The prognosis of liver failure is often determined by infectious and cholestatic complications. As HGF/c-Met and interleukin (IL)-6/gp130 control hepatic cytoprotective pathways, we here investigated their cooperative role during the onset of cholestatic liver injury. Conditional hepatocyte-specific (Δhepa) c-Met, gp130 and c-Met/gp130 knockout mice (Cre-loxP system) were subjected to bile duct ligation (BDL) and lipopolysaccharide (LPS) stimulation. gp130 Δhepa and c-Met/gp130 Δhepa mice displayed increased lethality associated with severe bacteraemia early after BDL, whereas c-Met Δhepa and wild-type mice showed normal survival. Analysis of the innate immune response and the regulation of hepatic antibacterial pathways showed that the LPS-triggered hepatocellular response via the Toll-like receptor-4 pathway was regulated differentially by HGF/c-Met and IL-6/gp130. Activation of p38MAPK, c-Jun N-terminal kinase and signalling transducer and activator of transcription-3 was impaired in gp130 Δ and c-Met Δhepa livers. In addition, the acute-phase response (APR) was reduced in c-Met Δhepa livers, whereas gp130 Δhepa displayed a completely abolished APR. In contrast, TNF-α-dependent NF-κB activation was enhanced in gp130 Δhepa and c-Met Δhepa mice and it was associated with a higher rate of apoptosis and inflammation. Moreover, expression of the neutrophil produced and secreted cathelin-related antimicrobial peptide and of genes related to the inflammasome complex correlated with the strength of the bacterial infection and with TNF-α expression. In conclusion, Gp130 and c-Met are involved in the hepatic antibacterial and innate immune response, control the APR and thus prevent sepsis and liver injury during cholestatic conditions. © 2012 USCAP, Inc All rights reserved.
CITATION STYLE
Giebeler, A., Brandenburg, L. O., Kaldenbach, M., Erschfeld, S., Wasmuth, H., Wruck, C., … Streetz, K. L. (2012). Lack of hepatic c-Met and gp130 expression is associated with an impaired antibacterial response and higher lethality after bile duct ligation. Laboratory Investigation, 92(12), 1726–1737. https://doi.org/10.1038/labinvest.2012.122
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