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      Genetic organization of the biosynthetic gene cluster for the indolocarbazole K-252a in Nonomuraea longicatena JCM 11136.

      Applied Microbiology and Biotechnology
      Actinomycetales, enzymology, genetics, Carbazoles, metabolism, Cloning, Molecular, Genetic Engineering, Indole Alkaloids, Multigene Family, Streptomyces

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          Abstract

          Indolocarbazole metabolite K-252a is a natural product that was previously reported as a potent protein kinase C inhibitor with in vitro and in vivo potency. From a biosynthetic viewpoint, this compound possesses structurally interesting features such as an unusual furanosyl sugar moiety, which are absent in the well-studied staurosporine and rebeccamycin. A cosmid library from genomic DNA of Nonomuraea longicatena JCM 11136 was constructed and screened for the presence of genes to be involved in the biosynthesis of indolocarbazole K-252a. Using as a probe an internal fragment of vioB, a Chromobacterium violaceum gene encoding a multifunctional enzyme that catalyzes tryptophan decarboxylation and condensation reaction in violacein biosynthesis, we isolated a DNA region that directed the biosynthesis of K-252a when introduced into the heterologous expression host Streptomyces albus. Sequence analysis of 45 kb revealed genes for indolocarbazole core formation, glycosylation, and sugar methylation, as well as a regulatory gene and two resistance/secretion genes. The cloned genes should help to elucidate the molecular basis for indolocarbazole biosynthesis and generate new indolocarbazole analogues by genetic engineering.

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          Author and article information

          Journal
          17396254
          10.1007/s00253-007-0924-x

          Chemistry
          Actinomycetales,enzymology,genetics,Carbazoles,metabolism,Cloning, Molecular,Genetic Engineering,Indole Alkaloids,Multigene Family,Streptomyces

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