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International Journal of Nanomedicine Volume 5, 2010 - Issue
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Original Research

In vitro and in vivo effects of polyethylene glycol (PEG)-modified lipid in DOTAP/cholesterol-mediated gene transfection

Torben Gjetting1 Department of Radiation Biology, Finsen Center
,
Nicolai Skovbjerg Arildsen1 Department of Radiation Biology, Finsen Center
,
Camilla Laulund Christensen1 Department of Radiation Biology, Finsen Center
,
Thomas Tuxen Poulsen1 Department of Radiation Biology, Finsen Center
,
Jack A Roth3 Thoracic Medical Oncology, MD Anderson Cancer Centre, Houston, TX, USA
,
Vagn Neerup Handlos2 RH Pharmacy, Copenhagen University Hospital, Copenhagen, Denmark
&
Hans Skovgaard Poulsen1 Department of Radiation Biology, Finsen CenterCorrespondence[email protected]
 show all
Pages 371-383 | Published online: 25 May 2010
 
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Abstract

Background

DOTAP/cholesterol-based lipoplexes are successfully used for delivery of plasmid DNA in vivo especially to the lungs, although low systemic stability and circulation have been reported. To achieve the aim of discovering the best method for systemic delivery of DNA to disseminated tumors we evaluated the potential of formulating DOTAP/cholesterol lipoplexes with a polyethylene glycol (PEG)-modified lipid, giving the benefit of the shielding and stabilizing properties of PEG in the bloodstream.

Method

A direct comparison of properties in vitro and in vivo of 4 different DOTAP/cholesterol-based lipoplexes containing 0%, 2%, 4%, and 10% PEG was performed using reporter gene activity and radioactive tracer lipid markers to monitor biodistribution.

Results

We found that 10% PEGylation of lipoplexes caused reduced retention in lung and heart tissues of nude mice compared to nonPEGylated lipoplexes, however no significant delivery to xenograft flank tumors was observed. Although PEGylated and nonPEGylated lipoplexes were delivered to cells the ability to mediate successful transfection is hampered upon PEGylation, presumably due to a changed uptake mechanism and intracellular processing.

Conclusion

The eminent in vivo transfection potency of DOTAP/cholesterol-based lipoplexes is well established for expression in lung tumors, but it is unsuitable for expression in non first pass organs such as xenograft flank tumors in mice even after addition of a PEG-lipid in the formulation.

Acknowledgements

The authors wish to extend their appreciation to Birgit Guldhammer for pathological evaluation of tissue section, Hanne Mørck Nielsen for access to Zetasizer, and Pia Pedersen for excellent technical assistance. This work was supported in part by a grant from the Danish Cancer Society and the Novo Nordisk Foundation. The authors report no conflicts of interest in this work.

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