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6. Harbor Porpoise Deaths Associated with Erysipelothrix rhusiopathiae, the Netherlands, 2021

Author

IJsseldijk, Lonneke L., Begeman, Lineke, Duim, Birgitta, Grone, Andrea, Kik, Marja J.L., Klijnstra, Mirjam D., Lakemeyer, Jan, Leopold, Mardik F., Munnink, Bas B. Oude, Doeschate, Mariel ten, van Schalkwijk, Linde, Zomer, Aldert, Bloois, Linda van der Graaf-van, and Broens, Els M.

Subjects
Porpoises -- Diseases -- Causes of, Wildlife diseases -- Causes of, Gram-positive bacterial infections -- Causes of, Emerging communicable diseases -- Causes of, Health
Abstract

Erysipelothrix bacteria cause infections in humans and other species after contact with infected animals or environmental sources (1). Illness ranges from mild to systemic, which can include septicemia and endocarditis. [...]

Published
2023

11. Extended period of selection for antimicrobial resistance due to recirculation of persistent antimicrobials in broilers.

Author

Swinkels, Aram F, Berendsen, Bjorn J A, Fischer, Egil A J, Zomer, Aldert L, and Wagenaar, Jaap A

Subjects
DRUG resistance in bacteria, ESCHERICHIA coli, DRUG resistance in microorganisms, ANIMAL behavior, FLUOROQUINOLONES
Abstract

Objectives Antimicrobials can select for antimicrobial-resistant bacteria. After treatment the active compound is excreted through urine and faeces. As some antimicrobials are chemically stable, recirculation of subinhibitory concentrations of antimicrobials may occur due to coprophagic behaviour of animals such as chickens. Methods The persistence of three antimicrobials over time and their potential effects on antimicrobial resistance were determined in four groups of broilers. Groups were left untreated (control) or were treated with amoxicillin (unstable), doxycycline or enrofloxacin (stable). Antimicrobials were extracted from the faecal samples and were measured by LC-MS/MS. We determined the resistome genotypically using shotgun metagenomics and phenotypically by using Escherichia coli as indicator microorganism. Results Up to 37 days after treatment, doxycycline and enrofloxacin had concentrations in faeces equal to or higher than the minimal selective concentration (MSC), in contrast to the amoxicillin treatment. The amoxicillin treatment showed a significant difference (P  ≤ 0.01 and P  ≤ 0.0001) in the genotypic resistance only directly after treatment. On the other hand, the doxycycline treatment showed approximately 52% increase in phenotypic resistance and a significant difference (P  ≤ 0.05 and P  ≤ 0.0001) in genotypic resistance throughout the trial. Furthermore, enrofloxacin treatment resulted in a complete non-WT E. coli population but the quantity of resistance genes was similar to the control group, likely because resistance is mediated by point mutations. Conclusions Based on our findings, we suggest that persistence of antimicrobials should be taken into consideration in the assessment of priority classification of antimicrobials in livestock. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Structural color in the bacterial domain: The ecogenomics of a 2-dimensional optical phenotype.

Author

Zomer, Aldert, Ingham, Colin J., von Meijenfeldt, F. A. Bastiaan, Doncel, Álvaro Escobar, van de Kerkhof, Gea T., Hamidjaja, Raditijo, Schouten, Sanne, Schertel, Lukas, Müller, Karin H., Catón, Laura, Hahnke, Richard L., Bolhuis, Henk, Vignolini, Silvia, and Dutilh, Bas E.

Subjects
*STRUCTURAL colors, *BACTERIAL genomes, *NANOSTRUCTURED materials, *MULTICELLULAR organisms, *SEAWATER
Abstract

Structural color is an optical phenomenon resulting from light interacting with nanostructured materials. Although structural color (SC) is widespread in the tree of life, the underlying genetics and genomics are not well understood. Here, we collected and sequenced a set of 87 structurally colored bacterial isolates and 30 related strains lacking SC. Optical analysis of colonies indicated that diverse bacteria from at least two different phyla (Bacteroidetes and Proteobacteria) can create two-dimensional packing of cells capable of producing SC. A pan-genome-wide association approach was used to identify genes associated with SC. The biosynthesis of uroporphyrin and pterins, as well as carbohydrate utilization and metabolism, was found to be involved. Using this information, we constructed a classifier to predict SC directly from bacterial genome sequences and validated it by cultivating and scoring 100 strains that were not part of the training set. We predicted that SCr is widely distributed within gram-negative bacteria. Analysis of over 13,000 assembled metagenomes suggested that SC is nearly absent from most habitats associated with multicellular organisms except macroalgae and is abundant in marine waters and surface/air interfaces. This work provides a large-scale ecogenomics view of SC in bacteria and identifies microbial pathways and evolutionary relationships that underlie this optical phenomenon. [ABSTRACT FROM AUTHOR]

Published
2024
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14. Antimicrobial Resistance in Salmonella enterica Serovar Paratyphi B Variant Java in Poultry from Europe and Latin America

Author

Castellanos, L. Ricardo, Bloois, Linda van der Graaf-van, Donado-Godoy, Pilar, Veldman, Kees, Duarte, Francisco, Acuna, Maria T., Jarquin, Claudia, Weill, Francois-Xavier, Mevius, Dik J., Wagenaar, Jaap A., Hordijk, Joost, and Zomer, Aldert L.

Subjects
Genomics, Drug resistance in microorganisms, Genomes, Poultry industry, Phylogeny, Salmonella, Health
Abstract

The d-Tartrate fermenting, nonparatyphoidal variant of Salmonella enterica serovar Paratyphi B, contemporarily known as variant Java, was first reported in 1935 by De Moor (1). From then until recently, Salmonella [...]

Published
2020
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15. Integrative and Conjugative Elements and Prophage DNA as Carriers of Resistance Genes in Erysipelothrix rhusiopathiae Strains from Domestic Geese in Poland.

Author

Dec, Marta, Zomer, Aldert, Webster, John, Nowak, Tomasz, Stępień-Pyśniak, Dagmara, and Urban-Chmiel, Renata

Subjects
*TRANSPOSONS, *WHOLE genome sequencing, *GEESE, *GENES, *DNA, *TRACE elements
Abstract

Goose erysipelas is a serious problem in waterfowl breeding in Poland. However, knowledge of the characteristics of Erysipelothrix rhusiopathiae strains causing this disease is limited. In this study, the antimicrobial susceptibility and serotypes of four E. rhusiopathiae strains from domestic geese were determined, and their whole-genome sequences (WGSs) were analyzed to detect resistance genes, integrative and conjugative elements (ICEs), and prophage DNA. Sequence type and the presence of resistance genes and transposons were compared with 363 publicly available E. rhusiopathiae strains, as well as 13 strains of other Erysipelothrix species. Four strains tested represented serotypes 2 and 5 and the MLST groups ST 4, 32, 242, and 243. Their assembled circular genomes ranged from 1.8 to 1.9 kb with a GC content of 36–37%; a small plasmid was detected in strain 1023. Strains 1023 and 267 were multidrug-resistant. The resistance genes detected in the genome of strain 1023 were erm47, tetM, and lsaE-lnuB-ant(6)-Ia-spw cluster, while strain 267 contained the tetM and ermB genes. Mutations in the gyrA gene were detected in both strains. The tetM gene was embedded in a Tn916-like transposon, which in strain 1023, together with the other resistance genes, was located on a large integrative and conjugative-like element of 130 kb designated as ICEEr1023. A minor integrative element of 74 kb was identified in strain 1012 (ICEEr1012). This work contributes to knowledge about the characteristics of E. rhusiopathiae bacteria and, for the first time, reveals the occurrence of erm47 and ermB resistance genes in strains of this species. Phage infection appears to be responsible for the introduction of the ermB gene into the genome of strain 267, while ICEs most likely play a key role in the spread of the other resistance genes identified in E. rhusiopathiae. [ABSTRACT FROM AUTHOR]

Published
2024
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17. Genomic analysis of European bovine Staphylococcus aureus from clinical versus subclinical mastitis

Author

Hoekstra, Jurriaan, Zomer, Aldert L., Rutten, Victor P. M. G., Benedictus, Lindert, Stegeman, Arjan, Spaninks, Mirlin P., Bennedsgaard, Torben W., Biggs, Andrew, De Vliegher, Sarne, Mateo, Demetrio Herrera, Huber-Schlenstedt, Reglindis, Katholm, Jørgen, Kovács, Péter, Krömker, Volker, Lequeux, Guillaume, Moroni, Paolo, Pinho, Luís, Smulski, Sebastian, Supré, Karlien, Swinkels, Jantijn M., Holmes, Mark A., Lam, Theo J. G. M., and Koop, Gerrit

Published
2020
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18. Characterising the gut microbiome of stranded harbour seals (Phoca vitulina) in rehabilitation.

Author

Rubio-Garcia, Ana, Zomer, Aldert L., Guo, Ruoshui, Rossen, John W. A., van Zeijl, Jan H., Wagenaar, Jaap A., and Luiken, Roosmarijn E. C.

