Your search keyword '"Ruda GF"' showing total 25 results

1. C8-substituted pyrido[3,4-d]pyrimidin-4(3H)-ones: Studies towards the identification of potent, cell penetrant Jumonji C domain containing histone lysine demethylase 4 subfamily (KDM4) inhibitors, compound profiling in cell-based target engagement assays

Author

Le Bihan, Y-V, Lanigan, RM, Atrash, B, McLaughlin, MG, Velupillai, S, Malcolm, AG, England, KS, Ruda, GF, Mok, NY, Tumber, A, Tomlin, K, Saville, H, Shehu, E, McAndrew, C, Carmichael, L, Bennett, JM, Jeganathan, F, Eve, P, Donovan, A, Hayes, A, Wood, F, Raynaud, FI, Fedorov, O, Brennan, PE, Burke, R, Van Montfort, RLM, Rossanese, OW, Blagg, J, and Bavetsias, V

Subjects

KDM4 subfamily, Jumonji Domain-Containing Histone Demethylases, Molecular Structure, Pyridines, Pyrimidinones, Crystallography, X-Ray, Article, Pyridopyrimidinones, Structure-Activity Relationship, Cell Line, Tumor, Humans, KDM inhibitors, Drug Screening Assays, Antitumor, Enzyme Inhibitors, KDM5 subfamily, Hydrophobic and Hydrophilic Interactions, Histone demethylases, Protein Binding

Abstract

Residues in the histone substrate binding sites that differ between the KDM4 and KDM5 subfamilies were identified. Subsequently, a C8-substituted pyrido[3,4-d]pyrimidin-4(3H)-one series was designed to rationally exploit these residue differences between the histone substrate binding sites in order to improve affinity for the KDM4-subfamily over KDM5-subfamily enzymes. In particular, residues E169 and V313 (KDM4A numbering) were targeted. Additionally, conformational restriction of the flexible pyridopyrimidinone C8-substituent was investigated. These approaches yielded potent and cell-penetrant dual KDM4/5-subfamily inhibitors including 19a (KDM4A and KDM5B Ki = 0.004 and 0.007 μM, respectively). Compound cellular profiling in two orthogonal target engagement assays revealed a significant reduction from biochemical to cell-based activity across multiple analogues; this decrease was shown to be consistent with 2OG competition, and suggests that sub-nanomolar biochemical potency will be required with C8-substituted pyrido[3,4-d]pyrimidin-4(3H)-one compounds to achieve sub-micromolar target inhibition in cells., Graphical abstract Image 1, Highlights • Targeting of KDM4A residues E169 and V313 to improve affinity for the KDM4-subfamily. • Potent and cell-penetrant KDM4/5-subfamily inhibitors such as 19a were identified. • Significant drop from biochemical to cell-based activity was observed. • Lower potency in cells is linked to competition with the 2OG co-substrate.

Published

2019

2. Applying a multitarget rational drug design strategy: The first set of modulators with potent and balanced activity toward dopamine D3 receptor and fatty acid amide hydrolase

Author

Gian Filippo Ruda, Andrea Cavalli, Tiziano Bandiera, Daniele Piomelli, Clara Albani, Giovanni Bottegoni, Alessio De Simone, Glauco Tarozzo, De Simone A, Ruda GF, Albani C, Tarozzo G, Bandiera T, Piomelli D, Cavalli A, and Bottegoni G

Subjects

Drug, media_common.quotation_subject, Drug design, Plasma protein binding, Pharmacology, Article, Catalysis, Amidohydrolases, Fatty acid amide hydrolase, Dopamine receptor D3, Materials Chemistry, Animals, Humans, Enzyme Inhibitors, Binding site, Receptor, media_common, chemistry.chemical_classification, Binding Sites, Receptors, Dopamine D3, Metals and Alloys, General Chemistry, Protein Structure, Tertiary, Rats, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, DRUG DISCOVERY, Molecular Docking Simulation, Enzyme, chemistry, Biochemistry, Drug Design, Dopamine Agonists, Ceramics and Composites, Protein Binding

Abstract

Combining computer-assisted drug design and synthetic efforts, we generated compounds with potent and balanced activities toward both D3 dopamine receptor and fatty acid amide hydrolase (FAAH) enzyme. By concurrently modulating these targets, our compounds hold great potential toward exerting a disease-modifying effect on nicotine addiction and other forms of compulsive behavior. © 2014 the Partner Organisations.

Published

2014

3. The X-linked histone demethylases KDM5C and KDM6A as regulators of T cell-driven autoimmunity in the central nervous system.

Author

Fazazi MR, Ruda GF, Brennan PE, and Rangachari M

Subjects

Animals, Female, Humans, Male, Mice, Central Nervous System, Histone Demethylases, Minor Histocompatibility Antigens, T-Lymphocytes, Autoimmunity, Encephalomyelitis, Autoimmune, Experimental

Abstract

T cell-driven autoimmune responses are subject to striking sex-dependent effects. While the contributions of sex hormones are well-understood, those of sex chromosomes are meeting with increased appreciation. Here, we outline what is known about the contribution of sex chromosome-linked factors to experimental autoimmune encephalomyelitis (EAE), a mouse model that recapitulates many of the T cell-driven mechanisms of multiple sclerosis (MS) pathology. Particular attention is paid to the KDM family of histone demethylases, several of which - KDM5C, KDM5D and KDM6A - are sex chromosome encoded. Finally, we provide evidence that functional inhibition of KDM5 molecules can suppress interferon (IFN)γ production from murine male effector T cells, and that an increased ratio of inflammatory Kdm6a to immunomodulatory Kdm5c transcript is observed in T helper 17 (Th17) cells from women with the autoimmune disorder ankylosing spondylitis (AS). Histone lysine demethlyases thus represent intriguing targets for the treatment of T cell-driven autoimmune disorders., Competing Interests: Declaration of Competing Interest The authors declare no competing interests., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

