GABAA receptor signalling mechanisms revealed by structural pharmacology

Masiulis, Simonas; Desai, Rushil; Uchański, Tomasz; Martin, I. Serna; Laverty, Duncan; Karia, Dimple; Malinauskas, Tomas; Zivanov, Jasenko; Pardon, Els; Kotecha, Abhay; Steyaert, Jan; Miller, Keith W.; Aricescu, A. Radu

doi:10.1038/s41586-018-0832-5

Cited by 444 publications

(593 citation statements)

References 69 publications

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“…Icilin/Ion channel TRPM8 (PDB:6NR3, EMD:0487) 41 ; LY2119620/M2R (PDB:6OIK, EMD:20079) 38 ; Iperoxo/M2R (PDB:6OIK, EMD:20079) 38 ; Saxitoxin/Nav1.7 (PDB: 6J8G, EMD:9781) 39 ; Biculine/GABAA (PDB:6HUK, EMD:0280) 37 ; Xanax/GABAA (PDB:6HUO, EMD:0282) 37 ; Valium, GABAA (PDB:6HUP, EMD:0283) 37 ; NDI-091143/ATP Citrate Lyase (PDB:6O0H, EMD:0567) 7 ; paroxetine/serotonin transporter (PDB:6DZW, EMD:8941) 40 ;…”

Section: Methodsmentioning

confidence: 99%

“…Using GlideEM we were able to identify candidate poses in this resolution range with cross correlations that were comparable to the deposited poses for all of the structures that we studied. For GABAA in complex with three different ligands 37 , the M2 muscarinic acetylcholine receptor in complex with two different ligands 38 , the sodium channel Nav1.7 with one ligand 39 , ATP citrate lyase with one ligand 7 , and the serotonin transporter with two different ligands 40 the poses we identified with GlideEM largely agreed with what was deposited in the PDB ( Supplementary Fig. 7) (although it should be noted that for the deposited structures of the M2 receptor and serotonin transporter the ligands were docked with the traditional version of Glide).…”

Section: Using Gemspot With 30-45 å Resolution Mapsmentioning

confidence: 99%

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GemSpot: A Pipeline for Robust Modeling of Ligands into CryoEM Maps

Robertson¹,

Zundert

Borrelli

et al. 2019

Preprint

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AbstractProducing an accurate atomic model of biomolecule-ligand interactions from maps generated by cryo-electron microscopy often presents challenges inherent to the methodology and the dynamic nature of ligand binding. Here we have developed GemSpot, a pipeline of computational chemistry methods that take into account EM map potentials, quantum mechanics energy calculations, and water molecule site prediction to generate candidate poses and provide a measure of the degree of confidence. The pipeline is validated through several published cryoEM structures of complexes in different resolution ranges and various types of ligands. In all cases, at least one identified pose produced both excellent interactions with the target and agreement with the map. GemSpot will be valuable for the robust identification of ligand poses and drug discovery efforts through cryoEM.

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Section: Methodsmentioning

confidence: 99%

Section: Using Gemspot With 30-45 å Resolution Mapsmentioning

confidence: 99%

GemSpot: A Pipeline for Robust Modeling of Ligands into CryoEM Maps

Robertson¹,

Zundert

Borrelli

et al. 2019

Preprint

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show abstract

“…We observed that the variant was in a highly conserved residue and the radius of the pore was narrowed at the gate in both closed and desensitized structures of the receptor. Having a residue like proline with a rigid side chain (or an alanine like in the β subunits with a non-rigid but very small side chain) at the intracellular -2' position allows tight control of the gating upon neurotransmitter extracellular binding, exerting rigid body motion of the TMH, as can be observed in recent GABAA and Gly receptors structures (26)(27)(28)51). Replacing the constraining proline with a leucine will permit changes in the backbone conformation (52).…”

Section: Discussionmentioning

confidence: 99%

“…It is near the Thr264, which interacts with the Thr292 (where the mutation Thr292Lys is) ( Figure 2B,D). Met263 is also part of the recently reported low affinity binding site for benzodiazepines, a group of sedative anticonvulsant drugs (28)(29)(30). In the desensitized GABAA α1β3γ2 receptor bound to Diazepam (DZP), Met263 is part of the opening of the pocket to the external molecular surface and its lateral chain sulfur establishes direct interaction with the diazepine ring of DZP (Supp.…”

Section: Structural Characterization Of the Novel And Previously Repomentioning

confidence: 99%

Structural analysis of pathogenic missense mutations in GABRA2 and identification of a novel de novo variant in the desensitization gate

Sanchis‐Juan

Hasenahuer

Baker

et al. 2019

Preprint

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AbstractCys-loop receptors are vital for controlling neuronal excitability in the brain and their dysfunction results in numerous neurological disorders. Recently, six de novo missense variants in GABRA2 gene, a member of this family, have been associated with early infantile epileptic encephalopathy (EIEE) and intellectual disability with seizures. Here, using whole-genome sequencing we identified a de novo missense variant in GABRA2 gene in a patient with EIEE and developmental delay. We perform protein structural analysis of the seven variants and show that all the mutations are in the transmembrane domain, either close to the desensitization gate, the activation gate or in inter-subunit interfaces. Further investigations demonstrated that the majority of pathogenic variants reported are at equivalent positions in other Cys-loop receptors, emphasizing the importance of these residues for the adequate function of the receptor. Also, a comparison of the distribution of the mutations in all the Cys-loop receptors showed that pathogenic variants are more common in the transmembrane helices, more specifically in the M2 helix, highlighting the importance of this segment. Our study expands the clinical spectrum of individuals with pathogenic missense mutations in GABRA2, defines the regions where pathogenic mutations are in the protein structure, and highlights the value of considering sequence, evolutionary, and structural information from other Cys-loop receptors as a strategy for variant interpretation of novel missense mutations in GABRA2.

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“…[8,9] Transport is regulated by controlling the opening and closing of channels (gating)i nr esponse to diverse stimuli, including changes in membrane potential, ligand binding or mechanical force. [10][11][12][13][14][15][16][17] Furthermore, the structural asymmetry observed in rectifying ion channels Ak ey conundrum in the constructiono fa na rtificial cell is to simultaneously maintain ar obust physical barriert ot he external environment, while also providing efficient exchange of informationa cross this barrier.B iomimicry provides an umber of avenues by which such requirementsm ight be met. Herein, we provide ab rief introductiont ot he challenges facing this field and explore progress to date.…”

Section: Ion Channelsmentioning

confidence: 99%

Artificial Signal Transduction across Membranes

2019

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A key conundrum in the construction of an artificial cell is to simultaneously maintain a robust physical barrier to the external environment, while also providing efficient exchange of information across this barrier. Biomimicry provides a number of avenues by which such requirements might be met. Herein, we provide a brief introduction to the challenges facing this field and explore progress to date.

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GABAA receptor signalling mechanisms revealed by structural pharmacology

Cited by 444 publications

References 69 publications

GemSpot: A Pipeline for Robust Modeling of Ligands into CryoEM Maps

GemSpot: A Pipeline for Robust Modeling of Ligands into CryoEM Maps

Structural analysis of pathogenic missense mutations in GABRA2 and identification of a novel de novo variant in the desensitization gate

Artificial Signal Transduction across Membranes

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