首页> 外文期刊>International Journal of Molecular Sciences >Toward G-Quadruplex-Based Anticancer Agents: Biophysical and Biological Studies of Novel AS1411 Derivatives
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Toward G-Quadruplex-Based Anticancer Agents: Biophysical and Biological Studies of Novel AS1411 Derivatives

机译:朝向基于G-Quadreplex的抗癌剂:新型AS1411衍生物的生物物理和生物学研究

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Certain G-quadruplex forming guanine-rich oligonucleotides (GROs), including AS1411, are endowed with cancer-selective antiproliferative activity. They are known to bind to nucleolin protein, resulting in the inhibition of nucleolin-mediated phenomena. However, multiple nucleolin-independent biological effects of GROs have also been reported, allowing them to be considered promising candidates for multi-targeted cancer therapy. Herein, with the aim of optimizing AS1411 structural features to find GROs with improved anticancer properties, we have studied a small library of AS1411 derivatives differing in the sequence length and base composition. The AS1411 derivatives were characterized by using circular dichroism and nuclear magnetic resonance spectroscopies and then investigated for their enzymatic resistance in serum and nuclear extract, as well as for their ability to bind nucleolin, inhibit topoisomerase I, and affect the viability of MCF-7 human breast adenocarcinoma cells. All derivatives showed higher thermal stability and inhibitory effect against topoisomerase I than AS1411. In addition, most of them showed an improved antiproliferative activity on MCF-7 cells compared to AS1411 despite a weaker binding to nucleolin. Our results support the hypothesis that the antiproliferative properties of GROs are due to multi-targeted effects.
机译:某些G-quadflex形成富含富含富含致癌的寡核苷酸(GROS),包括癌症选择性抗增殖活性。已知它们与核仁蛋白结合,导致核仁介导现象的抑制。然而,还报告了麦克风的多种核仁无关的生物学效应,使它们被认为是对多目标癌症治疗的有希望的候选者。这里,目的是优化具有改善的抗癌特性的GROS的AS1411结构特征,我们研究了在序列长度和基础组合物中不同的AS1411衍生物的小文库。通过使用圆形二色性和核磁共振谱来表征AS1411衍生物,然后在血清和核提取物中研究其酶促抗性,以及它们结合核仁抑制的能力,抑制拓扑异构酶I,并影响MCF-7人的可行性乳腺腺癌细胞。所有衍生物均显示出较高的热稳定性和抑制作用于拓扑异构酶I而不是AS1411。此外,尽管与核仁较弱,但它们中的大多数显示出对MCF-7细胞的改善的抗增殖活性。我们的研究结果支持该假设,即GROS的抗增殖性质是由于多目标的效果。

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