Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect

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Title:	Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect
Author(s):	Mathijssen, N.C.J. ; Masereeuw, R. ; Holme, P.A.; Kraaij, M.G.J. van ; Laros, B.A.P. ; Peyvandi, F.; Heerde, W.L. van
Publication year:	2013
Source:	Thrombosis Research, vol. 132, iss. 2, (2013), pp. 256-262
ISSN:	0049-3848
DOI:	https://doi.org/10.1016/j.thromres.2013.05.027
Publication type:	Article / Letter to editor
Please use this identifier to cite or link to this item : https://hdl.handle.net/2066/142204
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Subject:	N4i 2: Invasive mycoses and compromised host ONCOL 3: Translational research NCEBP 14: Cardiovascular diseases NCMLS 5: Membrane transport and intracellular motility IGMD 9: Renal disorder
Organization:	CHL Pharmacology-Toxicology Haematology Laboratory of Hematology
Journal title:	Thrombosis Research
Volume:	vol. 132
Issue:	iss. 2
Page start:	p. 256
Page end:	p. 262
Abstract:	INTRODUCTION: Prophylaxis with plasma-derived or recombinant activated factor VII is beneficial in severe factor VII deficiency. To understand why prophylactic treatment with both products is efficacious, we conducted a pharmacokinetic study. MATERIALS AND METHODS: Ten factor VII deficient patients were treated with either recombinant activated (20mug/kg) or plasma-derived (25IU/kg) factor VII in a cross-over design. Pharmacokinetic parameters were analyzed through activated factor VII activity, factor VII clotting activity, and factor VII antigen levels on depicted time points. RESULTS: Factor VII activity half-lifes, determined by non-compartmental and one-compartmental analysis (results in brackets), were shorter for recombinant activated (1.4h; 0.7h) than for plasma-derived factor VII (6.8h; 3.2h); both recombinant activated (5.1h; 2.1h and plasma-derived factor VII (5.8h; 3.2h) resulted in longer half-lives of factor VII antigen. Activated factor VII half-lives (based on activated factor VII activity levels) were significantly higher compared to factor VII clotting activity (1.6h; 0.9h). Volumes of distribution were significantly higher for activated factor VII (236ml/kg; 175ml/kg, measured by activated factor VII) as compared to plasma-derived factor VII (206ml/kg; 64ml/kg, measured by factor FVII activity), suggesting a plasma- and extracellular fluid distribution for recombinant activated factor VII. CONCLUSIONS: Recombinant activated factor VII showed significantly shorter half-lifes than plasma-derived factor VII. Volumes of distribution were significantly higher for treatment with recombinant activated factor VII. The longer half-life for plasma-derived factor VII, compared to recombinant activated factor VII, and the increased volume of distribution for recombinant activated factor VII, compared to plasma-derived factor VII may further elucidate the beneficial effect of prophylactic treatment of both products.