Inhibition of intracellular protein degradation by ethanol in perfused rat liver

A great part of our current understanding of mammalian macroautophagy is derived from studies of the liver. The term "autophagy" was introduced by Christian de Duve in part based on ultrastructural changes in rat liver following glucagon injection. Subsequent morphological, biochemical, and kinetics studies of autophagy in the liver defined the basic process of autophagosome formation, maturation, and degradation and the regulation of autophagy by hormones, phosphoinositide 3-kinases, and mammalian target of rapamycin. It is now clear that macroautophagy in the liver is important for the balance of energy and nutrients for basic cell functions, the removal of misfolded proteins resulting from genetic mutations or pathophysiological stimulations, and the turnover of major subcellular organelles such as mitochondria, endoplasmic reticulum, and peroxisomes under both normal and pathophysiological conditions. Disturbance of autophagy function in the liver could thus have a major impact on liver physiology and liver disease. (HEPATOLOGY 2008;47: 1773-1785.)

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Autophagy in the liver

Yin

2008

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Effects of Ethanol Administration on Components of the Ubiquitin Proteolytic Pathway in Rat Liver

et al. 1996

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creased catabolism of ubiquitin and its conjugates. Our Hepatic protein accumulation during ethanol adminfindings also provide no indication that the ethanol-elicistration may result partly from an ethanol-elicited deited reduction in hepatic proteolysis is because of a ubicline in hepatic protein degradation, which we have prequitin-mediated mechanism. (HEPATOLOGY 1996;23:1556-viously shown. We conducted the current studies to 1563.) examine the effects of ethanol administration on the levels of hepatic ubiquitin, an 8.5-kd protein which is an important mediator of extralysosomal protein cataboHepatomegaly is common in alcoholics and alcohollism. Rats were pair-fed liquid diets containing either fed experimental animals. It is closely associated with ethanol (36% of calories) or isocaloric maltose-dextrin increased levels of heptocellular protein that contribute for 1 to 5 weeks. Ubiquitin was immunochemically quan-to hepatocyte hypertrophy. Ubiquitin is found in all eukaryotic cells. It is a tin conjugating activity of crude and diethyl aminoethyl-fractionated liver cytosols of ethanol-fed rats had highly conserved 76-amino acid protein (relative molecequal capacities to those from controls in catalyzing the ular mass Å 8.5 kd) that covalently binds proteins desformation of ubiquitin-protein conjugates. Our findings tined for degradation. Three enzymes, E1, E2, and E3, indicate that chronic ethanol consumption increased catalyze the formation of ubiquitin-protein conjugates, the level of immunoreactive ubiquitin in rat liver. This a process called ubiquitylation (for reviews, see refermay have resulted from enhanced ubiquitin production ences 12-14). Cellular proteins targeted for degradation because of an ethanol-elicited stress response and/or de-are ubiquitylated at their NH 2 termini and at the eamino groups of lysine residues within the polypeptide chain. These conjugation points may each carry one substrate and recycles intact ubiquitin for further Received March 11, 1994; accepted January 12, 1996. rounds of ubiquitylation. 17Current address of Dr. Born is Indiana University Medical Center, 975The apparent role of the ubiquitin-mediated proteo-

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