Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions

All cosmetic ingredients registered in Europe must be evaluated for their safety using non-animal methods. Microphysiological systems (MPS) offer a more complex higher tier model to evaluate chemicals. Having established a skin and liver HUMIMIC Chip2 model demonstrating how dosing scenarios impact...

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Autores principales: Tao, Thi-Phuong, Maschmeyer, Ilka, LeCluyse, Edward L., Rogers, Eda, Brandmair, Katrin, Gerlach, Silke, Przibilla, Julia, Kern, Fredy, Genies, Camille, Jacques, Carine, Najjar, Abdulkarim, Schepky, Andreas, Marx, Uwe, Kühnl, Jochen, Hewitt, Nicola J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9946709/
https://www.ncbi.nlm.nih.gov/pubmed/36843954
http://dx.doi.org/10.3389/fphar.2023.1076254
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author Tao, Thi-Phuong
Maschmeyer, Ilka
LeCluyse, Edward L.
Rogers, Eda
Brandmair, Katrin
Gerlach, Silke
Przibilla, Julia
Kern, Fredy
Genies, Camille
Jacques, Carine
Najjar, Abdulkarim
Schepky, Andreas
Marx, Uwe
Kühnl, Jochen
Hewitt, Nicola J.
author_facet Tao, Thi-Phuong
Maschmeyer, Ilka
LeCluyse, Edward L.
Rogers, Eda
Brandmair, Katrin
Gerlach, Silke
Przibilla, Julia
Kern, Fredy
Genies, Camille
Jacques, Carine
Najjar, Abdulkarim
Schepky, Andreas
Marx, Uwe
Kühnl, Jochen
Hewitt, Nicola J.
author_sort Tao, Thi-Phuong
collection PubMed
description All cosmetic ingredients registered in Europe must be evaluated for their safety using non-animal methods. Microphysiological systems (MPS) offer a more complex higher tier model to evaluate chemicals. Having established a skin and liver HUMIMIC Chip2 model demonstrating how dosing scenarios impact the kinetics of chemicals, we investigated whether thyroid follicles could be incorporated to evaluate the potential of topically applied chemicals to cause endocrine disruption. This combination of models in the HUMIMIC Chip3 is new; therefore, we describe here how it was optimized using two chemicals known to inhibit thyroid production, daidzein and genistein. The MPS was comprised of Phenion(®) Full Thickness skin, liver spheroids and thyroid follicles co-cultured in the TissUse HUMIMIC Chip3. Endocrine disruption effects were determined according to changes in thyroid hormones, thyroxine (T(4)) and 3,3’,5-triiodothyronine (T(3)). A main part of the Chip3 model optimization was the replacement of freshly isolated thyroid follicles with thyrocyte-derived follicles. These were used in static incubations to demonstrate the inhibition of T(4) and T(3) production by genistein and daidzein over 4 days. Daidzein exhibited a lower inhibitory activity than genistein and both inhibitory activities were decreased after a 24 h preincubation with liver spheroids, indicating metabolism was via detoxification pathways. The skin-liver-thyroid Chip3 model was used to determine a consumer-relevant exposure to daidzein present in a body lotion based on thyroid effects. A “safe dose” of 0.235 μg/cm(2) i.e., 0.047% applied in 0.5 mg/cm(2) of body lotion was the highest concentration of daidzein which does not result in changes in T(3) and T(4) levels. This concentration correlated well with the value considered safe by regulators. In conclusion, the Chip3 model enabled the incorporation of the relevant exposure route (dermal), metabolism in the skin and liver, and the bioactivity endpoint (assessment of hormonal balance i.e., thyroid effects) into a single model. These conditions are closer to those in vivo than 2D cell/tissue assays lacking metabolic function. Importantly, it also allowed the assessment of repeated doses of chemical and a direct comparison of systemic and tissue concentrations with toxicodynamic effects over time, which is more realistic and relevant for safety assessment.
