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Fat-associated lymphoid clusters control local IgM secretion during pleural infection and lung inflammation

Authors :
Lucy H, Jackson-Jones
Sheelagh M, Duncan
Marlène S, Magalhaes
Sharon M, Campbell
Rick M, Maizels
Henry J, McSorley
Judith E, Allen
Cécile, Bénézech
Source :
Nature Communications
Publication Year :
2016

Abstract

Fat-associated lymphoid clusters (FALC) are inducible structures that support rapid innate-like B-cell immune responses in the serous cavities. Little is known about the physiological cues that activate FALCs in the pleural cavity and more generally the mechanisms controlling B-cell activation in FALCs. Here we show, using separate models of pleural nematode infection with Litomosoides sigmodontis and Altenaria alternata induced acute lung inflammation, that inflammation of the pleural cavity rapidly activates mediastinal and pericardial FALCs. IL-33 produced by FALC stroma is crucial for pleural B1-cell activation and local IgM secretion. However, B1 cells are not the direct target of IL-33, which instead requires IL-5 for activation. Moreover, lung inflammation leads to increased IL-5 production by type 2 cytokine-producing innate lymphoid cells (ILC2) in the FALC. These findings reveal a link between inflammation, IL-33 release by FALC stromal cells, ILC2 activation and pleural B-cell activation in FALCs, resulting in local and antigen-specific IgM production.<br />Fat-associated lymphoid clusters (FALC) in the serous cavities house rapid IgM-producing B1 cells, but how the clusters are activated to respond to infection is unclear. Here the authors show that in response to lung inflammation or pleural nematode infection adipose stromal cell-derived IL-33 activates ILC2s to produce IL-5, thus driving the B1 response in the FALCs.

Details

ISSN :
20411723
Volume :
7
Database :
OpenAIRE
Journal :
Nature communications
Accession number :
edsair.pmid..........f10836853590b41cdd9572ca42e965df