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Copper bis-Dipyridoquinoxaline Is a Potent DNA Intercalator that Induces Superoxide-Mediated Cleavage via the Minor Groove

机译:双二吡啶并喹喔啉铜是有效的DNA嵌入剂可通过小沟诱导超氧化物介导的裂解。

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摘要

Herein, we report the synthesis, characterisation, X-ray crystallography, and oxidative DNA binding interactions of the copper artificial metallo-nuclease [Cu(DPQ) (NO )](NO ), where DPQ = dipyrido[3,2- :2′,3′- ]quinoxaline. The cation [Cu(DPQ) ] (Cu-DPQ), is a high-affinity binder of duplex DNA and presents an intercalative profile in topoisomerase unwinding and viscosity experiments. Artificial metallo-nuclease activity occurs in the absence of exogenous reductant but is greatly enhanced by the presence of the reductant Na- -ascorbate. Mechanistically, oxidative DNA damage occurs in the minor groove, is mediated aerobically by the Cu(I) complex and is dependent on both superoxide and hydroxyl radical generation. To corroborate cleavage at the minor groove, DNA oxidation of a cytosine–guanine (5′-CCGG-3′)-rich oligomer was examined in tandem with a 5-methylcytosine (5′-C5mCGG-3′) derivative where 5mC served to sterically block the major groove and direct damage to the minor groove. Overall, both the DNA binding affinity and cleavage mechanism of Cu-DPQ depart from Sigman’s reagent [Cu(1,10-phenanthroline) ] ; however, both complexes are potent oxidants of the minor groove.
机译:在这里,我们报告的合成,表征,X射线晶体学和铜人工金属核酸酶[Cu(DPQ)(NO)](NO)的氧化DNA结合相互作用,其中DPQ =双吡啶[3,2-:2 ′,3′-]喹喔啉。阳离子[Cu(DPQ)](Cu-DPQ)是双链体DNA的高亲和力结合剂,在拓扑异构酶展开和粘度实验中表现出嵌入特征。人造金属核酸酶活性在不存在外源还原剂的情况下发生,但是由于存在还原剂Na-抗坏血酸盐而大大增强。从机理上讲,氧化性DNA损伤发生在小沟中,由Cu(I)络合物有氧介导,并且取决于超氧化物和羟基自由基的产生。为了证实在小沟处的裂解,与5-甲基胞嘧啶(5'-C5mCGG-3')衍生物串联检测了富含胞嘧啶-鸟嘌呤(5'-CCGG-3')的寡聚物的DNA氧化,其中5mC用于在空间上阻塞主要凹槽,并直接损坏次要凹槽。总体而言,Cu-DPQ的DNA结合亲和力和裂解机理均不同于Sigman试剂[Cu(1,10-phenanthroline)];但是,两种络合物都是小沟的强氧化剂。

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