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spelling pubmed-99467092023-02-23 Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions Tao, Thi-Phuong Maschmeyer, Ilka LeCluyse, Edward L. Rogers, Eda Brandmair, Katrin Gerlach, Silke Przibilla, Julia Kern, Fredy Genies, Camille Jacques, Carine Najjar, Abdulkarim Schepky, Andreas Marx, Uwe Kühnl, Jochen Hewitt, Nicola J. Front Pharmacol Pharmacology All cosmetic ingredients registered in Europe must be evaluated for their safety using non-animal methods. Microphysiological systems (MPS) offer a more complex higher tier model to evaluate chemicals. Having established a skin and liver HUMIMIC Chip2 model demonstrating how dosing scenarios impact the kinetics of chemicals, we investigated whether thyroid follicles could be incorporated to evaluate the potential of topically applied chemicals to cause endocrine disruption. This combination of models in the HUMIMIC Chip3 is new; therefore, we describe here how it was optimized using two chemicals known to inhibit thyroid production, daidzein and genistein. The MPS was comprised of Phenion(®) Full Thickness skin, liver spheroids and thyroid follicles co-cultured in the TissUse HUMIMIC Chip3. Endocrine disruption effects were determined according to changes in thyroid hormones, thyroxine (T(4)) and 3,3’,5-triiodothyronine (T(3)). A main part of the Chip3 model optimization was the replacement of freshly isolated thyroid follicles with thyrocyte-derived follicles. These were used in static incubations to demonstrate the inhibition of T(4) and T(3) production by genistein and daidzein over 4 days. Daidzein exhibited a lower inhibitory activity than genistein and both inhibitory activities were decreased after a 24 h preincubation with liver spheroids, indicating metabolism was via detoxification pathways. The skin-liver-thyroid Chip3 model was used to determine a consumer-relevant exposure to daidzein present in a body lotion based on thyroid effects. A “safe dose” of 0.235 μg/cm(2) i.e., 0.047% applied in 0.5 mg/cm(2) of body lotion was the highest concentration of daidzein which does not result in changes in T(3) and T(4) levels. This concentration correlated well with the value considered safe by regulators. In conclusion, the Chip3 model enabled the incorporation of the relevant exposure route (dermal), metabolism in the skin and liver, and the bioactivity endpoint (assessment of hormonal balance i.e., thyroid effects) into a single model. These conditions are closer to those in vivo than 2D cell/tissue assays lacking metabolic function. Importantly, it also allowed the assessment of repeated doses of chemical and a direct comparison of systemic and tissue concentrations with toxicodynamic effects over time, which is more realistic and relevant for safety assessment. Frontiers Media S.A. 2023-02-08 /pmc/articles/PMC9946709/ /pubmed/36843954 http://dx.doi.org/10.3389/fphar.2023.1076254 Text en Copyright © 2023 Tao, Maschmeyer, LeCluyse, Rogers, Brandmair, Gerlach, Przibilla, Kern, Genies, Jacques, Najjar, Schepky, Marx, Kühnl and Hewitt. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Tao, Thi-Phuong
Maschmeyer, Ilka
LeCluyse, Edward L.
Rogers, Eda
Brandmair, Katrin
Gerlach, Silke
Przibilla, Julia
Kern, Fredy
Genies, Camille
Jacques, Carine
Najjar, Abdulkarim
Schepky, Andreas
Marx, Uwe
Kühnl, Jochen
Hewitt, Nicola J.
Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title_full Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title_fullStr Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title_full_unstemmed Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title_short Development of a microphysiological skin-liver-thyroid Chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
title_sort development of a microphysiological skin-liver-thyroid chip3 model and its application to evaluate the effects on thyroid hormones of topically applied cosmetic ingredients under consumer-relevant conditions
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9946709/
https://www.ncbi.nlm.nih.gov/pubmed/36843954
http://dx.doi.org/10.3389/fphar.2023.1076254
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