Your search keyword '"Hugh J. Herdon"' showing total 31 results

1. Acylglycinamides as inhibitors of glycine transporter type 1

Author

Laurie J. Gordon, Gemma V. Puckey, Wyman Paul Adrian, David John Nash, Richard Blunt, Hugh J. Herdon, Simon Teague, Victoria Hadden, Stefano Fontana, Amanda Johns, and Roderick A. Porter

Subjects

Stereochemistry, Clinical Biochemistry, Glycine, Pharmaceutical Science, Glycine Plasma Membrane Transport Proteins, Biochemistry, Glycine transporter, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Structure–activity relationship, Solubility, Molecular Biology, Chemistry, Organic Chemistry, Combinatorial chemistry, Rats, Bioavailability, Lipophilicity, Molecular Medicine, Selectivity

Abstract

A screening hit was used as the basis for the core structure of a new series of acylglycinamide GlyT-1 inhibitors. Investigation of the SAR around four areas of diversity used facile chemistry to prepare compounds quickly. By focussing on reducing the lipophilicity and improving the aqueous solubility in the series we were able to prepare a compound (17e) with a good level of activity at GlyT-1, selectivity over GlyT-2 and moderate oral bioavailability.

Published

2011

2. Identification and evaluation of [11C]GSK931145 as a novel ligand for imaging the type 1 glycine transporter with positron emission tomography

Author

Roderick A. Porter, Cristian Salinas, Marc Laruelle, Hélène Audrain, Gabriella Gentile, Steen Jakobsen, Jan Passchier, Roger N. Gunn, and Hugh J. Herdon

Subjects

Pathology, medicine.medical_specialty, Time Factors, Swine, Kinetics, Ligands, Glycine transporter, Cellular and Molecular Neuroscience, Glycine Plasma Membrane Transport Proteins, In vivo, medicine, Animals, Carbon Radioisotopes, Hydrocarbons, Iodinated, Mesylates, Dose-Response Relationship, Drug, medicine.diagnostic_test, Chemistry, Ligand, Brain, Penetration (firestop), Drug development, Positron emission tomography, Positron-Emission Tomography, Biophysics, NMDA receptor, Radiopharmaceuticals

Abstract

The type-1 glycine transporter (GlyT1) is an important target for the development of new medications for schizophrenia. A specific and selective positron emission tomography (PET) GlyT1 ligand would facilitate drug development studies to determine whether a drug reaches this target and help establish suitable doses for clinical trials. This article describes the evaluation of three candidate GlyT1 PET radioligands (GSK931145, GSK565710, and GSK991022) selected from a library of compounds based on favorable physicochemical and pharmacological properties. Each candidate was successfully labeled using [11C]methyl iodide or [11C]methyl triflate and administered to a pig pre- and postadministration with a pharmacological dose of a GlyT1 inhibitor to determine their suitability as PET ligands in the porcine brain in vivo. All three candidate ligands were analyzed quantitatively with compartment analyses employing a plasma input function. [11C]GSK931145 showed good brain penetration and a heterogeneous distribution in agreement with reported GlyT1 localization. Following pretreatment with GSK565710, uptake of [11C]GSK931145 was reduced to homogeneous levels. Although [11C]GSK565710 also showed good brain penetration and a heterogeneous distribution, the apparent level of specific binding was reduced compared to [11C]GSK931145. In contrast, [11C]GSK991022 showed a much lower brain penetration and resultant signal following pretreatment with GSK565710. Based on these findings [11C]GSK931145 was identified as the most promising ligand for imaging GlyT1 in the porcine brain, possessing good brain penetration, specific signal, and reversible kinetics. [11C]GSK931145 is now being progressed into higher species. Synapse 64:542–549, 2010. © 2010 Wiley-Liss, Inc.

Published

2010

3. Orthosteric and Allosteric Modes of Interaction of Novel Selective Agonists of the M1 Muscarinic Acetylcholine Receptor

Author

Vimesh Ashvinkumar Avlani, Patrick M. Sexton, Benjamin G. Tehan, Elizabeth Guida, Arthur Christopoulos, Christopher J. Langmead, Martyn D. Wood, Hugh J. Herdon, and Jeannette M. Watson

Subjects

Agonist, Allosteric modulator, Stereochemistry, medicine.drug_class, Allosteric regulation, CHO Cells, Muscarinic Agonists, Quinolones, Radioligand Assay, Cricetulus, Allosteric Regulation, Piperidines, Cricetinae, Muscarinic acetylcholine receptor, medicine, Animals, Humans, Phosphorylation, Receptor, Pharmacology, Chemistry, Receptor, Muscarinic M1, Cooperative binding, Molecular Pharmacology, Transmembrane domain, Mutagenesis, Site-Directed, Molecular Medicine

Abstract

Recent years have witnessed the discovery of novel selective agonists of the M(1) muscarinic acetylcholine (ACh) receptor (mAChR). One mechanism invoked to account for the selectivity of such agents is that they interact with allosteric sites. We investigated the molecular pharmacology of two such agonists, 1-[3-(4-butyl-1-piperidinyl)propyl]-3,4-dihydro-2(1H)-quinolinone (77-LH-28-1) and 4-n-butyl-1-[4-(2-methylphenyl)-4-oxo-1-butyl] piperidine hydrogen chloride (AC-42), at the wild-type M(1) mAChR and three mutant M(1) mAChRs. Both agonists inhibited the binding of the orthosteric antagonist [(3)H]N-methyl scopolamine ([(3)H]NMS) in a manner consistent with orthosteric competition or high negative cooperativity. Functional interaction studies between 77-LH-28-1 and ACh also indicated a competitive mechanism. Dissociation kinetics assays revealed that the agonists could bind allosterically when the orthosteric site was prelabeled with [(3)H]NMS and that 77-LH-28-1 competed with the prototypical allosteric modulator heptane-1,7-bis-[dimethyl-3'-phthalimidopropyl]-ammonium bromide under these conditions. Mutation of the key orthosteric site residues Y(381)A (transmembrane helix 6) and W(101)A (transmembrane helix 3) reduced the affinity of prototypical orthosteric agonists but increased the affinity of the novel agonists. Divergent effects were also noted on agonist signaling efficacies at these mutants. We identified a novel mutation, F(77)I (transmembrane helix 2), which selectively reduced the efficacy of the novel agonists in mediating intracellular Ca(2+) elevation and phosphorylation of extracellular signal regulated kinase 1/2. Molecular modeling suggested a possible "bitopic" binding mode, whereby the agonists extend down into the orthosteric site as well as up toward extracellular receptor regions associated with an allosteric site. It is possible that this bitopic mode may explain the pharmacology of other selective mAChR agonists.

