID), e.g. Clostridium spp., Enterococcus spp. Genomic island- and pathogenicity island-like regions were also predicted, in which some showed association with tRNA and potential virulence factors. Conclusion Complete genome sequencing of Erysipelothrix rhusiopathiae, the causative agent of animal erysipelas, was performed. Molecular identification of various genomic elements pave the way to the better understanding of mechanisms underlying metabolic capabilities, pathogenicity of swine erysipelas and prospective vaccine targets besides the widely used SpaA antigens.
机译:背景红斑丹毒丝菌是动物丹毒的病原体,在少数情况下是人类丹毒的病原体。它在自然界是普遍存在的,在哺乳动物或鸟类到爬行动物和鱼类的各种野生或家养动物中都很普遍。对其毒力和致病性的机制了解甚少。结果利用了风疹大肠杆菌SY1027的完整基因组测序,并比较了三种高致病性菌株(SY1027,Fujisawa和ATCC19414),基因组结构和假定的功能元件(如致病岛(PAI)样区域)之间的比较基因组分析,确定了细菌的潜在毒力因子和水平转移基因。 SY1027菌株的基因组长1,752,910个碱基对,比藤泽菌株小30 kb,而相同的GC水平为36.36%。它包含GLIMMER 3.02预测的1,845个开放阅读框(ORF),其中1,775个由PGAAP注释,1,757个(约95.23%)由NCBI nr blast注释,1,209个由COG数据库注释,1,076个由KEGG数据库注释。 VFDB在SY1027菌株中注释了37种潜在毒力因子,而在这2株菌株中共有19种(〜51.35%)是常见的,其中7种可能与抗生素抗性有关,并且具有高度保守性(〜98-100%匹配同一性(ID ))在三种风湿性大肠杆菌病菌株中,并且与其他胃肠道硬膜菌(约40%匹配ID)具有中等同源性,例如梭状芽孢杆菌,肠球菌还预测了基因组岛状和致病性岛状区域,其中一些区域显示与tRNA和潜在的毒力因子相关。结论进行了动物丹毒的致病病原体红斑丹毒丝菌的完整基因组测序。除广泛使用的SpaA抗原外,各种基因组元素的分子鉴定为更好地理解潜在的代谢能力,猪丹毒的致病性和预期的疫苗靶标铺平了道路。

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