Your search keyword '"Tetrahydrofolates chemistry"' showing total 203 results

1. In vivo determination of the bioavailability of folic acid through the utilization of the PBPK model in conjunction with UPLC.

Author

Qi Y, Mao C, Zhou Y, Xie Z, Wu C, and Lin S

Subjects

Animals, Chromatography, High Pressure Liquid, Male, Rats, Rats, Sprague-Dawley, Tetrahydrofolates metabolism, Tetrahydrofolates chemistry, Liver metabolism, Liver chemistry, Humans, Folic Acid metabolism, Folic Acid administration & dosage, Folic Acid chemistry, Biological Availability, Models, Biological

Abstract

This paper employed a physiologically based pharmacokinetic model (PBPK) to investigate the transformations of folic acid and its metabolites in vivo. Additionally, an ultra-performance liquid chromatography (UPLC) method was developed to accurately measure the body's retention rate and conversion rate of folic acid, tetrahydrofolate, and 5-methyltetrahydrofolate. Furthermore, the bioavailability of folic acid in the body was assessed by combining this method with an evaluation technique for animal models. The study found that the gastric metabolism time was 2 h, while the small intestinal metabolism duration was 4 h. The maximum conversion rate was observed in plasma and liver after 6 h, and in the brain after 8 h. This serves as a framework for creating a model to assess the bioavailability of folic acid in living organisms, to enhance the safety and efficacy of folic acid intake., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

2. Key structural role of a conserved cis-proline revealed by the P285S variant of soybean serine hydroxymethyltransferase 8.

Author

Samarakoon V, Owuocha LF, Hammond J, Mitchum MG, and Beamer LJ

Subjects

Crystallography, X-Ray, Catalytic Domain, Pyridoxal Phosphate metabolism, Plant Proteins genetics, Plant Proteins metabolism, Plant Proteins chemistry, Models, Molecular, Amino Acid Substitution, Tetrahydrofolates metabolism, Tetrahydrofolates chemistry, Folic Acid metabolism, Animals, Glycine Hydroxymethyltransferase genetics, Glycine Hydroxymethyltransferase metabolism, Glycine Hydroxymethyltransferase chemistry, Glycine max enzymology, Glycine max genetics, Proline metabolism, Proline genetics, Proline chemistry

Abstract

The enzyme serine hydroxymethyltransferase (SHMT) plays a key role in folate metabolism and is conserved in all kingdoms of life. SHMT is a pyridoxal 5'-phosphate (PLP) - dependent enzyme that catalyzes the conversion of L-serine and (6S)-tetrahydrofolate to glycine and 5,10-methylene tetrahydrofolate. Crystal structures of multiple members of the SHMT family have shown that the enzyme has a single conserved cis proline, which is located near the active site. Here, we have characterized a Pro to Ser amino acid variant (P285S) that affects this conserved cis proline in soybean SHMT8. P285S was identified as one of a set of mutations that affect the resistance of soybean to the agricultural pathogen soybean cyst nematode. We find that replacement of Pro285 by serine eliminates PLP-mediated catalytic activity of SHMT8, reduces folate binding, decreases enzyme stability, and affects the dimer-tetramer ratio of the enzyme in solution. Crystal structures at 1.9-2.2 Å resolution reveal a local reordering of the polypeptide chain that extends an α-helix and shifts a turn region into the active site. This results in a dramatically perturbed PLP-binding pose, where the ring of the cofactor is flipped by ∼180° with concomitant loss of conserved enzyme-PLP interactions. A nearby region of the polypeptide becomes disordered, evidenced by missing electron density for ∼10 residues. These structural perturbations are consistent with the loss of enzyme activity and folate binding and underscore the important role of the Pro285 cis-peptide in SHMT structure and function., (© 2024 The Author(s). Published by Portland Press Limited on behalf of the Biochemical Society.)

Published

2024

3. Structure-based characterization and compound identification of the wild-type THF class-II riboswitch.

Author

Li C, Xu X, Geng Z, Zheng L, Song Q, Shen X, Wu J, Zhao J, Li H, He M, Tai X, Zhang L, Ma J, Dong Y, and Ren A

Subjects

Ligands, Models, Molecular, RNA Folding, Nucleotide Motifs, Mutation, Riboswitch genetics, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Nucleic Acid Conformation

Abstract

Riboswitches are conserved regulatory RNA elements participating in various metabolic pathways. Recently, a novel RNA motif known as the folE RNA motif was discovered upstream of folE genes. It specifically senses tetrahydrofolate (THF) and is therefore termed THF-II riboswitch. To unravel the ligand recognition mechanism of this newly discovered riboswitch and decipher the underlying principles governing its tertiary folding, we determined both the free-form and bound-form THF-II riboswitch in the wild-type sequences. Combining structural information and isothermal titration calorimetry (ITC) binding assays on structure-based mutants, we successfully elucidated the significant long-range interactions governing the function of THF-II riboswitch and identified additional compounds, including alternative natural metabolites and potential lead compounds for drug discovery, that interact with THF-II riboswitch. Our structural research on the ligand recognition mechanism of the THF-II riboswitch not only paves the way for identification of compounds targeting riboswitches, but also facilitates the exploration of THF analogs in diverse biological contexts or for therapeutic applications., (© The Author(s) 2024. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2024

4. The Second Class of Tetrahydrofolate (THF-II) Riboswitches Recognizes the Tetrahydrofolic Acid Ligand via Local Conformation Changes.

Author

Zhang M, Liu G, Zhang Y, Chen T, Feng S, Cai R, and Lu C

Subjects

Ligands, Nucleic Acid Conformation, Scattering, Small Angle, Tetrahydrofolates chemistry, Tetrahydrofolates genetics, Tetrahydrofolates metabolism, X-Ray Diffraction, Riboswitch

Abstract

Riboswitches are regulatory noncoding RNAs found in bacteria, fungi and plants, that modulate gene expressions through structural changes in response to ligand binding. Understanding how ligands interact with riboswitches in solution can shed light on the molecular mechanisms of this ancient regulators. Previous studies showed that riboswitches undergo global conformation changes in response to ligand binding to relay information. Here, we report conformation switching models of the recently discovered tetrahydrofolic acid-responsive second class of tetrahydrofolate (THF-II) riboswitches in response to ligand binding. Using a combination of selective 2'-hydroxyl acylation, analyzed by primer extension (SHAPE) assay, 3D modeling and small-angle X-ray scattering (SAXS), we found that the ligand specifically recognizes and reshapes the THF-II riboswitch loop regions, but does not affect the stability of the P3 helix. Our results show that the THF-II riboswitch undergoes only local conformation changes in response to ligand binding, rearranging the Loop1-P3-Loop2 region and rotating Loop1 from a ~120° angle to a ~75° angle. This distinct conformation changes suggest a unique regulatory mechanism of the THF-II riboswitch, previously unseen in other riboswitches. Our findings may contribute to the fields of RNA sensors and drug design.

Published

2022

5. The bioaccessibility of folate in breads and the stability of folate vitamers during in vitro digestion.

Author

Liu F, Edelmann M, Piironen V, and Kariluoto S

Subjects

Biological Availability, Folic Acid analogs & derivatives, Folic Acid chemistry, Folic Acid metabolism, In Vitro Techniques, Nutrients analysis, Tetrahydrofolates analysis, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Bread analysis, Digestion, Folic Acid analysis

Abstract

Both the liberation and stability of endogenous folate are relevant to the bioaccessibility of folate. Since folates are unstable, in addition to studying the natural folate content in foods, bioaccessibility should be considered. To understand folate changes during digestion, a mixture of standard folate compounds was subjected to a static in vitro gastrointestinal digestion assay. Next, different types of bread were analysed to study how food matrices influence folate bioaccessibility. Folates were identified and quantitated by a UHPLC-PDA/FL method. Folic acid and 10-formylfolic acid were stable throughout the digestion, and the conversions among formyl folates and 5,10-methenyltetrahydrofolate were triggered at the gastric phase. Tetrahydrofolate began to degrade during the oral phase and was lost completely during the gastric phase. During the intestinal phase, 5-methyltetrahydrofolate began to degrade and suffered a 60% loss. With bread matrices, folate conversions and the decrease of reduced folates were also common, but the extent of changes varied. Generally, rye breads had the highest (80-120%) bioaccessibility of folate, while oat breads had the lowest (31-102%). The high proportion of 5-methyltetrahydrofolate could result in low bioaccessibility because of its relatively low stability during digestion in bread matrices. An increase in 10-formylfolic acid content was observed for all the breads, but 10-formyldihydrofolate seemed to be more stable in rye breads than in oat and wheat breads. The results showed that folates undergo significant changes during digestion and that food matrices could be modified to affect these changes towards better folate bioaccessibility.

Published

2022

6. Improved Stability of a Stable Crystal Form C of 6S-5-Methyltetrahydrofolate Calcium Salt, Method Development and Validation of an LC-MS/MS Method for Rat Pharmacokinetic Comparison.

Author

Lian Z, Chen H, Liu K, Jia Q, Qiu F, and Cheng Y

Subjects

Animals, Crystallization, Drug Stability, Male, Rats, Rats, Sprague-Dawley, Chromatography, Liquid methods, Tandem Mass Spectrometry methods, Tetrahydrofolates chemistry, Tetrahydrofolates pharmacokinetics

Abstract

Folate is a vitamin beneficial for humans that plays an important role in metabolism, but it cannot be well supplemented by food; it is necessary to supplement it in other ways. Based on this consideration, a novel crystal form C of 6S-5-methyltetrahydrofolate calcium salt (MTHF CAC) was obtained. To explore the difference between MTHF CAC and the crystal form Ⅰ of 6S-5-methyltetrahydrofolate calcium salt (MTHF CA) as well as an amorphous product of 6S-5-methyltetrahydrofolate glucosamine salt (MTHF GA), their stability and pharmacokinetic behaviours were compared. The results of high-performance liquid chromatography coupled with ultraviolet detection analysis indicated that MTHF CAC showed a better stability than MTHF CA and MTHF GA. After oral administration of MTHF CAC, MTHF CA, and MTHF GA to male rats, the MTHF concentrations were analysed using a validated liquid chromatography-tandem mass spectrometry, and the pharmacokinetic parameters were compared. The mean residence times (0-t) of MTHF CAC, MTHF CA, and MTHF GA were 3.7 ± 1.9 h, 1.0 ± 0.2 h ( p < 0.01), and 1.5 ± 0.3 h ( p < 0.05), respectively. The relative bioavailability of MTHF CAC was calculated to be 351% and 218% compared with MTHF CA and MTHF GA, respectively, which suggests that MTHF CAC can be better absorbed and utilized for a longer period of time.

Published

2021

7. Role of Active Site Loop Dynamics in Mediating Ligand Release from E. coli Dihydrofolate Reductase.

Author

Singh A, Fenwick RB, Dyson HJ, and Wright PE

Subjects

Binding Sites, Catalytic Domain, Kinetics, Ligands, Magnetic Resonance Spectroscopy methods, Models, Molecular, Protein Conformation, Escherichia coli metabolism, Tetrahydrofolate Dehydrogenase chemistry, Tetrahydrofolate Dehydrogenase metabolism, Tetrahydrofolates chemistry

Abstract

Conformational fluctuations from ground-state to sparsely populated but functionally important excited states play a key role in enzyme catalysis. For Escherichia coli dihydrofolate reductase (DHFR), the release of the product tetrahydrofolate (THF) and oxidized cofactor NADP + occurs through exchange between closed and occluded conformations of the Met20 loop. A "dynamic knockout" mutant of E. coli DHFR, where the E. coli sequence in the Met20 loop is replaced by the human sequence (N23PP/S148A), models human DHFR and is incapable of accessing the occluded conformation. 1 H and 15 N CPMG relaxation dispersion analysis for the ternary product complex of the mutant enzyme with NADP + and the product analogue 5,10-dideazatetrahydrofolate (ddTHF) (E:ddTHF:NADP + ) reveals the mechanism by which NADP + is released when the Met20 loop cannot undergo the closed-to-occluded conformational transition. Two excited states were observed: one related to a faster, relatively high-amplitude conformational fluctuation in areas near the active site, associated with the shuttling of the nicotinamide ring of the cofactor out of the active site, and the other to a slower process where ddTHF undergoes small-amplitude motions within the binding site that are consistent with disorder observed in a room-temperature X-ray crystal structure of the N23PP/S148A mutant protein. These motions likely arise due to steric conflict of the pterin ring of ddTHF with the ribose-nicotinamide moiety of NADP + in the closed active site. These studies demonstrate that site-specific kinetic information from relaxation dispersion experiments can provide intimate details of the changes in catalytic mechanism that result from small changes in local amino acid sequence.

