Oxidative stress and hepatic stellate cell activation are key events in arsenic induced liver fibrosis in mice

S Ghatak, A Biswas, GK Dhali, A Chowdhury… - Toxicology and applied …, 2011 - Elsevier
S Ghatak, A Biswas, GK Dhali, A Chowdhury, JL Boyer, A Santra
Toxicology and applied pharmacology, 2011Elsevier
Arsenic is an environmental toxicant and carcinogen. Exposure to arsenic is associated with
development of liver fibrosis and portal hypertension through ill defined mechanisms. We
evaluated hepatic fibrogenesis after long term arsenic exposure in a murine model. BALB/c
mice were exposed to arsenic by daily gavages of 6μg/gm body weight for 1year and were
evaluated for markers of hepatic oxidative stress and fibrosis, as well as pro-inflammatory,
pro-apoptotic and pro-fibrogenic factors at 9 and 12months. Hepatic NADPH oxidase activity …
Arsenic is an environmental toxicant and carcinogen. Exposure to arsenic is associated with development of liver fibrosis and portal hypertension through ill defined mechanisms. We evaluated hepatic fibrogenesis after long term arsenic exposure in a murine model. BALB/c mice were exposed to arsenic by daily gavages of 6μg/gm body weight for 1year and were evaluated for markers of hepatic oxidative stress and fibrosis, as well as pro-inflammatory, pro-apoptotic and pro-fibrogenic factors at 9 and 12months. Hepatic NADPH oxidase activity progressively increased in arsenic exposure with concomitant development of hepatic oxidative stress. Hepatic steatosis with occasional collection of mononuclear inflammatory cells and mild portal fibrosis were the predominant liver lesion observed after 9months of arsenic exposure, while at 12months, the changes included mild hepatic steatosis, inflammation, necrosis and significant fibrosis in periportal areas. The pathologic changes in the liver were associated with markers of hepatic stellate cells (HSCs) activation, matrix reorganization and fibrosis including α-smooth muscle actin, transforming growth factor-β1, PDGF-Rβ, pro-inflammatory cytokines and enhanced expression of tissue inhibitor of metalloproteinase-1 and pro(α) collagen type I. Moreover, pro-apoptotic protein Bax was dominantly expressed and Bcl-2 was down-regulated along with increased number of TUNEL positive hepatocytes in liver of arsenic exposed mice. Furthermore, HSCs activation due to increased hepatic oxidative stress observed after in vivo arsenic exposure was recapitulated in co-culture model of isolated HSCs and hepatocytes exposed to arsenic. These findings have implications not only for the understanding of the pathology of arsenic related liver fibrosis but also for the design of preventive strategies in chronic arsenicosis.
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