Abstract
Analysis of sequencing data for 143 blaNDM-1- and blaOXA-48-positive Klebsiella pneumoniae isolates from 13 European national collections and the public domain resulted in the identification of 15 previously undetected multi-country transmission clusters. For 10 clusters, cases had prior travel/hospitalisation history in countries outside of the European Union including Egypt, Iran, Morocco, Russia, Serbia, Tunisia and Turkey. These findings highlight the benefit of European whole genome sequencing-based surveillance and data sharing for control of antimicrobial resistance.
Keywords: carbapenem-resistant Enterobacterales; carbapenemase; OXA-48, NDM-1; Klebsiella pneumonia; surveillance; whole genome sequencing; cross-border import
An alert regarding an outbreak of carbapenem-resistant Klebsiella pneumoniae carrying blaNDM-1 and blaOXA-48 carbapenemase-encoding genes was sent by Germany to European Union (EU)/European Economic Area (EEA) countries in October 2019 [1,2]. Since only limited whole genome sequencing (WGS) data on blaNDM-1- and blaOXA-48-positive K. pneumoniae were available in the public domain, national public health reference or equivalent expert laboratories from EU/EEA countries were invited to share WGS data from their national collections with the European Centre for Disease Prevention and Control (ECDC) to investigate the international dissemination of this epidemic strain. The analysis identified a Finnish case with an isolate closely related to the German outbreak strain and with an epidemiological link to St. Petersburg, Russia [1]. In addition, several other clusters of genetically related blaNDM-1- and blaOXA-48-positive K. pneumoniae unrelated to the German outbreak strain but affecting numerous EU/EEA countries were identified. The aim of this follow-up investigation was to characterise these clusters based on the integrated analysis of the WGS dataset on blaNDM-1- and blaOXA-48-positive K. pneumoniae submitted from 13 EU/EEA countries and additional epidemiological data.
Definitions and origin of samples and data
A case was defined as an individual with an isolate of K. pneumoniae carrying both blaNDM-1 and blaOXA-48. An epidemiological link to a specific country was defined as either documented hospitalisation in or travel to this country within 6 months before isolation of the respective isolate. Samples and epidemiological information on blaNDM-1- and blaOXA-48-positive K. pneumoniae were provided by 13 EU/EEA countries by 5 December 2019: Belgium (n = 1), Denmark (n = 5), Finland (n = 2), France (n = 18), Germany (n = 39), Ireland (n = 1), Italy (n = 1), the Netherlands (n = 15), Norway (n = 1), Slovenia (n = 7), Spain (n = 3), Sweden (n = 8) and the UK (n = 16). Worldwide publicly available WGS data were retrieved from the National Centre for Biotechnology Information (NCBI) database on 23 November 2019. In total, WGS data from 143 isolates, i.e. 117 isolates from national collections and 26 publicly available isolates, were included in the analysis.
Ethical statement
All data were anonymised and collected in accordance with the European Parliament and Council decisions on the epidemiological surveillance and control of communicable disease in the European Community. Ethical approval and informed consent were thus not required.
Whole genome sequencing analysis
Sequence data were processed as previously described [3]. The variants identified were used to create a pseudochromosome using a custom script (https://figshare.com/s/c7be54e5930e8b6a4103). The isolates were subjected to quality checks based on the highest proportion of reads mapping to K. pneumoniae obtained in Kraken, on sequencing coverage depth (range: 18–280×), on the number of heterozygous single nucleotide polymorphisms (SNP) which is indicative of contamination within species, and on mapped reference coverage at 5× (> 90%). Pairwise distance between isolates was calculated using SNP-sites v2.4.0 and snp-dists v0.6.3. Clusters of related isolates were identified using hierarchical clustering (Ward.D2) of 50 SNP. This more sensitive and less specific SNP threshold was chosen in the absence of a standard threshold acceptable for all K. pneumoniae sequence types (ST). A maximum likelihood tree was created using IQ-TREE with 1,000 bootstraps and a midpoint root based on SNP identified in 137 isolates over the entire chromosome. The maximum likelihood tree was visualised using iTOL [4]. Multilocus sequence types were identified as previously described [3]. All strains were screened for the presence of antimicrobial resistance (AMR) genes using ARIBA with the Resfinder database [5] except for 12 isolates with long-read data that were analysed using Kleborate [6]. Sequence data for all isolates have been submitted to the European Nucleotide Archive under study accession number PRJEB35890 [7].
