Mechanisms of activation and desensitization of full-length glycine receptor in lipid nanodiscs

Kumar, Arvind; Basak, Sandip; Rao, Shanlin; Gicheru, Yvonne; Mayer, Megan L.; Sansom, Mark S. P.; Chakrapani, Sudha

doi:10.1038/s41467-020-17364-5

Cited by 87 publications

(112 citation statements)

References 79 publications

(125 reference statements)

Supporting

Mentioning

100

Contrasting

Unclassified

Order By: Relevance

“…Conversely, a more compact transmembrane domain may also enhance coupling with the BZD site (Kim et al, 2020). Valine and threonine residues in GlyR and AchR aligning with V279 ( Figure 1-figure supplement 1) adopt a similar conformation (Kumar et al, 2020;Nemecz et al, 2016;Du et al, 2015), suggesting that this residue has a conserved role in other pLGICs.…”

Section: Discussionmentioning

confidence: 99%

“…For example, a compression of the ends of the M2–M3 linker would cause the middle of the linker to be squeezed outward toward the neighboring γ 2 subunit, potentially enhancing intersubunit coupling. Comparison of GlyR structures in apo or antagonist-bound versus agonist-bound conformations indicates that intersubunit interactions between the M2–M3 linker in the vicinity of the valine aligning with V279 and the following serine, and the top of the M1 helix in the adjacent subunit are weakened during channel activation ( Du et al, 2015 ; Kumar et al, 2020 ). Thus, a stronger intersubunit coupling in this area could potentially both reduce unliganded opening and enhance coupling with rearrangements of the γ 2 subunit upon BZD binding.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

A critical residue in the α1M2–M3 linker regulating mammalian GABAA receptor pore gating by diazepam

Nors

Gupta

Goldschen-Ohm

2021

eLife

View full text Add to dashboard Cite

Benzodiazepines (BZDs) are a class of widely prescribed psychotropic drugs that modulate activity of GABAA receptors (GABAARs), neurotransmitter-gated ion channels critical for synaptic transmission. However, the physical basis of this modulation is poorly understood. We explore the role of an important gating domain, the a1M2-M3 linker, in linkage between the BZD site and pore gate. To probe energetics of this coupling without complication from bound agonist we use a gain of function mutant (a1L9'Tb2g2L) directly activated by BZDs. We identify a specific residue whose mutation (a1V279A) more than doubles the energetic contribution of the BZD positive modulator diazepam (DZ) to pore opening and also enhances DZ-potentiation of GABA-evoked currents in a wild-type background. In contrast, other linker mutations have little effect on DZ efficiency, but generally impair unliganded pore opening. Our observations reveal an important residue regulating BZD-pore linkage, thereby shedding new light on the molecular mechanism of these drugs.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

A critical residue in the α1M2–M3 linker regulating mammalian GABAA receptor pore gating by diazepam

Nors

Gupta

Goldschen-Ohm

2021

eLife

View full text Add to dashboard Cite

show abstract

“…Structural and single channel functional studies on members of the muscle AChR have provided a picture of channel gating in which local agonist-induced structural changes propagate away from the binding site and produce motions in many parts of the protein ( Mukhtasimova et al, 2005 ; Mukhtasimova and Sine, 2007 ; Mukhtasimova et al, 2009 ; Mukhtasimova and Sine, 2018 ; Purohit and Auerbach, 2007a ; Purohit and Auerbach, 2007b ; Jha et al, 2007 ; Cadugan and Auerbach, 2010 ), ultimately resulting in dilation of the channel pore and permeation of hydrated ions. Recent cryo-electron microscopy studies have further clarified this picture by providing snapshots of the ‘closed’ and ‘open’ states of pLGICs, assigned based upon the size of the pore relative to the hydrated ions and molecular dynamics simulations of ion conduction ( Basak et al, 2018 ; Polovinkin et al, 2018 ; Kumar et al, 2020 ). Comparing the structures of these closed and open states, one sees that whereas the closed structures show narrow constrictions of the pore at the 9’ and −1’ positions, the open structures show expansion at these positions.…”

Section: Discussionmentioning

confidence: 99%

Unmasking coupling between channel gating and ion permeation in the muscle nicotinic receptor

Strikwerda

Sine

2021

eLife

View full text Add to dashboard Cite

Whether ion channel gating is independent of ion permeation has been an enduring, unresolved question. Here, applying single channel recording to the archetypal muscle nicotinic receptor, we unmask coupling between channel gating and ion permeation by structural perturbation of a conserved intramembrane salt bridge. A charge-neutralizing mutation suppresses channel gating, reduces unitary current amplitude, and increases fluctuations of the open channel current. Power spectra of the current fluctuations exhibit low- and high-frequency Lorentzian components, which increase in charge-neutralized mutant receptors. After aligning channel openings and closings at the time of transition, the average unitary current exhibits asymmetric relaxations just after channel opening and before channel closing. A theory in which structural motions contribute jointly to channel gating and ion conduction describes both the power spectrum and the current relaxations. Coupling manifests as a transient increase in the open channel current upon channel opening and a decrease upon channel closing.

show abstract

“…Here we will focus on the use of three different levels of computational study to explore the nature of the hydrophobic gate in these bilayer-embedded GlyR structures. 85 In particular, we will compare the closed (apo) state of the GlyR (PDB id 6UBS) with an open state of the channel (PDB id 6UD3) obtained by studying the GlyR in a complex with both the agonist (i.e., activator) glycine plus an open channel blocker, picrotoxin (PTX).…”

Section: Annotating New Structures: Three Recent Case Studiesmentioning

confidence: 99%

Section: Annotating New Structures: Three Recent Case Studiesmentioning

confidence: 99%

Molecular Simulations of Hydrophobic Gating of Pentameric Ligand Gated Ion Channels: Insights into Water and Ions

et al. 2021

Self Cite

View full text Add to dashboard Cite

Ion channels are proteins which form gated nanopores in biological membranes. Many channels exhibit hydrophobic gating, whereby functional closure of a pore occurs by local dewetting. The pentameric ligand gated ion channels (pLGICs) provide a biologically important example of hydrophobic gating. Molecular simulation studies comparing additive vs polarizable models indicate predictions of hydrophobic gating are robust to the model employed. However, polarizable models suggest favorable interactions of hydrophobic pore-lining regions with chloride ions, of relevance to both synthetic carriers and channel proteins. Electrowetting of a closed pLGIC hydrophobic gate requires too high a voltage to occur physiologically but may inform designs for switchable nanopores. Global analysis of ∼200 channels yields a simple heuristic for structure-based prediction of (closed) hydrophobic gates. Simulation-based analysis is shown to provide an aid to interpretation of functional states of new channel structures. These studies indicate the importance of understanding the behavior of water and ions within the nanoconfined environment presented by ion channels.

show abstract

Mechanisms of activation and desensitization of full-length glycine receptor in lipid nanodiscs

Cited by 87 publications

References 79 publications

A critical residue in the α1M2–M3 linker regulating mammalian GABAA receptor pore gating by diazepam

A critical residue in the α1M2–M3 linker regulating mammalian GABAA receptor pore gating by diazepam

Unmasking coupling between channel gating and ion permeation in the muscle nicotinic receptor

Molecular Simulations of Hydrophobic Gating of Pentameric Ligand Gated Ion Channels: Insights into Water and Ions

Contact Info

Product

Resources

About