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首页> 外文期刊>Angewandte Chemie >The Benzyl Moiety in a Quinoxaline-Based Scaffold Acts as a DNA Intercalation Switch
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The Benzyl Moiety in a Quinoxaline-Based Scaffold Acts as a DNA Intercalation Switch

机译:喹喔啉基支架中的苄基部分充当DNA嵌入开关

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Quinoxaline antibiotics intercalate dsDNA and exhibit antitumor properties. However, they are difficult to synthesize and their structural complexity impedes a clear mechanistic understanding of DNA binding. Therefore design and synthesis of minimal-intercalators, using only part of the antibiotic scaffold so as to retain the key DNA-binding property, is extremely important. Reported is a unique example of a monomeric quinoxaline derivative of a 6-nitroquinoxaline-2,3-diamine scaffold which binds dsDNA by two different modes. While benzyl derivatives bound DNA in a sequential fashion, with intercalation as the second event, nonbenzyl derivatives showed only the first binding event. The benzyl intercalation switch provides important insights about molecular architecture which control specific DNA binding modes and would be useful in designing functionally important monomeric quinoxaline DNA binders and benchmarking molecular simulations.
机译:喹喔啉抗生素插入dsDNA并显示出抗肿瘤特性。然而,它们难以合成,并且其结构复杂性阻碍了对DNA结合的清晰机械理解。因此,仅使用部分抗生素支架来保留关键的DNA结合特性的最小嵌入剂的设计和合成就非常重要。报告的是6-硝基喹喔啉-2,3-二胺支架的单体喹喔啉衍生物的独特实例,该支架通过两种不同方式结合dsDNA。虽然苄基衍生物以插入的方式作为第二事件以顺序方式结合DNA,但非苄基衍生物仅显示第一结合事件。苄基插层开关提供了有关控制特定DNA结合模式的分子结构的重要见解,将对设计功能上重要的单体喹喔啉DNA结合剂和基准分子模拟很有用。

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