4. The structural basis of fatty acid elongation by the ELOVL elongases.

Author

Nie L, Pascoa TC, Pike ACW, Bushell SR, Quigley A, Ruda GF, Chu A, Cole V, Speedman D, Moreira T, Shrestha L, Mukhopadhyay SMM, Burgess-Brown NA, Love JD, Brennan PE, and Carpenter EP

Subjects

Adrenoleukodystrophy enzymology, Animals, Binding Sites, Catalytic Domain, Cloning, Molecular, Coenzyme A metabolism, Crystallography, X-Ray, Fatty Acid Elongases antagonists & inhibitors, Fatty Acid Elongases metabolism, HEK293 Cells, Histidine chemistry, Humans, Imidazoles metabolism, Models, Molecular, Protein Binding, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Sf9 Cells, Spectrometry, Mass, Electrospray Ionization methods, Structure-Activity Relationship, Substrate Specificity, Fatty Acid Elongases chemistry, Fatty Acids metabolism

Abstract

Very long chain fatty acids (VLCFAs) are essential building blocks for the synthesis of ceramides and sphingolipids. The first step in the fatty acid elongation cycle is catalyzed by the 3-keto acyl-coenzyme A (CoA) synthases (in mammals, ELOVL elongases). Although ELOVLs are implicated in common diseases, including insulin resistance, hepatic steatosis and Parkinson's, their underlying molecular mechanisms are unknown. Here we report the structure of the human ELOVL7 elongase, which comprises an inverted transmembrane barrel surrounding a 35-Å long tunnel containing a covalently attached product analogue. The structure reveals the substrate-binding sites in the narrow tunnel and an active site deep in the membrane. We demonstrate that chain elongation proceeds via an acyl-enzyme intermediate involving the second histidine in the canonical HxxHH motif. The unusual substrate-binding arrangement and chemistry suggest mechanisms for selective ELOVL inhibition, relevant for diseases where VLCFAs accumulate, such as X-linked adrenoleukodystrophy.

Published

2021

5. Male sex chromosomal complement exacerbates the pathogenicity of Th17 cells in a chronic model of central nervous system autoimmunity.

Author

Doss PMIA, Umair M, Baillargeon J, Fazazi R, Fudge N, Akbar I, Yeola AP, Williams JB, Leclercq M, Joly-Beauparlant C, Beauchemin P, Ruda GF, Alpaugh M, Anderson AC, Brennan PE, Droit A, Lassmann H, Moore CS, and Rangachari M

Subjects

Animals, Autoimmunity, CD4-Positive T-Lymphocytes cytology, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Disease Models, Animal, Down-Regulation, Encephalomyelitis, Autoimmune, Experimental immunology, Encephalomyelitis, Autoimmune, Experimental metabolism, Female, Histone Demethylases genetics, Histone Demethylases metabolism, Humans, Interferon-gamma metabolism, Male, Mice, Mice, Inbred NOD, Mice, Transgenic, Middle Aged, Multiple Sclerosis immunology, Multiple Sclerosis pathology, Nuclear Receptor Subfamily 1, Group F, Member 3 metabolism, Severity of Illness Index, Th17 Cells cytology, Th17 Cells metabolism, Encephalomyelitis, Autoimmune, Experimental pathology, Sex Chromosomes genetics, Th17 Cells immunology

Abstract

Sex differences in multiple sclerosis (MS) incidence and severity have long been recognized. However, the underlying cellular and molecular mechanisms for why male sex is associated with more aggressive disease remain poorly defined. Using a T cell adoptive transfer model of chronic experimental autoimmune encephalomyelitis (EAE), we find that male Th17 cells induce disease of increased severity relative to female Th17 cells, irrespective of whether transferred to male or female recipients. Throughout the disease course, a greater frequency of male Th17 cells produce IFNγ, a hallmark of pathogenic Th17 responses. Intriguingly, XY chromosomal complement increases the pathogenicity of male Th17 cells. An X-linked immune regulator, Jarid1c, is downregulated in pathogenic male murine Th17 cells, and functional experiments reveal that it represses the severity of Th17-mediated EAE. Furthermore, Jarid1c expression is downregulated in CD4 + T cells from MS-affected individuals. Our data indicate that male sex chromosomal complement critically regulates Th17 cell pathogenicity., Competing Interests: Declaration of interests M.R. has received speaker honoraria from Boehringer-Ingelheim GmbH, EMD Serono Canada, F. Hoffmann-La Roche, and Biogen Canada and has a research contract with Remedy Pharmaceuticals. These interests are unrelated to the present work., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

6. Rapid Covalent-Probe Discovery by Electrophile-Fragment Screening.

Author

Resnick E, Bradley A, Gan J, Douangamath A, Krojer T, Sethi R, Geurink PP, Aimon A, Amitai G, Bellini D, Bennett J, Fairhead M, Fedorov O, Gabizon R, Gan J, Guo J, Plotnikov A, Reznik N, Ruda GF, Díaz-Sáez L, Straub VM, Szommer T, Velupillai S, Zaidman D, Zhang Y, Coker AR, Dowson CG, Barr HM, Wang C, Huber KVM, Brennan PE, Ovaa H, von Delft F, and London N

Subjects

HEK293 Cells, Humans, Ligands, Models, Molecular, Molecular Weight, Protein Conformation, Time Factors, Drug Evaluation, Preclinical methods, Electrons

Abstract

Covalent probes can display unmatched potency, selectivity, and duration of action; however, their discovery is challenging. In principle, fragments that can irreversibly bind their target can overcome the low affinity that limits reversible fragment screening, but such electrophilic fragments were considered nonselective and were rarely screened. We hypothesized that mild electrophiles might overcome the selectivity challenge and constructed a library of 993 mildly electrophilic fragments. We characterized this library by a new high-throughput thiol-reactivity assay and screened them against 10 cysteine-containing proteins. Highly reactive and promiscuous fragments were rare and could be easily eliminated. In contrast, we found hits for most targets. Combining our approach with high-throughput crystallography allowed rapid progression to potent and selective probes for two enzymes, the deubiquitinase OTUB2 and the pyrophosphatase NUDT7. No inhibitors were previously known for either. This study highlights the potential of electrophile-fragment screening as a practical and efficient tool for covalent-ligand discovery.

