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Abl family tyrosine kinases govern IgG extravasation in the skin in a murine pemphigus model

Author

Listed:
  • Sachiko Ono

    (Kyoto University Graduate School of Medicine)

  • Gyohei Egawa

    (Kyoto University Graduate School of Medicine)

  • Takashi Nomura

    (Kyoto University Graduate School of Medicine)

  • Akihiko Kitoh

    (Kyoto University Graduate School of Medicine)

  • Teruki Dainichi

    (Kyoto University Graduate School of Medicine)

  • Atsushi Otsuka

    (Kyoto University Graduate School of Medicine)

  • Saeko Nakajima

    (Kyoto University Graduate School of Medicine)

  • Masayuki Amagai

    (Keio University Graduate School of Medicine)

  • Fumi Matsumoto

    (Mitsubishi Tanabe Pharma Corporation)

  • Mami Yamamoto

    (Mitsubishi Tanabe Pharma Corporation)

  • Yoshiaki Kubota

    (Keio University School of Medicine)

  • Toshiyuki Takai

    (Tohoku University)

  • Tetsuya Honda

    (Kyoto University Graduate School of Medicine)

  • Kenji Kabashima

    (Kyoto University Graduate School of Medicine
    Technology and Research (A*STAR))

Abstract

The pathway of homeostatic IgG extravasation is not fully understood, in spite of its importance for the maintenance of host immunity, the management of autoantibody-mediated disorders, and the use of antibody-based biologics. Here we show in a murine model of pemphigus, a prototypic cutaneous autoantibody-mediated disorder, that blood-circulating IgG extravasates into the skin in a time- and dose-dependent manner under homeostatic conditions. This IgG extravasation is unaffected by depletion of Fcγ receptors, but is largely attenuated by specific ablation of dynamin-dependent endocytic vesicle formation in blood endothelial cells (BECs). Among dynamin-dependent endocytic vesicles, IgG co-localizes well with caveolae in cultured BECs. An Abl family tyrosine kinase inhibitor imatinib, which reduces caveolae-mediated endocytosis, impairs IgG extravasation in the skin and attenuates the murine pemphigus manifestations. Our study highlights the kinetics of IgG extravasation in vivo, which might be a clue to understand the pathological mechanism of autoantibody-mediated autoimmune disorders.

Suggested Citation

  • Sachiko Ono & Gyohei Egawa & Takashi Nomura & Akihiko Kitoh & Teruki Dainichi & Atsushi Otsuka & Saeko Nakajima & Masayuki Amagai & Fumi Matsumoto & Mami Yamamoto & Yoshiaki Kubota & Toshiyuki Takai &, 2019. "Abl family tyrosine kinases govern IgG extravasation in the skin in a murine pemphigus model," Nature Communications, Nature, vol. 10(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-12232-3
    DOI: 10.1038/s41467-019-12232-3
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