Hydroxychloroquine attenuates double-stranded RNA-stimulated hyper-phosphorylation of tristetraprolin/ZFP36 and AU-rich mRNA stabilization

IF 4.9 3区 医学 Q2 IMMUNOLOGY Immunology Pub Date : 2024-07-24 DOI:10.1111/imm.13835
Edward G. Hitti, Zeyad Muazzen, Walid Moghrabi, Suhad Al-Yahya, Khalid S. A. Khabar
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Abstract

The human innate immune system recognizes dsRNA as a pathogen-associated molecular pattern that induces a potent inflammatory response. The primary source of pathogenic dsRNA is cells infected with replicating viruses, but can also be released from uninfected necrotic cells. Here, we show that the dsRNA poly(I:C) challenge in human macrophages activates the p38 MAPK-MK2 signalling pathway and subsequently the phosphorylation of tristetraprolin (TTP/ZFP36). The latter is an mRNA decay-promoting protein that controls the stability of AU-rich mRNAs (AREs) that code for many inflammatory mediators. Hydroxychloroquine (HCQ), a common anti-malaria drug, is used to treat inflammatory and autoimmune disorders and, controversially, during acute COVID-19 disease. We found that HCQ reduced the dsRNA-dependent phosphorylation of p38 MAPK and its downstream kinase MK2. Subsequently, HCQ reduced the abundance and protein stability of the inactive (phosphorylated) form of TTP. HCQ reduced the levels and the mRNA stability of poly (I:C)-induced cytokines and inflammatory mRNAs like TNF, IL-6, COX-2, and IL-8 in THP-1 and primary blood monocytes. Our results demonstrate a new mechanism of the anti-inflammatory role of HCQ at post-transcriptional level (TTP phosphorylation) in a model of dsRNA activation, which usually occurs in viral infections or RNA release from necrotic tissue.

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羟氯喹可减轻双链 RNA 激发的 tristetraprolin/ZFP36 超磷酸化和富含 AU 的 mRNA 稳定。
人类先天性免疫系统可将 dsRNA 识别为病原体相关分子模式,从而诱发强烈的炎症反应。致病性 dsRNA 的主要来源是感染了复制病毒的细胞,但也可能从未感染的坏死细胞中释放出来。在这里,我们发现人巨噬细胞中的 dsRNA poly(I:C) 挑战激活了 p38 MAPK-MK2 信号通路,并随后激活了 tristetraprolin (TTP/ZFP36) 的磷酸化。后者是一种促进 mRNA 衰减的蛋白质,可控制富含 AU 的 mRNA(ARE)的稳定性,而 ARE 是许多炎症介质的编码。羟氯喹(HCQ)是一种常见的抗疟疾药物,可用于治疗炎症和自身免疫性疾病,在急性 COVID-19 疾病期间也有争议。我们发现,HCQ 可减少 p38 MAPK 及其下游激酶 MK2 依赖性 dsRNA 磷酸化。随后,HCQ 降低了 TTP 非活性(磷酸化)形式的丰度和蛋白质稳定性。HCQ 降低了 THP-1 和原代血单核细胞中由 poly (I:C) 诱导的细胞因子和炎症 mRNA(如 TNF、IL-6、COX-2 和 IL-8)的水平和 mRNA 的稳定性。我们的研究结果证明了 HCQ 在转录后水平(TTP 磷酸化)上的抗炎作用的新机制,这种作用通常发生在病毒感染或坏死组织释放 RNA 的 dsRNA 激活模型中。
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来源期刊
Immunology
Immunology 医学-免疫学
CiteScore
11.90
自引率
1.60%
发文量
175
审稿时长
4-8 weeks
期刊介绍: Immunology is one of the longest-established immunology journals and is recognised as one of the leading journals in its field. We have global representation in authors, editors and reviewers. Immunology publishes papers describing original findings in all areas of cellular and molecular immunology. High-quality original articles describing mechanistic insights into fundamental aspects of the immune system are welcome. Topics of interest to the journal include: immune cell development, cancer immunology, systems immunology/omics and informatics, inflammation, immunometabolism, immunology of infection, microbiota and immunity, mucosal immunology, and neuroimmunology. The journal also publishes commissioned review articles on subjects of topical interest to immunologists, and commissions in-depth review series: themed sets of review articles which take a 360° view of select topics at the heart of immunological research.
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