Synthesis and Biological Evaluation of a Series of Novel Inhibitor of Nek2/Hec1 Analogues

High expression in cancer 1 (Hec1) is an oncogene overly expressed in many human cancers. Small molecule inhibitor of Nek2/Hec1 (INH) targeting the Hec1 and its regulator, Nek2, in the mitotic pathway, was identified to inactivate Hec1/Nek2 function mediated by protein degradation that subsequently...

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Veröffentlicht in:Journal of medicinal chemistry 2009-03, Vol.52 (6), p.1757-1767
Hauptverfasser: Qiu, Xiao-Long, Li, Guideng, Wu, Guikai, Zhu, Jiewen, Zhou, Longen, Chen, Phang-Lang, Chamberlin, A. Richard, Lee, Wen-Hwa
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Sprache:eng
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Zusammenfassung:High expression in cancer 1 (Hec1) is an oncogene overly expressed in many human cancers. Small molecule inhibitor of Nek2/Hec1 (INH) targeting the Hec1 and its regulator, Nek2, in the mitotic pathway, was identified to inactivate Hec1/Nek2 function mediated by protein degradation that subsequently leads to chromosome mis-segregation and cell death. To further improve the efficacy of INH, a series of INH analogues were designed, synthesized, and evaluated. Among these 33 newly synthesized analogues, three of them, 6, 13, and 21, have 6−8 fold more potent cell killing activity than the previous lead compound INH1. Compounds 6 and 21 were chosen for analyzing the underlying action mechanism. They target directly the Hec1/Nek2 pathway and cause chromosome mis-alignment as well as cell death, a mechanism similar to that of INH1. This initial exploration of structural/functional relationship of INH may advance the progress for developing clinically applicable INH analogue.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm8015969