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A computational method for studying the relation between alternative splicing and DNA methylation

机译:研究可变剪接与DNA甲基化之间关系的一种计算方法

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摘要

Alternative splicing is an important mechanism in eukaryotes that expands the transcriptome and proteome significantly. It plays an important role in a number of biological processes. Understanding its regulation is hence an important challenge. Recently, increasing evidence has been collected that supports an involvement of intragenic DNA methylation in the regulation of alternative splicing. The exact mechanisms of regulation, however, are largely unknown, and speculated to be complex: different methylation profiles might exist, each of which could be associated with a different regulation mechanism. We present a computational technique that is able to determine such stable methylation patterns and allows to correlate these patterns with inclusion propensity of exons. Pattern detection is based on dynamic time warping (DTW) of methylation profiles, a sophisticated similarity measure for signals that can be non-trivially transformed. We design a flexible self-organizing map approach to pattern grouping. Exemplary application on available data sets indicates that stable patterns which correlate non-trivially with exon inclusion do indeed exist. To improve the reliability of these predictions, further studies on larger data sets will be required. We have thus taken great care that our software runs efficiently on modern hardware, so that it can support future studies on large-scale data sets.
机译:选择性剪接是真核生物显着扩展转录组和蛋白质组的重要机制。它在许多生物学过程中起着重要作用。因此,了解其法规是一项重要的挑战。最近,越来越多的证据支持基因内DNA甲基化参与选择性剪接的调控。然而,调控的确切机制在很大程度上尚不清楚,并且推测是复杂的:可能存在不同的甲基化谱,每种甲基化谱可能与不同的调控机制相关。我们提出了一种计算技术,能够确定这种稳定的甲基化模式,并允许将这些模式与外显子的包含倾向相关联。模式检测基于甲基化配置文件的动态时间规整(DTW),这是一种可以被简单转换的信号的复杂相似性度量。我们设计了一种灵活的自组织地图方法来进行模式分组。在可用数据集上的示例性应用表明确实存在确实存在与不重要的外显子包涵相关的稳定模式。为了提高这些预测的可靠性,将需要对更大的数据集进行进一步的研究。因此,我们非常注意我们的软件可以在现代硬件上高效运行,从而可以支持将来对大规模数据集的研究。

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