Published

2021

8. Formaldehyde regulates tetrahydrofolate stability and thymidylate synthase catalysis.

Author

Chen X, Chothia SY, Basran J, and Hopkinson RJ

Subjects

Biocatalysis, Enzyme Stability, Formaldehyde chemistry, Humans, Molecular Structure, Tetrahydrofolates chemistry, Thymidylate Synthase chemistry, Formaldehyde metabolism, Tetrahydrofolates metabolism, Thymidylate Synthase metabolism

Abstract

Tetrahydrofolic acid and formaldehyde are key human metabolites but their physiologically relevant chemistry is undefined. Our NMR studies confirm formaldehyde as a product of tetrahydrofolic acid degradation but also reveal their reaction regulates the stability of tetrahydrofolic acid. These observations identify a novel non-enzymatic feedback mechanism regulating formaldehyde and folate metabolism that has important implications for folate-targeting chemotherapy in cancer and other diseases.

Published

2021

9. Caught in Action: X-ray Structure of Thymidylate Synthase with Noncovalent Intermediate Analog.

Author

Kholodar SA, Finer-Moore JS, Świderek K, Arafet K, Moliner V, Stroud RM, and Kohen A

Subjects

Crystallography, X-Ray, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Deoxyuracil Nucleotides chemistry, Deoxyuracil Nucleotides metabolism, Models, Molecular, Protein Conformation, Catalytic Domain, Molecular Dynamics Simulation, Thymidine Monophosphate chemistry, Thymidine Monophosphate metabolism, Thymidylate Synthase chemistry, Thymidylate Synthase metabolism

Abstract

Methylation of 2-deoxyuridine-5'-monophosphate (dUMP) at the C5 position by the obligate dimeric thymidylate synthase (TSase) in the sole de novo biosynthetic pathway to thymidine 5'-monophosphate (dTMP) proceeds by forming a covalent ternary complex with dUMP and cosubstrate 5,10-methylenetetrahydrofolate. The crystal structure of an analog of this intermediate gives important mechanistic insights but does not explain the half-of-the-sites activity of the enzyme. Recent experiments showed that the C5 proton and the catalytic Cys are eliminated in a concerted manner from the covalent ternary complex to produce a noncovalent bisubstrate intermediate. Here, we report the crystal structure of TSase with a close synthetic analog of this intermediate in which it has partially reacted with the enzyme but in only one protomer, consistent with the half-of-the-sites activity of this enzyme. Quantum mechanics/molecular mechanics simulations confirmed that the analog could undergo catalysis. The crystal structure shows a new water 2.9 Å from the critical C5 of the dUMP moiety, which in conjunction with other residues in the network, may be the elusive general base that abstracts the C5 proton of dUMP during the reaction.

Published

2021

10. Folate Content and Yolk Color of Hen Eggs from Different Farming Systems.

Author

Czarnowska-Kujawska M, Draszanowska A, Gujska E, Klepacka J, and Kasińska M

Subjects

Adolescent, Adult, Animals, Chickens, Child, Child, Preschool, Color, Cooking, Female, Folic Acid chemistry, Humans, Infant, Male, Polyglutamic Acid analogs & derivatives, Polyglutamic Acid chemistry, Tetrahydrofolates chemistry, Young Adult, Agriculture, Egg Yolk chemistry, Eggs analysis, Folic Acid analysis

Abstract

This study aimed to compare folate contents in hen eggs from four different farming systems, namely organic, free range, barn, and cage one. Folate retention during egg boiling was studied as well. The contents of individual folate vitamers were determined using the high-performance liquid chromatography method (HPLC), following trienzyme treatment. Folate content in eggs differed significantly ( p < 0.05) due to the rearing system, with the highest mean content determined in the eggs from organic farming (113.8 µg/100 g). According to this study, one egg (60 g) may provide 40-86 µg of folates, which corresponds to 10-22% of the recommended daily intake for adults, 400 µg according to the Nutrition Standards for the Polish Population. The predominant folate form found in egg was 5-methyltetrahydrofolate, which showed considerably greater stability under boiling compared to 10-formylfolic acid present in a lower amount. In most eggs tested, the losses in total folate content did not exceed 15%. The color of yolk of the most folate-abundant organic eggs, had the highest value of lightness (L*) and the lowest value of redness (a*). This, however, does not correspond to consumer preferences of intense golden yolk color.

Published

2021

11. Four families of folate-independent methionine synthases.

Author

Price MN, Deutschbauer AM, and Arkin AP

Subjects

5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase metabolism, Archaeal Proteins metabolism, Bacterial Proteins metabolism, Biosynthetic Pathways genetics, Folic Acid chemistry, Folic Acid metabolism, Homocysteine chemistry, Homocysteine metabolism, Iron-Sulfur Proteins metabolism, Methionine chemistry, Methionine metabolism, Models, Chemical, Molecular Structure, Oxygen metabolism, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Vitamin B 12 analogs & derivatives, Vitamin B 12 chemistry, Vitamin B 12 metabolism, 5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase genetics, Archaeal Proteins genetics, Bacterial Proteins genetics, Multigene Family

Abstract

Although most organisms synthesize methionine from homocysteine and methyl folates, some have "core" methionine synthases that lack folate-binding domains and use other methyl donors. In vitro, the characterized core synthases use methylcobalamin as a methyl donor, but in vivo, they probably rely on corrinoid (vitamin B12-binding) proteins. We identified four families of core methionine synthases that are distantly related to each other (under 30% pairwise amino acid identity). From the characterized enzymes, we identified the families MesA, which is found in methanogens, and MesB, which is found in anaerobic bacteria and archaea with the Wood-Ljungdahl pathway. A third uncharacterized family, MesC, is found in anaerobic archaea that have the Wood-Ljungdahl pathway and lack known forms of methionine synthase. We predict that most members of the MesB and MesC families accept methyl groups from the iron-sulfur corrinoid protein of that pathway. The fourth family, MesD, is found only in aerobic bacteria. Using transposon mutants and complementation, we show that MesD does not require 5-methyltetrahydrofolate or cobalamin. Instead, MesD requires an uncharacterized protein family (DUF1852) and oxygen for activity., Competing Interests: The authors have declared that no competing interests exist.

Published

2021

12. Pharmacokinetics of Sodium and Calcium Salts of (6S)-5-Methyltetrahydrofolic Acid Compared to Folic Acid and Indirect Comparison of the Two Salts.

Author

Obeid R, Schön C, Pietrzik K, Menzel D, Wilhelm M, Smulders Y, Knapp JP, and Böhni R

Subjects

Adult, Area Under Curve, Cross-Over Studies, Double-Blind Method, Female, Folic Acid blood, Humans, Male, Tetrahydrofolates blood, Tetrahydrofolates chemistry, Young Adult, Folic Acid pharmacokinetics, Tetrahydrofolates pharmacokinetics

Abstract

(6S)-5-Methyltetrahydrofolic acid ((6S)-5-Methyl-THF) salts and folic acid may differ in their abilities to raise plasma (6S)-5-Methyl-THF levels. We compared the area under the curve (AUC), C max , and T max of plasma (6S)-5-Methyl-THF after intakes of (6S)-5-Methyl-THF-Na salt (Arcofolin ® ) and folic acid. Moreover, we compared the AUCs after intakes of (6S)-5-Methyl-THF-Na and the calcium salt, (6S)-5-Methyl-THF-Ca, that were tested against folic acid in two independent studies. The study was randomized, double blind, and cross over. Twenty-four adults (12 men and 12 women) received a single oral dose of 436 µg (6S)-5-Methyl-THF-Na and an equimolar dose of folic acid (400 µg) on two kinetic days with two weeks washout period in between. The plasma concentrations of (6S)-5-Methyl-THF were measured at 9 time points between 0 and 8 h. We found that the AUC 0-8 h of plasma (6S)-5-Methyl-THF (mean (SD) = 126.0 (33.6) vs. 56.0 (25.3) nmol/L*h) and C max (36.8 (10.8) vs. 11.1 (4.1) nmol/L) were higher after administration of (6S)-5-Methyl-THF-Na than after the administration of folic acid ( p < 0.001 for both). These differences were present in men and women. Only administration of folic acid resulted in a transient increase in plasma unmetabolized folic acid (2.5 (2.0) nmol/L after 0.5 h and 4.7 (2.9) nmol/L after 1 h). Intake of (6S)-5-Methyl-THF-Na was safe. The ratios of the AUC 0-8 h for (6S)-5-Methyl-THF-Na and (6S)-5-Methyl-THF-Ca to the corresponding folic acid reference group and the delta of these AUC 0-8 h did not differ between the studies. In conclusion, a single oral dose of (6S)-5-Methyl-THF-Na caused higher AUC 0-8 h and C max of plasma (6S)-5-Methyl-THF compared to folic acid. The Na- and Ca- salts of (6S)-5-Methyl-THF are not likely to differ in their pharmacokinetics. Further studies may investigate whether supplementation of the compounds for a longer time will lead to differences in circulating or intracellular/tissue folate concentrations.

Published

2020

13. Structures in Tetrahydrofolate Methylation in Desulfitobacterial Glycine Betaine Metabolism at Atomic Resolution.

Author

Badmann T and Groll M

Subjects

Bacterial Proteins chemistry, Bacterial Proteins metabolism, Betaine chemistry, Biocatalysis, Crystallography, X-Ray, Desulfitobacterium metabolism, Methylation, Models, Molecular, Molecular Structure, Tetrahydrofolates chemistry, Betaine metabolism, Desulfitobacterium chemistry, Tetrahydrofolates metabolism

Abstract

Enzymes orchestrating methylation between tetrahydrofolate (THF) and cobalamin (Cbl) are abundant among all domains of life. During energy production in Desulfitobacterium hafniense, MtgA catalyzes the methyl transfer from methylcobalamin (Cbl-CH 3 ) to THF in the catabolism of glycine betaine (GB). Despite its lack of sequence identity with known structures, we could show that MtgA forms a homodimeric complex of two TIM barrels. Atomic crystallographic insights into the interplay of MtgA with THF as well as analysis of a trapped reaction intermediate (THF-CH 3 ) + reveal conformational rearrangements during the transfer reaction. Whereas residues for THF methylation are conserved, the binding mode for the THF glutamyl-p-aminobenzoate moiety (THF tail) is unique. Apart from snapshots of individual reaction steps of MtgA, structure-based mutagenesis combined with enzymatic activity assays allowed a mechanistic description of the methyl transfer between Cbl-CH 3 and THF. Altogether, the THF-tail-binding motion observed in MtgA is unique compared to other THF methyltransferases and therefore contributes to the general understanding of THF-mediated methyl transfer., (© 2019 The Authors. Published by Wiley-VCH Verlag GmbH & Co. KGaA.)

Published

2020

14. Impaired folate binding of serine hydroxymethyltransferase 8 from soybean underlies resistance to the soybean cyst nematode.

