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Sialic Acid Ligands of CD28 Suppress Costimulation of T Cells

Landon J. Edgar, Andrew J. Thompson, Vincent F. Vartabedian, Chika Kikuchi, Jordan L. Woehl, John R. Teijaro, James C. Paulson

2021ACS Central Science71 citationsDOIOpen Access PDF

Abstract

Effector T cells comprise the cellular arm of the adaptive immune system and are essential for mounting immune responses against pathogens and cancer. To reach effector status, costimulation through CD28 is required. Here, we report that sialic acid-containing glycans on the surface of both T cells and APCs are alternative ligands of CD28 that compete with binding to its well-documented activatory ligand CD80 on the APC, resulting in attenuated costimulation. Removal of sialic acids enhances antigen-mediated activation of naïve T cells and also increases the revival of effector T cells made hypofunctional or exhausted via chronic viral infection. This occurs through a mechanism that is synergistic with antibody blockade of the inhibitory PD-1 axis. These results reveal a previously unrecognized role of sialic acid ligands in attenuation of CD28-mediated costimulation of T cells.

Topics & Concepts

CD28EffectorCD80Sialic acidCell biologyChemistryImmune systemT cellBiologyBiochemistryImmunologyCytotoxic T cellCD40In vitroImmune Cell Function and InteractionT-cell and B-cell ImmunologyImmunotherapy and Immune Responses
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