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Proteogenomic characterization of skull-base chordoma

Author

Listed:
  • Qilin Zhang

    (Fudan University
    Fudan University
    Massachusetts General Hospital and Harvard Medical School)

  • Ziyan Xu

    (Fudan University)

  • Rui Han

    (Fudan University
    Fudan University)

  • Yunzhi Wang

    (Fudan University)

  • Zhen Ye

    (Fudan University
    Fudan University)

  • Jiajun Zhu

    (Fudan University)

  • Yixin Cai

    (Fudan University
    Fudan University)

  • Fan Zhang

    (Fudan University)

  • Jiangyan Zhao

    (Fudan University)

  • Boyuan Yao

    (Fudan University
    Fudan University)

  • Zhaoyu Qin

    (Fudan University)

  • Nidan Qiao

    (Fudan University
    Fudan University)

  • Ruofan Huang

    (Fudan University
    Fudan University)

  • Jinwen Feng

    (Fudan University)

  • Yongfei Wang

    (Fudan University
    Fudan University)

  • Wenting Rui

    (Fudan University)

  • Fuchu He

    (Fudan University
    Research Unit of Proteomics Driven Cancer Precision Medicine. Chinese Academy of Medical Sciences)

  • Yao Zhao

    (Fudan University
    Fudan University
    Fudan University
    Shanghai Key Laboratory of Brain Function Restoration and Neural Regeneration)

  • Chen Ding

    (Fudan University
    Xinjiang Key Laboratory of Translational Biomedical Engineering)

Abstract

Skull-base chordoma is a rare, aggressive bone cancer with a high recurrence rate. Despite advances in genomic studies, its molecular characteristics and effective therapies remain unknown. Here, we conduct integrative genomics, transcriptomics, proteomics, and phosphoproteomics analyses of 187 skull-base chordoma tumors. In our study, chromosome instability is identified as a prognostic predictor and potential therapeutic target. Multi-omics data reveals downstream effects of chromosome instability, with RPRD1B as a putative target for radiotherapy-resistant patients. Chromosome 1q gain, associated with chromosome instability and upregulated mitochondrial functions, lead to poorer clinical outcomes. Immune subtyping identify an immune cold subtype linked to chromosome 9p/10q loss and immune evasion. Proteomics-based classification reveals subtypes (P-II and P-III) with high chromosome instability and immune cold features, with P-II tumors showing increased invasiveness. These findings, confirmed in 17 paired samples, provide insights into the biology and treatment of skull-base chordoma.

Suggested Citation

  • Qilin Zhang & Ziyan Xu & Rui Han & Yunzhi Wang & Zhen Ye & Jiajun Zhu & Yixin Cai & Fan Zhang & Jiangyan Zhao & Boyuan Yao & Zhaoyu Qin & Nidan Qiao & Ruofan Huang & Jinwen Feng & Yongfei Wang & Wenti, 2024. "Proteogenomic characterization of skull-base chordoma," Nature Communications, Nature, vol. 15(1), pages 1-32, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-52285-7
    DOI: 10.1038/s41467-024-52285-7
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