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Vol. 292, Issue 2, 664-671, February 2000
2A/D-Adrenoceptors1
Department of Pharmaceutical Sciences, Northeastern University,
Boston, Massachusetts (W.-T.T., R.C.D.); and Department of
Pharmaceutical Sciences, University of Tennessee, Memphis, Tennessee
(D.D.M.).
Agonists and GTP exert reciprocal effects on the stability of the G
protein-coupled receptor/G protein complex, implying bidirectional control over the receptor/G protein interface. To investigate this
relationship, we compared the ability of a series of
hydroxyl-substituted phenethylamine and imidazoline agonists to
stimulate [35S]guanosine
5'-O-(3-thio)triphosphate ([35S]GTP
S)
binding in membranes from 
2A/D-adrenergic
receptor-transfected PC12 cells with the magnitude of the GTP-induced
reduction in agonist affinity in [3H]rauwolscine-binding
studies. Agents previously described as full and partial agonists in
functional studies showed similar relative efficacies in promoting GTP
binding (r = 0.97) as well as similar relative
potencies (r = 0.94). Efficacy among agonists for
promotion of [35S]GTPS binding was closely correlated
with the relative influence of GTPS on agonist binding
(r = 0.97), consistent with a bidirectional allosteric influence by agonists and GTP on receptor/G protein complexation. In an additional series of tolazoline derivatives, a
range in efficacy from full agonism to strong inverse agonism was
observed, depending on the presence or absence of hydroxyl substituents. Together these results suggest that agonist-induced repositioning of transmembrane helices via their hydroxyl interactions is a critical determinant of the stability of the receptor/G protein complex and therefore of agonist efficacy.
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