Your search keyword '"Renee Sharon Martin"' showing total 13 results

1. AF-353, a novel, potent and orally bioavailable P2X3/P2X2/3 receptor antagonist

Author

David H Hackos, Anthony P.D.W. Ford, Werner Rubas, Rothschild Soto, Marcos E. Milla, Robert Henningsen, Geoffrey Burnstock, Joel R Gever, Michael Patrick Dillon, Renee Sharon Martin, Sandip Panicker, and Ian B Oglesby

Subjects

Pharmacology, Chemistry, medicine.drug_class, Purinergic receptor, Antagonist, Receptor antagonist, body regions, medicine.anatomical_structure, Heterotrimeric G protein, medicine, Patch clamp, Receptor, Ion channel, Sensitization

Abstract

Background and purpose: Purinoceptors containing the P2X3 subunit (P2X3 homotrimeric and P2X2/3 heterotrimeric) are members of the P2X family of ion channels gated by ATP and may participate in primary afferent sensitization in a variety of pain-related diseases. The current work describes the in vitro pharmacological characteristics of AF-353, a novel, orally bioavailable, highly potent and selective P2X3/P2X2/3 receptor antagonist.

Published

2010

2. Effects of cannabinoid receptor ligands on psychosis-relevant behavior models in the rat

Author

David A. Lowe, Renee Sharon Martin, Douglas W. Bonhaus, Linda Hedley, Martine Lemaire, Robert L. Secchi, and Eric Sung

Subjects

Male, Agonist, Reflex, Startle, Dextroamphetamine, Apomorphine, medicine.drug_class, Receptors, Drug, Poison control, Motor Activity, Pharmacology, Psychoses, Substance-Induced, Piperidines, Rimonabant, medicine, Haloperidol, Animals, Attention, Rats, Wistar, Receptors, Cannabinoid, Clozapine, Behavior, Animal, Dose-Response Relationship, Drug, Psychotomimetic, Cyclohexanols, Rats, Stereotypy (non-human), Hallucinogens, Pyrazoles, Dizocilpine Maleate, Stereotyped Behavior, Arousal, Psychology, Antipsychotic Agents, medicine.drug

Abstract

Rationale. Marijuana is known to have psychotropic effects in humans. In this study, we used rat models of sensorimotor gating, hyperactivity and stereotypy to explore whether CB1 receptor stimulation or blockade induces behavioral changes consistent with psychotomimetic or antipsychotic agents, respectively. Objectives. We determined whether (a) the cannabinoid agonist CP 55940 decreased pre-pulse inhibition (PPI) as might be expected from a psychotomimetic agent, and (b) the selective CB1 receptor antagonist, SR 141716A, had any effect on PPI on its own or following disruptions by psychotomimetic agents. In addition, we investigated the effects of SR 141716A on elevated levels of hyperactivity and stereotypy elicited by d-amphetamine. Methods. These studies were conducted in rats using standard methodologies for determination of PPI following acoustic stimuli, and d-amphetamine-induced hyperactivity and stereotypies. Results. Decreased startle responses to 120 dB stimuli were observed in rats treated with CP 55940 (0.1 mg/kg IP) in the absence and presence of a 73 dB pre-pulse. These effects were reversed by SR 141716A (5 and 10 mg/kg, respectively). SR 141716A (0.1, 5, 10 mg/kg) had no effect on PPI on its own or following disruptions by apomorphine, d-amphetamine or MK-801. Conversely, in separate experiments different antipsychotic agents reversed disruptions in PPI induced by d-amphetamine (haloperidol), apomorphine (haloperidol or clozapine) or MK-801 (clozapine or olanzapine). In addition, unlike haloperidol, SR 141716A (5 mg/kg) did not reverse d-amphetamine-mediated increases in hyperactivity or stereotypy. Conclusions. The CP 55940-mediated decreases in startle amplitude confound assessment of the effects of CB1 receptor activation on PPI. The failure of SR 141716A to reverse disruptions in PPI, hyperactivity or stereotypy induced by non-cannabinoid psychotomimetic agents suggests that blockade of the CB1 receptor on its own is not sufficient for antipsychotic therapy.

