Your search keyword '"MacDonald SJ"' showing total 12 results

1. Rational Design of Autotaxin Inhibitors by Structural Evolution of Endogenous Modulators.

Author

Keune WJ, Potjewyd F, Heidebrecht T, Salgado-Polo F, Macdonald SJ, Chelvarajan L, Abdel Latif A, Soman S, Morris AJ, Watson AJ, Jamieson C, and Perrakis A

Subjects

Allosteric Regulation, Carbon-13 Magnetic Resonance Spectroscopy, Crystallization, Mass Spectrometry, Molecular Structure, Proton Magnetic Resonance Spectroscopy, Phosphoric Diester Hydrolases drug effects

Abstract

Autotaxin produces the bioactive lipid lysophosphatidic acid (LPA) and is a drug target of considerable interest for numerous pathologies. We report the expedient, structure-guided evolution of weak physiological allosteric inhibitors (bile salts) into potent competitive Autotaxin inhibitors that do not interact with the catalytic site. Functional data confirms that our lead compound attenuates LPA mediated signaling in cells and reduces LPA synthesis in vivo, providing a promising natural product derived scaffold for drug discovery.

Published

2017

2. Design and Elaboration of a Tractable Tricyclic Scaffold To Synthesize Druglike Inhibitors of Dipeptidyl Peptidase-4 (DPP-4), Antagonists of the C-C Chemokine Receptor Type 5 (CCR5), and Highly Potent and Selective Phosphoinositol-3 Kinase δ (PI3Kδ) Inhibitors.

Author

Schwehm C, Kellam B, Garces AE, Hill SJ, Kindon ND, Bradshaw TD, Li J, Macdonald SJ, Rowedder JE, Stoddart LA, and Stocks MJ

Subjects

Class Ia Phosphatidylinositol 3-Kinase metabolism, Dipeptidyl Peptidase 4 metabolism, Drug Design, Humans, Molecular Docking Simulation, Protein Subunits antagonists & inhibitors, Protein Subunits metabolism, Receptors, CCR5 metabolism, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, CCR5 Receptor Antagonists chemistry, CCR5 Receptor Antagonists pharmacology, Dipeptidyl-Peptidase IV Inhibitors chemistry, Dipeptidyl-Peptidase IV Inhibitors pharmacology, Phosphoinositide-3 Kinase Inhibitors, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology

Abstract

A novel molecular scaffold has been synthesized, and its incorporation into new analogues of biologically active molecules across multiple target classes will be discussed. In these studies, we have shown use of the tricyclic scaffold to synthesize potent inhibitors of the serine peptidase DPP-4, antagonists of the CCR5 receptor, and highly potent and selective PI3K δ isoform inhibitors. We also describe the predicted physicochemical properties of the resulting inhibitors and conclude that the tractable molecular scaffold could have potential application in future drug discovery programs.

Published

2017

3. Structure-Activity Relationships of Small Molecule Autotaxin Inhibitors with a Discrete Binding Mode.

Author

Miller LM, Keune WJ, Castagna D, Young LC, Duffy EL, Potjewyd F, Salgado-Polo F, Engel García P, Semaan D, Pritchard JM, Perrakis A, Macdonald SJ, Jamieson C, and Watson AJ

Subjects

Binding Sites, Crystallography, X-Ray, Indoles chemical synthesis, Kinetics, Models, Chemical, Molecular Docking Simulation, Phosphodiesterase Inhibitors chemical synthesis, Picolinic Acids chemical synthesis, Structure-Activity Relationship, Indoles chemistry, Phosphodiesterase Inhibitors chemistry, Phosphoric Diester Hydrolases chemistry, Picolinic Acids chemistry

Abstract

Autotaxin (ATX) is a secreted enzyme responsible for the hydrolysis of lysophosphatidylcholine (LPC) to the bioactive lysophosphatidic acid (LPA) and choline. The ATX-LPA signaling pathway is implicated in cell survival, migration, and proliferation; thus, the inhibition of ATX is a recognized therapeutic target for a number of diseases including fibrotic diseases, cancer, and inflammation, among others. Many of the developed synthetic inhibitors for ATX have resembled the lipid chemotype of the native ligand; however, a small number of inhibitors have been described that deviate from this common scaffold. Herein, we report the structure-activity relationships (SAR) of a previously reported small molecule ATX inhibitor. We show through enzyme kinetics studies that analogues of this chemotype are noncompetitive inhibitors, and by using a crystal structure with ATX we confirm the discrete binding mode.

