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Genomic analysis of regulatory mechanisms involved in secondary metabolite production.

机译:涉及次级代谢产物生产的调控机制的基因组分析。

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摘要

Many secondary metabolites have beneficial uses for humans. In addition to their use as antibacterial and antifungal agents, secondary metabolites have been used as immunosuppressants, anti-tumor agents, and antiparasitics. Most of the secondary metabolites known today are produced by filamentous fungi or by members of the Streptomyces genus. Production of secondary metabolites by microorganisms involves a complex, dynamic system, with interconnected elements acting at different levels.;Diverse tools were used in this work to explore regulation of secondary metabolite production, mostly in Streptomyces. The tools have a common characteristic: they either generate large amounts of data, or require large amounts of data.;Regulation of secondary metabolite production in Streptomyces coelicolor was analyzed at the genome level, by using network modules inferred from a large transcriptome dataset. The upstream sequence of the elements in the network modules was searched for the presence of consensus sequences, and these results combined with information on known interactions, binding sites, and functional relatedness. The combination of this information resulted in a set of twenty networks that have a high likelihood of representing true interactions and represent a starting point for further experimental studies.;The characteristics of high productivity were analyzed by comparing the genomes of two strains of the clavulanic acid producer Streptomyces clavuligerus. One of the strains is a high producer of clavulanic acid. Next generation sequence data was used to perform a genome-wide screening to identify all the differences between the two genomes. In addition to mutations in genes involved in beta-lactam antibiotic production or their upstream region, structural differences were detected between the two strains.;Next generation sequencing technologies were also used to assemble a draft genome for the curdlan producer Agrobacterium sp. ATCC 31749. Curdlan production mimics that of secondary metabolites, it is triggered under starvation conditions.;These varied approaches exemplify some of the paths that can lead to a better understanding of secondary metabolism and its regulation.
机译:许多次级代谢产物对人类具有有益的用途。除了用作抗菌剂和抗真菌剂,次级代谢产物还用作免疫抑制剂,抗肿瘤剂和抗寄生虫药。今天已知的大多数次级代谢产物是由丝状真菌或链霉菌属的成员产生的。微生物产生次生代谢产物涉及一个复杂,动态的系统,相互连接的元素作用于不同的水平。这项工作中使用了多种工具来探索对次生代谢产物产生的调节,主要是在链霉菌中。这些工具具有一个共同的特征:它们要么生成大量数据,要么需要大量数据。;通过使用从大型转录组数据集推断出的网络模块,在基因组水平上分析了天蓝色链霉菌次生代谢产物的调控。搜索网络模块中元素的上游序列以寻找共有序列的存在,并将这些结果与已知相互作用,结合位点和功能相关性的信息结合在一起。这些信息的结合形成了一组二十个网络,这些网络很可能代表真实的相互作用,并为进一步的实验研究提供了起点。;通过比较两种克拉维酸菌株的基因组,分析了高生产率的特征生产者Streptomyces clavuligerus。菌株之一是高生产的棒酸。下一代序列数据用于进行全基因组筛选,以鉴定两个基因组之间的所有差异。除了与β-内酰胺类抗生素生产有关的基因突变或其上游区域,还检测到了这两种菌株之间的结构差异。下一代测序技术还被用于组装柯德兰生产商土壤杆菌属的基因组草图。 ATCC31749。Curdlan的产生模仿次生代谢产物的产生,它是在饥饿条件下触发的。;这些不同的方法例证了一些途径,可以使人们更好地理解次生代谢及其调控。

著录项

  • 作者

    Castro-Melchor, Marlene.;

  • 作者单位

    University of Minnesota.;

  • 授予单位 University of Minnesota.;
  • 学科 Biology Microbiology.;Engineering Chemical.;Biology Bioinformatics.
  • 学位 Ph.D.
  • 年度 2010
  • 页码 209 p.
  • 总页数 209
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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