Published

2003

3. Effects of cannabinoid receptor agonists on neuronally-evoked contractions of urinary bladder tissues isolated from rat, mouse, pig, dog, monkey and human

Author

Renee Sharon Martin, S J MacLennan, Richard M. Eglen, L. A. Luong, N J Welsh, and Graeme R. Martin

Subjects

Pharmacology, Agonist, education.field_of_study, medicine.medical_specialty, Cannabinoid receptor, medicine.drug_class, medicine.medical_treatment, Population, Cannabinoid Receptor Agonists, Biology, Endocrinology, Internal medicine, JWH-015, medicine, Cannabinoid receptor type 2, HU-210, Cannabinoid, education, medicine.drug

Abstract

This study investigated the cannabinoid receptor, known to inhibit neuronally-evoked contractions of the mouse isolated urinary bladder, in bladder sections isolated from mouse, rat, dog, pig non-human primate or human. The CB(1)-like pharmacology of the cannabinoid receptor in mouse isolated bladder observed previously was confirmed in this study by the rank order of agonist potencies: CP 55940>/=WIN 55212-2>HU 210>JWH 015>anandamide, the high affinity of the CB(1) selective antagonist, SR 141716A (apparent pK(B) 8.7), and the low affinity of the CB(2) antagonist, SR 144528 (apparent pK(B) or =WIN 55212-2>JWH 015). In this tissue, the maximal inhibitory effect of all agonists was lower than in the mouse bladder. Indeed, the effects of both HU 210 and anandamide were too modest to quantify potency accurately. In the rat isolated bladder, SR 141716A (30 nM) or SR 144528 (100 nM), reversed the inhibitory effect of WIN 55212-2 (apparent pK(B) = 8.4 and 8.0, respectively) or JWH 015 (apparent pK(B) = 8.2 and 7.4, respectively). These findings may demonstrate pharmacological differences between the rat and mouse orthologues of the CB(1) receptor. Alternatively, they may be attributed to a mixed population of CB(1) and CB(2) receptors that jointly influence neurogenic contraction of the rat bladder, but cannot be differentiated without more selective ligands. WIN 55212-2 had no effect on electrically-evoked contractions of bladder sections isolated from dog, pig, cynomolgus monkey and human. These findings suggest that the effect of cannabinoid agonists to inhibit neurogenic contraction of the mouse and rat bladder is not conserved across all mammalian species.

Published

2000

4. Mechanism of subendocardial cell proliferation in the rat and relevance for understanding drug-induced valvular heart disease in humans

Author

Mary Hassani, Hirdesh Uppal, Kyle L. Kolaja, Xingrong Liu, Rosario Garrido, Donald Button, Mark R. Fielden, Patricia Ann Day-Lollini, and Renee Sharon Martin

Subjects

Agonist, Male, medicine.medical_specialty, medicine.drug_class, Fenfluramine, Heart Valve Diseases, Biology, Toxicology, Pathology and Forensic Medicine, In vivo, Transforming Growth Factor beta, Internal medicine, Receptor, Serotonin, 5-HT2B, medicine, Animals, Humans, Proliferation Marker, Smad3 Protein, Rats, Wistar, Receptor, Cell Proliferation, Myocardium, Cell Biology, General Medicine, 5-HT2B receptor, Rats, Endocrinology, Ki-67 Antigen, Animal studies, Immunostaining, Serotonin 5-HT2 Receptor Agonists, medicine.drug

