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Kinesin-1 regulates antigen cross-presentation through the scission of tubulations from early endosomes in dendritic cells

Author

Listed:
  • Meriem Belabed

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163)

  • François-Xavier Mauvais

    (Université de Paris, INSERM, U1151, Institut Necker Enfants Malades; Université de Paris; CNRS, UMR8253)

  • Sophia Maschalidi

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163)

  • Mathieu Kurowska

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163)

  • Nicolas Goudin

    (Cell Imaging Facility, Université de Paris, Imagine Institute)

  • Jian-Dong Huang

    (The University of Hong Kong)

  • Alain Fischer

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163
    Necker Children’s Hospital, AP-HP
    Collège de France)

  • Geneviève Basile

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163)

  • Peter Endert

    (Université de Paris, INSERM, U1151, Institut Necker Enfants Malades; Université de Paris; CNRS, UMR8253)

  • Fernando E. Sepulveda

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163
    Centre national de la recherche scientifique (CNRS))

  • Gaël Ménasché

    (Laboratory of Molecular basis of altered immune homeostasis, INSERM UMR1163)

Abstract

Dendritic cells (DCs) constitute a specialized population of immune cells that present exogenous antigen (Ag) on major histocompatibility complex (MHC) class I molecules to initiate CD8 + T cell responses against pathogens and tumours. Although cross-presentation depends critically on the trafficking of Ag-containing intracellular vesicular compartments, the molecular machinery that regulates vesicular transport is incompletely understood. Here, we demonstrate that mice lacking Kif5b (the heavy chain of kinesin-1) in their DCs exhibit a major impairment in cross-presentation and thus a poor in vivo anti-tumour response. We find that kinesin-1 critically regulates antigen cross-presentation in DCs, by controlling Ag degradation, the endosomal pH, and MHC-I recycling. Mechanistically, kinesin-1 appears to regulate early endosome maturation by allowing the scission of endosomal tubulations. Our results highlight kinesin-1’s role as a molecular checkpoint that modulates the balance between antigen degradation and cross-presentation.

Suggested Citation

  • Meriem Belabed & François-Xavier Mauvais & Sophia Maschalidi & Mathieu Kurowska & Nicolas Goudin & Jian-Dong Huang & Alain Fischer & Geneviève Basile & Peter Endert & Fernando E. Sepulveda & Gaël Ména, 2020. "Kinesin-1 regulates antigen cross-presentation through the scission of tubulations from early endosomes in dendritic cells," Nature Communications, Nature, vol. 11(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-15692-0
    DOI: 10.1038/s41467-020-15692-0
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