| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 10594255 | Bioorganic & Medicinal Chemistry Letters | 2012 | 8 Pages |
Abstract
A high throughput screening (HTS) hit, 1 (Plk1 Ki = 2.2 μM) was optimized and evaluated for the enzymatic inhibition of Plk-1 kinase. Molecular modeling suggested the importance of adding a hydrophobic aromatic amine side chain in order to improve the potency by a classic kinase H-donor-acceptor binding mode. Extensive SAR studies led to the discovery of 49 (Plk1 Ki = 5 nM; EC50 = 1.05 μM), which demonstrated moderate efficacy at 100 mpk in a MiaPaCa tumor model, with no overt toxicity.
Keywords
Related Topics
Physical Sciences and Engineering
Chemistry
Organic Chemistry
Authors
Qingwei Zhang, Zhiren Xia, Michael J. Mitten, Loren M. Lasko, Vered Klinghofer, Jennifer Bouska, Eric F. Johnson, Thomas D. Penning, Yan Luo, Vincent L. Giranda, Alexander R. Shoemaker, Kent D. Stewart, Stevan W. Djuric, Anil Vasudevan,