Reduced Glycolysis and Cytotoxicity in Staphylococcus aureus Isolates from Chronic Rhinosinusitis as Strategies for Host Adaptation

GND
1137342919
ORCID
0000-0002-9328-5302
Zugehörigkeit
Institute of Medical Microbiology, Jena University Hospital
Tuchscherr, Lorena;
GND
1206553405
Zugehörigkeit
Institute of Medical Microbiology, Jena University Hospital
Wendler, Sindy;
GND
1120713781
Zugehörigkeit
Systems Biology and Bioinformatics Unit, Leibniz Institute for Natural Product Research and Infection Biology-Hans Knöll Institute, 07745 Jena
Santhanam, Rakesh;
GND
1316760030
Zugehörigkeit
Department of Otorhinolaryngology, Jena University Hospital
Priese, Juliane;
GND
1330842030
Zugehörigkeit
Leibniz Institute of Photonic Technology (IPHT), 07745 Jena
Reissig, Annett;
GND
1330843169
Zugehörigkeit
Leibniz Institute of Photonic Technology (IPHT), 07745 Jena
Müller, Elke;
GND
1299780431
Zugehörigkeit
Institute of Medical Microbiology, Jena University Hospital
Ali, Rida;
GND
12936231X
Zugehörigkeit
Institute of Immunology, University Hospital Jena
Müller, Sylvia;
GND
1182580505
Zugehörigkeit
Institute of Medical Microbiology, Jena University Hospital
Löffler, Bettina;
GND
1146226861
Zugehörigkeit
Leibniz Institute of Photonic Technology (IPHT), 07745 Jena
Monecke, Stefan;
GND
120759454
ORCID
0000-0002-6612-0043
Zugehörigkeit
Leibniz Institute of Photonic Technology (IPHT), 07745 Jena
Ehricht, Ralf;
GND
1078441464
ORCID
0000-0001-9671-0784
Zugehörigkeit
Department of Otorhinolaryngology, Jena University Hospital
Guntinas-Lichius, Orlando

Chronic rhinosinusitis (CRS) is a multifactorial infection of the nasal cavity and sinuses. In this study, nasal swabs from control donors (N = 128) and patients with CRS (N = 246) were analysed. Culture methods and metagenomics revealed no obvious differences in the composition of the bacterial communities between the two groups. However, at the functional level, several metabolic pathways were significantly enriched in the CRS group compared to the control group. Pathways such as carbohydrate transport metabolism, ATP synthesis, cofactors and vitamins, photosynthesis and transcription were highly enriched in CRS. In contrast, pathways related to lipid metabolism were more representative in the control microbiome. As S. aureus is one of the main species found in the nasal cavity, staphylococcal isolates from control and CRS samples were analysed by microarray and functional assays. Although no significant genetic differences were detected by microarray, S. aureus from CRS induced less cytotoxicity to lung cells and lower rates of glycolysis in host cells than control isolates. These results suggest the differential modulation of staphylococcal virulence by the environment created by other microorganisms and their interactions with host cells in control and CRS samples. These changes were reflected in the differential expression of cytokines and in the expression of Agr, the most important quorum-sensing regulator of virulence in S. aureus . In addition, the CRS isolates remained stable in their cytotoxicity, whereas the cytotoxic activity of S. aureus isolated from control subjects decreased over time during in vitro passage. These results suggest that host factors influence the virulence of S. aureus and promote its adaptation to the nasal environment during CRS.

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