Histone demethylase KDM4A mediating macrophage polarization: A potential mechanism of trichloroethylene induced liver injury

IF 3.3 3区生物学 Q3 CELL BIOLOGY Cell Biology International Pub Date : 2024-05-27 DOI:10.1002/cbin.12187

Jiaxiang Zhang, Hua Huang, Baiwang Ding, Zhibing Liu, Daojun Chen, Shulong Li, Tong Shen, Qixing Zhu

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Abstract

Trichloroethylene (TCE) is a commonly used organic solvent in industry. Our previous studies have found that TCE can cause liver injury accompanied by macrophage polarization, but the specific mechanism is unclear. The epigenetic regulation of macrophage polarization is mainly focused on histone modification. Histone lysine demethylase 4A (KDM4A) is involved in the activation of macrophages. In this study, we used a mouse model we investigated the role of KDM4A in the livers of TCE-drinking mice and found that the expression of KDM4A, M1-type polarization indicators, and related inflammatory factors in the livers of TCE-drinking mice. In the study, BALB/c mice were randomly divided into four groups: 2.5 mg/mL TCE dose group and 5.0 mg/mL TCE dose group, the vehicle control group, and the blank control group. We found that TCE triggered M1 polarization of mouse macrophages, characterized by the expression of CD11c and robust production of inflammatory cytokines. Notably, exposure to TCE resulted in markedly increased expression of KDM4A in macrophages. Functionally, the increased expression of KDM4A significantly impaired the expression of H3K9me3 and H3K9me2 and increased the expression of H3K9me1. In addition, KDM4A potentially represents a novel epigenetic modulator, with its upregulation connected to β-catenin activation, a signal critical for the pro-inflammatory activation of macrophages. Furthermore, KDM4A inhibitor JIB-04 treatment resulted in a decrease in β-catenin expression and prevented TCE-induced M1 polarization and the expression of the pro-inflammatory cytokines TNF-α and IL-1β. These results suggest that the association of KDM4A and Wnt/β-catenin cooperatively establishes the activation and polarization of macrophages and global changes in H3K9me3/me2/me1. Our findings identify KDM4A as an essential regulator of the polarization of macrophages and the expression of inflammatory cytokines, which might serve as a potential target for preventing and treating liver injury caused by TCE.

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组蛋白去甲基化酶 KDM4A 介导巨噬细胞极化：三氯乙烯诱导肝损伤的潜在机制。

三氯乙烯（TCE）是工业中常用的有机溶剂。我们之前的研究发现，三氯乙烯可导致肝损伤并伴有巨噬细胞极化，但具体机制尚不清楚。巨噬细胞极化的表观遗传调控主要集中在组蛋白修饰上。组蛋白赖氨酸去甲基化酶 4A（KDM4A）参与巨噬细胞的活化。本研究利用小鼠模型研究了 KDM4A 在饮用 TCE 小鼠肝脏中的作用，发现 KDM4A、M1 型极化指标及相关炎症因子在饮用 TCE 小鼠肝脏中的表达。研究将 BALB/c 小鼠随机分为四组：2.5 毫克/毫升 TCE 剂量组、5.0 毫克/毫升 TCE 剂量组、车辆对照组和空白对照组。我们发现 TCE 引发了小鼠巨噬细胞的 M1 极化，其特征是 CD11c 的表达和炎症细胞因子的大量产生。值得注意的是，暴露于 TCE 会导致巨噬细胞中 KDM4A 的表达明显增加。从功能上讲，KDM4A 的表达增加会显著降低 H3K9me3 和 H3K9me2 的表达，增加 H3K9me1 的表达。此外，KDM4A可能是一种新型的表观遗传调节剂，其上调与β-catenin的激活有关，而β-catenin是巨噬细胞促炎激活的关键信号。此外，KDM4A抑制剂JIB-04处理可导致β-catenin表达减少，并阻止TCE诱导的M1极化和促炎细胞因子TNF-α和IL-1β的表达。这些结果表明，KDM4A 和 Wnt/β-catenin 的关联合作建立了巨噬细胞的活化和极化以及 H3K9me3/me2/me1 的全局变化。我们的研究结果表明，KDM4A 是巨噬细胞极化和炎性细胞因子表达的重要调节因子，可作为预防和治疗 TCE 引起的肝损伤的潜在靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cell Biology International 生物-细胞生物学

CiteScore

7.60

自引率

0.00%

发文量

208

审稿时长

1 months

期刊介绍： Each month, the journal publishes easy-to-assimilate, up-to-the minute reports of experimental findings by researchers using a wide range of the latest techniques. Promoting the aims of cell biologists worldwide, papers reporting on structure and function - especially where they relate to the physiology of the whole cell - are strongly encouraged. Molecular biology is welcome, as long as articles report findings that are seen in the wider context of cell biology. In covering all areas of the cell, the journal is both appealing and accessible to a broad audience. Authors whose papers do not appeal to cell biologists in general because their topic is too specialized (e.g. infectious microbes, protozoology) are recommended to send them to more relevant journals. Papers reporting whole animal studies or work more suited to a medical journal, e.g. histopathological studies or clinical immunology, are unlikely to be accepted, unless they are fully focused on some important cellular aspect. These last remarks extend particularly to papers on cancer. Unless firmly based on some deeper cellular or molecular biological principle, papers that are highly specialized in this field, with limited appeal to cell biologists at large, should be directed towards journals devoted to cancer, there being very many from which to choose.