Endogenous IL-10 protects mice from death during septic peritonitis
Interleukin-10 -- immunology
Molecular Sequence Data
Peritonitis
Cytokines -- blood
Inbred C57BL
Sepsis -- immunology
Cecum -- surgery
Mice
Sepsis
Sepsis -- etiology
Animals
RNA, Messenger
Cecum
Sepsis -- mortality
DNA Primers
Base Sequence
Peritonitis -- mortality
Peritonitis -- immunology
Sciences bio-médicales et agricoles
Interleukin-10
3. Good health
Mice, Inbred C57BL
Messenger -- analysis
Peritonitis -- complications
RNA
Cytokines
Female
DOI:
10.4049/jimmunol.155.11.5397
Publication Date:
2022-12-31T12:18:14Z
AUTHORS (10)
ABSTRACT
Abstract
IL-10 production during endotoxic shock is part of a protective mechanism that involves IL-10-induced inhibition of TNF synthesis. We sought to determine the role of IL-10 in septic peritonitis induced by cecal ligation and puncture (CLP). CLP led to a rapid induction of IL-10 mRNA in various organs of C57BI/6 mice. In liver, IL-10 mRNA was detectable within 1 h following CLP, while in spleen and lungs, IL-10 mRNA was detected from 2 to 4 h and onward. IL-10 protein became detectable in plasma 2 h after CLP, reaching peak concentrations after 12 h (12.7 +/- 5.7 ng/ml). Pretreatment (-2 h) with anti-IL-10 mAb resulted in higher plasma TNF levels following CLP when compared with mice treated with control mAb. Plasma IL-1 activity and IFN-γ remained undetectable in virtually all mice. Anti-IL-10 enhanced mortality after CLP (p < 0.05 by log-rank test). Addition of anti-TNF mAb did not influence the increased mortality associated with anti-IL-10 treatment. Septic peritonitis is associated with sustained production of IL-10 in various organs, which serves to protect the host against lethality.
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