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18 results on '"Markus Fischer"'

1. Discovery and Development of a Small Molecule Library with Lumazine Synthase Inhibitory Activity

Author

Boris Illarionov, Gunda I. Georg, Adelbert Bacher, Mark Cushman, Qi Zhuang Ye, Meghan E. Breen, Arindam Talukdar, and Markus Fischer

Subjects
Stereochemistry, Stereoisomerism, Pyrimidinones, Article, Lumazine synthase, Small Molecule Libraries, Structure-Activity Relationship, chemistry.chemical_compound, Multienzyme Complexes, Schizosaccharomyces, Pyrimidinedione, Structure–activity relationship, Enzyme Inhibitors, chemistry.chemical_classification, Molecular Structure, biology, Organic Chemistry, Substrate (chemistry), Mycobacterium tuberculosis, biology.organism_classification, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein
Abstract

(E)-5-Nitro-6-(2-hydroxystyryl)pyrimidine-2,4(1H,3H)-dione (9) was identified as a novel inhibitor of Schizosaccharomyces pombe lumazine synthase by high-throughput screening of a 100000 compound library. The K(i) of 9 vs Mycobacterium tuberculosis lumazine synthase was 95 microM. Compound 9 is a structural analogue of the lumazine synthase substrate 5-amino-6-(d-ribitylamino)-2,4-(1H,3H)pyrimidinedione (1). This indicates that the ribitylamino side chain of the substrate is not essential for binding to the enzyme. Optimization of the enzyme inhibitory activity through systematic structure modification of the lead compound 9 led to (E)-5-nitro-6-(4-nitrostyryl)pyrimidine-2,4(1H,3H)-dione (26), which has a K(i) of 3.7 microM vs M. tuberculosis lumazine synthase.

Published
2009

2. Discovery and Development of the Covalent Hydrates of Trifluoromethylated Pyrazoles as Riboflavin Synthase Inhibitors with Antibiotic Activity Against Mycobacterium tuberculosis

Author

Adelbert Bacher, Yujie Zhao, Mark Cushman, Gunda I. Georg, Scott G. Franzblau, Baojie Wan, Markus Fischer, Phillip E. Fanwick, Qi Zhuang Ye, and Boris Illarionov

Subjects
Models, Molecular, Hydrocarbons, Fluorinated, Stereochemistry, Microbial Sensitivity Tests, Riboflavin Synthase, Mycobacterium tuberculosis, Structure-Activity Relationship, Riboflavin synthase, chemistry.chemical_compound, Minimum inhibitory concentration, Structure–activity relationship, Enzyme Inhibitors, chemistry.chemical_classification, Binding Sites, Trifluoromethyl, Molecular Structure, biology, Organic Chemistry, Water, Active site, Hydrogen Bonding, biology.organism_classification, Anti-Bacterial Agents, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Pyrazoles
Abstract

A high-throughput screening (HTS) hit compound displayed moderate inhibition of Mycobacterium tuberculosis and Escherichia coli riboflavin synthases. The structure of the hit compound provided by the commercial vendor was reassigned as [3-(4-chlorophenyl)-5-hydroxy-5-(trifluoromethyl)-4,5-dihydro-1H-pyrazol-1-yl](o-tolyl)methanone (18). The hit compound had a k(is) of 8.7 microM vs. M. tuberculosis riboflavin synthase and moderate antibiotic activity against both M. tuberculosis replicating phenotype and nonreplicating persistent phenotype. Molecular modeling studies suggest that two inhibitor molecules bind in the active site of the enzyme, and that the binding is stabilized by stacking between the benzene rings of two adjacent ligands. The most potent antibiotic in the series proved to be [5-(4-chlorophenyl)-5-hydroxy-3-(trifluoromethyl)-4,5-dihydro-1H-pyrazol-1-yl](m-tolyl)methanone (16), which displayed a minimum inhibitory concentration (MIC) of 36.6 microM vs. M. tuberculosis replicating phenotype and 48.9 microM vs. M. tuberculosis nonreplicating phenotype. The HTS hit compound and its analogues provide the first examples of riboflavin synthase inhibitors with antibiotic activity.

