Abstract

Coagulation Factor (F) VIII is mostly made in the liver. Its deficiency is the mot common inherited severe bleeding disorder. Present treatment involves intravenous infusions of FVIII. This therapy has drawbacks, and while efforts are underway to develop a form of somatic gene therapy, successful programs have yet to be achieved. The objective of this application is to develop an alternative approach, ectopically expressing FVIII in platelets. Preliminary studies show that transgenic mice expressing human (hu) FVIII driven by the murine (mu) Platelet Factor 4 (PF4) promoter can ameliorate the bleeding diathesis in FVIII-deficient (FVIII) mice.
Specific aims are as follows: (1) Complete the analysis of the initial founder lines expressing huFVIII. These studies will further document the platelet-specific nature of the huFVIII, document its level of expression, and more fully define the degree of correction of the FVII/I- phenotype. (2) Improve the efficiency of the construct for huFVIII expression in megakaryocytes.
This aim will try several construct variations to obtain higher levels of huFVIII expression platelets, and correlate levels of expression with phenotypic improvement. (3) Assess the efficacy of megakaryocyte expression of huFVIII in the context of a viral transfer system in a murine model. These studies will further test our model of whether huFVIII expression in hematopoietic stem cells is a viable approach for the treatment of Hemophilia A using retroviral constructs. These vectors will be tested on FVIII-mice recipients and the bleeding diathesis, the level of platelet huFVIII expression and the duration of correction will be determined. These studies will provide a useful pre-clinical evaluation of the proposed approach to genetic therapy for FVIII deficiency. We believe that ectopically expressed FVIII will be a viable way to treat FVIII deficiency, resulting in a longer FVIII half-life and in the delivery of FVIII in a concentrated fashion at the site of injury. We also believe that this approach may provide a source of """"""""protected"""""""" FVIII that would be useful in patients with inhibitors. Finally, we believe that this approach may serve as a model for gene therapy to deliver other proteins in concentrated fashion to a site of injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
1P01HL064190-01
Application #
6313240
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
2000-02-22
Project End
2004-11-30
Budget Start
2000-02-22
Budget End
2000-11-30
Support Year
1
Fiscal Year
2000
Total Cost
$187,524
Indirect Cost

  Institution

Name
Children's Hospital of Philadelphia
Department
Type
DUNS #
073757627
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

French, Robert A; Samelson-Jones, Benjamin J; Niemeyer, Glenn P et al. (2018) Complete correction of hemophilia B phenotype by FIX-Padua skeletal muscle gene therapy in an inhibitor-prone dog model. Blood Adv 2:505-508
George, Lindsey A; Sullivan, Spencer K; Giermasz, Adam et al. (2017) Hemophilia B Gene Therapy with a High-Specific-Activity Factor IX Variant. N Engl J Med 377:2215-2227
Gollomp, Kandace; Lambert, Michele P; Poncz, Mortimer (2017) Current status of blood 'pharming': megakaryoctye transfusions as a source of platelets. Curr Opin Hematol 24:565-571
Sim, Xiuli; Poncz, Mortimer; Gadue, Paul et al. (2016) Understanding platelet generation from megakaryocytes: implications for in vitro-derived platelets. Blood 127:1227-33
Marcos-Contreras, Oscar A; Smith, Shannon M; Bellinger, Dwight A et al. (2016) Sustained correction of FVII deficiency in dogs using AAV-mediated expression of zymogen FVII. Blood 127:565-71
Arruda, V R; Samelson-Jones, B J (2016) Gene therapy for immune tolerance induction in hemophilia with inhibitors. J Thromb Haemost 14:1121-34
High, Katherine A; Anguela, Xavier M (2016) Adeno-associated viral vectors for the treatment of hemophilia. Hum Mol Genet 25:R36-41
Siner, Joshua I; Samelson-Jones, Benjamin J; Crudele, Julie M et al. (2016) Circumventing furin enhances factor VIII biological activity and ameliorates bleeding phenotypes in hemophilia models. JCI Insight 1:e89371
Zhang, Nanyan; Zhi, Huiying; Curtis, Brian R et al. (2016) CRISPR/Cas9-mediated conversion of human platelet alloantigen allotypes. Blood 127:675-80
Antony-Debré, Iléana; Manchev, Vladimir T; Balayn, Nathalie et al. (2015) Level of RUNX1 activity is critical for leukemic predisposition but not for thrombocytopenia. Blood 125:930-40

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