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首页> 外文期刊>Iranian Journal of Microbiology >Toxin A and B genes expression of Clostridium difficile in the sub-minimum inhibitory concentration of clindamycin, vancomycin and in combination with ceftazidime
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Toxin A and B genes expression of Clostridium difficile in the sub-minimum inhibitory concentration of clindamycin, vancomycin and in combination with ceftazidime

机译:毒素A和B基因在克林霉素,万古霉素和头孢他啶结合的临少抑制浓度下梭菌差异的表达

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Background and Objectives: Antibiotics prescribed for infections have diverse effects on microbiota and the pathogen Clostridium difficile (C. difficile) as the most important antibiotic-associated diarrhea. This study aims to determine the gene expression of toxins A and B at the transcription level in the sub-MIC of vancomycin (VAN), clindamycin (CLI), and ceftazidime (CAZ) alone and in combination. Materials and Methods: The MIC and fractional inhibitory concentration (FIC) of two C. difficile samples (a clinical isolate and ATCC 9689) were determined by microdilution and checkerboard microdilution methods, respectively. The total RNA was extracted from the medium inoculated with ~10 6 CFU/mL of fresh bacteria in the pre-reduced medium containing ? MIC of antibiotics alone and ? FIC of antibiotics in combination. Real-time PCR was performed by sybrGreen methods in triplicate, and the data were analyzed by the comparative ?? CT method. Results: All antibiotics except CAZ (alone and in combination) decreased the gene expression of toxins A and B within 24 hours. VAN and CLI reduced toxin gene expression within 24 and 48 hours. However, CAZ alone and in combination with VAN as well as CLI increased the gene expression of toxins A and B. Conclusion: The results confirmed toxin gene transcription and toxin production are associated with the type of isolates and antibiotics, as well as the combined form of antibiotics. This could be the reason which can explain the occurrence of C. difficile infection among patients who were treated with the third generation of cephalosporins alone and in combination with another antibiotic in the form of combinational therapy.
机译:背景和目标:针对感染规定的抗生素对微生物群和病原体梭菌(C.艰难梭菌)具有多样化的抗生素作为最重要的抗生素相关的腹泻。该研究旨在确定毒素(van),Clindamycin(Cli)和Cittakidime(Ceftazidime(Cateface)和组合的转录水平的毒素A和B的基因表达。材料和方法:通过微量稀释和棋盘微稀释方法测定两种C.艰难梭菌样品(临床分离物和ATCC 9689)的MIC和分数抑制浓度(FIC)。从含有〜10 6 cfu / ml新鲜细菌的培养基中萃取总RNA,所述培养基中的预介质含有〜10 6 cfu / ml新鲜细菌?单独抗生素的MIC和?抗生素的FIC组合。通过Sybrgreen方法一式三份进行实时PCR,并通过比较分析数据CT方法。结果:除Caz(单独和组合)之外的所有抗生素会在24小时内降低毒素A和B的基因表达。范和CLI在24和48小时内降低了毒素基因表达。然而,CAZ独自和与面包车以及CLI增加了毒素A和B的基因表达。结论:结果证实了毒素基因转录和毒素生产与分离物和抗生素的类型相关,以及组合形式抗生素。这可能是可以解释用第三代头孢菌素治疗的患者C.艰难梭菌感染的原因,并与组合治疗形式的另一种抗生素组合。

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