Abstract

A number of drugs and drug candidates, including fenfluramine and ergot derivatives, are associated with valvulopathy in humans; however, these responses are poorly predicted from animal studies. In vitro and in vivo evidence suggests that these compounds exert their pathological effect through activation of serotonin 2B receptor (5HT2BR) signaling. However, the variable effect of fenfluramine and other 5HT2BR agonists in rodents has cast doubt on the relevance of animal findings to predicting human risk. Herein, a candidate compound, RO3013, induced subendocardial cell proliferation in the mitral and tricuspid valves in rats after only 3 days of daily dosing. Additionally, there was a treatment-related increase in immunostaining of the proliferation marker Ki67, and phosphorylated Smad3 in the heart indicative of TGFβ signaling co-localized with 5HT2BR expression. To substantiate the hypothesis that RO3013-induced valvular proliferation is secondary to 5HT2BR activation, the compound was evaluated in vitro and found to bind to the human 5HT2BR with a K i of 3.8 μM; however, it was virtually devoid of agonist activity in a functional assay in human cells. By contrast, RO3013 bound to the rat 5HT2BR with a K i of 1.2 μM and activated the receptor with an EC50 of 0.5 μM. This agonist potency estimate is in good agreement with the free plasma concentrations of RO3013 at which valvular proliferation was observed. These results suggest that the rat may be susceptible to 5HT2BR-mediated valvular proliferation similar to humans; yet, the significant differences between binding and functional activities can be a possible explanation for the observed species-selective receptor responses.

Published

2009

5. Kinetic and thermodynamic assessment of binding of serotonin transporter inhibitors

Author

Subbu Apparsundaram, Zhongjiang Jia, Becky Leung, Marcos E. Milla, Alexander Suen, Robert Henningsen, Renee Sharon Martin, and Rama K. Kondru

Subjects

Conformational change, Stereochemistry, Entropy, Enthalpy, Static Electricity, Plasma protein binding, Citalopram, Polar surface area, Radioligand Assay, Humans, Pharmacology, Serotonin Plasma Membrane Transport Proteins, Chemistry, Temperature, Ligand (biochemistry), Antidepressive Agents, Kinetics, Fluvoxamine, Molecular Medicine, Thermodynamics, Hydrophobic and Hydrophilic Interactions, Selective Serotonin Reuptake Inhibitors, Entropy (order and disorder), Protein Binding

Abstract

Several serotonin reuptake inhibitors are in clinical use for treatment of depression and anxiety disorders. However, to date, reported pharmacological differentiation of these ligands has focused mainly on their equilibrium binding affinities for the serotonin transporter. This study takes a new look at antidepressant binding modes using radioligand binding assays with [(3)H]S-citalopram to determine equilibrium and kinetic rate constants across multiple temperatures. The observed dissociation rate constants at 26 degrees C fall into a narrow range for all molecules. Conversely, association rate constants generally decreased with increasing equilibrium binding affinities. Consistent with this, the measured activation energy for S-citalopram association was relatively large (19.5 kcal . mol(-1)), suggesting conformational change upon ligand binding. For most of the drugs, including citalopram, the enthalpy (DeltaH(O)) and entropy (-TDeltaS(O)) contributions to reaction energetics were determined by van't Hoff analyses to be roughly equivalent (25-75% DeltaG(O)) and to correlate (positively for enthalpy) with the polar surface area of the drug. However, the binding of the drug fluvoxamine was predominantly entropically driven. When these data are considered in the context of the physicochemical properties of these ligands, two distinct binding modes can be proposed. The citalopram-type binding mode probably uses a polar binding pocket that allows charged or polar interactions between ligand and receptor with comparatively small loss in enthalpy due to dehydration. The fluvoxamine-type binding mode is fueled by energy released upon burying hydrophobic ligand moieties into a binding pocket that is flexible enough to suffer minimal loss in entropy from conformational constraint.

Published

2008

6. Antidepressants targeting the serotonin reuptake transporter act via a competitive mechanism

Author

Subbu Apparsundaram, Robert Henningsen, Daniel J. Stockdale, Marcos E. Milla, and Renee Sharon Martin

Subjects

medicine.medical_specialty, Serotonin, Fluvoxamine, Venlafaxine, Pharmacology, Citalopram, DASB, Binding, Competitive, chemistry.chemical_compound, Radioligand Assay, Internal medicine, Radioligand, medicine, Animals, Humans, Serotonin transporter, Cerebral Cortex, Serotonin Plasma Membrane Transport Proteins, biology, Chemistry, Cell Membrane, Antidepressive Agents, Rats, Endocrinology, Indatraline, biology.protein, Molecular Medicine, Selective Serotonin Reuptake Inhibitors, medicine.drug