Subjects
*HARBOR seal, *GUT microbiome, *REHABILITATION centers, *REHABILITATION, *HUMAN ecology
Abstract

Animal rehabilitation centres provide a unique opportunity to study the microbiome of wild animals because subjects will be handled for their treatment and can therefore be sampled longitudinally. However, rehabilitation may have unintended consequences on the animals' microbiome because of a less varied and suboptimal diet, possible medical treatment and exposure to a different environment and human handlers. Our study describes the gut microbiome of two large seal cohorts, 50 pups (0–30 days old at arrival) and 23 weaners (more than 60 days old at arrival) of stranded harbour seals admitted for rehabilitation at the Sealcentre Pieterburen in the Netherlands, and the effect of rehabilitation on it. Faecal samples were collected from all seals at arrival, two times during rehabilitation and before release. Only seals that did not receive antimicrobial treatment were included in the study. The average time in rehabilitation was 95 days for the pups and 63 days for the weaners. We observed that during rehabilitation, there was an increase in the relative abundance of some of the Campylobacterota spp and Actinobacteriota spp. The alpha diversity of the pups' microbiome increased significantly during their rehabilitation (p-value <0.05), while there were no significant changes in alpha diversity over time for weaners. We hypothesize that aging is the main reason for the observed changes in the pups' microbiome. At release, the sex of a seal pup was significantly associated with the microbiome's alpha (i.e., Shannon diversity was higher for male pups, p-value <0.001) and beta diversity (p-value 0.001). For weaners, variation in the microbiome composition (beta diversity) at release was partly explained by sex and age of the seal (p-values 0.002 and 0.003 respectively). We mainly observed variables known to change the gut microbiome composition (e.g., age and sex) and conclude that rehabilitation in itself had only minor effects on the gut microbiome of seal pups and seal weaners. [ABSTRACT FROM AUTHOR]

Published
2023
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19. Development of Kaptive databases for Vibrio parahaemolyticus O- and K-antigen genotyping

Author

van der Graaf-van Bloois, Linda, Chen, Hongyou, Wagenaar, Jaap A, Zomer, Aldert L, Klinische infectiologie en microb. lab., and Klinische infectiologie en microb. lab.

Subjects
Genotype, Epidemiology, O Antigens/genetics, K-locus, General Medicine, Serogroup, serotyping, Microbiology, genotyping, whole-genome sequencing, Genetics, Humans, O-locus, Vibrio parahaemolyticus, Serotyping, Molecular Biology
Abstract

Vibrio parahaemolyticus is an important food-borne human pathogen and presents immunogenic surface polysaccharides, which can be used to distinguish problematic and disease-causing lineages. V. parahaemolyticus is divided in 16 O-serotypes (O-antigen) and 71 K-serotypes (K-antigen). Agglutination tests are still the gold standard for serotyping, but many V. parahaemolyticus isolates are not typable by agglutination. An alternative for agglutination tests is genotyping using whole-genome sequencing data, by which K- and O- genotypes have been curated and identified previously for other clinically relevant organisms with the software tool Kaptive. In this study, V. parahaemolyticus isolates were serotyped and sequenced, and all known and several novel O- and K-loci were identified. We developed Kaptive databases for all O- and K-loci after manual curation of the loci. In our study, we could genotype the O- and K-loci of 98 and 93 % of the genomes, respectively, with a Kaptive confidence score higher than ‘none’. The newly developed Kaptive databases with the identified V. parahaemolyticus O- and K-loci can be used to identify the O- and K-genotypes of V. parahaemolyticus isolates from genome sequences.

Published
2023

20. Zoonotic Endocarditis in a Man, the Netherlands

Author

Sleutjens, Janneke, Meijer, Dennie, Meregalli, Paola G., Bakker, Leendert, Wagenaar, Jaap A., Duim, Birgitta, and Zomer, Aldert

Subjects
Endocarditis -- Case studies -- Diagnosis -- Care and treatment, Zoonoses -- Case studies -- Diagnosis -- Care and treatment, Heart valve diseases, DNA sequencing, Genomics, Spectroscopy, Penicillins, Prostheses and implants, Blood tests, Ionization, Infection, C-reactive protein, Genomes, Health
Abstract

On July 23, 2017, a 62-year-old man sought care at the emergency department of Tergooi Hospital (Hilversum, the Netherlands) for general malaise and fever up to 40.6[degrees]C (105.1[degrees]F). Nine months [...]

Published
2019
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21. Safety Evaluation of an Intranasally Applied Cocktail of Lactococcus lactis Strains in Pigs.

Author

Rattigan, Ruth, Wajda, Lukasz, Vlasblom, Abel A., Wolfe, Alan, Zomer, Aldert L., Duim, Birgitta, Wagenaar, Jaap A., and Lawlor, Peadar G.

Subjects
LACTOCOCCUS lactis, SWINE, INTRANASAL administration, LUNGS, PIGLETS, GENE expression, COCKTAILS
Abstract

Simple Summary: In this study, the safety of an intranasally applied cocktail of Lactococcus lactis was evaluated in new-born pigs. Prior to farrowing, twelve sows were assigned to either a placebo or cocktail group. Immediately after farrowing, either the placebo or cocktail was applied to both nostrils of all piglets in the corresponding group. Piglet health and growth were monitored at regular intervals, and on three occasions piglets were necropsied and samples were collected from the respiratory tract to identify any changes caused by the treatment. The results show that the cocktail did not negatively impact piglet growth or health, nor did it cause histological changes in the nasal conchae, tonsils or lung tissues; but it did alter the gene expression of pBD2, TLR9 and IL-1β in the nasal conchae. These findings indicate the cocktail is safe for administration to pigs. Three Lactococcus lactis strains from the nasal microbiota of healthy pigs were identified as candidates for reducing MRSA in pigs. The safety of nasal administration of a cocktail of these strains was examined in new-born piglets. Six days pre-farrowing, twelve sows were assigned to the placebo or cocktail group (n = 6/group). After farrowing, piglets were administered with either 0.5 mL of the placebo or the cocktail to each nostril. Health status and body weight were monitored at regular time points. Two piglets from three sows/treatment group were euthanised at 24 h, 96 h and 14 d after birth, and conchae, lung and tonsil samples were collected for histopathological and gene expression analysis. Health scores were improved in the cocktail group between d1–5. Body weight and daily gains did not differ between groups. Both groups displayed histological indications of euthanasia and inflammation in the lungs, signifying the findings were not treatment related. The expression of pBD2, TLR9 and IL-1β in the nasal conchae differed between groups, indicating the cocktail has the potential to modulate immune responses. In summary, the L. lactis cocktail was well tolerated by piglets and there was no negative impact on health scores, growth or lung histopathology indicating that it is safe for administration to new-born piglets. [ABSTRACT FROM AUTHOR]

Published
2023
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22. Advancing microbiome research with machine learning: key findings from the ML4Microbiome COST action.

Author

D'Elia, Domenica, Truu, Jaak, Lahti, Leo, Berland, Magali, Papoutsoglou, Georgios, Ceci, Michelangelo, Zomer, Aldert, Lopes, Marta B., Ibrahimi, Eliana, Gruca, Aleksandra, Nechyporenko, Alina, Frohme, Marcus, Klammsteiner, Thomas, Carrillo-de Santa Pau, Enrique, Marcos-Zambrano, Laura Judith, Hron, Karel, Pio, Gianvito, Simeon, Andrea, Suharoschi, Ramona, and Moreno-Indias, Isabel

Subjects
MACHINE learning, HUMAN microbiota, RESEARCH personnel, INDIVIDUALIZED medicine, NANOMEDICINE, ARTIFICIAL intelligence, COST
Abstract

The rapid development of machine learning (ML) techniques has opened up the data-dense field of microbiome research for novel therapeutic, diagnostic, and prognostic applications targeting a wide range of disorders, which could substantially improve healthcare practices in the era of precision medicine. However, several challenges must be addressed to exploit the benefits of ML in this field fully. In particular, there is a need to establish "gold standard" protocols for conducting ML analysis experiments and improve interactions between microbiome researchers and ML experts. The Machine Learning Techniques in Human Microbiome Studies (ML4Microbiome) COST Action CA18131 is a European network established in 2019 to promote collaboration between discovery-oriented microbiome researchers and data-driven ML experts to optimize and standardize ML approaches for microbiome analysis. This perspective paper presents the key achievements of ML4Microbiome, which include identifying predictive and discriminatory 'omics' features, improving repeatability and comparability, developing automation procedures, and defining priority areas for the novel development of ML methods targeting the microbiome. The insights gained from ML4Microbiome will help to maximize the potential of ML in microbiome research and pave the way for new and improved healthcare practices. [ABSTRACT FROM AUTHOR]

Published
2023
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23. Antimicrobial resistance in Campylobacter fetus : Emergence and genomic evolution

Author

van der Graaf-van Bloois, Linda, Duim, Birgitta, Looft, Torey, Veldman, Kees T, Zomer, Aldert L, Wagenaar, Jaap A, Klinische infectiologie en microb. lab., and Klinische infectiologie en microb. lab.

Subjects
Host Pathogen Interaction & Diagnostics, whole genome sequencing, Campylobacter fetus, ECOFF, plasmid, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Bacteriologie, Bacteriology, General Medicine, Bacteriology, Host Pathogen Interaction & Diagnostics, antimicrobial resistance, Host Pathogen Interactie & Diagnostiek
Abstract

Campylobacter fetus is a pathogen, which is primarily associated with fertility problems in sheep and cattle. In humans, it can cause severe infections that require antimicrobial treatment. However, knowledge on the development of antimicrobial resistance in C. fetus is limited. Moreover, the lack of epidemiological cut-off values (ECOFFs) and clinical breakpoints for C. fetus hinders consistent reporting about wild-type and non-wild-type susceptibility. The aim of this study was to determine the phenotypic susceptibility pattern of C. fetus and to determine the C. fetus resistome [the collection of all antimicrobial resistance genes (ARGs) and their precursors] to describe the genomic basis of antimicrobial resistance in C. fetus isolates over time. Whole-genome sequences of 295 C . fetus isolates, including isolates that were isolated in the period 1939 till the mid 1940s, before the usage of non-synthetic antimicrobials, were analysed for the presence of resistance markers, and phenotypic antimicrobial susceptibility was obtained for a selection of 47 isolates. C. fetus subspecies fetus (Cff) isolates showed multiple phenotypic antimicrobial resistances compared to C. fetus subspecies venerealis (Cfv) isolates that were only intrinsic resistant to nalidixic acid and trimethoprim. Cff isolates showed elevated minimal inhibitory concentrations for cefotaxime and cefquinome that were observed in isolates from 1943 onwards, and Cff isolates contained gyrA substitutions, which conferred resistance to ciprofloxacin. Resistances to aminoglycosides, tetracycline and phenicols were linked to acquired ARGs on mobile genetic elements. A plasmid-derived tet(O) gene in a bovine Cff isolate in 1999 was the first mobile genetic element observed, followed by detection of mobile elements containing tet(O)-aph(3′)-III and tet(44)-ant(6)-Ib genes, and a plasmid from a single human isolate in 2003, carrying aph(3′)-III-ant(6)-Ib and a chloramphenicol resistance gene (cat). The presence of ARGs in multiple mobile elements distributed among different Cff lineages highlights the risk for spread and further emergence of AMR in C. fetus . Surveillance for these resistances requires the establishment of ECOFFs for C. fetus .

