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The CD3ζ adaptor structure determines functional differences between human and mouse CD16 Fc receptor signaling

Oscar A. Aguilar, Lam‐Kiu Fong, Kenichi Ishiyama, William F. DeGrado, Lewis L. Lanier

2022The Journal of Experimental Medicine35 citationsDOIOpen Access PDF

Abstract

Natural killer (NK) cells can detect antibody-coated cells through recognition by the CD16 Fc receptor. The importance of CD16 in human NK cell biology has long been appreciated, but how CD16 functions in mouse NK cells remains poorly understood. Here, we report drastic differences between human and mouse CD16 functions in NK cells. We demonstrate that one of the adaptor molecules that CD16 associates with and signals through, CD3ζ, plays a critical role in these functional differences. Using a systematic approach, we demonstrate that residues in the transmembrane domain of the mouse CD3ζ molecule prevent efficient complex formation with mouse CD16, thereby dampening receptor function. Mutating these residues in mouse CD3ζ to those encoded by human CD3ζ resulted in rescue of CD16 receptor function. We reveal that the mouse CD3ζ transmembrane domain adopts a tightly packed confirmation, preventing association with CD16, whereas human CD3ζ adopts a versatile configuration that accommodates receptor assembly.

Topics & Concepts

CD16CD3Cell biologyTransmembrane proteinReceptorBiologySignal transducing adaptor proteinNatural killer cellSignal transductionImmunologyImmune systemBiochemistryCytotoxic T cellCD8In vitroImmune Cell Function and InteractionT-cell and B-cell ImmunologySynthesis and Biological Evaluation
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