Anaphylatoxin C5a actions in rat liver: Synergistic enhancement by C5a of lipopolysaccharide-dependent alpha(2)-macroglobulin gene expression in hepatocytes via IL-6 release from Kupffer cells
C. Mack et al., Anaphylatoxin C5a actions in rat liver: Synergistic enhancement by C5a of lipopolysaccharide-dependent alpha(2)-macroglobulin gene expression in hepatocytes via IL-6 release from Kupffer cells, J IMMUNOL, 167(7), 2001, pp. 3972-3979
The effects of the anaphylatoxins C5a and C3a on the liver are only poorly
characterized in contrast to their well known systemic actions. Recently, i
t has been demonstrated that the anaphylatoxin C5a enhanced glucose output
from hepatocytes (HC) indirectly via prostanoid release from Kupffer cells
(KC). In the present study, it is shown that recombinant rat C5a (rrC5a), t
ogether with LPS, activated the gene of the acute phase protein alpha (2)-m
acroglobulin (alpha (2)MG) in HC also indirectly via IL-6 release from KC.
RrC5a alone increased neither IL-6 mRNA in nor IL-6 release from KC, wherea
s LPS alone did so. However, rrC5a synergistically enhanced the LPS-depende
nt increase in IL-6 mRNA and IL-6 release. Only rIL-6, but not TNF-alpha or
IL-1 beta, enhanced a2MG mRNA in HC. In line with the actions of rrC5a and
LPS on KC, conditioned medium of KC stimulated only with rrC5a did not inc
rease alpha (2)MG mRNA in HC. However, medium of KC stimulated with rrC5a p
lus LPS induced alpha (2)MG mRNA expression in HC more strongly than medium
from cells stimulated only with LPS; thus, C5a acted synergistically with
LPS. The stimulatory effects of KC-conditioned medium could partially be in
hibited by a neutralizing anti-IL-6 All, indicating that KC-derived IL-6 wa
s a major mediator in C5a- plus LPS-elicited alpha (2)MG gene expression. T
hese results suggest that C5a, besides enhancing glucose output via prostan
oids, is involved in the initiation of the acute phase response in HC via p
roinflammatory cytokines from KC. This provides evidence for another import
ant function of C5a in the regulation of hepatocellular defense reactions.