Investigating the molecular transmission dynamics of blaNDM in antibiotic-selective environments.

IF 3 3区 生物学 Q3 MICROBIOLOGY
Journal of Bacteriology Pub Date : 2025-09-18 Epub Date: 2025-08-11 DOI:10.1128/jb.00133-25
Shashi Kumari, Lekshmi Narendrakumar, Meenal Chawla, Sanjib Das, Hemanta Koley, Bhabatosh Das
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引用次数: 0

Abstract

Carbapenem resistance mediated by blaNDM-encoded metallo-beta-lactamases is often linked to ISAba125, an insertion sequence from the IS30 family, which is widely distributed among critical and high-priority bacterial pathogens. The rapid dissemination of ISAba125-linked blaNDM in both nosocomial and community-acquired infections presents a serious challenge to healthcare systems and pharmaceutical industries. Despite the urgency of this issue, the factors driving blaNDM spread and the molecular mechanisms governing ISAba125 mobility remain poorly understood. In this study, we engineered the genomes of Vibrio cholerae and Escherichia coli to investigate the mobility of blaNDM under controlled conditions both with and without the genetically linked ISAba125. We also examined the transmission efficiency and the stability of blaNDM in environments with and without sublethal antibiotic concentrations. Our in vitro findings were validated in a rabbit ileal loop model. The results revealed that antibiotic pressure significantly influences the mobility of blaNDM, shedding light on the molecular dynamics of its transmission. These insights are crucial for developing strategies to curb the spread of blaNDM and mitigate the growing threat of carbapenem resistance in bacterial pathogens.IMPORTANCEInsertion sequences are the simplest form of mobile genetic elements that play a critical role in the adaptation of bacteria, allowing them to rapidly acquire new traits like resistance genes that enhance their survival. ISAba125 is one such insertion sequence that facilitates the spread of blaNDM, contributing to the global challenge of carbapenem resistance. In this study, we developed reporter strains that could be used as a valuable tool for investigating the dynamics of ISAba125-linked blaNDMsh-ble and evaluated the transposition frequency of ISAba125-linked blaNDMsh-ble in the presence and absence of sublethal concentration of antibiotics. Our results demonstrated that ISAba125 enhances the spread of blaNDMsh-ble under sublethal concentration of antibiotics that induces SOS response.

研究blaNDM在抗生素选择性环境中的分子传播动力学。
由blandm编码的金属- β -内酰胺酶介导的碳青霉烯耐药通常与IS30家族的一个插入序列ISAba125有关,该序列广泛分布于关键和高优先级细菌病原体中。在医院和社区获得性感染中,与isaba125相关的blaNDM的迅速传播对医疗保健系统和制药行业提出了严峻的挑战。尽管这一问题迫在眉睫,但驱动blaNDM传播的因素和控制ISAba125迁移的分子机制仍然知之甚少。在这项研究中,我们设计了霍乱弧菌和大肠杆菌的基因组,以研究在有和没有基因连锁的ISAba125的控制条件下blaNDM的移动性。我们还检查了blaNDM在有和没有亚致死抗生素浓度的环境中的传播效率和稳定性。我们的体外研究结果在兔回肠环模型中得到了验证。结果表明,抗生素压力显著影响blaNDM的移动性,揭示了其传播的分子动力学。这些见解对于制定策略来遏制blaNDM的传播和减轻细菌病原体中碳青霉烯耐药性日益增长的威胁至关重要。插入序列是可移动遗传元件的最简单形式,在细菌的适应中起着关键作用,使它们能够迅速获得新的特性,如提高其生存能力的抗性基因。ISAba125就是这样一个插入序列,它促进了blaNDM的传播,有助于全球碳青霉烯类耐药性的挑战。在这项研究中,我们开发了报告菌株,可以作为研究isaba125连锁blaNDMsh-ble的动态的有价值的工具,并评估了isaba125连锁blaNDMsh-ble在存在和不存在亚致死浓度抗生素的情况下的转位频率。我们的研究结果表明,ISAba125在亚致死浓度抗生素诱导的SOS反应下促进了blaNDMsh-ble的传播。
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
Journal of Bacteriology
Journal of Bacteriology 生物-微生物学
CiteScore
6.10
自引率
9.40%
发文量
324
审稿时长
1.3 months
期刊介绍: The Journal of Bacteriology (JB) publishes research articles that probe fundamental processes in bacteria, archaea and their viruses, and the molecular mechanisms by which they interact with each other and with their hosts and their environments.
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