内皮素-1 通过破坏 HDAC2/Sin3A/MeCP2 核心抑制复合物诱导人肺成纤维细胞结缔组织生长因子表达。
Endothelin-1 induces connective tissue growth factor expression in human lung fibroblasts by disrupting HDAC2/Sin3A/MeCP2 corepressor complex.
机构信息
Graduate Institute of Medical Sciences, College of Medicine, Taipei Medical University, 250 Wu-Hsing Street, Taipei, 110, Taiwan.
Research Center of Thoracic Medicine, Taipei Medical University, Taipei, Taiwan.
出版信息
J Biomed Sci. 2023 Jun 14;30(1):40. doi: 10.1186/s12929-023-00931-5.
BACKGROUND
Reduction of histone deacetylase (HDAC) 2 expression and activity may contribute to amplified inflammation in patients with severe asthma. Connective tissue growth factor (CTGF) is a key mediator of airway fibrosis in severe asthma. However, the role of the HDAC2/Sin3A/methyl-CpG-binding protein (MeCP) 2 corepressor complex in the regulation of CTGF expression in lung fibroblasts remains unclear.
METHODS
The role of the HDAC2/Sin3A/MeCP2 corepressor complex in endothelin (ET)-1-stimulated CTGF production in human lung fibroblasts (WI-38) was investigated. We also evaluated the expression of HDAC2, Sin3A and MeCP2 in the lung of ovalbumin-induced airway fibrosis model.
RESULTS
HDAC2 suppressed ET-1-induced CTGF expression in WI-38 cells. ET-1 treatment reduced HDAC2 activity and increased H3 acetylation in a time-dependent manner. Furthermore, overexpression of HDAC2 inhibited ET-1-induced H3 acetylation. Inhibition of c-Jun N-terminal kinase, extracellular signal-regulated kinase, or p38 attenuated ET-1-induced H3 acetylation by suppressing HDAC2 phosphorylation and reducing HDAC2 activity. Overexpression of both Sin3A and MeCP2 attenuated ET-1-induced CTGF expression and H3 acetylation. ET-1 induced the disruption of the HDAC2/Sin3A/MeCP2 corepressor complex and then prompted the dissociation of HDAC2, Sin3A, and MeCP2 from the CTGF promoter region. Overexpression of HDAC2, Sin3A, or MeCP2 attenuated ET-1-stimulated AP-1-luciferase activity. Moreover, Sin3A- or MeCP2-suppressed ET-1-induced H3 acetylation and AP-1-luciferase activity were reversed by transfection of HDAC2 siRNA. In an ovalbumin-induced airway fibrosis model, the protein levels of HDAC2 and Sin3A were lower than in the control group; however, no significant difference in MeCP2 expression was observed. The ratio of phospho-HDAC2/HDAC2 and H3 acetylation in the lung tissue were higher in this model than in the control group. Overall, without stimulation, the HDAC2/Sin3A/MeCP2 corepressor complex inhibits CTGF expression by regulating H3 deacetylation in the CTGF promoter region in human lung fibroblasts. With ET-1 stimulation, the HDAC2/Sin3A/MeCP2 corepressor complex is disrupted and dissociated from the CTGF promoter region; this is followed by AP-1 activation and the eventual initiation of CTGF production.
CONCLUSIONS
The HDAC2/Sin3A/MeCP2 corepressor complex is an endogenous inhibitor of CTGF in lung fibroblasts. Additionally, HDAC2 and Sin3A may be of greater importance than MeCP2 in the pathogenesis of airway fibrosis.
背景
组蛋白去乙酰化酶(HDAC)2 表达和活性的减少可能导致严重哮喘患者的炎症加剧。结缔组织生长因子(CTGF)是严重哮喘气道纤维化的关键介质。然而,HDAC2/Sin3A/甲基-CpG 结合蛋白(MeCP)2 核心抑制复合物在调节肺成纤维细胞中 CTGF 表达中的作用仍不清楚。
方法
研究了 HDAC2/Sin3A/MeCP2 核心抑制复合物在内皮素(ET)-1 刺激人肺成纤维细胞(WI-38)中 CTGF 产生中的作用。我们还评估了卵清蛋白诱导的气道纤维化模型中肺组织中 HDAC2、Sin3A 和 MeCP2 的表达。
结果
HDAC2 抑制 ET-1 诱导的 WI-38 细胞中 CTGF 的表达。ET-1 处理以时间依赖性方式降低 HDAC2 活性并增加 H3 乙酰化。此外,HDAC2 的过表达抑制 ET-1 诱导的 H3 乙酰化。c-Jun N-末端激酶、细胞外信号调节激酶或 p38 的抑制通过抑制 HDAC2 磷酸化和降低 HDAC2 活性来减弱 ET-1 诱导的 H3 乙酰化。Sin3A 和 MeCP2 的过表达均减弱 ET-1 诱导的 CTGF 表达和 H3 乙酰化。ET-1 诱导 HDAC2/Sin3A/MeCP2 核心抑制复合物的破坏,随后 HDAC2、Sin3A 和 MeCP2 从 CTGF 启动子区域解离。HDAC2、Sin3A 或 MeCP2 的过表达减弱 ET-1 刺激的 AP-1 荧光素酶活性。此外,Sin3A 或 MeCP2 抑制的 ET-1 诱导的 H3 乙酰化和 AP-1 荧光素酶活性通过转染 HDAC2 siRNA 得到逆转。在卵清蛋白诱导的气道纤维化模型中,HDAC2 和 Sin3A 的蛋白水平低于对照组;然而,MeCP2 的表达没有明显差异。该模型中肺组织中磷酸化-HDAC2/HDAC2 和 H3 乙酰化的比值高于对照组。总的来说,在没有刺激的情况下,HDAC2/Sin3A/MeCP2 核心抑制复合物通过调节 CTGF 启动子区域的 H3 去乙酰化来抑制人肺成纤维细胞中 CTGF 的表达。在 ET-1 刺激下,HDAC2/Sin3A/MeCP2 核心抑制复合物被破坏并从 CTGF 启动子区域解离;随后激活 AP-1,最终启动 CTGF 产生。
结论
HDAC2/Sin3A/MeCP2 核心抑制复合物是肺成纤维细胞中 CTGF 的内源性抑制剂。此外,HDAC2 和 Sin3A 在气道纤维化发病机制中的重要性可能高于 MeCP2。
Zotero 插件