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Activation of Dendritic Cells Alters the Mechanism of MHC Class II Antigen Presentation to CD4 T Cells

Kyungjin Cho, Satoshi Ishido, Laurence C. Eisenlohr, Paul A. Roche

2020The Journal of Immunology28 citationsDOIOpen Access PDF

Abstract

Abstract Both immature and mature dendritic cells (DCs) can process and present foreign Ags to CD4 T cells; however, the mechanism by which MHC class II (MHC-II) in mature DCs acquires antigenic peptides remains unknown. To address this, we have studied Ag processing and presentation of two distinct CD4 T cell epitopes of the influenza virus hemagglutinin coat protein by both immature and mature mouse DCs. We find that immature DCs almost exclusively use newly synthesized MHC-II targeted to DM+ late endosomes for presentation to influenza virus–specific CD4 T cells. By contrast, mature DCs exclusively use recycling MHC-II that traffics to both early and late endosomes for antigenic peptide binding. Rab11a knockdown partially inhibits recycling of MHC-II in mature DCs and selectively inhibits presentation of an influenza virus hemagglutinin CD4 T cell epitope generated in early endosomes. These studies highlight a “division of labor” in MHC-II peptide binding, in which immature DCs preferentially present Ags acquired in Rab11a− DM+ late endosomes, whereas mature DCs use recycling MHC-II to present antigenic peptides acquired in both Rab11a+ early endosomes and Rab11a− endosomes for CD4 T cell activation.

Topics & Concepts

EndosomeAntigen processingAntigen presentationMHC class ICell biologyMHC class IIEpitopeCross-presentationBiologyMajor histocompatibility complexMHC restrictionAntigenAntigen-presenting cellT cellImmune systemImmunologyIntracellularImmunotherapy and Immune ResponsesImmune Cell Function and InteractionT-cell and B-cell Immunology
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