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Rescue RM/CS-AKI by blocking strategy with one-dose anti-myoglobin RabMAb

Author

Listed:
  • Xinyue Wang

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Ning Li

    (Tianjin University
    Tianjin University
    Tianjin University
    Key Laboratory for Disaster Medicine Technology)

  • Lu Han

    (Chinese Academy of Medical Sciences & Peking Union Medical College
    Tianjin Institutes of Health Science)

  • Ou Qiao

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Xin Chen

    (Tianjin University
    Tianjin University
    Tianjin University
    Tianjin University)

  • Pengtao Wang

    (Tianjin First Center Hospital)

  • Lancao Zhang

    (Tianjin University
    Tianjin University)

  • Yingjie Hou

    (Tianjin University
    Tianjin University
    Tianjin University
    Tianjin University)

  • Fengjiao Bao

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Herui Hao

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Sania Saeed

    (Tianjin University
    Tianjin University
    Tianjin University
    Tianjin University)

  • Li Zhang

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Zizheng Li

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Xiaohong Duan

    (Tianjin University
    Tianjin University
    Tianjin University)

  • Shuquan Rao

    (Chinese Academy of Medical Sciences & Peking Union Medical College
    Tianjin Institutes of Health Science)

  • Zichuan Liu

    (Tianjin University
    Tianjin University)

  • Yanhua Gong

    (Tianjin University
    Tianjin University
    Tianjin University
    Key Laboratory for Disaster Medicine Technology)

Abstract

Rhabdomyolysis or Crush syndrome-related AKI (RM/CS-AKI) has high mortality, and there is no effective early on-site treatment method. The critical pathogenic factor of RM/CS-AKI is the excessive free myoglobin (Mb) in blood circulation. Here, based on the concept of creating a “mobile barrier”, we develop an anti-Mb rabbit monoclonal antibody (RabMAb) with high specificity, affinity, stability, and broad species reactivity. A single dose of anti-Mb RabMAb injection is sufficient for emergency rescue in both homologous and heterologous RM/CS-AKI male animal models. The main goal of blocking the passage of free Mb through the glomerular filtration barrier has been achieved by using the anti-Mb RabMAb, which has a long-term stable therapeutic effect within 14 days and promotes phagocytosis of Mb. The optimal administration strategy, pharmacokinetic analysis, toxicity evaluation for anti-Mb RabMAb, and the distribution of its immune complexes in RM/CS-AKI mice are investigated. Thus, we develop effective prevention and control strategies for RM/CS-AKI.

Suggested Citation

  • Xinyue Wang & Ning Li & Lu Han & Ou Qiao & Xin Chen & Pengtao Wang & Lancao Zhang & Yingjie Hou & Fengjiao Bao & Herui Hao & Sania Saeed & Li Zhang & Zizheng Li & Xiaohong Duan & Shuquan Rao & Zichuan, 2025. "Rescue RM/CS-AKI by blocking strategy with one-dose anti-myoglobin RabMAb," Nature Communications, Nature, vol. 16(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-56353-4
    DOI: 10.1038/s41467-025-56353-4
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