2015
DOI: 10.1124/jpet.115.227959
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Recruitment ofβ-Arrestin 1 and 2 to theβ2-Adrenoceptor: Analysis of 65 Ligands

Abstract: Beyond canonical signaling via G a s and cAMP, the concept of functional selectivity at b 2 -adrenoceptors (b 2 ARs) describes the ability of adrenergic drugs to stabilize ligand-specific receptor conformations to initiate further signaling cascades comprising additional G-protein classes or b-arrestins (barr). A set of 65 adrenergic ligands including 40 agonists and 25 antagonists in either racemic or enantiopure forms was used for barr recruitment experiments based on a split-luciferase assay in a cellular s… Show more

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Cited by 27 publications
(18 citation statements)
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“…We initiated the study of the desensitization mechanisms of b3AR in a heterologous expression model, b3AR transfected HEK293T cells. In HEK293T cells transiently transfected with Mock or pCDNA3.1HA-b3AR (HEK293T-b3AR cells) we evaluated receptor expression by binding experiments using [ 3 H]CGP-12177 a ligand for b1/2/3ARs commonly used as a general b blocker (Vrydag and Michel, 2007;Suarez et al, 2014;Gherbi et al, 2015;Littmann et al, 2015). We found a three-fold increase in [ 3 H]CGP-12177 binding sites in HEK293T-b3AR (3024 ± 172) respect to Mock transfected cells (902 ± 50) ( Figure 1A) and a right shift in Kd from 12.8 ± 3.2 to 85.9 ± 14.3.…”
Section: Characterization Of Human B3armentioning
confidence: 99%
“…We initiated the study of the desensitization mechanisms of b3AR in a heterologous expression model, b3AR transfected HEK293T cells. In HEK293T cells transiently transfected with Mock or pCDNA3.1HA-b3AR (HEK293T-b3AR cells) we evaluated receptor expression by binding experiments using [ 3 H]CGP-12177 a ligand for b1/2/3ARs commonly used as a general b blocker (Vrydag and Michel, 2007;Suarez et al, 2014;Gherbi et al, 2015;Littmann et al, 2015). We found a three-fold increase in [ 3 H]CGP-12177 binding sites in HEK293T-b3AR (3024 ± 172) respect to Mock transfected cells (902 ± 50) ( Figure 1A) and a right shift in Kd from 12.8 ± 3.2 to 85.9 ± 14.3.…”
Section: Characterization Of Human B3armentioning
confidence: 99%
“…A research group has studied 65 β 2 -agonists for biased agonism in the signaling pathways downstream of the β 2 -adrenoceptor, namely, G s , β-arrestin-1, and β-arrestin-2 [42][43][44]. These series of studies have included many FEN derivatives including (R,R')-FEN and (R,R')-MNF.…”
Section: Discussionmentioning
confidence: 99%
“…Studies from Clark and others (Carter and Hill, 2005;Moore et al, 2007;Gimenez et al, 2015;Masureel et al, 2018) demonstrated that salmeterol behaved as a biased ligand against b-arrestin recruitment and receptor desensitization relative to formoterol or epinephrine in assays using transfected cells, although another study suggested similar efficacies of salmeterol for G s -dependent signaling and b-arrestin-associated signaling (Drake et al, 2008). Littmann et al (2015) tested 40 b 2 -agonists in transfected HEK293 cells and reported a bias toward G s signaling over b-arrestin recruitment for many agonists, including salmeterol and fenoterol, relative to isoproterenol and formoterol. However, whether commonly used b 2 -agonists such as salmeterol exhibit functional bias in native systems still needs further investigation.…”
Section: B Currently Used B 2 -Agonist Drugs and Their Pharmacologicmentioning
confidence: 99%