The von Willebrand factor A-1 domain binding aptamer BT200 elevates plasma levels of von Willebrand factor and factor VIII: a first-in-human trial |
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| Authors: | Katarina D. Kovacevic,Jü rgen Grafeneder,Christian Schö rgenhofer,Georg Gelbenegger,Gloria Gager,Christa Firbas,Peter Quehenberger,Petra Jilma-Stohlawetz,Andrea Bileck,Shuhao Zhu,James C. Gilbert,Martin Beliveau,Bernd Jilma,Ulla Derhaschnig |
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| Affiliation: | 1.Department of Clinical Pharmacology, Medical University of Vienna, Vienna, Austria;2.Clinical Institute of Laboratory Medicine, Medical University of Vienna, Vienna, Austria;3.Joint Metabolome Facility, University of Vienna & Medical University of Vienna, Vienna, Austria;4.Guardian Therapeutics Inc., Lexington, KY, USA;5.Certara, Montreal, Quebec, Canada |
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| Abstract: | von Willebrand factor (VWF) and factor VIII (FVIII) circulate in a noncovalent complex in blood and promote primary hemostasis and clotting, respectively. A new VWF A1-domain binding aptamer, BT200, demonstrated good subcutaneous bioavailability and a long half-life in non-human primates. This first-in-human, randomized, placebo-controlled, double-blind trial tested the hypothesis that BT200 is well tolerated and has favorable pharmacokinetic and pharmacodynamic effects in 112 volunteers. Participants received one of the following: a single ascending dose of BT200 (0.18-48 mg) subcutaneously, an intravenous dose, BT200 with concomitant desmopressin or multiple doses. Pharmacokinetics were characterized, and the pharmacodynamic effects were measured by VWF levels, FVIII clotting activity, ristocetin-induced aggregation, platelet function under high shear rates, and thrombin generation. The mean half-lives ranged from 7-12 days and subcutaneous bioavailability increased dose-dependently exceeding 55% for doses of 6-48 mg. By blocking free A1 domains, BT200 dose-dependently decreased ristocetin-induced aggregation, and prolonged collagen-adenosine diphosphate and shear-induced platelet plug formation times. However, BT200 also increased VWF antigen and FVIII levels 4-fold (P<0.001), without increasing VWF propeptide levels, indicating decreased VWF/FVIII clearance. This, in turn, increased thrombin generation and accelerated clotting. Desmopressin-induced VWF/FVIII release had additive effects on a background of BT200. Tolerability and safety were generally good, but exaggerated pharmacology was seen at saturating doses. This trial identified a novel mechanism of action for BT200: BT200 dose-dependently increases VWF/FVIII by prolonging half-life at doses well below those which inhibit VWF-mediated platelet function. This novel property can be exploited therapeutically to enhance hemostasis in congenital bleeding disorders. |
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