首页> 外文期刊>Infection control and hospital epidemiology >Emergence and control of fluoroquinolone-resistant, toxin A-negative, toxin B-positive Clostridium difficile.
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Emergence and control of fluoroquinolone-resistant, toxin A-negative, toxin B-positive Clostridium difficile.

机译:耐氟喹诺酮,毒素A阴性,毒素B阳性艰难梭菌的出现和控制。

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BACKGROUND: Clostridium difficile is a major cause of infectious diarrhea in hospitalized patients. Between August 2003 and January 2004, we experienced an increase in the incidence of C. difficile-associated disease. We describe the investigation into and management of the outbreak in this article. METHODS: A total of 73 consecutive patients with nosocomial C. difficile-associated diarrhea were identified. C. difficile isolates were characterized using toxin-specific enzyme immunoassays, a tissue-culture fibroblast cytotoxicity assay, polymerase chain reaction (PCR), and antimicrobial susceptibility tests. Rates of recurrence and of C. difficile colitis were recorded. Changes in antibiotic use and infection control policies were documented. RESULTS: The incidence of C. difficile-associated diarrhea peaked at 21 cases per 1,000 patient admissions. Of the C. difficile isolates recovered, 85 (95%) were identical toxin A-negative and toxin B-positive strains, corresponding to toxinotype VIII and PCR ribotype 017. All clonal isolates were resistant to multiple antibiotics, including ofloxacin, ciprofloxacin, levofloxacin, moxifloxacin, and gatifloxacin (minimum inhibitory concentrations [MICs] of greater than 32 micro g/mL) and erythromycin, clarithromycin, and clindamycin (MICs of greater than 256 micro g/mL). Recurrent C. difficile-associated disease occurred in 26 (36%) of the patients. At least 10 (14%) of the patients developed C. difficile colitis. Additional infection control measures introduced included the use of ward memos, a hand-hygiene awareness campaign, increased environmental cleaning, attention to prescribing practices for antibiotics, increased awareness of diarrheal illness, and early isolation of affected patients. Total use of fluoroquinolones did not change throughout the study period. Despite persistence of this toxin-variant strain, the incidence of C. difficile-associated disease in our institution decreased to fewer than 5 cases per 1,000 admissions. CONCLUSIONS: We report on theemergence of a fluoroquinolone- and clindamycin-resistant, toxin A-negative, and toxin B-positive strain of C. difficile associated with an outbreak of C. difficile-associated disease in our institution during a 6-month period. We found that careful attention to improvement of infection control interventions was the most important means of controlling this nosocomial pathogen.
机译:背景:艰难梭菌是住院患者感染性腹泻的主要原因。在2003年8月至2004年1月之间,我们经历了艰难梭菌相关疾病的发病率上升。在本文中,我们描述了对爆发的调查和管理。方法:确定了73例连续的院内艰难梭菌相关性腹泻患者。艰难梭菌分离物的鉴定采用毒素特异性酶免疫测定,组织培养成纤维细胞细胞毒性测定,聚合酶链反应(PCR)和抗菌药敏试验。记录复发率和艰难梭菌结肠炎。记录了抗生素使用和感染控制政策的变化。结果:艰难梭菌相关性腹泻的发病率最高为每1,000名患者中21例。在回收的艰难梭菌分离物中,有85株(95%)是相同的毒素A阴性和毒素B阳性菌株,分别对应于VIII型毒素和PCR核糖体017型。所有克隆菌株均对多种抗生素具有抗性,包括氧氟沙星,环丙沙星,左氧氟沙星,莫西沙星和加替沙星(最小抑菌浓度[MICs]大于32 micro g / mL)以及红霉素,克拉霉素和克林霉素(MICs大于256 micro g / mL)。复发艰难梭菌相关疾病发生在26名患者中(36%)。至少有10名患者(14%)患有艰难梭菌结肠炎。引入的其他感染控制措施包括使用病房便笺,开展手卫生宣传运动,加强环境清洁工作,注意抗生素的处方做法,提高对腹泻病的意识以及及早隔离患病患者。在整个研究期间,氟喹诺酮类药物的总使用量没有变化。尽管这种毒素变异株持续存在,但在我们机构中,艰难梭菌相关疾病的发病率降至每千人入院少于5例。结论:我们报告了在我们机构的6个月内,出现了难辨梭菌的氟喹诺酮和克林霉素耐药毒素A阴性和毒素B阳性菌株的出现。 。我们发现,密切注意改善感染控制干预措施是控制这种医院病原体的最重要手段。

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