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Induced fit or conformational selection for RNA/U1A folding

机译:RNA / U1A折叠的诱导适合或构象选择

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摘要

The hairpin II of U1 snRNA can bind U1A protein with high affinity and specificity. NMR spectra suggest that the loop region of apo-RNA is largely unstructured and undergoes a transition from unstructured to well-folded upon U1Abinding. However, the mechanism that RNA folding coupled protein binding is poorly understood. To get an insight into the mechanism, we have performed explicit-solvent molecular dynamics (MD) to study the folding kinetics of bound RNA and apo-RNA. Room-temperature MD simulations suggest that the conformation of bound RNA has significant adjustment and becomes more stable upon U1A binding. Kinetic analysis of high-temperature MD simulations shows that bound RNA and apo-RNA unfold via a two-state process, respectively. Both kinetics and free energy landscape analyses indicate that bound RNA folds in the order of RNA contracting, U1A binding, and tertiary folding. The predicted Φ-values suggest that A8, C10, A11, and G16 are key bases for bound RNA folding. Mutant Arg52Gln analysis shows that electrostatic interaction and hydrogen bonds between RNA and U1A (Arg52Gln) decrease. These results are in qualitative agreement with experiments. Furthermore, this method could be used in other studies about biomolecule folding upon receptor binding.
机译:U1 snRNA的发夹II可以高亲和力和特异性结合U1A蛋白。 NMR谱表明,载脂蛋白RNA的环区域在很大程度上是非结构化的,并且在U1A结合后经历了从非结构化到折叠良好的转变。但是,RNA折叠耦合蛋白质结合的机制了解甚少。为了深入了解该机制,我们进行了显式溶剂分子动力学(MD)研究结合RNA和载脂蛋白RNA的折叠动力学。室温MD模拟表明,结合的RNA的构象具有显着的调节,并且在U1A结合后变得更加稳定。高温MD模拟的动力学分析表明,结合的RNA和载脂蛋白RNA分别通过两种状态过程展开。动力学和自由能态分析均表明,结合的RNA按RNA收缩,U1A结合和三次折叠的顺序折叠。预测的Φ值表明A8,C10,A11和G16是结合RNA折叠的关键碱基。突变的Arg52Gln分析表明,RNA与U1A(Arg52Gln)之间的静电相互作用和氢键减少。这些结果与实验定性一致。此外,该方法可用于其他有关受体结合后生物分子折叠的研究。

著录项

  • 来源
    《RNA》 |2010年第5期|1053-1061|共9页
  • 作者单位

    College of Life Sciences and Biotechnology, Shanghai Jiaotong University, Shanghai, 200240, China;

    College of Life Sciences and Biotechnology, Shanghai Jiaotong University, Shanghai, 200240, China;

    College of Life Sciences and Biotechnology, Shanghai Jiaotong University, Shanghai, 200240, China;

    Shanghai Center for Bioinformation Technology, Shanghai, 200235, China;

    Institute of Medical Science, School of Medicine, Shanghai Jiaotong University, Shanghai, 200025, China;

    College of Life Sciences and Biotechnology, Shanghai Jiaotong University, Shanghai, 200240, China|Shanghai Center for Bioinformation Technology, Shanghai, 200235, China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    mRNA splicing complex; RNA folding; binding; transition state; Φ-values;

    机译:mRNA剪接复合体;RNA折叠;结合;过渡态;Φ值;

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