Phylogenetic structure
Of the 117 isolates from national collections, three were excluded as they did not fulfil the case definition and two additional isolates were excluded because they contained a large number of heterozygous SNP sites (n = 2,498–9,766) indicating possible contamination. Of the 26 publicly accessible genomes, 18 had metadata on location of origin. After analysing the quality control of the sequences, one genome was removed because of the large number of heterozygous SNP sites (n = 650). The overall phylogenetic structure of the K. pneumoniae collection is presented in Figure 1. The resistome profiles were not entirely homogeneous within clusters, except for clusters 4, 12 and 15 (Figure 2).
Cross-border transmission
Cross-border transmission was reported if case isolates from two or more countries were found to belong to the same specific genetic cluster, and only clusters with samples from at least two different countries are presented here. Fifteen clusters were identified that affected at least two countries, indicative of cross-border transmission. Ten of these clusters included recent isolates detected in 2018 or 2019. The size of the clusters ranged from two to 13 samples, and involved up to three different countries (Table). Of the 13 EU/EEA countries submitting national data for this analysis, 10 countries had at least one isolate in one of the cross-border clusters. For 10 clusters, epidemiological data from the patient history suggested a possible link to a country outside the EU/EEA such as Egypt, Iran, Morocco, Russia, Serbia, Tunisia and Turkey (Table and Figure 3). However, Figure 3 also indicates transmission of isolates between EU/EEA countries (1 case) and within the same country (16 cases).
Table. Epidemiological links and genomic characteristics of blaNDM-1- and blaOXA-48-positive Klebsiella pneumoniae isolates by cluster involving at least two countries (n = 15 clusters, n = 56 isolates).
Cluster number (size) |
Sequence type |
Countries where isolates were detected (year) | SNP distance (range) | β-lactamase resistance genes shared by all isolates | β-lactamase resistance genes not shared by all isolates | Reported history of travel or hospitalisation outside the EU/EEA |
---|---|---|---|---|---|---|
1 (n = 2) | ST11 | France (2018), Omana | 38 | blaOXA-1, blaNDM-1, blaOXA-48, blaCTX-M-15, blaSHV-182 | blaTEM-1B | Tunisia (n = 1) |
2 (n = 2) | UK (2014), Pakistana | 35 | blaSHV-182, blaNDM-1, blaOXA-48 | blaOXA-1, blaCTX-M-15 | None | |
3 (n = 4) | ST14 | Germany (2016, 2017), the Netherlands (2016, 2017) | 0–29 | blaOXA-1, blaNDM-1, blaCTX-M-15, blaOXA-48 | blaSHV-16, blaSHV-70, blaSHV-73, blaTEM-1A, | Turkey (n = 1) |
4 (n = 3) | Germany (2019, n = 2), the Netherlands (2018) | 0–5 | blaOXA-1, blaNDM-1, blaOXA-48, blaCTX-M-15, blaSHV-70, blaTEM-1A | None | Turkey (n = 1) | |
