Restriction Profiling of 23S Microheterogenic Ribosomal Repeats for Detection and Characterizing of E. coli and Their Clonal, Pathogenic, and Phylogroups

IF 1.1 Q4 MICROBIOLOGY
Parvathi Jayasree Rajagopalan Nair, Sunita Singh
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引用次数: 0

Abstract

Correlating ribosomal microheterogenicity with unique restriction profiles can prove to be an efficacious and cost-effective approach compared with sequencing for microbial identification. An attempt to peruse restriction profiling of 23S ribosomal assemblage was ventured; digestion patterns with Bfa I discriminated E. coli from its colony morphovars, while Hae III profiles assisted in establishing distinct clonal groups. Among the gene pool of 399 ribosomal sequences extrapolated from 57 E. coli genomes, varying degree of predominance (I > III > IV > II) of Hae III pattern was observed. This was also corroborated in samples collected from clinical, commensal, and environmental origin. K-12 and its descendants showed type I pattern whereas E. coli-B and its descendants exhibited type IV, both of these patterns being exclusively present in E. coli. A near-possible association between phylogroups and Hae III profiles with presumable correlation between the clonal groups and different pathovars was established. The generic nature, conservation, and barcode gap of 23S rRNA gene make it an ideal choice and substitute to 16S rRNA gene, the most preferred region for molecular diagnostics in bacteria.
23S微异质核糖体重复序列的限制性内切分析用于大肠杆菌及其克隆、致病性和系统群的检测和鉴定
与测序相比,将核糖体微异质性与独特的限制性基因图谱相关联可以证明是一种有效且具有成本效益的微生物鉴定方法。尝试仔细研究23S核糖体组合的限制性谱;Bfa I的消化模式可以区分大肠杆菌的菌落形态,而Hae III的消化模式有助于建立不同的克隆群。在57个大肠杆菌基因组推断的399个核糖体序列基因库中,观察到不同程度的优势(I > III > IV > II)。从临床、共生和环境来源收集的样本也证实了这一点。K-12及其后代表现为I型,大肠杆菌b及其后代表现为IV型,这两种模式都只存在于大肠杆菌中。系统群与Hae III型基因谱之间存在近乎可能的关联,克隆群与不同的病原体之间可能存在相关性。23S rRNA基因的共性、保守性和条形码间隙使其成为细菌分子诊断最优选区域16S rRNA基因的理想选择和替代品。
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来源期刊
Journal of Pathogens
Journal of Pathogens MICROBIOLOGY-
自引率
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4
审稿时长
15 weeks
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