Substantive Similarities Between Synovial Fluid and Synovial Tissue T cells in Inflammatory Arthritis Via Single‐Cell RNA and T cell Receptor Sequencing

Author:

Durham Lucy E.1ORCID,Humby Frances C.2,Ng Nora2,Ryan Sarah1,Nuamah Rosamond2,Fung Kathy2,Kallayil Athul Menon2,Dhami Pawan2,Kirkham Bruce W.2ORCID,Taams Leonie S.1ORCID

Affiliation:

1. King's College London London United Kingdom

2. Guy's and St Thomas’ NHS Foundation Trust London United Kingdom

Abstract

ObjectiveSynovial fluid (SF)–derived T cells are frequently studied as a proxy for investigating the synovial tissue (ST) T cell infiltrate in inflammatory arthritis. However, because ST is the primary site of inflammatory activity, there is debate as to whether SF provides a true reflection of the ST T cell population.MethodsIn this study, we used single‐cell RNA sequencing paired with single‐cell T cell receptor (TCR) sequencing to directly compare memory T cells from paired samples of SF and ST from six patients with inflammatory arthritis to investigate their similarity in terms of TCR repertoire and T cell subset composition.ResultsThe TCR repertoires of SF and ST T cells were strikingly similar, particularly for CD8+ T cells. A median of 49% of the total CD8+ TCR repertoire in SF was shared with ST, compared with 20% shared with blood. Similarly, 47% of the ST CD8+ TCR repertoire was shared with SF compared to 25% with blood. Furthermore, once the effect of collagenase digestion on gene expression by ST T cells had been accounted for, the frequencies of specific CD8+ and CD4+ T cell subsets were, in general, similar in SF and ST and were distinct from blood.ConclusionOur results suggest that T cells migrate and equilibrate between the SF and ST and maintain similar phenotypes in both sites. We conclude that SF is an appropriate proxy for investigating the T cell infiltrate in inflamed synovium, particularly in terms of investigating the TCR repertoire.image

Funder

Medical Research Council

Publisher

Wiley

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