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2007 年至 2018 年期间,加拿大安大略省多伦多一家医院系统中产碳青霉烯酶 的基因组流行病学研究。

Genomic Epidemiology of Carbapenemase-Producing at a Hospital System in Toronto, Ontario, Canada, 2007 to 2018.

机构信息

Dalla Lana School of Public Health, University of Toronto, Toronto, Ontario, Canada.

Sinai Health System, Toronto, Ontario, Canada.

出版信息

Antimicrob Agents Chemother. 2021 Jul 16;65(8):e0036021. doi: 10.1128/AAC.00360-21.

Abstract

At a hospital system (H1) in Ontario, Canada, we investigated whether whole-genome sequencing (WGS) altered initial epidemiological interpretation of carbapenemase-producing (CPE) transmission. We included patients with CPE colonization/infection identified by population-based surveillance from October 2007 to August 2018 who received health care at H1 in the year before/after CPE detection. H1 reported epidemiological transmission clusters. We combined single nucleotide variant (SNV) analysis, plasmid characterization, and epidemiological data. Eighty-five patients were included. H1 identified 7 epidemiological transmission clusters, namely, A to G, involving 24/85 (28%) patients. SNV analysis confirmed transmission clusters C, D, and G and identified two additional cases belonging to cluster A. One was a travel-related case that was the likely index case (0 to 6 SNVs from other isolates); this case stayed on the same unit as the initially presumed index case 4 months prior to detection of the initially presumed index case on another unit. The second additional case occupied a room previously occupied by 5 cluster A cases. Plasmid sequence analysis excluded a case from cluster A and identified clusters E and F as possibly two parts of a single cluster. SNV analysis also identified a case without direct epidemiologic links that was 18 to 21 SNVs away from cluster B, suggesting possible undetected interhospital transmission. SNV and plasmid sequence analysis identified cases belonging to transmission clusters that conventional epidemiology missed and excluded other cases. Implementation of routine WGS to complement epidemiological transmission investigations has the potential to improve prevention and control of CPE in hospitals.

摘要

在加拿大安大略省的一家医院系统(H1),我们研究了全基因组测序(WGS)是否改变了对产碳青霉烯酶(CPE)传播的初始流行病学解释。我们纳入了 2007 年 10 月至 2018 年 8 月通过人群监测发现的在 CPE 检测前/后一年在 H1 接受医疗保健的 CPE 定植/感染患者。H1 报告了流行病学传播集群。我们结合了单核苷酸变异(SNV)分析、质粒特征和流行病学数据。共纳入 85 例患者。H1 确定了 7 个流行病学传播集群,即 A 到 G,涉及 24/85(28%)患者。SNV 分析证实了 C、D 和 G 传播集群,并确定了另外两例属于 A 集群的病例。其中一例是与旅行相关的病例,可能是原发病例(与其他分离株的 0 至 6 个 SNV);该病例在另一个单元发现原发病例前 4 个月与最初假定的原发病例在同一单元。第二例额外的病例居住在之前被 5 例 A 集群病例占据的房间里。质粒序列分析排除了 A 集群中的一个病例,并确定了 E 和 F 集群可能是一个集群的两个部分。SNV 分析还确定了一个与直接流行病学联系无关的病例,与 B 集群相隔 18 到 21 个 SNV,表明可能存在未被发现的医院间传播。SNV 和质粒序列分析确定了属于传播集群的病例,而常规流行病学则遗漏了这些病例,并排除了其他病例。实施常规 WGS 以补充流行病学传播调查有可能改善医院 CPE 的预防和控制。

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