Receptor-Ligand Interaction-Based Virtual Screening for Novel Eg5/Kinesin Spindle Protein Inhibitors

Authors
Nagarajan, ShanthiSkoufias, Dimitrios A.Kozielski, FrankPae, Ae Nim
Issue Date
2012-03-22
Publisher
AMER CHEMICAL SOC
Citation
JOURNAL OF MEDICINAL CHEMISTRY, v.55, no.6, pp.2561 - 2573
Abstract
Eg5/KSP is a promising mitotic spindle target for drug discovery in cancer chemotherapy and the development of agents against fungal diseases. A range of Eg5 targeting compounds identified by in vitro or cell-based screening is currently in development. We employed structure-based virtual screening of a database of 700 000 compounds to identify three novel Eg5 inhibitors bearing quinazoline (24) or thioxoimidazolidine (30 and 37) scaffolds. The new compounds inhibit Eg5 ATPase activity, show growth inhibition in proliferation assays, and induce monoastral spindles in cells, the characteristic phenotype for Eg5 inhibiting agents. This is the first successful reported procedure for the identification of Eg5 inhibitors via receptor-ligand interaction-based virtual screening.
Keywords
MITOTIC KINESIN KSP; CELL-CYCLE BLOCK; POTENT INHIBITORS; GENETIC ALGORITHM; FLEXIBLE DOCKING; MITOCHONDRIAL PATHWAY; MOLECULAR DOCKING; BINDING-AFFINITY; DRUG DISCOVERY; AML CELLS; MITOTIC KINESIN KSP; CELL-CYCLE BLOCK; POTENT INHIBITORS; GENETIC ALGORITHM; FLEXIBLE DOCKING; MITOCHONDRIAL PATHWAY; MOLECULAR DOCKING; BINDING-AFFINITY; DRUG DISCOVERY; AML CELLS; Kinesin spindle protein; Eg5; anticancer; virtual screening
ISSN
0022-2623
URI
https://pubs.kist.re.kr/handle/201004/129428
DOI
10.1021/jm201290v
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KIST Article > 2012
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