Published

2010

4. Pharmacological stimulation of NMDA receptors via co-agonist site suppresses fMRI response to phencyclidine in the rat

Author

Adam J. Schwarz, Alessandro Gozzi, Giuliano Turrini, Hugh J. Herdon, Angelo Bifone, Simone Bertani, and Valerio Crestan

Subjects

Male, Agonist, Time Factors, medicine.drug_class, fMRI, Glycine, PCP, d-serine, Gly-T1, phMRI, SSR504734, CBV, Allosteric regulation, Phencyclidine, Endogeny, Neurotransmission, Receptors, N-Methyl-D-Aspartate, Rats, Sprague-Dawley, Piperidines, Glycine Plasma Membrane Transport Proteins, mental disorders, Serine, medicine, Animals, Receptor, Pharmacology, Binding Sites, Blood Volume, Dose-Response Relationship, Drug, Chemistry, musculoskeletal, neural, and ocular physiology, Brain, Models, Theoretical, Magnetic Resonance Imaging, Rats, nervous system, Benzamides, Injections, Intravenous, NMDA receptor, Neuroscience, Endogenous agonist, medicine.drug

Abstract

Increasing experimental evidence suggests that impaired N-methyl-D: -aspartic acid (NMDA) receptor (NMDAr) function could be a key pathophysiological determinant of schizophrenia. Agonists at the allosteric glycine (Gly) binding site of the NMDA complex can promote NMDAr activity, a strategy that could provide therapeutic efficacy for the disorder. NMDAr antagonists like phencyclidine (PCP) can induce psychotic and dissociative symptoms similar to those observed in schizophrenia and are therefore widely used experimentally to impair NMDA neurotransmission in vivo.In the present study, we used pharmacological magnetic resonance imaging (phMRI) to investigate the modulatory effects of endogenous and exogenous agonists at the NMDAr Gly site on the spatiotemporal patterns of brain activation induced by acute PCP challenge in the rat. The drugs investigated were D: -serine, an endogenous agonist of the NMDAr Gly site, and SSR504734, a potent Gly transporter type 1 (GlyT-1) inhibitor that can potentiate NMDAr function by increasing synaptic levels of Gly.Acute administration of PCP induced robust and sustained activation of discrete cortico-limbo-thalamic circuits. Pretreatment with D: -serine (1 g/kg) or SSR504734 (10 mg/kg) completely inhibited PCP-induced functional activation. This effect was accompanied by weak but sustained deactivation particularly in cortical areas.These findings suggest that agents that stimulate NMDAr via Gly co-agonist site can potentiate NMDAr activity in the living brain and corroborate the potential for this class of drugs to provide selective enhancement of NMDAr neurotransmission in schizophrenia.

Published

2008

5. Characterization of a CNS penetrant, selective M1muscarinic receptor agonist, 77-LH-28-1

Author

Ceri H. Davies, Adrianna Teriakidis, Anita K. Roopun, James N.C. Kew, Andrew D. Randall, Zining Wu, Hugh J. Herdon, Jon T. Brown, Ross Jeggo, Nisha Patel, Ian Thomson Forbes, Clive Leslie Branch, Gareth A. Jones, Miles A. Whittington, Victoria Anne Honey Fry, Nigel E. Austin, Martyn D. Wood, Rosemary A. Melarange, Katherine A. Buchanan, Joanne Pardoe, Christopher J. Langmead, Claire Roberts, Kathryn R. Starr, Angelica Mazzali, Jeannette M. Watson, and Jim J. Hagan

Subjects

Pharmacology, Agonist, chemistry.chemical_classification, medicine.drug_class, Allosteric regulation, 77-LH-28-1, Muscarinic acetylcholine receptor M1, Biology, chemistry.chemical_compound, chemistry, In vivo, Muscarinic acetylcholine receptor, medicine, Inositol phosphate, Acetylcholine receptor

Abstract

Background and purpose: M1 muscarinic ACh receptors (mAChRs) represent an attractive drug target for the treatment of cognitive deficits associated with diseases such as Alzheimer's disease and schizophrenia. However, the discovery of subtype-selective mAChR agonists has been hampered by the high degree of conservation of the orthosteric ACh-binding site among mAChR subtypes. The advent of functional screening assays has enabled the identification of agonists such as AC-42 (4-n-butyl-1-[4-(2-methylphenyl)-4-oxo-1-butyl]-piperidine), which bind to an allosteric site and selectively activate the M1 mAChR subtype. However, studies with this compound have been limited to recombinantly expressed mAChRs. Experimental approach: In this study, we have compared the pharmacological profile of AC-42 and a close structural analogue, 77-LH-28-1 (1-[3-(4-butyl-1-piperidinyl)propyl]-3,4-dihydro-2(1H)-quinolinone) at human recombinant, and rat native, mAChRs by calcium mobilization, inositol phosphate accumulation and both in vitro and in vivo electrophysiology. Key results: Calcium mobilization and inositol phosphate accumulation assays revealed that both AC-42 and 77-LH-28-1 display high selectivity to activate the M1 mAChR over other mAChR subtypes. Furthermore, 77-LH-28-1, but not AC-42, acted as an agonist at rat hippocampal M1 receptors, as demonstrated by its ability to increase cell firing and initiate gamma frequency network oscillations. Finally, 77-LH-28-1 stimulated cell firing in the rat hippocampus in vivo following subcutaneous administration. Conclusions and implications: These data suggest that 77-LH-28-1 is a potent, selective, bioavailable and brain-penetrant agonist at the M1 mAChR and therefore that it represents a better tool than AC-42, with which to study the pharmacology of the M1 mAChR. British Journal of Pharmacology (2008) 154, 1104–1115; doi:10.1038/bjp.2008.152; published online 5 May 2008

Published

2008

6. 1,3-Diaminopropan-2-ol Sulfonamides as potent and selective inhibitors of the glycine transporter type 1

Author

Graham Francis Joiner, Steven Coulton, Hugh J. Herdon, Shahzad Sharooq Rahman, Jian Jin, and Roderick A. Porter

Subjects

Stereochemistry, High-throughput screening, Clinical Biochemistry, Drug Evaluation, Preclinical, Molecular Conformation, Pharmaceutical Science, Biochemistry, Glycine transporter, Structure-Activity Relationship, Isomerism, Glycine Plasma Membrane Transport Proteins, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Computer Simulation, Molecular Biology, Chromatography, High Pressure Liquid, Sulfonamides, Chemistry, Organic Chemistry, Sulfonamide (medicine), Transporter, In vitro, Rats, Cell culture, Molecular Medicine, NMDA receptor, Spectrophotometry, Ultraviolet, medicine.drug

Abstract

High throughput screening led to the discovery of a novel series of 1,3-diaminopropan-2-ol sulfonamides as selective GlyT-1 inhibitors. Structure-activity relationships of this novel series and optimisation of the initial hit that led to the identification of (2), a potent and selective GlyT-1 inhibitor, are also presented.

Published

2007

7. Probing the Molecular Mechanism of Interaction between 4-n-Butyl-1-[4-(2-methylphenyl)-4-oxo-1-butyl]-piperidine (AC-42) and the Muscarinic M1 Receptor: Direct Pharmacological Evidence That AC-42 Is an Allosteric Agonist

Author

Hugh J. Herdon, Christopher J. Langmead, Martyn D. Wood, Arthur Christopoulos, Victoria Anne Honey Fry, Clive Leslie Branch, and Ian Thomson Forbes

Subjects

Agonist, Carbachol, Stereochemistry, medicine.drug_class, Allosteric regulation, CHO Cells, Muscarinic Agonists, Radioligand Assay, Allosteric Regulation, Piperidines, Cricetinae, Muscarinic acetylcholine receptor, medicine, Animals, Receptor, Pharmacology, Chemistry, Receptor, Muscarinic M1, Muscarinic acetylcholine receptor M1, N-Methylscopolamine, Pirenzepine, Schild regression, Molecular Probes, Molecular Medicine, Calcium, medicine.drug

Abstract

4-n-Butyl-1-[4-(2-methylphenyl)-4-oxo-1-butyl]-piperidine hydrogen chloride (AC-42) is a selective agonist of the muscarinic M(1) receptor previously suggested to interact with an "ectopic" site on this receptor. However, the pharmacological properties of this site (i.e., whether it overlaps to any extent with the classic orthosteric site or represents a novel allosteric site) remain undetermined. In the present study, atropine or pirenzepine significantly inhibited the ability of either carbachol or AC-42 to stimulate inositol phosphate accumulation or intracellular calcium mobilization in Chinese hamster ovary (CHO) cells stably expressing the human M(1) receptor. However, the interaction between either of these antagonists and AC-42 was characterized by Schild slopes significantly less than unity. Increasing the concentrations of atropine revealed that the Schild regression was curvilinear, consistent with a negative allosteric interaction. More direct evidence for an allosteric mode of action of AC-42 was obtained in [(3)H]N-methylscopolamine ([(3)H]NMS) binding studies, in that both AC-42 and the prototypical modulator gallamine failed to fully inhibit specific [(3)H]NMS binding in a manner that was quantitatively described by an allosteric model applied to both modulator data sets. Furthermore, AC-42 and gallamine significantly retarded the rate of [(3)H]NMS dissociation from CHO-hM(1) cell membranes, conclusively demonstrating their ability to bind to a topographically distinct site to change M(1) receptor conformation. These data provide the first direct evidence that AC-42 is an allosteric agonist that activates M(1) receptors in the absence of the orthosteric agonist.

