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Profiling of basal and ligand-dependent GPCR activities by means of a polyvalent cell-based high-throughput platform

Manel Zeghal, Geneviève Laroche, Julia Douglas Freitas, Rebecca Wang, Patrick M. Giguère

2023Nature Communications24 citationsDOIOpen Access PDF

Abstract

Representing the most attractive and successful druggable receptors of the proteome, GPCRs regulate a myriad of physiological and pathophysiological functions. Although over half of present pharmaceuticals target GPCRs, the advancement of drug discovery is hampered by a lack of adequate screening tools, the majority of which are limited to probing agonist-induced G-protein and β-arrestin-2-mediated events as a measure of receptor activation. Here, we develop Tango-Trio, a comprehensive cell-based high-throughput platform comprising cumate-inducible expression of transducers, capable of the parallelized profiling of both basal and agonist-dependent GPCR activities. We capture the functional diversity of GPCRs, reporting β-arrestin-1/2 couplings, selectivities, and receptor internalization signatures across the GPCRome. Moreover, we present the construction of cumate-induced basal activation curves at approximately 200 receptors, including over 50 orphans. Overall, Tango-Trio's robustness is well-suited for the functional characterization and screening of GPCRs, especially for parallel interrogation, and is a valuable addition to the pharmacological toolbox.

Topics & Concepts

G protein-coupled receptorDruggabilityComputational biologyInternalizationAgonistReceptorDrug discoveryBiologyFunctional selectivityBioinformaticsBiochemistryGeneReceptor Mechanisms and SignalingNeuropeptides and Animal PhysiologyMonoclonal and Polyclonal Antibodies Research
Profiling of basal and ligand-dependent GPCR activities by means of a polyvalent cell-based high-throughput platform | Litcius