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Dysfunctional Sars-CoV-2-M protein-specific cytotoxic T lymphocytes in patients recovering from severe COVID-19

Author

Listed:
  • Hideki Ogura

    (Hyogo Medical University)

  • Jin Gohda

    (The University of Tokyo)

  • Xiuyuan Lu

    (Osaka University)

  • Mizuki Yamamoto

    (The University of Tokyo)

  • Yoshio Takesue

    (Hyogo Medical University
    Tokoname City Hospital)

  • Aoi Son

    (Hyogo Medical University)

  • Sadayuki Doi

    (Kawanishi City Hospital)

  • Kazuyuki Matsushita

    (Kyoritsu Hospital)

  • Fumitaka Isobe

    (Kyowa Marina Hospital/Wellhouse Nishinomiya)

  • Yoshihiro Fukuda

    (Dainikyoritsu Hospital)

  • Tai-Ping Huang

    (Kyoritsu Onsen Hospital)

  • Takamasa Ueno

    (Kumamoto University)

  • Naomi Mambo

    (Hyogo Medical University)

  • Hiromoto Murakami

    (Hyogo Medical University)

  • Yasushi Kawaguchi

    (The University of Tokyo
    The University of Tokyo)

  • Jun-ichiro Inoue

    (The University of Tokyo)

  • Kunihiro Shirai

    (Hyogo Medical University)

  • Sho Yamasaki

    (Osaka University
    Osaka University
    Kyushu University
    Chiba University)

  • Jun-Ichi Hirata

    (Hyogo Medical University)

  • Satoshi Ishido

    (Hyogo Medical University)

Abstract

Although the importance of virus-specific cytotoxic T lymphocytes (CTL) in virus clearance is evident in COVID-19, the characteristics of virus-specific CTLs related to disease severity have not been fully explored. Here we show that the phenotype of virus-specific CTLs against immunoprevalent epitopes in COVID-19 convalescents might differ according to the course of the disease. We establish a cellular screening method that uses artificial antigen presenting cells, expressing HLA-A*24:02, the costimulatory molecule 4-1BBL, SARS-CoV-2 structural proteins S, M, and N and non-structural proteins ORF3a and nsp6/ORF1a. The screen implicates SARS-CoV-2 M protein as a frequent target of IFNγ secreting CD8+ T cells, and identifies M198–206 as an immunoprevalent epitope in our cohort of HLA-A*24:02 positive convalescent COVID-19 patients recovering from mild, moderate and severe disease. Further exploration of M198–206-specific CD8+ T cells with single cell RNA sequencing reveals public TCRs in virus-specific CD8+ T cells, and shows an exhausted phenotype with less differentiated status in cells from the severe group compared to cells from the moderate group. In summary, this study describes a method to identify T cell epitopes, indicate that dysfunction of virus-specific CTLs might be an important determinant of clinical outcomes.

Suggested Citation

  • Hideki Ogura & Jin Gohda & Xiuyuan Lu & Mizuki Yamamoto & Yoshio Takesue & Aoi Son & Sadayuki Doi & Kazuyuki Matsushita & Fumitaka Isobe & Yoshihiro Fukuda & Tai-Ping Huang & Takamasa Ueno & Naomi Mam, 2022. "Dysfunctional Sars-CoV-2-M protein-specific cytotoxic T lymphocytes in patients recovering from severe COVID-19," Nature Communications, Nature, vol. 13(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-34655-1
    DOI: 10.1038/s41467-022-34655-1
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    References listed on IDEAS

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