Published
2009

3. Synthesis and Enzyme Inhibitory Activity of the S-Nucleoside Analogue of the Ribitylaminopyrimidine Substrate of Lumazine Synthase and Product of Riboflavin Synthase

Author

Boris Illarionov, Arindam Talukdar, Markus Fischer, Adelbert Bacher, and Mark Cushman

Subjects
Models, Molecular, Pyrimidine, Stereochemistry, Nitro compound, Crystallography, X-Ray, Lumazine synthase, Substrate Specificity, Riboflavin Synthase, chemistry.chemical_compound, Riboflavin synthase, Biosynthesis, Multienzyme Complexes, Escherichia coli, Enzyme Inhibitors, chemistry.chemical_classification, biology, Organic Chemistry, Mycobacterium tuberculosis, Pyrimidine Nucleosides, B vitamins, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Bacillus subtilis
Abstract

Lumazine synthase and riboflavin synthase catalyze the last two steps in the biosynthesis of riboflavin. To obtain structural and mechanistic probes of these two enzymes, as well as inhibitors of potential value as antibiotics, a sulfur analogue of the pyrimidine substrate of the lumazine synthase-catalyzed reaction and product of the riboflavin synthase-catalyzed reaction was designed. Facile syntheses of the S-nucleoside 5-amino-6-(D-ribitylthio)pyrimidine-2,4(1H,3H)-dione hydrochloride (15) and its nitro precursor 5-nitro-6-(D-ribitylthio)pyrimidine-2,4(1H,3H)-dione (14) are described. These compounds were tested against lumazine synthase and riboflavin synthase obtained from a variety of microorganisms. Compounds 14 and 15 were found to be inhibitors of both riboflavin synthase and lumazine synthase. Compound 14 is an inhibitor of Bacillus subtilis lumazine synthase (Ki 26 microM), Schizosaccharomyces pombe lumazine synthase (Ki 2.0 microM), Mycobacterium tuberculosis lumazine synthase (Ki 11 microM), Escherichia coli riboflavin synthase (Ki 2.7 microM), and Mycobacterium tuberculosis riboflavin synthase (Ki 0.56 muM), while compound 15 is an inhibitor of B. subtilis lumazine synthase (Ki 2.6 microM), S. pombe lumazine synthase (Ki 0.16 microM), M. tuberculosis lumazine synthase (Ki 31 microM), E. coli riboflavin synthase (Ki 47 microM), and M. tuberculosis riboflavin synthase (Ki 2.5 microM).

Published
2007

4. Preparation of flavocoenzyme isotopologues by biotransformation of purines

Author

Stefan Weber, Adelbert Bacher, Wolfgang Eisenreich, Feng Zhu, Boris Illarionov, and Markus Fischer

Subjects
Riboflavin, Flavoprotein, Flavin group, Bacillus subtilis, medicine.disease_cause, Ligands, Cofactor, Riboflavin Synthase, Biotransformation, medicine, Escherichia coli, Purine metabolism, biology, Flavoproteins, Chemistry, Pteridines, Organic Chemistry, biology.organism_classification, Biochemistry, Purines, Isotope Labeling, biology.protein
Abstract

Isotope-labeled flavins are crucial reporters for many biophysical studies of flavoproteins. A purine-deficient Escherichia coli strain engineered for expression of the ribAGH genes of Bacillus subtilis converts isotope-labeled purine supplements into the riboflavin precursor, 6,7-dimethyl-8-ribityllumazine, with yields up to 40%. The fermentation products can subsequently be converted into isotope-labeled riboflavin and the cognate flavocoenzymes, FMN and FAD, by in vitro biotransformation with better than 90% yield. Using this approach, more than 100 single or multiple (13)C-, (15)N-, (17)O-, and (18)O-labeled isotopologues of these cofactors and ligands become easily accessible, enabling advanced ligand-based spectroscopy of flavoproteins and lumazine receptor proteins at unprecedented resolution.

