Literature DB >> 17227834

Relative antithrombotic and antihemostatic effects of protein C activator versus low-molecular-weight heparin in primates.

András Gruber1, Ulla M Marzec, Leslie Bush, Enrico Di Cera, José A Fernández, Michelle A Berny, Erik I Tucker, Owen J T McCarty, John H Griffin, Stephen R Hanson.   

Abstract

The anticoagulant and anti-inflammatory enzyme, activated protein C (APC), naturally controls thrombosis without affecting hemostasis. We therefore evaluated whether the integrity of primary hemostasis was preserved during limited pharmacological antithrombotic protein C activator (PCA) treatment in baboons. The double-mutant thrombin (Trp215Ala/Glu217Ala) with less than 1% procoagulant activity was used as a relatively selective PCA and compared with systemic anticoagulation by APC and low-molecular-weight heparin (LMWH) at doses that inhibited fibrin deposition on thrombogenic segments of arteriovenous shunts. As expected, both systemic anticoagulants, APC (0.028 or 0.222 mg/kg for 70 minutes) and LMWH (0.325 to 2.6 mg/kg for 70 minutes), were antithrombotic and prolonged the template bleeding time. In contrast, PCA at doses (0.0021 to 0.0083 mg/kg for 70 minutes) that had antithrombotic effects comparable with LMWH did not demonstrably impair primary hemostasis. PCA bound to platelets and leukocytes, and accumulated in thrombi. APC infusion at higher circulating APC levels was less antithrombotic than PCA infusion at lower circulating APC levels. The observed dissociation of antithrombotic and antihemostatic effects during PCA infusion thus appeared to emulate the physiological regulation of intravascular blood coagulation (thrombosis) by the endogenous protein C system. Our data suggest that limited pharmacological protein C activation might exhibit considerable thrombosis specificity.

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Year:  2007        PMID: 17227834      PMCID: PMC1874578          DOI: 10.1182/blood-2006-07-035147

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  55 in total

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Authors:  S T Grey; W W Hancock
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2.  A recombinant hirudin (IK-HIR02) in healthy volunteers. I. Effects on coagulation parameters and bleeding time.

Authors:  J F Schenk; E Glusa; P Radziwon; A Butti; F Markwardt; H K Breddin
Journal:  Haemostasis       Date:  1996 May-Jun

3.  Importance of platelets in neutrophil adhesion and vasoconstriction after deep carotid arterial injury by angioplasty in pigs.

Authors:  Y Merhi; P Provost; R Guidoin; J G Latour
Journal:  Arterioscler Thromb Vasc Biol       Date:  1997-06       Impact factor: 8.311

4.  Protein engineering thrombin for optimal specificity and potency of anticoagulant activity in vivo.

Authors:  M Tsiang; L R Paborsky; W X Li; A K Jain; C T Mao; K E Dunn; D W Lee; S Y Matsumura; M D Matteucci; S E Coutré; L L Leung; C S Gibbs
Journal:  Biochemistry       Date:  1996-12-24       Impact factor: 3.162

5.  Functional mapping of the surface residues of human thrombin.

Authors:  M Tsiang; A K Jain; K E Dunn; M E Rojas; L L Leung; C S Gibbs
Journal:  J Biol Chem       Date:  1995-07-14       Impact factor: 5.157

6.  Conversion of thrombin into an anticoagulant by protein engineering.

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Journal:  Nature       Date:  1995-11-23       Impact factor: 49.962

7.  Antithrombotic effects of thrombin-induced activation of endogenous protein C in primates.

Authors:  S R Hanson; J H Griffin; L A Harker; A B Kelly; C T Esmon; A Gruber
Journal:  J Clin Invest       Date:  1993-10       Impact factor: 14.808

8.  New class of heparin derivatives with a potent antithrombotic effect and a very limited hemorrhagic activity.

Authors:  C Doutremepuich; F Azougagh Oualane; F Doutremepuich; J Fareed
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9.  Benefit of adding low molecular weight heparin to the conventional treatment of stable angina pectoris. A double-blind, randomized, placebo-controlled trial.

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10.  The haemorrhagic effect of low molecular weight heparins, dermatan sulphate and hirudin.

Authors:  S E Matthíasson; B Lindblad; U Stjernquist; D Bergqvist
Journal:  Haemostasis       Date:  1995 Sep-Oct
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  26 in total

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Authors:  D C Wood; L A Pelc; N Pozzi; M Wallisch; N G Verbout; E I Tucker; A Gruber; E Di Cera
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2.  Thrombin mutant W215A/E217A treatment improves neurological outcome and reduces cerebral infarct size in a mouse model of ischemic stroke.

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3.  Structural identification of the pathway of long-range communication in an allosteric enzyme.

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4.  Stabilization of the E* form turns thrombin into an anticoagulant.

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5.  Mechanism of the anticoagulant activity of thrombin mutant W215A/E217A.

Authors:  Prafull S Gandhi; Michael J Page; Zhiwei Chen; Leslie Bush-Pelc; Enrico Di Cera
Journal:  J Biol Chem       Date:  2009-07-08       Impact factor: 5.157

6.  Redesigning allosteric activation in an enzyme.

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Review 7.  Allostery in trypsin-like proteases suggests new therapeutic strategies.

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8.  Safety and antithrombotic efficacy of moderate platelet count reduction by thrombopoietin inhibition in primates.

Authors:  Erik I Tucker; Ulla M Marzec; Michelle A Berny; Sawan Hurst; Stuart Bunting; Owen J T McCarty; András Gruber; Stephen R Hanson
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9.  Thrombin mutant W215A/E217A treatment improves neurological outcome and attenuates central nervous system damage in experimental autoimmune encephalomyelitis.

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Review 10.  Activated protein C in sepsis: the promise of nonanticoagulant activated protein C.

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Journal:  Curr Opin Hematol       Date:  2008-09       Impact factor: 3.284

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