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Insights into the G-rich VEGF-binding aptamer V7t1: when two G-quadruplexes are better than one!

机译:洞察G-Rich的VEGF绑定适体V7T1:当两个G-Quadruplees优于一个时!

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摘要

The G-quadruplex-forming VEGF-binding aptamer V7t1 was previously found to be highly polymorphic in a K+-containing solution and, to restrict its conformational preferences to a unique, well-defined form, modified nucleotides (LNA and/or UNA) were inserted in its sequence. We here report an in-depth biophysical characterization of V7t1 in a Na+-rich medium, mimicking the extracellular environment in which VEGF targeting should occur, carried out combining several techniques to analyse the conformational behaviour of the aptamer and its binding to the protein. Our results demonstrate that, in the presence of high Na+ concentrations, V7t1 behaves in a very different way if subjected or not to annealing procedures, as evidenced by native gel electrophoresis, size exclusion chromatography and dynamic light scattering analysis. Indeed, not-annealed V7t1 forms both monomeric and dimeric G-quadruplexes, while the annealed oligonucleotide is a monomeric species. Remarkably, only the dimeric aptamer efficiently binds VEGF, showing higher affinity for the protein compared to the monomeric species. These findings provide new precious information for the development of improved V7t1 analogues, allowing more efficient binding to the cancer-related protein and the design of effective biosensors or theranostic devices based on VEGF targeting.
机译:先前发现G-quadrepled-形成的VEGF结合适体V7T1在K +型溶液中是高度多态性的,并且为了将其构象偏好限制为独特的明确定义的形式,修饰的核苷酸(LNA和/或UNA)是插入其顺序。我们在这里报告了v7t1在Na + -RICH培养基中的深入生物物理表征,模仿了应发生VEGF靶向的细胞外环境,结合了几种技术来分析适体的构象行为及其与蛋白质的结合。我们的研究结果表明,在高Na +浓度存在下,如果经过或不通过退火程序,V7T1的行为是非常不同的,如天然凝胶电泳,尺寸排阻色谱和动态光散射分析所证明。实际上,未退火的V7T1形成单体和二聚体G-四共混,而退火的寡核苷酸是单体物质。值得注意的是,只有二聚体适体有效结合VEGF,与单体物质相比,对蛋白质显示出更高的亲和力。这些发现为改进的V7T1类似物提供了新的珍贵信息,从而使癌症相关蛋白质更有效地结合和基于VEGF靶向的有效生物传感器或其治疗装置的设计。

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  • 来源
    《Nucleic Acids Research》 |2019年第15期|共14页
  • 作者单位

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

    Univ Naples Federico II Dept Chem Sci Via Cintia 21 I-80126 Naples Italy;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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