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Paris Margaritis, Valder R. Arruda, Majed Aljamali, Rodney M. Camire, Alexander Schlachterman, Katherine A. High
J Clin Invest. 2004;
113(7):1025
doi:10.1172/JCI20106
Abstract |
Full text
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H
emophilia is a bleeding disorder caused by mutations in the genes encoding coagulation Factor VIII (FVIII) or FIX. Current treatment is through intravenous infusion of the missing protein. The major complication of treatment is the development of neutralizing Ab’s to the clotting factor. Infusion of recombinant activated human Factor VII (rhFVIIa), driving procoagulant reactions independently of human FVIII (hFVIII) or hFIX, has been successful in such patients and could in theory provide hemostasis in all hemophilia patients. However, its high cost and short half-life have limited its use. Here, we report a novel treatment strategy with a recombinant adeno-associated virus vector delivering a modified FVII transgene that can be intracellularly processed and secreted as activated FVII (FVIIa). We show long-term expression, as well as phenotypic correction of hemophilia B mice following gene transfer of the murine FVIIa homolog, with no evidence of thrombotic complications at these doses. These data hold promise for a potential treatment for hemophilia and other bleeding disorders.
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Total citations by year
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Citations to this article
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(13)
| Title and authors |
Publication |
Year |
Expression of Recombinant Human Coagulation Factor VII by the Lizard Leishmania Expression System
Sina Mirzaahmadi, Golnaz Asaadi-Tehrani, Mojgan Bandehpour, Nooshin Davoudi, Leila Tahmasbi, Nahid Hosseinzadeh, Hasan Mirzahoseini, Kazem Parivar, Bahram Kazemi
|
Journal of Biomedicine and Biotechnology
|
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 |
Delivering multiple gene products in the brain from a single adeno-associated virus vector.
S B Foti, R J Samulski, T J McCown
|
Gene Ther
|
2009 |
Successful treatment of canine hemophilia by continuous expression of canine FVIIa.
Paris Margaritis, Elise Roy, Majed N Aljamali, Harre D Downey, Urs Giger, Shangzhen Zhou, Elizabeth Merricks, Aaron Dillow, Mirella Ezban, Timothy C Nichols, Katherine A High
|
Blood
|
2009 |
A viable mouse model of factor X deficiency provides evidence for maternal transfer of factor X.
S J Tai, R W Herzog, P Margaritis, V R Arruda, K Chu, J A Golden, P A Labosky, K A High
|
J. Thromb. Haemost.
|
2008 |
In vivo models of haemophilia – status on current knowledge of clinical phenotypes and therapeutic interventions
K. ØVLISEN, A. T. KRISTENSEN, M. TRANHOLM
|
Haemophilia
|
2008 |
Phenotypic Correction of Hemophilia A by Ectopic Expression of Activated Factor VII in Platelets
Tsukasa Ohmori, Akira Ishiwata, Yuji Kashiwakura, Seiji Madoiwa, Katsuyuki Mitomo, Hidenori Suzuki, Mamoru Hasegawa, Jun Mimuro, Yoichi Sakata
|
Mol Ther
|
2008 |
A guide to murine coagulation factor structure, function, assays, and genetic alterations
J. J. EMEIS, M. JIROUSKOVA, E.-M. MUCHITSCH, A. S. SHET, S. S. SMYTH, G. J. JOHNSON
|
Journal of Thrombosis and Haemostasis
|
2007 |
Stem cell–derived erythroid cells mediate long-term systemic protein delivery
Alex H Chang, Matthias T Stephan, Michel Sadelain
|
Nat Biotechnol
|
2006 |
Gene transfer for hemophilia: can therapeutic efficacy in large animals be safely translated to patients?
K. HIGH
|
Journal of Thrombosis and Haemostasis
|
2005 |
|