Your search keyword '"Lisa Dvorak"' showing total 16 results

1. High-affinity agonists reveal recognition motifs for the MRGPRD GPCR

Author

Chunyu Wang, Yongfeng Liu, Marion Lanier, Adam Yeager, Isha Singh, Ryan H. Gumpper, Brian E. Krumm, Chelsea DeLeon, Shicheng Zhang, Marcus Boehm, Richard Pittner, Alain Baron, Lisa Dvorak, Corinne Bacon, Brian K. Shoichet, Esther Martinborough, Jonathan F. Fay, Can Cao, and Bryan L. Roth

Subjects

CP: Molecular biology, Biology (General), QH301-705.5

Abstract

Summary: The human MRGPRD protein is a member of the Mas-related G protein-coupled receptors (MRGPRs) that is involved in the sensing of pain, itch, and other inflammatory stimuli. As with other MRGPRs, MRGPRD is a relatively understudied receptor with few known agonists. The most potent small-molecule agonist of MRGPRD reported so far is β-alanine, with an affinity in the micromole range, which largely restricts its functional study. Here, we report two MRGPRD agonists, EP-2825 and EP-3945, that are approximately 100-fold more potent than β-alanine and determine the structures of MRGPRD-Gq in complex with EP-2825 and EP-3945, respectively. The structures reveal distinct agonist binding modes of MRGPRD and large conformational plasticity of the orthosteric pocket. Collectively, the discovery of high-affinity MRGPRD agonists and their distinct binding modes will facilitate the functional study and the structure-based design of ligands targeting this understudied receptor.

Published

2024

2. Discovery and SAR studies of 2-alkyl-3-phenyl-2,4,5,6,7,8-hexahydropyrazolo[3,4-d]azepines as 5-HT

Author

Curt A, Dvorak, Dale A, Rudolph, Diane, Nepomuceno, Lisa, Dvorak, Brian, Lord, Ian, Fraser, Pascal, Bonaventure, Timothy, Lovenberg, and Nicholas I, Carruthers

Subjects

Dose-Response Relationship, Drug, Molecular Structure, Azepines, Haplorhini, Rats, Mice, Structure-Activity Relationship, Dogs, Receptors, Serotonin, Drug Discovery, Animals, Humans, Serotonin Antagonists, Receptors, Serotonin, 5-HT2

Abstract

We report here the synthesis and characterization of a dual 5-HT

Published

2020

3. Discovery and SAR studies of 2-alkyl-3-phenyl-2,4,5,6,7,8-hexahydropyrazolo[3,4-d]azepines as 5-HT7/2 inhibitors leading to the identification of a clinical candidate

Author

Pascal Bonaventure, Brian Lord, Ian Fraser, Curt A. Dvorak, Nicholas I. Carruthers, Dale A. Rudolph, Timothy W. Lovenberg, Diane Nepomuceno, and Lisa Dvorak

Subjects

010405 organic chemistry, 5-HT2A receptor, medicine.drug_class, Chemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Ligand (biochemistry), Receptor antagonist, 01 natural sciences, Biochemistry, 0104 chemical sciences, 5-HT7 receptor, 010404 medicinal & biomolecular chemistry, In vivo, Drug Discovery, medicine, Molecular Medicine, Inverse agonist, Receptor, Molecular Biology, Ex vivo

Abstract

We report here the synthesis and characterization of a dual 5-HT7 / 5-HT2 receptor antagonist 3-(4-Fluoro-phenyl)-2-isopropyl-2,4,5,6,7,8-hexahydro-1,2,6-triaza-azulene (4j). 4j is a high affinity 5-HT7 and 5-HT2A receptor ligand having a pKi = 8.1 at both receptors. It behaves as an antagonist in an in vitro functional assay for 5-HT2A and as an inverse agonist in an in vitro functional assay for 5-HT7. In a validated in vivo model for central 5-HT7 activity in rats, blockade of 5-carboxamidotryptamine (5-CT) induced hypothermia, 4j shows efficacy at low doses (ED50 = 0.05 mg/kg, p.o., 1 h) and maximal efficacy was observed at 0.3 mg/kg p.o. with a corresponding plasma concentration of ~27 ng/ml. In a validated in vivo model for central 5-HT2A activity, blockade of 2,5-dimethoxy-4-iodoamphetamine (DOI) induced head-twitches in mice, 4j shows efficacy at low doses with an ED50 = 0.3 mg/kg p.o. Ex vivo receptor binding studies demonstrate that 4j occupied 5-HT2A receptor binding sites in the frontal cortex of the rat brain with an ED50 in good agreement with the ED50 value for central functional effect mediated by 5-HT2A receptor (ED50 = 0.8 mg/kg, p.o., 1 h).