Published
2015

5. Random Isotopolog Libraries for Protein Perturbation Studies. 13C NMR Studies on Lumazine Protein of Photobacterium leiognathi

Author

Wolfgang Eisenreich, Markus Fischer, Adelbert Bacher, Chan Yong Lee, and Boris Illarionov

Subjects
Magnetic Resonance Spectroscopy, Stereochemistry, Riboflavin, Molecular Sequence Data, Ligands, Structure-Activity Relationship, Riboflavin synthase, Bacterial Proteins, Photobacterium leiognathi, Escherichia coli, Side chain, Amino Acid Sequence, chemistry.chemical_classification, Carbon Isotopes, Molecular Structure, biology, Photobacterium, Chemistry, Ligand, Pteridines, Chemical shift, Organic Chemistry, Carbon-13, Stereoisomerism, Reference Standards, Carbon-13 NMR, Luminescent Proteins, Glucose, Enzyme, biology.protein, Genetic Engineering
Abstract

[graph: see text] Lumazine proteins of luminescent bacteria are paralogs of riboflavin synthase which are devoid of catalytic activity but bind the riboflavin synthase substrate, 6,7-dimethyl-8-ribityllumazine, with high affinity and are believed to serve as optical transponders for bioluminescence emission. Lumazine protein of Photobacterium leiognathi was expressed in a recombinant Escherichia coli host and was reconstituted with mixtures (random libraries) of 13C-labeled isotopologs of 6,7-dimethyl-8-ribityllumazine or riboflavin that had been prepared by biotransformation of [U-(13)C6]-, [1-(13)C1]-, [2-(13)C1]-, and [3-(13)C1]glucose. 13C NMR analysis of the protein/ligand complexes afforded the assignments of the 13C NMR chemical shifts for all carbon atoms of the protein-bound ligands by isotopolog abundance editing. The carbon atoms of the ribityl groups of both ligands studied were shifted up to 6 ppm upon binding to the protein. Chemical shift modulation of the side chain and chromophore carbon atoms due to protein/ligand interaction is discussed on the basis of the sequence similarity between lumazine protein and riboflavin synthase.

Published
2005

6. Rapid Preparation of Isotopolog Libraries by in Vivo Transformation of 13C-Glucose. Studies on 6,7-Dimethyl-8-ribityllumazine, a Biosynthetic Precursor of Vitamin B2

Author

and Adelbert Bacher, Wolfgang Eisenreich, Boris Illarionov, Markus Fischer, and Chan Yong Lee

Subjects
biology, Stereochemistry, Metabolite, Organic Chemistry, Bacillus subtilis, biology.organism_classification, medicine.disease_cause, Enterobacteriaceae, chemistry.chemical_compound, chemistry, Biochemistry, Biosynthesis, Yield (chemistry), medicine, Ammonium chloride, Fermentation, Escherichia coli
Abstract

An Escherichia coli strain engineered for expression of the ribABGH genes of Bacillus subtilis was shown to produce 100 mg of the riboflavin precursor 6,7-dimethyl-8-ribityllumazine per liter of minimal medium. Growth of the recombinant strain in medium supplemented with [U-13C6]glucose and/or 15NH4Cl as single sources of carbon and/or nitrogen afforded 6,7-dimethyl-8-ribityllumazine universally labeled with 13C and/or 15N. The yield of [U-13C13]-6,7-dimethyl-8-ribityllumazine based on [U-13C6]glucose was 25 mg/g. Fermentation with [1-13C1]-, [2-13C1]-, or [3-13C1]glucose afforded mixtures of 6,7-dimethyl-8-ribityllumazine isotopologs, predominantly with 13C enrichment of single carbon atoms. The isotope-labeled samples enabled a comprehensive NMR analysis of 6,7-dimethyl-8-ribityllumazine. Isotopolog libraries of a wide variety of microbial metabolites can be produced by the same experimental approach.

Published
2004

7. 19F NMR Ligand Perturbation Studies on 6,7-Bis(trifluoromethyl)-8-ribityllumazine-7-hydrates and the Lumazine Synthase Complex of Bacillus subtilis. Site-Directed Mutagenesis Changes the Mechanism and the Stereoselectivity of the Catalyzed Haloform-Type Reaction

Author

Sevil Weinkauf, Markus Fischer, Johannes Scheuring, Mark Cushman, Adelbert Bacher, and Karl Kugelbrey

Subjects
chemistry.chemical_classification, biology, Chemistry, Stereochemistry, Organic Chemistry, Riboflavin synthase activity, Fluorine-19 NMR, Bacillus subtilis, biology.organism_classification, Lumazine synthase, Riboflavin synthase, Enzyme, biology.protein, Epimer, Site-directed mutagenesis
Abstract

