Long-Term Antithrombotic Protection by in Vivo Depletion of Platelet Glycoprotein VI in Mice

doi:10.1084/jem.193.4.459

Published online 19 February 2001.

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© The Rockefeller University Press, 0022-1007/2001/2/459/ $5.00
The Journal of Experimental Medicine, Volume 193, Number 4, February 19, 2001 459-470

Original Article

Long-Term Antithrombotic Protection by in Vivo Depletion of Platelet Glycoprotein VI in Mice

Bernhard Nieswandt^a, Valerie Schulte^a, Wolfgang Bergmeier^a, Rabée Mokhtari-Nejad^a, Kirsten Rackebrandt^a, Jean-Pierre Cazenave^b, Philippe Ohlmann^b, Christian Gachet^b, and Hubert Zirngibl^a

^a Department of Molecular Oncology, General Surgery, Witten/Herdecke University, 42117 Wuppertal, Germany
^b Institut National de la Sante et de la Recherche Medicale U.311, Etablissement Français du Sang-Alsace, BP 36, 67065 Strasbourg Cedex, France
Universität Witten/Herdecke, Ferdinand Sauerbruch Klinikum Elberfeld, Haus 10, Arrenbergerstr. 20, D-42117 Wuppertal, Germany.49-202-896-528349-202-896-5280

nieswand{at}klinikum-wuppertal.de

Coronary artery thrombosis is often initiated by abrupt disruptionof the atherosclerotic plaque and activation of platelets onthe subendothelial layers in the disrupted plaque. The extracellularmatrix protein collagen is the most thrombogenic constituentof the subendothelial layer; therefore, a selective inhibitionof the collagen activation pathway in platelets may providestrong antithrombotic protection while preserving other plateletfunctions. Here we demonstrate that treatment of mice with amonoclonal antibody against the activating platelet collagenreceptor glycoprotein VI (GPVI; JAQ1) results in specific depletionof the receptor from circulating platelets and abolished responsesof these cells to collagen and collagen-related peptides (CRPs).JAQ1-treated mice were completely protected for at least 2 wkagainst lethal thromboembolism induced by infusion of a mixtureof collagen (0.8 mg/kg) and epinephrine (60 µg/ml). Thetail bleeding times in JAQ1-treated mice were only moderatelyincreased compared with control mice probably because the treatmentdid not affect platelet activation by other agonists such asadenosine diphosphate or phorbol myristate acetate. These resultssuggest that GPVI might become a target for long-term prophylaxisof ischemic cardiovascular diseases and provide the first evidencethat it is possible to specifically deplete an activating glycoproteinreceptor from circulating platelets in vivo.

Key Words: thrombosis • immunotherapy • collagen • receptor • mouse

Abbreviations used in this paper: ADP, adenosine diphosphate;CRP, collagen-related peptide; ECL, enhanced chemiluminescence;GP, glycoprotein; prp, platelet-rich plasma; RT, room temperature;vWF, von Willebrand factor.

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