Immobilization of Papain in Chitosan Membranes as a Potential Alternative for Skin Wounds

Anne Emmanuelle Câmara da Silva Melo; Felipe Sanderson Ribeiro de Sousa; Alaine M Dos Santos-Silva; Ednaldo Gomes do Nascimento; Matheus F Fernandes-Pedrosa; Caroline Addison Carvalho Xavier de Medeiros; Arnóbio Antônio da Silva-Junior

doi:10.3390/pharmaceutics15122649

Immobilization of Papain in Chitosan Membranes as a Potential Alternative for Skin Wounds

Pharmaceutics. 2023 Nov 21;15(12):2649. doi: 10.3390/pharmaceutics15122649.

Authors

Anne Emmanuelle Câmara da Silva Melo¹, Felipe Sanderson Ribeiro de Sousa¹, Alaine M Dos Santos-Silva¹, Ednaldo Gomes do Nascimento¹, Matheus F Fernandes-Pedrosa¹, Caroline Addison Carvalho Xavier de Medeiros², Arnóbio Antônio da Silva-Junior¹

Affiliations

¹ Laboratory of Pharmaceutical Technology and Biotechnology, Department of Pharmacy, Federal University of Rio Grande do Norte, UFRN, Gal. Gustavo Cordeiro de Farias, Petrópolis, Natal 59072-570, Brazil.
² Department of Pharmacology and Biophysics, Federal University of Rio Grande do Norte, UFRN, Lagoa Nova, Natal 59072-970, Brazil.

Abstract

Papain (an enzyme from the latex of Carica papaya) is an interesting natural bioactive macromolecule used as therapeutic alternative for wound healing due to debridement action in devitalized or necrotic tissues. However, its use in high doses can induce potential skin irritation and side effects. In this study, experiments explored the ability of chitosan membrane to immobilize papain, consequently improving enzymatic activity and controlling enzyme release. Papain-loading capacity was tested via experiments of force microscopy (AFM), scanning electron microscopy (SEM-FEG), and X-ray diffraction analyses. Fourier transform infrared spectroscopy and thermal analyses assessed the enzyme interactions with the copolymer. The investigation of the feasibility of membranes included pH on the surface, elasticity, and breaking strength measurements. The surface wettability and swelling capacity of different formulations revealed the best formulation for in vitro papain release experiments. The membranes had a transparent, rough, crystalline characteristic, which was homogeneous with the membrane within the neutrality. The immobilization of papain in the chitosan membrane resulted in a decrease in the vibration band characteristic of pure papain, suggesting a displacement in the vibration bands in the FTIR spectrum. The presence of papain decreased hydrophobicity on the surface of the membrane and disturbed the membrane's ability to swell. Chitosan membranes containing papain 2.5% (0.04 g) and 5.0% (0.08 g) preserved feasible properties and improved the enzymatic activity compared (0.87 ± 0.12 AU/mg and 1.59 ± 0.10 AU/mg) with a free papain sample (0.0042 ± 0.001 AU/mg). Concentrations of over 10% (0.16 g) led to phase separation into membranes. Chitosan membranes exhibited a slow papain release behavior adjusted via the Higushi model. The experimental achievements suggest a novel and promising method for the enhancement of papain. The results indicate the potential for prolonged bioactivity for use on wounds.

Keywords: chitosan membrane; drug delivery systems; immobilization; papain; wound dressing.

Abstract

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