Crystal Structures of the Kainate Receptor GluR5 Ligand Binding Core Dimer with Novel GluR5-Selective Antagonists

doi:10.1523/JNEUROSCI.0123-06.2005

QUICK SEARCH:

[advanced]

	Author:		Keyword(s):
Year:		Vol:		Page:

HOME | SEARCH | ARCHIVE | SUBSCRIBE | CONTACT | HELP

The Journal of Neuroscience, March 15, 2006, 26(11):2852-2861; doi:10.1523/JNEUROSCI.0123-06.2005

This Article

Full Text

Full Text (PDF)

Supplemental data

Submit an eLetter

Alert me when this article is cited

Alert me when eLetters are posted

Alert me if a correction is posted

Citation Map

Services

Email this article to a friend

Similar articles in this journal

Similar articles in Web of Science

Similar articles in PubMed

Alert me to new issues of the journal

Download to citation manager

Citing Articles

Citing Articles via HighWire

Citing Articles via Web of Science (35)

Citing Articles via Google Scholar

Google Scholar

Articles by Mayer, M. L.

Articles by Jane, D. E.

Search for Related Content

PubMed

PubMed Citation

Articles by Mayer, M. L.

Articles by Jane, D. E.

Previous Article | Next Article
Cellular/Molecular
Crystal Structures of the Kainate Receptor GluR5 Ligand Binding Core Dimer with Novel GluR5-Selective Antagonists
Mark L. Mayer,¹ Alokesh Ghosal,¹ Nigel P. Dolman,² and David E. Jane²
¹Laboratory of Cellular and Molecular Neurophysiology, Porter Neuroscience Research Center, National Institute of Child Health and Human Development, National Institutes of Health, Department of Health and Human Services, Bethesda, Maryland 20892, and ²Department of Pharmacology, MRC Centre for Synaptic Plasticity, University of Bristol, Bristol BS8 1TD, United Kingdom
Correspondence should be addressed to Dr. Mark L. Mayer, National Institutes of Health, Building 35, Room 3B 1002, 35 Lincoln Drive, Bethesda, MD 20892-3712. Email: mayerm{at}mail.nih.gov
Glutamate receptor (GluR) ion channels mediate fast synaptictransmission in the mammalian CNS. Numerous crystallographicstudies, the majority on the GluR2-subtype AMPA receptor, haverevealed the structural basis for binding of subtype-specificagonists. In contrast, because there are far fewer antagonist-boundstructures, the mechanisms for antagonist binding are much lesswell understood, particularly for kainate receptors that existas multiple subtypes with a distinct biology encoded by theGluR5–7, KA1, and KA2 genes. We describe here high-resolutioncrystal structures for the GluR5 ligand-binding core complexwith UBP302 and UBP310, novel GluR5-selective antagonists. Thecrystal structures reveal the structural basis for the highselectivity for GluR5 observed in radiolabel displacement assaysfor the isolated ligand binding cores of the GluR2, GluR5, andGluR6 subunits and during inhibition of glutamate-activatedcurrents in studies on full-length ion channels. The antagonistsbind via a novel mechanism and do not form direct contacts withthe E723 side chain as occurs in all previously solved AMPAand kainate receptor agonist and antagonist complexes. Thisresults from a hyperextension of the ligand binding core comparedwith previously solved structures. As a result, in dimer assemblies,there is a 22 Å extension of the ion channel linkers inthe transition from antagonist- to glutamate-bound forms. Thislarge conformational change is substantially different fromthat described for AMPA receptors, was not possible to predictfrom previous work, and suggests that glutamate receptors arecapable of much larger movements than previously thought.

Key words: glutamate receptor; kainate; structure; gating; antagonist; crystallography

Received Jan. 11, 2006; revised Jan. 30, 2006; accepted Jan. 31, 2006.

Correspondence should be addressed to Dr. Mark L. Mayer, National Institutes of Health, Building 35, Room 3B 1002, 35 Lincoln Drive, Bethesda, MD 20892-3712. Email: mayerm{at}mail.nih.gov

This article has been cited by other articles:

A. J. R. Plested and M. L. Mayer
AMPA Receptor Ligand Binding Domain Mobility Revealed by Functional Cross Linking
J. Neurosci., September 23, 2009; 29(38): 11912 - 11923.
[Abstract] [Full Text] [PDF]

K. Frydenvang, L. L. Lash, P. Naur, P. A. Postila, D. S. Pickering, C. M. Smith, M. Gajhede, M. Sasaki, R. Sakai, O. T. Pentikainen, et al.
Full Domain Closure of the Ligand-binding Core of the Ionotropic Glutamate Receptor iGluR5 Induced by the High Affinity Agonist Dysiherbaine and the Functional Antagonist 8,9-Dideoxyneodysiherbaine
J. Biol. Chem., May 22, 2009; 284(21): 14219 - 14229.
[Abstract] [Full Text] [PDF]

M. Du, A. Rambhadran, and V. Jayaraman
Luminescence Resonance Energy Transfer Investigation of Conformational Changes in the Ligand Binding Domain of a Kainate Receptor
J. Biol. Chem., October 3, 2008; 283(40): 27074 - 27078.
[Abstract] [Full Text] [PDF]

M. F. Ireland, F. C. Lenal, A. R. Lorier, D. E. Loomes, T. Adachi, T. S. Alvares, J. J. Greer, and G. D. Funk
Distinct receptors underlie glutamatergic signalling in inspiratory rhythm-generating networks and motor output pathways in neonatal rat
J. Physiol., May 1, 2008; 586(9): 2357 - 2370.
[Abstract] [Full Text] [PDF]

H. Hald, P. Naur, D. S. Pickering, D. Sprogoe, U. Madsen, D. B. Timmermann, P. K. Ahring, T. Liljefors, A. Schousboe, J. Egebjerg, et al.
Partial Agonism and Antagonism of the Ionotropic Glutamate Receptor iGLuR5: STRUCTURES OF THE LIGAND-BINDING CORE IN COMPLEX WITH DOMOIC ACID AND 2-AMINO-3-[5-tert-BUTYL-3-(PHOSPHONOMETHOXY)-4-ISOXAZOLYL]PROPIONIC ACID
J. Biol. Chem., August 31, 2007; 282(35): 25726 - 25736.
[Abstract] [Full Text] [PDF]

P. Gorostiza, M. Volgraf, R. Numano, S. Szobota, D. Trauner, and E. Y. Isacoff
Mechanisms of photoswitch conjugation and light activation of an ionotropic glutamate receptor
PNAS, June 26, 2007; 104(26): 10865 - 10870.
[Abstract] [Full Text] [PDF]

M. C. Weston, C. Gertler, M. L. Mayer, and C. Rosenmund
Interdomain Interactions in AMPA and Kainate Receptors Regulate Affinity for Glutamate
J. Neurosci., July 19, 2006; 26(29): 7650 - 7658.
[Abstract] [Full Text] [PDF]