Published
2023

24. Genomics and pathotypes of the many faces of Escherichia coli

Author

Geurtsen, Jeroen, de Been, Mark, Weerdenburg, Eveline, Zomer, Aldert, McNally, Alan, Poolman, Jan, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
Infectious Diseases, Escherichia coli pathotypes, population dynamics, virulence factors, bacterial species, Microbiology, accessory genome, antibiotic resistance
Abstract

Escherichia coli is the most researched microbial organism in the world. Its varied impact on human health, consisting of commensalism, gastrointestinal disease, or extraintestinal pathologies, has generated a separation of the species into at least eleven pathotypes (also known as pathovars). These are broadly split into two groups, intestinal pathogenic E. coli (InPEC) and extraintestinal pathogenic E. coli (ExPEC). However, components of E. coli's infinite open accessory genome are horizontally transferred with substantial frequency, creating pathogenic hybrid strains that defy a clear pathotype designation. Here, we take a birds-eye view of the E. coli species, characterizing it from historical, clinical, and genetic perspectives. We examine the wide spectrum of human disease caused by E. coli, the genome content of the bacterium, and its propensity to acquire, exchange, and maintain antibiotic resistance genes and virulence traits. Our portrayal of the species also discusses elements that have shaped its overall population structure and summarizes the current state of vaccine development targeted at the most frequent E. coli pathovars. In our conclusions, we advocate streamlining efforts for clinical reporting of ExPEC, and emphasize the pathogenic potential that exists throughout the entire species.

Published
2022

25. Comparative Analysis of L-Fucose Utilization and Its Impact on Growth and Survival of Isolates

Author

Middendorf, Pjotr S, Jacobs-Reitsma, Wilma F, Zomer, Aldert L, den Besten, Heidy M W, and Abee, Tjakko

Subjects
Campylobacter jejuni, L-fucose consumption, Campylobacter coli, HPLC, animal and human origin, metabolism, fitness
Abstract

Campylobacter jejuni and Campylobacter coli were previously considered asaccharolytic, but are now known to possess specific saccharide metabolization pathways, including L-fucose. To investigate the influence of the L-fucose utilization cluster on Campylobacter growth, survival and metabolism, we performed comparative genotyping and phenotyping of the C. jejuni reference isolate NCTC11168 (human isolate), C. jejuni Ca1352 (chicken meat isolate), C. jejuni Ca2426 (sheep manure isolate), and C. coli Ca0121 (pig manure isolate), that all possess the L-fucose utilization cluster. All isolates showed enhanced survival and prolonged spiral cell morphology in aging cultures up to day seven in L-fucose-enriched MEMα medium (MEMαF) compared to MEMα. HPLC analysis indicated L-fucose utilization linked to acetate, lactate, pyruvate and succinate production, confirming the activation of the L-fucose pathway in these isolates and its impact on general metabolism. Highest consumption of L-fucose by C. coli Ca0121 is conceivably linked to its enhanced growth performance up to day 7, reaching 9.3 log CFU/ml compared to approximately 8.3 log CFU/ml for the C. jejuni isolates. Genetic analysis of the respective L-fucose clusters revealed several differences, including a 1 bp deletion in the Cj0489 gene of C. jejuni NCTC11168, causing a frameshift in this isolate resulting in two separate genes, Cj0489 and Cj0490, while no apparent phenotype could be linked to the presumed frameshift in this isolate. Additionally, we found that the L-fucose cluster of C. coli Ca0121 was most distant from C. jejuni NCTC11168, but confirmation of links to L-fucose metabolism associated phenotypic traits in C. coli versus C. jejuni isolates requires further studies.

Published
2022

28. Functional genome analysis of Bifidobacterium breve UCC2003 reveals type IVb tight adherence (Tad) pili as an essential and conserved host-colonization factor

Author

Motherway, Mary O'Connell, Zomer, Aldert, Leahy, Sinead C., Reunaner, Justus, Bottacini, Francesca, Claesson, Marcus J., O'Brien, Frances, Flynn, Kiera, Casey, Patrick G., Munoz, Jose Antonio Moreno, Kearney, Breda, Houston, Aileen M., O'Mahony, Caitlin, Higgins, Des G., Shanahan, Fergus, Palva, Airi, de Vos, Willem M., Fitzgerald, Gerald F., Ventura, Marco, O'Toole, Paul W., and van Sinderen, Douwe

Published
2011

29. Genomic Investigation of Two Acinetobacter baumannii Outbreaks in a Veterinary Intensive Care Unit in The Netherlands

Author

Naing, Soe Yu, Hordijk, Joost, Duim, Birgitta, Broens, Els, van der Graaf - van Bloois, Linda, Rossen, John W A, Robben, Joris, Leendertse, Masja, Wagenaar, Jaap, Zomer, Aldert, Klinische infectiologie en microb. lab., dI&I I&I-4, Intensieve zorgafdeling, dCSCA AVR, CS_Welfare & emerging diseases, and Microbes in Health and Disease (MHD)

Subjects
Acinetobacter baumannii, Microbiology (medical), whole-genome sequencing, antimicrobial resistance, veterinary medicine, Whole-genome sequencing, Infectious Diseases, General Immunology and Microbiology, Veterinary medicine, Immunology and Microbiology(all), Immunology and Allergy, Antimicrobial resistance, Molecular Biology
Abstract

Acinetobacter baumannii is a nosocomial pathogen that frequently causes healthcare-acquired infections. The global spread of multidrug-resistant (MDR) strains with its ability to survive in the environment for extended periods imposes a pressing public health threat. Two MDR A. baumannii outbreaks occurred in 2012 and 2014 in a companion animal intensive care unit (caICU) in the Netherlands. Whole-genome sequencing (WGS) was performed on dog clinical isolates (n = 6), environmental isolates (n = 5), and human reference strains (n = 3) to investigate if the isolates of the two outbreaks were related. All clinical isolates shared identical resistance phenotypes displaying multidrug resistance. Multi-locus Sequence Typing (MLST) revealed that all clinical isolates belonged to sequence type ST2. The core genome MLST (cgMLST) results confirmed that the isolates of the two outbreaks were not related. Comparative genome analysis showed that the outbreak isolates contained different gene contents, including mobile genetic elements associated with antimicrobial resistance genes (ARGs). The time-measured phylogenetic reconstruction revealed that the outbreak isolates diverged approximately 30 years before 2014. Our study shows the importance of WGS analyses combined with molecular clock investigations to reduce transmission of MDR A. baumannii infections in companion animal clinics.

Published
2022

30. Within-Household Transmission and Bacterial Diversity of Staphylococcus pseudintermedius

Author

Wegener, Alice, Duim, Birgitta, van der Graaf-van Bloois, Linda, Zomer, Aldert L, Visser, Caroline E, Spaninks, Mirlin, Timmerman, Arjen J, Wagenaar, Jaap A, Broens, Els M, Klinische infectiologie en microb. lab., FAH veterinaire epidemiologie, Klinische infectiologie en microb. lab., FAH veterinaire epidemiologie, and Medical Microbiology and Infection Prevention

Subjects
Microbiology (medical), Host Pathogen Interaction & Diagnostics, whole genome sequencing, General Immunology and Microbiology, Bacteriologie, bacterial diversity, transmission, Bacteriology, Bacteriology, Host Pathogen Interaction & Diagnostics, Host Pathogen Interactie & Diagnostiek, S. pseudintermedius, Infectious Diseases, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Immunology and Allergy, zoonotic, Molecular Biology, One health
Abstract

Staphylococcus pseudintermedius can be transmitted between dogs and their owners and can cause opportunistic infections in humans. Whole genome sequencing was applied to identify the relatedness between isolates from human infections and isolates from dogs in the same households. Genome SNP diversity and distribution of plasmids and antimicrobial resistance genes identified related and unrelated isolates in both households. Our study shows that within-host bacterial diversity is present in S. pseudintermedius, demonstrating that multiple isolates from each host should preferably be sequenced to study transmission dynamics.

