Your search keyword '"Agnes Rinaldo-Matthis"' showing total 40 results

1. Discovery of a small molecule that inhibits Bcl-3-mediated cyclin D1 expression in melanoma cells

Author

Karunakar Saamarthy, Kristofer Ahlqvist, Renée Daams, Navisraj Balagunaseelan, Agnes Rinaldo-Matthis, Julhash U. Kazi, Wondossen Sime, and Ramin Massoumi

Subjects

Melanoma, Bcl-3, Cyclin D1, Proliferation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Molecular targeted therapy using a drug that suppresses the growth and spread of cancer cells via inhibition of a specific protein is a foundation of precision medicine and treatment. High expression of the proto-oncogene Bcl-3 promotes the proliferation and metastasis of cancer cells originating from tissues such as the colon, prostate, breast, and skin. The development of novel drugs targeting Bcl-3 alone or in combination with other therapies can cure these patients or prolong their survival. As a proof of concept, in the present study, we focused on metastatic melanoma as a model system. High-throughput screening and in vitro experiments identified BCL3ANT as a lead molecule that could interfere with Bcl-3-mediated cyclin D1 expression and cell proliferation and migration in melanoma. In experimental animal models of melanoma, it was demonstrated that the use of a Bcl-3 inhibitor can influence the survival of melanoma cells. Since there are no other inhibitors against Bcl-3 in the clinical pipeline for cancer treatment, this presents a unique opportunity to develop a highly specific drug against malignant melanoma to meet an urgent clinical need.

Published

2024

2. Crystal structures of human MGST2 reveal synchronized conformational changes regulating catalysis

Author

Madhuranayaki Thulasingam, Laura Orellana, Emmanuel Nji, Shabbir Ahmad, Agnes Rinaldo-Matthis, and Jesper Z. Haeggström

Subjects

Science

Abstract

Microsomal glutathione S-transferase 2 (MGST2) produces leukotriene C4, an intracrine mediator of cell death. Structural, biochemical and computational analyses of human MGST2 suggest a mechanism employed by the enzyme to restrict catalysis to only one active site within the MGST2 trimer.

Published

2021

3. Structural and Functional Analysis of Calcium Ion Mediated Binding of 5-Lipoxygenase to Nanodiscs.

Author

Ramakrishnan B Kumar, Lin Zhu, Helena Idborg, Olof Rådmark, Per-Johan Jakobsson, Agnes Rinaldo-Matthis, Hans Hebert, and Caroline Jegerschöld

Subjects

Medicine, Science

Abstract

An important step in the production of inflammatory mediators of the leukotriene family is the Ca2+ mediated recruitment of 5 Lipoxygenase (5LO) to nuclear membranes. To study this reaction in vitro, the natural membrane mimicking environment of nanodiscs was used. Nanodiscs with 10.5 nm inner diameter were made with the lipid POPC and membrane scaffolding protein MSP1E3D1. Monomeric and dimeric 5LO were investigated. Monomeric 5LO mixed with Ca2+ and nanodiscs are shown to form stable complexes that 1) produce the expected leukotriene products from arachidonic acid and 2) can be, for the first time, visualised by native gel electrophoresis and negative stain transmission electron microscopy and 3) show a highest ratio of two 5LO per nanodisc. We interpret this as one 5LO on each side of the disc. The dimer of 5LO is visualised by negative stain transmission electron microscopy and is shown to not bind to nanodiscs. This study shows the advantages of nanodiscs to obtain basic structural information as well as functional information of a complex between a monotopic membrane protein and the membrane.

Published

2016

4. Structure and inhibition of mouse leukotriene C4 synthase.

Author

Damian Niegowski, Thea Kleinschmidt, Shabbir Ahmad, Abdul Aziz Qureshi, Michaela Mårback, Agnes Rinaldo-Matthis, and Jesper Z Haeggström

Subjects

Medicine, Science

Abstract

Leukotriene (LT) C4 synthase (LTC4S) is an integral membrane protein that catalyzes the conjugation reaction between the fatty acid LTA4 and GSH to form the pro-inflammatory LTC4, an important mediator of asthma. Mouse models of inflammatory disorders such as asthma are key to improve our understanding of pathogenesis and potential therapeutic targets. Here, we solved the crystal structure of mouse LTC4S in complex with GSH and a product analog, S-hexyl-GSH. Furthermore, we synthesized a nM inhibitor and compared its efficiency and binding mode against the purified mouse and human isoenzymes, along with the enzymes' steady-state kinetics. Although structural differences near the active site and along the C-terminal α-helix V suggest that the mouse and human LTC4S may function differently in vivo, our data indicate that mouse LTC4S will be a useful tool in future pharmacological research and drug development.

Published

2014

5. Investigation of calcium-dependent activity and conformational dynamics of zebra fish 12-lipoxygenase

Author

Monica Mittal, Navisraj Balagunaseelan, Craig E. Wheelock, Agnes Rinaldo-Matthis, Alexander Fauland, Olof Rådmark, Jesper Z. Haeggström, and Mahmudul Hasan

Subjects

Models, Molecular, 0301 basic medicine, Mutant, Biophysics, chemistry.chemical_element, Regulatory site, Calcium, Arachidonate 12-Lipoxygenase, Biochemistry, 03 medical and health sciences, Lipoxygenase, Protein structure, Animals, Humans, Amino Acid Sequence, Molecular Biology, Zebrafish, chemistry.chemical_classification, Binding Sites, Sequence Homology, Amino Acid, integumentary system, biology, Chemistry, Mutagenesis, food and beverages, Protein Structure, Tertiary, Amino acid, 030104 developmental biology, Enzyme, biology.protein, lipids (amino acids, peptides, and proteins)

Abstract

Background A 12-lipoxygenase in zebra fish (zf12-LOX) was found to be required for normal embryonic development and LOXs are of great interest for targeted drug designing. In this study, we investigate the structural-functional aspects of zf12-LOX in response to calcium. Methods A soluble version of zf12-LOX was created by mutagenesis. Based on multiple sequence alignment, we mutated the putative calcium-responsive amino acids in N-PLAT domain of soluble zf12-LOX. Using a series of biophysical methods, we ascertained the oligomeric state, stability, structural integrity and conformational changes of zf12-LOX in response to calcium. We also compared the biophysical properties of soluble zf12-LOX with the mutant in the absence and presence of calcium. Results Here we provide a detailed characterization of soluble zf12-LOX and the mutant. Both proteins exist as compact monomers in solution, however the enzyme activity of soluble zf12-LOX is significantly increased in presence of calcium. We find that the stimulatory effect of calcium on zf12-LOX is related to a change in protein structure as observed by SAXS, adopting an open-state. In contrast, enzyme with a mutated calcium regulatory site has reduced activity-response to calcium and restricted large re-modeling, suggesting that it retains a closed-state in response to calcium. Taken together, our study suggests that Ca2 +-dependent regulation is associated with different domain conformation(s) that might change the accessibility to substrate-binding site in response to calcium. General significance The study can be broadly implicated in better understanding the mode(s) of action of LOXs, and the enzymes regulated by calcium in general.

Published

2017

6. Trimeric microsomal glutathione transferase 2 displays one third of the sites reactivity

Author

Ralf Morgenstern, Shabbir Ahmad, Isolde Palombo, Agnes Rinaldo-Matthis, Madhuranayaki Thulasingam, Kenneth A. Johnson, Daniel O. Daley, and Jesper Z. Haeggström

Subjects

Molecular Sequence Data, Biophysics, Gene Expression, Calorimetry, Molecular Dynamics Simulation, Biochemistry, Pichia, Analytical Chemistry, chemistry.chemical_compound, Catalytic Domain, Microsomes, Gene expression, Dinitrochlorobenzene, Humans, Amino Acid Sequence, Molecular Biology, Polyacrylamide gel electrophoresis, Peptide sequence, Integral membrane protein, Glutathione Transferase, chemistry.chemical_classification, Sequence Homology, Amino Acid, Glutathione, Recombinant Proteins, Amino acid, Kinetics, chemistry, Eicosanoid, Microsome, Electrophoresis, Polyacrylamide Gel, Protein Multimerization, Sequence Alignment

Abstract

Human microsomal glutathione transferase 2 (MGST2) is a trimeric integral membrane protein that belongs to the membrane-associated proteins in eicosanoid and glutathione metabolism (MAPEG) family. The mammalian MAPEG family consists of six members where four have been structurally determined. MGST2 activates glutathione to form a thiolate that is crucial for GSH peroxidase activity and GSH conjugation reactions with electrophilic substrates, such as 1-chloro-2,4-dinitrobenzene (CDNB). Several studies have shown that MGST2 is able to catalyze a GSH conjugation reaction with the epoxide LTA4 forming the pro-inflammatory LTC4. Unlike its closest homologue leukotriene C4 synthase (LTC4S), MGST2 appears to activate its substrate GSH using only one of the three potential active sites [Ahmad S, et al. (2013) Biochemistry. 52, 1755-1764]. In order to demonstrate and detail the mechanism of one-third of the sites reactivity of MGST2, we have determined the enzyme oligomeric state, by Blue native PAGE and Differential Scanning Calorimetry, as well as the stoichiometry of substrate and substrate analog inhibitor binding to MGST2, using equilibrium dialysis and Isothermal Titration Calorimetry, respectively. Global simulations were used to fit kinetic data to determine the catalytic mechanism of MGST2 with GSH and CDNB (1-chloro-2,4-dinitrobenzene) as substrates. The best fit was observed with 1/3 of the sites catalysis as compared with a simulation where all three sites were active. In contrast to LTC4S, MGST2 displays a 1/3 the sites reactivity, a mechanism shared with the more distant family member MGST1 and recently suggested also for microsomal prostaglandin E synthase-1.

