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

Nicolas Krause; Jörg Mengwasser; Elpida Phithak; Francisca Beato; Marc Appis; Edgar Louis Milford; Johan Pratschke; Igor Sauer; Anja Kuehl; Arndt Vogel; Michael Goodyear; Linda Hammerich; Frank Tacke; Johanna Faith Haas; Tobias Müller; Nalan Utku

doi:10.3389/fimmu.2021.790775

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

Nicolas Krause, Jörg Mengwasser, Elpida Phithak, Francisca Beato, Marc Appis, Edgar Louis Milford, Johan Pratschke, Igor Sauer, Anja Kuehl, Arndt Vogel, Michael Goodyear, Linda Hammerich, Frank Tacke, Johanna Faith Haas, Tobias Müller, Nalan Utku

Medicine

Résultat de recherche: Article › examen par les pairs

1 Citation (Scopus)

Résumé

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.

Langue d'origine	English
Numéro d'article	790775
Journal	Frontiers in Immunology
Volume	12
DOI	https://doi.org/10.3389/fimmu.2021.790775
Statut de publication	Published - févr. 8 2022

Note bibliographique

Funding Information:
NU was supported by the BmBF German Grant Innovation for Individualized Medicine and by the European Union Fund for Regional Development (EFRE) (100394224). TM is supported by the German Research Foundation Grants MU 2864/1-3 and MU 2864/3-1.

Publisher Copyright:
Copyright © 2022 Krause, Mengwasser, Phithak, Beato, Appis, Milford, Pratschke, Sauer, Kuehl, Vogel, Goodyear, Hammerich, Tacke, Haas, Müller and Utku.

ASJC Scopus Subject Areas

Immunology and Allergy
Immunology

PubMed: MeSH publication types

Journal Article
Research Support, Non-U.S. Gov't

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10.3389/fimmu.2021.790775

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Krause, N., Mengwasser, J., Phithak, E., Beato, F., Appis, M., Milford, E. L., Pratschke, J., Sauer, I., Kuehl, A., Vogel, A., Goodyear, M., Hammerich, L., Tacke, F., Haas, J. F., Müller, T., & Utku, N. (2022). Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells. Frontiers in Immunology, 12, Article 790775. https://doi.org/10.3389/fimmu.2021.790775

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title = "Immune Regulatory 1 Cells: A Novel and Potent Subset of Human T Regulatory Cells",

abstract = "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.",

author = "Nicolas Krause and J{\"o}rg Mengwasser and Elpida Phithak and Francisca Beato and Marc Appis and Milford, {Edgar Louis} and Johan Pratschke and Igor Sauer and Anja Kuehl and Arndt Vogel and Michael Goodyear and Linda Hammerich and Frank Tacke and Haas, {Johanna Faith} and Tobias M{\"u}ller and Nalan Utku",

note = "Funding Information: NU was supported by the BmBF German Grant Innovation for Individualized Medicine and by the European Union Fund for Regional Development (EFRE) (100394224). TM is supported by the German Research Foundation Grants MU 2864/1-3 and MU 2864/3-1. Publisher Copyright: Copyright {\textcopyright} 2022 Krause, Mengwasser, Phithak, Beato, Appis, Milford, Pratschke, Sauer, Kuehl, Vogel, Goodyear, Hammerich, Tacke, Haas, M{\"u}ller and Utku.",

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doi = "10.3389/fimmu.2021.790775",

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T2 - A Novel and Potent Subset of Human T Regulatory Cells

AU - Krause, Nicolas

AU - Mengwasser, Jörg

AU - Phithak, Elpida

AU - Beato, Francisca

AU - Appis, Marc

AU - Milford, Edgar Louis

AU - Pratschke, Johan

AU - Sauer, Igor

AU - Kuehl, Anja

AU - Vogel, Arndt

AU - Goodyear, Michael

AU - Hammerich, Linda

AU - Tacke, Frank

AU - Haas, Johanna Faith

AU - Müller, Tobias

AU - Utku, Nalan

N1 - Funding Information: NU was supported by the BmBF German Grant Innovation for Individualized Medicine and by the European Union Fund for Regional Development (EFRE) (100394224). TM is supported by the German Research Foundation Grants MU 2864/1-3 and MU 2864/3-1. Publisher Copyright: Copyright © 2022 Krause, Mengwasser, Phithak, Beato, Appis, Milford, Pratschke, Sauer, Kuehl, Vogel, Goodyear, Hammerich, Tacke, Haas, Müller and Utku.

PY - 2022/2/8

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N2 - 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.

AB - 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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VL - 12

JO - Frontiers in Immunology

JF - Frontiers in Immunology

M1 - 790775

ER -

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

Résumé

Note bibliographique

ASJC Scopus Subject Areas

PubMed: MeSH publication types

Accès au document

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