PUBLICATION
CD14+/CD31+ Monocytes Expanded by UM171 Correct Hemophilia A in Zebrafish upon Lentiviral Gene Transfer of Factor VIII
- Authors
- Elnaggar, M., Al-Mohannadi, A., Hasan, W., Abdelrahman, D., Al-Kubaisi, M.J., Pavlovski, I., Gentlcore, G., Sathappan, A., Kizhakayil, D., Ali, A.I., Mohan, S., Olagunju, D., Cugno, C., Grivel, J.C., Borsotti, C., Follenzi, A., Da'as, S., Deola, S.
- ID
- ZDB-PUB-221209-9
- Date
- 2022
- Source
- Blood advances 7(5): 697-711 (Journal)
- Registered Authors
- Abdelrahman, Dou, Da'as, Sahar
- Keywords
- none
- MeSH Terms
-
- Animals
- Factor VIII/genetics
- Hematopoietic Stem Cells/metabolism
- Hemophilia A*/therapy
- Hemostatics*
- Humans
- Monocytes/metabolism
- Zebrafish/metabolism
- PubMed
- 36477543 Full text @ Blood Adv
Citation
Elnaggar, M., Al-Mohannadi, A., Hasan, W., Abdelrahman, D., Al-Kubaisi, M.J., Pavlovski, I., Gentlcore, G., Sathappan, A., Kizhakayil, D., Ali, A.I., Mohan, S., Olagunju, D., Cugno, C., Grivel, J.C., Borsotti, C., Follenzi, A., Da'as, S., Deola, S. (2022) CD14+/CD31+ Monocytes Expanded by UM171 Correct Hemophilia A in Zebrafish upon Lentiviral Gene Transfer of Factor VIII. Blood advances. 7(5):697-711.
Abstract
Emerging gene therapy (GT) clinical trials test the correction of hemophilia A (HA) by replacing factor VIII (FVIII) in autologous hematopoietic stem cells (HSC). Although it is known that platelets, monocyte/macrophages, and mesenchymal stromal cells can secrete transgenic FVIII, a systematic examination of blood lineages as extrahepatic sources of FVIII has not yet been performed. In this study, we sought to provide a comprehensive map of native and lentivirus-based transgenic FVIII production from HSC stage to mature blood cells, through a flow cytometry analysis. In addition, we generated a model of transient HA in zebrafish based on antisense RNA, to assess the corrective potential of the FVIII-transduced HSCs. We discovered that FVIII production begins at the CD34+ progenitor stage after cytokine stimulation in culture. Among all mature white blood cells, monocytes are the largest producers of native FVIII, and can maintain protein overexpression during differentiation from HSCs, when transduced by a FVIII lentiviral vector. Moreover, the addition of the HSC self-renewal agonist UM171 to CD34+ cells during transduction expanded a subpopulation of CD14+/CD31+ monocytes with excellent ability to carry the FVIII transgene, allowing the correction of HA phenotype in zebrafish. Finally, the HA zebrafish model showed that f8 RNA is predominantly localized in the hematopoietic system at the larval stage, which indicates a potential contributory role of FVIII in hematopoiesis that warrants further investigation. We believe that our study may be of broad interest to hematologists and researchers striving to advance knowledge and permanent treatments for patients with HA.
Genes / Markers
Expression
Phenotype
Mutations / Transgenics
Human Disease / Model
Sequence Targeting Reagents
Fish
Orthology
Engineered Foreign Genes
Mapping