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Enhanced thoracic gene delivery by magnetic nanobead-mediated vector

✍ Scribed by Wenzhong Li; Nan Ma; Lee-Lee Ong; Alexander Kaminski; Christian Skrabal; Murat Ugurlucan; Peter Lorenz; Hans-Heinrich Gatzen; Karola Lützow; Andreas Lendlein; Brigitte M. Pützer; Ren-Ke Li; Gustav Steinhoff


Book ID
102891000
Publisher
John Wiley and Sons
Year
2008
Tongue
English
Weight
634 KB
Volume
10
Category
Article
ISSN
1099-498X

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✦ Synopsis


Abstract

Background

Systemic gene delivery is limited by the adverse hydrodynamic conditions on the collection of gene carrier particles to the specific area. In the present study, a magnetic field was employed to guide magnetic nanobead (MNB)/polymer/DNA complexes after systemic administration to the left side of the mouse thorax in order to induce localized gene expression.

Methods

Nonviral polymer (poly ethyleneimine, PEI) vector‐gene complexes were conjugated to MNBs with the Sulfo‐NHS‐LC‐Biotin linker. In vitro transfection efficacy of MNB/PEI/DNA was compared with PEI/DNA in three different cell lines as well as primary endothelial cells under magnetic field stimulation. In vivo, MNB/PEI/DNA complexes were injected into the tail vein of mice and an epicardial magnet was employed to attract the circulating MNB/PEI/DNA complexes.

Results

Endocytotic uptake of MNB/PEI/DNA complexes and intracellular gene release with nuclear translocation were observed in vitro, whereas the residues of MNB/PEI complexes were localized at the perinuclear region. Compared with PEI/DNA complexes alone, MNB/PEI/DNA complexes had a 36‐ to 85‐fold higher transfection efficiency under the magnetic field. In vivo, the epicardial magnet effectively attracted MNB/PEI/DNA complexes in the left side of the thorax, resulting in strong reporter and therapeutic gene expression in the left lung and the heart. Gene expression in the heart was mainly within the endothelium.

Conclusions

MNB‐mediated gene delivery could comprise a promising method for gene delivery to the lung and the heart. Copyright © 2008 John Wiley & Sons, Ltd.


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