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Thromb Haemost 1994; 71(05): 576-580
DOI: 10.1055/s-0038-1642485
Review Article
Schattauer GmbH Stuttgart

Dermatan Sulfate Is a More Potent Inhibitor of Clot-bound Thrombin than Unfractionated and Low Molecular Weight Heparins

P Bendayan
1   The Laboratoire d’Hémostase, Centre de Transfusion and Service d’Angiologie, Hô;pital de Rangueil, Toulouse, France
1   Service d’Angiologie, Hôpital de Rangueil, Toulouse, France
,
H Boccalon
1   Service d’Angiologie, Hôpital de Rangueil, Toulouse, France
,
D Dupouy
1   The Laboratoire d’Hémostase, Centre de Transfusion and Service d’Angiologie, Hô;pital de Rangueil, Toulouse, France
,
B Boneu
1   The Laboratoire d’Hémostase, Centre de Transfusion and Service d’Angiologie, Hô;pital de Rangueil, Toulouse, France
› Author Affiliations
Further Information

Publication History

Received 21 February 1993

Accepted after revision 25 January 1994

Publication Date:
06 July 2018 (online)

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Summary

Clot-bound thrombin proteolyses fibrinogen and amplifies the coagulation cascade at its close vicinity, thereby ensuring the growth of fibrin-rich thrombus. The present study compares the ability of various glycosaminoglycans (GAGs) to inhibit these 2 properties. Unfractionated heparin (UH), 3 low molecular weight heparins (LMWHs) with increasing antifactor Xa/antifactor Ha ratio, the synthetic pentasaccharide (PS), devoid of antifactor Ha activity, and dermatan sulfate (DS), a catalyst of thrombin inhibition by heparin cofactor II, were selected on the basis of their different properties. Proteolysis of fibrinogen by clot-bound thrombin was evaluated by measuring fibrinopeptide A (FPA) generation after an incubation of standardized washed clots in plasma for 120 min in absence or in presence of increasing concentrations of heparins or of DS. The results were compared to those obtained when free a-thrombin (0.4 nM) was added to plasma in the same experimental conditions. On the basis of equivalent antithrombin units, UH and LMWHs gave identical results. To inhibit by 70% fibrinogen proteolysis induced by clot-bound thrombin (IC 70), 5- to 9-fold higher concentrations of UH or of LMWHs were required in comparison with those required to inhibit free thrombin. For DS, only a 1.3 times higher concentration was required. PS (final concentration 1 anti Xa U • ml-1) was devoid of any inhibitory effect. The amplification of the coagulation cascade induced by dot-bound thrombin was evaluated by measuring the shortening of whole blood clotting time (WBCT) resulting from the incubation of washed clots in native blood. In absence of GAG, clot-bound thrombin reduced WBCT from 18 ± 2 min to 9 ± 1 min. Each GAG prolonged WBCT in a dose-dependent manner but these prolongations were smaller in presence of washed clots. The most potent agent to suppress the shortening of WBCT was DS. LMWH and UH were less effective and PS (final concentration 1 anti Xa U/ml) was almost ineffective. Therefore, in these in vitro experiments, DS is a more potent inhibitor of clot-bound thrombin than heparin. Whether or not these observations are relevant for the treatment of established deep-vein thrombosis requires comparative clinical studies.

 

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