Opposing regulation of TNF responses by IFN-γ and a PGE2-cAMP axis that is apparent in rheumatoid and immune checkpoint inhibitor-induced arthritis human IL-1β+ macrophages.

IF 6.4 1区生物学 Q1 BIOLOGY

eLife Pub Date : 2025-07-15 DOI:10.7554/eLife.104367

Upneet K Sokhi, Ruoxi Yuan, Bikash Mishra, Yurii Chinenov, Anvita Singaraju, Karmela K Chan, Anne Bass, Richard D Bell, Laura Donlin, Lionel B Ivashkiv

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引用次数: 0

Abstract

IL-1β-expressing macrophages have been described in rheumatoid arthritis (RA), immune checkpoint inhibitor-induced inflammatory arthritis (ICI-arthritis), and pancreatic cancer and proposed to be pathogenic. IL-1β+ macrophages express genes cooperatively induced by PGE2 and TNF signaling, but mechanisms that induce these cells are not known. We used an integrated transcriptomic and epigenomic analysis in primary human monocytes to study PGE2-TNF crosstalk, and how it is regulated by IFN-γ, as occurs in RA synovial macrophages. We identified a TNF + PGE2 (TP) induced gene expression signature that is enriched in IL1β+ RA and ICI-arthritis monocytic subsets, and includes genes in pathogenic IL-1, Notch and neutrophil chemokine pathways. ICI-arthritis myeloid cells mapped primarily onto four previously defined RA synovial monocytic clusters, and TP genes were expressed in a manner suggestive of a new functional monocyte subset. TP signature genes are distinct from canonical inflammatory NF-κB target genes such as TNF, IL6 and IL12B and are activated by cooperation of PGE2-induced AP-1, CEBP and NR4A family transcription factors with TNF-induced NF-κB activity. Unexpectedly, IFN-γ suppressed induction of AP-1, CEBP and NR4A activity to ablate induction of IL-1, Notch and neutrophil chemokine genes, while promoting expression of distinct inflammatory genes such as TNF and T cell chemokines like CXCL10. The opposing cross-regulation of PGE2 and IFN signaling in vitro was reflected in vivo in mutually exclusive expression of TP and IFN signatures in different cell clusters in RA and ICI-arthritis monocytes. These results reveal the basis for synergistic induction of inflammatory genes by PGE2 and TNF, and a novel regulatory axis whereby IFN-γ and PGE2 oppose each other to determine the balance between two distinct TNF-induced inflammatory gene expression programs relevant for RA and ICI-arthritis.

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IFN-γ和PGE2-cAMP轴对TNF反应的相反调节在类风湿和免疫检查点抑制剂诱导的关节炎人IL-1β+巨噬细胞中是明显的。

表达il -1β的巨噬细胞在类风湿关节炎（RA）、免疫检查点抑制剂诱导的炎症性关节炎（ICI-arthritis）和胰腺癌中被描述，并被认为是致病的。IL-1β+巨噬细胞表达由PGE2和TNF信号共同诱导的基因，但诱导这些细胞的机制尚不清楚。我们在原代人单核细胞中使用综合转录组学和表观基因组学分析来研究PGE2-TNF串扰，以及IFN-γ如何调节它，就像在RA滑膜巨噬细胞中发生的那样。我们发现了TNF + PGE2 （TP）诱导的基因表达特征，该基因在IL-1 β+ RA和ci -关节炎单核细胞亚群中富集，包括致病性IL-1、Notch和中性粒细胞趋化因子途径中的基因。ici关节炎髓样细胞主要定位到四个先前定义的RA滑膜单核细胞簇，TP基因以一种新的功能单核细胞亚群的方式表达。TP特征基因不同于典型炎性NF-κB靶基因如TNF、IL6和IL12B，由pge2诱导的AP-1、CEBP和NR4A家族转录因子与TNF诱导的NF-κB活性协同激活。出乎意料的是，IFN-γ抑制AP-1、CEBP和NR4A活性的诱导，从而减弱IL-1、Notch和中性粒细胞趋化因子基因的诱导，同时促进不同炎症基因如TNF和T细胞趋化因子如CXCL10的表达。PGE2和IFN信号在体外的反向交叉调控在体内反映在RA和ici -关节炎单核细胞不同细胞簇中TP和IFN信号的互斥表达。这些结果揭示了PGE2和TNF协同诱导炎症基因的基础，以及IFN-γ和PGE2相互对立以确定两种不同的TNF诱导炎症基因表达程序之间平衡的新调控轴，这些炎症基因表达程序与RA和ici -关节炎相关。

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来源期刊

eLife BIOLOGY-

CiteScore

12.90

自引率

3.90%

发文量

3122

审稿时长

17 weeks

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