Your search keyword '"Erik T. Bodor"' showing total 7 results

1. C(8)-Substituted 1-azabicyclo[3.3.1]non-3-enes: a novel scaffold for muscarinic receptor ligands

Author

T. Kendall Harden, Harold Kohn, Myoung Goo Kim, and Erik T. Bodor

Subjects

Aza Compounds, Bicyclic molecule, Chemistry, Ligand, Stereochemistry, Spectrum Analysis, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biological activity, Muscarinic Antagonists, Ligands, Biochemistry, Chemical synthesis, Enol, Bridged Bicyclo Compounds, chemistry.chemical_compound, Competitive antagonist, COS Cells, Drug Discovery, Muscarinic acetylcholine receptor, Animals, Molecular Medicine, Receptor, Molecular Biology

Abstract

The [3.3.1]-bicyclic amine, exo -8-benzyloxymethyl-3-ethoxycarbonyl-4-hydroxy-1-azabicyclo[3.3.1]non-3-ene ( 1 ), has been shown to be a potent competitive antagonist against the hM 1 –hM 5 muscarinic receptors. This heterocyclic system has not been extensively evaluated despite the notable activities reported for other bicyclic amines. Synthetic strategies permitted the selective alteration of five structural sites in 1 . Pharmacological evaluation demonstrated that modification of either the C(3) alkoxycarbonyl or the C(4) enol units in 1 gave compounds with high affinity for the hM 1 –hM 5 muscarinic receptors with selectivity for the hM 2 receptor.

Published

2004

2. Purification and Functional Reconstitution of the Human P2Y12Receptor

Author

G L Waldo, Erik T. Bodor, T. Kendall Harden, Shelley B. Hooks, José L. Boyer, and James Corbitt

Subjects

Pharmacology, Agonist, P2Y receptor, biology, Receptors, Purinergic P2, medicine.drug_class, G protein, Membrane Proteins, Sf9, Transfection, Receptors, Purinergic P2Y12, Adenosine Diphosphate, RGS4, G beta-gamma complex, Biochemistry, Gq alpha subunit, Heterotrimeric G protein, COS Cells, Chlorocebus aethiops, biology.protein, medicine, Animals, Humans, Molecular Medicine

Abstract

The human P2Y12 receptor (P2Y12-R) is a member of the G protein coupled P2Y receptor family, which is intimately involved in platelet physiology. We describe here the purification and functional characterization of recombinant P2Y12-R after high-level expression from a baculovirus in Sf9 insect cells. Purified P2Y12-R, Gbeta1gamma2, and various Galpha-subunits were reconstituted in lipid vesicles, and steady-state GTPase activity was quantified. GTP hydrolysis in proteoliposomes formed with purified P2Y12-R and Galphai2beta1gamma2 was stimulated by addition of either 2-methylthio-ADP (2MeSADP) or RGS4 and was markedly enhanced by their combined presence. 2MeSADP was the most potent agonist (EC50 = 80 nM) examined, whereas ADP, the cognate agonist of the P2Y12-R, was 3 orders of magnitude less potent. ATP had no effect alone but inhibited the action of 2MeSADP; therefore, ATP is a relatively low-affinity antagonist of the P2Y12-R. The G protein selectivity of the P2Y12-R was examined by reconstitution with various G protein alpha-subunits in heterotrimeric form with Gbeta1gamma2. The most robust coupling of the P2Y12-R was to Galphai2, but effective coupling also occurred to Galphai1 and Galphai3. In contrast, little or no coupling occurred to Galphao or Galphaq. These results illustrate that the signaling properties of the P2Y12-R can be studied as a purified protein under conditions that circumvent the complications that occur in vivo because of nucleotide metabolism and interconversion as well as nucleotide release.

