Your search keyword '"S.V. Revtovich"' showing total 29 results

1. Conjugates of methionine γ-lyase with polysialic acid: Two approaches to antitumor therapy

Author

Elena A. Morozova, Tatyana V. Demidkina, Natalya V. Anufrieva, V. Timofeeva, A. Solovieva, Vasily Koval, E. Lesnova, S.V. Revtovich, A. Kushch, and Vitalia V. Kulikova

Subjects

Antineoplastic Agents, 02 engineering and technology, Conjugated system, Biochemistry, Mice, 03 medical and health sciences, chemistry.chemical_compound, Structural Biology, Cell Line, Tumor, Neoplasms, Animals, Humans, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, Mice, Inbred BALB C, 0303 health sciences, Methionine, Polysialic acid, General Medicine, Metabolism, 021001 nanoscience & nanotechnology, Lyase, In vitro, Carbon-Sulfur Lyases, Kinetics, Enzyme, chemistry, Cancer cell, MCF-7 Cells, Sialic Acids, Female, 0210 nano-technology

Abstract

The methionine dependence is a well known phenomenon in metabolism of cancer cells. Methionine γ-lyase (EC 4.4.1.11, MGL) catalyzes the γ-elimination reaction of L-methionine and thus could effectively inhibit the growth of malignant cells. Recently we have demonstrated that the mutant form of the enzyme C115H MGL can be used as a component of the pharmacological pair enzyme/S-(allyl/alkyl)-L-cysteine sulfoxides to yield thiosulfinates in situ. Thiosulfinates were shown to be toxic to various cancer cell lines. Therefore the application of the enzyme in enzyme pro-drug therapy may be promising. The conjugates of MGL and C115H MGL with polysialic acid were obtained and their kinetic and pharmacokinetic parameters were determined. The formation of polysialic shell around the enzyme was confirmed by atomic force microscopy. The half-life of conjugated enzymes increased 3–6 times compared to the native enzyme. The cytotoxic effect of conjugated MGL against methionine dependent cancer cell lines was increased two times compared to the values for the native enzymes. The anticancer efficiency of thiosulfinates produced by pharmacological pair C115H MGL/S-(allyl/alkyl)-L-cysteine sulfoxides was demonstrated in vitro. The results indicate that the conjugates of MGL with polysialic acid could be new antitumor drugs.

Published

2021

2. Encapsulated Methionine γ‑Lyase: Application in Enzyme Prodrug Therapy of Pseudomonas aeruginosa Infection

Author

Vitalia V. Kulikova, Lada Lebedeva, Elena A. Morozova, Egor Burmistrov, Marina Yu. Chernukha, Vasily Koval, Tatyana V. Demidkina, I.A. Shaginyan, Natalya V. Anufrieva, Lusine Avetisyan, S.V. Revtovich, and Olga Medvedeva

Subjects

chemistry.chemical_classification, Methionine, Pseudomonas aeruginosa, General Chemical Engineering, Mutant, General Chemistry, Prodrug, Lyase, medicine.disease, medicine.disease_cause, Cystic fibrosis, Microbiology, chemistry.chemical_compound, Chemistry, Enzyme, chemistry, Lung disease, medicine, QD1-999

Abstract

Lung disease caused by Pseudomonas aeruginosa is the leading reason for death in cystic fibrosis patients. Therapeutic efficacy of the pharmacological pairs, the naked/encapsulated mutant form of C...

Published

2020

3. Sulfoxides of sulfur-containing amino acids are suicide substrates of Citrobacter freundii methionine γ-lyase. Structural bases of the enzyme inactivation

Author

Tatyana V. Demidkina, Vitalia V. Kulikova, Vasiliy S. Koval, S.V. Revtovich, Elena A. Morozova, Natalya V. Anufrieva, and Alexei Nikulin

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, Ligands, Biochemistry, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, Cysteine, Amino Acids, Thiosulfinate, chemistry.chemical_classification, Methionine, 030102 biochemistry & molecular biology, biology, General Medicine, Lyase, biology.organism_classification, Citrobacter freundii, Amino acid, Carbon-Sulfur Lyases, Kinetics, 030104 developmental biology, Enzyme, chemistry, Sulfoxides

Abstract

Interactions of Citrobacter freundii methionine γ-lyase (MGL) with sulfoxides of typical substrates were investigated. It was found that sulfoxides are suicide substrates of the enzyme. The products of the β- and γ-elimination reactions of sulfoxides, thiosulfinates, oxidize three cysteine residues of the enzyme. Three-dimensional structures of MGL inactivated by dimethyl thiosulfinate and diethyl thiosulfinate were determined at 1.46 A and 1.59 A resolution. Analysis of the structures identified SH groups oxidized by thiosulfinates and revealed the structural bases of MGL inactivation. The extent of inactivation of MGL in the catalysis of the β-elimination reaction depends on the length of the «tail» at oxidized Cys115. Oxidation of Cys115 results in MGL incapable to catalyze the stage of methyl mercaptan elimination of the physiological reaction.

Published

2020

4. Methionine γ-lyase in enzyme prodrug therapy: An improvement of pharmacokinetic parameters of the enzyme

Author

Alexey N. Minakov, Georgij B Telegin, Natalya V. Anufrieva, Alexandr S. Chernov, Vitalia V. Kulikova, Vasily Koval, Elena A. Morozova, Tatyana V. Demidkina, and S.V. Revtovich

Subjects

Microbial Sensitivity Tests, 02 engineering and technology, Biochemistry, Polyethylene Glycols, 03 medical and health sciences, chemistry.chemical_compound, Anti-Infective Agents, Structural Biology, In vivo, Animals, Prodrugs, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, Mice, Inbred BALB C, 0303 health sciences, Methionine, biology, Biological activity, General Medicine, Prodrug, 021001 nanoscience & nanotechnology, Lyase, biology.organism_classification, Citrobacter freundii, Carbon-Sulfur Lyases, Enzyme, chemistry, Liposomes, Female, 0210 nano-technology, Antibacterial activity

Abstract

Citrobacter freundii methionine γ-lyase (MGL), in addition to the physiological reaction, catalyzes the β-elimination reaction of S-alk(en)yl-L-cysteine sulfoxides to yield thiosulfinates, which have antibacterial activity. We have obtained the mutant form C115H MGL, which cleaves S-alk(en)yl-L-cysteine sulfoxides more effectively than the wild type enzyme does. The binary system MGL/S-alk(en)yl-L-cysteine sulfoxides may be considered as a new pharmacological pair in enzyme prodrug therapy (EPT). Despite of the successful application of this pair in antibacterial studies in vitro, in vivo experiments may lead to several problems typical of therapeutic proteins including a relatively short-lasting biological activity. To circumvent these problems, we have investigated several approaches to improve safety and efficacy of the enzyme component of the pharmacological pair. This included covalent attachment of poly(ethylene glycol) to the enzyme, its encapsulation in liposomes and polymeric vesicles (PICsomes). The steady-state and pharmacokinetic parameters of modified/encapsulated enzyme were determined. It was demonstrated that the encapsulation in PICsomes prolongs in vivo stability of C115H MGL to over 42 h compared to PEGylated enzyme (3 h). Antibacterial activity of binary system (“pharmacological pair”) modified/encapsulated enzyme/S-alk(en)yl-L-cysteine sulfoxides was tested and remained the same as for the naked enzyme. Thus, the usage of MGL-loaded PICsomes as enzymatic nanoreactors in ETP to produce antimicrobial thiosulfinates is promising.