Published

2021

4. The discovery and synthesis of JNJ 31020028, a small molecule antagonist of the Neuropeptide Y Y2 receptor

Author

Pascal Bonaventure, Jill A. Jablonowski, Timothy W. Lovenberg, John R. Atack, Swanson Devin M, Curt A. Dvorak, Mark Seierstad, Lisa Dvorak, Diane Nepomuceno, Dale A. Rudolph, Victoria D. Wong, Nicholas I. Carruthers, Chandra R. Shah, and Kirsten L. Morton

Subjects

Neuropeptide Y receptor Y1, Neuropeptide Y receptor Y2, Chemistry, medicine.drug_class, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Receptor antagonist, Neuropeptide Y receptor, Biochemistry, Combinatorial chemistry, Small molecule, Drug Discovery, medicine, Molecular Medicine, Racemic mixture, Enantiomer, Molecular Biology

Abstract

A series of small molecules based on a chemotype identified from our compound collection were synthesized and tested for binding affinity (IC50) at the human Neuropeptide Y Y2 receptor (NPY Y2). Six of the 23 analogs tested possessed an NPY Y2 IC50 ⩽ 15 nM. One member of this series, JNJ 31020028, is a selective, high affinity, receptor antagonist existing as a racemic mixture. As such a synthetic route to the desired enantiomer was designed starting from commercially available (S)-(+)-mandelic acid.

Published

2011

5. Heterocyclic replacement of the central phenyl core of diamine-based histamine H3 receptor antagonists

Author

Timothy W. Lovenberg, Lisa Dvorak, Jamin D. Boggs, Brian Lord, Curt Mazur, Swanson Devin M, Pascal Bonaventure, Richard Apodaca, Chandra R. Shah, Kirsten L. Morton, Ann J. Barbier, Mark A. Feinstein, Sandy J. Wilson, Nicholas I. Carruthers, and Wei Xiao

Subjects

Pharmacology, Pyrazine, Stereochemistry, Organic Chemistry, General Medicine, Diamines, Cell Line, Rats, Rats, Sprague-Dawley, chemistry.chemical_compound, chemistry, Blood-Brain Barrier, Drug Discovery, Thiophene, Animals, Humans, Receptors, Histamine H3, Histamine H3 receptor, Isoxazole, Thiazole, H3 receptor antagonist, Histamine H3 Antagonists, Protein Binding, Pyrrole, Oxazole

Abstract

A series of small molecules consisting of a heterocyclic core flanked by two basic functionalities were synthesized and screened for in vitro affinity at the human histamine H 3 receptor (hH 3 R). Nine of the twenty-eight compounds tested were found to possess a hH 3 R K i of less than 5 nM and consisted of a diverse range of central hetero-aromatic linkers (pyridine, pyrazine, oxazole, isoxazole, thiazole, furan, thiophene, and pyrrole). One member of this series, (4-isopropyl-piperazin-1-yl)-(6-piperidin-1-ylmethyl-pyridin-3-yl)-methanone ( 37 ), was found to be a high affinity, selective antagonist that crosses the blood-brain barrier and occupies H 3 receptors after oral administration in the rat.

Published

2009

6. Novel imidazole-based histamine H3 antagonists

Author

Lisa Dvorak, Curt A. Dvorak, Curt Mazur, Kiev S. Ly, Michael Bogenstaetter, Jill A. Jablonowski, Brian Lord, Timothy W. Lovenberg, Jamin D. Boggs, Kirsten L. Miller, Nicholas I. Carruthers, and Sandy J. Wilson

Subjects

Stereochemistry, Chemistry, Pharmaceutical, Guinea Pigs, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Ligands, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Biogenic amine, Drug Discovery, Animals, Humans, Imidazole, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Imidazoles, Antagonist, Brain, In vitro, Rats, Models, Chemical, chemistry, Blood-Brain Barrier, Drug Design, Molecular Medicine, Histamine H3 receptor, Histamine, Histamine H3 Antagonists, Protein Binding

Abstract

A novel series of imidazole containing histamine H3 receptor ligands were investigated and found to be potent functional antagonists. After improving the stability of these molecules towards liver microsomes, these compounds were found to have no appreciable affinity for CYP P450s. Subsequent in vivo experiments showed significant brain uptake of (4-chloro-phenyl)-[2-(1-isopropyl-piperidin-4-ylmethoxy)-3-methyl-3H-imidazol-4-yl]-methanone 22.

