Cell
Volume 169, Issue 5, 18 May 2017, Pages 836-848.e15
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Article
Regulated Intron Removal Integrates Motivational State and Experience

https://doi.org/10.1016/j.cell.2017.05.006Get rights and content
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Highlights

  • Orb2A mRNA is expressed as an unspliced non-protein coding mRNA in the adult brain

  • Some, but not all, behavioral training increases spliced protein coding mRNA level

  • The splicing regulator pasilla controls the abundance of spliced mRNA level

  • Single-nucleotide substitution in the intron attenuates splicing and inhibits memory

Summary

Myriad experiences produce transient memory, yet, contingent on the internal state of the organism and the saliency of the experience, only some memories persist over time. How experience and internal state influence the duration of memory at the molecular level remains unknown. A self-assembled aggregated state of Drosophila Orb2A protein is required specifically for long-lasting memory. We report that in the adult fly brain the mRNA encoding Orb2A protein exists in an unspliced non-protein-coding form. The convergence of experience and internal drive transiently increases the spliced protein-coding Orb2A mRNA. A screen identified pasilla, the fly ortholog of mammalian Nova-1/2, as a mediator of Orb2A mRNA processing. A single-nucleotide substitution in the intronic region that reduces Pasilla binding and intron removal selectively impairs long-term memory. We posit that pasilla-mediated processing of unspliced Orb2A mRNA integrates experience and internal state to control Orb2A protein abundance and long-term memory formation.

Keywords

prion
amyloid
long-term memory
motivation
intron retention
detained-intron
poised splicing
pasilla
Nova

Cited by (0)

3

These authors contributed equally

4

Present address: Fellow, Division of Pediatric Neurology and Developmental Neuroscience, Baylor College of Medicine, Houston, Texas 77030, USA

5

Present address: Dovetail Genomics, Santa Cruz, CA 95060, USA

6

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