Your search keyword '"Mutant Proteins agonists"' showing total 46 results

1. Androgenic modulation of AR-Vs.

Author

Hillebrand AC, Pizzolato LS, Branchini G, and Brum IS

Subjects

Cell Line, Tumor, Gene Expression Regulation, Neoplastic drug effects, Humans, Ligands, Male, Polymorphism, Genetic, Prostatic Neoplasms genetics, Prostatic Neoplasms metabolism, Prostatic Neoplasms pathology, Protein Isoforms agonists, Protein Isoforms metabolism, Androgens pharmacology, Mutant Proteins agonists, Mutant Proteins genetics, Mutant Proteins metabolism, Receptors, Androgen genetics, Receptors, Androgen metabolism

Abstract

Purpose: The importance of androgen receptor variants (AR-Vs) is recognized in prostate cancer. AR-Vs have been the focus of many studies. Expression of AR-Vs has been proposed as a biomarker for resistance to androgen deprivation therapy for metastatic disease. Herein, we show dynamic changes in AR-Vs expression in response to androgen modulation., Methods: The C4-2B cell line was exposed to low (10 -13  M) and high (10 -8  M) androgen (dihydrotestosterone, DHT) levels, with or without flutamide. mRNA and protein expression levels were assessed by qPCR and immunohistochemistry, respectively., Results: We demonstrated that high levels of DHT downregulate AR-FL and AR-Vs. Even though AR-Vs did not present ligand-binding domain, thus were not capable of binding to DHT, they present dynamic changes under androgen treatment. Treatment with flutamide alone or in association with low levels of DHT stimulates growth of prostatic cells., Conclusions: Importantly, we provide evidence that AR-Vs respond differently to androgenic modulation. These findings have implications for a better understanding of the role of AR-Vs in prostate carcinogenesis.

Published

2018

2. p120RasGAP Protein Mediates Netrin-1 Protein-induced Cortical Axon Outgrowth and Guidance.

Author

Antoine-Bertrand J, Duquette PM, Alchini R, Kennedy TE, Fournier AE, and Lamarche-Vane N

Subjects

Amino Acid Substitution, Animals, Cells, Cultured, Cerebral Cortex cytology, Chickens, DCC Receptor, Embryo, Mammalian cytology, Glutathione Transferase genetics, Glutathione Transferase metabolism, HEK293 Cells, Humans, Mutant Proteins agonists, Mutant Proteins genetics, Mutant Proteins metabolism, Nerve Growth Factors antagonists & inhibitors, Nerve Growth Factors chemistry, Nerve Growth Factors genetics, Nerve Tissue Proteins antagonists & inhibitors, Nerve Tissue Proteins chemistry, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Netrin-1, Neurons cytology, Peptide Fragments antagonists & inhibitors, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Protein Interaction Domains and Motifs, Protein Transport, RNA Interference, Rats, Receptors, Cell Surface chemistry, Receptors, Cell Surface metabolism, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Tumor Suppressor Proteins antagonists & inhibitors, Tumor Suppressor Proteins chemistry, Tumor Suppressor Proteins genetics, p120 GTPase Activating Protein antagonists & inhibitors, p120 GTPase Activating Protein chemistry, p120 GTPase Activating Protein genetics, Axons metabolism, Cerebral Cortex metabolism, Nerve Growth Factors metabolism, Neurons metabolism, Receptors, Cell Surface agonists, Signal Transduction, Tumor Suppressor Proteins agonists, Tumor Suppressor Proteins metabolism, p120 GTPase Activating Protein metabolism

Abstract

The receptor deleted in colorectal cancer (DCC) mediates the attraction of growing axons to netrin-1 during brain development. In response to netrin-1 stimulation, DCC becomes a signaling platform to recruit proteins that promote axon outgrowth and guidance. The Ras GTPase-activating protein (GAP) p120RasGAP inhibits Ras activity and mediates neurite retraction and growth cone collapse in response to repulsive guidance cues. Here we show an interaction between p120RasGAP and DCC that positively regulates netrin-1-mediated axon outgrowth and guidance in embryonic cortical neurons. In response to netrin-1, p120RasGAP is recruited to DCC in growth cones and forms a multiprotein complex with focal adhesion kinase and ERK. We found that Ras/ERK activities are elevated aberrantly in p120RasGAP-deficient neurons. Moreover, the expression of p120RasGAP Src homology 2 (SH2)-SH3-SH2 domains, which interact with the C-terminal tail of DCC, is sufficient to restore netrin-1-dependent axon outgrowth in p120RasGAP-deficient neurons. We provide a novel mechanism that exploits the scaffolding properties of the N terminus of p120RasGAP to tightly regulate netrin-1/DCC-dependent axon outgrowth and guidance., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

3. Type I Interferon Signaling Is Decoupled from Specific Receptor Orientation through Lenient Requirements of the Transmembrane Domain.

Author

Sharma N, Longjam G, and Schreiber G

Subjects

Amino Acid Sequence, Cell Line, Computational Biology, Conserved Sequence, Gene Knockout Techniques, Humans, Kinetics, Mutagenesis, Insertional, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins metabolism, Peptide Fragments agonists, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Protein Conformation, Protein Interaction Domains and Motifs, Protein Structure, Tertiary, Receptor, Interferon alpha-beta chemistry, Receptor, Interferon alpha-beta genetics, Receptor, Interferon alpha-beta metabolism, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Interferon-alpha metabolism, Models, Molecular, Receptor, Interferon alpha-beta agonists, Signal Transduction

Abstract

Type I interferons serve as the first line of defense against pathogen invasion. Binding of IFNs to its receptors, IFNAR1 and IFNAR2, is leading to activation of the IFN response. To determine whether structural perturbations observed during binding are propagated to the cytoplasmic domain, multiple mutations were introduced into the transmembrane helix and its surroundings. Insertion of one to five alanine residues near either the N or C terminus of the transmembrane domain (TMD) likely promotes a rotation of 100° and a translation of 1.5 Å per added residue. Surprisingly, the added alanines had little effect on the binding affinity of IFN to the cell surface receptors, STAT phosphorylation, or gene induction. Similarly, substitution of the juxtamembrane residues of the TMD with alanines, or replacement of the TMD of IFNAR1 with that of IFNAR2, did not affect IFN binding or activity. Finally, only the addition of 10 serine residues (but not 2 or 4) between the extracellular domain of IFNAR1 and the TMD had some effect on signaling. Bioinformatic analysis shows a correlation between high sequence conservation of TMDs of cytokine receptors and the ability to transmit structural signals. Sequence conservation near the TMD of IFNAR1 is low, suggesting limited functional importance for this region. Our results suggest that IFN binding to the extracellular domains of IFNAR1 and IFNAR2 promotes proximity between the intracellular domains and that differential signaling is a function of duration of activation and affinity of binding rather than specific conformational changes transmitted from the outside to the inside of the cell., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

4. Structural Analysis on the Pathologic Mutant Glucocorticoid Receptor Ligand-Binding Domains.

Author

Hurt DE, Suzuki S, Mayama T, Charmandari E, and Kino T

Subjects

Amino Acid Motifs, Amino Acid Sequence, Carrier Proteins chemistry, Carrier Proteins metabolism, Dexamethasone pharmacology, HCT116 Cells, Humans, Leucine chemistry, Ligands, Models, Molecular, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins metabolism, Nerve Tissue Proteins chemistry, Nerve Tissue Proteins metabolism, Peptides chemistry, Peptides metabolism, Pregnatrienes pharmacology, Protein Binding drug effects, Protein Structure, Tertiary, Receptors, Glucocorticoid agonists, Static Electricity, Thermodynamics, Transcription, Genetic drug effects, Mutant Proteins chemistry, Mutant Proteins genetics, Mutation genetics, Receptors, Glucocorticoid chemistry, Receptors, Glucocorticoid genetics

Abstract

Glucocorticoid receptor (GR) gene mutations may cause familial or sporadic generalized glucocorticoid resistance syndrome. Most of the missense forms distribute in the ligand-binding domain and impair its ligand-binding activity and formation of the activation function (AF)-2 that binds LXXLL motif-containing coactivators. We performed molecular dynamics simulations to ligand-binding domain of pathologic GR mutants to reveal their structural defects. Several calculated parameters including interaction energy for dexamethasone or the LXXLL peptide indicate that destruction of ligand-binding pocket (LBP) is a primary character. Their LBP defects are driven primarily by loss/reduction of the electrostatic interaction formed by R611 and T739 of the receptor to dexamethasone and a subsequent conformational mismatch, which deacylcortivazol resolves with its large phenylpyrazole moiety and efficiently stimulates transcriptional activity of the mutant receptors with LBP defect. Reduced affinity of the LXXLL peptide to AF-2 is caused mainly by disruption of the electrostatic bonds to the noncore leucine residues of this peptide that determine the peptide's specificity to GR, as well as by reduced noncovalent interaction against core leucines and subsequent exposure of the AF-2 surface to solvent. The results reveal molecular defects of pathologic mutant receptors and provide important insights to the actions of wild-type GR.

Published

2016

5. Drosophila Avoids Parasitoids by Sensing Their Semiochemicals via a Dedicated Olfactory Circuit.

Author

Ebrahim SA, Dweck HK, Stökl J, Hofferberth JE, Trona F, Weniger K, Rybak J, Seki Y, Stensmyr MC, Sachse S, Hansson BS, and Knaden M

Subjects

Alkaloids pharmacology, Animals, Animals, Genetically Modified, Behavior, Animal drug effects, Bridged Bicyclo Compounds, Heterocyclic pharmacology, Drosophila Proteins genetics, Drosophila Proteins metabolism, Drosophila melanogaster genetics, Drosophila melanogaster parasitology, Drosophila melanogaster physiology, Female, Iridoids pharmacology, Larva drug effects, Larva genetics, Larva parasitology, Larva physiology, Mutant Proteins agonists, Mutant Proteins metabolism, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Odorants, Olfactory Bulb metabolism, Oviposition, Protein Isoforms agonists, Protein Isoforms metabolism, Pyridines pharmacology, Receptors, Odorant genetics, Receptors, Odorant metabolism, Sensory Receptor Cells metabolism, Signal Transduction, Terpenes pharmacology, Drosophila Proteins agonists, Drosophila melanogaster drug effects, Nerve Tissue Proteins agonists, Olfactory Bulb drug effects, Receptors, Odorant agonists, Sensory Receptor Cells drug effects, Wasps metabolism

Abstract

Detecting danger is one of the foremost tasks for a neural system. Larval parasitoids constitute clear danger to Drosophila, as up to 80% of fly larvae become parasitized in nature. We show that Drosophila melanogaster larvae and adults avoid sites smelling of the main parasitoid enemies, Leptopilina wasps. This avoidance is mediated via a highly specific olfactory sensory neuron (OSN) type. While the larval OSN expresses the olfactory receptor Or49a and is tuned to the Leptopilina odor iridomyrmecin, the adult expresses both Or49a and Or85f and in addition detects the wasp odors actinidine and nepetalactol. The information is transferred via projection neurons to a specific part of the lateral horn known to be involved in mediating avoidance. Drosophila has thus developed a dedicated circuit to detect a life-threatening enemy based on the smell of its semiochemicals. Such an enemy-detecting olfactory circuit has earlier only been characterized in mice and nematodes.

Published

2015

6. Activation of p53 in Human and Murine Cells by DNA-Damaging Agents Differentially Regulates Aryl Hydrocarbon Receptor Levels.

