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Macrophage-derived IGF-1 protects the neonatal intestine against necrotizing enterocolitis by promoting microvascular development

Xiaocai Yan, Elizabeth Managlia, You‐Yang Zhao, Xiao‐Di Tan, Isabelle G. De Plaen

2022Communications Biology29 citationsDOIOpen Access PDF

Abstract

Necrotizing enterocolitis (NEC) is a deadly bowel necrotic disease of premature infants. Low levels of plasma IGF-1 predispose premature infants to NEC. While increasing evidence suggests that defective perinatal intestinal microvascular development plays a role in NEC, the involved mechanism remains incompletely understood. We report here that serum and intestinal IGF-1 are developmentally regulated during the perinatal period in mice and decrease during experimental NEC. Neonatal intestinal macrophages produce IGF-1 and promote endothelial cell sprouting in vitro via IGF-1 signaling. In vivo, in the neonatal intestine, macrophage-derived IGF-1 promotes VEGF expression and endothelial cell proliferation and protects against experimental NEC. Exogenous IGF-1 preserves intestinal microvascular density and protects against experimental NEC. In human NEC tissues, villous endothelial cell proliferation and IGF-1- producing macrophages are decreased compared to controls. Together, our results suggest that defective IGF-1-production by neonatal macrophages impairs neonatal intestinal microvascular development and predisposes the intestine to necrotizing enterocolitis.

Topics & Concepts

Necrotizing enterocolitisEnterocolitisMacrophageImmunologyEndothelial stem cellBiologyCell growthMedicinePathologyInternal medicineIn vitroBiochemistryGeneticsInfant Nutrition and HealthNeonatal Respiratory Health ResearchCongenital Diaphragmatic Hernia Studies
Macrophage-derived IGF-1 protects the neonatal intestine against necrotizing enterocolitis by promoting microvascular development | Litcius