Decreased contact factor mediated fibrinolysis in cirrhosis

Summary. We studied extrinsic and intrinsic fibrinolysis in 20 patients with cirrhosis (nine mild/moderate, group 1:11 severe, group 2) and 19 normal controls to define the role of intrinsic (contact factor mediated) fibrinolysis in cirrhosis. Global plasma fibrinolytic activity (fibrin plate lysis) was similar in all groups. Dextran sulphate activated contact factor mediated fibrinolysis was decreased in group 2 (median 95.2%) compared with group 1 (121.0%) and controls (131.7%). Tissue plasminogen activator antigen (t‐PA Ag) levels were increased in group 2 (28.2 ng/ml) compared both with group 1(8.5 ng/ml) and controls (5.9 ng/ml). Plasma t‐PA activity was raised in group 2 (5.50 IU/ml) and group 1 (5.25 IU/ml) versus controls (0.82 IU/ml). Plasminogen activator inhibitor‐1 (PAI‐1 Ag) levels were raised in group 2 (28.0 IU/ml) versus controls (8.5 IU/ml) but PA1 activity was similar in all groups. Factor XII activity was decreased in group 2 (48.76 u/dl), but not group 1. versus controls (89.1 u/dl). Prekallikrein activity was decreased both in group 2 (27.27 u/dl) and group 1 (33.01 u/dl) versus controls (108.59 u/dl) and was lower in group 2 than group 1. C1‐esterase inhibitor chromogenic activity was decreased in group 1 (102.30 u/dl) and group 2 (58.76 u/dl) versus controls (116.24 u/dl). The normal global fibrinolytic activity despite increased t‐PA activity may be due to a concomitant increase in PAI. The decreased intrinsic fibrinolysis in severe cirrhosis, unaccompanied by a rise in C1‐esterase inhibitor, may be explained by the decreased factor XII and prekallikrein activity. These changes are probably due to reduced liver cell mass.