Cirrhosis Clinical Trial
Official title:
Impact on Morbidity and Mortality of Prophylactic Dosing of Low Molecular Weight Heparin in Child-Pugh B Cirrhotic Patients: a Randomized Controlled Study
Thrombosis occurring in the small intrahepatic, as well as in the large vessels is involved in the progression of cirrhosis. Anticoagulation could reduce morbidity and mortality in cirrhotic patients
Cirrhosis is the end-stage of all chronic liver diseases. Cirrhosis is a critical step in the
natural history of liver disease, as it is associated with the occurrence of complications
(so-called decompensation) and death. Life expectancy varies from 12-14 years in patients
with compensated cirrhosis, to 2-4 years after decompensation.
Cirrhosis is associated with thrombosis of the intrahepatic portal and hepatic venous systems
leading to parenchymal extinction (atrophy), liver dysfunction and portal hypertension.
Regeneration in the areas without microthrombosis, and inflammation are powerful factors
inducing liver cancer. Portal and hepatic venous thrombosis have been shown to participate in
remodeling the liver architecture and are associated with a worsening outcome. Thrombosis in
cirrhosis is thought to result from a procoagulant state due to an imbalance between pro and
anticoagulant factor plasma levels, inflammation in and around blood vessels, and a marked
slowing down of venous blood flow. Heparin administration, in animal models of liver
fibrosis, decreases extra cellular matrix protein synthesis and fibrous tissue deposition.
Recently, a reduction in liver decompensation and mortality has been shown in Child-Pugh
B7-C10 cirrhotic patients assigned to receive a low dose of enoxaparin (4000IU/d), a low
molecular weight heparin, for 48 weeks, compared to patients receiving no anticoagulation
therapy.
These results are in line with the hypothesis of a protective role of anticoagulation in
liver disease progression and a strong association between thrombosis and liver fibrosis.
So the main objective of the study is to compare the effect of a 2-year low dosing of
Enoxaparin (4000 IU/day) versus no treatment on morbidity and mortality in patients with
Child B7-C10 cirrhosis.
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