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寻找DNA修复抑制剂:核酸碱基-吖啶共轭物与含无碱基位点的DNA双链体的选择性结合。

Search for DNA repair inhibitors: selective binding of nucleic bases-acridine conjugates to a DNA duplex containing an abasic site.

作者信息

Berthet N, Constant J F, Demeunynck M, Michon P, Lhomme J

机构信息

L.E.D.S.S., Chimie Bioorganique, UMR CNRS 5616, Université Joseph Fourier, Grenoble, France.

出版信息

J Med Chem. 1997 Oct 10;40(21):3346-52. doi: 10.1021/jm970225t.

Abstract

The abasic site is one of the most frequent DNA lesions generated by spontaneous or enzymatic cleavage of the N-glycosidic bond. The abasic site is also an intermediate in the nucleotide and base excision DNA repair. We examined molecules which recognize and cleave DNA at the abasic site with high efficiency. These molecules incorporate in their structure a nucleic base for abasic site recognition, an intercalator for DNA binding, and a polyamino linker for ionic interaction and DNA cleavage. Such compounds, by interfering with abasic sites in DNA, are also inhibitors of DNA repair. In order to better understand the parameters of the interaction, we carried out a UV thermal denaturation study of synthetic oligonucleotides containing the lesion both in the absence and in the presence of the drugs. A similar study was also carried out using the corresponding nonmodified oligonucleotide. The results indicate selective binding of the base-chain-intercalator conjugates to the abasic site containing oligonucleotides.

摘要

无碱基位点是由N-糖苷键的自发或酶促裂解产生的最常见的DNA损伤之一。无碱基位点也是核苷酸和碱基切除DNA修复过程中的一个中间体。我们研究了能够高效识别并切割无碱基位点处DNA的分子。这些分子在其结构中包含用于无碱基位点识别的核酸碱基、用于DNA结合的嵌入剂以及用于离子相互作用和DNA切割的多氨基连接子。这类化合物通过干扰DNA中的无碱基位点,也是DNA修复的抑制剂。为了更好地理解相互作用的参数,我们对含有损伤的合成寡核苷酸在不存在和存在药物的情况下进行了紫外热变性研究。使用相应的未修饰寡核苷酸也进行了类似的研究。结果表明碱基-链-嵌入剂缀合物与含无碱基位点的寡核苷酸有选择性结合。

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