Published

2009

7. In-vitro and in-vivo characterization of JNJ-7925476, a novel triple monoamine uptake inhibitor

Author

Jamin D. Boggs, Brian Lord, Bruce E. Maryanoff, Lisa Dvorak, Leah Aluisio, Pascal Bonaventure, Timothy W. Lovenberg, Michael A. Letavic, Nicholas I. Carruthers, Sandy J. Wilson, Ian Fraser, and Ann J. Barbier

Subjects

Male, medicine.medical_specialty, Microdialysis, Motor Activity, Pharmacology, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Dopamine, Cell Line, Tumor, Internal medicine, medicine, Animals, Humans, Neurotransmitter Uptake Inhibitors, Pyrroles, Neurotransmitter, Serotonin transporter, Dopamine transporter, Brain Chemistry, Cerebral Cortex, Serotonin Plasma Membrane Transport Proteins, Dopamine Plasma Membrane Transport Proteins, biology, Chemistry, Stereoisomerism, Isoquinolines, Rats, Mice, Inbred C57BL, Monoamine neurotransmitter, Endocrinology, Hindlimb Suspension, Norepinephrine transporter, Blood-Brain Barrier, Area Under Curve, biology.protein, Autoradiography, Serotonin, Reuptake inhibitor, medicine.drug

Abstract

Triple reuptake inhibitors, which block the serotonin transporter (SERT), norepinephrine transporter (NET) and dopamine transporter (DAT) in the central nervous system have been described as therapeutic alternatives for classical selective serotonin reuptake inhibitors, with advantages due to their multiple mechanisms of action. JNJ-7925476 (trans-6-(4-ethynylphenyl)-1,2,3,5,6,10b-hexahydropyrrolo[2,1-a]isoquinoline) is a selective and potent inhibitor of the SERT, NET, and DAT (K(i)=0.9, 17 and 5.2 nM, respectively). Following subcutaneous dosing in rat, JNJ-7925476 was rapidly absorbed into the plasma, and drug concentrations in the brain tracked with those in the plasma but were 7-fold higher. The ED(50) values for JNJ-7925476 occupancy of the SERT, NET, and DAT in rat brain were 0.18, 0.09 and 2.4 mg/kg, respectively. JNJ-7925476 (0.1-10 mg/kg, s.c.) rapidly induced a robust, dose-dependent increase in extracellular serotonin, dopamine, and norepinephrine levels in rat cerebral cortex. The compound also showed potent antidepressant-like activity in the mouse tail suspension test (ED(50)=0.3 mg/kg, i.p.). These results demonstrate that JNJ-7925476 is a triple reuptake inhibitor with in-vivo efficacy in biochemical and behavioral models of depression.

Published

2008

8. Synthesis and biological activity of piperazine and diazepane amides that are histamine H3 antagonists and serotonin reuptake inhibitors

Author

Xiaohui Jiang, Kirsten L. Miller, Emily M. Stocking, Lisa Dvorak, Nicholas I. Carruthers, Jamin D. Boggs, Kiev S. Ly, Sandy J. Wilson, Brian Lord, Michael A. Letavic, Diane Nepomuceno, Jennifer M. Miller, John M. Keith, Pascal Bonaventure, and Ann J. Barbier

Subjects

Serotonin reuptake inhibitor, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Biochemistry, Chemical synthesis, Piperazines, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Neurotransmitter, Molecular Biology, Organic Chemistry, Brain, Biological activity, Azepines, Amides, Rats, Piperazine, chemistry, Molecular Medicine, Serotonin, Reuptake inhibitor, Selective Serotonin Reuptake Inhibitors, Histamine, Histamine H3 Antagonists

Abstract

The synthesis and biological activity of a new series of piperazine and diazepane amides is described. The new compounds are high affinity histamine H 3 ligands and serotonin reuptake inhibitors.

