ipso -Hydroxylation and Subsequent Fragmentation: a Novel Microbial Strategy To Eliminate Sulfonamide Antibiotics
0301 basic medicine
Sulfonamides
resistance genes
WASTEWATER TREATMENT; Sphingobium-xenophagum bayram; RESISTANCE GENES; BISPHENOL-A; BIODEGRADATION
waste-water treatment
Hydroxylation
NAD
biodegradation
cytochrome-p450
sphingobium-xenophagum bayram
Anti-Bacterial Agents
3. Good health
03 medical and health sciences
bisphenol-a
substitution
Actinomycetales
escherichia-coli
Environmental Pollutants
metabolism
Biotransformation
Metabolic Networks and Pathways
degradation
DOI:
10.1128/aem.00911-13
Publication Date:
2013-07-09T01:55:33Z
AUTHORS (12)
ABSTRACT
ABSTRACT
Sulfonamide antibiotics have a wide application range in human and veterinary medicine. Because they tend to persist in the environment, they pose potential problems with regard to the propagation of antibiotic resistance. Here, we identified metabolites formed during the degradation of sulfamethoxazole and other sulfonamides in
Microbacterium
sp. strain BR1. Our experiments showed that the degradation proceeded along an unusual pathway initiated by
ipso
-hydroxylation with subsequent fragmentation of the parent compound. The NADH-dependent hydroxylation of the carbon atom attached to the sulfonyl group resulted in the release of sulfite, 3-amino-5-methylisoxazole, and benzoquinone-imine. The latter was concomitantly transformed to 4-aminophenol. Sulfadiazine, sulfamethizole, sulfamethazine, sulfadimethoxine, 4-amino-
N
-phenylbenzenesulfonamide, and
N
-(4-aminophenyl)sulfonylcarbamic acid methyl ester (asulam) were transformed accordingly. Therefore,
ipso
-hydroxylation with subsequent fragmentation must be considered the underlying mechanism; this could also occur in the same or in a similar way in other studies, where biotransformation of sulfonamides bearing an amino group in the
para
-position to the sulfonyl substituent was observed to yield products corresponding to the stable metabolites observed by us.
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