Regulation of liver hepcidin expression by alcohol in vivo does not involve Kupffer cell activation or TNF-{alpha} signaling

doi:10.1152/ajpgi.90550.2008

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Am J Physiol Gastrointest Liver Physiol 296: G112-G118, 2009. First published November 13, 2008; doi:10.1152/ajpgi.90550.2008
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LIVER AND BILIARY TRACT

Regulation of liver hepcidin expression by alcohol in vivo does not involve Kupffer cell activation or TNF- ${alpha}$ signaling

Duygu Dee Harrison-Findik,¹ Elizabeth Klein,¹ John Evans,¹ and John Gollan¹^,2

¹Division of Gastroenterology/Hepatology, Department of Internal Medicine and ²Dean's Office, University of Nebraska Medical Center, Omaha, Nebraska

Submitted 16 September 2008 ; accepted in final form 10 November 2008

Alcohol downregulates hepcidin expression in the liver leadingto an increase in intestinal iron transport and liver iron storage.We have previously demonstrated that alcohol-mediated oxidativestress is involved in the inhibition of hepcidin transcriptionby alcohol in vivo. Kupffer cells and TNF- ${alpha}$ play a key role inalcohol-induced liver injury. The aim of this study was to definetheir involvement in the regulation of hepcidin expression byalcohol. Kupffer cells were inactivated or depleted by employinggadolinium chloride and liposomes containing clodronate, respectively.Rats pair fed with the alcohol-Lieber-DeCarli diet for 6 wkand mice fed with 20% ethanol in the drinking water for 1 wkwere used as experimental models. Interestingly, alcohol downregulatedhepcidin expression in the livers of rats and mice independentof gadolinium chloride or clodronate treatment. One week ofalcohol treatment was sufficient to induce a significant increasein TNF- ${alpha}$ levels and phosphorylation of NF- ${kappa}$ B subunit p65. Theneutralization of TNF- ${alpha}$ by specific antibodies inhibited p65phosphorylation. However, neither the neutralization of TNF- ${alpha}$ nor the lack of TNF- ${alpha}$ receptor expression reversed alcohol-inducedsuppression of liver hepcidin expression. The level of alcohol-inducedROS in the liver was also undiminished following Kupffer cellinactivation or depletion. Our results demonstrate that alcohol-inducedKupffer cell activation and TNF- ${alpha}$ signaling are not involvedin the suppression of liver hepcidin expression by alcohol-mediatedoxidative stress in vivo. Therefore, these findings suggestthat alcohol acts within hepatocytes to suppress hepcidin expressionand thereby influences iron homeostasis.

alcoholic liver disease; iron; liver injury; oxidative stress

Address for reprint requests and other correspondence: D. Harrison-Findik, 95820 UNMC, Omaha, NE 68198-5820 (e-mail: dharrisonfindik{at}unmc.edu)

Regulation of liver hepcidin expression by alcohol in vivo does not involve Kupffer cell activation or TNF- signaling

Regulation of liver hepcidin expression by alcohol in vivo does not involve Kupffer cell activation or TNF- ${alpha}$ signaling