Published

2015

7. Binding of Pro-Gly-Pro at the active site of leukotriene A 4 hydrolase/aminopeptidase and development of an epoxide hydrolase selective inhibitor

Author

Jesper Z. Haeggström, Roman A. Zubarev, Alena Stsiapanava, Min Wan, Dorothea Rutishauser, Agnes Rinaldo-Matthis, Ulrika Olsson, Thea K. Kleinschmidt, and Bengt Samuelsson

Subjects

Models, Molecular, animal structures, Proline, Protein Conformation, Stereochemistry, Leukotriene B4, Tripeptide, Aminopeptidase, Leukotriene-A4 hydrolase, chemistry.chemical_compound, X-Ray Diffraction, Tandem Mass Spectrometry, Catalytic Domain, Hydrolase, Escherichia coli, Humans, Epoxide hydrolase, Chromatography, High Pressure Liquid, Epoxide Hydrolases, Inflammation, Multidisciplinary, integumentary system, biology, Chemistry, Active site, Substrate (chemistry), Biological Sciences, Thiazoles, Biochemistry, biology.protein, Crystallization, Oligopeptides

Abstract

Leukotriene (LT) A4 hydrolase/aminopeptidase (LTA4H) is a bifunctional zinc metalloenzyme that catalyzes the committed step in the formation of the proinflammatory mediator LTB4. Recently, the chemotactic tripeptide Pro-Gly-Pro was identified as an endogenous aminopeptidase substrate for LTA4 hydrolase. Here, we determined the crystal structure of LTA4 hydrolase in complex with a Pro-Gly-Pro analog at 1.72 Å. From the structure, which includes the catalytic water, and mass spectrometric analysis of enzymatic hydrolysis products of Pro-Gly-Pro, it could be inferred that LTA4 hydrolase cleaves at the N terminus of the palindromic tripeptide. Furthermore, we designed a small molecule, 4-(4-benzylphenyl)thiazol-2-amine, denoted ARM1, that inhibits LTB4 synthesis in human neutrophils (IC50 of ∼0.5 μM) and conversion of LTA4 into LTB4 by purified LTA4H with a Ki of 2.3 μM. In contrast, 50- to 100-fold higher concentrations of ARM1 did not significantly affect hydrolysis of Pro-Gly-Pro. A 1.62-Å crystal structure of LTA4 hydrolase in a dual complex with ARM1 and the Pro-Gly-Pro analog revealed that ARM1 binds in the hydrophobic pocket that accommodates the ω-end of LTA4, distant from the aminopeptidase active site, thus providing a molecular basis for its inhibitory profile. Hence, ARM1 selectively blocks conversion of LTA4 into LTB4, although sparing the enzyme’s anti-inflammatory aminopeptidase activity (i.e., degradation and inactivation of Pro-Gly-Pro). ARM1 represents a new class of LTA4 hydrolase inhibitor that holds promise for improved anti-inflammatory properties.

Published

2014

8. Crystal Structures of Leukotriene C4 Synthase in Complex with Product Analogs

Author

Jesper Z. Haeggström, Thea Kleinschmidt, Ulrika Olsson, Agnes Rinaldo-Matthis, Shabbir Ahmad, and Damian Niegowski

Subjects

chemistry.chemical_classification, 0303 health sciences, Leukotriene, Leukotriene C4, biology, Stereochemistry, Leukotriene A4, Wild type, Active site, Cell Biology, Tripeptide, Lyase, Biochemistry, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Enzyme, chemistry, biology.protein, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Leukotriene (LT) C4 synthase (LTC4S) catalyzes the conjugation of the fatty acid LTA4 with the tripeptide GSH to produce LTC4, the parent compound of the cysteinyl leukotrienes, important mediators of asthma. Here we mutated Trp-116 in human LTC4S, a residue proposed to play a key role in substrate binding, into an Ala or Phe. Biochemical and structural characterization of these mutants along with crystal structures of the wild type and mutated enzymes in complex with three product analogs, viz. S-hexyl-, 4-phenyl-butyl-, and 2-hydroxy-4-phenyl-butyl-glutathione, provide new insights to binding of substrates and product, identify a new conformation of the GSH moiety at the active site, and suggest a route for product release, aided by Trp-116.

Published

2014

9. Product formation controlled by substrate dynamics in leukotriene A4 hydrolase

Author

Ramakrishnan B. Kumar, Mahmudul Hasan, Jesper Z. Haeggström, Fredrik Tholander, Damian Niegowski, Alena Stsiapanava, Abdul Aziz Qureshi, Marjolein M. G. M. Thunnissen, and Agnes Rinaldo-Matthis

Subjects

Models, Molecular, Stereochemistry, Molecular Sequence Data, Biophysics, Phenylalanine, Xenopus Proteins, Crystallography, X-Ray, Leukotriene B4, Biochemistry, Aminopeptidase, Substrate Specificity, Analytical Chemistry, Leukotriene-A4 hydrolase, Xenopus laevis, Catalytic Domain, Hydroxyeicosatetraenoic Acids, Animals, Humans, Amino Acid Sequence, Tyrosine, Epoxide hydrolase, Molecular Biology, Epoxide Hydrolases, chemistry.chemical_classification, Sequence Homology, Amino Acid, biology, Chemistry, Hydrolysis, Active site, Substrate (chemistry), Amino acid, Kinetics, biology.protein, Protein Multimerization

Abstract

Leukotriene A4 hydrolase/aminopeptidase (LTA4H) (EC 3.3.2.6) is a bifunctional zinc metalloenzyme with both an epoxide hydrolase and an aminopeptidase activity. LTA4H from the African claw toad, Xenopus laevis (xlLTA4H) has been shown to, unlike the human enzyme, convert LTA4 to two enzymatic metabolites, LTB4 and another biologically active product Δ(6)-trans-Δ(8)-cis-LTB4 (5(S),12R-dihydroxy-6,10-trans-8,14-cis-eicosatetraenoic acid). In order to study the molecular aspect of the formation of this product we have characterized the structure and function of xlLTA4H. We solved the structure of xlLTA4H to a resolution of 2.3Å. It is a dimeric structure where each monomer has three domains with the active site in between the domains, similar as to the human structure. An important difference between the human and amphibian enzyme is the phenylalanine to tyrosine exchange at position 375. Our studies show that mutating F375 in xlLTA4H to tyrosine abolishes the formation of the LTB4 isomeric product Δ(6)-trans-Δ(8)-cis-LTB4. In an attempt to understand how one amino acid exchange leads to a new product profile as seen in the xlLTA4H, we performed a conformer analysis of the triene part of the substrate LTA4. Our results show that the Boltzmann distribution of substrate conformers correlates with the observed distribution of products. We suggest that the observed difference in product profile between the human and the xlLTA4H arises from different level of discrimination between substrate LTA4 conformers.

Published

2014

10. Catalytic Characterization of Human Microsomal Glutathione S-Transferase 2: Identification of Rate-Limiting Steps

Author

Damian Niegowski, Jesper Z. Haeggström, Shabbir Ahmad, Agnes Rinaldo-Matthis, Ralf Morgenstern, and Anders Wetterholm

Subjects

chemistry.chemical_classification, biology, Chemistry, Stereochemistry, Kinetics, Substrate (chemistry), Glutathione, Biochemistry, Catalysis, Leukotriene C4, Substrate Specificity, chemistry.chemical_compound, Burst kinetics, Enzyme, Biosynthesis, Catalytic Domain, biology.protein, Humans, Sulfhydryl Compounds, Protons, Glutathione Transferase, Peroxidase

Abstract

Microsomal glutathione S-transferase 2 (MGST2) is a 17 kDa trimeric integral membrane protein homologous to leukotriene C4 synthase (LTC4S). MGST2 has been suggested to catalyze the biosynthesis of the pro-inflammatory mediator leukotriene C4 (LTC4) in cells devoid of LTC4S. A detailed biochemical study of MGST2 is critical for the understanding of its cellular function and potential role as an LTC4-producing enzyme. Here we have characterized the substrate specificity and catalytic properties of purified MGST2 by steady-state and pre-steady-state kinetic experiments. In comparison with LTC4S, which has a catalytic efficiency of 8.7 × 10(5) M(-1) s(-1), MGST2, with a catalytic efficiency of 1.8 × 10(4) M(-1) s(-1), is considerably less efficient in producing LTC4. However, the two enzymes display a similar KM(LTA4) of 30-40 μM. While LTC4S has one activated glutathione (GSH) (forming a thiolate) per enzyme monomer, the MGST2 trimer seems to display only third-of-the-sites reactivity for thiolate activation, which in part would explain its lower catalytic efficiency. Furthermore, MGST2 displays GSH-dependent peroxidase activity of ∼0.2 μmol min(-1) mg(-1) toward several lipid hydroperoxides. MGST2, but not LTC4S, is efficient in catalyzing conjugation of the electrophilic substrate 1-chloro-2,4-dinitrobenzene (CDNB) and the lipid peroxidation product 4-hydroxy-2-nonenal with GSH. Using stopped-flow pre-steady-state kinetics, we have characterized the full catalytic reaction of MGST2 with CDNB and GSH as substrates, showing an initial rapid equilibrium binding of GSH followed by thiolate formation. Burst kinetics for the CDNB-GSH conjugation step was observed only at low GSH concentrations (thiolate anion formation becoming rate-limiting under these conditions). Product release is rapid and does not limit the overall reaction. Therefore, in general, the chemical conjugation step is rate-limiting for MGST2 at physiological GSH concentrations. MGST2 and LTC4S exhibit distinct catalytic and mechanistic properties, reflecting adaptation to broad and specific physiological functions, respectively.