Author

Panchanathan R, Liu H, and Choubey D

Subjects

Animals, Antibiotics, Antineoplastic adverse effects, Basic Helix-Loop-Helix Transcription Factors chemistry, Basic Helix-Loop-Helix Transcription Factors genetics, Basic Helix-Loop-Helix Transcription Factors metabolism, Cell Line, Cell Line, Transformed, Cell Line, Tumor, Fibroblasts drug effects, Fibroblasts metabolism, Gene Expression Regulation drug effects, Humans, Ligands, Macrophages drug effects, Macrophages metabolism, Mice, Mutant Proteins agonists, Mutant Proteins metabolism, Osteosarcoma drug therapy, Osteosarcoma metabolism, Protein Stability drug effects, Receptors, Aryl Hydrocarbon chemistry, Receptors, Aryl Hydrocarbon genetics, Receptors, Aryl Hydrocarbon metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Species Specificity, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Antibiotics, Antineoplastic pharmacology, Basic Helix-Loop-Helix Transcription Factors agonists, Basic Helix-Loop-Helix Transcription Factors antagonists & inhibitors, Mutagens toxicity, Receptors, Aryl Hydrocarbon agonists, Receptors, Aryl Hydrocarbon antagonists & inhibitors, Teratogens toxicity, Tumor Suppressor Protein p53 agonists

Abstract

Aryl hydrocarbon receptor (AhR) is a ligand-activated transcription factor that regulates multiple cellular processes. The anticancer drug doxorubicin (DOX) can activate AhR-mediated transcription of target genes. Because DOX in cells activates a DNA damage response involving ataxia telangiectasia-mutated (ATM)-mediated activation of p53, we investigated whether the activation of the p53 in cells by DNA-damaging agents such as DOX or bleomycin could regulate the AhR levels. Here we report that activation of p53 by DNA-damaging agents in human cells increased levels of AhR through a posttranscriptional mechanism. Accordingly, fibroblasts from ATM patients, which are defective in p53 activation, expressed reduced constitutive levels of AhR and treatment of cells with bleomycin did not appreciably increase the AhR levels. Further, activation of p53 in cells stimulated the expression of AhR target genes. In murine cells, activation of p53 reduced the levels of AhR messenger RNA and protein and reduced the expression of AhR target genes. Our observations revealed that activation of p53 in human and murine cells differentially regulates AhR levels., (© The Author(s) 2015.)

Published

2015

7. The regulatory role of Streptomyces coelicolor TamR in central metabolism.

Author

Huang H, Sivapragasam S, and Grove A

Subjects

Aconitic Acid metabolism, Bacterial Proteins agonists, Bacterial Proteins genetics, Citric Acid metabolism, Enzyme Induction, Genes, Reporter, Isocitrate Dehydrogenase chemistry, Isocitrate Dehydrogenase genetics, Isocitrate Dehydrogenase metabolism, Ligands, Malate Dehydrogenase chemistry, Malate Dehydrogenase genetics, Malate Dehydrogenase metabolism, Malate Synthase chemistry, Malate Synthase genetics, Malate Synthase metabolism, Methyltransferases chemistry, Methyltransferases genetics, Mutant Proteins agonists, Mutant Proteins metabolism, Promoter Regions, Genetic, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Repressor Proteins genetics, Response Elements, Species Specificity, Streptomyces coelicolor enzymology, Bacterial Proteins metabolism, Citric Acid Cycle, Gene Expression Regulation, Bacterial, Methyltransferases metabolism, Repressor Proteins metabolism, Streptomyces coelicolor metabolism

Abstract

Trans-aconitate methyltransferase regulator (TamR) is a member of the ligand-responsive multiple antibiotic resistance regulator (MarR) family of transcription factors. In Streptomyces coelicolor, TamR regulates transcription of tamR (encoding TamR), tam (encoding trans-aconitate methyltransferase) and sacA (encoding aconitase); up-regulation of these genes promotes metabolic flux through the citric acid cycle. DNA binding by TamR is attenuated and transcriptional derepression is achieved on binding of ligands such as citrate and trans-aconitate to TamR. In the present study, we show that three additional genes are regulated by S. coelicolor TamR. Genes encoding malate synthase (aceB1; SCO6243), malate dehydrogenase (mdh; SCO4827) and isocitrate dehydrogenase (idh; SCO7000) are up-regulated in vivo when citrate and trans-aconitate accumulate, and TamR binds the corresponding gene promoters in vitro, a DNA binding that is attenuated by cognate ligands. Mutations to the TamR binding site attenuate DNA binding in vitro and result in constitutive promoter activity in vivo. The predicted TamR binding sites are highly conserved in the promoters of these genes in Streptomyces species that encode divergent tam-tamR gene pairs, suggesting evolutionary conservation. Like aconitase and trans-aconitate methyltransferase, malate dehydrogenase, isocitrate dehydrogenase and malate synthase are closely related to the citric acid cycle, either catalysing individual reaction steps or, in the case of malate synthase, participating in the glyoxylate cycle to produce malate that enters the citric acid cycle to replenish the intermediate pool. Taken together, our data suggest that TamR plays an important and conserved role in promoting metabolic flux through the citric acid cycle.

Published

2015

8. Free energy calculations of A(2A) adenosine receptor mutation effects on agonist binding.

Author

Keränen H, Åqvist J, and Gutiérrez-de-Terán H

Subjects

Adenosine A2 Receptor Agonists pharmacology, Binding Sites, Humans, Molecular Structure, Mutant Proteins genetics, Mutant Proteins metabolism, Mutation genetics, Receptor, Adenosine A2A metabolism, Adenosine A2 Receptor Agonists chemistry, Molecular Dynamics Simulation, Mutant Proteins agonists, Mutant Proteins chemistry, Receptor, Adenosine A2A chemistry, Receptor, Adenosine A2A genetics, Thermodynamics

Abstract

A general computational scheme to evaluate the effects of single point mutations on ligand binding is reported. This scheme is applied to characterize agonist binding to the A2A adenosine receptor, and is found to accurately explain how point mutations of different nature affect the binding affinity of a potent agonist.

Published

2015

9. Analyzing the roles of multi-functional proteins in cells: The case of arrestins and GRKs.

Author

Gurevich VV and Gurevich EV

Subjects

Animals, Arrestins agonists, Arrestins chemistry, Arrestins genetics, Enzyme Activation, G-Protein-Coupled Receptor Kinases chemistry, G-Protein-Coupled Receptor Kinases genetics, Gene Knockdown Techniques, Gene Knockout Techniques, Humans, Ligands, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Signal Transduction, Arrestins metabolism, G-Protein-Coupled Receptor Kinases metabolism, Models, Molecular

Abstract

Most proteins have multiple functions. Obviously, conventional methods of manipulating the level of the protein of interest in the cell, such as over-expression, knockout or knockdown, affect all of its functions simultaneously. The key advantage of these methods is that over-expression, knockout or knockdown does not require any knowledge of the molecular mechanisms of the function(s) of the protein of interest. The disadvantage is that these approaches are inadequate to elucidate the role of an individual function of the protein in a particular cellular process. An alternative is the use of re-engineered proteins, in which a single function is eliminated or enhanced. The use of mono-functional elements of a multi-functional protein can also yield cleaner answers. This approach requires detailed knowledge of the structural basis of each function of the protein in question. Thus, a lot of preliminary structure-function work is necessary to make it possible. However, when this information is available, replacing the protein of interest with a mutant in which individual functions are modified can shed light on the biological role of those particular functions. Here, we illustrate this point using the example of protein kinases, most of which have additional non-enzymatic functions, as well as arrestins, known multi-functional signaling regulators in the cell.

Published

2015

10. Activation of phenylalanine hydroxylase by phenylalanine does not require binding in the active site.

Author

Roberts KM, Khan CA, Hinck CS, and Fitzpatrick PF

Subjects

Allosteric Regulation, Allosteric Site, Amino Acid Substitution, Animals, Arginine chemistry, Catalytic Domain, Enzyme Activation, Kinetics, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins metabolism, Phenylalanine Hydroxylase chemistry, Phenylalanine Hydroxylase genetics, Protein Conformation, Protein Interaction Domains and Motifs, Rats, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Spectrometry, Fluorescence, Models, Molecular, Phenylalanine metabolism, Phenylalanine Hydroxylase metabolism

Abstract

Phenylalanine hydroxylase (PheH), a liver enzyme that catalyzes the hydroxylation of excess phenylalanine in the diet to tyrosine, is activated by phenylalanine. The lack of activity at low levels of phenylalanine has been attributed to the N-terminus of the protein's regulatory domain acting as an inhibitory peptide by blocking substrate access to the active site. The location of the site at which phenylalanine binds to activate the enzyme is unknown, and both the active site in the catalytic domain and a separate site in the N-terminal regulatory domain have been proposed. Binding of catecholamines to the active-site iron was used to probe the accessibility of the active site. Removal of the regulatory domain increases the rate constants for association of several catecholamines with the wild-type enzyme by ∼2-fold. Binding of phenylalanine in the active site is effectively abolished by mutating the active-site residue Arg270 to lysine. The k(cat)/K(phe) value is down 10⁴ for the mutant enzyme, and the K(m) value for phenylalanine for the mutant enzyme is >0.5 M. Incubation of the R270K enzyme with phenylalanine also results in a 2-fold increase in the rate constants for catecholamine binding. The change in the tryptophan fluorescence emission spectrum seen in the wild-type enzyme upon activation by phenylalanine is also seen with the R270K mutant enzyme in the presence of phenylalanine. Both results establish that activation of PheH by phenylalanine does not require binding of the amino acid in the active site. This is consistent with a separate allosteric site, likely in the regulatory domain.

Published

2014

11. Cystic fibrosis transmembrane conductance regulator (CFTR) potentiators protect G551D but not ΔF508 CFTR from thermal instability.

Author

Liu X and Dawson DC

Subjects

Amino Acid Substitution, Animals, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics, Cystic Fibrosis metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Female, Humans, Mutagenesis, Site-Directed, Mutant Proteins genetics, Oocytes metabolism, Protein Stability drug effects, Recombinant Proteins chemistry, Recombinant Proteins drug effects, Recombinant Proteins genetics, Temperature, Xenopus laevis, Aminophenols pharmacology, Cystic Fibrosis Transmembrane Conductance Regulator agonists, Cystic Fibrosis Transmembrane Conductance Regulator chemistry, Mutant Proteins agonists, Mutant Proteins chemistry, Quinolones pharmacology

Abstract

The G551D cystic fibrosis transmembrane conductance regulator (CFTR) mutation is associated with severe disease in ∼5% of cystic fibrosis patients worldwide. This amino acid substitution in NBD1 results in a CFTR chloride channel characterized by a severe gating defect that can be at least partially overcome in vitro by exposure to a CFTR potentiator. In contrast, the more common ΔF508 mutation is associated with a severe protein trafficking defect, as well as impaired channel function. Recent clinical trials demonstrated a beneficial effect of the CFTR potentiator, Ivacaftor (VX-770), on lung function of patients bearing at least one copy of G551D CFTR, but no comparable effect on ΔF508 homozygotes. This difference in efficacy was not surprising in view of the established difference in the molecular phenotypes of the two mutant channels. Recently, however, it was shown that the structural defect introduced by the deletion of F508 is associated with the thermal instability of ΔF508 CFTR channel function in vitro. This additional mutant phenotype raised the possibility that the differences in the behavior of ΔF508 and G551D CFTR, as well as the disparate efficacy of Ivacaftor, might be a reflection of the differing thermal stabilities of the two channels at 37 °C. We compared the thermal stability of G551D and ΔF508 CFTR in Xenopus oocytes in the presence and absence of CTFR potentiators. G551D CFTR exhibited a thermal instability that was comparable to that of ΔF508 CFTR. G551D CFTR, however, was protected from thermal instability by CFTR potentiators, whereas ΔF508 CFTR was not. These results suggest that the efficacy of VX-770 in patients bearing the G551D mutation is due, at least in part, to the ability of the small molecule to protect the mutant channel from thermal instability at human body temperature.

Published

2014

12. Mechanism of hERG channel block by the psychoactive indole alkaloid ibogaine.

Author

Thurner P, Stary-Weinzinger A, Gafar H, Gawali VS, Kudlacek O, Zezula J, Hilber K, Boehm S, Sandtner W, and Koenig X

Subjects

Amino Acid Substitution, Binding Sites drug effects, Cell Line, Cytosol metabolism, ERG1 Potassium Channel, Ether-A-Go-Go Potassium Channels chemistry, Ether-A-Go-Go Potassium Channels genetics, Ether-A-Go-Go Potassium Channels metabolism, Excitatory Amino Acid Antagonists adverse effects, Excitatory Amino Acid Antagonists chemistry, Hallucinogens adverse effects, Hallucinogens chemistry, Humans, Hydrogen-Ion Concentration, Ibogaine adverse effects, Ibogaine chemistry, Ion Channel Gating drug effects, Kinetics, Membrane Potentials drug effects, Membrane Transport Modulators pharmacology, Molecular Conformation, Molecular Docking Simulation, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Narcotic Antagonists adverse effects, Narcotic Antagonists chemistry, Nerve Tissue Proteins chemistry, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Ether-A-Go-Go Potassium Channels antagonists & inhibitors, Excitatory Amino Acid Antagonists pharmacology, Hallucinogens pharmacology, Ibogaine pharmacology, Narcotic Antagonists pharmacology, Nerve Tissue Proteins antagonists & inhibitors

Abstract

Ibogaine is a psychoactive indole alkaloid. Its use as an antiaddictive agent has been accompanied by QT prolongation and cardiac arrhythmias, which are most likely caused by human ether a go-go-related gene (hERG) potassium channel inhibition. Therefore, we studied in detail the interaction of ibogaine with hERG channels heterologously expressed in mammalian kidney tsA-201 cells. Currents through hERG channels were blocked regardless of whether ibogaine was applied via the extracellular or intracellular solution. The extent of inhibition was determined by the relative pH values. Block occurred during activation of the channels and was not observed for resting channels. With increasing depolarizations, ibogaine block grew and developed faster. Steady-state activation and inactivation of the channel were shifted to more negative potentials. Deactivation was slowed, whereas inactivation was accelerated. Mutations in the binding site reported for other hERG channel blockers (Y652A and F656A) reduced the potency of ibogaine, whereas an inactivation-deficient double mutant (G628C/S631C) was as sensitive as wild-type channels. Molecular drug docking indicated binding within the inner cavity of the channel independently of the protonation of ibogaine. Experimental current traces were fit to a kinetic model of hERG channel gating, revealing preferential binding of ibogaine to the open and inactivated state. Taken together, these findings show that ibogaine blocks hERG channels from the cytosolic side either in its charged form alone or in company with its uncharged form and alters the currents by changing the relative contribution of channel states over time.

