Expanding the Diversity of Allosteric Ber-Abl Inhibitors

Authors
Deng, XianmingOkram, BarunDing, QiangZhang, JianmingChoi, YongmunAdrian, Francisco J.Wojciechowski, AmyZhang, GuobaoChe, JianweiBursulaya, BadryCowan-Jacob, Sandra W.Rummel, GabrieleSim, TaeboGray, Nathanael S.
Issue Date
2010-10-14
Publisher
AMER CHEMICAL SOC
Citation
JOURNAL OF MEDICINAL CHEMISTRY, v.53, no.19, pp.6934 - 6946
Abstract
Inhibition of Bcr-Abl kinase activity by imatinib for the treatment of chronic myeloid leukemia (CM I.) currently serves as the paradigm or targeting dominant oncogenes with small molecules. We recently reported the discovery of GNF (1) and GNF (2) as selective non-ATP competitive inhibitors of cellular Bcr-Abl kinase activity that target the myristate binding site. Here, we used cell-based structure-activity relationships to guide the optimization and diversification of ligands that are capable of binding to the myristate binding site and rationalize the findings based upon an Abl-compound 1 cocrystal. We elucidate the structure-activity relationships required to obtain potent antiproliferative activity against Bcr-Abl transformed cells and report the discovery of new compounds (544, 5h, 6a, 14d, and 21j-1) that display improved potency or pharmacological properties. This work demonstrates that a variety of structures can effectively target the myristate binding site and provides new leads for developing drugs that can target this binding site.
Keywords
CHRONIC MYELOGENOUS LEUKEMIA; BCR-ABL; QUANTITATIVE-ANALYSIS; KINASE INHIBITOR; RESISTANCE; IMATINIB; PYRIMIDINES; MECHANISMS; BMS-354825; DISCOVERY; CHRONIC MYELOGENOUS LEUKEMIA; BCR-ABL; QUANTITATIVE-ANALYSIS; KINASE INHIBITOR; RESISTANCE; IMATINIB; PYRIMIDINES; MECHANISMS; BMS-354825; DISCOVERY
ISSN
0022-2623
URI
https://pubs.kist.re.kr/handle/201004/131007
DOI
10.1021/jm100555f
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KIST Article > 2010
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