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Capsular Polysaccharides in Bacteroides thetaiotaomicron and Their Role in Mediating Interactions with Host Immunity and Bacteriophage

机译:拟杆菌中的荚膜多糖及其在介导与宿主免疫和噬菌体相互作用中的作用

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摘要

Members of the Bacteroides and Parabacteroides genera, a prevalent portion of the gut microbiota, typically encode multiple loci for the synthesis of capsular polysaccharides (CPS). Strains may possess more than a dozen of these loci in a single genome, and locus expression is tightly regulated and may be highly dynamic. While some individual CPS have been characterized and confer advantageous properties on the bacterium (e.g. host immunomodulation), the functions of the majority of CPS are unknown. The model gut commensal Bacteroides thetaiotaomicron ( B. theta) encodes for 8 distinct CPS synthesis loci, and these are coordinately regulated with other cellular functions such as carbohydrate utilization. I created a novel set of isogenic B. theta strains that each express one of the bacterium's eight CPS. These strains enable the identification of advantages conferred by individual CPS, as well as the role that encoding and expressing multiple CPS may play in optimal survival within the host organism.;This collection of single CPS-expressing strains was pooled and inoculated into germ-free mice, in which we could alter host genetic and dietary parameters. We found that specific CPS provided an advantage over others when in direct competition, and that adjusting levels of host immune response (especially adaptive immunity and IgA levels) altered the stringency of intra-strain competition. The CPS5-expressing strain outcompeted all other single CPS-expressing strains in the presence of adaptive immunity and even successfully competed with the wild-type strain until the community was perturbed with antibiotics, which selected for the wild-type strain.;Additionally, I tested the ability of different CPS-expressing strains to be infected by bacteriophages. I determined that a large collection of bacteriophages isolated on this panel of B. theta strains are only able to infect a subset of the bacterial strains, directly linking CPS to bacteriophage resistance. Wild-type B. theta alters its CPS locus expression when exposed to bacteriophage and is able to quickly recover from phage infection, indicating that another purpose of encoding for the synthesis of multiple CPS is to render subpopulations of the bacterium phage resistant. My work describes roles for specific CPS, identifies advantages of switching between multiple CPS types, and provides a unique resource to further study CPS produced by human-associated commensal bacteria.
机译:拟杆菌和副细菌属的成员,肠道菌群的普遍部分,通常编码多个位点,用于合成荚膜多糖(CPS)。菌株在单个基因组中可能拥有十几个这些基因座,并且基因座表达受到严格调节,并且可能是高度动态的。虽然已经表征了一些单独的CPS并赋予细菌以有利的特性(例如宿主免疫调节),但大多数CPS的功能尚不清楚。模型肠道共生细菌拟杆菌(B. theta)编码8个不同的CPS合成基因座,并且它们与其他细胞功能(如碳水化合物利用)协同调节。我创建了一组新的同基因B. theta菌株,每个菌株均表达细菌的八个CPS之一。这些菌株能够鉴定单个CPS赋予的优势,以及编码和表达多种CPS可能在宿主生物体内的最佳存活中发挥的作用。;收集了表达CPS的单个菌株的集合并将其接种到无细菌中小鼠,我们可以改变宿主的遗传和饮食参数。我们发现,在直接竞争中,特定的CPS比其他CPS更具优势,并且调节宿主免疫应答的水平(尤其是适应性免疫和IgA水平)可以改变菌株竞争的严格性。在具有适应性免疫的情况下,表达CPS5的菌株胜过所有其他表达CPS的菌株,甚至成功地与野生型菌株竞争,直到社区被选择为野生型菌株的抗生素干扰为止。测试了不同表达CPS的菌株被噬菌体感染的能力。我确定在这组B. theta菌株中分离出的大量噬菌体只能感染一部分细菌菌株,从而直接将CPS与噬菌体抗性联系起来。当暴露于噬菌体时,野生型B. theta会改变其CPS基因座表达,并且能够从噬菌体感染中快速恢复,这表明编码多个CPS的合成的另一个目的是使细菌噬菌体的亚群具有抗性。我的工作描述了特定CPS的角色,确定了在多种CPS类型之间切换的优势,并提供了独特的资源来进一步研究由人类相关的共生细菌产生的CPS。

著录项

  • 作者

    Porter, Nathan T.;

  • 作者单位

    University of Michigan.;

  • 授予单位 University of Michigan.;
  • 学科 Microbiology.;Immunology.
  • 学位 Ph.D.
  • 年度 2017
  • 页码 158 p.
  • 总页数 158
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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