4.8 Article

A Role for Neuronal piRNAs in the Epigenetic Control of Memory-Related Synaptic Plasticity

Journal

CELL
Volume 149, Issue 3, Pages 693-707

Publisher

CELL PRESS
DOI: 10.1016/j.cell.2012.02.057

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Funding

  1. HHMI [P50 HG002806]
  2. NIH [P01 GM073047]
  3. NRSA [5F30MH086267]

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Small RNA-mediated gene regulation during development causes long-lasting changes in cellular phenotypes. To determine whether small RNAs of the adult brain can regulate memory storage, a process that requires stable and long-lasting changes in the functional state of neurons, we generated small RNA libraries from the Aplysia CNS. In these libraries, we discovered an unexpectedly abundant expression of a 28 nucleotide sized class of piRNAs in brain, which had been thought to be germline specific. These piRNAs have unique biogenesis patterns, predominant nuclear localization, and robust sensitivity to serotonin, a modulatory transmitter that is important for memory. We find that the Piwi/piRNA complex facilitates serotonin-dependent methylation of a conserved CpG island in the promoter of CREB2, the major inhibitory constraint of memory in Aplysia, leading to enhanced long-term synaptic facilitation. These findings provide a small RNA-mediated gene regulatory mechanism for establishing stable long-term changes in neurons for the persistence of memory.

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