Novel triazolopyridylbenzamides as potent and selective p38α inhibitors

Josep Aiguadé,Cristina Balagué,Inés Carranco,Francisco Caturla,María Domínguez,Paul Robert Eastwood,Cristina Esteve,Jacob González,Wenceslao Lumeras,Adelina Orellana,Sara Preciado,Ramón Roca,Laura Vidal,Bernat Vidal

Novel triazolopyridylbenzamides as potent and selective p38α inhibitors

2012

Josep Aiguadé
Cristina Balagué
Inés Carranco
Francisco Caturla
María Domínguez
Paul Robert Eastwood
Cristina Esteve
Jacob González
Wenceslao Lumeras
Adelina Orellana
Sara Preciado
Ramón Roca
Laura Vidal
Bernat Vidal

A new class of p38α inhibitors based on a biaryl-triazolopyridine scaffold was investigated. X-ray crystallographic data of the initial lead compound cocrystallised with p38α was crucial in order to uncover a unique binding mode of the inhibitor to the hinge region via a pair of water molecules. Synthesis and SAR was directed towards the improvement of binding affinity, as well as ADME properties for this new class of p38α inhibitors and ultimately afforded compounds showing good in vivo efficacy.

Keywords:

Lead compound
In vivo
ADME
Ligand (biochemistry)
Stereochemistry
Biochemistry
Chemistry
hinge region
crystallographic data

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