Use-Dependent Inhibition of the <i>N</i>-Methyl-D-aspartate Currents by Felbamate: a Gating Modifier with Selective Binding to the Desensitized Channels

Kuo, Chung‐Chin; Lin, Bei Jung; Chang, Huai Ren; Hsieh, Chi Pan

doi:10.1124/mol.65.2.370

Cited by 37 publications

(57 citation statements)

References 28 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Double-mutant cycle analysis of A652(NR1) and A651(NR2B) mutations consistent with the ideas that the foregoing residues are located in the external vestibule of the pore and are closely related to the activation gating control of the channel (see Introduction). In this regard, it is interesting to note that felbamate, the only approved anticonvulsant with significant gating-modification effects on NMDA receptors (Kuo et al, 2004), also binds to this region and acts as an "opportunistic" pore blocker with the "entrance" of its binding site undergoing a large gating conformational change Kuo, 2007a,b, 2008). Moreover, MT-SEA and MTSET modification of M3c (NR2B) is ϳ500-to 1000-fold faster in the activated than in the closed channels for the positions below A648 -A651 (Fig.…”

Section: Discussionmentioning

confidence: 99%

The Activation Gate and Gating Mechanism of the NMDA Receptor

Chang¹,

Kuo²

2008

J. Neurosci.

View full text Add to dashboard Cite

Section: Discussionmentioning

confidence: 99%

The Activation Gate and Gating Mechanism of the NMDA Receptor

Chang¹,

Kuo²

2008

J. Neurosci.

View full text Add to dashboard Cite

“…272,273 The drug acts as an allosteric modulator of channel gating, 274 with a preferential action to stabilize the inactivated state so as to produce a usedependent block. 275 This use-dependent action may selectively inhibit NMDA receptors that are excessively activated as is believed to occur during seizure discharges.…”

Section: Ionotropic Glutamate Receptorsmentioning

confidence: 99%

Molecular Targets for Antiepileptic Drug Development

2007

View full text Add to dashboard Cite

Summary:This review considers how recent advances in the physiology of ion channels and other potential molecular targets, in conjunction with new information on the genetics of idiopathic epilepsies, can be applied to the search for improved antiepileptic drugs (AEDs). Marketed AEDs predominantly target voltage-gated cation channels (the ␣ subunits of voltagegated Na ϩ channels and also T-type voltage-gated Ca 2ϩ channels) or influence GABA-mediated inhibition. Recently, ␣2-␦ voltage-gated Ca 2ϩ channel subunits and the SV2A synaptic vesicle protein have been recognized as likely targets. Genetic studies of familial idiopathic epilepsies have identified numerous genes associated with diverse epilepsy syndromes, including genes encoding Na ϩ channels and GABA A receptors, which are known AED targets. A strategy based on genes associated with epilepsy in animal models and humans suggests other potential AED targets, including various voltage-gated Ca 2ϩ channel subunits and auxiliary proteins, A-or M-type voltage-gated K ϩ channels, and ionotropic glutamate receptors. Recent progress in ion channel research brought about by molecular cloning of the channel subunit proteins and studies in epilepsy models suggest additional targets, including G-protein-coupled receptors, such as GABA B and metabotropic glutamate receptors; hyperpolarization-activated cyclic nucleotide-gated cation (HCN) channel subunits, responsible for hyperpolarization-activated current I h ; connexins, which make up gap junctions; and neurotransmitter transporters, particularly plasma membrane and vesicular transporters for GABA and glutamate. New information from the structural characterization of ion channels, along with better understanding of ion channel function, may allow for more selective targeting. For example, Na ϩ channels underlying persistent Na ϩ currents or GABA A receptor isoforms responsible for tonic (extrasynaptic) currents represent attractive targets. The growing understanding of the pathophysiology of epilepsy and the structural and functional characterization of the molecular targets provide many opportunities to create improved epilepsy therapies.

show abstract

“…However, this effect appears to be specific for GABA A receptors containing α1 or α2 subunits along with β2 or β3 subunits (Simeone and McClellan, 2000). In addition, felbamate at a concentration of 100 μM has been found to block NMDA receptor mediated synaptic responses (Pugliese et al, 1996) and to inhibit NMDA receptor currents in isolated neurons (K d , ~1 mM; Rho et al, 1994;Subramaniam et al, 1995;Kuo et al, 2004). Studies with recombinant NMDA receptor subunit combinations have indicated that felbamate selectively bocks NMDA receptors composed of NR2B subunits at lower concentrations (IC 50 , 0.5 mM), than other subunit combinations Harty and Rogawski, 2000).…”

Section: Carbamates: Flurofelbamate and Rwj-333369mentioning

confidence: 99%

Diverse mechanisms of antiepileptic drugs in the development pipeline

2006

View full text Add to dashboard Cite

There is a remarkable array of new chemical entities in the current antiepileptic drug (AED) development pipeline. In some cases, the compounds were synthesized in an attempt improve upon the activity of marketed AEDs. In other cases, the discovery of antiepileptic potential was largely serendipitous. Entry into the pipeline begins with the demonstration of activity in one or more animal screening models. Results from testing in a panel of such models provide a basis to differentiate agents and may offer clues as to the mechanism. Target activity may then be defined through cellbased studies, often years after the initial identification of activity. Some pipeline compounds are believed to act through conventional targets, whereas others are structurally novel and may act by novel mechanisms. Follow-on agents include the levetiracetam analogs brivaracetam and seletracetam that act as SV2A-ligands; the valproate-like agents valrocemide, valnoctamide, propylisopropyl acetamide, and isovaleramide; the felbamate analog flurofelbamate, a dicarbamate, and the unrelated carbamate RWJ-333369; the oxcarbazepine analog licarbazepine, which probably acts as a use-dependent sodium channel blockers, and its prodrug acetate BIA 2-093; and various selective partial benzodiazepine receptor agonists, including ELB139, which is a positive allosteric modulator of α3-containing GABA A receptors. A variety of AEDs that may act through novel targets are also in clinical development: lacosamide, a functionalized amino acid; talampanel, a 2,3-benzodiazepine selective noncompetitive AMPA receptor antagonist; NS1209, a competitive AMPA receptor antagonist; ganaxolone, a neuroactive steroid that acts as a positive modulator of GABA A receptors; retigabine, a KCNQ potassium channel opener with activity as a GABA A receptor positive modulator; the benzanilide KCNQ potassium channel opener ICA-27243 that is more selective than retigabine; and rufinamide, a triazole of unknown mechanism.

show abstract

Use-Dependent Inhibition of the N-Methyl-D-aspartate Currents by Felbamate: a Gating Modifier with Selective Binding to the Desensitized Channels

Cited by 37 publications

References 28 publications

The Activation Gate and Gating Mechanism of the NMDA Receptor

The Activation Gate and Gating Mechanism of the NMDA Receptor

Molecular Targets for Antiepileptic Drug Development

Diverse mechanisms of antiepileptic drugs in the development pipeline

Contact Info

Product

Resources

About