Pterostilbene improves neurological dysfunction and neuroinflammation after ischaemic stroke via HDAC3/Nrf1-mediated microglial activation.

IF 9.2 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Cellular & Molecular Biology Letters Pub Date : 2024-08-28 DOI:10.1186/s11658-024-00634-1
Yuhua Chen, Wei He, Junlin Qiu, Yangyang Luo, Chenlong Jiang, Feng Zhao, Hong Wei, Jiao Meng, Tianlin Long, Xin Zhang, Lingjian Yang, Quanhua Xu, Juning Wang, Chi Zhang
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Abstract

Background: Stroke is a type of acute brain damage that can lead to a series of serious public health challenges. Demonstrating the molecular mechanism of stroke-related neural cell degeneration could help identify a more efficient treatment for stroke patients. Further elucidation of factors that regulate microglia and nuclear factor (erythroid-derived 2)-like 1 (Nrf1) may lead to a promising strategy for treating neuroinflammation after ischaemic stroke. In this study, we investigated the possible role of pterostilbene (PTS) in Nrf1 regulation in cell and animal models of ischaemia stroke.

Methods: We administered PTS, ITSA1 (an HDAC activator) and RGFP966 (a selective HDAC3 inhibitor) in a mouse model of middle cerebral artery occlusion-reperfusion (MCAO/R) and a model of microglial oxygen‒glucose deprivation/reperfusion (OGD/R). The brain infarct size, neuroinflammation and microglial availability were also determined. Dual-luciferase reporter, Nrf1 protein stability and co-immunoprecipitation assays were conducted to analyse histone deacetylase 3 (HDAC3)/Nrf1-regulated Nrf1 in an OGD/R-induced microglial injury model.

Results: We found that PTS decreased HDAC3 expression and activity, increased Nrf1 acetylation in the cell nucleus and inhibited the interaction of Nrf1 with p65 and p65 accumulation, which reduced infarct volume and neuroinflammation (iNOS/Arg1, TNF-α and IL-1β levels) after ischaemic stroke. Furthermore, the CSF1R inhibitor PLX5622 induced elimination of microglia and attenuated the therapeutic effect of PTS following MCAO/R. In the OGD/R model, PTS relieved OGD/R-induced microglial injury and TNF-α and IL-1β release, which were dependent on Nrf1 acetylation through the upregulation of HDAC3/Nrf1 signalling in microglia. However, the K105R or/and K139R mutants of Nrf1 counteracted the impact of PTS in the OGD/R-induced microglial injury model, which indicates that PTS treatment might be a promising strategy for ischaemia stroke therapy.

Conclusion: The HDAC3/Nrf1 pathway regulates the stability and function of Nrf1 in microglial activation and neuroinflammation, which may depend on the acetylation of the lysine 105 and 139 residues in Nrf1. This mechanism was first identified as a potential regulatory mechanism of PTS-based neuroprotection in our research, which may provide new insight into further translational applications of natural products such as PTS.

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紫檀芪通过 HDAC3/Nrf1 介导的微神经胶质细胞活化改善缺血性中风后的神经功能紊乱和神经炎症。
背景:中风是一种急性脑损伤,可导致一系列严重的公共卫生问题。阐明中风相关神经细胞变性的分子机制有助于为中风患者找到更有效的治疗方法。进一步阐明小胶质细胞和类(红细胞衍生 2)核因子 1(Nrf1)的调控因子,可能会为治疗缺血性中风后的神经炎症提供一种有前景的策略。本研究探讨了紫檀芪(PTS)在缺血性中风细胞和动物模型中调节 Nrf1 的可能作用:方法:我们在大脑中动脉闭塞-再灌注(MCAO/R)小鼠模型和小胶质细胞缺氧-葡萄糖再灌注(OGD/R)模型中施用了 PTS、ITSA1(一种 HDAC 激活剂)和 RGFP966(一种选择性 HDAC3 抑制剂)。同时还测定了脑梗塞大小、神经炎症和小胶质细胞的可用性。在OGD/R诱导的小胶质细胞损伤模型中,通过双荧光素酶报告、Nrf1蛋白稳定性和共免疫沉淀实验分析组蛋白去乙酰化酶3(HDAC3)/Nrf1调控的Nrf1:结果:我们发现,PTS能降低HDAC3的表达和活性,增加细胞核中Nrf1的乙酰化,抑制Nrf1与p65的相互作用和p65的积累,从而减少缺血性脑卒中后的梗死体积和神经炎症(iNOS/Arg1、TNF-α和IL-1β水平)。此外,CSF1R抑制剂PLX5622可诱导小胶质细胞的清除,并减弱MCAO/R后PTS的治疗效果。在OGD/R模型中,PTS缓解了OGD/R诱导的小胶质细胞损伤以及TNF-α和IL-1β的释放,这依赖于通过上调小胶质细胞中的HDAC3/Nrf1信号的Nrf1乙酰化。然而,Nrf1的K105R或/和K139R突变体在OGD/R诱导的小胶质细胞损伤模型中抵消了PTS的影响,这表明PTS治疗可能是缺血中风治疗的一种有前途的策略:HDAC3/Nrf1通路调节Nrf1在小胶质细胞激活和神经炎症中的稳定性和功能,这可能取决于Nrf1中赖氨酸105和139残基的乙酰化。 我们的研究首次发现了这一机制是基于PTS的神经保护的潜在调控机制,这可能为PTS等天然产物的进一步转化应用提供了新的见解。
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来源期刊
Cellular & Molecular Biology Letters
Cellular & Molecular Biology Letters 生物-生化与分子生物学
CiteScore
11.60
自引率
13.30%
发文量
101
审稿时长
3 months
期刊介绍: Cellular & Molecular Biology Letters is an international journal dedicated to the dissemination of fundamental knowledge in all areas of cellular and molecular biology, cancer cell biology, and certain aspects of biochemistry, biophysics and biotechnology.
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