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两种不同淡水环境中铜绿微囊藻噬藻体的遗传多样性。

Genetic diversity of Microcystis cyanophages in two different freshwater environments.

机构信息

Laboratory of Marine Microbiology, Graduate School of Agriculture, Kyoto University, Kitashirakawa-Oiwake, Sakyo-ku, Kyoto, 606-8502, Japan.

出版信息

Arch Microbiol. 2014 Jun;196(6):401-9. doi: 10.1007/s00203-014-0980-4. Epub 2014 Mar 27.

DOI:10.1007/s00203-014-0980-4
PMID:24671440
Abstract

Bacteriophages rapidly diversify their genes through co-evolution with their hosts. We hypothesize that gene diversification of phages leads to locality in phages genome. To test this hypothesis, we investigated the genetic diversity and composition of Microcystis cyanophages using 104 sequences of Ma-LMM01-type cyanophages from two geographically distant sampling sites. The intergenetic region between the ribonucleotide reductase genes nrdA and nrdB was used as the genetic marker. This region contains the host-derived auxiliary metabolic genes nblA, an unknown function gene g04, and RNA ligase gene g03. The sequences obtained were conserved in the Ma-LMM01 gene order and contents. Although the genetic diversity of the sequences was high, it varied by gene. The genetic diversity of nblA was the lowest, suggesting that nblA is a highly significant gene that does not allow mutation. In contrast, g03 sequences had many point mutations. RNA ligase is involved in the counter-host's phage defense mechanism, suggesting that phage defense also plays an important role for rapid gene diversification. The maximum parsimony network and phylogenic analysis showed the sequences from the two sampling sites were distinct. These findings suggest Ma-LMM01-type phages rapidly diversify their genomes through co-evolution with hosts in each location and eventually provided locality of their genomes.

摘要

噬菌体通过与宿主的共同进化迅速多样化其基因。我们假设噬菌体基因的多样化导致噬菌体基因组的局部性。为了验证这一假设,我们使用来自两个地理位置遥远的采样点的 104 个 Ma-LMM01 型噬藻体序列,研究了微囊藻噬藻体的遗传多样性和组成。核糖体核苷酸还原酶基因 nrdA 和 nrdB 之间的基因间区被用作遗传标记。该区域包含宿主衍生的辅助代谢基因 nblA、一个未知功能基因 g04 和 RNA 连接酶基因 g03。获得的序列在 Ma-LMM01 基因顺序和内容上是保守的。尽管序列的遗传多样性很高,但因基因而异。nblA 的遗传多样性最低,表明 nblA 是一个高度重要的基因,不允许突变。相比之下,g03 序列有许多点突变。RNA 连接酶参与对抗宿主的噬菌体防御机制,这表明噬菌体防御对于快速基因多样化也起着重要作用。最大简约网络和系统发育分析显示,来自两个采样点的序列是不同的。这些发现表明,Ma-LMM01 型噬藻体通过与每个地点的宿主共同进化迅速多样化其基因组,并最终提供了其基因组的局部性。

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