Engineering Mesoscale T Cell Receptor Clustering by Plug‐and‐Play Nanotools

Author:

Sánchez M. Florencia1,Faria Sevi1,Frühschulz Stefan1,Werkmann Lars1,Winter Christian1,Karimian Tina2,Lanzerstorfer Peter2,Plochberger Birgit34,Weghuber Julian25,Tampé Robert1ORCID

Affiliation:

1. Institute of Biochemistry Biocenter Goethe University Frankfurt Max‐von‐Laue‐Str. 9 60438 Frankfurt am Main Germany

2. Center of Excellence Food Technology and Nutrition University of Applied Sciences Upper Austria Wels 4600 Austria

3. University of Applied Sciences Upper Austria Campus Linz Linz 4020 Austria

4. Ludwig Boltzmann Institute for Experimental and Clinical Traumatology Donaueschingenstr. 13 Vienna 1200 Austria

5. FFoQSI – Austrian Competence Centre for Feed and Food Quality Safety & Innovation FFoQSI GmbH Technopark 1D Tulln an der Donau 3430 Austria

Abstract

AbstractT cell receptor (TCR) clustering and formation of an immune synapse are crucial for TCR signaling. However, limited information is available about these dynamic assemblies and their connection to transmembrane signaling. In this work, TCR clustering is controlled via plug‐and‐play nanotools based on an engineered irreversible conjugation pair and a peptide‐loaded major histocompatibility complex (pMHC) molecule to compare receptor assembly in a ligand (pMHC)‐induced or ligand‐independent manner. A streptavidin‐binding peptide displayed in both tools enabled their anchoring in streptavidin‐pre‐structured matrices. Strikingly, pMHC‐induced clustering in the confined regions exhibit higher density and dynamics than the ligand‐free approach, indicating that the size and architecture of the pMHC ligand influences TCR assembly. This approach enables the control of membrane receptor clustering with high specificity and provides the possibility to explore different modalities of receptor activation.

Funder

Volkswagen Foundation

Austrian Science Fund

Christian Doppler Forschungsgesellschaft

Deutsche Forschungsgemeinschaft

Publisher

Wiley

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