Discovery of a Potent Class of PI3Kα Inhibitors
with Unique Binding Mode via Encoded Library Technology (ELT)

G. Joseph Franklin (1370352); Ghotas Evindar (1370346); Hongfang Yang (1370343); Jennifer L. DeLorey (1370328); Joelle L. Burgess (1370331); John
W. Cuozzo (1370322); Kaushik Raha (1370313); Kenneth E. Lind (1370316); Kurt R. Auger (449760); Matthew A. Clark (1370337); Michael D. Schaber (1370355); Nicholas D. Adams (1370334); Paolo
A. Centrella (1370349); Patricia Elkins (1370307); Patricia F. Medeiros (1370325); Ruth Lehr (1370319); Sibongile Mataruse (1370310); Stanley J. Schmidt (1370340); Steven D. Knight (1370304); Steven R. Skinner (1370358); Yun Ding (234322)

Discovery of a Potent Class of PI3Kα Inhibitors with Unique Binding Mode via Encoded Library Technology (ELT)

Abstract

In the search of PI3K p110α wild type and H1047R mutant selective small molecule leads, an encoded library technology (ELT) campaign against the desired target proteins was performed which led to the discovery of a selective chemotype for PI3K isoforms from a three-cycle DNA encoded library. An X-ray crystal structure of a representative inhibitor from this chemotype demonstrated a unique binding mode in the p110α protein

Similar works

Full text

Available Versions

FigShare

oai:figshare.com:article/20568...

Last time updated on 12/02/2018