Literature DB >> 25183668

Biased signaling regulates the pleiotropic effects of the urotensin II receptor to modulate its cellular behaviors.

Cédric Brulé1, Nicolas Perzo2, Jane-Eileen Joubert3, Xavier Sainsily4, Richard Leduc4, Hélène Castel3, Laurent Prézeau5.   

Abstract

Biased agonism by G-protein-coupled receptor ligands has opened up strategies for targeted physiological or therapeutic actions. We hypothesized that urotensin II (UII)-derived peptides displayed unexpected physiological effects because of such biased signaling on the UII human urotensin (hUT) receptor. We determined the coupling to G proteins and β-arrestins of the UII-activated hUT receptor expressed in HEK293 using bioluminescence resonance energy transfer (BRET) biosensors, as well as the production of IP1-3 and cAMP using homogenous time-resolved Forster resonance energy transfer (FRET) (HTRF)-based assays. The activated receptor coupled to Gi1, GoA, Gq, and G13, excluding Gs, and recruited β-arrestins 1 and 2. Integration of these pathways led to a 2-phase kinetic phosphorylation of ERK1/2 kinases. The tested peptides induced three different profiles: UII, urotensin-related peptide (URP), and UII4-11 displayed the full profile; [Orn(8)]UII and [Orn(5)]URP activated G proteins, although with pEC50s 5-10× higher, and did not or barely recruited β-arrestin; urantide also failed to recruit β-arrestin but displayed a reversed rank order for Gi and Gq vs. Go pEC50s (-8.79±0.20, -8.43±0.21, and -7.86±0.36, respectively, for urantide, -7.87±0.10, -7.23±0.27, and -8.55±0.19, respectively, for [Orn(5)]URP) and was a partial agonist of all G-protein pathways. Interestingly, the peptides differently modulated cell survival but similarly induced cell migration and adhesion. Thus, we demonstrate biased signaling between β-arrestin and G proteins, and between G-protein subtypes, which dictates the receptor's cellular responses. © FASEB.

Entities:  

Keywords:  G-protein signaling; G-protein-coupled receptor; partial agonism; β-arrestin signaling

Mesh:

Substances:

Year:  2014        PMID: 25183668     DOI: 10.1096/fj.14-249771

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  13 in total

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5.  The network map of urotensin-II mediated signaling pathway in physiological and pathological conditions.

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6.  A Practical Guide to Approaching Biased Agonism at G Protein Coupled Receptors.

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Authors:  Hélène Castel; Laurence Desrues; Jane-Eileen Joubert; Marie-Christine Tonon; Laurent Prézeau; Marie Chabbert; Fabrice Morin; Pierrick Gandolfo
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Review 8.  The Autophagy Machinery: A New Player in Chemotactic Cell Migration.

Authors:  Pierre-Michaël Coly; Pierrick Gandolfo; Hélène Castel; Fabrice Morin
Journal:  Front Neurosci       Date:  2017-02-16       Impact factor: 4.677

9.  Signal profiling of the β1AR reveals coupling to novel signalling pathways and distinct phenotypic responses mediated by β1AR and β2AR.

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Journal:  Sci Rep       Date:  2020-05-29       Impact factor: 4.379

10.  Identification of key phosphorylation sites in PTH1R that determine arrestin3 binding and fine-tune receptor signaling.

Authors:  Diana Zindel; Sandra Engel; Andrew R Bottrill; Jean-Philippe Pin; Laurent Prézeau; Andrew B Tobin; Moritz Bünemann; Cornelius Krasel; Adrian J Butcher
Journal:  Biochem J       Date:  2016-09-13       Impact factor: 3.857

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