PLoS Pathogens (Jun 2019)

NK cell-intrinsic FcεRIγ limits CD8+ T-cell expansion and thereby turns an acute into a chronic viral infection.

  • Vikas Duhan,
  • Thamer A Hamdan,
  • Haifeng C Xu,
  • Prashant Shinde,
  • Hilal Bhat,
  • Fanghui Li,
  • Yahya Al-Matary,
  • Dieter Häussinger,
  • Judith Bezgovsek,
  • Sarah-Kim Friedrich,
  • Cornelia Hardt,
  • Philipp A Lang,
  • Karl S Lang

DOI
https://doi.org/10.1371/journal.ppat.1007797
Journal volume & issue
Vol. 15, no. 6
p. e1007797

Abstract

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During viral infection, tight regulation of CD8+ T-cell functions determines the outcome of the disease. Recently, others and we determined that the natural killer (NK) cells kill hyperproliferative CD8+ T cells in the context of viral infection, but molecules that are involved in shaping the regulatory capability of NK cells remain virtually unknown. Here we used mice lacking the Fc-receptor common gamma chain (FcRγ, FcεRIγ, Fcer1g-/- mice) to determine the role of Fc-receptor and NK-receptor signaling in the process of CD8+ T-cell regulation. We found that the lack of FcRγ on NK cells limits their ability to restrain virus-specific CD8+ T cells and that the lack of FcRγ in Fcer1g-/- mice leads to enhanced CD8+ T-cell responses and rapid control of the chronic docile strain of the lymphocytic choriomeningitis virus (LCMV). Mechanistically, FcRγ stabilized the expression of NKp46 but not that of other killer cell-activating receptors on NK cells. Although FcRγ did not influence the development or activation of NK cell during LCMV infection, it specifically limited their ability to modulate CD8+ T-cell functions. In conclusion, we determined that FcRγ plays an important role in regulating CD8+ T-cell functions during chronic LCMV infection.