The riboflavin synthase/lumazine synthase complex of Bacillus subtilis catalyzes the last two steps in riboflavin biosynthesis. The protein comprises a capsid of 60 β subunits with lumazine synthase activity and a core of three α subunits with riboflavin synthase activity. The β subunits catalyze the formation of 6,7-dimethyl-8-ribityllumazine (3) from 5-amino-6-ribitylamino-2,4(1H,3H)-pyrimidinedione (1) and 3,4-dihydroxy-2-butanone 4-phosphate (2). Complexes of recombinant lumazine synthase (β60 capsids) with 6-trifluoromethyl-7-oxo-8-ribityllumazine (10) as well as 7S- or 7R-6,7-bistrifluoromethyl-8-ribityllumazine hydrate (11) were studied by 19F NMR spectroscopy. Despite the large molecular weight of approximately 960 kDa of the protein, spectra with separated signals of free and bound ligand could be obtained. An unusually large shift difference of 8 ppm was observed between the 7-trifluoromethyl signals of free and bound ligand for epimer B of 11 and the enzyme. The signal is sensitive to the repla...

Published
2001

8. O-Nucleoside, S-nucleoside, and N-nucleoside probes of lumazine synthase and riboflavin synthase

Author

Adelbert Bacher, Boris Illarionov, Yujie Zhao, Arindam Talukdar, Wei Lv, Markus Fischer, and Mark Cushman

Subjects
chemistry.chemical_classification, Models, Molecular, biology, Stereochemistry, Organic Chemistry, Nitro compound, Molecular Conformation, Nucleosides, Molecular Dynamics Simulation, Chemical synthesis, Lumazine synthase, Article, Riboflavin Synthase, B vitamins, Riboflavin synthase, chemistry.chemical_compound, Structure-Activity Relationship, Enzyme, chemistry, Biosynthesis, Multienzyme Complexes, biology.protein, heterocyclic compounds, Enzyme Inhibitors, Nucleoside
Abstract

Lumazine synthase catalyzes the penultimate step in the biosynthesis of riboflavin, while riboflavin synthase catalyzes the last step. O-Nucleoside, S-nucleoside, and N-nucleoside analogues of hypothetical lumazine biosynthetic intermediates have been synthesized in order to obtain structure and mechanism probes of these two enzymes, as well as inhibitors of potential value as antibiotics. Methods were devised for the selective cleavage of benzyl protecting groups in the presence of other easily reduced functionality by controlled hydrogenolysis over Lindlar catalyst. The deprotection reaction was performed in the presence of other reactive functionality including nitro groups, alkenes, and halogens. The target compounds were tested as inhibitors of lumazine synthase and riboflavin synthase obtained from a variety of microorganisms. In general, the S-nucleosides and N-nucleosides were more potent than the corresponding O-nucleosides as lumazine synthase and riboflavin synthase inhibitors, while the C-nucleosides were the least potent. A series of molecular dynamics simulations followed by free energy calculations using the Poisson-Boltzmann/surface area (MM-PBSA) method were carried out in order to rationalize the results of ligand binding to lumazine synthase, and the results provide insight into the dynamics of ligand binding as well as the molecular forces stabilizing the intermediates in the enzyme-catalyzed reaction.

Published
2012

9. Preparation of functionalized cyclic enol phosphates by halogen-magnesium exchange and directed deprotonation reactions

Author

Paul Knochel, Tomke Bresser, Fabian M. Piller, and Markus Fischer

Subjects
Cyclic compound, Chemistry, Magnesium, Organic Chemistry, chemistry.chemical_element, Cycloparaffins, Enol, Chemical synthesis, Catalysis, Camphor, Phosphates, chemistry.chemical_compound, Structure-Activity Relationship, Deprotonation, Halogens, Acyl chloride, Amide, Electrophile, Polymer chemistry, Indicators and Reagents, Protons
Abstract

Cyclic enol phosphates were magnesiated by a halogen/magnesium exchange reaction or deprotonation using TMP-derived magnesium amide bases. The resulting magnesium reagents react readily with a wide range of electrophiles like allyl bromides and acid chlorides or can be used in Pd-catalyzed cross-coupling reactions. Several optically pure enol phosphates were prepared starting from readily available d-(+)-camphor derivatives.

