首页> 外文OA文献 >Nystatin Biosynthesis and Transport: nysH and nysG Genes Encoding a Putative ABC Transporter System in Streptomyces noursei ATCC 11455 Are Required for Efficient Conversion of 10-Deoxynystatin to Nystatin
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Nystatin Biosynthesis and Transport: nysH and nysG Genes Encoding a Putative ABC Transporter System in Streptomyces noursei ATCC 11455 Are Required for Efficient Conversion of 10-Deoxynystatin to Nystatin

机译:制霉菌素的生物合成和运输:有效地将10-脱氧制霉菌素转化为制霉菌素需要在链霉菌ATCC 11455中编码推定的ABC转运蛋白系统的nysH和nysG基因。

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摘要

The genes nysH and nysG, encoding putative ABC-type transporter proteins, are located at the flank of the nystatin biosynthetic gene cluster in Streptomyces noursei ATCC 11455. To assess the possible roles of these genes in nystatin biosynthesis, they were inactivated by gene replacements leading to in-frame deletions. Metabolite profile analysis of the nysH and nysG deletion mutants revealed that both of them synthesized nystatin at a reduced level and produced considerable amounts of a putative nystatin analogue. Liquid chromatography-mass spectrometry and nuclear magnetic resonance structural analyses of the latter metabolite confirmed its identity as 10-deoxynystatin, a nystatin precursor lacking a hydroxyl group at C-10. Washing experiments demonstrated that both nystatin and 10-deoxynystatin are transported out of cells, suggesting the existence of an alternative efflux system(s) for the transport of nystatin-related metabolites. This notion was further corroborated in experiments with the ATPase inhibitor sodium o-vanadate, which affected the production of nystatin and 10-deoxynystatin in the wild-type strain and transporter mutants in a different manner. The data obtained in this study suggest that the efflux of nystatin-related polyene macrolides occurs through several transporters and that the NysH-NysG efflux system provides conditions favorable for C-10 hydroxylation.
机译:编码推定的ABC型转运蛋白的基因nysH和nysG位于牛链霉菌ATCC 11455中的制霉菌素生物合成基因簇的侧翼。为了评估这些基因在制霉菌素生物合成中的可能作用,它们被基因替换导致的失活删除框内。对nysH和nysG缺失突变体的代谢物谱分析表明,它们两者均以降低的水平合成制霉菌素,并产生大量推定的制霉菌素类似物。后者的代谢物的液相色谱-质谱和核磁共振结构分析证实了其与10-脱氧nystatin的身份,这是一种在C-10上没有羟基的制霉菌素前体。洗涤实验表明制霉菌素和10-脱氧制霉菌素均被转运出细胞,这表明存在与制霉菌素相关的代谢物的替代性外排系统。在实验中,ATPase抑制剂邻钒酸钠进一步证实了这一观点,后者以不同的方式影响野生型菌株和转运蛋白突变体中制霉菌素和10-脱氧制霉菌素的产生。在这项研究中获得的数据表明,制霉菌素相关的多烯大环内酯类化合物的流出是通过几种转运蛋白发生的,并且NysH-NysG的流出系统提供了有利于C-10羟基化的条件。

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