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Identification of Genome-Wide Mutations in Ciprofloxacin-Resistant F. tularensis LVS Using Whole Genome Tiling Arrays and Next Generation Sequencing

机译:使用全基因组切片阵列和下一代测序技术鉴定耐环丙沙星的土拉希沃特氏菌LVS的全基因组突变。

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摘要

Francisella tularensis is classified as a Class A bioterrorism agent by the U.S. government due to its high virulence and the ease with which it can be spread as an aerosol. It is a facultative intracellular pathogen and the causative agent of tularemia. Ciprofloxacin (Cipro) is a broad spectrum antibiotic effective against Gram-positive and Gram-negative bacteria. Increased Cipro resistance in pathogenic microbes is of serious concern when considering options for medical treatment of bacterial infections. Identification of genes and loci that are associated with Ciprofloxacin resistance will help advance the understanding of resistance mechanisms and may, in the future, provide better treatment options for patients. It may also provide information for development of assays that can rapidly identify Cipro-resistant isolates of this pathogen. In this study, we selected a large number of F. tularensis live vaccine strain (LVS) isolates that survived in progressively higher Ciprofloxacin concentrations, screened the isolates using a whole genome F. tularensis LVS tiling microarray and Illumina sequencing, and identified both known and novel mutations associated with resistance. Genes containing mutations encode DNA gyrase subunit A, a hypothetical protein, an asparagine synthase, a sugar transamine/perosamine synthetase and others. Structural modeling performed on these proteins provides insights into the potential function of these proteins and how they might contribute to Cipro resistance mechanisms.
机译:图拉弗朗西斯菌由于其高毒力和易于以气雾剂形式传播,被美国政府列为A类生物恐怖主义制剂。它是兼性的细胞内病原体和Tularemia的病原体。环丙沙星(Cipro)是一种广谱抗生素,可有效抵抗革兰氏阳性和革兰氏阴性细菌。当考虑对细菌感染进行医学治疗时,致病性微生物中Cipro耐药性的增加值得关注。鉴定与环丙沙星耐药相关的基因和基因座将有助于增进对耐药机制的了解,并可能在将来为患者提供更好的治疗选择。它还可以为开发可快速鉴定该病原体耐顺铂的分离物的测定提供信息。在这项研究中,我们选择了在较高环丙沙星浓度下存活的大量F. tularensis活疫苗株(LVS)分离株,使用全基因组F. tularensis LVS切片微阵列和Illumina测序筛选了分离株,并鉴定了已知的和已知的与抗性相关的新突变。含有突变的基因编码DNA促旋酶亚基A,一种假设的蛋白质,一种天冬酰胺合成酶,一种糖转胺/过氧化胺合成酶等。对这些蛋白质进行的结构建模可洞悉这些蛋白质的潜在功能,以及它们如何对Cipro抗性机制产生影响。

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