Published

2019

5. Identification ofO‐acetylhomoserine sulfhydrylase, a putative enzyme responsible for methionine biosynthesis inClostridioides difficile: Gene cloning and biochemical characterizations

Author

Elena A. Morozova, Yury Belyi, Natalya V. Anufrieva, S.V. Revtovich, Mikhail I. Kotlov, Vasiliy S. Koval, Bazhulina Np, Tatyana V. Demidkina, Hideyuki Hayashi, and Vitalia V. Kulikova

Subjects

0301 basic medicine, Carbon-Oxygen Lyases, Clinical Biochemistry, Glycine, Sequence Homology, Molecular cloning, Biochemistry, Genome, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Methionine, 0302 clinical medicine, Tetramer, Protein purification, Genetics, Amino Acid Sequence, Sulfhydryl Compounds, Cloning, Molecular, Molecular Biology, Pyridoxal, chemistry.chemical_classification, biology, Clostridioides difficile, Substrate (chemistry), Cell Biology, biology.organism_classification, 030104 developmental biology, Enzyme, chemistry, Alkynes, Pyridoxal Phosphate, 030220 oncology & carcinogenesis, Genome, Bacterial, Bacteria

Abstract

O-acetylhomoserine sulfhydrylase (OAHS) is a pyridoxal 5'-phosphate-dependent enzyme involved in microbial methionine biosynthesis. In this study, we report gene cloning, protein purification, and some biochemical characteristics of OAHS from Clostridioides difficile. The enzyme is a tetramer with molecular weight of 185 kDa. It possesses a high activity in the reaction of L-homocysteine synthesis, comparable to reported activities of OAHSes from other sources. OAHS activity is inhibited by metabolic end product L-methionine. L-Propargylglycine was found to be a suicide inhibitor of the enzyme. Substrate analogue Nγ -acetyl-L-2,4-diaminobutyric acid is a competitive inhibitor of OAHS with Ki = 0.04 mM. Analysis of C. difficile genome allows to suggest that the bacterium uses the way of direct sulfhydrylation for the synthesis of L-methionine. The data obtained may provide the basis for further study of the role of OAHS in the pathogenic bacterium and the development of potential inhibitors.

Published

2019

6. The Catalytic Mechanisms of the Reactions between Tryptophan Indole-Lyase and Nonstandard Substrates: The Role of the Ionic State of the Catalytic Group Accepting the Cα Proton of the Substrate

Author

Vitalia V. Kulikova, Konstantin A. Kochetkov, Marina A. Tsvetikova, N. G. Faleev, S.V. Revtovich, and Olga I. Gogoleva

Subjects

tryptophan indole-lyase, Leaving group, Tryptophan, Substrate (chemistry), mechanism, Biochemistry, Medicinal chemistry, L-serine, Catalysis, chemistry.chemical_compound, Acid catalysis, Hydrolysis, chemistry, kinetics, Functional group, Kinetic isotope effect, Molecular Medicine, β-chloro-L-alanine, Molecular Biology, Biotechnology, Research Article

Abstract

In the reaction between tryptophan indole-lyase (TIL) and a substrate containing a bad leaving group (L-serine), general acid catalysis is required for the group's elimination. During this stage, the proton originally bound to the C atom of the substrate is transferred to the leaving group, which is eliminated as a water molecule. As a result, the basic group that had accepted the C proton at the previous stage has to be involved in the catalytic stage following the elimination in its basic form. On the other hand, when the substrate contains a good leaving group (-chloro-L-alanine), general acid catalysis is not needed at the elimination stage and cannot be implemented, because there are no functional groups in enzymes whose acidity is strong enough to protonate the elimination of a base as weak as Cl- anion. Consequently, the group that had accepted the C proton does not lose its additional proton during the elimination stage and should take part in the subsequent stage in its acidic (not basic) form. To shed light on the mechanistic consequences of the changes in the ionic state of this group, we have considered the pH dependencies of the main kinetic parameters for the reactions of TIL with L-serine and -chloro-L-alanine and the kinetic isotope effects brought about by replacement of the ordinary water used as a solvent with 2H2O. We have found that in the reaction between TIL and -chloro-L-alanine, the aminoacrylate hydrolysis stage is sensitive to the solvent isotope effect, while in the reaction with L-serine it is not. We have concluded that in the first reaction, the functional group containing an additional proton fulfills a definite catalytic function, whereas in the reaction with L-serine, when the additional proton is absent, the mechanism of hydrolysis of the aminoacrylate intermediate should be fundamentally different. Possible mechanisms were considered.

Published

2019

7. O-acetylhomoserine sulfhydrylase from Clostridium novyi. Cloning, expression of the gene and characterization of the enzyme

Author

Elena A. Morozova, S.V. Revtovich, Vasiliy S. Koval, Mikhail I. Kotlov, Tatyana V. Demidkina, Yury Belyi, Vitalia V. Kulikova, and Natalya V. Anufrieva

Subjects

0106 biological sciences, Protein subunit, Carbon-Oxygen Lyases, Gene Expression, medicine.disease_cause, 01 natural sciences, Gene product, 03 medical and health sciences, Bacterial Proteins, 010608 biotechnology, medicine, Cloning, Molecular, Escherichia coli, Gene, 030304 developmental biology, chemistry.chemical_classification, Clostridium, 0303 health sciences, biology, Molecular mass, Chemistry, biology.organism_classification, Clostridium novyi, Recombinant Proteins, Enzyme, Biochemistry, Bacteria, Biotechnology

Abstract

The gene NT01CX_1210 of pathogenic bacterium Clostridium novyi annotated as encoding O-acetylhomoserine sulfhydrylase was cloned and expressed in Escherichia coli. The gene product having O-acetylhomoserine sulfhydrylase activity was purified to homogeneity. The protein showed molecular mass of approximately 184 kDa for the native form and 46 kDa for the subunit. The enzyme catalyzes the γ-substitution reaction of O-acetylhomoserine with maximum activity at pH 7.5. Analysis of C. novyi genome allowed us to suggest that there is only one way for the synthesis of l -methionine in the bacterium. The data obtained may provide the basis for further study of the role of OAHS in Clostridium bacteria and an ascertainment of its mechanism.