Published

2014

13. Thromboxane receptor hyper-responsiveness in hypoxic pulmonary hypertension requires serine 324.

Author

Santhosh KT, Sikarwar AS, Hinton M, Chelikani P, and Dakshinamurti S

Subjects

Amino Acid Substitution, Animals, Animals, Newborn, Calcium Signaling drug effects, Cell Hypoxia, Cells, Cultured, Cyclic AMP-Dependent Protein Kinases antagonists & inhibitors, Cyclic AMP-Dependent Protein Kinases chemistry, Enzyme Activators pharmacology, HEK293 Cells, Humans, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins genetics, Mutant Proteins metabolism, Myocytes, Smooth Muscle drug effects, Myocytes, Smooth Muscle metabolism, Myocytes, Smooth Muscle pathology, Persistent Fetal Circulation Syndrome enzymology, Persistent Fetal Circulation Syndrome pathology, Phosphorylation drug effects, Protein Kinase Inhibitors pharmacology, Pulmonary Artery drug effects, Pulmonary Artery pathology, Receptors, Thromboxane A2, Prostaglandin H2 antagonists & inhibitors, Receptors, Thromboxane A2, Prostaglandin H2 genetics, Receptors, Thromboxane A2, Prostaglandin H2 metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Specific Pathogen-Free Organisms, Sus scrofa, Thromboxane A2 analogs & derivatives, Thromboxane A2 metabolism, Thromboxane A2 pharmacology, Cyclic AMP-Dependent Protein Kinases metabolism, Disease Models, Animal, Persistent Fetal Circulation Syndrome metabolism, Protein Processing, Post-Translational drug effects, Pulmonary Artery metabolism, Receptors, Thromboxane A2, Prostaglandin H2 agonists, Serine metabolism

Abstract

Background and Purpose: Dysregulation of the thromboxane A₂ (TP) receptor, resulting in agonist hypersensitivity and hyper-responsiveness, contributes to exaggerated vasoconstriction in the hypoxic pulmonary artery in neonatal persistent pulmonary hypertension. We previously reported that hypoxia inhibits TP receptor phosphorylation, causing desensitization. Hence, we examined the role of PKA-accessible serine residues in determining TP receptor affinity, using site-directed mutational analysis., Experimental Approach: Vasoconstriction to a thromboxane mimetic and phosphorylation of TP receptor serine was examined in pulmonary arteries from neonatal swine with persistent pulmonary hypertension and controls. Effects of hypoxia were determined in porcine and human TP receptors. Human TPα serines at positions 324, 329 and 331 (C-terminal tail) were mutated to alanine and transiently expressed in HEK293T cells. Saturation binding and displacement kinetics of a TP antagonist and agonist were determined in porcine TP, wild-type human TPα and all TP mutants. Agonist-elicited calcium mobilization was determined for each TP mutant, in the presence of a PKA activator or inhibitor, and in hypoxic and normoxic conditions., Key Results: The Ser324A mutant was insensitive to PKA activation and hypoxia, had a high affinity for agonist and increased agonist-induced calcium mobilization. Ser329A was no different from wild-type TP receptors. Ser331A was insensitive to hypoxia and PKA with a decreased agonist-mediated response., Conclusions and Implications: In hypoxic pulmonary hypertension, loss of site-specific phosphorylation of the TP receptor causes agonist hyper-responsiveness. Ser324 is the primary residue phosphorylated by PKA, which regulates TP receptor-agonist interactions. Ser331 mutation confers loss of TP receptor-agonist interaction, regardless of PKA activity., (© 2013 The British Pharmacological Society.)

Published

2014

14. Shikonin inhibits thyroid cancer cell growth and invasiveness through targeting major signaling pathways.

Author

Yang Q, Ji M, Guan H, Shi B, and Hou P

Subjects

Animals, Antineoplastic Agents, Phytogenic adverse effects, Antineoplastic Agents, Phytogenic pharmacology, Apoptosis drug effects, Cell Line, Tumor, Cell Movement drug effects, Cyclin-Dependent Kinase Inhibitor p16 metabolism, Epithelial-Mesenchymal Transition drug effects, Humans, Inhibitory Concentration 50, Liver drug effects, Liver physiopathology, Mice, Mice, Nude, Mutant Proteins agonists, Mutant Proteins metabolism, Naphthoquinones adverse effects, Naphthoquinones pharmacology, Neoplasm Invasiveness prevention & control, Neoplasm Proteins agonists, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Retinoblastoma Protein metabolism, Thyroid Neoplasms pathology, Thyroid Neoplasms physiopathology, Tumor Cells, Cultured, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Xenograft Model Antitumor Assays, Antineoplastic Agents, Phytogenic therapeutic use, Cyclin-Dependent Kinase Inhibitor p16 agonists, Naphthoquinones therapeutic use, Retinoblastoma Protein agonists, Signal Transduction drug effects, Thyroid Neoplasms drug therapy, Tumor Suppressor Protein p53 agonists

Abstract

Context: Shikonin, which is an active naphthoquinone isolated from traditional Chinese herbal medicine Zi Cao, has been recently developed to use as an antitumor agent in colorectal cancer, melanoma, leukemia, breast cancer, and hepatocellular cancer. However, its antitumor effect in thyroid cancer remains largely unknown., Objectives: The aim of the study was to test the therapeutic potential of shikonin for thyroid cancer and explore the mechanisms underlying antitumor effects of shikonin., Experimental Design: We examined the effects of shikonin on proliferation, cell cycle, apoptosis, migration, invasion, and xenograft tumor growth in thyroid cancer cells and the effect of shikonin on proliferation of primary thyroid cancer cells., Results: Shikonin inhibited thyroid cancer cell proliferation in a dose- and time-dependent manner and induced cell cycle arrest. Moreover, shikonin induced cell apoptosis through reactive oxygen species-mediated DNA damage and activation of the p53 signaling pathway. Our data also showed that shikonin dramatically inhibited thyroid cancer cell migration and invasion by suppressing epithelial-mesenchymal transition and downregulating expression of Slug and MMP-2, -9, and -14. Further elucidation of the mechanisms involved revealed that shikonin markedly repressed the phosphorylation of Erk and Akt and activated the p16/Retinoblastoma protein (Rb) pathway in thyroid cancer cells. Growth of xenograft tumors derived from the thyroid cancer cell line FTC133 in nude mice was significantly inhibited by shikonin. Importantly, we did not find the effect of shikonin on liver function in mice., Conclusion: We for the first time demonstrated that shikonin is a potentially effective antitumor agent for thyroid cancers.

Published

2013

15. Ras palmitoylation is necessary for N-Ras activation and signal propagation in growth factor signalling.

Author

Song SP, Hennig A, Schubert K, Markwart R, Schmidt P, Prior IA, Böhmer FD, and Rubio I

Subjects

Amino Acid Substitution, Animals, Cell Line, Cells, Cultured, Chlorocebus aethiops, Embryo, Mammalian cytology, Enzyme Activation, GTP Phosphohydrolases genetics, Humans, Lipoylation, Membrane Proteins agonists, Membrane Proteins genetics, Mice, Mice, Knockout, Mutant Proteins agonists, Mutant Proteins metabolism, Protein Processing, Post-Translational, Protein Transport, Recombinant Proteins agonists, Recombinant Proteins metabolism, ras Proteins genetics, Cell Membrane metabolism, Down-Regulation, Epidermal Growth Factor metabolism, GTP Phosphohydrolases metabolism, Membrane Proteins metabolism, Palmitic Acid metabolism, Signal Transduction, ras Proteins metabolism

Abstract

Ras GTPases undergo post-translational modifications that govern their subcellular trafficking and localization. In particular, palmitoylation of the Golgi tags N-Ras and H-Ras for exocytotic transport and residency at the PM (plasma membrane). Following depalmitoylation, PM-Ras redistributes to all subcellular membranes causing an accumulation of palmitate-free Ras at endomembranes, including the Golgi and endoplasmic reticulum. Palmitoylation is unanimously regarded as a critical modification at the crossroads of Ras activity and trafficking control, but its precise relevance to native wild-type Ras function in growth factor signalling is unknown. We show in the present study by use of palmitoylation-deficient N-Ras mutants and via the analysis of palmitate content of agonist-activated GTP-loaded N-Ras that only palmitoylated N-Ras becomes activated by agonists. In line with an essential role of palmitoylation in Ras activation, dominant-negative RasS17N loses its blocking potency if rendered devoid of palmitoylation. Live-cell Ras-GTP imaging shows that N-Ras activation proceeds only at the PM, consistent with activated N-Ras-GTP being palmitoylated. Finally, palmitoylation-deficient N-Ras does not sustain EGF (epidermal growth factor) or serum-elicited mitogenic signalling, confirming that palmitoylation is essential for signal transduction by N-Ras. These findings document that N-Ras activation proceeds at the PM and suggest that depalmitoylation, by removing Ras from the PM, may contribute to the shutdown of Ras signalling.

Published

2013

16. Androgens increase survival of adult-born neurons in the dentate gyrus by an androgen receptor-dependent mechanism in male rats.

Author

Hamson DK, Wainwright SR, Taylor JR, Jones BA, Watson NV, and Galea LA

Subjects

Androgen Antagonists toxicity, Androgen-Insensitivity Syndrome chemically induced, Androgen-Insensitivity Syndrome drug therapy, Androgen-Insensitivity Syndrome metabolism, Androgens chemistry, Androgens pharmacology, Androgens therapeutic use, Animals, Biomarkers metabolism, Castration adverse effects, Cell Survival drug effects, Dentate Gyrus cytology, Dentate Gyrus drug effects, Dentate Gyrus pathology, Doublecortin Domain Proteins, Doublecortin Protein, Drug Resistance, Hormone Replacement Therapy, Male, Microtubule-Associated Proteins metabolism, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins metabolism, Neural Stem Cells cytology, Neural Stem Cells drug effects, Neural Stem Cells metabolism, Neural Stem Cells pathology, Neurons cytology, Neurons drug effects, Neurons pathology, Neuropeptides metabolism, Neuroprotective Agents antagonists & inhibitors, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Rats, Rats, Sprague-Dawley, Receptors, Androgen chemistry, Receptors, Androgen genetics, Testosterone Propionate antagonists & inhibitors, Testosterone Propionate pharmacology, Testosterone Propionate therapeutic use, Androgens metabolism, Dentate Gyrus metabolism, Neurogenesis drug effects, Neurons metabolism, Neuroprotective Agents metabolism, Receptors, Androgen metabolism, Signal Transduction drug effects

Abstract

Gonadal steroids are potent regulators of adult neurogenesis. We previously reported that androgens, such as testosterone (T) and dihydrotestosterone (DHT), but not estradiol, increased the survival of new neurons in the dentate gyrus of the male rat. These results suggest androgens regulate hippocampal neurogenesis via the androgen receptor (AR). To test this supposition, we examined the role of ARs in hippocampal neurogenesis using 2 different approaches. In experiment 1, we examined neurogenesis in male rats insensitive to androgens due to a naturally occurring mutation in the gene encoding the AR (termed testicular feminization mutation) compared with wild-type males. In experiment 2, we injected the AR antagonist, flutamide, into castrated male rats and compared neurogenesis levels in the dentate gyrus of DHT and oil-treated controls. In experiment 1, chronic T increased hippocampal neurogenesis in wild-type males but not in androgen-insensitive testicular feminization mutation males. In experiment 2, DHT increased hippocampal neurogenesis via cell survival, an effect that was blocked by concurrent treatment with flutamide. DHT, however, did not affect cell proliferation. Interestingly, cells expressing doublecortin, a marker of immature neurons, did not colabel with ARs in the dentate gyrus, but ARs were robustly expressed in other regions of the hippocampus. Together these studies provide complementary evidence that androgens regulate adult neurogenesis in the hippocampus via the AR but at a site other than the dentate gyrus. Understanding where in the brain androgens act to increase the survival of new neurons in the adult brain may have implications for neurodegenerative disorders.

