作者
William J Bowers, Michael A Mastrangelo, Darlene F Howard, Hilary A Southerland, Kathleen A Maguire-Zeiss, Howard J Federoff
发表日期
2006/3/1
期刊
Molecular Therapy
卷号
13
期号
3
页码范围
580-588
出版商
Elsevier
简介
The ability to modify genetically in utero the precursors of neuronal lineage contributing to multiple postmitotic cell types in the adult central nervous system would provide a means to evaluate strategies to ameliorate conditions affecting cellular patterning, metabolism, or survival. The herpes simplex virus (HSV)-derived amplicon, a vector devoid of viral genes and with the largest known payload capacity, normally exists episomally within nuclei of transduced cells, thus precluding conveyance during mitosis. Herein, we modify the Tc1-like Sleeping Beauty (SB) transposon system to create an integrating amplicon vector platform wherein provision of transposase in trans effectively catalyzes integration of a transgenomic segment. Cotransduction with a Rous sarcoma virus promoter-driven β-galactosidase–neomycin (βgeo) fusion flanked by SB terminal repeats (HSVT-βgeo) and a second expressing the SB …
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