fibrin and Hepatitis--Alcoholic

fibrin has been researched along with Hepatitis--Alcoholic* in 2 studies

Other Studies

2 other study(ies) available for fibrin and Hepatitis--Alcoholic

Article	Year
PKCε contributes to chronic ethanol-induced steatosis in mice but not inflammation and necrosis. Alcoholism, clinical and experimental research, 2014, Volume: 38, Issue:3 Protein kinase C epsilon (PKCε) has been shown to play a role in experimental steatosis by acute alcohol. The "two-hit" hypothesis implies that preventing steatosis should blunt more advanced liver damage (e.g., inflammation and necrosis). However, the role of PKCε in these pathologies is not yet known. The goal of this current work was to address this question in a model of chronic alcohol exposure using antisense oligonucleotides (ASO) against PKCε.. Accordingly, PKCε ASO- and saline-treated mice were fed high-fat control or ethanol (EtOH)-containing enteral diets for 4 weeks.. Chronic EtOH exposure significantly elevated hepatic lipid pools as well as activated PKCε. The PKCε ASO partially blunted the increases in hepatic lipids caused by EtOH. Administration of PKCε ASO also completely prevented the increase in the expression of fatty acid synthase, and tumor necrosis factor α caused by EtOH. Despite these protective effects, the PKCε ASO was unable to prevent the increases in inflammation and necrosis caused by chronic EtOH. These latter results correlated with an inability of the PKCε ASO to blunt the up-regulation of plasminogen activator inhibitor-1 (PAI-1) and the accumulation of fibrin. Importantly, PAI-1 has been previously shown to more robustly mediate inflammation and necrosis (vs. steatosis) after chronic EtOH exposure.. This study identifies a novel potential mechanism where EtOH, independent of steatosis, can contribute to liver damage. These results also suggest that PAI-1 and fibrin accumulation may be at the center of this PKCε-independent pathway. Topics: Animals; Biomarkers; Body Weight; Central Nervous System Depressants; Diglycerides; Enzyme Activation; Ethanol; Fatty Liver, Alcoholic; Fibrin; Gene Expression; Hepatitis, Alcoholic; Lipid Metabolism; Liver; Male; Mice; Mice, Inbred C57BL; Necrosis; Protein Kinase C-epsilon	2014
Fibrinous pericarditis in alcoholic liver disease. Journal of clinical gastroenterology, 1989, Volume: 11, Issue:1 The autopsy data at the University of Southern California Liver Unit was studied during a 6-year period to investigate the relationship of fibrinous pericarditis with liver diseases. We found 18 cases of fibrinous pericarditis in 220 patients with alcoholic liver disease but none in 32 patients with fulminant and subacute hepatitis without alcoholism or in 39 patients with nonalcoholic cirrhosis. Although all the 18 patients with pericarditis had azotemia, 3 patients had pericarditis develop only in mild renal function impairment. These findings suggest that chronic alcoholism may precipitate pericarditis during the hepatorenal syndrome. Topics: Adult; Aged; Aged, 80 and over; Fibrin; Hepatitis, Alcoholic; Humans; Liver Cirrhosis, Alcoholic; Male; Middle Aged; Pericarditis; Retrospective Studies; Uremia	1989

Article

Year

PKCε contributes to chronic ethanol-induced steatosis in mice but not inflammation and necrosis.

Alcoholism, clinical and experimental research, 2014, Volume: 38, Issue:3

Protein kinase C epsilon (PKCε) has been shown to play a role in experimental steatosis by acute alcohol. The "two-hit" hypothesis implies that preventing steatosis should blunt more advanced liver damage (e.g., inflammation and necrosis). However, the role of PKCε in these pathologies is not yet known. The goal of this current work was to address this question in a model of chronic alcohol exposure using antisense oligonucleotides (ASO) against PKCε.. Accordingly, PKCε ASO- and saline-treated mice were fed high-fat control or ethanol (EtOH)-containing enteral diets for 4 weeks.. Chronic EtOH exposure significantly elevated hepatic lipid pools as well as activated PKCε. The PKCε ASO partially blunted the increases in hepatic lipids caused by EtOH. Administration of PKCε ASO also completely prevented the increase in the expression of fatty acid synthase, and tumor necrosis factor α caused by EtOH. Despite these protective effects, the PKCε ASO was unable to prevent the increases in inflammation and necrosis caused by chronic EtOH. These latter results correlated with an inability of the PKCε ASO to blunt the up-regulation of plasminogen activator inhibitor-1 (PAI-1) and the accumulation of fibrin. Importantly, PAI-1 has been previously shown to more robustly mediate inflammation and necrosis (vs. steatosis) after chronic EtOH exposure.. This study identifies a novel potential mechanism where EtOH, independent of steatosis, can contribute to liver damage. These results also suggest that PAI-1 and fibrin accumulation may be at the center of this PKCε-independent pathway.

Topics: Animals; Biomarkers; Body Weight; Central Nervous System Depressants; Diglycerides; Enzyme Activation; Ethanol; Fatty Liver, Alcoholic; Fibrin; Gene Expression; Hepatitis, Alcoholic; Lipid Metabolism; Liver; Male; Mice; Mice, Inbred C57BL; Necrosis; Protein Kinase C-epsilon

2014

Fibrinous pericarditis in alcoholic liver disease.

Journal of clinical gastroenterology, 1989, Volume: 11, Issue:1

The autopsy data at the University of Southern California Liver Unit was studied during a 6-year period to investigate the relationship of fibrinous pericarditis with liver diseases. We found 18 cases of fibrinous pericarditis in 220 patients with alcoholic liver disease but none in 32 patients with fulminant and subacute hepatitis without alcoholism or in 39 patients with nonalcoholic cirrhosis. Although all the 18 patients with pericarditis had azotemia, 3 patients had pericarditis develop only in mild renal function impairment. These findings suggest that chronic alcoholism may precipitate pericarditis during the hepatorenal syndrome.

Topics: Adult; Aged; Aged, 80 and over; Fibrin; Hepatitis, Alcoholic; Humans; Liver Cirrhosis, Alcoholic; Male; Middle Aged; Pericarditis; Retrospective Studies; Uremia

1989