Published

2013

11. Catalytic Conversion of Lipophilic Substrates by Phase constrained Enzymes in the Aqueous or in the Membrane Phase

Author

Jerker Widengren, Madhuranayaki Thulasingam, Bengt Mannervik, Hiroshi Abe, Ralf Morgenstern, Marcus Cebula, Joseph Brock, Birgitta Sjödin, Agnes Rinaldo-Matthis, Ilke Simsek Turan, Engin U. Akkaya, Jesper Z. Haeggström, and Volodymyr Chmyrov

Subjects

0301 basic medicine, Boron Compounds, Models, Molecular, Octoxynol, Article, Catalysis, Substrate Specificity, Xenobiotics, 03 medical and health sciences, Cytosol, Phase (matter), Microsomes, Animals, Humans, Glucuronosyltransferase, Fluorescent Dyes, Glutathione Transferase, chemistry.chemical_classification, Epoxide Hydrolases, Membranes, Multidisciplinary, 030102 biochemistry & molecular biology, Chemistry, Substrate (chemistry), Enzymes, Immobilized, Combinatorial chemistry, Kinetics, 030104 developmental biology, Membrane, Enzyme, Eukaryotic Cells, Biocatalysis, Enzyme mechanisms, Inactivation, Metabolic, Sulfotransferases, Hydrophobic and Hydrophilic Interactions, Chemical modification

Abstract

Both soluble and membrane-bound enzymes can catalyze the conversion of lipophilic substrates. The precise substrate access path, with regard to phase, has however, until now relied on conjecture from enzyme structural data only (certainly giving credible and valuable hypotheses). Alternative methods have been missing. To obtain the first experimental evidence directly determining the access paths (of lipophilic substrates) to phase constrained enzymes we here describe the application of a BODIPY-derived substrate (PS1). Using this tool, which is not accessible to cytosolic enzymes in the presence of detergent and, by contrast, not accessible to membrane embedded enzymes in the absence of detergent, we demonstrate that cytosolic and microsomal glutathione transferases (GSTs), both catalyzing the activation of PS1, do so only within their respective phases. This approach can serve as a guideline to experimentally validate substrate access paths, a fundamental property of phase restricted enzymes. Examples of other enzyme classes with members in both phases are xenobiotic-metabolizing sulphotransferases/UDP-glucuronosyl transferases or epoxide hydrolases. Since specific GSTs have been suggested to contribute to tumor drug resistance, PS1 can also be utilized as a tool to discriminate between phase constrained members of these enzymes by analyzing samples in the absence and presence of Triton X-100.

Published

2016

12. Phosphorylation of Leukotriene C4 Synthase at Serine 36 Impairs Catalytic Activity*

Author

Fredrik Tholander, Madhuranayaki Thulasingam, Anders Wetterholm, Roman A. Zubarev, A. Jimmy Ytterberg, Tomas Bergman, Jesper Z. Haeggström, Agnes Rinaldo-Matthis, and Shabbir Ahmad

Subjects

0301 basic medicine, Protein subunit, Mutation, Missense, Biochemistry, Catalysis, Protein Structure, Secondary, 03 medical and health sciences, chemistry.chemical_compound, Mice, Serine, Animals, Humans, Phosphorylation, Molecular Biology, Glutathione Transferase, Leukotriene, Binding Sites, biology, ATP synthase, Leukotriene C4, Active site, Ribosomal Protein S6 Kinases, 70-kDa, Cell Biology, Lyase, Leukotriene A4, Enzyme assay, 030104 developmental biology, chemistry, Amino Acid Substitution, biology.protein, Enzymology

Abstract

Leukotriene C4 synthase (LTC4S) catalyzes the formation of the proinflammatory lipid mediator leukotriene C4 (LTC4). LTC4 is the parent molecule of the cysteinyl leukotrienes, which are recognized for their pathogenic role in asthma and allergic diseases. Cellular LTC4S activity is suppressed by PKC-mediated phosphorylation, and recently a downstream p70S6k was shown to play an important role in this process. Here, we identified Ser(36) as the major p70S6k phosphorylation site, along with a low frequency site at Thr(40), using an in vitro phosphorylation assay combined with mass spectrometry. The functional consequences of p70S6k phosphorylation were tested with the phosphomimetic mutant S36E, which displayed only about 20% (20 μmol/min/mg) of the activity of WT enzyme (95 μmol/min/mg), whereas the enzyme activity of T40E was not significantly affected. The enzyme activity of S36E increased linearly with increasing LTA4 concentrations during the steady-state kinetics analysis, indicating poor lipid substrate binding. The Ser(36) is located in a loop region close to the entrance of the proposed substrate binding pocket. Comparative molecular dynamics indicated that Ser(36) upon phosphorylation will pull the first luminal loop of LTC4S toward the neighboring subunit of the functional homotrimer, thereby forming hydrogen bonds with Arg(104) in the adjacent subunit. Because Arg(104) is a key catalytic residue responsible for stabilization of the glutathione thiolate anion, this phosphorylation-induced interaction leads to a reduction of the catalytic activity. In addition, the positional shift of the loop and its interaction with the neighboring subunit affect active site access. Thus, our mutational and kinetic data, together with molecular simulations, suggest that phosphorylation of Ser(36) inhibits the catalytic function of LTC4S by interference with the catalytic machinery.

Published

2016

13. Kinetic investigation of human 5-lipoxygenase with arachidonic acid

Author

Ramakrishnan B. Kumar, Monica Mittal, Caroline Jegerschöld, Agnes Rinaldo-Matthis, Navisraj Balagunaseelan, Olof Rådmark, Mats Hamberg, and Jesper Z. Haeggström

Subjects

0301 basic medicine, Reaction mechanism, Stereochemistry, Clinical Biochemistry, Kinetics, Pharmaceutical Science, 010402 general chemistry, 01 natural sciences, Biochemistry, 03 medical and health sciences, Structure-Activity Relationship, Drug Discovery, Kinetic isotope effect, Humans, Enzyme kinetics, Lipoxygenase Inhibitors, Molecular Biology, Arachidonate 5-Lipoxygenase, Arachidonic Acid, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Organic Chemistry, Substrate (chemistry), Active site, Regioselectivity, Rate-determining step, 0104 chemical sciences, enzymes and coenzymes (carbohydrates), 030104 developmental biology, biology.protein, Molecular Medicine, lipids (amino acids, peptides, and proteins)

Abstract

Human 5-lipoxygenase (5-LOX) is responsible for the formation of leukotriene (LT)A4, a pivotal intermediate in the biosynthesis of the leukotrienes, a family of proinflammatory lipid mediators. 5-LOX has thus gained attention as a potential drug target. However, details of the kinetic mechanism of 5-LOX are still obscure. In this Letter, we investigated the kinetic isotope effect (KIE) of 5-LOX with its physiological substrate, arachidonic acid (AA). The observed KIE is 20±4 on kcat and 17±2 on kcat/KM at 25°C indicating a non-classical reaction mechanism. The observed rates show slight temperature dependence at ambient temperatures ranging from 4 to 35°C. Also, we observed low Arrhenius prefactor ratio (AH/AD=0.21) and a small change in activation energy (Ea(D)-Ea(H)=3.6J/mol) which suggests that 5-LOX catalysis involves tunneling as a mechanism of H-transfer. The measured KIE for 5-LOX involves a change in regioselectivity in response to deuteration at position C7, resulting in H-abstraction form C10 and formation of 8-HETE. The viscosity experiments influence the (H)kcat, but not (D)kcat. However the overall kcat/KM is not affected for labeled or unlabeled AA, suggesting that either the product release or conformational rearrangement might be involved in dictating kinetics of 5-LOX at saturating conditions. Investigation of available crystal structures suggests the role of active site residues (F421, Q363 and L368) in regulating the donor-acceptor distances, thus affecting H-transfer as well as regiospecificity. In summary, our study shows that that the H-abstraction is the rate limiting step for 5-LOX and that the observed KIE of 5-LOX is masked by a change in regioselectivity.

Published

2016

14. Arginine 104 Is a Key Catalytic Residue in Leukotriene C4 Synthase

Author

Jesper Z. Haeggström, Agnes Rinaldo-Matthis, Ralf Morgenstern, Eva Ohlson, Daniel Martinez Molina, Damian Niegowski, Pär Nordlund, Johanna B. Holm, and Anders Wetterholm

Subjects

Enzyme Mutation, Arginine, Stereochemistry, Mutation, Missense, Enzyme Mechanisms, Crystallography, X-Ray, Biochemistry, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Catalytic Domain, Humans, Enzyme kinetics, Molecular Biology, Glutathione Transferase, 030304 developmental biology, 0303 health sciences, Leukotriene, Leukotriene C4, ATP synthase, biology, 030302 biochemistry & molecular biology, Thiolate Anion, Active site, Cell Biology, Glutathione, Lyase, Asthma, Amino Acid Substitution, chemistry, Mutagenesis, Site-Directed, Enzymology, Crystal Structure, biology.protein, Spectrophotometry, Ultraviolet, Oxidation-Reduction, Glutathione S-Transferase

Abstract

Human leukotriene C(4) synthase (hLTC(4)S) is an integral membrane enzyme that conjugates leukotriene (LT) A(4) with glutathione to form LTC(4), a precursor to the cysteinyl leukotrienes (LTC(4), LTD(4), and LTE(4)) that are involved in the pathogenesis of human bronchial asthma. From the crystal structure of hLTC(4)S, Arg-104 and Arg-31 have been implicated in the conjugation reaction. Here, we used site-directed mutagenesis, UV spectroscopy, and x-ray crystallography to examine the catalytic role of Arg-104 and Arg-31. Exchange of Arg-104 with Ala, Ser, Thr, or Lys abolished 94.3-99.9% of the specific activity against LTA(4). Steady-state kinetics of R104A and R104S revealed that the K(m) for GSH was not significantly affected. UV difference spectra of the binary enzyme-GSH complex indicated that GSH ionization depends on the presence of Arg-104 because no thiolate signal, with λ(max) at 239 nm, could be detected using R104A or R104S hLTC(4)S. Apparently, the interaction of Arg-104 with the thiol group of GSH reduces its pK(a) to allow formation of a thiolate anion and subsequent nucleophilic attack at C6 of LTA(4). On the other hand, exchange of Arg-31 with Ala or Glu reduced the catalytic activity of hLTC(4)S by 88 and 70%, respectively, without significantly affecting the k(cat)/K(m) values for GSH, and a crystal structure of R31Q hLTC(4)S (2.1 Å) revealed a Gln-31 side chain pointing away from the active site. We conclude that Arg-104 plays a critical role in the catalytic mechanism of hLTC(4)S, whereas a functional role of Arg-31 seems more elusive. Because Arg-104 is a conserved residue, our results pertain to other homologous membrane proteins and represent a structure-function paradigm probably common to all microsomal GSH transferases.

