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Validation of model-scale predictions of tall building performance using full-scale measurements.

机译:使用全尺寸测量值验证高层建筑性能的模型尺寸预测。

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摘要

The expansion of gene-specific trinucleotide repeats is responsible for a growing list of human disorders, including myotonic dystrophy type 1 (DM1). Repeat instability for most of these disorders, including DM1, is characterized by complex patterns of inherited and ongoing tissue-specific instability and pathogenesis. While the mechanistic basis behind the unique locus-specific instability of trinucleotide repeats is currently unknown, DNA metabolic processes are likely to play a role. My thesis involves investigating the contribution of DNA replication to the trinucleotide instability of myotonic dystrophy type 1.;To further my study of DNA replication in DM1 repeat instability, I have mapped the origin of replication adjacent to the DM1 locus in human patient cells and the tissues of DM1 transgenic mice actively undergoing repeat instability. The position of the replication origins adjacent to the repeat tract at the DM1 locus places several known cis-elements, including CTCF binding sites, in a position to alter replication as predicted by the fork-shift model. My analysis of the CTCF sites showed them capable of altering replication and repeat instability at the DM1 locus. Taken together these results suggest that the placement of replication origins, repeat tracts and cis-elements, may mark trinucleotide repeat tracts, such as the DM1, for locus-, tissue- and development-specific replication-associated repeat instability.;Herein I have designed an in vivo primate model system, based on the SV40 replication system, to assess the contribution of DNA replication to DM1 repeat instability. This system allows the assessment, under controlled conditions, and manipulation of variables that may affect replication-associated repeat instability, under a primate cellular system. Using the SV40 model system, I not only confirmed previous observations that repeat length and replication direction affect repeat instability, but also for the first time determined that the location of the replication origin relative to the repeat tract plays an important role in repeat instability. This novel observation allowed for the development of a fork-shift model of repeat instability, in which cis-elements adjacent to the repeat tract affect replication, in turn altering the propensity for repeat instability.
机译:基因特异性三核苷酸重复序列的扩增导致越来越多的人类疾病,包括1型强直性营养不良(DM1)。对于大多数此类疾病(包括DM1),其重复不稳定性的特征是继承和进行中的组织特异性不稳定性和发病机制复杂。尽管目前尚不清楚三核苷酸重复序列独特的基因座不稳定性背后的机制基础,但DNA代谢过程可能发挥了作用。我的论文涉及调查DNA复制对1型肌强直性营养不良三核苷酸不稳定性的贡献;为了进一步研究DM1重复不稳定性中的DNA复制,我绘制了人类患者细胞中DM1基因座附近的复制起点。积极经历重复不稳定的DM1转基因小鼠的组织。复制起点在DM1基因座上与重复序列相邻的位置将几个已知的顺式元素(包括CTCF结合位点)置于改变叉叉模型预测的复制的位置。我对CTCF位点的分析表明,它们能够改变复制并在DM1位点重复不稳定。综上所述,这些结果表明复制起点,重复序列和顺式元件的位置可能标志着三核苷酸重复序列,例如DM1,与基因座,组织和发育特异性复制相关的重复不稳定性有关。设计了一种基于SV40复制系统的体内灵长类动物模型系统,以评估DNA复制对DM1重复序列不稳定性的贡献。该系统允许在灵长类细胞系统中在受控条件下评估和操纵可能影响复制相关重复不稳定性的变量。使用SV40模型系统,我不仅确认了先前的观察,即重复长度和复制方向会影响重复不稳定性,而且还首次确定复制起点相对于重复道的位置在重复不稳定性中起重要作用。这一新颖的观察结果允许发展出重复不稳定性的叉移模型,其中邻近重复道的顺式元素影响复制,从而改变了重复不稳定性的倾向。

著录项

  • 作者

    Kilpatrick, John.;

  • 作者单位

    The University of Western Ontario (Canada).;

  • 授予单位 The University of Western Ontario (Canada).;
  • 学科 Engineering Architectural.;Engineering Civil.
  • 学位 Ph.D.
  • 年度 2007
  • 页码 371 p.
  • 总页数 371
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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