5 (n = 2) | France (2019), Germany (2016) | 47 | blaNDM-1, blaOXA-48, blaCTX-M-15, blaOXA-1 | blaSHV-70, blaTEM-1A | None | |
6 (n = 2) | France (2019), Germany (2018) | 34 | blaOXA-1, blaNDM-1, blaOXA-48, blaCTX-15 | blaTEM-1A, blaSHV-28, blaSHV-70 | None | |
7 (n = 4) | ST15 | Denmark (2016), France (2019; n = 2), Ireland (2019) | 5–37 | blaOXA-1, blaCMY-4, blaNDM-1, blaOXA-48 | blaSHV-12, blaSHV-28, blaSHV-185 | Morocco (n = 3)b |
8 (n = 4) | ST101c | Denmark (2017, 2018), Italy (2016), UK (2015) | 11–31 | blaSHV-28, blaOXA-9, blaNDM-1, blaOXA-48, blaTEM-1A | blaCTX-M-14b, blaCTX-M-15 | Egypt (n = 3)b |
9 (n = 6) | ST101 | Sloveniaa, Serbia (n = 5)a | 1–15 | blaSHV-28, blaOXA-10, blaSCO-1, blaNDM-1, blaOXA-48, blaCTX-M-15 | blaCMY-4, blaTEM-1A, blaTEM-1B | None |
10 (n = 2) | Denmark (2017), Slovenia (2014) | 19 |
blaNDM-1, blaOXA-48, blaCTX-M-15, blaOXA-1, blaSHV-28, blaCMY-4, blaTEM-1A, blaOXA-10 |
blaSCO-1 | Serbia (n = 1) | |
11 (n = 3) | ST147 | The Netherlands (2016), Spain (2016; n = 2) | 15–36 |
blaSHV-67, blaNDM-1, blaOXA-48, blaCTX-M-15 |
None | Egypt (n = 1) |
12 (n = 2) | Denmark (2016), the Netherlands (2018) | 21 | blaOXA-1, blaNDM-1, blaOXA-48, blaCTX-M-15, blaSHV-12, blaTEM-1B | None | Iran (n = 1) | |
13 (n = 3) | France (2018; n = 2), the Netherlands (2019) | 21–39 |
blaSHV-67, blaNDM-1, blaOXA-48, blaTEM-1B |
blaOXA-1, blaCTX-M-15 | Tunisia (n = 2)b | |
14 (n = 4) | ST147/ST2084c | France (2018; n = 2), France (2019), UK (2015) | 10–43 | blaSHV-67, blaNDM-1, blaOXA-48, blaCTX-M-15, blaOXA-1, blaTEM-1B | None | None |
15 (n = 13) | ST307 | Finland (2019), Germany (2019; n = 12) | 0–15 | blaSHV-28, blaNDM-1, blaOXA-48, blaCTX-M-15, blaTEM-1B | None | Russia (n = 1) |
EEA: European Economic Area; EU: European Union; SNP: single nucleotide polymorphism; UK: United Kingdom.
Including 48 genomes from national collections of EU/EEA countries, 2014–19, and 8 genomes accessed from the public domain available on 23 November 2019.
a Data from the public domain; year not available.
b Same country of travel or hospitalisation was reported for isolates within the cluster from at least two different EU/EEA countries.
c One isolate in cluster 8 and two isolates in cluster 14 had a single nucleotide variation in one multilocus sequence typing allele (rpoB in cluster 8 and mdh in cluster 14).
Discussion
The cross-border transmission or introduction of multidrug-resistant organisms (MDRO) such as blaNDM-1- and blaOXA-48-positive K. pneumoniae revealed in this study is a threat to public health and may lead to further spread within the EU/EEA as documented by recent outbreaks [1,8,9]. Our findings highlight the importance of including prior hospitalisation or recent travel to areas with a high prevalence MDRO as a risk a factor for hospital admission screening. Failing to detect carriage of MDRO may not only be detrimental for the individual patient, but also increases the likelihood of undetected transmission in the healthcare setting.
