Human Epidermal Keratinocytes in Culture: A Story of Multiple Recipes for a Single Cell Type

Poumay, Yves; Faway, Emilie

doi:10.1159/000534137

Cited by 4 publications

(2 citation statements)

References 56 publications

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“…They are designed to mimic the structure and function of human skin, making them suitable substitutes for animal testing (Duval et al, 2003;Flaten et al, 2015;Kandárová et al, 2006). RHE are the simplest model dedicated to analyze some epidermal properties in vitro (Poumay & Faway, 2023). However, the production of RHE models generally relies on the use of HKGS or other animal-originated (including human-originated) components.…”

Section: Discussionmentioning

confidence: 99%

“…Additionally, considerable problems with the supply of the HKGS product during COVID-19 pandemic occurred, stagnating the research of many scientists in the RHE research field (Poumay & Faway, 2023). To test new alternatives and obtain a wider perspective regarding the use of cdAOF supplements for RHE reconstruction, we tested three different types of human keratinocytes comparing HKGS against the cdAOF supplements.…”

Section: Discussionmentioning

confidence: 99%

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Characterization of Reconstructed Human Epidermis in a Chemically-defined, Animal Origin-free Cell Culture System

Bajsert,

De Glas,

Faway

et al. 2024

Preprint

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The Reconstructed Human Epidermis (RHE) model derived from epidermal keratinocytes offers an ethical and scientifically valid alternative to animal experimentation, particularly in cutaneous toxicology and dermatological research, where elimination of animal cruelty is of paramount importance. Moreover, safer cell- and tissue-based cutaneous therapies are also possible, where the removal of animal-originated products from the RHE culture media lessens the risk of adverse clinical events. Thus, we compared chemically-define animal origin-free (cdAOF) supplements and the historically utilized supplement (HKGS), which contains growth factors and bovine pituitary extract. Herein we present the first extended characterization of RHE using cdAOF culture systems with newborn, adult, and immortalized N/TERT keratinocytes. Culture of RHE in the cdAOF media produced histological features that were nearly identical to that produced using HKGS, with the exception that the basal keratinocytes were less cylindrical, and with some immunolocalization of involucrin in the basal layer. Additionally, increased mRNA expression of several inflammatory-proliferative markers was observed in the cdAOF RHEs as well. Importantly, in RHEs cultured in cdAOF media, expression and immunolocalization of other expected markers of keratinization, as well as monitoring of barrier function revealed results equal or close to those observed in RHE cultured in HKGS.

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