Vascular disease persistence in giant cell arteritis: are stromal cells neglected?

Maira Karabayas; Hafeez E Ibrahim; Anke J Roelofs; Gary Reynolds; Dana Kidder; Cosimo De Bari

doi:10.1136/ard-2023-225270

Vascular disease persistence in giant cell arteritis: are stromal cells neglected?

Ann Rheum Dis. 2024 Apr 29:ard-2023-225270. doi: 10.1136/ard-2023-225270. Online ahead of print.

Authors

Maira Karabayas^#¹, Hafeez E Ibrahim^#², Anke J Roelofs², Gary Reynolds³, Dana Kidder², Cosimo De Bari¹

Affiliations

¹ Centre for Arthritis and Musculoskeletal Health, University of Aberdeen, Aberdeen, UK maira.karabayas@abdn.ac.uk c.debari@abdn.ac.uk.
² Centre for Arthritis and Musculoskeletal Health, University of Aberdeen, Aberdeen, UK.
³ Centre for Immunology, Massachusetts General Hospital, Boston, Massachusetts, USA.

^# Contributed equally.

PMID: 38684323
DOI: 10.1136/ard-2023-225270

Abstract

Giant cell arteritis (GCA), the most common systemic vasculitis, is characterised by aberrant interactions between infiltrating and resident cells of the vessel wall. Ageing and breach of tolerance are prerequisites for GCA development, resulting in dendritic and T-cell dysfunction. Inflammatory cytokines polarise T-cells, activate resident macrophages and synergistically enhance vascular inflammation, providing a loop of autoreactivity. These events originate in the adventitia, commonly regarded as the biological epicentre of the vessel wall, with additional recruitment of cells that infiltrate and migrate towards the intima. Thus, GCA-vessels exhibit infiltrates across the vascular layers, with various cytokines and growth factors amplifying the pathogenic process. These events activate ineffective repair mechanisms, where dysfunctional vascular smooth muscle cells and fibroblasts phenotypically shift along their lineage and colonise the intima. While high-dose glucocorticoids broadly suppress these inflammatory events, they cause well known deleterious effects. Despite the emerging targeted therapeutics, disease relapse remains common, affecting >50% of patients. This may reflect a discrepancy between systemic and local mediators of inflammation. Indeed, temporal arteries and aortas of GCA-patients can show immune-mediated abnormalities, despite the treatment induced clinical remission. The mechanisms of persistence of vascular disease in GCA remain elusive. Studies in other chronic inflammatory diseases point to the fibroblasts (and their lineage cells including myofibroblasts) as possible orchestrators or even effectors of disease chronicity through interactions with immune cells. Here, we critically review the contribution of immune and stromal cells to GCA pathogenesis and analyse the molecular mechanisms by which these would underpin the persistence of vascular disease.

Keywords: Fibroblasts; Giant Cell Arteritis; Inflammation; Vasculitis.

Publication types

Review