Your search keyword '"Peter Coward"' showing total 27 results

1. Effects of peroxisome proliferator-activated receptor α/δ agonists on HDL-cholesterol in vervet monkeys

Author

Jeanne M. Wallace, Margrit Schwarz, Peter Coward, Jonathan Houze, Janet K. Sawyer, Kathryn L. Kelley, Anne Chai, and Lawrence L. Rudel

Subjects

animal model, apolipoprotein A-I, apolipoprotein A-II, atherosclerosis, high density lipoprotein particle size, lipoprotein metabolism, Biochemistry, QD415-436

Abstract

The objective of this study was to demonstrate the efficacy of a novel peroxisome proliferator-activated receptor (PPAR) agonist and known PPARα and PPARδ agonists to increase HDL-cholesterol (HDL-C) in the St. Kitts vervet, a nonhuman primate model of atherosclerosis. Four groups (n = 6) were studied and each group was assigned one of the following “treatments”: a) vehicle only (vehicle); b) the PPARδ selective agonist GW501516 (GW); c) the PPARα/δ agonist T913659 (T659); and d) the PPARα agonist TriCor® (fenofibrate). No statistically significant changes were seen in body weight, total plasma cholesterol, plasma triglycerides, VLDL-C, LDL-C, or apolipoprotein B (apoB) concentrations. Each of the PPARα and PPARδ agonists investigated in this study increased plasma HDL-C, apoA-I, and apoA-II concentrations and increased HDL particle size in St. Kitts vervets. The maximum percentage increase in HDL-C from baseline for each group was as follows: vehicle, 5%; GW, 43%; T659, 43%; and fenofibrate, 20%. Treatment with GW and T659 resulted in an increase in medium-sized HDL particles, whereas fenofibrate showed increases in large HDL particles.These data provide additional evidence that PPARα and PPARδ agonists (both mixed and selective) have beneficial effects on HDL-C in these experimental primates.

Published

2005

2. Characterization of a novel glucokinase activator in rat and mouse models.

Author

Min Lu, Pingping Li, Gautam Bandyopadhyay, William Lagakos, Walter E Dewolf, Taylor Alford, Mark Joseph Chicarelli, Lance Williams, Deborah A Anderson, Brian R Baer, Maralee McVean, Marion Conn, Murielle M Véniant, and Peter Coward

Subjects

Medicine, Science

Abstract

Glucokinase (GK) is a hexokinase isozyme that catalyzes the phosphorylation of glucose to glucose-6-phosphate. Glucokinase activators are being investigated as potential diabetes therapies because of their effects on hepatic glucose output and/or insulin secretion. Here, we have examined the efficacy and mechanisms of action of a novel glucokinase activator, GKA23. In vitro, GKA23 increased the affinity of rat and mouse glucokinase for glucose, and increased glucose uptake in primary rat hepatocytes. In vivo, GKA23 treatment improved glucose homeostasis in rats by enhancing beta cell insulin secretion and suppressing hepatic glucose production. Sub-chronic GKA23 treatment of mice fed a high-fat diet resulted in improved glucose homeostasis and lipid profile.

Published

2014

3. Discovery and optimization of N-(3-(1,3-dioxo-2,3-dihydro-1H-pyrrolo[3,4-c]pyridin-4-yloxy)phenyl)benzenesulfonamides as novel GPR119 agonists

Author

Karen Siegler, Bei Shan, Mark P. Grillo, Marion Conn, Jiang Zhu, Jian Ken Zhang, Yingcai Wang, Julio C. Medina, Ming Yu, Peter Coward, Frank Kayser, and Jiwen Jim Liu

Subjects

Agonist, Sulfonamides, Dose-Response Relationship, Drug, Molecular Structure, Pyridines, medicine.drug_class, Stereochemistry, Chemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Rats, Receptors, G-Protein-Coupled, Structure-Activity Relationship, GPR119, Drug Discovery, Microsomes, Liver, medicine, Animals, Humans, Molecular Medicine, Molecule, Molecular Biology

Abstract

The discovery and optimization of novel N-(3-(1,3-dioxo-2,3-dihydro-1H-pyrrolo[3,4-c]pyridin-4-yloxy)phenyl)benzenesulfonamide GPR119 agonists is described. Modification of the pyridylphthalimide motif of the molecule with R(1)=-Me and R(2)=-(i)Pr substituents, incorporated with a 6-fluoro substitution on the central phenyl ring offered a potent and metabolically stable tool compound 22.

Published

2014

4. Discovery and optimization of a series of liver X receptor antagonists

Author

Anne Chai, Stuart Donald Jones, Andrew K. Shiau, Marc Labelle, Frank Kayser, Peter Coward, Juan C. Jaen, Xianyun Jiao, Ben Fisher, Martin James Harrison, Patrick Escaron, David J. Kopecky, Derek E. Piper, Sharon McKendry, and Jean Danao

Subjects

Male, Agonist, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Ligands, digestive system, Biochemistry, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, In vivo, Drug Discovery, polycyclic compounds, medicine, Animals, Humans, Liver X receptor, Molecular Biology, Liver X Receptors, Sulfonamides, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Organic Chemistry, Antagonist, food and beverages, Hep G2 Cells, Orphan Nuclear Receptors, Rats, HEK293 Cells, Molecular Medicine, lipids (amino acids, peptides, and proteins)

Abstract

The present report describes our efforts to convert an existing LXR agonist into an LXR antagonist using a structure-based approach. A series of benzenesulfonamides was synthesized based on structural modification of a known LXR agonist and was determined to be potent dual liver X receptor (LXR α/β) ligands. Herein we report the identification of compound 54 as the first reported LXR antagonist that is suitable for pharmacological in vivo evaluation in rodents.

