Your search keyword '"Sharon Sadowski"' showing total 59 results

1. Cyclopentane-based human NK1 antagonists. Part 1: Discovery and initial SAR

Author

Gary G. Chicchi, Paul E. Finke, Joseph M. Metzger, Dorothy Levorse, Malcolm MacCoss, Margaret A. Cascieri, D. Euan MacIntyre, Laura C. Meurer, Kwei-Lan Tsao, Sharon Sadowski, and Sander G. Mills

Subjects

Molecular Structure, Tertiary amine, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Ether, Cyclopentanes, Receptors, Neurokinin-1, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Neurokinin-1 Receptor Antagonists, Solubility, chemistry, Morpholine, Drug Discovery, Humans, Molecular Medicine, Molecule, Structure–activity relationship, Cyclopentane, Molecular Biology

Abstract

An initial investigation of the novel cyclopentane scaffold 6 afforded low nanomolar human NK1 antagonists having enhanced water solubility properties compared to morpholine 1. A synthesis of this cyclopentane scaffold, having three contiguous chiral centers, and the unexpected determination that the 1,2-trans-2,3-trans-ring stereochemistry, as opposed to the cis-ether/phenyl configuration of the known structures 1-5, is optimal for this class of antagonist are described.

Published

2006

2. Combinatorial synthesis of 3-(Amidoalkyl) and 3-(Aminoalkyl)-2-arylindole derivatives: discovery of potent ligands for a variety of G-protein coupled receptors

Author

Madhumeeta J Dhar, Lorraine Malkowitz, Kevin T. Chapman, Kang Cheng, Steven M. Hutchins, Stephen G. Pacholok, Christopher A. Willoughby, Keith G. Rosauer, Gary G. Chicchi, David H. Weinberg, Sharon Sadowski, Smita Patel, and Jerry Di Salvo

Subjects

Indoles, Stereochemistry, G protein, medicine.drug_class, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Receptors, Cell Surface, Carboxamide, Ligands, Binding, Competitive, Biochemistry, Chemical synthesis, Structure-Activity Relationship, GTP-Binding Proteins, Drug Discovery, medicine, Combinatorial Chemistry Techniques, Humans, Amines, Receptor, Molecular Biology, Receptors, Tachykinin, G protein-coupled receptor, Bicyclic molecule, Chemistry, Ligand, Organic Chemistry, Amides, Receptors, Serotonin, Molecular Medicine, Receptors, Chemokine, Amine gas treating

Abstract

Preparation and screening of mixture libraries based on a 2-arylindole scaffold resulted in the discovery of potent ligands for a variety of G-protein coupled receptors.

Published

2002

3. The novel NK1 receptor antagonist MK–0869 (L–754,030) and its water soluble phosphoryl prodrug, L–758,298, inhibit acute and delayed cisplatin-induced emesis in ferrets

Author

Richard Hargreaves, D. E. Macintyre, G Mason, S Tye, E. Ber, F.D. Tattersall, Michael J Cumberbatch, J. J. Hale, Malcolm MacCoss, Margaret A. Cascieri, W. Rycroft, Paul E. Finke, Raymond G. Hill, Sharon Sadowski, David J. Williamson, and Sander G. Mills

Subjects

Male, Vomiting, medicine.drug_class, Morpholines, Antineoplastic Agents, CHO Cells, Pharmacology, Ondansetron, Cellular and Molecular Neuroscience, Acetals, Neurokinin-1 Receptor Antagonists, Cricetinae, medicine, Animals, Humans, Antiemetic, Prodrugs, Retching, Aprepitant, Cisplatin, Dose-Response Relationship, Drug, business.industry, Ferrets, Antagonist, Receptors, Neurokinin-1, Prodrug, Rats, Solubility, Acute Disease, COS Cells, Antiemetics, NK1 receptor antagonist, medicine.symptom, business, medicine.drug

Abstract

The anti-emetic profile of the novel brain penetrant tachykinin NK1 receptor antagonist MK-0869 (L-754,030) 2-(R)-(1-(R)-(3,5-bis(trifluoromethyl)phenylethoxy)-3-(S)-(4-fluor o)phenyl-4-(3-oxo-1,2,4-triazol-5-yl)methylmorpholine and its water soluble prodrug, L-758,298, has been examined against emesis induced by cisplatin in ferrets. In a 4 h observation period, MK-0869 and L-758,298 (3 mg/kg i.v. or p.o.) inhibited the emetic response to cisplatin (10 mg/kg i.v.). The anti-emetic protection afforded by MK-0869 (0.1 mg/kg i.v.) was enhanced by combined treatment with either dexamethasone (20 mg/kg i.v.) or the 5-HT3 receptor antagonist ondansetron (0.1 mg/kg i.v.). In a model of acute and delayed emesis, ferrets were dosed with cisplatin (5 mg/kg i.p.) and the retching and vomiting response recorded for 72 h. Pretreatment with MK-0869 (4-16 mg/kg p.o.) dose-dependently inhibited the emetic response to cisplatin. Once daily treatment with MK-0869 (2 and 4 mg/kg p.o.) completely prevented retching and vomiting in all ferrets tested. Further when daily dosing began at 24 h after cisplatin injection, when the acute phase of emesis had already become established, MK-0869 (4 mg/kg p.o. at 24 and 48 h after cisplatin) prevented retching and vomiting in three out of four ferrets. These data show that MK-0869 and its prodrug, L-758,298, have good activity against cisplatin-induced emesis in ferrets and provided a basis for the clinical testing of these agents for the treatment of emesis associated with cancer chemotherapy.

Published

2000

4. Characterization of a Novel, Non-peptidyl Antagonist of the Human Glucagon Receptor

Author

Margaret A. Cascieri, Malcolm MacCoss, Gary G. Chicchi, Gregory E. Koch, Sharon Sadowski, Stephen E. de Laszlo, Candice Hacker, E. Ber, William K. Hagmann, Pasquale P. Vicario, and Donna Louizides

Subjects

Agonist, endocrine system, Cations, Divalent, Pyridines, medicine.drug_class, Glucagon-Like Peptides, CHO Cells, Biochemistry, Glucagon, Glucagon-Like Peptide-1 Receptor, Hormone Antagonists, Cricetinae, Receptors, Glucagon, medicine, Animals, Humans, Pyrroles, Receptor, Molecular Biology, Glucagon-like peptide 1 receptor, Molecular Structure, Chemistry, digestive, oral, and skin physiology, Cell Biology, Enzyme Activation, Transmembrane domain, Mutation, Peptides, Glucagon receptor family, Glucagon receptor, hormones, hormone substitutes, and hormone antagonists, Adenylyl Cyclases, Protein Binding

Abstract

We have identified a series of potent, orally bioavailable, non-peptidyl, triarylimidazole and triarylpyrrole glucagon receptor antagonists. 2-(4-Pyridyl)-5-(4-chlorophenyl)-3-(5-bromo-2-propyloxyphenyl)p yrr ole (L-168,049), a prototypical member of this series, inhibits binding of labeled glucagon to the human glucagon receptor with an IC50 = 3. 7 +/- 3.4 nM (n = 7) but does not inhibit binding of labeled glucagon-like peptide to the highly homologous human glucagon-like peptide receptor at concentrations up to 10 microM. The binding affinity of L-168,049 for the human glucagon receptor is decreased 24-fold by the inclusion of divalent cations (5 mM). L-168,049 increases the apparent EC50 for glucagon stimulation of adenylyl cyclase in Chinese hamster ovary cells expressing the human glucagon receptor and decreases the maximal glucagon stimulation observed, with a Kb (concentration of antagonist that shifts the agonist dose-response 2-fold) of 25 nM. These data suggest that L-168,049 is a noncompetitive antagonist of glucagon action. Inclusion of L-168, 049 increases the rate of dissociation of labeled glucagon from the receptor 4-fold, confirming that the compound is a noncompetitive glucagon antagonist. In addition, we have identified two putative transmembrane domain residues, phenylalanine 184 in transmembrane domain 2 and tyrosine 239 in transmembrane domain 3, for which substitution by alanine reduces the affinity of L-168,049 46- and 4. 5-fold, respectively. These mutations do not alter the binding of labeled glucagon, suggesting that the binding sites for glucagon and L-168,049 are distinct.

