Novel bivalent securinine mimetics as topoisomerase I inhibitors
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Authors
Hou, Wen
Lin, Hui
Wang, Zhen-Ya
Banwell, Martin
Zeng, Ting
Sun, Ping-Hua
Lin, Jing
Chen, Wei-Min
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Royal Society of Chemistry
Abstract
A series of novel bivalent securinine mimetics incorporating different linkers between C-15 and C-15′ were
synthesized and their topoisomerase I (Topo I) inhibitory activities evaluated. It was thus revealed that mimetic
R2 incorporating a rigid m-substituted benzene linker exhibits Topo I inhibitory activity three times
that of parent securinine. Comprehensive structure–activity relationship analyses in combination with
docking studies were used to rationalize the potent activity of these bivalent mimetics. Mechanistic studies
served to confirm the deductions arising from docking studies that the active bivalent mimetics not only
inhibited complexation between Topo I and DNA but also stabilized the Topo I–DNA complex itself.
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Med. Chem. Commun.
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Open Access
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