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AlpW 途径特异性晚期调控因子的特征和操作揭示链霉菌属放线菌是 Kinamycins 的新产生菌。

Characterization and manipulation of the pathway-specific late regulator AlpW reveals Streptomyces ambofaciens as a new producer of Kinamycins.

机构信息

Université Henri Poincaré, UMR1128, Génétique et Microbiolog, Vandœuvre-lès-Nancy, France.

出版信息

J Bacteriol. 2011 Mar;193(5):1142-53. doi: 10.1128/JB.01269-10. Epub 2010 Dec 30.

Abstract

The genome sequence of Streptomyces ambofaciens, a species known to produce the congocidine and spiramycin antibiotics, has revealed the presence of numerous gene clusters predicted to be involved in the biosynthesis of secondary metabolites. Among them, the type II polyketide synthase-encoding alp cluster was shown to be responsible for the biosynthesis of a compound with antibacterial activity. Here, by means of a deregulation approach, we gained access to workable amounts of the antibiotics for structure elucidation. These compounds, previously designated as alpomycin, were shown to be known members of kinamycin family of antibiotics. Indeed, a mutant lacking AlpW, a member of the TetR regulator family, was shown to constitutively produce kinamycins. Comparative transcriptional analyses showed that expression of alpV, the essential regulator gene required for activation of the biosynthetic genes, is strongly maintained during the stationary growth phase in the alpW mutant, a stage at which alpV transcripts and thereby transcripts of the biosynthetic genes normally drop off. Recombinant AlpW displayed DNA binding activity toward specific motifs in the promoter region of its own gene and that of alpV and alpZ. These recognition sequences are also targets for AlpZ, the γ-butyrolactone-like receptor involved in the regulation of the alp cluster. However, unlike that of AlpZ, the AlpW DNA-binding ability seemed to be insensitive to the signaling molecules controlling antibiotic biosynthesis. Together, the results presented in this study reveal S. ambofaciens to be a new producer of kinamycins and AlpW to be a key late repressor of the cellular control of kinamycin biosynthesis.

摘要

链霉菌属 ambofaciens 的基因组序列,该物种已知产生 congocidine 和螺旋霉素抗生素,其存在许多基因簇,预测涉及次生代谢物的生物合成。其中,II 型聚酮合酶编码 alp 簇被证明负责合成具有抗菌活性的化合物。在这里,通过一种去调控方法,我们获得了可用于结构阐明的抗生素的可行量。这些化合物以前被指定为 alpomycin,被证明是已知的 kinamycin 抗生素家族的成员。事实上,缺乏 TetR 调节因子家族成员 AlpW 的突变体被证明持续产生 kinamycins。比较转录分析表明,激活生物合成基因所需的必需调节基因 alpV 的表达在 alpW 突变体的静止生长阶段得到强烈维持,在这个阶段,alpV 转录物和生物合成基因的转录物通常会下降。重组 AlpW 对其自身基因和 alpV 和 alpZ 启动子区域的特定基序显示出 DNA 结合活性。这些识别序列也是涉及 alp 簇调节的 γ-丁内酯样受体 AlpZ 的靶标。然而,与 AlpZ 不同的是,AlpW 的 DNA 结合能力似乎对控制抗生素生物合成的信号分子不敏感。总之,本研究结果表明链霉菌属 ambofaciens 是 kinamycins 的新生产者,而 AlpW 是 kinamycin 生物合成细胞控制的关键晚期抑制剂。

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