Caspofungin-Loaded Formulations for Treating Ocular Infections Caused by Candida spp
Metadata
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MDPI
Materia
Caspofungin Ocular drug delivery Ocular gels Poloxamer 407 Ocular infection
Date
2023-04-20Referencia bibliográfica
Pérez-González, N.; Rodríguez-Lagunas, M.J.; Calpena-Campmany, A.C.; Bozal-de Febrer, N.; Halbaut-Bellowa, L.; Mallandrich, M.; Clares-Naveros, B. Caspofungin-Loaded Formulations for Treating Ocular Infections Caused by Candida spp. Gels 2023, 9, 348. [https://doi.org/10.3390/ gels9040348]
Sponsorship
Spanish National Research Council (CSIC), project no. 202080E231; University of Barcelona and the University of Granada (Official State Gazette 311, on 27 November 2020)Abstract
Fungal keratitis causes corneal blindness worldwide. The treatment includes antibiotics,
with Natamycin being the most commonly used; however, fungal keratitis is difficult to treat, so
alternative therapies are needed. In situ gelling formulations are a promising alternative; this type of
formulation has the advantages of eye drops combined with the advantages of ointments. This study
was designed to develop and characterize three formulations containing 0.5% CSP: CSP-O1, CSP-O2,
and CSP-O3. CSP is an antifungal drug that acts against a diverse variety of fungi, and Poloxamer 407
(P407) is a polymer of synthetic origin that is able to produce biocompatible, biodegradable, highly
permeable gels and is known to be thermoreversible. Short-term stability showed that formulations
are best stored at 4 C, and rheological analysis showed that the only formulation able to gel in situ
was CSP-O3. In vitro release studies indicated that CSP-O1 releases CSP most rapidly, while in vitro
permeation studies showed that CSP-O3 permeated the most. The ocular tolerance study showed that
none of the formulations caused eye irritation. However, CSP-O1 decreased the cornea’s transparency.
Histological results indicate that the formulations are suitable for use, with the exception of CSP-O3,
which induced slight structural changes in the scleral structure. All formulations were shown to have
antifungal activity. In view of the results obtained, these formulations could be promising candidates
for use in the treatment of fungal keratitis.