Published

2008

9. Translational evaluation of JNJ-18038683, a 5-hydroxytryptamine type 7 receptor antagonist, on rapid eye movement sleep and in major depressive disorder

Author

Lisa Dvorak, Kirk Bertelsen, Wenying Chai, Brian Lord, Pascal Bonaventure, Ian Fraser, Leah Aluisio, Christine Dugovic, Timothy W. Lovenberg, Wilhelmus Drinkenburg, Jonathan Shelton, Peter de Boer, Jianing Di, Steve Sands, Nicholas J. Carruthers, Curt A. Dvorak, Jaskaran Singh, Diane Nepomuceno, Michelle Kramer, Abdellah Ahnaou, and Sue Wilson

Subjects

Adult, Male, Serotonin, Adolescent, medicine.drug_class, Rapid eye movement sleep, Sleep, REM, Hypothermia, Pharmacology, Citalopram, Placebo, Cohort Studies, Rats, Sprague-Dawley, Mice, Young Adult, Double-Blind Method, mental disorders, medicine, Escitalopram, Animals, Humans, Cell Line, Transformed, Depressive Disorder, Major, Cross-Over Studies, Tricarboxylic Acids, Azepines, Middle Aged, medicine.disease, Receptor antagonist, Sleep in non-human animals, Tail suspension test, Antidepressive Agents, Rats, Mice, Inbred C57BL, HEK293 Cells, Hindlimb Suspension, Anesthesia, Receptors, Serotonin, Molecular Medicine, Major depressive disorder, Female, Serotonin Antagonists, Psychology, medicine.drug

Abstract

In rodents 5-hydroxytryptamine type 7 (5-HT(7)) receptor blockade has been shown to be effective in models of depression and to increase the latency to rapid eye movement (REM) sleep and decrease REM duration. In the clinic, the REM sleep reduction observed with many antidepressants may serve as a biomarker. We report here the preclinical and clinical evaluation of a 5-HT(7) receptor antagonist, (3-(4-chlorophenyl)-1,4,5,6,7,8-hexahydro-1-(phenylmethyl)pyrazolo[3,4-d]azepine 2-hydroxy-1,2,3-propanetricarboxylate) (JNJ-18038683). In rodents, JNJ-18038683 increased the latency to REM sleep and decreased REM duration, and this effect was maintained after repeated administration for 7 days. The compound was effective in the mouse tail suspension test. JNJ-18038683 enhanced serotonin transmission, antidepressant-like behavior, and REM sleep suppression induced by citalopram in rodents. In healthy human volunteers JNJ-18038683 prolonged REM latency and reduced REM sleep duration, demonstrating that the effect of 5-HT(7) blockade on REM sleep translated from rodents to humans. Like in rats, JNJ-18038683 enhanced REM sleep suppression induced by citalopram in humans, although a drug-drug interaction could not be ruled out. In a double-blind, active, and placebo-controlled clinical trial in 225 patients suffering from major depressive disorder, neither treatment with pharmacologically active doses of JNJ-18038683 or escitalopram separated from placebo, indicating a failed study lacking assay sensitivity. Post hoc analyses using an enrichment window strategy, where all the efficacy data from sites with an implausible high placebo response [placebo group Montgomery-Åsberg Depression Rating Scale (MADRS)= 12] and from sites with no placebo response (MADRS= 28) are removed, there was a clinically meaningful difference between JNJ-18038683 and placebo. Further clinical studies are required to characterize the potential antidepressant efficacy of JNJ-18038683.

Published

2012

10. Novel tetrahydropyrido[3,2-c]pyrroles as 5-HT(7) antagonists

Author

Timothy W. Lovenberg, Dale A. Rudolph, Diane Nepomuceno, Curt A. Dvorak, Nicholas I. Carruthers, Lisa Dvorak, and Pascal Bonaventure

Subjects

Stereochemistry, Aryl, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Ring (chemistry), Biochemistry, Rats, Para position, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Receptors, Serotonin, Drug Discovery, Molecular Medicine, Animals, Amine gas treating, Pyrroles, Serotonin Antagonists, Receptor, Molecular Biology, Protein Binding

Abstract

The synthesis and SAR for a novel series of tetrahydropyrido[3,2-c]pyrroles is described. Optimization of the pendant aryl ring lead to high binding affinity at the 5-HT7 receptor when small lipophilic groups were placed in the para position. Modification of the N-benzyl group and secondary amine were not well tolerated. A representative set of compounds was shown to be functional antagonists of the 5-HT7 receptor.