Abstract

Although several antidepressants (including fluoxetine, imipramine, citalopram, venlafaxine, and duloxetine) are known to inhibit the serotonin transporter (SERT), whether or not these molecules compete with 5-hydroxytryptamine (serotonin) (5-HT) for binding to SERT has remained controversial. We have performed radioligand competition binding experiments and found that all data can be fitted via a simple competitive interaction model, using Cheng-Prusoff analysis ( Biochem Pharmacol 22:3099–3108, 1973). Two different SERT-selective radioligands, [ 3 H] N , N -dimethyl-2-(2-amino-4-cyanophenyl thio)-benzylamine (DASB) and [ 3 H] S -citalopram, were used to probe competitive binding to recombinantly expressed human SERT or native SERT in rat cortical membranes. All the SERT inhibitors that we tested were able to inhibit [ 3 H]DASB and [ 3 H] S -citalopram binding in a concentration-dependent manner, with unity Hill coefficient. In accordance with the Cheng-Prusoff relationship for a competitive interaction, we observed that test compound concentrations associated with 50% maximal inhibition of radiotracer binding (IC 50 ) increased linearly with increasing radioligand concentration for all ligands: 5-HT, S -citalopram, R -citalopram, paroxetine, clomipramine, fluvoxamine, imipramine venlafaxine, duloxetine, indatraline, cocaine, and 2-β-carboxy-3-β-(4-iodophenyl)tropane. The equilibrium dissociation constant of 5-HT and SERT inhibitors were also derived using Scatchard analysis of the data set, and they were found to be comparable with the data obtained using the Cheng-Prusoff relationship. Our studies establish a reference framework that will contribute to ongoing efforts to understand ligand binding modes at SERT by demonstrating that 5-HT and the SERT inhibitors tested bind to the serotonin transporter in a competitive manner.

Published

2008

7. Kinetic and thermodynamic assessment of binding of serotonin transporter (SERT) inhibitors

Author

A Suen, D Stockdale, Renee Sharon Martin, Robert Henningsen, Marcos E. Milla, and Subbu Apparsundaram

Subjects

biology, Biochemistry, Chemistry, Genetics, biology.protein, Molecular Biology, Serotonin transporter, Biotechnology

Published

2008

8. Attenuated Response to Stress and Novelty and Hypersensitivity to Seizures in 5-HT4 Receptor Knock-Out Mice

Author

Russell A. Gazzara, Renee Sharon Martin, Valérie Compan, Daniela Brunner, Aline Dumuis, René Hen, Mingming Zhou, Joël Bockaert, Régis Grailhe, Jay A. Gingrich, UFR Sciences de la Vie, de la Terre et de l'Environnement (Université de Bourgogne) ( UFR SVTE ), Université de Bourgogne ( UB ), Columbia University [New York], UFR Sciences de la Vie, de la Terre et de l'Environnement (Université de Bourgogne) (UFR SVTE), and Université de Bourgogne (UB)

Subjects

medicine.medical_specialty, [SDV.NEU.NB]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, 5-HT4 receptor, Convulsants, Anorexia, Environment, Eating, Mice, 03 medical and health sciences, 0302 clinical medicine, Seizures, Stress, Physiological, Neurobiology of Disease, Internal medicine, Hypophagia, medicine, Biological neural network, Animals, Receptor, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Behavior, Animal, General Neuroscience, Body Weight, Novelty, Null allele, Endocrinology, [ SDV.NEU.NB ] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, Gene Targeting, Knockout mouse, Pentylenetetrazole, Receptors, Serotonin, 5-HT4, Nerve Net, medicine.symptom, Psychology, Neuroscience, Locomotion, 030217 neurology & neurosurgery

Abstract

To study the functions of 5-HT4receptors, a null mutation was engineered in the corresponding gene. 5-HT4receptor knock-out mice displayed normal feeding and motor behaviors in baseline conditions but abnormal feeding and locomotor behavior in response to stress and novelty. Specifically, stress-induced hypophagia and novelty-induced exploratory activity were attenuated in the knock-out mice. In addition, pentylenetetrazol-induced convulsive responses were enhanced in the knock-out mice, suggesting an increase in neuronal network excitability. These results provide the first example of a genetic deficit that disrupts the ability of stress to reduce feeding and body weight and suggest that 5-HT4receptors may be involved in stress-induced anorexia and seizure susceptibility.