Published

2019

7. Design, Synthesis, Structure-Activity Relationship Studies, and Three-Dimensional Quantitative Structure-Activity Relationship (3D-QSAR) Modeling of a Series of O-Biphenyl Carbamates as Dual Modulators of Dopamine D3 Receptor and Fatty Acid Amide Hydrolase.

Author

De Simone A, Russo D, Ruda GF, Micoli A, Ferraro M, Di Martino RM, Ottonello G, Summa M, Armirotti A, Bandiera T, Cavalli A, and Bottegoni G

Subjects

Amidohydrolases antagonists & inhibitors, Animals, Biphenyl Compounds chemical synthesis, Biphenyl Compounds chemistry, Biphenyl Compounds pharmacokinetics, Biphenyl Compounds pharmacology, Blood-Brain Barrier metabolism, CHO Cells, Carbamates chemical synthesis, Carbamates pharmacokinetics, Cricetulus, HEK293 Cells, Humans, Male, Models, Molecular, Piperazine, Piperazines chemical synthesis, Piperazines pharmacokinetics, Quantitative Structure-Activity Relationship, Rats, Sprague-Dawley, Receptors, Dopamine D3 agonists, Receptors, Dopamine D3 antagonists & inhibitors, Amidohydrolases metabolism, Carbamates chemistry, Carbamates pharmacology, Drug Design, Piperazines chemistry, Piperazines pharmacology, Receptors, Dopamine D3 metabolism

Abstract

We recently reported molecules designed according to the multitarget-directed ligand paradigm to exert combined activity at human fatty acid amide hydrolase (FAAH) and dopamine receptor subtype D3 (D3R). Both targets are relevant for tackling several types of addiction (most notably nicotine addiction) and other compulsive behaviors. Here, we report an SAR exploration of a series of biphenyl-N-[4-[4-(2,3-substituted-phenyl)piperazine-1-yl]alkyl]carbamates, a novel class of molecules that had shown promising activities at the FAAH-D3R target combination in preliminary studies. We have rationalized the structural features conducive to activities at the main targets and investigated activities at two off-targets: dopamine receptor subtype D2 and endocannabinoid receptor CB 1. To understand the unexpected affinity for the CB 1 receptor, we devised a 3D-QSAR model, which we then prospectively validated. Compound 33 was selected for PK studies because it displayed balanced affinities for the main targets and clear selectivity over the two off-targets. 33 has good stability and oral bioavailability and can cross the blood-brain barrier.

Published

2017

8. Potent and Selective KDM5 Inhibitor Stops Cellular Demethylation of H3K4me3 at Transcription Start Sites and Proliferation of MM1S Myeloma Cells.

Author

Tumber A, Nuzzi A, Hookway ES, Hatch SB, Velupillai S, Johansson C, Kawamura A, Savitsky P, Yapp C, Szykowska A, Wu N, Bountra C, Strain-Damerell C, Burgess-Brown NA, Ruda GF, Fedorov O, Munro S, England KS, Nowak RP, Schofield CJ, La Thangue NB, Pawlyn C, Davies F, Morgan G, Athanasou N, Müller S, Oppermann U, and Brennan PE

Subjects

Cell Cycle Checkpoints drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Crystallography, X-Ray, Glycine chemistry, Glycine metabolism, Glycine pharmacology, HeLa Cells, Humans, Kaplan-Meier Estimate, Ketoglutaric Acids chemistry, Ketoglutaric Acids metabolism, Methylation, Multiple Myeloma metabolism, Multiple Myeloma mortality, Multiple Myeloma pathology, Niacinamide chemistry, Niacinamide metabolism, Niacinamide pharmacology, Protein Isoforms antagonists & inhibitors, Protein Isoforms genetics, Protein Isoforms metabolism, Pyridines chemistry, Pyridines metabolism, Pyridines pharmacology, Retinoblastoma-Binding Protein 2 antagonists & inhibitors, Retinoblastoma-Binding Protein 2 genetics, Transcription Initiation Site, Glycine analogs & derivatives, Histones metabolism, Niacinamide analogs & derivatives, Retinoblastoma-Binding Protein 2 metabolism

Abstract

Methylation of lysine residues on histone tail is a dynamic epigenetic modification that plays a key role in chromatin structure and gene regulation. Members of the KDM5 (also known as JARID1) sub-family are 2-oxoglutarate (2-OG) and Fe 2+ -dependent oxygenases acting as histone 3 lysine 4 trimethyl (H3K4me3) demethylases, regulating proliferation, stem cell self-renewal, and differentiation. Here we present the characterization of KDOAM-25, an inhibitor of KDM5 enzymes. KDOAM-25 shows biochemical half maximal inhibitory concentration values of <100 nM for KDM5A-D in vitro, high selectivity toward other 2-OG oxygenases sub-families, and no off-target activity on a panel of 55 receptors and enzymes. In human cell assay systems, KDOAM-25 has a half maximal effective concentration of ∼50 μM and good selectivity toward other demethylases. KDM5B is overexpressed in multiple myeloma and negatively correlated with the overall survival. Multiple myeloma MM1S cells treated with KDOAM-25 show increased global H3K4 methylation at transcriptional start sites and impaired proliferation., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2017

9. Assessing histone demethylase inhibitors in cells: lessons learned.

Author

Hatch SB, Yapp C, Montenegro RC, Savitsky P, Gamble V, Tumber A, Ruda GF, Bavetsias V, Fedorov O, Atrash B, Raynaud F, Lanigan R, Carmichael L, Tomlin K, Burke R, Westaway SM, Brown JA, Prinjha RK, Martinez ED, Oppermann U, Schofield CJ, Bountra C, Kawamura A, Blagg J, Brennan PE, Rossanese O, and Müller S

