From DNA damage to G2 arrest: the many roles of topoisomerase II.

Progress in cell cycle research Pub Date : 2003-01-01
Annette K Larsen, Alexandre E Escargueil, Andrzej Skladanowski
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引用次数: 0

Abstract

DNA topoisomerase II inhibitors are among the most widely used anticancer agents. These drugs are potent inducers of DNA strand breaks and G2 arrest. However, topoisomerase II is not only a target for anti-cancer drugs but also part of the cellular response to different types of DNA damage. Topoisomerase II forms molecular complexes with important cell cycle regulators including the p53 oncogene suppressor, the BRCT-containing protein TopBP1, 14-3-3 epsilon and Cdc2 kinase. The association between topoisomerase II and Cdc2 kinase likely represents the earliest step in mitotic chromatin condensation. Therefore, regulation of the topoisomerase II/Cdc2 interaction could represent a novel mechanism to delay mitotic onset.

从DNA损伤到G2阻滞:拓扑异构酶II的许多作用。
DNA拓扑异构酶II抑制剂是应用最广泛的抗癌药物之一。这些药物是DNA链断裂和G2阻滞的有效诱导剂。然而,拓扑异构酶II不仅是抗癌药物的靶标,也是细胞对不同类型DNA损伤反应的一部分。拓扑异构酶II与重要的细胞周期调节因子形成分子复合物,包括p53癌基因抑制因子、含有brct的蛋白TopBP1、14-3-3 epsilon和Cdc2激酶。拓扑异构酶II和Cdc2激酶之间的关联可能代表了有丝分裂染色质凝聚的最早步骤。因此,拓扑异构酶II/Cdc2相互作用的调控可能代表了一种延迟有丝分裂发生的新机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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