Published

2020

8. Antibacterial Effect of Thiosulfinates on Multiresistant Strains of Bacteria Isolated from Patients with Cystic Fibrosis

Author

Tatyana V. Demidkina, Vasily Koval, Elena A. Morozova, D G Kuliastova, L.R. Avetisyan, A N Rodionov, S.V. Revtovich, I.A. Shaginyan, Vitalia V. Kulikova, and M.Yu. Chernukha

Subjects

Allicin, biology, Microorganism, Antibacterial effect, biology.organism_classification, medicine.disease, Biochemistry, Cystic fibrosis, Microbiology, chemistry.chemical_compound, chemistry, medicine, Molecular Medicine, Antibacterial activity, Molecular Biology, Thiosulfinate, Antibiotic Drugs, Bacteria, Biotechnology

Abstract

The multiresistance of A. ruhlandii 155B, B. cenocepacia 122, and P. aeruginosa 48B strains isolated from patients with cystic fibrosis was established. The antibacterial effect of allicin, dimethyl thiosulfinate, and dipropyl thiosulfinate on multidrug-resistant strains was shown. Thiosulfinates can have both bacteriostatic and bactericidal effects depending on the microorganism and the concentration. The studied thiosulfinates may be candidates for the development of alternative antibiotic drugs to treat infections caused by multidrug-resistant pathogens.

Published

2018

9. Gene cloning, characterization, and cytotoxic activity of methionine γ-lyase fromClostridium novyi

Author

Mikhail I. Kotlov, Natalya P. Bazhulina, Tatyana V. Demidkina, Natalya V. Anufrieva, Andrea Mozzarelli, Edi Gabellieri, Patrizia Cioni, Vitalia V. Kulikova, Serena Faggiano, Samanta Raboni, Yury Belyi, Elena A. Morozova, and S.V. Revtovich

Subjects

0301 basic medicine, chemistry.chemical_classification, Methionine, 030102 biochemistry & molecular biology, biology, Clinical Biochemistry, Active site, Cell Biology, biology.organism_classification, Clostridium novyi, Lyase, Biochemistry, Citrobacter freundii, 03 medical and health sciences, chemistry.chemical_compound, Enzyme, chemistry, Genetics, Iodoacetamide, biology.protein, Molecular Biology, Cysteine

Abstract

The exploitation of methionine-depleting enzyme methionine γ-lyase (MGL) is a promising strategy against specific cancer cells that are strongly dependent on methionine. To identify MGL from different sources with high catalytic activity and efficient anticancer action, we have expressed and characterized MGL from Clostridium novyi and compared its catalytic efficiency with the previously studied MGL from Citrobacter freundii. The purified recombinant MGL exhibits kcat and kcat /Km for methionine γ-elimination reaction that are 2.4- and 1.36-fold higher than C. freundii enzyme, respectively, whereas absorption, fluorescence, and circular dichroism spectra are very similar, as expected on the basis of 87% sequence identity and high conservation of active site residues. The reactivity of cysteine residues with DTNB and iodoacetamide was investigated as well as the impact of their chemical modification on catalytic activity. This information is relevant because for increasing bioavailability and reducing immunogenity, MGL should be decorated with polyethylene glycol (PEG). It was found that Cys118 is a faster reacting residue, which results in a significant decrease in the γ-elimination activity. Thus, the protection of Cys118 before conjugation with cysteine-reacting PEG represents a valuable strategy to preserve MGL activity. The anticancer action of C. novyi MGL, evaluated in vitro against prostate (PC-3), chronic myelogenous leucemia (K562), and breast (MDA-MB-231 and MCF7) cancer cells, exhibits IC50 of 1.3 U mL-1 , 4.4 U mL-1 , 1.2 U mL-1 , and 3.4 U mL-1 , respectively. A higher cytotoxicity of C. novyi MGL was found against cancer cells with respect to C. freundii MGL, with the exception of PC-3, where a lower cytotoxicity was observed. © 2017 IUBMB Life, 69(9):668-676, 2017.

Published

2017

10. Pathological Metabolism of Methionine in Malignant Cells Is a Potential Target for the Antitumor Therapy

Author

V.S. Pokrovskii, D.Zh. Davydov, N.V. Davydov, D.D. Zhdanov, S.V. Revtovich, E.A. Morozova, T.V. Demidkina, and E.M. Treshchalina

Subjects

methionine, Methionine, methionine-γ-liase, business.industry, anticancer enzymes, Hematology, Metabolism, Pharmacology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Antitumor therapy, chemistry.chemical_compound, Oncology, chemistry, methionine dependency, cancer cells, cancer, Malignant cells, Medicine, business, Pathological, antitumor therapy

Abstract

This review presents the characteristics of the cellular metabolism of methionine, as well as known data on the mechanisms of the development of methionine dependence in malignant cells. The possibilities of using a non-methionine diet for the control of the tumor growth in patients with various forms of cancer are considered. The newest information about methionine-γ-lyase, an enzyme providing elimination of methionine from plasma, is grouped and summarised. Its role as a potential antitumor enzyme is disclosed. Data on methionine-γ-lyase producers, activity of this enzyme, obtained from various sources, and information on tumor models and cell cultures, showing methionine dependence are summarised.

Published

2017

11. Non-stereoselective decomposition of (±)-S-alk(en)yl- l -cysteine sulfoxides to antibacterial thiosulfinates catalyzed by C115H mutant methionine γ-lyase from Citrobacter freundii

Author

Elena A. Morozova, Vasily Koval, Tatyana V. Demidkina, S.V. Revtovich, A N Rodionov, Natalya V. Anufrieva, and Vitalia V. Kulikova

Subjects

0301 basic medicine, Stereochemistry, Microbial Sensitivity Tests, Alliin, Gram-Positive Bacteria, 01 natural sciences, Biochemistry, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Alliinase, Gram-Negative Bacteria, biology, 010405 organic chemistry, Stereoisomerism, Sulfoxide, General Medicine, Sulfinic Acids, Lyase, biology.organism_classification, Anti-Bacterial Agents, 0104 chemical sciences, Citrobacter freundii, Carbon-Sulfur Lyases, 030104 developmental biology, chemistry, Sulfoxides, Mutation, biology.protein, Stereoselectivity, Antibacterial activity, Cysteine

