CD4+ Tissue-resident Memory T Cells Expand and Are a Major Source of Mucosal Tumour Necrosis Factor α in Active Crohn’s Disease

Author:

Bishu Shrinivas1ORCID,El Zaatari Mohammed12,Hayashi Atsushi13,Hou Guoqing1,Bowers Nicole1,Kinnucan Jami12,Manoogian Beth12,Muza-Moons Michelle12,Zhang Min1,Grasberger Helmut1,Bourque Charlie1,Zou Weiping4,Higgins Peter D R12,Spence Jason R15,Stidham Ryan W12,Kamada Nobuhiko1,Kao John Y1

Affiliation:

1. Division of Gastroenterology, Department of Medicine, University of Michigan, AnnArbor, MI, USA

2. University of Michigan Crohn’s and Colitis Program, University of Michigan, AnnArbor, MI, USA

3. Tokyo R&D Center, Miyarisan Pharmaceutical, Tokyo, Japan

4. Department of Surgery, University of Michigan, AnnArbor, MI, USA

5. Department of Cell and Developmental Biology, University of Michigan, AnnArbor, MI, US

Abstract

Abstract Background and Aims Tumour necrosis factor [TNF]α- and IL-17A-producing T cells are implicated in Crohn’s disease [CD]. Tissue-resident memory T [TRM] cells are tissue-restricted T cells that are regulated by PR zinc finger domain 1 [PRDM1], which has been implicated in pathogenic Th17 cell responses. TRM cells provide host defence but their role in CD is unknown. We thus examined CD4+ TRM cells in CD. Methods Colon samples were prospectively collected at endoscopy or surgery in CD and control subjects. Flow cytometry and ex vivo assays were performed to characterise CD4+ TRM cells. Results CD4+ TRM cells are the most abundant memory T cell population and are the major T cell source of mucosal TNFα in CD. CD4+ TRM cells are expanded in CD and more avidly produce IL-17A and TNFα relative to control cells. There was a unique population of TNFα+IL-17A+ CD4+ TRM cells in CD which are largely absent in controls. PRDM1 was highly expressed by CD4+ TRM cells but not by other effector T cells. Suppression of PRDM1 was associated with impaired induction of IL17A and TNFA by CD4+ TRM cells Conclusions CD4+ TRM cells are expanded in CD and are a major source of TNFα, suggesting that they are important in CD. PRDM1 is expressed by TRM cells and may regulate their function. Collectively, this argues for prospective studies tracking CD4+ TRM cells over the disease course.

Funder

American Gastroenterological Association-Pfizer

National Institutes of Health

Publisher

Oxford University Press (OUP)

Subject

Gastroenterology,General Medicine

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