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基于转录组学对磷酸二(2-乙基己基)苯酯诱导的肝毒性及其在人肝细胞中的潜在代谢途径的评估

Evaluation of hepatotoxicity induced by 2-ethylhexyldiphenyl phosphate based on transcriptomics and its potential metabolism pathway in human hepatocytes.

作者信息

Zhu Lingfei, Huang Xiaohan, Li Zhenhua, Cao Gang, Zhu Xuanjin, She Shaohua, Huang Tenghao, Lu Gang

机构信息

Guangdong Key Laboratory of Environmental Pollution and Health, School of Environment, Jinan University, Guangzhou 510632, China.

The First Affiliated Hospital, Biomedical Translational Research Institute and School of Pharmacy, Jinan University, Guangzhou 510632, China.

出版信息

J Hazard Mater. 2021 Jul 5;413:125281. doi: 10.1016/j.jhazmat.2021.125281. Epub 2021 Jan 30.

DOI:10.1016/j.jhazmat.2021.125281
PMID:33582465
Abstract

Increasing use of organophosphorus flame retardants (OPFRs) has aroused great concern to their uncertain environment risk, especially to human health risk. In our study, hepatotoxicity screening of six aryl-OPFRs, potential hepatotoxicity mechanism of 2-ethylhexyldiphenyl phosphate (EHDPP) using RNA-sequencing and its metabolites were investigated in human hepatocytes (L02). The toxicity results demonstrated that EHDPP should be prioritized for further research with the highest toxicity. Further RNA-seq results through GO and KEGG enrichment analysis indicated that exposure to 10 mg/L of EHDPP significantly affected energy homeostasis, endoplasmic reticulum (ER) stress, apoptosis, cell cycle, and inflammation response in cells. The top 12 hub genes were validated by RT-qPCR and conformed to be mainly related to glycolysis and ER stress, followed by cell cycle and inflammation response. Western blot, apoptosis detection, glycolysis stress test, and cell cycle analysis were further performed to verify the above main pathways. Additionally, it was found in the metabolism experiment that detoxification of EHDPP by phase I and phase II metabolism in cells wasn't significant until 48 h with a metabolic rate of 6.12%. EHDPP was stable and still dominated the induction of toxicity. Overall, this study provided valuable information regarding the toxicity and potential metabolism pathway of EHDPP.

摘要

有机磷阻燃剂(OPFRs)使用的增加引发了人们对其不确定的环境风险,尤其是对人类健康风险的高度关注。在我们的研究中,对六种芳基OPFRs进行了肝毒性筛查,利用RNA测序研究了磷酸2-乙基己基二苯基酯(EHDPP)在人肝细胞(L02)中的潜在肝毒性机制及其代谢产物。毒性结果表明,EHDPP毒性最高,应优先进行进一步研究。通过GO和KEGG富集分析的进一步RNA测序结果表明,暴露于10mg/L的EHDPP会显著影响细胞中的能量稳态、内质网(ER)应激、凋亡、细胞周期和炎症反应。通过RT-qPCR验证了前12个关键基因,结果表明它们主要与糖酵解和内质网应激有关,其次是细胞周期和炎症反应。进一步进行蛋白质免疫印迹、凋亡检测、糖酵解应激试验和细胞周期分析以验证上述主要途径。此外,在代谢实验中发现,细胞中EHDPP的I相和II相代谢解毒作用直到48小时才显著,代谢率为6.12%。EHDPP稳定,仍然主导毒性诱导。总体而言,本研究提供了有关EHDPP毒性和潜在代谢途径的有价值信息。

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