4.6 Article

Coupling of conformational and proteolytic activation in the kinetic mechanism of plasminogen activation by streptokinase

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 279, Issue 35, Pages 36642-36649

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M405265200

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Funding

  1. NHLBI NIH HHS [HL 10082, HL 56181] Funding Source: Medline

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Binding of streptokinase (SK) to plasminogen (Pg) induces conformational activation of the zymogen and initiates its proteolytic conversion to plasmin (Pm). The mechanism of coupling between conformational activation and Pm formation was investigated in kinetic studies. Parabolic time courses of Pg activation by SK monitored by chromogenic substrate hydrolysis had initial rates (upsilon(1)) representing conformational activation and subsequent rates of activity increase (upsilon(2)) corresponding to the rate of Pm generation determined by a specific discontinuous assay. The upsilon(2) dependence on SK concentration for [Lys]Pg showed a maximum rate at a Pg to SK ratio of similar to2:1, with inhibition at high SK concentrations. [Glu]Pg and [Lys]Pg activation showed similar kinetic behavior but much slower activation of [Glu]Pg, due to an similar to12-fold lower affinity for SK and an similar to20-fold lower k(cat)/K-m. Blocking lysine-binding sites on Pg inhibited SK.Pg* cleavage of [Lys]Pg to a rate comparable with that of [Glu]Pg, whereas [Glu]Pg activation was not significantly affected. The results support a kinetic mechanism in which SK activates Pg conformationally by rapid equilibrium formation of the SK.Pg* complex, followed by intermolecular cleavage of Pg to Pm by SK.Pg* and subsequent cleavage of Pg by SK.Pm. A unified model of SK-induced Pg activation suggests that generation of initial Pm by SK.Pg* acts as a self-limiting triggering mechanism to initiate production of one SK equivalent of SK.Pm, which then converts the remaining free Pg to Pm.

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