Dipartimento di Scienze della Salute, Università degli Studi "Magna Græcia", Campus "S. Venuta", Viale Europa, Germaneto 88100, Catanzaro, Italy.
Dipartimento di Scienze della Vita e dell'Ambiente, Università degli Studi di Cagliari, Via Ospedale 72, Cagliari 09124, Italy.
Molecules. 2014 Dec 24;20(1):206-23. doi: 10.3390/molecules20010206.
Several ligands can bind to the non-canonical G-quadruplex DNA structures thereby stabilizing them. These molecules can act as effective anticancer agents by stabilizing the telomeric regions of DNA or by regulating oncogene expression. In order to better interact with the quartets of G-quadruplex structures, G-binders are generally characterized by a large aromatic core involved in π-π stacking. Some natural flexible cyclic molecules from Traditional Chinese Medicine have shown high binding affinity with G-quadruplex, such as berbamine and many other alkaloids. Using the structural information available on G-quadruplex structures, we performed a high throughput in silico screening of commercially available alkaloid derivative databases by means of a structure-based approach based on docking and molecular dynamics simulations against the human telomeric sequence d[AG3(T2AG3)3] and the c-myc promoter structure. We identified 69 best hits reporting an improved theoretical binding affinity with respect to the active set. Among them, a berberine derivative, already known to remarkably inhibit telomerase activity, was related to a better theoretical affinity versus c-myc.
几种配体可以与非经典 G-四链体 DNA 结构结合,从而稳定它们。这些分子可以通过稳定 DNA 的端粒区域或调节癌基因表达来作为有效的抗癌剂。为了更好地与 G-四链体结构的四联体相互作用,G-结合物通常的特征是涉及 π-π 堆积的大芳香核。一些来自中药的天然柔性环状分子显示出与 G-四链体的高结合亲和力,如小檗碱和许多其他生物碱。利用 G-四链体结构的可用结构信息,我们通过基于对接和分子动力学模拟的结构方法,对商业可用的生物碱衍生物数据库进行了高通量的计算机筛选,针对人端粒序列 d[AG3(T2AG3)3]和 c-myc 启动子结构。我们确定了 69 个最佳命中,报告相对于活性集提高了理论结合亲和力。其中,一种已知能显著抑制端粒酶活性的小檗碱衍生物与 c-myc 的理论亲和力更好。