Abstract

S-Alk(en)yl-l-cysteine sulfoxides, initially found in plants of the genus Allium, are converted to antimicrobial thiosulfinates by pyridoxal 5'-phosphate(PLP)-dependent alliinase (EC 4.4.1.4). It was found that methionine γ-lyase (MGL, EC 4.4.1.11) catalyzes the β-elimination reaction of (±)-S-alk(en)yl-l-cysteine sulfoxides to yield thiosulfinates. The efficient catalyst for the production of thiosulfinates, C115H mutant MGL, developed in our previous work, cleaves S-alk(en)yl-l-cysteine sulfoxides more effectively than the wild type enzyme. Thiosulfinates generated by the C115H MGL/sulfoxide system have demonstrated growth inhibition of Gram-positive, Gram-negative bacteria and clinical isolates of pathogenic bacteria from mice. In search of a more effective system for production of antibacterial thiosulfinates we synthesized S-substituted analogues of l-cysteine sulfoxide with a longer side chains - (±)-S-propyl-l-cysteine sulfoxide ((±)-propiin) and (±)-S-n-butyl-l-cysteine sulfoxide ((±)-butiin) and determined catalytic parameters of the β-elimination reaction of two sulfoxides. It was found that C115H MGL cleaves (±)-propiin with the highest rate, as compared to other (±)-S-alk(en)yl-l-cysteine sulfoxides. Studies on interaction of the enzyme with (+)- or (-)-S-alk(en)yl-l-cysteine sulfoxides revealed that C115H MGL can decompose both diastereomers equally. The antibacterial activity of the mixture of the mutant MGL with (±)-propiin is comparable with those of the mixtures with S-allyl-l-cysteine sulfoxide (alliin) and S-methyl-l-cysteine sulfoxide (methiin). The results make MGL/sulfoxide system more advantageous in preparing antibacterial thiosulfinates as compared to alliinase-based system, which preferably cleaves naturally occurring (+)-sulfoxides.

Published

2018

12. Mutant form C115H ofClostridium sporogenesmethionine γ-lyase efficiently cleaves S-Alk(en)yl-<scp>l</scp>-cysteine sulfoxides to antibacterial thiosulfinates

Author

Elena A. Morozova, S.V. Revtovich, Alexander S. Chernov, Georgii B. Telegin, Natalya V. Anufrieva, Vitalia V. Kulikova, and Tatyana V. Demidkina

Subjects

0301 basic medicine, chemistry.chemical_classification, Methionine, biology, Stereochemistry, Clostridium sporogenes, 030106 microbiology, Clinical Biochemistry, Mutant, Sulfoxide, Cell Biology, Lyase, biology.organism_classification, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Enzyme, chemistry, Genetics, Molecular Biology, Pyridoxal, Cysteine

Abstract

Pyridoxal 5'-phosphate-dependent methionine γ-lyase (MGL) catalyzes the β-elimination reaction of S-alk(en)yl-l-cysteine sulfoxides to thiosulfinates, which possess antimicrobial activity. Partial inactivation of the enzyme in the course of the reaction occurs due to oxidation of active site cysteine 115 conserved in bacterial MGLs. In this work, the C115H mutant form of Clostridium sporogenes MGL was prepared and the steady-state kinetic parameters of the enzyme were determined. The substitution results in an increase in the catalytic efficiency of the mutant form towards S-substituted l-cysteine sulfoxides compared to the wild type enzyme. We used a sulfoxide/enzyme system to generate antibacterial activity in situ. Two-component systems composed of the mutant enzyme and three S-substituted l-cysteine sulfoxides were demonstrated to be effective against Gram-positive and Gram-negative bacteria and three clinical isolates from mice. © 2016 IUBMB Life, 68(10):830-835, 2016.

Published

2016

13. Engineering methionine γ-lyase from Citrobacter freundii for anticancer activity

Author

Barbara Giabbai, Loredano Pollegioni, Serena Galati, Edi Gabellieri, Vitalia V. Kulikova, Andrea Mozzarelli, Alexey D. Nikulin, Chiara Cocconcelli, Patrizia Cioni, S.V. Revtovich, Nicola Demitri, Serena Faggiano, Samanta Raboni, Annamaria Buschini, Tatyana V. Demidkina, Paola Storici, Elena Rosini, and Elena A. Morozova

Subjects

0301 basic medicine, Cancer therapy, Pyridoxal 5′-phosphate dependent enzyme, Biophysics, Antineoplastic Agents, Crystallography, X-Ray, Protein Engineering, Biochemistry, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, Cytotoxicity activity, Methionine depletion, Protein engineering, Site-saturation mutagenesis, Molecular Biology, Bacterial Proteins, Catalytic Domain, Cell Proliferation, chemistry.chemical_classification, Methionine, biology, Mutagenesis, Wild type, Active site, Lyase, biology.organism_classification, Recombinant Proteins, Citrobacter freundii, Amino acid, Protein Structure, Tertiary, Pyridoxal 5?-phosphate dependent enzyme, Carbon-Sulfur Lyases, Kinetics, 030104 developmental biology, Enzyme, chemistry, biology.protein, Mutagenesis, Site-Directed

Abstract

Methionine deprivation of cancer cells, which are deficient in methionine biosynthesis, has been envisioned as a therapeutic strategy to reduce cancer cell viability. Methionine ?-lyase (MGL), an enzyme that degrades methionine, has been exploited to selectively remove the amino acid from cancer cell environment. In order to increase MGL catalytic activity, we performed sequence and structure conservation analysis of MGLs from various microorganisms. Whereas most of the residues in the active site and at the dimer interface were found to be conserved, residues located in the C-terminal flexible loop, forming a wall of the active site entry channel, were found to be variable. Therefore, we carried out site-saturation mutagenesis at four independent positions of the C-terminal flexible loop, P357, V358, P360 and A366 of MGL from Citrobacter freundii, generating libraries that were screened for activity. Among the active variants, V358Y exhibits a 1.9-fold increase in the catalytic rate and a 3-fold increase in KM, resulting in a catalytic efficiency similar to wild type MGL. V358Y cytotoxic activity was assessed towards a panel of cancer and nonmalignant cell lines and found to exhibit IC50 lower than the wild type. The comparison of the 3D-structure of V358Y MGL with other MGL available structures indicates that the C-terminal loop is either in an open or closed conformation that does not depend on the amino acid at position 358. Nevertheless, mutations at this position allosterically affects catalysis.