Published
2010

10. A new series of N-[2,4-dioxo-6-d-ribitylamino-1,2,3,4-tetrahydropyrimidin-5-yl]oxalamic acid derivatives as inhibitors of lumazine synthase and riboflavin synthase: design, synthesis, biochemical evaluation, crystallography, and mechanistic implications

Author

Ekaterina Morgunova, Guangyi Jin, Adelbert Bacher, Mark Cushman, Markus Fischer, Boris Illarionov, Rudolf Ladenstein, and Yanlei Zhang

Subjects
Models, Molecular, Conformational change, Stereochemistry, Bacillus subtilis, medicine.disease_cause, Crystallography, X-Ray, Lumazine synthase, Riboflavin Synthase, chemistry.chemical_compound, Riboflavin synthase, Structure-Activity Relationship, Biosynthesis, Multienzyme Complexes, Schizosaccharomyces, medicine, Escherichia coli, Enzyme Inhibitors, Oxamic Acid, Schiff base, biology, Molecular Structure, Organic Chemistry, Stereoisomerism, Mycobacterium tuberculosis, biology.organism_classification, Kinetics, chemistry, Biochemistry, Schizosaccharomyces pombe, biology.protein
Abstract

The penultimate step in the biosynthesis of riboflavin is catalyzed by lumazine synthase. Three metabolically stable analogues of the hypothetical intermediate proposed to arise after phosphate elimination in the lumazine synthase-catalyzed reaction were synthesized and evaluated as lumazine synthase inhibitors. All three intermediate analogues were inhibitors of Mycobacterium tuberculosis lumazine synthase, Bacillus subtilis lumazine synthase, and Schizosaccharomyces pombe lumazine synthase, while one of them proved to be an extremely potent inhibitor of Escherichia coli riboflavin synthase with a Ki of 1.3 nM. The crystal structure of M. tuberculosis lumazine synthase in complex with one of the inhibitors provides a model of the conformation of the intermediate occurring immediately after phosphate elimination, supporting a mechanism in which phosphate elimination occurs before a conformational change of the Schiff base intermediate toward a cyclic structure.

Published
2008

11. A new series of 3-alkyl phosphate derivatives of 4,5,6,7-tetrahydro-1-D-ribityl-1H-pyrazolo[3,4-d]pyrimidinedione as inhibitors of lumazine synthase: design, synthesis, and evaluation

Author

Guangyi Jin, Boris Illarionov, Yanlei Zhang, Markus Fischer, Adelbert Bacher, and Mark Cushman

Subjects
biology, Stereochemistry, Organic Chemistry, Pyrimidinones, Alkylation, Chemical synthesis, Lumazine synthase, Pyrazolopyrimidine, Organophosphates, Acylation, B vitamins, chemistry.chemical_compound, chemistry, Biosynthesis, Multienzyme Complexes, biology.protein, Pyrimidinedione, Pyrazoles, Enzyme Inhibitors
Abstract

Lumazine synthase catalyzes the penultimate step in the biosynthesis of riboflavin. A homologous series of three pyrazolopyrimidine analogues of a hypothetical intermediate in the lumazine synthase-catalyzed reaction were synthesized and evaluated as lumazine synthase inhibitors. The key steps of the synthesis were C-5 deprotonation of 4-chloro-2,6-dimethoxypyrimidine, acylation of the resulting anion, and conversion of the product to a pyrazolopyrimidine with hydrazine. Alkylation of the pyrazolopyrimidine with a substituted ribityl iodide and deprotection of the ribityl chain afforded the final set of three products. All three compounds were extremely potent inhibitors of the lumazine synthases of Mycobacterium tuberculosis, Magnaporthe grisea, Candida albicans, and Schizosaccharomyces pombe lumazine synthase, with inhibition constants in the low nanomolar to subnanomolar range. Molecular modeling of one of the homologues bound to Mycobacterium tuberculosis lumazine synthase suggests that both the hypothetical intermediate in the lumazine synthase-catalyzed reaction pathway and the metabolically stable analogues bind similarly.

