Decahydroquinoline amides as highly selective CB2 agonists: Role of selectivity on in vivo efficacy in a rodent model of analgesia

Peter J. Manley,Amy E. Zartman,Daniel V. Paone,Christopher S. Burgey,Darrell A. Henze,Kimberly Della Penna,Reshma Desai,Michael D. Leitl,Wei Lemaire,Rebecca B. White,Suzie Yeh,Mark O. Urban,Stefanie A. Kane,George D. Hartman,Mark T. Bilodeau,B. Wesley Trotter

Decahydroquinoline amides as highly selective CB2 agonists: Role of selectivity on in vivo efficacy in a rodent model of analgesia

2011

Peter J. Manley
Amy E. Zartman
Daniel V. Paone
Christopher S. Burgey
Darrell A. Henze
Kimberly Della Penna
Reshma Desai
Michael D. Leitl
Wei Lemaire
Rebecca B. White
Suzie Yeh
Mark O. Urban
Stefanie A. Kane
George D. Hartman
Mark T. Bilodeau
B. Wesley Trotter

A novel series of decahydroquinoline CB2 agonists is described. Optimization of the amide substituent led to improvements in CB2/CB1 selectivity as well as physical properties. Two key compounds were examined in the rat CFA model of acute inflammatory pain. A moderately selective CB2 agonist was active in this model. A CB2 agonist lacking functional CB1 activity was inactive in this model despite high in vivo exposure both peripherally and centrally.

Keywords:

Chemical synthesis
Selectivity
Agonist
Carboxamide
Organic chemistry
In vivo
Chemistry
Cannabinoid receptor
In vitro
Biochemistry
Stereochemistry
Analgesic

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