Published

2018

14. The role of active site tyrosine 58 in Citrobacter freundii methionine γ-lyase

Author

Alexei Nikulin, Elena A. Morozova, Yaroslav V. Tkachev, Nicolai G. Faleev, Vladimir P. Timofeev, Natalya V. Anufrieva, Tatyana V. Demidkina, Bazhulina Np, and S.V. Revtovich

Subjects

Magnetic Resonance Spectroscopy, Stereochemistry, Mutant, Biophysics, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, Catalytic Domain, Tyrosine, Molecular Biology, Pyridoxal, chemistry.chemical_classification, Methionine, biology, Active site, biology.organism_classification, Lyase, Citrobacter freundii, Carbon-Sulfur Lyases, Kinetics, Enzyme, chemistry, biology.protein

Abstract

In the spatial structure of methionine γ-lyase (MGL, EC 4.4.1.11) from Citrobacter freundii, Tyr58 is located at H-bonding distance to the oxygen atom of the phosphate “handle” of pyridoxal 5′-phosphate (PLP). It was replaced for phenylalanine by site-directed mutagenesis. The X-ray structure of the mutant enzyme was determined at 1.96 A resolution. Comparison of spatial structures and absorption spectra of wild-type and mutant holoenzymes demonstrated that the replacement did not result in essential changes of the conformation of the active site Tyr58Phe MGL. The Kd value of PLP for Tyr58Phe MGL proved to be comparable to the Kd value for the wild-type enzyme. The replacement led to a decrease of catalytic efficiencies in both γ- and β-elimination reactions of about two orders of magnitude as compared to those for the wild-type enzyme. The rates of exchange of C-α- and C-β- protons of inhibitors in D2O catalyzed by the mutant form are comparable with those for the wild-type enzyme. Spectral data on the complexes of the mutant form with the substrates and inhibitors showed that the replacement led to a change of rate the limiting step of the physiological reaction. The results allowed us to conclude that Tyr58 is involved in an optimal positioning of the active site Lys210 at some stages of γ- and β-elimination reactions. This article is part of a Special Issue entitled: Cofactor-dependent proteins: evolution, chemical diversity and bio-applications.

Published

2015

15. Pre-steady-state Kinetic and Structural Analysis of Interaction of Methionine γ-Lyase from Citrobacter freundii with Inhibitors

Author

Natalya V. Anufrieva, Elena A. Morozova, Olga S. Fedorova, Nikita A. Kuznetsov, S.V. Revtovich, Alexandra A. Kuznetsova, Alexei Nikulin, Nicolai G. Faleev, and Tatyana V. Demidkina

Subjects

Aldimine, Stereochemistry, Glycine, Gene Expression, Reaction intermediate, Crystallography, X-Ray, Biochemistry, chemistry.chemical_compound, Bacterial Proteins, Catalytic Domain, Escherichia coli, Cysteine, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Alanine, Methionine, biology, Valine, Cell Biology, biology.organism_classification, Lyase, Recombinant Proteins, Enzyme structure, Citrobacter freundii, Amino acid, Carbon-Sulfur Lyases, Kinetics, Models, Chemical, chemistry, Cycloserine, Pyridoxal Phosphate, Enzymology, Thermodynamics, Imines, Steady state (chemistry)

Abstract

Methionine γ-lyase (MGL) catalyzes the γ-elimination of l-methionine and its derivatives as well as the β-elimination of l-cysteine and its analogs. These reactions yield α-keto acids and thiols. The mechanism of chemical conversion of amino acids includes numerous reaction intermediates. The detailed analysis of MGL interaction with glycine, l-alanine, l-norvaline, and l-cycloserine was performed by pre-steady-state stopped-flow kinetics. The structure of side chains of the amino acids is important both for their binding with enzyme and for the stability of the external aldimine and ketimine intermediates. X-ray structure of the MGL·l-cycloserine complex has been solved at 1.6 A resolution. The structure models the ketimine intermediate of physiological reaction. The results elucidate the mechanisms of the intermediate interconversion at the stages of external aldimine and ketimine formation.

Published

2015

16. Serine 51 residue of Citrobacter freundii tyrosine phenol-lyase assists in C-α-proton abstraction and transfer in the reaction with substrate

Author

Nicolai G. Faleev, Robert S. Phillips, Marina A. Tsvetikova, Tatyana V. Demidkina, Natalia V. Anufrieva, Maria V. Barbolina, S.V. Revtovich, Vitalia V. Kulikova, and Paul Gollnick

Subjects

0301 basic medicine, Stereochemistry, Phenylalanine, Tyrosine phenol-lyase, Biochemistry, 03 medical and health sciences, Residue (chemistry), Elimination reaction, Methionine, Protein Domains, Side chain, Serine, Enzyme kinetics, Tyrosine, Tyrosine Phenol-Lyase, 030102 biochemistry & molecular biology, biology, Chemistry, Active site, General Medicine, biology.organism_classification, Citrobacter freundii, Kinetics, 030104 developmental biology, Amino Acid Substitution, biology.protein, Protein Multimerization, Protons

Abstract

In the spatial structure of tyrosine phenol-lyase, the Ser51 residue is located in the active site of the enzyme. The replacement of Ser51 with Ala by site-directed mutagenesis led to a decrease of the kcat/Km parameter for reactions with l -tyrosine and 3-fluoro- l -tyrosine by three orders of magnitude, compared to wild type enzyme. For the elimination reactions of S-alkylcysteines, the values of kcat/Km decreased by an average of two orders of magnitude. The results of spectral studies of the mutant enzyme gave evidence for a considerable change of the chiral properties of the active site as a result of the replacement. Fast kinetic studies for the complexes of the mutant form with competitive inhibitors allowed us to conclude that the Ser51 residue interacts with the side chain amino group of Lys257 at the stage of C-α-proton abstraction. This interaction ensures the correct orientation of the side chain of Lys257 accepting the C-α-proton of the external aldimine and stabilizes its ammonium form. Also, it is probable that Ser51 takes part in formation of a chain of hydrogen bonds which is necessary to perform the transfer of the C-α-proton to the C-4′-position of the leaving phenol group in the reaction with the natural substrate.

Published

2017

17. Crystal structure of mutant form Cys115His of Citrobacter freundii methionine γ-lyase complexed with l-norleucine

Author

Vitalia V. Kulikova, Tatyana V. Demidkina, Elena A. Morozova, Alexey D. Nikulin, Vasiliy S. Koval, S.V. Revtovich, Tatyana I. Osipova, and Natalya V. Anufrieva

Subjects

0301 basic medicine, Models, Molecular, Aldimine, Stereochemistry, Protein Conformation, Mutant, Norleucine, Biophysics, Mutation, Missense, Crystallography, X-Ray, Biochemistry, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, Bacterial Proteins, Catalytic Domain, Point Mutation, Molecular Biology, chemistry.chemical_classification, Methionine, biology, Active site, Lyase, biology.organism_classification, Citrobacter freundii, Carbon-Sulfur Lyases, 030104 developmental biology, chemistry, Amino Acid Substitution, biology.protein, Protein Binding

Abstract

The mutant form of Citrobacter freundii methionine γ-lyase with the replacement of active site Cys115 for His has been found to be inactive in the γ-elimination reaction of methionine while fully active in the γ-elimination reaction of O-acetyl-l-homoserine and in the β-elimination reaction of S-alk(en)yl-substituted cysteines. In this work, the crystal structure of the mutant enzyme complexed with competitive inhibitor, l-norleucine was determined at 1.45A resolution. At the enzyme active site the inhibitor proved to be bound both noncovalently and covalently, which corresponds to the two intermediates of the γ- and β-elimination reactions, Michaelis complex and the external aldimine. Analysis of the structure allowed us to suggest the possible reason for the inability of the mutant enzyme to catalyze the physiological reaction.

