Development of N-alkylated benzimidazole based cubosome hydrogel for topical treatment of burns

Maubashera Nawaz; Sofia Hayat; Umer Farooq; Muhammad Adnan Iqbal; Syed Haroon Khalid; Tan Wen Nee; Kooi Yeong Khaw; Rabia Munir; Muhammad Umar Ijaz

doi:10.1039/d4ra04816d

Development of N-alkylated benzimidazole based cubosome hydrogel for topical treatment of burns

RSC Adv. 2024 Oct 10;14(44):32008-32020. doi: 10.1039/d4ra04816d. eCollection 2024 Oct 9.

Authors

Maubashera Nawaz¹, Sofia Hayat¹, Umer Farooq¹, Muhammad Adnan Iqbal¹, Syed Haroon Khalid^{2

3}, Tan Wen Nee⁴, Kooi Yeong Khaw⁵, Rabia Munir², Muhammad Umar Ijaz⁶

Affiliations

¹ Department of Chemistry, University of Agriculture Faisalabad 38040 Pakistan [email protected].
² Department of Pharmaceutics, Government College University Faisalabad 38000 Pakistan.
³ Department of Pharmaceutical Technology, Faculty of Pharmacy, Universiti Teknologi Mara (UiTM) Puncak Alam 42300 Selangor Malaysia.
⁴ Chemistry Section, School of Distance Education, Universiti Sains Malaysia 11800 Malaysia.
⁵ School of Pharmacy, Monash University Malaysia Jalan Lagoon Selatan Bandar Sunway 47500 Selangor Malaysia.
⁶ Department of Zoology, Wildlife and Fisheries, University of Agriculture Faisalabad 38040 Pakistan.

Abstract

The current study focuses on assessing the activity of the N-alkylated benzimidazole based cubosomal hydrogel (cubogel) for the topical treatment of burn wounds. The study involves the synthesis of six benzimidazole derivatives (1-6) and their characterization by FT-IR and ¹H and ¹³C NMR spectroscopy. The further study involves the design and formation of nanoparticles known as cubosomes loaded with selected 1-benzyl-1-benzimidazole (API 6) and the development of a cubogel for the topical treatment of burn wounds. Cubosomes were prepared by the homogenization method, using glyceryl monooleate (GMO) as a lipid polymer and poloxamer 407 (P407) as a surfactant. Cubosomes undergo in vitro characterizations (measurement of particle size, zeta potential, polydispersity index (PDI), % entrapment efficiency, drug release in phosphate buffer saline of pH 6.8, and surface morphology by utilizing TEM (transmission electron microscopy). Formulation D3 (2.5% of GMO, 1% of P407, and 2.5% of PVA) emerged as the optimized formulation, displaying a minimum particle size (PS) of 129.9 ± 1 nm, entrapment efficiency (%EE) of 96.67 ± 0.89%, and a drug release of 86 ± 2.7% at 24 h. Carbopol 940 hydrogel was prepared and incorporated with the optimized formulation to prepare cubogel. This optimized cubogel provided 92.56 ± 0.014% in vitro drug release within 24 h. An in vivo histopathological study was conducted on an animal model (rabbit) to assess the efficacy of cubogel in wound healing and wound contraction. Then cubogel was compared with the commercially available creams Clotrimazole® and Polyfax®. The wound treated with newly developed cubogel has maximum wound contraction (96.70%) as compared to the standard creams. The findings revealed that the newly formulated cubogel was highly effective in treating burns, showing superior performance to commercial products without inducing side effects. Additionally, benzimidazole derivative loaded cubogel caused a sustained release for treating burn wounds without any bacterial infections. The current results further suggested phase 0 clinical trials.