Inhibition of NMDA receptors through a membrane-to-channel path

Wilcox, Madeleine R.; Nigam, Aparna; Glasgow, Nathan G.; Narangoda, Chamali; Phillips, Matthew B.; Patel, Dhilon S.; Mesbahi‐Vasey, Samaneh; Turcu, Andreea L.; Vázquez, Santiago; Kurnikova, Maria; Johnson, Jon W.

doi:10.1038/s41467-022-31817-z

Cited by 18 publications

(16 citation statements)

References 89 publications

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“…4G,H) and 100 µM memantine (Glasgow et al, 2018; Kolcheva et al, 2021). Recent data have shown that the GluN2A-M630 amino acid residue lines the fenestration of memantine via MCI (Wilcox et al, 2022). Therefore, we next assessed whether GluN1/GluN2A receptors with the mutated GluN2A-M630 residue exhibit altered MCI induced by K2060 (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…In addition, we observed a decrease in τ slow and A slow in the presence of Mg 2+ , which may also be attributable to the reduction of MCI induced by K2060 in the presence of Mg 2+ . In the case of memantine, MCI was explained by the presence of a fraction of the uncharged form that interacts with the membrane and then fenestrates into the ion channel of the GluN1/GluN2 receptor (Wilcox et al, 2022). The stronger MCI of K2060 may be explained by differential lipophilicity (memantine clogP = 2.07; MK-801 clogP = 3.31; K2060 clogP = 4.59; MarvinSketch software v. 23.8; estimated values), although both memantine and K2060 are likely to wash off the membrane in the order of seconds (Kotermanski and Johnson, 2009).…”

Section: Discussionmentioning

confidence: 99%

“…These different pharmacological effects in vivo likely result from their differences in the molecular mechanism of action at the NMDARs. Although both memantine and ketamine bind into ion channel pore relatively weakly (”low-affinity” open-channel blockers) (Song et al, 2018; Zhang et al, 2021), memantine—but not ketaminedisplays a second type of low-affinity inhibition (Blanpied et al, 1997; Sobolevsky et al, 1998; Kotermanski and Johnson, 2009; Glasgow et al, 2018), by accessing the binding site via a hydrophobic route from the plasma membrane to ion channel through a gated fenestration (named “membrane-to-channel inhibition” (MCI)) (Wilcox et al, 2022). On the contrary, the psychomimetic effect of MK-801 can be ascribed to its “high-affinity “and almost “irreversible” binding within the ion channel pore of GluN1/GluN2 receptors (Song et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

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Potent and reversible open-channel blocker of NMDA receptor derived from dizocilpine with enhanced membrane-to-channel inhibition

Misiachna,

Konecny,

Kolcheva

et al. 2024

Preprint

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N-methyl-D-aspartate receptors (NMDARs) play a significant role in developing several central nervous system (CNS) disorders. Currently, memantine, used for treating Alzheimer's disease, and ketamine, known for its anesthetic and antidepressant properties, are two clinically used NMDAR open-channel blockers. However, despite extensive research into NMDAR modulators, many have shown either harmful side effects or inadequate effectiveness. For instance, dizocilpine (MK-801) is recognized for its powerful psychomimetic effects due to its high-affinity and nearly irreversible inhibition of the GluN1/GluN2 NMDAR subtypes. Unlike ketamine, memantine and MK-801 also act through a unique, low-affinity "membrane-to-channel inhibition" (MCI). We aimed to develop an open-channel blocker based on MK-801 with distinct inhibitory characteristics from memantine and MK-801. Our novel compound, K2060, demonstrated effective voltage-dependent inhibition in the micromolar range at key NMDAR subtypes, GluN1/GluN2A and GluN1/GluN2B, even in the presence of Mg2+. K2060 showed reversible inhibitory dynamics and a partially trapping open-channel blocking mechanism with a significantly stronger MCI than memantine. Using hippocampal slices, 30 uM K2060 inhibited excitatory postsynaptic currents in CA1 hippocampal neurons by ~51%, outperforming 30 uM memantine (~21% inhibition). K2060 exhibited No Observed Adverse Effect Level (NOAEL) of 15 mg/kg upon intraperitoneal administration in mice. Administering K2060 at a 10 mg/kg dosage resulted in brain concentrations of approximately 2 uM, with peak concentrations (Tmax) achieved within 15 minutes. Finally, applying K2060 with trimedoxime and atropine in mice exposed to tabun improved treatment outcomes. These results underscore K2060's potential as a therapeutic agent for CNS disorders linked to NMDAR dysfunction.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Potent and reversible open-channel blocker of NMDA receptor derived from dizocilpine with enhanced membrane-to-channel inhibition

