Structure-based design and subsequent optimization of 2-tolyl-(1,2,3-triazol-1-yl-4-carboxamide) inhibitors of p38 MAP kinase

Derek Cogan,Ronald A. Aungst,E.C. Breinlinger,Tazmeen N. Fadra,Daniel R. Goldberg,Ming-Hong Hao,Rachel R. Kroe,Neil Moss,Christopher Pargellis,Kevin Chungeng Qian,Alan David Swinamer

Structure-based design and subsequent optimization of 2-tolyl-(1,2,3-triazol-1-yl-4-carboxamide) inhibitors of p38 MAP kinase

2008

Derek Cogan
Ronald A. Aungst
E.C. Breinlinger
Tazmeen N. Fadra
Daniel R. Goldberg
Ming-Hong Hao
Rachel R. Kroe
Neil Moss
Christopher Pargellis
Kevin Chungeng Qian
Alan David Swinamer

Abstract A computer-aided drug design strategy leads to the identification of a new class of p38 inhibitors based on the 2-tolyl-(1,2,3-triazol-1-yl-4-carboxamide) scaffold. The tolyl triazole amides provided a potent platform amenable to optimization. Further exploration leads to compounds with greater than 100-fold improvement in binding affinity to p38. Derivatives prepared to alter the physicochemical properties produced inhibitors with IC 50 ’s in human whole blood as low as 83 nM.

Keywords:

Triazole
Enzyme
Organic chemistry
Chemical synthesis
Ligand (biochemistry)
Stereochemistry
Carboxamide
Biochemistry
Enzyme inhibitor
In vitro
Chemistry
Transferase

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