Published

1999

5. Structural Optimization Affording 2-(R)-(1-(R)-3,5-Bis(trifluoromethyl)phenylethoxy)-3-(S)-(4-fluoro)phenyl-4- (3-oxo-1,2,4-triazol-5-yl)methylmorpholine, a Potent, Orally Active, Long-Acting Morpholine Acetal Human NK-1 Receptor Antagonist

Author

P. E. Finke, Gary G. Chicchi, Nadia M.J. Rupniak, George J. Eiermann, Nancy N. Tsou, E. Ber, Angela Williams, W. Rycroft, Margaret A. Cascieri, Sander G. Mills, Richard Hargreaves, M. Maccoss, Joe Metzger, D. E. Macintyre, Myra B. Kurtz, Sharon Sadowski, J. J. Hale, and F.D. Tattersall

Subjects

Male, Vomiting, medicine.drug_class, Stereochemistry, Morpholines, Urinary Bladder, Administration, Oral, Substance P, CHO Cells, Binding, Competitive, Cell Line, Capillary Permeability, chemistry.chemical_compound, Acetals, Esophagus, Neurokinin-1 Receptor Antagonists, Cricetinae, Morpholine, Drug Discovery, medicine, Animals, Humans, Receptor, IC50, Aprepitant, Inflammation, Trifluoromethyl, Behavior, Animal, Ferrets, Antagonist, Receptor antagonist, Hindlimb, Trachea, chemistry, Molecular Medicine, Female, Diterpenes, Gerbillinae, medicine.drug

Abstract

Structural modifications requiring novel synthetic chemistry were made to the morpholine acetal human neurokinin-1 (hNK-1) receptor antagonist 4, and this resulted in the discovery of 2-(R)-(1-(R)-3, 5-bis(trifluoromethyl)phenylethoxy)-3-(S)-(4-fluoro)phenyl-4-(3-ox o-1 ,2,4-triazol-5-yl)methyl morpholine (17). This modified compound is a potent, long-acting hNK-1 receptor antagonist as evidenced by its ability to displace [125I]Substance P from hNK-1 receptors stably expressed in CHO cells (IC50 = 0.09 +/- 0.06 nM) and by the measurement of the rates of association (k1 = 2.8 +/- 1.1 x 10(8) M-1 min-1) and dissociation (k-1 = 0.0054 +/- 0.003 min-1) of 17 from hNK-1 expressed in Sf9 membranes which yields Kd = 19 +/- 12 pM and a t1/2 for receptor occupancy equal to 154 +/- 75 min. Inflammation in the guinea pig induced by a resiniferatoxin challenge (with NK-1 receptor activation mediating the subsequent increase in vascular permeability) is inhibited in a dose-dependent manner by the oral preadmininstration of 17 (IC50 (1 h) = 0.008 mg/kg; IC90 (24 h) = 1.8 mg/kg), indicating that this compound has good oral bioavailbility and peripheral duration of action. Central hNK-1 receptor stimulation is also inhibited by the systemic preadministration of 17 as shown by its ability to block an NK-1 agonist-induced foot tapping response in gerbils (IC50 (4 h) = 0.04 +/- 0.006 mg/kg; IC50 (24 h) = 0.33 +/- 0.017 mg/kg) and by its antiemetic actions in the ferret against cisplatin challenge. The activity of 17 at extended time points in these preclinical animal models sets it apart from earlier morpholine antagonists (such as 4), and the piperidine antagonists 2 and 3 and could prove to be an advantage in the treatment of chronic disorders related to the actions of Substance P. In part on the basis of these data, 17 has been identified as a potential clinical candidate for the treatment of peripheral pain, migraine, chemotherapy-induced emesis, and various psychiatric disorders.

Published

1998

6. Distinct Mechanism for Antidepressant Activity by Blockade of Central Substance P Receptors

Author

Angela Williams, Raymond G. Hill, Guanghan Liu, Margaret A. Cascieri, John J. Sramek, John P. Feighner, Gary G. Chicchi, Ram K. Shrivastava, Malcolm MacCoss, Edward M. Scolnick, Duane B. Snavely, Emma J. Carlson, Louise Hewson, Christopher John Swain, Jeffrey J. Hale, Sharon Sadowski, N.R. Cutler, David D. Smith, Nadia M.J. Rupniak, Franz Hefti, Timothy Harrison, Edwina Wyatt-Knowles, Sander G. Mills, Scott A. Reines, Richard Hargreaves, John Carman, and Mark S. Kramer

Subjects

Adult, Male, Serotonin, medicine.medical_specialty, Adolescent, Morpholines, Guinea Pigs, Substance P, Norepinephrine, chemistry.chemical_compound, Neurokinin-1 Receptor Antagonists, Internal medicine, Monoaminergic, medicine, Animals, Humans, Receptor, Aged, Depressive Disorder, Multidisciplinary, Behavior, Animal, business.industry, Antagonist, Brain, Middle Aged, Receptors, Neurokinin-1, Amygdala, Paroxetine, Endocrinology, Monoamine neurotransmitter, Mechanism of action, chemistry, Antidepressive Agents, Second-Generation, Antidepressant, Female, NK1 receptor antagonist, Vocalization, Animal, medicine.symptom, Gerbillinae, business, Aprepitant, Stress, Psychological

Abstract

The localization of substance P in brain regions that coordinate stress responses and receive convergent monoaminergic innervation suggested that substance P antagonists might have psychotherapeutic properties. Like clinically used antidepressant and anxiolytic drugs, substance P antagonists suppressed isolation-induced vocalizations in guinea pigs. In a placebo-controlled trial in patients with moderate to severe major depression, robust antidepressant effects of the substance P antagonist MK-869 were consistently observed. In preclinical studies, substance P antagonists did not interact with monoamine systems in the manner seen with established antidepressant drugs. These findings suggest that substance P may play an important role in psychiatric disorders.

Published

1998

7. L-tryptophan urea amides as dual antagonists

Author

Margaret A. Cascieri, Sharon Sadowski, Malcolm MacCoss, Hongbo Qi, and Shrenik K. Shah

Subjects

integumentary system, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Tryptophan, Antagonist, Pharmaceutical Science, Nk2 receptor, hemic and immune systems, Biochemistry, Chemical synthesis, In vitro, law.invention, chemistry.chemical_compound, chemistry, law, Drug Discovery, Urea, Recombinant DNA, Molecular Medicine, Receptor, Molecular Biology

Abstract

We report that a systematic modification of an NK1 receptor selective antagonist resulted in the identification of novel compounds, 4c and 4d, with high affinity for both NK1 and NK2 receptors.

Published

1998

8. Serine derived NK1 antagonists 2: a pharmacophore model for arylsulfonamide binding

Author

Myra B. Kurtz, Gary G. Chicchi, Sharon Sadowski, Graeme Irvine Stevenson, Margaret A. Cascieri, Angus Murray Macleod, Jason Matthew Elliott, Ian Thomas Huscroft, and Howard B. Broughton

Subjects

chemistry.chemical_classification, Sulfonamides, Chemistry, Stereochemistry, Aryl, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Receptors, Neurokinin-1, Biochemistry, Sulfonamide, Serine, Structure-Activity Relationship, chemistry.chemical_compound, Models, Chemical, Neurokinin-1 Receptor Antagonists, Piperidines, Drug Discovery, Molecular Medicine, Pharmacophore, Molecular Biology

Abstract

Modifications to the spirocyclic aryl sulfonamide portion of serine derived NK1 antagonists allow a partial pharmacophore model to be developed.

Published

1998

9. High affinity, selective neurokinin 2 and neurokinin 3 receptor antagonists from a common structural template

Author

Timothy Harrison, Margaret A. Cascieri, Guy R. Seabrook, M. P. G. Korsgaard, Christopher John Swain, and Sharon Sadowski

Subjects

Lactams, Stereochemistry, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, chemistry.chemical_element, CHO Cells, Calcium, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Cricetinae, Drug Discovery, Animals, Humans, Receptor, Molecular Biology, Fluorescent Dyes, Chinese hamster ovary cell, Organic Chemistry, Antagonist, Receptors, Neurokinin-3, Receptors, Neurokinin-2, In vitro, Spectrometry, Fluorescence, chemistry, Lactam, Molecular Medicine, Fura-2, Neurokinin 3 receptor

Abstract

High affinity, selective hNK2 or hNK3 ligands can be prepared from the common template 1 in a few simple chemical operations. The hNK3 ligands 3 antagonise the calcium mobilisation caused by activation of hNK3 receptors expressed in CHO cells as measured using fura-2 microspectrofluorimetry.

