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首页> 外文期刊>Journal of Clinical Microbiology >Molecular epidemiology of an outbreak of multidrug-resistant Enterobacter aerogenes infections and in vivo emergence of imipenem resistance.
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Molecular epidemiology of an outbreak of multidrug-resistant Enterobacter aerogenes infections and in vivo emergence of imipenem resistance.

机译:多药耐药性产气肠杆菌感染和亚胺培南耐药性体内出现的分子流行病学研究。

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摘要

Molecular typing was used to investigate an outbreak of infection caused by multidrug-resistant Enterobacter aerogenes (MREA) susceptible only to gentamicin and imipenem in an intensive care unit (ICU). Over a 9-month period, ciprofloxacin-resistant E. aerogenes isolates were isolated from 34 patients, or 4.1% of ICU admissions, compared with a baseline rate of 0.1% in the previous period (P < 0.001). Infection developed in 15 (44%) patients. In vivo emergence of imipenem resistance (MIC, 32 micrograms/ml) of organisms causing deep-seated infection was observed in two (13%) of these patients following prolonged therapy with imipenem and gentamicin. Arbitrarily primed PCR (AP-PCR) analysis with ERIC1R and ERIC2 primers and pulsed-field gel electrophoresis (PFGE) analysis of XbaI macrorestriction patterns concordantly showed that outbreak-associated MREA isolates were clonally related and distinct from epidemiologically unrelated strains. AP-PCR and PFGE showed discrimination indices of 0.88 and 0.98, respectively. Space-time clustering of cases within units suggests that the epidemic-related MREA isolates were transmitted on the hands of the health care personnel. A case-control study and repeated environmental culture surveys failed to identify a common source or procedure associated with transmission. In spite of the early implementation of isolation measures, the incidence of MREA colonization remained stable until all colonized patients were discharged. This study confirms the usefulness of AP-PCR and PFGE analyses for the epidemiological study of E. aerogenes and underscores the difficulty of controlling the spread of multiresistant clones of this organism in the ICU setting. The emergence of imipenem resistance represents a threat because virtually no therapeutic option is available for such strains.
机译:分子分型被用于研究重症监护病房(ICU)中仅对庆大霉素和亚胺培南敏感的多重耐药性产气肠杆菌(MREA)引起的感染暴发。在9个月的时间内,从34例患者中分离出环丙沙星耐药的产气链球菌大肠杆菌,占ICU入院人数的4.1%,而上一期间的基线率为0.1%(P <0.001)。 15(44%)位患者发生感染。在经过亚胺培南和庆大霉素的长期治疗后,其中两名(13%)患者体内出现了亚胺培南耐药菌(MIC,32微克/毫升),引起深层次感染。使用ERIC1R和ERIC2引物的任意引物PCR(AP-PCR)分析和XbaI宏观限制性图谱的脉冲场凝胶电泳(PFGE)分析一致显示,与暴发相关的MREA分离株具有克隆相关性,与流行病学无关的菌株不同。 AP-PCR和PFGE的鉴别指数分别为0.88和0.98。单位内病例的时空聚类表明与流行病有关的MREA分离株是在卫生保健人员的手中传播的。病例对照研究和反复的环境文化调查未能确定与传播有关的共同来源或程序。尽管尽早实施了隔离措施,但MREA定植的发生率一直保持稳定,直到所有定植的患者出院为止。这项研究证实了AP-PCR和PFGE分析对于产气链球菌的流行病学研究的有效性,并强调了在ICU环境中控制该生物的多抗性克隆传播的难度。亚胺培南耐药性的出现是一个威胁,因为对于这种菌株实际上没有治疗选择。

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