Complement component C1q is an immunological rheostat that regulates Fc:FcγR interactions

Though binding sites for the complement factor C1q and the canonical fragment crystallizable (Fc) gamma receptors (Fc γ Rs) on immunoglobulin G (IgG) molecules overlap, how C1q decoration of immune complexes (ICs) influences their ability to engage Fc γ Rs remains unknown. In this report, we use rec...

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Veröffentlicht in:Immunogenetics (New York) 2023-08, Vol.75 (4), p.369-383
Hauptverfasser: So, Edward C., Zhou, Hua, Greenwell, Ariana, Burch, Erin E., Ji, Yaping, Mérigeon, Emmanuel Y., Olsen, Henrik S., Bentzen, Søren M., Block, David S., Zhang, Xiaoyu, Strome, Scott E.
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Sprache:eng
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Zusammenfassung:Though binding sites for the complement factor C1q and the canonical fragment crystallizable (Fc) gamma receptors (Fc γ Rs) on immunoglobulin G (IgG) molecules overlap, how C1q decoration of immune complexes (ICs) influences their ability to engage Fc γ Rs remains unknown. In this report, we use recombinant human Fc multimers as stable IC mimics to show that C1q engagement of ICs directly and transiently inhibits their interactions with Fc γ RIII (CD16) on human natural killer (NK) cells. This inhibition occurs by C1q engagement alone as well as in concert with other serum factors. Furthermore, the inhibition of Fc γ RIII engagement mediated by avid binding of C1q to ICs is directly associated with IC size and dependent on the concentrations of both C1q and Fc multimers present. Functionally, C1q-mediated Fc blockade limits the ability of NK cells to induce the upregulation of the cosignaling molecule, 4-1BB (CD137), and to mediate antibody-dependent cell-mediated cytotoxicity (ADCC). Although C1q is traditionally viewed as a soluble effector molecule, we demonstrate that C1q may also take on the role of an “immunologic rheostat,” buffering Fc γ R-mediated activation of immune cells by circulating ICs. These data define a novel role for C1q as a regulator of immune homeostasis and add to our growing understanding that complement factors mediate pleiotropic effects.
ISSN:0093-7711
1432-1211
DOI:10.1007/s00251-023-01311-x