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通过球形孢链霉菌1912鉴定编码参与抗肿瘤抗生素地霉素E生物合成的双功能加氧酶-还原酶的基因lndM2的功能,支持了最初确定的地霉素酮结构。

Identification of the function of gene lndM2 encoding a bifunctional oxygenase-reductase involved in the biosynthesis of the antitumor antibiotic landomycin E by Streptomyces globisporus 1912 supports the originally assigned structure for landomycinone.

作者信息

Zhu Lili, Ostash Bohdan, Rix Uwe, Nur-E-Alam Mohammad, Mayers Almuth, Luzhetskyy Andriy, Mendez Carmen, Salas Jose A, Bechthold Andreas, Fedorenko Victor, Rohr Jürgen

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy, University of Kentucky, 725 Rose Street, Lexington, Kentucky 40536-0082, USA.

出版信息

J Org Chem. 2005 Jan 21;70(2):631-8. doi: 10.1021/jo0483623.

Abstract

The angucycline antibiotic family of the landomycins displays potent antitumor activity. To elucidate early post polyketide synthase (PKS) tailoring steps of the landomycin E biosynthetic pathway in Streptomyces globisporus 1912, the mutant S. globisporus M12 was prepared through gene replacement experiment of lndM2. It encodes an enzyme with putative oxygenase and reductase domains, according to sequencing of the gene and its counterpart lanM2 from S. cyanogenus S136 landomycin A biosynthetic gene cluster. The isolation of the novel shunt products 11-hydroxytetrangomycin and 4-hydroxytetrangomycin along with the well-known angucyclines tetrangomycin and tetrangulol from the culture of S. globisporus M12 provides evidence for the involvement of lndM2 in the early biosynthetic pathway of the landomycins, in particular in the formation of the alicyclic 6-hydroxy function of the landomycin aglycon. We therefore propose LndM2 to be responsible for both hydroxylation of the 6-position and its subsequent reduction. These reactions are necessary before the glycosylation reactions can occur. The results are in agreement with the originally published structure of landomycin but do not support the recently suggested revised structure.

摘要

土霉素的安古霉素类抗生素家族具有强大的抗肿瘤活性。为了阐明球形链霉菌1912中土霉素E生物合成途径中聚酮合酶(PKS)后期修饰的早期步骤,通过对lndM2进行基因置换实验制备了突变体球形链霉菌M12。根据来自蓝绿色链霉菌S136土霉素A生物合成基因簇的该基因及其对应基因lanM2的测序结果,它编码一种具有推定加氧酶和还原酶结构域的酶。从球形链霉菌M12的培养物中分离出新型分流产物11 - 羟基四抗菌素和4 - 羟基四抗菌素以及著名的安古霉素类四抗菌素和四抗菌素醇,这为lndM2参与土霉素的早期生物合成途径提供了证据,特别是在土霉素苷元的脂环族6 - 羟基官能团的形成中。因此,我们提出LndM2负责6位的羟基化及其随后的还原反应。这些反应是糖基化反应发生之前所必需的。结果与最初发表的土霉素结构一致,但不支持最近提出的修订结构。

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