Subjects

Apoptosis drug effects, Biocatalysis, Catalytic Domain, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, HeLa Cells, Histone Demethylases genetics, Histone Demethylases metabolism, Histones metabolism, Humans, Inhibitory Concentration 50, Methylation drug effects, Microscopy, Fluorescence, Mutagenesis, Paclitaxel toxicity, Phylogeny, Protein Isoforms antagonists & inhibitors, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Stability drug effects, Enzyme Inhibitors metabolism, Histone Demethylases antagonists & inhibitors

Abstract

Background: Histone lysine demethylases (KDMs) are of interest as drug targets due to their regulatory roles in chromatin organization and their tight associations with diseases including cancer and mental disorders. The first KDM inhibitors for KDM1 have entered clinical trials, and efforts are ongoing to develop potent, selective and cell-active 'probe' molecules for this target class. Robust cellular assays to assess the specific engagement of KDM inhibitors in cells as well as their cellular selectivity are a prerequisite for the development of high-quality inhibitors. Here we describe the use of a high-content cellular immunofluorescence assay as a method for demonstrating target engagement in cells., Results: A panel of assays for the Jumonji C subfamily of KDMs was developed to encompass all major branches of the JmjC phylogenetic tree. These assays compare compound activity against wild-type KDM proteins to a catalytically inactive version of the KDM, in which residues involved in the active-site iron coordination are mutated to inactivate the enzyme activity. These mutants are critical for assessing the specific effect of KDM inhibitors and for revealing indirect effects on histone methylation status. The reported assays make use of ectopically expressed demethylases, and we demonstrate their use to profile several recently identified classes of KDM inhibitors and their structurally matched inactive controls. The generated data correlate well with assay results assessing endogenous KDM inhibition and confirm the selectivity observed in biochemical assays with isolated enzymes. We find that both cellular permeability and competition with 2-oxoglutarate affect the translation of biochemical activity to cellular inhibition., Conclusions: High-content-based immunofluorescence assays have been established for eight KDM members of the 2-oxoglutarate-dependent oxygenases covering all major branches of the JmjC-KDM phylogenetic tree. The usage of both full-length, wild-type and catalytically inactive mutant ectopically expressed protein, as well as structure-matched inactive control compounds, allowed for detection of nonspecific effects causing changes in histone methylation as a result of compound toxicity. The developed assays offer a histone lysine demethylase family-wide tool for assessing KDM inhibitors for cell activity and on-target efficacy. In addition, the presented data may inform further studies to assess the cell-based activity of histone lysine methylation inhibitors.

Published

2017

10. Kernel-Based, Partial Least Squares Quantitative Structure-Retention Relationship Model for UPLC Retention Time Prediction: A Useful Tool for Metabolite Identification.

Author

Falchi F, Bertozzi SM, Ottonello G, Ruda GF, Colombano G, Fiorelli C, Martucci C, Bertorelli R, Scarpelli R, Cavalli A, Bandiera T, and Armirotti A

Subjects

Algorithms, Least-Squares Analysis, Principal Component Analysis, Chromatography, Liquid, Models, Chemical

Abstract

We propose a new QSRR model based on a Kernel-based partial least-squares method for predicting UPLC retention times in reversed phase mode. The model was built using a combination of classical (physicochemical and topological) and nonclassical (fingerprints) molecular descriptors of 1383 compounds, encompassing different chemical classes and structures and their accurately measured retention time values. Following a random splitting of the data set into a training and a test set, we tested the ability of the model to predict the retention time of all the compounds. The best predicted/experimental R 2 value was higher than 0.86, while the best Q 2 value we observed was close to 0.84. A comparison of our model with traditional and simpler MLR and PLS regression models shows that KPLS better performs in term of correlation (R 2 ), prediction (Q 2 ), and support to MetID peak assignment. The KPLS model succeeded in two real-life MetID tasks by correctly predicting elution order of Phase I metabolites, including isomeric monohydroxylated compounds. We also show in this paper that the model's predictive power can be extended to different gradient profiles, by simple mathematical extrapolation using a known equation, thus offering very broad flexibility. Moreover, the current study includes a deep investigation of different types of chemical descriptors used to build the structure-retention relationship.

Published

2016

11. 8-Substituted Pyrido[3,4-d]pyrimidin-4(3H)-one Derivatives As Potent, Cell Permeable, KDM4 (JMJD2) and KDM5 (JARID1) Histone Lysine Demethylase Inhibitors.

Author

Bavetsias V, Lanigan RM, Ruda GF, Atrash B, McLaughlin MG, Tumber A, Mok NY, Le Bihan YV, Dempster S, Boxall KJ, Jeganathan F, Hatch SB, Savitsky P, Velupillai S, Krojer T, England KS, Sejberg J, Thai C, Donovan A, Pal A, Scozzafava G, Bennett JM, Kawamura A, Johansson C, Szykowska A, Gileadi C, Burgess-Brown NA, von Delft F, Oppermann U, Walters Z, Shipley J, Raynaud FI, Westaway SM, Prinjha RK, Fedorov O, Burke R, Schofield CJ, Westwood IM, Bountra C, Müller S, van Montfort RL, Brennan PE, and Blagg J

Subjects

Caco-2 Cells, Cell Membrane Permeability, Enzyme Inhibitors pharmacokinetics, Humans, Jumonji Domain-Containing Histone Demethylases chemistry, Jumonji Domain-Containing Histone Demethylases metabolism, Nuclear Proteins chemistry, Nuclear Proteins metabolism, Pyrimidinones pharmacokinetics, Repressor Proteins chemistry, Repressor Proteins metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Jumonji Domain-Containing Histone Demethylases antagonists & inhibitors, Nuclear Proteins antagonists & inhibitors, Pyrimidinones chemistry, Pyrimidinones pharmacology, Repressor Proteins antagonists & inhibitors

Abstract

We report the discovery of N-substituted 4-(pyridin-2-yl)thiazole-2-amine derivatives and their subsequent optimization, guided by structure-based design, to give 8-(1H-pyrazol-3-yl)pyrido[3,4-d]pyrimidin-4(3H)-ones, a series of potent JmjC histone N-methyl lysine demethylase (KDM) inhibitors which bind to Fe(II) in the active site. Substitution from C4 of the pyrazole moiety allows access to the histone peptide substrate binding site; incorporation of a conformationally constrained 4-phenylpiperidine linker gives derivatives such as 54j and 54k which demonstrate equipotent activity versus the KDM4 (JMJD2) and KDM5 (JARID1) subfamily demethylases, selectivity over representative exemplars of the KDM2, KDM3, and KDM6 subfamilies, cellular permeability in the Caco-2 assay, and, for 54k, inhibition of H3K9Me3 and H3K4Me3 demethylation in a cell-based assay.

