G Protein‐Coupled Receptors as Drug Targets

Abstract G protein-coupled receptors (GPCRs) modulate a variety of physiological functions and have been proven to be outstanding drug targets. However, approximately one-third of all non-olfactory GPCRs are still orphans in respect to their signal transduction and physiological functions. Receptors of the class of Adhesion GPCRs (aGPCRs) are among these orphan receptors. They are characterized by unique features in their structure and tissue-specific expression, which yields them interesting candidates for deorphanization and testing as potential therapeutic targets. Capable of G-protein coupling and non-G protein-mediated function, aGPCRs may extend our repertoire of influencing physiological function. Besides their described significance in the immune and central nervous systems, growing evidence indicates a high importance of these receptors in metabolic tissue. RNAseq analyses revealed high expression of several aGPCRs in pancreatic islets, adipose tissue, liver, and intestine but also in neurons governing food intake. In this review, we focus on aGPCRs and their function in regulating metabolic pathways. Based on current knowledge, this receptor class represents high potential for future pharmacological approaches addressing obesity and other metabolic diseases.

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Beyond the Flavour: The Potential Druggability of Chemosensory G Protein-Coupled Receptors

International Journal of Molecular Sciences ◽

10.3390/ijms20061402 ◽

2019 ◽

Vol 20 (6) ◽

pp. 1402 ◽

Cited By ~ 15

Author(s):

Antonella Di Pizio ◽

Maik Behrens ◽

Dietmar Krautwurst

Keyword(s):

G Protein ◽

Drug Targets ◽

Current Knowledge ◽

Chemical Space ◽

G Protein Coupled Receptors ◽

The Body ◽

Odorant Receptors ◽

Taste Receptors ◽

Umami Taste ◽

G Protein Coupled

G protein-coupled receptors (GPCRs) belong to the largest class of drug targets. Approximately half of the members of the human GPCR superfamily are chemosensory receptors, including odorant receptors (ORs), trace amine-associated receptors (TAARs), bitter taste receptors (TAS2Rs), sweet and umami taste receptors (TAS1Rs). Interestingly, these chemosensory GPCRs (csGPCRs) are expressed in several tissues of the body where they are supposed to play a role in biological functions other than chemosensation. Despite their abundance and physiological/pathological relevance, the druggability of csGPCRs has been suggested but not fully characterized. Here, we aim to explore the potential of targeting csGPCRs to treat diseases by reviewing the current knowledge of csGPCRs expressed throughout the body and by analysing the chemical space and the drug-likeness of flavour molecules.

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G-Protein-Coupled Receptors in Drug Discovery: Nanosizing Using Cell-Free Technologies and Molecular Biology Approaches

CrossRef Listing of Deleted DOIs ◽

10.1177/1087057105280517 ◽

2005 ◽

Vol 10 (8) ◽

pp. 765-779 ◽

Cited By ~ 30

Author(s):

Wayne R. Leifert ◽

Amanda L. Aloia ◽

Olgatina Bucco ◽

Richard V. Glatz ◽

Edward J. McMurchie

Keyword(s):

Signal Transduction ◽

G Protein ◽

Drug Targets ◽

G Protein Coupled Receptors ◽

Orphan Receptors ◽

Molecular Switching ◽

Physiological Processes ◽

Current Cell ◽

G Protein Coupled ◽

Signaling Components

Signal transduction by G-protein-coupled receptors (GPCRs) underpins a multitude of physiological processes. Ligand recognition by the receptor leads to activation of a genericmolecular switch involving heterotrimeric G-proteins and guanine nucleotides. Signal transduction has been studied extensively with both cell-based systems and assays comprising isolated signaling components. Interest and commercial investment in GPCRs in areas such as drug targets, orphan receptors, highthroughput screening, biosensors, and so on will focus greater attention on assay development to allow for miniaturization, ultra-high throughput and, eventually, microarray/biochip assay formats. Although cell-based assays are adequate for many GPCRs, it is likely that these formatswill limit the development of higher density GPCRassay platforms mandatory for other applications. Stable, robust, cell-free signaling assemblies comprising receptor and appropriate molecular switching components will form the basis of future GPCR assay platforms adaptable for such applications as microarrays. The authors review current cell-free GPCR assay technologies and molecular biological approaches for construction of novel, functional GPCR assays.