Published

2005

8. Characterisation of the binding of [3 H]-SB-674042, a novel nonpeptide antagonist, to the human orexin-1 receptor

Author

Jeffrey C. Jerman, Christopher J. Langmead, Hugh J. Herdon, Claire M. Scott, Stephen J. Brough, and Roderick A. Porter

Subjects

Pharmacology, Cell membrane, medicine.anatomical_structure, SB-334867, Scintillation proximity assay, Biochemistry, Chemistry, Chinese hamster ovary cell, Radioligand, medicine, Receptor, SB-408124, Orexin

Abstract

This study characterises the binding of a novel nonpeptide antagonist radioligand, [3H]SB-674042 (1-(5-(2-fluoro-phenyl)-2-methyl-thiazol-4-yl)-1-((S)-2-(5-phenyl-(1,3,4)oxadiazol-2-ylmethyl)-pyrrolidin-1-yl)-methanone), to the human orexin-1 (OX1) receptor stably expressed in Chinese hamster ovary (CHO) cells in both a whole cell assay and in a cell membrane-based scintillation proximity assay (SPA) format. Specific binding of [3H]SB-674042 was saturable in both whole cell and membrane formats. Analyses suggested a single high-affinity site, with Kd values of 3.76±0.45 and 5.03±0.31 nM, and corresponding Bmax values of 30.8±1.8 and 34.4±2.0 pmol mg protein−1, in whole cell and membrane formats, respectively. Kinetic studies yielded similar Kd values. Competition studies in whole cells revealed that the native orexin peptides display a low affinity for the OX1 receptor, with orexin-A displaying a ∼five-fold higher affinity than orexin-B (Ki values of 318±158 and 1516±597 nM, respectively). SB-334867, SB-408124 (1-(6,8-difluoro-2-methyl-quinolin-4-yl)-3-(4-dimethylamino-phenyl)-urea) and SB-410220 (1-(5,8-difluoro-quinolin-4-yl)-3-(4-dimethylamino-phenyl)-urea) all displayed high affinity for the OX1 receptor in both whole cell (Ki values 99±18, 57±8.3 and 19±4.5 nM, respectively) and membrane (Ki values 38±3.6, 27±4.1 and 4.5±0.2 nM, respectively) formats. Calcium mobilisation studies showed that SB-334867, SB-408124 and SB-410220 are all functional antagonists of the OX1 receptor, with potencies in line with their affinities, as measured in the radioligand binding assays, and with approximately 50-fold selectivity over the orexin-2 receptor. These studies indicate that [3H]SB-674042 is a specific, high-affinity radioligand for the OX1 receptor. The availability of this radioligand will be a valuable tool with which to investigate the physiological functions of OX1 receptors. British Journal of Pharmacology (2004) 141, 340–346. doi:10.1038/sj.bjp.0705610

Published

2004

9. Pharmacological assessment of the role of the glycine transporter GlyT-1 in mediating high-affinity glycine uptake by rat cerebral cortex and cerebellum synaptosomes

Author

S Coulton, A.M Brown, J.R Evans, W.J Cairns, F.M Godfrey, and Hugh J. Herdon

Subjects

Cerebellum, Sarcosine, Glycine, Glycine Plasma Membrane Transport Proteins, In Vitro Techniques, Biology, Glycine transporter, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Receptors, Glycine, medicine, Animals, Humans, Cerebral Cortex, Pharmacology, Synaptosome, Rats, Cortex (botany), Amino Acid Transport Systems, Neutral, medicine.anatomical_structure, Biochemistry, chemistry, Cerebral cortex, Carrier Proteins, Synaptosomes

Abstract

Two distinct types of glycine transporter, GlyT-1 and GlyT-2, have been characterised. GlyT-1 and GlyT-2 are known to be differentially expressed amongst CNS areas, but direct functional evidence for their relative contributions to high-affinity glycine uptake by brain tissues is lacking. In the present study, we have used the selective GlyT-1 inhibitor N[3-(4"-fluorophenyl)-3-(4"-phenylphenoxy)propyl]sarcosine (NFPS) to investigate the role of GlyT-1 in mediating glycine uptake. HEK293 cells expressing human GlyT-1c or GlyT-2 showed high levels of Na(+)-dependent glycine uptake, with K(m) values of 117+/-13 and 200+/-22 microM, respectively. NFPS potently inhibited uptake in GlyT-1c cells (IC(50) value 0.22+/-0.03 microM), being around 500-fold more potent than glycine or sarcosine, but had no effect on uptake in GlyT-2 cells (IC(50) >10 microM). Efflux of pre-loaded [3H]-glycine from GlyT-1c cells was increased by glycine or sarcosine, whereas NFPS had no effect on its own but blocked the effects of glycine or sarcosine. These results confirm that NFPS is a potent, selective and non-transportable GlyT-1 inhibitor. Rat cortex and cerebellum synaptosomes also showed a high-affinity Na(+)-dependent component of glycine uptake, with affinities similar to those observed for uptake in GlyT-1c or GlyT-2 cells. In cortex synaptosomes, NFPS and sarcosine produced the same maximal inhibition of uptake as glycine itself. However, in cerebellum synaptosomes, the maximal inhibition produced by NFPS and sarcosine was only half that produced by glycine. In both tissues NFPS was around 1000-fold more potent than glycine or sarcosine. Overall, our findings indicate that high-affinity glycine uptake in cerebral cortex occurs predominantly via GlyT-1. However, in cerebellum, only a part of the high-affinity uptake is mediated by GlyT-1, with the remaining NFPS-insensitive component most likely mediated by GlyT-2.

Published

2001

10. Characterization of the binding of [125 I]-human prolactin releasing peptide (PrRP) to GPR10, a novel G protein coupled receptor

Author

Jonathan K Chambers, Gary W. Price, Warren D. Hirst, Steven J Ratcliffe, Philip G. Szekeres, Christopher J. Langmead, Hugh J. Herdon, and Declan N.C. Jones

Subjects

Pharmacology, Biochemistry, G protein, Prolactin-releasing peptide, Radioligand, Neuropeptide FF, Binding site, Biology, Ligand (biochemistry), Receptor, G protein-coupled receptor

Abstract

GPR10 is a novel G-protein coupled receptor that is the human orthologue of rat Unknown Hypothalamic Receptor-1 (UHR-1). Human prolactin-releasing peptide (PrRP) has been identified as an endogenous ligand for GPR10, and occurs as 31 and 20 amino acid forms. The present study characterizes the binding of [125I]-PrRP-20 to HEK293 cells stably expressing GPR10 receptors. Specific binding of [125I]-PrRP-20 was saturable, and analysis suggested evidence of both high and low affinity sites, with KD values of 0.026±0.006 and 0.57±0.14 nM respectively, and Bmax values of 3010±400 and 8570±2240 fmol mg protein−1 respectively. Kinetic studies were unable to distinguish two sites, but single site analysis of association and dissociation data produced a KD of 0.012 nM. Competition studies revealed that human and rat PrRP-20 and PrRP-31 all display high affinity for GPR10. A range of other drugs which are known ligands at receptors which share limited homology with GPR10 were also tested. None of the drugs tested, including the RF-amide neuropeptide FF, demonstrated any affinity for GPR10. Human PrRP-20 failed to alter basal or forskolin-stimulated levels of intracellular cyclic AMP in HEK293-GPR10 cells, suggesting that GPR10 does not couple via either Gs or Gi. Functional studies using measurements of intracellular calcium confirmed that human and rat PrRP-20 and PrRP-31 are all potent, full agonists at the GPR10 receptor. The response was blocked both by thapsigargin, indicating mobilization of intracellular Ca2+ stores. These studies indicate that [125I]-PrRP-20 is a specific, high affinity radioligand for GPR10. The availability of this radioligand binding assay will be a valuable tool for the investigation of the key features involved in PrRP binding and studies on the localization and function of GPR10. British Journal of Pharmacology (2000) 131, 683–688; doi:10.1038/sj.bjp.0703617

