Development of a novel lipophilic, magnetic nanoparticle for in Vivo drug delivery

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Abstract

The aim of the present study was to evaluate the transfection potential of chitosan-coated, green-fluorescent magnetic nanoparticles (MNPs) (chi-MNPs) after encapsulation inside polyethylglycol (PEG)ylated liposomes that produced lipid-encapsulated chitosan-coated MNPs (lip-MNPs), and also to evaluate how these particles would distribute in vivo after systemic injection. The transfection potential of both chi-MNPs and lip-MNPs was evaluated in vitro in rat brain endothelial 4 (RBE4) cells with and without applying a magnetic field. Subsequently, the MNPs were evaluated in vivo in young rats. The in vitro investigations revealed that the application of a magnetic field resulted in an increased cellular uptake of the particles. The lip-MNPs were able to transfect the RBE4 cells with an incidence of approximately 20% of a commercial transfection agent. The in vivo distribution studies revealed that lip-MNPs had superior pharmacokinetic properties due to evasion of the RES, including hepatic Kuppfer cells and macrophages in the spleen. In conclusion, we were able to design a novel lipid-encapsulated MNP with the ability to carry genetic material, with favorable pharmacokinetic properties, and under the influence of a magnetic field with the capability to mediate transfection in vitro. © 2013 by the authors; licensee MDPI, Basel, Switzerland.

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Linemann, T., Thomsen, L. B., du Jardin, K. G., Laursen, J. C., Jensen, J. B., Lichota, J., & Moos, T. (2013). Development of a novel lipophilic, magnetic nanoparticle for in Vivo drug delivery. Pharmaceutics, 5(2), 246–260. https://doi.org/10.3390/pharmaceutics5020246

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