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Deciphering the spatial landscape and plasticity of immunosuppressive fibroblasts in breast cancer

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Listed:
  • Hugo Croizer

    (PSL Research University
    Inserm, U830)

  • Rana Mhaidly

    (PSL Research University
    Inserm, U830)

  • Yann Kieffer

    (PSL Research University
    Inserm, U830)

  • Geraldine Gentric

    (PSL Research University
    Inserm, U830)

  • Lounes Djerroudi

    (PSL Research University
    Inserm, U830
    Institut Curie Hospital Group)

  • Renaud Leclere

    (Institut Curie Hospital Group)

  • Floriane Pelon

    (PSL Research University
    Inserm, U830)

  • Catherine Robley

    (PSL Research University
    Inserm, U830)

  • Mylene Bohec

    (PSL Research University, ICGex Next-Generation Sequencing Platform
    PSL Research University, Single Cell Initiative)

  • Arnaud Meng

    (PSL Research University
    Inserm, U830)

  • Didier Meseure

    (Institut Curie Hospital Group)

  • Emanuela Romano

    (Center for Cancer Immunotherapy, Institut Curie)

  • Sylvain Baulande

    (PSL Research University, ICGex Next-Generation Sequencing Platform
    PSL Research University, Single Cell Initiative)

  • Agathe Peltier

    (PSL Research University
    Inserm, U830)

  • Anne Vincent-Salomon

    (Institut Curie Hospital Group)

  • Fatima Mechta-Grigoriou

    (PSL Research University
    Inserm, U830)

Abstract

Although heterogeneity of FAP+ Cancer-Associated Fibroblasts (CAF) has been described in breast cancer, their plasticity and spatial distribution remain poorly understood. Here, we analyze trajectory inference, deconvolute spatial transcriptomics at single-cell level and perform functional assays to generate a high-resolution integrated map of breast cancer (BC), with a focus on inflammatory and myofibroblastic (iCAF/myCAF) FAP+ CAF clusters. We identify 10 spatially-organized FAP+ CAF-related cellular niches, called EcoCellTypes, which are differentially localized within tumors. Consistent with their spatial organization, cancer cells drive the transition of detoxification-associated iCAF (Detox-iCAF) towards immunosuppressive extracellular matrix (ECM)-producing myCAF (ECM-myCAF) via a DPP4- and YAP-dependent mechanism. In turn, ECM-myCAF polarize TREM2+ macrophages, regulatory NK and T cells to induce immunosuppressive EcoCellTypes, while Detox-iCAF are associated with FOLR2+ macrophages in an immuno-protective EcoCellType. FAP+ CAF subpopulations accumulate differently according to the invasive BC status and predict invasive recurrence of ductal carcinoma in situ (DCIS), which could help in identifying low-risk DCIS patients eligible for therapeutic de-escalation.

Suggested Citation

  • Hugo Croizer & Rana Mhaidly & Yann Kieffer & Geraldine Gentric & Lounes Djerroudi & Renaud Leclere & Floriane Pelon & Catherine Robley & Mylene Bohec & Arnaud Meng & Didier Meseure & Emanuela Romano &, 2024. "Deciphering the spatial landscape and plasticity of immunosuppressive fibroblasts in breast cancer," Nature Communications, Nature, vol. 15(1), pages 1-28, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-47068-z
    DOI: 10.1038/s41467-024-47068-z
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