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Interferon-γ couples CD8+ T cell avidity and differentiation during infection.


ABSTRACT: Effective responses to intracellular pathogens are characterized by T cell clones with a broad affinity range for their cognate peptide and diverse functional phenotypes. How T cell clones are selected throughout the response to retain a breadth of avidities remains unclear. Here, we demonstrate that direct sensing of the cytokine IFN-γ by CD8+ T cells coordinates avidity and differentiation during infection. IFN-γ promotes the expansion of low-avidity T cells, allowing them to overcome the selective advantage of high-avidity T cells, whilst reinforcing high-avidity T cell entry into the memory pool, thus reducing the average avidity of the primary response and increasing that of the memory response. IFN-γ in this context is mainly provided by virtual memory T cells, an antigen-inexperienced subset with memory features. Overall, we propose that IFN-γ and virtual memory T cells fulfil a critical immunoregulatory role by enabling the coordination of T cell avidity and fate.

SUBMITTER: Uhl LFK 

PROVIDER: S-EPMC10593754 | biostudies-literature | 2023 Oct

REPOSITORIES: biostudies-literature

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Interferon-γ couples CD8<sup>+</sup> T cell avidity and differentiation during infection.

Uhl Lion F K LFK   Cai Han H   Oram Sophia L SL   Mahale Jagdish N JN   MacLean Andrew J AJ   Mazet Julie M JM   Piccirilli Theo T   He Alexander J AJ   Lau Doreen D   Elliott Tim T   Gerard Audrey A  

Nature communications 20231023 1


Effective responses to intracellular pathogens are characterized by T cell clones with a broad affinity range for their cognate peptide and diverse functional phenotypes. How T cell clones are selected throughout the response to retain a breadth of avidities remains unclear. Here, we demonstrate that direct sensing of the cytokine IFN-γ by CD8<sup>+</sup> T cells coordinates avidity and differentiation during infection. IFN-γ promotes the expansion of low-avidity T cells, allowing them to overco  ...[more]

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