Development of Soft Luliconazole Invasomes Gel for Effective Transdermal Delivery: Optimization to In-Vivo Antifungal Activity

Author:

Kumari Sunitha1,Alsaidan Omar Awad2ORCID,Mohanty Dibyalochan1,Zafar Ameeduzzafar2ORCID,Das Swagatika3ORCID,Gupta Jeetendra Kumar4ORCID,Khalid Mohammad5

Affiliation:

1. Department of Pharmaceutics, Anurag University, Hyderabad 500088, Telangana, India

2. Department of Pharmaceutics, College of Pharmacy, Jouf University, Sakaka 72341, Al-Jouf, Saudi Arabia

3. School of Pharmacy, Centurion University of Technology and Management, Gopalpur 756044, Odisha, India

4. Institute of Pharmaceutical Research, GLA University, Mathura 281406, Uttar Pradesh, India

5. Department of Pharmacognosy, College of Pharmacy, Prince Sattam Bin Abdulaziz University, Al-Kharj 11942, Riyadh, Saudi Arabia

Abstract

Luliconazole (LZ) is a good candidate for the treatment of fungal infection topically but has limitations, i.e., poor solubility and poor permeability to skin. Due to these limitations, multiple administrations for a long time are required to treat the inflection. The aim of the present study was to develop the invasomes (IVS) gel of LZ to improve the topical antifungal activity. The IVS was prepared by the thin-film hydration method and optimized by Box-Bhekhen design software. The optimized LZIVS (LZIVSopt) has 139.1 ± 4.32 nm of vesicle size, 88.21 ± 0.82% of entrapment efficiency, 0.301 ± 0.012 of PDI, and 19.5 mV (negative) of zeta potential. Scanning microscopy showed a spherical shape of the vesicle. FTIR spectra showed there is no interaction between the drug and lipid. Thermogram showed that the LZ is encapsulated into the LZIVS matrix. LZIVSopt gel (LZIVSopt-G3) exhibited optimum viscosity (6493 ± 27 cps) and significant spreadability (7.2 g·cm/s). LZIVSopt-G3 showed 2.47-fold higher permeation than pure LZ-gel. LZIVSopt-G3 did not show any edema or swelling in the skin, revealing that the developed formulation is non-irritant. LZIVSopt-G3 exhibited significant inhibition of the fungus infection (C. albicans) in the infected rats. The finding concluded that IVS gel is a good carrier and an attractive approach for the enhancement of topical delivery of LZ to treat the fungal infection.

Funder

Deputyship for Research and Innovation, Ministry of Education in Saudi Arabia

Publisher

MDPI AG

Subject

Polymers and Plastics,Organic Chemistry,Biomaterials,Bioengineering

Reference53 articles.

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4. Inhibition of ergosterol synthesis by novel antifungal compounds targeting C-14 reductase;Hata;Med. Mycol.,2010

5. Ivanov, M., Ćirić, A., and Stojković, D. (2022). Emerging Antifungal Targets and Strategies. Int. J. Mol. Sci., 23.

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