A191 THE NEURAL SIGNAL, CALCITONIN GENE-RELATED PEPTIDE (CGRG) ENHANCES A REGULATORY PHENOTYPE IN THE HUMAN IL-4-TREATED MACROPHAGE
B E Callejas Pina, J A Sousa, K Flannigan, A Wang, S Li, S Rajeev, R Panaccione, D McKay

TL;DR
This study shows that calcitonin gene-related peptide enhances the anti-inflammatory and wound-healing abilities of IL-4-treated macrophages in a mouse model of colitis.
Contribution
The novel finding is that CGRP signaling boosts the reparative and anti-colitic functions of IL-4-treated macrophages.
Findings
CGRP-treated IL-4 macrophages showed increased anti-colitic effects in mice compared to untreated macrophages.
Conditioned medium from CGRP-treated macrophages improved epithelial wound healing in vitro.
COX-1 and PGD2 are involved in the enhanced repair function of CGRP-treated macrophages.
Abstract
Interlukin-4 activated human macrophages (M(IL4) promote epithelial wound healing and exert an anti-colitic effect in a murine model. Blood monocyte-derived M(IL4)s from healthy donors and individuals with Crohn’s disease had increased mRNA expression of the calcitonin gene-related peptide (CGRP) receptor chain, RAMP1, raising the issue of neural modulation of the M(IL4)s reparative function. To determine if CGRP-RAMP1 signalling in human IL-4 treated macrophages enhances the anti-colitic phenotype. Peripheral blood mononuclear cells from healthy volunteers (HD) and individuals with Crohn’s disease were cultured on plastic (2h, 37°C) and non-adherent cells removed. The adherent cells were cultured with recombinant hM-CSF (10 ng/ml) for 7 days. The resultant macrophages (2.5×105) were differentiated with IL-4 (48h 10 ng/mL). In other cells, CGRP (10 nM) was added 24h after IL-4 and…
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Taxonomy
Topics14-3-3 protein interactions · Immune cells in cancer
