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NR4A1的重新激活抑制软骨细胞炎症并改善大鼠骨关节炎

Reactivation of NR4A1 Restrains Chondrocyte Inflammation and Ameliorates Osteoarthritis in Rats.

作者信息

Xiong Yan, Ran Jisheng, Xu Langhai, Tong Zhou, Adel Abdo Moqbel Safwat, Ma Chiyuan, Xu Kai, He Yuzhe, Wu Zhipeng, Chen Zhonggai, Hu Pengfei, Jiang Lifeng, Bao Jiapeng, Chen Weiping, Wu Lidong

机构信息

Department of Orthopedic Surgery, The Second Affiliated Hospital, School of Medicine, Zhejiang University, Hangzhou, China.

Department of Medical Oncology, The First Affiliated Hospital, Zhejiang University School of Medicine, Hangzhou, China.

出版信息

Front Cell Dev Biol. 2020 Mar 17;8:158. doi: 10.3389/fcell.2020.00158. eCollection 2020.

DOI:10.3389/fcell.2020.00158

PMID:32258036

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7090231/

Abstract

Osteoarthritis (OA) is the most prevalent joint disease and uncontrolled inflammation is now recognized to play vital roles in OA development. Targeting the endogenous counterpart of inflammation may develop new therapeutic approaches in resolving inflammation persistence and treating inflammatory disease including OA. The orphan nuclear receptor 4A1 (NR4A1) is a key negative regulator of inflammatory responses but its role in osteoarthritis remains unclear. In the present study, we found that the NR4A1 expression was elevated in human osteoarthritis cartilage and OA model, which could be blocked by NF-κB signal inhibitor JSH23. The overexpression of NR4A1 inhibited, whereas knockdown of NR4A1 enhanced IL-1β induced COX-2, iNOS, MMP3, MMP9 and MMP13 expression, and luciferase reporter activity of NF-κB response element. Though NR4A1 was upregulated in inflammatory stimulation and creates a negative feedback loop, persistent inflammatory stimulation inhibited NR4A1 expression and activation. The expression of NR4A1 declined rapidly after an initial peak in conditions of chronic IL-1β stimulation, which could be partially restored by HDACs inhibitor SAHA. The phosphorylation of NR4A1 was increased in human osteoarthritis cartilage, and p38 inhibitor SB203580, JNK inhibitor SP600125 and ERK inhibitor FR180204 could significantly inhibited IL-1β induced NR4A1 phosphorylation. Reactivation of NR4A1 by its agonist cytosporone B could inhibit IL-1β induced chondrocyte inflammation and expression of COX-2, iNOS, MMP3, MMP9, and MMP13. In rat OA model, intra-articular injection of cytosporone B protected cartilage damage and ameliorated osteoarthritis. Thus, our study demonstrated that the NR4A1 is a key endogenous inhibitor of chondrocyte inflammation, which was relatively inactivated under chronic inflammatory stimulation through HDACs mediated transcriptional suppression and MAKP dependent phosphorylation in osteoarthritis. NR4A1 agonist cytosporone B could reactivate and restore the inhibitory regulatory ability of NR4A1, prevent excessive inflammation, and ameliorates osteoarthritis.

摘要

骨关节炎（OA）是最常见的关节疾病，目前已认识到不受控制的炎症在OA发展中起着至关重要的作用。针对炎症的内源性对应物可能会开发出新的治疗方法，以解决炎症持续存在的问题并治疗包括OA在内的炎症性疾病。孤儿核受体4A1（NR4A1）是炎症反应的关键负调节因子，但其在骨关节炎中的作用仍不清楚。在本研究中，我们发现NR4A1在人骨关节炎软骨和OA模型中表达升高，这可被NF-κB信号抑制剂JSH23阻断。NR4A1的过表达抑制了IL-1β诱导的COX-2、iNOS、MMP3、MMP9和MMP13的表达以及NF-κB反应元件的荧光素酶报告活性，而敲低NR4A1则增强了这些表达。虽然NR4A1在炎症刺激中上调并形成负反馈环，但持续的炎症刺激会抑制NR4A1的表达和激活。在慢性IL-1β刺激条件下，NR4A1的表达在最初达到峰值后迅速下降，HDACs抑制剂SAHA可部分恢复其表达。在人骨关节炎软骨中，NR4A1的磷酸化增加，p38抑制剂SB203580、JNK抑制剂SP600125和ERK抑制剂FR180204可显著抑制IL-1β诱导的NR4A1磷酸化。其激动剂环孢菌素B对NR4A1的再激活可抑制IL-1β诱导的软骨细胞炎症以及COX-2、iNOS、MMP3、MMP9和MMP13的表达。在大鼠OA模型中，关节内注射环孢菌素B可保护软骨损伤并改善骨关节炎。因此，我们的研究表明，NR4A1是软骨细胞炎症的关键内源性抑制剂，在骨关节炎中，它通过HDACs介导的转录抑制和MAKP依赖性磷酸化在慢性炎症刺激下相对失活。NR4A1激动剂环孢菌素B可重新激活并恢复NR4A1的抑制调节能力

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b48/7090231/5587d12539f8/fcell-08-00158-g001.jpg

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NR4A1的重新激活抑制软骨细胞炎症并改善大鼠骨关节炎

Reactivation of NR4A1 Restrains Chondrocyte Inflammation and Ameliorates Osteoarthritis in Rats.

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