Ana M Castañeda-Meléndrez, José A Magaña-Lizárraga, Marcela Martínez-Valenzuela, Aldo F Clemente-Soto, Patricia C García-Cervantes, Francisco Delgado-Vargas, Rodolfo Bernal-Reynaga
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This study aims to sequence a multidrug-resistant UPEC isolate (UTI-U7) and assess the multilocus sequence typing (MLST), virulence factors, antimicrobial resistance profile, genes, serotype, and plasmid content. Antimicrobial susceptibility profiling was performed using the Kirby-Bauer disk diffusion. The antibacterial and anti-adherent effects of the methanol extracts (ME) of <i>Echeveria</i> (<i>E. craigiana</i>, <i>E. kimnachii</i>, and <i>E. subrigida</i>) against UTI-U7 were determined. The isolate was characterized as an O25:H4-B2-ST2279-CH40 subclone and had resistant determinants to aminoglycosides, β-lactams, fluoroquinolones/quinolones, amphenicols, and tetracyclines, which matched with the antimicrobial resistance profile. The virulence genes identified encode adherence factors, iron uptake, protectins/serum resistance, and toxins. Identified plasmids belonged to the IncF group (IncFIA, IncFIB, and IncFII), alongside several prophage-like elements. After an extensive genome analysis that confirmed the pathogenic status of UTI-U7 isolate, <i>Echeveria</i> extracts were tested to determine their antibacterial effects; as an extract, <i>E. subrigida</i> (MIC, 5 mg/mL) displayed the best inhibitory effect. 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引用次数: 0
摘要
尿路致病性大肠杆菌(UPEC)是与尿路感染有关的最常见细菌病原体,它以高昂的医疗费用和高发病率威胁着公共卫生系统。感染的成功建立与其基因组中编码的毒力因子以及抗菌耐药基因有关,这可能会限制感染的治疗和解决。从这个意义上讲,埃希维里亚属植物提取物传统上一直被用于治疗各种传染性疾病。然而,人们对这些提取物对细菌的影响及其潜在的作用机制知之甚少。本研究旨在对耐多药的 UPEC 分离物(UTI-U7)进行测序,并评估其多焦点序列分型(MLST)、毒力因子、抗菌药耐药性特征、基因、血清型和质粒含量。抗菌药敏感性分析采用 Kirby-Bauer 盘扩散法进行。测定了 Echeveria(E. craigiana、E. kimnachii 和 E. subrigida)甲醇提取物(ME)对UTI-U7 的抗菌和抗粘附作用。该分离株被鉴定为 O25:H4-B2-ST2279-CH40 亚克隆,对氨基糖苷类、β-内酰胺类、氟喹诺酮类/喹诺酮类、氨苯蝶啶类和四环素类药物具有耐药性,这与抗菌药耐药性特征相符。鉴定出的毒力基因编码粘附因子、铁吸收、保护素/血清抗性和毒素。鉴定出的质粒属于 IncF 组(IncFIA、IncFIB 和 IncFII),同时还发现了几个类似噬菌体的元件。经过广泛的基因组分析,确认了UTI-U7分离株的致病状态,然后对Echeveria提取物进行了测试,以确定其抗菌效果;作为一种提取物,E. subrigida(MIC,5 mg/mL)显示出最佳的抑制效果。然而,UTI-U7 和 HeLa 细胞之间的粘附性不受 E. subrigida 提取物 ME 的影响。
Genomic characterization of a multidrug-resistant uropathogenic Escherichia coli and evaluation of Echeveria plant extracts as antibacterials.
Uropathogenic Escherichia coli (UPEC) is the most common bacterial agent associated with urinary tract infections, threatening public health systems with elevated medical costs and high morbidity rates. The successful establishment of the infection is associated with virulence factors encoded in its genome, in addition to antibacterial resistance genes, which could limit the treatment and resolution of the infection. In this sense, plant extracts from the genus Echeveria have traditionally been used to treat diverse infectious diseases. However, little is known about the effects of these extracts on bacteria and their potential mechanisms of action. This study aims to sequence a multidrug-resistant UPEC isolate (UTI-U7) and assess the multilocus sequence typing (MLST), virulence factors, antimicrobial resistance profile, genes, serotype, and plasmid content. Antimicrobial susceptibility profiling was performed using the Kirby-Bauer disk diffusion. The antibacterial and anti-adherent effects of the methanol extracts (ME) of Echeveria (E. craigiana, E. kimnachii, and E. subrigida) against UTI-U7 were determined. The isolate was characterized as an O25:H4-B2-ST2279-CH40 subclone and had resistant determinants to aminoglycosides, β-lactams, fluoroquinolones/quinolones, amphenicols, and tetracyclines, which matched with the antimicrobial resistance profile. The virulence genes identified encode adherence factors, iron uptake, protectins/serum resistance, and toxins. Identified plasmids belonged to the IncF group (IncFIA, IncFIB, and IncFII), alongside several prophage-like elements. After an extensive genome analysis that confirmed the pathogenic status of UTI-U7 isolate, Echeveria extracts were tested to determine their antibacterial effects; as an extract, E. subrigida (MIC, 5 mg/mL) displayed the best inhibitory effect. However, the adherence between UTI-U7 and HeLa cells was unaffected by the ME of the E. subrigida extract.
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