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Single-cell analysis reveals immune cell abnormalities underlying the clinical heterogeneity of patients with systemic sclerosis

Author

Listed:
  • Hiroshi Shimagami

    (Osaka University
    Osaka University
    Osaka University)

  • Kei Nishimura

    (Osaka University
    Osaka University
    Chugai Pharmaceutical Co. Ltd)

  • Hiroaki Matsushita

    (Osaka University
    Osaka University
    Chugai Pharmaceutical Co. Ltd)

  • Shoichi Metsugi

    (Osaka University
    Osaka University
    Chugai Pharmaceutical Co. Ltd)

  • Yasuhiro Kato

    (Osaka University
    Osaka University
    Osaka University)

  • Takahiro Kawasaki

    (Osaka University
    Osaka University
    Osaka University)

  • Kohei Tsujimoto

    (Osaka University
    Osaka University
    Osaka University)

  • Ryuya Edahiro

    (Osaka University
    Osaka University
    RIKEN Center for Integrative Medical Sciences)

  • Eri Itotagawa

    (Osaka University
    Osaka University
    Osaka University)

  • Maiko Naito

    (Osaka University
    Osaka University
    Osaka University)

  • Shoji Kawada

    (Osaka University
    Osaka University
    Osaka University)

  • Daisuke Nakatsubo

    (Osaka University
    Osaka University
    Osaka University)

  • Kazuki Matsukawa

    (Osaka University
    Osaka University
    Osaka University)

  • Tomoko Namba-Hamano

    (Osaka University)

  • Kazunori Inoue

    (Osaka University)

  • Atsushi Takahashi

    (Osaka University)

  • Masayuki Mizui

    (Osaka University)

  • Seiya Kato

    (Osaka University)

  • Hayato Hikita

    (Osaka University)

  • Shigeaki Nakazawa

    (Osaka University)

  • Yoichi Kakuta

    (Osaka University)

  • Hachiro Konaka

    (Nippon Life Hospital)

  • Kensuke Mitsumoto

    (Nippon Life Hospital)

  • Nachi Ishikawa

    (Osaka International Medical & Science Center)

  • Jun Fujimoto

    (Osaka International Medical & Science Center)

  • Shinji Higa

    (Osaka International Medical & Science Center)

  • Ryusuke Omiya

    (Osaka University
    Chugai Pharmaceutical Co. Ltd)

  • Yoshitaka Isaka

    (Osaka University)

  • Tetsuo Takehara

    (Osaka University)

  • Norio Nonomura

    (Osaka University)

  • Yukinori Okada

    (Osaka University
    RIKEN Center for Integrative Medical Sciences
    Osaka University
    Osaka University)

  • Kunihiro Hattori

    (Osaka University
    Chugai Pharmaceutical Co. Ltd)

  • Masashi Narazaki

    (Osaka University
    Osaka University
    Osaka University)

  • Atsushi Kumanogoh

    (Osaka University
    Osaka University
    Osaka University
    Osaka University)

  • Masayuki Nishide

    (Osaka University
    Osaka University
    Osaka University)

Abstract

The autoimmune disease systemic sclerosis (SSc) presents with multiple organ manifestations that often complicate management strategies. To explore variations in immune cell subsets and their link to clinical heterogeneity, here we perform single-cell profiling of peripheral blood mononuclear cells (PBMC) from 21 SSc patients who never received immunosuppressive therapy. We identify a subset of EGR1+ CD14+ monocytes in patients with scleroderma renal crisis (SRC). This subset activates NF-kB signaling and differentiates into tissue-damaging macrophages, which accumulate at sites of tissue injury. Furthermore, we identify a CD8+ T cell subset with type II interferon signature in the peripheral blood and the lung tissue of patients with progressive interstitial lung disease (ILD), suggesting that chemokine-driven migration of these cells contributes to ILD progression. Thus, our single-cell analysis reveals distinct immune cell abnormalities associated with clinical organ manifestations, providing insights into tailored treatment strategies.

Suggested Citation

  • Hiroshi Shimagami & Kei Nishimura & Hiroaki Matsushita & Shoichi Metsugi & Yasuhiro Kato & Takahiro Kawasaki & Kohei Tsujimoto & Ryuya Edahiro & Eri Itotagawa & Maiko Naito & Shoji Kawada & Daisuke Na, 2025. "Single-cell analysis reveals immune cell abnormalities underlying the clinical heterogeneity of patients with systemic sclerosis," Nature Communications, Nature, vol. 16(1), pages 1-18, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-60034-7
    DOI: 10.1038/s41467-025-60034-7
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    References listed on IDEAS

    as
    1. Masayuki Nishide & Kei Nishimura & Hiroaki Matsushita & Ryuya Edahiro & Sachi Inukai & Hiroshi Shimagami & Shoji Kawada & Yasuhiro Kato & Takahiro Kawasaki & Kohei Tsujimoto & Hokuto Kamon & Ryusuke O, 2023. "Single-cell multi-omics analysis identifies two distinct phenotypes of newly-onset microscopic polyangiitis," Nature Communications, Nature, vol. 14(1), pages 1-14, December.
    2. C. T. Stankey & C. Bourges & L. M. Haag & T. Turner-Stokes & A. P. Piedade & C. Palmer-Jones & I. Papa & M. Silva dos Santos & Q. Zhang & A. J. Cameron & A. Legrini & T. Zhang & C. S. Wood & F. N. New, 2024. "A disease-associated gene desert directs macrophage inflammation through ETS2," Nature, Nature, vol. 630(8016), pages 447-456, June.
    3. Tracy Tabib & Mengqi Huang & Nina Morse & Anna Papazoglou & Rithika Behera & Minxue Jia & Melissa Bulik & Daisy E. Monier & Panayiotis V. Benos & Wei Chen & Robyn Domsic & Robert Lafyatis, 2021. "Myofibroblast transcriptome indicates SFRP2hi fibroblast progenitors in systemic sclerosis skin," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
    Full references (including those not matched with items on IDEAS)

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