| Literature DB >> 32470395 |
Lauren M Slosky1, Yushi Bai1, Krisztian Toth2, Caroline Ray1, Lauren K Rochelle1, Alexandra Badea3, Rahul Chandrasekhar1, Vladimir M Pogorelov4, Dennis M Abraham5, Namratha Atluri1, Satyamaheshwar Peddibhotla6, Michael P Hedrick6, Paul Hershberger6, Patrick Maloney6, Hong Yuan7, Zibo Li8, William C Wetsel9, Anthony B Pinkerton10, Lawrence S Barak11, Marc G Caron12.
Abstract
Small molecule neurotensin receptor 1 (NTSR1) agonists have been pursued for more than 40 years as potential therapeutics for psychiatric disorders, including drug addiction. Clinical development of NTSR1 agonists has, however, been precluded by their severe side effects. NTSR1, a G protein-coupled receptor (GPCR), signals through the canonical activation of G proteins and engages β-arrestins to mediate distinct cellular signaling events. Here, we characterize the allosteric NTSR1 modulator SBI-553. This small molecule not only acts as a β-arrestin-biased agonist but also extends profound β-arrestin bias to the endogenous ligand by selectively antagonizing G protein signaling. SBI-553 shows efficacy in animal models of psychostimulant abuse, including cocaine self-administration, without the side effects characteristic of balanced NTSR1 agonism. These findings indicate that NTSR1 G protein and β-arrestin activation produce discrete and separable physiological effects, thus providing a strategy to develop safer GPCR-targeting therapeutics with more directed pharmacological action.Entities:
Keywords: G protein-coupled recpetor; GPCR; NTSR1; PET; addiction; allosteric modulator; cocaine; dopamine; methamphetamine; neurotensin receptor 1; positron emission tomography; self-administration; β-arrestin
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Year: 2020 PMID: 32470395 PMCID: PMC7466280 DOI: 10.1016/j.cell.2020.04.053
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582