Pathogen Specific, IRF3-Dependent Signaling and Innate Resistance to Human Kidney Infection: e1001109

Pathogen Specific, IRF3-Dependent Signaling and Innate Resistance to Human Kidney Infection e1001109

The mucosal immune system identifies and fights invading pathogens, while allowing non-pathogenic organisms to persist. Mechanisms of pathogen/non-pathogen discrimination are poorly understood, as is the contribution of human genetic variation in disease susceptibility. We describe here a new, IRF3-...

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Bibliographic Details
Published in:PLoS pathogens Vol. 6; no. 9
Main Authors: Fischer, Hans, Lutay, Nataliya, Ragnarsdóttir, Bryndís, Yadav, Manisha, Jönsson, Klas, Urbano, Alexander, Hadad, Ahmed Al, Rämisch, Sebastian, Storm, Petter, Dobrindt, Ulrich, Salvador, Ellaine, Karpman, Diana, Jodal, Ulf, Svanborg, Catharina
Format: Journal Article
Language:English
Published: San Francisco Public Library of Science 01-09-2010
Subjects:
Bacterial infections
E coli
Experiments
Flora
Genetic diversity
Immune response
Immune system
Infections
Kidneys
Ligands
Medical research
Mortality
Pathogens
Phosphorylation
Risk assessment
Rodents
Signal transduction
Translocation
Urogenital system
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Summary:The mucosal immune system identifies and fights invading pathogens, while allowing non-pathogenic organisms to persist. Mechanisms of pathogen/non-pathogen discrimination are poorly understood, as is the contribution of human genetic variation in disease susceptibility. We describe here a new, IRF3-dependent signaling pathway that is critical for distinguishing pathogens from normal flora at the mucosal barrier. Following uropathogenic E. coli infection, Irf3-/- mice showed a pathogen-specific increase in acute mortality, bacterial burden, abscess formation and renal damage compared to wild type mice. TLR4 signaling was initiated after ceramide release from glycosphingolipid receptors, through TRAM, CREB, Fos and Jun phosphorylation and p38 MAPK-dependent mechanisms, resulting in nuclear translocation of IRF3 and activation of IRF3/IFNβ-dependent antibacterial effector mechanisms. This TLR4/IRF3 pathway of pathogen discrimination was activated by ceramide and by P-fimbriated E. coli, which use ceramide-anchored glycosphingolipid receptors. Relevance of this pathway for human disease was supported by polymorphic IRF3 promoter sequences, differing between children with severe, symptomatic kidney infection and children who were asymptomatic bacterial carriers. IRF3 promoter activity was reduced by the disease-associated genotype, consistent with the pathology in Irf3-/- mice. Host susceptibility to common infections like UTI may thus be strongly influenced by single gene modifications affecting the innate immune response.
ISSN:1553-7366
1553-7374
DOI:10.1371/journal.ppat.1001109