Published

2010

11. In vitro and in vivo characterization of JNJ-31020028 (N-(4-{4-[2-(diethylamino)-2-oxo-1-phenylethyl]piperazin-1-yl}-3-fluorophenyl)-2-pyridin-3-ylbenzamide), a selective brain penetrant small molecule antagonist of the neuropeptide Y Y(2) receptor

Author

Curt A. Dvorak, S. Timothy Motley, Timothy W. Lovenberg, Leah Aluisio, Diane Nepomuceno, Kirsten L. Morton, John R. Atack, Steve W. Sutton, Pascal Bonaventure, Nicholas I. Carruthers, Ian Fraser, Lisa Dvorak, Swanson Devin M, Natalie Welty, Ruggero Galici, James R. Shoblock, and Brian Lord

Subjects

Male, Stereochemistry, Injections, Subcutaneous, Microdialysis, Administration, Oral, CHO Cells, Biology, Anxiety, Transfection, Binding, Competitive, Hippocampus, Permeability, Piperazines, Rats, Sprague-Dawley, chemistry.chemical_compound, Eating, Mice, Norepinephrine, Cricetulus, Vas Deferens, In vivo, Cricetinae, Animals, Humans, Peptide YY, Rats, Wistar, Receptor, Pharmacology, Dose-Response Relationship, Drug, Chinese hamster ovary cell, Antagonist, Feeding Behavior, Neuropeptide Y receptor, Small molecule, In vitro, Anorexia, Rats, Receptors, Neuropeptide Y, Disease Models, Animal, chemistry, Biochemistry, Anti-Anxiety Agents, Benzamides, Injections, Intravenous, Autoradiography, Calcium, Penetrant (biochemical), Corticosterone

Abstract

The lack of potent, selective, brain penetrant Y(2) receptor antagonists has hampered in vivo functional studies of this receptor.Here, we report the in vitro and in vivo characterization of JNJ-31020028 (N-(4-{4-[2-(diethylamino)-2-oxo-1-phenylethyl]piperazin-1-yl}-3-fluorophenyl)-2-pyridin-3-ylbenzamide), a novel Y(2) receptor antagonist.The affinity of JNJ-31020028 was determined by inhibition of the PYY binding to human Y(2) receptors in KAN-Ts cells and rat Y(2) receptors in rat hippocampus. The functional activity was determined by inhibition of PYY-stimulated calcium responses in KAN-Ts cells expressing a chimeric G protein Gqi5 and in the rat vas deferens (a prototypical Y(2) bioassay). Ex vivo receptor occupancy was revealed by receptor autoradiography. JNJ-31020028 was tested in vivo with microdialysis, in anxiety models, and on corticosterone release.JNJ-31020028 bound with high affinity (pIC(50) = 8.07 +/- 0.05, human, and pIC(50) = 8.22 +/- 0.06, rat) and was100-fold selective versus human Y(1), Y(4), and Y(5) receptors. JNJ-31020028 was demonstrated to be an antagonist (pK(B) = 8.04 +/- 0.13) in functional assays. JNJ-31020028 occupied Y(2) receptor binding sites (approximately 90% at 10 mg/kg) after subcutaneous administration in rats. JNJ-31020028 increased norepinephrine release in the hypothalamus, consistent with the colocalization of norepinephrine and neuropeptide Y. In a variety of anxiety models, JNJ-31020028 was found to be ineffective, although it did block stress-induced elevations in plasma corticosterone, without altering basal levels, and normalized food intake in stressed animals without affecting basal food intake.These results suggest that Y(2) receptors may not be critical for acute behaviors in rodents but may serve modulatory roles that can only be elucidated under specific situational conditions.