Published

2000

11. Identification of (−)-cis-6-acetyl-4S-(3-chloro-4-fluoro-benzoylamino)-3,4-dihydro-2,2-dimethyl-2H-benzo[b]pyran-3S-ol as a potential antimigraine agent

Author

Wai N. Chan, Neil Upton, Andrew A. Parsons, Hugh J. Herdon, Jeffrey C. Jerman, John Morris Evans, Tania O. Stean, Simon Read, Mervyn Thompson, and Michael S. Hadley

Subjects

Time Factors, Migraine Disorders, Clinical Biochemistry, Pharmaceutical Science, Methylcellulose, Biochemistry, Medicinal chemistry, Chemical synthesis, Mice, chemistry.chemical_compound, Animal model, Seizures, In vivo, Drug Discovery, Animals, Benzopyrans, Molecular Biology, Dose-Response Relationship, Drug, Sumatriptan, Organic Chemistry, Temperature, Rats, chemistry, Pyran, Benzamides, Molecular Medicine, Enantiomer

Abstract

Optimisation of novel cis- and trans-4-(substituted-amido)benzopyran-3-ol derivatives has led to the identification of SB-220453 20 with an in vivo pre-clinical CNS profile predictive of potential antimigraine activity.

Published

1999

12. Characterization of the binding of [3 H]-SB-204269, a radiolabelled form of the new anticonvulsant SB-204269, to a novel binding site in rat brain membranes

Author

Jeffrey C. Jerman, Derek N. Middlemiss, Neil Upton, Vong Antonio Kuok Keong, Wai N. Chan, Tania O. Stean, Hugh J. Herdon, Mervyn Thompson, and John Morris Evans

Subjects

Pharmacology, HEPES, education.field_of_study, Seizure threshold, Stereochemistry, Chemistry, Population, Dissociation constant, Anticonvulsant Agent, chemistry.chemical_compound, Ethosuximide, Mechanism of action, medicine, medicine.symptom, Binding site, education, medicine.drug

Abstract

1 SB-204269 (trans-(+)-6-acetyl-4S-(4-fluorobenzoylamino)-3,4-dihydro-2,2-dimethyl-2H-benzol[b]pyran-3R-ol, hemihydrate) shows potent anticonvulsant activity in a range of animal seizure models, with a lack of neurological or cardiovascular side-effects. The profile of the compound suggests that it may have a novel mechanism of action. This study describes the characteristics of a binding site for [3H]-SB-204269 in rat forebrain membranes. 2 Specific [3H]-SB-204269 binding was saturable and analysis indicated binding to a homogenoeous population of non-interacting binding sites with a dissociation constant (KD) of 32±1 nM and a maximum binding capacity (Bmax) of 253±18 fmol mg−1 protein. Kinetic studies indicated monophasic association and dissociation. Binding was similar in HEPES or Tris-HCl buffers and was unaffected by Na+, K+, Ca2+ or Mg2+ ions. Specific binding was widely distributed in brain, but was minimal in a range of peripheral tissues. 3 Specific [3H]-SB-204269 binding was highly stereoselective, with a 1000 fold difference between the affinities of SB-204269 and its enantiomer SB-204268 for the binding site. The affinities of analogues of SB-204269 for binding can be related to their activities in the mouse maximal electroshock seizure threshold (MEST) test of anticonvulsant action. 4 None of the standard anticonvulsant drugs, phenobarbitone, phenytoin, sodium valproate, carbamazepine, diazepam and ethosuximide, or the newer anticonvulsants, lamotrigine, vigabatrin, gabapentin and levetiracetam, showed any affinity for the [3H]-SB-204269 binding site. A wide range of drugs active at amino acid receptors, Na+ or K+ channels or various other receptors did not demonstrate any affinity for the binding site. 5 These studies indicate that SB-204269 possesses a specific CNS binding site which may mediate its anticonvulsant activity. This binding site does not appear to be directly related to the sites of action of other known anticonvulsant agents, but may have an important role in regulating neuronal excitability. British Journal of Pharmacology (1997) 121, 1687–1691; doi:10.1038/sj.bjp.0701331

Published

1997

13. Profile of SB-204269, a mechanistically novel anticonvulsant drug, in rat models of focal and generalized epileptic seizures

Author

Martyn L. Evans, Penny D. King, John Morris Evans, Wai N. Chan, Thomas P. Blackburn, Mervyn Thompson, Colin A. Campbell, Tania O. Stean, Duncan Cooper, Neil Upton, Alison M. Ray, and Hugh J. Herdon

Subjects

Pharmacology, Seizure threshold, Chemistry, medicine.medical_treatment, Carbamazepine, Lamotrigine, medicine.disease, Anticonvulsant Agent, Epilepsy, Anticonvulsant, Convulsion, medicine, Pentylenetetrazol, medicine.symptom, medicine.drug

Abstract

1. Earlier optimization of structure-activity relationships in a novel series of 4-(benzoylamino)-benzopyrans, led to the discovery of SB-204269 (trans-(+)-6-acetyl-4S-(4-fluorobenzoylamino)-3,4-dihydro-2, 2-dimethyl-2H-benzo[b]pyran-3R-ol, hemihydrate), a potent orally-active anticonvulsant in the mouse maximal electroshock seizure threshold (MEST) test. 2. Studies have now been undertaken to determine the effects of SB-204269 in a range of seizure models and tests of neurological deficits in rats. In addition, the compound has been evaluated in a series of in vitro mechanistic assays. 3. SB-204269 proved to be an orally-effective anticonvulsant agent, at doses (0.1-30 mg Kg-1) devoid of overt behavioural depressant properties, in models of both electrically (MEST and maximal electroshock (MEST)) and chemically (i.v. pentylenetetrazol (PTZ) infusion)-evoked tonic extension seizures. However, the compound did not inhibit PTZ-induced myoclonic seizures at doses up to 30 mg kg-1, p.o. 4. SB-204269 also selectively reduced focal electrographic seizure activity in an in vitro elevated K+ rat hippocampal slice model at concentrations (0.1-10 microM) that had no effect on normal synaptic activity and neuronal excitability. 5. In all of these seizure models, SB-204269 was equivalent or better than the clinically established antiepileptic drugs carbamazepine and lamotrigine, in terms of anticonvulsant potency and efficacy. 6. Unlike SB-204269, the corresponding trans 3S,4R enantiomer, SB-204268, did not produce marked anticonvulsant effects, an observation in accord with previous findings for other related pairs of trans enantiomers in the benzopyran series. 7. In the rat accelerating rotarod test, a sensitive paradigm for the detection of neurological deficits such as sedation and motor incoordination, SB-204269 was inactive even at doses as high as 200 mg kg-1, p.o. This was reflected in the excellent therapeutic index (minimum significantly effective dose in the rotarod test/ED50 in the MES test) for SB-204269 of > 31, as compared to equivalent values of only 7 and 13 for carbamazepine and lamotrigine, respectively. 8. At concentrations (> or = 10 microM) well above those required to produce anticonvulsant activity in vivo (i.e. 0.1 microM in brain), SB-204269 did not interact with many of the well known mechanistic targets for established antiepileptic drugs (e.g. Na+ channels or GABAergic neurotransmission). Subsequent studies have shown that the anticonvulsant properties of SB-204269 are likely to be mediated by a novel stereospecific binding site present in the CNS. 9. The overall efficacy profile in rodent seizure models, together with a minimal liability for inducing neurological impairment and an apparently unique mechanism of action, highlight the therapeutic potential of SB-204269 for the treatment of refractory partial and generalized tonic-clonic seizures.

