化学信息学交叉阅读法揭示紫外线滤光片 Cinoxate 是一种致肥性过氧化物酶体增殖激活受体 γ 激动剂

IF 3.7 3区 医学 Q2 CHEMISTRY, MEDICINAL
Seungchan An, In Guk Park, Seok Young Hwang, Junpyo Gong, Yeonjin Lee, Sungjin Ahn and Minsoo Noh*, 
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引用次数: 0

摘要

本研究介绍了一种新颖的化学信息学交叉阅读方法,旨在识别潜在的环境肥胖原,即主要通过影响核荷尔蒙受体(NRs)来扰乱新陈代谢和诱发肥胖的物质。利用从 8435 种 Tox21 化合物的化学指纹中提取的实值二维特征,通过聚类分析和随后的统计测试,发现了 385 个富含与特定 NR 靶点相关的化合物的聚类。值得注意的是,有一个聚类在过氧化物酶体增殖激活受体γ(PPARγ)激动剂活性方面表现出选择性富集,其突出特点是甲氧基肉桂酸盐紫外线(UV)过滤剂和肥胖原相关化合物。实验验证证实,4-甲氧基肉桂酸 2-乙氧基乙基酯(一种有机紫外线滤光剂)可选择性地与 PPARγ 结合(Ki = 18.0 μM),在人骨髓间充质干细胞的致肥分化过程中诱发肥胖表型。分子对接和进一步的实验发现,寅草酸盐是一种强效的 PPARγ 完全激动剂,表明其偏好于辅助激活剂 SRC3 的招募。此外,在临床使用过程中接触到的正常人表皮角质细胞原代细胞中,cinoxate 能上调编码脂质代谢酶基因的转录水平。这项研究提供了令人信服的证据,证明了化学信息学交叉分析在确定潜在肥胖源的优先次序方面的功效,并展示了它在揭示氨甲环酸作为一种致肥 PPARγ 激动剂方面的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Cheminformatic Read-Across Approach Revealed Ultraviolet Filter Cinoxate as an Obesogenic Peroxisome Proliferator-Activated Receptor γ Agonist

Cheminformatic Read-Across Approach Revealed Ultraviolet Filter Cinoxate as an Obesogenic Peroxisome Proliferator-Activated Receptor γ Agonist

This study introduces a novel cheminformatic read-across approach designed to identify potential environmental obesogens, substances capable of disrupting metabolism and inducing obesity by mainly influencing nuclear hormone receptors (NRs). Leveraging real-valued two-dimensional features derived from chemical fingerprints of 8435 Tox21 compounds, cluster analysis and subsequent statistical testing revealed 385 clusters enriched with compounds associated with specific NR targets. Notably, one cluster exhibited selective enrichment in peroxisome proliferator-activated receptor γ (PPARγ) agonist activity, prominently featuring methoxy cinnamate ultraviolet (UV) filters and obesogen-related compounds. Experimental validation confirmed that 2-ethoxyethyl 4-methoxycinnamate, an organic UV filter cinoxate, could selectively bind to PPARγ (Ki = 18.0 μM), eliciting an obesogenic phenotype in human bone marrow-derived mesenchymal stem cells during adipogenic differentiation. Molecular docking and further experiments identified cinoxate as a potent PPARγ full agonist, demonstrating a preference for coactivator SRC3 recruitment. Moreover, cinoxate upregulated transcription levels of genes encoding lipid metabolic enzymes in normal human epidermal keratinocytes as primary cells exposed during clinical usage. This study provides compelling evidence for the efficacy of cheminformatic read-across analysis in prioritizing potential obesogens, showcasing its utility in unveiling cinoxate as an obesogenic PPARγ agonist.

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来源期刊
CiteScore
7.90
自引率
7.30%
发文量
215
审稿时长
3.5 months
期刊介绍: Chemical Research in Toxicology publishes Articles, Rapid Reports, Chemical Profiles, Reviews, Perspectives, Letters to the Editor, and ToxWatch on a wide range of topics in Toxicology that inform a chemical and molecular understanding and capacity to predict biological outcomes on the basis of structures and processes. The overarching goal of activities reported in the Journal are to provide knowledge and innovative approaches needed to promote intelligent solutions for human safety and ecosystem preservation. The journal emphasizes insight concerning mechanisms of toxicity over phenomenological observations. It upholds rigorous chemical, physical and mathematical standards for characterization and application of modern techniques.
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