A Molecular Determinant of Subtype-Specific Desensitization in Ionotropic Glutamate Receptors

Alsaloum, Matthew; Kazi, Rashek; Gan, Quan; Amin, Johansen; Wollmuth, Lonnie P.

doi:10.1523/jneurosci.2667-15.2016

Cited by 46 publications

(66 citation statements)

References 28 publications

(13 reference statements)

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“…Mutations of Pro to Ala, Gly, Ile, Leu as well as Gln increased the degree of desensitization relative to WT GluN2A, achieving steady-state levels that were only 20%, 29%, 29%, 1.5%, and 18% of the peak response, respectively, compared to 56% for WT GluN1/GluN2A (Fig 6D) (Table 7). This is consistent with a recent report showing strong effects on receptor desensitization by residues in the pre-M1 region [29]. NMDARs containing GluN2A-P552L showed no change in surface expression (S1 Fig), but underwent profound desensitization, showing greater than 98% reduction in current at steady-state (Fig 6E) (Table 7).…”

Section: Resultssupporting

confidence: 92%

“…This region is conserved across all NMDAR GluN2 subunits [29] (Fig 2A) and is in van der Waals contact with the M3 helix (Fig 2B–2D). The proximity to the D2 domain that moves with agonist binding may allow the pre-M1 region to influence movement and position of the M3 helices that form the channel gate (Fig 2B–2D).…”

Section: Resultsmentioning

confidence: 99%

“…We further evaluated NMDAR functional changes caused by five GRIN missense mutations in the pre-M1 region of the receptor found in children with developmental delay, intellectual disability, and/or epilepsy (Table 2). Among these mutations, we focused on the mutant GluN2A-P552R, since this Pro residue is conserved across GluN subunits in multiple species (Fig 2; [29]). Our data show that GluN2A-P552R should be considered a gain-of-function variant because it shows increased glutamate / glycine potency and pronounced slowing of the glutamate current response time course, without concomitant changes in receptor surface expression or response amplitude.…”

Section: Discussionmentioning

confidence: 99%

“…Fourth, the pre-M1 helix and adjacent regions harbor structural determinants for subunit-selective positive allosteric modulators of the GluN2C- and GluN2D-containing NMDARs [56,57]. Fifth, mutations in and near pre-M1 can alter NMDAR function [14,29]. The position of the pre-M1 helix in the closed AMPAR and NMDAR structures [10,12,18] evokes the hypothesis that these helices, in van der Waals contact with the M3 gate, may serve to stabilize the gate in the closed conformation or otherwise impede M3 movement during channel opening.…”

Section: Discussionmentioning

confidence: 99%

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Molecular Mechanism of Disease-Associated Mutations in the Pre-M1 Helix of NMDA Receptors and Potential Rescue Pharmacology

et al. 2017

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N-methyl-D-aspartate receptors (NMDARs), ligand-gated ionotropic glutamate receptors, play key roles in normal brain development and various neurological disorders. Here we use standing variation data from the human population to assess which protein domains within NMDAR GluN1, GluN2A and GluN2B subunits show the strongest signal for being depleted of missense variants. We find that this includes the GluN2 pre-M1 helix and linker between the agonist-binding domain (ABD) and first transmembrane domain (M1). We then evaluate the functional changes of multiple missense mutations in the NMDAR pre-M1 helix found in children with epilepsy and developmental delay. We find mutant GluN1/GluN2A receptors exhibit prolonged glutamate response time course for channels containing 1 or 2 GluN2A-P552R subunits, and a slow rise time only for receptors with 2 mutant subunits, suggesting rearrangement of one GluN2A pre-M1 helix is sufficient for rapid activation. GluN2A-P552R and analogous mutations in other GluN subunits increased the agonist potency and slowed response time course, suggesting a functionally conserved role for this residue. Although there is no detectable change in surface expression or open probability for GluN2A-P552R, the prolonged response time course for receptors that contained GluN2A-P552R increased charge transfer for synaptic-like activation, which should promote excitotoxic damage. Transfection of cultured neurons with GluN2A-P552R prolonged EPSPs, and triggered pronounced dendritic swelling in addition to excitotoxicity, which were both attenuated by memantine. These data implicate the pre-M1 region in gating, provide insight into how different subunits contribute to gating, and suggest that mutations in the pre-M1 helix can compromise neuronal health. Evaluation of FDA-approved NMDAR inhibitors on the mutant NMDAR-mediated current response and neuronal damage provides a potential clinical path to treat individuals harboring similar mutations in NMDARs.

