首页> 外文期刊>European journal of clinical microbiology and infectious diseases: Official publication of the European Society of Clinical Microbiology >Antimicrobial non-susceptibility of cervico-vaginal and rectal Escherichia coli isolates is associated with phylogeny and plasmid carriage.
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Antimicrobial non-susceptibility of cervico-vaginal and rectal Escherichia coli isolates is associated with phylogeny and plasmid carriage.

机译:宫颈阴道和直肠大肠杆菌分离株的抗菌非敏感性与系统发育和质粒运输有关。

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Uropathogenic Escherichia coli (UPEC) is the primary cause of urinary tract infections (UTIs) in adult women, which are increasingly refractory to antimicrobial treatment. UPEC colonizes the vagina prior to causing a UTI. Our hypothesis was that the vaginal flora would be enriched in UPEC and therefore have a greater prevalence of non-susceptibility relative to the rectal flora. We used disk diffusion to determine the antimicrobial susceptibilities of 100 cervico-vaginal E. coli (CVEC) and 100 rectal E. coli (REC) isolates from 200 different patients. Phylogeny, plasmid replicons, and antimicrobial resistance genes were detected by polymerase chain reaction (PCR). There were no significant differences between CVEC and REC, and the overall levels of non-susceptibility were 39.5% for ampicillin (AM), 11.5% for ampicillin-sulbactam (SAM), 11.5% for trimethoprim-sulfamethoxazole (SXT), 5% for ciprofloxacin (CIP), 2.5% for nitrofurantoin (F/M), 0.5% for ceftazidime (CAZ), 0.5% for cefotaxime (CTX), and 0% for fosfomycin (FOS). SXT non-susceptibility was associated with phylogenetic groups A and D compared with B2. AM and SXT non-susceptibility was associated with plasmid carriage. The vaginal flora is not enriched in antimicrobial non-susceptibility relative to the rectal flora. However, antimicrobial non-susceptibility was associated with phylogeny and plasmid carriage.
机译:泌尿道致病性大肠埃希菌(UPEC)是成年女性泌尿道感染(UTI)的主要原因,对抗菌药物的治疗越来越难。 UPEC在引起泌尿道感染之前先定植于阴道。我们的假设是阴道菌群将富含UPEC,因此与直肠菌群相比,非敏感性的患病率更高。我们使用纸片扩散法确定了200例不同患者的100例宫颈阴道大肠杆菌(CVEC)和100例直肠大肠杆菌(REC)分离株的抗药性。系统发育,质粒复制子和抗菌素耐药基因通过聚合酶链反应(PCR)检测。 CVEC和REC之间无显着差异,氨苄西林(AM)的总体不敏感性水平为39.5%,氨苄西林-舒巴坦(SAM)的总体不敏感性为11.5%,甲氧苄啶-磺胺甲恶唑(SXT)的总体不敏感性为5%环丙沙星(CIP),呋喃妥因(F / M)为2.5%,头孢他啶(CAZ)为0.5%,头孢噻肟(CTX)为0.5%,磷霉素(FOS)为0%。与B2相比,SXT的非敏感性与A和D的系统发育组相关。 AM和SXT的非敏感性与质粒的运输有关。相对于直肠菌群,阴道菌群未富含抗微生物药性。但是,抗菌素的非敏感性与系统发育和质粒运输有关。

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