Quasi-elastic Neutron Scattering Reveals Ligand-Induced Protein Dynamics of a G-Protein-Coupled Receptor

Shrestha, Utsab R.; Perera, Suchithranga M.D.C.; Bhowmik, Debsindhu; Chawla, Udeep; Mamontov, Eugene; Brown, Michael F.; Chu, Xiang-Qiang

doi:10.1021/acs.jpclett.6b01632

“…26 Here, we show the use of the powdered GPCR preparation method to investigate rhodopsin versus the ligand-free opsin apoprotein. Rhodopsin is a class A GPCR responsible for vision under dim light conditions in vertebrates.…”

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confidence: 99%

“…Current findings suggest the intrinsic dynamics of the protein are unlocked by the light-induced isomerization of the 11- cis retinal cofactor needed for interaction of the GPCR with its cognate G-protein (transducin). 26 …”

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confidence: 99%

“…44 Quasielastic neutron scattering methods enable one to probe molecular motions from picoseconds up to nanoseconds within the atomic to molecular length scales. 26 Upon hydrating the protein sample with D 2 O, the results of a QENS experiment are expressed as the dynamic structure factor, which is dominated by the contributions from non-exchangeable hydrogen atoms in the protein. The QENS data can be analyzed both in the energy domain by a model-free analysis, and in the time domain by introduction of motional models.…”

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confidence: 99%

“…26 For D 2 O-hydrated powders of rhodopsin/CHAPS detergent, the majority of the recorded signal is due to the protein dynamics, and the correction for the presence of the detergent is minimal during the subsequent data reduction and analysis. The QENS experiments were focused on studying how the dynamics of the protein were affected upon rhodopsin photoactivation.…”

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confidence: 99%

“…The QENS experiments were focused on studying how the dynamics of the protein were affected upon rhodopsin photoactivation. Protein dynamics of the dark-state rhodopsin were compared to those of ligand-free opsin, 26 which is structurally similar to active metarhodopin-II. 38 Previous neutron scattering studies conducted to unravel the local dynamics of bacteriorhodopsin and visual rhodopsin in the dark and light-activated states have revealed few significant differences.…”

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confidence: 99%

See 3 more Smart Citations

Powdered G-Protein-Coupled Receptors

Perera

¹

,

Chawla

²

,

Brown

³

2016

J. Phys. Chem. Lett.

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Preparation and storage of functional membrane proteins such as G-protein-coupled receptors (GPCRs) are crucial to the processes of drug delivery and discovery. Here we describe a method of preparing powdered GPCRs using rhodopsin as the prototype. We purified rhodopsin in CHAPS detergent with low detergent to protein ratio so the bulk of the sample represented protein (ca. 72% w/w). Our new method for generating powders of membrane proteins followed by rehydration paves the way for conducting functional and biophysical experiments. As an illustrative application powdered rhodopsin was prepared with and without the cofactor 11-cis retinal to enable partial rehydration of the protein with D2O in a controlled manner. Quasielastic neutron scattering studies using both spatial motion and energy landscape models form the basis for crucial insights into structural fluctuations and thermodynamics of GPCR activation.

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Activation of the G‐Protein‐Coupled Receptor Rhodopsin by Water

Chawla

¹

,

Perera

²

,

Fried

³

et al. 2020

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Visual rhodopsin is an important archetype for G‐protein‐coupled receptors, which are membrane proteins implicated in cellular signal transduction. Herein, we show experimentally that approximately 80 water molecules flood rhodopsin upon light absorption to form a solvent‐swollen active state. An influx of mobile water is necessary for activating the photoreceptor, and this finding is supported by molecular dynamics (MD) simulations. Combined force‐based measurements involving osmotic and hydrostatic pressure indicate the expansion occurs by changes in cavity volumes, together with greater hydration in the active metarhodopsin‐II state. Moreover, we discovered that binding and release of the C‐terminal helix of transducin is coupled to hydration changes as may occur in visual signal amplification. Hydration–dehydration explains signaling by a dynamic allosteric mechanism, in which the soft membrane matter (lipids and water) has a pivotal role in the catalytic G‐protein cycle.

show abstract

Activation of the G‐Protein‐Coupled Receptor Rhodopsin by Water

Chawla

¹

,

Perera

²

,

Fried

³

et al. 2020

Self Cite

View full text Add to dashboard Cite

Visual rhodopsin is an important archetype for G‐protein‐coupled receptors, which are membrane proteins implicated in cellular signal transduction. Herein, we show experimentally that approximately 80 water molecules flood rhodopsin upon light absorption to form a solvent‐swollen active state. An influx of mobile water is necessary for activating the photoreceptor, and this finding is supported by molecular dynamics (MD) simulations. Combined force‐based measurements involving osmotic and hydrostatic pressure indicate the expansion occurs by changes in cavity volumes, together with greater hydration in the active metarhodopsin‐II state. Moreover, we discovered that binding and release of the C‐terminal helix of transducin is coupled to hydration changes as may occur in visual signal amplification. Hydration–dehydration explains signaling by a dynamic allosteric mechanism, in which the soft membrane matter (lipids and water) has a pivotal role in the catalytic G‐protein cycle.

show abstract

Quasi-elastic Neutron Scattering Reveals Ligand-Induced Protein Dynamics of a G-Protein-Coupled Receptor

Cited by 29 publications

References 62 publications

Powdered G-Protein-Coupled Receptors

Powdered G-Protein-Coupled Receptors

Activation of the G‐Protein‐Coupled Receptor Rhodopsin by Water

Activation of the G‐Protein‐Coupled Receptor Rhodopsin by Water

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