Neonatal imprinting of alveolar macrophages via neutrophil-derived 12-HETE.
Erwan PernetSarah SunNicole SardenSaideep GonaAngela P NguyenNargis KhanMartin MawhinneyKim A TranJulia ChronopoulosDnyandeo AmberkarMina SadeghiAlexandre GrantShradha WaliRenaud PrevelJun DingJames G MartinAjitha ThanabalasuriarBryan G YippLuis B BarreiroMaziar DivangahiPublished in: Nature (2023)
Resident-tissue macrophages (RTMs) arise from embryonic precursors 1,2 , yet the developmental signals that shape their longevity remain largely unknown. Here we demonstrate in mice genetically deficient in 12-lipoxygenase and 15-lipoxygenase (Alox15 -/- mice) that neonatal neutrophil-derived 12-HETE is required for self-renewal and maintenance of alveolar macrophages (AMs) during lung development. Although the seeding and differentiation of AM progenitors remained intact, the absence of 12-HETE led to a significant reduction in AMs in adult lungs and enhanced senescence owing to increased prostaglandin E 2 production. A compromised AM compartment resulted in increased susceptibility to acute lung injury induced by lipopolysaccharide and to pulmonary infections with influenza A virus or SARS-CoV-2. Our results highlight the complexity of prenatal RTM programming and reveal their dependency on in trans eicosanoid production by neutrophils for lifelong self-renewal.
Keyphrases
- sars cov
- high fat diet induced
- lps induced
- lipopolysaccharide induced
- inflammatory response
- wild type
- pregnant women
- dna damage
- endothelial cells
- transcranial magnetic stimulation
- type diabetes
- genome wide
- dna methylation
- insulin resistance
- single cell
- quality improvement
- oxidative stress
- adipose tissue
- young adults
- skeletal muscle
- high frequency