Notch Signalling Drives Synovial Fibroblast Identity and Arthritis Pathology

Overview

Journal Nature

Specialty Science

Date 2020 Jun 6

PMID 32499639

Citations 203

Authors

Kevin Wei

Ilya Korsunsky

Jennifer L Marshall

Anqi Gao

Gerald F M Watts

Triin Major

Adam P Croft

Jordan Watts

Philip E Blazar

Jeffrey K Lange

Thomas S Thornhill

Andrew Filer

Karim Raza

Laura T Donlin

Christian W Siebel

Christopher D Buckley

Soumya Raychaudhuri

Michael B Brenner

Affiliations

Soon will be listed here.

Abstract

The synovium is a mesenchymal tissue composed mainly of fibroblasts, with a lining and sublining that surround the joints. In rheumatoid arthritis the synovial tissue undergoes marked hyperplasia, becomes inflamed and invasive, and destroys the joint. It has recently been shown that a subset of fibroblasts in the sublining undergoes a major expansion in rheumatoid arthritis that is linked to disease activity; however, the molecular mechanism by which these fibroblasts differentiate and expand is unknown. Here we identify a critical role for NOTCH3 signalling in the differentiation of perivascular and sublining fibroblasts that express CD90 (encoded by THY1). Using single-cell RNA sequencing and synovial tissue organoids, we found that NOTCH3 signalling drives both transcriptional and spatial gradients-emanating from vascular endothelial cells outwards-in fibroblasts. In active rheumatoid arthritis, NOTCH3 and Notch target genes are markedly upregulated in synovial fibroblasts. In mice, the genetic deletion of Notch3 or the blockade of NOTCH3 signalling attenuates inflammation and prevents joint damage in inflammatory arthritis. Our results indicate that synovial fibroblasts exhibit a positional identity that is regulated by endothelium-derived Notch signalling, and that this stromal crosstalk pathway underlies inflammation and pathology in inflammatory arthritis.

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