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MAPK signaling and a mobile scaffold complex regulate AMPA receptor transport to modulate synaptic strength

Frédéric J. Hoerndli, Penelope J. Brockie, Rui Wang, Jerry E. Mellem, Angy J. Kallarackal, Rachel L. Doser, Dayton M. Pierce, David M. Madsen, Andres V. Maricq

2022Cell Reports20 citationsDOIOpen Access PDF

Abstract

Synaptic plasticity depends on rapid experience-dependent changes in the number of neurotransmitter receptors. Previously, we demonstrated that motor-mediated transport of AMPA receptors (AMPARs) to and from synapses is a critical determinant of synaptic strength. Here, we describe two convergent signaling pathways that coordinate the loading of synaptic AMPARs onto scaffolds, and scaffolds onto motors, thus providing a mechanism for experience-dependent changes in synaptic strength. We find that an evolutionarily conserved JIP-protein scaffold complex and two classes of mitogen-activated protein kinase (MAPK) proteins mediate AMPAR transport by kinesin-1 motors. Genetic analysis combined with in vivo, real-time imaging in Caenorhabditis elegans revealed that CaMKII is required for loading AMPARs onto the scaffold, and MAPK signaling is required for loading the scaffold complex onto motors. Our data support a model where CaMKII signaling and a MAPK-signaling pathway cooperate to facilitate the rapid exchange of AMPARs required for early stages of synaptic plasticity.

Topics & Concepts

AMPA receptorScaffold proteinSynaptic plasticityCell biologyMAPK/ERK pathwaySynaptic scalingNeuroscienceBiologySignal transductionChemistryMetaplasticityReceptorGlutamate receptorBiochemistryGenetics, Aging, and Longevity in Model OrganismsMitochondrial Function and PathologyPhotoreceptor and optogenetics research