Published

2010

15. Structures and mechanisms of enzymes in the leukotriene cascade

Author

Jesper Z. Haeggström and Agnes Rinaldo-Matthis

Subjects

Models, Molecular, Leukotrienes, Protein Conformation, Biochemistry, Proinflammatory cytokine, Leukotriene-A4 hydrolase, 03 medical and health sciences, 0302 clinical medicine, Phospholipase A2, medicine, Animals, Humans, Glutathione Transferase, 030304 developmental biology, Epoxide Hydrolases, 0303 health sciences, Leukotriene, Arachidonate 5-Lipoxygenase, Arachidonic Acid, biology, Chemotaxis, General Medicine, Lipid signaling, 3. Good health, 030220 oncology & carcinogenesis, Arachidonate 5-lipoxygenase, biology.protein, Bronchoconstriction, Inflammation Mediators, medicine.symptom, Signal Transduction

Abstract

Leukotrienes are a family of proinflammatory lipid mediators of the innate immune response and are important signaling molecules in inflammatory and allergic conditions. The leukotrienes are formed from arachidonic acid, which is released from membranes by cPLA(2), and further converted by 5-lipoxygenase to form the labile epoxide leukotriene (LT) A(4). This intermediate is converted by either of the two enzymes, LTA(4) hydrolase or LTC(4) synthase, to form LTB(4) or LTC(4), respectively. In order for 5-lipoxygenase to work efficiently in cells, five-lipoxygenase-activating protein needs to be present. LTB(4) is one of the most powerful chemotactic agents whereas LTC(4) induces smooth muscle contractions, for example in the airways causing bronchoconstriction in asthmatic patients. The leukotrienes and the five enzymes/proteins involved in their formation have been subject to intense studies including drug design programs. Compounds blocking the formation or action of leukotrienes are potentially beneficial in treatment of several acute and chronic inflammatory diseases of the cardiovascular and respiratory systems. In order to succeed with drug development studies, knowledge of the molecular characteristics of the targets is indispensable. This chapter reviews the biochemistry, catalytic, and structural properties of the enzymes in the leukotriene cascade.

Published

2010

16. Advances in eicosanoid research novel therapeutic implications?

Author

Anders Wetterholm, Jesper Z. Haeggström, Agnes Rinaldo-Matthis, and Craig E. Wheelock

Subjects

Leukotrienes, Biomedical Research, 5-Lipoxygenase-Activating Proteins, Biophysics, Cellular homeostasis, Inflammation, Leukotriene metabolism, Biology, Pharmacology, Biochemistry, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Cytosol, 0302 clinical medicine, Eicosanoic Acids, medicine, Humans, Cyclooxygenase Inhibitors, Molecular Biology, 030304 developmental biology, Receptors, Leukotriene, 0303 health sciences, Leukotriene, Arachidonate 5-Lipoxygenase, Group IV Phospholipases A2, Membrane Proteins, Cell Biology, Lipid signaling, 3. Good health, Eicosanoid, chemistry, Thromboxanes, Drug Design, 030220 oncology & carcinogenesis, Leukotriene Antagonists, lipids (amino acids, peptides, and proteins), Arachidonic acid, medicine.symptom, Carrier Proteins, Neuroscience

Abstract

Eicosanoids are a family of oxygenated metabolites of arachidonic acid, including the prostaglandins, thromboxanes, leukotrienes and lipoxins. These lipid mediators play essential roles in normal cellular homeostasis as well as in a number of disease states. This review will focus on recent advances in the field of eicosanoids and highlight specific discoveries and achievements. Emphasis will be placed on structure and receptor biology, which are of significant pharmacological and clinical relevance.

Published

2010

17. A dynamic Asp-Arg interaction is essential for catalysis in microsomal prostaglandin E2 synthase

Author

Bengt Samuelsson, Joseph Brock, Michael C. Goodman, Navisraj Balagunaseelan, Agnes Rinaldo-Matthis, Emilia Strandback, Mats Hamberg, Jesper Z. Haeggström, and Ralf Morgenstern

Subjects

0301 basic medicine, Stereochemistry, Protein Conformation, 010402 general chemistry, Crystallography, X-Ray, Ligands, 01 natural sciences, Cofactor, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Catalytic Domain, Microsomes, medicine, Prostaglandin E2, Prostaglandin-E Synthases, chemistry.chemical_classification, Multidisciplinary, ATP synthase, biology, Mutagenesis, Glutathione, Lipid signaling, Dipeptides, Biological Sciences, Ligand (biochemistry), 0104 chemical sciences, Intramolecular Oxidoreductases, 030104 developmental biology, Enzyme, chemistry, biology.protein, Mutagenesis, Site-Directed, lipids (amino acids, peptides, and proteins), medicine.drug

Abstract

Microsomal prostaglandin E2 synthase type 1 (mPGES-1) is responsible for the formation of the potent lipid mediator prostaglandin E2 under proinflammatory conditions, and this enzyme has received considerable attention as a drug target. Recently, a high-resolution crystal structure of human mPGES-1 was presented, with Ser-127 being proposed as the hydrogen-bond donor stabilizing thiolate anion formation within the cofactor, glutathione (GSH). We have combined site-directed mutagenesis and activity assays with a structural dynamics analysis to probe the functional roles of such putative catalytic residues. We found that Ser-127 is not required for activity, whereas an interaction between Arg-126 and Asp-49 is essential for catalysis. We postulate that both residues, in addition to a crystallographic water, serve critical roles within the enzymatic mechanism. After characterizing the size or charge conservative mutations Arg-126-Gln, Asp-49-Asn, and Arg-126-Lys, we inferred that a crystallographic water acts as a general base during GSH thiolate formation, stabilized by interaction with Arg-126, which is itself modulated by its respective interaction with Asp-49. We subsequently found hidden conformational ensembles within the crystal structure that correlate well with our biochemical data. The resulting contact signaling network connects Asp-49 to distal residues involved in GSH binding and is ligand dependent. Our work has broad implications for development of efficient mPGES-1 inhibitors, potential anti-inflammatory and anticancer agents.

Published

2016

18. Leukotriene A4 Hydrolase and Leukotriene C4 Synthase

Author

Agnes Rinaldo-Matthis and Jesper Z. Haeggström

Subjects

Leukotriene-A4 hydrolase, chemistry.chemical_compound, Leukotriene, chemistry, Biochemistry, Leukotriene C4, Leukotriene B4, medicine, Chemotaxis, Inflammation, Lipid signaling, medicine.symptom, Proinflammatory cytokine

Abstract

Leukotrienes are potent proinflammatory and immune modulating lipid mediators synthesized along the 5-lipoxygenase pathway of arachidonic acid metabolism. Leukotriene B4 is one of the most potent chemotactic agents known while leukotriene C4, D4, and E4 are a powerful smooth muscle contracting agents, particularly in the respiratory tract and microcirculation. The committed steps in the biosynthesis of leukotriene B4 and C4 are catalyzed by the key enzymes leukotriene A 4 hydrolase and leukotriene C 4 synthase, respectively. In this chapter we discuss the most recent advances in the understanding of these two enzymes at a structural, functional, and biological level.

Published

2016

19. Structural and Functional Analysis of Calcium Ion Mediated Binding of 5-Lipoxygenase to Nanodiscs

Author

Ramakrishnan B. Kumar, Olof Rådmark, Lin Zhu, Hans Hebert, Agnes Rinaldo-Matthis, Helena Idborg, Per-Johan Jakobsson, and Caroline Jegerschöld

Subjects

0301 basic medicine, lcsh:Medicine, Plasma protein binding, Negative Staining, Biochemistry, Physical Chemistry, Polyacrylamide Gel Electrophoresis, chemistry.chemical_compound, lcsh:Science, Phospholipids, Gel Electrophoresis, Gel electrophoresis, Staining, Liposome, Multidisciplinary, Chemistry, Physics, Negative stain, Lipids, Biofysik, Native Polyacrylamide Gel Electrophoresis, Physical sciences, Membrane, Chromatography, Gel, Cellular Structures and Organelles, Dimerization, Protein Binding, Research Article, Chemical physics, Biophysics, Research and Analysis Methods, 03 medical and health sciences, Electrophoretic Techniques, Microscopy, Electron, Transmission, Humans, Vesicles, POPC, Nanodisc, Arachidonate 5-Lipoxygenase, lcsh:R, Biology and Life Sciences, Dimers (Chemical physics), Cell Biology, Nanostructures, 030104 developmental biology, Membrane protein, Chemical Properties, Specimen Preparation and Treatment, Liposomes, lcsh:Q, Calcium

Abstract

An important step in the production of inflammatory mediators of the leukotriene family is the Ca2+ mediated recruitment of 5 Lipoxygenase (5LO) to nuclear membranes. To study this reaction in vitro, the natural membrane mimicking environment of nanodiscs was used. Nanodiscs with 10.5 nm inner diameter were made with the lipid POPC and membrane scaffolding protein MSP1E3D1. Monomeric and dimeric 5LO were investigated. Monomeric 5LO mixed with Ca2+ and nanodiscs are shown to form stable complexes that 1) produce the expected leukotriene products from arachidonic acid and 2) can be, for the first time, visualised by native gel electrophoresis and negative stain transmission electron micros-copy and 3) show a highest ratio of two 5LO per nanodisc. We interpret this as one 5LO on each side of the disc. The dimer of 5LO is visualised by negative stain transmission electron microscopy and is shown to not bind to nanodiscs. This study shows the advantages of nanodiscs to obtain basic structural information as well as functional information of a complex between a monotopic membrane protein and the membrane. QC 20160428

Published

2016

20. Anopheles gambiaePurine Nucleoside Phosphorylase: Catalysis, Structure, and Inhibition

Author

Keith Z. Hazleton, Vern L. Schramm, Lei Li, Erika A. Taylor, Agnes Rinaldo-Matthis, Maria B. Cassera, Steven C. Almo, and Mahmoud Ghanem

Subjects

Purine, Protein Conformation, Stereochemistry, Anopheles gambiae, Molecular Sequence Data, Guanosine, Purine nucleoside phosphorylase, Crystallography, X-Ray, Biochemistry, Catalysis, chemistry.chemical_compound, Anopheles, medicine, Animals, Deoxyguanosine, Amino Acid Sequence, Purine metabolism, Inosine, Binding Sites, Sequence Homology, Amino Acid, biology, biology.organism_classification, Dissociation constant, Kinetics, Purine-Nucleoside Phosphorylase, chemistry, medicine.drug

