Thromb Haemost 1983; 50(04): 787-791
DOI: 10.1055/s-0038-1665313
Original Article
Schattauer GmbH Stuttgart

The Human Plasmin-Derived Light (B) Chain·Streptokinase Complex: A Second-Generation Thrombolytic Agent

K C Robbins
1   The Michael Reese Research Foundation, University of Chicago, Chicago, IL
2   The Departments of Medicine and Pathology, Pritzker School of Medicine, University of Chicago, Chicago, IL
,
L Summaria
1   The Michael Reese Research Foundation, University of Chicago, Chicago, IL
,
R C Wohl
1   The Michael Reese Research Foundation, University of Chicago, Chicago, IL
,
W R Bell
3   The Hematology Division, Johns Hopkins Hospital3, Baltimore, MD, U.S.A.
› Institutsangaben
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Publikationsverlauf

Received 17. Mai 1983

Accepted 17. August 1983

Publikationsdatum:
18. Juli 2018 (online)

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Summary

Specific assay methods for the human plasmin-derived light (B) chain · streptokinase (B·SK) complex, in terms of both streptokinase (SK) and urokinase (UK) International Units, are described. The kinetic properties of various SK activator complexes with plasminogen, Val 442-plasmin, and the plasmin-derived light (B) chain were compared to SK in terms of their catalytic efficiencies and Lineweaver-Burk plots. Similar kinetic data, and Lineweaver-Burk plots, are described for both highly purified high-molecular weight UK and low-molecular weight UK, including different clinical UK preparations. The B·SK complex has the highest catalytic efficiency of all the activator species studied. The Lineweaver-Burk plots of each of the various activator species are “fingerprints” of the enzymatic character of the activator. The B-SK complex is more like UK than SK, as an activator, in activating non-human plasminogen species. The biological halflife of the B·SK complex, in a dog model, was determined to be about 4 hr which is longer than the biological half-life(s) of SK in the same animal model, namely 0.6 hr (47%) and 2.8 hr (53%). This new second-generation activator complex may prove to be a useful thrombolytic agent in the treatment of thromboembolic diseases.