Published

1998

10. High affinity phenylglycinol-based NK 1 receptor antagonists

Author

Andrew Pate Owens, Margaret A. Cascieri, Timothy Harrison, J. D. Moseley, Christopher John Swain, and Sharon Sadowski

Subjects

Molecular Structure, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Glycine, Antagonist, Pharmaceutical Science, Biochemistry, Chemical synthesis, In vitro, Structure-Activity Relationship, Neurokinin-1 Receptor Antagonists, Ethanolamines, Drug Discovery, Triazole derivatives, Humans, Molecular Medicine, Receptor, Molecular Biology

Abstract

Heterocyclic replacements for the carboxamido group of the previously disclosed phenylglycinol-based human NK1 (hNK1) receptor antagonists have been investigated, ultimately leading to acyclic compounds with sub-nanomolar affinity for the hNK1 receptor.

Published

1998

11. 3-Benzyloxy-2-phenylpiperidine NK1 antagonists: the influence of alpha methyl substitution

Author

Joe Metzger, Gary G. Chicchi, Linda Elizabeth Keown, R. Baker, Margaret A. Cascieri, Simon C. Morton, Christopher John Swain, A. P. Watt, Silvi Luell, Sharon Sadowski, Andrew Pate Owens, D. E. Macintyre, Michael J. Forrest, Richard H. Herbert, Brian John Williams, and T. Ladduwahetty

Subjects

inorganic chemicals, Trifluoromethyl, Stereochemistry, organic chemicals, Metabolite, Organic Chemistry, Clinical Biochemistry, Diastereomer, Pharmaceutical Science, Ether, Metabolism, Biochemistry, Chemical synthesis, chemistry.chemical_compound, chemistry, Drug Discovery, Molecular Medicine, Molecular Biology, Benzoic acid, Methyl group

Abstract

In vitro metabolism studies on a series of 3,5-bis(trifluoromethyl)benzyl ethers have identified 3,5-bis(trifluoromethyl)benzoic acid as a significant metabolite possibly arising via oxidation of the benzylic position. A methyl group was introduced in an effort to suppress this route of metabolism. One diastereoisomer displayed an increase in affinity and a marked improvement in duration of action. In vitro metabolism studies on a series of 3,5-bis(trifluoromethyl)benzyl ethers have identified 3,5-bis(trifluoromethyl)benzoic acid as a significant metabolite possibly arising via oxidation at the benzylic position. A methyl group was introduced in an effort to suppress this route of metabolism. One diastereoisomer displayed an increase in affinity and a marked improvement in duration of action

Published

1997

12. Linear amides as substance P antagonists

Author

T. Harrison, J. D. Moseley, Andrew Pate Owens, Martin Richard Teall, Margaret A. Cascieri, and Sharon Sadowski

Subjects

High affinity binding, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Substance P, Ring (chemistry), Biochemistry, chemistry.chemical_compound, chemistry, Amide, Drug Discovery, Molecular Medicine, Molecular Biology

Abstract

In the present study we demonstrate that an amide linking group provides an excellent template for the positioning of a benzhydryl group and a suitably functionalized aromatic ring in an orientation which allows for high affinity binding to the hNK1 receptor.

Published

1996

13. N-Heteroaryl-2-phenyl-3-(benzyloxy)piperidines: A Novel Class of Potent Orally Active Human NK1 Antagonists

Author

F.D. Tattersall, D. E. Macintyre, D. W. Williamson, Karen Elizabeth Haworth, Raymond Baker, Alan P. Watt, Margaret A. Cascieri, Tamara Ladduwahetty, Joseph M. Metzger, Eileen Mary Seward, Simon Neil Owen, Linda Elizabeth Keown, W. Rycroft, Richard Hargreaves, Christopher John Swain, S. L. Shepheard, Sharon Sadowski, and Mark Stuart Chambers

Subjects

Male, Vomiting, Stereochemistry, Migraine Disorders, Guinea Pigs, Biological Availability, Ether, Chemical synthesis, chemistry.chemical_compound, Drug Stability, Neurokinin-1 Receptor Antagonists, Piperidines, Oral administration, In vivo, Drug Discovery, Animals, Humans, Potency, Inflammation, Trifluoromethyl, Chemistry, Ferrets, Receptors, Neurokinin-1, Triazoles, Macaca mulatta, Rats, Microsomes, Liver, Microsome, Molecular Medicine, Piperidine

Abstract

The preparation of a series of N-heteroarylpiperidine ether-based human NK1 antagonists is described. Two of the compounds 3-[-(2S,3S)-3-(((3,5-bis(trifluoromethyl)phenyl)methyl)oxy)- 2-phenylpiperidino}methyl]-1,2,4-triazole (11) and 5-[¿(2S,3S)-3-(((3,5-bis(trifluoromethyl)-phenyl)methyl)oxy)-2- phenylpiperidino}methyl]-3-oxo-1,2,4-triazolone (12)), in particular, are orally bioavailable and exhibited significant improvements in potency, both in vitro and in vivo, over the lead (carboxamidomethyl)piperidine ether 1. Rat liver microsome studies on a selected number of compounds from this series show the triazolone heterocycle to be considerably more stable than the others. Furthermore, both 11 and 12 have been profiled in a number of assays that may be predictive of the clinical utility of substance P antagonists.

Published

1996

14. 1,2,3-Trisubstituted cyclohexyl substance P antagonists: significance of the ring nitrogen in piperidine-based NK-1 receptor antagonists

Author

Catherine D. Strader, Margaret A. Cascieri, Sander G. Mills, Dennis J. Underwood, Richard J. Budhu, Shrenik K. Shah, Malcolm MacCoss, Daniel J. Miller, Paul E. Finke, and Sharon Sadowski

Subjects

Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, chemistry.chemical_element, Substance P, Ring (chemistry), Biochemistry, Nitrogen, chemistry.chemical_compound, chemistry, NK 1 Receptor Antagonists, Drug Discovery, Molecular Medicine, Piperidine, Receptor, Molecular Biology

Abstract

A stereocontrolled synthesis of 1-benzyloxy-2-phenylcyclohexane derivatives containing polar substituents at C3 is described. These compounds, designed to test the role of the ring nitrogen in a related series of potent piperidine-based substance P antagonists, show similar NK-1 receptor affinity, indicating that the nitrogen may serve a largely structural role in N-substituted piperidine antagonists.

Published

1995

15. Tryptophan-Derived NK1 Antagonists: Conformationally Constrained Heterocyclic Bioisosteres of the Ester Linkage

Author

Angus Murray Macleod, Ian Sanderson, Richard H. Herbert, Fintan Kelleher, Kevin John Merchant, Margaret A. Cascieri, Richard Thomas Lewis, Karst Hoogsteen, Sharon Sadowski, and Richard G. Ball

Subjects

Steric effects, Magnetic Resonance Spectroscopy, Stereochemistry, Molecular Conformation, CHO Cells, Crystallography, X-Ray, Transfection, Ring (chemistry), Chemical synthesis, Piperazines, Substance-P Receptor, Structure-Activity Relationship, chemistry.chemical_compound, Isomerism, Neurokinin-1 Receptor Antagonists, Heterocyclic Compounds, Cricetinae, Drug Discovery, Animals, Humans, Oxazolidinedione, Trifluoromethyl, Molecular Structure, Tryptophan, Esters, Receptors, Neurokinin-1, Solutions, chemistry, Molecular Medicine, Bioisostere

Abstract

The 3,5-bis(trifluoromethyl)benzyl ester of N-acetyl-L-tryptophan 1 (L-732,138) has been identified previously as a potent and selective substance P receptor antagonist. A series of analogs which introduced a 6-membered heterocyclic ring into the backbone of this structure were prepared for evaluation as bioisosteric replacements of the ester linkage of 1. The 2,5-dioxopiperazine 2 had very weak receptor affinity, but 2-oxopiperazine 5 exhibited modest activity. Examination of the conformations accessible to the substituents on these templates led to exploration of the corresponding 5-membered heterocyclic rings. This study culminated in the identification of oxazolidinedione 14 as a suitable ester mimic in terms of the retention of good NK1 binding affinity.

Published

1995

16. 1,2,4-Triacylpiperidine substance p antagonists: Separation of affinities for the NK-1 receptor and the L-type calcium channel

Author

Peter H. Hutson, Kerry L. Chapman, Sander G. Mills, Sharon Sadowski, Malcolm MacCoss, Smita Patel, and Margaret A. Cascieri

Subjects

Calcium channel, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Substance P, Biochemistry, Affinities, chemistry.chemical_compound, chemistry, Drug Discovery, Molecular Medicine, L-type calcium channel, Receptor, Molecular Biology

Abstract

A series of 1,2,4-triacylpiperidines are shown to be potent antagonists of the NK-1 (Substance P) receptor with significant affinity for the L-type calcium channel as well. The latter property can be diminished by suitable substitution on the terminal nitrogen while maintaining good NK-1 receptor binding.

