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天蓝色链霉菌中放线紫红素输出的起始

Initiation of actinorhodin export in Streptomyces coelicolor.

作者信息

Tahlan Kapil, Ahn Sang Kyun, Sing Anson, Bodnaruk Tetyana D, Willems Andrew R, Davidson Alan R, Nodwell Justin R

机构信息

Department of Biochemistry and Biomedical Sciences, McMaster University, Hamilton, ON, Canada.

出版信息

Mol Microbiol. 2007 Feb;63(4):951-61. doi: 10.1111/j.1365-2958.2006.05559.x.

Abstract

Many microorganisms produce molecules having antibiotic activity and expel them into the environment, presumably enhancing their ability to compete with their neighbours. Given that these molecules are often toxic to the producer, mechanisms must exist to ensure that the assembly of the export apparatus accompanies or precedes biosynthesis. Streptomyces coelicolor produces the polyketide antibiotic actinorhodin in a multistep pathway involving enzymes encoded by genes that are clustered together. Embedded within the cluster are genes for actinorhodin export, two of which, actR and actA resemble the classic tetR and tetA repressor/efflux pump-encoding gene pairs that confer resistance to tetracycline. Like TetR, which represses tetA, ActR is a repressor of actA. We have identified several molecules that can relieve repression by ActR. Importantly (S)-DNPA (an intermediate in the actinorhodin biosynthetic pathway) and kalafungin (a molecule related to the intermediate dihydrokalafungin), are especially potent ActR ligands. This suggests that along with the mature antibiotic(s), intermediates in the biosynthetic pathway might activate expression of the export genes thereby coupling export to biosynthesis. We suggest that this could be a common feature in the production of many bioactive natural products.

摘要

许多微生物会产生具有抗生素活性的分子,并将其释放到环境中,推测这会增强它们与邻近微生物竞争的能力。鉴于这些分子通常对产生者有毒,所以必然存在一些机制来确保输出装置的组装与生物合成同时进行或先于生物合成。天蓝色链霉菌通过一个多步骤途径产生聚酮类抗生素放线紫红素,该途径涉及由聚集在一起的基因编码的酶。在这个基因簇中嵌入了放线紫红素输出相关的基因,其中两个基因actR和actA类似于赋予四环素抗性的经典tetR和tetA阻遏物/外排泵编码基因对。与抑制tetA的TetR一样,ActR是actA的阻遏物。我们已经鉴定出几种可以解除ActR抑制作用的分子。重要的是,(S)-DNPA(放线紫红素生物合成途径中的一种中间体)和卡拉芬净(一种与中间体二氢卡拉芬净相关的分子)是特别有效的ActR配体。这表明,除了成熟的抗生素外,生物合成途径中的中间体可能会激活输出基因的表达,从而将输出与生物合成联系起来。我们认为这可能是许多生物活性天然产物生产中的一个共同特征。

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