Potent and highly selective benzimidazole inhibitors of PI3-kinase delta

…, D Chantry, M Flagella, DM Goldstein…

Index: Murray, Jeremy M.; Sweeney, Zachary K.; Chan, Bryan K.; Balazs, Mercedesz; Bradley, Erin; Castanedo, Georgette; Chabot, Christine; Chantry, David; Flagella, Michael; Goldstein, David M.; Kondru, Rama; Lesnick, John; Li, Jun; Lucas, Matthew C.; Nonomiya, Jim; Pang, Jodie; Price, Stephen; Salphati, Laurent; Safina, Brian; Savy, Pascal P. A.; Seward, Eileen M.; Ultsch, Mark; Sutherlin, Daniel P. Journal of Medicinal Chemistry, 2012 , vol. 55, # 17 p. 7686 - 7695

Full Text: HTML

Citation Number: 31

Abstract

Inhibition of PI3Kδ is considered to be an attractive mechanism for the treatment of inflammatory diseases and leukocyte malignancies. Using a structure-based design approach, we have identified a series of potent and selective benzimidazole-based inhibitors of PI3Kδ. These inhibitors do not occupy the selectivity pocket between Trp760 and Met752 that is induced by other families of PI3Kδ inhibitors. Instead, the selectivity of ...

 Related Synthetic Route
morpholine Structure

110-91-8

morpholine

2,6-Dichloro-9-methyl-9H-purine Structure

2382-10-7

2,6-Dichloro-9-...

~%

9H-Purine, 2-chloro-9-Methyl-6-(4-Morpholinyl)- Structure

1148003-35-3

9H-Purine, 2-ch...


Home | MSDS/SDS Database Search | Journals | Product Classification | Biologically Active Compounds | Selling Leads | About Us | Disclaimer

Copyright © 2024 ChemSrc All Rights Reserved