Published
2022

31. Comparative Analysis of L-Fucose Utilization and Its Impact on Growth and Survival of Campylobacter Isolates

Author

Middendorf, Pjotr S, Jacobs-Reitsma, Wilma F, Zomer, Aldert L, den Besten, Heidy M W, Abee, Tjakko, Klinische infectiologie en microb. lab., dI&I I&I-4, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
Microbiology (medical), Campylobacter, Virulence, Campylobacter coli, Biology, biology.organism_classification, medicine.disease_cause, Cell morphology, Campylobacter jejuni, Genetic analysis, Microbiology, Levensmiddelenmicrobiologie, fitness, L-fucose consumption, medicine, Food Microbiology, HPLC, Genotyping, Gene, animal and human origin, metabolism, VLAG
Abstract

Campylobacter jejuni and Campylobacter coli were previously considered asaccharolytic, but are now known to possess specific saccharides metabolization pathways, including L-fucose. To investigate the influence of the L-fucose utilization cluster on Campylobacter growth, survival and metabolism, we performed comparative genotyping and phenotyping of the C. jejuni reference isolate NCTC11168 (human isolate), C. jejuni Ca1352 (chicken meat isolate), C. jejuni Ca2426 (sheep isolate), and C. coli Ca0121 (pig manure isolate), that all possess the L-fucose utilization cluster.All isolates showed enhanced survival and prolonged spiral cell morphology in aging cultures up to day seven in L-fucose-enriched MEMα medium (MEMαF) compared to MEMα. HPLC analysis indicated L-fucose utilization linked to acetate, lactate, pyruvate and succinate production, confirming the activation of the L-fucose pathway in these isolates. Highest consumption of L-fucose by C. coli Ca0121, is conceivably linked to its enhanced growth performance up to day 7, reaching 9.3 log CFU/ml compared to approximately 8.3 log CFU/ml for the C. jejuni isolates. Genetic analysis of their respective L-fucose clusters revealed several differences, including a 1 bp deletion in the Cj0489 gene of C. jejuni NCTC11168, causing a frameshift in this isolate resulting in two separate genes, Cj0489 and Cj0490, while no apparent phenotype could be linked to the presumed frameshift in the NCTC11168 isolate. Additionally, we found that the L-fucose cluster of C. coli Ca0121 was most distant from C. jejuni NCTC11168, but confirmation of links to L-fucose metabolism associated phenotypic traits in C. coli versus C. jejuni isolates requires further studies.ImportanceCampylobacter is the leading cause of gastroenteritis in humans worldwide, with increasing incidence and prevalence in recent years. The most prevalent species are Campylobacter jejuni and C. coli with 83% and 10% of all Campylobacter cases, respectively. Previously it was found that the majority of Campylobacter isolates are able to metabolize L-fucose (fuc+ isolates), a sugar that is widely present in the human gut. Putative roles for L-fucose in fuc+ C. jejuni isolates were found in growth, biofilm formation and virulence. Despite this, relatively little is known about L-fucose metabolism and the impact on growth and survival in fuc+ Campylobacter isolates. The results from our comparative genotyping and phenotyping study demonstrate that L-fucose, in both C. jejuni and C. coli fuc+ isolates, is involved in enhanced survival, prolonged spiral cell morphology and changes in the general metabolism. Possible links between phenotypes and differences in respective L-fucose gene clusters are discussed.

Published
2022

32. Genome analysis of Bifidobacterium bifidum PRL2010 reveals metabolic pathways for host-derived glycan foraging

Author

Turroni, Francesca, Bottacini, Francesca, Foroni, Elena, Mulder, Imke, Kim, Jae-Han, Zomer, Aldert, Sánchez, Borja, Bidossi, Alessandro, Ferrarini, Alberto, Giubellini, Vanessa, Delledonne, Massimo, Henrissat, Bernard, Coutinho, Pedro, Oggioni, Marco, Fitzgerald, Gerald F., Mills, David, Margolles, Abelardo, Kelly, Denise, van Sinderen, Douwe, Ventura, Marco, and Klaenhammer, Todd R.

Published
2010

33. RFPlasmid: predicting plasmid sequences from short-read assembly data using machine learning

Author

van der Graaf-van Bloois, Linda, Wagenaar, Jaap A, Zomer, Aldert L, Klinische infectiologie en microb. lab., dI&I I&I-4, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
antibiotic resistance, Computational biology, Biology, Genome, chemistry.chemical_compound, Plasmid, plasmid, Methods, Escherichia coli, chromosome, Gene, Genomic Methodologies, Host Pathogen Interaction & Diagnostics, Whole genome sequencing, Whole Genome Sequencing, Contig, Bacteriologie, Chromosome, Bacteriology, General Medicine, Bacteriology, Host Pathogen Interaction & Diagnostics, Host Pathogen Interactie & Diagnostiek, machine learning, chemistry, Metagenomics, whole-genome sequencing, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Genome, Bacterial, DNA, Plasmids
Abstract

Antimicrobial-resistance (AMR) genes in bacteria are often carried on plasmids and these plasmids can transfer AMR genes between bacteria. For molecular epidemiology purposes and risk assessment, it is important to know whether the genes are located on highly transferable plasmids or in the more stable chromosomes. However, draft whole-genome sequences are fragmented, making it difficult to discriminate plasmid and chromosomal contigs. Current methods that predict plasmid sequences from draft genome sequences rely on single features, like k-mer composition, circularity of the DNA molecule, copy number or sequence identity to plasmid replication genes, all of which have their drawbacks, especially when faced with large single-copy plasmids, which often carry resistance genes. With our newly developed prediction tool RFPlasmid, we use a combination of multiple features, including k-mer composition and databases with plasmid and chromosomal marker proteins, to predict whether the likely source of a contig is plasmid or chromosomal. The tool RFPlasmid supports models for 17 different bacterial taxa, including Campylobacter , Escherichia coli and Salmonella , and has a taxon agnostic model for metagenomic assemblies or unsupported organisms. RFPlasmid is available both as a standalone tool and via a web interface.

Published
2021

34. Biomolecule sulphation and novel methylations related to guillain-barré syndrome-associated campylobacter jejuni serotype hs:19

Author

Heikema, Astrid P, Strepis, Nikolaos, Horst-Kreft, Deborah, Huynh, Steven, Zomer, Aldert, Kelly, David J, Cooper, Kerry K, Parker, Craig T, Klinische infectiologie en microb. lab., dI&I I&I-4, Klinische infectiologie en microb. lab., dI&I I&I-4, and Medical Microbiology & Infectious Diseases

Subjects
Whole genome sequencing, Serotype, Whole-genome sequencing, biology, Guillain-Barre syndrome, Epidemiology, General Medicine, Methylation, Serotype HS:19, biology.organism_classification, medicine.disease, Guillain-Barré syndrome, Sulphation, bacterial infections and mycoses, Campylobacter jejuni, Microbiology, Sulfation, 19 [Serotype HS], medicine, Genetics, Molecular Biology
Abstract

Campylobacter jejuni strains that produce sialylated lipooligosaccharides (LOS) can cause the immune-mediated disease Guillain-Barré syndrome (GBS). The risk of GBS after infection with C. jejuni Penner serotype HS:19 is estimated to be at least six times higher than the average risk. Aside from LOS biosynthesis genes, genomic characteristics that promote an increased risk for GBS following C. jejuni HS:19 infection, remain uncharacterized. We hypothesized that strains with the HS:19 serotype have unique genomic features that explain the increased risk for GBS. We performed genome sequencing, alignments, single nucleotide polymorphisms' analysis and methylome characterization on a subset, and pan-genome analysis on a large number of genomes to compare HS:19 with non-HS:19 C. jejuni genome sequences. Comparison of 36 C. jejuni HS:19 with 874 C. jejuni non-HS:19 genome sequences led to the identification of three single genes and ten clusters containing contiguous genes that were significantly associated with C. jejuni HS:19. One gene cluster of seven genes, localized downstream of the capsular biosynthesis locus, was related to sulphation of biomolecules. This cluster also encoded the campylobacter sialyl transferase Cst-I. Interestingly, sulphated bacterial biomolecules such as polysaccharides can promote immune responses and, therefore, (in the presence of sialic acid) may play a role in the development of GBS. Additional gene clusters included those involved in persistence-mediated pathogenicity and gene clusters involved in restriction-modification systems. Furthermore, characterization of methylomes of two HS:19 strains exhibited novel methylation patterns (5′-CATG-3 and 5′-m6AGTNNNNNNRTTG-3) that could differentially effect gene-expression patterns of C. jejuni HS:19 strains. Our study provides novel insight into specific genetic features and possible virulence factors of C. jejuni associated with the HS:19 serotype that may explain the increased risk of GBS.

Published
2021

35. Complete genome sequence of a clinical campylobacter isolate identical to a novel campylobacter species

Author

Duim, Birgitta, van der Graaf-van Bloois, Linda, Timmerman, Arjen, Wagenaar, Jaap A, Flipse, Jacky, Wallinga, Janny, Bloembergen, Peter, Miller, William G, Zomer, Aldert L, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
Epidemiology, Bioinformatica & Diermodellen, Biology, medicine.disease_cause, Microbiology, 03 medical and health sciences, Immunology and Microbiology (miscellaneous), Bio-informatics & Animal models, medicine, Genetics, Life Science, Epidemiology, Bio-informatics & Animal models, Molecular Biology, 030304 developmental biology, Sequence (medicine), Whole genome sequencing, Host Pathogen Interaction & Diagnostics, Epidemiologie, 0303 health sciences, 030306 microbiology, Strain (biology), Campylobacter, Genome Sequences, Bacteriologie, Bacteriology, Bacteriology, Host Pathogen Interaction & Diagnostics, Sequence identity, Host Pathogen Interactie & Diagnostiek, Metagenomics, Epidemiologie, Bioinformatica & Diermodellen, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Candidatus, Campylobacter species
Abstract

Here, we present the complete genome sequence of a Campylobacter strain isolated in the Netherlands from a patient with gastroenteritis. The strain showed >98% sequence identity to the novel Campylobacter species sequence recently recovered from metagenomic data, isolated from breastfed infants with diarrheal disease, and named “Candidatus Campylobacter infans.”