Published

2016

12. N-myristoyltransferase is a cell wall target in Aspergillus fumigatus.

Author

Fang W, Robinson DA, Raimi OG, Blair DE, Harrison JR, Lockhart DE, Torrie LS, Ruda GF, Wyatt PG, Gilbert IH, and van Aalten DM

Subjects

Acyltransferases chemistry, Acyltransferases metabolism, Aminopyridines chemistry, Aminopyridines pharmacology, Antifungal Agents chemistry, Aspergillus fumigatus enzymology, Aspergillus fumigatus genetics, Aspergillus fumigatus growth & development, Catalytic Domain, Cell Wall chemistry, Cell Wall enzymology, Crystallography, X-Ray, Fungal Proteins chemistry, Fungal Proteins genetics, Fungal Proteins metabolism, Kinetics, Microbial Sensitivity Tests, Protein Binding, Protein Structure, Secondary, Pyrazoles chemistry, Pyrazoles pharmacology, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Acyltransferases antagonists & inhibitors, Antifungal Agents pharmacology, Aspergillus fumigatus drug effects, Cell Wall drug effects, Fungal Proteins antagonists & inhibitors, Protein Processing, Post-Translational

Abstract

Treatment of filamentous fungal infections relies on a limited repertoire of antifungal agents. Compounds possessing novel modes of action are urgently required. N-myristoylation is a ubiquitous modification of eukaryotic proteins. The enzyme N-myristoyltransferase (NMT) has been considered a potential therapeutic target in protozoa and yeasts. Here, we show that the filamentous fungal pathogen Aspergillus fumigatus possesses an active NMT enzyme that is essential for survival. Surprisingly, partial repression of the gene revealed downstream effects of N-myristoylation on cell wall morphology. Screening a library of inhibitors led to the discovery of a pyrazole sulphonamide compound that inhibits the enzyme and is fungicidal under partially repressive nmt conditions. Together with a crystallographic complex showing the inhibitor binding in the peptide substrate pocket, we provide evidence of NMT being a potential drug target in A. fumigatus.

Published

2015

13. K2P channel gating mechanisms revealed by structures of TREK-2 and a complex with Prozac.

Author

Dong YY, Pike AC, Mackenzie A, McClenaghan C, Aryal P, Dong L, Quigley A, Grieben M, Goubin S, Mukhopadhyay S, Ruda GF, Clausen MV, Cao L, Brennan PE, Burgess-Brown NA, Sansom MS, Tucker SJ, and Carpenter EP

Subjects

Amino Acid Sequence, Arachidonic Acid pharmacology, Binding Sites, Crystallography, X-Ray, Fluoxetine analogs & derivatives, Fluoxetine chemistry, Fluoxetine metabolism, Fluoxetine pharmacology, Humans, Models, Molecular, Molecular Dynamics Simulation, Molecular Sequence Data, Potassium metabolism, Potassium Channels, Tandem Pore Domain antagonists & inhibitors, Potassium Channels, Tandem Pore Domain metabolism, Protein Conformation, Protein Folding, Protein Structure, Secondary, Protein Structure, Tertiary, Ion Channel Gating, Potassium Channels, Tandem Pore Domain chemistry

Abstract

TREK-2 (KCNK10/K2P10), a two-pore domain potassium (K2P) channel, is gated by multiple stimuli such as stretch, fatty acids, and pH and by several drugs. However, the mechanisms that control channel gating are unclear. Here we present crystal structures of the human TREK-2 channel (up to 3.4 angstrom resolution) in two conformations and in complex with norfluoxetine, the active metabolite of fluoxetine (Prozac) and a state-dependent blocker of TREK channels. Norfluoxetine binds within intramembrane fenestrations found in only one of these two conformations. Channel activation by arachidonic acid and mechanical stretch involves conversion between these states through movement of the pore-lining helices. These results provide an explanation for TREK channel mechanosensitivity, regulation by diverse stimuli, and possible off-target effects of the serotonin reuptake inhibitor Prozac., (Copyright © 2015, American Association for the Advancement of Science.)

Published

2015

14. Development of 3-alkyl-6-methoxy-7-hydroxy-chromones (AMHCs) from natural isoflavones, a new class of fluorescent scaffolds for biological imaging.

Author

Miao J, Cui H, Jin J, Lai F, Wen H, Zhang X, Ruda GF, Chen X, and Yin D

Subjects

Animals, Hep G2 Cells, Humans, Mice, Solubility, Biological Products chemistry, Chromones chemistry, Fluorescent Dyes chemistry, Isoflavones chemistry, Optical Imaging methods

Abstract

Starting from 7-hydroxyisoflavones, we developed a new class of fluorescent scaffolds, 3-alkyl-6-methoxy-7-hydroxy-chromones (AMHCs, MW∼ 205.19, λab∼ 350 nm, λem∼ 450 nm) via a trial and error process. AMHCs have the advantages of being a small molecular moiety, having strong fluorescence in basic buffers, reasonable solubility and stability, non-toxicity, and are conveniently linked to pharmacophores. AMHCs were successfully used in fluorescence microscopy imaging of cells and tissues.

Published

2015

15. Applying a multitarget rational drug design strategy: the first set of modulators with potent and balanced activity toward dopamine D3 receptor and fatty acid amide hydrolase.

