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Comparative genomic analysis of novel Acinetobacter symbionts: A combined systems biology and genomics approach

机译:新型不动杆菌共生体的比较基因组分析:系统生物学和基因组学相结合的方法

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摘要

The increasing trend of antibiotic resistance in Acinetobacter drastically limits the range of therapeutic agents required to treat multidrug resistant (MDR) infections. This study focused on analysis of novel Acinetobacter strains using a genomics and systems biology approach. Here we used a network theory method for pathogenic and non-pathogenic Acinetobacter spp. to identify the key regulatory proteins (hubs) in each strain. We identified nine key regulatory proteins, guaA, guaB, rpsB, rpsI, rpsL, rpsE, rpsC, rplM and trmD, which have functional roles as hubs in a hierarchical scale-free fractal protein-protein interaction network. Two key hubs (guaA and guaB) were important for insect-associated strains, and comparative analysis identified guaA as more important than guaB due to its role in effective module regulation. rpsI played a significant role in all the novel strains, while rplM was unique to sheep-associated strains. rpsM, rpsB and rpsI were involved in the regulation of overall network topology across all Acinetobacter strains analyzed in this study. Future analysis will investigate whether these hubs are useful as drug targets for treating Acinetobacter infections.
机译:不动杆菌中抗生素耐药性的增加趋势极大地限制了治疗多药耐药性(MDR)感染所需的治疗剂的范围。这项研究的重点是使用基因组学和系统生物学方法分析新型不动杆菌。在这里,我们对致病性和非致病性不动杆菌属使用网络理论方法。以确定每个菌株中的关键调节蛋白(集线器)。我们鉴定了九种关键调节蛋白,guaA,guaB,rpsB,rpsI,rpsL,rpsE,rpsC,rplM和trmD,它们在无等级的无形分形蛋白-蛋白相互作用网络中起着枢纽的作用。两个关键中枢(guaA和guaB)对于昆虫相关菌株很重要,比较分析发现guaA比guaB更重要,因为它在有效的模块调控中发挥了作用。 rpsI在所有新菌株中都起着重要作用,而rplM是绵羊相关菌株所独有的。 rpsM,rpsB和rpsI参与了本研究中分析的所有不动杆菌菌株的整体网络拓扑结构的调控。未来的分析将调查这些集线器是否可用作治疗不动杆菌感染的药物靶标。

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