Published

2003

3. C(8) Substituted 1-Azabicyclo[3.3.1]non-3-enes and C(8) Substituted 1-Azabicyclo[3.3.1]nonan-4-ones: Novel Muscarinic Receptor Antagonists

Author

Erik T. Bodor, Myoung Goo Kim, Chen Wang, Harold Kohn, and T. Kendall Harden

Subjects

Magnetic Resonance Spectroscopy, Stereochemistry, Inositol Phosphates, Substituent, Muscarinic Antagonists, Crystallography, X-Ray, Binding, Competitive, Chemical synthesis, Cell Line, Radioligand Assay, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Pyridine, Animals, Humans, Membranes, Bicyclic molecule, Diastereomer, Stereoisomerism, Bridged Bicyclo Compounds, Heterocyclic, Enol, chemistry, Molecular Medicine, Ethyl acrylate, Piperidine

Abstract

Expedient syntheses of C(8) substituted 1-azabicyclo[3.3.1]non-3-enes and C(8) substituted 1-azabicyclo[3.3.1]nonan-4-ones are reported to begin with 2,5-disubstituted pyridines. Catalytic reduction of the pyridine to the piperidine followed by treatment with ethyl acrylate and Dieckmann cyclization gave diastereomeric mixtures of C(8) substituted 3-ethoxycarbonyl-4-hydroxy-1-azabicyclo[3.3.1]non-3-enes, which were separable by chromatography. We found that the catalytic reduction (PtO2, H2) procedure provided the cis-substituted piperidine but that pyridine reduction was accompanied by competitive cleavage of the C(2) pyridyl substituent. Accordingly, an alternative route was devised that afforded a diastereomeric mixture of the cis- and trans-2,5-disubstituted piperidine. Treatment of the substituted pyridine with m-CPBA gave the pyridine N-oxide, which was reduced to the piperidine by sequential reduction with ammonium formate in the presence of Pd-C followed by NaBH3CN. Addition of ethyl acrylate completed the synthesis of the substituted piperidine. The overall four-step reaction gave higher yields (57%) than the two-step procedure (13%) with little cleavage of the C(2) pyridyl substituent. Acid decarboxylation of the bicyclo[3.3.1]non-3-enes provided the C(8) substituted 1-azabicyclo[3.3.1]nonan-4-ones. Structural studies revealed diagnostic 13C NMR signals that permit assignment of the orientation of the C(8) substituent. Pharmacological investigations documented that 3-ethoxycarbonyl-4-hydroxy-1-azabicyclo[3.3.1]non-3-enes efficiently bind to the human M1-M5 muscarinic receptors and function as antagonists. We observed that exo-8-benzyloxymethyl-3-ethoxycarbonyl-4-hydroxy-1-azabicyclo[3.3.1]non-3-ene (3) displayed the highest affinity, exhibiting Ki values at all five muscarinic receptors that were approximately 10-50 times lower than carbachol and approximately 30-230 times lower than arecoline. Receptor selectivity was observed for 3. Compound 3 contained two different pharmacophores found in many muscarinic receptor ligands, and preliminary findings indicated the importance of both structural elements for maximal activity. Compound 3 serves as a novel lead compound for further drug development.

Published

2003

4. Nicotinic acid: pharmacological effects and mechanisms of action

Author

Andreas Gille, Kashan Ahmed, Stefan Offermanns, and Erik T. Bodor

Subjects

medicine.medical_specialty, Hyperlipidemias, Receptors, Nicotinic, Toxicology, Niacin, chemistry.chemical_compound, Internal medicine, medicine, Animals, Humans, Receptor, G protein-coupled receptor, Hypolipidemic Agents, Pharmacology, Clinical Trials as Topic, Nicotinamide, Cholesterol, Atherosclerosis, B vitamins, Endocrinology, Nicotinic agonist, Mechanism of action, chemistry, Cardiovascular Diseases, medicine.symptom, Lipoprotein