Published

2004

9. A 5-HT4 Receptor Transmembrane Network Implicated in the Activity of Inverse Agonists but Not Agonists*

Author

Michèle Sebben, Robin D. Clark, Aline Dumuis, Joël Bockaert, Sylvie Claeysen, Renee Sharon Martin, Anne-Sophie Bessis, Lara Joubert, Centre CNRS-INSERM de Pharmacologie Endocrinologie (CCIPE), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and Neurobiology Unit, Roche Bioscience

Subjects

Agonist, Models, Molecular, medicine.drug_class, [SDV]Life Sciences [q-bio], medicine.disease_cause, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, medicine, Inverse agonist, Animals, Serotonin Antagonists, Receptor, Molecular Biology, 030304 developmental biology, DNA Primers, 0303 health sciences, Mutation, biology, Base Sequence, Chemistry, 030302 biochemistry & molecular biology, Cell Biology, Transmembrane protein, Serotonin Receptor Agonists, Transmembrane domain, Rhodopsin, Receptors, Serotonin, COS Cells, biology.protein, Biophysics, Receptors, Serotonin, 5-HT4, 030217 neurology & neurosurgery

Abstract

International audience; Activation of G protein-coupled receptors is thought to involve disruption of intramolecular interactions that stabilize their inactive conformation. Such disruptions are induced by agonists or by constitutively active mutations. In the present study, novel potent inverse agonists are described to inhibit the constitutive activity of 5-HT 4 receptors. Using these compounds and specific receptor mutations, we investigated the mechanisms by which inverse agonists may reverse the disruption of intramolecular interactions that causes constitutive activation. Two mutations (D100 3.32 A in transmembrane domain (TMD)-III and F275 6.51 A in TMD-VI) were found to completely block inverse agonist effects without impairing their binding properties nor the molecular activation switches induced by agonists. Based on the rhodopsin model, we propose that these mutated receptors are in equilibrium between two states R and R* but are unable to reach a third "silent" state stabilized by inverse agonists. We also found another mutation in TMD-VI (W272 6.48 A) that stabilized this silent state. This mutant remained fully activated by agonists. Molecular modeling indicated that Asp-100, Phe-275, and Trp-272 might constitute a network required for stabilization of the silent state by the described inverse agonists. However, this network is not necessary for agonist activity.

Published

2002

10. Pharmacological comparison of a recombinant CB1 cannabinoid receptor with its G(alpha 16) fusion product

Author

Joyce J. Calixto, Stephen J. Maclennan, Renee Sharon Martin, Paul Shartzer Dietrich, Christian L. Reyes, Paul H. Reynen, Douglas W. Bonhaus, and Thomas Chang

Subjects

G protein, Receptors, Drug, Recombinant Fusion Proteins, Biology, Sulfur Radioisotopes, Tritium, Biochemistry, Analytical Chemistry, Cannabinoid receptor type 2, Enzyme-linked receptor, Cyclic AMP, Humans, 5-HT5A receptor, Receptors, Cannabinoid, G protein-coupled receptor, G protein-coupled receptor kinase, Cyclohexanols, G protein-coupled bile acid receptor, Molecular biology, Heterotrimeric GTP-Binding Proteins, GPR119, Guanosine 5'-O-(3-Thiotriphosphate), Molecular Medicine, GTP-Binding Protein alpha Subunits, Gq-G11, Calcium, Biotechnology

