A Novel Class of Dopamine D 4 Receptor Ligands Bearing an Imidazoline Nucleus

A Novel Class of Dopamine D 4 Receptor Ligands Bearing an Imidazoline Nucleus

Over the years, the 2‐substituted imidazoline nucleus has been demonstrated to be a bioversatile structural motif. In this study, novel imidazoline derivatives bearing a 3‐ and/or 4‐hydroxy‐ or methoxy‐substituted phenyl ring, linked by an ethylene bridge to position 2 of an N ‐benzyl‐ or N ‐pheneth...

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Veröffentlicht in:ChemMedChem 2016-08, Vol.11 (16), p.1819-1828
Hauptverfasser: Mammoli, Valerio, Bonifazi, Alessandro, Dal Ben, Diego, Giannella, Mario, Giorgioni, Gianfabio, Piergentili, Alessandro, Pigini, Maria, Quaglia, Wilma, Thomas, Ajiroghene, Newman, Amy H., Ferré, Sergi, Sanchez‐Soto, Marta, Keck, Thomas M., Del Bello, Fabio
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container_end_page 1828
container_issue 16
container_start_page 1819
container_title ChemMedChem
container_volume 11
creator Mammoli, Valerio
Bonifazi, Alessandro
Dal Ben, Diego
Giannella, Mario
Giorgioni, Gianfabio
Piergentili, Alessandro
Pigini, Maria
Quaglia, Wilma
Thomas, Ajiroghene
Newman, Amy H.
Ferré, Sergi
Sanchez‐Soto, Marta
Keck, Thomas M.
Del Bello, Fabio
description Over the years, the 2‐substituted imidazoline nucleus has been demonstrated to be a bioversatile structural motif. In this study, novel imidazoline derivatives bearing a 3‐ and/or 4‐hydroxy‐ or methoxy‐substituted phenyl ring, linked by an ethylene bridge to position 2 of an N ‐benzyl‐ or N ‐phenethyl‐substituted imidazoline nucleus, were prepared and studied against D 2 ‐like receptor subtypes. Binding studies highlighted that a set of N ‐phenethylimidazoline compounds are selective for D 4 over D 2 and D 3 receptors. In functional assays, the 3‐methoxy‐substituted derivative, endowed with the highest D 4 affinity value, and its 3‐hydroxy analogue behaved as partial agonists with low intrinsic efficacy and as competitive D 4 antagonists when tested in the presence of the D 2 ‐like receptor agonist quinpirole. Molecular docking analysis, performed using a homology model of the human D 4 receptor developed using the X‐ray crystal structure of the antagonist‐bound human D 3 receptor as a template, was in accordance with the binding results and provided useful information for the design of novel imidazoline D 4 receptor ligands based on this new scaffold.
doi_str_mv 10.1002/cmdc.201600022
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title A Novel Class of Dopamine D 4 Receptor Ligands Bearing an Imidazoline Nucleus
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