Author

De Simone A, Ruda GF, Albani C, Tarozzo G, Bandiera T, Piomelli D, Cavalli A, and Bottegoni G

Subjects

Amidohydrolases metabolism, Animals, Binding Sites, Dopamine Agonists chemistry, Dopamine Agonists metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Humans, Molecular Docking Simulation, Protein Binding, Protein Structure, Tertiary, Rats, Receptors, Dopamine D3 metabolism, Amidohydrolases antagonists & inhibitors, Drug Design, Receptors, Dopamine D3 agonists

Abstract

Combining computer-assisted drug design and synthetic efforts, we generated compounds with potent and balanced activities toward both D3 dopamine receptor and fatty acid amide hydrolase (FAAH) enzyme. By concurrently modulating these targets, our compounds hold great potential toward exerting a disease-modifying effect on nicotine addiction and other forms of compulsive behavior.

Published

2014

16. Synthesis and structure-activity relationship studies of O-biphenyl-3-yl carbamates as peripherally restricted fatty acid amide hydrolase inhibitors.

Author

Moreno-Sanz G, Duranti A, Melzig L, Fiorelli C, Ruda GF, Colombano G, Mestichelli P, Sanchini S, Tontini A, Mor M, Bandiera T, Scarpelli R, Tarzia G, and Piomelli D

Subjects

Animals, Carbamates pharmacology, Enzyme Inhibitors pharmacology, Male, Mice, Structure-Activity Relationship, Amidohydrolases antagonists & inhibitors, Carbamates chemical synthesis, Enzyme Inhibitors chemical synthesis

Abstract

The peripherally restricted fatty acid amide hydrolase (FAAH) inhibitor URB937 (3, cyclohexylcarbamic acid 3'-carbamoyl-6-hydroxybiphenyl-3-yl ester) is extruded from the brain and spinal cord by the Abcg2 efflux transporter. Despite its inability to enter the central nervous system (CNS), 3 exerts profound antinociceptive effects in mice and rats, which result from the inhibition of FAAH in peripheral tissues and the consequent enhancement of anandamide signaling at CB1 cannabinoid receptors localized on sensory nerve endings. In the present study, we examined the structure-activity relationships (SAR) for the biphenyl region of compound 3, focusing on the carbamoyl and hydroxyl groups in the distal and proximal phenyl rings. Our SAR studies generated a new series of peripherally restricted FAAH inhibitors and identified compound 35 (cyclohexylcarbamic acid 3'-carbamoyl-5-hydroxybiphenyl-3-yl ester) as the most potent brain-impermeant FAAH inhibitor disclosed to date.

Published

2013

17. Automated design of ligands to polypharmacological profiles.

Author

Besnard J, Ruda GF, Setola V, Abecassis K, Rodriguiz RM, Huang XP, Norval S, Sassano MF, Shin AI, Webster LA, Simeons FR, Stojanovski L, Prat A, Seidah NG, Constam DB, Bickerton GR, Read KD, Wetsel WC, Gilbert IH, Roth BL, and Hopkins AL

Subjects

Animals, Automation, Drug Delivery Systems, Female, Male, Mice, Mice, Inbred C57BL, Models, Theoretical, Pharmacological Phenomena, Reproducibility of Results, Drug Design, Ligands

Abstract

The clinical efficacy and safety of a drug is determined by its activity profile across many proteins in the proteome. However, designing drugs with a specific multi-target profile is both complex and difficult. Therefore methods to design drugs rationally a priori against profiles of several proteins would have immense value in drug discovery. Here we describe a new approach for the automated design of ligands against profiles of multiple drug targets. The method is demonstrated by the evolution of an approved acetylcholinesterase inhibitor drug into brain-penetrable ligands with either specific polypharmacology or exquisite selectivity profiles for G-protein-coupled receptors. Overall, 800 ligand-target predictions of prospectively designed ligands were tested experimentally, of which 75% were confirmed to be correct. We also demonstrate target engagement in vivo. The approach can be a useful source of drug leads when multi-target profiles are required to achieve either selectivity over other drug targets or a desired polypharmacology.

Published

2012

18. Site-directed mutagenesis provides insights into the selective binding of trityl derivatives to Plasmodium falciparum dUTPase.

Author

Recio E, Musso-Buendía A, Vidal AE, Ruda GF, Kasinathan G, Nguyen C, Ruiz-Pérez LM, Gilbert IH, and González-Pacanowska D

Subjects

Amino Acid Sequence, Antimalarials chemistry, Antimalarials pharmacology, Binding Sites drug effects, Cloning, Molecular, Deoxyuridine metabolism, Drug Design, Escherichia coli, Humans, Kinetics, Lysine metabolism, Malaria, Falciparum enzymology, Malaria, Falciparum parasitology, Molecular Sequence Data, Mutagenesis, Site-Directed, Mutation, Phenylalanine metabolism, Plasmodium falciparum chemistry, Plasmodium falciparum genetics, Protein Binding drug effects, Pyrophosphatases chemistry, Pyrophosphatases genetics, Pyrophosphatases metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Sequence Alignment, Structure-Activity Relationship, Substrate Specificity, Trityl Compounds pharmacology, Lysine chemistry, Phenylalanine chemistry, Plasmodium falciparum enzymology, Pyrophosphatases antagonists & inhibitors, Recombinant Proteins metabolism, Trityl Compounds chemistry

Abstract

We have previously identified a series of triphenylmethane derivatives of deoxyuridine with antimalarial activity in vitro which selectively inhibit Plasmodium falciparum deoxyuridine triphosphate nucleotidohydrolase (PfdUTPase) compared to the human enzyme. The crystal structure of PfdUTPase in complex with one of these inhibitors suggested that the triphenylmethane derivative was selective due to a series of interactions between the trityl group and the side chains of residues Phe(46), Ile(117) and Lys(96) located in a hydrophobic pocket distinct from the phosphate binding site. Here we show by site-directed mutagenesis that the hydrophobic nature of the trityl binding site and in particular aromatic interactions established between the inhibitor and residue Phe(46) contribute significantly to the binding of uracil-based derivatives containing trityl groups in the 5'-position. Thus, changing Phe(46) for alanine resulted in increased K(i) values for all compounds tested. Conversely, substitution of the polar residue Lys(96) for Ala results in smaller K(i) values and an increase in selectivity with regard to human dUTPase. This information will aid in the design of inhibitors with improved activity against the Plasmodium enzyme., (Copyright © 2011 Elsevier Masson SAS. All rights reserved.)

