Structure−Activity Studies of 6-Substituted Decahydroisoquinoline-3-carboxylic Acid AMPA Receptor Antagonists. 2. Effects of Distal Acid Bioisosteric Substitution, Absolute Stereochemical Preferences, and in Vivo Activity

Ornstein, Paul L.; Mb, Arnold; Nk, Allen; Bleisch, Thomas J.; Ps, Borromeo; rd, Lugar Cw; Jd, Leander; Lodge, David; Dd, Schoepp

doi:10.1021/jm950913h

Cited by 32 publications

(15 citation statements)

References 18 publications

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“…Crystal structures have not yet been reported for ligands from the extensive series of decahydroisoquinolines which have been developed as glutamate receptor antagonists (Clarke et al, 1997; Ornstein et al, 1996; Ornstein et al, 1992; Weiss et al, 2006). Of this series we chose to study LY466195, one of the most potent GluK1 antagonists reported to date.…”

Section: Resultsmentioning

confidence: 99%

Binding site and ligand flexibility revealed by high resolution crystal structures of GluK1 competitive antagonists

2011

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The availability of crystal structures for the ligand binding domains of ionotropic glutamate receptors, combined with their key role in synaptic function in the normal and diseased brain, offers a unique selection of targets for pharmaceutical research compared to other drug targets for which the atomic structure of the ligand binding sites is not known. Currently only a few antagonist structures have been solved, and these reveal ligand specific conformational changes that hinder rational drug design. Here we report high resolution crystal structures for three kainate receptor GluK1 antagonist complexes which reveal new and unexpected modes of binding, highlighting the continued need for experimentally determined receptor-ligand complexes.

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Section: Resultsmentioning

confidence: 99%

Binding site and ligand flexibility revealed by high resolution crystal structures of GluK1 competitive antagonists

2011

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“…administration of ATPA, the tert -butyl analogue of AMPA. In previous studies, ATPA was identified as an AMPA agonist (Ornstein et al, 1996), but was later discovered to be a selective agonist of the GluK1 (formerly GluR5) kainate receptor (Hoo et al, 1999; Jane et al, 2009). In the present study, ATPA (30 mg/kg, i.p.)…”

Section: Resultsmentioning

confidence: 99%

Effects of the selective kainate receptor antagonist ACET on altered sensorimotor gating in a genetic model of reduced NMDA receptor function

Duncan¹,

Koller²,

Moy³

2012

Brain Research

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The pathophysiology of schizophrenia may involve reduced NMDA receptor function. Accordingly, experimental models of NMDA receptor hypofunction may be useful for testing potential new antipsychotic agents and for characterizing neurobiological abnormalities relevant to schizophrenia. We demonstrated previously that mice under-expressing the NR1 subunit of the NMDA receptor show supersensitive behavioral responses to kainic acid and that a kainate receptor antagonist normalized altered behaviors in the mutant mice (NR1neo/neo). The present work examined effects of another selective kainate receptor antagonist, (S)-1-(2-Amino-2-carboxyethyl)-3-(2-carboxy-5-phenylthiophene-3-yl-methylpyrimidine-2,4-dione (ACET), on altered behavioral phenotypes in the genetic model of NMDA receptor hypofunction. ACET, at a dose of 15 mg/kg, partially reversed the deficits in prepulse inhibition produced by the mutation. The 15 mg/kg dose of ACET was also effective in reversing behavioral effects of the selective kainate agonist ATPA. However, ACET did not significantly reduce the increased locomotor activity and rearing behavior observed in the NR1neo/neo mice. These findings show that a highly selective kainate receptor antagonist can affect the deficits in sensorimotor gating in the NR1neo/neo mice. The results also provide further support for the idea that selective kainate receptor antagonists could be novel therapeutic candidates for schizophrenia. Section: Disease-Related Neuroscience

