Frontiers in Immunology (Apr 2023)

Regulator of G-protein signaling 1 critically supports CD8+ TRM cell-mediated intestinal immunity

  • Diego von Werdt,
  • Bilgi Gungor,
  • Juliana Barreto de Albuquerque,
  • Thomas Gruber,
  • Daniel Zysset,
  • Cheong K. C. Kwong Chung,
  • Cheong K. C. Kwong Chung,
  • Antonia Corrêa-Ferreira,
  • Regina Berchtold,
  • Nicolas Page,
  • Mirjam Schenk,
  • John H. Kehrl,
  • Doron Merkler,
  • Beat A. Imhof,
  • Beat A. Imhof,
  • Jens V. Stein,
  • Jun Abe,
  • Gleb Turchinovich,
  • Daniela Finke,
  • Adrian C. Hayday,
  • Adrian C. Hayday,
  • Nadia Corazza,
  • Christoph Mueller,
  • Christoph Mueller

DOI
https://doi.org/10.3389/fimmu.2023.1085895
Journal volume & issue
Vol. 14

Abstract

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Members of the Regulator of G-protein signaling (Rgs) family regulate the extent and timing of G protein signaling by increasing the GTPase activity of Gα protein subunits. The Rgs family member Rgs1 is one of the most up-regulated genes in tissue-resident memory (TRM) T cells when compared to their circulating T cell counterparts. Functionally, Rgs1 preferentially deactivates Gαq, and Gαi protein subunits and can therefore also attenuate chemokine receptor-mediated immune cell trafficking. The impact of Rgs1 expression on tissue-resident T cell generation, their maintenance, and the immunosurveillance of barrier tissues, however, is only incompletely understood. Here we report that Rgs1 expression is readily induced in naïve OT-I T cells in vivo following intestinal infection with Listeria monocytogenes-OVA. In bone marrow chimeras, Rgs1-/- and Rgs1+/+ T cells were generally present in comparable frequencies in distinct T cell subsets of the intestinal mucosa, mesenteric lymph nodes, and spleen. After intestinal infection with Listeria monocytogenes-OVA, however, OT-I Rgs1+/+ T cells outnumbered the co-transferred OT-I Rgs1-/- T cells in the small intestinal mucosa already early after infection. The underrepresentation of the OT-I Rgs1-/- T cells persisted to become even more pronounced during the memory phase (d30 post-infection). Remarkably, upon intestinal reinfection, mice with intestinal OT-I Rgs1+/+ TRM cells were able to prevent the systemic dissemination of the pathogen more efficiently than those with OT-I Rgs1-/- TRM cells. While the underlying mechanisms are not fully elucidated yet, these data thus identify Rgs1 as a critical regulator for the generation and maintenance of tissue-resident CD8+ T cells as a prerequisite for efficient local immunosurveillance in barrier tissues in case of reinfections with potential pathogens.

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