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阿卡波糖产生菌 Actinoplanes sp. SE50/110 的全基因组序列。

The complete genome sequence of the acarbose producer Actinoplanes sp. SE50/110.

机构信息

Senior research group in Genome Research of Industrial Microorganisms, Center for Biotechnology, Bielefeld University, Germany.

出版信息

BMC Genomics. 2012 Mar 23;13:112. doi: 10.1186/1471-2164-13-112.

Abstract

BACKGROUND

Actinoplanes sp. SE50/110 is known as the wild type producer of the alpha-glucosidase inhibitor acarbose, a potent drug used worldwide in the treatment of type-2 diabetes mellitus. As the incidence of diabetes is rapidly rising worldwide, an ever increasing demand for diabetes drugs, such as acarbose, needs to be anticipated. Consequently, derived Actinoplanes strains with increased acarbose yields are being used in large scale industrial batch fermentation since 1990 and were continuously optimized by conventional mutagenesis and screening experiments. This strategy reached its limits and is generally superseded by modern genetic engineering approaches. As a prerequisite for targeted genetic modifications, the complete genome sequence of the organism has to be known.

RESULTS

Here, we present the complete genome sequence of Actinoplanes sp. SE50/110 [GenBank:CP003170], the first publicly available genome of the genus Actinoplanes, comprising various producers of pharmaceutically and economically important secondary metabolites. The genome features a high mean G + C content of 71.32% and consists of one circular chromosome with a size of 9,239,851 bp hosting 8,270 predicted protein coding sequences. Phylogenetic analysis of the core genome revealed a rather distant relation to other sequenced species of the family Micromonosporaceae whereas Actinoplanes utahensis was found to be the closest species based on 16S rRNA gene sequence comparison. Besides the already published acarbose biosynthetic gene cluster sequence, several new non-ribosomal peptide synthetase-, polyketide synthase- and hybrid-clusters were identified on the Actinoplanes genome. Another key feature of the genome represents the discovery of a functional actinomycete integrative and conjugative element.

CONCLUSIONS

The complete genome sequence of Actinoplanes sp. SE50/110 marks an important step towards the rational genetic optimization of the acarbose production. In this regard, the identified actinomycete integrative and conjugative element could play a central role by providing the basis for the development of a genetic transformation system for Actinoplanes sp. SE50/110 and other Actinoplanes spp. Furthermore, the identified non-ribosomal peptide synthetase- and polyketide synthase-clusters potentially encode new antibiotics and/or other bioactive compounds, which might be of pharmacologic interest.

摘要

背景

放线菌属 SE50/110 是已知的α-葡萄糖苷酶抑制剂阿卡波糖的野生型产生菌,阿卡波糖是一种在全球范围内用于治疗 2 型糖尿病的有效药物。随着全球糖尿病发病率的迅速上升,预计对阿卡波糖等糖尿病药物的需求将不断增加。因此,自 1990 年以来,具有更高阿卡波糖产量的衍生放线菌菌株已在大规模工业分批发酵中使用,并通过常规诱变和筛选实验不断优化。该策略已达到极限,通常被现代基因工程方法所取代。作为靶向遗传修饰的前提,必须了解生物体的完整基因组序列。

结果

在这里,我们介绍了放线菌属 SE50/110 的完整基因组序列[GenBank:CP003170],这是放线菌属的第一个公开基因组,其中包含各种具有药用和经济重要性的次生代谢产物的产生菌。该基因组的平均 G+C 含量为 71.32%,由一个大小为 9239851bp 的圆形染色体组成,其中包含 8270 个预测的蛋白质编码序列。核心基因组的系统发育分析表明,与其他已测序的微单孢子科物种的关系相当遥远,而放线菌属 utahensis 是基于 16S rRNA 基因序列比较发现的最接近的物种。除了已发表的阿卡波糖生物合成基因簇序列外,还在放线菌属基因组上鉴定了几个新的非核糖体肽合成酶、聚酮合酶和杂交簇。基因组的另一个重要特征是发现了一个功能性放线菌整合子和转座子。

结论

放线菌属 SE50/110 的完整基因组序列标志着朝着理性遗传优化阿卡波糖生产迈出了重要一步。在这方面,鉴定出的放线菌整合子和转座子可以通过为放线菌属 SE50/110 和其他放线菌属 spp 的遗传转化系统的发展提供基础,发挥核心作用。此外,鉴定出的非核糖体肽合成酶和聚酮合酶簇可能编码新的抗生素和/或其他具有生物活性的化合物,这些化合物可能具有药理学意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4df5/3364876/d410acfcfb66/1471-2164-13-112-1.jpg

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