Two new tailoring enzymes, a glycosyltransferase and an oxygenase, involved in biosynthesis of the angucycline antibiotic urdamycin A in Streptomyces fradiae Tü2717
               This paper is dedicated to Professor Heinz Floss, a pioneer in the field of antibiotics, on the occasion of his 65th birthday.
            
            
               The GenBank accession numbers for the sequences reported in this paper are AF164960 and AF164961.

Faust, Bettina; Hoffmeister, Dirk; Weitnauer, Gabriele; Westrich, Lucia; Haag, Sabine; Schneider, Peter B.; Decker, Heinrich; Künzel, Eva; Rohr, Jürgen; Bechthold, Andreas

doi:10.1099/00221287-146-1-147

Cited by 97 publications

(85 citation statements)

References 29 publications

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“…3 With the revised sequences in hand, we can put LanM2/LndM2 proteins in the group of UrdM-like bifunctional reductases-oxygenases, 15,20 which are common for angucycline biosynthesis. Indeed, in most cloned gene clusters for angucycline biosynthesis we encounter lanM2/lndM2 homologues.…”

Section: Resultsmentioning

confidence: 99%

“…Rabelomycin (9) was isolated from the mutant S. fradiae ΔM. 14,20 The feeding experiments were carried out using the mutant S. globisporus F133 10 in which the PKS-associated fourth ring cyclase gene lndF was inactivated. Thus, this mutant cannot produce any correctly cyclized polyketides 10 but can still express all downstream enzymes necessary for the landomycin E production when fed with an intermediate containing a completed polyketide moiety.…”

Section: Feeding Experimentsmentioning

confidence: 99%

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Identification of the Function of Gene lndM2 Encoding a Bifunctional Oxygenase-Reductase Involved in the Biosynthesis of the Antitumor Antibiotic Landomycin E by Streptomyces globisporus 1912 Supports the Originally Assigned Structure for Landomycinone

et al. 2004

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The angucycline antibiotic family of the landomycins displays potent antitumor activity. To elucidate early post polyketide synthase (PKS) tailoring steps of the landomycin E biosynthetic pathway in Streptomyces globisporus 1912, the mutant S. globisporus M12 was prepared through gene replacement experiment of lndM2. It encodes an enzyme with putative oxygenase and reductase domains, according to sequencing of the gene and its counterpart lanM2 from S. cyanogenus S136 landomycin A biosynthetic gene cluster. The isolation of the novel shunt products 11-hydroxytetrangomycin and 4-hydroxytetrangomycin along with the well-known angucyclines tetrangomycin and tetrangulol from the culture of S. globisporus M12 provides evidence for the © 2005 American Chemical Society jrohr2@uky.edu. Supporting Information Available: Original NMR spectra obtained after the acetate feeding experiments on landomycin A and a newly generated 1 H NMR spectrum of natural landomycinone supporting the original landomycin structure. This material is available free of charge via the Internet at http://pubs.acs.org. NIH Public Access NIH-PA Author ManuscriptNIH-PA Author Manuscript NIH-PA Author Manuscript involvement of lndM2 in the early biosynthetic pathway of the landomycins, in particular in the formation of the alicyclic 6-hydroxy function of the landomycin aglycon. We therefore propose LndM2 to be responsible for both hydroxylation of the 6-position and its subsequent reduction. These reactions are necessary before the glycosylation reactions can occur. The results are in agreement with the originally published structure of landomycin but do not support the recently suggested revised structure.

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Section: Resultsmentioning

confidence: 99%

Section: Feeding Experimentsmentioning

confidence: 99%

Identification of the Function of Gene lndM2 Encoding a Bifunctional Oxygenase-Reductase Involved in the Biosynthesis of the Antitumor Antibiotic Landomycin E by Streptomyces globisporus 1912 Supports the Originally Assigned Structure for Landomycinone

et al. 2004

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“…Thus, as is the case for ActR, at least one step in the induction of the LanK target operon involves the interaction of the repressor with an immature landomycin intermediate. TFRs are also located in the biosynthesis clusters for the related angucyclinone antibiotics urdamycin and saquayamycin, but the role of these TFRs in regulating antibiotic biosynthesis and export has not been investigated (83,84).…”

