S-Adenosyl-l-methionine and mitochondrial reduced glutathione depletion in alcoholic liver disease

Fernández-Checa, José C; Colell, Anna; Garcı́a-Ruiz, Carmen

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Volume 27, Issue 3 , Pages 179-183, July 2002

S-Adenosyl-l-methionine and mitochondrial reduced glutathione depletion in alcoholic liver disease☆

José C Fernández-Checa
- Corresponding author. Liver Unit, Hospital Clinic I Provincial, Villarroel, 170, 08036 Barcelona, Spain. Tel.: +34-93-227-5709; fax: +34-93-451-5272.
- Liver Unit, Hospital Clinic I Provincial, 08036 Barcelona, Spain
- Instituto Investigaciones Biomedicas de Barcelona, IDIBAPS, 08036 Barcelona, Spain
- Consejo Superior Investigaciones Cientificas, 08036 Barcelona, Spain
Anna Colell
- Liver Unit, Hospital Clinic I Provincial, 08036 Barcelona, Spain
- Instituto Investigaciones Biomedicas de Barcelona, IDIBAPS, 08036 Barcelona, Spain
- Consejo Superior Investigaciones Cientificas, 08036 Barcelona, Spain
Carmen Garcı́a-Ruiz
- Liver Unit, Hospital Clinic I Provincial, 08036 Barcelona, Spain
- Instituto Investigaciones Biomedicas de Barcelona, IDIBAPS, 08036 Barcelona, Spain
- Consejo Superior Investigaciones Cientificas, 08036 Barcelona, Spain

Received 4 February 2002; received in revised form 28 March 2002; accepted 28 March 2002.

Abstract

The pathogenesis of alcohol-induced liver disease is not well understood, and many factors have been described to contribute to the progressive loss of liver functions, including the overgeneration of reactive oxygen species. Mitochondria are specific targets of the toxic effects of ethanol, reflected in the loss of phosphorylative oxidation and defective ATP generation, which underlie one of the hallmarks of the hepatic alterations induced by chronic alcohol intake. Mitochondrial reduced glutathione (GSH), whose primary function is to maintain a competitive functional organelle, becomes depleted by alcohol intake. Furthermore, GSH depletion in hepatocyte mitochondria has been revealed as an important mechanism in the sensitization of liver to alcohol-induced injury. This depletion of the mitochondrial GSH level is determined by an impaired transport of GSH from the cytosol into the mitochondrial matrix owing to a partial inactivation of mitochondrial GSH carrier. The loss of function of this specific mitochondrial transporter is due to the alterations in the physicochemical properties of the inner mitochondrial membrane caused by alcohol. Because of the primary defect in the transport of cytosolic GSH into mitochondria, GSH precursors are inefficient in replenishing the levels of mitochondrial GSH despite significant increase in cytosolic GSH. Supplementation of S-adenosyl-l-methionine (SAM) to rats fed alcohol chronically has been shown to replete the mitochondrial GSH levels because of normalization of the microviscosity of the mitochondrial inner membrane. Because of the instrumental role of GSH in mitochondria in hepatocyte survival against inflammatory cytokines, its repletion by SAM feeding may underlie the potential therapeutic use of this hepatoprotective agent in the treatment of alcohol-induced liver injury.

Keywords: Ethanol, Lipid peroxidation, Oxidative stress, Cell death, Necrosis, Apoptosis, Tumor necrosis factor-α