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

Natascha C J Mathijssen; R. Masereeuw; Pal Andre Holme; Marian G J van Kraaij; Britta A P Laros-van Gorkom; Flora Peyvandi; Waander L van Heerde

doi:10.1016/j.thromres.2013.05.027

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

Natascha C J Mathijssen, R. Masereeuw, Pal Andre Holme, Marian G J van Kraaij, Britta A P Laros-van Gorkom, Flora Peyvandi, Waander L van Heerde

Pharmacology

Research output: Contribution to journal › Article › Academic › peer-review

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 (20 μg/kg) or plasma-derived (25 IU/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 (236 ml/kg; 175 ml/kg, measured by activated factor VII) as compared to plasma-derived factor VII (206 ml/kg; 64 ml/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.

Original language	English
Pages (from-to)	256-62
Number of pages	7
Journal	Thrombosis Research
Volume	132
Issue number	2
DOIs	https://doi.org/10.1016/j.thromres.2013.05.027
Publication status	Published - Aug 2013

Bibliographical note

Keywords

Adult
Blood Coagulation Tests
Cross-Over Studies
Factor VII Deficiency
Factor VIIa
Female
Half-Life
Hemostasis
Humans
Male
Middle Aged
Recombinant Proteins
Young Adult

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10.1016/j.thromres.2013.05.027

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Mathijssen, N. C. J., Masereeuw, R., Holme, P. A., van Kraaij, M. G. J., Laros-van Gorkom, B. A. P., Peyvandi, F., & van Heerde, W. L. (2013). Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect. Thrombosis Research, 132(2), 256-62. https://doi.org/10.1016/j.thromres.2013.05.027

@article{a9887e9a0b0940af9d9bd7eeee1d701b,

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",

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 (20 μg/kg) or plasma-derived (25 IU/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 (236 ml/kg; 175 ml/kg, measured by activated factor VII) as compared to plasma-derived factor VII (206 ml/kg; 64 ml/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.",

keywords = "Adult, Blood Coagulation Tests, Cross-Over Studies, Factor VII Deficiency, Factor VIIa, Female, Half-Life, Hemostasis, Humans, Male, Middle Aged, Recombinant Proteins, Young Adult",

author = "Mathijssen, {Natascha C J} and R. Masereeuw and Holme, {Pal Andre} and {van Kraaij}, {Marian G J} and {Laros-van Gorkom}, {Britta A P} and Flora Peyvandi and {van Heerde}, {Waander L}",

year = "2013",

month = aug,

doi = "10.1016/j.thromres.2013.05.027",

language = "English",

volume = "132",

pages = "256--62",

journal = "Thrombosis Research",

issn = "0049-3848",

publisher = "Elsevier Ltd",

number = "2",

}

Mathijssen, NCJ, Masereeuw, R, Holme, PA, van Kraaij, MGJ, Laros-van Gorkom, BAP, Peyvandi, F & van Heerde, WL 2013, 'Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect', Thrombosis Research, vol. 132, no. 2, pp. 256-62. https://doi.org/10.1016/j.thromres.2013.05.027

Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect. / Mathijssen, Natascha C J; Masereeuw, R.; Holme, Pal Andre et al.
In: Thrombosis Research, Vol. 132, No. 2, 08.2013, p. 256-62.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - Increased volume of distribution for recombinant activated factor VII and longer plasma-derived factor VII half-life may explain their long lasting prophylactic effect

AU - Mathijssen, Natascha C J

AU - Masereeuw, R.

AU - Holme, Pal Andre

AU - van Kraaij, Marian G J

AU - Laros-van Gorkom, Britta A P

AU - Peyvandi, Flora

AU - van Heerde, Waander L

PY - 2013/8

Y1 - 2013/8

N2 - 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 (20 μg/kg) or plasma-derived (25 IU/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 (236 ml/kg; 175 ml/kg, measured by activated factor VII) as compared to plasma-derived factor VII (206 ml/kg; 64 ml/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.

AB - 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 (20 μg/kg) or plasma-derived (25 IU/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 (236 ml/kg; 175 ml/kg, measured by activated factor VII) as compared to plasma-derived factor VII (206 ml/kg; 64 ml/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.

KW - Adult

KW - Blood Coagulation Tests

KW - Cross-Over Studies

KW - Factor VII Deficiency

KW - Factor VIIa

KW - Female

KW - Half-Life

KW - Hemostasis

KW - Humans

KW - Male

KW - Middle Aged

KW - Recombinant Proteins

KW - Young Adult

U2 - 10.1016/j.thromres.2013.05.027

DO - 10.1016/j.thromres.2013.05.027

M3 - Article

C2 - 23834817

SN - 0049-3848

VL - 132

SP - 256

EP - 262

JO - Thrombosis Research

JF - Thrombosis Research

IS - 2

ER -

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

Abstract

Bibliographical note

Keywords

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