Klebsiella pneumoniae sequence type 147: a high-risk clone increasingly associated with plasmids carrying both resistance and virulence elements

IF 2.4 4区 医学 Q3 MICROBIOLOGY Journal of medical microbiology Pub Date : 2024-04-17 DOI:10.1099/jmm.0.001823
Jane F. Turton, Claire Perry, Kim McGowan, Jack A. Turton and Russell Hope
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Abstract

Introduction. The first hybrid resistance/virulence plasmid, combining elements from virulence plasmids described in hypervirulent types of Klebsiella pneumoniae with those from conjugative resistance plasmids, was described in an isolate of sequence type (ST) 147 from 2016. Subsequently, this type has been increasingly associated with these plasmids. Hypothesis or gap statement. The extent of carriage of hybrid virulence/resistance plasmids in nosocomial isolates of K. pneumoniae requires further investigation. Aim. To describe the occurrence of virulence/resistance plasmids among isolates of K. pneumoniae received by the UK reference laboratory, particularly among representatives of ST147, and to compare their sequences. Methodology. Isolates received by the laboratory during 2022 and the first half of 2023 (n=1278) were screened for virulence plasmids by PCR detection of rmpA/rmpA2 and typed by variable-number tandem repeat analysis. Twenty-nine representatives of ST147 (including a single-locus variant) from seven hospital laboratories were subjected to long-read nanopore sequencing using high-accuracy q20 chemistry to provide complete assemblies. Results. rmpA/rmpA2 were detected in 110 isolates, of which 59 belonged to hypervirulent K1-ST23, K2-ST86 and K2-ST65/375. Of the remainder, representatives of ST147 formed the largest group, with 22 rmpA/rmpA2-positive representatives (out of 47 isolates). Representatives were from 19 hospital laboratories, with rmpA/rmpA2-positive isolates from 10. Nanopore sequencing of 29 representatives of ST147 divided them into those with no virulence plasmid (n=12), those with non-New Delhi metallo-β-lactamase (NDM) virulence plasmids (n=6) and those carrying bla NDM-5 (n=9) or bla NDM-1 (n=2) virulence plasmids. These plasmids were of IncFIB(pNDM-Mar)/IncHI1B(pNDM-MAR) replicon types. Most of the non-NDM virulence plasmids were highly similar to the originally described KpvST147L_NDM plasmid. Those carrying bla NDM-5 were highly similar to one another and to previously described plasmids in ST383 and carried an extensive array of resistance genes. Comparison of the fully assembled chromosomes indicated multiple introductions of ST147 in UK hospitals. Conclusion. This study highlights the high proportion of representatives of ST147 that carry IncFIB(pNDM-Mar)/IncHI1B(pNDM-MAR) hybrid resistance virulence plasmids. It is important to be aware of the high probability that representatives of this type carry these plasmids combining resistance and virulence determinants and of the consequent increased risk to patients.
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肺炎克雷伯菌序列 147 型:与携带抗性和毒力元件的质粒日益相关的高风险克隆
导言。2016 年,在一个序列类型(ST)147 的分离株中首次描述了抗性/毒力混合质粒,该质粒结合了在肺炎克雷伯氏菌高毒力类型中描述的毒力质粒元素和共轭抗性质粒元素。随后,该类型越来越多地与这些质粒有关。肺炎克雷伯菌的鼻腔分离物中携带混合毒力/耐药性质粒的程度需要进一步调查。描述英国参考实验室收到的肺炎克雷伯菌分离株中毒力/耐药性质粒的发生情况,尤其是 ST147 的代表株,并比较其序列。通过 PCR 检测 rmpA/rmpA2 筛选实验室在 2022 年和 2023 年上半年收到的分离株(n=1278)中的毒力质粒,并通过变数串联重复分析进行分型。对来自 7 家医院实验室的 29 个 ST147 代表株(包括一个单病灶变异株)使用高精度 q20 化学方法进行了长读程纳米孔测序,以提供完整的组合。在其余的分离物中,ST147 的代表构成了最大的群体,有 22 个 rmpA/rmpA2 阳性的代表(在 47 个分离物中)。这些代表来自 19 家医院实验室,其中 10 家实验室的分离物为 rmpA/rmpA2 阳性。对 29 个 ST147 代表株进行了纳米孔测序,将其分为无毒力质粒(12 个)、非新德里金属β-内酰胺酶(NDM)毒力质粒(6 个)和携带 blaNDM-5 (9 个)或 blaNDM-1 (2 个)毒力质粒的代表株。这些质粒属于 IncFIB(pNDM-Mar)/IncHI1B(pNDM-MAR) 复制子类型。大多数非 NDM 毒力质粒与最初描述的 KpvST147L_NDM 质粒高度相似。携带 blaNDM-5 的质粒彼此高度相似,也与之前描述的 ST383 中的质粒高度相似,并携带大量抗性基因。比较完全组装的染色体表明,ST147 在英国医院中多次引入。本研究强调了 ST147 中携带 IncFIB(pNDM-Mar)/IncHI1B(pNDM-MAR) 杂交抗性毒力质粒的高比例代表。我们必须意识到这种类型的细菌极有可能携带这些结合了抗药性和毒力决定因子的质粒,从而增加了患者的风险。
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来源期刊
Journal of medical microbiology
Journal of medical microbiology 医学-微生物学
CiteScore
5.50
自引率
3.30%
发文量
143
审稿时长
4.5 months
期刊介绍: Journal of Medical Microbiology provides comprehensive coverage of medical, dental and veterinary microbiology, and infectious diseases. We welcome everything from laboratory research to clinical trials, including bacteriology, virology, mycology and parasitology. We publish articles under the following subject categories: Antimicrobial resistance; Clinical microbiology; Disease, diagnosis and diagnostics; Medical mycology; Molecular and microbial epidemiology; Microbiome and microbial ecology in health; One Health; Pathogenesis, virulence and host response; Prevention, therapy and therapeutics
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