Author

Korasick DA, Kandoth PK, Tanner JJ, Mitchum MG, and Beamer LJ

Subjects

Animals, Binding Sites, Conserved Sequence, Glycine Hydroxymethyltransferase chemistry, Kinetics, Ligands, Models, Biological, Models, Molecular, Plant Proteins chemistry, Pyridoxal Phosphate metabolism, Static Electricity, Structural Homology, Protein, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Disease Resistance, Folic Acid metabolism, Glycine Hydroxymethyltransferase metabolism, Nematoda physiology, Plant Diseases parasitology, Plant Proteins metabolism, Glycine max enzymology

Abstract

Management of the agricultural pathogen soybean cyst nematode (SCN) relies on the use of SCN-resistant soybean cultivars, a strategy that has been failing in recent years. An underutilized source of resistance in the soybean genotype Peking is linked to two polymorphisms in serine hydroxy-methyltransferase 8 (SHMT8). SHMT is a pyridoxal 5'-phosphate-dependent enzyme that converts l-serine and (6 S )-tetrahydrofolate to glycine and 5,10-methylenetetrahydrofolate. Here, we determined five crystal structures of the 1884-residue SHMT8 tetramers from the SCN-susceptible cultivar (cv.) Essex and the SCN-resistant cv. Forrest (whose resistance is derived from the SHMT8 polymorphisms in Peking); the crystal structures were determined in complex with various ligands at 1.4-2.35 Å resolutions. We find that the two Forrest-specific polymorphic substitutions (P130R and N358Y) impact the mobility of a loop near the entrance of the (6 S )-tetrahydrofolate-binding site. Ligand-binding and kinetic studies indicate severely reduced affinity for folate and dramatically impaired enzyme activity in Forrest SHMT8. These findings imply widespread effects on folate metabolism in soybean cv. Forrest that have implications for combating the widespread increase in virulent SCN., (© 2020 Korasick et al.)

Published

2020

15. Mutational landscape screening of methylene tetrahydrofolate reductase to predict homocystinuria associated variants: An integrative computational approach.

Author

Nagarajan H, Narayanaswamy S, and Vetrivel U

Subjects

Allosteric Site, Amino Acid Motifs, Catalytic Domain, Crystallography, X-Ray, Gene Expression, Homocystinuria enzymology, Homocystinuria pathology, Humans, Isoenzymes chemistry, Isoenzymes genetics, Isoenzymes metabolism, Machine Learning, Methylenetetrahydrofolate Reductase (NADPH2) genetics, Methylenetetrahydrofolate Reductase (NADPH2) metabolism, Molecular Docking Simulation, Molecular Dynamics Simulation, NADP chemistry, NADP metabolism, Protein Binding, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Interaction Domains and Motifs, S-Adenosylmethionine metabolism, Substrate Specificity, Tetrahydrofolates metabolism, Thermodynamics, Homocystinuria genetics, Methylenetetrahydrofolate Reductase (NADPH2) chemistry, Mutation, Missense, S-Adenosylmethionine chemistry, Tetrahydrofolates chemistry

Abstract

Methylene tetrahydrofolate reductase (MTHFR) is a flavoprotein, involved in one-carbon pathway and is responsible for folate and homocysteine metabolism. Regulation of MTHFR is pivotal for maintaining the cellular concentrations of methionine and SAM (S-adenosyl methionine) which are essential for the synthesis of nucleotides and amino acids, respectively. Therefore, mutations in MTHFR leads to its dysfunction resulting in conditions like homocystinuria, cardiovascular diseases, and neural tube defects in infants. Among these conditions, homocystinuria has been highly explored, as it manifests ocular disorders, cognitive disorders and skeletal abnormalities. Hence, in this study, we intend to explore the mutational landscape of human MTHFR isoform-1 (h.MTHFR-1) to decipher the most pathogenic variants pertaining to homocystinuria. Thus, a multilevel stringent prioritization of non-synonymous mutations in h.MTHFR-1 by integrative machine learning approaches was implemented to delineate highly deleterious variants based on its pathogenicity, impact on structural stability and functionality. Subsequently, extended molecular dynamics simulations and molecular docking studies were also integrated in order to prioritize the mutations that perturbs structural stability and functionality of h.MTHFR-1. In addition, displacement of Loop (Arg157-Tyr174) and helix α9 (His263-Ser272) involved in open/closed conformation of substrate binding domain were also probed to confirm the functional loss. On juxtaposed analysis, it was inferred that among 126 missense mutations screened, along with known pathogenic mutations (H127 T, A222 V, T227 M, F257 V and G387D) predicted that W500C, P254S and D585 N variants could be potentially driving homocystinuria. Thus, uncovering the prospects for inclusion of these mutations in diagnostic panels based on further experimental validations., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

16. A flap motif in human serine hydroxymethyltransferase is important for structural stabilization, ligand binding, and control of product release.

Author

Ubonprasert S, Jaroensuk J, Pornthanakasem W, Kamonsutthipaijit N, Wongpituk P, Mee-Udorn P, Rungrotmongkol T, Ketchart O, Chitnumsub P, Leartsakulpanich U, Chaiyen P, and Maenpuen S

Subjects

Amino Acid Motifs, Binding Sites, Enzyme Stability, Glycine Hydroxymethyltransferase genetics, Glycine Hydroxymethyltransferase metabolism, Humans, Kinetics, Molecular Dynamics Simulation, Mutagenesis, Protein Binding, Protein Multimerization, Protein Structure, Quaternary, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Substrate Specificity, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Glycine Hydroxymethyltransferase chemistry, Ligands

Abstract

Human cytosolic serine hydroxymethyltransferase (hcSHMT) is a promising target for anticancer chemotherapy and contains a flexible "flap motif" whose function is yet unknown. Here, using size-exclusion chromatography, analytical ultracentrifugation, small-angle X-ray scattering (SAXS), molecular dynamics (MD) simulations, and ligand-binding and enzyme-kinetic analyses, we studied the functional roles of the flap motif by comparing WT hcSHMT with a flap-deleted variant (hcSHMT/Δflap). We found that deletion of the flap results in a mixture of apo-dimers and holo-tetramers, whereas the WT was mostly in the tetrameric form. MD simulations indicated that the flap stabilizes structural compactness and thereby enhances oligomerization. The hcSHMT/Δflap variant exhibited different catalytic properties in (6 S )-tetrahydrofolate (THF)-dependent reactions compared with the WT but had similar activity in THF-independent aldol cleavage of β-hydroxyamino acid. hcSHMT/Δflap was less sensitive to THF inhibition than the WT ( K i of 0.65 and 0.27 mm THF at pH 7.5, respectively), and the THF dissociation constant of the WT was also 3-fold lower than that of hcSHMT/Δflap, indicating that the flap is important for THF binding. hcSHMT/Δflap did not display the burst kinetics observed in the WT. These results indicate that, upon removal of the flap, product release is no longer the rate-limiting step, implying that the flap is important for controlling product release. The findings reported here improve our understanding of the functional roles of the flap motif in hcSHMT and provide fundamental insight into how a flexible loop can be involved in controlling the enzymatic reactions of hcSHMT and other enzymes., (© 2019 Ubonprasert et al.)

Published

2019

17. Metabolic Intermediates in Tumorigenesis and Progression.

Author

He Y, Gao M, Tang H, Cao Y, Liu S, and Tao Y

Subjects

Acetyl Coenzyme A chemistry, Acetyl Coenzyme A metabolism, Acetyl Coenzyme A physiology, Cell Proliferation drug effects, Disease Progression, Flavin-Adenine Dinucleotide chemistry, Flavin-Adenine Dinucleotide metabolism, Flavin-Adenine Dinucleotide physiology, Humans, NAD chemistry, NAD metabolism, NAD physiology, Neoplasm Invasiveness, Neoplasms pathology, Neoplasms therapy, S-Adenosylmethionine chemistry, S-Adenosylmethionine metabolism, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Tetrahydrofolates physiology, Antineoplastic Agents adverse effects, Carcinogenesis metabolism, Neoplasms metabolism

Abstract

Traditional antitumor drugs inhibit the proliferation and metastasis of tumour cells by restraining the replication and expression of DNA. These drugs are usually highly cytotoxic. They kill tumour cells while also cause damage to normal cells at the same time, especially the hematopoietic cells that divide vigorously. Patients are exposed to other serious situations such as a severe infection caused by a decrease in the number of white blood cells. Energy metabolism is an essential process for the survival of all cells, but differs greatly between normal cells and tumour cells in metabolic pathways and metabolic intermediates. Whether this difference could be used as new therapeutic target while reducing damage to normal tissues is the topic of this paper. In this paper, we introduce five major metabolic intermediates in detail, including acetyl-CoA, SAM, FAD, NAD + and THF. Their contents and functions in tumour cells and normal cells are significantly different. And the possible regulatory mechanisms that lead to these differences are proposed carefully. It is hoped that the key enzymes in these regulatory pathways could be used as new targets for tumour therapy., Competing Interests: Competing Interests: The authors have declared that no competing interest exists.

Published

2019

18. The Bacterial [Fe]-Hydrogenase Paralog HmdII Uses Tetrahydrofolate Derivatives as Substrates.

Author

Watanabe T, Wagner T, Huang G, Kahnt J, Ataka K, Ermler U, and Shima S

Subjects

Biocatalysis, Crystallization, Guanine analogs & derivatives, Guanine biosynthesis, Hydrogenation, Oxidation-Reduction, Protein Binding, Protein Conformation, Pyridines, Bacteria enzymology, Bacterial Proteins metabolism, Hydrogenase metabolism, Iron-Sulfur Proteins metabolism, Tetrahydrofolates chemistry

Abstract

[Fe]-hydrogenase (Hmd) catalyzes the reversible hydrogenation of methenyl-tetrahydromethanopterin (methenyl-H 4 MPT + ) with H 2 . H 4 MPT is a C1-carrier of methanogenic archaea. One bacterial genus, Desulfurobacterium, contains putative genes for the Hmd paralog, termed HmdII, and the HcgA-G proteins. The latter are required for the biosynthesis of the prosthetic group of Hmd, the iron-guanylylpyridinol (FeGP) cofactor. This finding is intriguing because Hmd and HmdII strictly use H 4 MPT derivatives that are absent in most bacteria. We identified the presence of the FeGP cofactor in D. thermolithotrophum. The bacterial HmdII reconstituted with the FeGP cofactor catalyzed the hydrogenation of derivatives of tetrahydrofolate, the bacterial C1-carrier, albeit with low enzymatic activities. The crystal structures show how Hmd recognizes tetrahydrofolate derivatives. These findings have an impact on future biotechnology by identifying a bacterial Hmd paralog., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

19. Design strategy for serine hydroxymethyltransferase probes based on retro-aldol-type reaction.

Author

Nonaka H, Nakanishi Y, Kuno S, Ota T, Mochidome K, Saito Y, Sugihara F, Takakusagi Y, Aoki I, Nagatoishi S, Tsumoto K, and Sando S

Subjects

Biomarkers chemistry, Crystallography, X-Ray, Fluorescent Dyes, Fluorine-19 Magnetic Resonance Imaging, Glycine chemistry, High-Throughput Screening Assays, Humans, Serine chemistry, Tetrahydrofolates chemistry, Aldehydes metabolism, Glycine Hydroxymethyltransferase antagonists & inhibitors, Glycine Hydroxymethyltransferase metabolism, Molecular Probes metabolism

Abstract

Serine hydroxymethyltransferase (SHMT) is an enzyme that catalyzes the reaction that converts serine to glycine. It plays an important role in one-carbon metabolism. Recently, SHMT has been shown to be associated with various diseases. Therefore, SHMT has attracted attention as a biomarker and drug target. However, the development of molecular probes responsive to SHMT has not yet been realized. This is because SHMT catalyzes an essential yet simple reaction; thus, the substrates that can be accepted into the active site of SHMT are limited. Here, we focus on the SHMT-catalyzed retro-aldol reaction rather than the canonical serine-glycine conversion and succeed in developing fluorescent and 19 F NMR molecular probes. Taking advantage of the facile and direct detection of SHMT, the developed fluorescent probe is used in the high-throughput screening for human SHMT inhibitors, and two hit compounds are obtained.

