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. 2025 Jul 7;222(7):e20242007.
doi: 10.1084/jem.20242007. Epub 2025 Apr 22.

Prenatally derived macrophages support choroidal health and decline in age-related macular degeneration

Seth D Fortmann  1   2 Blake F Frey  1   3 Robert F Rosencrans  1   2 Yvonne Adu-Rutledge  2 Edgar Ready V  2 Kameron V Kilchrist  4 Robert S Welner  5 Michael E Boulton  2 Daniel R Saban  6 Maria B Grant  2
Affiliations

Prenatally derived macrophages support choroidal health and decline in age-related macular degeneration

Seth D Fortmann et al. J Exp Med. .

Abstract

Hallmark findings in age-related macular degeneration (AMD) include the accumulation of extracellular lipid and vasodegeneration of the choriocapillaris. Choroidal inflammation has long been associated with AMD, but little is known about the immune landscape of the human choroid. Using 3D multiplex immunofluorescence, single-cell RNA sequencing, and flow cytometry, we unravel the cellular composition and spatial organization of the human choroid and the immune cells within it. We identify two populations of choroidal macrophages with distinct FOLR2 expression that account for the majority of myeloid cells. FOLR2+ macrophages predominate in the nondiseased eye, express lipid-handling machinery, uptake lipoprotein particles, and contain high amounts of lipid. In AMD, FOLR2+ macrophages are decreased in number and exhibit dysfunctional lipoprotein metabolism. In mice, FOLR2+ macrophages are negative for the postnatal fate-reporter Ms4a3, and their depletion causes an accelerated AMD-like phenotype. Our results show that prenatally derived resident macrophages decline in AMD and are implicated in multiple hallmark functions known to be compromised in the disease.

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Conflict of interest statement

Disclosures: K.V. Kilchrist reported personal fees from Kodiak Sciences Inc. during the conduct of the study. No other disclosures were reported.

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