Published

1995

17. Synthesis and Biological Evaluation of NK1 Antagonists Derived from L-Tryptophan

Author

Kevin John Merchant, Angus Murray Macleod, D. E. Macintyre, Tung M. Fong, Sharon Sadowski, Joe Metzger, Margaret A. Cascieri, Hardwicke S, S. L. Shepheard, and Richard Thomas Lewis

Subjects

Male, Ketone, Stereochemistry, medicine.drug_class, Guinea Pigs, Molecular Sequence Data, Ether, CHO Cells, Substance P, Cardiovascular System, Chemical synthesis, Aminoketone, Structure-Activity Relationship, chemistry.chemical_compound, Neurokinin-1 Receptor Antagonists, Piperidines, Heterocyclic Compounds, Cricetinae, Amide, Drug Discovery, medicine, Animals, Humans, Hypnotics and Sedatives, Moiety, Amino Acid Sequence, Amines, chemistry.chemical_classification, Binding Sites, Trifluoromethyl, Biphenyl Compounds, Ferrets, Tryptophan, Esters, Receptors, Neurokinin-1, Solubility, chemistry, Molecular Medicine, Female, Extravasation of Diagnostic and Therapeutic Materials, Quinuclidine

Abstract

The 3,5-bis(trifluoromethyl)benzyl ester of N-acetyl-L-tryptophan (3), which was derived from the screening lead N-ethyl-L-tryptophan benzyl ester, has been used as a starting point to identify high-affinity substance P receptor antagonists with improved in vivo activity. Altering the ester moiety to an amide or ether led to a substantial loss in binding affinity, but conversion to a ketone provided compounds with affinity comparable to the equivalent esters. A homochiral synthesis of the key intermediate amino ketone 15 was developed which allows its preparation on a large scale. From this intermediate a range of amine-containing acylamino derivatives were prepared with affinity optimized in the morpholinylbutyramide 161 which has an IC 50 of 0.17 nM at the human NK1 receptor. In addition to improving affinity, the amino group also provided aqueous solubility for a number of these derivatives. When tested in vivo the quinuclidine derivative L-737,488 (16i) was found to be an orally active (ID 50 = 1.8 mg/kg) inhibitor of substance P-induced dermal extravasation in the guinea pig.

Published

1995

18. Piperidine-ether based hNK1 antagonists 2: Investigation of the effect of N-substitution

Author

R. Baker, Brian John Williams, T. Harrison, Christopher John Swain, Sharon Sadowski, Margaret A. Cascieri, Peter H. Hutson, and Andrew Pate Owens

Subjects

Substance p antagonist, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Substitution (logic), Pharmaceutical Science, Ether, Biochemistry, chemistry.chemical_compound, chemistry, Drug Discovery, Molecular Medicine, Piperidine, Receptor, Molecular Biology

Abstract

The effect of nitrogen substitution on the binding affinity of the piperidine-ether substance P antagonist L-733,060 for the hNK 1 receptor and L-type Ca 2+ channel is discussed.

Published

1995

19. Acyclic NK1 antagonists: Replacements for the benzhydryl group

Author

Andrew Pate Owens, Christopher John Swain, Sharon Sadowski, M. B. Van Niel, Brian John Williams, Walfred S. Saari, Catherine D. Strader, Martin Richard Teall, and Margaret A. Cascieri

Subjects

Stereochemistry, Group (periodic table), Chemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Stereoselectivity, Ring (chemistry), Molecular Biology, Biochemistry, Combinatorial chemistry

Abstract

An exploration of benzhydryl replacements is described. Whilst bridged and fused polynuclear aromatic systems both incur a reduction in affinity it was possible to replace the benzhydryl by a single phenyl ring with only a modest reduction in affinity. In contrast to the analogous diphenylalanyl ethers the binding was also shown to be stereoselective.

Published

1994

20. Acyclic NK-1 antagonists: 2-benzhydryl-2-aminoethyl ethers

Author

Catherine D. Strader, Timothy Harrison, Martin Richard Teall, Margaret A. Cascieri, Christopher John Swain, Sharon Sadowski, Raymond Baker, Jeffrey Mc Kenna, and Brian John Williams

Subjects

Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Channel (broadcasting), Receptor, Molecular Biology, Biochemistry, Combinatorial chemistry

Abstract

A series of 2-aminoethyl ethers based on diphenylalaninol have been shown to have significant affinity for the human NK 1 receptor and reduced affinity at the L-type Ca ++ channel compared with quinuclidines related to CP 96,345.

Published

1994

21. Morpholine-based substance P antagonists: assessment of the 3-point binding model

Author

Sharon Sadowski, Margaret A. Cascieri, Linda Elizabeth Keown, and T. Ladduwahetty

Subjects

Substance p antagonist, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Heteroatom, Pharmaceutical Science, Substance P, Biochemistry, chemistry.chemical_compound, Morpholine, Drug Discovery, Molecular Medicine, Receptor, Molecular Biology

Abstract

The carbon-linked morpholine analogues of the Substance P antagonist CP-99,994 were synthesised. The activities of the resulting compounds suggest that there is a specific interaction between the benzylic heteroatom of these antagonists and the NK 1 receptor.

Published

1994

22. Identification of L-Tryptophan Derivatives with Potent and Selective Antagonist Activity at the NK1 Receptor

Author

M A Casiceri, Fintan Kelleher, Andrew Pate Owens, F Brookfield, Christopher J. Swain, Angus Murray Macleod, Graeme Irvine Stevenson, E. Ber, Kevin John Merchant, and Sharon Sadowski

Subjects

Male, Models, Molecular, Stereochemistry, Acylation, Guinea Pigs, Molecular Sequence Data, Molecular Conformation, CHO Cells, Substance P, Dermatitis, Contact, Substance-P Receptor, Structure-Activity Relationship, Neurokinin-1 Receptor Antagonists, Cricetinae, Drug Discovery, Animals, Humans, Structure–activity relationship, Computer Simulation, Amino Acid Sequence, Indole test, Molecular Structure, Chemistry, Tryptophan, Antagonist, Biological activity, Receptors, Neurokinin-1, Recombinant Proteins, Molecular Medicine, Sample collection

Abstract

As part of a program of screening the Merck sample collection, N-ethyl-L-tryptophan benzyl ester was identified as a weak antagonist at the substance P (NK1) receptor. Structure-activity studies showed that the indole ring system could be replaced by 3,4-dichlorophenyl, alpha- or beta-naphthyl, or benzthiophene with retention or only small loss of affinity. It was found that acylation of the tryptophan nitrogen gave compounds with higher affinity than N-ethyl or other basic amines. Optimization of substitution on the benzyl ester led to the identification of the 3,5-bis-(trifluoromethyl)benzyl ester of N-acetyl-L-tryptophan 26 as a potent and selective substance P receptor antagonist. Compound 26 blocked substance P induced dermal extravasation in vivo and was the most potent compound from this structurally novel class of antagonists which further adds to the diversity of small molecules that bind to the (NK1) receptor.

Published

1994

23. Characterization of the interaction of N-acyl-L-tryptophan benzyl ester neurokinin antagonists with the human neurokinin-1 receptor

Author

Catherine D. Strader, Margaret A. Cascieri, Henry Yu, Kevin John Merchant, Christopher John Swain, Sharon Sadowski, Angus Murray Macleod, Dennis J. Underwood, E. Ber, and Lin-Lin Shiao

Subjects

Stereochemistry, Chinese hamster ovary cell, Substance P, Cell Biology, Biochemistry, chemistry.chemical_compound, chemistry, Competitive antagonist, Tachykinin receptor 1, Neurokinin A, Binding site, Receptor, Molecular Biology, Quinuclidine

Abstract

We have recently shown that a series of N-acyl-L-tryptophan benzyl esters are potent substance P antagonists (Macleod, A. M., Merchant, K. J., Cascieri, M. A., Sadowski, S., Ber, E., Swain, C. J., and Baker, R. (1993) J. Med Chem. 14, 2044-2045). We now report the detailed characterization of the interaction of N-acetyl-L-tryptophan-3,5-bistrifluoromethyl benzyl ester (L-732,138) with the human neurokinin-1 (NK-1) receptor. L-732,138 inhibits the binding of 125I-substance P to the cloned human NK1 receptor expressed in Chinese hamster ovary cells with an IC50 of 2.3 +/- 0.7 nM. In contrast, it has 200-fold lower affinity for the cloned rat NK-1 receptor and has > 1000-fold lower affinity for the human NK-2 and NK-3 receptors. L-732,138 acts as a competitive antagonist of substance P, as shown by functional Schild analysis of the inhibition of substance P-induced inositol phosphate synthesis, by kinetic analysis of the dissociation rate, and by thermodynamic analysis of the equilibrium binding of 125I-substance P to the NK-1 receptor. L-732,138 also competitively inhibits the binding of the quinuclidine amine antagonist, [125I]L-703,606, to the receptor. The compound has 230- and 10-fold reduced affinity for mutant NK-1 receptors in which histidine 265 or histidine 197, respectively, are replaced with alanine. We have previously shown that these residues play key roles in the binding of quinuclidine antagonists to the NK-1 receptor. These results suggest that the tryptophan and quinuclidine series of NK-1 antagonists bind to similar binding sites on the human NK-1 receptor.

