Abstract
Liver injury is characterized by hepatocyte apoptosis and collagen-producing activated hepatic stellate cells (HSC). Hepatocyte apoptosis promotes liver injury and fibrosis, whereas activated HSC apoptosis limits hepatic fibrosis. Pharmacological inhibition of liver cell apoptosis may potentially attenuate liver injury and fibrosis by blocking hepatocyte apoptosis or promote fibrosis by permitting accumulation of activated HSCs. To ascertain the net effect of inhibiting liver cell apoptosis on liver injury, inflammation, and hepatic fibrogenesis, we examined the effect of a pancaspase inhibition IDN-6556 on these parameters in the bile duct ligated (BDL) mouse. Hepatocyte apoptosis was assessed by the terminal deoxynucleotidyl transferase dUTP nick-end labeling assay and immunofluorescence for active caspases 3/7, and liver injury by histopathology and serum alanine aminotransferase (ALT) determinations. Real-time polymerase chain reaction was used to measure mRNA transcripts for markers of hepatic inflammation, HSC activation, and fibrosis. Immunohistochemistry for α-smooth muscle actin was performed to identify HSC activation. Collagen deposition was quantitated by Sirius red staining and digital imaging techniques. Hepatocyte apoptosis and liver injury (bile infarcts and serum ALT values) were reduced in IDN-6556-treated versus saline-treated 3-day BDL mice. Markers for liver inflammation [chemokine (C-X-C) ligand 1 and macrophage inflammatory protein-2 chemokine expression] and hepatic fibrogenesis (transforming growth factor-β and collagen I expression) were also attenuated. Consistent with these data, HSC activation as assessed by α-smooth muscle actin mRNA expression and immunohistochemistry was markedly reduced in both 3- and 10-day BDL animals. Collectively, these data suggest hepatocyte apoptosis initiates cascades culminating in liver injury and fibrosis. The pan-caspase inhibitor IDN-6556 is a promising agent for cholestatic liver injury.
Footnotes
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This work was supported by a fellowship grant from the Postdoctoral Program of the German Academic Exchange Service (to A.C.), National Institutes of health Grant DK 41876 (to G.J.G.), and the Mayo Foundation.
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DOI: 10.1124/jpet.103.060129.
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ABBREVIATIONS: HSC, hepatic stellate cell; BDL, bile duct ligation/ligated; TUNEL, terminal deoxynucleotidyl transferase dUTP nick-end labeling; ALT, alanine aminotransferase; TGF, transforming growth factor; PCR, polymerase chain reaction; KC, chemokine (C-X-C) ligand 1; MIP, macrophage inflammatory protein; α-SMA, alpha smooth muscle actin.
- Received September 16, 2003.
- Accepted November 10, 2003.
- The American Society for Pharmacology and Experimental Therapeutics
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