Published

2013

17. Flavanoids induce expression of the suppressor of cytokine signalling 3 (SOCS3) gene and suppress IL-6-activated signal transducer and activator of transcription 3 (STAT3) activation in vascular endothelial cells.

Author

Wiejak J, Dunlop J, Mackay SP, and Yarwood SJ

Subjects

AMP-Activated Protein Kinases antagonists & inhibitors, AMP-Activated Protein Kinases metabolism, Animals, Anti-Inflammatory Agents, Non-Steroidal antagonists & inhibitors, Cell Line, Cells, Cultured, Chlorocebus aethiops, Cytokine Receptor gp130 metabolism, Endothelium, Vascular cytology, Endothelium, Vascular drug effects, Flavonoids antagonists & inhibitors, Gene Expression Regulation drug effects, Human Umbilical Vein Endothelial Cells cytology, Human Umbilical Vein Endothelial Cells drug effects, Human Umbilical Vein Endothelial Cells metabolism, Humans, Interleukin-6 metabolism, Interleukin-6 Receptor alpha Subunit metabolism, Mice, Mutant Proteins agonists, Mutant Proteins metabolism, Promoter Regions, Genetic drug effects, Protein Kinase Inhibitors pharmacology, Recombinant Proteins agonists, Recombinant Proteins metabolism, STAT3 Transcription Factor metabolism, Signal Transduction drug effects, Suppressor of Cytokine Signaling 3 Protein, Suppressor of Cytokine Signaling Proteins genetics, Suppressor of Cytokine Signaling Proteins metabolism, Anti-Inflammatory Agents, Non-Steroidal metabolism, Cytokine Receptor gp130 antagonists & inhibitors, Endothelium, Vascular metabolism, Flavonoids metabolism, Interleukin-6 antagonists & inhibitors, STAT3 Transcription Factor antagonists & inhibitors, Suppressor of Cytokine Signaling Proteins agonists

Abstract

The atherogenic cytokine IL-6 (interleukin-6) induces pro-inflammatory gene expression in VECs (vascular endothelial cells) by activating the JAK (Janus kinase)/STAT3 (signal transducer and activator of transcription 3) signalling pathway, which is normally down-regulated by the STAT3-dependent induction of the E3 ubiquitin ligase component SOCS3 (suppressor of cytokine signalling 3). Novel treatments based on the regulation of SOCS3 protein levels could therefore have value in the treatment of diseases with an inflammatory component, such as atherosclerosis. To this end we carried out a screen of 1031 existing medicinal compounds to identify inducers of SOCS3 gene expression and identified the flavanoids naringenin and flavone as effective inducers of SOCS3 protein, mRNA and promoter activity. This was in contrast with the action of traditional JAK/STAT3 inhibitors and the polyphenol resveratrol, which effectively suppress SOCS3 gene expression. Both naringenin and flavone also effectively suppressed IL-6-stimulated phosphorylation of STAT3 (Tyr⁷⁰⁵) which led to suppression of IL-6-induction of the atherogenic STAT3 target gene MCP1 (monocyte chemotactic protein-1), suggesting that their ability to induce SOCS3 gene expression is STAT3-independent. Supporting this idea was the observation that the general kinase inhibitor compound C inhibits flavone- and cAMP-dependent, but not JAK-dependent, SOCS3 induction in VECs. Indeed, the ability of flavanoids to induce SOCS3 expression requires activation of the ERK (extracellular-signal-regulated kinase)-dependent transcription factor SP3, and not STAT3. In the present paper we therefore describe novel molecular actions of flavanoids, which control SOCS3 gene induction and suppression of STAT3 signalling in VECs. These mechanisms could potentially be exploited to develop novel anti-atherogenic therapies.

Published

2013

18. S100A11 is involved in the regulation of the stability of cell cycle regulator p21(CIP1/WAF1) in human keratinocyte HaCaT cells.

Author

Foertsch F, Teichmann N, Kob R, Hentschel J, Laubscher U, and Melle C

Subjects

Apoptosis drug effects, Cell Line, Cyclin-Dependent Kinase Inhibitor p21 agonists, Cyclin-Dependent Kinase Inhibitor p21 antagonists & inhibitors, Cyclin-Dependent Kinase Inhibitor p21 genetics, Gene Silencing, Glycogen Synthase Kinase 3 antagonists & inhibitors, Glycogen Synthase Kinase 3 chemistry, Glycogen Synthase Kinase 3 genetics, Glycogen Synthase Kinase 3 metabolism, Humans, Keratinocytes drug effects, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins metabolism, Phosphatidylinositol 3-Kinase metabolism, Phosphorylation drug effects, Proteasome Endopeptidase Complex chemistry, Proteasome Endopeptidase Complex metabolism, Proteasome Inhibitors pharmacology, Protein Kinase Inhibitors pharmacology, Protein Processing, Post-Translational drug effects, Protein Stability drug effects, Proto-Oncogene Proteins c-akt metabolism, Recombinant Proteins agonists, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins metabolism, S100 Proteins antagonists & inhibitors, S100 Proteins genetics, Signal Transduction drug effects, Cyclin-Dependent Kinase Inhibitor p21 metabolism, Down-Regulation drug effects, Keratinocytes metabolism, S100 Proteins metabolism, Up-Regulation drug effects

Abstract

The cyclin-dependent kinase inhibitor p21(CIP1/WAF1) is a regulatory factor of the cell cycle. Its transcriptional activation and protein stability are tightly controlled by several distinct mechanisms. S100A11 is a member of the S100 family of Ca²⁺-binding proteins involved in several biological processes, including cell cycle progression and signal transduction. In the present study, we show that down-regulation of S100A11 results in the reduction of p21 protein in human HaCaT keratinocytes. It appears that a ubiquitin-independent proteasomal degradation process is involved in p21 degradation in S100A11 down-regulated cells. The application of a proteasome inhibitor stabilized p21 protein in these cells. Analysis of distinct signal transduction pathways revealed a disturbed phosphatidylinositol-3-kinase/Akt pathway after S100A11 knockdown. We determined that the glycogen synthase kinase-3, which is negatively regulated by phosphatidylinositol 3-kinase/Akt, was activated in cells possessing knocked-down S100A11 and appears to be involved in p21 protein destabilization. The application of a specific inhibitor of glycogen synthase kinase 3 resulted in an increase of the p21 protein level in S100A11 down-regulated HaCaT cells. Glycogen synthase kinase 3 is able to phosphorylate p21 at T57, which induces p21 proteasomal turnover. Mutation of the glycogen synthase kinase 3 site threonine 57 into alanine (T57A) stabilizes p21 in HaCaT cells lacking S100A11. Beside decreased p21 protein, down-regulation of S100A11 triggered the induction of apoptosis in HaCaT cells. These observations suggest that S100A11 is involved in the maintenance of p21 protein stability and appears to function as an inhibitor of apoptosis in human HaCaT keratinocyte cells. Thus, the data shed light on a novel pathway regulating p21 protein stability., (© 2013 FEBS.)

Published

2013

19. Molecular basis for benzodiazepine agonist action at the type 1 cholecystokinin receptor.

Author

Harikumar KG, Cawston EE, Lam PCH, Patil A, Orry A, Henke BR, Abagyan R, Christopoulos A, Sexton PM, and Miller LJ

Subjects

Amino Acid Sequence, Animals, Benzodiazepines chemistry, CHO Cells, Cricetinae, Cricetulus, Models, Molecular, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins metabolism, ROC Curve, Receptor, Cholecystokinin A chemistry, Receptor, Cholecystokinin A metabolism, Receptor, Cholecystokinin B chemistry, Receptor, Cholecystokinin B metabolism, Recombinant Proteins agonists, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Sequence Alignment, Benzodiazepines pharmacology, Receptor, Cholecystokinin A agonists

Abstract

Understanding the molecular basis of drug action can facilitate development of more potent and selective drugs. Here, we explore the molecular basis for action of a unique small molecule ligand that is a type 1 cholecystokinin (CCK) receptor agonist and type 2 CCK receptor antagonist, GI181771X. We characterize its binding utilizing structurally related radioiodinated ligands selective for CCK receptor subtypes that utilize the same allosteric ligand-binding pocket, using wild-type receptors and chimeric constructs exchanging the distinct residues lining this pocket. Intracellular calcium assays were performed to determine biological activity. Molecular models for docking small molecule agonists to the type 1 CCK receptor were developed using a ligand-guided refinement approach. The optimal model was distinct from the previous antagonist model for the same receptor and was mechanistically consistent with the current mutagenesis data. This study revealed a key role for Leu(7.39) that was predicted to interact with the isopropyl group in the N1 position of the benzodiazepine that acts as a "trigger" for biological activity. The molecular model was predictive of binding of other small molecule agonists, effectively distinguishing these from 1065 approved drug decoys with an area under curve value of 99%. The model also selectively enriched for agonist compounds, with 130 agonists identified by ROC analysis when seeded in 2175 non-agonist ligands of the type 1 CCK receptor (area under curve 78%). Benzodiazepine agonists in this series docked in consistent pose within this pocket, with a key role played by Leu(7.39), whereas the role of this residue was less clear for chemically distinct agonists.

Published

2013

20. Impact of clinically relevant mutations on the pharmacoregulation and signaling bias of the calcium-sensing receptor by positive and negative allosteric modulators.

Author

Leach K, Wen A, Cook AE, Sexton PM, Conigrave AD, and Christopoulos A

Subjects

Allosteric Regulation, Amino Acid Substitution, Calcium Signaling drug effects, Cinacalcet, Extracellular Signal-Regulated MAP Kinases metabolism, HEK293 Cells, Humans, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins genetics, Mutant Proteins metabolism, Naphthalenes pharmacology, Receptors, Calcium-Sensing agonists, Receptors, Calcium-Sensing antagonists & inhibitors, Recombinant Proteins agonists, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins genetics, Recombinant Proteins metabolism, Mutation, Receptors, Calcium-Sensing genetics, Receptors, Calcium-Sensing metabolism

Abstract

Cinacalcet is predominantly used to treat secondary hyperparathyroidism due to end-stage renal failure, but, more recently, its potential clinical efficacy in treating patients with loss-of-function mutations in the calcium-sensing receptor (CaSR) has been recognized. Many clinically relevant CaSR mutations are located in the heptahelical membrane spanning and extracellular loop regions of the receptor, where allosteric modulators are predicted to bind. The aim of the present study was to investigate the impact of such mutations on the pharmacoregulation of the CaSR by the positive and negative allosteric modulators, cinacalcet and NPS-2143, respectively. Both cinacalcet and NPS-2143 effectively rescued mutants whose cell surface expression was substantially impaired, suggesting that both classes of drug can stabilize a receptor conformation that is trafficked more effectively to the cell surface. In addition, functional impairments in almost all mutant CaSRs were rescued by either cinacalcet or NPS-2143 via restoration of intracellular signaling. There was a significantly greater ability of both compounds to modulate agonist-stimulated intracellular Ca(2+) mobilization than ERK1/2 phosphorylation, indicating that the allosteric modulators engender bias in agonist-stimulated CaSR signaling to different pathways. Three mutations (G(670)R, P(748)R, and L(773)R) altered the binding affinity of allosteric modulators to the CaSR, and 3 mutations (V(817)I, L(773)R, and E(767)K) altered the cooperativity between the allosteric modulator and Ca(2+)(o). These findings have important implications for the treatment of diseases associated with CaSR mutations using allosteric CaSR modulators and for analyzing the effects of mutations on the function and pharmacoregulation of the CaSR.

Published

2013

21. The crystal structure of the cysteine protease Xylellain from Xylella fastidiosa reveals an intriguing activation mechanism.

