Department of Oncology and Hemato-Oncology, University of Milan, Milan, Italy.
Infectious Diseases Unit, Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milan, Italy.
Antimicrob Resist Infect Control. 2024 Jul 3;13(1):70. doi: 10.1186/s13756-024-01429-x.
Genomic surveillance of Klebsiella pneumoniae carbapenemase-producing Klebsiella pneumoniae (KPC-Kp) is crucial for virulence, drug-resistance monitoring, and outbreak containment.
Genomic analysis on 87 KPC-Kp strains isolated from 3 Northern Italy hospitals in 2019-2021 was performed by whole genome sequencing (WGS), to characterize resistome, virulome, and mobilome, and to assess potential associations with phenotype resistance and clinical presentation. Maximum Likelihood and Minimum Spanning Trees were used to determine strain correlations and identify potential transmission clusters.
Overall, 15 different STs were found; the predominant ones included ST307 (35, 40.2%), ST512/1519 (15, 17.2%), ST20 (12, 13.8%), and ST101 (7, 8.1%). 33 (37.9%) KPC-Kp strains were noticed to be in five transmission clusters (median number of isolates in each cluster: 5 [3-10]), four of them characterized by intra-hospital transmission. All 87 strains harbored Tn4401a transposon, carrying bla (48, 55.2%), bla (38, 43.7%), and in one case (1.2%) bla the latter gene conferred resistance to ceftazidime/avibactam (CZA). Thirty strains (34.5%) harbored porin mutations; of them, 7 (8.1%) carried multiple Tn4401a copies. These strains were characterized by significantly higher CZA minimum inhibitory concentration compared with strains with no porin mutations or single Tn4401a copy, respectively, even if they did not overcome the resistance breakpoint of 8 ug/mL. Median 2 (IQR:1-2) virulence factors per strain were detected. The lowest number was observed in ST20 compared to the other STs (p<0.001). While ST307 was associated with infection events, a trend associated with colonization events could be observed for ST20.
Integration of genomic, resistance score, and clinical data allowed us to define a relative diversification of KPC-Kp in Northern Italy between 2019 and 2021, characterized by few large transmission chains and rare inter-hospital transmission. Our results also provided initial evidence of correlation between KPC-Kp genomic signatures and higher MIC levels to some antimicrobial agents or colonization/infection status, once again underlining WGS's importance in bacterial surveillance.
对产碳青霉烯酶肺炎克雷伯菌(KPC-Kp)进行基因组监测对于了解其毒力、耐药性监测和疫情控制至关重要。
对 2019 年至 2021 年意大利北部 3 家医院分离的 87 株 KPC-Kp 菌株进行全基因组测序(WGS)进行基因组分析,以鉴定其耐药组、毒力组和可移动组,并评估其与表型耐药性和临床特征的潜在关联。最大似然法和最小生成树用于确定菌株相关性并识别潜在的传播簇。
共发现 15 种不同的 ST,其中主要的包括 ST307(35,40.2%)、ST512/1519(15,17.2%)、ST20(12,13.8%)和 ST101(7,8.1%)。33(37.9%)株 KPC-Kp 被认为存在于五个传播簇中(每个簇的中位分离株数:5[3-10]),其中四个簇具有院内传播特征。所有 87 株菌均携带 Tn4401a 转座子,携带 bla(48,55.2%)、bla(38,43.7%),其中一株携带 bla 基因,该基因对头孢他啶/阿维巴坦(CZA)具有耐药性。30 株菌(34.5%)携带孔蛋白突变;其中 7 株(8.1%)携带多个 Tn4401a 拷贝。与无孔蛋白突变或单个 Tn4401a 拷贝的菌株相比,这些菌株的 CZA 最小抑菌浓度明显更高,尽管它们没有超过 8ug/ml 的耐药断点。每株菌检测到中位数为 2(IQR:1-2)的毒力因子。与其他 ST 相比,ST20 检测到的毒力因子数量最低(p<0.001)。ST307 与感染事件相关,而 ST20 则与定植事件相关。
基因组、耐药评分和临床数据的整合使我们能够确定 2019 年至 2021 年间意大利北部 KPC-Kp 的相对多样化,其特征是少数大型传播链和罕见的医院间传播。我们的研究结果还提供了 KPC-Kp 基因组特征与某些抗菌药物的更高 MIC 水平或定植/感染状态之间相关性的初步证据,再次强调了 WGS 在细菌监测中的重要性。
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