Repressing cytokine storm-like response in macrophages by targeting the eIF2α-integrated stress response pathway

IF 4.8 2区医学 Q2 IMMUNOLOGY

International immunopharmacology Pub Date : 2025-02-06 DOI:10.1016/j.intimp.2024.113965

Xiaoyun Wang , Chaochao Dai , Wen Cheng , Jianli Wang , Xiaopei Cui , Guopin Pan , Ye Chen , Yu Han , Xiaosun Guo , Fan Jiang

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Abstract

Cytokine storm is a life-threatening systemic hyper-inflammatory state caused by different etiologies, in which the bulk production of pro-inflammatory cytokines from activated macrophages has a central role. Integrated stress response (ISR) comprises several protective signaling pathways, leading to phosphorylation of eukaryotic initiation factor 2α (eIF2α) and repression of protein translation. Emerging evidence suggests that ISR induction may elicit anti-inflammatory effects. Currently, however, it is unclear whether targeting eIF2α phosphorylation is sufficient to inhibit the cytokine storm-like response in macrophages. Here we carried out a proof-of-concept study, employing two approaches: (1) ectopic expression of the eIF2α-S51D mutant (mimicking the phosphorylated eIF2α); (2) treatment with salubrinal, a small molecule inhibitor of eIF2α dephosphorylation. Experiments were performed in lipopolysaccharides (LPS)-stimulated macrophages and in murine models with LPS-induced acute endotoxemia. We demonstrated that in macrophages, ectopic expression of eIF2α-S51D, treatment with salubrinal, and gene silencing of PP1/GADD34 (the phosphatase holoenzyme mediating eIF2α dephosphorylation) significantly inhibited LPS-induced cytokine productions without changing their mRNA levels. Polysome PCR and puromycin incorporation assays confirmed that salubrinal suppressed de novo protein translation of the cytokines. In vivo, salubrinal pre-treatment mitigated LPS-induced acute lung injury and significantly reduced the concentration of circulating TNF-α. Salubrinal did not exhibit any effects on the Toll-like receptor 4-mediated signaling or the activation of mammalian target of rapamycin (mTOR). Our data suggest that direct manipulation of eIF2α phosphorylation, thereby bypassing all associated upstream signaling events, may suppress the cytokine storm-like response in activated macrophages, likely by decoupling the gene transcription and protein translation. Inhibiting eIF2α dephosphorylation with small molecule inhibitors may be a viable therapeutic strategy to treat disorders involving cytokine storm-like responses.

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通过eif2 α-整合应激反应途径抑制巨噬细胞细胞因子风暴样反应。

细胞因子风暴是一种由不同病因引起的危及生命的系统性高炎症状态，其中活化的巨噬细胞大量产生促炎细胞因子起着核心作用。综合应激反应（Integrated stress response， ISR）包括多种保护性信号通路，可导致真核起始因子2α (eIF2α)的磷酸化和蛋白质翻译的抑制。新出现的证据表明，ISR诱导可能引起抗炎作用。然而，目前尚不清楚靶向eIF2α磷酸化是否足以抑制巨噬细胞的细胞因子风暴样反应。在这里，我们进行了一项概念验证研究，采用两种方法：(1)异位表达eIF2α- s51d突变体（模仿磷酸化的eIF2α）；(2)用小分子eIF2α去磷酸化抑制剂salubrinal处理。实验在脂多糖（LPS）刺激的巨噬细胞和LPS诱导的急性内毒素血症小鼠模型中进行。我们证明，在巨噬细胞中，eIF2α- s51d的异位表达、salubrinal处理和PP1/GADD34（介导eIF2α去磷酸化的磷酸酶全酶）的基因沉默显著抑制lps诱导的细胞因子产生，而不改变其mRNA水平。聚合体PCR和嘌呤霉素掺入实验证实，钠盐抑制了细胞因子的新生蛋白翻译。在体内，盐水预处理可减轻lps诱导的急性肺损伤，并显著降低循环TNF-α浓度。Salubrinal对toll样受体4介导的信号传导或哺乳动物雷帕霉素靶蛋白（mTOR）的激活没有任何影响。我们的数据表明，直接操纵eIF2α磷酸化，从而绕过所有相关的上游信号事件，可能通过使基因转录和蛋白质翻译脱钩，抑制活化巨噬细胞的细胞因子风暴样反应。用小分子抑制剂抑制eIF2α去磷酸化可能是治疗涉及细胞因子风暴样反应的疾病的一种可行的治疗策略。

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

International immunopharmacology 医学-免疫学

CiteScore

8.40

自引率

3.60%

发文量

935

审稿时长

53 days

期刊介绍： International Immunopharmacology is the primary vehicle for the publication of original research papers pertinent to the overlapping areas of immunology, pharmacology, cytokine biology, immunotherapy, immunopathology and immunotoxicology. Review articles that encompass these subjects are also welcome. The subject material appropriate for submission includes: • Clinical studies employing immunotherapy of any type including the use of: bacterial and chemical agents; thymic hormones, interferon, lymphokines, etc., in transplantation and diseases such as cancer, immunodeficiency, chronic infection and allergic, inflammatory or autoimmune disorders. • Studies on the mechanisms of action of these agents for specific parameters of immune competence as well as the overall clinical state. • Pre-clinical animal studies and in vitro studies on mechanisms of action with immunopotentiators, immunomodulators, immunoadjuvants and other pharmacological agents active on cells participating in immune or allergic responses. • Pharmacological compounds, microbial products and toxicological agents that affect the lymphoid system, and their mechanisms of action. • Agents that activate genes or modify transcription and translation within the immune response. • Substances activated, generated, or released through immunologic or related pathways that are pharmacologically active. • Production, function and regulation of cytokines and their receptors. • Classical pharmacological studies on the effects of chemokines and bioactive factors released during immunological reactions.

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