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Characterization of transcript isoform variations in human and chimpanzee.

机译:人类和黑猩猩转录本亚型变异的表征。

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摘要

Transcript expression and pre-mRNA processing are emerging as important mechanisms that increase the complexity of eukaryotic transcriptomes. These processes allow a genomic locus to produce a number of mRNAs and proteins with distinct properties that affect function, stability, and sub-cellular localization by controlling the rate of transcript expression, by varying the initiation or termination of transcription and by modulating the inclusion of exons (alternative splicing) in mature mRNAs. Thus, it is crucial to determine the extent of these types of variations to better understand their importance in creating organism diversity. The studies described in this thesis provide the first genome-wide estimations of how single nucleotide polymorphisms (SNPs) affect the regulation of transcript expression and pre-mRNA processing in a human population as well as between humans and chimpanzees using a microarray-based approach. We first demonstrated that transcript expression changes at the isoform level are common between two unrelated individuals and that these changes are heritable and therefore have an underlying genetic component. We then investigated what proportion was under genetic control in a normal human population by conducting a genome-wide association analysis between single nucleotide polymorphisms and transcript isoform variants. We found that 50-55% of transcript expression variation is isoform based. We also extended our comparison of human transcript isoform variation to chimpanzee. We showed that genetic substitutions in regulatory sequences are responsible for some of the isoform variations observed between these two closely related species. We ascertained that in our study these isoform variations are responsible for certain phenotypic differences mostly related to immune responses. These results constitute an important change in the way genetic variations are viewed in humans and chimpanzees and they highlight the need for broader investigation into these types of variation and how they affect gene expression. In the last two chapters of this thesis we also provide solutions for some of the methodological and analysis issues we encountered because they could be of a great benefit to scientist conducting experiments with the Exon Array.
机译:转录物表达和mRNA的前处理正在成为增加真核转录组复杂性的重要机制。这些过程允许基因组基因座通过控制转录物表达的速率,改变转录的起始或终止以及通过调节转录因子的包含来产生具有影响功能,稳定性和亚细胞定位的不同特性的许多mRNA和蛋白质。成熟mRNA中的外显子(选择性剪接)。因此,至关重要的是确定这些类型的变异的程度,以更好地了解它们在创造生物多样性中的重要性。本论文中描述的研究提供了第一个全基因组范围的估计,即使用基于微阵列的方法,单核苷酸多态性(SNP)如何影响人类以及人类与黑猩猩之间的转录表达和前mRNA加工的调控。我们首先证明,在两个无关的个体之间,同工型水平上的转录表达变化是常见的,并且这些变化是可遗传的,因此具有潜在的遗传成分。然后,我们通过在单核苷酸多态性和转录亚型变异体之间进行全基因组关联分析,调查了正常人群中遗传控制下的比例。我们发现转录物表达变化的50-55%是基于亚型的。我们还扩大了人类转录本同工型变异到黑猩猩的比较。我们表明,在调控序列中的遗传取代是这两个密切相关物种之间观察到的某些同工型变异的原因。我们确定在我们的研究中,这些同工型变异是造成某些主要与免疫反应有关的表型差异的原因。这些结果构成了人类和黑猩猩观察遗传变异方式的重要变化,并且它们强调需要对这些变异类型及其如何影响基因表达进行更广泛的研究。在本文的后两章中,我们还为遇到的一些方法和分析问题提供了解决方案,因为它们可能对科学家进行Exon Array实验带来极大的好处。

著录项

  • 作者

    Benovoy, David.;

  • 作者单位

    McGill University (Canada).;

  • 授予单位 McGill University (Canada).;
  • 学科 Biology Genetics.;Biology Bioinformatics.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 203 p.
  • 总页数 203
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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