Published
2021

36. Global Distribution of O Serotypes and Antibiotic Resistance in Extraintestinal Pathogenic Escherichia coli Collected From the Blood of Patients With Bacteremia Across Multiple Surveillance Studies.

Author

Weerdenburg, Eveline, Davies, Todd, Morrow, Brian, Zomer, Aldert L, Hermans, Peter, Go, Oscar, Spiessens, Bart, van den Hoven, Thijs, Geet, Gunter van, Aitabi, Moussa, DebRoy, Chitrita, Dudley, Edward G, Bonten, Marc, Poolman, Jan, and Geurtsen, Jeroen

Subjects
ESCHERICHIA coli, BACTEREMIA, RETROSPECTIVE studies, SEROTYPES, RISK assessment, MULTIDRUG resistance, INTESTINAL parasites, DESCRIPTIVE statistics, DISEASE risk factors, DISEASE complications
Abstract

Background Extraintestinal pathogenic Escherichia coli (ExPEC) is the leading cause of bacteremia worldwide, with older populations having increased risk of invasive bacterial disease. Increasing resistance to first-line antibiotics and emergence of multidrug-resistant (MDR) strains represent major treatment challenges. ExPEC O serotypes are key targets for potential multivalent conjugate vaccine development. Therefore, we evaluated the O serotype distribution and antibiotic resistance profiles of ExPEC strains causing bloodstream infections across 4 regions. Methods Blood culture isolates from patients aged ≥60 years collected during 5 retrospective E. coli surveillance studies in Europe, North America, Asia-Pacific, and South America (2011–2017) were analyzed. Isolates were O serotyped by agglutination; O genotyping was performed for nontypeable isolates. Antimicrobial susceptibility testing was also conducted. Results Among 3217 ExPEC blood culture isolates, the most ubiquitous O serotype was O25 (n = 737 [22.9%]), followed by O2, O6, O1, O75, O15, O8, O16, O4, O18, O77 group, O153, O9, O101/O162, O86, and O13 (prevalence of ≥1%). The prevalence of these O serotypes was generally consistent across regions, apart from South America; together, these 16 O serotypes represented 77.6% of all ExPEC bacteremia isolates analyzed. The overall MDR frequency was 10.7%, with limited variation between regions. Within the MDR subset (n = 345), O25 showed a dominant prevalence of 63.2% (n = 218). Conclusions Predominant O serotypes among ExPEC bacteremia isolates are widespread across different regions. O25 was the most prevalent O serotype overall and particularly dominant among MDR isolates. These findings may inform the design of multivalent conjugate vaccines that can target the predominant O serotypes associated with invasive ExPEC disease in older adults. [ABSTRACT FROM AUTHOR]

Published
2023
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37. Absence of host-specific genes in canine and human staphylococcus pseudintermedius as inferred from comparative genomics

Author

Wegener, Alice, Broens, Els M, van der Graaf-van Bloois, Linda, Zomer, Aldert L, Visser, Caroline E, van Zeijl, Jan, van der Meer, Coby, Kusters, Johannes G, Friedrich, Alex W, Kampinga, Greetje A, Sips, Gregorius J, Smeets, Leonard, van Kerckhoven, Manfred E J, Timmerman, Arjen J, Wagenaar, Jaap A, Duim, Birgitta, dI&I I&I-4, Klinische infectiologie en microb. lab., Medical Microbiology and Infection Prevention, dI&I I&I-4, Klinische infectiologie en microb. lab., Microbes in Health and Disease (MHD), and Medical Microbiology & Infectious Diseases

Subjects
Staphylococcus pseudintermedius, Epidemiology, Genome-wide association study, Antimicrobial resistance, Biochemistry, EMERGENCE, Pharmacology, Toxicology and Pharmaceutics(all), Plasmid, pseudintermedius, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Pathogen, Genetics, 0303 health sciences, biology, Bacteriologie, Bacteriology, Host Pathogen Interaction & Diagnostics, INSIGHTS, S. pseudintermedius, Infectious Diseases, INFECTIONS, INTERMEDIUS GROUP, Microbiology (medical), Bioinformatica & Diermodellen, RM1-950, Microbiology, Article, Host association, 03 medical and health sciences, Antibiotic resistance, SDG 3 - Good Health and Well-being, Bio-informatics & Animal models, Epidemiology, Bio-informatics & Animal models, Gene, 030304 developmental biology, Pharmacology, Host Pathogen Interaction & Diagnostics, Epidemiologie, Comparative genomics, 030306 microbiology, Bacteriology, biology.organism_classification, Host Pathogen Interactie & Diagnostiek, Multiple drug resistance, Toxicology and Pharmaceutics(all), Epidemiologie, Bioinformatica & Diermodellen, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Therapeutics. Pharmacology
Abstract

Staphylococcus pseudintermedius is an important pathogen in dogs that occasionally causes infections in humans as an opportunistic pathogen of elderly and immunocompromised people. This study compared the genomic relatedness and antimicrobial resistance genes using genome-wide association study (GWAS) to examine host association of canine and human S. pseudintermedius isolates. Canine (n = 25) and human (n = 32) methicillin-susceptible S. pseudintermedius (MSSP) isolates showed a high level of genetic diversity with an overrepresentation of clonal complex CC241 in human isolates. This clonal complex was associated with carriage of a plasmid containing a bacteriocin with cytotoxic properties, a CRISPR-cas domain and a pRE25-like mobile element containing five antimicrobial resistance genes. Multi-drug resistance (MDR) was predicted in 13 (41%) of human isolates and 14 (56%) of canine isolates. CC241 represented 54% of predicted MDR isolates from humans and 21% of predicted MDR canine isolates. While it had previously been suggested that certain host-specific genes were present the current GWAS analysis did not identify any genes that were significantly associated with human or canine isolates. In conclusion, this is the first genomic study showing that MSSP is genetically diverse in both hosts and that multidrug resistance is important in dog and human-associated S. pseudintermedius isolates.

Published
2021

38. The Equine Faecal Microbiota of Healthy Horses and Ponies in The Netherlands: Impact of Host and Environmental Factors

Author

Theelen, Mathijs J P, Luiken, Roosmarijn E C, Wagenaar, Jaap A, Sloet van Oldruitenborgh-Oosterbaan, Marianne M, Rossen, John W A, Zomer, Aldert L, Equine Internal Medicine, dES AVR, dI&I I&I-4, Klinische infectiologie en microb. lab., dIRAS RA-I&I I&I, CS_Welfare & emerging diseases, Equine Internal Medicine, dES AVR, dI&I I&I-4, Klinische infectiologie en microb. lab., dIRAS RA-I&I I&I, CS_Welfare & emerging diseases, and Microbes in Health and Disease (MHD)

Subjects
0301 basic medicine, Veterinary medicine, Future studies, 040301 veterinary sciences, Firmicutes, Location, Pony, Pasture, Article, 0403 veterinary science, 03 medical and health sciences, fluids and secretions, Age, biology.animal, pony, SF600-1100, microbiota, gender, equine, geography, geography.geographical_feature_category, General Veterinary, biology, Host (biology), Equine, Microbiota, faecal, Illumina miseq, Horse, Bacteroidetes, Gender, 04 agricultural and veterinary sciences, biology.organism_classification, veterinary(all), Diet, pasture, 030104 developmental biology, QL1-991, age, Animal Science and Zoology, Season, diet, Zoology, season, Faecal, location
Abstract

Simple Summary Several studies have described the bacterial composition in the intestines of horses, and several factors of influence have been detected. Variation in the results between studies, however, is substantial. Therefore, the current study aimed to study the bacterial composition in the faeces of healthy horses and ponies kept under standard housing and management condition in The Netherlands. Seventy-nine horses and ponies originating from two farms were included. Several factors, such as location, age, the season of sampling, horse type (horses vs. ponies) and pasture access significantly affected the bacterial composition. The current study provides important baseline information on variation in the bacterial composition in healthy horses and ponies under standard housing and management conditions. The aforementioned factors identified in this study to affect the bacterial population of the gut should be considered in future studies regarding the bacterial population of the equine gut. Abstract Several studies have described the faecal microbiota of horses and the factors that influence its composition, but the variation in results is substantial. This study aimed to investigate the microbiota composition in healthy equids in The Netherlands under standard housing and management conditions and to evaluate the effect of age, gender, horse type, diet, pasture access, the season of sampling and location on it. Spontaneously produced faecal samples were collected from the stall floor of 79 healthy horses and ponies at two farms. The validity of this sampling technique was evaluated in a small pilot study including five ponies showing that the microbiota composition of faecal samples collected up to 6 h after spontaneous defaecation was similar to that of the samples collected rectally. After DNA extraction, Illumina Miseq 16S rRNA sequencing was performed to determine microbiota composition. The effect of host and environmental factors on microbiota composition were determined using several techniques (NMDS, PERMANOVA, DESeq2). Bacteroidetes was the largest phylum found in the faecal microbiota (50.1%), followed by Firmicutes (28.4%). Alpha-diversity and richness decreased significantly with increasing age. Location, age, season, horse type and pasture access had a significant effect on beta-diversity. The current study provides important baseline information on variation in faecal microbiota in healthy horses and ponies under standard housing and management conditions. These results indicate that faecal microbiota composition is affected by several horse-related and environment-related factors, and these factors should be considered in future studies of the equine faecal microbiota.