Published

2019

20. Theoretical Evaluation of the Reaction Mechanism of Serine Hydroxymethyltransferase.

Author

Santatiwongchai J, Gleeson D, and Gleeson MP

Subjects

Biocatalysis, Catalytic Domain, Models, Chemical, Molecular Dynamics Simulation, Plasmodium vivax enzymology, Pyridoxal Phosphate chemistry, Quantum Theory, Serine chemistry, Tetrahydrofolates chemistry, Glycine Hydroxymethyltransferase chemistry

Abstract

Serine hydroxymethyltransferase (SHMT) is a pyridoxal phosphate (PLP)-dependent enzyme that catalyzes the reversible conversion of serine and tetrahydrofolate (THF) to glycine and 5,10-methylene THF. SHMT is a folate pathway enzyme and is therefore of considerable medical interest due to its role as an important intervention point for antimalarial, anticancer, and antibacterial treatments. Despite considerable experimental effort, the precise reaction mechanism of SHMT remains unclear. In this study, we explore the mechanism of SHMT to determine the roles of active site residues and the nature and the sequence of chemical steps. Molecular dynamics (MD) methods were employed to generate a suitable starting structure which then underwent analysis using hybrid quantum mechanical/molecular mechanical (QM/MM) simulations. The QM region consisted of 12 key residues, two substrates, and explicit solvent. Our results show that the catalytic reaction proceeds according to a retro-aldol synthetic process with His129 acting as the general base in the reaction. The rate-determining step involves the cleavage of the PLP-serine aldimine C α -C β bond and the formation of formaldehyde in line with experimental evidence. The pyridyl ring of the PLP-serine aldimine substrate exists in deprotonated form, being stabilized directly by Asp208 via a strong H-bond, as well as through interactions with Arg371, Lys237, and His211, and with the surrounding protein which was electrostatically embedded. This knowledge has the potential to impact the design and development of new inhibitors.

Published

2019

21. Handling and Analysis of 5-Formyl-, 5,10-Methenyl-, 10-Formyl-, 5-Formimno-, and 5,10-Methylenetetrahydrofolates.

Author

Lewin AH and Silinski P

Subjects

Chromatography, High Pressure Liquid methods, Mass Spectrometry methods, Oxidation-Reduction, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Metabolomics methods, Tetrahydrofolates analysis

Abstract

As the principal one-carbon carriers in mammalian biology, tetrahydrofolates are crucial for normal and malignant cells to synthesize and repair DNA and are the target of extensive research, including metabolomics analysis. The susceptibility of tetrahydrofolates to oxidization, as well as the propensity of substituted tetrahydrofolates to chemical degradation, mandates the use of carefully controlled experimental conditions to ensure their integrity. Analytical protocols for LC analysis along with handling and storage conditions for 5-formyl-, 5,10-methenyl-,10-formyl-, 5-formimno-, and 5,10-methylenetetrahydrofolate are described.

Published

2019

22. Parallel reaction pathways and noncovalent intermediates in thymidylate synthase revealed by experimental and computational tools.

Author

Kholodar SA, Ghosh AK, Świderek K, Moliner V, and Kohen A

Subjects

Catalysis, Deoxyuracil Nucleotides chemistry, Deoxyuracil Nucleotides metabolism, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Kinetics, Molecular Dynamics Simulation, Quantum Theory, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Thymidylate Synthase chemistry, Thymidylate Synthase metabolism

Abstract

Thymidylate synthase was one of the most studied enzymes due to its critical role in molecular pathogenesis of cancer. Nevertheless, many atomistic details of its chemical mechanism remain unknown or debated, thereby imposing limits on design of novel mechanism-based anticancer therapeutics. Here, we report unprecedented isolation and characterization of a previously proposed intact noncovalent bisubstrate intermediate formed in the reaction catalyzed by thymidylate synthase. Free-energy surfaces of the bisubstrate intermediates interconversions computed with quantum mechanics/molecular mechanics (QM/MM) methods and experimental assessment of the corresponding kinetics indicate that the species is the most abundant productive intermediate along the reaction coordinate, whereas accumulation of the covalent bisubstrate species largely occurs in a parallel nonproductive pathway. Our findings not only substantiate relevance of the previously proposed noncovalent intermediate but also support potential implications of the overstabilized covalent intermediate in drug design targeting DNA biosynthesis., Competing Interests: The authors declare no conflict of interest., (Copyright © 2018 the Author(s). Published by PNAS.)

Published

2018

23. Structure of 6-hydroxymethyl-7,8-dihydropterin pyrophosphokinase-dihydropteroate synthase from Plasmodium vivax sheds light on drug resistance.

Author

Yogavel M, Nettleship JE, Sharma A, Harlos K, Jamwal A, Chaturvedi R, Sharma M, Jain V, Chhibber-Goel J, and Sharma A

Subjects

Amino Acids chemistry, Amino Acids genetics, Crystallography, X-Ray, Dihydropteroate Synthase genetics, Diphosphotransferases genetics, Drug Resistance genetics, Humans, Malaria, Vivax parasitology, Mutation, Plasmodium falciparum, Plasmodium vivax genetics, Plasmodium vivax pathogenicity, Sulfadoxine therapeutic use, Tetrahydrofolates chemistry, Dihydropteroate Synthase chemistry, Diphosphotransferases chemistry, Malaria, Vivax drug therapy, Plasmodium vivax chemistry, Sulfadoxine chemistry

Abstract

The genomes of the malaria-causing Plasmodium parasites encode a protein fused of 6-hydroxymethyl-7,8-dihydropterin pyrophosphokinase (HPPK) and dihydropteroate synthase (DHPS) domains that catalyze sequential reactions in the folate biosynthetic pathway. Whereas higher organisms derive folate from their diet and lack the enzymes for its synthesis, most eubacteria and a number of lower eukaryotes including malaria parasites synthesize tetrahydrofolate via DHPS. Plasmodium falciparum ( Pf ) and Plasmodium vivax ( Pv ) HPPK-DHPSs are currently targets of drugs like sulfadoxine (SDX). The SDX effectiveness as an antimalarial drug is increasingly diminished by the rise and spread of drug-resistant mutations. Here, we present the crystal structure of Pv HPPK-DHPS in complex with four substrates/analogs, revealing the bifunctional Pv HPPK-DHPS architecture in an unprecedented state of enzymatic activation. SDX's effect on HPPK-DHPS is due to 4-amino benzoic acid ( p ABA) mimicry, and the Pv HPPK-DHPS structure sheds light on the SDX-binding cavity, as well as on mutations that effect SDX potency. We mapped five dominant drug resistance mutations in Pv HPPK-DHPS: S382A, A383G, K512E/D, A553G, and V585A, most of which occur individually or in clusters proximal to the p ABA-binding site. We found that these resistance mutations subtly alter the intricate enzyme/ p ABA/SDX interactions such that DHPS affinity for p ABA is diminished only moderately, but its affinity for SDX is changed substantially. In conclusion, the Pv HPPK-DHPS structure rationalizes and unravels the structural bases for SDX resistance mutations and highlights architectural features in HPPK-DHPSs from malaria parasites that can form the basis for developing next-generation anti-folate agents to combat malaria parasites., (© 2018 Yogavel et al.)

Published

2018

24. In Vivo Assimilation of One-Carbon via a Synthetic Reductive Glycine Pathway in Escherichia coli.

Author

Yishai O, Bouzon M, Döring V, and Bar-Even A

Subjects

Amino Acid Oxidoreductases metabolism, Carbon metabolism, Carbon Dioxide metabolism, Carrier Proteins metabolism, Formates chemistry, Formates metabolism, Multienzyme Complexes metabolism, Serine metabolism, Tetrahydrofolates chemistry, Transferases metabolism, Escherichia coli metabolism, Glycine metabolism

Abstract

Assimilation of one-carbon compounds presents a key biochemical challenge that limits their use as sustainable feedstocks for microbial growth and production. The reductive glycine pathway is a synthetic metabolic route that could provide an optimal way for the aerobic assimilation of reduced C1 compounds. Here, we show that a rational integration of native and foreign enzymes enables the tetrahydrofolate and glycine cleavage/synthase systems to operate in the reductive direction, such that Escherichia coli satisfies all of its glycine and serine requirements from the assimilation of formate and CO 2 . Importantly, the biosynthesis of serine from formate and CO 2 does not lower the growth rate, indicating high flux that is able to provide 10% of cellular carbon. Our findings assert that the reductive glycine pathway could support highly efficient aerobic assimilation of C1-feedstocks.

Published

2018

25. Synthesis and physicochemical characterization of (6S)-5-formiminotetrahydrofolate; a reference standard for metabolomics.

Author

Lewin AH, Silinski P, Zhong D, Gilbert A, Mascarella SW, and Seltzman HH

Subjects

Carbon chemistry, Chemistry Techniques, Synthetic methods, Formates chemical synthesis, Oxidation-Reduction, Reference Standards, Tetrahydrofolates chemical synthesis, Formates chemistry, Metabolomics methods, Tetrahydrofolates chemistry

Abstract

The one-carbon carrier of the formate oxidation level derived from the interaction of tetrahydrofolate and formiminoglutamate, which has been tentatively identified as 5-formiminoltetrahydrofolate, has been prepared by chemical synthesis. Treatment of a solution of (6S)-tetrahydrofolate in aqueous base with excess ethyl formimidate in the presence of anti-oxidant under anaerobic conditions afforded a gummy solid which, based on mass spectral analysis, conformed to a monoformimino derivative of tetrahydrofolate. Further physicochemical characterization by validated methods strongly suggested that the product of chemical synthesis was identical to the enzymatically produced material and that it was, in fact, (6S)-5-formiminotetrahydrofolate. Conditions and handling methods toward maintaining the integrity of this highly sensitive compound were identified and are described, as is analytical methodology, useful for research studies using it.

Published

2018

26. A Single Mutation Traps a Half-Sites Reactive Enzyme in Midstream, Explaining Asymmetry in Hydride Transfer.

Author

Finer-Moore JS, Lee TT, and Stroud RM

Subjects

Binding Sites, Catalytic Domain, Crystallography, X-Ray, Escherichia coli enzymology, Folic Acid chemistry, Hydrogen chemistry, Models, Molecular, Mutation, Substrate Specificity, Tetrahydrofolates chemistry, Thymidylate Synthase genetics, Escherichia coli chemistry, Folic Acid analogs & derivatives, Protein Conformation, Quinazolines chemistry, Thymidylate Synthase chemistry

Abstract

In Escherichia coli thymidylate synthase (EcTS), rate-determining hydride transfer from the cofactor 5,10-methylene-5,6,7,8-tetrahydrofolate to the intermediate 5-methylene-2'-deoxyuridine 5'-monophosphate occurs by hydrogen tunneling, requiring precise alignment of reactants and a closed binding cavity, sealed by the C-terminal carboxyl group. Mutations that destabilize the closed conformation of the binding cavity allow small molecules such as β-mercaptoethanol (β-ME) to enter the active site and compete with hydride for addition to the 5-methylene group of the intermediate. The C-terminal deletion mutant of EcTS produced the β-ME adduct in proportions that varied dramatically with cofactor concentration, from 50% at low cofactor concentrations to 0% at saturating cofactor conditions, suggesting communication between active sites. We report the 2.4 Å X-ray structure of the C-terminal deletion mutant of E. coli TS in complex with a substrate and a cofactor analogue, CB3717. The structure is asymmetric, with reactants aligned in a manner consistent with hydride transfer in only one active site. In the second site, CB3717 has shifted to a site where the normal cofactor would be unlikely to form 5-methylene-2'-deoxyuridine 5'-monophosphate, consistent with no formation of the β-ME adduct. The structure shows how the binding of the cofactor at one site triggers hydride transfer and borrows needed stabilization from substrate binding at the second site. It indicates pathways through the dimer interface that contribute to allostery relevant to half-sites reactivity.