Published

2017

18. Alliin is a suicide substrate ofCitrobacter freundiimethionine γ-lyase: structural bases of inactivation of the enzyme

Author

S.V. Revtovich, Natalya V. Anufrieva, Tatyana V. Demidkina, Vitalia V. Kulikova, Alexey D. Nikulin, and Elena A. Morozova

Subjects

Models, Molecular, Methionine gamma-lyase, Protein Conformation, Stereochemistry, Alliin, Crystallography, X-Ray, chemistry.chemical_compound, Structural Biology, Alliinase, Point Mutation, Cysteine, chemistry.chemical_classification, Methionine, Allicin, biology, General Medicine, Lyase, biology.organism_classification, Amino acid, Citrobacter freundii, Enzyme Activation, Carbon-Sulfur Lyases, Biochemistry, chemistry, biology.protein

Abstract

The interaction ofCitrobacter freundiimethionine γ-lyase (MGL) and the mutant form in which Cys115 is replaced by Ala (MGL C115A) with the nonprotein amino acid (2R)-2-amino-3-[(S)-prop-2-enylsulfinyl]propanoic acid (alliin) was investigated. It was found that MGL catalyzes the β-elimination reaction of alliin to form 2-propenethiosulfinate (allicin), pyruvate and ammonia. The β-elimination reaction of alliin is followed by the inactivation and modification of SH groups of the wild-type and mutant enzymes. Three-dimensional structures of inactivated wild-type MGL (iMGL wild type) and a C115A mutant form (iMGL C115A) were determined at 1.85 and 1.45 Å resolution and allowed the identification of the SH groups that were oxidized by allicin. On this basis, the mechanism of the inactivation of MGL by alliin, a new suicide substrate of MGL, is proposed.

Published

2014

19. Engineered Citrobacter freundii methionine γ-lyase effectively produces antimicrobial thiosulfinates

Author

Elena A. Morozova, Vitalia V. Kulikova, S.V. Revtovich, A N Rodionov, Natalya V. Anufrieva, and Tatyana V. Demidkina

Subjects

0301 basic medicine, Mutation, Missense, Microbial Sensitivity Tests, Biochemistry, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Methionine, Anti-Infective Agents, Bacterial Proteins, Histidine, Cysteine, chemistry.chemical_classification, Alanine, 030102 biochemistry & molecular biology, biology, Chemistry, General Medicine, biology.organism_classification, Lyase, Antimicrobial, Sulfinic Acids, Citrobacter freundii, Carbon-Sulfur Lyases, 030104 developmental biology, Enzyme, Metabolic Engineering, Spectrophotometry, Sulfoxides, Biocatalysis, Antibacterial activity

Abstract

Antimicrobial activity of thiosulfinates in situ produced by mixtures of Citrobacter freundii methionine γ-lyase (MGL) with new substrates, l-methionine and S-(alkyl/allyl)-l-cysteine sulfoxides has been recently demonstrated (Anufrieva et al., 2015). This opens a way to the rational design of a new biotechnologically relevant antimicrobial drug producer. To increase the efficiency of the enzyme toward sulfoxides, the mutant forms of MGL, with the replacements of active site cysteine 115 with alanine (C115A MGL) and histidine (C115H MGL) were obtained. The replacement of cysteine 115 by histidine results in the loss of activity of the mutant enzyme in the γ-elimination reaction of physiological substrate, whereas the activity in the β-elimination reaction of characteristic substrates persists. However, the catalytic efficiency of C115H MGL in the β-elimination reaction of S-substituted l-cysteine sulfoxides is increased by about an order of magnitude compared to the wild type MGL. The antibacterial activity of C115H MGL mixtures with a number of sulfoxides was assessed against Gram-positive and Gram-negative bacteria. The bacteriostatic effect was more pronounced against Gram-positive than against Gram-negative bacteria, while antibacterial potential proved to be quite similar. Thus, the mutant enzyme C115H MGL is an effective catalyst, in particular, for decomposition of sulfoxides and the pharmacological couples of the mutant form with sulfoxides might be new antimicrobial agents.

Published

2016

20. Identification of methionine γ-lyase in genomes of some pathogenic bacteria

Author

Tatyana V. Demidkina, E. A. Morozova, Yu. F. Belyi, N.V. Anufrieva, M. I. Kotlov, and S.V. Revtovich

Subjects

Molecular Sequence Data, Biophysics, medicine.disease_cause, Polymerase Chain Reaction, Biochemistry, Genome, law.invention, chemistry.chemical_compound, law, medicine, Amino Acid Sequence, Peptide sequence, Polymerase chain reaction, DNA Primers, chemistry.chemical_classification, Genetics, Methionine, Base Sequence, Sequence Homology, Amino Acid, Pathogenic bacteria, General Chemistry, General Medicine, Lyase, Amino acid, Carbon-Sulfur Lyases, chemistry, Biocatalysis, Identification (biology), Genome, Bacterial

Published

2012

21. Methionine γ-lyase: Mechanistic deductions from the kinetic pH-effects

Author

Radii M. Khomutov, S.V. Revtovich, Marina A. Tsvetikova, Nicolai G. Faleev, M. M. Vorob'ev, Robert S. Phillips, Tatyana V. Demidkina, Elena N. Khurs, Elena A. Morozova, and Kirill V. Alferov

Subjects

chemistry.chemical_classification, Methionine, biology, Stereochemistry, Biophysics, Active site, Lyase, Biochemistry, Analytical Chemistry, Catalysis, chemistry.chemical_compound, Elimination reaction, chemistry, Zwitterion, biology.protein, Thiol, Molecular Biology, Cysteine

Abstract

We have studied and compared the pH-dependencies of the main kinetic parameters for the α,γ-elimination reactions of methionine γ-lyase (MGL) of Citrobacter intermedius with natural substrate, l -methionine, with its phosphinic analogue, and for α,β-elimination reaction with S-methyl- l -cysteine. From the pH-dependency of k cat / K m for the reaction with l -methionine we have concluded that MGL is selective with respect to the zwitterionic form of its natural substrate. For the reaction of MGL with 1-amino-3-methylthiopropylphosphinic acid the p K a of the substrate's amino group, equal to 7.55, is not reflected in the pH-profile of k cat / K m . Consequently, the enzyme does not manifest well-defined selectivity with respect to the zwitterion and anion ionic forms of the substrate. The ascending limbs of pH-dependencies of k cat / K m for reactions with l -methionine and S-methyl- l -cysteine are controlled by a single p K a equal to 7.1–7.2, while for the reaction with 1-amino-3-methylthiopropylphosphinic acid two equal p K a s of 6.2 were found in the respective pH-profile. The descending limbs of pH-dependencies of k cat / K m for the reactions with S-methyl- l -cysteine and racemic 1-amino-3-methylthiopropylphosphinic acid are very similar and are controlled by two acidic groups having average p K a values of 8.7. On the basis of these results we suggest a mechanism of catalytic action of MGL. According to this mechanism Tyr 113, in its conjugated base form, acts as an acceptor of the proton from the amino group of the substrate upon its binding in the active site. Elimination of the leaving thiol groups during both α,γ- and α,β-elimination reactions is assisted by the acidic groups of Tyr 113 and Tyr 58. Both tyrosyl residues are able to fulfill this catalytic function with different efficiencies depending on the type of elimination reaction. Tyr 113 residue plays the determining role in the α,γ-elimination, and Tyr 58 — in the α,β-elimination process.

