A Novel Chimaeric Derivative of Saruplase, rscu-PA-40kDA/Hir, Binds to Thrombin and Exerts Thrombus-specific Fibrinolysis in Arterial and Venous Thrombosis in Dogs

J Schneider; R Hauser; H-H Hennies; J Korioth; G Steffens; S Wnendt

doi:10.1055/s-0038-1656002

Thrombosis and Haemostasis, Inhaltsverzeichnis

Thromb Haemost 1997; 77(03): 535-539
DOI: 10.1055/s-0038-1656002

Fibrinolysis

Schattauer GmbH Stuttgart

A Novel Chimaeric Derivative of Saruplase, rscu-PA-40kDA/Hir, Binds to Thrombin and Exerts Thrombus-specific Fibrinolysis in Arterial and Venous Thrombosis in Dogs

J Schneider

The Grünenthal GmbH, Centre of Research, Aachen, Germany

,

R Hauser

The Grünenthal GmbH, Centre of Research, Aachen, Germany

,

H-H Hennies

The Grünenthal GmbH, Centre of Research, Aachen, Germany

,

J Korioth

The Grünenthal GmbH, Centre of Research, Aachen, Germany

,

G Steffens

The Grünenthal GmbH, Centre of Research, Aachen, Germany

,

S Wnendt

The Grünenthal GmbH, Centre of Research, Aachen, Germany

› Institutsangaben

Abstract

als PDF herunterladen

Summary

The chimaeric molecule rscu-PA-40kDA/Hir (M23) comprises the kringle and protease domain of saruplase (rscu-PA) and a thrombin inhibitory domain fused to the C-terminus of the protease domain. The 27 amino acid long thrombin inhibitory domain contains a sequence directed to the active site of thrombin and a fragment from the C-terminal region of hirudin. ¹²⁵I-radiolabelled M23 (0.03 µM) bound to thrombin that was immobilised onto CNBr-activated sepharose beads. Unlabelled M23 (0.01-10 |xM) and hirudin (0.001-10 µµM) concentra-tion-dependently displaced ¹²⁵I-M23 from its binding to thrombin. Saruplase (up to 10 (iM) did not influence the thrombin binding of M23. The fibrinolytic properties of M23 and saruplase were compared in anaesthetized dogs with femoral artery and saphenous vein thrombosis. Under concomitant heparinization, the intravenous bolus injections of 1 mg/kg M23 or saruplase induced reperfusion of thrombotically occluded femoral arteries in 4 out of 5 treated animals in each case. There was one reocclusion in the M23-treated group. Time to reperfusion (23 ± 4 vs 25 ± 11 min) and maximal height of reperfusion blood flow (98 ± 21 vs 108 ± 15 % of baseline flow) did not differ significantly between the treatment groups. The time course of the lysis of incorporated ¹²⁵I-fibrin radioactivity in thrombosed saphenous veins was similar after bolus injections of M23 and saruplase. The maximal dissolution of ¹²⁵I-fibrin in the venous thrombosis model was 91 ± 1 % in M23-and 88 ± 5 % in saruplase-treated animals. Plasma levels of fibrinogen were not influenced and a₂-antiplasmin levels were slightly reduced (-27 ± 3 %) after bolus injection of M23. In contrast, bolus injection of saruplase was accompanied by a significant decrease of fibrinogen (-55 ± 19 %) and a₂-antiplasmin (-75 ±11%) plasma levels. Template bleeding times virtually did not differ before (2.8 ± 0.3 min) and 60 min after bolus injection of M23 (3.1 ± 0.3 min), whereas treatment with saruplase resulted in a significant prolongation of template bleeding time from 2.6 ± 0.2 min to 28 ± 13 min. It is concluded that the saruplase derivative M23, while inducing equieffective thrombolysis after intravenous bolus injection in dogs, causes much fewer haemostatic side effects than its parent molecule. The high thrombus-specific activity of M23 is tentatively attributed to its affinity to clot-bound thrombin.

