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乙基甲苯在肝细胞模型中调节炎症和细胞纤维化信号传导。

Ethyltoluenes Regulate Inflammatory and Cell Fibrosis Signaling in the Liver Cell Model.

作者信息

Niture Suryakant, Gadi Sashi, Hoang Hieu, Rios-Colon Leslimar, Bodnar Wanda, Levine Keith E, Kumar Deepak

机构信息

The Julius L. Chambers Biomedical/Biotechnology Research Institute (JLC-BBRI), North Carolina Central University (NCCU), Durham, NC 27707, USA.

NCCU-RTI Center for Applied Research in Environmental Sciences (CARES), RTI International, Durham, NC 27707, USA.

出版信息

Toxics. 2024 Nov 27;12(12):856. doi: 10.3390/toxics12120856.

Abstract

Crude oil naphtha fraction C9 alkylbenzenes consist of trimethylbenzenes, ethyltoluenes, cumene, and n-propylbenzene. The major fraction of C9 alkylbenzenes is ethyltoluenes (ETs) consisting of three isomers: 2-ethyltoluene (2-ET), 3-ethyltoluene (3-ET), and 4-ethyltoluene (4-ET). Occupational and environmental exposure to ETs can occur via inhalation and ingestion and cause several health problems. Exposure to ETs causes eye and upper respiratory tract irritation, coughing, gagging, vomiting, griping, diarrhea, distress, and depressed respiration. Previous studies suggest that ETs target the respiratory tract and liver and produce several lesions in the nose, lungs, and liver areas. In the current study, we investigated the impact of low concentrations of ETs on cell metabolism, cell inflammation, steatosis, and fibrosis signaling in liver cell models in vitro. Dose-dependent exposure of 2-ET, 3-ET, and 4-ET to HepaRG and hepatocellular carcinoma (HCC) HepG2 and SK-Hep1 cells affects cell survival/real-time proliferation and increases ROS production. ETs induce inflammatory and gene expression. Exposure of 2-ET, 3-ET, and 4-ET to HepaRG and HCC HepG2 and SK-Hep1 cells affects mitochondrial respiration/cellular energetics and upregulates metabolic and gene expression. However, no significant change in lipogenesis-related gene expression and modulation of cell steatosis was observed after ET exposure. Acute exposure to induvial ETs and in combination or chronic 2-ET exposure alone modulates cell fibrosis markers such as and in liver cell models, suggesting that ETs target liver cells and may dysregulate liver function.

摘要

原油石脑油馏分C9烷基苯由三甲苯、乙苯、异丙苯和正丙苯组成。C9烷基苯的主要馏分为乙苯(ETs),由三种异构体组成:2-乙苯(2-ET)、3-乙苯(3-ET)和4-乙苯(4-ET)。职业和环境接触ETs可通过吸入和摄入发生,并导致多种健康问题。接触ETs会引起眼睛和上呼吸道刺激、咳嗽、作呕、呕吐、腹痛、腹泻、不适和呼吸抑制。先前的研究表明,ETs以呼吸道和肝脏为靶点,并在鼻、肺和肝脏区域产生多种病变。在本研究中,我们在体外肝细胞模型中研究了低浓度ETs对细胞代谢、细胞炎症、脂肪变性和纤维化信号传导的影响。2-ET、3-ET和4-ET对HepaRG和肝癌(HCC)HepG2及SK-Hep1细胞的剂量依赖性暴露会影响细胞存活/实时增殖并增加活性氧(ROS)的产生。ETs可诱导炎症和基因表达。2-ET、3-ET和4-ET对HepaRG和HCC HepG2及SK-Hep1细胞的暴露会影响线粒体呼吸/细胞能量代谢,并上调代谢和基因表达。然而,ET暴露后未观察到脂肪生成相关基因表达的显著变化和细胞脂肪变性的调节。在肝细胞模型中,单独急性暴露于个别ETs及其组合或单独慢性暴露于2-ET会调节细胞纤维化标志物,如 和 ,这表明ETs以肝细胞为靶点,可能会使肝功能失调。

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