Published
2021

40. Sources and transmission routes of campylobacteriosis : A combined analysis of genome and exposure data

Author

Mughini-Gras, Lapo, Pijnacker, Roan, Coipan, Claudia, Mulder, Annemieke C., Veludo, Adriana Fernandes, de Rijk, Sharona, van Hoek, Angela H.A.M., Buij, Ralph, Muskens, Gerard, Koene, Miriam, Veldman, Kees, Duim, Birgitta, Graaf-van Bloois, Linda van der, van der Weijden, Coen, Kuiling, Sjoerd, Verbruggen, Anjo, van der Giessen, Joke, Opsteegh, Marieke, van der Voort, Menno, Castelijn, Greetje A.A., Schets, Franciska M., Blaak, Hetty, Wagenaar, Jaap A., Zomer, Aldert L., Franz, Eelco, IRAS OH Epidemiology Microbial Agents, dIRAS RA-I&I I&I, LS IRAS EEPI GRA (Gezh.risico-analyse), Dep Infectieziekten Immunologie, Klinische infectiologie en microb. lab., dI&I I&I-4, LS IRAS VPH VV (veterinaire volksgezh.), Dep IRAS, IRAS OH Epidemiology Microbial Agents, dIRAS RA-I&I I&I, LS IRAS EEPI GRA (Gezh.risico-analyse), Dep Infectieziekten Immunologie, Klinische infectiologie en microb. lab., dI&I I&I-4, LS IRAS VPH VV (veterinaire volksgezh.), and Dep IRAS

Subjects
0301 basic medicine, Veterinary medicine, Swine, Epidemiology, Moleculaire Biologie & AMR, medicine.disease_cause, Molecular Biology & AMR, Poultry, Zoonosis, 0302 clinical medicine, Campylobacter Infections, 030212 general & internal medicine, Netherlands, Core-genome MLST, Source attribution, Campylobacter, Infectious Diseases, Dierecologie, Female, Livestock, Animal Ecology, Microbiology (medical), Bioinformatica & Diermodellen, 030106 microbiology, Campylobacteriosis, Biology, Campylobacter jejuni, 03 medical and health sciences, Dogs, Team Bacteriology, Bio-informatics & Animal models, medicine, Animals, Team Bacteriologie, Epidemiology, Bio-informatics & Animal models, Raw meat, Feces, Epidemiologie, Team Bacteriologie, Moleculaire Biologie & AMR, Sheep, Team Bacteriology, Molecular Biology & AMR, business.industry, biology.organism_classification, medicine.disease, Risk factors, Epidemiologie, Bioinformatica & Diermodellen, Cats, Multilocus sequence typing, Cattle, business, Chickens, Multilocus Sequence Typing
Abstract

Summary Objectives To determine the contributions of several animal and environmental sources of human campylobacteriosis and identify source-specific risk factors. Methods 1417 Campylobacter jejuni/coli isolates from the Netherlands in 2017–2019 were whole-genome sequenced, including isolates from human cases (n = 280), chickens/turkeys (n = 238), laying hens (n = 56), cattle (n = 158), veal calves (n = 49), sheep/goats (n = 111), pigs (n = 110), dogs/cats (n = 100), wild birds (n = 62), and surface water (n = 253). Questionnaire-based exposure data was collected. Source attribution was performed using core-genome multilocus sequence typing. Risk factors were determined on the attribution estimates. Results Cases were mostly attributed to chickens/turkeys (48.2%), dogs/cats (18.0%), cattle (12.1%), and surface water (8.5%). Of the associations identified, never consuming chicken, as well as frequent chicken consumption, and rarely washing hands after touching raw meat, were risk factors for chicken/turkey-attributable infections. Consuming unpasteurized milk or barbecued beef increased the risk for cattle-attributable infections. Risk factors for infections attributable to environmental sources were open water swimming, contact with dog faeces, and consuming non-chicken/turkey avian meat like game birds. Conclusions Poultry and cattle are the main livestock sources of campylobacteriosis, while pets and surface water are important non-livestock sources. Foodborne transmission is only partially consistent with the attributions, as frequency and alternative pathways of exposure are significant.

Published
2021

41. Differential analysis of longitudinal methicillin-resistant staphylococcus aureus colonization in relation to microbial shifts in the nasal microbiome of neonatal piglets

Author

Patel, Shriram, Vlasblom, Abel A, Verstappen, Koen M, Zomer, Aldert L, Fluit, Ad C, Rogers, Malbert R C, Wagenaar, Jaap A, Claesson, Marcus J, Duim, Birgitta, Klinische infectiologie en microb. lab., dI&I I&I-4, LS Klinisch Onderzoek Wagenaar, Klinische infectiologie en microb. lab., dI&I I&I-4, and LS Klinisch Onderzoek Wagenaar

Subjects
Colonization, Identification, Epidemiology, Physiology, Assay, Human pathogen, MRSA, medicine.disease_cause, Biochemistry, 2. Zero hunger, 0303 health sciences, Ecology, Transmission (medicine), Bacteriologie, Bacteriology, Host Pathogen Interaction & Diagnostics, QR1-502, Computer Science Applications, PCR, Staphylococcus aureus, Modeling and Simulation, Research Article, Porcine nasal microbiome, Evolution, Bioinformatica & Diermodellen, Firmicutes, Biology, Microbiology, 03 medical and health sciences, Behavior and Systematics, Modelling and Simulation, Bio-informatics & Animal models, medicine, Genetics, Epidemiology, Bio-informatics & Animal models, Microbiome, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Host Pathogen Interaction & Diagnostics, Epidemiologie, 030306 microbiology, Microbial shifts, Bacteriology, biochemical phenomena, metabolism, and nutrition, 16S ribosomal RNA, biology.organism_classification, bacterial infections and mycoses, Methicillin-resistant Staphylococcus aureus, Host Pathogen Interactie & Diagnostiek, Bacterial interference, Epidemiologie, Bioinformatica & Diermodellen, Bacteriologie, Host Pathogen Interactie & Diagnostiek
Abstract

Methicillin-resistant Staphylococcus aureus (MRSA) is an important human pathogen and often colonizes pigs. To lower the risk of MRSA transmission to humans, a reduction of MRSA prevalence and/or load in pig farms is needed. The nasal microbiome contains commensal species that may protect against MRSA colonization and may be used to develop competitive exclusion strategies. To obtain a comprehensive understanding of the species that compete with MRSA in the developing porcine nasal microbiome, and the moment of MRSA colonization, we analyzed nasal swabs from piglets in two litters. The swabs were taken longitudinally, starting directly after birth until 6 weeks. Both 16S rRNA and tuf gene sequencing data with different phylogenetic resolutions and complementary culture-based and quantitative real-time PCR (qPCR)-based MRSA quantification data were collected. We employed a compositionally aware bioinformatics approach (CoDaSeq + rmcorr) for analysis of longitudinal measurements of the nasal microbiota. The richness and diversity in the developing nasal microbiota increased over time, albeit with a reduction of Firmicutes and Actinobacteria, and an increase of Proteobacteria. Coabundant groups (CAGs) of species showing strong positive and negative correlation with colonization of MRSA and S. aureus were identified. Combining 16S rRNA and tuf gene sequencing provided greater Staphylococcus species resolution, which is necessary to inform strategies with potential protective effects against MRSA colonization in pigs. IMPORTANCE The large reservoir of methicillin-resistant Staphylococcus aureus (MRSA) in pig farms imposes a significant zoonotic risk. An effective strategy to reduce MRSA colonization in pig farms is competitive exclusion whereby MRSA colonization can be reduced by the action of competing bacterial species. We complemented 16S rRNA gene sequencing with Staphylococcus-specific tuf gene sequencing to identify species anticorrelating with MRSA colonization. This approach allowed us to elucidate microbiome dynamics and identify species that are negatively and positively associated with MRSA, potentially suggesting a route for its competitive exclusion.

Published
2021

42. Identification of conditionally essential genes for Streptococcus suis infection in pigs

Author

Arenas, Jesús, Zomer, Aldert, Harders-Westerveen, Jose, Bootsma, Hester J, De Jonge, Marien I, Stockhofe-Zurwieden, Norbert, Smith, Hilde E, De Greeff, Astrid, Klinische infectiologie en microb. lab., dI&I I&I-4, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
Microbiology (medical), transposon mutagenesis, Streptococcus suis, Immunology, Mutant, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Tn-Seq, Virulence, Infectious and parasitic diseases, RC109-216, Microbiology, Genome, Sepsis, 03 medical and health sciences, Immune system, medicine, Gene, 030304 developmental biology, Host Pathogen Interaction & Diagnostics, 0303 health sciences, biology, 030306 microbiology, pathogenesis, Bacteriologie, Wild type, streptococcus suis, zoonotic pathogen, Bacteriology, Bacteriology, Host Pathogen Interaction & Diagnostics, medicine.disease, biology.organism_classification, Host Pathogen Interactie & Diagnostiek, infection, Infectious Diseases, Bacteriologie, Host Pathogen Interactie & Diagnostiek, tn-seq, Parasitology
Abstract

Streptococcus suis is a Gram-positive bacterium and zoonotic pathogen that causes meningitis and sepsis in pigs and humans. The aim of this study was to identify genes required for S. suis infection. We created Tn-Seq libraries in a virulent S. suis strain 10, which was used to inoculate pigs in an intrathecal experimental infection. Comparative analysis of the relative abundance of mutants recovered from different sites of infection (blood, cerebrospinal fluid, and meninges of the brain) identified 361 conditionally essential genes, i.e. required for infection, which is about 18% of the genome. The conditionally essential genes were primarily involved in metabolic and transport processes, regulation, ribosomal structure and biogenesis, transcription, and cell wall membrane and envelope biogenesis, stress defenses, and immune evasion. Directed mutants were created in a set of 10 genes of different genetic ontologies and their role was determined in ex vivo models. Mutants showed different levels of sensitivity to survival in whole blood, serum, cerebrospinal fluid, thermic shock, and stress conditions, as compared to the wild type. Additionally, the role of three selected mutants was validated in co-infection experiments in which pigs were infected with both wild type and isogenic mutant strains. The genetic determinants of infection identified in this work contribute to novel insights in S. suis pathogenesis and could serve as targets for novel vaccines or antimicrobial drugs.

