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Induction of a distinct macrophage population and protection from lung injury and fibrosis by Notch2 blockade

Mayra Cruz Tleugabulova, Sandra P. Melo, Aaron K. Wong, Alexander Arlantico, Meizi Liu, Joshua D. Webster, J. Lau, Antonie Lechner, Basak Corak, Jonathan J. Hodgins, Venkata Garlapati, Marco De Simone, Ben Korin, Shimrit Avraham, Jessica Lund, Surinder Jeet, Alexander Reiss, Hannah Bender, Cary D. Austin, Spyros Darmanis, Zora Modrušan, Hans D. Brightbill, Steffen Durinck, Michael Diamond, Christoph Schneider, Andréy S. Shaw, Maximilian Nitschké

2024Nature Communications30 citationsDOIOpen Access PDF

Abstract

Macrophages are pleiotropic and diverse cells that populate all tissues of the body. Besides tissue-specific resident macrophages such as alveolar macrophages, Kupffer cells, and microglia, multiple organs harbor at least two subtypes of other resident macrophages at steady state. During certain circumstances, like tissue insult, additional subtypes of macrophages are recruited to the tissue from the monocyte pool. Previously, a recruited macrophage population marked by expression of Spp1, Cd9, Gpnmb, Fabp5, and Trem2, has been described in several models of organ injury and cancer, and has been linked to fibrosis in mice and humans. Here, we show that Notch2 blockade, given systemically or locally, leads to an increase in this putative pro-fibrotic macrophage in the lung and that this macrophage state can only be adopted by monocytically derived cells and not resident alveolar macrophages. Using a bleomycin and COVID-19 model of lung injury and fibrosis, we find that the expansion of these macrophages before lung injury does not promote fibrosis but rather appears to ameliorate it. This suggests that these damage-associated macrophages are not, by themselves, drivers of fibrosis in the lung. Macrophages are pleiotropic and can have different functions and phenotypes. Here the authors show that a population of macrophages, previously described as pro-fibrotic, can be induced through Notch2 blockade and that in a mouse lung injury and fibrosis model this macrophage population does not promote inflammation or fibrosis.

Topics & Concepts

BlockadeMacrophageFibrosisPopulationPulmonary fibrosisMedicineImmunologyLungBiologyPathologyInternal medicineGeneticsEnvironmental healthReceptorIn vitroImmune cells in cancerIL-33, ST2, and ILC PathwaysMesenchymal stem cell research
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