PDF (1629 kb)

Referenzen

References
57 Reiner JS, Wasserman AG. The role of thrombolytic therapy for acute myocardial infarction. Cor Art Dis 1994; 5: 0373-0379
58 Simes RJ, Topol EJ, Holmes DR, White HD, Rutsch WR, Vahanian A, Simoons ML, Morris D, Betriu A, Califf RM, Ross AM. Link between the angiographic substudy and mortality outcomes in a large randomized trial of myocardial reperfusion. Importance of early and complete infarct artery reperfusion. Circulation 1995; 91: 1923-1928
3 Shammas NW, Zeitler R, Fitzpatrick P. Intravenous thrombolytic therapy in myocardial infarction: an analytical review. Clin Cardiol 1993; 16: 0283-0292
4 Verstraete M. Advances in thrombolytic therapy. Cardiovasc Drugs Ther 1992; 6: 0111-0124
5 Francis CW, Markham RE, Barlow GH, Florack ThM, Dobrzynski DM, Marder VJ. Thrombin activity of fibrin thrombi and soluble plasmic derivatives. J Lab Clin Med 1983; 102: 0220-0230
6 Phaneuf MD, Ozaki CK, Johnstone MT, Loza JP, Quist WC, LoGerfo FW. Covalent linkage of streptokinase to recombinant hirudin: a novel thrombolytic agent with antithrombotic properties. Thromb Haemostas 1994; 71: 0481-0487
7 Wnendt S, Janocha E, Schneider J, Steffens GJ. Construction and structure/function relationships of chimeric prourokinase derivatives with intrinsic thrombin-inhibitory potential. Protein Engineering 1996; 9: 0213-0223
8 Hanbiicken FW, Schneider J, Günzler WA, Friderichs E, Giertz H, Flohé L. Selective fibrinolytic activity of recombinant non-glycosylated human prourokinase (single chain urokinase-type plasminogen activator) from bacteria. Arznm Forsch/Drug Res 1987; 37: 0993-0997
9 Lijnen HR, Wnendt S, Schneider J, Janocha E, van Hoef B, Collen D, Steffens GJ. Functional properties of a recombinant chimeric protein with combined thrombin inhibitory and plasminogen-activating potential. Eur J Bio-chem 1995; 234: 0350-0357
10 Schneider J, Wnendt S, Saunders D, Heinzel-Wieland R, Wilffert B, Steffens G. Thrombin inhibitory and clot-specific fibrinolytic activities of the urokinase variant, M23 (rscu-PA-40 kDA/Hir). Eur J Pharmacol 1996; 302: 0069-0077
11 Bolton AE, Hunter WM. The labelling of proteins to high specific radioactivities by conjugation to a ¹²⁵I-containing acylating agent. Biochem J 1973; 133: 0529-0539
12 Clauss A. Rapid physiological coagulation method for the determination of fibrinogen. Acta Haematol 1957; 17: 0237-0246
13 Lefkovits J, Topol EJ. Direct thrombin inhibitors in cardiovascular medicine. Circulation 1994; 90: 1522-1536
14 Seitz R, Blanke H, Pratorius G, Strauer BE, Egbring R. Increased thrombin activity during thrombolysis. Thromb Haemostas 1988; 59: 0541-0542
15 Gulba DC, Barthels M, Westhoff-Bleck M, Jost S, Raffenbeul W, Daniel WG, Hecker H, Lichtlen PR. Increased thrombin levels during thrombolytic therapy in acute myocardial infarction. Circulation 1991; 83: 0937-0944
16 PRIMI-trial study group. Randomized double-blind trial of recombinant pro-urokinase against streptokinase in acute myocardial infarction. The Lancet 22.04.1989; 8643: 0863-0868
17 Rapold HJ, Wu Z, Stassen T, van de Werf F, Collen D. Comparison of intravenous bolus injection or continuous infusion of recombinant single chain urokinase-type plasminogen activator (saruplase) for thrombolysis. A canine model of combined coronary arterial and femoral venous thrombosis. Blood 1990; 76: 1558-1563
18 Sohngen W, Mickelson JK, Simpson PJ, Lucchesi BR. Recombinant single-chain urokinase-type plasminogen activator (rscu-PA) induces thrombolysis and systemic fibrinolysis in a canine model of coronary artery thrombosis. Thromb Res 1988; 51: 0063-0074