ePoster

SINGLE-CELL SPATIAL TRANSCRIPTOMIC PROFILING DEFINES A PATHOGENIC INFLAMMATORY NICHE IN CHRONIC ACTIVE MULTIPLE SCLEROSIS LESIONS

Ruoqing Feng

German Center for Neurodegenerative Diseases

FENS Forum 2026 (2026)

Barcelona, Spain

Board PS03-08AM-011

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Board: PS03-08AM-011

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SINGLE-CELL SPATIAL TRANSCRIPTOMIC PROFILING DEFINES A PATHOGENIC INFLAMMATORY NICHE IN CHRONIC ACTIVE MULTIPLE SCLEROSIS LESIONS poster preview

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PS03-08AM-011

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Abstract

Compartmentalized inflammation is a key driver of multiple sclerosis (MS) progression, but the mechanisms sustaining its persistence remain unclear. A hallmark of this persistent and slowly evolving inflammatory process is chronic active MS lesions. We generated a high-resolution, single-cell molecular and spatial atlas of such lesions by combining single-nucleus RNA sequencing (snRNA-seq) with multiplexed error-robust fluorescence in situ hybridization (MERFISH). Within lesion rims, we identified CD8⁺ T cell niches associated with inflamed microglia displaying an interferon response and upregulated lipid metabolism. To investigate their function, we deleted ATP-binding cassette transporters A1 and G1 (ABCA1/G1) in the microglia of mice with experimental autoimmune encephalomyelitis (EAE), which increased the formation of lipid-storing phagocytes that amplified inflammation. Moreover, pharmacologically targeting sterol metabolism mitigated foam cell formation and inflammatory demyelination in EAE. Thus, our high-resolution map of immune niches in chronic active MS lesions identifies a role for lipid-storing, dysfunctional microglia in persistent neuroinflammation.

SINGLE-CELL SPATIAL TRANSCRIPTOMIC PROFILING DEFINES A PATHOGENIC INFLAMMATORY NICHE IN CHRONIC ACTIVE MULTIPLE SCLEROSIS LESIONS

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