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Aiolos represses CD4+ T cell cytotoxic programming via reciprocal regulation of TFH transcription factors and IL-2 sensitivity

Author

Listed:
  • Kaitlin A. Read

    (The Ohio State University College of Medicine and Wexner Medical Center
    Biomedical Sciences Graduate Program)

  • Devin M. Jones

    (The Ohio State University College of Medicine and Wexner Medical Center
    Biomedical Sciences Graduate Program)

  • Srijana Pokhrel

    (The Ohio State University College of Medicine and Wexner Medical Center)

  • Emily D. S. Hales

    (The Ohio State University College of Medicine and Wexner Medical Center)

  • Aditi Varkey

    (The Ohio State University College of Medicine and Wexner Medical Center)

  • Jasmine A. Tuazon

    (The Ohio State University College of Medicine and Wexner Medical Center
    Biomedical Sciences Graduate Program
    Medical Scientist Training Program)

  • Caprice D. Eisele

    (Biomedical Sciences Graduate Program
    The Ohio State University College of Medicine and Wexner Medical Center)

  • Omar Abdouni

    (The Ohio State University College of Medicine and Wexner Medical Center)

  • Abbey Saadey

    (The Ohio State University College of Medicine and Wexner Medical Center
    Biomedical Sciences Graduate Program)

  • Melissa R. Leonard

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State University College of Veterinary Medicine)

  • Robert T. Warren

    (The Ohio State University College of Medicine and Wexner Medical Center)

  • Michael D. Powell

    (Emory University School of Medicine)

  • Jeremy M. Boss

    (Emory University School of Medicine)

  • Emily A. Hemann

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State University College of Medicine and Wexner Medical Center)

  • Jacob S. Yount

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State University College of Medicine and Wexner Medical Center)

  • Gang Xin

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

  • Hazem E. Ghoneim

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

  • Chan-Wang J. Lio

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

  • Aharon G. Freud

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

  • Patrick L. Collins

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

  • Kenneth J. Oestreich

    (The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State University College of Medicine and Wexner Medical Center
    The Ohio State Comprehensive Cancer Center)

Abstract

During intracellular infection, T follicular helper (TFH) and T helper 1 (TH1) cells promote humoral and cell-mediated responses, respectively. Another subset, CD4-cytotoxic T lymphocytes (CD4-CTLs), eliminate infected cells via functions typically associated with CD8+ T cells. The mechanisms underlying differentiation of these populations are incompletely understood. Here, we identify the transcription factor Aiolos as a reciprocal regulator of TFH and CD4-CTL programming. We find that Aiolos deficiency results in downregulation of key TFH transcription factors, and consequently reduced TFH differentiation and antibody production, during influenza virus infection. Conversely, CD4-CTL programming is elevated, including enhanced Eomes and cytolytic molecule expression. We further demonstrate that Aiolos deficiency allows for enhanced IL-2 sensitivity and increased STAT5 association with CD4-CTL gene targets, including Eomes, effector molecules, and IL2Ra. Thus, our collective findings identify Aiolos as a pivotal regulator of CD4-CTL and TFH programming and highlight its potential as a target for manipulating CD4+ T cell responses.

Suggested Citation

  • Kaitlin A. Read & Devin M. Jones & Srijana Pokhrel & Emily D. S. Hales & Aditi Varkey & Jasmine A. Tuazon & Caprice D. Eisele & Omar Abdouni & Abbey Saadey & Melissa R. Leonard & Robert T. Warren & Mi, 2023. "Aiolos represses CD4+ T cell cytotoxic programming via reciprocal regulation of TFH transcription factors and IL-2 sensitivity," Nature Communications, Nature, vol. 14(1), pages 1-18, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-37420-0
    DOI: 10.1038/s41467-023-37420-0
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    References listed on IDEAS

    as
    1. Paul W. McDonald & Kaitlin A. Read & Chandra E. Baker & Ashlyn E. Anderson & Michael D. Powell & André Ballesteros-Tato & Kenneth J. Oestreich, 2016. "IL-7 signalling represses Bcl-6 and the TFH gene program," Nature Communications, Nature, vol. 7(1), pages 1-12, April.
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