Ceftazidime-avibactam tolerance and persistence among difficult-to-treat KPC-producing Klebsiella pneumoniae clinical isolates from bloodstream infections.

IF 3.7 3区医学 Q2 INFECTIOUS DISEASES European Journal of Clinical Microbiology & Infectious Diseases Pub Date : 2025-02-01 Epub Date: 2024-11-30 DOI:10.1007/s10096-024-05005-4

N Abichabki, G G Gaspar, L R Bortolato, D A F S Lima, L N Silva, R H C Pocente, J C Ferreira, T C Ogasawara, D Pereira, R R Guerra, C Wilhelm, P Barth, A F Martins, A Barth, G U L Braga, E C P De Martinis, J Bengtsson-Palme, F Bellissimo-Rodrigues, V R Bollela, A L C Darini, L N Andrade

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引用次数: 0

Abstract

Purpose: Tolerance and persistence occur "silently" in bacteria categorized as susceptible by antimicrobial susceptibility testing in clinical microbiology laboratories. They are different from resistance phenomena, not well-studied, and often remain unnoticeable. We aimed to investigate and characterize ceftazidime-avibactam (CZA) tolerance/persistence in 80 Klebsiella pneumoniae isolates from bloodstream infections.

Methods: We used the Tolerance Disk Test (TDtest) to detect CZA tolerance/persistence and investigate the avibactam (AVI) influence on them, and time-kill assays with minimal duration for killing (MDK) determination to characterize/differentiate CZA tolerance from persistence, for selected isolates. Whole genome sequencing was performed for 49/80 selected isolates to investigate genes related to beta-lactam tolerance/persistence and resistance as well as phylogeny studies.

Results: Tolerance/persistence to CZA was detected in 48/80 (60%) isolates, all extensively drug-resistant (XDR) or multidrug-resistant, carbapenem-resistant K. pneumoniae (CRKp), KPC producers, and previously categorized as susceptible (not resistant) to CZA. No heteroresistance was detected. CZA tolerance/persistence occurred due to ceftazidime tolerance/persistence and was not related to AVI in the CZA combination. 5/11 isolates were characterized as CZA-tolerant and 5/11 as CZA-persistent. The single (1/11) XDR and CRKp non-KPC producer was truly susceptible. All the CZA-tolerant/persistent isolates (ST11, ST258, ST340, ST437, ST16, ST17, and ST307) harbored the carbapenemase-encoding gene bla_KPC-2. Mutation in only two genes (rpoS and degQ) related to beta-lactam tolerance/persistence was found in only 7/49 CZA-tolerant/persistent isolates, suggesting the presence of yet unknown beta-lactam tolerance/persistence genes.

Conclusion: Among the K. pneumoniae bloodstream isolates studied, 60%, previously categorized as susceptible to CZA, were, actually, tolerant/persistent to this antibiotic, all these KPC producers.

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血液感染难治性产kpc肺炎克雷伯菌临床分离株头孢他啶-阿维巴坦耐受性和持久性

目的：耐受性和持久性在临床微生物实验室中通过抗菌药物敏感性试验被分类为敏感的细菌中“无声地”发生。它们不同于抗性现象，没有得到充分的研究，往往不被注意到。我们的目的是研究80株肺炎克雷伯菌血液感染分离株ceftazidime-avibactam （CZA）的耐受性和持久性。方法：采用耐药盘试验（TDtest）检测CZA耐受性/持久性，研究阿维巴坦（AVI）对其的影响，并采用最小杀伤时间（MDK）测定法对所选菌株进行CZA耐受性和持久性的表征和区分。选择49/80株菌株进行全基因组测序，研究与β -内酰胺耐受性/持久性和耐药性相关的基因，并进行系统发育研究。结果：在48/80株（60%）分离株中检测到对CZA的耐受性/持久性，这些分离株均为广泛耐药（XDR）或多重耐药，碳青霉烯耐药肺炎克雷伯菌（CRKp）， KPC生产者，先前被归类为对CZA敏感（不耐药）。未发现异抗。CZA耐受性/持久性是由于头孢他啶耐受性/持久性而发生的，与CZA联合用药的AVI无关。5/11分离株为cza耐受性菌株，5/11分离株为cza持久性菌株。单一（1/11）XDR和CRKp非kpc生产者是真正敏感的。所有耐cza /持久性菌株（ST11、ST258、ST340、ST437、ST16、ST17和ST307）都含有碳青霉烯酶编码基因blaKPC-2。在7/49株cza耐受性/持久性菌株中，仅发现与β -内酰胺耐受性/持久性相关的两个基因（rpoS和degQ）发生突变，表明存在未知的β -内酰胺耐受性/持久性基因。结论：在研究的肺炎克雷伯菌血液分离株中，60%以前被归类为CZA敏感的菌株实际上对这种抗生素具有耐受性/持久性，所有这些菌株都是KPC的产生者。

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来源期刊

European Journal of Clinical Microbiology & Infectious Diseases 医学-传染病学

CiteScore

10.40

自引率

2.20%

发文量

138

审稿时长

1 months

期刊介绍： EJCMID is an interdisciplinary journal devoted to the publication of communications on infectious diseases of bacterial, viral and parasitic origin.