Benzothiazole derivatives as human DNA topoisomerase IIα inhibitors

被引:0
作者
Cigdem Kaplan-Ozen
Betul Tekiner-Gulbas
Egemen Foto
Ilkay Yildiz
Nuran Diril
Esin Aki
Ismail Yalcin
机构
[1] Hacettepe University,Biology Department, Molecular Biology Section, Faculty of Science
[2] Bilkent University,BilGen Genetics and Biotechnology Center, Department of Molecular Biology and Genetics
[3] Ankara University,Pharmaceutical Chemistry Department, Faculty of Pharmacy
来源
Medicinal Chemistry Research | 2013年 / 22卷
关键词
Benzothiazole derivatives; Human topoisomerase IIα; DNA binding; Intercalation; Catalytic inhibitor; Anticancer drugs;
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中图分类号
学科分类号
摘要
Benzothiazole derivatives resembling the structure of DNA purine bases were tested to determine their topoisomerase inhibition activities. Based on DNA topoisomerase I and II relaxation assay results, all 12 derivatives acted as human topoisomerase IIα inhibitors, whereas only two compounds inhibited Calf thymus topoisomerase I. 3-amino-2-(2-bromobenzyl)-1,3-benzothiazol-3-ium 4-methylbenzensulfonate (BM3) was observed to be the most effective human topoisomerase IIα inhibitor with the lowest IC50 value of 39 nM. The mechanistic studies suggested that BM3 was neither a DNA intercalator nor a topoisomerase poison, it was only a DNA minor groove-binding agent. BM3 initially bound to the DNA topoisomerase IIα enzyme, then to DNA. As a result, the tested benzothiazole derivatives were obtained as strong topoisomerase IIα inhibitors. The benzothiazole tosylated salt form BM3 was found as the most effective topoisomerase IIα inhibitor. BM3’s mechanisms of action might be its direct interaction with the enzyme. BM3’s minor groove-binding property might also contribute to this action. Hence, BM3 could be a good candidate as a new anticancer agent.
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页码:5798 / 5808
页数:10
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