Published

2011

19. Modified 5'-trityl nucleosides as inhibitors of Plasmodium falciparum dUTPase.

Author

Ruda GF, Nguyen C, Ziemkowski P, Felczak K, Kasinathan G, Musso-Buendia A, Sund C, Zhou XX, Kaiser M, Ruiz-Pérez LM, Brun R, Kulikowski T, Johansson NG, González-Pacanowska D, and Gilbert IH

Subjects

Animals, Enzyme Inhibitors chemistry, Nucleosides chemistry, Structure-Activity Relationship, Enzyme Inhibitors pharmacology, Nucleosides pharmacology, Plasmodium falciparum enzymology, Pyrophosphatases antagonists & inhibitors

Abstract

2'-Deoxyuridine triphosphate nucleotidohydrolase (dUTPase) is a potential drug target for the treatment of malaria. We previously reported the discovery of 5'-tritylated analogues of deoxyuridine as selective inhibitors of this Plasmodium falciparum enzyme. Herein we report further structure-activity studies; in particular, variations of the 5'-trityl group, the introduction of various substituents at the 3'-position of deoxyuridine, and modifications of the base. Compounds were tested against both the enzyme and the parasite. Variations of the 5'-trityl group and of the 3'-substituent were well tolerated and yielded active compounds. However, there is a clear requirement for the uracil base for activity, because modifications of the uracil ring result in loss of enzyme inhibition and significant decreases in antiplasmodial action., (Copyright © 2011 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2011

20. Exploring new inhibitors of Plasmodium falciparum purine nucleoside phosphorylase.

Author

Cui H, Ruda GF, Carrero-Lérida J, Ruiz-Pérez LM, Gilbert IH, and González-Pacanowska D

Subjects

Animals, Chromatography, Liquid, Enzyme Inhibitors chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Spectrometry, Mass, Electrospray Ionization, Enzyme Inhibitors pharmacology, Plasmodium falciparum enzymology, Purine-Nucleoside Phosphorylase antagonists & inhibitors

Abstract

Plasmodium falciparum purine nucleoside phosphorylase (PfPNP) has a central role in purine salvage and inhibitors of the enzyme have been shown to have antiplasmodial activity. The enzyme preferentially uses inosine as substrate (K(m)=5 μM, k(cat)/K(m)=7.4×10(4) M(-1) s(-1)), but can also use uridine, albeit less efficiently (K(m)=85 μM, k(cat)/K(m)=306 M(-1) s(-1)). In an effort to identify new PfPNP inhibitors, two series of compounds were prepared. Series 1 was based on known human uridine phosphorylase inhibitors whilst series 2 was uracil equivalents of purine-based PNP transition state inhibitors. These two series of compounds were assayed for inhibition of both PfPNP activity and growth of P. falciparum. The transition state analogues were found to be moderate inhibitors of PfPNP (most potent compound, K(i)=6 μM)., (Copyright © 2010 Elsevier Masson SAS. All rights reserved.)

Published

2010

21. Aryl phosphoramidates of 5-phospho erythronohydroxamic acid, a new class of potent trypanocidal compounds.

Author

Ruda GF, Wong PE, Alibu VP, Norval S, Read KD, Barrett MP, and Gilbert IH

Subjects

Animals, Blood, Buffers, Drug Stability, Humans, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, In Vitro Techniques, Mice, Microsomes, Liver metabolism, Organophosphorus Compounds chemistry, Organophosphorus Compounds pharmacology, Prodrugs chemistry, Prodrugs metabolism, Structure-Activity Relationship, Trypanocidal Agents chemistry, Trypanocidal Agents pharmacology, Trypanosoma brucei brucei drug effects, Hydroxamic Acids chemical synthesis, Organophosphorus Compounds chemical synthesis, Prodrugs chemical synthesis, Trypanocidal Agents chemical synthesis

Abstract

RNAi and enzymatic studies have shown the importance of 6-phosphogluconate dehydrogenase (6-PGDH) in Trypanosoma brucei for the parasite survival and make it an attractive drug target for the development of new treatments against human African trypanosomiasis. 2,3-O-Isopropylidene-4-erythrono hydroxamate is a potent inhibitor of parasite Trypanosoma brucei 6-phosphogluconate dehydrogenase (6-PGDH), the third enzyme of the pentose phosphate pathway. However, this compound does not have trypanocidal activity due to its poor membrane permeability. Consequently, we have previously reported a prodrug approach to improve the antiparasitic activity of this inhibitor by converting the phosphate group into a less charged phosphate prodrug. The activity of prodrugs appeared to be dependent on their stability in phosphate buffer. Here we have successfully further extended the development of the aryl phosphoramidate prodrugs of 2,3-O-isopropylidene-4-erythrono hydroxamate by synthesizing a small library of phosphoramidates and evaluating their biological activity and stability in a variety of assays. Some of the compounds showed high trypanocidal activity and good correlation of activity with their stability in fresh mouse blood.

Published

2010

22. Virtual fragment screening for novel inhibitors of 6-phosphogluconate dehydrogenase.

Author

Ruda GF, Campbell G, Alibu VP, Barrett MP, Brenk R, and Gilbert IH

Subjects

Drug Design, Humans, Models, Molecular, Phosphogluconate Dehydrogenase chemistry, Protein Binding, Structure-Activity Relationship, Trypanosomiasis, African drug therapy, Phosphogluconate Dehydrogenase antagonists & inhibitors, Phosphogluconate Dehydrogenase metabolism, Trypanocidal Agents chemistry, Trypanocidal Agents pharmacology, Trypanosoma brucei brucei enzymology

Abstract

The enzyme 6-phosphogluconate dehydrogenase is a potential drug target for the parasitic protozoan Trypanosoma brucei, the causative organism of human African trypanosomiasis. This enzyme has a polar active site to accommodate the phosphate, hydroxyl and carboxylate groups of the substrate, 6-phosphogluconate. A virtual fragment screen was undertaken of the enzyme to discover starting points for the development of inhibitors which are likely to have appropriate physicochemical properties for an orally bioavailable compound. A virtual screening library was developed, consisting of compounds with functional groups that could mimic the phosphate group of the substrate, but which have a higher pKa. Following docking, hits were clustered and appropriate compounds purchased and assayed against the enzyme. Three fragments were identified that had IC50 values in the low micromolar range and good ligand efficiencies. Based on these initial hits, analogues were procured and further active compounds were identified. Some of the fragments identified represent potential starting points for a medicinal chemistry programme to develop potent drug-like inhibitors of the enzyme., (Copyright (c) 2010 Elsevier Ltd. All rights reserved.)

