CCR2 receptor antagonists: Optimization of biaryl sulfonamides to increase activity in whole blood

Gren Z. Wang,Pamela A. Haile,Tom Daniel,Benjamin Belot,Andrew Q. Viet,Krista B. Goodman,Deyou Sha,Sarah E. Dowdell,Norbert Varga,Xuan Hong,Subhas J. Chakravorty,Christine L. Webb,Carla A. Cornejo,Alan R. Olzinski,Roberta E. Bernard,Christopher Evans,Amanda Emmons,Jacques Briand,Chun-wa Chung,Ruben Quek,Dennis Lee,Peter J. Gough,Clark A. Sehon

CCR2 receptor antagonists: Optimization of biaryl sulfonamides to increase activity in whole blood

2011

Abstract A series of biarylsulfonamides was identified as hCCR2 receptor antagonist but suffered from high plasma protein binding resulting in a >100 fold shift in activity in a functional GTPγS assay run in tandem in the presence and absence of human serum albumin. Introduction of an aryl amide with ethylenediamine linker led to compounds with reduced shifts and improved activity in whole blood.

Keywords:

CCR2
Receptor antagonist
Aryl
Amide
Human serum albumin
Biochemistry
Organic chemistry
Plasma protein binding
Ethylenediamine
Chemistry
Receptor
Linker
Whole blood

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