Published

1994

24. 1,4-Diacylpiperazine-2-(S)-[(N-aminoalkyl)carboxamides] as novel, potent substance P receptor antagonists

Author

Sharon Sadowski, William J. Greenlee, Catherine D. Strader, Sander G. Mills, Margaret A. Cascieri, Richard J. Budhu, Mu Tsu Wu, Conrad P. Dorn, and Malcolm MacCoss

Subjects

medicine.drug_class, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Substance P, Carboxamide, Substance P Receptor Antagonists, Biochemistry, Chemical synthesis, chemistry.chemical_compound, chemistry, Drug Discovery, medicine, Molecular Medicine, Peptide bond, Receptor, Molecular Biology

Abstract

A series of N,N′-diacylpiperazine-2-carboxamides are shown to be antagonists of the NK-1 (Substance P) receptor. Elaboration of the C2 sidechain with aminoalkyl groups leads to two series of potent antagonists, one containing simple dialkylamino groups and the second featuring 2-methoxybenzylamino derivatives with divergent SARs with respect to substitution at the C2 amide bond.

Published

1993

25. Quinuclidine based NK-1 antagonists 2: determination of the absolute stereochemical requirements

Author

Richard G. Ball, R. Baker, Verity Margaret Sabin, Christopher John Swain, Sharon Sadowski, Catherine D. Strader, Simon Neil Owen, Eileen Mary Seward, and Margaret A. Cascieri

Subjects

High affinity binding, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, chemistry.chemical_compound, Drug Discovery, Molecular Medicine, Molecule, Epimer, Molecular Biology, Quinuclidine

Abstract

The relative and absolute stereochemical requirements for high affinity binding to the human NK-1 receptor are defined for a series of quinuclidine ethers. Whilst the S stereochemistry at C-3 is essential for high afifnity, surprising both epimers at C-2 are active.

Published

1993

26. Quinuclidine-based NK-1 antagonists I: 3-benzyloxy-1-azabicyclo[2.2.2]octanes

Author

Kevin John Merchant, Christopher John Swain, Sharon Sadowski, Catherine D. Strader, Margaret A. Cascieri, Eileen Mary Seward, Raymond Baker, Verity Margaret Sabin, and Simon Neil Owen

Subjects

chemistry.chemical_compound, chemistry, Benzyl ether, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Receptor, Molecular Biology, Biochemistry, Quinuclidine

Abstract

A series of 3-benzyloxy-derivatives of CP-96,345 has been evaluated and found to have significant affinity for the human NK1 receptor. 3,5-Disubstitution of the benzyl ether has been identified to be essential for high affinity.

Published

1993

27. ChemInform Abstract: Acyclic NK-1 Antagonists: 2-Benzhydryl-2-aminoethyl Ethers

Author

R. Baker, Brian John Williams, T. Harrison, J. C. Mc Kenna, Christopher John Swain, Sharon Sadowski, Catherine D. Strader, Martin Richard Teall, and Margaret A. Cascieri

Subjects

Chemistry, General Medicine, Medicinal chemistry, Diphenylmethane derivatives

Published

2010

28. ChemInform Abstract: Morpholine-Based Substance P Antagonists: Assessment of the 3-Point Binding Model

Author

Margaret A. Cascieri, Linda Elizabeth Keown, T. Ladduwahetty, and Sharon Sadowski

Subjects

Substance p antagonist, chemistry.chemical_compound, chemistry, Stereochemistry, Morpholine, Heteroatom, Substance P, General Medicine, Receptor

Abstract

The carbon-linked morpholine analogues of the Substance P antagonist CP-99,994 were synthesised. The activities of the resulting compounds suggest that there is a specific interaction between the benzylic heteroatom of these antagonists and the NK 1 receptor.

Published

2010

29. ChemInform Abstract: Acyclic NK1 Antagonists: Replacements for the Benzhydryl Group

Author

Catherine D. Strader, Walfred S. Saari, Martin Richard Teall, Margaret A. Cascieri, Christopher John Swain, Sharon Sadowski, Andrew Pate Owens, M. B. Van Niel, and Brian John Williams

Subjects

Chemistry, Group (periodic table), Stereochemistry, Stereoselectivity, General Medicine, Ring (chemistry)

Abstract

An exploration of benzhydryl replacements is described. Whilst bridged and fused polynuclear aromatic systems both incur a reduction in affinity it was possible to replace the benzhydryl by a single phenyl ring with only a modest reduction in affinity. In contrast to the analogous diphenylalanyl ethers the binding was also shown to be stereoselective.

Published

2010

30. ChemInform Abstract: 1,2,3-Trisubstituted Cyclohexyl Substance P Antagonists: Significance of the Ring Nitrogen in Piperidine-Based NK-1 Receptor Antagonists

Author

Sharon Sadowski, Paul E. Finke, Daniel J. Miller, Shrenik K. Shah, Malcolm MacCoss, Catherine D. Strader, Dennis J. Underwood, Margaret A. Cascieri, Richard J. Budhu, and Sander G. Mills

Subjects

chemistry.chemical_compound, chemistry, Stereochemistry, NK 1 Receptor Antagonists, chemistry.chemical_element, Substance P, General Medicine, Piperidine, Receptor, Ring (chemistry), Nitrogen

Abstract

A stereocontrolled synthesis of 1-benzyloxy-2-phenylcyclohexane derivatives containing polar substituents at C3 is described. These compounds, designed to test the role of the ring nitrogen in a related series of potent piperidine-based substance P antagonists, show similar NK-1 receptor affinity, indicating that the nitrogen may serve a largely structural role in N-substituted piperidine antagonists.

Published

2010

31. ChemInform Abstract: Piperidine-Ether Based hNK1 Antagonists. Part 2. Investigation of the Effect of N-Substitution

Author

Timothy Harrison, Brian J. Williams, Margaret A. Cascieri, Christopher John Swain, Raymond Baker, Sharon Sadowski, Peter H. Hutson, and Andrew Pate Owens

Subjects

chemistry.chemical_compound, Chemistry, Substitution (logic), Ether, General Medicine, Piperidine, Medicinal chemistry

Published

2010

32. ChemInform Abstract: Identification of a Series of 3-(Benzyloxy)-1-azabicyclo(2.2.2)octane Human NK1 Antagonists

Author

Richard H. Herbert, Kevin John Merchant, Christopher John Swain, Tung Ming Fong, Sharon Sadowski, Brian John Williams, D. E. Macintyre, M. B. Vanniel, Richard G. Ball, Eileen Mary Seward, Verity Margaret Sabin, R. Baker, Simon Neil Owen, Catherine D. Strader, Martin Richard Teall, Margaret A. Cascieri, and Andrew Pate Owens

Subjects

chemistry.chemical_classification, chemistry.chemical_compound, Series (mathematics), Chemistry, Identification (biology), General Medicine, Bridged compounds, Combinatorial chemistry, Octane

Published

2010

33. ChemInform Abstract: 2(S)-((3,5-Bis(trifluoromethyl)benzyl)oxy)-3(S)-phenyl-4-((3-oxo-1,2,4- triazol-5-yl)methyl)morpholine: A Potent, Orally Active, Morpholine- Based Human Neurokinin-1 Receptor Antagonist

Author

D. E. Macintyre, Hongbo Qi, David J. Mathre, Sander G. Mills, J. J. Hale, M. Maccoss, Catherine D. Strader, Joseph M. Metzger, Margaret A. Cascieri, Sharon Sadowski, and S. K. Shah

Subjects

chemistry.chemical_compound, Orally active, Trifluoromethyl, Stereochemistry, Chemistry, Morpholine, Tachykinin receptor 1, Antagonist, General Medicine

Published

2010

34. ChemInform Abstract: Linear Amides as Substance P Antagonists

Author

J. D. Moseley, Andrew Pate Owens, Martin Richard Teall, Margaret A. Cascieri, Sharon Sadowski, and T. Harrison

Subjects

chemistry.chemical_compound, High affinity binding, Chemistry, Stereochemistry, Amide, Substance P, General Medicine, Ring (chemistry), Combinatorial chemistry

Abstract

In the present study we demonstrate that an amide linking group provides an excellent template for the positioning of a benzhydryl group and a suitably functionalized aromatic ring in an orientation which allows for high affinity binding to the hNK1 receptor.

