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NR4A1 deletion promotes pro-angiogenic polarization of macrophages derived from classical monocytes in a mouse model of neovascular age-related macular degeneration

Steven Droho, Andrew P. Voigt, Jacob Sterling, Amrita Rajesh, Kyle S. Chan, Carla M. Cuda, Harris Perlman, Jeremy A. Lavine

2023Journal of Neuroinflammation19 citationsDOIOpen Access PDF

Abstract

Abstract Background Neovascular age-related macular degeneration causes vision loss from destructive angiogenesis, termed choroidal neovascularization (CNV). Cx3cr1 −/− mice display alterations in non-classical monocytes and microglia with increased CNV size, suggesting that non-classical monocytes may inhibit CNV formation. NR4A1 is a transcription factor that is necessary for maturation of non-classical monocytes from classical monocytes. While Nr4a1 −/− mice are deficient in non-classical monocytes, results are confounded by macrophage hyper-activation. Nr4a1 se2/se2 mice lack a transcriptional activator, resulting in non-classical monocyte loss without macrophage hyper-activation. Main body We subjected Nr4a1 −/− and Nr4a1 se2/se2 mice to the laser-induced CNV model and performed multi-parameter flow cytometry. We found that both models lack non-classical monocytes, but only Nr4a1 −/− mice displayed increased CNV area. Additionally, CD11c + macrophages were increased in Nr4a1 −/− mice. Single-cell transcriptomic analysis uncovered that CD11c + macrophages were enriched from Nr4a1 −/− mice and expressed a pro-angiogenic transcriptomic profile that was disparate from prior reports of macrophage hyper-activation. Conclusions These results suggest that non-classical monocytes are dispensable during CNV, and NR4A1 deficiency results in increased recruitment of pro-angiogenic macrophages.

Topics & Concepts

Choroidal neovascularizationMacular degenerationCD11cMicrogliaMonocyteMacrophageMacrophage polarizationAngiogenesisImmunologyCancer researchTranscriptomeMacrophage colony-stimulating factorFlow cytometryCD68BiologyCCL2MedicineCell biologyInflammationGene expressionGeneGeneticsChemokinePhenotypeOphthalmologyImmunohistochemistryIn vitroNeuroinflammation and Neurodegeneration MechanismsNuclear Receptors and SignalingAngiogenesis and VEGF in Cancer
NR4A1 deletion promotes pro-angiogenic polarization of macrophages derived from classical monocytes in a mouse model of neovascular age-related macular degeneration | Litcius