首页> 外文期刊>Applied and Environmental Microbiology >Pleiotropic Control of Secondary Metabolism and Morphological Development by KsbC, a Butyrolactone Autoregulator Receptor Homologue in Kitasatospora setae
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Pleiotropic Control of Secondary Metabolism and Morphological Development by KsbC, a Butyrolactone Autoregulator Receptor Homologue in Kitasatospora setae

机译:KsbC,丁内酯自调节器的丁内酯自动调节受体同源物对次生代谢和形态发育的多亲性控制。

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The γ-butyrolactone autoregulator signaling cascades have been shown to control secondary metabolism and/or morphological development among many Streptomyces species. However, the conservation and variation of the regulatory systems among actinomycetes remain to be clarified. The genome sequence of Kitasatospora setae, which also belongs to the family Streptomycetaceae containing the genus Streptomyces, has revealed the presence of three homologues of the autoregulator receptor: KsbA, which has previously been confirmed to be involved only in secondary metabolism; KsbB; and KsbC. We describe here the characterization of ksbC, whose regulatory cluster closely resembles the Streptomyces virginiae barA locus responsible for the autoregulator signaling cascade. Deletion of the gene ksbC resulted in lowered production of bafilomycin and a defect of aerial mycelium formation, together with the early and enhanced production of a novel β-carboline alkaloid named kitasetaline. A putative kitasetaline biosynthetic gene cluster was identified, and its expression in a heterologous host led to the production of kitasetaline together with JBIR-133, the production of which is also detected in the ksbC disruptant, and JBIR-134 as novel β-carboline alkaloids, indicating that these genes were biosynthetic genes for β-carboline alkaloid and thus are the first such genes to be discovered in bacteria.
机译:γ-丁内酯自调节信号转导级联已显示出可控制许多链霉菌物种中的次级代谢和/或形态发育。然而,放线菌之间的调节系统的保存和变化仍有待澄清。 Kitasatospora setae的基因组序列也属于含有Streptomyces属的 Streptomycetaceae 家族,该基因组揭示了自身调节受体的三个同源物:KsbA,先前已证实仅与次生代谢KsbB;和KsbC。我们在这里描述 ksbC 的特征,其调控簇与负责自动调控信号级联的 Streptomyces virginiae barA 位点非常相似。基因 ksbC 的缺失导致巴氟霉素的产量降低和气生菌丝体形成缺陷,以及新型和新颖的β-咔啉生物碱基他他林的早期生产和增强生产。确定了假定的基他他林生物合成基因簇,并且其在异源宿主中的表达导致了基他他林与JBIR-133的产生,在 ksbC 破坏剂和JBIR-中也检测到了该酶的产生。 134是新的β-咔啉生物碱,表明这些基因是β-咔啉生物碱的生物合成基因,因此是细菌中最早发现的此类基因。

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