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Targeting Complement C5a Receptor 1 for the Treatment of Immunosuppression in Sepsis

Oliver Sommerfeld, Anna Medyukhina, Sophie Neugebauer, Mohamed Ghait, Svenja Ulferts, Amelie Lupp, Rainer König, Reinhard Wetzker, Stefan Schulz, Marc Thilo Figge, Michael Bauer, Adrian T. Press

2020Molecular Therapy48 citationsDOIOpen Access PDF

Abstract

Complement factor C5a was originally identified as a powerful promoter of inflammation through activation of the C5a receptor 1 (C5ar1). Recent evidence suggests involvement of C5a not only in pro- but also in anti-inflammatory signaling. The present study aims to unveil the role of C5ar1 as potential therapeutic target in a murine sepsis model. Our study discloses a significantly increased survival in models of mild to moderate but not severe sepsis of C5ar1-deficient mice. The decreased mortality of C5ar1-deficient mice is accompanied by improved pathogen clearance and largely preserved liver function. C5ar1-deficient mice exhibited a significantly increased production of the pro-inflammatory mediator interferon-γ (IFN-γ) and a decreased production of the anti-inflammatory cytokine interleukin-10 (IL-10). Together, these data uncover C5a signaling as a mediator of immunosuppressive processes during sepsis and describe the C5ar1 and related changes of the IFN-γ to IL-10 ratio as markers for the immunological (dys)function accompanying sepsis.

Topics & Concepts

C5a receptorSepsisImmunologyComplement systemMediatorInflammationBiologyCytokineComplement factor IImmunosuppressionProinflammatory cytokineReceptorImmune systemEndocrinologyBiochemistryComplement system in diseasesMechanical Circulatory Support DevicesInflammation biomarkers and pathways
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