Monomeric agonist peptide/MHCII complexes activate T‐cells in an autonomous fashion

Author:

Platzer René1,Hellmeier Joschka2ORCID,Göhring Janett1ORCID,Perez Iago Doel1,Schatzlmaier Philipp1,Bodner Clara2ORCID,Focke‐Tejkl Margarete3ORCID,Schütz Gerhard J2,Sevcsik Eva2,Stockinger Hannes1ORCID,Brameshuber Mario2ORCID,Huppa Johannes B1ORCID

Affiliation:

1. Center for Pathophysiology, Infectiology, Immunology, Institute for Hygiene and Applied Immunology Medical University of Vienna Vienna Austria

2. TU Wien, Institute of Applied Physics Vienna Austria

3. Center for Pathophysiology, Infectiology, Immunology, Institute for Pathophysiology and Allergy Research Medical University of Vienna Vienna Austria

Abstract

AbstractMolecular crowding of agonist peptide/MHC class II complexes (pMHCIIs) with structurally similar, yet per se non‐stimulatory endogenous pMHCIIs is postulated to sensitize T‐cells for the recognition of single antigens on the surface of dendritic cells and B‐cells. When testing this premise with the use of advanced live cell microscopy, we observe pMHCIIs as monomeric, randomly distributed entities diffusing rapidly after entering the APC surface. Synaptic TCR engagement of highly abundant endogenous pMHCIIs is low or non‐existent and affects neither TCR engagement of rare agonist pMHCII in early and advanced synapses nor agonist‐induced TCR‐proximal signaling. Our findings highlight the capacity of single freely diffusing agonist pMHCIIs to elicit the full T‐cell response in an autonomous and peptide‐specific fashion with consequences for adaptive immunity and immunotherapeutic approaches.

Funder

Austrian Science Fund

Boehringer Ingelheim Fonds

Vienna Science and Technology Fund

Publisher

Springer Science and Business Media LLC

Subject

Genetics,Molecular Biology,Biochemistry

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