Author

Leite NR, Faro AR, Dotta MA, Faim LM, Gianotti A, Silva FH, Oliva G, and Thiemann OH

Subjects

Amino Acid Substitution, Bacterial Proteins agonists, Bacterial Proteins genetics, Bacterial Proteins metabolism, Biocatalysis, Catalytic Domain, Crystallography, X-Ray, Cysteine Proteases genetics, Cysteine Proteases metabolism, Cysteine Proteinase Inhibitors pharmacology, Enzyme Activation, Kinetics, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Point Mutation, Protein Folding, Protein Structure, Quaternary, Recombinant Proteins agonists, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Uridine Diphosphate chemistry, Uridine Diphosphate metabolism, Bacterial Proteins chemistry, Cysteine Proteases chemistry, Models, Molecular, Xylella enzymology

Abstract

Xylella fastidiosa is responsible for a wide range of economically important plant diseases. We report here the crystal structure and kinetic data of Xylellain, the first cysteine protease characterized from the genome of the pathogenic X. fastidiosa strain 9a5c. Xylellain has a papain-family fold, and part of the N-terminal sequence blocks the enzyme active site, thereby mediating protein activity. One novel feature identified in the structure is the presence of a ribonucleotide bound outside the active site. We show that this ribonucleotide plays an important regulatory role in Xylellain enzyme kinetics, possibly functioning as a physiological mediator., (Copyright © 2013 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2013

22. EphrinA2 regulates clathrin mediated KSHV endocytosis in fibroblast cells by coordinating integrin-associated signaling and c-Cbl directed polyubiquitination.

Author

Dutta D, Chakraborty S, Bandyopadhyay C, Valiya Veettil M, Ansari MA, Singh VV, and Chandran B

Subjects

Cells, Cultured, Ephrin-A2 agonists, Ephrin-A2 antagonists & inhibitors, Ephrin-A2 genetics, Fibroblasts cytology, Fibroblasts metabolism, Gene Expression Regulation, Viral, HEK293 Cells, Humans, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Phosphorylation, Protein Interaction Domains and Motifs, Protein Processing, Post-Translational, RNA Interference, RNA, Small Interfering, Signal Transduction, Ubiquitination, Up-Regulation, Viral Proteins biosynthesis, Viral Proteins genetics, Viral Proteins metabolism, Virus Internalization, Clathrin-Coated Vesicles metabolism, Endocytosis, Ephrin-A2 metabolism, Fibroblasts virology, Herpesvirus 8, Human physiology, Integrins metabolism, Proto-Oncogene Proteins c-cbl metabolism

Abstract

Kaposi's sarcoma-associated herpesvirus (KSHV) interacts with human dermal endothelial cell surface tyrosine kinase EphrinA2 (EphA2) and integrins (α3β1 and αVβ3) in the lipid raft (LR) region, and EphA2 regulates macropinocytic virus entry by coordinating integrin-c-Cbl associated signaling. In contrast, KSHV enters human foreskin fibroblast (HFF) cells by LR-independent clathrin mediated endocytosis. The present studies conducted to identify the key molecules regulating KSHV entry in HFF cells showed that KSHV induces association with integrins (αVβ5, αVβ3 and α3β1) and EphA2 in non-LR regions early during infection and activates EphA2, which in turn associates with phosphorylated c-Cbl, myosin IIA, FAK, Src, and PI3-K, as well as clathrin and its adaptor AP2 and effector Epsin-15 proteins. EphA2 knockdown significantly reduced these signal inductions, virus internalization and gene expression. c-Cbl knockdown ablated the c-Cbl mediated K63 type polyubiquitination of EphA2 and clathrin association with EphA2 and KSHV. Mutations in EphA2's tyrosine kinase domain (TKD) or sterile alpha motif (SAM) abolished its interaction with c-Cbl. Mutations in tyrosine kinase binding (TKB) or RING finger (RF) domains of c-Cbl resulted in very poor association of c-Cbl with EphA2 and decreased EphA2 polyubiquitination. These studies demonstrated the contributions of these domains in EphA2 and c-Cbl association, EphA2 polyubiquitination and virus-EphA2 internalization. Collectively, these results revealed for the first time that EphA2 influences the tyrosine phosphorylation of clathrin, the role of EphA2 in clathrin mediated endocytosis of a virus, and c-Cbl mediated EphA2 polyubiquitination directing KSHV entry in HFF cells via coordinated signal induction and progression of endocytic events, all of which suggest that targeting EphA2 and c-Cbl could block KSHV entry and infection.

Published

2013

23. Role of matrix metalloproteinase-10 in the BMP-2 inducing osteoblastic differentiation.

Author

Mao L, Yano M, Kawao N, Tamura Y, Okada K, and Kaji H

Subjects

Activin Receptors, Type I genetics, Activin Receptors, Type I metabolism, Amino Acid Substitution, Animals, Bone Morphogenetic Protein 2 agonists, Bone Morphogenetic Protein 2 genetics, Bone Morphogenetic Protein Receptors, Type I genetics, Bone Morphogenetic Protein Receptors, Type I metabolism, Cell Line, Collagen Type I agonists, Collagen Type I genetics, Collagen Type I metabolism, Humans, Matrix Metalloproteinase 10 chemistry, Matrix Metalloproteinase 10 genetics, Mice, Mutant Proteins agonists, Mutant Proteins metabolism, Myoblasts cytology, Myoblasts enzymology, Myoblasts metabolism, Osteoblasts enzymology, Osteoblasts metabolism, Osteocalcin agonists, Osteocalcin genetics, Osteocalcin metabolism, RNA Interference, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Smad6 Protein agonists, Smad6 Protein genetics, Smad6 Protein metabolism, Smad7 Protein agonists, Smad7 Protein genetics, Smad7 Protein metabolism, Sp7 Transcription Factor, Transcription Factors agonists, Transcription Factors genetics, Transcription Factors metabolism, Bone Morphogenetic Protein 2 metabolism, Cell Differentiation, Gene Expression Regulation, Enzymologic, Matrix Metalloproteinase 10 metabolism, Osteoblasts cytology, Signal Transduction

Abstract

Fibrodysplasia ossificans progressiva (FOP) is a skeletal disorder with progressive heterotopic ossification in skeletal muscle. A mutation causing constitutive activation in a bone morphogenetic protein (BMP) type 1 receptor [ALK2(R206H)] is found in most patients with FOP. However, the details in the heterotopic ossification of muscle in FOP and the role of matrix metalloproteinase-10 (MMP-10) in bone remain to be fully elucidated. In the present study, we investigated the role of MMP-10 in the differentiation of mouse myoblastic C2C12 cells into osteoblasts. MMP-10 was extracted as a factor, whose expression was most extensively enhanced by ALK2 (R206H) transfection in C2C12 cells. MMP-10 significantly augmented the levels of Osterix, type 1 collagen, alkaline phosphatase (ALP) and osteocalcin mRNA as well as ALP activity enhanced by BMP-2 in C2C12 cells. Moreover, a reduction in endogenous MMP-10 levels by siRNA significantly decreased the levels of Runx2, Osterix, type 1 collagen, ALP and osteocalcin mRNA enhanced by BMP-2 in these cells. In addition, MMP-10 increased the phosphorylation of Smad1/5/8 as well as enhanced the levels of Smad6 and Smad7 mRNA induced by BMP-2. In conclusion, the present study first demonstrated that MMP-10 promotes the differentiation of myoblasts into osteoblasts by interacting with the BMP signaling pathway. MMP-10 may play some important role in the heterotopic ossification of muscle in FOP.

Published

2013

24. Structural basis for native agonist and synthetic inhibitor recognition by the Pseudomonas aeruginosa quorum sensing regulator PqsR (MvfR).

Author

Ilangovan A, Fletcher M, Rampioni G, Pustelny C, Rumbaugh K, Heeb S, Cámara M, Truman A, Chhabra SR, Emsley J, and Williams P

Subjects

Alkylation, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents metabolism, Anti-Bacterial Agents pharmacology, Bacterial Proteins agonists, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins chemistry, Binding Sites, Biofilms drug effects, Drug Design, Gene Expression Regulation, Bacterial, Ligands, Molecular Conformation, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Peptide Fragments agonists, Peptide Fragments antagonists & inhibitors, Peptide Fragments chemistry, Peptide Fragments metabolism, Protein Interaction Domains and Motifs, Pseudomonas aeruginosa drug effects, Pseudomonas aeruginosa pathogenicity, Quinolones chemistry, Quinolones pharmacology, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Structure-Activity Relationship, Transcription Factors agonists, Transcription Factors antagonists & inhibitors, Transcription Factors chemistry, Virulence drug effects, Bacterial Proteins metabolism, Pseudomonas aeruginosa physiology, Quinolones metabolism, Quorum Sensing drug effects, Signal Transduction drug effects, Transcription Factors metabolism

Abstract

Bacterial populations co-ordinate gene expression collectively through quorum sensing (QS), a cell-to-cell communication mechanism employing diffusible signal molecules. The LysR-type transcriptional regulator (LTTR) protein PqsR (MvfR) is a key component of alkyl-quinolone (AQ)-dependent QS in Pseudomonas aeruginosa. PqsR is activated by 2-alkyl-4-quinolones including the Pseudomonas quinolone signal (PQS; 2-heptyl-3-hydroxy-4(1H)-quinolone), its precursor 2-heptyl-4-hydroxyquinoline (HHQ) and their C9 congeners, 2-nonyl-3-hydroxy-4(1H)-quinolone (C9-PQS) and 2-nonyl-4-hydroxyquinoline (NHQ). These drive the autoinduction of AQ biosynthesis and the up-regulation of key virulence determinants as a function of bacterial population density. Consequently, PqsR constitutes a potential target for novel antibacterial agents which attenuate infection through the blockade of virulence. Here we present the crystal structures of the PqsR co-inducer binding domain (CBD) and a complex with the native agonist NHQ. We show that the structure of the PqsR CBD has an unusually large ligand-binding pocket in which a native AQ agonist is stabilized entirely by hydrophobic interactions. Through a ligand-based design strategy we synthesized and evaluated a series of 50 AQ and novel quinazolinone (QZN) analogues and measured the impact on AQ biosynthesis, virulence gene expression and biofilm development. The simple exchange of two isosteres (OH for NH₂) switches a QZN agonist to an antagonist with a concomitant impact on the induction of bacterial virulence factor production. We also determined the complex crystal structure of a QZN antagonist bound to PqsR revealing a similar orientation in the ligand binding pocket to the native agonist NHQ. This structure represents the first description of an LTTR-antagonist complex. Overall these studies present novel insights into LTTR ligand binding and ligand-based drug design and provide a chemical scaffold for further anti-P. aeruginosa virulence drug development by targeting the AQ receptor PqsR.

Published

2013

25. Functions of the third intracellular loop of the human melanocortin-3 receptor.

Author

Wang ZQ and Tao YX

Subjects

Affinity Labels metabolism, Amino Acid Substitution, HEK293 Cells, Humans, Kinetics, Ligands, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins metabolism, Protein Interaction Domains and Motifs, Protein Structure, Tertiary, Radioligand Assay, Receptor, Melanocortin, Type 3 agonists, Receptor, Melanocortin, Type 3 chemistry, Receptor, Melanocortin, Type 3 genetics, Recombinant Proteins chemistry, Recombinant Proteins metabolism, alpha-MSH analogs & derivatives, Receptor, Melanocortin, Type 3 metabolism, Signal Transduction, alpha-MSH metabolism

Abstract

The melanocortin-3 receptor (MC3R) is a G protein-coupled receptor involved in regulating energy metabolism, cardiovascular function, and inflammation. To gain a better understanding of the structure-function relationship of the MC3R, we used alanine-scanning mutagenesis to investigate the functions of residues 247-273 in the third intracellular loop (ICL3) of the human MC3R (hMC3R). Ligand binding and signaling parameters of the mutants were measured. The results showed that six mutants at the N terminus of ICL3 had decreased receptor occupancy (an estimate of relative binding capacity) whereas six mutants at the C terminus of ICL3 had increased receptor occupancy. M247A, R252A, H254A, and K256A had decreased maximal responses (M247A also had increased EC50) whereas F250A, P262A, and H272A had increased maximal responses. None of the mutants was constitutively active. The binding and signaling properties of the other mutants were not significantly different from that of the wild type hMC3R. In summary, we presented detailed functional data on the functions of the residues in ICL3 of hMC3R, providing important constraints for modeling ligand binding and G protein coupling/activation in the hMC3R.

