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Novel Fri1-like Viruses Infecting Acinetobacterbaumannii—vB_AbaP_AS11 and vB_AbaP_AS12—Characterization Comparative Genomic Analysis and Host-Recognition Strategy

机译:新型Fri1样病毒感染不动杆菌。baumannii-vB_AbaP_AS11和vB_AbaP_AS12-特征化比较基因组分析和宿主识别策略

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摘要

Acinetobacter baumannii is a gram-negative, non-fermenting aerobic bacterium which is often associated with hospital-acquired infections and known for its ability to develop resistance to antibiotics, form biofilms, and survive for long periods in hospital environments. In this study, we present two novel viruses, vB_AbaP_AS11 and vB_AbaP_AS12, specifically infecting and lysing distinct multidrug-resistant clinical A. baumannii strains with K19 and K27 capsular polysaccharide structures, respectively. Both phages demonstrate rapid adsorption, short latent periods, and high burst sizes in one-step growth experiments. The AS11 and AS12 linear double-stranded DNA genomes of 41,642 base pairs (bp) and 41,402 bp share 86% nucleotide sequence identity with the most variable regions falling in host receptor–recognition genes. These genes encode tail spikes possessing depolymerizing activities towards corresponding capsular polysaccharides which are the primary bacterial receptors. We described AS11 and AS12 genome organization and discuss the possible regulation of transcription. The overall genomic architecture and gene homology analyses showed that the phages are new representatives of the recently designated Fri1virus genus of the Autographivirinae subfamily within the Podoviridae family.
机译:鲍曼不动杆菌是革兰氏阴性,非发酵性好氧细菌,通常与医院获得性感染有关,并以其对抗生素产生抗药性,形成生物膜并在医院环境中长期存活的能力而闻名。在这项研究中,我们介绍了两种新型病毒,vB_AbaP_AS11和vB_AbaP_AS12,分别感染和裂解具有K19和K27荚膜多糖结构的独特的多重耐药临床鲍曼不动杆菌菌株。两种噬菌体在一步法生长实验中均显示出快速吸附,短潜伏期和高爆裂尺寸。 AS11和AS12线性双链DNA基因组的41,642个碱基对(bp)和41,402 bp具有86%的核苷酸序列同一性,其中最大的可变区属于宿主受体识别基因。这些基因编码尾钉,其具有对作为主要细菌受体的相应荚膜多糖的解聚活性。我们描述了AS11和AS12基因组的组织,并讨论了转录的可能调控。总体基因组结构和基因同源性分析表明,噬菌体是Podoviridae家族中Autographivirinae亚科最近指定的Fri1virus属的新代表。

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