Published

2009

22. Structure of methionine γ-lyase from Clostridium sporogenes

Author

Elena A. Morozova, S.V. Revtovich, Tatyana V. Demidkina, Natalya V. Anufrieva, Alexey D. Nikulin, and Vitalia V. Kulikova

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, alpha-Helical, Methionine gamma-lyase, Clostridium sporogenes, Biophysics, Crystallography, X-Ray, Biochemistry, Microbiology, Research Communications, 03 medical and health sciences, chemistry.chemical_compound, Entamoeba histolytica, Clostridium, Methionine, Bacterial Proteins, Structural Biology, Catalytic Domain, Genetics, Protein Interaction Domains and Motifs, Protein Structure, Quaternary, 030102 biochemistry & molecular biology, biology, Hydrogen Bonding, Condensed Matter Physics, biology.organism_classification, Lyase, Pseudomonas putida, Citrobacter freundii, Carbon-Sulfur Lyases, Kinetics, chemistry, Pyridoxal Phosphate, Crystallization, Protein Binding

Abstract

Methionine γ-lyase (MGL) is a pyridoxal 5′-phosphate-dependent enzyme that catalyzes the γ-elimination reaction of L-methionine. The enzyme is a promising target for therapeutic intervention in some anaerobic pathogens and has attracted interest as a potential cancer treatment. The crystal structure of MGL fromClostridium sporogeneshas been determined at 2.37 Å resolution. The fold of the protein is similar to those of homologous enzymes fromCitrobacter freundii,Entamoeba histolytica,Pseudomonas putidaandTrichomonas vaginalis. A comparison of these structures revealed differences in the conformation of two flexible regions of the N- and C-terminal domains involved in the active-site architecture.

Published

2015

23. Crystal structure of the external aldimine of Citrobacter freundii methionine γ-lyase with glycine provides insight in mechanisms of two stages of physiological reaction and isotope exchange of α- and β-protons of competitive inhibitors

Author

S.V. Revtovich, Tatyana V. Demidkina, Alexey D. Nikulin, Natalya V. Anufrieva, Elena A. Morozova, and Nicolai G. Faleev

Subjects

Models, Molecular, Aldimine, Stereochemistry, Glycine, Crystallography, X-Ray, Biochemistry, Binding, Competitive, chemistry.chemical_compound, Methionine, Bacterial Proteins, Catalytic Domain, Nitriles, Enzyme Inhibitors, chemistry.chemical_classification, biology, Concerted reaction, Chemistry, Active site, General Medicine, Lyase, biology.organism_classification, Citrobacter freundii, Amino acid, Carbon-Sulfur Lyases, biology.protein, Imines, Protein Binding

Abstract

The three-dimensional structure of the external aldimine of Citrobacter freundii methionine γ-lyase with competitive inhibitor glycine has been determined at 2.45 A resolution. It revealed subtle conformational changes providing effective binding of the inhibitor and facilitating labilization of Cα-protons of the external aldimine. The structure shows that 1, 3-prototropic shift of Cα-proton to C4′-atom of the cofactor may proceed with participation of active site Lys210 residue whose location is favorable for performing this transformation by a concerted mechanism. The observed stereoselectivity of isotopic exchange of enantiotopic Cα-protons of glycine may be explained on the basis of external aldimine structure. The exchange of Cα- pro -(R)-proton of the external aldimine might proceed in the course of the concerted transfer of the proton from Cα-atom of glycine to C4′-atom of the cofactor. The exchange of Cα- pro -(S)-proton may be performed with participation of Tyr113 residue which should be present in its basic form. The isotopic exchange of β-protons, which is observed for amino acids bearing longer side groups, may be effected by two catalytic groups: Lys210 in its basic form, and Tyr113 acting as a general acid.

Published

2013

24. KINETIC PARAMETERS AND CYTOTOXIC ACTIVITY OF RECOMBINANT METHIONINE γ-LYASE FROM CLOSTRIDIUM TETANI, CLOSTRIDIUM SPOROGENES, PORPHYROMONAS GINGIVALIS AND CITROBACTER FREUNDII

Author

N. Y. Anisimova, Tatyana V. Demidkina, D. V. Yashin, Vadim S. Pokrovsky, Elena A. Morozova, S.V. Revtovich, Yury Belyi, Natalya V. Anufrieva, M. I. Kotlov, and Vitalia V. Kulikova

Subjects

Clostridium tetani, Clostridium sporogenes, oligomeric structure, Biology, medicine.disease_cause, Biochemistry, law.invention, chemistry.chemical_compound, law, medicine, METHIONINE γ-LYASE, Molecular Biology, Porphyromonas gingivalis, pathogenic microorganisms, chemistry.chemical_classification, Methionine, kinetic parameters, Lyase, biology.organism_classification, Citrobacter freundii, Enzyme, chemistry, Recombinant DNA, cytotoxicity, Molecular Medicine, Research Article, Biotechnology

Abstract

The steady-state kinetic parameters of pyridoxal 5-phosphate-dependent recombinant methionine -lyase from three pathogenic bacteria, Clostridium tetani, Clostridium sporogenes, and Porphyromonas gingivalis, were determined in - and -elimination reactions. The enzyme from C. sporogenes is characterized by the highest catalytic efficiency in the -elimination reaction of L-methionine. It was demonstrated that the enzyme from these three sources exists as a tetramer. The N-terminal poly-histidine fragment of three recombinant enzymes influences their catalytic activity and facilitates the aggregation of monomers to yield dimeric forms under denaturing conditions. The cytotoxicity of methionine -lyase from C. sporogenes and C. tetani in comparison with Citrobacter freundii was evaluated using K562, PC-3, LnCap, MCF7, SKOV-3, and L5178y tumor cell lines. K562 (IC50=0.4-1.3 U/ml), PC-3 (IC50=0.1-0.4 U/ml), and MCF7 (IC50=0.04-3.2 U/ml) turned out to be the most sensitive cell lines.

