A novel three-dimensional Nrf2 reporter epidermis model for skin sensitization assessment

K Brandmair; D Dising; D Finkelmeier; A Schepky; J Kuehnl; J Ebmeyer; A Burger-Kentischer

doi:10.1016/j.tox.2024.153743

A novel three-dimensional Nrf2 reporter epidermis model for skin sensitization assessment

Toxicology. 2024 Mar:503:153743. doi: 10.1016/j.tox.2024.153743. Epub 2024 Feb 9.

Authors

K Brandmair¹, D Dising², D Finkelmeier², A Schepky¹, J Kuehnl¹, J Ebmeyer³, A Burger-Kentischer⁴

Affiliations

¹ Beiersdorf AG, Beiersdorfstraße 1-9, Hamburg 20245, Germany.
² Fraunhofer Institute for Interfacial Engineering and Biotechnology IGB, Cell and Tissue Technologies, Nobelstraße 12, Stuttgart 70569, Germany.
³ Beiersdorf AG, Beiersdorfstraße 1-9, Hamburg 20245, Germany. Electronic address: Johanna.Ebmeyer@Beiersdorf.com.
⁴ Fraunhofer Institute for Interfacial Engineering and Biotechnology IGB, Cell and Tissue Technologies, Nobelstraße 12, Stuttgart 70569, Germany. Electronic address: Anke.BurgerKentischer@igb.fraunhofer.de.

PMID: 38341018
DOI: 10.1016/j.tox.2024.153743

Abstract

Skin sensitization assessment has progressed from the use of animal models towards the application of New Approach Methodologies (NAMs). Several skin sensitization NAMs are accepted for regulatory use, but a majority relies on submerged in vitro cell cultures that limit their applicability domain, posing challenges for testing hydrophobic chemicals and mixtures. A newly developed three-dimensional (3D) Nrf2 reporter epidermis model for skin sensitization assessment is reported. This NAM may help to overcome these limitations. The NAM combines the in vivo-like biology and exposure conditions of 3D epidermis models with the reliability, convenience, and cost-effectiveness of secreted reporter gene technology. The Keap1-Nrf2-ARE pathway was chosen as the reporter gene read-out, as it is induced by most skin sensitizers and already adopted in OECD Test guideline 442D. Immortalized human primary keratinocytes (Ker-CT) were stably transfected with the pIGB-Nrf2-SEAP vector to construct a Nrf2 reporter cell line. Ker-CT Nrf2 reporter cells showed negligible basal expression of the Secreted Embryonic Alkaline Phosphatase (SEAP) reporter, which was induced 13.5-fold by exposure to the skin sensitizer cinnamic aldehyde (CA). Co-exposure to CA and the Nrf2 inhibitor glucocorticoid clobetasol propionate significantly suppressed the CA-induced SEAP expression, confirming dependance of the SEAP expression on Nrf2 activation. Using air-liquid interface and animal constituent free culture conditions, the Ker-CT Nrf2 reporter cells differentiated to stratified 3D epidermis models with an in vivo-like skin architecture and functional skin barrier. Evaluation of a Ker-CT Nrf2 reporter cell-based 2D assay by testing 10 conventional reference chemicals showed a predictive accuracy for skin sensitization potential of 80% and 70% compared to LLNA and human data in two independent laboratories and a high intra- and interlaboratory reproducibility. Moreover, the 3D epidermis models predicted 3 sensitizing and 2 non-sensitizing reference chemicals correctly in a first proof-of-concept study. Further investigations foresee the testing of additional chemicals, including hydrophobic compounds and mixtures to confirm the potential of the 3D epidermis models to broaden the applicability domain for NAM-based skin sensitization assessment.

Keywords: 3D epidermis model; Nrf2; Skin sensitization; applicability domain; new approach methodology; reporter gene.

MeSH terms

Animal Testing Alternatives
Animals
Dermatitis, Allergic Contact*
Epidermis / metabolism
Humans
Kelch-Like ECH-Associated Protein 1 / metabolism
Keratinocytes / metabolism
Local Lymph Node Assay
NF-E2-Related Factor 2* / metabolism
Reproducibility of Results
Skin / metabolism

Substances

NF-E2-Related Factor 2
Kelch-Like ECH-Associated Protein 1