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The CD16 and CD32b Fc-gamma receptors regulate antibody-mediated responses in mouse natural killer cells

Oscar A. Aguilar, Maria D. R. Gonzalez-Hinojosa, Janice Arakawa‐Hoyt, Alberto J. Millan, Dagmar Gotthardt, Tsukasa Nabekura, Lewis L. Lanier

2023Journal of Leukocyte Biology20 citationsDOIOpen Access PDF

Abstract

Natural killer (NK) cells are innate lymphocytes capable of mediating immune responses without prior sensitization. NK cells express Fc-gamma receptors (FcγRs) that engage the Fc region of IgG. Studies investigating the role of FcγRs on mouse NK cells have been limited due to lack specific reagents. In this study, we characterize the expression and biological consequences of activating mouse NK cells through their FcγRs. We demonstrate that most NK cells express the activating CD16 receptor, and a subset of NK cells also expresses the inhibitory CD32b receptor. Critically, these FcγRs are functional on mouse NK cells and can modulate antibody-mediated responses. We also characterized mice with conditional knockout alleles of Fcgr3 (CD16) or Fcgr2b (CD32b) in the NK and innate lymphoid cell (ILC) lineage. NK cells in these mice did not reveal any developmental defects and were responsive to cross-linking activating NK receptors, cytokine stimulation, and killing of YAC-1 targets. Importantly, CD16-deficient NK cells failed to induce antibody-directed cellular cytotoxicity of antibody-coated B-cell lymphomas in in vitro assays. In addition, we demonstrate the important role of CD16 on NK cells using an in vivo model of cancer immunotherapy using anti-CD20 antibody treatment of B-cell lymphomas.

Topics & Concepts

CD16BiologyJanus kinase 3Interleukin 21Fc receptorInterleukin 12AntibodyLymphokine-activated killer cellImmunologyNK-92Cell biologyNatural killer cellReceptorCD49bInnate immune systemImmune systemT cellCD3In vitroCytotoxic T cellCD8BiochemistryImmune Cell Function and InteractionT-cell and B-cell ImmunologyMonoclonal and Polyclonal Antibodies Research
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