Fragment-Based Drug Discovery of Potent Protein Kinase C Iota Inhibitors.
Jacek KwiatkowskiBoping LiuDoris Hui Ying TeeGuoying ChenNur Huda Binte AhmadYun Xuan WongZhi Ying PohShi Hua AngEldwin Sum Wai TanEsther Hq Ongnull Nurul DinieAnders PoulsenVishal PendharkarKanda SangthongpitagMay Ann LeeSugunavathi SepramaniamSoo Yei HoJoseph CherianJeffrey HillThomas H KellerAlvin W HungPublished in: Journal of medicinal chemistry (2018)
Protein kinase C iota (PKC-ι) is an atypical kinase implicated in the promotion of different cancer types. A biochemical screen of a fragment library has identified several hits from which an azaindole-based scaffold was chosen for optimization. Driven by a structure-activity relationship and supported by molecular modeling, a weakly bound fragment was systematically grown into a potent and selective inhibitor against PKC-ι.