Published

2018

27. Assay and Analysis of Dimethylsulfoniopropionate Demethylase.

Author

Reisch CR

Subjects

Bacterial Proteins chemistry, Bacterial Proteins isolation & purification, Chemical Fractionation instrumentation, Chemical Fractionation methods, Chromatography, High Pressure Liquid instrumentation, Chromatography, High Pressure Liquid methods, Demethylation, Enzyme Assays instrumentation, Methyltransferases chemistry, Methyltransferases isolation & purification, Sulfonium Compounds metabolism, Tetrahydrofolates chemistry, Aquatic Organisms metabolism, Bacteria metabolism, Bacterial Proteins metabolism, Enzyme Assays methods, Methyltransferases metabolism

Abstract

Dimethylsulfoniopropionate (DMSP) demethylase is a tetrahydrofolate-dependent enzyme that initiates the DMSP demethylation pathway in marine bacteria. This enzyme is important for understanding of organic sulfur flux from the oceans because it directs the sulfur from DMSP away from dimethylsulfide. This enzyme has been purified and characterized from two marine bacteria from different ecological niches. Both enzymes were confirmed to catalyze the tetrahydrofolate-dependent demethylation of DMSP and possessed similar properties. In this chapter a description of the steps for performing enzyme assays and measuring enzyme activity is provided., (© 2018 Elsevier Inc. All rights reserved.)

Published

2018

28. Bioengineering of crop plants for improved tetrahydrofolate production.

Author

Chaudhary B, Singh N, and Pandey DK

Subjects

Aldehyde-Lyases chemistry, Aldehyde-Lyases metabolism, Allosteric Regulation, Amino Acid Sequence, Bioengineering methods, Escherichia coli classification, Escherichia coli enzymology, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Feedback, Physiological, Models, Molecular, Phylogeny, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Sequence Alignment, Sequence Homology, Amino Acid, Tetrahydrofolates chemistry, Nicotiana enzymology, Transgenes, Aldehyde-Lyases genetics, Escherichia coli genetics, Escherichia coli Proteins genetics, Plants, Genetically Modified, Tetrahydrofolates biosynthesis, Nicotiana genetics

Abstract

De novo synthesis of folates in plants is tightly regulated through feedback-regulation of certain pathway catalysts. Recently, we investigated the prospects of incessant production of folates in an evolutionary conjunction, through the overexpression of feedback targeted and evolutionarily conserved heterologous E.coli dihydroneopterin aldolase (EcDHNA) in tobacco. 1 The enhanced production of folates in the transgenic lines was associated with differential allosteric regulatory cavities accessible at EcDHNA surface having critical amino-acid differences as Ile 64 (His&#95;63), Val 70 (Phe&#95;69), His 75 (Arg&#95;78) and Arg 79 (Glu&#95;72). These structural characteristics are indicative of evolutionary signatures of the catalytic feedback-regulation of folate manufacturing. We exploited the biotechnological potential of such allosterically diverged trans-DHNA for improved folate production in plants. Nonetheless, genetic manipulation of single enzymes modulating complex pathways such as folate biosynthesis is often inadequate to achieve desired phenotypes; therefore, multi-gene integration with explicit genic-combination for folate enrichment in plants has also been projected for future folate agri-biofortification schemes.

Published

2018

29. Exploring the Active Center of the LSD1/CoREST Complex by Molecular Dynamics Simulation Utilizing Its Co-crystallized Co-factor Tetrahydrofolate as a Probe.

Author

Zalloum WA and Zalloum HM

Subjects

Binding Sites, Catalytic Domain, Cluster Analysis, Co-Repressor Proteins chemistry, Crystallization, Crystallography, X-Ray, Histone Demethylases chemistry, Humans, Molecular Dynamics Simulation, Nerve Tissue Proteins chemistry, Protein Binding, Protein Conformation, Tetrahydrofolates chemistry, Co-Repressor Proteins metabolism, Histone Demethylases metabolism, Nerve Tissue Proteins metabolism, Tetrahydrofolates metabolism

Abstract

Epigenetic targeting of cancer is a recent effort to manipulate the gene without destroying the genetic material. Lysine-specific demethylase 1 (LSD1) is one of the enzymes associated with the chromatin for post-translational modifications, where it demethylates lysine amino acid in the chromatin H3 tail. Many studies showed that inhibiting LSD1 could potentially be used to treat cancer epigenetically. LSD1 is associated with its corepressor protein CoREST, and it uses tetrahydrofolate as a co-factor to accept CH 2 from the demethylation process. In this study, the co-crystallized co-factor tetrahydrofolate was utilized to determine possible binding regions in the active center of the LSD1/CoREST complex. Also, the flexibility of the complex has been investigated by molecular dynamics simulation and subsequent analysis by clustering and principal component analysis. This research supported other studies and showed that LSD1/CoREST complex exists in two main conformational structures: open and closed. Furthermore, this study showed that tetrahydrofolate stably binds to the LSD1/CoREST complex, in its open conformation, at its entrance. It then binds to the core of the complex, inducing the closed conformation. Furthermore, the interactions of tetrahydrofolate to these two binding regions and the corresponding binding mode of tetrahydrofolate were investigated to be used in structure-based drug design.

Published

2017

30. Flavin-dependent thymidylate synthase: N5 of flavin as a Methylene carrier.

Author

Karunaratne K, Luedtke N, Quinn DM, and Kohen A

Subjects

Flavins metabolism, Flavoproteins metabolism, Methylation, Tetrahydrofolates metabolism, Thymidine Monophosphate biosynthesis, Thymidine Monophosphate chemistry, Thymidylate Synthase metabolism, Flavins chemistry, Flavoproteins chemistry, Tetrahydrofolates chemistry, Thymidylate Synthase chemistry

Abstract

Thymidylate is synthesized de novo in all living organisms for replication of genomes. The chemical transformation is reductive methylation of deoxyuridylate at C5 to form deoxythymidylate. All eukaryotes including humans complete this well-understood transformation with thymidylate synthase utilizing 6R-N 5 -N 10 -methylene-5,6,7,8-tetrahydrofolate as both a source of methylene and a reducing hydride. In 2002, flavin-dependent thymidylate synthase was discovered as a new pathway for de novo thymidylate synthesis. The flavin-dependent catalytic mechanism is different than thymidylate synthase because it requires flavin as a reducing agent and methylene transporter. This catalytic mechanism is not well-understood, but since it is known to be very different from thymidylate synthase, there is potential for mechanism-based inhibitors that can selectively inhibit the flavin-dependent enzyme to target many human pathogens with low host toxicity., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

31. Determination of Escitalopram Oxalate and L-Methylfolate in Tablet by Spectrophotometric and Reverse Phase High-Performance Liquid Chromatographic Methods.

Author

Sheladia S and Patel B

Subjects

Citalopram chemistry, Limit of Detection, Linear Models, Reproducibility of Results, Spectrophotometry, Ultraviolet methods, Tablets, Tetrahydrofolates chemistry, Chromatography, High Pressure Liquid methods, Citalopram analysis, Tetrahydrofolates analysis

Abstract

Two new simple and selective assay methods have been presented for the analysis of Escitalopram Oxalate (ESC) and L-Methylfolate (L-MF) in pharmaceutical formulations. The ultraviolet (UV)-Spectrophotometric simultaneous equation method was based on the measurement of absorbance at 238 nm (ʎmax of ESC) and 284 nm (ʎmax of L-MF) in methanol. The assay was linear over the concentration ranges 0.5-12.0 μg/mL for ESC and 0.5-9.0 μg/mL for L-MF. The quantitation limits for ESC and L-MF were found to be 0.912 and 0.667 μg/mL; while the detection limits were 0.301 and 0.220 μg/mL for ESC and L-MF, respectively. The second method involved isocratic reversed-phase liquid chromatography using a mobile phase composed of methanol-0.02 M phosphate buffer (pH 5.5) (75:25, v/v), Hypersil BDS-C18 Column (5 µm, 250 mm × 4.6 mm i.d.) with detection at 270 nm. The linearity ranges were found to be 3.0-30.0 and 0.75-22.5 μg/mL for ESC and L-MF, respectively. The limits of detection were found to be 1.065 and 1.160 μg/mL for ESC and L-MF, respectively. The limits of quantitation were found to be 3.226 and 3.515 μg/mL for ESC and L-MF, respectively. The proposed methods were successfully applied to the determination of commercially available tablets with a high percentage of recovery, good accuracy and precision., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2017

32. Reduction of Folate by Dihydrofolate Reductase from Thermotoga maritima.

Author

Loveridge EJ, Hroch L, Hughes RL, Williams T, Davies RL, Angelastro A, Luk LY, Maglia G, and Allemann RK

Subjects

Bacterial Proteins genetics, Bacterial Proteins metabolism, Catalytic Domain, Escherichia coli chemistry, Escherichia coli enzymology, Escherichia coli genetics, Folic Acid metabolism, Gene Expression, Hydrogen-Ion Concentration, Kinetics, NADP chemistry, NADP metabolism, Oxidation-Reduction, Protein Folding, Protein Structure, Secondary, Species Specificity, Temperature, Tetrahydrofolate Dehydrogenase genetics, Tetrahydrofolate Dehydrogenase metabolism, Tetrahydrofolates metabolism, Thermodynamics, Thermotoga maritima chemistry, Thermotoga maritima genetics, Bacterial Proteins chemistry, Folic Acid chemistry, Protons, Tetrahydrofolate Dehydrogenase chemistry, Tetrahydrofolates chemistry, Thermotoga maritima enzymology

Abstract

Mammalian dihydrofolate reductases (DHFRs) catalyze the reduction of folate more efficiently than the equivalent bacterial enzymes do, despite typically having similar efficiencies for the reduction of their natural substrate, dihydrofolate. In contrast, we show here that DHFR from the hyperthermophilic bacterium Thermotoga maritima can catalyze reduction of folate to tetrahydrofolate with an efficiency similar to that of reduction of dihydrofolate under saturating conditions. Nuclear magnetic resonance and mass spectrometry experiments showed no evidence of the production of free dihydrofolate during either the EcDHFR- or TmDHFR-catalyzed reductions of folate, suggesting that both enzymes perform the two reduction steps without release of the partially reduced substrate. Our results imply that the reaction proceeds more efficiently in TmDHFR than in EcDHFR because the more open active site of TmDHFR facilitates protonation of folate. Because T. maritima lives under extreme conditions where tetrahydrofolate is particularly prone to oxidation, this ability to salvage folate may impart an advantage to the bacterium by minimizing the squandering of a valuable cofactor.

Published

2017

33. Allosteric pathways in tetrahydrofolate sensing riboswitch with dynamics correlation network.

Author

Zhang JM, Jiang C, Ye W, Luo R, and Chen HF

Subjects

Allosteric Regulation, Magnetic Resonance Spectroscopy, Molecular Conformation, Nucleic Acid Conformation, RNA, Messenger genetics, Tetrahydrofolates metabolism, Molecular Dynamics Simulation, RNA, Messenger chemistry, Riboswitch, Tetrahydrofolates chemistry

Abstract

Riboswitches are cis-acting genetic control elements. Due to their fundamental importance in bacteria gene regulation, they have been proposed as antibacterial drug targets. Tetrahydrofolate (THF) is an essential cofactor of one-carbon transfer reactions and downregulates the expression of downstream genes. However, information on how to transfer from the binding site of THF to the expression platform is still unavailable. Herein, a nucleotide/nucleotide dynamics correlation network based on an all-atom molecular dynamic simulation was used to reveal the regulation mechanism of a THF-sensing riboswitch. Shortest pathway analysis based on the network illustrates that there is an allosteric pathway through the P2 helix to the pseudoknot, then to the P1 helix in the THF-riboswitch. Thus the hypothesis of "THF-binding induced allosteric switching" was proposed and evaluated using THF and pseudoknot weakened experiments. Furthermore, a possible allosteric pathway of C30-C31-G33-A34-G35-G36-G37-A38-G48-G47-U46-A90-U91-C92-G93-C94-G95-C96 was identified and confirmed through the perturbation of the network. The proposed allosteric mechanism and the underlying allosteric pathway provide fundamental insights for the regulation of THF sensing riboswitches.

