| Literature DB >> 26863047 |
B E Hjelm1, C Grunseich2, G Gowing1, P Avalos1, J Tian1, B C Shelley1, M Mooney2, K Narwani1, Y Shi2, C N Svendsen1, J H Wolfe3,4, K H Fischbeck2, T M Pierson1,5.
Abstract
Numerous gene and cell therapy strategies are being developed for the treatment of neurodegenerative disorders. Many of these strategies use constitutive expression of therapeutic transgenic proteins, and although functional in animal models of disease, this method is less likely to provide adequate flexibility for delivering therapy to humans. Ligand-inducible gene expression systems may be more appropriate for these conditions, especially within the central nervous system (CNS). Mifepristone's ability to cross the blood-brain barrier makes it an especially attractive ligand for this purpose. We describe the production of a mifepristone-inducible vector system for regulated expression of transgenes within the CNS. Our inducible system used a lentivirus-based vector platform for the ex vivo production of mifepristone-inducible murine neural progenitor cells that express our transgenes of interest. These cells were processed through a series of selection steps to ensure that the cells exhibited appropriate transgene expression in a dose-dependent and temporally controlled manner with minimal background activity. Inducible cells were then transplanted into the brains of rodents, where they exhibited appropriate mifepristone-inducible expression. These studies detail a strategy for regulated expression in the CNS for use in the development of safe and efficient gene therapy for neurological disorders.Entities:
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Year: 2016 PMID: 26863047 PMCID: PMC4976764 DOI: 10.1038/gt.2016.13
Source DB: PubMed Journal: Gene Ther ISSN: 0969-7128 Impact factor: 5.250