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J. Biol. Chem., Vol. 264, Issue 14, 7957-7961, May, 1989
J Wojta, R Beckmann, L Turcu, OF Wagner, AJ van Zonneveld and BR Binder
Fibrin interacts with tissue-type plasminogen activator (tPA) via the
finger and the kringle 2 domains. Three monoclonal antibodies against tPA,
designated MPW3VPA, MPW6VPA, and MPW7VPA, which react with epitopes in the
tPA molecule involved in fibrin binding, were characterized. The IgM
monoclonal antibody MPW6VPA, directed against an epitope close to the
finger and epidermal growth factor domains, stimulated plasminogen
activation only in the absence of CNBr- fibrinogen fragments by increasing
kcat in a dose-dependent fashion, an effect which was not restricted to the
intact molecule. These results suggest that MPW6VPA mimics the initial
effect of fibrin bound to the tPA molecule, which results in a change of
kcat values. The MPW6VPA effect was reversed by another antibody, MPW3VPA,
also directed against epidermal growth factor and finger domains. The
latter antibody also inhibited plasminogen activation by tPA in the
presence of CNBr- fibrinogen fragments in a dose-dependent, apparently
noncompetitive way. No effect of MPW3VPA was seen in the absence of
CNBr-fibrinogen fragments. MPW7VPA directed against kringle 2 of tPA
inhibited plasminogen activation by tPA only when CNBr-fibrinogen fragments
were present. This inhibition was apparently competitive and
dose-dependent. These data suggest that MPW3VPA interferes with the first
phase of fibrin binding to tPA, whereas MPW7VPA interferes with the second
phase of fibrin binding to the tPA molecule via kringle 2, resulting in Km
changes.
Functional characterization of monoclonal antibodies directed against fibrin binding domains of tissue-type plasminogen activator
Department of Medical Physiology, University of Vienna, Austria.
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