Early Pheromone Experience Modifies a Synaptic Activity to Influence Adult Pheromone Responses of C. elegans

  • Myeongjin Hong
  • , Leesun Ryu
  • , Maria C. Ow
  • , Jinmahn Kim
  • , A. Reum Je
  • , Satya Chinta
  • , Yang Hoon Huh
  • , Kea Joo Lee
  • , Rebecca A. Butcher
  • , Hongsoo Choi
  • , Piali Sengupta
  • , Sarah E. Hall
  • , Kyuhyung Kim

Research output: Contribution to journalArticlepeer-review

27 Scopus citations

Abstract

Experiences during early development can influence neuronal functions and modulate adult behaviors [1, 2]. However, the molecular mechanisms underlying the long-term behavioral effects of these early experiences are not fully understood. The C. elegans ascr#3 (asc-ΔC9; C9) pheromone triggers avoidance behavior in adult hermaphrodites [3–7]. Here, we show that hermaphrodites that are briefly exposed to ascr#3 immediately after birth exhibit increased ascr#3-specific avoidance as adults, indicating that ascr#3-experienced animals form a long-lasting memory or imprint of this early ascr#3 exposure [8]. ascr#3 imprinting is mediated by increased synaptic activity between the ascr#3-sensing ADL neurons and their post-synaptic SMB motor neuron partners via increased expression of the odr-2 glycosylated phosphatidylinositol (GPI)-linked signaling gene in the SMB neurons. Our study suggests that the memory for early ascr#3 experience is imprinted via alteration of activity of a single synaptic connection, which in turn shapes experience-dependent plasticity in adult ascr#3 responses. Hong et al. show that early pheromone experience in C. elegans hermaphrodites is imprinted via alteration of activity of a single synaptic connection and, in turn, modulates behavioral responses to the pheromone as adults.

Original languageEnglish
Pages (from-to)3168-3177.e3
JournalCurrent Biology
Volume27
Issue number20
DOIs
StatePublished - Oct 23 2017

Keywords

  • GPI-anchored protein
  • neuronal activity
  • pheromone
  • sensory imprinting
  • synapse

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