Published

2009

12. Diamine-based human histamine H3 receptor antagonists: (4-aminobutyn-1-yl)benzylamines

Author

Curt A. Dvorak, Richard Apodaca, Pascal Bonaventure, Kirsten L. Miller, Christine Dugovic, Lisa Dvorak, Jonathan Shelton, Wei Xiao, Jill A. Jablonowski, Brian Lord, Timothy W. Lovenberg, and Nicholas I. Carruthers

Subjects

Male, Benzylamines, Tertiary amine, Stereochemistry, Diamines, Chemical synthesis, Cell Line, Rats, Sprague-Dawley, chemistry.chemical_compound, Structure-Activity Relationship, Benzylamine, Diamine, Drug Discovery, Moiety, Animals, Humans, Receptors, Histamine H3, Wakefulness, Pharmacology, Organic Chemistry, General Medicine, Rats, chemistry, Amine gas treating, Histamine H3 receptor, Sleep, Histamine, Histamine H3 Antagonists, Protein Binding

Abstract

A series of (4-aminobutyn-1-yl)benzylamines were prepared and the SAR around three key areas: (1) the amine attached to the butynyl linker (R(3)R(4)N-); (2) the benzylamine moiety (R(1)R(2)N-); and (3) the point of attachment of the benzylamine group (R(1)R(2)N- in the ortho, meta, or para positions) was examined. One compound, 4-[3-(4-piperidin-1-yl-but-1-ynyl)-benzyl]-morpholine (9s) was chosen for further profiling and found to be a selective histamine H(3) antagonist with desirable drug-like properties. Ex vivo receptor occupancy studies established that 9s does occupy H(3) binding sites in the brain of rats after oral administration. Subcutaneous doses of 9s (10mg/kg) given during the natural sleep phase demonstrated robust wake-promoting effects.

Published

2009

13. 2-Alkyl-4-aryl-pyrimidine fused heterocycles as selective 5-HT2A antagonists

Author

Dale A. Rudolph, Curt A. Dvorak, Brock T. Shireman, Timothy W. Lovenberg, Nicholas I. Carruthers, Diane Nepomuceno, Pascal Bonaventure, Lisa Dvorak, and Kirsten L. Miller

Subjects

Pyrimidine, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, CHO Cells, Biochemistry, Chemical synthesis, Binding, Competitive, chemistry.chemical_compound, Mice, Radioligand Assay, Structure-Activity Relationship, Cricetulus, Cricetinae, Drug Discovery, Receptor, Serotonin, 5-HT2B, Serotonin 5-HT2 Receptor Antagonists, Receptor, Serotonin, 5-HT2C, Structure–activity relationship, Animals, Humans, Receptor, Serotonin, 5-HT2A, Serotonin Antagonists, Molecular Biology, Alkyl, chemistry.chemical_classification, Molecular Structure, Aryl, Organic Chemistry, Azepines, Pyrimidines, chemistry, NIH 3T3 Cells, Molecular Medicine, Selectivity

Abstract

The synthesis and SAR for a novel series of 2-alkyl-4-aryl-tetrahydro-pyrido-pyrimidines and 2-alkyl-4-aryl-tetrahydro-pyrimido-azepines is described. Representative compounds were shown to be subtype selective 5-HT(2A) antagonists. Optimal placement of a basic nitrogen relative to the pyrimidine and the presence of a 4-fluorophenyl group in the pyrimidine 4-position was found to have a profound effect on affinity and selectivity.

Published

2007

14. Lead identification of acetylcholinesterase inhibitors-histamine H3 receptor antagonists from molecular modeling

Author

Kirsten L. Miller, Scott D. Bembenek, Leah Aluisio, Nicholas I. Carruthers, Richard Apodaca, Timothy W. Lovenberg, Lisa Dvorak, Ann J. Barbier, Michael A. Letavic, and John M. Keith

Subjects

Models, Molecular, medicine.drug_class, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Quantitative Structure-Activity Relationship, Pharmacology, Biochemistry, chemistry.chemical_compound, Alzheimer Disease, Drug Discovery, medicine, Humans, Receptor, Molecular Biology, biology, Chemistry, Organic Chemistry, Antagonist, Receptor antagonist, Symptomatic relief, Acetylcholinesterase, Enzyme inhibitor, biology.protein, Molecular Medicine, Cholinesterase Inhibitors, Histamine H3 receptor, Histamine, Histamine H3 Antagonists

