LRRTM2 Functions as a Neurexin Ligand in Promoting Excitatory Synapse Formation

  • Jaewon Ko
  • , Marc V. Fuccillo
  • , Robert C. Malenka
  • , Thomas C. Südhof

Research output: Contribution to journalArticlepeer-review

318 Scopus citations

Abstract

Recently, leucine-rich repeat transmembrane proteins (LRRTMs) were found to be synaptic cell-adhesion molecules that, when expressed in nonneuronal cells, induce presynaptic differentiation in contacting axons. We now demonstrate that LRRTM2 induces only excitatory synapses, and that it also acts to induce synapses in transfected neurons similarly to neuroligin-1. Using affinity chromatography, we identified α- and β-neurexins as LRRTM2 ligands, again rendering LRRTM2 similar to neuroligin-1. However, whereas neuroligins bind neurexins containing or lacking an insert in splice site #4, LRRTM2 only binds neurexins lacking an insert in splice site #4. Binding of neurexins to LRRTM2 can produce cell-adhesion junctions, consistent with a trans-interaction regulated by neurexin alternative splicing, and recombinant neurexin-1β blocks LRRTM2's ability to promote presynaptic differentiation. Thus, our data suggest that two unrelated postsynaptic cell-adhesion molecules, LRRTMs and neuroligins, unexpectedly bind to neurexins as the same presynaptic receptor, but that their binding is subject to distinct regulatory mechanisms.

Original languageEnglish
Pages (from-to)791-798
Number of pages8
JournalNeuron
Volume64
Issue number6
DOIs
StatePublished - 24 Dec 2009

Bibliographical note

Funding Information:
We thank Eunjoon Kim for the gifts of pan-NGL antibody and expression construct (NGL3-EGFP). This work was supported by grants from the NIMH and Simons Foundation (to T.C.S.), and by fellowships from the Human Frontier Science Program (to J.K.) and the NIH (to M.V.F.).

Keywords

  • CELLBIO
  • MOLNERO
  • SIGNALING

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