Published

1997

14. Conformational preference of the 6-acetyl group in novel anticonvulsant trans 4S-benzamido-benzo[b]pyran-3R-ols

Author

Wai N. Chan, Hugh J. Herdon, Mervyn Thompson, John Morris Evans, Neil Upton, Helen Kate Ann Morgan, and Michael S. Hadley

Subjects

chemistry.chemical_classification, Steric effects, Ketone, Bicyclic molecule, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Benzopyran, chemistry.chemical_compound, Pyran, Drug Discovery, Molecular Medicine, Potency, Stereoselectivity, Molecular Biology

Abstract

Conformationally restricted ketones derived from the novel anticonvulsant 4 S (4-fluorobenzoylamino)benzopyran SB-204269 1 have revealed a preferred “in plane” conformation which is essential for optimal potency at a unique receptor site.

Published

1997

15. Relationship between glycine transporter 1 inhibition as measured with positron emission tomography and changes in cognitive performances in nonhuman primates

Author

Hugh J. Herdon, David Weinzimmer, Roger N. Gunn, Richard E. Carson, Yiyun Huang, Ming-Qiang Zheng, Marc Laruelle, Brooke M. Roberts, Graham V. Williams, Eugenii A. Rabiner, N V Murthy, Khanum Ridler, and Stacy A. Castner

Subjects

Male, N-Methylaspartate, Tetrahydronaphthalenes, Glycine Plasma Membrane Transport Proteins, Neuropsychological Tests, Spatial memory, Org 25935, medicine, Animals, Carbon Radioisotopes, Spatial Memory, Pharmacology, biology, Working memory, Brain, medicine.disease, Macaca mulatta, Psychiatry and Mental health, Memory, Short-Term, Schizophrenia, Glycine transporter 1, Positron-Emission Tomography, Glycine, Benzamides, biology.protein, NMDA receptor, Female, Ketamine, Original Article, Radiopharmaceuticals, Psychology, Neuroscience, Excitatory Amino Acid Antagonists, Central Nervous System Agents

Abstract

Several lines of evidence suggest that schizophrenia is associated with deficits in glutamatergic transmission at the N-methyl-d-aspartate (NMDA) receptors. Glycine is a NMDA receptor co-agonist, and extracellular levels of glycine are regulated in the forebrain by the glycine type-1 transporters (GlyT-1). GlyT-1 inhibitors elevate extracellular glycine and thus potentiate NMDA transmission. This mechanism represents a promising new avenue for the treatment of schizophrenia. Here, the recently introduced positron emission tomography radiotracer [11C]GSK931145 was used to quantify the relationship between occupancy of GlyT-1 by a GlyT-1 inhibitor, Org 25935, and its impact on spatial working memory performances in rhesus monkeys. The effect of Org 25935 on working memory was assessed both in control conditions and during a state of relative NMDA hypofunction induced by ketamine administration, at a dose selected for each animal to reduce task performance by about 50%. Under control conditions, Org 25935 had no effect on working memory at GlyT-1 occupancies lower than 75% and significantly impaired working memory at occupancies higher than 75%. Under ketamine conditions, Org 25935 reversed the deficit in working memory induced by ketamine and did so optimally in the 40–70% GlyT-1 occupancy range. The results confirm the efficacy of this mechanism to correct working memory deficits associated with NMDA hypofunction. These data also suggest the existence of an inverted-U dose–response curve in the potential therapeutic effect of this class of compounds.

Published

2012

16. SB 201823-A, a neuronal Ca2+ antagonist is neuroprotective in two models of cerebral ischaemia

Author

S.R. Patel, T.H. Brown, Alan L. Rothaul, Hugh J. Herdon, S.J. Smith, Mark H Harries, Jennifer C. Roberts, Christopher D. Benham, M.L. Evans, J.E. Meakin, K.L. Murkitt, D.G. Cooper, Nigel I. Wood, and A. J. Hunter

Subjects

Agonist, medicine.drug_class, Pharmacology, Gerbil, Neuroprotection, Sodium Channels, Brain Ischemia, Brain ischemia, Cellular and Molecular Neuroscience, Piperidines, Ganglia, Spinal, medicine, Animals, Carotid Artery Thrombosis, Neurons, Afferent, Voltage-dependent calcium channel, business.industry, Sodium channel, Antagonist, Calcium Channel Blockers, medicine.disease, Rats, Electrophysiology, Potassium, Gerbillinae, business, Neuroscience, Synaptosomes

Abstract

We have characterised the Ca2+ channel blocking properties of a new non-peptide Ca2+ channel antagonist, SB 201823-A, in cultures of rat sensory neurones. The IC50 for SB 201823-A against total Ca2+ current in sensory neurones was 4.9 microM. SB 201823-A showed little selectivity for sub-types of neuronal Ca2+ channel but was selective for Ca2+ channels over Na+ and K+ channels. Efficacy against other types of cation channel such as agonist gated channels was not assessed. SB 201823-A was neuroprotective in vivo when administered post-ischaemia in one focal and one global model of neuronal ischaemia. In the rat photothrombotic focal lesion model, SB 201823-A administered i.p. 10 min post-ischaemia resulted in a dramatic reduction in lesion volume. In the gerbil bilateral carotid artery occlusion global model, SB 201823-A dosed i.p. 30 min post-occlusion resulted in both histological and functional improvements when compared to vehicle treated animals. These data suggest that such novel neuronal Ca2+ channel antagonists may have potential in ameliorating both the pathological and functional consequences of stroke in man.

Published

1993

17. ChemInform Abstract: Synthesis of Novel trans-4-(Substituted-benzamido)-3,4-dihydro-2H- benzo(b)pyran-3-ol Derivatives as Potential Anticonvulsant Agents with a Distinctive Binding Profile

Author

Vong Antonio Kuok Keong, Wai N. Chan, Jeffrey C. Jerman, Tania O. Stean, Helen Kate Ann Morgan, Michael S. Hadley, Neil Upton, John Morris Evans, Hugh J. Herdon, and Mervyn Thompson

Subjects

Anticonvulsant Agent, Binding profile, chemistry.chemical_compound, Chemistry, Stereochemistry, Pyran, Organic chemistry, General Medicine

Published

2010

18. ChemInform Abstract: Identification of a Series of 1,2,3,4-Tetrahydroisoquinolinyl Benzamides with Potential Anticonvulsant Activity

Author

Tania O. Stean, Jeffrey C. Jerman, Neil Upton, Hugh J. Herdon, Michael S. Hadley, Robert William Ward, Barry Sidney Orlek, Mervyn Thompson, John David Harling, and Wai N. Chan

Subjects

Anticonvulsant, Stereochemistry, Chemistry, medicine.medical_treatment, medicine, Identification (biology), General Medicine, Binding site

Abstract

A series of N-(tetrahydroisoquinolinyl)-2-methoxybenzamides was identified by high-throughput screening at the novel SB-204269 binding site. SAR studies have provided compounds 4 and 14 with high affinity and good anticonvulsant activity in animal models.