Abstract

The purine salvage pathway of Anopheles gambiae, a mosquito that transmits malaria, has been identified in genome searches on the basis of sequence homology with characterized enzymes. Purine nucleoside phosphorylase (PNP) is a target for the development of therapeutic agents in humans and purine auxotrophs, including malarial parasites. The PNP from Anopheles gambiae (AgPNP) was expressed in Escherichia coli and compared to the PNPs from Homo sapiens (HsPNP) and Plasmodium falciparum (PfPNP). AgPNP has kcat values of 54 and 41 s-1 for 2'-deoxyinosine and inosine, its preferred substrates, and 1.0 s-1 for guanosine. However, the chemical step is fast for AgPNP at 226 s-1 for guanosine in pre-steady-state studies. 5'-Deaza-1'-aza-2'-deoxy-1'-(9-methylene)-Immucillin-H (DADMe-ImmH) is a transition-state mimic for a 2'-deoxyinosine ribocation with a fully dissociated N-ribosidic bond and is a slow-onset, tight-binding inhibitor with a dissociation constant of 3.5 pM. This is the tightest-binding inhibitor known for any PNP, with a remarkable Km/Ki* of 5.4 x 10(7), and is consistent with enzymatic transition state predictions of enhanced transition-state analogue binding in enzymes with enhanced catalytic efficiency. Deoxyguanosine is a weaker substrate than deoxyinosine, and DADMe-Immucillin-G is less tightly bound than DADMe-ImmH, with a dissociation constant of 23 pM for AgPNP as compared to 7 pM for HsPNP. The crystal structure of AgPNP was determined in complex with DADMe-ImmH and phosphate to a resolution of 2.2 A to reveal the differences in substrate and inhibitor specificity. The distance from the N1' cation to the phosphate O4 anion is shorter in the AgPNP.DADMe-ImmH.PO4 complex than in HsPNP.DADMe-ImmH.SO4, offering one explanation for the stronger inhibitory effect of DADMe-ImmH for AgPNP.

Published

2007

21. Neighboring Group Participation in the Transition State of Human Purine Nucleoside Phosphorylase

Author

Matthew R Birck, Erika A. Taylor, Agnes Rinaldo-Matthis, Steven C. Almo, Wuxian Shi, Vern L. Schramm, and Andrew S. Murkin

Subjects

Base Sequence, Transition (genetics), Protein Conformation, Hydrogen bond, Stereochemistry, Chemistry, Mutagenesis, Purine nucleoside phosphorylase, Crystallography, X-Ray, Biochemistry, Catalysis, Article, Kinetics, Protein structure, Purine-Nucleoside Phosphorylase, Kinetic isotope effect, Mutagenesis, Site-Directed, medicine, Humans, Purine metabolism, Inosine, DNA Primers, medicine.drug

Abstract

The X-ray crystal structures of human purine nucleoside phosphorylase (PNP) with bound inosine or transition-state analogues show His257 within hydrogen bonding distance of the 5'-hydroxyl. The mutants His257Phe, His257Gly, and His257Asp exhibited greatly decreased affinity for Immucillin-H (ImmH), binding this mimic of an early transition state as much as 370-fold (Km/Ki) less tightly than native PNP. In contrast, these mutants bound DADMe-ImmH, a mimic of a late transition state, nearly as well as the native enzyme. These results indicate that His257 serves an important role in the early stages of transition-state formation. Whereas mutation of His257 resulted in little variation in the PNP x DADMe-ImmH x SO4 structures, His257Phe x ImmH x PO4 showed distortion at the 5'-hydroxyl, indicating the importance of H-bonding in positioning this group during progression to the transition state. Binding isotope effect (BIE) and kinetic isotope effect (KIE) studies of the remote 5'-(3)H for the arsenolysis of inosine with native PNP revealed a BIE of 1.5% and an unexpectedly large intrinsic KIE of 4.6%. This result is interpreted as a moderate electronic distortion toward the transition state in the Michaelis complex with continued development of a similar distortion at the transition state. The mutants His257Phe, His257Gly, and His257Asp altered the 5'-(3)H intrinsic KIE to -3, -14, and 7%, respectively, while the BIEs contributed 2, 2, and -2%, respectively. These surprising results establish that forces in the Michaelis complex, reported by the BIEs, can be reversed or enhanced at the transition state.

Published

2007

22. Inhibition and Structure of Trichomonas vaginalis Purine Nucleoside Phosphorylase with Picomolar Transition State Analogues

Author

Corin Wing, Agnes Rinaldo-Matthis, Peng Wu, Steven C. Almo, Mahmoud Ghanem, Hua Deng, Arti Gupta, Richard Hubert Furneaux, Ching C. Wang, Gary B. Evans, Peter C. Tyler, and Vern L. Schramm

Subjects

Models, Molecular, Purine, Adenosine, Pyrrolidines, Stereochemistry, Purine nucleoside phosphorylase, Crystallography, X-Ray, Biochemistry, Article, Substrate Specificity, chemistry.chemical_compound, Catalytic Domain, Trichomonas vaginalis, medicine, Animals, biology, Transition (genetics), Hydrogen bond, Adenine, biology.organism_classification, Tautomer, Dissociation constant, Crystallography, Purine-Nucleoside Phosphorylase, chemistry, Crystallization, Imma, medicine.drug

Abstract

Trichomonas vaginalis is a parasitic protozoan purine auxotroph possessing a unique purine salvage pathway consisting of a bacterial type purine nucleoside phosphorylase (PNP) and a purine nucleoside kinase. Thus, T. vaginalis PNP (TvPNP) functions in the reverse direction relative to the PNPs in other organisms. Immucillin-A (ImmA) and DADMe-Immucillin-A (DADMe-ImmA) are transition state mimics of adenosine with geometric and electrostatic features that resemble early and late transition states of adenosine at the transition state stabilized by TvPNP. ImmA demonstrates slow-onset tight-binding inhibition with TvPNP, to give an equilibrium dissociation constant of 87 pM, an inhibitor release half-time of 17.2 min, and a Km/Kd ratio of 70,100. DADMe-ImmA resembles a late ribooxacarbenium ion transition state for TvPNP to give a dissociation constant of 30 pM, an inhibitor release half-time of 64 min, and a Km/Kd ratio of 203,300. The tight binding of DADMe-ImmA supports a late SN1 transition state. Despite their tight binding to TvPNP, ImmA and DADMe-ImmA are weak inhibitors of human and P. falciparum PNPs. The crystal structures of the TvPNP x ImmA x PO4 and TvPNP x DADMe-ImmA x PO4 ternary complexes differ from previous structures with substrate analogues. The tight binding with DADMe-ImmA is in part due to a 2.7 A ionic interaction between a PO4 oxygen and the N1' cation of the hydroxypyrrolidine and is weaker in the TvPNP x ImmA x PO4 structure at 3.5 A. However, the TvPNP x ImmA x PO4 structure includes hydrogen bonds between the 2'-hydroxyl and the protein that are not present in TvPNP x DADMe-ImmA x PO4. These structures explain why DADMe-ImmA binds tighter than ImmA. Immucillin-H is a 12 nM inhibitor of TvPNP but a 56 pM inhibitor of human PNP. And this difference is explained by isotope-edited difference infrared spectroscopy with [6-18O]ImmH to establish that O6 is the keto tautomer in TvPNP x ImmH x PO4, causing an unfavorable leaving-group interaction.

Published

2006

23. Structural Basis for Substrate Specificity of the Human Mitochondrial Deoxyribonucleotidase

Author

Vera Bianchi, Agnes Rinaldo-Matthis, Benedetta Ruzzenente, Pär Nordlund, and Karin Walldén

Subjects

Models, Molecular, Stereochemistry, Electrons, Biology, Crystallography, X-Ray, Substrate Specificity, chemistry.chemical_compound, Structural Biology, Hydrolase, Serine, Thymidine Monophosphate, Humans, Deoxyguanosine, Isoleucine, 5'-Nucleotidase, Molecular Biology, chemistry.chemical_classification, Binding Sites, Nucleosides, Ribonucleoside, Deoxyuridine, Uridine, Mitochondria, Kinetics, Enzyme, chemistry, Biochemistry, Mutagenesis, Site-Directed, Thymidine, Nucleoside, Dinucleoside Phosphates, Protein Binding

Abstract

Summary The human mitochondrial deoxyribonucleotidase catalyzes the dephosphorylation of thymidine and deoxyuridine monophosphates and participates in the regulation of the dTTP pool in mitochondria. We present seven structures of the inactive D41N variant of this enzyme in complex with thymidine 3′-monophosphate, thymidine 5′-monophosphate, deoxyuridine 5′-monophosphate, uridine 5′-monophosphate, deoxyguanosine 5′-monophosphate, uridine 2′-monophosphate, and the 5′-monophosphate of the nucleoside analog 3′-deoxy 2′3′-didehydrothymidine, and we draw conclusions about the substrate specificity based on comparisons with enzyme activities. We show that the enzyme's specificity for the deoxyribo form of nucleoside 5′-monophosphates is due to Ile-133, Phe-49, and Phe-102, which surround the 2′ position of the sugar and cause an energetically unfavorable environment for the 2′-hydroxyl group of ribonucleoside 5′-monophosphates. The close binding of the 3′-hydroxyl group of nucleoside 5′-monophosphates to the enzyme indicates that nucleoside analog drugs that are substituted with a bulky group at this position will not be good substrates for this enzyme.

