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Genome-wide Analysis of Chromatin Structure across Diverse Human Cell Types.

机译:跨人类细胞类型的染色质结构的全基因组分析。

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摘要

Chromatin structure plays an important role in gene regulation, especially in differentiating the diverse cell types in humans. In this dissertation, we analyze the nucleosome positioning and open chromatin profiles genome-wide and investigate the relationship with transcription initiation, the activity of regulatory elements, and expression levels. We mainly focus on the results of DNase-seq experiments, but also employ annotations from MNase-seq, FAIRE-seq, ChIP-seq, CAGE, and RNA microarrays. Our methods are based on computational approaches including managing large data sets, statistical analysis, and machine learning. We find that different transcription initiation patterns lead to distinct chromatin structures, suggesting diverse regulatory strategies. Moreover, we present a tool for comparing genome-wide annotation tracks and evaluate DNase-seq against a unique assay for detecting open chromatin. We also demonstrate how DNase-seq can be used to successfully predict rotationally stable nucleosomes that are conserved across cell types. We conclude that DNase-seq can be used to study genome-wide chromatin structure in an effort to better understand how it regulates gene expression.
机译:染色质结构在基因调节中起着重要作用,尤其是在区分人类的多种细胞类型中。在本文中,我们分析了核小体在全基因组中的定位和染色质概况,并研究了与转录起始,调节元件活性和表达水平的关系。我们主要关注DNase-seq实验的结果,但也使用MNase-seq,FAIRE-seq,ChIP-seq,CAGE和RNA微阵列的注释。我们的方法基于包括管理大型数据集,统计分析和机器学习在内的计算方法。我们发现不同的转录起始模式导致不同的染色质结构,表明不同的调控策略。此外,我们提出了一种工具,用于比较全基因组注释轨道并针对检测开放染色质的独特测定法评估DNase-seq。我们还演示了如何将DNase-seq用于成功预测跨细胞类型保守的旋转稳定核小体。我们得出结论,DNase-seq可用于研究全基因组染色质结构,以更好地了解其如何调节基因表达。

著录项

  • 作者

    Winter, Deborah Rachelle.;

  • 作者单位

    Duke University.;

  • 授予单位 Duke University.;
  • 学科 Biology Molecular.;Biology Bioinformatics.;Biology Cell.
  • 学位 Ph.D.
  • 年度 2013
  • 页码 211 p.
  • 总页数 211
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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