Development of CXCR3 antagonists. Part 4: Discovery of 2-amino-(4-tropinyl)quinolines

Roland L. Knight,Daniel Rees Allen,Helen L. Birch,Gayle A. Chapman,Frances Celia Anne Galvin,Louise A. Jopling,Christopher James Lock,Johannes W.G. Meissner,David Alan Owen,Gilles Raphy,Robert John Watson,Sophie Caroline Williams

Development of CXCR3 antagonists. Part 4: Discovery of 2-amino-(4-tropinyl)quinolines

2008

Roland L. Knight
Daniel Rees Allen
Helen L. Birch
Gayle A. Chapman
Frances Celia Anne Galvin
Louise A. Jopling
Christopher James Lock
Johannes W.G. Meissner
David Alan Owen
Gilles Raphy
Robert John Watson
Sophie Caroline Williams

Abstract The synthesis and biological evaluation of a novel series of 2-aminoquinoline substituted piperidines and tropanes incorporating a homotropene moiety is herein described. The series exhibits potent antagonism of the CXCR3 receptor and superior physicochemical properties. Compound 24d was found to be orally bioavailable, and PK/PD studies suggested it as a suitable tool for studying the role of CXCR3 in models of disease.

Keywords:

Alkaloid
Antagonism
Organic chemistry
Moiety
Bicyclic molecule
Quinoline
Receptor
Chemistry
Biochemistry
Pharmacokinetics
Carboxamide
Stereochemistry
Tropane
In vitro

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