Frontiers in Molecular Neuroscience (Oct 2024)

Spatially resolved transcriptomic signatures of hippocampal subregions and Arc-expressing ensembles in active place avoidance memory

  • Isaac Vingan,
  • Shwetha Phatarpekar,
  • Victoria Sook Keng Tung,
  • Alejandro Iván Hernández,
  • Alejandro Iván Hernández,
  • Alejandro Iván Hernández,
  • Oleg V. Evgrafov,
  • Oleg V. Evgrafov,
  • Oleg V. Evgrafov,
  • Oleg V. Evgrafov,
  • Juan Marcos Alarcon,
  • Juan Marcos Alarcon,
  • Juan Marcos Alarcon

DOI
https://doi.org/10.3389/fnmol.2024.1386239
Journal volume & issue
Vol. 17

Abstract

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The rodent hippocampus is a spatially organized neuronal network that supports the formation of spatial and episodic memories. We conducted bulk RNA sequencing and spatial transcriptomics experiments to measure gene expression changes in the dorsal hippocampus following the recall of active place avoidance (APA) memory. Through bulk RNA sequencing, we examined the gene expression changes following memory recall across the functionally distinct subregions of the dorsal hippocampus. We found that recall induced differentially expressed genes (DEGs) in the CA1 and CA3 hippocampal subregions were enriched with genes involved in synaptic transmission and synaptic plasticity, while DEGs in the dentate gyrus (DG) were enriched with genes involved in energy balance and ribosomal function. Through spatial transcriptomics, we examined gene expression changes following memory recall across an array of spots encompassing putative memory-associated neuronal ensembles marked by the expression of the IEGs Arc, Egr1, and c-Jun. Within samples from both trained and untrained mice, the subpopulations of spatial transcriptomic spots marked by these IEGs were transcriptomically and spatially distinct from one another. DEGs detected between Arc + and Arc− spots exclusively in the trained mouse were enriched in several memory-related gene ontology terms, including “regulation of synaptic plasticity” and “memory.” Our results suggest that APA memory recall is supported by regionalized transcriptomic profiles separating the CA1 and CA3 from the DG, transcriptionally and spatially distinct IEG expressing spatial transcriptomic spots, and biological processes related to synaptic plasticity as a defining the difference between Arc + and Arc− spatial transcriptomic spots.

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