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揭示导致新生儿感染性休克死亡的新型阴沟肠杆菌复合种:一项队列研究。

Uncovering the novel Enterobacter cloacae complex species responsible for septic shock deaths in newborns: a cohort study.

作者信息

Girlich Delphine, Ouzani Souad, Emeraud Cécile, Gauthier Lauraine, Bonnin Rémy A, Le Sache N, Mokhtari Mostafa, Langlois Isabelle, Begasse Christine, Arangia Nicolas, Fournier Sandra, Fortineau Nicolas, Naas Thierry, Dortet Laurent

机构信息

Team Resist UMR1184 Immunology of Viral, Auto-immune, Hematological, and Bacterial diseases, INSERM, Paris-Saclay University, Faculty of Medicine, Paris, France.

Bacteriology-Hygiene unit, Assistance Publique-Hôpitaux de Paris, Bicêtre Hospital, Paris, France.

出版信息

Lancet Microbe. 2021 Oct;2(10):e536-e544. doi: 10.1016/S2666-5247(21)00098-7. Epub 2021 Jul 23.

Abstract

BACKGROUND

Enterobacter cloacae complex contains nosocomial pathogens responsible for infection outbreaks. Identification at the species level within the E cloacae complex remains difficult. Using whole genome sequencing, our aim was to decipher the transmission routes that led to the death of six of seven neonates who had bacteraemia caused by E cloacae complex isolates in a neonatal intensive care unit (NICU) over a 13 month period.

METHODS

In this cohort study, E cloacae complex isolates were taken from 186 newborns in an NICU: 14 were clinical samples (eg, blood cultures), 728 rectal swab samples, and 38 environmental samples (20 from siphons, 18 from incubators, and one from a mattress). The samples were analysed to decipher the possible role of manual cross transmission or environmental source in an outbreak of fatal septic shocks related to E cloacae complex bacteraemia. After the replacement of the incubators suspected to be the reservoir of some outbreak-related isolates on Feb 1, 2018, E cloacae complex strains were screened again for 10 months (503 rectal swab samples from 163 newborns). The 71 E cloacae complex isolates recovered from screening, clinical, and environmental samples across both study periods were compared by whole genome sequencing. The pathogenicity of E cloacae complex isolates responsible for fatal septic shocks was assessed using a Galleria mellonella in-vivo model.

FINDINGS

From Dec 9, 2016, to Jan 31, 2018, 249 (34%) of 728 rectal swab samples were positive for E cloacae complex, with 66 (35%) of 186 newborns colonised. E cloacae complex were also recovered from four (20%) of 20 siphons and 11 (61%) of 18 incubators. During this period, whole genome sequencing identified that the isolates responsible for the six fatal septic shocks were all Enterobacter bugandensis. A G mellonella infection model showed a higher virulence of E bugandensis. Genomic analysis highlighted the role of incubators as a long-term reservoir and source of cross contamination, leading to their replacement on Feb 1, 2018. Following incubator replacement, a 10-month follow-up investigation identified a physiological gut colonisation with polyclonal E cloacae complex in 52 (34%) of 163 neonates within a median of 9 days (5-14), but no E cloacae complex-related septic shocks.

INTERPRETATION

Despite around 30% of neonates being physiologically colonised with E cloacae complex, fatal sepsis was systematically linked with bacteraemia caused by E bugandensis. Our findings highlight the need for accurate identification methods to detect the hypervirulent species within the E cloacae complex recovered in neonates.

FUNDING

Assistance Publique-Hôpitaux de Paris.

摘要

背景

阴沟肠杆菌复合体包含导致医院感染暴发的病原菌。在阴沟肠杆菌复合体内进行种水平的鉴定仍然困难。我们的目的是利用全基因组测序来解读在13个月期间导致新生儿重症监护病房(NICU)中7例由阴沟肠杆菌复合体分离株引起菌血症的新生儿中有6例死亡的传播途径。

方法

在这项队列研究中,从一个NICU的186名新生儿中采集阴沟肠杆菌复合体分离株:14份为临床样本(如血培养),728份直肠拭子样本,以及38份环境样本(20份来自虹吸管,18份来自 incubators,1份来自床垫)。对这些样本进行分析,以解读在与阴沟肠杆菌复合体菌血症相关的致命性感染性休克暴发中,人工交叉传播或环境源的可能作用。在2018年2月1日更换了被怀疑是某些与暴发相关分离株储存源的 incubators后,对阴沟肠杆菌复合体菌株再次进行了10个月的筛查(来自163名新生儿的503份直肠拭子样本)。通过全基因组测序对在两个研究期间从筛查、临床和环境样本中分离出的71株阴沟肠杆菌复合体进行比较。使用大蜡螟体内模型评估导致致命性感染性休克的阴沟肠杆菌复合体分离株的致病性。

结果

从2016年12月9日至2018年1月31日期间,728份直肠拭子样本中有249份(34%)阴沟肠杆菌复合体呈阳性,186名新生儿中有66名(35%)被定植。在20个虹吸管中的4个(20%)以及18个 incubators中的11个(61%)也分离出阴沟肠杆菌复合体。在此期间,全基因组测序确定导致6例致命性感染性休克的分离株均为布氏肠杆菌。大蜡螟感染模型显示布氏肠杆菌的毒力更高。基因组分析突出了 incubators作为长期储存源和交叉污染源的作用,导致其在2018年2月1日被更换。更换 incubators后,为期10个月的随访调查发现,163名新生儿中有52名(34%)在中位数为9天(5 - 14天)时出现多克隆阴沟肠杆菌复合体的生理性肠道定植,但未出现与阴沟肠杆菌复合体相关的感染性休克。

解读

尽管约30%的新生儿生理性定植有阴沟肠杆菌复合体,但致命性败血症与布氏肠杆菌引起的菌血症有系统性关联。我们的研究结果强调需要准确的鉴定方法来检测在新生儿中分离出的阴沟肠杆菌复合体内的高毒力菌种。

资金来源

巴黎公立医院集团。

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