Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation

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The mechanism of T cell antigen receptor (TCR-CD3) signaling remains elusive. Here, we identify mutations in the transmembrane region of TCRβ or CD3ζ that augment peptide T cell antigen receptor (pMHC)-induced signaling not explicable by enhanced ligand binding, lateral diffusion, clustering, or co-...

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Autores principales: Lanz, Anna-Lisa, Masi, Giulia, Porciello, Nicla, Cohnen, André, Cipria, Deborah, Prakaash, Dheeraj, Bálint, Štefan, Raggiaschi, Roberto, Galgano, Donatella, Cole, David K., Lepore, Marco, Dushek, Omer, Dustin, Michael L., Sansom, Mark S.P., Kalli, Antreas C., Acuto, Oreste
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8293630/
https://www.ncbi.nlm.nih.gov/pubmed/34260912
http://dx.doi.org/10.1016/j.celrep.2021.109375
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author Lanz, Anna-Lisa
Masi, Giulia
Porciello, Nicla
Cohnen, André
Cipria, Deborah
Prakaash, Dheeraj
Bálint, Štefan
Raggiaschi, Roberto
Galgano, Donatella
Cole, David K.
Lepore, Marco
Dushek, Omer
Dustin, Michael L.
Sansom, Mark S.P.
Kalli, Antreas C.
Acuto, Oreste
author_facet Lanz, Anna-Lisa
Masi, Giulia
Porciello, Nicla
Cohnen, André
Cipria, Deborah
Prakaash, Dheeraj
Bálint, Štefan
Raggiaschi, Roberto
Galgano, Donatella
Cole, David K.
Lepore, Marco
Dushek, Omer
Dustin, Michael L.
Sansom, Mark S.P.
Kalli, Antreas C.
Acuto, Oreste
author_sort Lanz, Anna-Lisa
collection PubMed
description The mechanism of T cell antigen receptor (TCR-CD3) signaling remains elusive. Here, we identify mutations in the transmembrane region of TCRβ or CD3ζ that augment peptide T cell antigen receptor (pMHC)-induced signaling not explicable by enhanced ligand binding, lateral diffusion, clustering, or co-receptor function. Using a biochemical assay and molecular dynamics simulation, we demonstrate that the gain-of-function mutations loosen the interaction between TCRαβ and CD3ζ. Similar to the activating mutations, pMHC binding reduces TCRαβ cohesion with CD3ζ. This event occurs prior to CD3ζ phosphorylation and at 0°C. Moreover, we demonstrate that soluble monovalent pMHC alone induces signaling and reduces TCRαβ cohesion with CD3ζ in membrane-bound or solubilised TCR-CD3. Our data provide compelling evidence that pMHC binding suffices to activate allosteric changes propagating from TCRαβ to the CD3 subunits, reconfiguring interchain transmembrane region interactions. These dynamic modifications could change the arrangement of TCR-CD3 boundary lipids to license CD3ζ phosphorylation and initiate signal propagation.
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spelling pubmed-82936302021-07-23 Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation Lanz, Anna-Lisa Masi, Giulia Porciello, Nicla Cohnen, André Cipria, Deborah Prakaash, Dheeraj Bálint, Štefan Raggiaschi, Roberto Galgano, Donatella Cole, David K. Lepore, Marco Dushek, Omer Dustin, Michael L. Sansom, Mark S.P. Kalli, Antreas C. Acuto, Oreste Cell Rep Article The mechanism of T cell antigen receptor (TCR-CD3) signaling remains elusive. Here, we identify mutations in the transmembrane region of TCRβ or CD3ζ that augment peptide T cell antigen receptor (pMHC)-induced signaling not explicable by enhanced ligand binding, lateral diffusion, clustering, or co-receptor function. Using a biochemical assay and molecular dynamics simulation, we demonstrate that the gain-of-function mutations loosen the interaction between TCRαβ and CD3ζ. Similar to the activating mutations, pMHC binding reduces TCRαβ cohesion with CD3ζ. This event occurs prior to CD3ζ phosphorylation and at 0°C. Moreover, we demonstrate that soluble monovalent pMHC alone induces signaling and reduces TCRαβ cohesion with CD3ζ in membrane-bound or solubilised TCR-CD3. Our data provide compelling evidence that pMHC binding suffices to activate allosteric changes propagating from TCRαβ to the CD3 subunits, reconfiguring interchain transmembrane region interactions. These dynamic modifications could change the arrangement of TCR-CD3 boundary lipids to license CD3ζ phosphorylation and initiate signal propagation. Cell Press 2021-07-13 /pmc/articles/PMC8293630/ /pubmed/34260912 http://dx.doi.org/10.1016/j.celrep.2021.109375 Text en © 2021 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lanz, Anna-Lisa
Masi, Giulia
Porciello, Nicla
Cohnen, André
Cipria, Deborah
Prakaash, Dheeraj
Bálint, Štefan
Raggiaschi, Roberto
Galgano, Donatella
Cole, David K.
Lepore, Marco
Dushek, Omer
Dustin, Michael L.
Sansom, Mark S.P.
Kalli, Antreas C.
Acuto, Oreste
Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title_full Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title_fullStr Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title_full_unstemmed Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title_short Allosteric activation of T cell antigen receptor signaling by quaternary structure relaxation
title_sort allosteric activation of t cell antigen receptor signaling by quaternary structure relaxation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8293630/
https://www.ncbi.nlm.nih.gov/pubmed/34260912
http://dx.doi.org/10.1016/j.celrep.2021.109375
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