Published
2007

12. A novel lumazine synthase inhibitor derived from oxidation of 1,3,6,8-tetrahydroxy-2,7-naphthyridine to a tetraazaperylenehexaone derivative

Author

Yanlei Zhang, Boris Illarionov, Qi Zhuang Ye, David Vander Velde, Markus Fischer, Phillip E. Fanwick, Yunlong Song, Gunda Georg, Adelbert Bacher, and Mark Cushman

Subjects
Reaction mechanism, Stereochemistry, Crystallography, X-Ray, Lumazine synthase, Article, chemistry.chemical_compound, Non-competitive inhibition, Heterocyclic Compounds, Multienzyme Complexes, Schizosaccharomyces, Phenol, Phenols, Enzyme Inhibitors, Naphthyridines, Perylene, Aza Compounds, biology, Molecular Structure, Chemistry, Organic Chemistry, Kinetics, biology.protein, Oxidative coupling of methane, Oxidation-Reduction, Derivative (chemistry)
Abstract

Air oxidation of 1,3,6,8-tetrahydroxy-2,7-naphthyridine afforded 2,5,8,11-tetraaza-5,11-dihydro-4,10-dihydroxyperylene-1,3,6,7,9,12-hexaone. X-ray crystallography of the product revealed that it exists in the meso form in the solid state. The mechanism of product formation most likely involves oxidative phenolic coupling and oxidation. The product proved to be a competitive inhibitor of Schizosaccharomyces pombe lumazine synthase with a Ki of 66+/-13 microM in Tris buffer and 22+/-4 microM in phosphate buffer. This is significantly more potent than the reactant (Ki 350+/-76 microM, competitive inhibition), which had previously been identified as a lumazine synthase inhibitor by high-throughput screening. Ab initio calculations indicate that the meso form is slightly less stable than the enantiomeric form, and that the two forms interconvert rapidly at room temperature.

Published
2007

13. Design, synthesis, and biochemical evaluation of 1,5,6,7-tetrahydro-6,7-dioxo-9-D-ribitylaminolumazines bearing alkyl phosphate substituents as inhibitors of lumazine synthase and riboflavin synthase

Author

Mark, Cushman, Guangyi, Jin, Thota, Sambaiah, Boris, Illarionov, Markus, Fischer, Rudolf, Ladenstein, and Adelbert, Bacher

Subjects
Models, Molecular, Stereochemistry, Antitubercular Agents, Chemical synthesis, Lumazine synthase, Article, Riboflavin Synthase, Riboflavin synthase, chemistry.chemical_compound, Biosynthesis, Multienzyme Complexes, Binding site, Enzyme Inhibitors, chemistry.chemical_classification, biology, Molecular Structure, Pteridines, Organic Chemistry, Alkyl phosphate, Mycobacterium tuberculosis, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Bacillus subtilis
Abstract

The last two steps in the biosynthesis of riboflavin, an essential metabolite that is involved in electron transport, are catalyzed by lumazine synthase and riboflavin synthase. In order to obtain structural probes and inhibitors of these two enzymes, two ribityllumazinediones bearing alkyl phosphate substituents were synthesized. The synthesis involved the generation of the ribityl side chain, the phosphate side chain, and the lumazine system in protected form, followed by the simultaneous removal of three different types of protecting groups. The products were designed as intermediate analog inhibitors of lumazine synthase that would bind to its phosphate-binding site as well as its lumazine binding site. Both compounds were found to be effective inhibitors of both Bacillus subtilis lumazine synthase as well as Escherichia coli riboflavin synthase. Molecular modeling of the binding of one of the two compounds provided a structural explanation for how these compounds are able to effectively inhibit both enzymes. In phosphate-free buffer, the phosphate moieties of the inhibitors were found to contribute positively to their binding to Mycobacterium tuberculosis lumazine synthase, resulting in very potent inhibitors with Ki values in the low nanomolar range. The additional carbonyl in the dioxolumazine system vs. the purinetrione system was found to make a positive contribution to its binding to E. coli riboflavin synthase.

Published
2005

14. Design, synthesis, and evaluation of acyclic C-nucleoside and N-methylated derivatives of the ribitylaminopyrimidine substrate of lumazine synthase as potential enzyme inhibitors and mechanistic probes

Author

Boris Illarionov, Markus Fischer, Jinhua Chen, Adelbert Bacher, Mark Cushman, and Thota Sambaiah

Subjects
Models, Molecular, Stereochemistry, Riboflavin, Nitro compound, Substituent, Molecular Conformation, Chemical synthesis, Methylation, Lumazine synthase, Riboflavin Synthase, chemistry.chemical_compound, Riboflavin synthase, Biosynthesis, Multienzyme Complexes, Moiety, Enzyme Inhibitors, chemistry.chemical_classification, biology, Organic Chemistry, food and beverages, Substrate (chemistry), General Medicine, Pyrimidine Nucleosides, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Nucleic acid
Abstract