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Section: Resultssupporting

confidence: 92%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Molecular Mechanism of Disease-Associated Mutations in the Pre-M1 Helix of NMDA Receptors and Potential Rescue Pharmacology

et al. 2017

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“…Typical 10–90% rise times were 200-300 μs, as measured from junction potentials at the open tip of the patch pipette after recordings. Since we recorded GluA2-mediated currents in whole-cell mode, the time constants of deactivation and desensitization were somewhat larger than the corresponding values measured using outside-out recordings (Alsaloum et al, 2016; Carbone and Plested, 2012; Robert et al, 2005; Weston et al, 2006; Yelshansky et al, 2004). Nevertheless, despite the apparent overestimation of the absolute values of these parameters, we believe that the differences in kinetics of the corresponding constructs are faithfully reflected in the data.…”

Section: Star Methodsmentioning

confidence: 80%

Structural Bases of Desensitization in AMPA Receptor-Auxiliary Subunit Complexes

Twomey

Yelshanskaya

Grassucci

et al. 2017

Neuron

100

161

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SUMMARY Fast excitatory neurotransmission is mediated by AMPA-subtype ionotropic glutamate receptors (AMPARs). AMPARs, localized at post-synaptic densities, are regulated by transmembrane auxiliary subunits that modulate AMPAR assembly, trafficking, gating and pharmacology. Aberrancies in AMPAR-mediated signaling are associated with numerous neurological disorders. Here, we report cryo-EM structures of an AMPAR in complex with the auxiliary subunit GSG1L in the closed and desensitized states. GSG1L favors the AMPAR desensitized state, where channel closure is facilitated by profound structural rearrangements in the AMPAR extracellular domain, with ligand-binding domain dimers losing their local two-fold rotational symmetry. Our structural and functional experiments suggest that AMPAR auxiliary subunits share a modular architecture and use a common transmembrane scaffold for distinct extracellular modules to differentially regulate AMPAR gating. By comparing the AMPAR-GSG1L complex structures, we map conformational changes accompanying AMPAR recovery from desensitization and reveal structural bases for regulation of synaptic transmission by auxiliary subunits.

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NMDA Receptors in the Central Nervous System

Hansen

Perszyk

et al. 2017

Methods in Molecular Biology

126

102

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NMDA-type glutamate receptors are ligand-gated ion channels that mediate a major component of excitatory neurotransmission in the central nervous system (CNS). They are widely distributed at all stages of development and are critically involved in normal brain functions, including neuronal development and synaptic plasticity. NMDA receptors are also implicated in the pathophysiology of numerous neurological and psychiatric disorders, such as ischemic stroke, traumatic brain injury, Alzheimer's disease, epilepsy, mood disorders, and schizophrenia. For these reasons, NMDA receptors have been intensively studied in the past several decades to elucidate their physiological roles and to advance them as therapeutic targets. Seven NMDA receptor subunits exist that assemble into a diverse array of tetrameric receptor complexes, which are differently regulated, have distinct regional and developmental expression, and possess a wide range of functional and pharmacological properties. The diversity in subunit composition creates NMDA receptor subtypes with distinct physiological roles across neuronal cell types and brain regions, and enables precise tuning of synaptic transmission. Here, we will review the relationship between NMDA receptor structure and function, the diversity and significance of NMDA receptor subtypes in the CNS, as well as principles and rules by which NMDA receptors operate in the CNS under normal and pathological conditions.

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A Molecular Determinant of Subtype-Specific Desensitization in Ionotropic Glutamate Receptors

Cited by 46 publications

References 28 publications

Molecular Mechanism of Disease-Associated Mutations in the Pre-M1 Helix of NMDA Receptors and Potential Rescue Pharmacology

Molecular Mechanism of Disease-Associated Mutations in the Pre-M1 Helix of NMDA Receptors and Potential Rescue Pharmacology

Structural Bases of Desensitization in AMPA Receptor-Auxiliary Subunit Complexes

NMDA Receptors in the Central Nervous System

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