Published

2017

4. Development of Autotaxin Inhibitors: An Overview of the Patent and Primary Literature.

Author

Castagna D, Budd DC, Macdonald SJ, Jamieson C, and Watson AJ

Subjects

Benzoxazoles chemistry, Boronic Acids chemistry, Enzyme Inhibitors chemistry, Humans, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Benzoxazoles pharmacology, Boronic Acids pharmacology, Enzyme Inhibitors pharmacology, Phosphoric Diester Hydrolases metabolism

Abstract

The autotaxin-lysophophatidic acid (ATX-LPA) signaling pathway is implicated in a variety of human disease states including angiogenesis, autoimmune diseases, cancer, fibrotic diseases, inflammation, neurodegeneration, and neuropathic pain, among others. As a result, ATX-LPA has become of significant interest within both the industrial and the academic communities. This review aims to provide a concise overview of the development of novel ATX inhibitors, including the disclosure of the first ATX clinical trial data.

Published

2016

5. Physicochemical descriptors of aromatic character and their use in drug discovery.

Author

Ritchie TJ and Macdonald SJ

Subjects

Chemistry, Pharmaceutical trends, Drug Discovery trends, Forecasting, Molecular Structure, Reproducibility of Results, Chemistry, Pharmaceutical methods, Drug Discovery methods, Hydrocarbons, Aromatic chemistry, Pharmaceutical Preparations chemistry, Terminology as Topic

Abstract

Published physicochemical descriptors of molecules that convey aromaticity-related character are reviewed in the context of drug design and discovery. Studies that have employed aromatic descriptors are discussed, and several descriptors are compared and contrasted.

Published

2014

6. Nonsteroidal glucocorticoid agonists: tetrahydronaphthalenes with alternative steroidal A-ring mimetics possessing dissociated (transrepression/transactivation) efficacy selectivity.

Author

Biggadike K, Boudjelal M, Clackers M, Coe DM, Demaine DA, Hardy GW, Humphreys D, Inglis GG, Johnston MJ, Jones HT, House D, Loiseau R, Needham D, Skone PA, Uings I, Veitch G, Weingarten GG, McLay IM, and Macdonald SJ

Subjects

Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Binding Sites, Cell Line, Drug Partial Agonism, Humans, Mammary Tumor Virus, Mouse genetics, Models, Molecular, Molecular Mimicry, NF-kappa B genetics, Receptors, Glucocorticoid antagonists & inhibitors, Stereoisomerism, Structure-Activity Relationship, Tetrahydronaphthalenes chemistry, Tetrahydronaphthalenes pharmacology, Transcription, Genetic drug effects, Transcriptional Activation drug effects, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Receptors, Glucocorticoid agonists, Tetrahydronaphthalenes chemical synthesis

Abstract

The synthesis and biological activity of tetrahydronaphthalene derivatives coupled to various heterocycles are described. These compounds are potent glucocorticoid receptor agonists with efficacy selectivity in an NFkappaB glucocorticoid receptor (GR) agonist assay (representing transrepression effects) over an MMTV GR agonist assay (representing transactivation effects). Quinolones, indoles, and C- and N-linked quinolines are some of the heterocycles that provide efficacy selectivity. For example, the isoquinoline 49D1E2 has NFkappaB agonism with pIC50 of 8.66 (89%) and reduced efficacy in MMTV agonism (6%), and the quinoline 55D1E1 has NFkappaB agonism with pIC50 of 9.30 (101%) and reduced efficacy in MMTV agonism with pEC50 of 8.02 (47%). A description of how a compound from each class is modeled in the active site of the receptor is given.

Published

2007

7. Dissociated nonsteroidal glucocorticoid receptor modulators; discovery of the agonist trigger in a tetrahydronaphthalene-benzoxazine series.

Author

Barker M, Clackers M, Copley R, Demaine DA, Humphreys D, Inglis GG, Johnston MJ, Jones HT, Haase MV, House D, Loiseau R, Nisbet L, Pacquet F, Skone PA, Shanahan SE, Tape D, Vinader VM, Washington M, Uings I, Upton R, McLay IM, and Macdonald SJ

Subjects

Administration, Topical, Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Benzoxazines chemistry, Benzoxazines pharmacology, Binding, Competitive, Cell Line, Dexamethasone pharmacology, Humans, Hypersensitivity, Delayed drug therapy, Mice, Models, Molecular, Radioligand Assay, Receptors, Glucocorticoid antagonists & inhibitors, Receptors, Glucocorticoid genetics, Stereoisomerism, Structure-Activity Relationship, Tetrahydronaphthalenes chemistry, Tetrahydronaphthalenes pharmacology, Transcription, Genetic drug effects, Transcriptional Activation drug effects, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Benzoxazines chemical synthesis, Receptors, Glucocorticoid agonists, Tetrahydronaphthalenes chemical synthesis

Abstract

The tetrahydronaphthalene-benzoxazine glucocorticoid receptor (GR) partial agonist 4b was optimized to produce potent full agonists of GR. Aromatic ring substitution of the tetrahydronaphthalene leads to weak GR antagonists. Discovery of an "agonist trigger" substituent on the saturated ring of the tetrahydronaphthalene leads to increased potency and efficacious GR agonism. These compounds are efficacy selective in an NFkB GR agonist assay (representing transrepression effects) over an MMTV GR agonist assay (representing transactivation effects). 52 and 60 have NFkB pIC(50) = 8.92 (105%) and 8.69 (92%) and MMTV pEC(50) = 8.20 (47%) and 7.75 (39%), respectively. The impact of the trigger substituent on agonism is modeled within GR and discussed. 36, 52, and 60 have anti-inflammatory activity in a mouse model of inflammation after topical dosing with 52 and 60, having an effect similar to that of dexamethasone. The original lead was discovered by a manual agreement docking method, and automation of this method is also described.

