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Structural features based genome-wide characterization and prediction of nucleosome organization

机译:基于结构特征的全基因组表征和核小体组织的预测

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Background Nucleosome distribution along chromatin dictates genomic DNA accessibility and thus profoundly influences gene expression. However, the underlying mechanism of nucleosome formation remains elusive. Here, taking a structural perspective, we systematically explored nucleosome formation potential of genomic sequences and the effect on chromatin organization and gene expression in S. cerevisiae. Results We analyzed twelve structural features related to flexibility, curvature and energy of DNA sequences. The results showed that some structural features such as DNA denaturation, DNA-bending stiffness, Stacking energy, Z-DNA, Propeller twist and free energy, were highly correlated with in vitro and in vivo nucleosome occupancy. Specifically, they can be classified into two classes, one positively and the other negatively correlated with nucleosome occupancy. These two kinds of structural features facilitated nucleosome binding in centromere regions and repressed nucleosome formation in the promoter regions of protein-coding genes to mediate transcriptional regulation. Based on these analyses, we integrated all twelve structural features in a model to predict more accurately nucleosome occupancy in vivo than the existing methods that mainly depend on sequence compositional features. Furthermore, we developed a novel approach, named DLaNe, that located nucleosomes by detecting peaks of structural profiles, and built a meta predictor to integrate information from different structural features. As a comparison, we also constructed a hidden Markov model (HMM) to locate nucleosomes based on the profiles of these structural features. The result showed that the meta DLaNe and HMM-based method performed better than the existing methods, demonstrating the power of these structural features in predicting nucleosome positions. Conclusions Our analysis revealed that DNA structures significantly contribute to nucleosome organization and influence chromatin structure and gene expression regulation. The results indicated that our proposed methods are effective in predicting nucleosome occupancy and positions and that these structural features are highly predictive of nucleosome organization. The implementation of our DLaNe method based on structural features is available online.
机译:背景沿着染色质的核小体分布决定了基因组DNA的可及性,因此深刻影响基因表达。但是,核小体形成的潜在机制仍然难以捉摸。在这里,从结构的角度,我们系统地探索了基因组序列的核小体形成潜力以及对酿酒酵母中染色质组织和基因表达的影响。结果我们分析了与DNA序列的柔韧性,曲率和能量有关的十二种结构特征。结果表明,DNA变性,DNA弯曲刚度,堆积能,Z-DNA,螺旋桨扭曲和自由能等一些结构特征与体内和体外核小体的占有率高度相关。具体来说,它们可分为两类,一类与核小体的占有呈正相关。这两种结构特征促进了着丝粒区域中核小体的结合并抑制了蛋白质编码基因启动子区域中核小体的形成,以介导转录调控。基于这些分析,我们将所有十二种结构特征整合到模型中,以比主要依赖于序列组成特征的现有方法更准确地预测体内核小体的占有率。此外,我们开发了一种名为DLaNe的新方法,该方法通过检测结构轮廓的峰来定位核小体,并建立了元预测变量以整合来自不同结构特征的信息。作为比较,我们还构建了一个隐马尔可夫模型(HMM),以基于这些结构特征的概况定位核小体。结果表明,基于DLaNe和HMM的元方法比现有方法表现更好,证明了这些结构特征在预测核小体位置中的作用。结论我们的分析表明,DNA结构显着促进了核小体的组织并影响了染色质的结构和基因表达的调控。结果表明,我们提出的方法可以有效地预测核小体的占有率和位置,并且这些结构特征可以高度预测核小体的组织。在线提供基于结构特征的DLaNe方法的实现。

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