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  • BibTeX
Structure-based development of a subtype-selective orexin 1 receptor antagonist
Proceedings of the National Academy of Sciences - PNAS, 2020-07, Vol.117 (30), p.18059-18067
2020

Details

Autor(en) / Beteiligte
Titel
Structure-based development of a subtype-selective orexin 1 receptor antagonist
Ist Teil von
  • Proceedings of the National Academy of Sciences - PNAS, 2020-07, Vol.117 (30), p.18059-18067
Ort / Verlag
United States: National Academy of Sciences
Erscheinungsjahr
2020
Link zum Volltext
Quelle
EZB Electronic Journals Library
Beschreibungen/Notizen
  • Orexins are neuropeptides that activate the rhodopsin-like G proteincoupled receptors OX1R and OX2R. The orexin system plays an important role in the regulation of the sleep-wake cycle and the regulation of feeding and emotions. The nonselective orexin receptor antagonist suvorexant has been the first drug on the market targeting the orexin system and is prescribed for the treatment of insomnia. Subtype-selective OX1R antagonists are valuable tools to further investigate the functions and physiological role of the OX1R in vivo and promising lead compounds for the treatment of drug addiction, anxiety, pain or obesity. Starting from the OX1R and OX2R crystal structures bound to suvorexant, we exploited a single amino acid difference in the orthosteric binding site by using molecular docking and structure-based drug design to optimize ligand interactions with the OX1R while introducing repulsive interactions with the OX2R. A newly established enantiospecific synthesis provided ligands showing up to 75-fold selectivity for the OX1R over the OX2R subtype. The structure of a new OX1R antagonist with subnanomolar affinity (JH112) was determined by crystallography in complex with the OX1R and corresponded closely to the dockingpredicted geometry. JH112 exhibits high selectivity over a panel of different GPCRs, is able to cross the blood–brain barrier and acts as slowly diffusing and insurmountable antagonist for Gq protein activation and in particular β-arrestin-2 recruitment at OX1R. This study demonstrates the potential of structure-based drug design to develop more subtype-selective GPCR ligands with potentially reduced side effects and provides an attractive probe molecule and lead compound.
Sprache
Englisch
Identifikatoren
ISSN: 0027-8424
eISSN: 1091-6490
DOI: 10.1073/pnas.2002704117
Titel-ID: cdi_pubmedcentral_primary_oai_pubmedcentral_nih_gov_7395530
Format
Schlagworte
Amino acids, Arrestin, BASIC BIOLOGICAL SCIENCES, Binding Sites, Biological Sciences, Blood-brain barrier, Crystal structure, Crystallography, Design optimization, Diffusion barriers, Diffusion rate, Drug addiction, Drug Design, Drug development, G protein-coupled receptors, In vivo methods and tests, Insomnia, Kinetics, Lead, Lead compounds, Ligands, Molecular docking, Molecular Docking Simulation, Molecular Dynamics Simulation, Molecular structure, Neuropeptides, Orexin Receptor Antagonists - chemistry, Orexin Receptor Antagonists - pharmacology, Orexin Receptors - chemistry, Orexin Receptors - metabolism, Orexins, Pain, Protein Binding, Protein Conformation, Proteins, Receptors, Receptors, G-Protein-Coupled - antagonists & inhibitors, Receptors, G-Protein-Coupled - chemistry, Rhodopsin, Selectivity, Side effects, Sleep and wakefulness, Sleep disorders, Structure-Activity Relationship

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