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首页> 外文期刊>Journal of Clinical Microbiology >Evaluation of Molecular Methods for Serotyping Shigella flexneri
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Evaluation of Molecular Methods for Serotyping Shigella flexneri

机译:弗氏志贺氏菌血清分型的分子方法评价

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摘要

Shigella flexneri can be phenotypically serotyped using antisera raised to type-specific somatic antigens and group factor antigens and genotypically serotyped using PCR targeting O-antigen synthesis or modification genes. The aim of this study was to evaluate a real-time PCR for serotyping S. flexneri and to use whole-genome sequencing (WGS) to investigate the phenotypic and genotypic serotype identifications. Of the 244 cultures tested retrospectively, 226 (92.6%) had concordant results between phenotypic serotyping and PCR. Seventy of the 244 isolates (including 15 of the 18 isolates where a serotype-PCR mismatch was identified) were whole-genome sequenced, and the serotype was derived from the genome. Discrepant results between the phenotypic and genotypic tests were attributed to insertions/deletions or point mutations identified in O-antigen synthesis or modification genes, rendering them dysfunctional; inconclusive serotyping results due to nonspecific cross-reactions; or novel genotypes. Phylogenetic analysis of the WGS data indicated that the serotype, regardless of whether it was phenotypically or genotypically determined, was a weak predictor of phylogenetic relationships between strains of S. flexneri. WGS data provided both genome-derived serotyping, thus supporting backward compatibility with historical data and facilitating data exchange in the community, and more robust and discriminatory typing at the single-nucleotide-polymorphism level.
机译:弗氏志贺氏菌可以使用针对特定类型的体细胞抗原和群因子抗原的抗血清进行表型血清分型,并使用靶向O抗原合成或修饰基因的PCR进行基因型血清分型。这项研究的目的是评估实时PCR进行弗氏链球菌血清分型,并使用全基因组测序(WGS)来研究表型和基因型血清型鉴定。回顾性测试的244种培养物中,有226种(92.6%)在表型血清分型和PCR之间具有一致的结果。对244个分离株中的70个(包括在18个分离株中鉴定出血清型-PCR错配的15个分离株)进行了全基因组测序,并且血清型来源于基因组。表型和基因型测试之间的差异是由于O抗原合成或修饰基因中发现的插入/缺失或点突变,导致它们功能失调。由于非特异性交叉反应,无法得出确定的血清分型结果;或新的基因型。 WGS数据的系统发育分析表明,无论是表型还是基因型确定的血清型,都是弗氏链球菌菌株之间系统发生关系的弱预测因子。 WGS数据提供了基因组衍生的血清型,从而支持了与历史数据的向后兼容性,并促进了社区中的数据交换,并在单核苷酸多态性水平上提供了更强大且更具区分性的分型。

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