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Heterodimers of G protein-coupled receptors as novel and distinct drug targets

Drug Discovery Today Therapeutic Strategies ◽

10.1016/j.ddstr.2006.11.001 ◽

2006 ◽

Vol 3 (4) ◽

pp. 437-443 ◽

Cited By ~ 4

Author(s):

Raphael Rozenfeld ◽

Fabien M. Décaillot ◽

Adriaan P. IJzerman ◽

Lakshmi A. Devi

Keyword(s):

G Protein ◽

Drug Targets ◽

G Protein Coupled Receptors ◽

G Protein Coupled

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Development of OPLS-AA/M Parameters for Simulations of G Protein-Coupled Receptors and Other Membrane Proteins

10.1101/2022.01.05.475148 ◽

2022 ◽

Author(s):

Michael J. Robertson ◽

Georgios Skiniotis

Keyword(s):

Membrane Proteins ◽

Force Field ◽

G Protein ◽

Drug Targets ◽

G Protein Coupled Receptors ◽

Dynamic Nature ◽

Post Translational Modifications ◽

Dynamics Simulations ◽

High Level ◽

G Protein Coupled

G protein-coupled receptors (GPCRs) and other membrane proteins are valuable drug targets, and their dynamic nature makes them attractive systems for study with molecular dynamics simulations and free energy approaches. Here, we report the development, implementation, and validation of OPLS-AA/M force field parameters to enable simulations of these systems. These efforts include the introduction of post-translational modifications including lipidations and phosphorylation. We also modify previously reported parameters for lipids to be more consistent with the OPLS-AA force field standard and extend their coverage. These new parameters are validated on a variety of test systems, with the results compared to high-level quantum mechanics calculations, experimental data, and simulations with CHARMM36m where relevant. The results demonstrate that the new parameters reliably reproduce the behavior of membrane protein systems.

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Lipid nanoparticle technologies for the study of G protein-coupled receptors in lipid environments

Biophysical Reviews ◽

10.1007/s12551-020-00775-5 ◽

2020 ◽

Vol 12 (6) ◽

pp. 1287-1302 ◽

Cited By ~ 1

Author(s):

Steven Lavington ◽

Anthony Watts

Keyword(s):

Membrane Proteins ◽

G Protein ◽

Drug Targets ◽

Large Family ◽

G Protein Coupled Receptors ◽

Integral Membrane Proteins ◽

Lipid Nanoparticle ◽

Wide Range ◽

Biophysical Studies ◽

G Protein Coupled

AbstractG protein-coupled receptors (GPCRs) are a large family of integral membrane proteins which conduct a wide range of biological roles and represent significant drug targets. Most biophysical and structural studies of GPCRs have been conducted on detergent-solubilised receptors, and it is clear that detergents can have detrimental effects on GPCR function. Simultaneously, there is increasing appreciation of roles for specific lipids in modulation of GPCR function. Lipid nanoparticles such as nanodiscs and styrene maleic acid lipid particles (SMALPs) offer opportunities to study integral membrane proteins in lipid environments, in a form that is soluble and amenable to structural and biophysical experiments. Here, we review the application of lipid nanoparticle technologies to the study of GPCRs, assessing the relative merits and limitations of each system. We highlight how these technologies can provide superior platforms to detergents for structural and biophysical studies of GPCRs and inform on roles for protein-lipid interactions in GPCR function.

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Orphan G protein-coupled receptors (GPCRs): biological functions and potential drug targets

Acta Pharmacologica Sinica ◽

10.1038/aps.2011.210 ◽

2012 ◽

Vol 33 (3) ◽

pp. 363-371 ◽

Cited By ~ 83

Author(s):

Xiao-long Tang ◽

Ying Wang ◽

Da-li Li ◽

Jian Luo ◽

Ming-yao Liu

Keyword(s):

G Protein ◽

Drug Targets ◽

G Protein Coupled Receptors ◽

Potential Drug ◽

Biological Functions ◽

G Protein Coupled ◽

Potential Drug Targets

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Regulation of G Protein-Coupled Receptors by Ubiquitination

10.20944/preprints201704.0135.v1 ◽

2017 ◽

Cited By ~ 1

Author(s):

Kamila Skieterska ◽

Pieter Rondou ◽

Kathleen Van Craenenbroeck

Keyword(s):

