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含端粒 DNA 序列中 DNA 靶向 9-氨基吖啶顺铂类似物的序列选择性。

The sequence selectivity of DNA-targeted 9-aminoacridine cisplatin analogues in a telomere-containing DNA sequence.

机构信息

School of Biotechnology and Biomolecular Sciences, University of New South Wales, Sydney, Australia.

出版信息

J Biol Inorg Chem. 2011 Jun;16(5):735-43. doi: 10.1007/s00775-011-0774-y. Epub 2011 Apr 5.

Abstract

In this study, the detailed DNA sequence specificity of four acridine Pt complexes was examined and compared with that of cisplatin. The DNA sequence specificity was determined in a telomere-containing DNA sequence using a polymerase stop assay, with a fluorescent primer and an automated capillary DNA sequencer. The Pt compounds included an acridine intercalating moiety that was modified to give a 9-aminoacridine derivative, a 7-methoxy-9-aminoacridine derivative, a 7-fluoro-9-aminoacridine derivative and a 9-ethanolamine-acridine derivative. Compared with cisplatin, the DNA sequence specificity was most altered for the 7-methoxy-9-aminoacridine compound, followed by the 9-aminoacridine derivative, the 7-fluoro-9-aminoacridine compound and the 9-ethanolamine-acridine derivative. The DNA sequence selectivity for the four acridine Pt complexes was shifted away from runs of consecutive guanines towards single guanine bases, especially 5'-GA dinucleotides and sequences that contained 5'-CG. The sequence specificity was examined in telomeric and non-telomeric DNA sequences. Although it was found that telomeric DNA sequences were extensively damaged by the four acridine Pt complexes, there was no extra preference for telomeric sequences.

摘要

在这项研究中,详细检查了四种吖啶铂配合物的 DNA 序列特异性,并将其与顺铂进行了比较。使用聚合酶停止测定法、荧光引物和自动毛细管 DNA 测序仪,在含有端粒的 DNA 序列中确定了 DNA 序列特异性。Pt 化合物包括吖啶嵌入部分,其被修饰为 9-氨基吖啶衍生物、7-甲氧基-9-氨基吖啶衍生物、7-氟-9-氨基吖啶衍生物和 9-乙醇胺-吖啶衍生物。与顺铂相比,7-甲氧基-9-氨基吖啶化合物的 DNA 序列特异性改变最大,其次是 9-氨基吖啶衍生物、7-氟-9-氨基吖啶化合物和 9-乙醇胺-吖啶衍生物。四种吖啶铂配合物的 DNA 序列选择性从连续鸟嘌呤的延伸转移到单个鸟嘌呤碱基,特别是 5'-GA 二核苷酸和含有 5'-CG 的序列。在端粒和非端粒 DNA 序列中检查了序列特异性。虽然发现四种吖啶铂配合物广泛损伤端粒 DNA 序列,但对端粒序列没有额外的偏好。

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