Published

2005

24. Structural and Mutational Studies of the Carboxylate Cluster in Iron-Free Ribonucleotide Reductase R2

Author

Wolfgang Blodig, Yuhe Liang, Britt-Marie Sjöberg, Agnes Rinaldo-Matthis, Martin Högbom, Martin E. Andersson, Bert Ove Persson, Pär Nordlund, and Xiao-Dong Su

Subjects

Base Sequence, Protein Conformation, Hydrogen bond, Stereochemistry, Iron, Mutagenesis, Carboxylic Acids, Protonation, Crystallography, X-Ray, medicine.disease_cause, Biochemistry, chemistry.chemical_compound, Ribonucleotide reductase, chemistry, Ribonucleotide Reductases, Mutagenesis, Site-Directed, medicine, Side chain, Carboxylate, Crystallization, Escherichia coli, Histidine, DNA Primers

Abstract

The R2 protein of ribonucleotide reductase features a di-iron site deeply buried in the protein interior. The apo form of the R2 protein has an unusual clustering of carboxylate side chains at the empty metal-binding site. In a previous study, it was found that the loss of the four positive charge equivalents of the diferrous site in the apo protein appeared to be compensated for by the protonation of two histidine and two carboxylate side chains. We have studied the consequences of removing and introducing charged residues on the local hydrogen-bonding pattern in the region of the carboxylate cluster of Corynebacterium ammoniagenes and Escherichia coli protein R2 using site-directed mutagenesis and X-ray crystallography. The structures of the metal-free forms of wild-type C. ammoniagenes R2 and the mutant E. coli proteins D84N, S114D, E115A, H118A, and E238A have been determined and their hydrogen bonding and protonation states have been structurally assigned as far as possible. Significant alterations to the hydrogen-bonding patterns, protonation states, and hydration is observed for all mutant E. coli apo proteins as compared to wild-type apo R2. Further structural variations are revealed by the wild-type apo C. ammoniagenes R2 structure. The protonation and hydration effects seen in the carboxylate cluster appear to be due to two major factors: conservation of the overall charge of the site and the requirement of electrostatic shielding of clustered carboxylate residues. Very short hydrogen-bonding distances between some protonated carboxylate pairs are indicative of low-barrier hydrogen bonding.

Published

2004

25. Structure and inhibition of mouse leukotriene C4 synthase

Author

Jesper Z. Haeggström, Thea Kleinschmidt, Damian Niegowski, Abdul Aziz Qureshi, Agnes Rinaldo-Matthis, Michaela Mårback, and Shabbir Ahmad

Subjects

Models, Molecular, Protein Conformation, Competitive Inhibitors, lcsh:Medicine, Biochemistry, chemistry.chemical_compound, Mice, 0302 clinical medicine, Medicine and Health Sciences, Cloning, Molecular, Enzyme Inhibitors, lcsh:Science, Integral membrane protein, Glutathione Transferase, chemistry.chemical_classification, 0303 health sciences, Leukotriene, Multidisciplinary, ATP synthase, Fatty Acids, Lipids, Enzyme structure, 3. Good health, Enzymes, Isoenzymes, 030220 oncology & carcinogenesis, Research Article, Protein Structure, Inflammatory Diseases, Molecular Sequence Data, Biology, 03 medical and health sciences, Lipid Mediators, In vivo, Transferases, Chemical Biology, Animals, Humans, Enzyme kinetics, Amino Acid Sequence, 030304 developmental biology, Enzyme Kinetics, Leukotriene C4, lcsh:R, Biology and Life Sciences, Proteins, Biochemical Activity, Enzyme, chemistry, Enzyme Structure, biology.protein, Biocatalysis, Enzymology, lcsh:Q

Abstract

Leukotriene (LT) C4 synthase (LTC4S) is an integral membrane protein that catalyzes the conjugation reaction between the fatty acid LTA4 and GSH to form the pro-inflammatory LTC4, an important mediator of asthma. Mouse models of inflammatory disorders such as asthma are key to improve our understanding of pathogenesis and potential therapeutic targets. Here, we solved the crystal structure of mouse LTC4S in complex with GSH and a product analog, S-hexyl-GSH. Furthermore, we synthesized a nM inhibitor and compared its efficiency and binding mode against the purified mouse and human isoenzymes, along with the enzymes’ steady-state kinetics. Although structural differences near the active site and along the C-terminal α-helix V suggest that the mouse and human LTC4S may function differently in vivo, our data indicate that mouse LTC4S will be a useful tool in future pharmacological research and drug development.

Published

2014

26. The Crystal Structure of an Azide Complex of the Diferrous R2 Subunit of Ribonucleotide Reductase Displays a Novel Carboxylate Shift with Important Mechanistic Implications for Diiron-Catalyzed Oxygen Activation

Author

Kerstin Andersson, Britt-Marie Sjöberg, Martin E. Andersson, Martin Högbom, Pär Nordlund, and Agnes Rinaldo-Matthis

Subjects

chemistry.chemical_classification, Stereochemistry, Protein subunit, chemistry.chemical_element, General Chemistry, Crystal structure, Biochemistry, Oxygen, Catalysis, chemistry.chemical_compound, Colloid and Surface Chemistry, Ribonucleotide reductase, chemistry, Oxidoreductase, Carboxylate, Azide

Abstract

The crystal structure of an azide complex of the diferrous R2 subunit of ribonucleotide reductase displays a novel carboxylate shift with important mechanistic implications for diiron-catalyzed oxygen activation

Published

1999

27. Crystal structures of leukotriene C4 synthase in complex with product analogs: implications for the enzyme mechanism

Author

Damian, Niegowski, Thea, Kleinschmidt, Ulrika, Olsson, Shabbir, Ahmad, Agnes, Rinaldo-Matthis, and Jesper Z, Haeggström

Subjects

Models, Molecular, Protein Conformation, Tryptophan, Membrane Proteins, LTC4 Synthase, Crystallography, X-Ray, Leukotriene A4, Glutathione, Lipids, Leukotriene C4, Asthma, Glutathion, Lipid-binding Protein, Substrate Specificity, Kinetics, LTA4, Biocatalysis, LTC4, Humans, Mutant Proteins, Glutathione Transferase, Leukotriene

Abstract

Background: Leukotriene (LT) C4 synthase (LTC4S) is a membrane protein catalyzing the formation of pathogenic mediators of asthma. Results: Crystal structures of complexes of WT and mutated LTC4S with three product analogs. Conclusion: Evidence for the binding mode of LTA4 and LTC4 at the active site of LTC4S and a mechanistic model. Significance: New insights into the molecular mechanism of LTC4S., Leukotriene (LT) C4 synthase (LTC4S) catalyzes the conjugation of the fatty acid LTA4 with the tripeptide GSH to produce LTC4, the parent compound of the cysteinyl leukotrienes, important mediators of asthma. Here we mutated Trp-116 in human LTC4S, a residue proposed to play a key role in substrate binding, into an Ala or Phe. Biochemical and structural characterization of these mutants along with crystal structures of the wild type and mutated enzymes in complex with three product analogs, viz. S-hexyl-, 4-phenyl-butyl-, and 2-hydroxy-4-phenyl-butyl-glutathione, provide new insights to binding of substrates and product, identify a new conformation of the GSH moiety at the active site, and suggest a route for product release, aided by Trp-116.

Published

2013

28. A mutation interfering with 5-lipoxygenase domain interaction leads to increased enzyme activity

Author

Bettina Hofmann, Bengt Samuelsson, Colin D. Funk, Marija Rakonjac Ryge, Agnes Rinaldo-Matthis, Bengt Persson, Olof Rådmark, Xin-Sheng Chen, Takashi Watanabe, Dieter Steinhilber, Patrick Provost, and Michiharu Tanabe

Subjects

Models, Molecular, Leukotrienes, Stereochemistry, Molecular Sequence Data, Biophysics, medicine.disease_cause, Biochemistry, Catalysis, Catalytic Domain, medicine, Humans, Point Mutation, Amino Acid Sequence, Molecular Biology, Mutation, Arachidonate 5-Lipoxygenase, integumentary system, biology, Chemistry, Hydrogen bond, food and beverages, Active site, Enzyme assay, Yeast, Protein Structure, Tertiary, Enzyme Activation, Arachidonate 5-lipoxygenase, Helix, biology.protein, Mutagenesis, Site-Directed

Abstract

5-Lipoxygenase (5-LOX) catalyzes two steps in conversion of arachidonic acid to proinflammatory leukotrienes. Lipoxygenases, including human 5-LOX, consist of an N-terminal C2-like β-sandwich and a catalytic domain. We expressed the 5-LOX domains separately, these were found to interact in the yeast two-hybrid system. The 5-LOX structure suggested association between Arg(101) in the β-sandwich and Asp(166) in the catalytic domain, due to electrostatic interaction as well as hydrogen bonds. Indeed, mutagenic replacements of these residues led to loss of two-hybrid interaction. Interestingly, when Arg(101) was mutated to Asp in intact 5-LOX, enzyme activity was increased. Thus, higher initial velocity of the reaction (vinit) and increased final amount of products were monitored for 5-LOX-R101D, at several different assay conditions. In the 5-LOX crystal structure, helix α2 and adjacent loops (including Asp(166)) of the 5-LOX catalytic domain has been proposed to form a flexible lid controlling access to the active site, and lid movement would be determined by bonding of lid residues to the C2-like β-sandwich. The more efficient catalysis following disruption of the R101-D166 ionic association supports the concept of such a flexible lid in human 5-LOX.

