The biosynthetic origin of the pyridone ring of efrotomycin

The biosynthetic origin of the pyridone ring of efrotomycin

Nocardia lactamdurans has been shown to catabolyse uracil via the reductive pathway. The end product of this pathway, beta-alanine, is incorporated into the pyridone ring of efrotomycin. Support for this proposal includes: (1) reversal of thymine inhibition of efrotomycin biosynthesis by dihydrourac...

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Veröffentlicht in:Journal of Industrial Microbiology 1991-11, Vol.8 (4), p.265-271
Hauptverfasser: DARLAND, G, ARISON, B, KAPLAN, L
Format: Artikel
Sprache:eng
Schlagworte:
Anti-Bacterial Agents - antagonists & inhibitors
Anti-Bacterial Agents - biosynthesis
Anti-Bacterial Agents - chemistry
Antibiotics (antibacterial agents, antifungal agents)
Antibiotics, microbial producers, chemotherapic agents, antiseptics, disinfecting agents
Applied microbiology
Biological and medical sciences
Biotechnology
Fermentation
Fundamental and applied biological sciences. Psychology
Microbiology
Molecular Structure
Mutagenesis
Nocardia - genetics
Nocardia - metabolism
Oxidation-Reduction
Pyridones - antagonists & inhibitors
Pyridones - chemistry
Thymidine - pharmacology
Thymine - pharmacology
Uracil - antagonists & inhibitors
Uracil - metabolism
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Zusammenfassung:Nocardia lactamdurans has been shown to catabolyse uracil via the reductive pathway. The end product of this pathway, beta-alanine, is incorporated into the pyridone ring of efrotomycin. Support for this proposal includes: (1) reversal of thymine inhibition of efrotomycin biosynthesis by dihydrouracil and N-carbamoyl-beta-aline, two intermediates of the catabolic pathway; (2) incorporation of [5,6-3H]-uracil into efrotomycin with a relative molar specific activity of approximately 0.5, close to the theoretical maximum; and (3) 13C coupling at C4 and C5 of efrotomycin after feeding resting cells with [4,5-13C]-uracil. Our results do not rule out the possibility of an alternative source of beta-alanine or the coexistence of uracil catabolism via oxidative reactions.
ISSN:0169-4146
1476-5535
DOI:10.1007/BF01576065