Your search keyword '"Histamine Agonists pharmacology"' showing total 37 results

1. Cardiac Effects of Novel Histamine H 2 Receptor Agonists.

Author

Gergs U, Büxel ML, Bresinsky M, Kirchhefer U, Fehse C, Höring C, Hofmann B, Marušáková M, Čináková A, Schwarz R, Pockes S, and Neumann J

Subjects

Aged, Animals, Dose-Response Relationship, Drug, Female, Histamine pharmacology, Humans, Isolated Heart Preparation methods, Male, Mice, Mice, Transgenic, Middle Aged, Myocardial Contraction physiology, Heart Atria drug effects, Heart Atria metabolism, Histamine Agonists pharmacology, Myocardial Contraction drug effects, Receptors, Histamine H2 metabolism

Abstract

In an integrative approach, we studied cardiac effects of recently published novel H 2 receptor agonists in the heart of mice that overexpress the human H 2 receptor (H 2 -TG mice) and littermate wild type (WT) control mice and in isolated electrically driven muscle preparations from patients undergoing cardiac surgery. Under our experimental conditions, the H 2 receptor agonists UR-Po563, UR-MB-158, and UR-MB-159 increased force of contraction in left atrium from H 2 -TG mice with pEC 50 values of 8.27, 9.38, and 8.28, respectively, but not in WT mice. Likewise, UR-Po563, UR-MB-158, and UR-MB-159 increased the beating rate in right atrium from H 2 -TG mice with pEC 50 values of 9.01, 9.24, and 7.91, respectively, but not from WT mice. These effects could be antagonized by famotidine, a H 2 receptor antagonist. UR-Po563 (1 µM) increased force of contraction in Langendorff-perfused hearts from H 2 -TG but not WT mice. Similarly, UR-Po563, UR-MB-158, or UR-MB-159 increased the left ventricular ejection fraction in echocardiography of H 2 -TG mice. Finally, UR-Po563 increased force of contraction in isolated human right atrial muscle strips. The contractile effects of UR-Po563 in H 2 -TG mice were accompanied by an increase in the phosphorylation state of phospholamban. In summary, we report here three recently developed agonists functionally stimulating human cardiac H 2 receptors in vitro and in vivo. We speculate that these compounds might be of some merit to treat neurologic disorders if their cardiac effects are blocked by concomitantly applied receptor antagonists that cannot pass through the blood-brain barrier or might be useful to treat congestive heart failure in patients. SIGNIFICANCE STATEMENT: Recently, a new generation of histamine H 2 receptor (H 2 R) agonists has been developed as possible treatment option for Alzheimer's disease. Here, possible cardiac (side) effects of these novel H 2 R agonists have been evaluated., (Copyright © 2021 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2021

2. No evidence for histamine H4 receptor in human monocytes.

Author

Werner K, Neumann D, Buschauer A, and Seifert R

Subjects

Adult, Guanidines pharmacology, HEK293 Cells, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Humans, Imidazoles pharmacology, Male, Monocytes drug effects, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled antagonists & inhibitors, Receptors, Histamine H4, U937 Cells, Monocytes metabolism, Receptors, G-Protein-Coupled biosynthesis, Receptors, Histamine biosynthesis

Abstract

The histamine H4 receptor (H4R) is a classic pertussis toxin-sensitive Gi protein-coupled receptor that mediates increases in intracellular calcium concentration ([Ca(2+)]i). The presence of H4R in human eosinophils has been rigorously documented by several independent groups. It has also been suggested that H4R is expressed in human monocytes, but this suggestion hinges in part on H4R antibodies with questionable specificity. This situation prompted us to reinvestigate H4R expression in human monocytes. As positive control, we studied human embryonic kidney 293T cells stably expressing the human H4R (hH4R). In these cells, histamine (HA) and the H4R agonist UR-PI376 (2-cyano-1-[4-(1H-imidazol-4-yl)butyl]-3-[(2-phenylthio)ethyl]guanidine) induced pertussis toxin-sensitive [Ca(2+)]i increases. However, in quantitative real-time polymerase chain reaction studies we failed to detect hH4R mRNA in human monocytes and U937 promonocytes. In human monocytes, ATP and N-formyl-l-methionyl-l-leucyl-l-phenylalanine increased [Ca(2+)]i, but HA, UR-PI376, and 5-methylhistamine (a dual H4R/H2 receptor agonist) did not. In U937 promonocytes and differentiated U937 cells, HA increased [Ca(2+)]i, but this increase was mediated via HA H1 receptor. In conclusion, there is no evidence for the presence of H4R in human monocytes., (Copyright © 2014 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2014

3. Identification of the antiarrhythmic drugs amiodarone and lorcainide as potent H3 histamine receptor inverse agonists.

