Recombinant GPVI-Fc added to single or dual antiplatelet therapy in vitro prevents plaque-induced platelet thrombus formation

Recombinant GPVI-Fc added to single or dual antiplatelet therapy in vitro prevents plaque-induced platelet thrombus formation

Summary The efficiency of current dual antiplatelet therapy might be further improved by its combination with a glycoprotein (GP) VI-targeting strategy without increasing bleeding. GPVI-Fc, a recombinant dimeric fusion protein binding to plaque collagen and concealing binding sites for platelet GPVI...

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Veröffentlicht in:Thrombosis and haemostasis 2017-08, Vol.117 (8), p.1651-1659
Hauptverfasser: Mojica Muñoz, Ann-Katrin, Jamasbi, Janina, Uhland, Kerstin, Degen, Heidrun, Münch, Götz, Ungerer, Martin, Brandl, Richard, Megens, Remco, Weber, Christian, Lorenz, Reinhard, Siess, Wolfgang
Format: Artikel
Sprache:eng
Schlagworte:
Adenosine - analogs & derivatives
Adenosine - pharmacology
Adenosine - toxicity
Antibodies, Monoclonal - pharmacology
Antibodies, Monoclonal - toxicity
Aspirin - pharmacology
Aspirin - toxicity
Atherosclerosis and Ischaemic Disease
Blood Coagulation - drug effects
Blood Platelets - drug effects
Blood Platelets - metabolism
Drug Therapy, Combination
Glycoproteins - pharmacology
Glycoproteins - toxicity
Hemorrhage - chemically induced
Humans
Immunoglobulin Fab Fragments - pharmacology
Immunoglobulin Fab Fragments - toxicity
Immunoglobulin Fc Fragments - pharmacology
Immunoglobulin Fc Fragments - toxicity
Plaque, Atherosclerotic
Platelet Adhesiveness - drug effects
Platelet Aggregation - drug effects
Platelet Aggregation Inhibitors - pharmacology
Platelet Aggregation Inhibitors - toxicity
Purinergic P2Y Receptor Antagonists - pharmacology
Purinergic P2Y Receptor Antagonists - toxicity
Thrombosis - blood
Thrombosis - pathology
Thrombosis - prevention & control
Time Factors
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Zusammenfassung:Summary The efficiency of current dual antiplatelet therapy might be further improved by its combination with a glycoprotein (GP) VI-targeting strategy without increasing bleeding. GPVI-Fc, a recombinant dimeric fusion protein binding to plaque collagen and concealing binding sites for platelet GPVI, acts as a lesion-focused antiplatelet drug, and does not increase bleeding in vivo. We investigated, whether GPVI-Fc added in vitro on top of acetylsalicylic acid (ASA), the P2Y 12 antagonist ticagrelor, and the fibrinogen receptor antagonist abciximab alone or in combination would increase inhibition of platelet activation by atherosclerotic plaque. Under static conditions, GPVI-Fc inhibited plaque-induced platelet aggregation by 53%, and increased platelet inhibition by ASA (51%) and ticagrelor (64%) to 66% and 80%, respectively. Under arterial flow, GPVI-Fc inhibited plaque-induced platelet aggregation by 57%, and significantly increased platelet inhibition by ASA (28%) and ticagrelor (47%) to about 81% each. The triple combination of GPVI-Fc, ASA and ticagrelor achieved almost complete inhibition of plaque-induced platelet aggregation (93%). GPVI-Fc alone or in combination with ASA or ticagrelor did not increase closure time measured by the platelet function analyzer (PFA)-200. GPVI-Fc added on top of abciximab, a clinically used anti-fibrinogen receptor antibody which blocks platelet aggregation, strongly inhibited total (81%) and stable (89%) platelet adhesion. We conclude that GPVI-Fc added on top of single or dual antiplatelet therapy with ASA and/or a P2Y 12 antagonist is likely to improve anti-atherothrombotic protection without increasing bleeding risk. In contrast, the strong inhibition of platelet adhesion by GPVI-Fc in combination with GPIIb/IIIa inhibitors could be harmful. Note: The review process for this manuscript was fully handled by Gregory Y. H. Lip, Editor in Chief. Supplementary Material to this article is available at www.thrombosis-online.com.
ISSN:0340-6245
2567-689X
DOI:10.1160/TH16-11-0856