Published

2010

19. ChemInform Abstract: Identification of (-)-cis-6-Acetyl-4S- (3-chloro-4-fluorobenzoylamino)-3,4-dihydro-2,2-dimethyl-2H-benzo [b]pyran-3S-ol (I) as a Potential Antimigraine Agent

Author

Michael S. Hadley, Wai N. Chan, Jeffrey C. Jerman, Andrew A. Parsons, Tania O. Stean, Simon Read, John Morris Evans, Mervyn Thompson, Hugh J. Herdon, and Neil Upton

Subjects

chemistry.chemical_compound, chemistry, Pyran, Stereochemistry, Identification (biology), General Medicine

Published

2010

20. Pharmacological characterisation of the GlyT-1 glycine transporter using two novel radioligands

Author

Hugh J. Herdon, Roderick A. Porter, Jennifer C. Roberts, and Steve Coulton

Subjects

Tris, Male, Stereochemistry, Biology, Binding, Competitive, Glycine transporter, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Radioligand Assay, Glycine Plasma Membrane Transport Proteins, Radioligand, medicine, Animals, Humans, Pharmacology, HEPES, Binding Sites, Brain, Human brain, Rats, medicine.anatomical_structure, Membrane, HEK293 Cells, chemistry, Biochemistry, Cerebral cortex, NMDA receptor

Abstract

Inhibitors of the glycine transporter GlyT-1 are being developed as potential treatments for schizophrenia. Here we report on the use of two novel radioligands, [ 3 H]-SB-733993 and [ 3 H]-GSK931145, for the characterisation of GlyT-1 in both cells and native tissue. Binding was evaluated in membranes either from HEK293 cells expressing recombinant human GlyT-1 (hGlyT-1) or from rat cerebral cortex. Specific binding of both [ 3 H]-SB-733993 and [ 3 H]-GSK931145 to hGlyT-1 HEK293 cell membranes and rat cerebral cortex membranes was saturable and comprised >90% of total binding. K d and B max values for the two radioligands were fairly similar, with K d values of 1–2 nM and B max values of around 7000 fmol/mg protein in hGlyT-1 membranes and 3000 fmol/mg protein in rat cortex membranes. Association of [ 3 H]-SB-733993 was faster, with binding reaching equilibrium within 30 min compared with 90 min for [ 3 H]-GSK931145. Dissociation was also much slower for [ 3 H]-GSK931145 than for [ 3 H]-SB-733993, with 50% of specific binding being dissociated by approximately 40 min and 5 min, respectively. Autoradiography studies with [ 3 H]-GSK931145 showed widespread distribution of binding in rat brain, with generally higher binding in caudal compared with rostral areas. Initial studies in human frontal cortex membranes showed clear specific binding of [ 3 H]-GSK931145, though with much lower density ( B max 570 fmol/mg protein) and slightly lower affinity (K d 4.5 nM) compared with rat cortex. A human brain autoradiography study showed higher specific binding in cerebellum compared with frontal cortex. All GlyT-1 inhibitors tested, as well as glycine itself, competed fully for the binding of both [ 3 H]-SB-733993 and [ 3 H]-GSK931145 in both hGlyT-1 and rat cortex membranes. Studies on the effect of varying NaCl concentration showed that [ 3 H]-SB-733993 binding was reduced by >90% in the absence of added Na + ions, whilst [ 3 H]-GSK931145 binding was unaffected. Glycine produced concentration-dependent decreases in binding affinity of both radioligands without major changes in B max values, suggesting that both [ 3 H]-SB-733993 and [ 3 H]-GSK931145 bind to sites on GlyT-1 that are orthosteric to the site at which glycine itself binds. Overall, these results show that both [ 3 H]-SB-733993 and [ 3 H]-GSK931145 are useful radioligands for studies on GlyT-1 in both cell lines and native tissues, with [ 3 H]-GSK931145 being the radioligand of choice for further studies on GlyT-1 expression and pharmacology.

Published

2010

21. Glycine transporter 1 (GlyT1) inhibitors exhibit anticonvulsant properties in the rat maximal electroshock threshold (MEST) test

Author

Simon Teague, Andrea M. Bradford, Mikhail Kalinichev, Roderick A. Porter, Hugh J. Herdon, and Kathryn R. Starr

Subjects

Agonist, Male, medicine.drug_class, medicine.medical_treatment, Glycine, Neurotransmission, Pharmacology, Org 25935, Rats, Sprague-Dawley, Glycine binding, Phenols, Glycine Plasma Membrane Transport Proteins, Seizures, medicine, Animals, Molecular Biology, Electroshock, biology, Chemistry, General Neuroscience, Potentiator, Rats, Anticonvulsant, Glycine transporter 1, Benzamides, biology.protein, Anticonvulsants, Neurology (clinical), Developmental Biology

Abstract

Glycine can act as either an inhibitory neurotransmitter or as a potentiator of NMDA-dependent excitatory neurotransmission. There is some evidence that glycine can have both pro- and anticonvulsant properties in various rodent models of epilepsy. In the present study we tested several glycine transporter 1 (GlyT1) inhibitors including NFPS, SSR 504734, Lu AA21279, Org 25935, SB-710622, GSK931145, as well as the glycine agonist d -serine, in the maximal electroshock threshold (MEST) test in the rat. In a series of experiments, male Sprague–Dawley rats (n = 12/group) were pre-treated with a compound of interest and then received an electric shock delivered via corneal electrodes. A cohort of satellite animals (n = 3/group) was also used to measure blood and brain levels of Org 25935. All GlyT1 inhibitors increased seizure thresholds dose-dependently, indicative of anticonvulsant activity. SB-710622 and GSK931145 had lower minimum effective doses (MEDs) in the MEST test than other GlyT1 inhibitors. At estimated tmax, increases in dose administered were paralleled by increases in blood and brain concentrations of Org 25935. Thus, increasing extracellular concentration of glycine via inhibition of its uptake protects from electroshock-induced seizures in the rat. Whether strychnine-sensitive or strychnine-insensitive glycine binding sites are involved in this effect remains to be determined.

Published

2009

22. Structure-function studies of allosteric agonism at M2 muscarinic acetylcholine receptors

Author

Patrick M. Sexton, Arthur Christopoulos, Hugh J. Herdon, Vimesh Ashvinkumar Avlani, Martyn D. Wood, Christopher J. Langmead, and Lauren T. May

Subjects

Agonist, Stereochemistry, medicine.drug_class, Allosteric regulation, GTPgammaS, Guanosine, CHO Cells, Muscarinic Agonists, chemistry.chemical_compound, Structure-Activity Relationship, Cricetulus, Allosteric Regulation, Piperidines, Cricetinae, Muscarinic acetylcholine receptor, medicine, Animals, Binding site, Pharmacology, Receptor, Muscarinic M2, Chemistry, (4-(m-Chlorophenylcarbamoyloxy)-2-butynyl)trimethylammonium Chloride, Cooperative binding, N-Methylscopolamine, Acetylcholine, Molecular Medicine, Allosteric Site, medicine.drug