Abstract

Pharmacological doses of nicotinic acid induce a profound change in the plasma levels of various lipids and lipoproteins. The ability of nicotinic acid to strongly increase the plasma concentration of high-density lipoprotein (HDL) cholesterol has in recent years led to an increased interest in the pharmacological potential of nicotinic acid. There is increasing evidence that nicotinic acid alone or in addition to LDL cholesterol–lowering drugs can reduce the progression of atherosclerosis and reduce the risk of cardiovascular events. The clinical use of nicotinic acid is, however, hindered by harmless but unpleasant side effects, especially by a strong cutaneous vasodilation called flushing. The recent discovery of the G protein–coupled receptor GPR109A (HM74A or PUMA-G) as a receptor for nicotinic acid has allowed for better understanding of the mechanisms underlying the metabolic and vascular effects of nicotinic acid. On the basis of recent progress in understanding the pharmacological effects of nicotinic acid, new strategies are in development to better exploit the pharmacological potential of nicotinic acid. New drugs acting via the nicotinic acid receptor or related receptors, as well as new co-medications that suppress unwanted effects of nicotinic acid, will most likely be introduced as new therapeutic options in the treatment of dyslipidemia and the prevention of cardiovascular diseases.

Published

2007

5. RGS6, RGS7, RGS9, and RGS11 Stimulate GTPase Activity of G i Family G-proteins with Differential Selectivity and Maximal Activity

Author

Shelley B. Hooks, Erik T. Bodor, Andrejs M. Krumins, James Corbitt, T. Kendall Harden, and G L Waldo

Subjects

GTPase-activating protein, biology, G protein, GTP-Binding Protein alpha Subunits, Hydrolysis, GTPase-Activating Proteins, fungi, Cell Biology, GTPase, Spodoptera, GTP-Binding Protein alpha Subunits, Gi-Go, biology.organism_classification, Biochemistry, Heterotrimeric GTP-Binding Proteins, Cell biology, GTP-Binding Proteins, Heterotrimeric G protein, RGS9, Animals, Guanosine Triphosphate, sense organs, Molecular Biology, RGS Proteins

Abstract

Regulator of G-protein signaling (RGS) proteins are GTPase activating proteins (GAPs) of heterotrimeric G-proteins that alter the amplitude and kinetics of receptor-promoted signaling. In this study we defined the G-protein alpha-subunit selectivity of purified Sf9 cell-derived R7 proteins, a subfamily of RGS proteins (RGS6, -7, -9, and -11) containing a Ggamma-like (GGL) domain that mediates dimeric interaction with Gbeta(5). Gbeta(5)/R7 dimers stimulated steady state GTPase activity of Galpha-subunits of the G(i) family, but not of Galpha(q) or Galpha(11), when added to proteoliposomes containing M2 or M1 muscarinic receptor-coupled G-protein heterotrimers. Concentration effect curves of the Gbeta(5)/R7 proteins revealed differences in potencies and efficacies toward Galpha-subunits of the G(i) family. Although all four Gbeta(5)/R7 proteins exhibited similar potencies toward Galpha(o), Gbeta(5)/RGS9 and Gbeta(5)/RGS11 were more potent GAPs of Galpha(i1), Galpha(i2), and Galpha(i3) than were Gbeta(5)/RGS6 and Gbeta(5)/RGS7. The maximal GAP activity exhibited by Gbeta(5)/RGS11 was 2- to 4-fold higher than that of Gbeta(5)/RGS7 and Gbeta(5)/RGS9, with Gbeta(5)/RGS6 exhibiting an intermediate maximal GAP activity. Moreover, the less efficacious Gbeta(5)/RGS7 and Gbeta(5)/RGS9 inhibited Gbeta(5)/RGS11-stimulated GTPase activity of Galpha(o). Therefore, R7 family RGS proteins are G(i) family-selective GAPs with potentially important differences in activities.