Published

2016

34. Overcoming a hemihedral twinning problem in tetrahydrofolate-dependent O-demethylase crystals by the microseeding method.

Author

Harada A, Sato Y, Kamimura N, Venugopalan N, Masai E, and Senda T

Subjects

Amino Acid Sequence, Bacterial Proteins genetics, Bacterial Proteins metabolism, Cloning, Molecular, Crystallization, Crystallography, X-Ray, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression, Oxidoreductases, O-Demethylating genetics, Oxidoreductases, O-Demethylating metabolism, Plasmids chemistry, Plasmids metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sphingomonadaceae enzymology, Tetrahydrofolates metabolism, X-Ray Diffraction, Bacterial Proteins chemistry, Oxidoreductases, O-Demethylating chemistry, Sphingomonadaceae chemistry, Tetrahydrofolates chemistry

Abstract

A tetrahydrofolate-dependent O-demethylase, LigM, from Sphingobium sp. SYK-6 was crystallized by the hanging-drop vapour-diffusion method. However, the obtained P3 1 21 or P3 2 21 crystals, which diffracted to 2.5-3.3 Å resolution, were hemihedrally twinned. To overcome the twinning problem, microseeding using P3 1 21/P3 2 21 crystals as microseeds was performed with optimization of the reservoir conditions. As a result, another crystal form was obtained. The newly obtained crystal diffracted to 2.5-3.0 Å resolution and belonged to space group P2 1 2 1 2, with unit-cell parameters a = 102.0, b = 117.3, c = 128.1 Å. The P2 1 2 1 2 crystals diffracted to better than 2.0 Å resolution after optimizing the cryoconditions. Phasing using the single anomalous diffraction method was successful at 3.0 Å resolution with a Pt-derivative crystal. This experience suggested that microseeding is an effective method to overcome the twinning problem, even when twinned crystals are utilized as microseeds.

Published

2016

35. Tetrahydrofolate increases suspension growth of dihydrofolate reductase-deficient chinese hamster ovary DG44 cells in chemically defined media.

Author

Kim BG and Park HW

Subjects

Animals, CHO Cells, Cell Proliferation drug effects, Cell Survival drug effects, Cells, Cultured, Cricetulus, Culture Media chemistry, Dose-Response Relationship, Drug, Structure-Activity Relationship, Tetrahydrofolate Dehydrogenase deficiency, Tetrahydrofolates chemistry, Culture Media pharmacology, Tetrahydrofolate Dehydrogenase metabolism, Tetrahydrofolates pharmacology

Abstract

Adaptation of dihydrofolate reductase (DHFR)-deficient Chinese hamster ovary (CHO) DG44 cells to chemically defined suspension culture conditions is a time-consuming and labor-intensive process because nonadapted DHFR-deficient CHO DG44 cells normally show poor growth in chemically defined medium (CDM). We examined the effects of folate derivatives, ribonucleotides, and nucleobases on the growth of suspension-adapted DHFR-deficient CHO DG44 cells in CDM. Among the tested additives, tetrahydrofolate (THF) was identified as an effective component for increasing cell growth. THF supplementation in the range of 0.2-359 μM enhanced cell growth in in-house CDM. Addition of 3.6 μM THF to in-house CDM resulted in a more than 2.5-fold increase in maximum viable cell density. Moreover, supplementation of six different commercial CDMs with 3.6 μM THF yielded up to 2.9-fold enhancement of maximum viable cell density. An anchorage- and serum-dependent DHFR-deficient CHO DG44 cell line was adapted within two consecutive passages to suspension growth in in-house CDM supplemented with 3.6 μM THF. These data indicate that supplementation of chemically defined cell culture media with greater than 0.2 μM THF can help achieve a high density of suspension-adapted DHFR-deficient CHO DG44 cells and may facilitate rapid adaptation of nonadapted DHFR-deficient CHO DG44 cells to suspension culture. © 2016 American Institute of Chemical Engineers Biotechnol. Prog., 32:1539-1546, 2016., (© 2016 American Institute of Chemical Engineers.)

Published

2016

36. Folate deficiency affects histone methylation.

Author

Garcia BA, Luka Z, Loukachevitch LV, Bhanu NV, and Wagner C

Subjects

Catalytic Domain, Epigenesis, Genetic, Escherichia coli metabolism, Folic Acid chemistry, Humans, Lysine chemistry, Mass Spectrometry, Models, Theoretical, Pilot Projects, Protein Processing, Post-Translational, Sarcosine Dehydrogenase chemistry, Tetrahydrofolates chemistry, DNA Methylation, Folic Acid Deficiency immunology, Histone Demethylases chemistry, Histones chemistry

Abstract

Formaldehyde is extremely toxic reacting with proteins to crosslinks peptide chains. Formaldehyde is a metabolic product in many enzymatic reactions and the question of how these enzymes are protected from the formaldehyde that is generated has largely remained unanswered. Early experiments from our laboratory showed that two liver mitochondrial enzymes, dimethylglycine dehydrogenase (DMGDH) and sarcosine dehydrogenase (SDH) catalyze oxidative demethylation reactions (sarcosine is a common name for monomethylglycine). The enzymatic products of these enzymes were the demethylated substrates and formaldehyde, produced from the removed methyl group. Both DMGDH and SDH contain FAD and both have tightly bound tetrahydrofolate (THF), a folate coenzyme. THF binds reversibly with formaldehyde to form 5,10-methylene-THF. At that time we showed that purified DMGDH, with tightly bound THF, reacted with formaldehyde generated during the reaction to form 5,10-methylene-THF. This effectively scavenged the formaldehyde to protect the enzyme. Recently, post-translational modifications on histone tails have been shown to be responsible for epigenetic regulation of gene expression. One of these modifications is methylation of lysine residues. The first enzyme discovered to accomplish demethylation of these modified histones was histone lysine demethylase (LSD1). LSD1 specifically removes methyl groups from di- and mono-methylated lysines at position 4 of histone 3. This enzyme contained tightly bound FAD and the products of the reaction were the demethylated lysine residue and formaldehyde. The mechanism of LSD1 demethylation is analogous to the mechanism previously postulated for DMGDH, i.e. oxidation of the N-methyl bond to the methylene imine followed by hydrolysis to generate formaldehyde. This suggested that THF might also be involved in the LSD1 reaction to scavenge the formaldehyde produced. Our hypotheses are that THF is bound to native LSD1 by analogy to DMGDH and SDH and that the bound THF serves to protect the FAD class of histone demethylases from the destructive effects of formaldehyde generation by formation of 5,10-methylene-THF. We present pilot data showing that decreased folate in livers as a result of dietary folate deficiency is associated with increased levels of methylated lysine 4 of histone 3. This can be a result of decreased LSD1 activity resulting from the decreased folate available to scavenge the formaldehyde produced at the active site caused by the folate deficiency. Because LSD1 can regulate gene expression this suggests that folate may play a more important role than simply serving as a carrier of one-carbon units and be a factor in other diseases associated with low folate., (Copyright © 2016 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2016

37. Structural Insights into Mycobacterium tuberculosis Rv2671 Protein as a Dihydrofolate Reductase Functional Analogue Contributing to para-Aminosalicylic Acid Resistance.

Author

Cheng YS and Sacchettini JC

Subjects

Aminosalicylic Acid pharmacology, Antitubercular Agents chemistry, Antitubercular Agents metabolism, Antitubercular Agents pharmacology, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins genetics, Bacterial Proteins metabolism, Catalytic Domain, Drug Resistance, Bacterial, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Folic Acid Antagonists chemistry, Folic Acid Antagonists metabolism, Folic Acid Antagonists pharmacology, Kinetics, Ligands, Molecular Conformation, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis growth & development, NADP metabolism, Nucleotide Deaminases antagonists & inhibitors, Nucleotide Deaminases genetics, Nucleotide Deaminases metabolism, Phylogeny, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Tetrahydrofolate Dehydrogenase genetics, Tetrahydrofolate Dehydrogenase metabolism, Tetrahydrofolates metabolism, Trimethoprim chemistry, Trimethoprim metabolism, Trimethoprim pharmacology, Trimetrexate chemistry, Trimetrexate metabolism, Trimetrexate pharmacology, Bacterial Proteins chemistry, Models, Molecular, Mycobacterium tuberculosis enzymology, NADP chemistry, Nucleotide Deaminases chemistry, Tetrahydrofolate Dehydrogenase chemistry, Tetrahydrofolates chemistry

Abstract

Mycobacterium tuberculosis (Mtb) Rv2671 is annotated as a 5-amino-6-ribitylamino-2,4(1H,3H)-pyrimidinedione 5'-phosphate (AROPP) reductase (RibD) in the riboflavin biosynthetic pathway. Recently, a strain of Mtb with a mutation in the 5' untranslated region of Rv2671, which resulted in its overexpression, was found to be resistant to dihydrofolate reductase (DHFR) inhibitors including the anti-Mtb drug para-aminosalicylic acid (PAS). In this study, a biochemical analysis of Rv2671 showed that it was able to catalyze the reduction of dihydrofolate (DHF) to tetrahydrofolate (THF), which explained why the overexpression of Rv2671 was sufficient to confer PAS resistance. We solved the structure of Rv2671 in complex with the NADP(+) and tetrahydrofolate (THF), which revealed the structural basis for the DHFR activity. The structures of Rv2671 complexed with two DHFR inhibitors, trimethoprim and trimetrexate, provided additional details of the substrate binding pocket and elucidated the differences between their inhibitory activities. Finally, Rv2671 was unable to catalyze the reduction of AROPP, which indicated that Rv2671 and its closely related orthologues are not involved in riboflavin biosynthesis.

Published

2016

38. Bacterial Thymidylate Synthase Binds Two Molecules of Substrate and Cofactor without Cooperativity.

Author

Sapienza PJ, Falk BT, and Lee AL

Subjects

Allosteric Regulation, Binding Sites, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Thermodynamics, Uridine Monophosphate analogs & derivatives, Uridine Monophosphate chemistry, Uridine Monophosphate metabolism, Coenzymes metabolism, Escherichia coli enzymology, Thymidylate Synthase chemistry, Thymidylate Synthase metabolism

Abstract

Thymidylate synthase (TSase) is a clinically important enzyme because it catalyzes synthesis of the sole de novo source of deoxy-thymidylate. Without this enzyme, cells die a "thymineless death" since they are starved of a crucial DNA synthesis precursor. As a drug target, TSase is well studied in terms of its structure and reaction mechanism. An interesting mechanistic feature of dimeric TSase is that it is "half-the-sites reactive", which is a form of negative cooperativity. Yet, the basis for this is not well-understood. Some experiments point to cooperativity at the binding steps of the reaction cycle as being responsible for the phenomenon, but the literature contains conflicting reports. Here we use ITC and NMR to resolve these inconsistencies. This first detailed thermodynamic dissection of multisite binding of dUMP to E. coli TSase shows the nucleotide binds to the free and singly bound forms of the enzyme with nearly equal affinity over a broad range of temperatures and in multiple buffers. While small but significant differences in ΔC°P for the two binding events show that the active sites are not formally equivalent, there is little-to-no allostery at the level of ΔG°bind. In addition NMR titration data reveal that there is minor intersubunit cooperativity in formation of a ternary complex with the mechanism based inhibitor, 5F-dUMP, and cofactor. Taken together, the data show that functional communication between subunits is minimal for both binding steps of the reaction coordinate.

