AI Article Synopsis

  • Streptomyces sp. NTK937 produces the antibiotic caboxamycin and its methyl ester derivative, O-methylcaboxamycin, with the latter's synthesis involving genes located outside the primary biosynthetic cluster.
  • The caboxamycin gene cluster includes one regulatory gene and nine structural genes, of which five are essential for its production, while the other five have paralogues that can compensate if their cluster counterparts are inactive.
  • Genetic manipulation led to the discovery of a new compound, 3'-hydroxycaboxamycin, formed from the interaction between the caboxamycin and enterobactin biosynthetic pathways in a mutant strain lacking salicylate synthase.

Article Abstract

Streptomyces sp. NTK937, producer of benzoxazole antibiotic caboxamycin, produces in addition a methyl ester derivative, O-methylcaboxamycin. Caboxamycin cluster, comprising one regulatory and nine structural genes, has been delimited, and each gene has been individually inactivated to demonstrate its role in the biosynthetic process. The O-methyltransferase potentially responsible for O-methylcaboxamycin synthesis would reside outside this cluster. Five of the genes, cbxR, cbxA, cbxB, cbxD and cbxE, encoding a SARP transcriptional regulator, salicylate synthase, 3-oxoacyl-ACP-synthase, ACP and amidohydrolase, respectively, have been found to be essential for caboxamycin biosynthesis. The remaining five structural genes were found to have paralogues distributed throughout the genome, capable of partaking in the process when their cluster homologue is inactivated. Two of such paralogues, cbxC' and cbxI', coding an AMP-dependent synthetase-ligase and an anthranilate synthase, respectively, have been identified. However, the other three genes might simultaneously have more than one paralogue, given that cbxF (DAHP synthase), cbxG (2,3-dihydro-2,3-dihydroxybenzoate dehydrogenase) and cbxH (isochorismatase) have three, three and five putative paralogue genes, respectively, of similar function within the genome. As a result of genetic manipulation, a novel benzoxazole (3'-hydroxycaboxamycin) has been identified in the salicylate synthase-deficient mutant strain ΔcbxA. 3'-hydroxycaboxamycin derives from the cross-talk between the caboxamycin and enterobactin pathways.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5481532PMC
http://dx.doi.org/10.1111/1751-7915.12716DOI Listing

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Background: The biosynthesis pathway of benzoxazole compounds caboxamycin and nataxazole have been recently elucidated. Both compounds share one of their precursors, 3-hydroxyanthranilate (two units in the case of nataxazole). In addition, caboxamycin structure includes a salicylate moiety while 6-methylsalycilate is the third scaffold in nataxazole.

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Article Synopsis
  • Streptomyces sp. NTK937 produces the antibiotic caboxamycin and its methyl ester derivative, O-methylcaboxamycin, with the latter's synthesis involving genes located outside the primary biosynthetic cluster.
  • The caboxamycin gene cluster includes one regulatory gene and nine structural genes, of which five are essential for its production, while the other five have paralogues that can compensate if their cluster counterparts are inactive.
  • Genetic manipulation led to the discovery of a new compound, 3'-hydroxycaboxamycin, formed from the interaction between the caboxamycin and enterobactin biosynthetic pathways in a mutant strain lacking salicylate synthase.
View Article and Find Full Text PDF

Caboxamycin, a new benzoxazole antibiotic, was detected by HPLC-diode array screening in extracts of the marine strain Streptomyces sp. NTK 937, which was isolated from deep-sea sediment collected in the Canary Basin. The structure of caboxamycin was determined by mass spectrometry, NMR experiments and X-ray analysis.

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