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两株铜绿微囊藻中微囊藻毒素的生物合成:从结构到基因,反之亦然。

Microcyclamide biosynthesis in two strains of Microcystis aeruginosa: from structure to genes and vice versa.

作者信息

Ziemert Nadine, Ishida Keishi, Quillardet Philippe, Bouchier Christiane, Hertweck Christian, de Marsac Nicole Tandeau, Dittmann Elke

机构信息

Department of Molecular Ecology, Institute of Biology, Humboldt University Berlin, 10115 Berlin, Germany.

出版信息

Appl Environ Microbiol. 2008 Mar;74(6):1791-7. doi: 10.1128/AEM.02392-07. Epub 2008 Feb 1.

Abstract

Comparative analysis of related biosynthetic gene clusters can provide new insights into the versatility of these pathways and allow the discovery of new natural products. The freshwater cyanobacterium Microcystis aeruginosa NIES298 produces the cytotoxic peptide microcyclamide. Here, we provide evidence that the cyclic hexapeptide is formed by a ribosomal pathway through the activity of a set of processing enzymes closely resembling those recently shown to be involved in patellamide biosynthesis in cyanobacterial symbionts of ascidians. Besides two subtilisin-type proteases and a heterocyclization enzyme, the gene cluster discovered in strain NIES298 encodes six further open reading frames, two of them without similarity to enzymes encoded by the patellamide gene cluster. Analyses of genomic data of a second cyanobacterial strain, M. aeruginosa PCC 7806, guided the discovery and structural elucidation of two novel peptides of the microcyclamide family. The identification of the microcyclamide biosynthetic genes provided an avenue by which to study the regulation of peptide synthesis at the transcriptional level. The precursor genes were strongly and constitutively expressed throughout the growth phase, excluding the autoinduction of these peptides, as has been observed for several peptide pheromone families in bacteria.

摘要

对相关生物合成基因簇的比较分析能够为这些途径的多功能性提供新的见解,并有助于发现新的天然产物。淡水蓝藻铜绿微囊藻NIES298能产生具有细胞毒性的肽类微环酰胺。在此,我们提供证据表明,这种环六肽是通过核糖体途径,由一组加工酶的活性形成的,这些酶与最近在海鞘蓝藻共生体中参与帕台酰胺生物合成的酶极为相似。除了两种枯草杆菌蛋白酶样蛋白酶和一种杂环化酶外,在NIES298菌株中发现的基因簇还编码另外六个开放阅读框,其中两个与帕台酰胺基因簇编码的酶没有相似性。对第二种蓝藻菌株铜绿微囊藻PCC 7806的基因组数据分析,引导了微环酰胺家族两种新型肽的发现和结构解析。微环酰胺生物合成基因的鉴定提供了一条在转录水平研究肽合成调控的途径。前体基因在整个生长阶段都强烈且组成型表达,排除了这些肽的自诱导现象,这与在细菌中观察到的几个肽类信息素家族的情况相同。

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