Published

2010

35. ChemInform Abstract: N-Heteroaryl-2-phenyl-3-(benzyloxy)piperidines: A Novel Class of Potent Orally Active Human NK1 Antagonists

Author

W. Rycroft, S. L. Shepheard, Raymond Baker, Christopher John Swain, Simon Neil Owen, Sharon Sadowski, Linda Elizabeth Keown, Richard Hargreaves, Margaret A. Cascieri, F.D. Tattersall, Eileen Mary Seward, Karen Elizabeth Haworth, Tamara Ladduwahetty, D. W. Williamson, Alan P. Watt, Mark Stuart Chambers, Joseph M. Metzger, and D. E. Macintyre

Subjects

chemistry.chemical_compound, Trifluoromethyl, Orally active, chemistry, Stereochemistry, In vivo, Microsome, Potency, Ether, General Medicine, Piperidine, In vitro

Abstract

The preparation of a series of N-heteroarylpiperidine ether-based human NK1 antagonists is described. Two of the compounds (3-[{(2S,3S)-3-(((3,5-bis(trifluoromethyl)phenyl)methyl)oxy)-2-phenylpiperidino}methyl]-1,2,4-triazole (11) and 5-[{(2S,3S)-3-(((3,5-bis(trifluoromethyl)phenyl)methyl)oxy)-2-phenylpiperidino}methyl]-3-oxo-1,2,4-triazolone (12)), in particular, are orally bioavailable and exhibited significant improvements in potency, both in vitro and in vivo, over the lead (carboxamidomethyl)piperidine ether 1. Rat liver microsome studies on a selected number of compounds from this series show the triazolone heterocycle to be considerably more stable than the others. Furthermore, both 11 and 12 have been profiled in a number of assays that may be predictive of the clinical utility of substance P antagonists.

Published

2010

36. ChemInform Abstract: High Affinity Phenylglycinol-Based NK1 Receptor Antagonists

Author

Margaret A. Cascieri, Andrew Pate Owens, Timothy Harrison, J. D. Moseley, Christopher John Swain, and Sharon Sadowski

Subjects

Chemistry, Stereochemistry, Triazole derivatives, General Medicine, Receptor

Abstract

Heterocyclic replacements for the carboxamido group of the previously disclosed phenylglycinol-based human NK1 (hNK1) receptor antagonists have been investigated, ultimately leading to acyclic compounds with sub-nanomolar affinity for the hNK1 receptor.

Published

2010

37. ChemInform Abstract: High Affinity, Selective Neurokinin 2 and Neurokinin 3 Receptor Antagonists from a Common Structural Template

Author

M. P. G. Korsgaard, Guy R. Seabrook, Christopher John Swain, Sharon Sadowski, Margaret A. Cascieri, and Timothy Harrison

Subjects

chemistry, Chinese hamster ovary cell, Biophysics, chemistry.chemical_element, General Medicine, Calcium, Receptor, Neurokinin 3 receptor

Abstract

High affinity, selective hNK2 or hNK3 ligands can be prepared from the common template 1 in a few simple chemical operations. The hNK3 ligands 3 antagonise the calcium mobilisation caused by activation of hNK3 receptors expressed in CHO cells as measured using fura-2 microspectrofluorimetry.

Published

2010

38. ChemInform Abstract: L-Tryptophan Urea Amides as NK1/NK2 Dual Antagonists

Author

Margaret A. Cascieri, Malcolm MacCoss, Sharon Sadowski, Shrenik K. Shah, and Hongbo Qi

Subjects

chemistry.chemical_compound, integumentary system, Biochemistry, Chemistry, Urea, Tryptophan, Nk2 receptor, hemic and immune systems, General Medicine, Selective antagonist, Receptor

Abstract

We report that a systematic modification of an NK1 receptor selective antagonist resulted in the identification of novel compounds, 4c and 4d, with high affinity for both NK1 and NK2 receptors.

Published

2010

39. Identification and isolation of a membrane protein necessary for leukotriene production

Author

John A. Rodkey, Jilly F. Evans, John W. Gillard, Sharon Sadowski, Irving S. Sigal, Peter Charleson, Philip J. Vickers, Catherine D. Strader, Rejean Fortin, Anthony W. Ford-Hutchinson, Richard A. F. Dixon, Jacques Yves Gauthier, C. Leveillé, Joseph A. Mancini, C. Rouzer, Ronda Rosen, and Douglas K. Miller

Subjects

Azides, Leukotrienes, Indoles, Neutrophils, Molecular Sequence Data, Leukotriene Production, Cell, Inflammation, chemistry.chemical_compound, medicine, Animals, Humans, Amino Acid Sequence, 5-lipoxygenase-activating protein, Leukotriene, Multidisciplinary, biology, Leukotriene A4, Membrane Proteins, Affinity Labels, Transfection, Rats, Molecular Weight, Kinetics, medicine.anatomical_structure, Biochemistry, chemistry, biology.protein, Leukotriene Antagonists, Electrophoresis, Polyacrylamide Gel, Arachidonic acid, medicine.symptom

Abstract

Several inflammatory diseases, including asthma, arthritis and psoriasis are associated with the production of leukotrienes by neutrophils, mast cells and macrophages. The initial enzymatic step in the formation of leukotrienes is the oxidation of arachidonic acid by 5-lipoxygenase (5-LO) to leukotriene A4. Osteosarcoma cells transfected with 5-LO express active enzyme in broken cell preparations, but no leukotriene metabolites are produced by these cells when stimulated with the calcium ionophore A23187, indicating that an additional component is necessary for cellular 5-LO activity. A new class of indole leukotriene inhibitor has been described that inhibits the formation of cellular leukotrienes but has no direct inhibitory effect on soluble 5-LO activity. We have now used these potent agents to identify and isolate a novel membrane protein of relative molecular mass 18,000 which is necessary for cellular leukotriene synthesis.

Published

1990

40. Cyclopentane-based human NK1 antagonists. Part 2: development of potent, orally active, water-soluble derivatives

Author

Laura C. Meurer, Gary G. Chicchi, Karen Owens, Nadia M.J. Rupniak, Angela Williams, Richard G. Ball, Paul E. Finke, Silvi Luell, Nancy N. Tsou, Malcolm MacCoss, Margaret A. Cascieri, Sander G. Mills, Richard Hargreaves, D. Euan MacIntyre, Joseph M. Metzger, Linda A. Egger, Kwei-Lan Tsao, and Sharon Sadowski

Subjects

Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Context (language use), CHO Cells, Cyclopentanes, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Neurokinin-1 Receptor Antagonists, In vivo, Oral administration, Cricetinae, Drug Discovery, medicine, Animals, Humans, Cyclopentane, Molecular Biology, Aprepitant, Molecular Structure, Chemistry, Organic Chemistry, Antagonist, Water, Receptors, Neurokinin-1, In vitro, Solubility, Molecular Medicine, medicine.drug

Abstract

The synthesis and optimization of a cyclopentane-based hNK1 antagonist scaffold 3, having four chiral centers, will be discussed in the context of its enhanced water solubility properties relative to the marketed anti-emetic hNK1 antagonist EMEND® (Aprepitant). Sub-nanomolar hNK1 binding was achieved and oral activity comparable to Aprepitant in two in vivo models will be described.