Abstract

The M2 muscarinic acetylcholine receptor (mAChR) possesses at least one binding site for allosteric modulators that is dependent on the residues (172)EDGE(175), Tyr(177), and Thr(423). However, the contribution of these residues to actions of allosteric agonists, as opposed to modulators, is unknown. We created mutant M2 mAChRs in which the charge of the (172)EDGE(175) sequence had been neutralized and each Tyr(177) and Thr(423) was substituted with alanine. Radioligand binding experiments revealed that these mutations had a profound inhibitory effect on the prototypical modulators gallamine, alcuronium, and heptane-1,7-bis-[dimethyl-3'-phthalimidopropyl]-ammonium bromide (C7/3-phth) but minimal effects on the orthosteric antagonist [3H]N-methyl scopolamine. In contrast, the allosteric agonists 4-I-[3-chlorophenyl]carbamoyloxy)-2-butynyltrimethylammnonium chloride (McN-A-343), 4-n-butyl-1-[4-(2-methylphenyl)-4-oxo-1-butyl] piperidine hydrogen chloride (AC-42), and the novel AC-42 derivative 1-[3-(4-butyl-1-piperidinyl)propyl]-3,4-dihydro-2(1H)-quinolinone (77-LH-28-1) demonstrated an increased affinity or proportion of high-affinity sites at the combined EDGE-YT mutation, indicating a different mode of binding to the prototypical modulators. Subsequent functional assays of extracellular signal-regulated kinase (ERK)1/2 phosphorylation and guanosine 5'-(gamma-[(35)S]thio)triphosphate ([(35)S]GTPgammaS) binding revealed minimal effects of the mutations on the orthosteric agonists acetylcholine (ACh) and pilocarpine but a significant increase in the efficacy of McN-A-343 and potency of 77-LH-28-1. Additional mutagenesis experiments found that these effects were predominantly mediated by Tyr(177) and Thr(423), rather than the (172)EDGE(175) sequence. The functional interaction between each of the allosteric agonists and ACh was characterized by high negative cooperativity but was consistent with an increased allosteric agonist affinity at the combined EDGE-YT mutant M2 mAChR. This study has thus revealed a differential role of critical allosteric site residues on the binding and function of allosteric agonists versus allosteric modulators of M2 mAChRs.

Published

2007

23. Synthesis of Novel trans-4-(Substituted-benzamido)-3,4-dihydro-2H-benzo[b]pyran-3-ol Derivatives as Potential Anticonvulsant Agents with a Distinctive Binding Profile

Author

Mervyn Thompson, John Morris Evans, Jeffrey C. Jerman, Tania O. Stean, Neil Upton, Vong Antonio Kuok Keong, Wai N. Chan, Helen Kate Ann Morgan, Michael S. Hadley, and Hugh J. Herdon

Subjects

Binding Sites, Bicyclic molecule, Chemistry, Stereochemistry, medicine.drug_class, Stereoisomerism, Carboxamide, Tritium, Chemical synthesis, Rats, Mice, Radioligand Assay, chemistry.chemical_compound, Anticonvulsant Agent, Pyran, Benzamides, Drug Discovery, medicine, Animals, Molecular Medicine, Anticonvulsants, Benzopyrans, Stereoselectivity, Binding site

Published

1996

24. Characterisation of the binding of [3H]-SB-674042, a novel nonpeptide antagonist, to the human orexin-1 receptor

Author

Christopher J, Langmead, Jeffrey C, Jerman, Stephen J, Brough, Claire, Scott, Rod A, Porter, and Hugh J, Herdon

Subjects

Receptors, Neuropeptide, Benzoxazoles, Pyrrolidines, CHO Cells, Tritium, Receptors, G-Protein-Coupled, Thiazoles, Orexin Receptors, Cricetinae, Papers, Animals, Humans, Urea, Naphthyridines, Protein Binding

Abstract

1. This study characterises the binding of a novel nonpeptide antagonist radioligand, [(3)H]SB-674042 (1-(5-(2-fluoro-phenyl)-2-methyl-thiazol-4-yl)-1-((S)-2-(5-phenyl-(1,3,4)oxadiazol-2-ylmethyl)-pyrrolidin-1-yl)-methanone), to the human orexin-1 (OX(1)) receptor stably expressed in Chinese hamster ovary (CHO) cells in both a whole cell assay and in a cell membrane-based scintillation proximity assay (SPA) format. 2. Specific binding of [(3)H]SB-674042 was saturable in both whole cell and membrane formats. Analyses suggested a single high-affinity site, with K(d) values of 3.76+/-0.45 and 5.03+/-0.31 nm, and corresponding B(max) values of 30.8+/-1.8 and 34.4+/-2.0 pmol mg protein(-1), in whole cell and membrane formats, respectively. Kinetic studies yielded similar K(d) values. 3. Competition studies in whole cells revealed that the native orexin peptides display a low affinity for the OX(1) receptor, with orexin-A displaying a approximately five-fold higher affinity than orexin-B (K(i) values of 318+/-158 and 1516+/-597 nm, respectively). 4. SB-334867, SB-408124 (1-(6,8-difluoro-2-methyl-quinolin-4-yl)-3-(4-dimethylamino-phenyl)-urea) and SB-410220 (1-(5,8-difluoro-quinolin-4-yl)-3-(4-dimethylamino-phenyl)-urea) all displayed high affinity for the OX(1) receptor in both whole cell (K(i) values 99+/-18, 57+/-8.3 and 19+/-4.5 nm, respectively) and membrane (K(i) values 38+/-3.6, 27+/-4.1 and 4.5+/-0.2 nm, respectively) formats. 5. Calcium mobilisation studies showed that SB-334867, SB-408124 and SB-410220 are all functional antagonists of the OX(1) receptor, with potencies in line with their affinities, as measured in the radioligand binding assays, and with approximately 50-fold selectivity over the orexin-2 receptor. 6. These studies indicate that [(3)H]SB-674042 is a specific, high-affinity radioligand for the OX(1) receptor. The availability of this radioligand will be a valuable tool with which to investigate the physiological functions of OX(1) receptors.

Published

2003

25. Evaluation of a series of anticonvulsant 1,2,3,4-tetrahydroisoquinolinyl-benzamides

Author

Neil Upton, Barry Sidney Orlek, Michael S. Hadley, Graham J. Riley, Mervyn Thompson, Robert William Ward, Wai N. Chan, Rachel E.A. Stead, Hugh J. Herdon, Tania O. Stean, and John David Harling

Subjects

Male, Models, Molecular, Molecular model, medicine.drug_class, Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Carboxamide, Biochemistry, Chemical synthesis, Mice, Radioligand Assay, Structure-Activity Relationship, Seizures, Drug Discovery, medicine, Animals, Benzopyrans, Binding site, Molecular Biology, Brain Chemistry, Binding Sites, Bicyclic molecule, Molecular Structure, Chemistry, Organic Chemistry, Isoquinolines, Rats, Anticonvulsant, Drug Design, Benzamides, Molecular Medicine, Anticonvulsants

Abstract

SAR studies around a series of N-(tetrahydroisoquinolinyl)-2-methoxybenzamides, identified by high-throughput screening at the novel SB-204269 binding site, have provided compounds such as 13, 29-33 with high affinity and excellent anticonvulsant activity in animal models.

Published

2000

26. Use of the radioligand [(125)I]-SB-217644 in the characterisation and solubilisation of the novel binding site for the anticonvulsant SB-204269 in rat brain membranes and cell lines

Author

Fiona M Godfrey, Hugh J. Herdon, and Wai N. Chan

Subjects

Male, Cerebellum, Detergents, Biology, Cell Line, Iodine Radioisotopes, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, Radioligand Assay, Neuroblastoma, medicine, Radioligand, Animals, Benzopyrans, Binding site, Pharmacology, Binding Sites, Membranes, medicine.disease, Rats, Kinetics, Membrane, medicine.anatomical_structure, Cell culture, Forebrain, Benzamides, Biophysics, Neuroscience, Astrocyte