Published

2012

5. Discovery of a new binding mode for a series of liver X receptor agonists

Author

Derek E. Piper, Frank Kayser, Marc Labelle, Peter Coward, Patrick Escaron, Sharon McKendry, Jean Danao, Ben Fisher, Anne Chai, Juan C. Jaen, David J. Kopecky, Xian Yun Jiao, and Andrew K. Shiau

Subjects

Agonist, medicine.drug_class, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Crystallography, X-Ray, Transfection, Biochemistry, Partial agonist, Structure-Activity Relationship, Genes, Reporter, Drug Discovery, medicine, Humans, Protein Isoforms, Pyrroles, Liver X receptor, Molecular Biology, Liver X Receptors, Binding Sites, Series (mathematics), Chemistry, Organic Chemistry, Orphan Nuclear Receptors, HEK293 Cells, Nuclear receptor, Molecular Medicine, Caco-2 Cells, Protein Binding

Abstract

Structural modification of a series of dual LXRα/β agonists led to the identification of a new class of LXRβ partial agonists. An X-ray co-crystal structure shows that a representative member of this series, pyrrole 5, binds to LXRβ with a reversed orientation compared to 1.

Published

2012

6. Identification and Characterization of a Non-retinoid Ligand for Retinol-binding Protein 4 Which Lowers Serum Retinol-binding Protein 4 Levels in Vivo

Author

Richard V. Connors, Steve Thibault, Zhulun Wang, Pingchen Fan, Alykhan Motani, Haoda Xu, Nigel Walker, Ying Zhang, Qingxiang Liu, Hoa Le, Guifen Xu, Karen Siegler, Bei Shan, Sheree Johnstone, Yingcai Wang, Peter Coward, and Marion Conn

Subjects

medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Crystallography, X-Ray, Ligands, Biochemistry, Mice, chemistry.chemical_compound, Insulin resistance, Piperidines, Internal medicine, Diabetes Mellitus, medicine, Animals, Humans, Insulin, Retinoid, Vitamin A, Molecular Biology, Mice, Knockout, Retinol binding protein 4, biology, Binding protein, Retinol, Cell Biology, medicine.disease, Dietary Fats, Protein Structure, Tertiary, Metabolism and Bioenergetics, Transthyretin, Retinol binding protein, Endocrinology, chemistry, biology.protein, Insulin Resistance, Heterocyclic Compounds, 3-Ring, Retinol-Binding Proteins, Plasma

Abstract

Retinol-binding protein 4 (RBP4) transports retinol from the liver to extrahepatic tissues, and RBP4 lowering is reported to improve insulin sensitivity in mice. We have identified A1120, a high affinity (Ki = 8.3 nm) non-retinoid ligand for RBP4, which disrupts the interaction between RBP4 and its binding partner transthyretin. Analysis of the RBP4-A1120 co-crystal structure reveals that A1120 induces critical conformational changes at the RBP4-transthyretin interface. Administration of A1120 to mice lowers serum RBP4 and retinol levels but, unexpectedly, does not improve insulin sensitivity. In addition, we show that Rpb4-/- mice display normal insulin sensitivity and are not protected from high fat diet-induced insulin resistance. We conclude that lowering RBP4 levels does not improve insulin sensitivity in mice. Therefore, RBP4 lowering may not be an effective strategy for treating diabetes.

Published

2009

7. Effects of peroxisome proliferator-activated receptor α/δ agonists on HDL-cholesterol in vervet monkeys

Author

Janet K. Sawyer, Kathryn L. Kelley, Jeanne M. Wallace, Lawrence L. Rudel, Anne Chai, Margrit Schwarz, Peter Coward, and Jonathan B. Houze

Subjects

Male, Agonist, medicine.medical_specialty, Apolipoprotein B, medicine.drug_class, Apolipoprotein A-II, apolipoprotein A-I, Peroxisome proliferator-activated receptor, QD415-436, Biochemistry, GW501516, chemistry.chemical_compound, apolipoprotein A-II, Endocrinology, Internal medicine, Chlorocebus aethiops, medicine, Animals, PPAR alpha, high density lipoprotein particle size, Particle Size, Receptor, lipoprotein metabolism, chemistry.chemical_classification, Fenofibrate, biology, Cholesterol, animal model, Cholesterol, HDL, nutritional and metabolic diseases, Cell Biology, medicine.disease, PPAR gamma, Thiazoles, chemistry, biology.protein, lipids (amino acids, peptides, and proteins), atherosclerosis, medicine.drug

Abstract

The objective of this study was to demonstrate the efficacy of a novel peroxisome proliferator-activated receptor (PPAR) agonist and known PPARalpha and PPARdelta agonists to increase HDL-cholesterol (HDL-C) in the St. Kitts vervet, a nonhuman primate model of atherosclerosis. Four groups (n = 6) were studied and each group was assigned one of the following "treatments": a) vehicle only (vehicle); b) the PPARdelta selective agonist GW501516 (GW); c) the PPARalpha/delta agonist T913659 (T659); and d) the PPARalpha agonist TriCor (fenofibrate). No statistically significant changes were seen in body weight, total plasma cholesterol, plasma triglycerides, VLDL-C, LDL-C, or apolipoprotein B (apoB) concentrations. Each of the PPARalpha and PPARdelta agonists investigated in this study increased plasma HDL-C, apoA-I, and apoA-II concentrations and increased HDL particle size in St. Kitts vervets. The maximum percentage increase in HDL-C from baseline for each group was as follows: vehicle, 5%; GW, 43%; T659, 43%; and fenofibrate, 20%. Treatment with GW and T659 resulted in an increase in medium-sized HDL particles, whereas fenofibrate showed increases in large HDL particles. These data provide additional evidence that PPARalpha and PPARdelta agonists (both mixed and selective) have beneficial effects on HDL-C in these experimental primates.

