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Conformation and Stability of Intramolecular Telomeric G-Quadruplexes: Sequence Effects in the Loops

机译:分子内端粒G四联体的构象和稳定性:循环中的序列效应。

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摘要

Telomeres are guanine-rich sequences that protect the ends of chromosomes. These regions can fold into G-quadruplex structures and their stabilization by G-quadruplex ligands has been employed as an anticancer strategy. Genetic analysis in human telomeres revealed extensive allelic variation restricted to loop bases, indicating that the variant telomeric sequences maintain the ability to fold into G-quadruplex. To assess the effect of mutations in loop bases on G-quadruplex folding and stability, we performed a comprehensive analysis of mutant telomeric sequences by spectroscopic techniques, molecular dynamics simulations and gel electrophoresis. We found that when the first position in the loop was mutated from T to C or A the resulting structure adopted a less stable antiparallel topology; when the second position was mutated to C or A, lower thermal stability and no evident conformational change were observed; in contrast, substitution of the third position from A to C induced a more stable and original hybrid conformation, while mutation to T did not significantly affect G-quadruplex topology and stability. Our results indicate that allelic variations generate G-quadruplex telomeric structures with variable conformation and stability. This aspect needs to be taken into account when designing new potential anticancer molecules.
机译:端粒是富含鸟嘌呤的序列,可保护染色体末端。这些区域可以折叠成G-四链体结构,它们通过G-四链体配体的稳定作用已被用作抗癌策略。人类端粒的遗传分析显示,广泛的等位基因变异仅限于环碱基,这表明变异的端粒序列保持了折叠成G-四链体的能力。为了评估环突变对G-四链体折叠和稳定性的影响,我们通过光谱技术,分子动力学模拟和凝胶电泳对突变型端粒序列进行了全面分析。我们发现,当循环中的第一个位置从T突变为C或A时,所得结构采用了较不稳定的反平行拓扑。当第二个位置突变为C或A时,热稳定性较低,没有观察到明显的构象变化。相反,从A到C的第三个位置取代引起了更稳定和原始的杂交构象,而向T的突变并没有显着影响G-四链体的拓扑和稳定性。我们的结果表明,等位基因变异产生具有可变构象和稳定性的G-四链体端粒结构。在设计新的潜在抗癌分子时需要考虑这一方面。

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