Presence of hypervirulence-associated determinants in Klebsiella pneumoniae from hospitalised patients in Germany

IF 4.5 3区 医学 Q1 MICROBIOLOGY International Journal of Medical Microbiology Pub Date : 2024-02-08 DOI:10.1016/j.ijmm.2024.151601
Anika Wahl , Martin A. Fischer , Kathleen Klaper , Annelie Müller , Stefan Borgmann , Johannes Friesen , Klaus-Peter Hunfeld , Arkadius Ilmberger , Susanne Kolbe-Busch , Michael Kresken , Norman Lippmann , Christoph Lübbert , Matthias Marschner , Bernd Neumann , Niels Pfennigwerth , Michael Probst-Kepper , Jürgen Rödel , Marco H. Schulze , Andreas E. Zautner , Guido Werner , Yvonne Pfeifer
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Today, <em>K. pneumoniae</em> is one of the most persistent nosocomial pathogens worldwide and poses a severe threat/burden to public health by causing urinary tract infections, pneumonia and bloodstream infections. Infections mainly affect immunocompromised individuals and hospitalised patients. In recent years, a new type of <em>K. pneumoniae</em> has emerged associated with community-acquired infections such as pyogenic liver abscess in otherwise healthy individuals and is therefore termed hypervirulent <em>K. pneumoniae</em> (hv<em>Kp</em>). The aim of this study was the characterisation of <em>K. pneumoniae</em> isolates with properties of hypervirulence from Germany.</p></div><div><h3>Methods</h3><p>A set of 62 potentially hypervirulent <em>K. pneumoniae</em> isolates from human patients was compiled. Inclusion criteria were the presence of at least one determinant that has been previously associated with hypervirulence: (I) clinical manifestation, (II) a positive string test as a marker for hypermucoviscosity, and (III) presence of virulence associated genes <em>rmpA</em> and/or <em>rmpA2</em> and/or <em>magA</em>. Phenotypic characterisation of the isolates included antimicrobial resistance testing by broth microdilution. Whole genome sequencing (WGS) was performed using Illumina® MiSeq/NextSeq to investigate the genetic repertoire such as multi-locus sequence types (ST), capsule types (K), further virulence associated genes and resistance genes of the collected isolates. For selected isolates long-read sequencing was applied and plasmid sequences with resistance and virulence determinants were compared.</p></div><div><h3>Results</h3><p>WGS analyses confirmed presence of several signature genes for hv<em>Kp</em>. Among them, the most prevalent were the siderophore loci <em>iuc</em> and <em>ybt</em> and the capsule regulator genes <em>rmpA</em> and <em>rmpA2</em>. The most dominant ST among the hv<em>Kp</em> isolates were ST395 capsule type K2 and ST395 capsule type K5; both have been described previously and were confirmed by our data as multidrug-resistant (MDR) isolates. ST23 capsule type K1 was the second most abundant ST in this study; this ST has been described as commonly associated with hypervirulence. In general, resistance to beta-lactams caused by the production of extended-spectrum beta-lactamases (ESBL) and carbapenemases was observed frequently in our isolates, confirming the threatening rise of MDR-hv<em>Kp</em> strains.</p></div><div><h3>Conclusions</h3><p>Our study results show that <em>K. pneumoniae</em> strains that carry several determinants of hypervirulence are present for many years in Germany. The detection of carbapenemase genes and hypervirulence associated genes on the same plasmid is highly problematic and requires intensified screening and molecular surveillance. However, the non-uniform definition of hv<em>Kp</em> complicates their detection. Testing for hypermucoviscosity alone is not specific enough to identify hv<em>Kp</em>. 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Abstract

Background

Klebsiella (K.) pneumoniae is a ubiquitous Gram-negative bacterium and a common coloniser of animals and humans. Today, K. pneumoniae is one of the most persistent nosocomial pathogens worldwide and poses a severe threat/burden to public health by causing urinary tract infections, pneumonia and bloodstream infections. Infections mainly affect immunocompromised individuals and hospitalised patients. In recent years, a new type of K. pneumoniae has emerged associated with community-acquired infections such as pyogenic liver abscess in otherwise healthy individuals and is therefore termed hypervirulent K. pneumoniae (hvKp). The aim of this study was the characterisation of K. pneumoniae isolates with properties of hypervirulence from Germany.

Methods

A set of 62 potentially hypervirulent K. pneumoniae isolates from human patients was compiled. Inclusion criteria were the presence of at least one determinant that has been previously associated with hypervirulence: (I) clinical manifestation, (II) a positive string test as a marker for hypermucoviscosity, and (III) presence of virulence associated genes rmpA and/or rmpA2 and/or magA. Phenotypic characterisation of the isolates included antimicrobial resistance testing by broth microdilution. Whole genome sequencing (WGS) was performed using Illumina® MiSeq/NextSeq to investigate the genetic repertoire such as multi-locus sequence types (ST), capsule types (K), further virulence associated genes and resistance genes of the collected isolates. For selected isolates long-read sequencing was applied and plasmid sequences with resistance and virulence determinants were compared.

