4.6 Article

Cyclofaulknamycin with the Rare Amino Acid D-capreomycidine Isolated from a Well-Characterized Streptomyces albus Strain

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MICROORGANISMS
卷 9, 期 8, 页码 -

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MDPI
DOI: 10.3390/microorganisms9081609

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D-capreomycidine; cyclofaulknamycin; cyclopeptide; Streptomyces

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Targeted genome mining is used to prioritize biosynthetic gene clusters, with this study identifying two different types containing capreomycidine biosynthesis genes and arginine hydroxylase gene respectively. Analysis of the flk cluster from Streptomyces albus led to the discovery of a cyclic peptide containing a rare D-capreomycidine moiety for the first time.
Targeted genome mining is an efficient method of biosynthetic gene cluster prioritization within constantly growing genome databases. Using two capreomycidine biosynthesis genes, alpha-ketoglutarate-dependent arginine beta-hydroxylase and pyridoxal-phosphate-dependent aminotransferase, we identified two types of clusters: one type containing both genes involved in the biosynthesis of the abovementioned moiety, and other clusters including only arginine hydroxylase. Detailed analysis of one of the clusters, the flk cluster from Streptomyces albus, led to the identification of a cyclic peptide that contains a rare D-capreomycidine moiety for the first time. The absence of the pyridoxal-phosphate-dependent aminotransferase gene in the flk cluster is compensated by the XNR_1347 gene in the S. albus genome, whose product is responsible for biosynthesis of the abovementioned nonproteinogenic amino acid. Herein, we report the structure of cyclofaulknamycin and the characteristics of its biosynthetic gene cluster, biosynthesis and bioactivity profile.

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