Amelioration of hepatic inflammation in a mouse model of NASH using a dithiocarbamate derivative

Purpose The process whereby liver inflammation develops in non-alcoholic steatohepatitis (NASH) is not fully understood. While modification of the inflammatory milieu is an attractive target to prevent the development of hepatocellular injury, most antiinflammatory agents have proven ineffective in...

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Bibliographic Details
Published in:Hepatology international 2013-06, Vol.7 (2), p.600-609
Main Authors: Schwartz, Jason J., Emerson, Lyska, Hillas, Elaine, Phan, Ann, Thiesset, Heather, Firpo, Matthew, Sorensen, Jeffrey, Kennedy, Thomas, Rinella, Mary
Format: Article
Language:English
Subjects:
Colorectal Surgery
Hepatology
Medicine
Medicine & Public Health
Original Article
Surgery
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Summary:Purpose The process whereby liver inflammation develops in non-alcoholic steatohepatitis (NASH) is not fully understood. While modification of the inflammatory milieu is an attractive target to prevent the development of hepatocellular injury, most antiinflammatory agents have proven ineffective in this setting. Tetraethylthiuram disulfide (TDSF) is able to induce S-glutathionylation of NF-κB along with critical signaling proteins involved with inflammation, especially when complexed with a heavy metal. For this reason, we hypothesized that administration of TDSF would function to ameliorate necroinflammatory activity in a mouse model of NASH. Methods Mice were divided into five groups and received control chow versus a methionine-choline-deficient diet. After 6 weeks of TDSF versus sham gavage, animals were necropsied. Using conventional H&E staining, livers were examined using the Brunt scoring system by a hepatopathologist blinded to treatment groups. Validated mouse primer sets were used for quantitative real-time PCR to evaluate changes in mRNA expression. Results Livers treated with TDSF demonstrated a qualitative reduction in lobular inflammation, lipogranuloma formation, and Kupffer cell accumulation, but not steatosis. Significant reductions in inflammatory transcripts for α-1-collagen, TGF-β, Mmp2, MCP-1, and TNF-1α were also observed. Conclusions Animals treated with TDSF exhibit a reduction in lobular inflammation that is independent of lipid accumulation when administered MCD diet. Similar reductions are seen in several inflammatory transcripts associated with NASH. Additional work in this area may reveal a therapeutic role for TDSF or similar agents in curtailing inflammatory signaling within the liver.
ISSN:1936-0533
1936-0541
DOI:10.1007/s12072-013-9426-3