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人肠道噬菌体-细菌宿主动态的无菌小鼠模型。

Gnotobiotic mouse model of phage-bacterial host dynamics in the human gut.

机构信息

Center for Genome Sciences and Systems Biology, Washington University School of Medicine, St. Louis, MO 63108.

出版信息

Proc Natl Acad Sci U S A. 2013 Dec 10;110(50):20236-41. doi: 10.1073/pnas.1319470110. Epub 2013 Nov 20.

Abstract

Bacterial viruses (phages) are the most abundant biological group on Earth and are more genetically diverse than their bacterial prey/hosts. To characterize their role as agents shaping gut microbial community structure, adult germ-free mice were colonized with a consortium of 15 sequenced human bacterial symbionts, 13 of which harbored one or more predicted prophages. One member, Bacteroides cellulosilyticus WH2, was represented by a library of isogenic transposon mutants that covered 90% of its genes. Once assembled, the community was subjected to a staged phage attack with a pool of live or heat-killed virus-like particles (VLPs) purified from the fecal microbiota of five healthy humans. Shotgun sequencing of DNA from the input pooled VLP preparation plus shotgun sequencing of gut microbiota samples and purified fecal VLPs from the gnotobiotic mice revealed a reproducible nonsimultaneous pattern of attack extending over a 25-d period that involved five phages, none described previously. This system allowed us to (i) correlate increases in specific phages present in the pooled VLPs with reductions in the representation of particular bacterial taxa, (ii) provide evidence that phage resistance occurred because of ecological or epigenetic factors, (iii) track the origin of each of the five phages among the five human donors plus the extent of their genome variation between and within recipient mice, and (iv) establish the dramatic in vivo fitness advantage that a locus within a B. cellulosilyticus prophage confers upon its host. Together, these results provide a defined community-wide view of phage-bacterial host dynamics in the gut.

摘要

细菌病毒(噬菌体)是地球上最丰富的生物群体,其遗传多样性超过其细菌猎物/宿主。为了研究它们作为塑造肠道微生物群落结构的因子的作用,我们用 15 种已测序的人类细菌共生体组成的混合物使成年无菌小鼠定殖,其中 13 种共生体携带一个或多个预测的前噬菌体。其中一个成员是纤维素分解梭菌 WH2,它有一个包含其 90%基因的转座子突变体文库。一旦组装完成,就用来自 5 个健康人的粪便微生物群中纯化的活或热失活病毒样颗粒 (VLP) 池对群落进行分阶段噬菌体攻击。输入的混合 VLP 制剂的 DNA 进行鸟枪法测序,以及无菌小鼠的肠道微生物群样本和纯化的粪便 VLP 的 DNA 进行鸟枪法测序,揭示了一种可重复的非同时攻击模式,持续 25 天,涉及 5 种噬菌体,以前都没有描述过。该系统使我们能够:(i) 将混合 VLP 中存在的特定噬菌体的增加与特定细菌类群的代表性减少相关联;(ii) 提供证据表明,噬菌体抗性是由于生态或表观遗传因素引起的;(iii) 追踪这 5 种噬菌体中的每一种在 5 个供体中的起源以及它们在受体小鼠之间和之内的基因组变异程度;(iv) 确定纤维素分解梭菌前噬菌体内部的一个基因座在体内赋予其宿主的巨大适应优势。这些结果共同提供了肠道中噬菌体-细菌宿主动力学的全面社区视角。

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