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一种新型卡里曼他星/巴图霉素相关聚酮类抗生素的分离纯化及其生物合成基因簇的解析

Isolation and purification of a new kalimantacin/batumin-related polyketide antibiotic and elucidation of its biosynthesis gene cluster.

作者信息

Mattheus Wesley, Gao Ling-Jie, Herdewijn Piet, Landuyt Bart, Verhaegen Jan, Masschelein Joleen, Volckaert Guido, Lavigne Rob

机构信息

Laboratory of Gene Technology, Katholieke Universiteit Leuven, Leuven B-3000, Belgium.

出版信息

Chem Biol. 2010 Feb 26;17(2):149-59. doi: 10.1016/j.chembiol.2010.01.014.

DOI:10.1016/j.chembiol.2010.01.014
PMID:20189105
Abstract

Kal/bat, a polyketide, isolated to high purity (>95%) is characterized by strong and selective antibacterial activity against Staphylococcus species (minimum inhibitory concentration, 0.05 microg/mL), and no resistance was observed in strains already resistant to commonly used antibiotics. The kal/bat biosynthesis gene cluster was determined to a 62 kb genomic region of Pseudomonas fluorescens BCCM_ID9359. The kal/bat gene cluster consists of 16 open reading frames (ORF), encoding a hybrid PKS-NRPS system, extended with trans-acting tailoring functions. A full model for kal/bat biosynthesis is postulated and experimentally tested by gene inactivation, structural confirmation (using NMR spectroscopy), and complementation. The structural and microbiological study of biosynthetic kal/bat analogs revealed the importance of the carbamoyl group and 17-keto group for antibacterial activity. The mechanism of self-resistance lies within the production of an inactive intermediate, which is activated in a one-step enzymatic oxidation upon export. The genetic basis and biochemical elucidation of the biosynthesis pathway of this antibiotic will facilitate rational engineering for the design of novel structures with improved activities. This makes it a promising new therapeutic option to cope with multidrug-resistant clinical infections.

摘要

卡尔/巴特(Kal/bat)是一种聚酮化合物,分离得到的纯度较高(>95%),其特点是对葡萄球菌具有强大且具选择性的抗菌活性(最低抑菌浓度为0.05微克/毫升),并且在对常用抗生素已产生耐药性的菌株中未观察到耐药现象。卡尔/巴特生物合成基因簇定位于荧光假单胞菌BCCM_ID9359的一个62 kb基因组区域。卡尔/巴特基因簇由16个开放阅读框(ORF)组成,编码一个杂交的聚酮合酶-非核糖体肽合成酶(PKS-NRPS)系统,并扩展有反式作用的修饰功能。通过基因失活、结构确证(使用核磁共振光谱)和互补作用,提出并通过实验测试了卡尔/巴特生物合成的完整模型。对生物合成的卡尔/巴特类似物的结构和微生物学研究揭示了氨甲酰基和17-酮基对抗菌活性的重要性。自我耐药机制在于产生一种无活性的中间体,该中间体在输出时通过一步酶促氧化被激活。这种抗生素生物合成途径的遗传基础和生化阐明将有助于合理设计具有更高活性的新结构。这使其成为应对多重耐药临床感染的一个有前景的新治疗选择。

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