SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation

A numerous number of positive and negative signals via various molecules modulate T-cell activation. Within the various transmembrane proteins, SIRPγ is of interest since it is not expressed in rodents. SIRPγ interaction with CD47 is reevaluated in this study. Indeed, we show that the anti-SIRPγ mAb...

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Autores principales: Dehmani, Safa, Nerrière-Daguin, Véronique, Néel, Mélanie, Elain-Duret, Nathan, Heslan, Jean-Marie, Belarif, Lyssia, Mary, Caroline, Thepenier, Virginie, Biteau, Kevin, Poirier, Nicolas, Blancho, Gilles, Haspot, Fabienne
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8671138/
https://www.ncbi.nlm.nih.gov/pubmed/34925315
http://dx.doi.org/10.3389/fimmu.2021.732530
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author Dehmani, Safa
Nerrière-Daguin, Véronique
Néel, Mélanie
Elain-Duret, Nathan
Heslan, Jean-Marie
Belarif, Lyssia
Mary, Caroline
Thepenier, Virginie
Biteau, Kevin
Poirier, Nicolas
Blancho, Gilles
Haspot, Fabienne
author_facet Dehmani, Safa
Nerrière-Daguin, Véronique
Néel, Mélanie
Elain-Duret, Nathan
Heslan, Jean-Marie
Belarif, Lyssia
Mary, Caroline
Thepenier, Virginie
Biteau, Kevin
Poirier, Nicolas
Blancho, Gilles
Haspot, Fabienne
author_sort Dehmani, Safa
collection PubMed
description A numerous number of positive and negative signals via various molecules modulate T-cell activation. Within the various transmembrane proteins, SIRPγ is of interest since it is not expressed in rodents. SIRPγ interaction with CD47 is reevaluated in this study. Indeed, we show that the anti-SIRPγ mAb clone LSB2.20 previously used by others has not been appropriately characterized. We reveal that the anti-SIRPα clone KWAR23 is a Pan anti-SIRP mAb which efficiently blocks SIRPα and SIRPγ interactions with CD47. We show that SIRPγ expression on T cells varies with their differentiation and while being expressed on Tregs, is not implicated in their suppressive functions. SIRPγ spatial reorganization at the immune synapse is independent of its interaction with CD47. In vitro SIRPα-γ/CD47 blockade with KWAR23 impairs IFN-γ secretion by chronically activated T cells. In vivo in a xeno-GvHD model in NSG mice, the SIRPγ/CD47 blockade with the KWAR23 significantly delays the onset of the xeno-GvHD and deeply impairs human chimerism. In conclusion, we have shown that T-cell interaction with CD47 is of importance notably in chronic stimulation.
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spelling pubmed-86711382021-12-16 SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation Dehmani, Safa Nerrière-Daguin, Véronique Néel, Mélanie Elain-Duret, Nathan Heslan, Jean-Marie Belarif, Lyssia Mary, Caroline Thepenier, Virginie Biteau, Kevin Poirier, Nicolas Blancho, Gilles Haspot, Fabienne Front Immunol Immunology A numerous number of positive and negative signals via various molecules modulate T-cell activation. Within the various transmembrane proteins, SIRPγ is of interest since it is not expressed in rodents. SIRPγ interaction with CD47 is reevaluated in this study. Indeed, we show that the anti-SIRPγ mAb clone LSB2.20 previously used by others has not been appropriately characterized. We reveal that the anti-SIRPα clone KWAR23 is a Pan anti-SIRP mAb which efficiently blocks SIRPα and SIRPγ interactions with CD47. We show that SIRPγ expression on T cells varies with their differentiation and while being expressed on Tregs, is not implicated in their suppressive functions. SIRPγ spatial reorganization at the immune synapse is independent of its interaction with CD47. In vitro SIRPα-γ/CD47 blockade with KWAR23 impairs IFN-γ secretion by chronically activated T cells. In vivo in a xeno-GvHD model in NSG mice, the SIRPγ/CD47 blockade with the KWAR23 significantly delays the onset of the xeno-GvHD and deeply impairs human chimerism. In conclusion, we have shown that T-cell interaction with CD47 is of importance notably in chronic stimulation. Frontiers Media S.A. 2021-12-01 /pmc/articles/PMC8671138/ /pubmed/34925315 http://dx.doi.org/10.3389/fimmu.2021.732530 Text en Copyright © 2021 Dehmani, Nerrière-Daguin, Néel, Elain-Duret, Heslan, Belarif, Mary, Thepenier, Biteau, Poirier, Blancho and Haspot https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Dehmani, Safa
Nerrière-Daguin, Véronique
Néel, Mélanie
Elain-Duret, Nathan
Heslan, Jean-Marie
Belarif, Lyssia
Mary, Caroline
Thepenier, Virginie
Biteau, Kevin
Poirier, Nicolas
Blancho, Gilles
Haspot, Fabienne
SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title_full SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title_fullStr SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title_full_unstemmed SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title_short SIRPγ-CD47 Interaction Positively Regulates the Activation of Human T Cells in Situation of Chronic Stimulation
title_sort sirpγ-cd47 interaction positively regulates the activation of human t cells in situation of chronic stimulation
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8671138/
https://www.ncbi.nlm.nih.gov/pubmed/34925315
http://dx.doi.org/10.3389/fimmu.2021.732530
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