Wang Xiaoli, Meng Tianjiao, Dai Yunqi, Ou Hong-Yu, Wang Meng, Tang Bin, Sun Jingyong, Cheng Decui, Pan Tingting, Tan Ruoming, Qu Hongping
Department of Critical Care Medicine, Ruijin Hospital, Shanghai Jiao Tong University School of Medicine, No. 197, Ruijin ER Road, Shanghai, 200025, China.
State Key Laboratory of Microbial Metabolism, Joint International Laboratory on Metabolic & Developmental Sciences, School of Life Sciences & Biotechnology, Shanghai Jiao Tong University, Shanghai, 200030, China.
Infection. 2025 Feb;53(1):271-283. doi: 10.1007/s15010-024-02365-z. Epub 2024 Aug 14.
We aimed to explore the prevalence and within-host evolution of resistance in polymyxin-heteroresistant carbapenem-resistant Klebsiella pneumoniae (PHR-CRKP) in critically ill patients.
We performed an epidemiological analysis of consecutive patients with PHR-CRKP from clinical cases. Our study investigated the within-host resistance evolution and its clinical significance during polymyxin exposure. Furthermore, we explored the mechanisms underlying the dynamic evolution of polymyxin resistance at both subpopulation and genetic levels, involved population analysis profile test, time-killing assays, competition experiments, and sanger sequencing. Additionally, comparative genomic analysis was performed on 713 carbapenemase-producing K. pneumoniae strains.
We enrolled 109 consecutive patients, and PHR-CRKP was found in 69.7% of patients without previous polymyxin exposure. 38.1% of PHR-CRKP isolates exhibited polymyxin resistance and led to therapeutic failure in critically ill scenarios. An increased frequency of resistant subpopulations was detected during PHR-CRKP evolution, with rapid regrowth of resistant subpopulations under high polymyxin concentrations, and a fitness cost in an antibiotic-free environment. Mechanistic analysis revealed that diverse mgrB insertions and pmrB hypermutations contributed to the dynamic changes in polymyxin susceptibility in dominant resistant subpopulations during PHR evolution, which were validated by comparative genomic analysis. Several deleterious mutations (e.g. pmrB, pmrB) were firstly detected during PHR-CRKP evolution. Indeed, specific sequence types of K. pneumoniae demonstrated unique deletions and deleterious mutations.
Our study emphasizes the high prevalence of pre-existing heteroresistance in CRKP, which can lead to polymyxin resistance and fatal outcomes. Hence, it is essential to continuously monitor and observe the treatment response to polymyxins in appropriate critically ill scenarios.
我们旨在探究重症患者中多粘菌素异质性耐药碳青霉烯类耐药肺炎克雷伯菌(PHR-CRKP)的耐药流行情况及其体内进化。
我们对临床病例中连续的PHR-CRKP患者进行了流行病学分析。我们的研究调查了多粘菌素暴露期间体内耐药性的演变及其临床意义。此外,我们在亚群和基因水平上探索了多粘菌素耐药动态演变的机制,涉及群体分析谱测试、时间杀菌试验、竞争实验和桑格测序。此外,对713株产碳青霉烯酶的肺炎克雷伯菌菌株进行了比较基因组分析。
我们纳入了109例连续患者,在69.7%既往未接触过多粘菌素的患者中发现了PHR-CRKP。38.1%的PHR-CRKP分离株表现出多粘菌素耐药,并在重症情况下导致治疗失败。在PHR-CRKP进化过程中检测到耐药亚群的频率增加,在高浓度多粘菌素作用下耐药亚群迅速再生,且在无抗生素环境中有适应性代价。机制分析表明,多种mgrB插入和pmrB超突变导致了PHR进化过程中优势耐药亚群多粘菌素敏感性的动态变化,这通过比较基因组分析得到了验证。在PHR-CRKP进化过程中首次检测到一些有害突变(如pmrB、pmrB)。事实上,肺炎克雷伯菌的特定序列类型表现出独特的缺失和有害突变。
我们的研究强调了CRKP中预先存在的异质性耐药的高流行率,这可能导致多粘菌素耐药和致命后果。因此,在适当的重症情况下持续监测和观察对多粘菌素的治疗反应至关重要。
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