Lumazine synthase and riboflavin synthase catalyze the last two steps in the biosynthesis of riboflavin, a vitamin that is involved in many critical biochemical reactions that are essential for the maintenance of life. To obtain inhibitors and structural probes that could be useful in studying the structures of bound reaction intermediates, the ribitylamino N-H moiety of the lumazine synthase substrate was replaced by CH(2) and N-CH(3) groups. The CH(2) replacement unexpectedly and completely abolished the affinity for lumazine synthase, thus revealing a critical, yet unexplained, role of the ribitylamino N-H moiety in conferring affinity for the enzyme. In contrast, the N-CH(3) replacement resulted in an inhibitor of both lumazine synthase and riboflavin synthase. Replacement of the ribitylamino N-H moiety with epimeric C-F moieties led to inhibition of lumazine synthase and riboflavin synthase when combined with the replacement of the 5-amino group with a nitro substituent.

Published
2004

15. Design, synthesis, and evaluation of 9-D-ribitylamino-1,3,7,9-tetrahydro-2,6,8-purinetriones bearing alkyl phosphate and alpha,alpha-difluorophosphonate substituents as inhibitors of tiboflavin synthase and lumazine synthase

Author

Adelbert Bacher, Mark Cushman, Boris Illarionov, Guangyi Jin, Markus Fischer, and Thota Sambaiah

Subjects
Models, Molecular, Stereochemistry, Organophosphonates, Alkylation, Chemical synthesis, Binding, Competitive, Lumazine synthase, Riboflavin Synthase, Riboflavin synthase, chemistry.chemical_compound, Biosynthesis, Multienzyme Complexes, Escherichia coli, Enzyme Inhibitors, Ribitol, chemistry.chemical_classification, biology, ATP synthase, Organic Chemistry, Alkyl phosphate, Organophosphates, Recombinant Proteins, Kinetics, Enzyme, chemistry, Purines, Drug Design, biology.protein, Bacillus subtilis
Abstract

Lumazine synthase and riboflavin synthase catalyze the last two steps in the biosynthesis of riboflavin, an essential metabolite that is involved in electron transport processes. To obtain structural probes of these two enzymes, as well as inhibitors of potential value as antibiotics, a series of ribitylpurinetriones bearing alkyl phosphate and alpha,alpha-difluorophosphonate substituents were synthesized. Since the purinetrione ring system and the ribityl hydroxyl groups can be alkylated, the synthesis required the generation of these two moieties in protected form before the desired alkylation reaction could be carried out. These substances were designed as intermediate analogue inhibitors of lumazine synthase that would bind to its phosphate-binding site. All of the compounds were found to be effective inhibitors of both Bacillus subtilis lumazine synthase as well as Escherichia coli riboflavin synthase. Molecular modeling of the binding of 3-(1,3,7,9-tetrahydro-9-D-ribityl-2,6,8-trioxopurin-7-yl)propane 1-phosphate provided a structural explanation for how these compounds are able to effectively inhibit both enzymes. Interestingly, the enzyme kinetics of these new compounds in comparison with the parent purinetrione demonstrated unexpectedly that the phosphate and phosphonate substituents contributed negatively to the binding. A possible explanation for these effects on lumazine synthase would be that the inorganic phosphate in the assay buffer competes with the substituted purinetriones for binding to the enzyme. This would be consistent with the observed increase in K(m) of the 3,4-dihydroxybutanone-4-phosphate substrate from 5.2 microM in Tris buffer or from 6.7 microM in MOPS buffer to 50 microM in phosphate buffer when tested on Bacillus subtilis lumazine synthase. However, when tested in Tris buffer vs Mycobacterium tuberculosis lumazine synthase, three of the phosphate inhibitors displayed inhibition constants in the 4-5 nM range, indicating that they are much more potent than the parent purinetrione. Under these conditions, the phosphate moieties of the inhibitors do contribute positively to their binding. The alpha,alpha-difluorophosphonate analogue, which is expected to have enhanced metabolic stability relative to the phosphates, was also found to be an inhibitor of Mycobacterium tuberculosis lumazine synthase with a K(i) of 60 nM.

