T cell specific deletion of IRF4 with Ox40-Cre impairs effector and memory T cell responses in heart transplantation

T cell specific deletion of IRF4 with Ox40-Cre impairs effector and memory T cell responses in heart transplantation

IRF4 is the pioneer factor for effector T cell maturation. Here we investigated the function of IRF4 in maintaining OX40-related T cell responses following alloantigen activation in a mouse heart transplantation model. Irf4flox/flox mice were bred with Ox40cre/+ mice to generate Irf4flox/floxOx40cre...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:Clinical immunology (Orlando, Fla.) Fla.), 2023-07, Vol.252, p.109647-109647, Article 109647
Hauptverfasser: Chen, Yuqi, Liu, Zongtao, Liu, Fayuan, Xu, Li, Li, Geng, Qiao, Weihua, Wang, Yixuan, Dong, Nianguo
Format: Artikel
Sprache:eng
Schlagworte:
Heart transplantation
T cell differentiation
Transplant tolerance
Transplantantion immunity
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
Beschreibung
Zusammenfassung:IRF4 is the pioneer factor for effector T cell maturation. Here we investigated the function of IRF4 in maintaining OX40-related T cell responses following alloantigen activation in a mouse heart transplantation model. Irf4flox/flox mice were bred with Ox40cre/+ mice to generate Irf4flox/floxOx40cre/+ mice. Wild type C57BL/6, Irf4flox/floxOx40cre/+ mice were transplanted with BALB/c heart allografts, with or without BALB/c skin-sensitization. CD4+ TEa T cells co-transfer experiments and flow cytometric analysis were conducted to investigate the amount of CD4+ T cells and the percentage of the T effector subset. Irf4flox/floxOx40cre/+ and Irf4flox/floxOx40cre/+ TEa mice were constructed successfully. IRF4 ablation in activated OX40-mediated alloantigen specific CD4+ TEa T cells reduced effector T cell differentiation (CD44hiCD62Llo, Ki67, IFN-γ), which caused long-term allograft survival (> 100 d) in the chronic rejection model. In the donor skin-sensitized heart transplantation model, the formation and function of alloantigen-specific memory CD4+ TEa cells were also impaired in Irf4flox/floxOx40cre/+ mice. Additionally, deletion of IRF4 after T cell activation in Irf4flox/floxOx40cre/+ mice reduced T cell reactivation in vitro. IRF4 ablation after OX40-related T cell activation could reduce effector and memory T cell formation and inhibit their function in response to alloantigen stimulation. These findings could have significant implications in targeting activated T cells to induce transplant tolerance. •Irf4flox/floxOx40cre/+ and Irf4flox/floxOx40cre/+ TEa mice was successfully constructed.•Ox40-specific IRF4 knockout prevented chronic rejection and secondary response in mice heart transplantation.•IRF4 was needed after OX40 related-T cell priming for antigen-specific effector and memory T cell responses.•Ablation of IRF4 after T cell activation in Irf4flox/floxOx40cre/+ mice also reduced T cell reactivation in vitro.
ISSN:1521-6616
1521-7035
DOI:10.1016/j.clim.2023.109647