Published

2003

6. Delineation of ligand binding and receptor signaling activities of purified P2Y receptors reconstituted with heterotrimeric G proteins

Author

Erik T. Bodor, T. Kendall Harden, Rainer Blaesius, and G L Waldo

Subjects

G protein-coupled receptor kinase, GTPase-activating protein, G protein, P2Y receptor, G protein coupled receptor, Review, Cell Biology, receptor purification, Biology, RGS proteins, Cellular and Molecular Neuroscience, Biochemistry, Heterotrimeric G protein, platelets, Protease-activated receptor, RGS Proteins, Molecular Biology, RGS2, nucleotide(s), G protein-coupled receptor

Abstract

P2Y receptors are G protein coupled receptors that respond to extracellular nucleotides to promote a multitude of signaling events. Our laboratory has purified several P2Y receptors with the goal of providing molecular insight into their: (1) ligand binding properties, (2) G protein signaling selectivities, and (3) regulation by RGS proteins and other signaling cohorts. The human P2Y(1) receptor and the human P2Y(12) receptor, both of which are intimately involved in ADP-mediated platelet aggregation, were purified to near homogeneity and studied in detail. After high-level expression from recombinant baculovirus infection of Sf9 insect cells, approximately 50% of the receptors were successfully extracted with digitonin. Purification of nearly homogeneous epitope-tagged P2Y receptor was achieved using metal-affinity chromatography followed by other traditional chromatographic steps. Yields of purified P2Y receptors range from 10 to 100 mug/l of infected cells. Once purified, the receptors were reconstituted in model lipid vesicles along with their cognate G proteins to assess receptor function. Agonist-promoted increases in steady-state GTPase assays demonstrated the functional activity of the reconstituted purified receptor. We have utilized this reconstitution system to assess the action of various nucleotide agonists and antagonists, the relative G protein selectivity, and the influence of other proteins, such as phospholipase C, on P2Y receptor-promoted signaling. Furthermore, we have identified the RGS expression profile of platelets and have begun to assess the action of these RGS proteins in a reconstituted P2Y receptor/G protein platelet model.

7. Structure of Gαi1 Bound to a GDP-Selective Peptide Provides Insight into Guanine Nucleotide Exchange

Author

Rainer Blaesius, Val J. Watts, Erik T. Bodor, T. Kendall Harden, Miller B. Jones, Christopher A. Johnston, Francis S. Willard, Zoey Fredericks, Mark R. Jezyk, J. Kevin Ramer, John Sondek, and David P. Siderovski

Subjects

Models, Molecular, Time Factors, G protein, Protein Conformation, Amino Acid Motifs, Molecular Sequence Data, Electrons, Enzyme-Linked Immunosorbent Assay, Plasma protein binding, Biosensing Techniques, Buffers, GTP-Binding Protein alpha Subunits, Gi-Go, Crystallography, X-Ray, Article, 03 medical and health sciences, GTP-binding protein regulators, Protein structure, Structural Biology, Peptide Library, Heterotrimeric G protein, Catalytic Domain, Guanine Nucleotide Exchange Factors, Nucleotide, Magnesium, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Sequence Homology, Amino Acid, Nucleotides, 030302 biochemistry & molecular biology, Stereoisomerism, Surface Plasmon Resonance, Guanine Nucleotides, Protein Structure, Tertiary, G beta-gamma complex, Kinetics, chemistry, Biochemistry, Biophysics, Guanine nucleotide exchange factor, Peptides, Dimerization, Protein Binding, Signal Transduction

Abstract

Heterotrimeric G proteins are molecular switches that regulate numerous signaling pathways involved in cellular physiology. This characteristic is achieved by the adoption of two principal states: an inactive, GDP bound state and an active, GTP bound state. Under basal conditions, G proteins exist in the inactive, GDP bound state; thus, nucleotide exchange is crucial to the onset of signaling. Despite our understanding of G protein signaling pathways, the mechanism of nucleotide exchange remains elusive. We employed phage display technology to identify nucleotide state-dependent Galpha binding peptides. Herein, we report a GDP-selective Galpha binding peptide, KB-752, that enhances spontaneous nucleotide exchange of Galpha(i) subunits. Structural determination of the Galpha(i1)/peptide complex reveals unique changes in the Galpha switch regions predicted to enhance nucleotide exchange by creating a GDP dissociation route. Our results cast light onto a potential mechanism by which Galpha subunits adopt a conformation suitable for nucleotide exchange.