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Single cell immunoprofile of synovial fluid in rheumatoid arthritis with TNF/JAK inhibitor treatment

Author

Listed:
  • Xuyang Xia

    (Sichuan University
    Sichuan University
    Sichuan University
    Sichuan University)

  • Chenjia He

    (Sichuan University)

  • Zhinan Xue

    (Sichuan University)

  • Yuelan Wang

    (Sichuan University)

  • Yun Qin

    (Sichuan University)

  • Zhixiang Ren

    (Sichuan University)

  • Yupeng Huang

    (Sichuan University)

  • Han Luo

    (Sichuan University)

  • Hai-Ning Chen

    (Sichuan University
    Sichuan University)

  • Wei-Han Zhang

    (Sichuan University
    Sichuan University)

  • Li-Bin Huang

    (Sichuan University
    Sichuan University)

  • Yunying Shi

    (Sichuan University)

  • Yangjuan Bai

    (Sichuan University)

  • Bei Cai

    (Sichuan University)

  • Lanlan Wang

    (Sichuan University)

  • Feng Zhang

    (Quzhou People’s Hospital)

  • Maoxiang Qian

    (Children’s Hospital of Fudan University
    Fudan University)

  • Wei Zhang

    (Central South University)

  • Yang Shu

    (Sichuan University
    Sichuan University
    Sichuan University)

  • Geng Yin

    (Sichuan University
    Sichuan University)

  • Heng Xu

    (Sichuan University
    Sichuan University
    Sichuan University
    Tianfu Jincheng Laboratory)

  • Qibing Xie

    (Sichuan University)

Abstract

Numerous patients with rheumatoid arthritis (RA) manifest severe syndromes, including elevated synovial fluid volumes (SF) with abundant immune cells, which can be controlled by TNF/JAK inhibitors. Here, we apply single-cell RNA sequencing (scRNA-seq) and subsequent validations in SF from RA patients. These analyses of synovial tissue show reduced density of SF-derived pathogenic cells (e.g., SPP1+ macrophages and CXCL13+CD4+ T cells), altered gene expression (e.g., SPP1 and STAT1), molecular pathway changes (e.g., JAK/STAT), and cell-cell communications in drug-specific manners in samples from patients pre-/post-treated with adalimumab/tofacitinib. Particularly, SPP1+ macrophages exhibit pronounced communication with CXCL13+CD4+ T cells, which are abolished after treatment and correlate with treatment efficacy. These pathogenic cell types alone or in combination can augment inflammation of fibroblast-like synoviocytes in vitro, while conditional Spp1 knocking-out reduces RA-related cytokine expression in collagen-induced arthritis mice models. Our study shows the functional role of SF-derived pathogenic cells in progression and drug-specific treatment outcomes in RA.

Suggested Citation

  • Xuyang Xia & Chenjia He & Zhinan Xue & Yuelan Wang & Yun Qin & Zhixiang Ren & Yupeng Huang & Han Luo & Hai-Ning Chen & Wei-Han Zhang & Li-Bin Huang & Yunying Shi & Yangjuan Bai & Bei Cai & Lanlan Wang, 2025. "Single cell immunoprofile of synovial fluid in rheumatoid arthritis with TNF/JAK inhibitor treatment," Nature Communications, Nature, vol. 16(1), pages 1-23, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57361-0
    DOI: 10.1038/s41467-025-57361-0
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