IL-23 drives uveitis by acting on a novel population of tissue-resident entheseal T cells

Author:

Hedley Robert,Ward AmyORCID,Chu Colin JORCID,Coupland Sarah EORCID,Kiriakidis SerafimORCID,Taylor Peter CORCID,Dakin Stephanie GORCID, ,Buckley Christopher DORCID,Sherlock Jonathan,Dick Andrew DORCID,Copland David AORCID

Abstract

AbstractRecurrent acute anterior uveitis is a frequent extra-articular manifestation of the axial spondyloarthropathies (AxSpA); chronic inflammatory diseases affecting the spine, enthesis, peripheral joints, skin, and gastrointestinal tract. Pathology in AxSpA has been associated with local tissue-resident populations of interleukin (IL)-23 responsive lymphoid cells. Here we reveal a novel population of ocular T cells defined by CD3+CD4-CD8-γδTCR+IL-23R+ that reside within the anterior uvea as an ocular entheseal analogue of the mouse eye. Localised cytokine expression demonstrates that uveal IL-23R+ IL-17A-producing cells are both necessary and sufficient to drive uveitis in response to IL-23. This T cell population is also present in humans, occupying extravascular tissues of the anterior uveal compartment. Consistent with the concept of IL-23 as a unifying mediator in AxSpA, we present evidence that IL-23 can also act locally on tissue resident T cells in the anterior compartment of the eye at sites analogous to the enthesis to drive ocular inflammation.

Publisher

Cold Spring Harbor Laboratory

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