Retinoic acid–responsive CD8 effector T cells are selectively increased in IL-23–rich tissue in gastrointestinal GVHD | Zendy

Jennifer Ball | Zendy; Andrew Clear | Zendy; James Aries | Zendy; Sarah Charrot | Zendy; Caroline Besley | Zendy; Matt Mee | Zendy; Andrew J. Stagg | Zendy; James O. Lindsay | Zendy; Jamie Cavenagh | Zendy; Maria Calaminci | Zendy; John G. Gribben | Zendy; Jeff Davies | Zendy

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Retinoic acid–responsive CD8 effector T cells are selectively increased in IL-23–rich tissue in gastrointestinal GVHD

Author(s) -

Jennifer Ball,

Andrew Clear,

James Aries,

Sarah Charrot,

Caroline Besley,

Matt Mee,

Andrew J. Stagg,

James O. Lindsay,

Jamie Cavenagh,

Maria Calaminci,

John G. Gribben,

Jeff Davies

Publication year - 2020

Publication title -

blood

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.515

H-Index - 465

eISSN - 1528-0020

pISSN - 0006-4971

DOI - 10.1182/blood.2020005170

Subject(s) - cd8 , biology , immunology , cytotoxic t cell , peripheral blood mononuclear cell , t cell , haematopoiesis , graft versus host disease , population , cancer research , stem cell , immune system , microbiology and biotechnology , medicine , in vitro , biochemistry , environmental health

Gastrointestinal (GI) graft-versus-host disease (GVHD) is a major barrier in allogeneic hematopoietic stem cell transplantation (allo-HSCT). The metabolite retinoic acid (RA) potentiates GI-GVHD in mice via alloreactive T cells expressing the RA receptor-α (RARα), but the role of RA-responsive cells in human GI-GVHD remains undefined. Therefore, we used conventional and novel sequential immunostaining and flow cytometry to scrutinize RA-responsive T cells in tissues and blood of patients who had received allo-HSCT and to characterize the impact of RA on human T-cell alloresponses. Expression of RARα by human mononuclear cells was increased after exposure to RA. RARαhi mononuclear cells were increased in GI-GVHD tissue, contained more cellular RA-binding proteins, localized with tissue damage, and correlated with GVHD severity and mortality. By using a targeted candidate protein approach, we predicted the phenotype of RA-responsive T cells in the context of increased microenvironmental interleukin-23 (IL-23). Sequential immunostaining confirmed the presence of a population of RARαhi CD8 T cells with the predicted phenotype that coexpressed the effector T-cell transcription factor T-bet and the IL-23–specific receptor (IL-23R). These cells were increased in GI- but not skin-GVHD tissues and were also selectively expanded in the blood of patients with GI-GVHD. Finally, functional approaches demonstrated that RA predominantly increased alloreactive GI-tropic RARαhi CD8 effector T cells, including cells with the phenotype identified in vivo. IL-23–rich conditions potentiated this effect by selectively increasing β7 integrin expression on CD8 effector T cells and reducing CD4 T cells with a regulatory cell phenotype. In summary, we have identified a population of RA-responsive effector T cells with a distinctive phenotype that is selectively expanded in human GI-GVHD and that represents a potential new therapeutic target.

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