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Majed N. Aljamali, Paris Margaritis, Alexander Schlachterman, Shing Jen Tai, Elise Roy, Ralph Bunte, Rodney M. Camire, Katherine A. High
J Clin Invest. 2008;
118(5):1825
doi:10.1172/JCI32878
Abstract |
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ntravenous infusion of recombinant human activated Factor VII (FVIIa) has been used for over a decade in the successful management of bleeding episodes in patients with inhibitory antibodies to Factor VIII or Factor IX. Previously, we showed that expression of murine FVIIa (mFVIIa) from an adeno-associated viral (AAV) vector corrected abnormal hemostatic parameters in hemophilia B mice. To pursue this as a therapeutic approach, we sought to define safe and effective levels of FVIIa for continuous expression. In mice transgenic for mFVIIa or injected with AAV-mFVIIa, we analyzed survival, expression levels, in vitro and in vivo coagulation tests, and histopathology for up to 16 months after birth/mFVIIa expression. We found that continuous expression of mFVIIa at levels at or below 1.5 μg/ml was safe, effective, and compatible with a normal lifespan. However, expression levels of 2 μg/ml or higher were associated with thrombosis and early mortality, with pathologic findings in the heart and lungs that were rescued in a low–factor X (low-FX) mouse background, suggesting a FX-mediated effect. The findings from these mouse models of continuous FVIIa expression have implications for the development of a safe gene transfer approach for hemophilia and are consistent with the possibility of thromboembolic risk of continuously elevated FVIIa levels.
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Citations to this article
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(16)
| Title and authors |
Publication |
Year |
Progress in Molecular Biology and Translational Science
Denise E. Sabatino, Timothy C. Nichols, Elizabeth Merricks, Dwight A. Bellinger, Roland W. Herzog, Paul E. Monahan
|
Animal Models of Molecular Pathology
|
2012 |
Pharmacokinetics, pharmacodynamics and safety of recombinant canine FVIIa in a study dosing one haemophilia A and one haemostatically normal dog
T. KNUDSEN, A. T. KRISTENSEN, T. C. NICHOLS, H. AGERSØ, A. L. JENSEN, M. KJALKE, M. EZBAN, M. TRANHOLM
|
Haemophilia
|
2011 |
Catalytic domain modification and viral gene delivery of activated factor VII confers hemostasis at reduced expression levels and vector doses in vivo.
Paris Margaritis, Elise Roy, Armida Faella, Harre D Downey, Lacramioara Ivanciu, Giulia Pavani, Shangzhen Zhou, Ralph M Bunte, Katherine A High
|
Blood
|
2011 |
Gene therapy for haemophilia: a long and winding road
K. A. HIGH
|
Journal of Thrombosis and Haemostasis
|
2011 |
A zymogen-like factor Xa variant corrects the coagulation defect in hemophilia
Lacramioara Ivanciu, Raffaella Toso, Paris Margaritis, Giulia Pavani, Haein Kim, Alexander Schlachterman, Jian-Hua Liu, Valerie Clerin, Debra D Pittman, Rosalind Rose-Miranda
|
Nat Biotechnol
|
2011 |
Characterization of canine coagulation factor VII and its complex formation with tissue factor: canine-human cross-species compatibility
T. KNUDSEN, A. T. KRISTENSEN, B. B. SØRENSEN, O. H. OLSEN, H. R. STENNICKE, L. C. PETERSEN
|
Journal of Thrombosis and Haemostasis
|
2010 |
Long-term expression of canine FVIIa in hemophilic dogs.
Paris Margaritis
|
Thrombosis Research
|
2010 |
A ferric chloride induced arterial injury model used as haemostatic effect model
F. MØLLER, M. TRANHOLM
|
Haemophilia
|
2010 |
Gene therapy in haemophilia - going for cure?
P. MARGARITIS, K. A. HIGH
|
Haemophilia
|
2010 |
Animal models of FVIIa gene expression: their role in the future development of haemophilia treatment
A. OBERGFELL, T. NICHOLS, M. EZBAN
|
Haemophilia
|
2010 |
|