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A Study on the Effect of an Aptamer with an Embedded Phosphate-Methylated Nucleotide on the Binding of a Target Molecule Using Molecular Simulation

机译:分子模拟研究包埋有磷酸化甲基化核苷酸的适体对目标分子结合的影响

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Uncharged DNA analogues are frequently used to be synthesized as oligomers or combined with nucleic acids to synthesize chimeric oligomers. Owing to their special structures and the uncharged property, the oligomers with DNA analogues are useful in many applications, like fluorescence in situ hybridization (FISH), biosensors, gene chips, etc. In this study, we try to investigate the effect of an uncharged phosphate-methylated nucleotide embedded on the aptamer sequence with high affinity to IgG1 by using the computational approach. The simulation results predict that the embedded phosphate-methylated nucleotide can cause the changes in the tertiary structure and spatial charge distribution of aptamer and further influence the binding between the aptamer and IgG1. From this study, we obtain an aptamer modified with the phosphate-methylated nucleotide, named as Apt8#n10, can have an improved binding affinity to IgGl. According to these consequences, the embedded phosphate-methylated nucleotide can play a role in the aptamer sequence for tuning the binding affinity of the aptamer to its target molecule.
机译:不带电荷的DNA类似物通常被用作寡聚物或与核酸结合以合成嵌合寡聚物。由于其特殊的结构和不带电的特性,带有DNA类似物的寡聚体可用于许多应用,例如荧光原位杂交(FISH),生物传感器,基因芯片等。在本研究中,我们尝试研究不带电的效应。通过使用计算方法,将磷酸化甲基化核苷酸嵌入到与IgG1高度亲和的适体序列上。模拟结果预测,嵌入的磷酸甲基化核苷酸可引起适体的三级结构和空间电荷分布的变化,并进一步影响适体与IgG1之间的结合。从该研究中,我们获得了用磷酸甲基化核苷酸修饰的适体,称为Apt8#n10,可以具有对IgG1的改善的结合亲和力。根据这些结果,嵌入的磷酸甲基化核苷酸可以在适体序列中起作用,以调节适体与其靶分子的结合亲和力。

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