Design and synthesis of a functionally selective D3 agonist and its in vivo delivery via the intranasal route.

Julian Blagg,Charlotte Moira Norfor Allerton,David V. Batchelor,Andrew Douglas Baxter,Denise J. Burring,Christopher L. Carr,Andrew S. Cook,Carly L. Nichols,Joanne Phipps,Vivienne Sanderson,Hugh Verrier,Stephen K.-F. Wong

Design and synthesis of a functionally selective D3 agonist and its in vivo delivery via the intranasal route.

2007

Julian Blagg
Charlotte Moira Norfor Allerton
David V. Batchelor
Andrew Douglas Baxter
Denise J. Burring
Christopher L. Carr
Andrew S. Cook
Carly L. Nichols
Joanne Phipps
Vivienne Sanderson
Hugh Verrier
Stephen K.-F. Wong

Abstract This paper reports the synthesis and biological activity of a novel series of aryl-morpholine dopamine receptor agonists. Several compounds show high levels of functional selectivity for the D3 over the D2 dopamine receptor. Compound 26 has >1000-fold functional selectivity and has been successfully progressed in vivo using an intranasal delivery route.

Keywords:

Nasal administration
Functional selectivity
Dopamine
In vivo
Dopamine receptor D3
Agonist
Biochemistry
Dopamine receptor
Biological activity
Chemistry
Receptor
Structure–activity relationship
Pharmacology

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