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Simultaneous Folding of Alternative RNA Structures with Mutual Constraints: An Application to Next-Generation Sequencing-based RNA Structure Probing

机译:具有相互约束的交替RNA结构的同时折叠:在基于下一代测序的RNA结构探测中的应用

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摘要

>Recent advances in next-generation sequencing technology have significantly promoted high-throughput experimental probing of RNA secondary structures. The resulting enzymatic or chemical probing information is then incorporated into a minimum free energy folding algorithm to predict more accurate RNA secondary structures. A drawback of this approach is that it does not consider the presence of alternative RNA structures. In addition, the alternative RNA structures may contaminate experimental probing information of each other and direct the minimum free-energy folding to a wrong direction. In this article, we present a combinatorial solution for this problem, where two alternative structures can be folded simultaneously given the experimental probing information regarding the mixture of these two alternative structures. We have tested our algorithm with artificially generated mixture probing data on adenine riboswitch and thiamine pyrophosphate (TPP) riboswitch. The experimental results show that our algorithm can successfully recover the ON and OFF structures of these riboswitches.
机译:>下一代测序技术的最新进展显着促进了RNA二级结构的高通量实验探测。然后将所得的酶或化学探测信息合并到最小自由能折叠算法中,以预测更准确的RNA二级结构。该方法的缺点是它不考虑替代RNA结构的存在。此外,其他RNA结构可能会污染彼此的实验探测信息,并将最小的自由能折叠指向错误的方向。在本文中,我们提供了针对此问题的组合解决方案,其中,在给出有关这两种替代结构混合的实验探测信息的情况下,可以同时折叠两种替代结构。我们已经使用人工生成的关于腺嘌呤核糖开关和硫胺焦磷酸盐(TPP)核糖开关的混合物探测数据测试了我们的算法。实验结果表明,该算法能够成功恢复这些核糖开关的通断结构。

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