| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 4322050 | Neuron | 2011 | 14 Pages |
SummaryNeurexin and neuroligin, which undergo heterophilic interactions with each other at the synapse, are mutated in some patients with autism spectrum disorder, a set of disorders characterized by deficits in social and emotional learning. We have explored the role of neurexin and neuroligin at sensory-to-motor neuron synapses of the gill-withdrawal reflex in Aplysia, which undergoes sensitization, a simple form of learned fear. We find that depleting neurexin in the presynaptic sensory neuron or neuroligin in the postsynaptic motor neuron abolishes both long-term facilitation and the associated presynaptic growth induced by repeated pulses of serotonin. Moreover, introduction into the motor neuron of the R451C mutation of neuroligin-3 linked to autism spectrum disorder blocks both intermediate-term and long-term facilitation. Our results suggest that activity-dependent regulation of the neurexin-neuroligin interaction may govern transsynaptic signaling required for the storage of long-term memory, including emotional memory that may be impaired in autism spectrum disorder.
► Neurexin in the presynaptic neuron mediates LTF and presynaptic structural changes ► Neuroligin in the postsynaptic neuron mediates LTF and presynaptic structural changes ► Neurexin and neuroligin are also important for persistence of long-term facilitation ► Neuroligin autism-linked mutant blocks intermediate-term and long-term facilitation
