Thromb Haemost 2001; 86(03): 909-913
DOI: 10.1055/s-0037-1616149
Review Articles
Schattauer GmbH

Selective and Sustained Inhibition of Surface-bound Thrombin Activity by Intimatan/Heparin Cofactor II and Its Relevance to Assessing Systemic Anticoagulation In Vivo, Ex Vivo and In Vitro

Michael R. Buchanan
1   Department of Pathology and Molecular Medicine, McMaster University, Hamilton
,
Glenn A. Maclean*
1   Department of Pathology and Molecular Medicine, McMaster University, Hamilton
,
Stephanie J. Brister
2   University of Toronto, The Toronto Hospital, Cardiovascular Surgery, Toronto, Ontario, Canada
› Author Affiliations
Further Information

Publication History

Received 27 March 2000

Accepted after resubmission 11 January 2001

Publication Date:
14 December 2017 (online)

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Summary

We compare the relative activities of surface-bound and fluid-phase thrombin and their inhibition by heparin and Intimatan, a novel heparin cofactor II (HCII) agonist. In vitro, we compared the observed amidolytic activities of fluid-phase and surface-bound thrombin with the expected activities based upon 125I-specific activity. In vivo, we compared the inhibitory effects of heparin and Intimatan on thrombin activity bound to injured vessel walls. In vitro, the correlations between observed and expected activities of fluid-phase and surface-bound thrombin, were: r = 0.9974, p < 0.001; and r = 0.9678, p < 0.001; respectively. In vivo, injured vessel wall surface-bound thrombin activity persisted for > 24 h. This activity was not inhibited by heparin, but was inhibited by Intimatan, p < 0.001.

We conclude that surface-bound thrombin is as active as fluid-phase thrombin and remains protected from inhibition by heparin, thereby contributing to vessel wall thrombogenicity following injury. In contrast, surface-bound thrombin is inhibited by Intimatan, thereby effectively decreasing vessel wall thrombogenicity following injury in vivo.

* Current address: Mr. G. A. Maclean, Department of Pathology, Queens University, Kingston, Ontario.