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DeepCLIP: predicting the effect of mutations on protein-RNA binding with deep learning

机译:DeepClip:预测突变对与深度学习蛋白质-RNA结合的影响

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摘要

Nucleotide variants can cause functional changes by altering protein-RNA binding in various ways that are not easy to predict. This can affect processes such as splicing, nuclear shuttling, and stability of the transcript. Therefore, correct modeling of protein-RNA binding is critical when predicting the effects of sequence variations. Many RNA-binding proteins recognize a diverse set of motifs and binding is typically also dependent on the genomic context, making this task particularly challenging. Here, we present DeepCLIP, the first method for context-aware modeling and predicting protein binding to RNA nucleic acids using exclusively sequence data as input. We show that DeepCLIP outperforms existing methods formodeling RNA-protein binding. Importantly, we demonstrate that DeepCLIP predictions correlate with the functional outcomes of nucleotide variants in independent wet lab experiments. Furthermore, we show how DeepCLIP binding profiles can be used in the design of therapeutically relevant antisense oligonucleotides, and to uncover possible position-dependent regulation in a tissue-specific manner. DeepCLIP is freely available as a stand-alone application and as a webtool at http://deepclip.compbio.sdu.dk.
机译:通过以各种方式改变蛋白质-RNA结合来改变不容易预测的蛋白质-RNA结合可以引起功能性变化。这可以影响剪接,核穿梭和转录物的稳定性等过程。因此,当预测序列变化的影响时,蛋白质-RNA结合的正确建模是关键的。许多RNA结合蛋白识别多样化的基序和结合通常也取决于基因组背景,使得这项任务特别具有挑战性。在这里,我们介绍DeepClip,使用专门的序列数据作为输入的第一种方法感知建模和预测与RNA核酸结合的蛋白质。我们表明,DeepClip优于现有方法形成RNA蛋白结合。重要的是,我们证明了深度预测与独立湿实验室实验中的核苷酸变体的功能结果相关。此外,我们展示了深度结合型材如何在治疗相关的反义寡核苷酸设计中使用,并以组织特异性方式揭示可能的位置依赖性调节。 DeepClip作为独立应用程序自由地提供,并在http://deepclip.compbio.sdu.dk上作为webtool。

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