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Effect of Linker Length and Composition on Heterobivalent Ligand‐Mediated Receptor Cross‐Talk between the A 1 Adenosine and β 2 Adrenergic Receptors
Author(s) -
Barlow Nicholas,
Baker Stephen P.,
Scammells Peter J.
Publication year - 2013
Publication title -
chemmedchem
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.817
H-Index - 100
eISSN - 1860-7187
pISSN - 1860-7179
DOI - 10.1002/cmdc.201300286
Subject(s) - agonist , receptor , chemistry , moiety , adenosine , adenosine receptor , ligand (biochemistry) , stereochemistry , linker , alprenolol , adrenergic receptor , pharmacophore , partial agonist , biochemistry , computer science , operating system
Heterobivalent ligands that possess pharmacophores designed to interact with both the A 1 adenosine receptor (A 1 AR) and the β 2 adrenergic receptor (β 2 AR) were prepared. More specifically, these ligands contain an adenosine moiety that is linked via its N 6 ‐position to the amino group of the saligenin‐substituted ethanolamine moiety present in the well‐known β 2 AR agonist, salbutamol. The affinities of these ligands were determined at both receptors and found to vary with linker length and composition. With all compounds, affinity and functional potencies were found to have selectivity for the A 1 AR over the β 2 AR. In all cases, cAMP accumulation (a β 2 AR‐mediated response) was mainly observed when the A 1 AR was blocked or its function decreased by pertussis toxin or chronic agonist treatment. This suggests that heterobivalent compounds for receptors that mediate opposite responses might be useful for elucidating the mechanisms of receptor cross‐talk and how this interaction, in terms of responsiveness, may change under pathophysiological conditions.