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Applications of high throughput technologies in modern genomics.

机译:高通量技术在现代基因组学中的应用。

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摘要

DNA microarrays and high throughput sequencing (HTS) have allowed investigators to characterize nucleic acids (DNA and RNA) across tissues, treatments, samples, and species, providing a wealth of information in efficient and cost-effective ways. This dissertation presents an application of DNA microarrays and two novel methods for analysis of HTS data.;Bacterial and fungal species that live in and on the human body are believed to play important roles in the maintenance of health and prevention of disease. To study these communities in the human vagina, we developed the VChip, a DNA microarray with probes representing 313 strains of bacteria as well as 716 human immunity genes. This array was validated using mock bacterial communities and tested using DNA and cDNA from vaginal swabs. The VChip produced results that accurately reflected the composition of the mock bacterial communities, and produced results similar to those obtained from 16S rRNA amplicon pyrosequencing.;Assembly by Reduced Complexity (ARC), is a software package that facilitates iterative, reference seeded assembly of HTS datasets. This strategy is useful for datasets that can be divided into several discreet subsets that can each be assembled independently. A set of reference or "target" sequences is used to recruit initial subsets of reads, each subset is assembled independently into contigs, these contigs are then used to recruit a new set of reads. This process is iterated, to grow assemblies until stopping conditions are met. I showed that ARC works well even with moderately divergent references, and is not plagued by reference bias, a serious limitation of mapping based strategies.;StopGap is a strategy for improving genome assemblies. Gap spanning Pacific Biosciences continuous long reads are identified and used to guide assembly of high quality Illumina or 454 reads with the ARC pipeline. Two assembly merging programs were tested for their ability to take advantage of these gap-bridging contigs. I show that this approach was able to produce more contiguous assemblies and better represent repeated sequences within the assembly. Although StopGap was used here to improve the assembly of a bacterial genome, this approach could be used in the assembly of more complex eukaryotic genomes as well.
机译:DNA微阵列和高通量测序(HTS)使研究人员能够表征组织,治疗,样品和物种之间的核酸(DNA和RNA),从而以有效和具有成本效益的方式提供大量信息。本论文介绍了DNA芯片的应用和两种分析高温超导数据的新颖方法。人体中和人体上的细菌和真菌物种被认为在维持健康和预防疾病中起着重要的作用。为了研究人类阴道中的这些群落,我们开发了VChip,这是一种DNA微阵列,具有代表313个细菌菌株以及716个人类免疫基因的探针。该阵列使用模拟细菌群落进行验证,并使用阴道拭子的DNA和cDNA进行测试。 VChip产生的结果准确反映了模拟细菌群落的组成,并且产生的结果类似于从16S rRNA扩增子焦磷酸测序获得的结果。降低复杂性(ARC)组装是一个软件包,可简化HTS的迭代,参考种子组装数据集。此策略对于可以分为几个离散子集的数据集很有用,每个子集可以独立地组装。一组参考或“靶标”序列用于募集读段的初始子集,每个子​​集独立地组装成重叠群,然后将这些重叠群用于募集新的一组读段。重复此过程,以增长装配,直到满足停止条件为止。我证明ARC即使在中等差异的参考下也能很好地工作,并且不受参考偏差的困扰,这是基于映射的策略的严重限制。; StopGap是一种用于改善基因组装配的策略。可以识别出跨越太平洋生物科学公司的连续连续读取的间隙,并用于指导高质量Illumina或ARC管线的454读取的组装。测试了两个程序集合并程序利用这些空缺重叠群的能力。我展示了这种方法能够产生更多连续的程序集,并更好地表示程序集中的重复序列。尽管此处使用StopGap来改善细菌基因组的组装,但是这种方法也可以用于更复杂的真核生物基因组的组装。

著录项

  • 作者

    Hunter, Samuel S.;

  • 作者单位

    University of Idaho.;

  • 授予单位 University of Idaho.;
  • 学科 Bioinformatics.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 109 p.
  • 总页数 109
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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