Convergence of multidrug resistance and efflux-mediated biocide tolerance in klebsiella pneumoniae ST307: implications for nosocomial infection control in Iranian hospitals.

IF 3.4 3区医学 Q2 INFECTIOUS DISEASES

BMC Infectious Diseases Pub Date : 2025-06-03 DOI:10.1186/s12879-025-11178-w

Rezvan Goodarzi, Sima Kazemi, Mohammad Hossein Nasershariati, Babak Asghari

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引用次数: 0

Abstract

Background: The relentless evolution of K. pneumoniae ST307 into a "superbug" with dual resistance to last-line antibiotics and hospital disinfectants poses an existential threat to infection control. This study characterizes the molecular epidemiology, resistance profiles, and biocide tolerance of ST307 isolates from Iranian hospitals, highlighting its role in nosocomial outbreaks.

Methods: A multicenter cross-sectional analysis of 500 K. pneumoniae isolates (2022-2024) utilized CLSI-compliant disk diffusion, broth microdilution, and PCR for resistance genes (bla_CTX-M-15, bla_NDM-1,cepA, qacED1). Biocide MICs were correlated with genetic markers.

Results: ST307 accounted for 30% (150/500) of isolates, predominantly from ICUs. Resistance rates included meropenem (60.0%; MIC₅₀ >32 µg/mL), ciprofloxacin (75.3%), and gentamicin (45.3%). Colistin retained efficacy (85.3% susceptibility). Elevated biocide MICs (chlorhexidine ≥ 0.5% [70.0%]; benzalkonium chloride ≥ 0.1% [65.3%]) correlated with cepA (65.3%) and qacED1 (70.0%) positivity (p < 0.01). Carbapenemase genes bla_OXA-48 (22.0%) and bla_NDM-1 (10.0%) co-occurred with ESBLs.

Conclusions: ST307's convergence of resistance mechanisms represents a catastrophic failure of current infection control frameworks. Without immediate interventions-such as ICU closures for deep disinfection, restricted colistin/tigecycline use, and genomic surveillance mandates-this clone will dominate Iranian hospitals within 3-5 years.

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肺炎克雷伯菌ST307多药耐药和外排介导的杀菌剂耐受趋同：对伊朗医院感染控制的影响

背景：肺炎克雷伯菌ST307不断进化为对最后一线抗生素和医院消毒剂具有双重耐药性的“超级细菌”，对感染控制构成了生存威胁。本研究分析了伊朗医院ST307分离株的分子流行病学、耐药性和杀菌剂耐受性，强调了其在医院暴发中的作用。方法：对500株（2022-2024）肺炎克雷伯菌分离株进行多中心横断面分析，采用符合clsi标准的圆盘扩散、肉汤微量稀释和PCR检测耐药基因（blaCTX-M-15、blaNDM-1、cepA、qacED1）。杀菌剂mic与遗传标记相关。结果：ST307占30%(150/500)，主要来自icu。耐药率包括美罗培南(60.0%；MIC₅₀>32µg/mL)，环丙沙星（75.3%）和庆大霉素（45.3%）。粘菌素保留疗效（敏感性85.3%）。杀菌剂mic升高(氯己定≥0.5% [70.0%]；苯并氯铵≥0.1%[65.3%])与cepA（65.3%）、qacED1（70.0%）阳性相关(OXA-48（22.0%）、blaNDM-1（10.0%）与ESBLs共发生。结论：ST307耐药机制的趋同代表了当前感染控制框架的灾难性失败。如果不立即采取干预措施，如关闭ICU进行深度消毒，限制粘菌素/替加环素的使用，以及强制进行基因组监测，这种克隆病毒将在3-5年内主导伊朗的医院。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

BMC Infectious Diseases 医学-传染病学

CiteScore

6.50

自引率

0.00%

发文量

860

审稿时长

3.3 months

期刊介绍： BMC Infectious Diseases is an open access, peer-reviewed journal that considers articles on all aspects of the prevention, diagnosis and management of infectious and sexually transmitted diseases in humans, as well as related molecular genetics, pathophysiology, and epidemiology.