Published

2015

39. Mathematical analysis of the regulation of competing methyltransferases.

Author

Reed MC, Gamble MV, Hall MN, and Nijhout HF

Subjects

Arsenic chemistry, Arsenic metabolism, Bangladesh, Folic Acid chemistry, Folic Acid metabolism, Folic Acid therapeutic use, Glycine N-Methyltransferase metabolism, Inactivation, Metabolic, Kinetics, Methyltransferases metabolism, Protein Binding, Substrate Specificity, Tetrahydrofolates metabolism, Glycine N-Methyltransferase chemistry, Metabolic Networks and Pathways, Methyltransferases chemistry, Models, Chemical, Tetrahydrofolates chemistry

Abstract

Background: Methyltransferase (MT) reactions, in which methyl groups are attached to substrates, are fundamental to many aspects of cell biology and human physiology. The universal methyl donor for these reactions is S-adenosylmethionine (SAM) and this presents the cell with an important regulatory problem. If the flux along one pathway is changed then the SAM concentration will change affecting all the other MT pathways, so it is difficult for the cell to regulate the pathways independently., Methods: We created a mathematical model, based on the known biochemistry of the folate and methionine cycles, to study the regulatory mechanisms that enable the cell to overcome this difficulty. Some of the primary mechanisms are long-range allosteric interactions by which substrates in one part of the biochemical network affect the activity of enzymes at distant locations in the network (not distant in the cell). Because of these long-range allosteric interactions, the dynamic behavior of the network is very complicated, and so mathematical modeling is a useful tool for investigating the effects of the regulatory mechanisms and understanding the complicated underlying biochemistry and cell biology., Results: We study the allosteric binding of 5-methyltetrahydrofolate (5 mTHF) to glycine-N-methyltransferase (GNMT) and explain why data in the literature implies that when one molecule binds, GNMT retains half its activity. Using the model, we quantify the effects of different regulatory mechanisms and show how cell processes would be different if the regulatory mechanisms were eliminated. In addition, we use the model to interpret and understand data from studies in the literature. Finally, we explain why a full understanding of how competing MTs are regulated is important for designing intervention strategies to improve human health., Conclusions: We give strong computational evidence that once bound GNMT retains half its activity. The long-range allosteric interactions enable the cell to regulate the MT reactions somewhat independently. The low K m values of many MTs also play a role because the reactions then run near saturation and changes in SAM have little effect. Finally, the inhibition of the MTs by the product S-adenosylhomocysteine also stabilizes reaction rates against changes in SAM.

Published

2015

40. Role of long-range protein dynamics in different thymidylate synthase catalyzed reactions.

Author

Abeysinghe T and Kohen A

Subjects

Catalysis, Deoxyuracil Nucleotides chemistry, Escherichia coli metabolism, Kinetics, Protons, Temperature, Tetrahydrofolates chemistry, Thermodynamics, Proteins chemistry, Thymidylate Synthase chemistry

Abstract

Recent studies of Escherichia coli thymidylate synthase (ecTSase) showed that a highly conserved residue, Y209, that is located 8 Å away from the reaction site, plays a key role in the protein's dynamics. Those crystallographic studies indicated that Y209W mutant is a structurally identical but dynamically altered relative to the wild type (WT) enzyme, and that its turnover catalytic rate governed by a slow hydride-transfer has been affected. The most challenging test of an examination of a fast chemical conversion that precedes the rate-limiting step has been achieved here. The physical nature of both fast and slow C-H bond activations have been compared between the WT and mutant by means of observed and intrinsic kinetic isotope effects (KIEs) and their temperature dependence. The findings indicate that the proton abstraction step has not been altered as much as the hydride transfer step. Additionally, the comparison indicated that other kinetic steps in the TSase catalyzed reaction were substantially affected, including the order of the substrate binding. Enigmatically, although Y209 is H-bonded to 3'-OH of 2'-deoxyuridine-5'-mono-phosphate (dUMP), its altered dynamics is more pronounced on the binding of the remote cofactor, (6R)-N5,N10-methylene-5,6,7,8-tetrahydrofolate (CH2H4folate), revealing the importance of long-range dynamics of the enzymatic complex and its catalytic function.

Published

2015

41. Stability of microencapsulated L-5-methyltetrahydrofolate in fortified noodles.

Author

Liu Y, Green TJ, and Kitts DD

Subjects

Biological Availability, Cooking, Folic Acid analysis, Folic Acid chemistry, Water chemistry, Ascorbic Acid chemistry, Drug Compounding, Flour analysis, Food Analysis methods, Tetrahydrofolates chemistry

Abstract

Here we report on the comparative stability of free and microencapsulated L-5-methyltetrahydrofolate (L-5-MTHF) with free folic acid (FA) when exposed to thermal cooking conditions that are common to noodle making. Fortifying noodle flour with free L-5-MTHF produced the greatest loss of the vitamin when noodles were cooked. In contrast, the percentage recovery of microencapsulated L-5-MTHF in both fresh and cooked noodles was not significantly different to noodles that were similarly processed with fortified FA. The addition of sodium ascorbate along with L-5-MTHF enabled a sustained stability of the folate after boiling, and also after frying. The dispersal of microencapsulated folate in flour showed better homogeneity compared to similar practices used with free form L-5-MTHF and FA, respectively. We conclude that microencapsulating L-5-MTHF along with sodium ascorbate is effective to produce a stable folate in fortified noodles, a staple food for Asian populations that may require improved dietary folate intake., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

42. Screening and in vitro testing of antifolate inhibitors of human cytosolic serine hydroxymethyltransferase.

Author

Paiardini A, Fiascarelli A, Rinaldo S, Daidone F, Giardina G, Koes DR, Parroni A, Montini G, Marani M, Paone A, McDermott LA, Contestabile R, and Cutruzzolà F

Subjects

Glycine Hydroxymethyltransferase metabolism, Humans, Methotrexate chemistry, Methotrexate pharmacology, Molecular Docking Simulation, Quinazolines chemistry, Quinazolines pharmacology, Tetrahydrofolates chemistry, Tetrahydrofolates pharmacology, Thiophenes chemistry, Thiophenes pharmacology, Folic Acid Antagonists chemistry, Folic Acid Antagonists pharmacology, Glycine Hydroxymethyltransferase antagonists & inhibitors

Abstract

Metabolic reprogramming of tumor cells toward serine catabolism is now recognized as a hallmark of cancer. Serine hydroxymethyltransferase (SHMT), the enzyme providing one-carbon units by converting serine and tetrahydrofolate (H4 PteGlu) to glycine and 5,10-CH2 -H4 PteGlu, therefore represents a target of interest in developing new chemotherapeutic drugs. In this study, 13 folate analogues under clinical evaluation or in therapeutic use were in silico screened against SHMT, ultimately identifying four antifolate agents worthy of closer evaluation. The interaction mode of SHMT with these four antifolate drugs (lometrexol, nolatrexed, raltitrexed, and methotrexate) was assessed. The mechanism of SHMT inhibition by the selected antifolate agents was investigated in vitro using the human cytosolic isozyme. The results of this study showed that lometrexol competitively inhibits SHMT with inhibition constant (Ki ) values in the low micromolar. The binding mode of lometrexol to SHMT was further investigated by molecular docking. These results thus provide insights into the mechanism of action of antifolate drugs and constitute the basis for the rational design of novel and more potent inhibitors of SHMT., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

43. The cobalamin-independent methionine synthase enzyme captured in a substrate-induced closed conformation.

Author

Ubhi DK and Robertus JD

Subjects

Amino Acid Substitution, Catalytic Domain, Methionine biosynthesis, Methyltransferases ultrastructure, Protein Binding, Substrate Specificity, Homocysteine chemistry, Methyltransferases chemistry, Tetrahydrofolates chemistry

Abstract

The cobalamin-independent methionine synthase enzyme catalyzes a challenging reaction: the direct transfer of a methyl from 5-methyl-tetrahydrofolate-glutamate3 to the l-homocysteine thiol. The enzyme has a dual (βα)8 TIM barrel structure that binds, activates and brings the reactants into reaction proximity by conformational movements. In the previously observed open structures, the substrates bind too far apart to react, but we have captured a ternary complex with both substrates bound in a closed form of the enzyme. The closing is described in terms of a hinge between the N- and C-terminal TIM barrels and a rearrangement of key loops within the C domain. The substrate specificity can now be rationalized and the structure reveals His707 as the acid that protonates the THF leaving group through a water molecule trapped in the closed active site. The substrates are correctly oriented for an in-line attack by l-homocysteine on the N(5)-methyl., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

44. High-level QM/MM calculations support the concerted mechanism for Michael addition and covalent complex formation in thymidylate synthase.

Author

Kaiyawet N, Lonsdale R, Rungrotmongkol T, Mulholland AJ, and Hannongbua S

Subjects

Molecular Structure, Tetrahydrofolates metabolism, Thymidine Monophosphate metabolism, Thymidylate Synthase metabolism, Quantum Theory, Tetrahydrofolates chemistry, Thymidine Monophosphate chemistry, Thymidylate Synthase chemistry

Abstract

Thymidylate synthase (TS) is a promising cancer target, due to its crucial function in thymine synthesis. It performs the reductive methylation of 2'-deoxyuridine-5'-phosphate (dUMP) to thymidine-5'-phosphate (dTMP), using N-5,10-methylene-5,6,7,8-tetrahydrofolate (mTHF) as a cofactor. After the formation of the dUMP/mTHF/TS noncovalent complex, and subsequent conformational activation, this complex has been proposed to react via nucleophilic attack (Michael addition) by Cys146, followed by methylene-bridge formation to generate the ternary covalent intermediate. Herein, QM/MM (B3LYP-D/6-31+G(d)-CHARMM27) methods are used to model the formation of the ternary covalent intermediate. A two-dimensional potential energy surface reveals that the methylene-bridged intermediate is formed via a concerted mechanism, as indicated by a single transition state on the minimum energy pathway and the absence of a stable enolate intermediate. A range of different QM methods (B3LYP, MP2 and SCS-MP2, and different basis sets) are tested for the calculation of the activation energy barrier for the formation of the methylene-bridged intermediate. We test convergence of the QM/MM results with respect to size of the QM region. Inclusion of Arg166, which interacts with the nucleophilic thiolate, in the QM region is important for reliable results; the MM model apparently does not reproduce energies for distortion of the guanidinium side chain correctly. The spin component scaled-Møller-Plessett perturbation theory (SCS-MP2) approach was shown to be in best agreement (within 1.1 kcal/mol) while the results obtained with MP2 and B3LYP also yielded acceptable values (deviating by less than 3 kcal/mol) compared with the barrier derived from experiment. Our results indicate that using a dispersion-corrected DFT method, or a QM method with an accurate treatment of electron correlation, increases the agreement between the calculated and experimental activation energy barriers, compared with the semiempirical AM1 method. These calculations provide important insight into the reaction mechanism of TS and may be useful in the design of new TS inhibitors.