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“…Replacement of the tetrazole with a sulphonyltriazole moiety resulted in an enhancement of potency and selectivity for AMPA receptors (ICso = 0.16 ± 0.79,umol/1 for antagonism of AMPA-mediated depolarizations in the cortical wedge assay) (ORNSTEIN et al 1996b). The activity was found to reside in the (-)- (3 S,4aR,6 S,8aR)-isomer (ICso 0.6,umolll for displacement of [3H]AMPA binding).…”

Section: Decahydroisoquinoiinesmentioning

confidence: 99%

“…Thus it would appear that the decahydroisoquinoline ring imposes a unique conformation on the molecule. It was observed that for both C-6 epimers it is the compound with the S absolute stereochemistry at C-3 which has the AMPA receptor antagonist activity (ORNSTEIN et al 1996b). This contrasts with observation that for the decahydroisoquinoline series of NMDA receptor antagonists the activity was found to reside in the isomer with R absolute stereochemistry at C-3.…”

Section: Decahydroisoquinoiinesmentioning

confidence: 99%

Glutamate Receptor Ion Channels: Activators and Inhibitors

Jane¹,

Tse²,

Skifter³

et al. 2000

Pharmacology of Ionic Channel Function: Activators and Inhibitors

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The classification of excitatory amino acid (EAA) receptors into N-methyl-oaspartic acid (NMDA) and non-NMDA receptors was based mainly on the discovery of selective agonists and antagonists (for a review see WATKINS and EVANS 1981). Thus the selective NMDA receptor antagonist, o-aaminoadipate blocked responses due to NMDA but not those due to quisqualate or kainate in the frog and rat spinal cord. Evidence for more than one type of non-NMDA receptor came from the observation that responses due to quisqualate but not those due to kainate are depressed by L-glutamic acid diethyl ester (GDEE) (McLENNAN and LOOGE 1979; while responses to kainate can be selectively antagonized by y"oglutamylglycine (rDGG) . In addition, receptors present on dorsal root fibers were shown to be sensitive to kainate but not quisqualate ). These observations resulted in the classification of EAA receptors into NMDA, quisqualate and kainate receptors. Such receptors are linked to ionic fluxes and are now known as ionotropic glutamate receptors (iGluRs) as distinct from the more recently discovered metabotropic glutamate receptors (mGluRs) linked to G-protein coupled metabolic changes (CONN and PIN 1997). The isoxazole analogue, (S)-2-amino-3-(3-hydroxy-5-methyl-4-isoxazolyl)propionic acid (AMPA) was reported to be more selective for the quisqualate type of iGluR than quisqualate itself (KROGSGAARO-LARSEN et al. 1980 and this led to this ionotropic receptor being renamed the AMPA receptor to avoid confusion with quisqualate-activated mGluRs (MONAGHAN et al. 1989;). Molecular biology has identified a large number of subtypes of both iGluRs and mGluRs.Progress in defining the role of EAA receptors in CNS function has also followed the development of receptor-selective antagonists. With the availability of NMDA receptor antagonists, it was possible to demonstrate a role of NMDA receptors in polysynaptic responses in the vertebrate spinal cord EVANS et al. 1979) and in hippocampal long term potentiation (COLLINGRIDGE et al. 1983;HARRIS et al. 1984

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Structure−Activity Studies of 6-Substituted Decahydroisoquinoline-3-carboxylic Acid AMPA Receptor Antagonists. 2. Effects of Distal Acid Bioisosteric Substitution, Absolute Stereochemical Preferences, and in Vivo Activity

Cited by 32 publications

References 18 publications

Binding site and ligand flexibility revealed by high resolution crystal structures of GluK1 competitive antagonists

Binding site and ligand flexibility revealed by high resolution crystal structures of GluK1 competitive antagonists

Effects of the selective kainate receptor antagonist ACET on altered sensorimotor gating in a genetic model of reduced NMDA receptor function

Glutamate Receptor Ion Channels: Activators and Inhibitors

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