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Freshwater viral metagenome reveals novel and functional phage-borne antibiotic resistance genes

机译:淡水病毒偏心蛋白酶揭示了新颖和功能性噬菌体抗生素抗生素基因

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BACKGROUND:Antibiotic resistance developed by bacteria is a significant threat to global health. Antibiotic resistance genes (ARGs) spread across different bacterial populations through multiple dissemination routes, including horizontal gene transfer mediated by bacteriophages. ARGs carried by bacteriophages are considered especially threatening due to their prolonged persistence in the environment, fast replication rates, and ability to infect diverse bacterial hosts. Several studies employing qPCR and viral metagenomics have shown that viral fraction and viral sequence reads in clinical and environmental samples carry many ARGs. However, only a few ARGs have been found in viral contigs assembled from metagenome reads, with most of these genes lacking effective antibiotic resistance phenotypes. Owing to the wide application of viral metagenomics, nevertheless, different classes of ARGs are being continuously found in viral metagenomes acquired from diverse environments. As such, the presence and functionality of ARGs encoded by bacteriophages remain up for debate.RESULTS:We evaluated ARGs excavated from viral contigs recovered from urban surface water viral metagenome data. In virome reads and contigs, diverse ARGs, including polymyxin resistance genes, multidrug efflux proteins, and β-lactamases, were identified. In particular, when a lenient threshold of e value of ≤ 1 × e-5 and query coverage of ≥ 60% were employed in the Resfams database, the novel β-lactamases blaHRV-1 and blaHRVM-1 were found. These genes had unique sequences, forming distinct clades of class A and subclass B3 β-lactamases, respectively. Minimum inhibitory concentration analyses for E. coli strains harboring blaHRV-1 and blaHRVM-1 and catalytic kinetics of purified HRV-1 and HRVM-1 showed reduced susceptibility to penicillin, narrow- and extended-spectrum cephalosporins, and carbapenems. These genes were also found in bacterial metagenomes, indicating that they were harbored by actively infecting phages.CONCLUSION:Our results showed that viruses in the environment carry as-yet-unreported functional ARGs, albeit in small quantities. We thereby suggest that environmental bacteriophages could be reservoirs of widely variable, unknown ARGs that could be disseminated via virus-host interactions. Video abstract.
机译:背景:细菌产生的抗生素抗性是对全球健康的重大威胁。通过多种传播途径在不同的细菌群体中蔓延的抗生素抗性基因(Args),包括由噬菌体介导的水平基因转移。由于它们在环境,快速复制率和感染不同的细菌宿主的能力,噬菌体携带的噬菌体携带的噬菌体被认为特别威胁。采用QPCR和病毒偏心组虫的几项研究表明,临床和环境样品中的病毒级分和病毒序列携带许多args。然而,只有几种args在从梅塔群读数中组装的病毒角中发现,大多数这些基因缺乏有效的抗生素抗性表型。然而,由于病毒性偏心组合的广泛应用,在从各种环境中获得的病毒群体中不断发现不同类别的args。因此,由噬菌体编码的Args的存在和功能仍然是辩论。结果:我们评估了从城市地表水病群数据中回收的病毒角质挖掘的args。在病毒读数和体谱中,鉴定了多样化的args,包括多药素抗性基因,多药中排出蛋白和β-内酰胺酶。特别地,当在RES特征数据库中使用≤1×e-5的Δ1×e-5的升温阈值并在RES特征数据库中使用≥60%时,发现新型β-内酰胺酶BLAHRV-1和BLAHRVM-1。这些基因分别具有独特的序列,分别形成了A和亚类B3β-内酰胺酶的不同曲线。含有BlahRv-1和Blahrvm-1的大肠杆菌菌株的最小抑制浓度分析和纯化的HRV-1和HRVM-1的催化动力学表现出对青霉素,窄和扩展谱孢子的易感性降低,群体和肉豆蔻血症。这些基因也被发现在细菌偏心组中,表明它们是通过主动感染噬菌体而覆盖的。结论:我们的结果表明,环境中的病毒携带了尚未报告的功能args,尽管少量少量。因此,我们表明,环境噬菌体可能是广泛变量的储层,通过病毒 - 宿主相互作用可以传播的未知args。视频摘要。

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