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Genome-wide mapping of mesoscale neuronal RNA organization and condensation

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NIAID Data Ecosystem2026-05-02 收录
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https://www.ncbi.nlm.nih.gov/bioproject/PRJNA1241813
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Subcellular RNA organization can affect critical cellular functions. However, our understanding of RNA microenvironments, particularly biomolecular condensates, remains limited, largely due to a lack of technologies to comprehensively interrogate mesoscale RNA organization. Here, we adapt Split-Pool Recognition of Interactions by Tag Extension to map micron-scale RNA-RNA spatial proximity genome-wide across cell regions (RNA-SPRITE). Deploying RNA-SPRITE, we find evidence of extensive, conserved organization of mature mRNAs, with increased colocalization between mRNAs that share RNA-binding protein (RBP) motifs or encode functionally related proteins. Both effects are especially strong in dendrites and axons, suggesting prevalent mRNA co-regulation. Moreover, mRNAs with less compact folding, lower translation efficiency, and specific RBP motifs are more likely to be in RNA-rich condensates. However, perturbations that broadly dissolve or enhance condensation reveal that RBP motif and encoded protein-mediated colocalizations largely remain intact, independent of condensation. These results demonstrate the power of RNA-SPRITE in revealing critical aspects of RNA's functional organization.
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2025-03-25
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