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Engineering Mesoscale T Cell Receptor Clustering by Plug-and-Play Nanotools.

M Florencia SánchezSevi FariaStefan FrühschulzLars WerkmannChristian WinterTina KarimianPeter LanzerstorferBirgit PlochbergerJulian WeghuberRobert Tampé
Published in: Advanced materials (Deerfield Beach, Fla.) (2024)
T 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. Here, we controlled TCR clustering 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 exhibited higher density and dynamics than the ligand-free approach, indicating that the size and architecture of the pMHC ligand influences TCR assembly. Our approach enables the control of membrane receptor clustering with high specificity and provide the possibility to explore different modalities of receptor activation. This article is protected by copyright. All rights reserved.
Keyphrases
  • single cell
  • regulatory t cells
  • rna seq
  • binding protein
  • healthcare
  • high glucose
  • diabetic rats
  • oxidative stress
  • immune response