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Efficient in vivo gene delivery using modified Tat peptide with cationic lipids
Authors:Seiichi Yamano  Jisen Dai  Shigeru Hanatani  Ken Haku  Takuto Yamanaka  Mika Ishioka  Tadahiro Takayama  Amr M Moursi
Institution:1. Department of Prosthodontics, New York University College of Dentistry, 345 East 24th Street, 4W, New York, NY, 10010, USA
2. Department of Pediatric Dentistry, New York University College of Dentistry, New York, NY, 10010, USA
Abstract:A combination of modified HIV-1 Tat (mTat) peptide and cationic lipids, FuGENE HD (FH), dramatically enhanced transfection efficiency across a range of cell lines when compared to mTat or FH alone (Biomaterials 35:1705–1715 2014). The efficiency of this Tat peptide combination was significantly higher than many commercial non-viral vectors. In this present study, we tested the feasibility of this non-viral vector, mTat/FH, in vivo using plasmid DNA encoding a luciferase gene. The results of the in vivo studies showed that animals administered mTat/FH/DNA intramuscularly had significantly higher and longer luciferase expression (≈7 months) than those with mTat/DNA, FH/DNA, or DNA alone. Histological evaluation showed little immune response in the muscles, livers, and kidneys of mice administered with the mTat/FH. The combination of mTat with FH could significantly improve transfection efficiency, expanding the potential use of non-viral gene vectors in vivo.
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