thromboplastin and Alcoholism

thromboplastin has been researched along with Alcoholism* in 2 studies

Other Studies

2 other study(ies) available for thromboplastin and Alcoholism

Article	Year
Chronic ethanol consumption decreases serum sulfatide levels by suppressing hepatic cerebroside sulfotransferase expression in mice. Archives of toxicology, 2014, Volume: 88, Issue:2 Epidemiological studies demonstrate a possible relationship between chronic ethanol drinking and thrombotic diseases, such as myocardial infarction and stroke. However, the precise mechanism for this association remains unclear. Sulfatides are endogenous glycosphingolipids composed of ceramide, galactose, and sulfate, known to have anti-thrombotic properties. Low (0.5 g/kg/day), middle (1.5 g/kg/day), and high (3.0 g/kg/day) doses of ethanol were administered for 21 days intraperitoneally to female wild-type mice, and serum/liver sulfatide levels were measured. No significant changes in cholesterol and triglycerides were seen in serum and liver by ethanol treatment. However, serum/liver sulfatide levels were significantly decreased by middle- and high-dose ethanol treatment, likely due to downregulation of hepatic cerebroside sulfotransferase (CST) levels. Marked decreases in the expression of catalase and superoxide dismutases and ensuing increases in lipid peroxides were also observed in the livers of mice with middle- and high-dose ethanol treatment, suggesting the association between the suppression of hepatic CST expression and enhancement of oxidative stress. Furthermore, serum levels of tissue factor, a typical pro-coagulant molecule, were significantly increased in the mice with middle- and high-dose ethanol treatment showing decreases in serum sulfatide levels. Collectively, these results demonstrate that chronic ethanol consumption reduces serum sulfatide levels by increasing oxidative stress and decreasing the expression of CST in the liver. These findings could provide a mechanism by which chronic ethanol drinking increases thrombotic events. Topics: Alcoholism; Animals; Dose-Response Relationship, Drug; Ethanol; Female; Ganglioside Galactosyltransferase; Lipid Metabolism; Liver; Mice; Mice, Inbred Strains; Oxidative Stress; Sulfoglycosphingolipids; Sulfotransferases; Thromboplastin	2014
[Blood coagulating and anticoagulant properties of the tissues in experimental chronic alcoholism in albino rats]. Gematologiia i transfuziologiia, 1990, Volume: 35, Issue:7 A study was made of thromboplastin, antiheparin and antithrombin activity of the brain, heart and liver tissues of rats in experimental chronic alcoholization. Appreciable changes in the tissue factors of coagulation according to the dyscoagulemia type depending on the duration and gravity of alcoholic intoxication may aggravate hemostatic disorders. Topics: Alcoholism; Animals; Antithrombin III; Blood Coagulation; Brain; Disease Models, Animal; Ethanol; Liver; Myocardium; Platelet Factor 4; Rats; Thromboplastin	1990

Article

Year

Chronic ethanol consumption decreases serum sulfatide levels by suppressing hepatic cerebroside sulfotransferase expression in mice.

Archives of toxicology, 2014, Volume: 88, Issue:2

Epidemiological studies demonstrate a possible relationship between chronic ethanol drinking and thrombotic diseases, such as myocardial infarction and stroke. However, the precise mechanism for this association remains unclear. Sulfatides are endogenous glycosphingolipids composed of ceramide, galactose, and sulfate, known to have anti-thrombotic properties. Low (0.5 g/kg/day), middle (1.5 g/kg/day), and high (3.0 g/kg/day) doses of ethanol were administered for 21 days intraperitoneally to female wild-type mice, and serum/liver sulfatide levels were measured. No significant changes in cholesterol and triglycerides were seen in serum and liver by ethanol treatment. However, serum/liver sulfatide levels were significantly decreased by middle- and high-dose ethanol treatment, likely due to downregulation of hepatic cerebroside sulfotransferase (CST) levels. Marked decreases in the expression of catalase and superoxide dismutases and ensuing increases in lipid peroxides were also observed in the livers of mice with middle- and high-dose ethanol treatment, suggesting the association between the suppression of hepatic CST expression and enhancement of oxidative stress. Furthermore, serum levels of tissue factor, a typical pro-coagulant molecule, were significantly increased in the mice with middle- and high-dose ethanol treatment showing decreases in serum sulfatide levels. Collectively, these results demonstrate that chronic ethanol consumption reduces serum sulfatide levels by increasing oxidative stress and decreasing the expression of CST in the liver. These findings could provide a mechanism by which chronic ethanol drinking increases thrombotic events.

Topics: Alcoholism; Animals; Dose-Response Relationship, Drug; Ethanol; Female; Ganglioside Galactosyltransferase; Lipid Metabolism; Liver; Mice; Mice, Inbred Strains; Oxidative Stress; Sulfoglycosphingolipids; Sulfotransferases; Thromboplastin

2014

[Blood coagulating and anticoagulant properties of the tissues in experimental chronic alcoholism in albino rats].

Gematologiia i transfuziologiia, 1990, Volume: 35, Issue:7

A study was made of thromboplastin, antiheparin and antithrombin activity of the brain, heart and liver tissues of rats in experimental chronic alcoholization. Appreciable changes in the tissue factors of coagulation according to the dyscoagulemia type depending on the duration and gravity of alcoholic intoxication may aggravate hemostatic disorders.

Topics: Alcoholism; Animals; Antithrombin III; Blood Coagulation; Brain; Disease Models, Animal; Ethanol; Liver; Myocardium; Platelet Factor 4; Rats; Thromboplastin

1990