Dendritic cell-derived hepcidin sequesters iron from the microbiota to promote mucosal healing
Citation:
Bessman NJ, Mathieu JRR, Renassia C, Zhou L, Fung TC, Fernandez KC, Austin C, Moeller JB, Zumerle S, Louis S, Vaulont S, Ajami NJ, Sokol H, Putzel GG, Arvedson T, Sockolow RE, Lakhal-Littleton S, Cloonan SM, Arora M, Peyssonnaux C, Sonnenberg GF. Dendritic cell-derived hepcidin sequesters iron from the microbiota to promote mucosal healing, Science, 2020 Apr 10;368(6487):186-189Download Item:
Abstract:
Bleeding and altered iron distribution occur in multiple gastrointestinal diseases, but theimportance and regulation of these changes remain unclear. We found that hepcidin, themaster regulator of systemic iron homeostasis, is required for tissue repair in the mouseintestine after experimental damage. This effect was independent of hepatocyte-derivedhepcidin or systemic iron levels. Rather, we identified conventional dendritic cells (cDCs) asa source of hepcidin that is induced by microbial stimulation in mice, prominent in theinflamed intestine of humans, and essential for tissue repair. cDC-derived hepcidin actedon ferroportin-expressing phagocytes to promote local iron sequestration, which regulated themicrobiota and consequently facilitated intestinal repair. Collectively, these results identify apathway whereby cDC-derived hepcidin promotes mucosal healing in the intestine throughmeans of nutritional immunity.
Sponsor
Grant Number
Science Foundation Ireland
FRL4862
Author's Homepage:
http://people.tcd.ie/cloonasDescription:
PUBLISHED
Author: Cloonan, Suzanne
Type of material:
Journal ArticleCollections
Series/Report no:
Science (New York, N.Y.);368;
6487;
Availability:
Full text availableDOI:
http://dx.doi.org/10.1126/science.aau6481ISSN:
0036-8075Metadata
Show full item recordLicences: