Your search keyword '"Kathleen M. Metters"' showing total 62 results

1. Identification of an indole series of prostaglandin D2 receptor antagonists

Author

Bruno Roy, Claudio Sturino, Nicolas Lachance, Robert Zamboni, Kathleen M. Metters, Christine Brideau, Lianhai Li, John Scheigetz, Danielle Denis, Deborah Slipetz, Marie-Claude Carrière, Elizabeth Cauchon, Gillian Greig, Gary P. O'Neill, Carl Berthelette, Michael J. Boyd, Marie-Claude Mathieu, Sonia Lamontagne, Nicole Sawyer, Robert N. Young, Nancy N. Tsou, Zhaoyin Wang, Stacia Kargman, and Marc Labelle

Subjects

Indole test, Indoles, Molecular Structure, Chemistry, Receptors, Prostaglandin, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Biochemistry, Chemical synthesis, In vitro, Structure-Activity Relationship, chemistry.chemical_compound, Safrole, Drug Discovery, Molecular Medicine, Prostaglandin D2, Receptors, Immunologic, Receptor, Molecular Biology, Prostaglandin G2, Prostaglandin D2 receptor

Abstract

A novel indole series of PGD2 receptor (DP receptor) antagonists is presented. Optimization of this series led to the identification of potent and selective DP receptor antagonists. In particular, antagonists 35 and 36 were identified with Ki values of 2.6 and 1.8 nM, respectively. These two antagonists are also potent in a DP functional assay where they inhibit the PGD2 induced cAMP production in platelet rich plasma with IC50 values of 7.9 and 8.6 nM, respectively. The structure–activity relationships of this indole series of DP receptor antagonists will also be discussed.

Published

2006

2. Antagonism of the prostaglandin D 2 receptor 1 suppresses nicotinic acid-induced vasodilation in mice and humans

Author

Keith M. Gottesdiener, Kenneth K. Wu, Kang Cheng, Samuel D. Wright, Kathleen M. Metters, Eseng Lai, M. Gerard Waters, Claudio Sturino, Zhaoyin Wang, Tsuei-Ju Wu, and Gary P. O'Neill

Subjects

Adult, Male, Agonist, medicine.medical_specialty, Adolescent, medicine.drug_class, Receptors, Prostaglandin, Prostaglandin, Vasodilation, Niacin, Mice, chemistry.chemical_compound, Internal medicine, Flushing, medicine, Animals, Humans, Receptors, Immunologic, Receptor, Prostaglandin D2 receptor, Mice, Knockout, Multidisciplinary, Aspirin, Prostaglandin D2, Chemistry, Hydantoins, Middle Aged, Biological Sciences, Mice, Inbred C57BL, Endocrinology, Nicotinic agonist, Prostaglandin-Endoperoxide Synthases, Female

Abstract

Nicotinic acid (NA) is commonly used to treat dyslipidemia, but it elicits an adverse effect, termed flushing, which consists of cutaneous vasodilation with associated discomfort. An animal model of NA-induced flushing has been established in mice. As in humans, NA stimulated vasodilation in a dose-dependent manner, was associated with an increase of the vasodilatory prostaglandin (PG) D 2 in plasma and could be blocked by pretreatment with aspirin. Two PGD 2 receptors have been identified: PGD 2 receptor 1 (DP1, also called DP) and PGD 2 receptor 2 (DP2, sometimes termed CRTH2). DP2 does not mediate NA-induced vasodilation; the DP2-specific agonist DK-PGD 2 (13,14-dihydro-15-keto-PGD 2 ) did not induce cutaneous vasodilation, and DP2 −/− mice had a normal vasodilatory response to NA. By contrast, BW245C, a DP1-selective agonist, induced vasodilation in mice, and MK-0524, a DP1-selective antagonist, blocked both PGD 2 - and NA-induced vasodilation. NA-induced vasodilation was also studied in DP1 +/+ , DP1 +/− , and DP1 −/− mice; although NA-induced vasodilation depended almost completely on DP1 in female mice, it depended only partially on DP1 in male mice. The residual NA-induced vasodilation in male DP −/− mice was aspirin-sensitive. Thus, in the mouse, DP1 appears to be an important component involved in NA-induced vasodilation, but other cyclooxygenase-dependent mechanisms also may be involved. A clinical study in healthy men and women demonstrated that treatment with MK-0524 reduced the symptoms of flushing and the increase in skin perfusion after the administration of NA. These studies suggest that DP1 receptor antagonism may be an effective means to suppress NA-induced flushing in humans.

Published

2006

3. 2,3-Diarylthiophenes as selective EP1 receptor antagonists

Author

Richard Friesen, Gillian Greig, Nicole Sawyer, Bernard Cote, Stacia Kargman, Sonia Lamontagne, Kathleen M. Metters, Richard Frenette, Yves Ducharme, Gary P. O'Neill, François Nantel, Marie-Claude Carrière, Evelyn Martins, Anne Chateauneuf, Danielle Denis, and Marc Blouin

Subjects

Clinical Biochemistry, Pharmaceutical Science, Thiophenes, Pharmacology, Biochemistry, Chemical synthesis, Cell Line, Structure-Activity Relationship, Pharmacokinetics, In vivo, Drug Discovery, Animals, Humans, Receptors, Prostaglandin E, Structure–activity relationship, Tissue Distribution, Receptor, Molecular Biology, Chemistry, Organic Chemistry, Antagonist, Brain, Receptors, Prostaglandin E, EP1 Subtype, In vitro, Rats, Cell culture, Molecular Medicine, Half-Life

Abstract

The synthesis and the EP(1) receptor binding affinity of 2,3-diarylthiophene derivatives are described. The evaluation of the structure-activity relationship (SAR) in this series led to the identification of compounds 4, 7, and 12a, which exhibit high affinity for the human EP(1) receptor and a selectivity greater than 100-fold against the EP(2), EP(3), EP(4), DP, FP, and IP receptors and greater than 25-fold versus the TP receptor. These three antagonists present good pharmacokinetics in rats and significant differences in the way they are distributed in the brain.

Published

2005

4. Expression of prostaglandin D synthase and the prostaglandin D2 receptors DP and CRTH2 in human nasal mucosa

Author

Kathleen M. Metters, Martin Desrosiers, Gary P. O'Neill, François G. Gervais, Carolyn Fong, Sonia Lamontagne, François Nantel, D. Hamish Wright, and Adel Giaid

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Physiology, T-Lymphocytes, Receptors, Prostaglandin, Prostaglandin, Mucous membrane of nose, Thymus Gland, In situ hybridization, Lipocalin, Biochemistry, Prostaglandin-D synthase, chemistry.chemical_compound, Nasal Polyps, Hypersensitivity, Humans, Medicine, Mast Cells, RNA, Messenger, Receptors, Immunologic, Receptor, In Situ Hybridization, Aged, Inflammation, Pharmacology, biology, business.industry, Cell Biology, Middle Aged, respiratory system, Lipocalins, Eosinophils, Intramolecular Oxidoreductases, Nasal Mucosa, Gene Expression Regulation, chemistry, biology.protein, Immunohistochemistry, Female, Lymph Nodes, Prostaglandin D2, business

Abstract

Rationale Prostaglandin D 2 (PGD 2 ) is released from mast cells during the allergic response. Since PGD 2 has been shown to induce nasal congestion in humans, we investigated the distribution of hematopoietic Prostaglandin D synthase (PGDS) and the two PGD 2 receptors, DP and CRTH2 in human nasal mucosa from healthy subjects and subjects suffering from polyposis, a severe form of chronic rhinosinusitis. Methods DP mRNA expression was detected by in situ hybridization while PGDS, CRTH2 and various leukocyte markers expression was revealed by immunohistochemistry. Results In the normal mucosa, PGDS was only detected in few resident mast cells while CRTH2 was undetectable. In contrast, DP receptor mRNA was detected in epithelial goblet cells, serous glands and in the vasculature. In the nasal mucosa of subjects suffering from polyposis: 1) PGDS was detected in mast cells and other large infiltrating inflammatory cells, 2) both DP mRNA and CRTH2 were detected in eosinophils and 3) CRTH2 was detected on a subset of infiltrating T-cells. Although DP mRNA could not be detected in the T-cells invading the nasal mucosa, it was found to be expressed in the T-cells present in the lymph node and the thymus from normal individuals. Conclusions This study indicates that cells capable of producing PGD 2 are present in the nasal mucosa and that both PGD 2 receptors, DP and CRTH2, might play a role in inflammatory disease of the upper airways.

Published

2004

5. Molecular pharmacology of the human prostaglandin D2receptor, CRTH2

Author

Elizabeth Cauchon, Nicole Sawyer, François G. Gervais, Rani P.G. Cruz, Gary P. O'Neill, Donald W. Nicholson, Kathleen M. Metters, and Anne Chateauneuf

Subjects

Pharmacology, education.field_of_study, Ligand binding assay, Population, respiratory system, Biology, Molecular biology, Dissociation constant, chemistry.chemical_compound, chemistry, Biochemistry, Potency, lipids (amino acids, peptides, and proteins), Prostaglandin D2, Binding site, Receptor, education, Prostaglandin D2 receptor

Abstract

1. The recombinant human prostaglandin D(2) (PGD(2)) receptor, hCRTH2, has been expressed in HEK293(EBNA) and characterized with respect to radioligand binding and signal transduction properties. High and low affinity binding sites for PGD(2) were identified in the CRTH2 receptor population by saturation analysis with respective equilibrium dissociation constants (K(D)) of 2.5 and 109 nM. This revealed that the affinity of PGD(2) for CRTH2 is eight times less than its affinity for the DP receptor. 2. Equilibrium competition binding assays revealed that of the compounds tested, only PGD(2) and several related metabolites bound with high affinity to CRTH2 (K(i) values ranging from 2.4 to 34.0 nM) with the following rank order of potency: PGD(2)>13,14-dihydro-15-keto PGD(2)>15-deoxy-Delta(12,14)-PGJ(2)>PGJ(2)>Delta(12)-PGJ(2)>15(S)-15 methyl-PGD(2). This is in sharp contrast with the rank order of potency obtained at DP : PGD(2)>PGJ(2)>Delta(12)-PGJ(2)>15-deoxy-Delta(12,14)-PGJ(2) >>>13,14-dihydro-15-keto-PGD(2). 3. Functional studies demonstrated that PGD(2) activation of recombinant CRTH2 results in decrease of intracellular cAMP in a pertussis toxin-sensitive manner. Therefore, we showed that CRTH2 can functionally couple to the G-protein G(alphai/o). PGD(2) and related metabolites were tested and their rank order of potency followed the results of the membrane binding assay. 4. By Northern blot analysis, we showed that, besides haemopoietic cells, CRTH2 is expressed in many other tissues such as brain, heart, thymus, spleen and various tissues of the digestive system. In addition, in situ hybridization studies revealed that CRTH2 mRNA is expressed in human eosinophils. Finally, radioligand binding studies demonstrated that two eosinophilic cell lines, butyric acid-differentiated HL-60 and AML 14.3D10, also endogenously express CRTH2.

Published

2002

6. Selective modulation of chemokinesis, degranulation, and apoptosis in eosinophils through the PGD2 receptors CRTH2 and DP

Author

Anne Chateauneuf, Gary P. O'Neill, Rani P.G. Cruz, Stephen Gale, François G. Gervais, François Nantel, Kathleen M. Metters, and Nicole Sawyer

Subjects

Receptors, Prostaglandin, Immunology, Chemokinesis, Eosinophil-derived neurotoxin, Apoptosis, Biology, medicine.disease_cause, Cell Degranulation, chemistry.chemical_compound, Cell Movement, medicine, Humans, Immunology and Allergy, Eosinophil degranulation, RNA, Messenger, Receptors, Immunologic, Cells, Cultured, Eosinophil cationic protein, Prostaglandin D2, Degranulation, respiratory system, Eosinophil, Eosinophils, medicine.anatomical_structure, chemistry, Allergic response, lipids (amino acids, peptides, and proteins)

Abstract

Background: PGD 2 is the major prostanoid released by mast cells during an allergic response. Its role in the allergic response, however, remains unclear. Objective: Because the accumulation of eosinophils is a feature of allergic reactions, we investigated the role of PGD 2 in the modulation of eosinophil function. Methods: Circulating human eosinophils were isolated and challenged with PGD 2 . The effects of PGD 2 on various eosinophil functions were then analyzed. Results: PGD 2 binds with high affinity preferentially to 2 receptors, DP and chemoattractant receptor-homologous molecule expressed on T H 2 cells (CRTH2). We show that both DP and CRTH2 are detectable on circulating eosinophils. We demonstrate that PGD 2 (1-10 nmol/L) induces a rapid change in human eosinophil morphology and an increase in chemokinesis and promotes eosinophil degranulation. These effects are induced by the CRTH2-selective agonist 13-14-dihydro-15-keto-PGD 2 (DK-PGD 2 ) but not by the DP-selective agonist BW245C. These results suggest a role for CRTH2 in the modulation of eosinophil movement and in triggering the release of cytotoxic proteins. Finally, we demonstrate that BW245C, but not DK-PGD 2 , can delay the onset of apoptosis in cultured eosinophils, presumably through interaction with DP. Conclusion: These data support the hypothesis that PGD 2 controls eosinophil functions through 2 pharmacologically distinct receptors with independent functions. Blockade of PGD 2 -mediated effects on human eosinophils may reduce the damage caused by these cells during an allergic response, but inhibition of both receptors may be required. (J Allergy Clin Immunol 2001;108:982-8.)

Published

2001

7. Preclinical pharmacological studies with montelukast (Singulair), a selective cysteinyl leukotriene receptor (CysLT1) antagonist

Author

Thomas R. Jones, Kathleen M. Metters, and Jillian F. Evans

Subjects

business.industry, Immunology, Antagonist, medicine, Immunology and Allergy, Pharmacology, business, Cysteinyl leukotriene receptor, Montelukast, medicine.drug

Published

2001

8. Sequestration and phosphorylation of the prostaglandin E2 EP4 receptor: dependence on the C-terminal tail33Abbreviations: PGE2, prostaglandin E2, GRK, G-protein coupled receptor kinase; PKA, protein kinase A; PKC, protein kinase C; PCR, polymerase chain reaction; DMEM, Dulbecco’s modified Eagle’s medium; PAS, protein A Sepharose; ECL, electrochemiluminescence; BCA, 2-bicinchoninic acid; IR, immunoreactivity; HBSS, Hanks’ buffered salt solution; TBS, Tris-buffered saline; cAMP, cyclic AMP; PMA, phorbol 12-myristate 13 acetate; and β2-AR, β2-adrenergic receptor

Author

Kathleen M. Metters, Natalie Brewer, Deborah Slipetz, Stephanie Buchanan, Cameron D. Mackereth, Vanessa Pellow, Mark Abramovitz, Chuan-ming Hao, and Mohammed Adam

Subjects

Pharmacology, medicine.medical_specialty, Forskolin, EP4 Receptor, Biology, Biochemistry, Molecular biology, Adenylyl cyclase, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Phorbol, medicine, Phosphorylation, Receptor, Protein kinase A, Protein kinase C

Abstract

The prostaglandin E 2 (PGE 2 ) EP 4 subtype is one of four prostanoid receptors that use PGE 2 as the preferred ligand. We have investigated the agonist-mediated regulation of EP 4 using a multifaceted approach. Short-term (30 min) agonist challenge of recombinant EP 4 expressed in human embryonic kidney 293 cells (EP 4 -HEK293 cells) with PGE 2 (1 μM) resulted in the desensitization of intracellular cyclic AMP (cAMP) accumulation and a reduction in cell surface [ 3 H]PGE 2 specific binding sites. These events correlated with sequestration of EP 4 , as visualized by immunofluorescence confocal microscopy and phosphorylation, as shown by [ 32 P]orthophosphate labeling of the receptor. Stimulation of protein kinase A activity in EP 4 -HEK293 cells (10 μM forskolin or 1 mM 8-bromo-cAMP) did not induce EP 4 desensitization, sequestration, or phosphorylation. In contrast, stimulation of protein kinase C activity (100 nM phorbol 12-myristate 13-acetate) attenuated PGE 2 -induced adenylyl cyclase activity and increased EP 4 phosphorylation, but did not induce sequestration or a reduction in [ 3 H]PGE 2 specific binding sites. EP 4 receptors containing a third intracellular loop deletion [EP 4 (del. 215–263)] or a carboxyl-terminal tail truncation [EP 4 (del. 355)] of EP 4 were used to demonstrate that the C-terminal tail governs sequestration as well as phosphorylation of the receptor.

Published

2001

9. Prostaglandin Receptor EP4 Mediates the Bone Anabolic Effects of PGE2

Author

Marc Labelle, Nicolas Lachance, Sevgi B. Rodan, G. Seedor, Michel Gallant, Kathleen M. Metters, Mohamed Machwate, Chi-Tai Leu, Deborah A. Slipetz, S. Hutchins, Nicole Sawyer, Gideon A. Rodan, Shun-ichi Harada, and Robert N. Young

Subjects

Male, medicine.medical_specialty, Anabolism, medicine.medical_treatment, Prostaglandin, Thiophenes, Bone and Bones, Dinoprostone, Rats, Sprague-Dawley, chemistry.chemical_compound, In vivo, Periosteum, Internal medicine, medicine, Animals, Humans, Receptors, Prostaglandin E, Sulfhydryl Compounds, Prostaglandin receptor, Receptor, Cells, Cultured, Pharmacology, Antagonist, Prostanoid, Rats, Endocrinology, chemistry, Molecular Medicine, Receptors, Prostaglandin E, EP4 Subtype, Prostaglandin E

Abstract

Prostaglandin (PG) E(2) is a potent inducer of cortical and trabecular bone formation in humans and animals. Although the bone anabolic action of PGE(2) is well documented, the cellular and molecular mechanisms that mediate this effect remain unclear. This study was undertaken to examine the effect of pharmacological inactivation of the prostanoid receptor EP(4), one of the PGE(2) receptors, on PGE(2)-induced bone formation in vivo. We first determined the ability of EP(4)A, an EP(4)-selective ligand, to act as an antagonist. PGE(2) increases intracellular cAMP and suppresses apoptosis in the RP-1 periosteal cell line. Both effects were reversed by EP(4)A, suggesting that EP(4)A acts as an EP(4) antagonist in the cells at concentrations consistent with its in vitro binding to EP(4). We then examined the effect of EP(4) on bone formation induced by PGE(2) in young rats. Five- to 6-week-old rats were treated with PGE(2) (6 mg/kg/day) in the presence or absence of EP(4)A (10 mg/kg/day) for 12 days. We found that treatment with EP(4)A suppresses the increase in trabecular bone volume induced by PGE(2). This effect is accompanied by a suppression of bone formation indices: serum osteocalcin, extent of labeled surface, and extent of trabecular number, suggesting that the reduction in bone volume is due most likely to decreased bone formation. The pharmacological evidence presented here provides strong support for the hypothesis that the bone anabolic effect of PGE(2) in rats is mediated by the EP(4) receptor.

Published

2001

10. The human prostanoid DP receptor stimulates mucin secretion in LS174T cells

Author

Kathleen M. Metters, Kris Chadee, D. Hamish Wright, and Anthony W. Ford-Hutchinson

Subjects

Pharmacology, medicine.medical_specialty, Prostaglandin E2 receptor, Mucin, Prostaglandin, Prostanoid, In situ hybridization, Biology, Molecular biology, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, medicine, lipids (amino acids, peptides, and proteins), Prostaglandin D2, Signal transduction, Receptor

Abstract

This study demonstrates the localization of the prostaglandin (PG)D2 receptor (DP) within the mucous-secreting globlet cells of the human colon by in situ hybridization, which suggests a role for DP in mucous secretion. Selective high affinity ligands were used, therefore, to evaluate DP regulation of mucous secretion in LS174T human colonic adenocarcinoma cells. The expression of hDP in LS174T cells was confirmed at the mRNA level by reverse transcriptase-polymerase chain reaction, and at the protein level by radioligand binding assays and signal transduction (cyclic AMP accumulation) assays. PGD2 and the highly selective DP-specific agonist L-644,698 ((4-(3-(3-(3-hydroxyoctyl)-4-oxo-2-thiazolidinyl) propyl) benzoic acid) (racemate)), but not PGE2 competed for [3H]-PGD2-specific binding to LS174T cell membranes (Ki values of 0.4 nM and 7 nM, respectively). The DP-specific agonists PGD2, PGJ2, BW245C (5-(6-carboxyhexyl)-1-(3-cyclohexyl-3-hydroxypropylhydantoin)), and L-644,698 showed similar potencies in stimulating cyclic AMP accumulation (EC50 values: 45–90 nM) and demonstrated the expected rank order of potency. PGE2 also elicited cyclic AMP production in this cell line (EC50 value: 162 nM). The activation of cyclic AMP production by PGD2 and L-644,698, but not PGE2, was inhibited by the selective DP antagonist BW A868C. Thus, PGD2 and L-644,698 act through hDP in LS174T cells. PGD2, L-644,698 and PGE2 (an established mucin secretagogue) potently stimulated mucin secretion in LS174T cells in a concentration-dependent manner (EC50

Published

2000

11. Characterization of the Human Cysteinyl Leukotriene 2 Receptor

Author

Qingyun Liu, Tuan V. Nguyen, David J. Figueroa, Rino Stocco, Kevin R. Lynch, Mark Abramovitz, Lei Ma, Jilly F. Evans, Dong Soon Im, Regina Cheng, Christopher P. Austin, Susan R. George, Brian F. O'Dowd, Zhizhen Zeng, Christopher E. Heise, Nathalie Coulombe, Michelle K. Clements, Julie N. Bellefeuille, Kathleen M. Metters, Gary P. O'Neill, David L. Williams, Yuan Liu, and Nicole Sawyer

Subjects

Models, Molecular, Leukotrienes, Biology, Pharmacology, Biochemistry, Leukotriene D4, Estrogen-related receptor alpha, Enzyme-linked receptor, Humans, Tissue Distribution, 5-HT5A receptor, Cysteine, Cloning, Molecular, Lung, Molecular Biology, Protease-activated receptor 2, Leukotriene E4, Receptors, Leukotriene, Sequence Homology, Amino Acid, Myocardium, Membrane Proteins, Sequence Analysis, DNA, Cell Biology, respiratory system, Leukotriene C4, Recombinant Proteins, Interleukin 10, Cysteinyl leukotriene receptor 1, Cysteinyl leukotriene receptor 2, Adrenal Medulla, Interleukin-21 receptor, Leukotriene Antagonists, SRS-A, lipids (amino acids, peptides, and proteins)

Abstract

The contractile and inflammatory actions of the cysteinyl leukotrienes (CysLTs), LTC(4), LTD(4), and LTE(4), are thought to be mediated through at least two distinct but related CysLT G protein-coupled receptors. The human CysLT(1) receptor has been recently cloned and characterized. We describe here the cloning and characterization of the second cysteinyl leukotriene receptor, CysLT(2), a 346-amino acid protein with 38% amino acid identity to the CysLT(1) receptor. The recombinant human CysLT(2) receptor was expressed in Xenopus oocytes and HEK293T cells and shown to couple to elevation of intracellular calcium when activated by LTC(4), LTD(4), or LTE(4). Analyses of radiolabeled LTD(4) binding to the recombinant CysLT(2) receptor demonstrated high affinity binding and a rank order of potency for competition of LTC(4) = LTD(4) LTE(4). In contrast to the dual CysLT(1)/CysLT(2) antagonist, BAY u9773, the CysLT(1) receptor-selective antagonists MK-571, montelukast (Singulair(TM)), zafirlukast (Accolate(TM)), and pranlukast (Onon(TM)) exhibited low potency in competition for LTD(4) binding and as antagonists of CysLT(2) receptor signaling. CysLT(2) receptor mRNA was detected in lung macrophages and airway smooth muscle, cardiac Purkinje cells, adrenal medulla cells, peripheral blood leukocytes, and brain, and the receptor gene was mapped to chromosome 13q14, a region linked to atopic asthma.

Published

2000

12. Distribution and regulation of cyclooxygenase-2 in carrageenan-induced inflammation

Author

Kathleen M. Metters, Maria Cirino, Chi-Chung Chan, François Nantel, Robert Gordon, Angela Northey, and Danielle Denis

Subjects

Pharmacology, medicine.medical_specialty, biology, Prostanoid, Prostaglandin, Inflammation, Carrageenan, chemistry.chemical_compound, Endocrinology, chemistry, Edema, Internal medicine, Hyperalgesia, medicine, biology.protein, Cyclooxygenase, medicine.symptom, Prostaglandin E2, medicine.drug

Abstract

1 We characterized the regulation of cyclooxygenase-2 (COX-2) at the mRNA, protein and mediator level in two rat models of acute inflammation, carrageenan-induced paw oedema and mechanical hyperalgesia. 2 Carrageenan was injected in the hind paw of rat at low (paw oedema) and high doses (hyperalgesia). COX-2 and prostaglandin E2 (PGE2) levels were measured by RT-PCR and immunological assays. We also determined the distribution of COX-2 by immunohistochemistry. 3 The injection of carrageenan produced a significant and parallel induction of both COX-2 and PGE2. This induction was significantly higher in hyperalgesia than in paw oedema. This was probably due to the 9 fold higher concentration of carrageenan used to provoke hyperalgesia. 4 Immunohistochemical examination showed COX-2 immunoreactivity in the epidermis, skeletal muscle and inflammatory cells of rats experiencing hyperalgesia. In paw oedema however, only the epidermis showed positive COX-2 immunoreactivity. 5 Pretreatment with indomethacin completely abolished the induction of COX-2 in paw oedema but not in hyperalgesia. 6 These results suggest that multiple mechanisms regulate COX-2 induction especially in the more severe model. In carrageenan-induced paw oedema, prostanoid production have been linked through the expression of the COX-2 gene which suggest the presence of a positive feedback loop mechanism.

Published

1999

13. Characterization of the recombinant human prostanoid DP receptor and identification of L-644,698, a novel selective DP agonist

Author

Kathleen M. Metters, D. Hamish Wright, Anthony W. Ford-Hutchinson, and Mark Abramovitz

Subjects

Pharmacology, Agonist, chemistry.chemical_classification, Stereochemistry, Chemistry, medicine.drug_class, Prostaglandin E2 receptor, Prostanoid, Adenosine, chemistry.chemical_compound, Adenine nucleotide, medicine, Nucleotide, Signal transduction, Receptor, medicine.drug

Abstract

1. A human embryonic kidney cell line [HEK 293(EBNA)] stably expressing the human recombinant prostaglandin D2 (PGD2) receptor (hDP) has been characterized with respect to radioligand binding and signal transduction properties by use of prostanoids and prostanoid analogues. Radioligand binding studies included saturation analyses, the effects of nucleotide analogues, the initial rate of ligand-receptor association and equilibrium competition assays. In addition, adenosine 3':5'-cyclic monophosphate (cyclic AMP) generation in response to ligand challenge was also measured, as this is the predominant hDP signalling pathway. 2. L-644,698 ((4-(3-(3-(3-hydroxyoctyl)-4-oxo-2-thiazolidinyl) propyl) benzoic acid) (racemate)) was identified as a novel ligand having high affinity for hDP with an inhibitor constant (Ki) of 0.9 nM. This Ki value was comparable to the Ki values obtained in this study for ligands that have previously shown high affinity for DP: PGD2 (0.6 nM), ZK 110841 (0.3 nM), BW245C (0.4 nM), and BW A868C (2.3 nM). 3. L-644,698 was found to be a full agonist with an EC50 value of 0.5 nM in generating cyclic AMP following activation of hDP. L-644,698 is, therefore, comparable to those agonists with known efficacy at the DP receptor (EC50): PGD2 (0.5 nM), ZK 110841 (0.2 nM) and BW245C (0.3 nM). 4. L-644,698 displayed a high degree of selectivity for hDP when compared to the family of cloned human prostanoid receptors: EP1 (> 25,400 fold), EP2 (approximately 300 fold), EP3-III (approximately 4100 fold), EP4 (approximately 10000 fold), FP (> 25,400 fold), IP (> 25,400 fold) and TP (> 25,400 fold). L-644,698 is, therefore, one of the most selective DP agonists as yet described. 5. PGJ2 and delta12-PGJ2, two endogenous metabolites of PGD2, were also tested in this system and shown to be effective agonists with Ki and EC50 values in the nanomolar range for both compounds. In particular, PGJ2 was equipotent to known DP specific agonists with a Ki value of 0.9 nM and an EC50 value of 1.2 nM.

Published

1998

14. A series of non-quinoline cysLT1 receptor antagonists: Sar study on pyridyl analogs of singulair®

Author

C. S. Mcfarlane, Robert Zamboni, C. Rochette, M. McAuliffe, Claude Dufresne, P. Prasit, Jacques-Yves Gauthier, Nicole Sawyer, P. Roy, Kathleen M. Metters, Thomas R. Jones, and Daniel Guay

Subjects

Cyclopropanes, Leukotriene D4, Pyridines, Stereochemistry, Guinea Pigs, Clinical Biochemistry, Pharmaceutical Science, Acetates, Sulfides, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Anti-Asthmatic Agents, Receptor, Saimiri, Molecular Biology, Montelukast, Receptors, Leukotriene, Leukotriene, Bicyclic molecule, Chemistry, Organic Chemistry, Quinoline, Membrane Proteins, Rats, Quinolines, Leukotriene Antagonists, Molecular Medicine, medicine.drug

Abstract

The structure-activity relationship of a series of styrylpyridine analogs of MK-0476 (montelukast, Singulair) is described. This work has led to the identification of a number of potent and orally active cysLT1 receptor (LTD4 receptor) antagonists including 2ab (L-733,321) as an optimized candidate.

Published

1998

15. Molecular cloning and characterization of the four rat prostaglandin E2 prostanoid receptor subtypes

Author

Gerhard Püschel, Deborah Slipetz, Yves Boie, Frank Neuschäfer-Rube, Rino Stocco, Mark Abramovitz, Nicole Sawyer, Mark Ungrin, and Kathleen M. Metters

Subjects

Male, endocrine system, Prostaglandin E2 receptor, Molecular Sequence Data, EP4 Receptor, Prostaglandin, Biology, Kidney, Ligands, Dinoprostone, Cell Line, Thromboxane receptor, Mice, Radioligand Assay, 03 medical and health sciences, chemistry.chemical_compound, Aequorin, 0302 clinical medicine, medicine, Animals, Humans, Receptors, Prostaglandin E, Amino Acid Sequence, Cloning, Molecular, Prostaglandin E2, Receptor, 030304 developmental biology, Pharmacology, 0303 health sciences, Cell Membrane, Prostanoid, respiratory system, Blotting, Northern, musculoskeletal system, Rats, Liver, chemistry, Biochemistry, Luminescent Measurements, cardiovascular system, lipids (amino acids, peptides, and proteins), Prostaglandin D2, Spleen, 030217 neurology & neurosurgery, medicine.drug

Abstract

We have characterized the rat prostanoid EP1, EP2, EP3alpha and EP4 receptor subtypes cloned from spleen, hepatocyte and/or kidney cDNA libraries. Comparison of the deduced amino acid sequences of the rat EP receptors with their respective homologues from mouse and human showed 91% to 98% and 82% to 89% identity, respectively. Radioreceptor binding assays and functional assays were performed on EP receptor expressing human embryonic kidney (HEK) 293 cells. The KD values obtained with prostaglandin E2 for the prostanoid receptor subtypes EP1, EP2, EP3alpha and EP4 were approximately 24, 5, 1 and 1 nM, respectively. The rank order of affinities for various prostanoids at the prostanoid receptor subtypes EP2, EP3alpha and EP4 receptor subtypes was prostaglandin E2 = prostaglandin E1iloprostprostaglandin F2alphaprostaglandin D2U46619. The rank order at the prostanoid EP1 receptor was essentially the same except that iloprost had the highest affinity of the prostanoids tested. Of the selective ligands, butaprost was selective for prostanoid EP2, MB28767 and sulprostone were selective for EP3alpha and enprostil displayed dual selectivity, interacting with both prostanoid receptor subtypes EP1 and EP3alpha. All four receptors coupled to their predominant signal transduction pathways in HEK 293 cells. Notably, using a novel aequorin luminescence assay to monitor prostanoid EP1 mediated increases in intracellular calcium, both iloprost and sulprostone were identified as partial agonists. Finally, by Northern blot analysis EP3 transcripts were most abundant in liver and kidney whereas prostanoid EP2 receptor mRNA was expressed in spleen, lung and testis and prostanoid EP1 receptor mRNA transcripts were predominantly expressed in the kidney. The rat prostanoid EP1 probes also detected additional and abundant transcripts present in all the tissues examined. These were found to be related to the expression of a novel protein kinase gene and not the prostanoid EP1 gene [Batshake, B., Sundelin, J., 1996. The mouse genes for the EP1 prostanoid receptor and the novel protein kinase overlap. Biochem. Biophys. Res. Commun. 227. 1329-1333].

Published

1997

16. New class of potent ligands for the human peripheral cannabinoid receptor

Author

Yves Leblanc, Michel Gallant, Nathalie Tremblay, Marc Labelle, Claude Dufresne, Deborah Slipetz, C. Rochette, P. Prasit, Kathleen M. Metters, Daniel Guay, Yves Gareau, and Nicole Sawyer

Subjects

Indole test, Cannabinoid receptor, Chemistry, Ligand, Stereochemistry, medicine.medical_treatment, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Drug Discovery, medicine, Molecular Medicine, Cannabinoid, Receptor, Selectivity, Molecular Biology

Abstract

A new class of potent ligand for the human peripheral cannabinoid (hCB 2 ) receptor is described. Two indole analogs 13 and 17 exhibited nanomolar potencies (K i ) with good selectivity for the hCB 2 receptor over the human central cannabinoid (hCB 1 ) receptor.

Published

1996

17. Discovery of L-740,515, a potent thienopyridine cysLT1 receptor (LTD4 receptor) antagonist

Author

M. Belley, Yves Leblanc, Kathleen M. Metters, M. McAuliffe, Nicole Sawyer, Claude Dufresne, Anthony W. Ford-Hutchinson, Robert Zamboni, Deborah Slipetz, Thomas R. Jones, Cheuk K. Lau, Robert N. Young, C.B. Pickett, C. Rochette, C. S. Mcfarlane, Zhaoyin Wang, Helene Perrier, Nathalie Ouimet, Marc Labelle, Yves Gareau, and Xiang Yi Bin

Subjects

Thienopyridine, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Quinoline, Antagonist, Pharmaceutical Science, Ring (chemistry), Biochemistry, In vitro, chemistry.chemical_compound, In vivo, Drug Discovery, medicine, Molecular Medicine, Receptor, Molecular Biology, Montelukast, medicine.drug

Abstract

Structure-activity studies leading to the discovery of a new series of non-quinoline cysLT 1 receptor (LTD 4 receptor) antagonists are described. These studies demonstrated that the quinoline ring system of montelukast ( 5 ) may be replaced by an appropriately substituted thienopyridine system, yielding potent compounds. Two other molecular features of montelukast, the terminal phenyl ring substitution and the vinyl link, were also reevaluated. These studies led to the identification of 1 (L-740,515) , a compound with optimized in vitro and in vivo biological profiles.

Published

1995

18. Evolution of a series of non-quinoline leukotriene D4 receptor antagonist; synthesis and sar of benzothiazoles and thiazoles substituted benzyl alcohols as potent LTD4 antagonists

Author

C. Rochette, Robert Zamboni, Anthony W. Ford-Hutchinson, Claude Dufresne, Marc Labelle, Deborah Slipetz, C. S. Mcfarlane, Thomas R. Jones, Yves Gareau, Lau Cheuk-Kun, Robert N. Young, L. Charette, Kathleen M. Metters, M. McAuliffe, and Nicole Sawyer

Subjects

LTD4 receptor, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Quinoline, Antagonist, Pharmaceutical Science, Biochemistry, Combinatorial chemistry, chemistry.chemical_compound, Orally active, Leukotriene D4 receptor, chemistry, Drug Discovery, Molecular Medicine, Pharmacophore, Molecular Biology

Abstract

Replacement of the quinoline pharmacophore of verlukast by alkylthiazoles and benzothiazoles has lead to the discovery of a new series of potent and orally active LTD4 receptor antagonists. The synthesis and structure activity relationships of this series of compounds are described.

Published

1995

19. Molecular Cloning and Characterization of the Human Prostanoid DP Receptor

Author

Deborah Slipetz, Mark Abramovitz, Nicole Sawyer, Kathleen M. Metters, and Yves Boie

Subjects

Molecular Sequence Data, Receptors, Prostaglandin, Molecular cloning, Biology, Biochemistry, Complementary DNA, Cyclic AMP, Humans, 5-HT5A receptor, Amino Acid Sequence, Cloning, Molecular, Receptors, Immunologic, Receptor, Molecular Biology, Peptide sequence, Cells, Cultured, Base Sequence, Prostaglandin D2, Cell Biology, Blotting, Northern, Molecular biology, Prostaglandin analog, Interleukin-21 receptor, Calcium, lipids (amino acids, peptides, and proteins), Signal transduction

Abstract

A cDNA encoding a functional human prostanoid DP (hDP) receptor has been constructed from a genomic clone and a fragment cloned by 3′-rapid amplification of cDNA ends-polymerase chain reaction. The hDP receptor consists of 359 amino acid residues with a predicted molecular mass of 40,276 and has the putative heptahelical transmembrane domains characteristic of G-protein-coupled receptors. The deduced amino acid sequence of the hDP receptor, when compared with all other members of the prostanoid receptor family, shows the highest degree of identity with the hIP and hEP2 receptors, followed by the hEP4 receptor. Radioreceptor binding studies using membranes prepared from mammalian COS-M6 cells transiently transfected with an expression vector containing the DP receptor cDNA showed that the rank order of affinities for prostaglandins and prostaglandin analogs, in competition for [3H]prostaglandin D2 (PGD2) specific binding sites, was as predicted for the DP receptor, with PGD2 PGE2 > PGF2ɑ = iloprost > U46619. The signal transduction pathway of the cloned hDP receptor was studied by transfecting the hDP expression vector into HEK 293(EBNA) cells. Activation of the hDP receptor with PGD2 resulted in an elevation of intracellular cAMP and in mobilization of Ca2+, but did not lead to generation of inositol 1,4,5-trisphosphate. Northern blot analysis of human tissues showed that the hDP receptor has a very discrete tissue distribution and was detectable only in retina and small intestine. In summary, we have cloned and expressed a functional cDNA for the hDP receptor.

Published

1995

20. Discovery of MK-0476, a potent and orally active leukotriene D4 receptor antagonist devoid of peroxisomal enxyme induction

Author

C.B. Pickett, Thomas R. Jones, Marc Labelle, M. Belley, Robert N. Young, D.H. Patrick, Robert Zamboni, Nicole Sawyer, Anthony W. Ford-Hutchinson, Y. B. Xiang, S. G. Grossman, Nathalie Ouimet, R. Gordon, Yves Leblanc, Jacques-Yves Gauthier, C. S. Mcfarlane, H. Piechuta, Kathleen M. Metters, Daniel Guay, P. Masson, C. Rochette, M. McAuliffe, and Yves Gareau

Subjects

Leukotriene D4, biology, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Pharmacology, Peroxisome, Biochemistry, In vitro, chemistry.chemical_compound, chemistry, In vivo, Drug Discovery, biology.protein, Molecular Medicine, Potency, Inducer, Enzyme inducer, Molecular Biology

Abstract

Structure-activity studies leading to the discovery of 1 (MK-0476) are described. The initial compound of this series, 2, was a potent leukotriene D4 (LTD4) antagonist, but was also a peroxisomal enzyme inducer in the mouse. Structure-activity relationships around the thioether chain were explored to remove this undesirable feature. It was found that alkyl substituents in the s position relative to the carboxylic acid reduce the potency as a peroxisomal enzyme inducer while preserving the LTD4 antagonistic properties. Dialkyl substitution essentially eliminates the enzyme induction. The optimal styryl quinoline 1 exhibited high in vitro potency and in vivo activity on oral dosing without significant liver enzyme induction in the mouse.

Published

1995

21. Microsomal glutathione S-transferase is the predominant leukotriene C4 binding site in cellular membranes

Author

Kathleen M. Metters, Nicole Sawyer, and Donald W. Nicholson

Subjects

biology, GTP', Leukotriene C4, Leukotriene B4 receptor, Cell Biology, Glutathione, respiratory system, Biochemistry, Molecular biology, chemistry.chemical_compound, Glutathione S-transferase, Membrane, chemistry, biology.protein, lipids (amino acids, peptides, and proteins), Binding site, Receptor, Molecular Biology

Abstract

Dimethyl sulfoxide-differentiated U937 (dU937) cells express high affinity G-protein-coupled receptors for leukotriene (LT)D4 and LTB4 and, as described here, specific binding sites for LTC4. The specific binding of [3H]LTC4 was of low affinity (KD = 26 nM) and high abundance (Bmax = 33 pmol/mg of protein), as compared to LTD4 and LTB4 receptors. In addition, although [3H]LTC4 specific binding was enhanced by divalent cations, it was not inhibited by nonhydrolyzable GTP analogs. [3H]LTC4 specific binding to dU937 cell membranes does not have, therefore, the characteristics of binding to a G-protein-coupled receptor. Competition for [3H]LTC4 specific binding to dU937 cell membranes by leukotrienes and related analogs, including N-methylated LTC4, as well as glutathione, suggested a dependence on the presence of an arachidonic acid backbone, although varying degrees of saturation were well tolerated, and that the glutathione moiety of LTC4 in particular was important in determining affinity. The possibility that [3H]LTC4 specific binding was to a member of the glutathione S-transferase (GST) family of enzymes, such as LTC4 synthase, cytosolic GST, or microsomal GST, was therefore investigated. [3H]LTC4 specific binding sites could be separated from LTC4 synthase and cytosolic GSTs by differential detergent solubilization, but cofractionated with microsomal GST during solubilization and subsequent anion exchange chromatography. In membranes that were depleted of LTC4 synthase and cytosolic GSTs, 125I-azido-LTC4 (a photoaffinity probe based on LTC4) specifically photolabeled in a cation-dependent manner a 17-kDa polypeptide that was comparable in mass to the microsomal GST polypeptide. Furthermore, [3H]LTC4 bound specifically to purified human microsomal GST with the same characteristics as to the endogenous dU937-cell membrane specific binding sites. The principal [3H]LTC4 specific binding site present in dU937 cells, therefore, is not a G-protein-coupled receptor, LTC4 synthase, or cytosolic GSTs, but is microsomal GST. Finally, the 1:3 stoichiometry of [3H]LTC4 specific binding to purified microsomal GST is consistent with the enzyme functioning as a homotrimer.

Published

1994

22. The discovery of L-699,392, a novel potent and orally active leukotriene D4 receptor antagonist

Author

Robert Zamboni, Deborah A. Nicoll-Griffith, Thomas R. Jones, P. Masson, M. Belley, H. Piechuta, J. Yergey, Robert N. Young, Kathleen M. Metters, A. Lord, R. Gordon, C. Rochette, Karst Hoogsteen, Y. B. Xiang, M. McAuliffe, Anthony W. Ford-Hutchinson, Nicole Sawyer, C. S. Mcfarlane, Marc Labelle, E. Champion, Nathalie Ouimet, Yves Leblanc, and C.B. Pickett

Subjects

Leukotriene, Leukotriene D4, Organic Chemistry, Clinical Biochemistry, Quinoline, Antagonist, Pharmaceutical Science, Pharmacology, Biochemistry, chemistry.chemical_compound, Leukotriene D4 receptor, Orally active, Thioether, chemistry, Oral administration, Drug Discovery, Molecular Medicine, Molecular Biology

Abstract

The styryl quinoline thioether 5 (L-699,392) is a potent and orally active leukotriene D4 antagonist. The structure-activity studies leading to its discovery are described.

Published

1994

23. Cloning and expression of three isoforms of the human EP3prostanoid receptor

Author

Thomas H. Rushmore, Yves Boie, Mark Abramovitz, Mohamed Adam, Gretchen Müller, Katherine T. McKee, Kathleen M. Metters, and Lison Bastien

Subjects

Agonist, Gene isoform, medicine.drug_class, Prostaglandin E2, Molecular Sequence Data, Biophysics, Gene Expression, Biology, Transfection, Polymerase Chain Reaction, Biochemistry, Cell Line, Mice, Structural Biology, Genetics, medicine, Animals, Humans, Receptors, Prostaglandin E, Amino Acid Sequence, Cloning, Molecular, Receptor, Molecular Biology, Peptide sequence, chemistry.chemical_classification, Prostanoid receptor, COS cells, Base Sequence, Sequence Homology, Amino Acid, cDNA library, Cell Biology, Ligand (biochemistry), Rats, Amino acid, Molecular Weight, chemistry, EP3 cDNA, Receptor binding, Cattle, lipids (amino acids, peptides, and proteins), DNA Probes

Abstract

Functional cDNA clones coding for three isoforms of the human prostaglandin E receptor EP3 subtype have been isolated from kidney and uterus cDNA libraries. The three isoforms, designated hEP3-I, hEP3-II and hEP3-III, have open reading frames corresponding to 390, 388 and 365 amino acids, respectively. They differ only in the length and amino acid composition of their carboxy-terminal regions, beginning at position 360. The human EP3 receptor has seven predicted transmembrane spanning domains and therefore belongs to the G-protein-coupled receptor family. The rank order of potency for prostaglandins and related analogs in competition for [3H]PGE2 specific binding to membranes prepared from transfected COS cells was comparable for all three isoforms, and as predicted for the EP3 receptor, with PGE2 = PGE1 >> PGF2 alpha = iloprost > PGD2 >> U46619. In addition, the EP3-selective agonist MB28767 was a potent competing ligand with an IC50 value of 0.3 nM, whereas the EP1-selective antagonist AH6909 gave IC50 values of 2-7 microM and the EP2-selective agonist butaprost was inactive. In summary, we have cloned three isoforms of the human EP3 receptor having comparable ligand binding properties.

Published

1994

24. Cloning and expression of a cDNA for the human prostanoid FP receptor

Author

M.A. Bayne, Deborah Slipetz, Yves Boie, Kathleen M. Metters, Mark Abramovitz, Ryszard Grygorczyk, Thomas H. Rushmore, and Truyen Nguyen

Subjects

cDNA library, Prostaglandin, Cell Biology, Biology, Biochemistry, Molecular biology, chemistry.chemical_compound, Prostaglandin analog, chemistry, Cell surface receptor, Complementary DNA, Enzyme-linked receptor, lipids (amino acids, peptides, and proteins), Receptor, Molecular Biology, Prostacyclin receptor

Abstract

A cDNA clone coding for a functional human prostanoid FP receptor has been isolated from a uterus cDNA library. The human FP receptor consists of 359 amino acid residues with a predicted molecular mass of 40,060, and has the seven putative transmembrane domains characteristic of G-protein-coupled receptors. Challenge of Xenopus oocytes expressing the FP receptor with 10 nM of either prostaglandin (PG) F2 alpha or the selective FP-receptor agonist fluprostenol resulted in an elevation in intracellular Ca2+. Radioreceptor binding studies using membranes prepared from mammalian COS cells transfected with the FP receptor cDNA showed that the rank order of potency for prostaglandins and prostaglandin analogs in competition for [3H]PGF2 alpha specific binding sites was as predicted for the FP receptor, with PGF2 alpha approximately fluprostenol > PGD2 > PGE2 > U46619 > iloprost. In summary, we have cloned the human prostanoid FP receptor which is functionally coupled to the Ca2+ signalling pathway.

Published

1994

25. Identification and target-size analysis of the leukotriene D4 receptor in the human THP-1 cell line

Author

Kathleen M. Metters, Donald W. Nicholson, and C. Rochette

Subjects

Leukotrienes, Leukotriene D4, G protein, Cell Line, Cell membrane, chemistry.chemical_compound, medicine, Humans, THP1 cell line, Receptors, Immunologic, Binding site, Receptor, Molecular Biology, Receptors, Leukotriene, Leukotriene, Cell Membrane, Cell Biology, Tunicamycin, Molecular Weight, medicine.anatomical_structure, Biochemistry, chemistry, Leukemia, Monocytic, Acute, Quinolines, Guanosine Triphosphate, Propionates

Abstract

The human acute monocytic leukemia cell line THP-1 has been identified, by radioligand binding, as expressing the leukotriene D 4 receptor at a high level (4000 binding sites per cell), without the need for further cell differentiation. [ 3 H]Leukotriene D 4 -specific binding to THP-1 cell membranes was of high affinity ( K D = 0.47 nM) and saturable, enhanced by divalent cations but inhibited by both monovalent cations and non-hydrolyzable GTP analogs. The cysteinyl leukotrienes competed for [ 3 H]leukotriene D 4 -specific binding with the following rank order of potency: leukotriene D 4 ⪢ leukotriene E 4 〉 leukotriene C 4 In addition, leukotriene D 4 -receptor antagonists from two structural classes, the quinolines MK-571 and L-697,008, and the indole ICI 204,219, displayed nanomolar potency in [ 3 H]leukotriene D 4 competition assays. These data show that [ 3 H]leukotriene D 4 -specific binding to THP-1 cell membranes fulfils the criteria for binding to a leukotriene D 4 receptor regulated through interaction with a G protein. Several novel features of the THP-1 leukotriene D 4 receptor were investigated. Culture of THP-1 cells in the presence of tunicamycin, an inhibitor of N -glycosylation, resulted in a 6-fold decrease in the number of detectable [ 3 H]leukotriene D 4 -specific binding sites. Target-size analysis by radiation inactivation estimated a molecular mass of 65 kDa for the [ 3 H]leukotriene D 4 specific binding site(s) present in THP-1 cell membranes. Together, these results suggest that the human THP-1 cell leukotriene D 4 receptor is a glycosylated protein with a molecular mass of approx. 65 kDa within the membrane environment.

Published

1993

26. A new series of potent LTD4 antagonists in the styrylquinoline class

Author

Kathleen M. Metters, Robert Zamboni, Jacques-Yves Gauthier, Daniel Guay, and Patrick Roy

Subjects

chemistry.chemical_compound, Class (set theory), Leukotriene D4, Series (mathematics), chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Molecular Biology, Biochemistry

Abstract

A structurally new series of potent leukotriene D4 antagonists has evolved from modification of L-695,499.

Published

1993

27. Photoaffinity labeling of the leukotriene D4 receptor in guinea pig lung

Author

Kathleen M. Metters and Robert Zamboni

Subjects

chemistry.chemical_classification, Leukotriene, Leukotriene D4, Photoaffinity labeling, GTP', Ligand binding assay, Cell Biology, respiratory system, Biochemistry, Divalent, Guinea pig, chemistry.chemical_compound, chemistry, lipids (amino acids, peptides, and proteins), Receptor, Molecular Biology

Abstract

The leukotriene (LT)D4 receptor has been defined as a G-protein-coupled receptor. In order to characterize this receptor, an iodinated, photoactivatable azido derivative of LTD4 (125I-azido-LTD4) has been synthesized for use as a photoaffinity probe. The characteristics of 125I-azido-LTD4 specific binding to guinea pig lung membranes were directly comparable to those of [3H]LTD4 specific binding to this tissue. 125I-Azido-LTD4 specific binding was saturable and of high affinity, enhanced by divalent cations and inhibited by sodium ions, but not potassium ions. 125I-Azido-LTD4 specific binding was also strongly inhibited by the nonhydrolyzable GTP analog, GTP gamma S, with ATP gamma S being 100-fold less potent, suggesting this inhibition was due to selective interaction with a G-protein. The cysteinyl leukotrienes competed for 125I-azido-LTD4 specific binding to guinea pig lung membranes with the following rank order of potency: LTD4 > LTE4 > LTC4, while the non-cysteinyl LTB4 was virtually inactive. Two structurally different LTD4 receptor antagonists, MK-571 and ICI 204,219, also competed for 125I-azido-LTD4 specific binding with nanomolar potency, whereas the leukotriene synthesis inhibitor, MK-886, was 10,000-fold less active. These data are in agreement with 125I-azido-LTD4 binding specifically to a G-protein-coupled LTD4 receptor. Photolysis of 125I-azido-LTD4 under equilibrium binding conditions resulted in the selective radiolabeling of a 45-kDa guinea pig lung membrane protein. The photolabeling of this 45-kDa protein was saturable, modulated by cations and inhibited by nucleotide analogs in an analogous way to 125I-azido-LTD4 specific binding. In addition, the photolabeling of this protein was inhibited in a concentration-dependent manner by all competing ligands, with the same rank order of potency and IC50 values as determined in the 125I-azido-LTD4 binding assay. It is proposed, therefore, that this novel 45-kDa protein is the guinea pig lung LTD4 receptor.

Published

1993

28. Characterization of the leukotriene D4 receptor in dimethylsulphoxide-differentiated U937 cells: comparison with the leukotriene D4 receptor in human lung and guinea-pig lung

Author

Elizabeth A. Frey, Kathleen M. Metters, and Donald W. Nicholson

Subjects

Male, Indoles, Leukotriene D4, Cations, Divalent, Guinea Pigs, Phenylcarbamates, Biology, Binding, Competitive, Monocytes, Tosyl Compounds, chemistry.chemical_compound, Tumor Cells, Cultured, medicine, Animals, Humans, Dimethyl Sulfoxide, Receptors, Immunologic, Binding site, Receptor, Lung, Receptors, Leukotriene, Pharmacology, Sulfonamides, Leukotriene E4, Leukotriene, Leukotriene C4, Monocyte, Cell Membrane, Cell Differentiation, Ligand (biochemistry), medicine.anatomical_structure, chemistry, Biochemistry, Quinolines, Leukotriene Antagonists, SRS-A, Propionates

Abstract

The leukotriene D4 receptor has been fully characterized by radioligand binding in membrane preparations from dimethyl sulphoxide-differentiated U937 cells, a human monocyte leukemia cell line, and, in parallel experiments, compared with leukotriene D4 receptor found in human lung and guinea-pig lung preparations. [3H]Leukotriene D4 specific binding in differentiated U937 cell membranes is of high affinity (KD = 0.35 nM), saturable (Bmax = 287 fmol/mg protein), with differentiation resulting in a 3–5-fold increase in the number of detectable binding sites. [3H]Leukotriene D4-specific binding in differentiated U937 cell membranes displays several features of G-protein-cupled receptors, being inhibited by GTP analogues and sodium ions, but increased by divalent cations. These characteristics are shared with [3H]leukotriene D4-specific binding in human and guinea-pig lung preparations. However, differences between these leukotriene D4 receptor types were observed. [3H]Leukotriene D4 equilibrium binding to differentiated U937 cell membranes could be dissociated to non-specific binding levels by 1000-fold excess of competing ligand, whereas binding to guinea-pig lung membranes was only partially dissociated under these conditions. In addition, differences in potency were demonstrated in competition studies with leukotriene E4 and leukotriene C4, although leukotriene D4 and the leukotriene D4-receptor antagonists MK-571 and ICI 204,219 were equipotent in competing for [3H]leukotriene D4-specific binding in all three membranes preparations. In conclusion, the leukotriene D4 receptor in differentiated U937 cell membranes resembles that in human lung, validating the use of this cell line as a suitable source of receptor in the development of potent specific antagonists.

Published

1993

29. Photoaffinity labelling and radiation inactivation of the leukotriene B4 receptor in human myeloid cells

Author

Deborah Slipetz, Kylie A. Scoggan, Kathleen M. Metters, and Donald W. Nicholson

Subjects

Male, GTP', Neutrophils, Photochemistry, Affinity label, Population, Receptors, Leukotriene B4, In Vitro Techniques, Radioligand Assay, Cations, Tumor Cells, Cultured, Humans, Receptors, Immunologic, Binding site, education, Receptor, Chromatography, High Pressure Liquid, Pharmacology, Gel electrophoresis, education.field_of_study, biology, Ligand binding assay, Cell Membrane, Leukotriene B4 receptor, Proteins, Affinity Labels, hemic and immune systems, Molecular biology, Molecular Weight, Biochemistry, Gamma Rays, Leukemia, Myeloid, biology.protein, lipids (amino acids, peptides, and proteins), Guanosine Triphosphate

Abstract

The leukotriene (LT) B4 receptor has been characterized in the human monocyte leukemia THP-1 cell line. Scatchard analysis of [3H]LTB4 specific binding to THP-1 cell membranes revealed a single population of high affinity (KD = 56 pM) and saturable (2000 receptors/cell) binding sites. [3H]LTB4 specific binding was enhanced by divalent cations, but inhibited by both monovalent cations and a non-hydrolysable GTP analogue. Treatment with GTP analogue resulted in a concentration-dependent reduction in the number of high affinity binding sites, accompanied by the appearance of an equal number of binding sites of lower affinity (KD = 1250 pM). In contrast, Scatchard analysis with human polymorphonuclear leukocyte (PMN) membranes consistently revealed two populations of LTB4 receptors (KD = 48 pM and 270 pM). Treatment with GTP analogue, however, converted all these detectable binding sites to the lower affinity state. These data suggest that the LTB4 receptor in both THP-1 cell and PMN membranes exists in interconverting affinity states modulated by G-protein coupling. The similarity between the LTB4 receptors present in these two cell types was also substantiated by target-size analysis by radiation inactivation, which estimated a comparable molecular mass of 56.5 kDa and 52.8 kDa for the THP-1 cell and PMN LTB4 receptors, respectively. Finally, the presence of a single LTB4 receptor in PMN was demonstrated by direct photolabelling. Irradiation of frozen [3H]LTB4 equilibrium binding assay incubations resulted in complete photolysis of [3H]LTB4. Subsequent resolution of the tritiated PMN proteins by sodium dodecyl sulphate (SDS)-polyacrylamide gel electrophoresis (PAGE) revealed one major radioactive peak migrating with an apparent molecular weight of 61,000. This peak was identified as the LTB4 receptor since radiolabelling could be completely inhibited by the presence of excess unlabelled LTB4 or the LTB4-receptor antagonist, L-662,328. Photolabelling was also partially inhibited by pretreatment with GTP analogue, consistent with G-protein uncoupling reagents reducing receptor affinity without complete inhibition. In summary, the LTB4 receptor identified in human myeloid cells is a G-protein coupled receptor with interconvertible high and low affinity states, having a molecular mass of 53-61 kDa.

Published

1993

30. Structure–activity relationship on the human EP3 prostanoid receptor by use of solid-support chemistry

Author

Marie-Claude Carrière, Yves Gareau, Nathalie Tremblay, Helene Juteau, Sonia Lamontagne, Danielle Denis, Marc Labelle, Kathleen M. Metters, and Nicole Sawyer

Subjects

Stereochemistry, Carboxylic acid, Clinical Biochemistry, Pharmaceutical Science, Ligands, Biochemistry, Chemical synthesis, Cinnamic acid, Structure-Activity Relationship, chemistry.chemical_compound, Suzuki reaction, Drug Discovery, Combinatorial Chemistry Techniques, Humans, Receptors, Prostaglandin E, Cinnamates, Structure–activity relationship, Molecular Biology, chemistry.chemical_classification, Molecular Structure, Ligand, Organic Chemistry, Combinatorial chemistry, chemistry, Benzyl bromide, Receptors, Prostaglandin E, EP3 Subtype, Molecular Medicine

Abstract

Potent and selective EP3 receptor ligands were found by making a library using solid-support chemistry. These compounds can be obtained by a Suzuki coupling reaction of a solid-supported benzyl bromide using various boronic acids. The yields obtained for this reaction were in the range of 24-95% of arylmethyl cinnamic acid 1 after cleavage from the Wang resin.

Published

2001

31. ChemInform Abstract: The Discovery of L-699,392, a Novel Potent and Orally Active Leukotriene D4 Receptor Antagonist

Author

Robert Zamboni, E. Champion, Karst Hoogsteen, Y. B. Xiang, M. Belley, M. McAuliffe, Nathalie Ouimet, R. Gordon, Kathleen M. Metters, Marc Labelle, P. Masson, C. Rochette, H. Piechuta, Anthony W. Ford-Hutchinson, A. Lord, C. S. Mcfarlane, Nicole Sawyer, Deborah A. Nicoll-Griffith, Yves Leblanc, C.B. Pickett, Thomas R. Jones, and J. Yergey

Subjects

Leukotriene D4 receptor, Orally active, Chemistry, Stereochemistry, Antagonist, General Medicine, Pharmacology

Published

2010

32. ChemInform Abstract: Discovery of L-740,515, a Potent Thienopyridine cysLT1 Receptor (LTD4 Receptor) Antagonist

Author

Yves Leblanc, Robert N. Young, Helene Perrier, Claude Dufresne, Cheuk K. Lau, C. S. Mcfarlane, Thomas R. Jones, Kathleen M. Metters, Robert Zamboni, C.B. Pickett, Marc Labelle, Anthony W. Ford-Hutchinson, Nicole Sawyer, Nathalie Ouimet, Deborah Slipetz, M. McAuliffe, Zhaoyin Wang, C. Rochette, Yves Gareau, Xiang Yi Bin, and M. Belley

Subjects

Thienopyridine, Stereochemistry, Quinoline, Antagonist, General Medicine, Ring (chemistry), In vitro, chemistry.chemical_compound, chemistry, In vivo, medicine, Receptor, Montelukast, medicine.drug

Abstract

Structure-activity studies leading to the discovery of a new series of non-quinoline cysLT 1 receptor (LTD 4 receptor) antagonists are described. These studies demonstrated that the quinoline ring system of montelukast ( 5 ) may be replaced by an appropriately substituted thienopyridine system, yielding potent compounds. Two other molecular features of montelukast, the terminal phenyl ring substitution and the vinyl link, were also reevaluated. These studies led to the identification of 1 (L-740,515) , a compound with optimized in vitro and in vivo biological profiles.

Published

2010

33. ChemInform Abstract: New Class of Potent Ligands for the Human Peripheral Cannabinoid Receptor

Author

C. Rochette, Yves Gareau, Marc Labelle, Deborah Slipetz, Kathleen M. Metters, Nathalie Tremblay, Claude Dufresne, Michel Gallant, Yves Leblanc, P. Prasit, Daniel Guay, and Nicole Sawyer

Subjects

Indole test, Cannabinoid receptor, Chemistry, Stereochemistry, Ligand, medicine.medical_treatment, medicine, General Medicine, Cannabinoid, Receptor, Peripheral

Abstract

A new class of potent ligand for the human peripheral cannabinoid (hCB 2 ) receptor is described. Two indole analogs 13 and 17 exhibited nanomolar potencies (K i ) with good selectivity for the hCB 2 receptor over the human central cannabinoid (hCB 1 ) receptor.

Published

2010

34. The discovery of a new structural class of potent orally active leukotriene D4 antagonists

Author

M. Belley, Eugene G. Herold, Marc Labelle, Kathleen M. Metters, E. Grimm, Helene Perrier, Y. B. Xiang, Robert N. Young, D.H. Patrick, Patrick Roy, Lau Cheuk-Kun, John G. DeLuca, Anthony W. Ford-Hutchinson, Daniel Guay, L. Charette, E. Champion, P. Masson, H. Piechuta, A. Lord, Serge Leger, Thomas R. Jones, Jacques-Yves Gauthier, Petpiboon Prasit, Robert Zamboni, Nathalie Ouimet, Yves Leblanc, Claude Dufresne, C.B. Pickett, Zhaoyin Wang, Scott J. Grossman, Richard Frenette, C. S. Mcfarlane, M. McAuliffe, Haydn W. R. Williams, and Marc Blouin

Subjects

Leukotriene D4, medicine.drug_class, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Receptor antagonist, Biochemistry, chemistry.chemical_compound, Orally active, chemistry, Leukotriene D, Drug Discovery, medicine, Molecular Medicine, Molecular Biology, Structural class

Abstract

A new, potent, orally active leukotriene D 4 receptor antagonist has been discovered. The structure -activity relationship leading to L-695,499 is described.

Published

1992

35. Characterization of the leukotriene D4 receptor in hyperreactive rat lung

Author

Kathleen M. Metters, Anthony W. Ford-Hutchinson, and Elizabeth A. Frey

Subjects

Male, medicine.medical_specialty, Indazoles, Leukotriene D4, Guanine, In Vitro Techniques, Biology, Divalent, Radioligand Assay, chemistry.chemical_compound, Internal medicine, Hypersensitivity, medicine, Animals, Potency, Nucleotide, Receptors, Immunologic, Lung, Chromatography, High Pressure Liquid, Receptors, Leukotriene, Pharmacology, chemistry.chemical_classification, Ligand binding assay, Proteins, respiratory system, Molecular biology, In vitro, Rats, Kinetics, Endocrinology, medicine.anatomical_structure, chemistry, Quinolines, SRS-A, Propionates

Abstract

A [3H]leukotriene D4 radioreceptor binding assay has been established in rat lung and has been used to fully characterize the leukotriene D4 receptor in lung membranes from an inbred strain of rats displaying non-specific bronchial hyperreactivity. [3H]leukotriene D4 specific binding in this tissue is of high affinity (KD 0.12 nM), saturable (Bmax 42 fmol/mg protein), inhibited by both guanine nucleotide analogues and sodium ions and increased by divalent cations. In addition, Ki values show that agonists, but not antagonists, compete for [3H]leukotriene D4 binding in rat lung with the same potency as they compete for [3H]leukotriene D4 binding in guinea-pig lung, the classical tissue for leukotriene D4 receptor studies. Finally, [3H]leukotriene D4 binding in hyperreactive rat lung has been compared with [3H]leukotrien D4 binding in lung tissue from Fischer rats, which are a less responsive strain.

Published

1991

36. Immunolocalization of cyclooxygenase-2 in the macula densa of human elderly

Author

Kathleen M. Metters, Emily Meadows, Brett Connolly, Adel Giaid, Danielle Denis, and François Nantel

Subjects

Adult, Male, medicine.medical_specialty, Macula densa, Adolescent, Medullary cavity, Renal cortex, Biophysics, Biology, Kidney, Immunofluorescence, Biochemistry, Immunohistology, Age groups, Reference Values, Structural Biology, Internal medicine, Genetics, medicine, Humans, Kidney Tubules, Distal, Molecular Biology, Aged, Aged, 80 and over, Staining and Labeling, medicine.diagnostic_test, urogenital system, Membrane Proteins, Cell Biology, Middle Aged, Cyclooxygenase, Isoenzymes, Endocrinology, medicine.anatomical_structure, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Cyclooxygenase 1, biology.protein, Immunohistochemistry, Female, Human

Abstract

To gain insight into the role of prostanoids in human kidney function, we examined the distribution of cyclooxygenase (COX) 1 and COX-2 by immunofluorescence and immunohistochemistry in human kidneys from adults of various age groups. COX-1 was detected in the collecting ducts, thin loops of Henle and portions of the renal vasculature. COX-2 was detected in the renal vasculature, medullary interstitial cells, and the macula densa. In addition, COX-2 immunoreactivity was noted in afferent arteries and the macula densa of the renal cortex and was more evident in the kidneys of older adults.

Published

1999

37. Pharmacokinetics, pharmacodynamics, and safety of a prostaglandin D2 receptor antagonist

Author

D Hilliard, I De Lepeleire, J. N. de Hoon, KG Gottesdiener, Fang Liu, A. Van Hecken, Marleen Depré, JA Wagner, Larissa Wenning, E Lai, Gary P. O'Neill, Howard E. Greenberg, Kathleen M. Metters, and TM Crumley

Subjects

Adult, Male, medicine.medical_specialty, Indoles, Thromboxane, Receptors, Prostaglandin, Prostaglandin, Pharmacology, chemistry.chemical_compound, Pharmacokinetics, Double-Blind Method, Oral administration, Internal medicine, Medicine, Humans, Pharmacology (medical), Receptors, Immunologic, Prostaglandin D2 receptor, Dose-Response Relationship, Drug, business.industry, Antagonist, Headache, Middle Aged, Endocrinology, chemistry, Pharmacodynamics, business, Laropiprant

Abstract

Laropiprant is a selective antagonist of the prostaglandin D(2) (PGD(2)) receptor subtype 1 (DP1). Three double-blind, randomized, placebo-controlled studies evaluated the safety, tolerability, pharmacokinetics, and pharmacodynamics of single and multiple oral doses of laropiprant in healthy male volunteers. Single doses up to 900 mg and multiple doses up to 450 mg were generally well tolerated. Laropiprant exhibited dose-proportional pharmacokinetics. Oral absorption is rapid (T(max)=0.8-2.0 h) and the terminal half-life is approximately 12-18 h. The pharmacokinetics of laropiprant was not affected by food. Single doses of 6 mg and higher were effective in suppressing PGD(2)-induced cyclic AMP accumulation in platelets, demonstrating laropiprant target engagement with DP1. Laropiprant has detectable off-target antagonist effects at the thromboxane A(2) receptor but no clinically significant effect on collagen-induced platelet aggregation or bleeding times with multiple doses up to 200 mg.

Published

2007

38. Discovery of a potent and selective prostaglandin D2 receptor antagonist, [(3R)-4-(4-chloro-benzyl)-7-fluoro-5-(methylsulfonyl)-1,2,3,4-tetrahydrocyclopenta[b]indol-3-yl]-acetic acid (MK-0524)

Author

Laird A. Trimble, Kevin P. Bateman, Michael Boyd, Yves Aubin, Nicolas Lachance, Carl Berthelette, Jose H. Silva, Sonia Lamontagne, Deborah A. Nicoll-Griffith, Marc Labelle, Bruno Roy, Stephen H. Day, John Scheigetz, Thomas T. Jones, Nathalie Chauret, Robert Zamboni, Young Robert N, Jean François Lévesque, Gillian Greig, Hana Piechuta, Marie Claude Mathieu, Nicole Sawyer, Gary O'Neill, Carmai Seto, Lianhai Li, Zhaoyin Wang, Deborah A. Slipetz, Claudio F. Sturino, D Denis, Marie Claude Carriere, Stacia Kargman, Kathleen M. Metters, Malia McAuliffe, Nancy Tsou, and William M. Abraham

Subjects

Male, Indoles, Stereochemistry, Receptors, Prostaglandin, Cmax, In Vitro Techniques, Chemical synthesis, Binding, Competitive, Sulfone, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Dogs, Pharmacokinetics, In vivo, Microsomes, Drug Discovery, Animals, Bile, Humans, Receptors, Immunologic, Prostaglandin D2 receptor, Sheep, Chemistry, Antagonist, Stereoisomerism, Rats, Airway Obstruction, Macaca fascicularis, Nasal Decongestants, Hepatocytes, Molecular Medicine, Prostaglandin D2, Protein Binding

Abstract

The discovery of the potent and selective prostaglandin D2 (PGD2) receptor (DP) antagonist [(3R)-4-(4-chlorobenzyl)-7-fluoro-5-(methylsulfonyl)-1,2,3,4-tetrahydrocyclopenta[b]indol-3-yl]-acetic acid (13) is presented. Initial lead antagonists 6 and 7 were found to be potent and selective DP antagonists (DP Ki = 2.0 nM for each); however, they both suffered from poor pharmacokinetic profiles, short half-lives and high clearance rates in rats. Rat bile duct cannulation studies revealed that high concentrations of parent drug were present in the biliary fluid (Cmax = 1100 microM for 6 and 3900 microM for 7). This pharmacokinetic liability was circumvented by replacing the 7-methylsulfone substituent present in 6 and 7 with a fluorine atom resulting in antagonists with diminished propensity for biliary excretion and with superior pharmacokinetic profiles. Further optimization led to the discovery of the potent and selective DP antagonist 13.

Published

2007

39. Comparison between two classes of selective EP(3) antagonists and their biological activities

Author

Kathleen M. Metters, Deborah Slipetz, Nicolas Lachance, Marc Labelle, Danielle Denis, Chi-Chung Chan, Michel Gallant, Robert Zamboni, Sonia Lamontagne, Gillian Greig, Yves Gareau, Nicole Sawyer, Nathalie Tremblay, Helene Juteau, Karine Houde, Chun Li, Marie-Claude Carrière, Nathalie Chauret, Robert Gordon, and Michel Belley

Subjects

Prostaglandin E receptor 3, Sulfonamides, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Anti inflammation, Biochemistry, Cinnamates, Drug Discovery, Benzene derivatives, Molecular Medicine, Humans, Receptors, Prostaglandin E, Molecular Biology

Abstract

Two different series of very potent and selective EP(3) antagonists have been reported: a novel series of ortho-substituted cinnamic acids [Belley, M., Gallant, M., Roy, B., Houde, K., Lachance, N., Labelle, M., Trimble, L., Chauret, N., Li, C., Sawyer, N., Tremblay, N., Lamontagne, S., Carriere, M.-C., Denis, D., Greig, G. M., Slipetz, D., Metters, K. M., Gordon, R., Chan, C. C., Zamboni, R. J. Bioorg. Med. Chem. Lett.2005, 15, 527] and the acylsulfonamides of ortho-(arylmethyl)cinnamates. [(a) Juteau, H., Gareau, Y., Labelle, M., Sturino, C. F., Sawyer, N., Tremblay, N., Lamontagne, S., Carriere, M.-C., Denis, D., Metters, K. M. Bioorg. Med. Chem. 2001, 9, 1977; (b) Juteau, H., Gareau, Y., Labelle, M., Lamontagne, S., Tremblay, N., Carriere, M.-C., Denis, D., Sawyer, N., Metters, K. M. Bioorg. Med. Chem. Lett.2001, 11, 747] The structural differences between the two series, along with their biological activity in vivo, in vitro, and metabolism, are analyzed. Some of those compounds, including hybrids containing the best structural features of both series, possess K(i) as low as 0.6 nM on the EP(3) receptor.

Published

2006

40. Structure-activity relationship studies on ortho-substituted cinnamic acids, a new class of selective EP(3) antagonists

Author

Chun Li, Nicolas Lachance, Gillian Greig, Michel Gallant, Chi-Chung Chan, Sonia Lamontagne, Nicole Sawyer, Danielle Denis, Deborah Slipetz, Laird A. Trimble, Marc Labelle, Marie-Claude Carrière, R. Gordon, Michel Belley, Kathleen M. Metters, Nathalie Chauret, Bruno Roy, Robert Zamboni, Karine Houde, and Nathalie Tremblay

Subjects

Agonist, medicine.drug_class, Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Cell Line, Structure-Activity Relationship, In vivo, Drug Discovery, medicine, Cyclic AMP, Structure–activity relationship, Humans, Receptors, Prostaglandin E, Pharmacokinetics, Receptor, Molecular Biology, Chemistry, Organic Chemistry, Receptors, Prostaglandin E, EP2 Subtype, In vitro, Cinnamates, Receptors, Prostaglandin E, EP3 Subtype, Molecular Medicine, Selectivity, Prostaglandin E, Protein Binding

Abstract

A series of novel ortho -substituted cinnamic acids have been synthesized, and their binding activity and selectivity on the four prostaglandin E 2 receptors evaluated. Many of them are very potent and selective EP 3 antagonists ( K i 3–10 nM), while compound 9 is a very good and selective EP 2 agonist ( K i 8 nM). The biological profile of the EP 2 agonist 9 in vivo and the metabolic profile of selected EP 3 antagonists are also reported.

Published

2004

41. Structure-activity relationship of triaryl propionic acid analogues on the human EP3 prostanoid receptor

Author

Kathleen M. Metters, Deborah Slipetz, Danielle Denis, Jean François Truchon, Michel Gallant, Nicolas Lachance, Michel Belley, Anne Chateauneuf, Marie-Claude Carrière, Marc Labelle, Nicole Sawyer, and Sonia Lamontagne

Subjects

Stereochemistry, Protein Conformation, Carboxylic acid, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Cyclic AMP, Structure–activity relationship, Moiety, Animals, Humans, Receptors, Prostaglandin E, Receptor, Molecular Biology, chemistry.chemical_classification, Chemistry, Ligand, Organic Chemistry, Prostanoid, In vitro, Rats, Kinetics, Receptors, Prostaglandin E, EP3 Subtype, Molecular Medicine, lipids (amino acids, peptides, and proteins), Indicators and Reagents

Abstract

Potent and selective ligands for the human EP3 prostanoid receptor are described. Triaryl compounds bearing an ortho-substituted propionic acid moiety were identified as potent EP3 antagonists based on the SAR described herein. The binding affinities of key compound on all eight human prostanoid receptors is reported.

Published

2003

42. Discovery of a Potent and Selective Agonist of the Prostaglandin EP4 Receptor

Author

Robert N. Young, Anne Chateauneuf, Kathleen M. Metters, Gillian Greig, Deborah Slipetz, Danielle Denis, Marie Claude Mathieu, Nathalie Chauret, and Xavier Billot

Subjects

Agonist, Stereochemistry, medicine.drug_class, medicine.medical_treatment, Clinical Biochemistry, EP4 Receptor, Pharmaceutical Science, Tetrazoles, Prostaglandin, Ring (chemistry), Biochemistry, Partial agonist, Dinoprostone, Cell Line, chemistry.chemical_compound, Drug Discovery, medicine, Inverse agonist, Humans, Receptors, Prostaglandin E, Potency, Prostaglandin E2, Receptor, Molecular Biology, Organic Chemistry, Cell Membrane, General Medicine, Pyrrolidinones, chemistry, Drug Design, Lactam, Molecular Medicine, Indicators and Reagents, Receptors, Prostaglandin E, EP4 Subtype, Endogenous agonist, medicine.drug, Prostaglandin E, Half-Life, Hormone

Abstract

Analogues of PGE(2) wherein the hydroxycyclopentanone ring has been replaced by a lactam have been prepared and evaluated as ligands for the EP(4) receptor. An optimized compound (19a) shows high potency and agonist efficacy at the EP(4) receptor and is highly selective over the other seven known prostaglandin receptors.

Published

2003

43. Molecular pharmacology of the human prostaglandin D2 receptor, CRTH2

Author

Nicole, Sawyer, Elizabeth, Cauchon, Anne, Chateauneuf, Rani P G, Cruz, Donald W, Nicholson, Kathleen M, Metters, Gary P, O'Neill, and Francois G, Gervais

Subjects

integumentary system, Gene Expression Regulation, Receptors, Prostaglandin, Papers, Humans, lipids (amino acids, peptides, and proteins), HL-60 Cells, RNA, Messenger, Receptors, Immunologic, Transfection, Binding, Competitive, Recombinant Proteins, Cell Line

Abstract

1. The recombinant human prostaglandin D(2) (PGD(2)) receptor, hCRTH2, has been expressed in HEK293(EBNA) and characterized with respect to radioligand binding and signal transduction properties. High and low affinity binding sites for PGD(2) were identified in the CRTH2 receptor population by saturation analysis with respective equilibrium dissociation constants (K(D)) of 2.5 and 109 nM. This revealed that the affinity of PGD(2) for CRTH2 is eight times less than its affinity for the DP receptor. 2. Equilibrium competition binding assays revealed that of the compounds tested, only PGD(2) and several related metabolites bound with high affinity to CRTH2 (K(i) values ranging from 2.4 to 34.0 nM) with the following rank order of potency: PGD(2)13,14-dihydro-15-keto PGD(2)15-deoxy-Delta(12,14)-PGJ(2)PGJ(2)Delta(12)-PGJ(2)15(S)-15 methyl-PGD(2). This is in sharp contrast with the rank order of potency obtained at DP : PGD(2)PGJ(2)Delta(12)-PGJ(2)15-deoxy-Delta(12,14)-PGJ(2)13,14-dihydro-15-keto-PGD(2). 3. Functional studies demonstrated that PGD(2) activation of recombinant CRTH2 results in decrease of intracellular cAMP in a pertussis toxin-sensitive manner. Therefore, we showed that CRTH2 can functionally couple to the G-protein G(alphai/o). PGD(2) and related metabolites were tested and their rank order of potency followed the results of the membrane binding assay. 4. By Northern blot analysis, we showed that, besides haemopoietic cells, CRTH2 is expressed in many other tissues such as brain, heart, thymus, spleen and various tissues of the digestive system. In addition, in situ hybridization studies revealed that CRTH2 mRNA is expressed in human eosinophils. Finally, radioligand binding studies demonstrated that two eosinophilic cell lines, butyric acid-differentiated HL-60 and AML 14.3D10, also endogenously express CRTH2.

Published

2002

44. Structure-activity relationship of biaryl acylsulfonamide analogues on the human EP(3) prostanoid receptor

Author

Marie-Claude Carrière, Helene Juteau, Deborah Slipetz, Kathleen M. Metters, Yves Gareau, Sonia Lamontagne, C. Rochette, Claude Godbout, Rejean Ruel, Nicolas Lachance, Nicole Sawyer, Nathalie Tremblay, Gillian Greig, D. Denis, Patrick Lacombe, Michel Gallant, Marc Labelle, and Anne Chateauneuf

Subjects

Prostaglandin E receptor 3, Sulfonamides, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Prostanoid, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Drug Discovery, Receptors, Prostaglandin E, EP3 Subtype, Molecular Medicine, Structure–activity relationship, Moiety, Humans, Receptors, Prostaglandin E, lipids (amino acids, peptides, and proteins), Receptor, Molecular Biology

Abstract

Potent and selective ligands for the human EP3 prostanoid receptor are described. Biaryl compounds bearing a tethered ortho substituted acidic moiety were identified as potent EP3 antagonists based on the SAR described herein. The binding affinity of key compounds on all eight human prostanoid receptors is reported.

Published

2002

45. Localization of phosphodiesterase-4 isoforms in the medulla and nodose ganglion of the squirrel monkey

Author

Douglas J. Pon, Eric S. Muise, Kathleen M. Metters, François Nantel, Annette Robichaud, Denis Normandin, Sonia Lamontagne, Louise Boulet, Pauline Luk, George S. Robertson, and Emily Meadows

Subjects

Gene isoform, Male, medicine.medical_specialty, Vomiting, Blotting, Western, Molecular Sequence Data, In situ hybridization, Substance P, Internal medicine, Reflex, medicine, Animals, Molecular Biology, Saimiri, Medulla, In Situ Hybridization, Medulla Oblongata, biology, Base Sequence, General Neuroscience, Area postrema, Squirrel monkey, Nodose Ganglion, RNA Probes, biology.organism_classification, Immunohistochemistry, Cyclic Nucleotide Phosphodiesterases, Type 4, Isoenzymes, Endocrinology, nervous system, Microscopy, Fluorescence, 3',5'-Cyclic-AMP Phosphodiesterases, Medulla oblongata, Locus coeruleus, Female, Neurology (clinical), Developmental Biology

Abstract

Pre-clinical and clinical studies are currently underway to evaluate the potential of phosphodiesterase-4 (PDE4) inhibitors for the treatment of chronic obstructive pulmonary disease and other inflammatory conditions of the airways. The most common side effect associated with this class of compounds is emesis. The squirrel monkey provides a model for evaluating the efficacy of PDE4 inhibitors and their emetic potential. The distribution of three PDE4 isoforms (A, C and D) has been investigated in the squirrel monkey medulla and nodose ganglion to determine which isoform(s) could be responsible for the emetic adverse effects. The distribution of PDE4 isoforms was delineated using immunohistochemistry with antibodies specific for PDE4A, PDE4C and PDE4D and by in situ hybridization with isoform-selective riboprobes. PDE4A was present in the medulla where expression was mostly restricted to glial cells and the vasculature. PDE4C was not detected in either the medulla or nodose ganglion. Finally, the PDE4D isoform was localized to neurons in the nodose ganglion and found through many structures of medulla including the area postrema, neurons of the nucleus tractus solitarius and locus coeruleus. These data are consistent with a role for PDE4D in the emetic response.