Published

2006

41. 2(S)-((3,5-Bis(trifluoromethyl)benzyl)oxy)-3(S)-phenyl-4-((3-oxo-1,2,4-triazol- 5-yl)methyl)morpholine (1): A Potent, Orally Active, Morpholine-Based Human Neurokinin-1 Receptor Antagonist

Author

D. E. Macintyre, Catherine D. Strader, J. J. Hale, Margaret A. Cascieri, S. K. Shah, Sharon Sadowski, Joseph M. Metzger, Hongbo Qi, M. Maccoss, D J Mathre, and Sander G. Mills

Subjects

Trifluoromethyl, Morpholines, Antagonist, Administration, Oral, Nk2 receptor, Neurokinin-1 Receptor Antagonists, CHO Cells, Medicinal chemistry, Chemical synthesis, chemistry.chemical_compound, Orally active, chemistry, Cricetinae, Morpholine, Drug Discovery, Tachykinin receptor 1, Animals, Humans, Molecular Medicine

Published

1996

42. Spirocyclic NK(1) antagonists I: [4.5] and [5.5]-spiroketals

Author

Karen Elizabeth Haworth, Timothy Harrison, Richard H. Herbert, Eileen Mary Seward, Fintan Kelleher, Simon Neil Owen, J. D. Moseley, Christopher John Swain, Marc M. Kurtz, Emma J. Carlson, Sharon Sadowski, Andrew Pate Owens, and Brian John Williams

Subjects

Bicyclic molecule, Stereochemistry, Chemistry, Organic Chemistry, Clinical Biochemistry, Acetal, Pharmaceutical Science, Neurokinin-1 Receptor Antagonists, Ring (chemistry), Biochemistry, Chemical synthesis, Cns penetration, chemistry.chemical_compound, Spiroether, Drug Discovery, Triazole derivatives, Molecular Medicine, Spiro Compounds, Molecular Biology

Abstract

A series of novel spiroketal-based NK(1) antagonists is described. The effect of modifications to the spiroether ring and aromatic substituents are discussed, leading to the identification of compounds with high affinity and excellent CNS penetration.

Published

2002

43. Phosphorylated morpholine acetal human neurokinin-1 receptor antagonists as water-soluble prodrugs

Author

Gary G. Chicchi, Joseph M. Metzger, R. A. Reamer, C. P. Dorn, Nadia M.J. Rupniak, Angela Williams, W. Rycroft, Erin McGowan, D. E. Macintyre, Paul E. Finke, Sharon Sadowski, Sander G. Mills, Shuet-Hing Lee Chiu, Brian Dean, M. Maccoss, F.D. Tattersall, Su-Er W. Huskey, J. J. Hale, Debra Luffer-Atlas, William P. Feeney, Richard J. Budhu, E. Ber, Richard Hargreaves, Margaret A. Cascieri, and Marc M. Kurtz

Subjects

Vomiting, Morpholines, Guinea Pigs, Drug Evaluation, Preclinical, Antineoplastic Agents, Pharmacology, Guinea pig, chemistry.chemical_compound, Structure-Activity Relationship, Acetals, Dogs, Neurokinin-1 Receptor Antagonists, In vivo, Morpholine, Drug Discovery, Animals, Humans, Prodrugs, Receptor, Trifluoromethyl, Chemistry, Anti-Inflammatory Agents, Non-Steroidal, Ferrets, Water, Biological activity, Stereoisomerism, Prodrug, In vitro, Rats, Biochemistry, Solubility, Molecular Medicine, Antiemetics, Cisplatin, Aprepitant

Abstract

The regioselective dibenzylphosphorylation of 2 followed by catalytic reduction in the presence of N-methyl-D-glucamine afforded 2-(S)-(1-(R)-(3, 5-bis(trifluoromethyl)phenyl)ethoxy)-3-(S)-(4-fluoro)phenyl-4-(5-(2- phosphoryl-3-oxo-4H,-1,2,4-triazolo)methylmorpholine, bis(N-methyl-D-glucamine) salt, 11. Incubation of 11 in rat, dog, and human plasma and in human hepatic subcellular fractions in vitro indicated that conversion to 2 would be expected to occur in vivo most readily in humans during hepatic circulation. Conversion of 11 to 2 occurred rapidly in vivo in the rat and dog with the levels of 11 being undetectable within 5 min after 1 and 8 mg/kg doses iv in the rat and within 15 min after 0.5, 2, and 32 mg/kg doses iv in the dog. Compound 11 has a 10-fold lower affinity for the human NK-1 receptor as compared to 2, but it is functionally equivalent to 2 in preclinical models of NK-1-mediated inflammation in the guinea pig and cisplatin-induced emesis in the ferret, indicating that 11 acts as a prodrug of 2. Based in part on these data, 11 was identified as a novel, water-soluble prodrug of the clinical candidate 2 suitable for intravenous administration in humans.

Published

2000

44. Serine derived NK1 antagonists. 1: The effect of modifications to the serine substituents

Author

Kevin John Merchant, Fintan Kelleher, Sharon Sadowski, Gary G. Chicchi, Jason Matthew Elliott, Richard Thomas Lewis, Graeme Irvine Stevenson, S. Davies, Angus Murray Macleod, Marc M. Kurtz, T. Ladduwahetty, and Margaret A. Cascieri

Subjects

inorganic chemicals, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Stereoisomerism, urologic and male genital diseases, Biochemistry, Chemical synthesis, Serine, Structure-Activity Relationship, Neurokinin-1 Receptor Antagonists, Piperidines, Drug Discovery, polycyclic compounds, medicine, Structure–activity relationship, heterocyclic compounds, Molecular Biology, Chemistry, organic chemicals, Organic Chemistry, In vitro, Chain length, Molecular Medicine

Abstract

A series of novel serine derived NK1 antagonists is described. The effect of variations in the N-benzyl, O-benzyl and serine groups are used to define the elements which are necessary for binding.

Published

1999

45. 4,4-Disubstituted piperidine high-affinity NK1 antagonists: structure-activity relationships and in vivo activity

Author

Graeme Irvine Stevenson, Gary G. Chicchi, Angus Murray Macleod, Tamara Ladduwahetty, Joseph M. Metzger, D. E. Macintyre, Timothy Harrison, Michael I. Graham, Fintan Kelleher, Balbinder Sohal, Marc M. Kurtz, Andrew Pate Owens, Kevin John Merchant, Christopher John Swain, Sharon Sadowski, Ian Thomas Huscroft, and Margaret A. Cascieri

Subjects

Male, Pyrrolidines, Stereochemistry, Inositol Phosphates, Guinea Pigs, Ether, CHO Cells, Chemical synthesis, Capillary Permeability, chemistry.chemical_compound, Radioligand Assay, Structure-Activity Relationship, Esophagus, Neurokinin-1 Receptor Antagonists, Piperidines, In vivo, Cricetinae, Drug Discovery, Side chain, Animals, Sulfonyl, chemistry.chemical_classification, Trifluoromethyl, Receptors, Neurokinin-1, Thiazoles, chemistry, Molecular Medicine, NK1 receptor antagonist, Piperidine, Diterpenes

Abstract

Previously reported studies from these laboratories described the design of a novel series of high-affinity NK1 antagonists based on the 4,4-disubstituted piperidine ring system. Further structure-activity studies have now established that for high NK1 affinity the benzyl ether side chain must be 3,5-disubstituted and highly lipophilic, the optimal side chain being the 3, 5-bis(trifluoromethyl)benzyl ether, 12 (hNK1 IC50 = 0.95 nM). Additional studies have shown that this class of NK1 antagonist tolerates a wider range of substituents on the piperidine nitrogen, including acyl (38) (hNK1 IC50 = 5.3 nM) and sulfonyl (39) (hNK1 IC50 = 5.7 nM) derivatives. Following preliminary pharmacokinetic analysis, two compounds (32 and 43) were selected for in vivo study in the resiniferotoxin-induced vascular leakage model, both showing excellent profiles (ID50 = 0.22 and 0.28 mg/kg, respectively).

Published

1998

46. In vitro and in vivo predictors of the anti-emetic activity of tachykinin NK1 receptor antagonists

Author

Angela Williams, W. Rycroft, Ian Thomas Huscroft, Emma J. Carlson, E. Ber, Jeffrey J. Hale, Sander G. Mills, Nadia M.J. Rupniak, F. David Tattersall, Malcolm MacCoss, Christopher John Swain, Richard Hargreaves, Sharon Sadowski, Eileen Mary Seward, Simon Neil Owen, Margaret A. Cascieri, and Raymond G. Hill

Subjects

medicine.drug_class, Stereochemistry, Administration, Oral, CHO Cells, Pharmacology, Substance P, Radioligand Assay, Pharmacokinetics, Neurokinin-1 Receptor Antagonists, In vivo, Cricetinae, medicine, Antiemetic, Animals, Humans, Cloning, Molecular, Receptor, Infusions, Intravenous, Membranes, Chemistry, Antagonist, Ferrets, Brain, Biological activity, In vitro, Peptide Fragments, Antiemetics, Cisplatin, Gerbillinae

