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Photochemically enhanced transduction of polymer-complexed adenovirus targeted to the epidermal growth factor receptor

✍ Scribed by Anette Bonsted; Birgit Øvstebø Engesæter; Anders Høgset; Gunhild M. Mælandsmo; Lina Prasmickaite; Christine D'Oliveira; Wim E. Hennink; Jan Hein van Steenis; Kristian Berg


Publisher
John Wiley and Sons
Year
2006
Tongue
English
Weight
233 KB
Volume
8
Category
Article
ISSN
1099-498X

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✦ Synopsis


Abstract

Background

The development of methods for specific delivery of genes into target tissues is an important issue for the further progress of gene therapy. Biological and physical targeting techniques may be combined to redirect gene therapy vectors to specific cells and enhance gene transfer.

Methods

The polymer poly(2‐(dimethylamino)ethyl methacrylate) (pDMAEMA) was conjugated with avidin or poly(ethylene glycol) (PEG) and complexed with adenovirus serotype 5 (Ad5). Targeting of polymer‐coated Ad5 to the epidermal growth factor receptor (EGFR) was accomplished by the binding of biotin‐EGF to pDMAEMA‐avidin. A photochemical treatment procedure using photosensitizer and light was applied to increase transduction with EGFR‐targeted viral complexes.

Results

pDMAEMA‐avidin efficiently enhanced transduction through unspecific viral uptake into cells, while pDMAEMA‐PEG provided charge shielding of the complexes and increased the specificity to EGFR when biotin‐EGF ligands were used. Transduction of PEG‐containing, EGFR‐targeted viral complexes was inhibited by 66% in coxsackie and adenovirus receptor (CAR)‐deficient RD cells and by 47% in CAR‐expressing DU 145 cells in receptor antibody experiments. The photochemical treatment had a substantial effect on transduction, enhancing the percentage of reporter gene positive cells from 20% to 75% of the total viable RD cell population and from 10% to 70% in DU 145 cells.

Conclusion

Photochemical treatment of cells infected with targeted viral vectors exhibiting a neutral surface charge is a potent method for enhancing transgene expression. Copyright © 2005 John Wiley & Sons, Ltd.


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