Published

2005

8. C5-Alkyl-2-methylurea-Substituted Pyridines as a New Class of Glucokinase Activators

Author

Vatee Pattaropong, Jaehyeon Park, Xianyun Jiao, Mark Joseph Chicarelli, Thanhvien Tran, Bencsik Josef Roland, Paul John Dransfield, Kevin Ronald Condroski, Sujen Lai, Julio C. Medina, Brian R. Baer, Boyd Steven A, Mohr Peter, Deborah A. Anderson, Jonathan B. Houze, Walter E. DeWolf, Yumei Xiong, Marion Conn, Zice Fu, Jasmine Davda, Lixia Jin, Xiaohui Du, Jerry Yang, Peter Coward, Bin Wang, Murielle M. Véniant, Ronald Jay Hinklin, Todd J. Kohn, David Chow, and Thomas Daniel Aicher

Subjects

chemistry.chemical_classification, Glucokinase, Organic Chemistry, Pharmacology, Metabolic stability, Biochemistry, In vitro, chemistry.chemical_compound, Enzyme, chemistry, Drug Discovery, Pyridine, Potency, Glucose homeostasis, Alkyl

Abstract

Glucokinase (GK) activators represent a class of type 2 diabetes therapeutics actively pursued due to the central role that GK plays in regulating glucose homeostasis. Herein we report a novel C5-alkyl-2-methylurea-substituted pyridine series of GK activators derived from our previously reported thiazolylamino pyridine series. Our efforts in optimizing potency, enzyme kinetic properties, and metabolic stability led to the identification of compound 26 (AM-9514). This analogue showed a favorable combination of in vitro potency, enzyme kinetic properties, acceptable pharmacokinetic profiles in preclinical species, and robust efficacy in a rodent PD model.

Published

2014

9. Structure-assisted discovery of the first non-retinoid ligands for Retinol-Binding Protein 4

Author

Zhulun Wang, Yingcai Wang, Marion Conn, Xiaodong Wang, Richard V. Connors, Qingxiang Liu, Jiwen Liu, Nigel Walker, Peter Coward, Frank Kayser, Stephen T. Thibault, Mark P. Grillo, Zhongyu Wang, Pingchen Fan, Julio C. Medina, Alykhan Motani, Haoda Xu, Sheree Johnstone, and Ying Zhang

Subjects

Male, Models, Molecular, Clinical Biochemistry, Pharmaceutical Science, Plasma protein binding, Crystallography, X-Ray, Ligands, Biochemistry, Small Molecule Libraries, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Vitamin A, Molecular Biology, Retinol binding protein 4, biology, Dose-Response Relationship, Drug, Molecular Structure, Binding protein, Organic Chemistry, Retinol, Transport protein, Rats, Transthyretin, Retinol binding protein, Fenretinide, chemistry, biology.protein, Molecular Medicine, Retinol-Binding Proteins, Plasma

Abstract

Retinol-Binding Protein 4 (RBP4) is a plasma protein that transports retinol (vitamin A) from the liver to peripheral tissues. This Letter highlights our efforts in discovering the first, to our knowledge, non-retinoid small molecules that bind to RBP4 at the retinol site and reduce serum RBP4 levels in mice, by disrupting the interaction between RBP4 and transthyretin (TTR), a plasma protein that binds RBP4 and protects it from renal excretion. Potent compounds were discovered and optimized quickly from high-throughput screen (HTS) hits utilizing a structure-based approach. Inhibitor co-crystal X-ray structures revealed unique disruptions of RBP4-TTR interactions by our compounds through induced loop conformational changes instead of steric hindrance exemplified by fenretinide. When administered to mice, A1120, a representative compound in the series, showed concentration-dependent retinol and RBP4 lowering.

Published

2014

10. 4-Hydroxytamoxifen binds to and deactivates the estrogen-related receptor γ

Author

Doris Lee, Mitchell V. Hull, Peter Coward, and Jürgen M. Lehmann

Subjects

Transcriptional Activation, genetic structures, Recombinant Fusion Proteins, Molecular Sequence Data, Estrogen receptor, Biology, Cell Line, Estrogen-related receptor, Chlorocebus aethiops, Animals, Estrogen Receptor beta, Humans, Amino Acid Sequence, Receptor, Diethylstilbestrol, Peptide sequence, Estrogen receptor beta, chemistry.chemical_classification, Multidisciplinary, Estrogen Antagonists, Estrogen Receptor alpha, Biological Sciences, eye diseases, Amino acid, Tamoxifen, Receptors, Estrogen, chemistry, Biochemistry, Trans-Activators, Estrogen-related receptor gamma, Estrogen receptor alpha

Abstract

The estrogen-related receptors (ERRα, ERRβ, and ERRγ) form a family of orphan nuclear receptors that share significant amino acid identity with the estrogen receptors, but for which physiologic roles remain largely unknown. By using a peptide sensor assay, we have identified the stilbenes diethylstilbestrol (DES), tamoxifen (TAM), and 4-hydroxytamoxifen (4-OHT) as high-affinity ligands for ERRγ. In direct binding assays, 4-OHT had a K d value of 35 nM, and both DES and TAM displaced radiolabeled 4-OHT with K i values of 870 nM. In cell-based assays, 4-OHT binding caused a dissociation of the complex between ERRγ and the steroid receptor coactivator-1, and led to an inhibition of the constitutive transcriptional activity of ERRγ. ERRα did not bind 4-OHT, but replacing a single amino acid predicted to be in the ERRα ligand-binding pocket with the corresponding ERRγ residue allowed high-affinity 4-OHT binding. These results demonstrate the existence of high-affinity ligands for the ERR family of orphan receptors, and identify 4-OHT as a molecule that can regulate the transcriptional activity of ERRγ.

Published

2001

11. Conditional expression of a G i -coupled receptor causes ventricular conduction delay and a lethal cardiomyopathy

Author

Daniel Bernstein, Nathalie Cotte, Charles H. Redfern, Michael Y. Degtyarev, Tania Nanevicz, Anthony J. Baker, Janet A. Warrington, Nicholas Fidelman, Kavin H. Desai, Glenn I. Fishman, Karen Vranizan, Bruce R. Conklin, Nila Shah, Peter Coward, Elena K. Lee, Andrew T. Kwa, and Nathan Salomonis

Subjects

medicine.medical_specialty, Cardiomyopathy, Mice, Transgenic, Disease, GTP-Binding Protein alpha Subunits, Gi-Go, Biology, Electrocardiography, Mice, Transactivation, Internal medicine, medicine, Animals, Ventricular Function, Virulence Factors, Bordetella, Receptor, Survival analysis, Doxycycline, Multidisciplinary, Myosin Heavy Chains, medicine.diagnostic_test, Myocardium, Receptors, Opioid, kappa, Tetracycline Resistance, Heart, Biological Sciences, medicine.disease, Survival Analysis, Endocrinology, Tachycardia, Ventricular, Signal transduction, Cardiomyopathies, Signal Transduction, medicine.drug

Abstract

Cardiomyopathy is a major cause of morbidity and mortality. Ventricular conduction delay, as shown by prolonged deflections in the electrocardiogram caused by delayed ventricular contraction (wide QRS complex), is a common feature of cardiomyopathy and is associated with a poor prognosis. Although the G i -signaling pathway is up-regulated in certain cardiomyopathies, previous studies suggested this up-regulation was compensatory rather than a potential cause of the disease. Using the tetracycline transactivator system and a modified G i -coupled receptor (Ro1), we provide evidence that increased G i signaling in mice can result in a lethal cardiomyopathy associated with a wide QRS complex arrhythmia. Induced expression of Ro1 in adult mice resulted in a >90% mortality rate at 16 wk, whereas suppression of Ro1 expression after 8 wk protected mice from further mortality and allowed partial improvement in systolic function. Results of DNA-array analysis of over 6,000 genes from hearts expressing Ro1 are consistent with hyperactive G i signaling. DNA-array analysis also identified known markers of cardiomyopathy and hundreds of previously unknown potential diagnostic markers and therapeutic targets for this syndrome. Our system allows cardiomyopathy to be induced and reversed in adult mice, providing an unprecedented opportunity to dissect the role of G i signaling in causing cardiac pathology.

Published

2000

12. Chimeric G Proteins Allow a High-Throughput Signaling Assay of Gi-Coupled Receptors

Author

Bruce R. Conklin, H. G. Wada, Peter Coward, S. D. H. Chan, and G. M. Humphries

Subjects

G protein, Recombinant Fusion Proteins, Molecular Sequence Data, Biophysics, CHO Cells, Biology, Transfection, Biochemistry, GTP-Binding Proteins, Cricetinae, Animals, Humans, Fluorometry, 5-HT5A receptor, Amino Acid Sequence, Receptor, Molecular Biology, DNA Primers, G protein-coupled receptor, G protein-coupled receptor kinase, Base Sequence, Cell Biology, RGS17, Nociceptin receptor, Opioid Peptides, Receptors, Opioid, Calcium, Signal transduction, Signal Transduction

Abstract

G-protein-coupled receptors are a major target for potential therapeutics; yet, a large number of these receptors couple to the Gi pathway, generating signals that are difficult to detect. We have combined chimeric G proteins, automated sample handling, and simultaneous 96-well fluorometric imaging to develop a high-throughput assay system for Gi signaling. The chimeric G proteins alter receptor coupling so that signaling can occur through Gq and result in mobilization of intracellular calcium stores. An automated signaling assay device, the fluorometric imaging plate reader (FLIPR), can simultaneously measure this response in real time in 96-well microplates, allowing two people to process more than 10,000 points per day. We used the chimeric G protein/FLIPR system to characterize signaling by the Gi-coupled human opioid receptors. We show that the mu, delta, and kappa opioid receptors and the related nociceptin receptor, ORL1, each couple to Galphaqi5, Galphaqo5, and Galpha16 (Galphaqi5 and Galphaqo5 refer to Galphaq proteins containing the five carboxyl-terminal amino acids from Galphai and Galphao, respectively) and that different receptor/G protein combinations show different levels of maximal activation. We tested 31 opioid ligands for agonist activity at the opioid receptors (124 ligand-receptor combinations); all 31 activated at least one receptor type, and several activated multiple receptors with differing potencies. This high-throughput assay could be useful for dissecting the complex ligand-receptor relationships that are common in nature.

Published

1999

13. Conditional expression and signaling of a specifically designed Gi-coupled receptor in transgenic mice

Author

Hermann Bujard, Charles H. Redfern, Michael Y. Degtyarev, Peter Coward, Elena K. Lee, Bruce R. Conklin, Glenn I. Fishman, Andrew T. Kwa, and Lothar Hennighausen

Subjects

Agonist, medicine.medical_specialty, Pyrrolidines, medicine.drug_class, G protein, Transgene, Biomedical Engineering, Mice, Transgenic, Bioengineering, GTP-Binding Protein alpha Subunits, Gi-Go, Biology, Applied Microbiology and Biotechnology, Mice, Transactivation, Opioid receptor, Internal medicine, Bradycardia, medicine, Animals, Humans, Cloning, Molecular, Receptor, Receptors, Opioid, kappa, Cell biology, Endocrinology, Molecular Medicine, Receptor activated solely by a synthetic ligand, Signal transduction, Signal Transduction, Biotechnology

Abstract

To control G protein signaling in vivo, we have modified G protein-coupled receptors to respond exclusively to synthetic small molecule agonists and not to their natural agonist(s). These engineered receptors are designated RASSLs (receptor activated solely by a synthetic ligand). A prototype RASSL (Ro1) based on the Gi-coupled K opioid receptor was expressed in transgenic mice under the control of the tetracycline transactivator (tet) system. Activation of Ro1 expressed in the heart decreased heart rate by up to 80%, an expected effect of increased Gi signaling. Maximal heart rate changes occurred in less than 1 min, demonstrating the speed of this inducible signaling system. This Ro1-mediated slowing of heart rate was also subject to desensitization, which lasted more than 24 h. Both the initial effect on heart rate and the desensitization occurred, even though Ro1 is derived from a human opioid receptor not normally involved in heart rate control. In addition, the tet system was used to induce Ro1 expression in hepatocytes and salivary gland, where Gi signaling is known to control physiologic events such as proliferation and secretion. These studies demonstrate that a RASSL can be inducibly expressed in several mouse tissues and used in vivo to activate G protein signaling in a controllable fashion.

Published

1999

14. Controlling signaling with a specifically designed G i -coupled receptor

Author

Matthew S. Falk, H. Gary Wada, Huda Akil, Fan Meng, Bruce R. Conklin, Peter Coward, and Sam D. H. Chan

Subjects

Narcotics, G protein, medicine.drug_class, Recombinant Fusion Proteins, Molecular Sequence Data, CHO Cells, Biology, Binding, Competitive, Protein Structure, Secondary, Opioid receptor, Cricetinae, medicine, Animals, Humans, Amino Acid Sequence, Receptor, Opioid peptide, Multidisciplinary, Receptors, Opioid, kappa, Chinese hamster ovary cell, Spiradoline, Biological Sciences, Cell biology, Biochemistry, Drug Design, COS Cells, Receptor activated solely by a synthetic ligand, Signal transduction, Adenylyl Cyclases, Signal Transduction

Abstract

We are developing a system to control G protein signaling in vivo to regulate a broad range of physiologic responses. Our system utilizes G protein-coupled peptide receptors engineered to respond exclusively to synthetic small molecule ligands and not to their natural ligand(s). These engineered receptors are designated RASSLs (receptor activated solely by a synthetic ligand). We have made two prototype RASSLs that are based on the human κ opioid receptor. Small molecule drugs that activate the κ receptor are nonaddictive and safe to administer in vivo . Binding and signaling assays reveal 200–2000-fold reductions in the ability of our RASSLs to bind or be activated by dynorphin, an endogenous peptide ligand of the κ opioid receptor. In a high-throughput signaling assay, these prototype RASSLs expressed in Chinese hamster ovary K1 cells showed little or no response to a panel of 21 opioid peptides but still signaled normally in response to small molecule drugs such as spiradoline. Activation of a RASSL by spiradoline also caused proliferation of rat-1a tissue culture cells. These data provide evidence that G protein-coupled receptors can be made into RASSLs. The potential in vivo applications for RASSLs include the positive enrichment of transfected cells and the development of new animal models of disease.

Published

1998

15. Discovery and optimization of 5-(2-((1-(phenylsulfonyl)-1,2,3,4-tetrahydroquinolin-7-yl)oxy)pyridin-4-yl)-1,2,4-oxadiazoles as novel gpr119 agonists

Author

Mark P. Grillo, Karen Siegler, Ming Yu, Jiang Zhu, Peter Coward, Jian Ken Zhang, Frank Kayser, Bei Shan, Yingcai Wang, Julio C. Medina, Marion Conn, and Jiwen Jim Liu

Subjects

Oxadiazoles, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Oxadiazole, Ring (chemistry), Biochemistry, Rats, Receptors, G-Protein-Coupled, chemistry.chemical_compound, Macaca fascicularis, Structure-Activity Relationship, Aniline, GPR119, Free fraction, Drug Discovery, Quinolines, Molecular Medicine, Animals, Humans, Molecular Biology

Abstract

We describe the discovery and optimization of 5-(2-((1-(phenylsulfonyl)-1,2,3,4-tetrahydroquinolin-7-yl)oxy)pyridin-4-yl)-1,2,4-oxadiazoles as novel agonists of GPR119. Previously described aniline 2 had suboptimal efficacy in signaling assays using cynomolgus monkey (cyno) GPR119 making evaluation of the target in preclinical models difficult. Replacement of the aniline ring with a tetrahydroquinoline ring constrained the rotation of the aniline C–N bond and gave compounds with increased efficacy on human and cyno receptors. Additional optimization led to the discovery of 10, which possesses higher free fraction in plasma and improved pharmacokinetic properties in rat and cyno compared to 2.

Published

2013

16. Characterization of a novel glucokinase activator in rat and mouse models

Author

Lance Williams, Walter E. DeWolf, Maralee McVean, Murielle M. Véniant, Taylor Alford, Pingping Li, William S. Lagakos, Deborah A. Anderson, Peter Coward, Marion Conn, Mark Joseph Chicarelli, Min Lu, Brian R. Baer, and Gautam Bandyopadhyay

Subjects

Blood Glucose, Male, Anatomy and Physiology, Mouse, Glucose uptake, medicine.medical_treatment, lcsh:Medicine, Aminopyridines, Biochemistry, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Endocrinology, Insulin-Secreting Cells, Glucokinase, Insulin Secretion, Glucose homeostasis, Homeostasis, Insulin, Phosphorylation, lcsh:Science, Glucose tolerance test, Multidisciplinary, medicine.diagnostic_test, Animal Models, Enzymes, Liver, Area Under Curve, Medicine, Beta cell, Research Article, medicine.medical_specialty, Enzyme Activators, Carbohydrate metabolism, Biology, Catalysis, Diabetes Mellitus, Experimental, Model Organisms, Internal medicine, Thiadiazoles, medicine, Animals, Obesity, Enzyme Kinetics, Diabetic Endocrinology, Hexokinase, lcsh:R, Glucose Tolerance Test, Diabetes Mellitus Type 2, Rats, Mice, Inbred C57BL, Kinetics, Glucose, chemistry, Small Molecules, Hepatocytes, Rat, lcsh:Q, Physiological Processes, Energy Metabolism

Abstract

Glucokinase (GK) is a hexokinase isozyme that catalyzes the phosphorylation of glucose to glucose-6-phosphate. Glucokinase activators are being investigated as potential diabetes therapies because of their effects on hepatic glucose output and/or insulin secretion. Here, we have examined the efficacy and mechanisms of action of a novel glucokinase activator, GKA23. In vitro, GKA23 increased the affinity of rat and mouse glucokinase for glucose, and increased glucose uptake in primary rat hepatocytes. In vivo, GKA23 treatment improved glucose homeostasis in rats by enhancing beta cell insulin secretion and suppressing hepatic glucose production. Sub-chronic GKA23 treatment of mice fed a high-fat diet resulted in improved glucose homeostasis and lipid profile.

Published

2013

17. Discovery and optimization of arylsulfonyl 3-(pyridin-2-yloxy)anilines as novel GPR119 agonists

Author

Jiang Zhu, Bei Shan, Peter Coward, Mark P. Grillo, Frank Kayser, Yingcai Wang, Ming Yu, John Eksterowicz, Jian Ken Zhang, Marion Conn, Julio C. Medina, Jiwen Jim Liu, An-Rong Li, and Karen Siegler

Subjects

Models, Molecular, Aniline Compounds, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Receptors, G-Protein-Coupled, Mice, Structure-Activity Relationship, GPR119, Pharmacokinetics, Diabetes Mellitus, Type 2, Drug Discovery, Molecular Medicine, Animals, Humans, Gpr119 agonist, Molecular Biology

Abstract

We describe the discovery of a series of arylsulfonyl 3-(pyridin-2-yloxy)anilines as GPR119 agonists derived from compound 1. Replacement of the three methyl groups in 1 with metabolically stable moieties led to the identification of compound 34, a potent and efficacious GPR119 agonist with improved pharmacokinetic (PK) properties.

Published

2013

18. Functional comparison of the Mus musculus molossinus and Mus musculus domesticus Sry genes

Author

Robert A. Dubin, Yun-Fai Chris Lau, Harry Ostrer, and Peter Coward

Subjects

Transcriptional Activation, Sex Determination Analysis, Saccharomyces cerevisiae Proteins, CHO Cells, Biology, Transfection, Fungal Proteins, Mice, Open Reading Frames, chemistry.chemical_compound, Endocrinology, Genes, Reporter, Transcription (biology), Cricetinae, Animals, Humans, Molecular Biology, Gene, Transcription factor, Reporter gene, Binding Sites, Base Sequence, Point mutation, Nuclear Proteins, DNA, General Medicine, Molecular biology, Sex-Determining Region Y Protein, DNA-Binding Proteins, Open reading frame, Testis determining factor, chemistry, HeLa Cells, Transcription Factors

Abstract

The Sry gene functions as a genetic switch initiating testicular development of the indifferent mammalian gonad. The Mus musculus molossinus Sry open reading frame (ORF) encodes a 395-amino acid transcription factor (mSry) that specifically binds and bends DNA through its N-terminal HMG domain and activates transcription through its long C-terminal (residues 144-366) glutamine/histidine-rich activation domain. The M. m. domesticus Sry ORF encodes a highly homologous, truncated protein (dSry) of approximately 230 amino acids, and the molecular basis for truncation is a point mutation that creates an amber stop codon within the activation domain. The mSry protein activates transcription of a Sry-responsive reporter gene in HeLa cells, but dSry does not. Gene swapping and in vitro DNA binding experiments revealed that lack of transcriptional activation by dSry was not the result of polymorphisms within the first 137 amino acids of the protein. Direct analysis of the C-terminal glutamine/histidine-rich domain revealed that dSry lacked a functional transcriptional activation domain. Fusion of the GAL4 DNA-binding domain to the C-terminal deletion mutants of the GAL4-mSry chimeric protein indicated that residues 263-345 of the glutamine/histidine-rich domain were necessary for high level transactivation. Furthermore, readthrough of the premature amber stop codon by transfer RNA suppression resulted in a strong GAL4-dSry transactivator. This demonstrated that the premature stop codon is the only polymorphism responsible for the inability of the dSry glutamine/histidine-rich region to transactivate.

