Axl and MerTK regulate synovial inflammation and are modulated by IL-6 inhibition in rheumatoid arthritis

Author:

Nerviani AlessandraORCID,Boutet Marie-Astrid,Ghirardi Giulia MariaORCID,Goldmann Katriona,Sciacca ElisabettaORCID,Rivellese FeliceORCID,Pontarini ElenaORCID,Prediletto EdoardoORCID,Abatecola FedericoORCID,Caliste Mattia,Pagani Sara,Mauro Daniele,Bellan Mattia,Cubuk Cankut,Lau RachelORCID,Church Sarah E.ORCID,Hudson Briana M.,Humby Frances,Bombardieri Michele,Lewis Myles J.ORCID,Pitzalis CostantinoORCID

Abstract

AbstractThe TAM tyrosine kinases, Axl and MerTK, play an important role in rheumatoid arthritis (RA). Here, using a unique synovial tissue bioresource of patients with RA matched for disease stage and treatment exposure, we assessed how Axl and MerTK relate to synovial histopathology and disease activity, and their topographical expression and longitudinal modulation by targeted treatments. We show that in treatment-naive patients, high AXL levels are associated with pauci-immune histology and low disease activity and inversely correlate with the expression levels of pro-inflammatory genes. We define the location of Axl/MerTK in rheumatoid synovium using immunohistochemistry/fluorescence and digital spatial profiling and show that Axl is preferentially expressed in the lining layer. Moreover, its ectodomain, released in the synovial fluid, is associated with synovial histopathology. We also show that Toll-like-receptor 4-stimulated synovial fibroblasts from patients with RA modulate MerTK shedding by macrophages. Lastly, Axl/MerTK synovial expression is influenced by disease stage and therapeutic intervention, notably by IL-6 inhibition. These findings suggest that Axl/MerTK are a dynamic axis modulated by synovial cellular features, disease stage and treatment.

Funder

RCUK | Medical Research Council

DH | NIHR | Efficacy and Mechanism Evaluation Programme

DH | National Institute for Health Research

RCUK | MRC | Medical Research Foundation

Versus Arthritis [Experimental Arthritis Treatment Centre, grant number 20022]

Versus Arthritis, grant number 21890

Fondation pour la Recherche Médicale

Inserm “ATIP-Avenir” program

Publisher

Springer Science and Business Media LLC

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