Pharmacology and Structural Analysis of Ligand Binding to the Orthosteric Site of Glutamate-Like GluD2 Receptors

The GluD2 receptor is a fundamental component of postsynaptic sites in Purkinje neurons, and is required for normal cerebellar function. GluD2 and the closely related GluD1 are classified as members of the ionotropic glutamate receptor (iGluR) superfamily on the basis of sequence similarity, but do...

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Veröffentlicht in:	Molecular pharmacology 2016-02, Vol.89 (2), p.253-262
Hauptverfasser:	Kristensen, Anders S., Hansen, Kasper B., Naur, Peter, Olsen, Lars, Kurtkaya, Natalie L., Dravid, Shashank M., Kvist, Trine, Yi, Feng, Pøhlsgaard, Jacob, Clausen, Rasmus P., Gajhede, Michael, Kastrup, Jette S., Traynelis, Stephen F.
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Sprache:	eng
Schlagworte:	Animals Binding Sites - physiology Crystallography, X-Ray Dose-Response Relationship, Drug Female Ligands Protein Binding - physiology Protein Structure, Secondary Protein Structure, Tertiary Rats Receptors, Glutamate - chemistry Receptors, Glutamate - metabolism Serine - chemistry Serine - metabolism Serine - pharmacology Stereoisomerism Structure-Activity Relationship Xenopus laevis
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container_title	Molecular pharmacology
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creator	Kristensen, Anders S. Hansen, Kasper B. Naur, Peter Olsen, Lars Kurtkaya, Natalie L. Dravid, Shashank M. Kvist, Trine Yi, Feng Pøhlsgaard, Jacob Clausen, Rasmus P. Gajhede, Michael Kastrup, Jette S. Traynelis, Stephen F.
description	The GluD2 receptor is a fundamental component of postsynaptic sites in Purkinje neurons, and is required for normal cerebellar function. GluD2 and the closely related GluD1 are classified as members of the ionotropic glutamate receptor (iGluR) superfamily on the basis of sequence similarity, but do not bind l-glutamate. The amino acid neurotransmitter D-Ser is a GluD2 receptor ligand, and endogenous D-Ser signaling through GluD2 has recently been shown to regulate endocytosis of α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid–type iGluRs during synaptic plasticity in the cerebellum, such as long-term depression. Here, we investigate the pharmacology of the orthosteric binding site in GluD2 by examining the activity of analogs of D-Ser and GluN1 glycine site competitive antagonists at GluD2 receptors containing the lurcher mutation (GluD2LC), which promotes spontaneous channel activation. We identify several compounds that modulate GluD2LC, including a halogenated alanine analog as well as the kynurenic acid analog 7-chloro-4-oxo-1H-quinoline-2-carboxylic acid (7-chlorokynurenic acid; 7-CKA). By correlating thermodynamic and structural data for 7-CKA binding to the isolated GluD2 ligand binding domain (GluD2-LBD), we find that binding 7-CKA to GluD2-LBD differs from D-Ser by inducing an intermediate cleft closure of the clamshell-shaped LBD. The GluD2 ligands identified here can potentially serve as a starting point for development of GluD2-selective ligands useful as tools in studies of the signaling role of the GluD2 receptor in the brain.
doi_str_mv	10.1124/mol.115.100909
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GluD2 and the closely related GluD1 are classified as members of the ionotropic glutamate receptor (iGluR) superfamily on the basis of sequence similarity, but do not bind l-glutamate. The amino acid neurotransmitter D-Ser is a GluD2 receptor ligand, and endogenous D-Ser signaling through GluD2 has recently been shown to regulate endocytosis of α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid–type iGluRs during synaptic plasticity in the cerebellum, such as long-term depression. Here, we investigate the pharmacology of the orthosteric binding site in GluD2 by examining the activity of analogs of D-Ser and GluN1 glycine site competitive antagonists at GluD2 receptors containing the lurcher mutation (GluD2LC), which promotes spontaneous channel activation. We identify several compounds that modulate GluD2LC, including a halogenated alanine analog as well as the kynurenic acid analog 7-chloro-4-oxo-1H-quinoline-2-carboxylic acid (7-chlorokynurenic acid; 7-CKA). By correlating thermodynamic and structural data for 7-CKA binding to the isolated GluD2 ligand binding domain (GluD2-LBD), we find that binding 7-CKA to GluD2-LBD differs from D-Ser by inducing an intermediate cleft closure of the clamshell-shaped LBD. 