Published

1995

19. ChemInform Abstract: Discovery and Optimization of a Novel Neuromedin B Receptor Antagonist

Author

Stephen J. Shuttleworth, Anne Chai, Jiasheng Fu, Richard V. Connors, and Peter Coward

Subjects

Stereochemistry, Chemistry, Core (graph theory), Antagonist, General Medicine, Neuromedin B receptor, Combinatorial chemistry, Small molecule, respiratory tract diseases

Abstract

The discovery and parallel synthesis of potent, small molecule antagonists of Neuromedin B receptor based on the ary-hexahydro-dibenzodiazepin-1-one core is described.

Published

2009

20. Discovery and optimization of a novel Neuromedin B receptor antagonist

Author

Peter Coward, Jiasheng Fu, Anne Chai, Stephen J. Shuttleworth, and Richard V. Connors

Subjects

Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Pharmaceutical Science, Electrons, Neuromedin B receptor, Ligands, Biochemistry, Chemical synthesis, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Molecular Biology, Benzodiazepinones, Dose-Response Relationship, Drug, Chemistry, Organic Chemistry, Antagonist, Small molecule, respiratory tract diseases, Bombesin receptor, Receptors, Bombesin, Gastrin-Releasing Peptide, Models, Chemical, Drug Design, Benzene derivatives, Molecular Medicine, Peptides, HeLa Cells

Abstract

The discovery and parallel synthesis of potent, small molecule antagonists of Neuromedin B receptor based on the ary-hexahydro-dibenzodiazepin-1-one core is described.

Published

2009

21. Identification of a PPARdelta agonist with partial agonistic activity on PPARgamma

Author

Nigel Walker, Athena Sudom, Steve Hiscock, Peter Coward, Brian M. Fox, Alex Zhang, Yang Li, Sheree Johnstone, Anne Chai, Martin Harrison, Marc Labelle, Richard V. Connors, Jinsong Liu, Michael Dore, Malgorzata Wanska, Zhulun Wang, and Karen Siegler

Subjects

Agonist, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Peroxisome proliferator-activated receptor, Pharmacology, Crystallography, X-Ray, Biochemistry, Rats sprague dawley, Rats, Sprague-Dawley, Drug Discovery, medicine, Agonistic behaviour, Animals, Computer Simulation, PPAR delta, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Biological activity, Rats, PPAR gamma, Thiazoles, chemistry, Nuclear receptor, Molecular Medicine, Peroxisome proliferator-activated receptor delta

Abstract

The discovery and optimization of a series of potent PPARdelta full agonists with partial agonistic activity against PPARgamma is described.

Published

2009

22. Application of an allosteric model to describe the interactions among retinol binding protein 4, transthyretin, and small molecule retinol binding protein 4 ligands

Author

Fei Xiong, Jeff D. Reagan, Marion Conn, Anthony Menjares, Peter Coward, and Jie Tang

Subjects

Retinyl Esters, Allosteric modulator, Fenretinide, Biophysics, Retinyl acetate, Ligands, Biochemistry, Models, Biological, chemistry.chemical_compound, Structure-Activity Relationship, Fluorescence Resonance Energy Transfer, Humans, Prealbumin, Binding site, Vitamin A, Molecular Biology, Retinol binding protein 4, Binding Sites, biology, Binding protein, nutritional and metabolic diseases, Cell Biology, Transthyretin, Retinol binding protein, Kinetics, chemistry, biology.protein, Diterpenes, Retinol-Binding Proteins, Plasma

Abstract

Retinol binding protein 4 (RBP4) is a serum protein that serves as the major transport protein for retinol (vitamin A). Recent reports suggest that elevated levels of RBP4 are associated with insulin resistance and that insulin sensitivity may be improved by reducing serum RBP4 levels. This can be accomplished by administration of small molecules, such as fenretinide, that compete with retinol for binding to RBP4 and disrupt the protein-protein interaction between RBP4 and transthyretin (TTR), another serum protein that protects RBP4 from renal clearance. We developed a fluorescence resonance energy transfer (FRET) assay that measures the interaction between RBP4 and TTR and can be used to determine the binding affinities of RBP4 ligands. We present an allosteric model that describes the pharmacology of interaction among RBP4, TTR, retinol, and fenretinide, and we show data that support the model. We show that retinol increases the affinity of RBP4 for TTR by a factor of 4 and determine the affinity constants of fenretinide and retinyl acetate. The assay may be useful for characterizing small molecule ligands that bind to RBP4 and disrupt its interaction with TTR. In addition, such a model could be used to describe other protein-protein interactions that are modulated by small molecules.

Published

2008

23. Tools for dissecting signaling pathways in vivo: Receptors activated solely by synthetic ligands

Author

Peter Coward, Bruce R. Conklin, Charles H. Redfern, and Kimberly Scearce-Levie

Subjects

Activator (genetics), G protein, Binding site, Signal transduction, Biology, Ligand (biochemistry), Receptor, Small molecule, Cell biology, G protein-coupled receptor

Abstract

Publisher Summary The diversity of G protein-coupled receptors (GPCRs) presents a challenge to understanding the connection between a single receptor signaling pathway and a specific physiological or pathological response. Receptors activated solely by synthetic ligands (RASSLs) offer control over the location, timing, and specificity of a G protein signal in vivo. These novel, reversible switches for G protein signaling have clarified the role of Gi signaling in cardiac physiology and are now being used to probe sensory transduction and complex neurobehavioral responses. This chapter summarizes the design of RASSLs and their first use in vivo. Existing RASSLs will allow study of the effects of Gi signaling in specific tissues under specific circumstances. New RASSLs can be developed by using many of the same principles used to develop the existing Gi-coupled RASSLs. The ideal RASSL activator should be a small molecule drug that is readily available from commercial sources. Its binding site should be well characterized. It must be highly specific for a single receptor subtype to minimize effects of the drug at non-RASSL receptors. Ideally, this could be a synthetic system in which the ligand would not activate endogenous receptors.

