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Genome Analysis of the Fruiting Body-Forming Myxobacterium Chondromyces crocatus Reveals High Potential for Natural Product Biosynthesis

机译:形成果实的粘多糖线粒体软骨细菌的基因组分析显示天然产物生物合成的高潜力

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摘要

Here, we report the complete genome sequence of the type strain of the myxobacterial genus Chondromyces, Chondromyces crocatus Cm c5. It presents one of the largest prokaryotic genomes featuring a single circular chromosome and no plasmids. Analysis revealed an enlarged set of tRNA genes, along with reduced pressure on preferred codon usage compared to that of other bacterial genomes. The large coding capacity and the plethora of encoded secondary metabolite biosynthetic gene clusters are in line with the capability of Cm c5 to produce an arsenal of antibacterial, antifungal, and cytotoxic compounds. Known pathways of the ajudazol, chondramide, chondrochloren, crocacin, crocapeptin, and thuggacin compound families are complemented by many more natural compound biosynthetic gene clusters in the chromosome. Whole-genome comparison of the fruiting-body-forming type strain (Cm c5, DSM 14714) to an accustomed laboratory strain which has lost this ability (nonfruiting phenotype, Cm c5 fr−) revealed genetic changes in three loci. In addition to the low synteny found with the closest sequenced representative of the same family, Sorangium cellulosum, extensive genetic information duplication and broad application of eukaryotic-type signal transduction systems are hallmarks of this 11.3-Mbp prokaryotic genome.
机译:在这里,我们报告的黏细菌属软骨型,克氏杆菌Cm c5型菌株的完整基因组序列。它提供了最大的原核基因组之一,具有单个环状染色体且无质粒。分析显示,与其他细菌基因组相比,tRNA基因集扩大了,同时对优选密码子使用的压力降低了。大的编码能力和编码的次级代谢产物生物合成基因簇的过多与Cm c5产生一系列抗菌,抗真菌和细胞毒性化合物的能力是一致的。阿杜唑,软骨酰胺,软骨素,crocacin,crocapeptin和thuggacin化合物家族的已知途径在染色体中被更多的天然化合物生物合成基因簇所补充。将子实体形成型菌株(Cm c5,DSM 14714)与已丧失此能力的常规实验室菌株(非子实体表型,Cm c5 fr-)的全基因组比较显示三个位点的遗传变化。除了与同一家族的最接近序列代表的低同音外,纤维素膜,广泛的遗传信息重复和真核型信号转导系统的广泛应用是该11.3Mbp原核基因组的标志。

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