"Alcoholic steatosis is a fundamental metabolic disorder in die progression of alcoholic liver disease. Zinc deficiency is one of the most consistently observed biochemical/nutritional manifestations of alcoholic liver disease," investigators in the United States report (see also Alcoholism).

"The purpose of this study is to determine whether dietary zinc supplementation to mice previously exposed to alcohol could reverse alcoholic steatosis. Male 129S mice were pair-fed an alcohol or isocaloric maltose dextrin liquid diet for 16 weeks with or without dietary zinc supplementation for the last 4 weeks. Zinc supplementation significantly attenuated alcohol-mediated increases in hepatic triglyceride, cholesterol, and free fatty acids in association with accelerated hepatic fatty acid oxidation and very low density lipoproteins (VLDL) secretion. Hepatic genes related to fatty acid oxidation and VLDL secretion were up-regulated by zinc supplementation, which was accompanied by restoring activity of hepatocyte nuclear factor-4 alpha (HNF-4 alpha) and peroxisome proliferators activated receptor-alpha (PPAR-alpha). Zinc supplementation enhanced alcohol metabolism and attenuated oxidative stress and liver injury. Zinc supplementation also normalized alcohol-mediated increases in plasma triglycerides and partially reversed decrease in gonadal adipose depot mass. Studies in HepG2 cells showed that zinc deprivation significantly suppressed the DNA-binding activities of HNF-4 alpha and PPAR-alpha, and reduced HNF-4 alpha and PPAR-alpha target proteins. Consequently, zinc deprivation caused cellular accumulation of lipid droplets, triglycerides and free fatty acids in the HepG2 cells," wrote Y.Q. Kang and colleagues, University of Louisville, Medical Department.

The researchers concluded: "Zinc supplementation reverses alcoholic steatosis, and reactivation of HNF-4 alpha and PPAR-alpha by increasing zinc availability and inhibiting oxidative stress are potential mechanisms underlying these beneficial effects of zinc on hepatic lipid homeostasis. (HEPATOLOGY 2009;50: 1241-1250.)."

Kang and colleagues published their study in Hepatology (Zinc Supplementation Reverses Alcohol-Induced Steatosis in Mice Through Reactivating Hepatocyte Nuclear Factor-4 alpha and Peroxisome Proliferator-Activated Receptor-alpha. Hepatology, 2009;50(4):1241-1250).

For additional information, contact Z.X. Zhou, University of Louisville, School Medical, Dept. of Medical, 511 S Floyd St., MDR 529, Louisville, KY 40292, USA.

The publisher of the journal Hepatology can be contacted at: John Wiley & Sons Inc., 111 River St., Hoboken, NJ 07030, USA.