Local and
Sustained Gene Delivery in Silica-Collagen Nanocomposites
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Abstract
Local
delivery of biomolecules from hydrogels is highly challenging because
of their rapid diffusion and degradation. Gene therapy represents
an alternative that allows for the prolonged production of proteins
by transfected cells. In this study, we have developed nanocomposites
consisting of DNA-polyethylenimine-silica nanoparticle complexes coencapsulated
with fibroblasts within collagen hydrogels. Through the modulation
of the particle size and polyethylenimine molecular weight, it was
possible to achieve “in-gel” transfection permitting
the sustained production of biomolecules from hydrogels over 1 week.
Alternative configurations consisting of particle addition to cellularized
gels and cell culture in the presence of complex-containing hydrogels
were also investigated. These studies demonstrated that particle encapsulation
limits DNA and silica dissemination outside the collagen hydrogels.
They also show the key role of cell proliferation within collagen
hydrogels on the transfection efficiency. Such nanocomposites therefore
constitute promising materials for the development of novel gene delivery
systems to promote tissue repair