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By correlating thermodynamic and structural data for 7-CKA binding to the isolated GluD2 ligand binding domain (GluD2-LBD), we find that binding 7-CKA to GluD2-LBD differs from D-Ser by inducing an intermediate cleft closure of the clamshell-shaped LBD. The GluD2 ligands identified here can potentially serve as a starting point for development of GluD2-selective ligands useful as tools in studies of the signaling role of the GluD2 receptor in the brain.</description><subject>Animals</subject><subject>Binding Sites - physiology</subject><subject>Crystallography, X-Ray</subject><subject>Dose-Response Relationship, Drug</subject><subject>Female</subject><subject>Ligands</subject><subject>Protein Binding - physiology</subject><subject>Protein Structure, Secondary</subject><subject>Protein Structure, Tertiary</subject><subject>Rats</subject><subject>Receptors, Glutamate - chemistry</subject><subject>Receptors, Glutamate - metabolism</subject><subject>Serine - chemistry</subject><subject>Serine - metabolism</subject><subject>Serine - pharmacology</subject><subject>Stereoisomerism</subject><subject>Structure-Activity Relationship</subject><subject>Xenopus laevis</subject><issn>0026-895X</issn><issn>1521-0111</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2016</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNp1kcFP2zAUxi20aZRu1x0nH3dJ8UtsJ7kgQWGAVAlEN2k3y3VeWm9JXGwHqf_9XBUQHHaxn_X9_Pk9f4R8BTYDyPlp77pUiBkwVrP6iExA5JAxAPhAJozlMqtq8fuYnITwhzHgomKfyHEupQTGiwnZ3m-077VxnVvvqB4auox-NHH0uqPng-52wQbqWrqw6716YYfGDmsaHY0bpHc-blyI6K2hSxtxT153Y9S9jpgt7F_cHy9z-oAGt9H58Jl8bHUX8MvzPiW_flz9nN9ki7vr2_n5IjOCiZjWymDeFADlStYFVFgYqAEFb1tZS6zakhVoZMtRmAYklGKVhMJwKXXe8mJKzg6-23HVY2NwiGkktfW2136nnLbqvTLYjVq7J8VLLnklksH3ZwPvHkcMUfU2GOw6PaAbg4JSsoRVvE7o7IAa70Lw2L4-A0ztY1IpplQIdYgpXfj2trlX_CWXBFQHANMXPVn0KhiLg8HGejRRNc7-z_sftJ2i8g</recordid><startdate>20160201</startdate><enddate>20160201</enddate><creator>Kristensen, Anders S.</creator><creator>Hansen, Kasper B.</creator><creator>Naur, Peter</creator><creator>Olsen, Lars</creator><creator>Kurtkaya, Natalie L.</creator><creator>Dravid, Shashank M.</creator><creator>Kvist, Trine</creator><creator>Yi, Feng</creator><creator>Pøhlsgaard, Jacob</creator><creator>Clausen, Rasmus P.</creator><creator>Gajhede, Michael</creator><creator>Kastrup, Jette S.</creator><creator>Traynelis, Stephen F.</creator><general>Elsevier Inc</general><general>The American Society for Pharmacology and Experimental Therapeutics</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><scope>5PM</scope></search><sort><creationdate>20160201</creationdate><title>Pharmacology and Structural Analysis of Ligand Binding to the Orthosteric Site of Glutamate-Like GluD2 Receptors</title><author>Kristensen, Anders S. ; 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By correlating thermodynamic and structural data for 7-CKA binding to the isolated GluD2 ligand binding domain (GluD2-LBD), we find that binding 7-CKA to GluD2-LBD differs from D-Ser by inducing an intermediate cleft closure of the clamshell-shaped LBD. The GluD2 ligands identified here can potentially serve as a starting point for development of GluD2-selective ligands useful as tools in studies of the signaling role of the GluD2 receptor in the brain.</abstract><cop>United States</cop><pub>Elsevier Inc</pub><pmid>26661043</pmid><doi>10.1124/mol.115.100909</doi><tpages>10</tpages><oa>free_for_read</oa></addata></record>
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source	MEDLINE; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; Alma/SFX Local Collection; Free Full-Text Journals in Chemistry
subjects	Animals Binding Sites - physiology Crystallography, X-Ray Dose-Response Relationship, Drug Female Ligands Protein Binding - physiology Protein Structure, Secondary Protein Structure, Tertiary Rats Receptors, Glutamate - chemistry Receptors, Glutamate - metabolism Serine - chemistry Serine - metabolism Serine - pharmacology Stereoisomerism Structure-Activity Relationship Xenopus laevis
title	Pharmacology and Structural Analysis of Ligand Binding to the Orthosteric Site of Glutamate-Like GluD2 Receptors
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