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Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells

A subset of T regulatory cells (Tregs), identified by TIRC7 (T cell immune response cDNA 7) expression is designated as Immune Regulatory 1 Cells (IR1 cells). TIRC7 is an immune checkpoint inhibitor, co-localized with the T- cell receptor, HLA-DR and CTLA-4 during T-cell activation, which delivers r...

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Autores principales: Krause, Nicolas, Mengwasser, Jörg, Phithak, Elpida, Beato, Francisca, Appis, Marc, Milford, Edgar Louis, Pratschke, Johan, Sauer, Igor, Kuehl, Anja, Vogel, Arndt, Goodyear, Michael, Hammerich, Linda, Tacke, Frank, Haas, Johanna Faith, Müller, Tobias, Utku, Nalan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8867398/
https://www.ncbi.nlm.nih.gov/pubmed/35222353
http://dx.doi.org/10.3389/fimmu.2021.790775
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author Krause, Nicolas
Mengwasser, Jörg
Phithak, Elpida
Beato, Francisca
Appis, Marc
Milford, Edgar Louis
Pratschke, Johan
Sauer, Igor
Kuehl, Anja
Vogel, Arndt
Goodyear, Michael
Hammerich, Linda
Tacke, Frank
Haas, Johanna Faith
Müller, Tobias
Utku, Nalan
author_facet Krause, Nicolas
Mengwasser, Jörg
Phithak, Elpida
Beato, Francisca
Appis, Marc
Milford, Edgar Louis
Pratschke, Johan
Sauer, Igor
Kuehl, Anja
Vogel, Arndt
Goodyear, Michael
Hammerich, Linda
Tacke, Frank
Haas, Johanna Faith
Müller, Tobias
Utku, Nalan
author_sort Krause, Nicolas
collection PubMed
description A subset of T regulatory cells (Tregs), identified by TIRC7 (T cell immune response cDNA 7) expression is designated as Immune Regulatory 1 Cells (IR1 cells). TIRC7 is an immune checkpoint inhibitor, co-localized with the T- cell receptor, HLA-DR and CTLA-4 during T-cell activation, which delivers regulatory signals via binding to its ligand, HLA-DR α2 domain. IR1 cells express FOXP3, and multiple other markers associated with immune suppression. They constitute as much as 10% of Tregs. IR1 cells strongly inhibit proliferation in mixed lymphocyte reactions, where they express high levels of IL-10. Ex vivo expansion of Tregs over 2 weeks in the presence of an agonist TIRC7 antibody disproportionately expands the IR1 Treg subset, while maintaining high expression of suppressive markers including CD39, IL-10, LAP and GARP. Ex vivo expanded IR1 cells are a potent, homogeneous, stable set of suppressor Tregs with the potential to modulate immune dysregulation. The characteristics of IR1 cells suggest a therapeutic advantage over polyclonal Tregs for therapeutic interventions. Early restoration of immune homeostasis using IR1 cells has the potential to fundamentally alter the natural history of conditions characterized by abnormalities in the T regulatory cell compartment.
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spelling pubmed-88673982022-02-25 Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells Krause, Nicolas Mengwasser, Jörg Phithak, Elpida Beato, Francisca Appis, Marc Milford, Edgar Louis Pratschke, Johan Sauer, Igor Kuehl, Anja Vogel, Arndt Goodyear, Michael Hammerich, Linda Tacke, Frank Haas, Johanna Faith Müller, Tobias Utku, Nalan Front Immunol Immunology A subset of T regulatory cells (Tregs), identified by TIRC7 (T cell immune response cDNA 7) expression is designated as Immune Regulatory 1 Cells (IR1 cells). TIRC7 is an immune checkpoint inhibitor, co-localized with the T- cell receptor, HLA-DR and CTLA-4 during T-cell activation, which delivers regulatory signals via binding to its ligand, HLA-DR α2 domain. IR1 cells express FOXP3, and multiple other markers associated with immune suppression. They constitute as much as 10% of Tregs. IR1 cells strongly inhibit proliferation in mixed lymphocyte reactions, where they express high levels of IL-10. Ex vivo expansion of Tregs over 2 weeks in the presence of an agonist TIRC7 antibody disproportionately expands the IR1 Treg subset, while maintaining high expression of suppressive markers including CD39, IL-10, LAP and GARP. Ex vivo expanded IR1 cells are a potent, homogeneous, stable set of suppressor Tregs with the potential to modulate immune dysregulation. The characteristics of IR1 cells suggest a therapeutic advantage over polyclonal Tregs for therapeutic interventions. Early restoration of immune homeostasis using IR1 cells has the potential to fundamentally alter the natural history of conditions characterized by abnormalities in the T regulatory cell compartment. Frontiers Media S.A. 2022-02-08 /pmc/articles/PMC8867398/ /pubmed/35222353 http://dx.doi.org/10.3389/fimmu.2021.790775 Text en Copyright © 2022 Krause, Mengwasser, Phithak, Beato, Appis, Milford, Pratschke, Sauer, Kuehl, Vogel, Goodyear, Hammerich, Tacke, Haas, Müller and Utku 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
Krause, Nicolas
Mengwasser, Jörg
Phithak, Elpida
Beato, Francisca
Appis, Marc
Milford, Edgar Louis
Pratschke, Johan
Sauer, Igor
Kuehl, Anja
Vogel, Arndt
Goodyear, Michael
Hammerich, Linda
Tacke, Frank
Haas, Johanna Faith
Müller, Tobias
Utku, Nalan
Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title_full Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title_fullStr Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title_full_unstemmed Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title_short Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells
title_sort immune regulatory 1 cells: a novel and potent subset of human t regulatory cells
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8867398/
https://www.ncbi.nlm.nih.gov/pubmed/35222353
http://dx.doi.org/10.3389/fimmu.2021.790775
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