Published

2006

8. Design and synthesis of new nonsteroidal glucocorticoid modulators through application of an "agreement docking" method.

Author

Barker M, Clackers M, Demaine DA, Humphreys D, Johnston MJ, Jones HT, Pacquet F, Pritchard JM, Salter M, Shanahan SE, Skone PA, Vinader VM, Uings I, McLay IM, and Macdonald SJ

Subjects

Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Cell Line, Cell Line, Tumor, Humans, Ligands, Mice, Models, Molecular, Stereoisomerism, Structure-Activity Relationship, Tetrahydronaphthalenes chemistry, Tetrahydronaphthalenes pharmacology, Transcription, Genetic drug effects, Transcriptional Activation drug effects, Anti-Inflammatory Agents chemical synthesis, Receptors, Glucocorticoid agonists, Receptors, Glucocorticoid antagonists & inhibitors, Receptors, Glucocorticoid chemistry, Tetrahydronaphthalenes chemical synthesis

Abstract

Structurally related glucocorticoid receptor (GR) binders were docked into the GR active site to select the binding mode closest to the true docking mode. This process, termed an "agreement docking method", led to the design of tetrahydronaphthalene 9. The method was validated by the syntheses of 9 and related analogues, which are potent binders of GR. 15a is a partial agonist while 9e and 15a are micromolar antagonists in a mouse mammary tumor virus transactivation assay.

Published

2005

9. Dimeric zanamivir conjugates with various linking groups are potent, long-lasting inhibitors of influenza neuraminidase including H5N1 avian influenza.

Author

Macdonald SJ, Cameron R, Demaine DA, Fenton RJ, Foster G, Gower D, Hamblin JN, Hamilton S, Hart GJ, Hill AP, Inglis GG, Jin B, Jones HT, McConnell DB, McKimm-Breschkin J, Mills G, Nguyen V, Owens IJ, Parry N, Shanahan SE, Smith D, Watson KG, Wu WY, and Tucker SP

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Antiviral Agents pharmacology, Cell Line, Crystallization, Dimerization, Guanidines, Influenza A virus enzymology, Influenza B virus enzymology, Lung drug effects, Lung enzymology, Lung virology, Male, Membranes, Artificial, Mice, Models, Molecular, Molecular Weight, Orthomyxoviridae Infections virology, Pyrans, Rats, Rats, Sprague-Dawley, Sialic Acids pharmacokinetics, Sialic Acids pharmacology, Stereoisomerism, Viral Plaque Assay, Zanamivir, Antiviral Agents chemical synthesis, Influenza A Virus, H5N1 Subtype, Influenza A virus drug effects, Influenza B virus drug effects, Neuraminidase antagonists & inhibitors, Orthomyxoviridae Infections prevention & control, Sialic Acids chemical synthesis, Sialic Acids chemistry

Abstract

The synthesis, antiviral and pharmacokinetic properties of zanamivir (ZMV) dimers 8 and 13 are described. The compounds are highly potent neuraminidase (NA) inhibitors which, along with dimer 3, are being investigated as potential second generation inhaled therapies both for the treatment of influenza and for prophylactic use. They show outstanding activity in a 1 week mouse influenza prophylaxis assay, and compared with ZMV, high concentrations of 8 and 13 are found in rat lung tissue after 1 week. Retention of compounds in rat lung tissue correlated both with molecular weight (excluding 3 and 15) and with a capacity factor K' derived from immobilized artificial membrane (IAM) chromatography (including 3 and 15). Pharmacokinetic parameters for 3, 8 and 13 in rats show the compounds have short to moderate plasma half-lives, low clearances and low volumes of distribution. Dimer 3 shows NA inhibitory activity against N1 viruses including the recent highly pathogenic H5N1 A/Chicken/Vietnam/8/2004. In plaque reduction assays, 3, 8 and 13 show good to outstanding potency against a panel of nine flu A and B virus strains. Consistent with its shorter and more rigid linking group, dimer 8 has been successfully crystallized.

Published

2005

10. Discovery of further pyrrolidine trans-lactams as inhibitors of human neutrophil elastase (HNE) with potential as development candidates and the crystal structure of HNE complexed with an inhibitor (GW475151).

