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Host-hijacking and planktonic piracy: how phages command the microbial high seas

机译:劫持主机和浮游海盗行为:噬菌体如何控制微生物公海

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摘要

Microbial communities living in the oceans are major drivers of global biogeochemical cycles. With nutrients limited across vast swathes of the ocean, marine microbes eke out a living under constant assault from predatory viruses. Viral concentrations exceed those of their bacterial prey by an order of magnitude in surface water, making these obligate parasites the most abundant biological entities in the ocean. Like the pirates of the 17th and 18th centuries that hounded ships plying major trade and exploration routes, viruses have evolved mechanisms to hijack microbial cells and repurpose their cargo and indeed the vessels themselves to maximise viral propagation. Phenotypic reconfiguration of the host is often achieved through Auxiliary Metabolic Genes – genes originally derived from host genomes but maintained and adapted in viral genomes to redirect energy and substrates towards viral synthesis. In this review, we critically evaluate the literature describing the mechanisms used by bacteriophages to reconfigure host metabolism and to plunder intracellular resources to optimise viral production. We also highlight the mechanisms used when, in challenging environments, a ‘batten down the hatches’ strategy supersedes that of ‘plunder and pillage’. Here, the infecting virus increases host fitness through phenotypic augmentation in order to ride out the metaphorical storm, with a concomitant impact on host substrate uptake and metabolism, and ultimately, their interactions with their wider microbial community. Thus, the traditional view of the virus-host relationship as predator and prey does not fully characterise the variety or significance of the interactions observed. Recent advances in viral metagenomics have provided a tantalising glimpse of novel mechanisms of viral metabolic reprogramming in global oceans. Incorporation of these new findings into global biogeochemical models requires experimental evidence from model systems and major improvements in our ability to accurately predict protein function from sequence data.
机译:生活在海洋中的微生物群落是全球生物地球化学循环的主要驱动力。由于营养成分限制在广阔的海洋中,海洋微生物在不断受到掠夺性病毒侵袭的情况下养成了生计。在地表水中,病毒的浓度比其细菌的浓度高一个数量级,使这些专性寄生虫成为海洋中最丰富的生物实体。就像17世纪和18世纪的海盗一样,病毒束缚着沿主要贸易和探索路线航行的船只,病毒已经进化出劫持微生物细胞,重新利用其货物,甚至使船只本身最大化病毒传播的机制。宿主的表型重配置通常是通过辅助代谢基因实现的-辅助基因最初源自宿主基因组,但在病毒基因组中得以维持和适应,以将能量和底物重新定向至病毒合成。在这篇综述中,我们严格地评估了描述噬菌体用来重新配置宿主代谢和掠夺细胞内资源以优化病毒生产的机制的文献。我们还将重点介绍在充满挑战的环境中,“严密控制”战略取代“掠夺和掠夺”战略所使用的机制。在这里,感染病毒通过表型增强来增加宿主的适应性,以度过隐喻风暴,并伴随宿主基质摄取和代谢,以及最终与其广泛微生物群落的相互作用。因此,传统的将病毒与宿主关系视为掠食者和猎物的观点并不能完全表征观察到的相互作用的多样性或重要性。病毒宏基因组学的最新进展为全球海洋中的病毒代谢重编程的新机制提供了诱人的一瞥。将这些新发现整合到全球生物地球化学模型中需要模型系统提供实验证据,并且需要我们从序列数据中准确预测蛋白质功能的能力得到重大改进。

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