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A Dynamic Structural Model of Expanded RNA CAG Repeats: A Refined X-ray Structure and Computational Investigations Using Molecular Dynamics and Umbrella Sampling Simulations

机译:扩展的RNA CAG重复序列的动态结构模型:精细的X射线结构和使用分子动力学和伞采样模拟的计算研究

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摘要

One class of functionally important RNA is repeating transcripts that cause disease through various mechanisms. For example, expanded CAG repeats can cause Huntington's and other disease through translation of toxic proteins. Herein, a crystal structure of r[5'UUGGGC- (CAG)_3GUCC]_2, a model of CAG expanded transcripts, refined to 1.65 A resolution is disclosed that shows both anti- anti and syn-anti orientations for 1 × 1 nucleotide AA internal loops. Molecular dynamics (MD) simulations using AMBER force field in explicit solvent were run for over 500 ns on the model systems r(5'GCGCAGCGC)_2 (MS1) and r(5'CCGCAGCGG)_2 (MS2). In these MD simulations, both anti-anti and syn-anti AA base pairs appear to be stable. While anti-anti AA base pairs were dynamic and sampled multiple anti-anti conformations, no syn-anti ↔ anti-anti transformations were observed. Umbrella sampling simulations were run on MS2, and a 2D free energy surface was created to extract transformation pathways. In addition, an explicit solvent MD simulation over 800 ns was run on r[5'GGGC(CAG)_3GUCC]_2, which closely represents the refined crystal structure. One of the terminal AA base pairs (syn-anti conformation), transformed to anti-anti conformation. The pathway followed in this transformation was the one predicted by umbrella sampling simulations. Further analysis showed a binding pocket near AA base pairs in syn-anti conformations. Computational results combined with the refined crystal structure show that global minimum conformation of 1 × 1 nucleotide AA internal loops in r(CAG) repeats is anti-anti but can adopt syn-anti depending on the environment. These results are important to understand RNA dynamic-function relationships and to develop small molecules that target RNA dynamic ensembles.
机译:一类功能重要的RNA是通过多种机制引起疾病的重复转录本。例如,扩展的CAG重复序列可以通过毒性蛋白的翻译而导致亨廷顿舞蹈病和其他疾病。在此,揭示了r [5'UUGGGC-(CAG)_3GUCC] _2的晶体结构,其是CAG扩展的转录本模型,其精炼为1.65 A的分辨率,显示了1×1核苷酸AA的抗-和顺-抗取向内部循环。在模型系统r(5'GCGCAGCGC)_2(MS1)和r(5'CCGCAGCGG)_2(MS2)上,在明确溶剂中使用AMBER力场进行的分子动力学(MD)模拟运行了500 ns以上。在这些MD模拟中,抗AA和抗AA碱基对似乎都是稳定的。尽管抗-抗AA碱基对是动态的,并采样了多个抗-抗构象,但未观察到同抗-抗-抗-转化。在MS2上进行了伞采样模拟,并创建了2D自由能表面以提取转化途径。此外,在r [5'GGGC(CAG)_3GUCC] _2上进行了800 ns的显式溶剂MD模拟,该模拟紧密地代表了精炼的晶体结构。末端AA碱基对之一(syn-反构象),被转化为反-反构象。这种转换所遵循的途径是伞状抽样模拟所预测的途径。进一步的分析显示,在反-构象的AA碱基对附近有一个结合袋。计算结果与精确的晶体结构相结合表明,r(CAG)重复序列中1×1个核苷酸AA内部环的整体最小构象是抗-抗性,但可以根据环境采用同-抗性。这些结果对于理解RNA动态功能关系以及开发靶向RNA动态集合体的小分子非常重要。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2013年第9期|3528-3538|共11页
  • 作者单位

    Department of Chemistry and International Institute for Nanotechnology, Northwestern University, Evanston, Illinois 60208, United States;

    Translational Research Institute The Scripps Research Institute, Jupiter, Florida 33458, United States;

    Department of Chemistry, The Scripps Research Institute, Jupiter, Florida 33458, United States;

    Department of Chemistry and International Institute for Nanotechnology, Northwestern University, Evanston, Illinois 60208, United States;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
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  • 入库时间 2022-08-18 03:12:29

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