| Literature DB >> 33727664 |
Masataka Kawakita1, Taiki Oyama1, Ikuma Shirai1, Shuto Tanaka1, Kotaro Akaki1, Shinya Abe2, Takuma Asahi2,3, Guangwei Cui2, Fumie Itoh4, Masato Sasaki4, Nobuyuki Shibata4, Koichi Ikuta2, Tomomitsu Hatakeyama5, Kazuhiko Takahara6.
Abstract
Severe infection often causes a septic cytokine storm followed by immune exhaustion/paralysis. Not surprisingly, many pathogens are equipped with various anti-inflammatory mechanisms. Such mechanisms might be leveraged clinically to control septic cytokine storms. Here we show that N-glycan from pathogenic C. albicans ameliorates mouse sepsis through immunosuppressive cytokine IL-10. In a sepsis model using lipopolysaccharide (LPS), injection of the N-glycan upregulated serum IL-10, and suppressed pro-inflammatory IL-1β, TNF-α and IFN-γ. The N-glycan also improved the survival of mice challenged by LPS. Analyses of structurally defined N-glycans from several yeast strains revealed that the mannose core is key to the upregulation of IL-10. Knocking out the C-type lectin Dectin-2 abrogated the N-glycan-mediated IL-10 augmentation. Furthermore, C. albicans N-glycan ameliorated immune exhaustion/immune paralysis after acute inflammation. Our results suggest a strategy where the immunosuppressive mechanism of one pathogen can be applied to attenuate a severe inflammation/cytokine storm caused by another pathogen.Entities:
Year: 2021 PMID: 33727664 PMCID: PMC7966402 DOI: 10.1038/s42003-021-01870-3
Source DB: PubMed Journal: Commun Biol ISSN: 2399-3642