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Comparative evaluation of the extended and minimal hammerheads suggests a shared dynamic pathway.

机译:扩展锤头和最小锤头的比较评估表明了共享的动态路径。

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摘要

The discovery of RNA catalysis in the early 1980's marked a shift in a long standing paradigm in enzymology; no longer were proteins considered the sole catalytic cellular agents, but RNA was now included in that category. Following this initial discovery, numerous other catalytic RNAs, ribozymes, were soon identified. Even twenty years later new ribozymes continue to be identified or generated. Clearly, the field of catalytic RNA study continues to grow and broaden in scope and focus. In order to obtain a better overall understanding of RNA catalytic function it is necessary to examine specific ribozymes.;The hammerhead is a well studied ribozyme that causes a site specific transesterification in the RNA backbone leading to a 2', 3'-cyclic phosphate and 5'-hydroxyl termini. Until four years ago minimal hammerheads were primarily used to investigate the requirements of the reaction. However, in 2003 the importance of added sequence elements, present in the natural sequences where the hammerhead motif was originally identified, as able to enhance catalysis was appreciated. This discovery again caused another shift in focus of study, this time from "minimal" hammerheads towards naturally derived "extended" hammerheads.;The work included in this thesis focuses on understanding the enhancement of the extended hammerhead on catalysis and comparing its enhancement to that which is observed for the minimal hammerhead. For this purpose it is necessary to establish the experimental validity of using hybrid hammerheads, hammerheads containing both minimal and extended sequences.;This system, once validated, is then used to test the metal ion binding properties of an extended hammerhead with phosphorothioate substitutions. Kapp [Cd2+] values are obtained for extended hammerheads with a phosphorothioate substitution at either P1.1 or P.9. The same experiments are performed on a mutant version of the extended hammerhead as well as on a minimal hammerhead. The results show that while the extended hammerhead binds cadmium ions tighter than the minimal hammerhead, the trends in K app [Cd2+] values for the different phosphorothioate substitutions compared to the all oxygen control in both backgrounds are very similar.;Furthermore, a recent crystal structure of an extended hammerhead showed a novel core interaction between residues G8 and C3. This interaction is explored in both the extended and minimal background by introducing single point mutations followed by the compensatory double mutation. Additionally, the possible synergistic relationship between the identity of the cleavage site nucleotide and the different N8-N3 nucleotides is explored. The similar behavior in response to this set of mutations for the minimal and extended hammerhead suggests that the two share a dynamic pathway. Therefore, in the final chapter, the large existing body of biochemical data collected in the minimal hammerhead is evaluated in the background of the extended hammerhead structure where it maybe better understood.
机译:在1980年代初期,RNA催化的发现标志着酶学长期存在的范例的转变。不再将蛋白质视为唯一的催化细胞因子,但现在将RNA包括在该类别中。在此最初发现之后,很快又鉴定出许多其他催化性RNA,即核酶。甚至二十年后,新的核酶仍继续被发现或产生。显然,催化RNA研究领域继续发展并扩大了范围和重点。为了更好地全面了解RNA催化功能,有必要检查特定的核酶。锤头是一种经过充分研究的核酶,其在RNA主链中引起位点特异性酯交换反应,导致2',3'-环磷酸酯和5'-羟基末端。直到四年前,最小的锤头才主要用于研究反应的要求。然而,在2003年,人们认识到了添加序列元素的重要性,这种元素存在于最初鉴定锤头基序的自然序列中,能够增强催化作用。这一发现再次引起了研究重点的转变,这次是从“最小”锤头向自然衍生的“扩展”锤头。;本论文中的工作着重于了解扩展的锤头在催化上的增强作用,并将其增强与催化作用进行比较。观察到最小的锤头。为此目的,有必要建立使用混合锤头的实验有效性,该锤头同时包含最小序列和扩展序列。该系统一经验证,便被用于测试硫代磷酸酯取代的扩展锤头的金属离子结合性能。对于在P1.1或P.9处有硫代磷酸酯取代的扩展锤头,将获得Kapp [Cd2 +]值。在扩展版本的锤头和最小锤头上进行相同的实验。结果表明,尽管扩展的锤头比最小锤头更紧密地结合了镉离子,但在两种背景下,与所有氧气控制相比,不同硫代磷酸酯取代的K app [Cd2 +]值趋势非常相似。扩展的锤头结构显示残基G8和C3之间有新的核心相互作用。通过引入单点突变,然后引入补偿性双突变,可以在扩展背景和最小背景下探索这种相互作用。另外,探索了切割位点核苷酸的身份和不同的N8-N3核苷酸之间的可能的协同关系。针对最小和扩展锤头的这组突变,类似的行为表明两者共享一条动态途径。因此,在最后一章中,在扩展的锤头结构背景下评估了在最小的锤头中收集的大量现有生化数据,可能会更好地理解该结构。

著录项

  • 作者

    Nelson, Jennifer A.;

  • 作者单位

    University of Colorado at Boulder.;

  • 授予单位 University of Colorado at Boulder.;
  • 学科 Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2007
  • 页码 152 p.
  • 总页数 152
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学 ;
  • 关键词

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