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Macrophages and nociceptor neurons form a sentinel unit around fenestrated capillaries to defend the synovium from circulating immune challenge

Hasegawa, Tetsuo and Lee, Colin Y. C. and Hotchen, Andrew J. and Fleming, Aaron and Singh, Rahul and Suzuki, Kunimichi and Yuzaki, Michisuke and Watanabe, Masahiko and Birch, Mark A. and McCaskie, Andrew W. and Lénárt, Nikolett and Tóth, Krisztina and Dénes, Ádám and Liu, Zhaoyuan and Ginhoux, Florent and Richoz, Nathan and Clatworthy, Menna R. (2024) Macrophages and nociceptor neurons form a sentinel unit around fenestrated capillaries to defend the synovium from circulating immune challenge. NATURE IMMUNOLOGY, 25 (12). pp. 2270-2283. ISSN 1529-2908

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Abstract

A wide variety of systemic pathologies, including infectious and autoimmune diseases, are accompanied by joint pain or inflammation, often mediated by circulating immune complexes (ICs). How such stimuli access joints and trigger inflammation is unclear. Whole-mount synovial imaging revealed PV1 + fenestrated capillaries at the periphery of the synovium in the lining–sublining interface. Circulating ICs extravasated from these PV1 + capillaries, and nociceptor neurons and three distinct macrophage subsets formed a sentinel unit around them. Macrophages showed subset-specific responses to systemic IC challenge; LYVE1 + CX 3 CR1 + macrophages orchestrated neutrophil recruitment and activated calcitonin gene-related peptide + (CGRP + ) nociceptor neurons via interleukin-1β. In contrast, major histocompatibility complex class II + CD11c + (MHCII + CD11c + ) and MHCII + CD11c – interstitial macrophages formed tight clusters around PV1 + capillaries in response to systemic immune stimuli, a feature enhanced by nociceptor-derived CGRP. Altogether, we identify the anatomical location of synovial PV1 + capillaries and subset-specific macrophage–nociceptor cross-talk that forms a blood–joint barrier protecting the synovium from circulating immune challenges.

Item Type: Article
Uncontrolled Keywords: Innate immunity, Monocytes and macrophages, Neuroimmunology, Systemic lupus erythematosus
Subjects: R Medicine / orvostudomány > R1 Medicine (General) / orvostudomány általában
SWORD Depositor: MTMT SWORD
Depositing User: MTMT SWORD
Date Deposited: 13 Dec 2024 10:40
Last Modified: 13 Dec 2024 10:40
URI: https://real.mtak.hu/id/eprint/211623

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