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Publication : C5a regulates NKT and NK cell functions in sepsis.

First Author  Fusakio ME Year  2011
Journal  J Immunol Volume  187
Issue  11 Pages  5805-12
PubMed ID  22058413 Mgi Jnum  J:179685
Mgi Id  MGI:5302894 Doi  10.4049/jimmunol.1100338
Citation  Fusakio ME, et al. (2011) C5a regulates NKT and NK cell functions in sepsis. J Immunol 187(11):5805-12
abstractText  Complement, NKT, and NK cells play critical roles in the first line defense against pathogens. Functional roles for both C5a receptors, that is, complement receptor C5a (C5aR) and C5a receptor-like 2 (C5L2), in sepsis have been demonstrated. However, the role of C5a in innate lymphocyte activation during sepsis remains elusive. In this article, we show that naive NKT and NK cells already express high levels of C5aR and minor levels of C5L2 mRNA, but no protein. Upon Escherichia coli-induced sepsis, we found C5aR surface expression on subpopulations of NKT and NK cells, suggesting rapid translation into C5aR protein on bacterial encounter. Importantly, significantly increased survival in the absence of C5aR, NKT, and NK cells, but not of C5L2, was associated with reduced IFN-gamma and TNF-alpha serum levels. Sepsis induction in C5aR(+)/C5aR(-) mixed bone marrow chimeras identified cognate engagement of C5aR on NKT cells as an important factor for the recruitment of NKT cells. Furthermore, we found synergistic interaction between C5aR and TLRs enhancing the production of TNF-alpha and IFN-gamma from NKT and NK cells in cocultures with dendritic cells. Our results identify C5aR activation as a novel pathway driving detrimental effects of NKT and NK cells during early experimental sepsis.
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