Published

2013

26. The pharmacological profile of ELIC, a prokaryotic GABA-gated receptor.

Author

Thompson AJ, Alqazzaz M, Ulens C, and Lummis SC

Subjects

Amino Acid Sequence, Animals, Bacterial Proteins agonists, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins metabolism, Cells, Cultured, Computer Simulation, Databases, Protein, Female, Kinetics, Ligand-Gated Ion Channels agonists, Ligand-Gated Ion Channels antagonists & inhibitors, Ligand-Gated Ion Channels metabolism, Ligands, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Patch-Clamp Techniques, Protein Binding, Protein Conformation, Recombinant Proteins agonists, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Sequence Alignment, Xenopus laevis, Bacterial Proteins chemistry, Erwinia metabolism, GABA Agonists pharmacology, GABA Antagonists pharmacology, Ligand-Gated Ion Channels chemistry, gamma-Aminobutyric Acid metabolism

Abstract

The Erwinia ligand-gated ion channel (ELIC) is a bacterial homologue of vertebrate Cys-loop ligand-gated ion channels. It is activated by GABA, and this property, combined with its structural similarity to GABA(A) and other Cys-loop receptors, makes it potentially an excellent model to probe their structure and function. Here we characterise the pharmacological profile of ELIC, examining the effects of compounds that could activate or inhibit the receptor. We confirm that a range of amino acids and classic GABA(A) receptor agonists do not elicit responses in ELIC, and we show the receptor can be at least partially activated by 5-aminovaleric acid and γ-hydroxybutyric acid, which are weak agonists. A range of GABA(A) receptor non-competitive antagonists inhibit GABA-elicited ELIC responses including α-endosulfan (IC₅₀ = 17 μM), dieldrin (IC₅₀ = 66 μM), and picrotoxinin (IC₅₀ = 96 μM) which were the most potent. Docking suggested possible interactions at the 2' and 6' pore-lining residues, and mutagenesis of these residues supports this hypothesis for α-endosulfan. A selection of compounds that act at Cys-loop and other receptors also showed some efficacy at blocking ELIC responses, but most were of low potency (IC₅₀ > 100 μM). Overall our data show that a number of compounds can inhibit ELIC, but it has limited pharmacological similarity to GLIC and to Cys-loop receptors., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

27. Use of an α3β4 nicotinic acetylcholine receptor subunit concatamer to characterize ganglionic receptor subtypes with specific subunit composition reveals species-specific pharmacologic properties.

Author

Stokes C and Papke RL

Subjects

Acetylcholine agonists, Acetylcholine antagonists & inhibitors, Alkaloids metabolism, Alkaloids pharmacology, Animals, Azocines metabolism, Azocines pharmacology, Benzazepines metabolism, Benzazepines pharmacology, Drug Partial Agonism, Evoked Potentials drug effects, Humans, Ligands, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins genetics, Mutant Proteins metabolism, Nerve Tissue Proteins agonists, Nerve Tissue Proteins antagonists & inhibitors, Nerve Tissue Proteins genetics, Nicotine agonists, Nicotine antagonists & inhibitors, Nicotine metabolism, Nicotinic Agonists pharmacology, Nicotinic Antagonists pharmacology, Oocytes drug effects, Oocytes metabolism, Protein Subunits agonists, Protein Subunits antagonists & inhibitors, Protein Subunits genetics, Quinolizines metabolism, Quinolizines pharmacology, Quinoxalines metabolism, Quinoxalines pharmacology, Rats, Receptors, Nicotinic chemistry, Receptors, Nicotinic genetics, Recombinant Fusion Proteins agonists, Recombinant Fusion Proteins antagonists & inhibitors, Recombinant Fusion Proteins metabolism, Species Specificity, Varenicline, Xenopus laevis, Acetylcholine metabolism, Ganglia metabolism, Nerve Tissue Proteins metabolism, Nicotinic Agonists metabolism, Nicotinic Antagonists metabolism, Protein Subunits metabolism, Receptors, Nicotinic metabolism

Abstract

Drug development for nicotinic acetylcholine receptors (nAChR) is challenged by subtype diversity arising from variations in subunit composition. On-target activity for neuronal heteromeric receptors is typically associated with CNS receptors that contain α4 and other subunits, while off-target activity could be associated with ganglionic-type receptors containing α3β4 binding sites and other subunits, including β4, β2, α5, or α3 as a structural subunit in the pentamer. Additional interest in α3 β4 α5-containing receptors arises from genome-wide association studies linking these genes, and a single nucleotide polymorphism (SNP) in α5 in particular, to lung cancer and heavy smoking. While α3 and β4 readily form receptors in expression system such as the Xenopus oocyte, since α5 is not required for function, simple co-expression approaches may under-represent α5-containing receptors. We used a concatamer of human α3 and β4 subunits to form ligand-binding domains, and show that we can force the insertions of alternative structural subunits into the functional pentamers. These α3β4 variants differ in sensitivity to ACh, nicotine, varenicline, and cytisine. Our data indicated lower efficacy for varenicline and cytisine than expected for β4-containing receptors, based on previous studies of rodent receptors. We confirm that these therapeutically important α4 receptor partial agonists may present different autonomic-based side-effect profiles in humans than will be seen in rodent models, with varenicline being more potent for human than rat receptors and cytisine less potent. Our initial characterizations failed to find functional effects of the α5 SNP. However, our data validate this approach for further investigations., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

28. Site-directed mutations and the polymorphic variant Ala160Thr in the human thromboxane receptor uncover a structural role for transmembrane helix 4.

Author

Chakraborty R, Pydi SP, Gleim S, Dakshinamurti S, Hwa J, and Chelikani P

Subjects

15-Hydroxy-11 alpha,9 alpha-(epoxymethano)prosta-5,13-dienoic Acid metabolism, 15-Hydroxy-11 alpha,9 alpha-(epoxymethano)prosta-5,13-dienoic Acid pharmacology, Alanine chemistry, Alanine genetics, Alanine metabolism, Amino Acid Sequence, Animals, Binding Sites genetics, Binding, Competitive, Bridged Bicyclo Compounds, Heterocyclic, COS Cells, Calcium metabolism, Chlorocebus aethiops, Fatty Acids, Unsaturated, Glycine chemistry, Glycine genetics, Glycine metabolism, HEK293 Cells, Humans, Hydrazines metabolism, Hydrazines pharmacology, Microscopy, Fluorescence, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins metabolism, Polymorphism, Single Nucleotide, Radioligand Assay, Receptors, Thromboxane A2, Prostaglandin H2 metabolism, Structure-Activity Relationship, Temperature, Mutation, Missense, Protein Structure, Secondary, Receptors, Thromboxane A2, Prostaglandin H2 chemistry, Receptors, Thromboxane A2, Prostaglandin H2 genetics

Abstract

The human thromboxane A2 receptor (TP), belongs to the prostanoid subfamily of Class A GPCRs and mediates vasoconstriction and promotes thrombosis on binding to thromboxane (TXA2). In Class A GPCRs, transmembrane (TM) helix 4 appears to be a hot spot for non-synonymous single nucleotide polymorphic (nsSNP) variants. Interestingly, A160T is a novel nsSNP variant with unknown structure and function. Additionally, within this helix in TP, Ala160(4.53) is highly conserved as is Gly164(4.57). Here we target Ala160(4.53) and Gly164(4.57) in the TP for detailed structure-function analysis. Amino acid replacements with smaller residues, A160S and G164A mutants, were tolerated, while bulkier beta-branched replacements, A160T and A160V showed a significant decrease in receptor expression (Bmax). The nsSNP variant A160T displayed significant agonist-independent activity (constitutive activity). Guided by molecular modeling, a series of compensatory mutations were made on TM3, in order to accommodate the bulkier replacements on TM4. The A160V/F115A double mutant showed a moderate increase in expression level compared to either A160V or F115A single mutants. Thermal activity assays showed decrease in receptor stability in the order, wild type>A160S>A160V>A160T>G164A, with G164A being the least stable. Our study reveals that Ala160(4.53) and Gly164(4.57) in the TP play critical structural roles in packing of TM3 and TM4 helices. Naturally occurring mutations in conjunction with site-directed replacements can serve as powerful tools in assessing the importance of regional helix-helix interactions.

Published

2012

29. Activation of G-protein-coupled receptors and thyroid malignant tumors: the jury is still out.

Author

Gagel RF

Subjects

Animals, Bone Density Conservation Agents adverse effects, Bone Density Conservation Agents pharmacology, Carcinoma, Neuroendocrine, Drug Approval, Drugs, Investigational pharmacology, Evidence-Based Medicine, Glucagon-Like Peptide 1 adverse effects, Glucagon-Like Peptide 1 analogs & derivatives, Glucagon-Like Peptide 1 pharmacology, Glucagon-Like Peptide-1 Receptor, Humans, Hypoglycemic Agents adverse effects, Hypoglycemic Agents pharmacology, Liraglutide, Mutant Proteins agonists, Mutant Proteins metabolism, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Osteosarcoma chemically induced, Osteosarcoma metabolism, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled metabolism, Receptors, Glucagon agonists, Receptors, Glucagon genetics, Receptors, Glucagon metabolism, Teriparatide adverse effects, Teriparatide pharmacology, Thyroid Gland metabolism, Thyroid Neoplasms metabolism, United States, United States Food and Drug Administration, Drugs, Investigational adverse effects, Neoplasm Proteins agonists, Receptors, G-Protein-Coupled agonists, Thyroid Gland drug effects, Thyroid Neoplasms chemically induced

Published

2011

30. Mutation-specific cystic fibrosis treatments on verge of approval.

Author

Dolgin E

Subjects

Aminophenols therapeutic use, Cystic Fibrosis Transmembrane Conductance Regulator agonists, Cystic Fibrosis Transmembrane Conductance Regulator chemistry, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Drug Approval, Drug Discovery, Humans, Models, Molecular, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins genetics, Mutation, Quinolones therapeutic use, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics

Published

2011

31. Orphan cystic fibrosis drugs find sister diseases.

Author

Dolgin E

Subjects

Aminophenols therapeutic use, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator agonists, Cystic Fibrosis Transmembrane Conductance Regulator antagonists & inhibitors, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Drug Discovery, Humans, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins genetics, Quinolones therapeutic use, Cystic Fibrosis drug therapy, Orphan Drug Production

Published

2011

32. Reactivation of p53: from peptides to small molecules.

Author

Brown CJ, Cheok CF, Verma CS, and Lane DP

Subjects

ADP-Ribosylation Factors metabolism, Animals, Antineoplastic Agents chemistry, Cell Cycle Proteins, Drug Design, Humans, Molecular Conformation, Molecular Mimicry, Mutant Proteins agonists, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins metabolism, Peptides chemistry, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Proto-Oncogene Proteins c-mdm2 metabolism, Tumor Suppressor Protein p53 chemistry, Tumor Suppressor Protein p53 genetics, Ubiquitin-Protein Ligases antagonists & inhibitors, Ubiquitin-Protein Ligases metabolism, Antineoplastic Agents pharmacology, Peptides pharmacology, Tumor Suppressor Protein p53 agonists, Tumor Suppressor Protein p53 metabolism

Abstract

Approximately 27 million people are living with a tumour in which the tumour suppressing activity of p53 has been inactivated. In half of these tumours, p53 itself is not mutated but the pathway is partially abrogated. Mechanisms include the overexpression of negative regulators of p53, such as MDM2 and MDM4, and deletion or epigenetic inactivation of the positive regulators of p53 such as ARF. In the other half of tumours, in which p53 is inactivated, p53 is mutated and ∼95% of these mutations lie in the core DNA-binding domain, which reflects the key role of p53 as a transcriptional activator. Reactivation of the tumour suppressive properties of p53 is a key therapeutic goal, and the use of peptides in p53 research has led directly to the development of two alternative small molecule approaches: stabilization of mutant p53 to rescue its DNA-binding activity and inhibition of MDM2 or MDM4., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

33. Allosteric rescuing of loss-of-function FFAR2 mutations.

Author

Swaminath G, Jaeckel P, Guo Q, Cardozo M, Weiszmann J, Lindberg R, Wang Y, Schwandner R, and Li Y

Subjects

Acetamides pharmacology, Acetic Acid metabolism, Allosteric Regulation, Allosteric Site genetics, Amino Acid Motifs, Humans, In Vitro Techniques, Kinetics, Ligands, Models, Molecular, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Receptors, Cell Surface agonists, Receptors, Cell Surface metabolism, Recombinant Proteins agonists, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Receptors, Cell Surface chemistry, Receptors, Cell Surface genetics

