NEUROPEPTIDE ARCHITECTURE OF THE DORSAL RAPHE NUCLEUS AND ITS MODULATION BY HIGH-FAT DIET
Stockholm University
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Date TBA
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Poster Board
PS07-10AM-044
Poster
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Beyond classical neurotransmitters, the DR expresses a diverse repertoire of neuropeptides and receptors implicated in energy balance, including Neuropeptide Y, Somatostatin, Cholecystokinin, Galanin, and the Melanocortin-4 receptor. However, the spatial organization of these signalling systems and their cell-type-specific expression within the DR remain understudied. To address this, we employed Xenium, an imaging-based spatial transcriptomics platform enabling highly multiplexed, single-cell RNA detection while preserving tissue architecture. Applied to the mouse DR, Xenium enabled simultaneous mapping of neurotransmitter markers, neuropeptides, and receptor transcripts, revealing molecularly defined cell populations and their spatial relationships across DR subdomains. This approach provides a spatially resolved framework for understanding neuropeptide organization in the DR.
Building on this baseline, we examined the effects of chronic high-fat diet (HFD) in mice, a widely used model of Western-style diets that promote obesity and metabolic dysfunction and are associated with altered feeding and affective behaviour. Using Xenium, we find that HFD induces cell-type-specific alterations in neuropeptide and neurotransmitter gene expression within discrete DR populations, suggesting that diet is associated with remodelling of local DR networks.
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