The available epidemiological information suggested several possible countries of origin for the described transmission clusters. However, the data collection was restricted to countries with the national capacity and funding to generate WGS data. Unfortunately, epidemiological evidence for a link with a non-EU/EEA country could not be substantiated by WGS results because WGS data from the potential countries of origin were not available. The evidence that epidemiologically linked countries were the sources for the respective isolates is therefore inconclusive. However, the hypothesis of potential countries of origin including Egypt, Iran, Morocco, Russia, Tunisia and Turkey is supported by the reported occurrence of blaNDM-1- and blaOXA-48-positive K. pneumoniae in those countries [10-15].
Currently established European AMR surveillance systems did not detect these multinational clusters. This study highlights the benefit of international collaboration and data sharing as these clusters were only identified by pooling of WGS data from 13 national collections. Development of WGS-based surveillance is under way with the European Antimicrobial Resistance Genes Surveillance Network (EURGen-Net), but is not yet established. The EU/EEA countries that do not perform WGS for AMR control [16,17], lack the information to elucidate cross-border transmission routes. Consequently, the identified transmission clusters may involve many more countries than described here. In addition to data sharing as part of EU-wide outbreak investigations, archiving of WGS data in the public domain provides epidemiological context for interpreting local and national data and enhances the identification of the putative sources of an outbreak with a wider benefit for AMR control.
The repeated cross-border spread of MDRO challenges the control of AMR in the EU/EEA including in countries with good detection capacity, vigorous infection prevention and control (IPC) measures and good antibiotic stewardship practices. Detection requires adequate clinical laboratory capacity to detect carbapenemase-producing Enterobacterales, sufficient WGS capacity in all EU/EEA countries to characterise the isolates and secure mechanisms for rapid sharing of WGS data at European and international level. Control requires sufficient resources for the implementation of IPC measures and cooperation with and provision of support in all these areas to countries neighbouring the EU/EEA as well as worldwide.
Conflict of interest: K. L. H. is a member of PHE’s Antimicrobial Resistance and Healthcare Associated Infections Reference Unit, which has received financial support for conference attendance, lectures, research projects, or contracted evaluations from numerous sources, including Accelerate Diagnostics, Achaogen Inc, Allecra Therapeutics, Amplex, AstraZeneca UK Ltd, AusDiagnostics, Basilea Pharmaceutica, Becton Dickinson Diagnostics, bioMérieux, Bio-Rad Laboratories, British Society for Antimicrobial Chemotherapy, Cepheid, Check-Points B.V., Cubist Pharmaceuticals, Department of Health, Enigma Diagnostics, the European Centre for Disease Prevention and Control, Food Standards Agency, GenePOC, GlaxoSmithKline Services Ltd, Helperby Therapeutics, Henry Stewart Talks, International Health Management Associates Ltd, Innovate UK, Kalidex Pharmaceuticals, Melinta Therapeutics, Merck Sharpe and Dohme, Meiji Seika Pharma Co Ltd, Mobidiag, Momentum Biosciences Ltd, Neem Biotech, NIHR, Nordic Pharma Ltd, Norgine Pharmaceuticals, Paratek, Rabiotics Rx, Rempex Pharmaceuticals Ltd, Roche, Rokitan Ltd, Smith and Nephew UK Ltd, Shionogi and Co Ltd, Tetraphase Pharmaceuticals, Trius Therapeutics, VenatoRx Pharmaceuticals, Wockhardt Ltd, and the World Health Organization.
Authors’ contributions: CL: design of study, bioinformatic analysis and drafting of the manuscript; FL: statistical analysis and drafting of the manuscript; EA: bioinformatic analysis, NK: bioinformatic analysis; BA: design of study and drafting of the manuscript; TH, OD, AMH, HH, JJ, KR, LD, ABJ, SG, SH, MC, WB, MDG, MM, LS, OS, MP, TC, JOI, MPV, KS, PE, KLH: design of study, compilation and analysis of national data, interpretation of results; KJ, MJS, DP, DLM: design of study and interpretation of results; AK: coordination of study and drafting of manuscript. All authors: review of manuscript.
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