Molecular epidemiology and clinical characterization of carbapenemase-producing Enterobacter spp. from an international cohort

Jianping Jiang, Lauren Komarow, Carol Hill, Angelique E Boutzoukas, Blake Hanson, Cesar A Arias, Robert A Bonomo, Scott Evans, Yohei Doi, Michael J Satlin, Gregory Weston, Eric Cober, Sandra Liliana Valderrama-Beltran, Soraya Salcedo Mendoza, Zhengyin Liu, Bettina C Fries, Paul Ananth Tambyah, Henry F Chambers, Vance G Fowler, David van Duin, Barry N Kreiswirth, Liang Chen
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Abstract

Background Despite the global public health threat posed by carbapenem-resistant Enterobacter spp., clinical and molecular epidemiological studies on international isolates remain scarce. Historically, the taxonomy of Enterobacter has been challenging, limiting our understanding of the clinical characteristics and outcomes of carbapenemase-producing Enterobacter spp. infections. Methods Hospitalized patients enrolled in the CRACKLE-2 study (ClinicalTrials.gov, NCT03646227) from 2016-2018 with cultures positive for carbapenemase-producing Enterobacter spp. were included. Clinical and microbiologic data were collected from health records. Whole genome sequencing was performed, and the population structures of selected predominant clones were analyzed. Results We enrolled 136 hospitalized patients with carbapenemase-producing Enterobacter spp. from 30 hospitals in 7 countries. Among the 136 isolates, eleven Enterobacter species were identified, with most isolates belonging to E. xiangfangensis (n=81, 60%) and E. hoffmannii (n=17, 13%), and carrying blaKPC (n=106, 78%) and blaNDM (n=12, 9%). Clinical characteristics and outcomes were similar among patients with E. xiangfangensis, E. hoffmannii or the other Enterobacter spp. 30-day mortality was 20% and older age at enrollment (adjusted odds ratio 1.42, 95% confidence interval 1.08-1.87) was associated with increased mortality. Sequence type (ST)171 E. xiangfangensis, ST78 E. hoffmannii, and ST93 E. xiangfangensis were the predominant clones, and the acquisition of fluoroquinolone resistance-associated mutations and carbapenemase-encoding plasmids contributed to their formation and global dissemination. Conclusions Our findings demonstrated that E. xiangfangensis and E. hoffmannii are common species among international carbapenemase-producing Enterobacter spp., potentially linked to the clonal spread of a few predominant clones that have acquired fluoroquinolone resistance and carbapenemase-encoding plasmids.
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国际队列中产碳青霉烯酶肠杆菌属的分子流行病学和临床特征描述
背景尽管耐碳青霉烯肠杆菌对全球公共卫生构成威胁,但国际分离株的临床和分子流行病学研究仍然很少。从历史上看,肠杆菌的分类一直具有挑战性,限制了我们对产碳青霉烯酶肠杆菌感染的临床特征和结果的理解。方法纳入2016-2018年纳入CRACKLE-2研究(ClinicalTrials.gov, NCT03646227)的产碳青霉烯酶肠杆菌培养阳性的住院患者。从健康记录中收集临床和微生物学数据。进行全基因组测序,分析筛选出的优势无性系群体结构。结果我们纳入了来自7个国家30家医院的136例产碳青霉烯酶肠杆菌住院患者。136株分离菌中鉴定出11种肠杆菌,其中香方肠杆菌(n=81, 60%)和霍夫曼肠杆菌(n=17, 13%)最多,携带blaKPC (n=106, 78%)和blaNDM (n=12, 9%)。湘坊肠杆菌、霍夫曼肠杆菌或其他肠杆菌患者的临床特征和结果相似,30天死亡率为20%,入组时年龄较大(校正优势比1.42,95%可信区间1.08-1.87)与死亡率增加相关。序列型(ST)171、ST78和ST93是优势克隆,氟喹诺酮类药物耐药相关突变和碳青霉烯酶编码质粒的获得是其形成和全球传播的主要原因。结论香房伊氏杆菌和霍夫曼伊氏杆菌是产碳青霉烯酶的国际肠杆菌中常见的种,可能与少数获得氟喹诺酮类药物抗性和碳青霉烯酶编码质粒的优势克隆的无性传播有关。
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