Published

2013

25. Three-dimensional structures of noncovalent complexes of Citrobacter freundii methionine γ-lyase with substrates

Author

E. A. Morozova, R. M. Khomutov, L.N. Zakomirdina, Alexey D. Nikulin, Tatyana V. Demidkina, S.V. Revtovich, and E. N. Khurs

Subjects

Models, Molecular, Stereochemistry, Biochemistry, Substrate Specificity, chemistry.chemical_compound, Bacterial Proteins, Organic chemistry, Cysteine, Enzyme Inhibitors, Pyridoxal, chemistry.chemical_classification, Methionine, Binding Sites, biology, Active site, General Medicine, biology.organism_classification, Lyase, Amino acid, Citrobacter freundii, Carbon-Sulfur Lyases, Kinetics, Enzyme, chemistry, Covalent bond, biology.protein, Hydrophobic and Hydrophilic Interactions

Abstract

Crystal structures of Citrobacter freundii methionine γ-lyase complexes with the substrates of γ- (L-1-amino-3-methylthiopropylphosphinic acid) and β- (S-ethyl-L-cysteine) elimination reactions and the competitive inhibitor L-norleucine have been determined at 1.45, 1.8, and 1.63 Å resolution, respectively. All three amino acids occupy the active site of the enzyme but do not form a covalent bond with pyridoxal 5'-phosphate. Hydrophobic interactions between the active site residues and the side groups of the substrates and the inhibitor are supposed to cause noncovalent binding. Arg374 and Ser339 are involved in the binding of carboxyl groups of the substrates and the inhibitor. The hydroxyl of Tyr113 is a potential acceptor of a proton from the amino groups of the amino acids.

Published

2011

26. High-resolution structure of methionine gamma-lyase from Citrobacter freundii

Author

Tatyana V. Demidkina, Stanislav Nikonov, S.V. Revtovich, Elena A. Morozova, Alexei Nikulin, N. Nevskaya, and Maria Garber

Subjects

Models, Molecular, Methionine gamma-lyase, Stereochemistry, Molecular Sequence Data, Crystallography, X-Ray, Protein Structure, Secondary, chemistry.chemical_compound, Protein structure, Structural Biology, Amino Acid Sequence, Pyridoxal, chemistry.chemical_classification, Cofactor binding, Methionine, Binding Sites, biology, General Medicine, biology.organism_classification, Lyase, Amino acid, Citrobacter freundii, Protein Structure, Tertiary, Carbon-Sulfur Lyases, Biochemistry, chemistry

Abstract

Pyridoxal 5'-phosphate-dependent methionine gamma-lyase (MGL) is involved in the metabolism of sulfur-containing amino acids. The enzyme is a promising target in some anaerobic pathogens and is effective in cancer-cell treatment. The structure of the MGL holoenzyme from Citrobacter freundii has previously been determined at 1.9 A resolution. By modification of the crystallization procedure, the previously determined structure of C. freundii MGL has been improved to 1.35 A resolution with R and R(free) values of 0.152 and 0.177, respectively. This high-resolution structure makes it possible to analyze the interactions between the monomers in detail and to reveal the structurally invariant regions that are responsible for monomer-monomer recognition during the formation of the active enzyme. Details of the mode of cofactor binding and of the flexible regions that may be involved in substrate recognition and binding are also described.

Published

2007

27. Structure of Citrobacter freundii l-methionine γ-­lyase

Author

Stanislav Nikonov, Elena A. Morozova, S.V. Revtovich, Maria Garber, Alexey D. Nikulin, Daria Mamaeva, and Tatyana V. Demidkina

Subjects

Biophysics, medicine.disease_cause, Crystallography, X-Ray, Biochemistry, Protein Structure, Secondary, chemistry.chemical_compound, Protein structure, fluids and secretions, Bacterial Proteins, Structural Biology, Genetics, medicine, polycyclic compounds, Protein Structure Communications, Binding site, Pyridoxal, chemistry.chemical_classification, Binding Sites, biology, Molecular Structure, biochemical phenomena, metabolism, and nutrition, Condensed Matter Physics, biology.organism_classification, Lyase, equipment and supplies, Pseudomonas putida, Citrobacter freundii, Carbon-Sulfur Lyases, Enzyme, chemistry, bacteria, Trichomonas vaginalis

Abstract

L-Methionine gamma-lyase (MGL) is a pyridoxal 5'-phosphate (PLP) dependent enzyme that catalyzes gamma-elimination of L-methionine. The crystal structure of MGL from Citrobacter freundii has been determined at 1.9 A resolution. The spatial fold of the protein is similar to those of MGLs from Pseudomonas putida and Trichomonas vaginalis. The comparison of these structures revealed that there are differences in PLP-binding residues and positioning of the surrounding flexible loops.

Published

2005

28. Role of N-terminal helix in interaction of ribosomal protein S15 with 16S rRNA

Author

Stanislav Nikonov, S.V. Revtovich, and Alexey D. Nikulin

Subjects

Models, Molecular, Ribosomal Proteins, Stereochemistry, Eukaryotic Large Ribosomal Subunit, Thermus thermophilus, 5.8S ribosomal RNA, General Medicine, Ribosomal RNA, Biology, Biochemistry, Molecular biology, Protein Structure, Secondary, 5S ribosomal RNA, Bacterial Proteins, Ribosomal protein, 23S ribosomal RNA, RNA, Ribosomal, 16S, Protein Interaction Mapping, Eukaryotic Ribosome, Crystallization, 50S, Bacillus subtilis

Abstract

The position and conformation of the N-terminal helix of free ribosomal protein S15 was earlier found to be modified under various conditions. This variability was supposed to provide the recognition by the protein of its specific site on 16S rRNA. To test this hypothesis, we substituted some amino acid residues in this helix and assessed effects of these substitutions on the affinity of the protein for 16S rRNA. The crystal structure of the complex of one of these mutants (Thr3Cys S15) with the 16S rRNA fragment was determined, and a computer model of the complex containing another mutant (Gln8Met S15) was designed. The available and new information was analyzed in detail, and the N-terminal helix was concluded to play no significant role in the specific binding of the S15 protein to its target on 16S rRNA.

Published

2005

29. Identification of RNA-recognizing modules on the surface of ribosomal proteins

Author

Stanislav Nikonov, O. S. Nikonov, M. B. Garber, S.V. Revtovich, and N. Nevskaya

Subjects

Genetics, 5S ribosomal RNA, Structural Biology, Ribosomal protein, Eukaryotic Large Ribosomal Subunit, Biophysics, 30S, Computational biology, Ribosomal RNA, Biology, Eukaryotic Ribosome, 18S ribosomal RNA, 50S

Abstract

Specific binding of ribosomal proteins to rRNA has been analyzed, and the method for determining the recognizing modules on the protein surface has been proposed. This method is based on the search for the atoms on the protein molecule that are involved in the conserved hydrogen bonds with rRNA and form invariant spatial structure in both free and RNA-bound ribosomal proteins. The potential of this method is illustrated by determining the rRNA-recognizing modules on the surface of ribosomal proteins S8, S15, and L5.