2,4-Disubstituted piperidines as selective CC chemokine receptor 3 (CCR3) antagonists : Synthesis and selectivity

Paul S. Watson,Bin Jiang,Kim Harrison,Nao Asakawa,Patricia K. Welch,Maryanne Covington,Nicole Stowell,Eric A. Wadman,Paul Davies,Kimberly A. Solomon,Robert C. Newton,George L. Trainor,Steven M. Friedman,Carl P. Decicco,Soo S. Ko

2,4-Disubstituted piperidines as selective CC chemokine receptor 3 (CCR3) antagonists : Synthesis and selectivity

2006

Paul S. Watson
Bin Jiang
Kim Harrison
Nao Asakawa
Patricia K. Welch
Maryanne Covington
Nicole Stowell
Eric A. Wadman
Paul Davies
Kimberly A. Solomon
Robert C. Newton
George L. Trainor
Steven M. Friedman
Carl P. Decicco
Soo S. Ko

Abstract Linear unselective CCR3 antagonist leads with IC 50 values in the 200 nM range were converted into low nM binding compounds selective at CCR3 by moving the piperidine nitrogen substituent to the carbon at the 2-position of the ring. Substitution of the piperidine nitrogen with simple alkyl and acyl groups was found to improve the selectivity of this new compound class. In particular, N -{3-[(2 S , 4 R )-1-(propyl)-4-(4-fluorobenzyl)piperidinyl]propyl}- N ′-(3-acetylphenyl)urea exhibited single digit nanomolar IC 50 values for CCR3 with >100-fold selectivity against an extensive counter screen panel.

Keywords:

Antagonist
Selectivity
Chemical synthesis
Organic chemistry
Alkyl
Urea
CC chemokine receptors
Biochemistry
Piperidine
Substituent
Stereochemistry
Chemistry

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