Expanded high-throughput screening and chemotype-enrichment analysis of the phase II: e1k ToxCast library for human sodium-iodide symporter (NIS) inhibition

被引:0
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作者
Jun Wang
Ann M. Richard
Ashley S. Murr
Angela R. Buckalew
Ryan R. Lougee
Mahmoud Shobair
Daniel R. Hallinger
Susan C. Laws
Tammy E. Stoker
机构
[1] U.S. Environmental Protection Agency,Neurological and Endocrine Toxicology Branch, Public Health and Integrated Toxicology Division, Center for Public Health & Environmental Assessment, Office of Research and Development
[2] U.S. Department of Energy,Oak Ridge Institute for Science and Education
[3] U.S. Environmental Protection Agency,Computational Chemistry & Cheminformatics Branch, Center for Computational Toxicology & Exposure, Office of Research and Development
来源
Archives of Toxicology | 2021年 / 95卷
关键词
Sodium-iodide symporter; Thyroid; Endocrine disruptor; High-throughput in vitro screening assay; ToxPrint; Chemotype;
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学科分类号
摘要
The sodium-iodide symporter (NIS) mediates the uptake of iodide into the thyroid. Inhibition of NIS function by xenobiotics has been demonstrated to suppress circulating thyroid hormones and perturb related physiological functions. Until recently, few environmental chemicals had been screened for NIS inhibition activity. We previously screened over 1000 chemicals from the ToxCast Phase II (ph1v2 and ph2) libraries using an in vitro radioactive iodide uptake (RAIU) with the hNIS-HEK293T cell line to identify NIS inhibitors. Here, we broaden the chemical space by expanding screening to include the ToxCast e1k library (804 unique chemicals) with initial screening for RAIU at 1 × 10–4 M. Then 209 chemicals demonstrating > 20% RAIU inhibition were further tested in multiple-concentration, parallel RAIU and cell viability assays. This identified 55 chemicals as active, noncytotoxic RAIU inhibitors. Further cytotoxicity-adjusted potency scoring (with NaClO4 having a reference score of 200) revealed five chemicals with moderate to strong RAIU inhibition (scored > 100). These data were combined with our previous PhII screening data to produce binary hit-calls for ~ 1800 unique chemicals (PhII + e1k) with and without cytotoxicity filtering. Results were analyzed with a ToxPrint chemotype-enrichment workflow to identify substructural features significantly enriched in the NIS inhibition hit-call space. We assessed the applicability of enriched PhII chemotypes to prospectively predict NIS inhibition in the e1k dataset. Chemotype enrichments derived for the combined ~ 1800 dataset also identified additional enriched features, as well as chemotypes affiliated with cytotoxicity. These enriched chemotypes provide important new information that can support future data interpretation, structure–activity relationship, chemical use, and regulation.
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页码:1723 / 1737
页数:14
相关论文
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  • [1] Expanded high-throughput screening and chemotype-enrichment analysis of the phase II: e1k ToxCast library for human sodium-iodide symporter (NIS) inhibition
    Wang, Jun
    Richard, Ann M.
    Murr, Ashley S.
    Buckalew, Angela R.
    Lougee, Ryan R.
    Shobair, Mahmoud
    Hallinger, Daniel R.
    Laws, Susan C.
    Stoker, Tammy E.
    [J]. ARCHIVES OF TOXICOLOGY, 2021, 95 (05) : 1723 - 1737
  • [2] High-throughput screening and chemotype-enrichment analysis of ToxCast phase II chemicals evaluated for human sodium-iodide symporter (NIS) inhibition
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    Hallinger, Daniel R.
    Murr, Ashley S.
    Buckalew, Angela R.
    Lougee, Ryan R.
    Richard, Ann M.
    Laws, Susan C.
    Stoker, Tammy E.
    [J]. ENVIRONMENT INTERNATIONAL, 2019, 126 : 377 - 386
  • [3] High-Throughput Screening and Quantitative Chemical Ranking for Sodium-Iodide Symporter Inhibitors in ToxCast Phase I Chemical Library
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    Buckalew, Angela R.
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    [J]. ENVIRONMENTAL SCIENCE & TECHNOLOGY, 2018, 52 (09) : 5417 - 5426
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