Published

2010

23. Synthesis and biological evaluation of phosphate prodrugs of 4-phospho-D-erythronohydroxamic acid, an inhibitor of 6-phosphogluconate dehydrogenase.

Author

Ruda GF, Alibu VP, Mitsos C, Bidet O, Kaiser M, Brun R, Barrett MP, and Gilbert IH

Subjects

Animals, Enzyme Inhibitors pharmacology, Hydroxamic Acids pharmacology, Phosphogluconate Dehydrogenase antagonists & inhibitors, Prodrugs chemical synthesis, Prodrugs pharmacology, Sugar Phosphates pharmacology, Trypanosoma brucei brucei drug effects

Abstract

We have previously reported the discovery of potent and selective inhibitors of 6-phosphogluconate dehydrogenase, the third enzyme of the phosphate pentose pathway, from Trypanosoma brucei, the causative organism of human African trypanosomiasis. These inhibitors were charged phosphate derivatives with restricted capacity to enter cells. Herein, we report the synthesis of five different classes of prodrugs: phosphoramidate; bis-S-acyl thioethyl esters (bis-SATE); bis-pivaloxymethyl (bis-POM); CycloSaligenyl; and phenyl, S-acyl thioethyl mixed phosphate esters (mix-SATE). Prodrugs were studied for stability and activity against the intact parasites. Most prodrugs caused inhibition of the growth of the parasites. The activity of the prodrugs against the parasites appeared to be related to their stability in aqueous buffer.

Published

2007

24. Crystal structures of a bacterial 6-phosphogluconate dehydrogenase reveal aspects of specificity, mechanism and mode of inhibition by analogues of high-energy reaction intermediates.

Author

Sundaramoorthy R, Iulek J, Barrett MP, Bidet O, Ruda GF, Gilbert IH, and Hunter WN

Subjects

Amino Acid Sequence, Animals, Binding Sites, Catalysis, Coenzymes metabolism, Crystallography, X-Ray, Enzyme Inhibitors chemistry, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, Lactococcus lactis metabolism, Models, Molecular, Molecular Sequence Data, Phosphogluconate Dehydrogenase metabolism, Protein Conformation, Substrate Specificity, Sugar Phosphates chemistry, Trypanosoma brucei brucei metabolism, Lactococcus lactis enzymology, Phosphogluconate Dehydrogenase chemistry, Trypanosoma brucei brucei enzymology

Abstract

Crystal structures of recombinant Lactococcus lactis 6-phosphogluconate dehydrogenase (LlPDH) in complex with substrate, cofactor, product and inhibitors have been determined. LlPDH shares significant sequence identity with the enzymes from sheep liver and the protozoan parasite Trypanosoma brucei for which structures have been reported. Comparisons indicate that the key residues in the active site are highly conserved, as are the interactions with the cofactor and the product ribulose 5-phosphate. However, there are differences in the conformation of the substrate 6-phosphogluconate which may reflect distinct states relevant to catalysis. Analysis of the complex formed with the potent inhibitor 4-phospho-d-erythronohydroxamic acid, suggests that this molecule does indeed mimic the high-energy intermediate state that it was designed to. The analysis also identified, as a contaminant by-product of the inhibitor synthesis, 4-phospho-d-erythronamide, which binds in similar fashion. LlPDH can now serve as a model system for structure-based inhibitor design targeting the enzyme from Trypanosoma species.

Published

2007

25. Acyclic nucleoside analogues as inhibitors of Plasmodium falciparum dUTPase.

Author

Nguyen C, Ruda GF, Schipani A, Kasinathan G, Leal I, Musso-Buendia A, Kaiser M, Brun R, Ruiz-Pérez LM, Sahlberg BL, Johansson NG, Gonzalez-Pacanowska D, and Gilbert IH

Subjects

Animals, Antimalarials pharmacology, Erythrocytes drug effects, Erythrocytes parasitology, Humans, In Vitro Techniques, Models, Molecular, Nucleosides pharmacology, Plasmodium falciparum drug effects, Pyrophosphatases chemistry, Stereoisomerism, Structure-Activity Relationship, Trityl Compounds pharmacology, Uracil pharmacology, Antimalarials chemical synthesis, Nucleosides chemical synthesis, Plasmodium falciparum enzymology, Pyrophosphatases antagonists & inhibitors, Trityl Compounds chemical synthesis, Uracil analogs & derivatives, Uracil chemical synthesis

Abstract

We report the discovery of novel uracil-based acyclic compounds as inhibitors of deoxyuridine 5'-triphosphate nucleotidohydrolase (dUTPase), an enzyme involved in nucleotide metabolism that has been identified as a promising target for the development of antimalarial drugs. Compounds were assayed against both P.falciparum dUTPase and intact parasites. A good correlation was observed between enzyme inhibition and cellular assays. Acyclic uracil derivatives were identified that showed greater or similar potency and in general increased selectivity compared to previously reported inhibitors. The most active compound reported here against the P. falciparum enzyme had a K(i) of 0.2 microM. Molecular modeling studies provided a good rationale for the observed activities. Preliminary ADME studies indicated that some of the lead compounds are drug-like molecules. These compounds are useful tools for further investigating P. falciparum dUTPase for the development of much-needed novel antimalarial drugs.

Published

2006