Published

2013

29. Zinc Leukotriene A4 Hydrolase/Aminopeptidase Dual Activity

Author

Jesper Z. Haeggström and Agnes Rinaldo-Matthis

Published

2013

30. A picomolar transition state analogue inhibitor of MTAN as a specific antibiotic for Helicobacter pylori

Author

Quan Du, Agnes Rinaldo-Matthis, Shanzhi Wang, A.M. Haapalainen, Steven C. Almo, Peter C. Tyler, Funing Yan, Gary B. Evans, Vern L. Schramm, Gillian E. Norris, and Rosemary L. Brown

Subjects

Models, Molecular, Menaquinone synthesis, Pyrrolidines, Helicobacter pylori, medicine.drug_class, Campylobacter, Adenine, Antibiotics, Biology, medicine.disease_cause, biology.organism_classification, Biochemistry, Article, Microbiology, Anti-Bacterial Agents, Helicobacter Infections, Transition state analog, Growth arrest, Hydrolase, medicine, Humans, Enzyme Inhibitors, Helicobacter species, N-Glycosyl Hydrolases

Abstract

Campylobacter and Helicobacter species express a 6-amino-6-deoxyfutalosine N-ribosylhydrolase (HpMTAN) proposed to function in menaquinone synthesis. BuT-DADMe-ImmA is a 36 pM transition state analogue of HpMTAN, and the crystal structure of the enzyme–inhibitor complex reveals the mechanism of inhibition. BuT-DADMe-ImmA has a MIC90 value of

Published

2012

31. Pre-steady-state kinetic characterization of thiolate anion formation in human leukotriene C₄ synthase

Author

Agnes, Rinaldo-Matthis, Shabbir, Ahmad, Anders, Wetterholm, Peter, Lachmann, Ralf, Morgenstern, and Jesper Z, Haeggström

Subjects

Protein Conformation, Anti-Inflammatory Agents, Non-Steroidal, Hydrogen-Ion Concentration, Arginine, Leukotriene A4, Binding, Competitive, Glutathione, Leukotriene C4, Recombinant Proteins, Isoenzymes, Kinetics, Protein Subunits, Catalytic Domain, Biocatalysis, Humans, Cysteine, Molecular Targeted Therapy, Enzyme Inhibitors, Glutathione Transferase

Abstract

Human leukotriene C₄ synthase (hLTC4S) is an integral membrane protein that catalyzes the committed step in the biosynthesis of cysteinyl-leukotrienes, i.e., formation of leukotriene C₄ (LTC₄). This molecule, together with its metabolites LTD₄ and LTE₄, induces inflammatory responses, particularly in asthma, and thus, the enzyme is an attractive drug target. During the catalytic cycle, glutathione (GSH) is activated by hLTC4S that forms a nucleophilic thiolate anion that will attack LTA₄, presumably according to an S(N)2 reaction to form LTC₄. We observed that GSH thiolate anion formation is rapid and occurs at all three monomers of the homotrimer and is concomitant with stoichiometric release of protons to the medium. The pK(a) (5.9) for enzyme-bound GSH thiol and the rate of thiolate formation were determined (k(obs) = 200 s⁻¹). Taking advantage of a strong competitive inhibitor, glutathionesulfonic acid, shown here by crystallography to bind in the same location as GSH, we determined the overall dissociation constant (K(d((GS) = 14.3 μM). The release of the thiolate was assessed using a GSH release experiment (1.3 s⁻¹). Taken together, these data establish that thiolate anion formation in hLTC4S is not the rate-limiting step for the overall reaction of LTC₄ production (k(cat) = 26 s⁻¹), and compared to the related microsomal glutathione transferase 1, which displays very slow GSH thiolate anion formation and one-third of the sites reactivity, hLTC4S has evolved a different catalytic mechanism.

Published

2012

32. A High Affinity Adenosine Kinase from Anopheles gambiae

Author

Meng-Chiao Ho, Emmanuel S. Burgos, Emilio F. Merino, Vern L. Schramm, Agnes Rinaldo-Matthis, Steven C. Almo, and Maria B. Cassera

Subjects

Purine, Models, Molecular, Adenosine, Protein Conformation, Adenosine kinase, Crystallography, X-Ray, Biochemistry, Article, Substrate Specificity, chemistry.chemical_compound, parasitic diseases, Anopheles, medicine, Transferase, Animals, Humans, Nucleotide, Adenosine Kinase, chemistry.chemical_classification, Binding Sites, Genome, biology, Hydrogen Bonding, Enzyme, chemistry, biology.protein, Insect Proteins, Nucleoside, Ap4A, medicine.drug

Abstract

Genome analysis revealed a mosquito orthologue of adenosine kinase in Anopheles gambiae (AgAK; the most important vector for the transmission of Plasmodium falciparum in Africa). P. falciparum are purine auxotrophs and do not express an adenosine kinase but rely on their hosts for purines. AgAK was kinetically characterized and found to have the highest affinity for adenosine (K(m) = 8.1 nM) of any known adenosine kinase. AgAK is specific for adenosine at the nucleoside site, but several nucleotide triphosphate phosphoryl donors are tolerated. The AgAK crystal structure with a bound bisubstrate analogue Ap(4)A (2.0 Å resolution) reveals interactions for adenosine and ATP and the geometry for phosphoryl transfer. The polyphosphate charge is partly neutralized by a bound Mg(2+) ion and an ion pair to a catalytic site Arg. The AgAK structure consists of a large catalytic core in a three-layer α/β/α sandwich, and a small cap domain in contact with adenosine. The specificity and tight binding for adenosine arise from hydrogen bond interactions of Asn14, Leu16, Leu40, Leu133, Leu168, Phe168, and Thr171 and the backbone of Ile39 and Phe168 with the adenine ring as well as through hydrogen bond interactions between Asp18, Gly64, and Asn68 and the ribosyl 2'- and 3'-hydroxyl groups. The structure is more similar to that of human adenosine kinase (48% identical) than to that of AK from Toxoplasma gondii (31% identical). With this extraordinary affinity for AgAK, adenosine is efficiently captured and converted to AMP at near the diffusion limit, suggesting an important role for this enzyme in the maintenance of the adenine nucleotide pool. mRNA analysis verifies that AgAK transcripts are produced in the adult insects.

Published

2011

33. Four generations of transition-state analogues for human purine nucleoside phosphorylase

Author

Meng-Chiao Ho, Agnes Rinaldo-Matthis, Steven C. Almo, Keith Clinch, Vern L. Schramm, Wuxian Shi, Peter C. Tyler, and Gary B. Evans

Subjects

chemistry.chemical_classification, Models, Molecular, Multidisciplinary, Pyrrolidines, Stereochemistry, Protein Conformation, Binding energy, Leaving group, Purine nucleoside phosphorylase, Crystal structure, Purine Nucleosides, Pyrimidinones, Biological Sciences, Enzyme structure, Protein structure, Enzyme, chemistry, Purine-Nucleoside Phosphorylase, Catalytic Domain, Animals, Humans, Thermodynamics, Cattle, Enzyme Inhibitors, Purine metabolism

Abstract

Inhibition of human purine nucleoside phosphorylase (PNP) stops growth of activated T-cells and the formation of 6-oxypurine bases, making it a target for leukemia, autoimmune disorders, and gout. Four generations of ribocation transition-state mimics bound to PNP are structurally characterized. Immucillin-H ( , first-generation) contains an iminoribitol cation with four asymmetric carbons. DADMe-Immucillin-H ( , second-generation), uses a methylene-bridged dihydroxypyrrolidine cation with two asymmetric centers. DATMe-Immucillin-H ( , third-generation) contains an open-chain amino alcohol cation with two asymmetric carbons. SerMe-ImmH ( , fourth-generation) uses achiral dihydroxyaminoalcohol seramide as the ribocation mimic. Crystal structures of PNPs establish features of tight binding to be; 1) ion-pair formation between bound phosphate (or its mimic) and inhibitor cation, 2) leaving-group interactions to N1, O6, and N7 of 9-deazahypoxanthine, 3) interaction between phosphate and inhibitor hydroxyl groups, and 4) His257 interacting with the 5′-hydroxyl group. The first generation analogue is an imperfect fit to the catalytic site with a long ion pair distance between the iminoribitol and bound phosphate and weaker interactions to the leaving group. Increasing the ribocation to leaving-group distance in the second- to fourth-generation analogues provides powerful binding interactions and a facile synthetic route to powerful inhibitors. Despite chemical diversity in the four generations of transition-state analogues, the catalytic site geometry is almost the same for all analogues. Multiple solutions in transition-state analogue design are available to convert the energy of catalytic rate enhancement to binding energy in human PNP.

Published

2010

34. Transition state analogs of 5'-methylthioadenosine nucleosidase disrupt quorum sensing

Author

Meng-Chiao Ho, Agnes Rinaldo-Matthis, Jemy A. Gutierrez, Tamara Crowder, Steven C. Almo, and Vern L. Schramm

Subjects

Models, Molecular, Pyrrolidines, medicine.disease_cause, Article, Substrate Specificity, Methylthioadenosine nucleosidase, Transition state analog, medicine, Molecular Biology, Escherichia coli, N-Glycosyl Hydrolases, Vibrio cholerae, chemistry.chemical_classification, Molecular Structure, Chemistry, Adenine, Escherichia coli Proteins, Biofilm, Quorum Sensing, Cell Biology, Gene Expression Regulation, Bacterial, Quorum sensing, Enzyme, Biochemistry, Biofilms, Enterohemorrhagic Escherichia coli, Autoinducer

Abstract

5'-Methylthioadenosine/S-adenosylhomocysteine nucleosidase (MTAN) is a bacterial enzyme involved in S-adenosylmethionine-related quorum sensing pathways that induce bacterial pathogenesis factors. Transition state analogs MT-DADMe-Immucillin-A, EtT-DADMe-Immucillin-A and BuT-DADMe-Immucillin-A are slow-onset, tight-binding inhibitors of Vibrio cholerae MTAN (VcMTAN), with equilibrium dissociation constants of 73, 70 and 208 pM, respectively. Structural analysis of VcMTAN with BuT-DADMe-Immucillin-A revealed interactions contributing to the high affinity. We found that in V. cholerae cells, these compounds are potent MTAN inhibitors with IC(50) values of 27, 31 and 6 nM for MT-, EtT- and BuT-DADMe-Immucillin-A, respectively; the compounds disrupt autoinducer production in a dose-dependent manner without affecting growth. MT- and BuT-DADMe-Immucillin-A also inhibited autoinducer-2 production in enterohemorrhagic Escherichia coli O157:H7 with IC(50) values of 600 and 125 nM, respectively. BuT-DADMe-Immucillin-A inhibition of autoinducer-2 production in both strains persisted for several generations and caused reduction in biofilm formation. These results support MTAN's role in quorum sensing and its potential as a target for bacterial anti-infective drug design.

