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Formulation and Optimization of Butenafine-Loaded Topical Nano Lipid Carrier-Based Gel: Characterization, Irritation Study, and Anti-Fungal Activity
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The present study aims to prepare and optimize butenafine hydrochloride NLCs formulation using solid and liquid lipid. The optimized selected BF-NLCopt was further converted into Carbopol-based gel for topical application for the treatment of fungal infection. Box Behnken design was employed to optimize the nanostructure lipids carriers (NLCs) using the lipid content (A), Tween 80 (B), and homogenization cycle (C) as formulation factors at three levels. Their effects were observed on the particle size (Y1) and entrapment efficiency (Y2). The selected formulation was converted into gel and further assessed for gel characterization, drug release, anti-fungal study, irritation study, and stability study. The solid lipid (Compritol 888 ATO), liquid lipid (Labrasol), and surfactant (tween 80) were selected based on maximum solubility. The optimization result showed a particle size of 111 nm with high entrapment efficiency of 86.35% for BF-NLCopt. The optimized BF-NLCopt converted to gel (1% w/v, Carbopol 934) and showed ideal gel evaluation results (drug content 99.45 ± 2.11, pH 6.5 ± 0.2, viscosity 519 ± 1.43 CPs). The drug release study result depicted a prolonged drug release (65.09 ± 4.37%) with high drug permeation 641.37 ± 46.59 µg (32.07 ± 2.32%) than BF conventional gel. The low value of irritation score (0.17) exhibited negligible irritation on the skin after application. The anti-fungal result showed greater efficacy than the BF gel at both time points. The overall conclusion of the results revealed NLCs-based gel of BF as an ideal delivery system to treat the fungal infection.
Title: Formulation and Optimization of Butenafine-Loaded Topical Nano Lipid Carrier-Based Gel: Characterization, Irritation Study, and Anti-Fungal Activity
Description:
The present study aims to prepare and optimize butenafine hydrochloride NLCs formulation using solid and liquid lipid.
The optimized selected BF-NLCopt was further converted into Carbopol-based gel for topical application for the treatment of fungal infection.
Box Behnken design was employed to optimize the nanostructure lipids carriers (NLCs) using the lipid content (A), Tween 80 (B), and homogenization cycle (C) as formulation factors at three levels.
Their effects were observed on the particle size (Y1) and entrapment efficiency (Y2).
The selected formulation was converted into gel and further assessed for gel characterization, drug release, anti-fungal study, irritation study, and stability study.
The solid lipid (Compritol 888 ATO), liquid lipid (Labrasol), and surfactant (tween 80) were selected based on maximum solubility.
The optimization result showed a particle size of 111 nm with high entrapment efficiency of 86.
35% for BF-NLCopt.
The optimized BF-NLCopt converted to gel (1% w/v, Carbopol 934) and showed ideal gel evaluation results (drug content 99.
45 ± 2.
11, pH 6.
5 ± 0.
2, viscosity 519 ± 1.
43 CPs).
The drug release study result depicted a prolonged drug release (65.
09 ± 4.
37%) with high drug permeation 641.
37 ± 46.
59 µg (32.
07 ± 2.
32%) than BF conventional gel.
The low value of irritation score (0.
17) exhibited negligible irritation on the skin after application.
The anti-fungal result showed greater efficacy than the BF gel at both time points.
The overall conclusion of the results revealed NLCs-based gel of BF as an ideal delivery system to treat the fungal infection.
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