Crystal structure of the adenosine A
            <sub>2A</sub>
            receptor bound to an antagonist reveals a potential allosteric pocket

Sun, Bingfa; Bachhawat, Priti; Chu, Matthew; Wood, Martyn; Ceska, Tom; Sands, Zara A.; Mercier, Joël; Lebon, Florence; Kobilka, Tong Sun; Kobilka, Brian K.

doi:10.1073/pnas.1621423114

Cited by 116 publications

(110 citation statements)

References 32 publications

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“…Ye et al utilized an XAC ligand affinity column as an additional chromatography step during purification (Ye et al, 2016) that we did not include in this study. Our purification is similar to what has been published in structural studies of A 2A R, following a general purification scheme of IMAC followed by size exclusion chromatography prior to crystallization in detergent (Hino et al, 2012;Carpenter et al, 2016;Sun et al, 2017) or lipidic cubic phase (Jaakola et al, 2008;Liu et al, 2012b;Xu et al, 2011). These structures contain A 2A R bound to agonists, antagonists, or in complex with an engineered 'mini-Gs' protein.…”

Section: Purificationmentioning

confidence: 95%

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

Clark

Dikiy

Chapman

et al. 2018

Biophysical Journal

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GPCRs regulate all aspects of human physiology, and biophysical studies have deepened our understanding of GPCR conformational regulation by different ligands. Yet there is no experimental evidence for how sidechain dynamics control allosteric transitions between GPCR conformations. To address this deficit, we generated samples of a wild-type GPCR (A 2A R) that are deuterated apart from 1 H/ 13 C NMR probes at isoleucine d1 methyl groups, which facilitated 1 H/ 13 C methyl TROSY NMR measurements with opposing ligands. Our data indicate that low [Na + ] is required to allow large agonist-induced structural changes in A 2A R, and that patterns of sidechain dynamics substantially differ between agonist (NECA) and inverse agonist (ZM241385) bound receptors, with the inverse agonist suppressing fast ps-ns timescale motions at the G protein binding site. Our approach to GPCR NMR creates a framework for exploring how different regions of a receptor respond to different ligands or signaling proteins through modulation of fast ps-ns sidechain dynamics.

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Section: Purificationmentioning

confidence: 95%

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

Clark

Dikiy

Chapman

et al. 2018

Biophysical Journal

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“…[1] Theadenosine 2A receptor (A 2A R) represents ap romising target for Parkinsonsd isease [2] and drug development efforts led to the discovery of Cmpd-1, ad ual antagonist to the A 2A Ra nd the N-methyl d-aspartate receptor subtype 2B (NR2B). [3] Them ethylphenyl and aminotriazole rings of Cmpd-1 occupy adeeply buried position similar to the widely- Figure 1. [3] Them ethylphenyl and aminotriazole rings of Cmpd-1 occupy adeeply buried position similar to the widely- Figure 1.…”

mentioning

confidence: 82%

“…Cmpd-1, composed of three rings including ac entral aminotriazole,amethylphenyl and amethoxyphenyl, was crystallised in complex with the A 2A R (Figure 1). [4] B,C) Superimposing A 2A Rbound to ZM 241385 (5OLG, [5] grey,StaR2, cytochrome b562-RIL (BRIL) in ICL3 -o mitted for clarity,and 3PWH, [4] light green, StaR2, no ICL3 insert), Cmpd-1 (5UIG, [3] orange, wild type with BRIL in ICL3) and caffeine (3RFM, [4] blue, StaR2, no ICL3 insert) reveals the unusual outward movement of helix Vwith Cmpd-1. A) Depending on the construct used, the phenyl moiety of ZM 241385 either points towards ECL2 (grey) or aligns with the methoxyphenyl moiety of Cmpd-1 pointing down towards helix I(light green (thermostabilised StaR2) with Cmpd-1 in orange).…”

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confidence: 99%

“…This is consistent with the published rationalisation of the 19 Fc hemical shift on V229 6.31 Cs ite where increased electronic shielding was linked to solvent exposure. [3] It is generally accepted that GPCR antagonists function by stabilising an inactive form of the receptor, through ac ombination of ligand-receptor interactions and intra-receptor contacts (e.g.the ionic lock). [3] It is generally accepted that GPCR antagonists function by stabilising an inactive form of the receptor, through ac ombination of ligand-receptor interactions and intra-receptor contacts (e.g.the ionic lock).…”

mentioning

confidence: 99%

“…[16] Cmpd-1 exchanges between equally populated MS4 and 5and thus occupies an extended orthosteric site and am etastable allosteric site with equal probability. [3] However,t he binding to the extended orthosteric site, although important, might be only part of the binding picture. [3] However,t he binding to the extended orthosteric site, although important, might be only part of the binding picture.…”

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confidence: 99%

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The Aminotriazole Antagonist Cmpd‐1 Stabilises a Distinct Inactive State of the Adenosine 2A Receptor

et al. 2019

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The widely expressed G-protein coupled receptors (GPCRs) are versatile signal transducer proteins that are attractive drug targets but structurally challenging to study. GPCRs undergo anumber of conformational rearrangements when transitioning from the inactive to the active state but have so far been believed to adopt af airly conserved inactive conformation. Using 19 FNMR spectroscopya nd advanced molecular dynamics simulations we describe an ovel inactive state of the adenosine 2A receptor which is stabilised by the aminotriazole antagonist Cmpd-1. We demonstrate that the ligand stabilises aunique conformation of helix Vand present data on the putative binding mode of the compound involving contacts to the transmembrane bundle as well as the extracellular loop 2.

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Structure‐Based Drug Design for G Protein‐Coupled Receptors

Congreve

Christopher

Graaf

2021

Burger's Medicinal Chemistry and Drug Discovery

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A transformation in the structural biology of membrane‐associated receptors, particularly of G Protein‐Coupled Receptors (GPCRs), has occurred over the last 10 years and continues to build momentum today. Remarkable new protein–ligand X‐ray crystal and latterly cryo‐EM structures have been published giving a detailed appreciation of how molecules bind to a plethora of fascinating binding sites. The profound impact of these new data on design of ligands for drug discovery, a detailed consideration of the consequences to the computational chemistry community, and a description of some representative applications of Structure‐Based Drug Design (SBDD) are described in this article, with a focus on GPCRs.

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Crystal structure of the adenosine A _2A receptor bound to an antagonist reveals a potential allosteric pocket

Cited by 116 publications

References 32 publications

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

The Aminotriazole Antagonist Cmpd‐1 Stabilises a Distinct Inactive State of the Adenosine 2A Receptor

Structure‐Based Drug Design for G Protein‐Coupled Receptors

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Crystal structure of the adenosine A 2A receptor bound to an antagonist reveals a potential allosteric pocket

Cited by 116 publications

References 32 publications

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

Ligand Modulation of Sidechain Dynamics in a Wild-Type Human GPCR

The Aminotriazole Antagonist Cmpd‐1 Stabilises a Distinct Inactive State of the Adenosine 2A Receptor

Structure‐Based Drug Design for G Protein‐Coupled Receptors

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Crystal structure of the adenosine A _2A receptor bound to an antagonist reveals a potential allosteric pocket