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Neuron-Specific Regulation of Associative Learning and Memory by MAGI-1 in C. elegans
Author(s) -
Attila Steták,
Frédéric Hörndli,
Andres V. Maricq,
Sander van den Heuvel,
Alex Hajnal
Publication year - 2009
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0006019
Subject(s) - neuroscience , associative learning , biology , memory consolidation , synaptic plasticity , pdz domain , neuron , glutamatergic , biological neural network , glutamate receptor , hippocampus , microbiology and biotechnology , receptor , biochemistry
Background Identifying the molecular mechanisms and neural circuits that control learning and memory are major challenges in neuroscience. Mammalian MAGI/S-SCAM is a multi-PDZ domain synaptic scaffolding protein that interacts with a number of postsynaptic signaling proteins and is thereby thought to regulate synaptic plasticity [1] , [2] , [3] . Principal Findings While investigating the behavioral defects of C. elegans nematodes carrying a mutation in the single MAGI ortholog magi-1 , we have identified specific neurons that require MAGI-1 function for different aspects of associative learning and memory. Various sensory stimuli and a food deprivation signal are associated in RIA interneurons during learning, while additional expression of MAGI-1 in glutamatergic AVA, AVD and possibly AVE interneurons is required for efficient memory consolidation, i.e. the ability to retain the conditioned changes in behavior over time. During associative learning, MAGI-1 in RIA neurons controls in a cell non-autonomous fashion the dynamic remodeling of AVA, AVD and AVE synapses containing the ionotropic glutamate receptor (iGluR) GLR-1 [4] . During memory consolidation, however, MAGI-1 controls GLR-1 clustering in AVA and AVD interneurons cell-autonomously and depends on the ability to interact with the β-catenin HMP-2. Significance Together, these results indicate that different aspects of associative learning and memory in C. elegans are likely carried out by distinct subsets of interneurons. The synaptic scaffolding protein MAGI-1 plays a critical role in these processes in part by regulating the clustering of iGluRs at synapses.

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