Results

WGS analyses confirmed presence of several signature genes for hvKp. Among them, the most prevalent were the siderophore loci iuc and ybt and the capsule regulator genes rmpA and rmpA2. The most dominant ST among the hvKp isolates were ST395 capsule type K2 and ST395 capsule type K5; both have been described previously and were confirmed by our data as multidrug-resistant (MDR) isolates. ST23 capsule type K1 was the second most abundant ST in this study; this ST has been described as commonly associated with hypervirulence. In general, resistance to beta-lactams caused by the production of extended-spectrum beta-lactamases (ESBL) and carbapenemases was observed frequently in our isolates, confirming the threatening rise of MDR-hvKp strains.

Conclusions

Our study results show that K. pneumoniae strains that carry several determinants of hypervirulence are present for many years in Germany. The detection of carbapenemase genes and hypervirulence associated genes on the same plasmid is highly problematic and requires intensified screening and molecular surveillance. However, the non-uniform definition of hvKp complicates their detection. Testing for hypermucoviscosity alone is not specific enough to identify hvKp. Thus, we suggest that the classification of hvKp should be applied to isolates that not only fulfil phenotypical criteria (severe clinical manifestations, hypermucoviscosity) but also (I) the presence of at least two virulence loci e.g. iuc and ybt, and (II) the presence of rmpA and/or rmpA2.

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德国住院病人肺炎克雷伯氏菌中存在与高致病力相关的决定因子
背景肺炎克雷伯氏菌(K. pneumoniae)是一种无处不在的革兰氏阴性菌,是动物和人类的常见定植菌。如今,肺炎克雷伯菌是全球最顽固的医院病原体之一,可引起尿路感染、肺炎和血流感染,对公共卫生构成严重威胁/负担。感染主要影响免疫力低下的人和住院病人。近年来,出现了一种新型肺炎克氏菌,它与社区获得性感染(如健康人的化脓性肝脓肿)有关,因此被称为高病毒性肺炎克氏菌(hvKp)。本研究的目的是分析德国分离出的具有高病毒特性的肺炎克菌。纳入标准是至少存在一个以前与高致病力相关的决定因素:(I) 临床表现,(II) 作为高黏液性标记的字符串测试呈阳性,(III) 存在与致病力相关的基因 rmpA 和/或 rmpA2 和/或 magA。分离物的表型特征包括肉汤微稀释法抗菌药耐药性测试。利用 Illumina® MiSeq/NextSeq 进行了全基因组测序(WGS),以研究收集到的分离物的基因谱系,如多焦点序列类型(ST)、胶囊类型(K)、进一步的毒力相关基因和抗性基因。结果WGS分析证实了hvKp存在多个特征基因。其中最普遍的是嗜苷基因座 iuc 和 ybt 以及胶囊调节基因 rmpA 和 rmpA2。hvKp 分离物中最主要的 ST 是 ST395 胶囊 K2 型和 ST395 胶囊 K5 型;这两种类型以前都曾被描述过,我们的数据证实它们是耐多药(MDR)分离物。ST23 胶囊型 K1 是本研究中数量第二多的 ST;据描述,这种 ST 通常与高病毒性有关。总体而言,在我们的分离株中经常观察到因产生广谱β-内酰胺酶(ESBL)和碳青霉烯酶而导致的对β-内酰胺类药物的耐药性,这证实了 MDR-hvKp 菌株的威胁性上升。在同一质粒上检测碳青霉烯酶基因和高致病力相关基因问题很大,需要加强筛查和分子监测。然而,由于 hvKp 的定义不统一,导致检测工作变得复杂。仅检测高粘度不足以特异性地识别 hvKp。因此,我们建议 hvKp 的分类应适用于不仅符合表型标准(严重的临床表现、高黏液性),而且(I) 存在至少两个毒力基因座(如 iuc 和 ybt)和 (II) 存在 rmpA 和/或 rmpA2 的分离物。
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来源期刊
CiteScore
9.70
自引率
0.00%
发文量
18
审稿时长
45 days
期刊介绍: Pathogen genome sequencing projects have provided a wealth of data that need to be set in context to pathogenicity and the outcome of infections. In addition, the interplay between a pathogen and its host cell has become increasingly important to understand and interfere with diseases caused by microbial pathogens. IJMM meets these needs by focussing on genome and proteome analyses, studies dealing with the molecular mechanisms of pathogenicity and the evolution of pathogenic agents, the interactions between pathogens and host cells ("cellular microbiology"), and molecular epidemiology. To help the reader keeping up with the rapidly evolving new findings in the field of medical microbiology, IJMM publishes original articles, case studies and topical, state-of-the-art mini-reviews in a well balanced fashion. All articles are strictly peer-reviewed. Important topics are reinforced by 2 special issues per year dedicated to a particular theme. Finally, at irregular intervals, current opinions on recent or future developments in medical microbiology are presented in an editorial section.
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