Comprehensive Evaluation System for Post-Metabolic Activity of Potential Thyroid-Disrupting Chemicals

Yurim Jang; Ji Hyun Moon; Byung Kwan Jeon; Ho Jin Park; Hong Jin Lee; Do Yup Lee

doi:10.4014/jmb.2301.01036

Comprehensive Evaluation System for Post-Metabolic Activity of Potential Thyroid-Disrupting Chemicals

J Microbiol Biotechnol. 2023 Oct 28;33(10):1351-1360. doi: 10.4014/jmb.2301.01036. Epub 2023 Jun 12.

Authors

Yurim Jang¹, Ji Hyun Moon², Byung Kwan Jeon³, Ho Jin Park⁴, Hong Jin Lee⁴, Do Yup Lee^{1

2

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Affiliations

¹ Interdisciplinary Program in Agricultural Genomics, Seoul National University, Seoul 08826, Republic of Korea.
² Department of Agricultural Biotechnology, Seoul National University, Seoul 08826, Republic of Korea.
³ Department of Bio and Fermentation Convergence Technology, Kookmin University, Seoul 02707, Republic of Korea.
⁴ Department of Food Science and Biotechnology, Chung-Ang University, Anseong 17546, Republic of Korea.
⁵ Center for Food and Bioconvergence, and Research Institute of Agriculture and Life Sciences, CALS, Seoul National University, Seoul 08826, Republic of Korea.

Abstract

Endocrine-disrupting chemicals (EDCs) are compounds that disturb hormonal homeostasis by binding to receptors. EDCs are metabolized through hepatic enzymes, causing altered transcriptional activities of hormone receptors, and thus necessitating the exploration of the potential endocrine-disrupting activities of EDC-derived metabolites. Accordingly, we have developed an integrative workflow for evaluating the post-metabolic activity of potential hazardous compounds. The system facilitates the identification of metabolites that exert hormonal disruption through the integrative application of an MS/MS similarity network and predictive biotransformation based on known hepatic enzymatic reactions. As proof-of-concept, the transcriptional activities of 13 chemicals were evaluated by applying the in vitro metabolic module (S9 fraction). Identified among the tested chemicals were three thyroid hormone receptor (THR) agonistic compounds that showed increased transcriptional activities after phase I+II reactions (T3, 309.1 ± 17.3%; DITPA, 30.7 ± 1.8%; GC-1, 160.6 ± 8.6% to the corresponding parents). The metabolic profiles of these three compounds showed common biotransformation patterns, particularly in the phase II reactions (glucuronide conjugation, sulfation, GSH conjugation, and amino acid conjugation). Data-dependent exploration based on molecular network analysis of T3 profiles revealed that lipids and lipid-like molecules were the most enriched biotransformants. The subsequent subnetwork analysis proposed 14 additional features, including T4 in addition to 9 metabolized compounds that were annotated by prediction system based on possible hepatic enzymatic reaction. The other 10 THR agonistic negative compounds showed unique biotransformation patterns according to structural commonality, which corresponded to previous in vivo studies. Our evaluation system demonstrated highly predictive and accurate performance in determining the potential thyroid-disrupting activity of EDC-derived metabolites and for proposing novel biotransformants.

Keywords: Thyroid-disrupting chemical; biotransformant prediction; metabolomics; molecular networking; reporter gene assay.

MeSH terms

Biotransformation
Tandem Mass Spectrometry*
Thyroid Gland*