Misiachna,

Konecny,

Kolcheva

et al. 2024

Preprint

View full text Add to dashboard Cite

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“…The memantine/perampanel CLD-GA paradigm that is effective against CPZ-induced white matter injury was based on doses an order of magnitude below the clinical treatment range for these drugs and is an attractive alternative to full-dose co-administration such as that tested in stage II clinical trials for glioblastoma (eg., 34 ). Membrane-to-channel inhibition has recently been described for lipophilic antagonists of NMDA and AMPA receptors, which can diffuse from the cell membrane into the receptor protein via gated fenestration 35,36 . To take advantage of this phenomena and further extend the clinical potential of the CLD approach, we tested a combination of two experimental antagonists that are structural analogues of myelin-targeting fluorescent dyes.…”

Section: New Ex Vivo Models Of Acute Demyelinationmentioning

confidence: 99%

Sub-clinical glutamate receptor antagonist combinations prevent progressive demyelination

Mitchener,

Bulman,

Mellor

et al. 2024

Preprint

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Multiple sclerosis (MS) affects almost 3 million people globally who suffer demyelination as a series of relapses and remissions that tend towards progressive deterioration over time. The proximate cause is auto-immune attack by the adaptive immune system; therapies directed against this are effective during the relapsing-remitting phase but are less effective or ineffective during progression where other injury mechanisms may be significant. LPS- and cuprizone- induced experimental demyelination share features of progressive demyelination in MS but the underlying mechanisms are not well understood. We show here that these demyelination models can be reproduced ex vivo using short protocols, revealing that combined antagonism of two types of glutamate receptor, NMDA and AMPA, using clinically approved antagonists at sub-clinical doses, can protect against these forms of demyelination. Combined low dose therapy was subsequently shown to be effective in vivo against dietary cuprizone and experimental autoimmune-encephalomyelitis (EAE) models of demyelination and, in particular, protected the smaller myelinated axons that are the main substrate of the function loss in progressive MS.

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“…Fenestrations in the pore walls are observed in all available structures and density consistent with a lipid is present in both agonist-free and fructose-bound BmGr9 structures, suggesting that the lipids form part of a stable pore structure. Fenestrations opening the ion path to the membrane environment have been observed in several other ion channel families, including ionotropic glutamate receptors, cys-loop receptors, voltage-gated potassium channels and sodium channels, and mechanosensitive two-pore domain potassium (K2P) channels [35][36][37][38][39] . In some channels, such fenestrations are transient, while in others they are observed in both closed and open channel states.…”

Section: Pore-penetrating Lipids As a Common Feature Of Grs And Orsmentioning

confidence: 99%

Structure of an insect gustatory receptor

Frank,

Walujkar,

Walsh

et al. 2023

Preprint

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SUMMARYGustatory Receptors (GRs) are critical for insect chemosensation and are potential targets for controlling pests and disease vectors. However, GR structures have not been experimentally determined. We present structures ofBombyx moriGr9 (BmGr9), a fructose-gated cation channel, in agonist-free and fructose-bound states. BmGr9 forms a tetramer similar to distantly related insect Olfactory Receptors (ORs). Upon fructose binding, BmGr9’s ion channel gate opens through helix S7b movements. In contrast to ORs, BmGR9’s ligand-binding pocket, shaped by a kinked helix S4 and a shorter extracellular S3-S4 loop, is larger and solvent accessible in both agonist-free and fructose-bound states. Also unlike ORs, fructose binding by BmGr9 involves helix S5 and a binding pocket lined with aromatic and polar residues. Structure-based sequence alignments reveal distinct patterns of ligand-binding pocket residue conservation in GR subfamilies associated with distinct ligand classes. These data provide insight into the molecular basis of GR ligand specificity and function.

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Inhibition of NMDA receptors through a membrane-to-channel path

Cited by 18 publications

References 89 publications

Potent and reversible open-channel blocker of NMDA receptor derived from dizocilpine with enhanced membrane-to-channel inhibition

Potent and reversible open-channel blocker of NMDA receptor derived from dizocilpine with enhanced membrane-to-channel inhibition

Sub-clinical glutamate receptor antagonist combinations prevent progressive demyelination

Structure of an insect gustatory receptor

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