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Formulation and Evaluation of Topical Nano-Lipid-Based Delivery of Butenafine: In Vitro Characterization and Antifungal Activity
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The present research work was designed to prepare butenafine (BN)-loaded bilosomes (BSs) by the thin-film hydration method. BN is a sparingly water-soluble drug having low permeability and bioavailability. BSs are lipid-based nanovesicles used to entrap water-insoluble drugs for enhanced permeation across the skin. BSs were prepared by the thin-film hydration method and optimized by the Box–Behnken design (BBD) using lipid (A), span 60 (B), and sodium deoxycholate (C) as independent variables. The selected formulation (BN-BSo) was converted into the gel using Carbopol 940 as a gelling agent. The prepared optimized gel (BN-BS-og) was further evaluated for the gel characterization, drug release, drug permeation, irritation, and anti-fungal study. The optimized bilosomes (BN-BSo) showed a mean vesicle size of 215 ± 6.5 nm and an entrapment efficiency of 89.2 ± 1.5%. The DSC study showed that BN was completely encapsulated in the BS lipid matrix. BN-BSog showed good viscosity, consistency, spreadability, and pH. A significantly (p < 0.05) high release (81.09 ± 4.01%) was achieved from BN-BSo compared to BN-BSog (65.85 ± 4.87%) and pure BN (17.54 ± 1.37 %). The permeation study results revealed that BN-BSo, BN-BSog, and pure BN exhibited 56.2 ± 2.7%, 39.2 ± 2.9%, and 16.6 ± 2.3%. The enhancement ratio of permeation flux was found to be 1.4-fold and 3.4-fold for the BN-BS-og and pure BN dispersion. The HET-CAM study showed that BN-BSog was found to be nonirritant as the score was found within the limit. The antifungal study revealed a significant (p < 0.05) enhanced antifungal activity against C. albicans and A. niger. The findings of the study revealed that BS is an important drug delivery system for transdermal delivery.
Title: Formulation and Evaluation of Topical Nano-Lipid-Based Delivery of Butenafine: In Vitro Characterization and Antifungal Activity
Description:
The present research work was designed to prepare butenafine (BN)-loaded bilosomes (BSs) by the thin-film hydration method.
BN is a sparingly water-soluble drug having low permeability and bioavailability.
BSs are lipid-based nanovesicles used to entrap water-insoluble drugs for enhanced permeation across the skin.
BSs were prepared by the thin-film hydration method and optimized by the Box–Behnken design (BBD) using lipid (A), span 60 (B), and sodium deoxycholate (C) as independent variables.
The selected formulation (BN-BSo) was converted into the gel using Carbopol 940 as a gelling agent.
The prepared optimized gel (BN-BS-og) was further evaluated for the gel characterization, drug release, drug permeation, irritation, and anti-fungal study.
The optimized bilosomes (BN-BSo) showed a mean vesicle size of 215 ± 6.
5 nm and an entrapment efficiency of 89.
2 ± 1.
5%.
The DSC study showed that BN was completely encapsulated in the BS lipid matrix.
BN-BSog showed good viscosity, consistency, spreadability, and pH.
A significantly (p < 0.
05) high release (81.
09 ± 4.
01%) was achieved from BN-BSo compared to BN-BSog (65.
85 ± 4.
87%) and pure BN (17.
54 ± 1.
37 %).
The permeation study results revealed that BN-BSo, BN-BSog, and pure BN exhibited 56.
2 ± 2.
7%, 39.
2 ± 2.
9%, and 16.
6 ± 2.
3%.
The enhancement ratio of permeation flux was found to be 1.
4-fold and 3.
4-fold for the BN-BS-og and pure BN dispersion.
The HET-CAM study showed that BN-BSog was found to be nonirritant as the score was found within the limit.
The antifungal study revealed a significant (p < 0.
05) enhanced antifungal activity against C.
albicans and A.
niger.
The findings of the study revealed that BS is an important drug delivery system for transdermal delivery.
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