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Structure-Function Analysis of the Conserved Histone Chaperone Spt6.

机译:保守组蛋白伴侣蛋白Spt6的结构-功能分析。

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摘要

Chromatin structure is crucial to regulate access to the genome for processes such as transcription, recombination, DNA repair, and DNA replication. Spt6, a key factor involved in regulating chromatin structure, is conserved throughout eukaryotes. Spt6 has been shown to function in many aspects of gene expression, including nucleosome assembly, transcription initiation and elongation, and mRNA processing and export. In addition, Spt6 has several conserved domains; however, little is known about their functions. I have performed a structure-function analysis of Spt6 using three separate approaches. First, I employed a random insertion mutagenesis that has identified sixty-seven mutants. While these mutants did not provide information regarding known domains, some have phenotypes that may prove useful for future study. Second, in a collaborative project with the Romier lab, I studied the functional roles of the Spt6 SH2 domains. I have shown that deletion of the region of SPT6 encoding the SH2 domains causes severe mutant phenotypes without affecting Spt6 protein levels, demonstrating the importance of the SH2 domains of Spt6. Third, in an additional collaboration with the Romier lab, I showed that mutations that alter the region of Spt6 that interacts with the conserved transcription factor Spn1 impair Spt6 functions in vivo. Overall, this multi-pronged structure-function analysis of Spt6 has provided new insights into the tandem SH2 domains of Spt6, the Spt6-Spn1 interaction, and the uses and limitations of insertion mutagenesis.;In addition, I have attempted to explore a possible role for Spt6 in transcription-associated mutagenesis. After employing several types of in vivo assays, I conclude that a possible role for Spt6 in transcription-associated mutagenesis is uncertain, as the results (with respect to a role for Spt6) reproducibly vary depending on the assay used. Thus, understanding this aspect of Spt6 biology awaits better assays and understanding of transcription-associated mutagenesis. Overall, the work in this dissertation will serve to further elucidate the mechanisms of Spt6 in chromatin regulation, transcription, and DNA damage repair.
机译:染色质结构对于调节转录,重组,DNA修复和DNA复制等过程对基因组的访问至关重要。 Spt6是参与调节染色质结构的关键因素,在整个真核生物中均被保守。已经显示Spt6在基因表达的许多方面起作用,包括核小体装配,转录起始和延伸以及mRNA加工和输出。另外,Spt6具有几个保守域。但是,对其功能知之甚少。我已经使用三种单独的方法对Spt6进行了结构功能分析。首先,我采用了随机插入诱变技术,已鉴定出67个突变体。尽管这些突变体没有提供有关已知域的信息,但有些具有可能被证明对未来研究有用的表型。其次,在与Romier实验室的合作项目中,我研究了Spt6 SH2域的功能角色。我已经表明,删除编码SH2域的SPT6区域会导致严重的突变表型,而不影响Spt6蛋白水平,这证明了Spt6 SH2域的重要性。第三,在与Romier实验室的另一项合作中,我表明,改变与保守转录因子Spn1相互作用的Spt6区域的突变会破坏体内的Spt6功能。总的来说,对Spt6的这种多管齐下的结构功能分析为Spt6的串联SH2域,Spt6-Spn1相互作用以及插入诱变的用途和局限性提供了新的见解。此外,我试图探索一种可能的方法。 Spt6在转录相关诱变中的作用。在采用了几种类型的体内分析后,我得出结论:Spt6在转录相关诱变中的可能作用尚不确定,因为结果(就Spt6的作用而言)可重复地根据所使用的分析而变化。因此,了解Spt6生物学的这一方面等待更好的分析方法和对转录相关诱变的了解。总体而言,本论文的工作将有助于进一步阐明Spt6在染色质调节,转录和DNA损伤修复中的机制。

著录项

  • 作者

    Loeliger, Erin Michelle.;

  • 作者单位

    Harvard University.;

  • 授予单位 Harvard University.;
  • 学科 Biology Genetics.;Biology General.;Biology Molecular.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 208 p.
  • 总页数 208
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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