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糖脂生物合成的生化多样性是球石藻噬菌体竞争生态的驱动力。

Biochemical diversity of glycosphingolipid biosynthesis as a driver of Coccolithovirus competitive ecology.

机构信息

Department of Marine and Coastal Sciences, Rutgers University, New Brunswick, NJ, 08901, USA.

Scottish Association for Marine Science, Scottish Marine Institute, Oban, Argyll, PA37 1QA, Scotland, UK.

出版信息

Environ Microbiol. 2019 Jun;21(6):2182-2197. doi: 10.1111/1462-2920.14633. Epub 2019 May 20.

DOI:10.1111/1462-2920.14633
PMID:31001863
Abstract

Coccolithoviruses (EhVs) are large, double-stranded DNA-containing viruses that infect the single-celled, marine coccolithophore Emiliania huxleyi. Given the cosmopolitan nature and global importance of E. huxleyi as a bloom-forming, calcifying, photoautotroph, E. huxleyi-EhV interactions play a key role in oceanic carbon biogeochemistry. Virally-encoded glycosphingolipids (vGSLs) are virulence factors that are produced by the activity of virus-encoded serine palmitoyltransferase (SPT). Here, we characterize the dynamics, diversity and catalytic production of vGSLs in an array of EhV strains in relation to their SPT sequence composition and explore the hypothesis that they are a determinant of infectivity and host demise. vGSL production and diversity was positively correlated with increased virulence, virus replication rate and lytic infection dynamics in laboratory experiments, but they do not explain the success of less-virulent EhVs in natural EhV communities. The majority of EhV-derived SPT amplicon sequences associated with infected cells in the North Atlantic derived from slower infecting, less virulent EhVs. Our lab-, field- and mathematical model-based data and simulations support ecological scenarios whereby slow-infecting, less-virulent EhVs successfully compete in North Atlantic populations of E. huxleyi, through either the preferential removal of fast-infecting, virulent EhVs during active infection or by having access to a broader host range.

摘要

钙板金藻病毒(EhV)是感染单细胞海洋钙板金藻的大型双链 DNA 病毒。鉴于钙板金藻是一种形成浮游生物、钙化、光合自养的全球性生物,其与 EhV 的相互作用对海洋碳生物地球化学起着关键作用。病毒编码的糖脂(vGSL)是由病毒编码丝氨酸棕榈酰转移酶(SPT)产生的毒力因子。在这里,我们描述了一系列 EhV 株系中 vGSL 的动态、多样性和催化产生情况,以及它们与 SPT 序列组成的关系,并探讨了它们是决定感染力和宿主死亡的假说。在实验室实验中,vGSL 的产生和多样性与增加的毒力、病毒复制率和裂解感染动态呈正相关,但它们并不能解释在自然 EhV 群落中,低毒 EhV 成功的原因。与北大西洋受感染细胞相关的大多数 EhV 衍生的 SPT 扩增子序列来自感染较慢、毒力较弱的 EhV。我们的实验室、现场和基于数学模型的数据和模拟支持生态场景,即通过在活跃感染期间优先去除感染较快、毒力较强的 EhV,或者通过具有更广泛的宿主范围,感染较慢、毒力较弱的 EhV 可以在北大西洋的钙板金藻种群中成功竞争。

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