Trans-synaptic adhesion between NGL-3 and LAR regulates the formation of excitatory synapses

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Synaptic adhesion molecules regulate multiple steps of synapse formation and maturation. The great diversity of neuronal synapses predicts the presence of a large number of adhesion molecules that control synapse formation through trans-synaptic and heterophilic adhesion. We identified a previously unknown trans-synaptic interaction between netrin-G ligand-3 (NGL-3), a postsynaptic density (PSD) 95-interacting postsynaptic adhesion molecule, and leukocyte common antigen-related (LAR), a receptor protein tyrosine phosphatase. NGL-3 and LAR expressed in heterologous cells induced pre-and postsynaptic differentiation in contacting axons and dendrites of cocultured rat hippocampal neurons, respectively. Neuronal overexpression of NGL-3 increased presynaptic contacts on dendrites of transfected neurons. Direct aggregation of NGL-3 on dendrites induced coclustering of excitatory postsynaptic proteins. Knockdown of NGL-3 reduced the number and function of excitatory synapses. Competitive inhibition by soluble LAR reduced NGL-3-induced presynaptic differentiation. These results suggest that the trans-synaptic adhesion between NGL-3 and LAR regulates excitatory synapse formation in a bidirectional manner.
Publisher
NATURE PUBLISHING GROUP
Issue Date
2009-04
Language
English
Article Type
Article
Keywords

PROTEIN-TYROSINE-PHOSPHATASE; LIPRIN-ALPHA; NEURITE OUTGROWTH; NERVOUS-SYSTEM; BETA-NEUREXINS; RECEPTOR; LIGAND; MOLECULES; NETRIN; DIFFERENTIATION

Citation

NATURE NEUROSCIENCE, v.12, no.4, pp.428 - 437

ISSN
1097-6256
DOI
10.1038/nn.2279
URI
http://hdl.handle.net/10203/18588
Appears in Collection
BS-Journal Papers(저널논문)
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