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2009年至2012年德国一家新生儿重症监护病房产超广谱β-内酰胺酶肺炎克雷伯菌暴发的原因是什么?通过流行病学分析和全基因组测序重建传播途径。

What caused the outbreak of ESBL-producing Klebsiella pneumoniae in a neonatal intensive care unit, Germany 2009 to 2012? Reconstructing transmission with epidemiological analysis and whole-genome sequencing.

作者信息

Haller Sebastian, Eller Christoph, Hermes Julia, Kaase Martin, Steglich Matthias, Radonić Aleksandar, Dabrowski Piotr Wojtek, Nitsche Andreas, Pfeifer Yvonne, Werner Guido, Wunderle Werner, Velasco Edward, Abu Sin Muna, Eckmanns Tim, Nübel Ulrich

机构信息

Postgraduate Training for Applied Epidemiology, Berlin, Germany, affiliated to the European Programme for Intervention Epidemiology Training, European Centre for Disease Prevention and Control, Stockholm, Sweden Division of Healthcare-Associated Infections, Surveillance of Antimicrobial Resistance and Consumption, Department for Infectious Disease Epidemiology, Robert Koch Institute, Berlin, Germany.

Division of Nosocomial Pathogens and Antibiotic Resistances, Department for Infectious Diseases, Robert Koch Institute, Wernigerode, Germany Department of Laboratory Medicine, University Hospital Halle, Halle, Germany.

出版信息

BMJ Open. 2015 May 11;5(5):e007397. doi: 10.1136/bmjopen-2014-007397.

Abstract

OBJECTIVE

We aimed to retrospectively reconstruct the timing of transmission events and pathways in order to understand why extensive preventive measures and investigations were not sufficient to prevent new cases.

METHODS

We extracted available information from patient charts to describe cases and to compare them to the normal population of the ward. We conducted a cohort study to identify risk factors for pathogen acquisition. We sequenced the available isolates to determine the phylogenetic relatedness of Klebsiella pneumoniae isolates on the basis of their genome sequences.

RESULTS

The investigation comprises 37 cases and the 10 cases with ESBL (extended-spectrum beta-lactamase)-producing K. pneumoniae bloodstream infection. Descriptive epidemiology indicated that a continuous transmission from person to person was most likely. Results from the cohort study showed that 'frequent manipulation' (a proxy for increased exposure to medical procedures) was significantly associated with being a case (RR 1.44, 95% CI 1.02 to 2.19). Genome sequences revealed that all 48 bacterial isolates available for sequencing from 31 cases were closely related (maximum genetic distance, 12 single nucleotide polymorphisms). Based on our calculation of evolutionary rate and sequence diversity, we estimate that the outbreak strain was endemic since 2008.

CONCLUSIONS

Epidemiological and phylogenetic analyses consistently indicated that there were additional, undiscovered cases prior to the onset of microbiological screening and that the spread of the pathogen remained undetected over several years, driven predominantly by person-to-person transmission. Whole-genome sequencing provided valuable information on the onset, course and size of the outbreak, and on possible ways of transmission.

摘要

目的

我们旨在回顾性地重建传播事件的时间和途径,以了解为何广泛的预防措施和调查不足以预防新病例。

方法

我们从患者病历中提取可用信息来描述病例,并将其与病房的正常人群进行比较。我们进行了一项队列研究以确定病原体感染的风险因素。我们对可用分离株进行测序,以根据肺炎克雷伯菌分离株的基因组序列确定其系统发育相关性。

结果

该调查包括37例病例以及10例产超广谱β-内酰胺酶(ESBL)的肺炎克雷伯菌血流感染病例。描述性流行病学表明,最有可能存在人与人之间的持续传播。队列研究结果显示,“频繁操作”(代表增加了医疗程序暴露)与成为病例显著相关(相对风险1.44,95%置信区间1.02至2.19)。基因组序列显示,从31例病例中获得的所有48株可用于测序的细菌分离株密切相关(最大遗传距离为12个单核苷酸多态性)。根据我们对进化速率和序列多样性的计算,我们估计暴发菌株自2008年以来呈地方性流行。

结论

流行病学和系统发育分析一致表明,在微生物筛查开始之前存在其他未被发现的病例,并且病原体的传播在数年中未被发现,主要由人传人驱动。全基因组测序为暴发的起始、过程和规模以及可能的传播方式提供了有价值的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b3f/4431171/f8998c714473/bmjopen2014007397f01.jpg

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