In vitro screening of topical formulation excipients for epithelial toxicity in cancerous and non-cancerous cell lines

Article


Forouz, Farzaneh, Mohammed, Yousuf, Shobeiri Nejad, Hamid S. A., Roberts, Michael S. and Grice, Jeffrey E.. 2023. "In vitro screening of topical formulation excipients for epithelial toxicity in cancerous and non-cancerous cell lines ." EXCLI journal . 22, pp. 1173-1199. https://doi.org/10.17179/excli2023-6072
Article Title

In vitro screening of topical formulation excipients for epithelial toxicity in cancerous and non-cancerous cell lines

Article CategoryArticle
AuthorsForouz, Farzaneh, Mohammed, Yousuf, Shobeiri Nejad, Hamid S. A., Roberts, Michael S. and Grice, Jeffrey E.
Journal TitleEXCLI journal
Journal Citation22, pp. 1173-1199
Number of Pages27
Year2023
Place of PublicationGermany
ISSN1611-2156
Digital Object Identifier (DOI)https://doi.org/10.17179/excli2023-6072
Web Address (URL)https://www.excli.de/index.php/excli/article/view/6072
Abstract

Chemical excipients used in topical formulations may be toxic to living skin cells. Here, we compared the in vitro toxicity of some common solubilizing excipients against human melanoma cells, human keratinocytes (HaCaT) and primary skin fibroblasts (FB) as examples of cancerous, immortalized and primary human skin cells, often used as experimental models representative of in vivo conditions. Two distinct endpoint assays (3-(4,5-Dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) and crystal violet (CV)) were used. The mechanism of cell death after excipient exposure was assessed through Reactive Oxygen Species (ROS) production, cell membrane integrity and cell cycle progression. Results showed that the surfactants, Labrasol®, Labrafil® and Transcutol®, were less toxic than Triton X-100 (a model irritant) in all cell types whereas the oil, Labrafac®, was non-toxic. The human melanoma WM164 cell line showed the greatest sensitivity toward cytotoxicity after chemical exposure, while the other cell lines were more resistant. The relative excipient cytotoxicity responses observed in the MTT and CV assays were comparable and similar trends were seen in their estimated 50 % inhibitory concentration (IC50) values. DNA fragmentation by flow cytometry after exposing the cells to IC50 concentrations of the excipients showed negligible apoptotic populations. ROS production was increased in all cell types after toxic exposure; however, ROS elevation did not lead to apoptosis. The toxicity profiles of each excipient are not only relevant to their use in formulating safe topical products but also in the potential synergistic efficacy in the topical treatment of melanoma.

KeywordsPharmaceutical excipients; cytotoxicity cell sensitivity; MTT; crystal violet; ROS; cell cycle analysis
Contains Sensitive ContentDoes not contain sensitive content
ANZSRC Field of Research 2020310199. Biochemistry and cell biology not elsewhere classified
Byline AffiliationsUniversity of Queensland
School of Mathematics, Physics and Computing
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