Topic Highlight
Copyright ©2011 Baishideng Publishing Group Co., Limited. All rights reserved.
World J Gastroenterol. May 28, 2011; 17(20): 2558-2562
Published online May 28, 2011. doi: 10.3748/wjg.v17.i20.2558
Proteasome inhibitor treatment in alcoholic liver disease
Fawzia Bardag-Gorce
Fawzia Bardag-Gorce, Department of Pathology, Los Angeles Biomedical Research Institute, Harbor UCLA Medical Center, 1124 W. Carson St., Torrance, CA 90502, United States
Author contributions: Bardag-Gorce F wrote this review.
Supported by NIH/NIAAA 8116 and by a Pilot Project Funding from the Alcohol Center Grant on Liver and Pancreas P50-011999
Correspondence to: Fawzia Bardag-Gorce, PhD, Department of Pathology, Los Angeles Biomedical Research Institute, Harbor UCLA Medical Center, 1124 W. Carson St., Torrance, CA 90502, United States. fgorce@labiomed.org
Telephone: +1-310-2221846 Fax: +1-310-2223614
Received: January 6, 2011
Revised: February 2, 2011
Accepted: February 9, 2011
Published online: May 28, 2011
Abstract

Oxidative stress, generated by chronic ethanol consumption, is a major cause of hepatotoxicity and liver injury. Increased production of oxygen-derived free radicals due to ethanol metabolism by CYP2E1 is principally located in the cytoplasm and in the mitochondria, which does not only injure liver cells, but also other vital organs, such as the heart and the brain. Therefore, there is a need for better treatment to enhance the antioxidant response elements. To date, there is no established treatment to attenuate high levels of oxidative stress in the liver of alcoholic patients. To block this oxidative stress, proteasome inhibitor treatment has been found to significantly enhance the antioxidant response elements of hepatocytes exposed to ethanol. Recent studies have shown in an experimental model of alcoholic liver disease that proteasome inhibitor treatment at low dose has cytoprotective effects against ethanol-induced oxidative stress and liver steatosis. The beneficial effects of proteasome inhibitor treatment against oxidative stress occurred because antioxidant response elements (glutathione peroxidase 2, superoxide dismutase 2, glutathione synthetase, glutathione reductase, and GCLC) were up-regulated when rats fed alcohol were treated with a low dose of PS-341 (Bortezomib, Velcade®). This is an important finding because proteasome inhibitor treatment up-regulated reactive oxygen species removal and glutathione recycling enzymes, while ethanol feeding alone down-regulated these antioxidant elements. For the first time, it was shown that proteasome inhibition by a highly specific and reversible inhibitor is different from the chronic ethanol feeding-induced proteasome inhibition. As previously shown by our group, chronic ethanol feeding causes a complex dysfunction in the ubiquitin proteasome pathway, which affects the proteasome system, as well as the ubiquitination system. The beneficial effects of proteasome inhibitor treatment in alcoholic liver disease are related to proteasome inhibitor reversibility and the rebound of proteasome activity 72 h post PS-341 administration.

Keywords: Alcoholic liver disease; Glutathione; Oxidative stress; Proteasome inhibitor treatment; Steatosis