Section: Tfrs Regulating Self-resistance In Antibiotic-producing Orgamentioning

confidence: 99%

The TetR Family of Regulators

Cuthbertson

Nodwell

2013

Microbiol Mol Biol Rev

465

512

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SUMMARY The most common prokaryotic signal transduction mechanisms are the one-component systems in which a single polypeptide contains both a sensory domain and a DNA-binding domain. Among the >20 classes of one-component systems, the TetR family of regulators (TFRs) are widely associated with antibiotic resistance and the regulation of genes encoding small-molecule exporters. However, TFRs play a much broader role, controlling genes involved in metabolism, antibiotic production, quorum sensing, and many other aspects of prokaryotic physiology. There are several well-established model systems for understanding these important proteins, and structural studies have begun to unveil the mechanisms by which they bind DNA and recognize small-molecule ligands. The sequences for more than 200,000 TFRs are available in the public databases, and genomics studies are identifying their target genes. Three-dimensional structures have been solved for close to 200 TFRs. Comparison of these structures reveals a common overall architecture of nine conserved α helices. The most important open question concerning TFR biology is the nature and diversity of their ligands and how these relate to the biochemical processes under their control.

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“…As a rare exception, a CGT that catalyzed the C-glucosylation of the siderophore enterobactin has been characterized in Escherichia coli (3). Similarly, an enzyme (UrdGT2) that C-conjugated a polyketide intermediate with D-olivose has also been identified as a component of the pathway leading to the biosynthesis of the antibiotic urdamycin A in Streptomyces fradiae (4,5). Analyses of the amino acid sequences of these two CGTs place them in family 1 of the 91 glycosyltransferase families classified to date (6).…”

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confidence: 99%

The C-Glycosylation of Flavonoids in Cereals

Brazier-Hicks

Evans

Gershater

et al. 2009

Journal of Biological Chemistry

265

262

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Flavonoids normally accumulate in plants as O-glycosylated derivatives, but several species, including major cereal crops, predominantly synthesize flavone-C-glycosides, which are stable to hydrolysis and are biologically active both in planta and as dietary components. An enzyme (OsCGT) catalyzing the UDPglucose-dependent C-glucosylation of 2-hydroxyflavanone precursors of flavonoids has been identified and cloned from rice (Oryza sativa ssp. indica), with a similar protein characterized in wheat (Triticum aestivum L.). OsCGT is a 49-kDa family 1 glycosyltransferase related to known O-glucosyltransferases. The recombinant enzyme C-glucosylated 2-hydroxyflavanones but had negligible O-glucosyltransferase activity with flavonoid acceptors. Enzyme chemistry studies suggested that OsCGT preferentially C-glucosylated the dibenzoylmethane tautomers formed in equilibrium with 2-hydroxyflavanones. The resulting 2-hydroxyflavanone-C-glucosides were unstable and spontaneously dehydrated in vitro to yield a mixture of 6C-and 8C-glucosyl derivatives of the respective flavones. In contrast, in planta, only the respective 6C-glucosides accumulated. Consistent with this selectivity in glycosylation product, a dehydratase activity that preferentially converted 2-hydroxyflavanone-Cglucosides to the corresponding flavone-6C-glucosides was identified in both rice and wheat. Our results demonstrate that cereal crops synthesize C-glucosylated flavones through the concerted action of a CGT and dehydratase acting on activated 2-hydroxyflavanones, as an alternative means of generating flavonoid metabolites.

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Cited by 97 publications

References 29 publications

Identification of the Function of Gene lndM2 Encoding a Bifunctional Oxygenase-Reductase Involved in the Biosynthesis of the Antitumor Antibiotic Landomycin E by Streptomyces globisporus 1912 Supports the Originally Assigned Structure for Landomycinone

Identification of the Function of Gene lndM2 Encoding a Bifunctional Oxygenase-Reductase Involved in the Biosynthesis of the Antitumor Antibiotic Landomycin E by Streptomyces globisporus 1912 Supports the Originally Assigned Structure for Landomycinone

The TetR Family of Regulators

The C-Glycosylation of Flavonoids in Cereals

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