Abstract

The ability of tachykinin NK1 receptor antagonists to inhibit GR73632 (D-Ala-[L-Pro9,Me-Leu8]substance P-(7-11))-induced foot tapping in gerbils was employed as an indirect measure of brain penetration and this was compared with their ability to prevent acute emesis induced by cisplatin in ferrets. (+)-GR203040 ((2S,3S and 2R,3R)-2-methoxy-5-tetrazol-1-yl-benzyl-(2-phenyl-piperidin- 3-yl)-amine), CP-99,994 ((2S,3S)-cis-3-(2-methoxybenzylamino)-2-phenyl piperidine) dihydrochloride), and L-742,694 (2-(S)-(3,5-bis(trifluoromethyl)benzyloxy)-3-(S)-phenyl-4-(5-(3-oxo-1,2, 4-triazolo)methylmorpholine) potently inhibited GR73632-induced foot tapping (ID50or = 0.85 mg/kg), and acute retching induced by cisplatin (ID50or = 0.18 mg/kg). RPR100893 ((3aS,4S,7aS)-7,7-diphenyl-4-(2-methoxyphenyl)-2-[(S)-2-(2-m ethoxyphenyl)proprionyl] perhydroisoindol-4-ol) was not a potent antagonist of retching (ID50 4.1 mg/kg) or foot tapping (ID5010 mg/kg). High doses (3-10 mg/kg) of CGP49823 ((2R,4S)-2-benzyl-1-(3,5-dimethylbenzoyl)-N-[(4-quinolinyl)methyl] -4-piperineamine) dihydrochloride), FK888 (N2-[(4R)-4-hydroxy-1-(1-methyl-1H-indol-3-yl)carbonyl-L-propyl]-N-methy l-N-phenylmethyl-L-3-(2-naphthyl)-alaninamide), and LY303870 ((R)-1-[N-(2-methoxybenzyl)acetylamino]-3-(1H-indol-3-yl)-2-[N-(2-(4-(pi peridinyl)piperidin-1-yl)acetyl)amino]propane) were required to inhibit foot tapping; these agents were not anti-emetic in this dose range. SR140333 ((S)-1-[2-[3-(3,4-dichlorphenyl)-1 (3-isopropoxyphenylacetyl)piperidin-3-yl] ethyl]-4-phenyl-1 azaniabicyclo [2.2.2]octane; 3-10 mg/kg) failed to inhibit foot tapping or emesis. Affinities for the human and ferret tachykinin NK1 receptor were highly correlated (r = 0.93, P = 0.0008). Inhibition of foot tapping in gerbils, but not NK1 receptor binding affinity, predicted anti-emetic activity in ferrets (r = 0.75, P0.01). These findings confirm that the anti-emetic activity of tachykinin NK1 receptor antagonists is dependent on brain penetration.

Published

1997

47. Characterization of the binding and activity of a high affinity, pseudoirreversible morpholino tachykinin NK1 receptor antagonist

Author

Michael R. Tota, Lin-Lin Shiao, Jeffrey J. Hale, Tung Ming Fong, E. Ber, Sander G. Mills, Catherine D. Strader, Malcolm MacCoss, Frank Tang, Margaret A. Cascieri, and Sharon Sadowski

Subjects

Agonist, Stereochemistry, medicine.drug_class, Morpholines, Substance P, CHO Cells, Spodoptera, Binding, Competitive, Cell Line, chemistry.chemical_compound, Neurokinin-1 Receptor Antagonists, Cricetinae, Tachykinin receptor 1, medicine, Animals, Humans, Binding site, Receptor, Pharmacology, Binding Sites, Chemistry, Antagonist, Receptors, Neurokinin-1, Recombinant Proteins, Kinetics, Competitive antagonist, Mutagenesis, Site-Directed, NK1 receptor antagonist, Baculoviridae

Abstract

2(S)-((3,5-Bis(trifluoromethyl)benzyl)-oxy)-3(S)-phenyl-4-((3-oxo-1,2,4-triazol-5-yl)methyl)morpholine (L-742,694) is a selective morpholino tachykinin NK1 receptor antagonist that inhibits the binding of 125I-substance P to the human tachykinin NK1 receptor with a Kd=37 pM. Increasing concentrations of L-742,694 added to cells 15 min prior to agonist progressively increase the apparent EC50 of substance P for inducing the synthesis of inositol phosphate in Chinese hamster ovary (CHO) cells expressing human tachykinin NK1 receptor and decrease the maximal level of stimulation observed. In contrast, addition of substance P and L-742,694 to the cells at the same time results in an increase in the EC50 for substance P with no decrease in the maximal level of stimulation. The compound also decreases the apparent number of binding sites for 125I-substance P observed by Scatchard analysis. Analysis of the binding of [3H]L-742,694 to the tachykinin NK1 receptor shows that it associates with the receptor with ka=3.98×108 M−1 min−1, and dissociates with kd=0.026 min−1 and t1/2=27 min at 22°C. The slow rate of dissociation of L-742,694 from the tachykinin NK1 receptor and the observation that altering the order of addition of antagonist and substance P attenuates the effect of the antagonist on the maximal activation suggest that L-742,694 is a competitive antagonist that can behave as a pseudoirreversible antagonist under some experimental conditions. L-742,694 has reduced affinity for tachykinin NK1 receptors in which alanine has been substituted for Gln165, His197 or His265 in transmembrane helices 4, 5 and 6, respectively. These three residues have previously been shown to be present in the binding site of tachykinin NK1 receptor antagonists of several structural classes. In addition, L-742,694 inhibits binding of the quinuclidine antagonist (2S,3S)-cis-2-(diphenyl methyl)-N-[(2-iodophenyl)-methyl]-1-azabicyclo[2.2.2]octane 3-amine ([125I]L-703,606) with the same affinity as it inhibits binding of 125I-substance P. These data indicate that L-742,694 binds to the same site within the transmembrane domain of the receptor as previously described competitive antagonists. © 1997 Elsevier Science B.V.

Published

1997

48. 4,4-Disubstituted piperidines: a new class of NK1 antagonist

Author

Graeme Irvine Stevenson, Angus Murray Macleod, Margaret A. Cascieri, Sharon Sadowski, Ian Thomas Huscroft, and Raymond Baker

Subjects

Structure-Activity Relationship, Neurokinin-1 Receptor Antagonists, Piperidines, Chemistry, Stereochemistry, Drug Discovery, Antagonist, Molecular Medicine, Structure–activity relationship, Humans, NK1 receptor antagonist, Selectivity, Chemical synthesis

Published

1995

49. N-Acyl-L-tryptophan benzyl esters: potent substance P receptor antagonists

Author

Raymond Baker, E. Ber, Kevin John Merchant, Sharon Sadowski, Margaret A. Cascieri, Angus Murray Macleod, and Christopher J. Swain

Subjects

Bicyclic molecule, Stereochemistry, Chemistry, Tryptophan, Antagonist, Esters, Biological activity, Receptors, Neurokinin-1, Alkylation, Peptide hormone, Substance P Receptor Antagonists, Receptors, Neurotransmitter, Structure-Activity Relationship, Benzyl Compounds, Drug Discovery, Humans, Molecular Medicine

Published

1993

50. Endothelial cell prostacyclin production induced by activated neutrophils

Author

Denis D. Soderman, Douglas K. Miller, Sharon Sadowski, and F A Kuehl

Subjects

medicine.medical_specialty, Leukotriene, biology, Neutrophile, Prostaglandin, hemic and immune systems, Prostacyclin, Cell Biology, Biochemistry, Molecular biology, Superoxide dismutase, Endothelial stem cell, Azurophilic granule, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, cardiovascular system, biology.protein, medicine, lipids (amino acids, peptides, and proteins), Arachidonic acid, Molecular Biology, circulatory and respiratory physiology, medicine.drug

Abstract

A bovine aortic endothelial cell (EC) line released prostacyclin (greater than 1 pmol/10(+5) EC cells) when incubated with fMet-Leu-Phe (FMLP)-stimulated rat and human neutrophils (PMNs). This prostaglandin (PG) I2 was shown to come from the ECs and not from the PMNs by radioactive, high-performance liquid chromatography, and immunochemical criteria. Both FMLP-stimulated rat peritoneal and human peripheral PMNs as well as their stimulated cell-free supernatants and unstimulated sonicates could elicit the release of PGI2 from ECs. Since phorbol myristate acetate stimulated PMN adherence but elicited little PGI2 release from ECs, the PGI2 stimulation in ECs is unrelated to PMN adhesion. The addition of catalase and superoxide dismutase to FMLP-stimulated PMNs enhanced rather than reduced PGI2 formation, indicating that activated oxygen products of the PMN are not responsible for the induction of PGI2. Incubation of ECs with leukotriene (LT) B4, LTC4, or LTD4 did not trigger PGI2 release nor did aspirin pretreatment of the PMNs reduce the PGI2 induction. These data suggest that arachidonic acid metabolites of the PMNs were not responsible for the PGI2 induction. Available data indicates that the PMN factor that stimulates PGI2 from ECs is either released concomitantly with the azurophilic granules or is closely related to this event.

Published

1985