Published

2002

24. Tools for dissecting signaling pathways in vivo: receptors activated solely by synthetic ligands

Author

Kimberly, Scearce-Levie, Peter, Coward, Charles H, Redfern, and Bruce R, Conklin

Subjects

Mice, Knockout, Mice, Doxycycline, Receptors, Opioid, delta, Molecular Sequence Data, Animals, Amino Acid Sequence, Ligands, Signal Transduction

Published

2001

25. Engineering receptors activated solely by synthetic ligands (RASSLs)

Author

Kimberly Scearce-Levie, Peter Coward, Charles H. Redfern, and Bruce R. Conklin

Subjects

Pharmacology, Analgesics, Pyrrolidines, Transgene, Receptors, Opioid, kappa, Recombinant Fusion Proteins, Endogeny, Receptor signaling, Mice, Transgenic, Receptors, Cell Surface, Biology, Toxicology, Mice, In vivo, Heart Rate, Animals, Humans, Technology, Pharmaceutical, Signal transduction, Receptor, Neuroscience, Synthetic ligands, G protein-coupled receptor, Signal Transduction

Abstract

The functional and molecular diversity of G-protein-coupled receptors presents a significant challenge to understanding the connection between a single receptor signaling pathway and a specific physiological or pathological response. To gain control over the timing and specificity of a G-protein signal, receptors activated solely by synthetic ligands (RASSLs) have been developed. These engineered receptors no longer respond to endogenous peptides, but can still be activated by a specific small-molecule drug. Further control over the location of the signal can be achieved by using RASSLs in conjunction with tissue-specific expression systems in vivo. Existing RASSLs have clarified the role of G(i) signaling in cardiac physiology and are currently being used to study cardiomyopathy, muscle remodeling, sensory transduction and complex neurobehavioral responses.

Published

2001

26. Polymorphism of a CAG trinucleotide repeat within Sry correlates with B6.YDom sex reversal

Author

Peter Coward, Degao Chen, Claude M. Nagamine, Harrison D. Thomas, Yun-Fai Chris Lau, and Kozo Nagai

Subjects

Male, Sex Determination Analysis, Molecular Sequence Data, Disorders of Sex Development, Mice, Inbred Strains, Biology, Y chromosome, Mice, Y Chromosome, Genetics, Animals, Amino Acid Sequence, Allele, Gene, DNA Primers, Repetitive Sequences, Nucleic Acid, Polymorphism, Genetic, Base Sequence, Sequence Homology, Amino Acid, Laboratory mouse, Nuclear Proteins, DNA, Sex reversal, Sex-Determining Region Y Protein, DNA-Binding Proteins, Mice, Inbred C57BL, Testis determining factor, Oligodeoxyribonucleotides, Microsatellite, Female, Trinucleotide repeat expansion, Transcription Factors

Abstract

Breeding the Y chromosome from certain Mus musculus domesticus strains onto the inbred laboratory mouse strain, C57BL/6J (B6), results in hermaphroditic progeny. This strain–dependent sex reversal suggests that there may be significant allelic variation in the murine sex determining gene, Sry. We have analysed the Sry genes from several domesttcus–type Y chromosomes and show that they encode smaller proteins than the molossinus–type alleles SryB6 and Sry129. We have also identified a polymorphic stretch of trinucleotide repeats that is unique to strains causing sex reversal and show that specific changes in the predicted polyglutamine amino acid sequence at this site are associated with different degrees of sex reversal.

Published

1994

27. A critical period of vulnerability to hyperactive Gq signaling revealed by inducible and heart-specific expression of Gq∗ in transgenic mice

Author

Nathalie Cotte, Tim McKinsey, Anthony J. Baker, Peter Coward, Nathan Salomonis, Janet A. Warrington, Nila Shah, Eric N. Olson, Peter Mikus, Bruce R. Conklin, Seigo Izumo, Tetsuo Shioi, Charles H. Redfern, Andrew T. Kwa, and Michael Y. Degtyarev

Subjects

Genetics, Basic research, business.industry, Period (gene), Medicine, Theology, Cardiology and Cardiovascular Medicine, business

Abstract

037 A Critical Period of Vulnerability to Hyperactive Gq Signaling Revealed by Inducible and Heart-Specific Expression of Gq* in Transgenic Mice Nathalie Cotte, 1 Charles H. Redfern, 1'2 Peter Mikus, 1 Nathan Salomonis, 1 Michael Y. Degtyarev] Peter S. Coward, 1 Andrew Kwa, 1 Tetsuo Shioi, 4 Nila Shah, 5 Tim McKinsey, 3 Eric Olson, s Seigo Izumo, a Janet Wartington, s Anthony J. Baker, 2 Brace R. Conklin~'2; 1Gladstone Institute of Cardiovascular Disease, Gladstone Institute of Neurological Disease, 2Department of Medicine, University of California, San Francisco, CA, 3Hamon Center for Basic Research in Cancer, University of Texas Southwestern Medical Center, Dallas, TX, 4Beth Israel Deaconess Medical Center, Harvard University, Boston, MA, SAffymetrix Inc, Santa Clara, CA

Published

1999