Published
2020

43. An interactive regulatory network controls stress response in Bifidobacterium breve UCC2003

Author

Zomer, Aldert, Fernandez, Matilde, Kearney, Breda, Fitzgerald, Gerald F., Ventura, Marco, and van Sinderen, Douwe

Subjects
Bifidobacterium -- Health aspects, Bifidobacterium -- Research, Gastrointestinal system -- Physiological aspects, Gastrointestinal system -- Research, Biological sciences
Abstract

Members of the genus Bifidobacterium are gram-positive bacteria that commonly are found in the gastrointestinal tract (GIT) of mammals, including humans. Because of their perceived probiotic properties, they frequently are incorporated as functional ingredients in food products. From probiotic production to storage and GIT delivery, bifidobacteria encounter a plethora of stresses. To cope with these environmental challenges, they need to protect themselves through stress-induced adaptive responses. We have determined the response of B. breve UCC2003 to various stresses (heat, osmotic, and solvent) using transcriptome analysis, DNA-protein interactions, and GusA reporter fusions, and we combined these with results from an in silico analysis. The integration of these results allowed the formulation of a model for an interacting regulatory network for stress response in B. breve UCC2003 where HspR controls the SOS response and the CIgR regulon, which in turn regulates and is regulated by HrcA. This model of an interacting regulatory network is believed to represent the paradigm for stress adaptation in bifidobacteria. doi: 10.1128/JB.00897-09

Published
2009

44. A Case of Persistent Diarrhea in a Man with the Molecular Detection of Various Campylobacter species and the First Isolation of candidatus Campylobacter infans

Author

Flipse, Jacky, Duim, Birgitta, Wallinga, Janny A., de Wijkerslooth, Laetitia R. H., Graaf-van Bloois, Linda van der, Timmerman, Arjen J., Zomer, Aldert L., Veldman, Kees T., Wagenaar, Jaap A., Bloembergen, Peter, Klinische infectiologie en microb. lab., dI&I I&I-4, Klinische infectiologie en microb. lab., and dI&I I&I-4

Subjects
Microbiology (medical), Tetracycline, Epidemiology, Bioinformatica & Diermodellen, lcsh:Medicine, Campylobacter spp, Case Report, medicine.disease_cause, Azithromycin, Microbiology, Bio-informatics & Animal models, non-jejuni/coli infection, medicine, Immunology and Allergy, Epidemiology, Bio-informatics & Animal models, Molecular Biology, culture versus PCR, Epidemiologie, General Immunology and Microbiology, business.industry, Lymphogranuloma venereum, Campylobacter, lcsh:R, 16S ribosomal RNA, medicine.disease, Lymphoma, Ciprofloxacin, Infectious Diseases, Epidemiologie, Bioinformatica & Diermodellen, Candidatus, business, medicine.drug
Abstract

A man with a well-controlled HIV infection, previously diagnosed with lymphogranuloma venereum and treated for Hodgkin’s lymphoma, was suffering from chronic diarrhea. He travelled to Indonesia in the month prior to the start of complaints. Over a 15-month period, sequences related to Campylobactertroglodytis/upsaliensis, C. pinnepediorum/mucosalis/concisus and C. hominis were detected by 16S rRNA qPCR-based assays in various stool samples and in a colon biopsy. Culture revealed the first isolation of “candidatus Campylobacter infans”, a species identified recently by molecular methods only. The patient was treated with azithromycin, ciprofloxacin and tetracycline. To identify potential continuous exposure of the patient to Campylobacter, stool samples of the partner and the cat of the patient were analyzed and C. pinnepediorum/mucosalis/concisus and C. helveticus, respectively, were detected. The diversity in detected species in this immunocompromised patient with a lack of repeatedly consistent findings resulted in the conclusion that not any of the Campylobacter species was the primary cause of the clinical condition. This study shows the challenges in detection and interpretation of diagnostic results regarding Campylobacter.

Published
2020

45. After the bite: bacterial transmission from grey seals ( Halichoerus grypus ) to harbour porpoises ( Phocoena phocoena )

Author

Gilbert, Maarten J., IJsseldijk, Lonneke L., Rubio-García, Ana, Gröne, Andrea, Duim, Birgitta, Rossen, John, Zomer, Aldert L., Wagenaar, Jaap A., dI&I I&I-4, VPDC pathologie, dPB CR, VP pathologie, dPB I&I, Klinische infectiologie en microb. lab., dI&I I&I-4, VPDC pathologie, dPB CR, VP pathologie, dPB I&I, Klinische infectiologie en microb. lab., and Microbes in Health and Disease (MHD)

Subjects
Epidemiology, Bioinformatica & Diermodellen, Zoology, microbiome, Phocoena, Oral cavity, bacterial transmission, Phoca, Seal (mechanical), 03 medical and health sciences, MARINE MAMMALS, FEVER, biology.animal, Bio-informatics & Animal models, INFECTION, Epidemiology, Bio-informatics & Animal models, harbour porpoise, North sea, lcsh:Science, CLINICAL SPECIMENS, 030304 developmental biology, computer.programming_language, Epidemiologie, 0303 health sciences, Multidisciplinary, STREPTOCOCCUS-PHOCAE, biology, 030306 microbiology, Transmission (medicine), Genetics and Genomics, biology.organism_classification, common seal, SP NOV, Epidemiologie, Bioinformatica & Diermodellen, Harbour, lcsh:Q, computer, Porpoise, Research Article, grey seal
Abstract

Recent population growth of the harbour porpoise ( Phocoena phocoena ), grey seal ( Halichoerus grypus ) and common seal ( Phoca vitulina ) in the North Sea has increased potential interaction between these species. Grey seals are known to attack harbour porpoises. Some harbour porpoises survive initially, but succumb eventually, often showing severely infected skin lesions. Bacteria transferred from the grey seal oral cavity may be involved in these infections and eventual death of the animal. In humans, seal bites are known to cause severe infections. In this study, a 16S rRNA-based microbiome sequencing approach is used to identify the oral bacterial diversity in harbour porpoises, grey seals and common seals; detect the potential transfer of bacteria from grey seals to harbour porpoises by biting and provide insights in the bacteria with zoonotic potential present in the seal oral cavity. β-diversity analysis showed that 12.9% (4/31) of the harbour porpoise skin lesion microbiomes resembled seal oral microbiomes, while most of the other skin lesion microbiomes also showed seal-associated bacterial species, including potential pathogens. In conclusion, this study shows that bacterial transmission from grey seals to harbour porpoises by biting is highly likely and that seal oral cavities harbour many bacterial pathogens with zoonotic potential.

Published
2020

46. Incompatibility and phylogenetic relationship of I-complex plasmids

Author

Rozwandowicz, Marta, Hordijk, Joost, Bossers, Alex, Zomer, Aldert, Wagenaar, Jaap A, Mevius, Dik J, Brouwer, Michael S M, dI&I I&I-4, Klinische infectiologie en microb. lab., dI&I I&I-4, and Klinische infectiologie en microb. lab.

Subjects
DNA Replication, Cell division, Epidemiology, Bioinformatica & Diermodellen, Population, Biology, medicine.disease_cause, Plasmid, Genomic Instability, Bacterial cell structure, 03 medical and health sciences, IncZ, Drug Resistance, Bacterial, Bio-informatics & Animal models, Escherichia coli, medicine, Epidemiology, Bio-informatics & Animal models, Dislodgement, education, Molecular Biology, Phylogeny, 030304 developmental biology, Genetics, Host Pathogen Interaction & Diagnostics, Epidemiologie, 0303 health sciences, education.field_of_study, 030306 microbiology, Electroporation, Bacteriologie, Incompatibility IncB/O, Bacteriology, Genomics, Sequence Analysis, DNA, Bacteriology, Host Pathogen Interaction & Diagnostics, Phenotype, Host Pathogen Interactie & Diagnostiek, Mutagenesis, Conjugation, Genetic, Epidemiologie, Bioinformatica & Diermodellen, Bacteriologie, Host Pathogen Interactie & Diagnostiek, Transformation, Bacterial, Phylogenetic relationship, Plasmids
Abstract

Plasmid incompatibility is the inability of two plasmids to be stably maintained in one cell, resulting in loss of one of the plasmids in daughter cells. Dislodgement is a phenotypically distinct form of incompatibility, described as an imperfect reproduction, manifesting in rapid exclusion of a resident plasmid after superinfection. The relationship between plasmids of the phenotypic incompatibility groups IncB/O and IncZ is unclear. Their inability to co-exist was initially referred to as dislodgement while other research reached the conclusion that IncB/O and IncZ plasmids are incompatible. In this manuscript we re-evaluated the relationship between IncB/O and IncZ plasmids to settle these conflicting conclusions. We performed dislodgement testing of R16Δ (IncB/O) and pSFE-059 (IncZ) plasmids by electroporation in a bacterial cell and checked their stability. Stability tests of the obtained plasmid pair showed that the IncB/O plasmid was exclusively and almost completely lost from the heteroplasmid Escherichia coli population. Other IncB/O - IncZ pairs could not form a heteroplasmid population, using conjugation or electroporation. Our data supports the previous suggestion that IncB/O and IncZ plasmids may be considered phenotypically incompatible.

