Publication

Structural and mechanistic determinants of a novel site for non-competitive inhibition of GluN2D-containing NMDA receptors

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Last modified
  • 02/20/2025
Type of Material
Authors
    Kasper B. Hansen, Emory UniversityStephen Traynelis, Emory University
Language
  • English
Date
  • 2011-03-09
Publisher
  • Society for Neuroscience
Publication Version
Copyright Statement
  • © 2011 The Authors
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 0270-6474
Volume
  • 31
Issue
  • 10
Start Page
  • 3650
End Page
  • 3661
Grant/Funding Information
  • National Institute of Neurological Disorders and Stroke : NINDS
  • This work was supported by NIH-NINDS (NS036654, NS065371, S.F.T.), the Villum Kann Rasmussen Foundation (K.B.H.), and the Lundbeck Foundation (K.B.H.).
Abstract
  • N-methyl-D-aspartate (NMDA) receptors are ionotropic glutamate receptors that mediate excitatory synaptic transmission and have been implicated in several neurological diseases. We have evaluated the mechanism of action of a class of novel subunit-selective NMDA receptor antagonists, typified by (E)-4-(6-methoxy-2-(3-nitrostyryl)-4-oxoquinazolin-3(4H)-yl)-benzoic acid (QNZ46). We found that QNZ46 inhibits NMDA receptor function in a non-competitive and voltage-independent manner by an unconventional mechanism that requires binding of glutamate to the GluN2 subunit, but not glycine binding to the GluN1 subunit. This dependency of antagonist association on glutamate binding to GluN2 renders these compounds nominally use-dependent, since inhibition will rely on synaptic release of glutamate. Evaluation of the structural determinants responsible for the subunit-selectivity of QNZ46 revealed that these compounds act at a new site that has not previously been described. Residues residing in the part of the agonist binding domain immediately adjacent to the transmembrane helices appear to control selectivity of QNZ46 for GluN2C- and GluN2D-containing receptors. These residues are well-positioned to sense glutamate binding to GluN2 and thus mediate glutamate-dependent actions. This new class of non-competitive antagonists could provide an opportunity for the development of pharmacological tools and therapeutic agents that target NMDA receptors at a new site and modulate function by a novel mechanism.
Author Notes
  • Corresponding author: Kasper B. Hansen, Department of Pharmacology, Emory University School of Medicine, 1510 Clifton Road, Rollins Research Center, Atlanta, Georgia 30322, USA Phone: +1 404-727-1375, Fax: +1 404-727-0365, kbhanse@emory.edu
Keywords
Research Categories
  • Biology, Neuroscience
  • Health Sciences, Pharmacology

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