The activities of the hepatic monoamine oxidase (MAO) were studies when cholestasis was induced and acute ethanol intoxication developed, or cholestasis following chronic ethanol intoxication for manifestation of the biochemical background of alcohol intoxication in hepatobiliary disease. There were marked increases in the mitochondrial 5-hydroxytryptamine-MAO (5HT-MAO) and benzyla-mine-MAO (Benz-MAO) activities of the liver of the rats treated with chronic ethanol intoxication, and showed significant increase in the mitochondrial Benz-MAO after treatment with acute ethanol intoxication. When common bile duct was ligated in the rats, mitochondrial 5HT-MAO and Benz-MAO activities in the liver significantly decreased. When common bile duct was ligated after chronic ethanol intoxication and acute ethanol intoxication was done after common bile duct ligation, the activities of mitochondrial 5HT-MAO and Benz-MAO in the liver decreased more significantly than in the group only with ethanol intoxication was performed. However, the activities showed a higher degree on the same time points than the groups only with the common bile duct ligation. And microsomal 5HT-MAO and Benz-MAO activities in the liver showed significant increase when treated both with the chronic or the acute ethanol intoxication. According to the above results, the hepatic MAO seems to be an enzyme in which its activity increases in acute and chronic ethanol intoxication. And MAO in the liver is the enzyme with increased activities in ethanol intoxidation with cholestasis more than in cholestasis. The cause of the increase is the development of biosynthesis. Accordingly, these results will be the data supporting that alcoholic drink is enzymologically harmful in hepatobillary disease.