Published
2004

16. Incorporation of an amide into 5-phosphonoalkyl-6-D-ribitylaminopyrimidinedione lumazine synthase inhibitors results in an unexpected reversal of selectivity for riboflavin synthase vs lumazine synthase

Author

Stefan Gerhardt, Jeffrey T. Mihalic, Donglai Yang, Jinhua Chen, Adelbert Bacher, Mark Cushman, Klaus Kis, Robert Huber, and Markus Fischer

Subjects
Models, Molecular, Magnetic Resonance Spectroscopy, Stereochemistry, Protein Conformation, Pyrimidinones, Crystallography, X-Ray, Ligands, Lumazine synthase, Riboflavin Synthase, Riboflavin synthase, Structure-Activity Relationship, Multienzyme Complexes, Escherichia coli, Enzyme Inhibitors, Glutamine amidotransferase, chemistry.chemical_classification, Binding Sites, ATP synthase, biology, Molecular Structure, Chemistry, Pteridines, Organic Chemistry, Active site, Ligand (biochemistry), Amides, Kinetics, Enzyme, Biochemistry, Enzyme inhibitor, Drug Design, biology.protein
Abstract

Several analogues of a hypothetical intermediate in the reaction catalyzed by lumazine synthase were synthesized and tested as inhibitors of both Bacillus subtilis lumazine synthase and Escherichia coli riboflavin synthase. The new compounds were designed by replacement of a two-carbon fragment of several 5-phosphonoalkyl-6-D-ribitylaminopyrimidinedione lumazine synthase inhibitors with an amide linkage that was envisioned as an analogue of a Schiff base moiety of a hypothetical intermediate in the enzyme-catalyzed reaction. The incorporation of the amide group led to an unexpected reversal in selectivity for inhibition of lumazine synthase vs riboflavin synthase. Whereas the parent 5-phosphonoalkyl-6-D-ribitylaminopyrimidinediones were lumazine synthase inhibitors and did not inhibit riboflavin synthase, the amide-containing derivatives inhibited riboflavin synthase and were only very weak or inactive as lumazine synthase inhibitors. Molecular modeling of inhibitor-lumazine synthase complexes did not reveal a structural basis for these unexpected findings. However, molecular modeling of one of the inhibitors with E. coli riboflavin synthase demonstrated that the active site of the enzyme could readily accommodate two ligand molecules.

Published
2002

17. Investigation of the binding of epimer A of the covalent hydrate of 6,7-bis(trifluoromethyl)-8-D-ribityllumazine to a recombinant F22W Bacillus subtilis lumazine synthase mutant by (15)N[(19)F] REDOR NMR

Author

Jacob Schaefer, Daniel R. Studelska, Anil K. Mehta, Kristina Kemter, Andreas Giessauf, Cushman Mark S, Adelbert Bacher, and Markus Fischer

Subjects
Fluorine Radioisotopes, Magnetic Resonance Spectroscopy, Stereochemistry, Macromolecular Substances, Molecular Conformation, Bacillus subtilis, Crystallography, X-Ray, Lumazine synthase, Catalysis, Riboflavin Synthase, Riboflavin synthase, chemistry.chemical_compound, Multienzyme Complexes, Side chain, Trifluoromethyl, Binding Sites, Nitrogen Radioisotopes, biology, Bicyclic molecule, Molecular Structure, Chemistry, Pteridines, Organic Chemistry, Stereoisomerism, Fluorine, biology.organism_classification, Kinetics, Covalent bond, biology.protein, Epimer, Protein Binding
Abstract

The two epimeric covalent hydrates A and B of 6,7-bis(trifluoromethyl)-8-D-ribityllumazine are metabolically stable analogues of hypothetical intermediates proposed in the reactions catalyzed by riboflavin synthase and lumazine synthase. To confirm the stereochemical assignments previously based solely on results for epimer B, a 15 N{ 19 F} REDOR NMR study was performed on the complex formed from epimer A and a recombinant, uniformly 15 N-labeled F22W mutant of Bacillus subtilis lumazine synthase. The results indicate that the fluorines of the ligands are closer to the side chain nitrogens of Arg127 and farther away from the side chain nitrogens of Lys135 in epimer B than in epimer A. These results are consistent with the assignment of the earlier 7R configuration of epimer A and the 7S configuration of epimer B.

Published
2002

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