Published
2020

47. Complete genome sequence of the prototype lactic acid bacterium Lactococcus lactis subsp. cremoris MG1363

Author

Wegmann, Udo, O'Connell-Motherway, Mary, Zomer, Aldert, Buist, Girbe, Shearman, Claire, Canchaya, Carlos, Ventura, Marco, Goesmann, Alexander, Gasson, Michael J., Kuipers, Oscar P., van Sinderen, Douwe, and Kok, Jan

Subjects
Genomes -- Research, Lactococcus -- Genetic aspects, Lactococcus -- Research, Lactic acid -- Research, Streptococcus -- Genetic aspects, Streptococcus -- Research, Biological sciences
Abstract

Lactococcus lactis is of great importance for the nutrition of hundreds of millions of people worldwide. This paper describes the genome sequence of Lactococcus lactis subsp, cremoris MG1363, the lactococcal strain most intensively studied throughout the world. The 2,529,478-bp genome contains 81 pseudogenes and encodes 2,436 proteins. Of the 530 unique proteins, 47 belong to the COG (clusters of orthologous groups) functional category 'carbohydrate metabolism and transport,' by far the largest category of novel proteins in comparison with L. lactis subsp, lactis IL1403. Nearly one-fifth of the 71 insertion elements are concentrated in a specific 56.kb region. This integration hot-spot region carries genes that are typically associated with lactococcal plasmids and a repeat sequence specifically found on plasmids and in the 'lateral gene transfer hot spot' in the genome of Streptococcus thermophilus. Although the parent of L. lactis MG1363 was used to demonstrate lysogeny in Lactococcus, L. lactis MG1363 carries four remnant/satellite phages and two apparently complete prophages. The availability of the L. lactis MG1363 genome sequence will reinforce its status as the prototype among lactic acid bacteria through facilitation of further applied and fundamental research.

Published
2007

48. Time-resolved determination of the CcpA regulon of Lactococcus lactis subsp. cremoris MG1363

Author

Zomer, Aldert L., Buist, Girbe, Larsen, Rasmus, Kok, Jan, and Kuipers, Oscar P.

Subjects
Gene expression -- Research, Lactococcus -- Genetic aspects, Lactococcus -- Research, Protein-protein interactions -- Research, Biological sciences
Abstract

Carbon catabolite control protein A (CcpA) is the main regulator involved in carbon catabolite repression in gram-positive bacteria. Time series gene expression analyses of Lactococcus lactis MG1363 and L. lactis MG1363[DELTA]ccpA using DNA microarrays were used to define the CcpA regulon of L. lactis. Based on a comparison of the transcriptome data with putative CcpA binding motifs (cre sites) in promoter sequences in the genome of L. lactis, 82 direct targets of CcpA were predicted. The main differences in time-dependent expression of CcpA-regulated genes were differences between the exponential and transition growth phases. Large effects were observed for carbon and nitrogen metabolic genes in the exponential growth phase. Effects on nucleotide metabolism genes were observed primarily in the transition phase. Analysis of the positions of putative cre sites revealed that there is a link between either repression or activation and the location of the cre site within the promoter region. Activation was observed when putative cre sites were located upstream of the hexameric -35 sequence at an average position of -56.5 or further upstream with decrements of 10.5 bp. Repression was observed when the cre site was located in or downstream of putative -35 and -10 sequences. The highest level of repression was observed when the cre site was present at a defined side of the DNA helix relative to the canonical -10 sequence. Gel retardation experiments, Northern blotting, and enzyme assays showed that CcpA represses its own expression and activates the expression of the divergently oriented prolidase-encoding pepQ gene, which constitutes a link between regulation of carbon metabolism and regulation of nitrogen metabolism.

Published
2007

49. Whole-genome sequencing of dog-specific assemblages C and D of Giardia duodenalis from single and pooled cysts indicates host-associated genes

Author

Kooyman, Frans N J, Wagenaar, Jaap A, Zomer, Aldert, LS Klinisch Onderzoek Wagenaar, dI&I I&I-4, LS Klinisch Onderzoek Wagenaar, and dI&I I&I-4

Subjects
Epidemiology, Bioinformatica & Diermodellen, parasitology, medicine.disease_cause, Genome, DNA sequencing, diplomonad, Bio-informatics & Animal models, parasitic diseases, medicine, Giardia lamblia, heterozygosity, Epidemiology, Bio-informatics & Animal models, cathepsin, Gene, Epidemiologie, Whole genome sequencing, Genetics, biology, synteny, Multiple displacement amplification, Giardia, General Medicine, multiple displacement amplification, biology.organism_classification, Diplomonad, Epidemiologie, Bioinformatica & Diermodellen
Abstract

Giardia duodenalis (syn. Giardia intestinalis or Giardia lamblia) infSAects over 280 million people each year and numerous animals. G. duodenalis can be subdivided into eight assemblages with different host specificity. Unculturable assemblages have so far resisted genome sequencing efforts. In this study, we isolated single and pooled cysts of assemblages C and D from dog faeces by FACS, and sequenced them using multiple displacement amplification and Illumina paired-end sequencing. The genomes of assemblages C and D were compared with genomes of assemblages A and B from humans and assemblage E from ruminants and pigs. The genomes obtained from the pooled cysts and from the single cysts were considered complete (>99 % marker genes observed) and the allelic sequence heterozygosity (ASH) values of assemblages C and D were 0.89 and 0.74 %, respectively. These ASH values were slightly higher than for assemblage B (>0.43 %) and much higher than for assemblages A and E, which ranged from 0.002 to 0.037 %. The flavohaemoglobin and 4Fe-4S binding domain family encoding genes involved in O2 and NO detoxification were only present in assemblages A, B and E. Cathepsin B orthologs were found in all genomes. Six clades of cathepsin B orthologs contained one gene of each genome, while in three clades not all assemblages were represented. We conclude that whole-genome sequencing from a single Giardia cyst results in complete draft genomes, making the genomes of unculturable Giardia assemblages accessible. Observed differences between the genomes of assemblages C and D on one hand and the assemblages A, B and E on the other hand are possibly associated with host specificity.

Published
2019

50. Short-Term Hypoxia Dampens Inflammation in vivo via Enhanced Adenosine Release and Adenosine 2B Receptor Stimulation

Author

Kiers, Dorien, Wielockx, Ben, Peters, Esther, van Eijk, Lucas T, Gerretsen, Jelle, John, Aaron, Janssen, Emmy, Groeneveld, Rianne, Peters, Mara, Damen, Lars, Meneses, Ana M, Krüger, Anja, Langereis, Jeroen D, Zomer, Aldert L, Blackburn, Michael R, Joosten, Leo A, Netea, Mihai G, Riksen, Niels P, van der Hoeven, Johannes G, Scheffer, Gert-Jan, Eltzschig, Holger K, Pickkers, Peter, Kox, Matthijs, LS Klinisch Onderzoek Wagenaar, dI&I I&I-4, LS Klinisch Onderzoek Wagenaar, and dI&I I&I-4

Subjects
0301 basic medicine, Adenosine, medicine.medical_treatment, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], lcsh:Medicine, Inflammation, Pharmacology, Systemic inflammation, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, All institutes and research themes of the Radboud University Medical Center, Endotoxin, medicine, Animals, Humans, Hypoxia, Adenosine 2B receptor, lcsh:R5-920, business.industry, lcsh:R, Receptors, Purinergic P1, Interleukin, Vascular damage Radboud Institute for Molecular Life Sciences [Radboudumc 16], General Medicine, Hypoxia (medical), Purinergic signalling, Hypoxia-Inducible Factor 1, alpha Subunit, Endotoxemia, 3. Good health, Interleukin-10, Up-Regulation, Interleukin 10, Disease Models, Animal, 030104 developmental biology, Cytokine, Reconstructive and regenerative medicine Radboud Institute for Molecular Life Sciences [Radboudumc 10], Cytokines, medicine.symptom, business, lcsh:Medicine (General), 030217 neurology & neurosurgery, medicine.drug, Research Paper
Abstract

Hypoxia and inflammation are closely intertwined phenomena. Critically ill patients often suffer from systemic inflammatory conditions and concurrently experience short-lived hypoxia. We evaluated the effects of short-term hypoxia on systemic inflammation, and show that it potently attenuates pro-inflammatory cytokine responses during murine endotoxemia. These effects are independent of hypoxia-inducible factors (HIFs), but involve augmented adenosine levels, in turn resulting in an adenosine 2B receptor-mediated post-transcriptional increase of interleukin (IL)-10 production. We translated our findings to humans using the experimental endotoxemia model, where short-term hypoxia resulted in enhanced plasma concentrations of adenosine, augmentation of endotoxin-induced circulating IL-10 levels, and concurrent attenuation of the pro-inflammatory cytokine response. Again, HIFs were shown not to be involved. Taken together, we demonstrate that short-term hypoxia dampens the systemic pro-inflammatory cytokine response through enhanced purinergic signaling in mice and men. These effects may contribute to outcome and provide leads for immunomodulatory treatment strategies for critically ill patients., Highlights • Short-term hypoxia attenuates the systemic pro-inflammatory cytokine response in vivo in both mice and men • The underlying mechanism involves adenosine 2B receptor-mediated enhanced production of anti-inflammatory interleukin-10 • These effects may contribute to outcome and provide leads for novel treatment strategies for critically ill patients Inflammation and short bouts of low oxygen levels are frequently encountered phenomena in severely ill patients admitted to the Intensive Care unit. This study investigated the effect of short-term low oxygen levels on the inflammatory response in both mice and humans. The results show that a short period of low levels of oxygen potently dampens inflammation, and identify the underlying mechanisms. These effects of low oxygen levels may contribute to the outcome of severely ill patients. Furthermore, the increased understanding of the underlying mechanisms provided by this study can be used to develop therapies to dampen inflammation in patients.

Published
2018

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