Inhibition of human DNA topoisomerase I by new DNA minor groove ligands: derivatives of oligo-1,3-thiazolecarboxamides.

D. V. Bugreev, E. Vasyutina, V. Ryabinin, A. Sinyakov, V. Buneva, G. Nevinsky
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引用次数: 3

Abstract

A series of novel thiazole-containing oligopeptides (oligo-1,3-thiazolecarboxamides) interesting specifically with the minor groove of DNA was shown to inhibit human DNA topoisomerase I (topo I). Inhibitory effects of thiazole-containing oligopeptides (TCO) increase with the number of thiazole units in such compounds. Inhibitory properties of TCO containing 3 or 4 thiazole units were shown to be 3-10 times better than those of the well-known natural antibiotic, distamycin A containing pyrrole rings. The structure of various additional groups attached to the N-terminus and C-terminus of TCO had no significant effect on TCO interaction with the complex of DNA and topo I. TCO were shown to be capable of binding with double-stranded DNA (dsDNA), and the majority of TCO analyzed were more effective in binding with dsDNA than distamycin A. Possible reasons for the different effects of distamycin A and TCO on the reaction of relaxation catalyzed by topo I are discussed.
新的DNA小槽配体对人DNA拓扑异构酶I的抑制作用:低聚1,3-噻唑羧基酰胺衍生物。
一系列新型的含噻唑的寡肽(oligo-1,3-thiazolecarboxamides)具有抑制人类DNA拓扑异构酶I (topo I)的作用,其抑制作用随着这些化合物中噻唑单位的数量而增加。含有3或4个噻唑单位的TCO的抑制性能比含有吡咯环的著名天然抗生素双霉素A的抑制性能好3-10倍。各种其他基团的结构的n端和糖基对TCO TCO没有显著影响相互作用的复杂的DNA和威尼斯平底渔船I TCO被证明能够绑定与双链DNA (dsDNA),和大多数的TCO分析更有效的绑定与dsDNA distamycin A distamycin不同效果的可能原因和TCO放松催化的反应我威尼斯平底渔船进行了讨论。
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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