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Exact calculation of loop formation probability identifies folding motifs in RNA secondary structures

机译:环形形成概率的精确计算识别RNA二级结构中的折叠基序

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摘要

RNA secondary structure prediction is widely used to analyze RNA sequences. In an RNA partition function calculation, free energy nearest neighbor parameters are used in a dynamic programming algorithm to estimate statistical properties of the secondary structure ensemble. Previously, partition functions have largely been used to estimate the probability that a given pair of nucleotides form a base pair, the conditional stacking probability, the accessibility to binding of a continuous stretch of nucleotides, or a representative sample of RNA structures. Here it is demonstrated that an RNA partition function can also be used to calculate the exact probability of formation of hairpin loops, internal loops, bulge loops, or multibranch loops at a given position. This calculation can also be used to estimate the probability of formation of specific helices. Benchmarking on a set of RNA sequences with known secondary structures indicated that loops that were calculated to be more probable were more likely to be present in the known structure than less probable loops. Furthermore, highly probable loops are more likely to be in the known structure than the set of loops predicted in the lowest free energy structures.
机译:RNA二级结构预测广泛用于分析RNA序列。在RNA分区功能计算中,在动态编程算法中使用自由能量最近的邻接参数来估计二次结构集合的统计特性。以前,分区功能大大用于估计给定对核苷酸形成碱基对的概率,条件堆叠概率,与连续核苷酸的结合的可接近性,或RNA结构的代表性样品。在这里,证明RNA分区功能也可用于计算在给定位置处形成发夹环,内部环,凸起环或多刺圈环的精确概率。该计算还可用于估计特定螺旋形成的概率。具有已知二次结构的一组RNA序列上的基准测试表明,计算出更容易可能的循环更可能存在于已知结构中而不是较少的可能环。此外,高度可能的环比在最低自由能结构中预测的循环集中更容易处于已知结构中。

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