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

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

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 p...

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Main Authors: Sreeharsha Nagaraja, Girish Meravanige Basavarajappa, Mahesh Attimarad, Swati Pund
Format: Article
Language:English
Published: MDPI AG 2021-06-01
Series:Pharmaceutics
Subjects:
self-emulsifying
chrysin
ex vivo permeation
nanoemulgel
in vitro cytotoxicity
Online Access:https://www.mdpi.com/1999-4923/13/6/902
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spelling doaj-5a560846025741d884feffc359f5edda2021-07-01T00:29:03ZengMDPI AGPharmaceutics1999-49232021-06-011390290210.3390/pharmaceutics13060902Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-TechnologySreeharsha Nagaraja0Girish Meravanige Basavarajappa1Mahesh Attimarad2Swati Pund3Department of Pharmaceutical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Hofuf, Al-Ahsa 31982, Saudi ArabiaDepartment of Biomedical Sciences, College of Medicine, King Faisal University, Al-Hofuf, Al-Ahsa 31982, Saudi ArabiaDepartment of Pharmaceutical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Hofuf, Al-Ahsa 31982, Saudi ArabiaNanomedicine Laboratory, Department of Biosciences and Bioengineering, Indian Institute of Technology-Bombay, Mumbai 400076, Maharashtra, IndiaThe 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<sup>®</sup> 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<sup>®</sup> 90 surfactant, Tween<sup>®</sup> 80, and co-solvent Transcutol<sup>®</sup> 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.https://www.mdpi.com/1999-4923/13/6/902self-emulsifyingchrysinex vivo permeationnanoemulgelin vitro cytotoxicityex vivo permeation
collection DOAJ
language English
format Article
sources DOAJ
author Sreeharsha Nagaraja
Girish Meravanige Basavarajappa
Mahesh Attimarad
Swati Pund
spellingShingle Sreeharsha Nagaraja
Girish Meravanige Basavarajappa
Mahesh Attimarad
Swati Pund
Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
Pharmaceutics
self-emulsifying
chrysin
ex vivo permeation
nanoemulgel
in vitro cytotoxicity
ex vivo permeation
author_facet Sreeharsha Nagaraja
Girish Meravanige Basavarajappa
Mahesh Attimarad
Swati Pund
author_sort Sreeharsha Nagaraja
title Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
title_short Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
title_full Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
title_fullStr Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
title_full_unstemmed Topical Nanoemulgel for the Treatment of Skin Cancer: Proof-of-Technology
title_sort topical nanoemulgel for the treatment of skin cancer: proof-of-technology
publisher MDPI AG
series Pharmaceutics
issn 1999-4923
publishDate 2021-06-01
description 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<sup>®</sup> 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<sup>®</sup> 90 surfactant, Tween<sup>®</sup> 80, and co-solvent Transcutol<sup>®</sup> 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.
topic self-emulsifying
chrysin
ex vivo permeation
nanoemulgel
in vitro cytotoxicity
ex vivo permeation
url https://www.mdpi.com/1999-4923/13/6/902
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AT girishmeravanigebasavarajappa topicalnanoemulgelforthetreatmentofskincancerproofoftechnology
AT maheshattimarad topicalnanoemulgelforthetreatmentofskincancerproofoftechnology
AT swatipund topicalnanoemulgelforthetreatmentofskincancerproofoftechnology
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