Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library

BACKGROUND: Thyroid hormone receptors (TRs) are critical endocrine receptors that regulate a multitude of processes in adult and developing organisms, and thyroid hormone disruption is of high concern for neurodevelopmental and reproductive toxicities in particular. To date, only a small number of c...

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Autores principales: Paul-Friedman, Katie, Martin, Matt, Crofton, Kevin M., Hsu, Chia-Wen, Sakamuru, Srilatha, Zhao, Jinghua, Xia, Menghang, Huang, Ruili, Stavreva, Diana A., Soni, Vikas, Varticovski, Lyuba, Raziuddin, Razi, Hager, Gordon L., Houck, Keith A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Environmental Health Perspectives 2019
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6792352/
https://www.ncbi.nlm.nih.gov/pubmed/31566444
http://dx.doi.org/10.1289/EHP5314
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author Paul-Friedman, Katie
Martin, Matt
Crofton, Kevin M.
Hsu, Chia-Wen
Sakamuru, Srilatha
Zhao, Jinghua
Xia, Menghang
Huang, Ruili
Stavreva, Diana A.
Soni, Vikas
Varticovski, Lyuba
Raziuddin, Razi
Hager, Gordon L.
Houck, Keith A.
author_facet Paul-Friedman, Katie
Martin, Matt
Crofton, Kevin M.
Hsu, Chia-Wen
Sakamuru, Srilatha
Zhao, Jinghua
Xia, Menghang
Huang, Ruili
Stavreva, Diana A.
Soni, Vikas
Varticovski, Lyuba
Raziuddin, Razi
Hager, Gordon L.
Houck, Keith A.
author_sort Paul-Friedman, Katie
collection PubMed
description BACKGROUND: Thyroid hormone receptors (TRs) are critical endocrine receptors that regulate a multitude of processes in adult and developing organisms, and thyroid hormone disruption is of high concern for neurodevelopmental and reproductive toxicities in particular. To date, only a small number of chemical classes have been identified as possible TR modulators, and the receptors appear highly selective with respect to the ligand structural diversity. Thus, the question of whether TRs are an important screening target for protection of human and wildlife health remains. OBJECTIVE: Our goal was to evaluate the hypothesis that there is limited structural diversity among environmentally relevant chemicals capable of modulating TR activity via the collaborative interagency Tox21 project. METHODS: We screened the Tox21 chemical library (8,305 unique structures) in a quantitative high-throughput, cell-based reporter gene assay for TR agonist or antagonist activity. Active compounds were further characterized using additional orthogonal assays, including mammalian one-hybrid assays, coactivator recruitment assays, and a high-throughput, fluorescent imaging, nuclear receptor translocation assay. RESULTS: Known agonist reference chemicals were readily identified in the TR transactivation assay, but only a single novel, direct agonist was found, the pharmaceutical betamipron. Indirect activation of TR through activation of its heterodimer partner, the retinoid-X-receptor (RXR), was also readily detected by confirmation in an RXR agonist assay. Identifying antagonists with high confidence was a challenge with the presence of significant confounding cytotoxicity and other, non-TR-specific mechanisms common to the transactivation assays. Only three pharmaceuticals—mefenamic acid, diclazuril, and risarestat—were confirmed as antagonists. DISCUSSION: The results support limited structural diversity for direct ligand effects on TR and imply that other potential target sites in the thyroid hormone axis should be a greater priority for bioactivity screening for thyroid axis disruptors. https://doi.org/10.1289/EHP5314
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spelling pubmed-67923522019-11-06 Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library Paul-Friedman, Katie Martin, Matt Crofton, Kevin M. Hsu, Chia-Wen Sakamuru, Srilatha Zhao, Jinghua Xia, Menghang Huang, Ruili Stavreva, Diana A. Soni, Vikas Varticovski, Lyuba Raziuddin, Razi Hager, Gordon L. Houck, Keith A. Environ Health Perspect Research BACKGROUND: Thyroid hormone receptors (TRs) are critical endocrine receptors that regulate a multitude of processes in adult and developing organisms, and thyroid hormone disruption is of high concern for neurodevelopmental and reproductive toxicities in particular. To date, only a small number of chemical classes have been identified as possible TR modulators, and the receptors appear highly selective with respect to the ligand structural diversity. Thus, the question of whether TRs are an important screening target for protection of human and wildlife health remains. OBJECTIVE: Our goal was to evaluate the hypothesis that there is limited structural diversity among environmentally relevant chemicals capable of modulating TR activity via the collaborative interagency Tox21 project. METHODS: We screened the Tox21 chemical library (8,305 unique structures) in a quantitative high-throughput, cell-based reporter gene assay for TR agonist or antagonist activity. Active compounds were further characterized using additional orthogonal assays, including mammalian one-hybrid assays, coactivator recruitment assays, and a high-throughput, fluorescent imaging, nuclear receptor translocation assay. RESULTS: Known agonist reference chemicals were readily identified in the TR transactivation assay, but only a single novel, direct agonist was found, the pharmaceutical betamipron. Indirect activation of TR through activation of its heterodimer partner, the retinoid-X-receptor (RXR), was also readily detected by confirmation in an RXR agonist assay. Identifying antagonists with high confidence was a challenge with the presence of significant confounding cytotoxicity and other, non-TR-specific mechanisms common to the transactivation assays. Only three pharmaceuticals—mefenamic acid, diclazuril, and risarestat—were confirmed as antagonists. DISCUSSION: The results support limited structural diversity for direct ligand effects on TR and imply that other potential target sites in the thyroid hormone axis should be a greater priority for bioactivity screening for thyroid axis disruptors. https://doi.org/10.1289/EHP5314 Environmental Health Perspectives 2019-09-30 /pmc/articles/PMC6792352/ /pubmed/31566444 http://dx.doi.org/10.1289/EHP5314 Text en EHP is an open-access journal published with support from the National Institute of Environmental Health Sciences, National Institutes of Health. All content is public domain unless otherwise noted.
spellingShingle Research
Paul-Friedman, Katie
Martin, Matt
Crofton, Kevin M.
Hsu, Chia-Wen
Sakamuru, Srilatha
Zhao, Jinghua
Xia, Menghang
Huang, Ruili
Stavreva, Diana A.
Soni, Vikas
Varticovski, Lyuba
Raziuddin, Razi
Hager, Gordon L.
Houck, Keith A.
Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title_full Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title_fullStr Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title_full_unstemmed Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title_short Limited Chemical Structural Diversity Found to Modulate Thyroid Hormone Receptor in the Tox21 Chemical Library
title_sort limited chemical structural diversity found to modulate thyroid hormone receptor in the tox21 chemical library
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6792352/
https://www.ncbi.nlm.nih.gov/pubmed/31566444
http://dx.doi.org/10.1289/EHP5314
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