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Mast cells crosstalk with B cells in the gut and sustain IgA response in the inflamed intestine

Valeri, Viviana
•
Tonon, Silvia
•
Vibhushan, Shamila
altro
Pucillo, Carlo
2020
  • journal article

Periodico
EUROPEAN JOURNAL OF IMMUNOLOGY
Abstract
B lymphocytes are among the cell types whose effector functions are modulated by mast cells (MCs). The B/MC crosstalk emerged in several pathological settings, notably the colon of inflammatory bowel disease (IBD) patients is a privileged site in which MCs and IgA+ cells physically interact. Herein, by inducing conditional depletion of MCs in red MC and basophil (RMB) mice, we show that MCs control B cell distribution in the gut and IgA serum levels. Moreover, in dextran sulfate sodium (DSS)-treated RMB mice, the presence of MCs is fundamental for the enlargement of the IgA+ population in the bowel and the increase of systemic IgA production. Since both conventional B-2 and peritoneal-derived B cells populate the intestine and communicate with MCs in physiological conditions and during inflammation, we further explored this interplay through the use of co-cultures. We show that MCs finely regulate different aspects of splenic B cell biology while peritoneal B cells are unresponsive to the supporting effects provided by MCs. Interestingly, peritoneal B cells induce a pro-inflammatory skewing in MCs, characterized by increased ST2 and TNF-alpha expression. Altogether, this study uncovers the versatility of the B/MC liaison and highlights key aspects for the resolution of intestinal inflammation. This article is protected by copyright. All rights reserved.
DOI
10.1002/eji.202048668
WOS
WOS:000577677200001
Archivio
http://hdl.handle.net/11390/1191382
info:eu-repo/semantics/altIdentifier/scopus/2-s2.0-85092561891
Diritti
metadata only access
Soggetti
  • Cell-to-cell interpla...

  • Coliti

  • IgA

  • Innate-like B cell

  • Mast cells

Scopus© citazioni
2
Data di acquisizione
Jun 14, 2022
Vedi dettagli
Web of Science© citazioni
6
Data di acquisizione
Mar 22, 2024
Visualizzazioni
22
Data di acquisizione
Apr 19, 2024
Vedi dettagli
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