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In vivo efficacy of platelet-delivered, high specific activity factor VIII variants.

Abstract
Ectopically expressed, human B-domainless (hB) factor 8 (F8) in platelets improves hemostasis in hemophilia A mice in several injury models. However, in both a cuticular bleeding model and a cremaster laser arteriole/venule injury model, there were limitations to platelet-derived (p) hBF8 efficacy, including increased clot embolization. We now address whether variants of F8 with enhanced activity, inactivation resistant F8 (IR8) and canine (c) BF8, would improve clotting efficacy. In both transgenic and lentiviral murine model approaches, pIR8 expressed at comparable levels to phBF8, but pcBF8 expressed at only approximately 30%. Both variants were more effective than hBF8 in cuticular bleeding and FeCl(3) carotid artery models. However, in the cremaster injury model, only pcBF8 was more effective, markedly decreasing clot embolization. Because inhibitors of F8 are stored in platelet granules and IR8 is not protected by binding to von Willebrand factor, we also tested whether pIR8 was effective in the face of inhibitors and found that pIR8 is protected from the inhibitors. In summary, pF8 variants with high specific activity are more effective in controlling bleeding, but this improved efficacy was inconsistent between bleeding models, perhaps reflecting the underlying mechanism(s) for the increased specific activity of the studied F8 variants.
AuthorsTeshell K Greene, Cheng Wang, Jessica D Hirsch, Li Zhai, Jamie Gewirtz, Michael A Thornton, Hongzhi Z Miao, Steven W Pipe, Randal J Kaufman, Rodney M Camire, Valder R Arruda, M Anna Kowalska, Mortimer Poncz
JournalBlood (Blood) Vol. 116 Issue 26 Pg. 6114-22 (Dec 23 2010) ISSN: 1528-0020 [Electronic] United States
PMID20852129 (Publication Type: Journal Article, Research Support, N.I.H., Extramural)
Chemical References
  • Factor VIII
Topics
  • Animals
  • Blood Platelets (metabolism)
  • Carotid Arteries (metabolism, pathology)
  • Disease Models, Animal
  • Dogs
  • Factor VIII (administration & dosage, genetics, metabolism)
  • Hemophilia A (prevention & control)
  • Hemorrhage (prevention & control)
  • Humans
  • Mice
  • Mice, Transgenic
  • Thrombosis (prevention & control)

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