Abstract

FFAR2 (GPR43) is a receptor for short-chain fatty acids (SCFAs), acetate and propionate. In the current study, we investigate the molecular determinants contributing to receptor activation by endogenous ligands. Mutational analysis revealed several important residues located in transmembrane domains (TM) 3, 4, 5, 6, and 7 for acetate binding. Interestingly, mutations that abolished acetate activity, including the mutation in the well-conserved D(E)RY motif, could be rescued by a recently identified synthetic allosteric agonist. These findings provide additional insight into agonist binding and activation which may aid in designing allosteric ligands for targeting receptor function in various diseases., (Copyright © 2010 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2010

34. FAD mutations in amyloid precursor protein do not directly perturb intracellular calcium homeostasis.

Author

Stieren E, Werchan WP, El Ayadi A, Li F, and Boehning D

Subjects

Alzheimer Disease genetics, Alzheimer Disease metabolism, Amyloid beta-Protein Precursor agonists, Amyloid beta-Protein Precursor biosynthesis, Amyloid beta-Protein Precursor metabolism, Animals, Biological Transport drug effects, Cytosol metabolism, Endoplasmic Reticulum drug effects, Endoplasmic Reticulum metabolism, Gene Expression Regulation, Homeostasis drug effects, Humans, Inositol 1,4,5-Trisphosphate Receptors metabolism, Intracellular Space drug effects, Mutant Proteins agonists, Mutant Proteins biosynthesis, Mutant Proteins metabolism, PC12 Cells, Rats, Alzheimer Disease pathology, Amyloid beta-Protein Precursor genetics, Calcium metabolism, Homeostasis genetics, Intracellular Space metabolism, Mutant Proteins genetics, Mutation

Abstract

Disturbances in intracellular calcium homeostasis are likely prominent and causative factors leading to neuronal cell death in Alzheimer's disease (AD). Familial AD (FAD) is early-onset and exhibits autosomal dominant inheritance. FAD-linked mutations have been found in the genes encoding the presenilins and amyloid precursor protein (APP). Several studies have shown that mutated presenilin proteins can directly affect calcium release from intracellular stores independently of Abeta production. Although less well established, there is also evidence that APP may directly modulate intracellular calcium homeostasis. Here, we directly examined whether overexpression of FAD-linked APP mutants alters intracellular calcium dynamics. In contrast to previous studies, we found that overexpression of mutant APP has no effects on basal cytosolic calcium, ER calcium store size or agonist-induced calcium release and subsequent entry. Thus, we conclude that mutated APP associated with FAD has no direct effect on intracellular calcium homeostasis independently of Abeta production.

Published

2010

35. Structural requirements of bitter taste receptor activation.

Author

Brockhoff A, Behrens M, Niv MY, and Meyerhof W

Subjects

Amino Acid Sequence, Amino Acid Substitution, Base Sequence, Binding Sites, Cell Line, DNA Primers genetics, Humans, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Protein Conformation, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled genetics, Recombinant Fusion Proteins agonists, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Sequence Homology, Amino Acid, Taste genetics, Receptors, G-Protein-Coupled chemistry, Receptors, G-Protein-Coupled physiology, Taste physiology

Abstract

An important question in taste research is how 25 receptors of the human TAS2R family detect thousands of structurally diverse compounds. An answer to this question may arise from the observation that TAS2Rs in general are broadly tuned to interact with numerous substances. Ultimately, interaction with chemically diverse agonists requires architectures of binding pockets tailored to combine flexibility with selectivity. The present study determines the structure of hTAS2R binding pockets. We focused on a subfamily of closely related hTAS2Rs exhibiting pronounced amino acid sequence identities but unique agonist activation spectra. The generation of chimeric and mutant receptors followed by calcium imaging analyses identified receptor regions and amino acid residues critical for activation of hTAS2R46, -R43, and -R31. We found that the carboxyl-terminal regions of the investigated receptors are crucial for agonist selectivity. Intriguingly, exchanging two residues located in transmembrane domain seven between hTAS2R46, activated by strychnine, and hTAS2R31, activated by aristolochic acid, was sufficient to invert agonist selectivity. Further mutagenesis revealed additional positions involved in agonist interaction. The transfer of functionally relevant amino acids identified in hTAS2R46 to the corresponding positions of hTAS2R43 and -R31 resulted in pharmacological properties indistinguishable from the parental hTAS2R46. In silico modeling of hTAS2R46 allowed us to visualize the putative mode of interaction between agonists and hTAS2Rs. Detailed structure-function analyses of hTAS2Rs may ultimately pave the way for the development of specific antagonists urgently needed for more sophisticated analyses of human bitter taste perception.

Published

2010

36. Agonists and antagonists bind to an A-A interface in the heteromeric 5-HT3AB receptor.

Author

Lochner M and Lummis SC

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Cell Line, Granisetron metabolism, Humans, Ligands, Mice, Models, Molecular, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Mutant Proteins metabolism, Protein Subunits chemistry, Protein Subunits metabolism, Receptors, Serotonin, 5-HT3 chemistry, Receptors, Serotonin, 5-HT3 metabolism, Serotonin metabolism, Structural Homology, Protein, Xenopus, Protein Multimerization, Serotonin 5-HT3 Receptor Agonists, Serotonin 5-HT3 Receptor Antagonists

Abstract

The 5-HT3 receptor is a member of the Cys-loop family of transmitter receptors. It can function as a homopentamer (5-HT3A-only subunits) or as a heteropentamer. The 5-HT3AB receptor is the best characterized heteropentamer. This receptor differs from a homopentamer in its kinetics, voltage dependence, and single-channel conductance, but its pharmacology is similar. To understand the contribution of the 5-HT3B subunit to the binding site, we created homology models of 5-HT3AB receptors and docked 5-HT and granisetron into AB, BA, and BB interfaces. To test whether ligands bind in any or all of these interfaces, we mutated amino acids that are important for agonist and antagonist binding in the 5-HT3A subunit to their corresponding residues in the 5-HT3B subunit and vice versa. Changes in [3H]granisetron binding affinity (Kd) and 5-HT EC50 were determined using receptors expressed in HEK-293 cells and Xenopus oocytes, respectively. For all A-to-B mutant receptors, except T181N, antagonist binding was altered or eliminated. Functional studies revealed that either the receptors were nonfunctional or the EC50 values were increased. In B-to-A mutant receptors there were no changes in Kd, although EC50 values and Hill slopes, except for N170T mutant receptors, were similar to those for 5-HT3A receptors. Thus, the experimental data do not support a contribution of the 5-HT3B subunit to the binding pocket, and we conclude that both 5-HT and granisetron bind to an AA binding site in the heteromeric 5-HT3AB receptor., (Copyright 2010 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published

2010

37. Alda-1 is an agonist and chemical chaperone for the common human aldehyde dehydrogenase 2 variant.

Author

Perez-Miller S, Younus H, Vanam R, Chen CH, Mochly-Rosen D, and Hurley TD

Subjects

Aldehyde Dehydrogenase genetics, Aldehyde Dehydrogenase, Mitochondrial, Crystallography, X-Ray, Humans, Models, Molecular, Mutant Proteins agonists, Mutant Proteins genetics, Mutation, Missense, Point Mutation, Protein Binding, Protein Structure, Quaternary, Aldehyde Dehydrogenase chemistry, Aldehyde Dehydrogenase metabolism, Benzamides metabolism, Benzodioxoles metabolism, Molecular Chaperones metabolism, Mutant Proteins chemistry, Mutant Proteins metabolism

Abstract

In approximately one billion people, a point mutation inactivates a key detoxifying enzyme, aldehyde dehydrogenase (ALDH2). This mitochondrial enzyme metabolizes toxic biogenic and environmental aldehydes, including the endogenously produced 4-hydroxynonenal (4HNE) and the environmental pollutant acrolein, and also bioactivates nitroglycerin. ALDH2 is best known, however, for its role in ethanol metabolism. The accumulation of acetaldehyde following the consumption of even a single alcoholic beverage leads to the Asian alcohol-induced flushing syndrome in ALDH2*2 homozygotes. The ALDH2*2 allele is semidominant, and heterozygotic individuals show a similar but less severe phenotype. We recently identified a small molecule, Alda-1, that activates wild-type ALDH2 and restores near-wild-type activity to ALDH2*2. The structures of Alda-1 bound to ALDH2 and ALDH2*2 reveal how Alda-1 activates the wild-type enzyme and how it restores the activity of ALDH2*2 by acting as a structural chaperone.

Published

2010

38. The constitutively active V2 receptor mutants conferring NSIAD are weakly sensitive to agonist and antagonist regulation.

Author

Tenenbaum J, Ayoub MA, Perkovska S, Adra-Delenne AL, Mendre C, Ranchin B, Bricca G, Geelen G, Mouillac B, Durroux T, and Morin D

Subjects

Animals, Arrestins metabolism, COS Cells, Chlorocebus aethiops, Fluorescence Resonance Energy Transfer, Humans, Protein Binding drug effects, Vasopressins pharmacology, beta-Arrestins, Antidiuretic Hormone Receptor Antagonists, Inappropriate ADH Syndrome metabolism, Mutant Proteins agonists, Mutant Proteins antagonists & inhibitors, Receptors, Vasopressin agonists

Abstract

Patients having the nephrogenic syndrome of inappropriate antidiuresis present either the R137C or R137L V2 mutated receptor. While the clinical features have been characterized, the molecular mechanisms of functioning of these two mutants remain elusive. In the present study, we compare the pharmacological properties of R137C and R137L mutants with the wild-type and the V2 D136A receptor, the latter being reported as a highly constitutively active receptor. We have performed binding studies, second messenger measurements and BRET experiments in order to evaluate the affinities of the ligands, their agonist and antagonist properties and the ability of the receptors to recruit beta-arrestins, respectively. The R137C and R137L receptors exhibit small constitutive activities regarding the G(s) protein activation. In addition, these two mutants induce a constitutive beta-arrestin recruitment. Of interest, they also exhibit weak sensitivities to agonist and to inverse agonist in term of G(s) protein coupling and beta-arrestin recruitment. The small constitutive activities of the mutants and the weak regulation of their functioning by agonist suggest a poor ability of the antidiuretic function to be adapted to the external stimuli, giving to the environmental factors an importance which can explain some of the phenotypic variability in patients having NSIAD.

Published

2009

39. Vibrational spectroscopic investigation of the ligand binding domain of kainate receptors.

Author

Du M, Rambhadran A, and Jayaraman V

Subjects

Binding Sites physiology, Cell Line, Glutamic Acid pharmacology, Humans, Kainic Acid pharmacology, Ligands, Mutant Proteins agonists, Patch-Clamp Techniques, Protein Binding physiology, Protein Structure, Secondary, Protein Structure, Tertiary, Receptors, AMPA metabolism, Receptors, Kainic Acid agonists, Spectrum Analysis methods, Vibration, GluK2 Kainate Receptor, Mutant Proteins metabolism, Receptors, Kainic Acid metabolism

Abstract

Fourier transform infrared spectroscopy has been used to probe the agonist-protein interactions in the ligand binding domain of the GluR6 subunit, one subunit of the kainate subtype of glutamate receptors. In order to study the changes in the interactions over a range of activations the investigations were performed using the wild type, N690S, and T661E mutations. These studies show that the strength of the interactions at the alpha-amine group of the agonist, as probed by studying the environment of the nondisulphide bonded Cys 432, acts as a switch with weaker interactions at lower activations and stronger interactions at higher activations. The alpha-carboxylate interactions of the agonist, however, are not significantly different over the wide range of activations, as measured by the maximum currents mediated by the receptors at saturating concentrations of agonists. Previous investigations of AMPA receptors show a similar dependence of the alpha-amine interactions on activation indicating that the roles of the alpha-amine interactions in mediating receptor activation are similar for both subtypes of receptors; however, in the case of the AMPA receptors a tug of war type of change was observed between the alpha-amine and alpha-carboxylate interactions and this is not observed in kainate receptors. This decoupling of the two interactions could arise due to the larger cleft observed in kainate receptors, which allows for a more flexible interaction for the alpha-amine and alpha-carboxylate groups of the agonists.

