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The equilibrium partition function and base pair binding probabilities for RNA secondary structure

机译:用于RNA二级结构的平衡分区功能和基对结合概率

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摘要

A novel application of dynamic programming to the folding problem for RNA enables one to calculate the full equilibrium partition function for secondary structure and the probabilities of various substructures. In particular, both the partition function and the probabilities of all base pairs are computed by a recursive scheme of polynomial order N3 in the sequence length N. The temperature dependence of the partition function gives information about melting behavior for the secondary structure. The pair binding probabilities, the computation of which depends on the partition function, are visually summarized in a "box matrix" display and this provides a useful tool for examining the full ensemble of probable alternative equilibrium structures. The calculation of this ensemble representation allows a proper application and assessment of the predictive power of the secondary structure method, and yields important information on alternatives and intermediates in addition to local information about base pair opening and slippage. The results are illustrated for representative tRNA, 5S RNA, and self-replicating and self-splicing RNA molecules, and allow a direct comparison with enzymatic structure probes. The effect of changes in the thermodynamic parameters on the equilibrium ensemble provides a further sensitivity check to the predictions.
机译:动态编程的一个新的应用到折叠问题为RNA使得能够计算用于二级结构和完全平衡分区功能的各种子结构的概率。特别地,这两个分函数和所有碱基对的概率由多项式阶N3在序列长度N的分函数对温度的依赖性提供了有关的二级结构熔融行为的信息的递推方案计算的。所述一对结合概率,计算其依赖于分函数,在视觉上总结在“盒子矩阵”显示器,这提供用于检查可能的替代平衡结构的完整集合的有用工具。这个集合表示的计算允许的二级结构的方法的预测能力的适当应用和评估,并产生上除了大约碱基对开口和滑移的局部信息的替代品和中间体的重要信息。结果被示出为代表的tRNA,5S RNA和自我复制和自剪接的RNA分子,并允许具有酶活结构的探针的直接比较。在对平衡合奏的热力学参数变化的影响提供了进一步的灵敏度检查到的预测。

著录项

  • 作者

    J. S. McCaskill;

  • 作者单位
  • 年度 1990
  • 总页数
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类

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