2023
DOI: 10.1021/acsomega.3c00914
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Design of Cinnamaldehyde- and Gentamicin-Loaded Double-Layer Corneal Nanofiber Patches with Antibiofilm and Antimicrobial Effects

Abstract: In this study, two-layer poly(vinyl alcohol)/gelatin (PVA/GEL) nanofiber patches containing cinnamaldehyde (CA) in the first layer and gentamicin (GEN) in the second layer were produced by the electrospinning method. The morphology, chemical structures, and thermal temperatures of the produced pure (PVA/GEL), CA-loaded (PVA/GEL/CA), GEN-loaded (PVA/GEL/GEN), and combined drug-loaded (PVA/GEL/CA/GEN) nanofiber patches were determined by scanning electron microscopy (SEM), Fourier transform infrared spectroscopy… Show more

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Cited by 7 publications
(3 citation statements)
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References 49 publications
(95 reference statements)
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“…The release of hydrophobic molecules from a carrier material that contains PVA can be influenced by several factors, such as drug carrier interactions, size, and shape of model cargo. PVA is a hydrophilic polymer, and model cargos like NR can form weak and reversible binding interactions including van der Waals, hydrophobic interactions with PVA . During the initial phase of release, the model cargo present at or near the surface of the NP can be easily released due to these weak interactions, which could explain the initial burst release.…”
Section: Resultsmentioning
confidence: 99%
See 1 more Smart Citation
“…The release of hydrophobic molecules from a carrier material that contains PVA can be influenced by several factors, such as drug carrier interactions, size, and shape of model cargo. PVA is a hydrophilic polymer, and model cargos like NR can form weak and reversible binding interactions including van der Waals, hydrophobic interactions with PVA . During the initial phase of release, the model cargo present at or near the surface of the NP can be easily released due to these weak interactions, which could explain the initial burst release.…”
Section: Resultsmentioning
confidence: 99%
“…PVA is a hydrophilic polymer, and model cargos like NR can form weak and reversible binding interactions including van der Waals, hydrophobic interactions with PVA. 46 During the initial phase of release, the model cargo present at or near the surface of the NP can be easily released due to these weak interactions, which could explain the initial burst release. Alternatively, the initial burst release could be due to a swelling process, which was also indicated by the stability measurements.…”
Section: Resultsmentioning
confidence: 99%
“…While antibiotic eye drops are commonly employed, they suffer from limitations such as poor bioavailability and the potential to foster antibiotic‐resistant strains of bacteria. [ 8 ] Recently, biomedical patches have been developed to incorporate antibacterial or bioactive materials for infected cornea utilizing various techniques such as hydrogel, [ 9–12 ] microneedle, [ 13,14 ] three‐dimensional (3D) printing, [ 15,16 ] electrospinning, [ 17,18 ] and microfluidics. [ 19,20 ] However, these patches often fall short in multiple areas: they are typically mono‐functional and possess inadequate mechanical strength and tissue adhesion.…”
Section: Introductionmentioning
confidence: 99%