首页> 外文期刊>Journal of Clinical Microbiology >Application of Whole-Genome Sequencing Data for O-Specific Antigen Analysis and In Silico Serotyping of Pseudomonas aeruginosa Isolates
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Application of Whole-Genome Sequencing Data for O-Specific Antigen Analysis and In Silico Serotyping of Pseudomonas aeruginosa Isolates

机译:全基因组测序数据在铜绿假单胞菌分离物的O特异抗原分析和计算机血清分型中的应用

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Accurate typing methods are required for efficient infection control. The emergence of whole-genome sequencing (WGS) technologies has enabled the development of genome-based methods applicable for routine typing and surveillance of bacterial pathogens. In this study, we developed the Pseudomonas aeruginosa serotyper (PAst) program, which enabled in silico serotyping of P. aeruginosa isolates using WGS data. PAst has been made publically available as a web service and aptly facilitates high-throughput serotyping analysis. The program overcomes critical issues such as the loss of in vitro typeability often associated with P. aeruginosa isolates from chronic infections and quickly determines the serogroup of an isolate based on the sequence of the O-specific antigen (OSA) gene cluster. Here, PAst analysis of 1,649 genomes resulted in successful serogroup assignments in 99.27% of the cases. This frequency is rarely achievable by conventional serotyping methods. The limited number of nontypeable isolates found using PAst was the result of either a complete absence of OSA genes in the genomes or the artifact of genomic misassembly. With PAst, P. aeruginosa serotype data can be obtained from WGS information alone. PAst is a highly efficient alternative to conventional serotyping methods in relation to outbreak surveillance of serotype O12 and other high-risk clones, while maintaining backward compatibility to historical serotype data.
机译:有效的感染控制需要准确的打字方法。全基因组测序(WGS)技术的出现使得能够开发出适用于细菌病原体常规分型和监测的基于基因组的方法。在这项研究中,我们开发了铜绿假单胞菌血清分型(PAst)程序,该程序可以使用WGS数据对铜绿假单胞菌分离株进行 in silico 血清分型。 PAst已作为Web服务公开提供,并适当地促进了高通量血清分型分析。该程序克服了一些关键问题,例如经常与慢性感染的铜绿假单胞菌分离株相关的体外丧失型性,并根据O特异性抗原(OSA)的序列快速确定了分离株的血清型。 )基因簇。在这里,对1649个基因组的PAst分析在99.27%的病例中成功完成了血清群分配。传统的血清分型方法很少能达到这个频率。使用PAst发现的数量有限的不可分型的分离物是由于基因组中OSA基因完全不存在或基因组错配伪像的结果。使用PAst,可以仅从WGS信息获得铜绿假单胞菌血清型数据。在对O12型血清型和其他高风险克隆进行暴发监测时,PAst是常规血清型方法的高效替代品,同时保持了对历史血清型数据的向后兼容性。

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