The original MALDI-MSI raw data from aged/young adult mouse brain
收藏Figshare2026-03-13 更新2026-04-28 收录
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Spatial transcriptomics (ST) and spatial metabolomics (SM) provide complementary insights into cellular communication within complex tissues, yet their integration is hindered by mismatched resolution and dimensionality. We introduce Spatial Cross-Omics Fitting (SCrOFit), a computational framework that enables cellular-resolution alignment of SM and ST data. SCrOFit leverages a minimum-cost optimal transport model to couple SM pixels with ST-defined cell identities, effectively bridging the resolution gap, achieving precise cross-modality integration. This approach reveals the transcriptomic mechanisms underlying metabolomic features at the single-cell level. Applying SCrOFit to the aging mouse brain, we identify a distinct spatial metabolic reprogramming in the hippocampus, characterized by a transition from glycogen catabolism to ketone body utilization. Mechanistically, we show that downregulation of phosphorylase kinase in aging astrocytes serves as a molecular bottleneck for glycogen degradation, driving these observed metabolic shifts. SCrOFit provides a robust tool for spatially resolved multi-omics analysis, offering new opportunities to dissect molecular dynamics across diverse biological contexts.
创建时间:
2026-03-13



