Dynamic and specific interaction between synaptic NR2-NMDA receptor and PDZ proteins

Bard, Lucie; Sainlos, Matthieu; Bouchet, Delphine; Cousins, Sarah; Mikasova, Lenka; Breillat, Christelle; Stephenson, F. Anne; Imperiali, Barbara; Choquet, Daniel; Groc, Laurent

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Bard, Lucie; Sainlos, Matthieu; Bouchet, Delphine; Cousins, Sarah; Mikasova, Lenka; ... Show more

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Abstract

The relative content of NR2 subunits in the NMDA receptor confers specific signaling properties and plasticity to synapses. However, the mechanisms that dynamically govern the retention of synaptic NMDARs, in particular 2A-NMDARs, remain poorly understood. Here, we investigate the dynamic interaction between NR2 C termini and proteins containing PSD-95/Discs-large/ZO-1 homology (PDZ) scaffold proteins at the single molecule level by using high-resolution imaging. We report that a biomimetic divalent competing ligand, mimicking the last 15 amino acids of NR2A C terminus, specifically and efficiently disrupts the interaction between 2A-NMDARs, but not 2B-NMDARs, and PDZ proteins on the time scale of minutes. Furthermore, displacing 2A-NMDARs out of synapses lead to a compensatory increase in synaptic NR2B-NMDARs, providing functional evidence that the anchoring mechanism of 2A- or 2B-NMDARs is different. These data reveal an unexpected role of the NR2 subunit divalent arrangement in providing specific anchoring within synapses, highlighting the need to study such dynamic interactions in native conditions.

Date issued

2010-10

URI

http://hdl.handle.net/1721.1/84594

Department

Massachusetts Institute of Technology. Department of Biology; Massachusetts Institute of Technology. Department of Chemistry

Journal

Proceedings of the National Academy of Sciences

Publisher

National Academy of Sciences (U.S.)

Citation

Bard, L., M. Sainlos, D. Bouchet, S. Cousins, L. Mikasova, C. Breillat, F. A. Stephenson, B. Imperiali, D. Choquet, and L. Groc. “Dynamic and specific interaction between synaptic NR2-NMDA receptor and PDZ proteins.” Proceedings of the National Academy of Sciences 107, no. 45 (November 9, 2010): 19561-19566.

Version: Final published version

ISSN

0027-8424

1091-6490

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