What question did this study set out to answer?

The study aims to develop nanofiber-based ophthalmic inserts to improve the solubility and delivery of AmphB for treating fungal keratitis.

April 12, 2026Open Access

Development and Formulation of Nanofiber-Based Ophthalmic Inserts for the Treatment of Fungal Keratitis

Key Points

The study aims to develop nanofiber-based ophthalmic inserts to improve the solubility and delivery of AmphB for treating fungal keratitis.
Developed AmphB-loaded PVA nanofiber inserts using electrospinning
Evaluated drug content and in vitro release using Weibull modeling
Assessed antifungal activity against specific fungi and ocular cytocompatibility using the HET-CAM test
Characterized structural properties with SEM, FTIR, and XRD
Achieved bead-free nanofibers with diameters between 216 nm and 310 nm
Confirmed complete amorphization of AmphB in the nanofiber matrix
Demonstrated rapid release of AmphB (≈100% in 60 min) with Fickian diffusion
Showed effective inhibition against key fungal species
Classified as practically non-irritant with favorable stability after storage

Abstract

Background/Objectives: Fungal keratitis remains a vision-threatening infection, and current amphotericin B (AmphB) eye drops suffer from low corneal residence time, poor aqueous solubility, and the need for frequent dosing. This study develops electrospun nanofiber-based ophthalmic inserts combining polyvinyl alcohol (PVA), gamma-cyclodextrin (γ-CD), and sodium taurocholate (STC) to enhance AmphB solubility and provide a non-invasive, rapidly dissolving ophthalmic dosage form. Methods: γ-CD and STC-enhanced AmphB-loaded PVA nanofiber-based ophthalmic inserts with varying γ-CD and STC concentrations were prepared by electrospinning and characterized by scanning electron microscopy (SEM), Fourier transform infrared spectroscopy (FTIR), and X-ray diffraction (XRD). Drug content, in vitro release (Weibull modeling), antifungal activity against Candida albicans, Fusarium solani, and Aspergillus fumigatus, ocular cytocompatibility using the Hen’s Egg Test on Chorioallantoic Membrane (HET-CAM), and accelerated stability (40 ± 2 °C, 75 ± 5% relative humidity, 4 weeks) were evaluated. Results: Bead-free nanofibers with mean diameters between 216 ± 33 nm and 310 ± 35 nm were obtained, and XRD confirmed complete amorphization of AmphB within the PVA nanofiber matrix, forming an amorphous solid dispersion. All formulations showed rapid and nearly complete AmphB release (≈100% within 60 min), with Weibull β values < 0.75, indicating Fickian diffusion-controlled release. AmphB-loaded PVA nanofiber-based ophthalmic inserts produced inhibition zones and broth susceptibility profiles comparable to AmphB in dimethyl sulfoxide (DMSO), demonstrating preserved antifungal activity. HET-CAM scores (0–0.9) classified the inserts as practically non-irritant, and SEM/FTIR after accelerated storage showed no relevant morphological or physicochemical changes. Conclusions: These γ-CD and STC-enhanced AmphB-loaded PVA nanofiber-based ophthalmic inserts provide a non-invasive, rapidly dissolving ophthalmic dosage form that combines amorphous AmphB, immediate drug availability, and good ocular tolerance, supporting their further development as a patient-friendly treatment option for fungal keratitis.

Development and Formulation of Nanofiber-Based Ophthalmic Inserts for the Treatment of Fungal Keratitis

Key Points

Abstract

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