Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology

Sreeharsha Nagaraja; Girish Meravanige Basavarajappa; Mahesh Attimarad; Swati Pund

doi:10.3390/pharmaceutics13060902

Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology

Pharmaceutics. 2021 Jun 18;13(6):902. doi: 10.3390/pharmaceutics13060902.

Authors

Sreeharsha Nagaraja^{1

2}, Girish Meravanige Basavarajappa³, Mahesh Attimarad¹, Swati Pund⁴

Affiliations

¹ Department of Pharmaceutical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Hofuf, Al-Ahsa 31982, Saudi Arabia.
² Department of Pharmaceutics, Vidya Siri College of Pharmacy, Off Sarjapura Road, Bangalore 560035, Karnataka, India.
³ Department of Biomedical Sciences, College of Medicine, King Faisal University, Al-Hofuf, Al-Ahsa 31982, Saudi Arabia.
⁴ Nanomedicine Laboratory, Department of Biosciences and Bioengineering, Indian Institute of Technology-Bombay, Mumbai 400076, Maharashtra, India.

Abstract

The present study is a mechanistic validation of 'proof-of-technology' for the effective topical delivery of chrysin nanoemulgel for localized, efficient treatment of melanoma-affected skin.

Background: Currently available treatments for skin cancer are inefficient due to systemic side effects and poor transcutaneous permeation, thereby presenting a formidable challenge for the development of novel nanocarriers.

Methods: We opted for a novel approach and formulated a nanocomplex system composed of hydrophobic chrysin dissolved in a lipid mix, which was further nanoemulsified in Pluronic^® F-127 gel to enhance physicochemical and biopharmaceutic characteristics. Chrysin, a flavone extracted from passion flowers, exhibits potential anti-cancer activities; however, it has limited applicability due to its poor solubility. Pseudo-ternary phase diagrams were constructed to identify the best self-nanoemulsifying region by varying the compositions of oil, Caproyl^® 90 surfactant, Tween^® 80, and co-solvent Transcutol^® HP. Chrysin-loaded nanoemulsifying compositions were characterized for various physicochemical properties.

Results: This thermodynamically stable, self-emulsifying drug delivery system showed a mean droplet size of 156.9 nm, polydispersity index of 0.26, and viscosity of 9100 cps after dispersion in gel. Mechanical characterization using Texture Analyzer exhibited that the gel had a hardness of 487 g and adhesiveness of 500 g. Ex vivo permeation through rat abdominal skin revealed significant improvement in percutaneous absorption measured as flux, the apparent permeability coefficient, the steady-state diffusion coefficient, and drug deposition. In vitro cytotoxicity on A375 and SK-MEL-2 cell lines showed a significantly improved therapeutic effect, thus ensuring reduction in dose. The safety of the product was established through biocompatibility testing on the L929 cell line.

Conclusion: Aqueous, gel-based, topical, nanoemulsified chrysin is a promising technology approach for effective localized transcutaneous delivery that will help reduce the frequency and overall dose usage and ultimately improve the therapeutic index.

Keywords: chrysin; ex vivo permeation; in vitro cytotoxicity; nanoemulgel; self-emulsifying.

Grants and funding

206070/Deanship of Scientific Research, King Faisal University