Abstract

Currently, the only clinically effective treatment for Alzheimer's disease (AD) is the use of acetylcholinesterase (AChE) inhibitors. These inhibitors have limited efficacy in that they only treat the symptoms and not the disease itself. Additionally, they often have unpleasant side effects. Here we consider the viability of a single molecule having the actions of both an AChE inhibitor and histamine H(3) receptor antagonist. Both histamine H(3) receptor antagonists and AChE inhibitors improve and augment cholinergic neurotransmission in the cortex. However, whereas an AChE inhibitor will impart its effect everywhere, a histamine H(3) antagonist will raise acetylcholine levels mostly in the brain as its mode of action will primarily be on the central nervous system. Therefore, the combination of both activities in a single molecule could be advantageous. Indeed, studies suggest an appropriate dual-acting compound may offer the desired therapeutic effect with fewer unpleasant side effects [CNS Drugs2004, 18, 827]. Further, recent studies(2) indicate the peripheral anionic site (PAS) of AChE interacts with the beta-amyloid (betaA) peptide. Consequently, a molecule capable of disrupting this interaction may have a significant impact on the production of or the aggregation of betaA. This may result in slowing down the progression of the disease rather than only treating the symptoms as current therapies do. Here, we detail how the use of the available crystal structure information, pharmacophore modeling and docking (automated, manual, classical, and QM/MM) lead to the identification of an AChE inhibitor-histamine H(3) receptor antagonist. Further, based on our models we speculate that this dual-acting compound may interact with the PAS. Such a dual-acting compound may be able to affect the pathology of AD in addition to providing symptomatic relief.

Published

2007

15. Pharmacological characterization of JNJ-28583867, a histamine H(3) receptor antagonist and serotonin reuptake inhibitor

Author

Lisa Dvorak, Leah Aluisio, Sandy J. Wilson, Cindy Pudiak, Kirsten L. Miller, Nicholas I. Carruthers, Brian Lord, Timothy W. Lovenberg, Ian Fraser, Ann J. Barbier, Pascal Bonaventure, Jamin D. Boggs, Jonathan Shelton, Christine Dugovic, Ying Qu, Michael A. Letavic, and Curt Mazur

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Serotonin reuptake inhibitor, Histamine Antagonists, CHO Cells, Pharmacology, Cell Line, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Cricetulus, Dogs, Internal medicine, Cricetinae, Tetrahydroisoquinolines, medicine, Animals, Humans, Receptors, Histamine H3, Neurotransmitter, Serotonin transporter, Serotonin Plasma Membrane Transport Proteins, Dopamine Plasma Membrane Transport Proteins, Mice, Inbred BALB C, Norepinephrine Plasma Membrane Transport Proteins, biology, Brain, Receptor antagonist, Tail suspension test, Rats, Endocrinology, chemistry, biology.protein, Serotonin, Reuptake inhibitor, Histamine, Selective Serotonin Reuptake Inhibitors

Abstract

Wake-promoting agents such as modafinil are used in the clinic as adjuncts to antidepressant therapy in order to alleviate lethargy. The wake-promoting action of histamine H(3) receptor antagonists has been evidenced in numerous animal studies. They may therefore be a viable strategy for use as an antidepressant therapy in conjunction with selective serotonin reuptake inhibitors. JNJ-28583867 (2-Methyl-4-(4-methylsulfanyl-phenyl)-7-(3-morpholin-4-yl-propoxy)-1,2,3,4-tetrahydro-isoquinoline) is a selective and potent histamine H(3) receptor antagonist (K(i)=10.6 nM) and inhibitor of the serotonin transporter (SERT) (K(i)=3.7 nM), with 30-fold selectivity for SERT over the dopamine and norepinephrine transporters. After subcutaneous administration, JNJ-28583867 occupied both the histamine H(3) receptor and the SERT in rat brain at low doses (

Published

2007

16. Corrigendum to '2-Alkyl-4-aryl-pyrimidine fused heterocycles as selective 5-HT2A antagonists' [Bioorg. Med. Chem. Lett. 18 (2008) 2103–2108]

Author

Lisa Dvorak, Diane Nepomuceno, Pascal Bonaventure, Curt A. Dvorak, Nicholas I. Carruthers, Dale A. Rudolph, Kirsten L. Miller, Timothy W. Lovenberg, and Brock T. Shireman

Subjects

chemistry.chemical_classification, Pyrimidine, Chemistry, Stereochemistry, Aryl, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, chemistry.chemical_compound, Drug Discovery, Molecular Medicine, Molecular Biology, Alkyl

Published

2008