Published

2009

40. Pharmacochaperone-mediated rescue of calcium-sensing receptor loss-of-function mutants.

Author

White E, McKenna J, Cavanaugh A, and Breitwieser GE

Subjects

Allosteric Regulation genetics, Allosteric Site genetics, Cell Membrane metabolism, Cells, Cultured, Humans, Models, Biological, Mutant Proteins genetics, Mutant Proteins metabolism, Mutant Proteins physiology, Polymorphism, Single Nucleotide physiology, Receptors, Calcium-Sensing agonists, Receptors, Calcium-Sensing metabolism, Allosteric Regulation drug effects, Molecular Chaperones pharmacology, Mutant Proteins agonists, Receptors, Calcium-Sensing genetics, Receptors, Calcium-Sensing physiology

Abstract

The calcium sensing receptor (CaSR) is a Family C/3 G protein-coupled receptor that translates changes in extracellular Ca(2+) into diverse intracellular signals. Loss-of-function mutations in human CaSR cause familial hypocalciuric hypercalcemia and neonatal severe hyperparathyroidism. CaSR must navigate a number of endoplasmic reticulum quality control checkpoints during biosynthesis, including a conformational/functional checkpoint. Here we examine the biosynthesis of 25 CaSR mutations causing familial hypocalciuric hypercalcemia /neonatal severe hyperparathyroidism using immunoprecipitation, biotinylation, and functional assays. We define classes of CaSR mutants based on their biosynthetic profile. Class I CaSR mutants are not rescued to the plasma membrane. To dissect the organellar compartments that class I mutants can access, we engineered a cleavage site for the proprotein convertase furin into the extracellular domain of wild-type CaSR and class I mutants. Based on absence or presence of cleavage fragments, we find most mutants are degraded from the endoplasmic reticulum (no furin-mediated cleavage), whereas others access the Golgi (furin-mediated cleavage) before degradation. Class II CaSR mutants show increased expression and/or enhanced plasma membrane localization upon treatment with MG132 or the pharmacochaperone NPS R-568, permitting assay of functional activity. Of the 10 CaSR mutants that exhibit plasma membrane localization, only two did not show enhanced functional activity after rescue with NPS R-568. The established approaches can be used with current and newly identified CaSR mutations to identify the location of biosynthetic block and to determine the likelihood of rescue by allosteric agonists.

Published

2009

41. The molecular basis of species-specific ligand activation of trace amine-associated receptor 1 (TAAR(1)).

Author

Tan ES, Naylor JC, Groban ES, Bunzow JR, Jacobson MP, Grandy DK, and Scanlan TS

Subjects

Amino Acid Sequence, Animals, Humans, Ligands, Mice, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins genetics, Protein Structure, Secondary, Rats, Receptors, G-Protein-Coupled genetics, Sequence Alignment, Structure-Activity Relationship, Thyronines chemistry, Tyramine metabolism, Tyramine pharmacology, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled chemistry, Thyronines pharmacology

Abstract

The trace amine-associated receptor 1 (TAAR(1)) is an aminergic G protein-coupled receptor (GPCR) potently activated by 3-iodothyronamine (1), an endogenous derivative of thyroid hormone. Structure-activity relationship studies on 1 and related agonists showed that the rat and mouse species of TAAR(1) accommodated structural modifications and functional groups on the ethylamine portion and the biaryl ether moiety of the molecule. However, the two receptors clearly exhibited distinct, species-specific ligand preferences despite being remarkably similar with 93% sequence similarity. In this study, we generated single and double mutants of rat and mouse TAAR(1) to probe the molecular recognition of agonists and the underlying basis for the ligand selectivity of rat and mouse TAAR(1). Key, nonconserved specificity determinant residues in transmembranes helices 4 and 7 within the ligand binding site appear to be the primary source of a number of the observed ligand preferences. Residue 7.39 in transmembrane 7 dictated the preference for a beta-phenyl ring, while residue 4.56 in transmembrane 4 was partially responsible for the lower potency of 1 and tyramine for the mouse receptor. Additionally, 1 and tyramine were found to have the same binding mode in rat TAAR(1) despite structure-activity relationship data suggesting the possibility of each molecule having different binding orientations. These findings provide valuable insights into the critical binding site residues involved in the ligand-receptor interaction that can influence compound selectivity and functional activity of aminergic GPCRs.

Published

2009

42. Generation of an agonistic binding site for blockers of the M(3) muscarinic acetylcholine receptor.

Author

Thor D, Schulz A, Hermsdorf T, and Schöneberg T

Subjects

Animals, Atropine pharmacology, Binding Sites genetics, COS Cells, Chlorocebus aethiops, Muscarinic Antagonists metabolism, Mutant Proteins agonists, Mutant Proteins metabolism, Mutation physiology, Rats, Receptor, Muscarinic M3 agonists, Receptor, Muscarinic M3 physiology, Saccharomyces cerevisiae, Substrate Specificity genetics, Transfection, Atropine metabolism, Mutagenesis, Receptor, Muscarinic M3 genetics, Receptor, Muscarinic M3 metabolism

Abstract

GPCRs (G-protein-coupled receptors) exist in a spontaneous equilibrium between active and inactive conformations that are stabilized by agonists and inverse agonists respectively. Because ligand binding of agonists and inverse agonists often occurs in a competitive manner, one can assume an overlap between both binding sites. Only a few studies report mutations in GPCRs that convert receptor blockers into agonists by unknown mechanisms. Taking advantage of a genetically modified yeast strain, we screened libraries of mutant M(3)Rs {M(3) mAChRs [muscarinic ACh (acetylcholine) receptors)]} and identified 13 mutants which could be activated by atropine (EC50 0.3-10 microM), an inverse agonist on wild-type M(3)R. Many of the mutations sensitizing M(3)R to atropine activation were located at the junction of intracellular loop 3 and helix 6, a region known to be involved in G-protein coupling. In addition to atropine, the pharmacological switch was found for other M(3)R blockers such as scopolamine, pirenzepine and oxybutynine. However, atropine functions as an agonist on the mutant M(3)R only when expressed in yeast, but not in mammalian COS-7 cells, although high-affinity ligand binding was comparable in both expression systems. Interestingly, we found that atropine still blocks carbachol-induced activation of the M(3)R mutants in the yeast expression system by binding at the high-affinity-binding site (Ki approximately 10 nM). Our results indicate that blocker-to-agonist converting mutations enable atropine to function as both agonist and antagonist by interaction with two functionally distinct binding sites.

Published

2008

43. The 2alpha-(3-hydroxypropyl) group as an active motif in vitamin D3 analogues as agonists of the mutant vitamin D receptor (Arg274Leu).

Author

Honzawa S, Yamamoto Y, Yamashita A, Sugiura T, Kurihara M, Arai MA, Kato S, and Kittaka A

Subjects

Drug Design, Humans, Mutation, Missense, Structure-Activity Relationship, Transcription, Genetic drug effects, Cholecalciferol analogs & derivatives, Mutant Proteins agonists, Receptors, Calcitriol agonists, Receptors, Calcitriol genetics

Abstract

We designed and synthesized 1alpha- and 1beta-hydroxymethyl-2alpha-(3-hydroxypropyl)-25-hydroxyvitamin D(3) (2a,b) and related analogues 2alpha-(3-hydroxypropyl)-25-hydroxyvitamin D(3) (3), Posner's analogues of 1alpha- and 1beta-hydroxymethyl-25-hydroxyvitamin D(3) (4a,b), as well as 2alpha-(3-hydroxypropyl)-1alpha,25-dihydroxyvitamin D(3) (5), to confirm the effect of the 1alpha-hydroxy group and/or 2alpha-(3-hydroxypropyl) group of vitamin D(3) analogues with the modified A-ring moiety on the mutant vitamin D receptor, VDR(Arg274Leu). The 2alpha-(3-hydroxypropyl) group showed better effect on enhancement of the transcriptional activity through the mutant VDR than the 1alpha- and 1beta-hydroxymethyl groups.

Published

2008

44. Synthesis of N6-substituted 3'-ureidoadenosine derivatives as highly potent agonists at the mutant A3 adenosine receptor.

Author

Jeong LS, Choe SA, Kim AY, Kim HO, Gao ZG, Jacobson KA, Chun MW, and Moon HR

Subjects

Deoxyadenosines chemistry, Drug Design, Structure-Activity Relationship, Adenosine A3 Receptor Agonists, Deoxyadenosines chemical synthesis, Deoxyadenosines pharmacology, Mutant Proteins agonists, Nitrogen chemistry

Abstract

Several N6-substituted 3 '-ureidoadenosine derivatives were efficiently synthesized starting from D-glucose for the development of H272E mutant A3 adenosine receptor (AR) agonists. Among compounds tested, 3 '-ureido-N6-(3-iodobenzyl)adenosine (2c) exhibited the highest binding affinity (Ki = 0.22 micro M) at the H272E mutant A3 AR without binding to the natural A3AR.

Published

2007

45. Movement of 'gating charge' is coupled to ligand binding in a G-protein-coupled receptor.

Author

Ben-Chaim Y, Chanda B, Dascal N, Bezanilla F, Parnas I, and Parnas H

Subjects

Acetylcholine metabolism, Animals, Electric Conductivity, Ion Channel Gating, Ligands, Membrane Potentials physiology, Movement, Mutant Proteins agonists, Mutant Proteins genetics, Mutant Proteins metabolism, Mutation genetics, Oocytes metabolism, Protein Binding, Receptor, Muscarinic M1 agonists, Receptor, Muscarinic M1 genetics, Receptor, Muscarinic M1 metabolism, Receptor, Muscarinic M2 agonists, Receptor, Muscarinic M2 genetics, Receptor, Muscarinic M2 metabolism, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled chemistry, Receptors, G-Protein-Coupled genetics, Signal Transduction, Xenopus, Receptors, G-Protein-Coupled metabolism

Abstract

Activation by agonist binding of G-protein-coupled receptors (GPCRs) controls most signal transduction processes. Although these receptors span the cell membrane, they are not considered to be voltage sensitive. Recently it was shown that both the activity of GPCRs and their affinity towards agonists are regulated by membrane potential. However, it remains unclear whether GPCRs intrinsically respond to changes in membrane potential. Here we show that two prototypical GPCRs, the m2 and m1 muscarinic receptors (m2R and m1R), display charge-movement-associated currents analogous to 'gating currents' of voltage-gated channels. The gating charge-voltage relationship of m2R correlates well with the voltage dependence of the affinity of the receptor for acetylcholine. The loop that couples m2R and m1R to their G protein has a crucial function in coupling voltage sensing to agonist-binding affinity. Our data strongly indicate that GPCRs serve as sensors for both transmembrane potential and external chemical signals.

Published

2006

46. Ghrelin receptor inverse agonists: identification of an active peptide core and its interaction epitopes on the receptor.

Author

Holst B, Lang M, Brandt E, Bach A, Howard A, Frimurer TM, Beck-Sickinger A, and Schwartz TW

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Binding Sites, COS Cells, Cells, Cultured, Chlorocebus aethiops, Ghrelin, Humans, Ligands, Models, Molecular, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins chemistry, Peptide Hormones metabolism, Protein Binding, Receptors, G-Protein-Coupled chemistry, Receptors, Ghrelin, Structure-Activity Relationship, Substance P chemistry, Epitopes metabolism, Peptides chemistry, Receptors, G-Protein-Coupled agonists, Substance P analogs & derivatives

Abstract

[D-Arg1,D-Phe5,D-Trp7,9,Leu11]Substance P functions as a low-potency antagonist but a high-potency full inverse agonist on the ghrelin receptor. Through a systematic deletion and substitution analysis of this peptide, the C-terminal carboxyamidated pentapeptide wFwLX was identified as the core structure, which itself displayed relatively low inverse agonist potency. Mutational analysis at 17 selected positions in the main ligand-binding crevice of the ghrelin receptor demonstrated that ghrelin apparently interacts only with residues in the middle part of the pocket [i.e., between transmembrane (TM)-III, TM-VI and TM-VII]. In contrast, the inverse agonist peptides bind in a pocket that extends all the way from the extracellular end of TM-II (AspII:20) across between TM-III and TM-VI/VII to TM-V and TM-IV. The potency of the main inverse agonist could be improved up to 20-fold by a number of space-generating mutants located relatively deep in the binding pocket at key positions in TM-III, TM-IV and TM-V. It is proposed that the inverse agonists prevent the spontaneous receptor activation by inserting relatively deeply across the main ligand-binding pocket and sterically blocking the movement of TM-VI and TM-VII into their inward-bend, active conformation. The combined structure-functional analysis of both the ligand and the receptor allowed for the design of a novel, N-terminally Lys-extended analog of wFwLL, which rescued the high-potency, selective inverse agonism that was dependent upon both AspII:20 and GluIII:09. The identified pharmacophore can possibly serve as the basis for targeted discovery of also nonpeptide inverse agonists for the ghrelin receptor.

Published

2006