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首页> 外文期刊>PLoS One >Unsupervised tensor decomposition-based method to extract candidate transcription factors as histone modification bookmarks in post-mitotic transcriptional reactivation
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Unsupervised tensor decomposition-based method to extract candidate transcription factors as histone modification bookmarks in post-mitotic transcriptional reactivation

机译:无监督的张量分解的方法将候选转录因子提取为后临床转录重新激活中的组蛋白改性书签

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The histone group added to a gene sequence must be removed during mitosis to halt transcription during the DNA replication stage of the cell cycle. However, the detailed mechanism of this transcription regulation remains unclear. In particular, it is not realistic to reconstruct all appropriate histone modifications throughout the genome from scratch after mitosis. Thus, it is reasonable to assume that there might be a type of “bookmark” that retains the positions of histone modifications, which can be readily restored after mitosis. We developed a novel computational approach comprising tensor decomposition (TD)-based unsupervised feature extraction (FE) to identify transcription factors (TFs) that bind to genes associated with reactivated histone modifications as candidate histone bookmarks. To the best of our knowledge, this is the first application of TD-based unsupervised FE to the cell division context and phases pertaining to the cell cycle in general. The candidate TFs identified with this approach were functionally related to cell division, suggesting the suitability of this method and the potential of the identified TFs as bookmarks for histone modification during mitosis.
机译:在细胞循环的DNA复制阶段期间,必须在丝分裂期间除去添加到基因序列的组蛋白基团以停止转录。然而,这种转录法规的详细机制仍然不清楚。特别地,在丝分裂后重建在整个基因组中的所有适当的组蛋白修饰是不现实的。因此,可以合理地假设可能存在一种类型的“书签”,其保留组蛋白修饰的位置,这可以在有丝分裂后容易地恢复。我们开发了一种新的计算方法,包括张量分解(Td) - 基于无监督的特征提取(Fe),以鉴定与与重新激活的组蛋白修改相关的基因的转录因子(TFS)作为候选组蛋白书签。据我们所知,这是第一次将TD的无人监督FE应用于细胞分裂的上下文和与细胞周期有关的阶段。用这种方法鉴定的候选TFS与细胞分裂有关,表明该方法的适用性和所识别的TFS的潜力作为在有丝分裂过程中组蛋白修饰的书签。

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