G Protein ◽

Posttranslational Modifications ◽

Drug Targets ◽

Current Knowledge ◽

G Protein Coupled Receptors ◽

Membrane Receptors ◽

Deubiquitinating Enzymes ◽

Range Of Functions ◽

Beta Arrestins ◽

G Protein Coupled

G protein-coupled receptors (GPCRs) comprise the largest family of membrane receptors that control many cellular processes and consequently often serve as drug targets. These receptors undergo a strict regulation by mechanisms such as internalization and desensitization, which are strongly influenced by posttranslational modifications. Ubiquitination is a posttranslational modification with a broad range of functions that is currently gaining increased appreciation as a regulator of GPCR activity. The role of ubiquitination in directing GPCRs for lysosomal degradation has already been well-established. Furthermore, this modification can also play a role in targeting membrane and endoplasmic reticulum-associated receptors to the proteasome. Most recently, ubiquitination was also shown to be involved in GPCR signaling. In this review, we present current knowledge on the molecular basis of GPCR regulation by ubiquitination, and highlight the importance of E3 ubiquitin ligases, deubiquitinating enzymes and β-arrestins. Finally, we discuss classical and newly-discovered functions of ubiquitination in controlling GPCR activity.

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Structural and Functional Characterization of G Protein-Coupled Receptors with Deep Mutational Scanning

10.1101/623108 ◽

2019 ◽

Cited By ~ 5

Author(s):

Eric M. Jones ◽

Nathan B. Lubock ◽

AJ Venkatakrishnan ◽

Jeffrey Wang ◽

Alex M. Tseng ◽

...

Keyword(s):

G Protein ◽

Drug Targets ◽

Functional Characterization ◽

Structure And Function ◽

G Protein Coupled Receptors ◽

Single Amino Acid ◽

Loss Of Function ◽

And Function ◽

Drug Receptors ◽

G Protein Coupled

AbstractIn humans, the 813 G protein-coupled receptors (GPCRs) are responsible for transducing diverse chemical stimuli to alter cell state, and are the largest class of drug targets. Their myriad structural conformations and various modes of signaling make it challenging to understand their structure and function. Here we developed a platform to characterize large libraries of GPCR variants in human cell lines with a barcoded transcriptional reporter of G-protein signal transduction. We tested 7,800 of 7,828 possible single amino acid substitutions to the beta-2 adrenergic receptor (β2AR) at four concentrations of the agonist isoproterenol. We identified residues specifically important for β2AR signaling, mutations in the human population that are potentially loss of function, and residues that modulate basal activity. Using unsupervised learning, we resolve residues critical for signaling, including all major structural motifs and molecular interfaces. We also find a previously uncharacterized structural latch spanning the first two extracellular loops that is highly conserved across Class A GPCRs and is conformationally rigid in both the inactive and active states of the receptor. More broadly, by linking deep mutational scanning with engineered transcriptional reporters, we establish a generalizable method for exploring pharmacogenomics, structure and function across broad classes of drug receptors.

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Ligand Docking Methods to Recognize Allosteric Inhibitors for G-protein Coupled Receptors

10.20944/preprints202012.0085.v1 ◽

2020 ◽

Author(s):

K Harini ◽

S Jayashree ◽

Vikas Tiwari ◽

Sneha Vishwanath ◽

Ramanathan Sowdhamini

Keyword(s):

Binding Site ◽

G Protein ◽

Drug Targets ◽

G Protein Coupled Receptors ◽

Ligand Docking ◽

Computational Docking ◽

Cellular Processes ◽

Activation Mechanisms ◽

Approved Drugs ◽

G Protein Coupled

G-protein coupled receptors (GPCRs) are large protein families known to be important in many cellular processes. They are well known for their allosteric activation mechanisms. They are drug targets for several FDA-approved drugs. We have investigated the diversity of the ligand binding site for these class of proteins against their cognate ligands using computational docking, even if their structures are known in the ligand-complexed form. The cognate ligand of some of these receptors dock at allosteric binding site, with better score than the binding at the conservative site. Further, ligands obtained from GLASS database, which consists of experimentally verified GPCR ligands, also show allosteric binding to GPCRs. The allosteric binders show strong affinity to the binding site, though the residues at the binding site are not conserved across GPCR subfamilies.

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