SAR and biological evaluation of 3-azabicyclo[3.1.0]hexane derivatives as μ opioid ligands.

Graham Lunn,Lee R. Roberts,Douglas James Critcher,Sara Douglas,Ashley Edward Fenwick,David Morris Gethin,Graham Goodwin,David H.J. Greenway,Sean D.W. Greenwood,Kim Thomas Hall,Martin Thomas,Stephen Thompson,David H. Williams,Gavin Wood,Andrew Wylie

SAR and biological evaluation of 3-azabicyclo[3.1.0]hexane derivatives as μ opioid ligands.

2012

Graham Lunn
Lee R. Roberts
Douglas James Critcher
Sara Douglas
Ashley Edward Fenwick
David Morris Gethin
Graham Goodwin
David H.J. Greenway
Sean D.W. Greenwood
Kim Thomas Hall
Martin Thomas
Stephen Thompson
David H. Williams
Gavin Wood
Andrew Wylie

Abstract 3-Azabicyclo[3.1.0]hexane compounds were designed as novel achiral μ opioid receptor ligands for the treatment of pruritus in dogs. In this paper, we describe the SAR of this class of opioid ligand, highlighting changes to the lead structure which led to compounds having picomolar binding affinity, selective for the μ receptor over δ and κ subtypes. Some subtleties of functional activity will also be described.

Keywords:

Hexane
Stereochemistry
Organic chemistry
Ligand (biochemistry)
Opioid receptor
Opioid
Receptor
Chemistry
Ligand
Chirality (chemistry)
biological evaluation
Structure–activity relationship

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