Author

Macdonald SJ, Dowle MD, Harrison LA, Clarke GD, Inglis GG, Johnson MR, Shah P, Smith RA, Amour A, Fleetwood G, Humphreys DC, Molloy CR, Dixon M, Godward RE, Wonacott AJ, Singh OM, Hodgson ST, and Hardy GW

Subjects

Animals, Combinatorial Chemistry Techniques, Crystallography, X-Ray, Dogs, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors pharmacology, Humans, Lactams pharmacokinetics, Lactams pharmacology, Leukocyte Elastase blood, Leukocyte Elastase chemistry, Male, Models, Molecular, Molecular Structure, Pyrroles pharmacokinetics, Pyrroles pharmacology, Pyrrolidines pharmacokinetics, Pyrrolidines pharmacology, Rats, Stereoisomerism, Structure-Activity Relationship, Sulfonamides pharmacokinetics, Sulfonamides pharmacology, Swine, Enzyme Inhibitors chemical synthesis, Lactams chemical synthesis, Leukocyte Elastase antagonists & inhibitors, Pyrroles chemical synthesis, Pyrrolidines chemical synthesis, Sulfonamides chemical synthesis

Abstract

Described herein is a modern approach to the rapid preparation and evaluation of compounds as potential back-up drug candidates. GW311616A, 1, a derivative of pyrrolidine trans-lactams, has previously been described as a potent, orally active inhibitor of human neutrophil elastase (HNE) for the treatment of respiratory disease. These properties made it a suitable candidate for development. Described here is the discovery of three further derivatives of pyrrolidine trans-lactams, which fulfill the criteria required for back-up candidates 28, 29, and 32. These include increased activity in inhibiting HNE in human whole blood (HWB) and comparable pharmacokinetic properties, in particular clearance, in two species. To provide a rapid assessment of clearance, cassette dosing in dog was used. Modern array techniques, including the synthesis of mixtures, were used to synthesize compounds rapidly. Having selected three potential compounds as back-up candidates, they were prepared as single enantiomers and profiled in in vitro and in vivo assays and evaluated pharmacokinetically in rat and dog. These compounds are highly potent and selective HNE inhibitors, with a prolonged pharmacodynamic action. Pharmacokinetically, these compounds are comparable with 1 while they are more potent in HWB. Compound 28, however, has a higher clearance. One of these compounds, 32, was cocrystallized with HNE, and features of this structure are described and compared with the cocrystal structure of 1 in porcine pancreatic elastase.

Published

2002

11. Acylating agents as enzyme inhibitors and understanding their reactivity for drug design.

Author

Sykes NO, Macdonald SJ, and Page MI

Subjects

Acylation, Drug Design, Hydrolysis, Kinetics, Pancreatic Elastase antagonists & inhibitors, Propanols chemistry, Spectrophotometry, Ultraviolet, Structure-Activity Relationship, Thermodynamics, Trifluoroethanol chemistry, Water, Bridged Bicyclo Compounds, Heterocyclic chemistry, Lactams chemistry, Lactones chemistry, Pancreatic Elastase chemistry, Serine Proteinase Inhibitors chemistry

Abstract

A series of bicyclic trans-fused gamma-lactones and gamma-lactams have been previously described for the inhibition of human neutrophil elastase and as possible development candidates. During the discovery program, it had been assumed that their acylating power was due in part to the inherent strain energy in the bicyclic structure that was released upon ring opening. This is now shown not to be the case, and in fact, these compounds are no more reactive than simple but analogous gamma-lactams and gamma-lactones. The strain energy is not released in the transition state for alkaline hydrolysis or alcoholysis because the reaction proceeds with rate-limiting formation of the tetrahedral intermediate. A reactivity index of k(OH) is proposed as a simple guide to determine the usefulness of a potential inhibitor as an enzyme acylating agent.

Published

2002

12. Syntheses of trans-5-oxo-hexahydro-pyrrolo[3,2-b]pyrroles and trans-5-oxo-hexahydro-furo[3,2-b]pyrroles (pyrrolidine trans-lactams and trans-lactones): new pharmacophores for elastase inhibition.

Author

Macdonald SJ, Belton DJ, Buckley DM, Spooner JE, Anson MS, Harrison LA, Mills K, Upton RJ, Dowle MD, Smith RA, Molloy CR, and Risley C

Subjects

Azetidines pharmacology, Humans, Lactams pharmacology, Lactones pharmacology, Piperazines pharmacology, Serine Proteinase Inhibitors pharmacology, Structure-Activity Relationship, Lactams chemical synthesis, Lactones chemical synthesis, Leukocyte Elastase antagonists & inhibitors, Neutrophils enzymology, Serine Proteinase Inhibitors chemical synthesis

Published

1998