Local amplifiers of IL-4R alpha-mediated macrophage activation promote repair in lung and liver
Minutti, Carlos M.; Jackson-Jones, Lucy H.; Garcia-Fojeda, Belen; Knipper, Johanna A.; Sutherland, Tara E.; Logan, Nicola; Rinqvist, Emma; Guillamat-Prats, Raquel; Ferenbach, David A.; Artigas, Antonio; Stamme, Cordula; Chroneos, Zissis C.; Zaiss, Dietmar
SCIENCE
2017
VL / 356 - BP / 1076 - EP / 1080
abstract
The type 2 immune response controls helminth infection and maintains tissue homeostasis but can lead to allergy and fibrosis if not adequately regulated. We have discovered local tissue-specific amplifiers of type 2-mediated macrophage activation. In the lung, surfactant protein A (SP-A) enhanced interleukin-4 (IL-4)-dependent macrophage proliferation and activation, accelerating parasite clearance and reducing pulmonary injury after infection with a lung-migrating helminth. In the peritoneal cavity and liver, C1q enhancement of type 2 macrophage activation was required for liver repair after bacterial infection, but resulted in fibrosis after peritoneal dialysis. IL-4 drives production of these structurally related defense collagens, SP-A and C1q, and the expression of their receptor, myosin 18A. These findings reveal the existence within different tissues of an amplification system needed for local type 2 responses.
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