GM-CSF Calibrates Macrophage Defense and Wound Healing Programs during Intestinal Infection and Inflammation

GM-CSF在肠道感染和炎症期间调节巨噬细胞防御和伤口愈合程序

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作者:Tomas Castro-Dopico ,Aaron Fleming ,Thomas W Dennison ,John R Ferdinand ,Katherine Harcourt ,Benjamin J Stewart ,Zaeem Cader ,Zewen K Tuong ,Chenzhi Jing ,Laurence S C Lok ,Rebeccah J Mathews ,Anaïs Portet ,Arthur Kaser ,Simon Clare ,Menna R Clatworthy

Abstract

Macrophages play a central role in intestinal immunity, but inappropriate macrophage activation is associated with inflammatory bowel disease (IBD). Here, we identify granulocyte-macrophage colony stimulating factor (GM-CSF) as a critical regulator of intestinal macrophage activation in patients with IBD and mice with dextran sodium sulfate (DSS)-induced colitis. We find that GM-CSF drives the maturation and polarization of inflammatory intestinal macrophages, promoting anti-microbial functions while suppressing wound-healing transcriptional programs. Group 3 innate lymphoid cells (ILC3s) are a major source of GM-CSF in intestinal inflammation, with a strong positive correlation observed between ILC or CSF2 transcripts and M1 macrophage signatures in IBD mucosal biopsies. Furthermore, GM-CSF-dependent macrophage polarization results in a positive feedback loop that augmented ILC3 activation and type 17 immunity. Together, our data reveal an important role for GM-CSF-mediated ILC-macrophage crosstalk in calibrating intestinal macrophage phenotype to enhance anti-bacterial responses, while inhibiting pro-repair functions associated with fibrosis and stricturing, with important clinical implications.

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