Herein, a novel designed heterogeneous catalytic system constructed of volcanic pumice magnetic particles (VPMPs), cellulose (CLS) as a natural polymeric matrix, and copper nanoparticles (Cu NPs) is presented.
This study describes an efficient antimicrobial drug
delivery system
composed of iron oxide magnetic nanoparticles (Fe3O4 NPs) coated by an MOF-199 network. Then, the prepared vancomycin
(VAN)-loaded carrier was fully packed in a lattice of beta-cyclodextrin
(BCD). For cell adhesion, beta-cyclodextrin has been functionalized
with guanidine (Gn) groups within in situ synthetic processes. Afterward,
drug loading efficiency and the release patterns were investigated
through precise analytical methods. Confocal microscopy has shown
that the prepared cargo (formulated as [VAN@Fe3O4/MOF-199]BCD-Gn) could be attached to the Staphylococcus
aureus (S. aureus)
and Escherichia coli (E. coli) bacterial cells in a higher rate than the
individual VAN. The presented system considerably increased the antibacterial
effects of the VAN with a lower dosage of drug. The cellular experiments
such as the zone of inhibition and optical density (OD600) have confirmed the enhanced antibacterial effect of the designed
cargo. In addition, the MIC/MBC (minimum inhibitory and bactericidal
concentrations) values have been estimated for the prepared cargo
compared to the individual VAN, revealing high antimicrobial potency
of the VAN@Fe3O4/MOF-199]BCD-Gn cargo.
In the field of targeted drug delivery, the effects of size and morphology of drug nanocarriers are of great importance and need to be discussed in depth.
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