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通过长读长宏基因组学发现更广泛的宿主范围和一类与插入序列相关的原噬菌体。

Discovering Broader Host Ranges and an IS-bound Prophage Class Through Long-Read Metagenomics.

作者信息

Wirbel Jakob, Hickey Angela S, Chang Daniel, Enright Nora J, Dvorak Mai, Chanin Rachael B, Schmidtke Danica T, Bhatt Ami S

机构信息

Division of Hematology, Department of Medicine, Stanford University, Stanford, CA.

Department of Genetics, Stanford University, Stanford, CA.

出版信息

bioRxiv. 2025 May 10:2025.05.09.652943. doi: 10.1101/2025.05.09.652943.

DOI:10.1101/2025.05.09.652943
PMID:40654884
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12247996/
Abstract

Gut bacteriophages profoundly impact microbial ecology and human health, yet they are greatly understudied. Using deep, long-read bulk metagenomic sequencing, a technique that overcomes fundamental limitations of short-read approaches, we tracked prophage integration dynamics in 12 longitudinal stool samples from six healthy individuals, spanning a two-year timescale. While most prophages remain stably integrated into their host over two years, we discover that ~5% of phages are dynamically gained or lost from persistent bacterial hosts. Within the same sample, we find evidence of population heterogeneity in which identical bacterial hosts with and without a given integrated prophage coexist simultaneously. Furthermore, we demonstrate that phage induction, when detected, occurs predominantly at low levels (1-3x coverage compared to the host region). Interestingly, we identify multiple instances of integration of the same phage into bacteria of different taxonomic families, challenging the dogma that phage are specific to a host of a given species or strain. Lastly, we describe a new class of phages, which we name "IScream phages". These phages co-opt bacterial IS30 transposases to mediate their integration, representing a previously unrecognized form of phage domestication of selfish bacterial elements. Taken together, these findings illuminate fundamental aspects of phage-bacterial dynamics in the human gut microbiome and expand our understanding of the evolutionary mechanisms that drive horizontal gene transfer and microbial genome plasticity in this ecosystem.

摘要

肠道噬菌体对微生物生态和人类健康有着深远影响,但它们却极少被研究。我们运用深度、长读长的宏基因组测序技术(该技术克服了短读长方法的根本局限),在跨越两年时间尺度的情况下,对来自6名健康个体的12份纵向粪便样本中的前噬菌体整合动态进行了追踪。虽然大多数前噬菌体在两年时间里保持稳定整合在其宿主中,但我们发现约5%的噬菌体在持续存在的细菌宿主中会动态获得或丢失。在同一样本中,我们发现了种群异质性的证据,即携带和不携带特定整合前噬菌体的相同细菌宿主同时共存。此外,我们证明,当检测到噬菌体诱导时,其主要以低水平发生(与宿主区域相比,覆盖度为1 - 3倍)。有趣的是,我们识别出同一噬菌体整合到不同分类家族细菌中的多个实例,这对噬菌体特定于给定物种或菌株宿主的教条提出了挑战。最后,我们描述了一类新的噬菌体,我们将其命名为“IScream噬菌体”。这些噬菌体利用细菌IS30转座酶来介导它们的整合,代表了一种以前未被认识的噬菌体对自私细菌元件的驯化形式。综上所述,这些发现阐明了人类肠道微生物群中噬菌体 - 细菌动态的基本方面,并扩展了我们对驱动该生态系统中水平基因转移和微生物基因组可塑性的进化机制的理解。

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本文引用的文献

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Abundance measurements reveal the balance between lysis and lysogeny in the human gut microbiome.丰度测量揭示了人类肠道微生物群中裂解和溶原性之间的平衡。
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Long-read sequencing reveals extensive gut phageome structural variations driven by genetic exchange with bacterial hosts.
长读测序揭示了广泛的肠道噬菌体组结构变异,这些变异是由与细菌宿主的基因交换驱动的。
Sci Adv. 2024 Aug 16;10(33):eadn3316. doi: 10.1126/sciadv.adn3316. Epub 2024 Aug 14.
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Nanopore and Illumina sequencing reveal different viral populations from human gut samples.纳米孔和 Illumina 测序揭示了来自人类肠道样本的不同病毒群体。
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Phage transmission strategies: are phages farming their host?噬菌体传播策略:噬菌体在“养殖”宿主吗?
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