Published

2015

45. Arg-265: a critical residue of L.donovani cytosolic SHMT in maintaining the binding of THF and catalysis.

Author

Gandhi S, Gaur N, Krishna S, Siddiqi MI, and Saxena JK

Subjects

Alanine chemistry, Alanine genetics, Amino Acid Sequence, Arginine chemistry, Arginine genetics, Cloning, Molecular, Cytosol enzymology, DNA, Protozoan chemistry, Escherichia coli genetics, Genetic Vectors, Glycine Hydroxymethyltransferase chemistry, Glycine Hydroxymethyltransferase genetics, Leishmania donovani enzymology, Molecular Sequence Data, Mutagenesis, Site-Directed, Plasmids, Protein Structure, Secondary, Spectrum Analysis, Tetrahydrofolates chemistry, Arginine physiology, Glycine Hydroxymethyltransferase metabolism, Leishmania donovani metabolism, Tetrahydrofolates metabolism

Abstract

Serine hydroxymethyltransferase belongs to the class of pyridoxal-5-phosphate enzymes along with aspartate aminotransferase. To explore the function of residue(s) involved in binding of the carboxylate group of Tetrahydrofolic acid (THF) to L. donovani cytosolic serine hydroxymethyltransferase (LdcSHMT), the gene was cloned in pET-28(a) vector, overexpressed and purified to homogeneity. With the help of docking results of THF to the active site of protein, the key residues involved in interaction were identified. In an attempt to unravel the function of Arg265 residue involved in binding of the carboxylate group of THF, Arg-265 was mutated to Ala by site-directed mutagenesis. The Arg265Ala-LdcSHMT showed increased Km value (threefold) and decreased kcat/Km value (threefold) for H₄-folate as compared with wild type enzyme. The wild and mutant enzymes exhibited similar Km and kcat/Km values for L-allo-threonine. Unlike the wild type enzyme, mutant failed to form characteristic quinonoid intermediate and was unable to carry out the exchange of α-proton from glycine in the presence of Tetrahydrofolate. These results suggested that Arg265 residue is required for the binding of Tetrahydrofolate and may be the base that abstracts α-proton from glycine, leading to formation of quinonoid intermediate in cytosolic SHMT of L. donovani., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2015

46. In vivo kinetics of formate metabolism in folate-deficient and folate-replete rats.

Author

Morrow GP, MacMillan L, Lamarre SG, Young SK, MacFarlane AJ, Brosnan ME, and Brosnan JT

Subjects

Animals, Choline chemistry, Dimethylglycine Dehydrogenase, Formaldehyde chemistry, Glycine chemistry, Histidine chemistry, Liver metabolism, Male, Methionine chemistry, Mitochondria, Liver metabolism, Oxygen chemistry, Rats, Rats, Sprague-Dawley, Sarcosine Dehydrogenase metabolism, Serine chemistry, Tetrahydrofolates chemistry, Folic Acid chemistry, Folic Acid Deficiency metabolism, Formates chemistry, Mitochondria metabolism

Abstract

It is now established that the mitochondrial production of formate is a major process in the endogenous generation of folate-linked one-carbon groups. We have developed an in vivo approach involving the constant infusion of [(13)C]formate until isotopic steady state is attained to measure the rate of endogenous formate production in rats fed on either a folate-replete or folate-deficient diet. Formate was produced at a rate of 76 μmol·h(-1)·100 g of body weight(-1) in the folate-replete rats, and this was decreased by 44% in folate-deficient rats. This decreased formate production was confirmed in isolated rat liver mitochondria where formate production from serine, the principal precursor of one-carbon groups, was decreased by 85%, although formate production from sarcosine and dimethylglycine (choline metabolites) was significantly increased. We attribute this unexpected result to the demonstrated production of formaldehyde by sarcosine dehydrogenase and dimethylglycine dehydrogenase from their respective substrates in the absence of tetrahydrofolate and subsequent formation of formate by formaldehyde dehydrogenase. Comparison of formate production with the ingestion of dietary formate precursors (serine, glycine, tryptophan, histidine, methionine, and choline) showed that ∼75% of these precursors were converted to formate, indicating that formate is a significant, although underappreciated end product of choline and amino acid oxidation. Ingestion of a high protein diet did not result in increased production of formate, suggesting a regulation of the conversion of these precursors at the mitochondrial level to formate., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

47. Structures of Plasmodium vivax serine hydroxymethyltransferase: implications for ligand-binding specificity and functional control.

Author

Chitnumsub P, Jaruwat A, Riangrungroj P, Ittarat W, Noytanom K, Oonanant W, Vanichthanankul J, Chuankhayan P, Maenpuen S, Chen CJ, Chaiyen P, Yuthavong Y, and Leartsakulpanich U

Subjects

Binding Sites, Humans, Ligands, Models, Molecular, Plasmodium vivax chemistry, Plasmodium vivax metabolism, Protein Binding, Serine chemistry, Serine metabolism, Tetrahydrofolates chemistry, Tetrahydrofolates metabolism, Glycine Hydroxymethyltransferase chemistry, Glycine Hydroxymethyltransferase metabolism, Malaria, Vivax parasitology, Plasmodium vivax enzymology

Abstract

Plasmodium parasites, the causative agent of malaria, rely heavily on de novo folate biosynthesis, and the enzymes in this pathway have therefore been explored extensively for antimalarial development. Serine hydroxymethyltransferase (SHMT) from Plasmodium spp., an enzyme involved in folate recycling and dTMP synthesis, has been shown to catalyze the conversion of L- and D-serine to glycine (Gly) in a THF-dependent reaction, the mechanism of which is not yet fully understood. Here, the crystal structures of P. vivax SHMT (PvSHMT) in a binary complex with L-serine and in a ternary complex with D-serine (D-Ser) and (6R)-5-formyltetrahydrofolate (5FTHF) provide clues to the mechanism underlying the control of enzyme activity. 5FTHF in the ternary-complex structure was found in the 6R form, thus differing from the previously reported structures of SHMT-Gly-(6S)-5FTHF from other organisms. This suggested that the presence of D-Ser in the active site can alter the folate-binding specificity. Investigation of binding in the presence of D-Ser and the (6R)- or (6S)-5FTHF enantiomers indicated that both forms of 5FTHF can bind to the enzyme but that only (6S)-5FTHF gives rise to a quinonoid intermediate. Likewise, a large surface area with a highly positively charged electrostatic potential surrounding the PvSHMT folate pocket suggested a preference for a polyglutamated folate substrate similar to the mammalian SHMTs. Furthermore, as in P. falciparum SHMT, a redox switch created from a cysteine pair (Cys125-Cys364) was observed. Overall, these results assert the importance of features such as stereoselectivity and redox status for control of the activity and specificity of PvSHMT.

Published

2014

48. The loss of 5-methyltetrahydrofolate in human serum under suboptimal preanalytical conditions can only partially be recovered by an oxidation product.

Author

Fazili Z, Sternberg MR, Paladugula N, Whitehead RD Jr, Chen H, and Pfeiffer CM

Subjects

Chromatography, High Pressure Liquid methods, Folic Acid blood, Folic Acid chemistry, Folic Acid metabolism, Humans, Limit of Detection, Oxidation-Reduction, Sensitivity and Specificity, Tandem Mass Spectrometry methods, Temperature, Tetrahydrofolates chemistry, Time Factors, Blood Specimen Collection standards, Tetrahydrofolates blood

Abstract

Background: Maintaining folate stability during sample handling is important, yet challenging., Objective: We investigated the effects of suboptimal preanalytical conditions on serum folate stability., Methods: By using an HPLC-tandem MS method we measured folates [5-methyltetrahydrofolate (5-methylTHF), folic acid, MeFox (5-methylTHF oxidation product, pyrazino-s-triazine derivative of 4α-hydroxy-5-methylTHF), and other minor folate forms at or below the limit of detection] in human serum exposed to suboptimal conditions., Results: Whole blood samples (n = 21) stored at 32°C for ≤ 3 d (Expt. 1: delayed processing) showed significant decreases in serum total folate (tFOL; sum of folate forms: 11-32%, 5.5-15.9 nmol/L) and 5-methylTHF (36-62%, 14.5-25.1 nmol/L) and a significant increase in MeFox (346-415%, 7.17-8.63 nmol/L). Serum samples (n = 21) stored at 11°C for 7-14 d (Expt. 2: delayed freezing) also showed significant decreases in tFOL (4.6-10.4%, 2.3-5.1 nmol/L) and 5-methylTHF (8.4-29%, 3.4-11.6 nmol/L) and significant increases in MeFox (88-320%, 1.82-6.62 nmol/L). The molar loss in 5-methylTHF exceeded the gain in MeFox in these 2 experiments. When we exposed 3 serum pools (tFOL: 16.7-58.3 nmol/L) for 24 h to an elevated temperature of 37°C (Expt. 3), the significant decrease in 5-methylTHF (33% on average) was compensated for by an equimolar gain in MeFox. Repeated freeze/thaw cycles (≤ 3 cycles) of serum [closed (Expt. 4) and open (Expt. 5) vials] showed generally stable folates with small (<1 nmol/L) changes. Long-term (≤ 12 mo) exposure of 3 serum pools (tFOL: 17.5-63.7 nmol/L) to a suboptimal (-20°C) freezing temperature (Expt. 6) showed significant decreases in tFOL (5% on average) already after 3 mo. The molar loss in 5-methylTHF exceeded the gain in MeFox. Folic acid generally showed good stability., Conclusions: To avoid folate losses, unprocessed whole blood should be protected from elevated temperatures and serum should not be refrigerated for >2 d or for a long term stored at -20°C., (© 2014 American Society for Nutrition.)

Published

2014

49. Excited state electronic structures of 5,10-methenyltetrahydrofolate and 5,10-methylenetetrahydrofolate determined by Stark spectroscopy.

Author

Pauszek RF 3rd, Kodali G, and Stanley RJ

Subjects

Models, Molecular, Molecular Conformation, Photolysis, Quantum Theory, Electrons, Spectrum Analysis, Tetrahydrofolates chemistry

Abstract

Folates are ubiquitous cofactors that participate in a wide variety of critical biological processes. 5,10-Methenyltetrahydrofolate and its photodegradation product 5,10-methylenetetrahydrofolate are both associated with the light-driven DNA repair protein DNA photolyase and its homologues (e.g., cryptochromes). The excited state electronic properties of these folate molecules have been studied here using Stark spectroscopy and complementary quantum calculations. The tetrahydrofolates have relatively large difference dipole moments (ca. 6-8 Debye) and difference polarizabilities (ca. 100 Å(3)). This extensive excited state charge redistribution appears to be due largely to the pendant p-aminobenzoic acid group, which helps shuttle charge over the entirety of the molecule. Simple calculations based on the experimental difference dipole moments suggest that tetrahydrofolates should have large two photon cross sections sufficient to enable two photon microscopy to selectively detect and follow folate-containing proteins both in vitro and in vivo.

Published

2014

50. Folate in demethylation: the crystal structure of the rat dimethylglycine dehydrogenase complexed with tetrahydrofolate.

Author

Luka Z, Pakhomova S, Loukachevitch LV, Newcomer ME, and Wagner C

Subjects

Amino Acid Sequence, Animals, Binding Sites, Catalytic Domain, Crystallization, Crystallography, X-Ray, Dimethylglycine Dehydrogenase metabolism, Humans, Kinetics, Mitochondrial Proteins metabolism, Models, Molecular, Molecular Sequence Data, Rats, Sarcosine analogs & derivatives, Tetrahydrofolates metabolism, Dimethylglycine Dehydrogenase chemistry, Mitochondrial Proteins chemistry, Tetrahydrofolates chemistry

Abstract

Dimethylglycine dehydrogenase (DMGDH) is a mammalian mitochondrial enzyme which plays an important role in the utilization of methyl groups derived from choline. DMGDH is a flavin containing enzyme which catalyzes the oxidative demethylation of dimethylglycine in vitro with the formation of sarcosine (N-methylglycine), hydrogen peroxide and formaldehyde. DMGDH binds tetrahydrofolate (THF) in vivo, which serves as an acceptor of formaldehyde and in the cell the product of the reaction is 5,10-methylenetetrahydrofolate instead of formaldehyde. To gain insight into the mechanism of the reaction we solved the crystal structures of the recombinant mature and precursor forms of rat DMGDH and DMGDH-THF complexes. Both forms of DMGDH reveal similar kinetic parameters and have the same tertiary structure fold with two domains formed by N- and C-terminal halves of the protein. The active center is located in the N-terminal domain while the THF binding site is located in the C-terminal domain about 40Å from the isoalloxazine ring of FAD. The folate binding site is connected with the enzyme active center via an intramolecular channel. This suggests the possible transfer of the intermediate imine of dimethylglycine from the active center to the bound THF where they could react producing a 5,10-methylenetetrahydrofolate. Based on the homology of the rat and human DMGDH the structural basis for the mechanism of inactivation of the human DMGDH by naturally occurring His109Arg mutation is proposed., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014