Abstract

The pharmacology of G protein-coupled receptors is widely accepted to depend on the G protein subunit to which the agonist-stimulated receptor couples. In order to investigate whether CB(1) agonist-mediated signal transduction via an engineered G(alpha 16) system is different than that of the G(i/o) coupling normally preferred by the CB(1) receptor, we transfected the human recombinant CB(1) receptor (hCB(1)) or a fusion protein comprising the hCB(1) receptor and G(alpha 16) (hCB(1)-G(alpha 16)) into HEK293 cells. From competition binding studies, the rank order of ligand affinities at the hCB(1)-G(alpha 16) fusion protein was found to be similar to that for hCB(1): HU 210 > CP 55,940 > or = SR 141716A > WIN 55212-2 > anandamide > JWH 015. Agonists increased [(35)S]GTP gamma S binding or inhibited forskolin-stimulated cAMP, presumably by coupling to G(i/o), in cells expressing hCB(1) but not hCB(1)-G(alpha 16). However, an analogous rank order of potencies was observed for these agonists in their ability to evoke increases in intracellular calcium concentration in cells expressing hCB(1)-G(alpha 16) but not hCB(1). These data demonstrate that ligand affinities for the hCB(1) receptor are not affected by fusion to the G(alpha 16) subunit. Furthermore, there is essentially no difference in the function of the hCB(1) receptor when coupled to G(i/o) or G (alpha 16).

Published

2002

11. Thermodynamic analysis of P2X7 purinoceptor ligand binding

Author

Subbu Apparsundaram, Joel R Gever, Renee Sharon Martin, David H Hackos, Patrick Weber, Marcos E. Milla, Sandip Panicker, and Robert Henningsen

Subjects

Chemistry, Stereochemistry, Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2008

12. Electrophysiological determination of antagonist mechanism of action at a P2X2‐3 chimeric receptor

Author

David H Hackos, Robert Henningsen, Joel R Gever, Renee Sharon Martin, Sandip Panicker, and Rothschild Soto

Subjects

Electrophysiology, Mechanism of action, Chemistry, Genetics, medicine, Antagonist, medicine.symptom, Pharmacology, Receptor, Molecular Biology, Biochemistry, Biotechnology

Published

2008

13. Selective 5HT(2A) and 5HT(6) receptor antagonists promote sleep in rats

Author

Renee Sharon Martin, Linda Hedley, Judith Flores, Thomas S. Kilduff, and Stephen R. Morairty

Subjects

Male, medicine.medical_specialty, Zolpidem, Indoles, medicine.drug_class, Rapid eye movement sleep, Sleep, REM, Serotonergic Mechanisms and Sleep, Non-rapid eye movement sleep, Piperazines, Body Temperature, Hypnotic, Rats, Sprague-Dawley, Piperidines, Physiology (medical), Internal medicine, medicine, Animals, Wakefulness, Behavior, Animal, musculoskeletal, neural, and ocular physiology, Antagonist, Sleep in non-human animals, Rats, Fluorobenzenes, Endocrinology, Receptors, Serotonin, Serotonin 5-HT2 Receptor Antagonists, Neurology (clinical), Serotonin, Psychology, psychological phenomena and processes, medicine.drug

Abstract

Study objectives Serotonin (5-HT) has long been implicated in the control of sleep and wakefulness. This study evaluated the hypnotic efficacy of the 5-HT6 antagonist RO4368554 (RO) and the 5-HT2A receptor antagonist MDL100907 (MDL) relative to zolpidem. Design A randomized, repeated-measures design was utilized in which Wistar rats received intraperitoneal injections of RO (1.0, 3.0, and 10 mg/kg), MDL (0.1, 1.0 and 3.0 mg/kg), zolpidem (10 mg/kg), or vehicle in the middle of the dark (active) period. Electroencephalogram, electromyogram, body temperature (Tb) and locomotor activity were analyzed for 6 hours after injection. Measurements and results RO, MDL, and zolpidem all produced significant increases in sleep and decreases in waking, compared with vehicle control. All 3 doses of MDL produced more consolidated sleep, increased non-rapid eye movement sleep (NREM) sleep, and increased electroencephalographic delta power during NREM sleep. The highest dose of RO (10.0 mg/kg) produced significant increases in sleep and decreases in waking during hour 2 following dosing. These increases in sleep duration were associated with greater delta power during NREM sleep. ZO Zolpidem induced sleep with the shortest latency and significantly increased NREM sleep and delta power but also suppressed rapid eye movement sleep sleep; in contrast, neither RO nor MDL affected rapid eye movement sleep. Whereas RO did not affect Tb, both zolpidem and MDL reduced Tb relative to vehicle-injected controls. Conclusions These results support a role for 5-HT2A receptor modulation in NREM sleep and suggest a previously unrecognized role for 5-HT6 receptors in sleep-wake regulation.