Published

2008

35. L-Enantiomers of transition state analogue inhibitors bound to human purine nucleoside phosphorylase

Author

Richard H. Furneaux, Vern L. Schramm, Agnes Rinaldo-Matthis, Keith Clinch, Gary B. Evans, Udupi A. Ramagopal, Peter C. Tyler, Andrew S. Murkin, Simon Peter Harold Mee, and Steven C. Almo

Subjects

Pyrrolidines, Transition (genetics), Stereochemistry, Chemistry, Protein Conformation, Leaving group, Purine nucleoside phosphorylase, Stereoisomerism, General Chemistry, Purine Nucleosides, Pyrimidinones, Crystallography, X-Ray, Biochemistry, Catalysis, Article, Substrate Specificity, Colloid and Surface Chemistry, Protein structure, Purine-Nucleoside Phosphorylase, Transition state analog, Transferase, Humans, Enzyme Inhibitors, Purine metabolism

Abstract

Human purine nucleoside phosphorylase (PNP) was crystallized with transition-state analogue inhibitors Immucillin-H and DADMe-Immucillin-H synthesized with ribosyl mimics of l-stereochemistry. The inhibitors demonstrate that major driving forces for tight binding of these analogues are the leaving group interaction and the cationic mimicry of the transition state, even though large geometric changes occur with d-Immucillins and l-Immucillins bound to human PNP.

Published

2007

36. Crystal structures of human and murine deoxyribonucleotidases: Insights into recognition of substrates and nucleotide analogues

Author

Benedetta Ruzzenente, Pär Nordlund, Agnes Rinaldo-Matthis, Karin Walldén, Vera Bianchi, and Chiara Rampazzo

Subjects

Models, Molecular, Stereochemistry, Protein Conformation, Molecular Sequence Data, Biology, Crystallography, X-Ray, Biochemistry, Substrate Specificity, Dephosphorylation, chemistry.chemical_compound, Mice, Animals, Humans, Nucleotide, Amino Acid Sequence, Phosphorylation, 5'-Nucleotidase, chemistry.chemical_classification, Sequence Homology, Amino Acid, DNA replication, Active site, Deoxyuridine, Deoxyribonucleoside, Enzyme, chemistry, biology.protein, Nucleoside

Abstract

Cytosolic 5'(3')-deoxyribonucleotidase (cdN) and mitochondrial 5'(3')-deoxyribonucleotidase (mdN) catalyze the dephosphorylation of deoxyribonucleoside monophosphates and regulate dTTP formation in cytosol and mitochondria, protecting DNA replication from imbalanced precursor pools. They can also interfere with the phosphorylation-dependent activation of nucleoside analogues used in anticancer and antiviral treatment. To understand the relatively narrow substrate specificity of these two enzymes and their ability to use nucleotide analogues as substrates, we determined the crystal structures of human cdN in complex with deoxyuridine, murine cdN in complex with dUMP and dGMP, and human mdN in complex with the nucleotide analogues AZTMP and BVdUMP. Our results show that the active site residues Leu45 and Tyr65 in cdN form a more favorable binding surface for purine nucleotides than the corresponding Trp75 and Trp76 in mdN, explaining why cdN has higher activity for purine nucleotides than does mdN. The molecular interactions of mdN with AZTMP and BVdUMP indicate why these nucleotide analogues are poorer substrates as compared with the physiological substrate, and they provide a structural rationale for the design of drugs that are less prone to inactivation by the deoxyribonucleotidases. We suggest that introduction of substituents in the 3'-position may result in nucleoside analogues with increased resistance to dephosphorylation.

Published

2007

37. Reaction mechanism of deoxyribonucleotidase: a theoretical study

Author

Fahmi Himo, ‡ and Agnes Rinaldo-Matthis, P. Nordlund, and Jing-Dong Guo

Subjects

Models, Molecular, Reaction mechanism, Binding Sites, Models, Statistical, Stereochemistry, Hydrolysis, Crystal structure, Phosphate, Crystallography, X-Ray, Organophosphates, Surfaces, Coatings and Films, Deoxyribonucleoside, Dephosphorylation, chemistry.chemical_compound, chemistry, Nucleophile, Models, Chemical, Nat, Materials Chemistry, Quantum Theory, Physical and Theoretical Chemistry, Phosphorylation, Nucleoside, 5'-Nucleotidase

Abstract

The reaction mechanism of human deoxyribonucleotidase (dN) is studied using high-level quantum-chemical methods. dN catalyzes the dephosphorylation of deoxyribonucleoside monophosphates (dNMPs) to their nucleoside form in human cells. Large quantum models are employed (99 atoms) based on a recent X-ray crystal structure [Rinaldo-Matthis et al. Nat. Struct. Biol. 2002, 9, 779]. The calculations support the proposed mechanism in which Asp41 performs a nucleophilic attack on the phosphate to form a phospho−enzyme intermediate. Asp43 acts in the first step as an acid, protonating the leaving nucleoside, and in the second step as a base, deprotonating the lytic water. No pentacoordinated intermediates could be located.

Published

2006

38. Crystal structure of a human mitochondrial deoxyribonucleotidase

Author

Peter Reichard, Agnes Rinaldo-Matthis, Vera Bianchi, Chiara Rampazzo, and Pär Nordlund

Subjects

Molecular Sequence Data, Sequence alignment, Biology, Crystallography, X-Ray, Biochemistry, Nucleotidases, Fluorides, Structural Biology, Nucleotidase, Genetics, Humans, Nucleotide, Amino Acid Sequence, 5'-Nucleotidase, chemistry.chemical_classification, Binding Sites, Phosphoserine phosphatase, Mitochondria, Protein Structure, Tertiary, Enzyme, chemistry, Beryllium, Nucleoside, Sequence Alignment, Mitochondrial DNA replication, Thymidine

Abstract

5′ nucleotidases are ubiquitous enzymes that dephosphorylate nucleoside monophosphates and participate in the regulation of nucleotide pools. The mitochondrial 5′-(3′) deoxyribonucleotidase (dNT-2) specifically dephosphorylates dUMP and dTMP, thereby protecting mitochondrial DNA replication from excess dTTP. We have solved the structure of dNT-2, the first of a mammalian 5′ nucleotidase. The structure reveals a relationship to the HAD family, members of which use an aspartyl nucleophile as their common catalytic strategy, with a phosphoserine phosphatase as the most similar neighbor. A structure-based sequence alignment of dNT-2 with other 5′ nucleotidases also suggests a common origin for these enzymes. Here we study the structures of dNT-2 in complex with bound phosphate and beryllium trifluoride plus thymidine as model for a phosphoenzyme–product complex. Based on these structures, determinants for substrate specificity recognition and the catalytic action of dNT-2 are outlined.

Published

2002

39. Structural studies on leukotriene A4 hydrolases reveal their catalytic mechanism

Author

Mahmudul Hasan, Marjolein M. G. M. Thunnissen, and Agnes Rinaldo-Matthis

Subjects

Inorganic Chemistry, chemistry.chemical_compound, chemistry, Structural Biology, Stereochemistry, Leukotriene A4, General Materials Science, Physical and Theoretical Chemistry, Condensed Matter Physics, Biochemistry, Mechanism (sociology), Catalysis

Abstract

Vertebrate leukotriene A4 hydrolases are zinc metalloenzymes with an epoxide hydrolase and aminopeptidase activity belonging to the M1 family of aminopeptidases. Bestatin, an amino peptidase inhibitor, can inhibit both the activities. The human enzyme produces LTB4, a powerful mediator of inflammation and is implicated in a wide variety of rheumatoid diseases. The yeast homolog scLTA4H contains only a rudimentary epoxide hydrolase activity. Both the structure of the human enzyme and recently the structure of scLTA4H and have been solved to investigate the molecular architecture of the active site both with and without inhibitor Bestatin. The structure of scLTA4H shows large domain movements creating an open active site. In the human enzyme the LTA4 binding side is a narrow hydrophobic channel. Upon inhibitor a domain shifts occurs and the final binding pocket is formed. The fact that scLTA4H displays this induced fit is an interesting observation. Many members of the M1 family seem to display a certain degree of induced fit, a feature, which however, has never been observed for humLTA4H. Our recent solution SAXS studies show that humLTA4H does not make any conformational changes upon inhibitor binding which is consistent with our previous speculation that it functions by a lock and key mechanism rather than induced fit and is better suited to supply the protective and precise environment for hydrolysis of LTA4 into LTB4. On the other hand Xenopus LTA4H shows conformational change in the higher/wide angular region ( >1 nm-1) and decrease in Porod volume of approximately 20 nm3 but no change in Rg or Dmax was observed. It is also observed that like in crystal structure Xenopus LTA4H forms dimer in solution. Similarly scLTA4H forms dimer in solution, which is unlike the crystal structure, and also make conformational changes upon inhibitor binding. Taken together, Xenopus and scLTA4H makes more compact form, with decrease in flexibility, to perform it's catalytic action.

Published

2014

40. Crystal structures of the mitochondrial deoxyribonucleotidase in complex with two specific inhibitors.

Author

Agnes, Rinaldo-Matthis, Chiara, Rampazzo, Jan, Balzarini, Peter, Reichard, Vera, Bianchi, and Pr, Nordlund

Abstract

Monophosphate nucleotidases are enzymes that dephosphorylate nucleotides to their corresponding nucleosides. They play potentially important roles in controlling the activation of nucleotide-based drugs targeted against viral infections or cancer cells. The human mitochondrial deoxyribonucleotidase (dNT-2) dephosphorylates thymidine and deoxyuridine monophosphates. We describe the high resolution structures of the dNT-2 enzyme in complex with two potent nucleoside phosphonate inhibitors, (S)-1-[2'-deoxy-3',5'-O-(1-phosphono) benzylidene-beta-d-threo-pentofuranosyl]thymine (DPB-T) at 1.6-A resolution and (+/-)-1-trans-(2-phosphonomethoxycyclopentyl)uracil (PMcP-U) at 1.4-A resolution. The mixed competitive inhibitor DPB-T and the competitive inhibitor PMcP-U both bind in the active site of dNT-2 but in distinctly different binding modes, explaining their different kinetics of inhibition. The pyrimidine part of the inhibitors binds with very similar hydrogen bond interactions to the protein but with their phosphonate moieties in different binding sites compared with each other and to the previously determined position of phosphate bound to dNT-2. Together, these phosphate/phosphonate binding sites describe what might constitute a functionally relevant phosphate entrance tunnel to the active site. The structures of the inhibitors in complex with dNT-2, being the first such complexes of any nucleotidase, might provide important information for the design of more specific inhibitors to control the activation of nucleotide-based drugs.

Published

2004