隐性宿主表型异质性驱动噬菌体λ多样化

Caesar A. De La Fuente, Nehme Lahoud, Justin R. Meyer
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摘要

噬菌体是种类最丰富、基因最多样的生命形式,但它们似乎违背了基本的生态学理论,因为它们比其众多的细菌猎物表现出更大的多样性。这一悖论提出了寄生虫多样性的内在机制问题。为了研究这个问题,我们利用了一个令人惊讶的实验结果:当噬菌体λ持续供应给一个宿主时,λ在同一烧瓶中反复演化出多种基因型,这些基因型在受体使用方面各不相同。对受体专家之间频率依赖性负选择的测量表明,多样化选择推动了它们的进化和维持。然而,产生这种选择所需的环境异质性来源尚不清楚,因为只提供了单一的同源宿主,并每八小时补充一次。我们的实验表明,对不同专科噬菌体的选择在 8 小时的孵育期内会发生振荡,这反映了 λ 的两种受体(大肠杆菌外膜蛋白 LamB 和 OmpF)基因表达的振荡。这些受体表达的变化可归因于细胞间受体表达的变化和细菌的快速进化,我们利用表型抗性测定和群体基因组测序记录了这些变化。我们的研究结果表明,由非遗传表型异质性和快速进化引起的宿主隐性表型变异可能在驱动病毒多样性方面起着关键作用。
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Cryptic host phenotypic heterogeneity drives diversification of bacteriophage λ
Bacteriophages, the most abundant and genetically diverse life forms, seemingly defy fundamental ecological theory by exhibiting greater diversity than their numerous bacterial prey. This paradox raises questions about the mechanisms underlying parasite diversity. To investigate this, we took advantage of a surprising experimental result: when bacteriophage λ is continually supplied a single host, λ repeatedly evolves multiple genotypes within the same flask that vary in their receptor use. Measurements of negative frequency-dependent selection between receptor specialists revealed that diversifying selection drove their evolution and maintenance. However, the source of environmental heterogeneity necessary to generate this type of selection was unclear, as only a single isogenic host was provided and replenished every eight hours. Our experiments showed that selection for different specialist phages oscillated over the 8-hour incubation period, mirroring oscillations in gene expression of λ’s two receptors (Escherichia coli outer membrane proteins LamB and OmpF). These receptor expression changes were attributed to both cell-to-cell variation in receptor expression and rapid bacterial evolution, which we documented using phenotypic resistance assays and population genome sequencing. Our findings suggest that cryptic phenotypic variation in hosts, arising from non-genetic phenotypic heterogeneity and rapid evolution, may play a key role in driving viral diversity.
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