Abstract

SB-204269 (trans-(+)-6-acetyl-4S-(4-fluorobenzoylamino)-3, 4-dihydro-2,2-dimethyl-2H-benzo[b]pyran-3R-ol) shows anticonvulsant activity in a range of animal seizure models, with a high therapeutic index and a lack of side-effects. We have previously reported the characterisation of a novel binding site for [(3)H]-SB-204269 in rat forebrain, which has a unique profile unrelated to other known anticonvulsant sites of action. We now describe the use of a [(125)I]-labelled form of SB-217644 (trans-6-acetyl-4S-(3-iodobenzoylamino)-3,4-dihydro-2, 2-dimethyl-2H-benzo[b]pyran-3R-ol), an analogue of SB-204269, for studies on this novel binding site. In rat forebrain membranes, [(125)I]-SB-217644 shows a similar binding profile to that of [(3)H]-SB-204269, with a maximum specific binding capacity (B(max)) of 286+/-12 fmol/mg protein, but has twenty-fold higher affinity (K(d) value 1.7+/-0.1 nM). The high affinity and high specific activity of [(125)I]-SB-217644 allowed it to be used for detection and characterisation of the detergent-solubilised form of the binding site. Specific [(125)I]-SB-217644 binding to cholate-solubilised rat cerebellum showed a K(d) value of 2.7+/-0.3 nM and a B(max) value of 55+/-11 fmol/mg protein, with a 7.3+/-0.3% yield of solubilised binding sites. [(125)I]-SB-217644 was also used in whole-cell binding assays for investigation of the properties of the novel binding site in a range of cell lines. Both rat brain neuronal and glial primary cultures and several CNS-related cell lines were found to have levels of specific [(125)I]-SB-217644 binding similar to those present in rat forebrain membranes. The solubilisation of this novel binding site, and the ability to quantify and characterise it in solubilised tissues and whole cells using [(125)I]-SB217644, will allow further studies towards the ultimate identification of the molecular target of SB-204269.

Published

2000

27. Identification of a series of 1,2,3,4-tetrahydroisoquinolinyl-benzamides with potential anticonvulsant activity

Author

Jeffrey C. Jerman, Michael S. Hadley, Wai N. Chan, Robert William Ward, Barry Sidney Orlek, Tania O. Stean, John David Harling, Mervyn Thompson, Hugh J. Herdon, and Neil Upton

Subjects

Models, Molecular, Molecular model, Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Mice, Structure-Activity Relationship, Seizures, Drug Discovery, medicine, Animals, Benzopyrans, Binding site, Molecular Biology, Binding Sites, Chemistry, Organic Chemistry, Anticonvulsant, Benzamides, Quinolines, Molecular Medicine, Identification (biology), Anticonvulsants

Abstract

A series of N-(tetrahydroisoquinolinyl)-2-methoxybenzamides was identified by high-throughput screening at the novel SB-204269 binding site. SAR studies have provided compounds 4 and 14 with high affinity and good anticonvulsant activity in animal models.

Published

1999

28. The novel anticonvulsant SB 204269 binds to a stereospecific site in the mouse brain

Author

Derek N. Middlemiss, Tania O. Stean, Neil Upton, Jeff Jerman, Hugh J. Herdon, and Wai Chan

Subjects

Pharmacology, medicine.medical_specialty, Binding Sites, Membranes, Seizure threshold, Stereochemistry, Chemistry, medicine.medical_treatment, Biological activity, Mice, Membrane, Endocrinology, Anticonvulsant, Stereospecificity, Prosencephalon, Mechanism of action, Internal medicine, Forebrain, Benzamides, medicine, Animals, Anticonvulsants, Benzopyrans, Binding site, medicine.symptom

Abstract

The novel compound SB 204269 ( trans -(+)-6-acetyl-4 S -(4-fluorobenzoylamino)-3,4-dihydro-2,2-dimethyl-2 H -benzo[ b ]pyran-3 R -ol,hemihydrate) shows potent anticonvulsant activity in the mouse maximal electroshock seizure threshold test. The binding of [ 3 H]SB 204269 to mouse forebrain membranes is saturable ( B max 217 fmol/mg protein, K d 32 nM) and stereospecific. The excellent anticonvulsant profile of SB 204269, combined with the identification of a unique central binding site for the compound, suggest that it has potential clinical utility as a novel treatment for epilepsy.

Published

1996

29. [11C]GSK931145: A new pet ligand for glycine transporter 1

Author

Graham E. Searle, R. Fagg, N. Venkatesha Murthy, Mark Slifstein, S. Sutherland, Santiago Bullich, Roger N. Gunn, Ana M. Catafau, Jan Passchier, Roderick A. Porter, M. Neve, Hugh J. Herdon, Magí Farré, Raul Herance, Marc Laruelle, and Marina Suarez

Subjects

Neurology, biology, Biochemistry, Chemistry, Cognitive Neuroscience, Glycine transporter 1, Pet ligand, biology.protein, 11C-GSK931145

Published

2008

30. Diethylstilbestrol regulates the number of α- and β-adrenergic binding sites in incubated hypothalamus and amygdala

Author

Michael Wilkinson and Hugh J. Herdon

Subjects

Male, medicine.medical_specialty, Adrenergic receptor, medicine.drug_class, Hypothalamus, Diethylstilbestrol, Estrogen receptor, Adrenergic, Dihydroergotoxine, Biology, Adrenergic receptor binding, Clomiphene, Culture Techniques, Internal medicine, Receptors, Adrenergic, beta, Cyclic AMP, medicine, Animals, Castration, Molecular Biology, General Neuroscience, Rats, Inbred Strains, Receptors, Adrenergic, alpha, Amygdala, Rats, Receptors, Adrenergic, Tamoxifen, Endocrinology, Estrogen, Dihydroalprenolol, Ovariectomized rat, Female, Neurology (clinical), hormones, hormone substitutes, and hormone antagonists, Developmental Biology, medicine.drug

Abstract

Previous work has identified an effect of circulating estrogens on the number of central adrenergic binding sites. We have further characterized this effect by performing the experiments in vitro and have taken advantage of a well-described hypothalamic preparation in which diethylstilbestrol (DES), is known to elevate cAMP levels through a pathway which involves adrenoreceptors. We show that DES induces a reciprocal change in the numbers of alpha- and beta-adrenergic binding sites in incubated hypothalami obtained from intact immature female rats as well as from ovariectomized adult rats. The alpha-adrenergic binding sites are reduced by 25-30% whereas the beta-adrenergic sites are increased by 60-100%. The effect is maximal at 3 h in vitro (20 microM DES) and largely reversible following a 2 h wash in the absence of DES. Using the change in beta-adrenergic binding sites as a probe, we were further able to show that estradiol (100 microM) and 2-hydroxyestradiol (50 microM) had no effect. Further, the effect of DES was not blocked by the anti-estrogens clomiphene or tamoxifen. Since DES is able to elevate beta-adrenergic binding sites in hypothalamus and amygdala (brain areas known to contain high levels of estrogen receptors) but has no effect in cerebellum, we conclude that we have observed an effect of DES not shared by estradiol but which may be confined to estrogen target areas of the brain.

Published

1982

31. Changes in hypothalamic dopamine D-2 receptors during sexual maturation in male and female rats

Author

Hugh J. Herdon and Catherine A. Wilson

Subjects

Male, medicine.medical_specialty, Sex Differentiation, Hypothalamus, Biology, Receptors, Dopamine, Dopamine, Internal medicine, medicine, Sexual maturity, Animals, Testosterone, Sexual Maturation, Receptor, Gonadal Steroid Hormones, Molecular Biology, Sex Characteristics, Sexual differentiation, Receptors, Dopamine D2, General Neuroscience, Rats, Inbred Strains, Rats, Sexual dimorphism, Endocrinology, Animals, Newborn, Female, Neurology (clinical), Developmental Biology, Sex characteristics, medicine.drug

Abstract

We have examined variations in hypothalamic dopamine D-2 receptor levels occurring during sexual maturation in male and female rats, using a [3H]domperidone radioligand binding assay. A major decrease in D-2 receptor levels was observed during sexual development, and was accompanied by the appearance of a sexual dimorphism in receptor levels, which appeared to be the result of neonatal sexual differentiation. These changes may be linked with the alterations in hormone levels which occur during sexual maturation.

Published

1985