Published

2001

46. Altered Bronchodilation and Pulmonary Inflammation in Prostanoid EP2 Receptor Knockout Mice

Author

Simon Wong, Kathleen M. Metters, Gary P. O'Neill, Maria Cirino, Richard M. Breyer, P. Masson, François Nantel, Denis Normandin, and Danielle Denis

Subjects

Agonist, endocrine system, medicine.drug_class, Prostaglandin E2 receptor, Prostanoid, Stimulation, Pharmacology, Adenylyl cyclase, chemistry.chemical_compound, chemistry, Bronchodilation, medicine, lipids (amino acids, peptides, and proteins), Prostaglandin E2, Receptor, medicine.drug

Abstract

Small clinical studies of asthma [1–5] found that inhaled prostaglandin E2 (PGE2) induced bronchodilation and reduced the influx of inflammatory cells in the airways. PGE2 activates four receptors identified as EP1–4 [6,7]. The activation of two of those receptors, the EP2 and the EP4, leads to the stimulation of the adenylyl cyclase and increases intracellular cyclic AMP levels. Therefore, a specific EP2 or EP4 agonist could be considered as a potential treatment for asthma.

Published

2001

47. Cellular distribution of prostanoid EP receptors mRNA in the rat gastrointestinal tract

Author

François Nantel, Maria Cirino, Kathleen M. Metters, Danielle Denis, and Angela Northey

Subjects

Male, Physiology, medicine.medical_treatment, Prostaglandin, In situ hybridization, Biology, Biochemistry, RNA, Complementary, Rats, Sprague-Dawley, chemistry.chemical_compound, Intestine, Small, medicine, Animals, Receptors, Prostaglandin E, Intestine, Large, RNA, Messenger, Intestinal Mucosa, Receptor, In Situ Hybridization, Pharmacology, Gastrointestinal tract, Stomach, Muscle, Smooth, Cell Biology, Molecular biology, Small intestine, Rats, Gastric chief cell, medicine.anatomical_structure, chemistry, Immunology, Prostaglandin E

Abstract

The inhibition of PGE 2 synthesis resulting from sustained NSAIDs therapy has been linked to gastrointestinal irritations and ulceration. The multiple physiological effects of PGE 2 in the gut are mediated through the activation of four receptors termed EP 1–4 . The aim of the study was to determine the precise distribution of the four prostaglandin E 2 receptors in the rat stomach, small intestine, and colon. We used non-radioactive in situ hybridization techniques on paraffin-embedded tissue. Mucous cells of the stomach and goblet cells of the small intestine and colon were found to express mRNA for all four EP subtypes. A positive hybridization signal for EP 1 , EP 3 , and EP 4 was detected in the parietal cells of the stomach whereas the chief cells expressed low levels of EP 1 and EP 3 . The EP 1 and EP 3 receptor mRNA could also be detected in the muscularis mucosa, longitudinal muscle and enteric ganglias of the stomach and small intestine. However, close examination of the enteric ganglias indicated that most of the positive labeling was localized to the glial cells, although some neurons did express EP 3 . In conclusion, we have detailed the distribution of prostanoid EP receptors in the gut at the cellular level, giving new insights to the role of prostaglandins in gastrointestinal functions.

Published

2000

48. The utilization of recombinant prostanoid receptors to determine the affinities and selectivities of prostaglandins and related analogs

Author

Yves Boie, Claude Dufresne, Marc Labelle, Michel Gallant, Mohammed Adam, C. Rochette, Yves Gareau, Nathalie Tremblay, Nathalie Ouimet, Rejean Ruel, Mark Abramovitz, Helene Juteau, Marie-Claude Carrière, Kathleen M. Metters, Sonia Lamontagne, Michel Belley, Nicole Sawyer, Danielle Denis, and Claude Godbout

Subjects

HEK 293 cells, Cell Membrane, Receptors, Prostaglandin, Prostaglandin, Prostanoid, Cell Biology, Biology, Ligands, Binding, Competitive, Radioligand Assay, Recombinant Proteins, law.invention, Cell Line, chemistry.chemical_compound, Prostaglandin analog, chemistry, Biochemistry, law, Cell culture, Recombinant DNA, Prostaglandins, Humans, Receptor, Molecular Biology

Abstract

Stable cell lines that individually express the eight known human prostanoid receptors (EP(1), EP(2), EP(3), EP(4), DP, FP, IP and TP) have been established using human embryonic kidney (HEK) 293(EBNA) cells. These recombinant cell lines have been employed in radioligand binding assays to determine the equilibrium inhibitor constants of known prostanoid receptor ligands at these eight receptors. This has allowed, for the first time, an assessment of the affinity and selectivity of several novel compounds at the individual human prostanoid receptors. This information should facilitate interpretation of pharmacological studies that employ these ligands as tools to study human tissues and cell lines and should, therefore, result in a greater understanding of prostanoid receptor biology.

Published

2000

49. Characterization of the cloned guinea pig leukotriene B4 receptor: comparison to its human orthologue

Author

Rino Stocco, Takehiko Yokomizo, Takao Shimizu, Yves Boie, Gillian Greig, Deborah Slipetz, Mark Abramovitz, Kathleen M. Metters, Stacia Kargman, Gary P. O'Neill, and Nicole Sawyer

Subjects

Agonist, Leukotriene D4, DNA, Complementary, Leukotriene B4, medicine.drug_class, Xenopus, Guinea Pigs, Molecular Sequence Data, Melanophores, Receptors, Leukotriene B4, Biology, Transfection, Binding, Competitive, Cell Line, Guinea pig, chemistry.chemical_compound, Radioligand Assay, Aequorin, medicine, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Receptor, Pharmacology, Leukotriene, Base Sequence, Sequence Homology, Amino Acid, Leukotriene B4 receptor, HEK 293 cells, Cell Membrane, Sequence Analysis, DNA, chemistry, Biochemistry, Luminescent Measurements, Sequence Alignment

Abstract

A cDNA clone coding for the guinea pig leukotriene B4 (BLT) receptor has been isolated from a lung cDNA library. The guinea pig BLT receptor has an open reading frame corresponding to 348 amino acids and shares 73% and 70% identity with human and mouse BLT receptors, respectively. Scatchard analysis of membranes prepared from guinea pig and human BLT receptor-transfected human embryonic kidney (HEK) 293 EBNA (Epstein–Bar Virus Nuclear Antigen) cells showed that both receptors displayed high affinity for leukotriene B4 (Kd value of ∼0.4 nM) and were expressed at high levels (Bmax values ranging from 9 to 12 pmol/mg protein). The rank order of potency for leukotrienes and related analogs in competition for [ 3 H ]leukotriene B4 specific binding at the recombinant guinea pig BLT receptor is leukotriene B4>20-OH-leukotriene B4>12(R)-HETE ((5Z,8Z,10E,12(R)14Z)-12-hydroxyeicosatetraen-1-oic acid)>12(S)-HETE ((5Z,8Z,10E,12(S)14Z)-12-Hydroxyeicosatetraen-1-oic acid)>20-COOH-leukotriene B4>U75302 (6-(6-(3-hydroxy-1E,5Z-undecadienyl)-2-pyridinyl)-1,5-hexanediol)≫leukotriene C4=leukotriene D4=leukotriene E4. For the human receptor the rank order of 12(S)-HETE, 20-COOH-leukotriene B4 and U75302 was reversed. Xenopus melanophore and HEK aequorin-based reporter gene assays were used to demonstrate that the guinea pig and human BLT receptors can couple to both the cAMP inhibitory and intracellular Ca2+ mobilization signaling pathways. However, in the case of the aequorin-expressing HEK cells (designated AEQ17-293) transfected with either the guinea pig or human BLT receptor, expression of Gα16 was required to achieve a robust Ca2+ driven response. Leukotriene B4 was a potent agonist in functional assays of both the guinea pig and human BLT receptors. U-75302 a leukotriene B4 analogue which possesses both agonistic and antagonistic properties behaved as a full agonist of the guinea pig and human BLT receptors in AEQ17-293 cells and not as an antagonist. The recombinant guinea pig BLT receptor will permit the comparison of the intrinsic potencies of leukotriene B4 receptor antagonists used in guinea pig in vivo models of allergic and inflammatory disorders.

Published

1999

50. A novel biological role for prostaglandin D2 is suggested by distribution studies of the rat DP prostanoid receptor

Author

D. Hamish Wright, Anthony W. Ford-Hutchinson, Kathleen M. Metters, and François Nantel

Subjects

Agonist, medicine.medical_specialty, medicine.drug_class, Prostaglandin E2 receptor, Recombinant Fusion Proteins, Molecular Sequence Data, Receptors, Prostaglandin, Prostaglandin, Gene Expression, In situ hybridization, Biology, Binding, Competitive, Cell Line, chemistry.chemical_compound, Epitopes, Radioligand Assay, Internal medicine, medicine, Cyclic AMP, Animals, Humans, Tissue Distribution, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Receptors, Immunologic, Receptor, In Situ Hybridization, Prostaglandin D2 receptor, Pharmacology, Sequence Homology, Amino Acid, Prostaglandin D2, Cell Membrane, RNA Probes, Molecular biology, Rats, Endocrinology, chemistry, Peptides, Oligopeptides

Abstract

We report the cloning, functional expression and cell-specific localization of the rat homologue of the prostaglandin D2 receptor (DP). In situ hybridization, utilizing multiple digoxigenin-labelled riboprobes and their complementary sense controls, was performed to determine the detailed distribution of DP receptor mRNA in the central nervous system and the gastrointestinal tract. Within the brain, the leptomeninges and choroid plexus expressed DP receptor mRNA. Transcripts detected in the spinal cord were localized to the sensory and motor neurons of the dorsal and ventral horns, respectively, suggesting a role for the DP receptor in the modulation of central nervous system processes, including pain transmission. Within the gastrointestinal tract (stomach, duodenum, ileum and colon) signals were highly localized to the mucous-secreting goblet cells and the columnar epithelium. These findings suggest a novel biological role for prostaglandin D2-mediated activity at the DP receptor, namely mucous secretion. In addition, radioligand binding assays (saturation analyses and equilibrium competition assays) and functional assays (measuring cAMP accumulation) were performed to characterize the recombinant rat DP receptor expressed in human embryonic kidney (HEK) 293(EBNA) cells. A single site of binding (K(D) = 14 nM, Bmax = 115 fmol/mg protein) was measured for prostaglandin D2-specific binding to the rat DP receptor. Prostaglandin D2 proved to be a potent agonist at the rat DP receptor (EC50 = 5 nM). The rank order of efficacy for DP receptor specific agonists [prostaglandin D2 = prostaglandin J2 = BW 245C (5-(6-carboxyhexyl)-1-(3-cyclohexyl-3-hydroxypropylhydantoin)) > L-644,698 ((4-(3-(3-(3-hydroxyoctyl)-4-oxo-2-thiazolidinyl) propyl) benzoic acid) (racemate)] reflected the affinity with which the ligands bound to the receptor.

Published

1999