Aminopurine based JNK inhibitors for the prevention of ischemia reperfusion injury.

Veronique Plantevin-Krenitsky,Mercedes Delgado,Lisa Nadolny,Kiran Sahasrabudhe,Leticia Ayala,Steven S. Clareen,Robert Hilgraf,Ronald J. Albers,Adam Kois,Kevin S. Hughes,Jonathan Wright,Jacek Nowakowski,Elise Sudbeck,Sutapa Ghosh,Sogole Bahmanyar,Philip P. Chamberlain,J. Muir,Brian E. Cathers,David Giegel,Li Xu,Maria Celeridad,Mehran F. Moghaddam,Oleg Khatsenko,Paul Omholt,Jason Katz,Sema Pai,Rachel Fan,Yang Tang,Michael A. Shirley,Brent Benish,Kate Blease,Heather Raymon,Shripad S. Bhagwat,Ian Henderson,Andrew G. Cole,Brydon L. Bennett,Yoshitaka Satoh

Aminopurine based JNK inhibitors for the prevention of ischemia reperfusion injury.

2012

In this Letter we describe the optimization of an aminopurine lead (1) with modest potency and poor overall kinase selectivity which led to the identification of a series of potent, selective JNK inhibitors. Improvement in kinase selectivity was enabled by introduction of an aliphatic side chain at the C-2 position. CC-359 (2) was selected as a potential clinical candidate for diseases manifested by ischemia reperfusion injury.

Keywords:

Side chain
Ischemia
Selectivity
Drug
Potency
Kinase
Reperfusion injury
Biochemistry
Aminopurine
Chemistry
Enzyme activator
Structure–activity relationship
2-Aminopurine

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations