The exploitation of curcumin for
oral disease treatment is limited
by its low solubility, poor bioavailability, and low stability. Surface-functionalized
poly-lactic-co-glycolic acid (PLGA) nanoparticles
(NPs) have shown promising results to ameliorate selective delivery
of drugs to the gastro-intestinal tract. In this study, curcumin-loaded
PLGA NPs (C-PLGA NPs) of about 200 nm were surface-coated with chitosan
(CS) for gastro-intestinal mucosa adhesion, wheat germ agglutinin
(WGA) for colon targeting or GE11 peptide for tumor colon targeting.
Spectrometric and zeta potential analyses confirmed the successful
functionalization of the C-PLGA NPs. Real-time label-free assessment
of the cell membrane-NP interactions and NP cell uptake were performed
by quartz crystal microbalance coupled with supported lipid bilayers
and by surface plasmon resonance coupled with living cells. The study
showed that CS-coated C-PLGA NPs interact with cells by the electrostatic
mechanism, while both WGA- and GE11-coated C-PLGA NPs interact and
are taken up by cells by specific active mechanisms. In vitro cell
uptake studies corroborated the real-time label-free assessment by
yielding a curcumin cell uptake of 7.3 ± 0.3, 13.5 ± 1.0,
27.3 ± 4.9, and 26.0 ± 1.3 μg per 104 HT-29
cells for noncoated, CS-, WGA-, and GE11-coated C-PLGA NPs, respectively.
Finally, preliminary in vivo studies showed that the WGA-coated C-PLGA
NPs efficiently accumulate in the colon after oral administration
to healthy Balb/c mice. In summary, the WGA- and GE11-coated C-PLGA
NPs displayed high potential for application as active targeted carriers
for anticancer drug delivery to the colon.
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