Author

Del Tredici AL, Ma JN, Piu F, and Burstein ES

Subjects

Amiodarone chemistry, Amiodarone metabolism, Animals, Anti-Arrhythmia Agents chemistry, Anti-Arrhythmia Agents metabolism, Benzeneacetamides chemistry, Benzeneacetamides metabolism, Cell Proliferation drug effects, HEK293 Cells, Histamine Agonists chemistry, Histamine Agonists metabolism, Humans, Mice, NIH 3T3 Cells, Piperidines chemistry, Piperidines metabolism, Rats, Amiodarone pharmacology, Anti-Arrhythmia Agents pharmacology, Benzeneacetamides pharmacology, Drug Inverse Agonism, Histamine Agonists pharmacology, Piperidines pharmacology, Receptors, Histamine H3 metabolism

Abstract

Use of molecular pharmacology to reprofile older drugs discovered before the advent of recombinant technologies is a fruitful method to elucidate mechanisms of drug action, expand understanding of structure-activity relationships between drugs and receptors, and in some cases, repurpose approved drugs. The H3 histamine receptor is a G-protein-coupled receptor (GPCR) primarily expressed in the central nervous system where among many things it modulates cognitive processes, nociception, feeding and drinking behavior, and sleep/wakefulness. In binding assays and functional screens of the H3 histamine receptor, the antiarrhythmic drugs lorcainide and amiodarone were identified as potent, selective antagonists/inverse agonists of human and rat H3 histamine receptors, with relatively little or no activity at over 20 other monoamine GPCRs, including H1, H2, and H4 receptors. Potent antagonism of H3 receptors was unique to amiodarone and lorcainide of 20 antiarrhythmic drugs tested, representing six pharmacological classes. These results expand the pharmacophore of H3 histamine receptor antagonist/inverse agonists and may explain, in part, the effects of lorcainide on sleep in humans.

Published

2014

4. Natriuretic peptide-induced catecholamine release from cardiac sympathetic neurons: inhibition by histamine H3 and H4 receptor activation.

Author

Chan NY, Robador PA, and Levi R

Subjects

Animals, Calcium metabolism, Cyclic AMP metabolism, Cyclic AMP-Dependent Protein Kinases metabolism, Cyclic GMP-Dependent Protein Kinases antagonists & inhibitors, Cyclic Nucleotide Phosphodiesterases, Type 3 metabolism, Guinea Pigs, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Humans, Neurons metabolism, Norepinephrine metabolism, PC12 Cells, Protein Kinase Inhibitors pharmacology, Rats, Receptors, Histamine H3 genetics, Receptors, Histamine H4, Sympathetic Nervous System metabolism, Synaptosomes drug effects, Synaptosomes metabolism, Transfection, Heart innervation, Natriuretic Peptide, Brain pharmacology, Neurons drug effects, Norepinephrine antagonists & inhibitors, Receptors, G-Protein-Coupled metabolism, Receptors, Histamine metabolism, Receptors, Histamine H3 metabolism, Sympathetic Nervous System drug effects

Abstract

We reported previously that natriuretic peptides, including brain natriuretic peptide (BNP), promote norepinephrine release from cardiac sympathetic nerves and dopamine release from differentiated pheochromocytoma PC12 cells. These proexocytotic effects are mediated by an increase in intracellular calcium secondary to cAMP/protein kinase A (PKA) activation caused by a protein kinase G (PKG)-mediated inhibition of phosphodiesterase type 3 (PDE3). The purpose of the present study was to search for novel means to prevent the proadrenergic effects of natriuretic peptides. For this, we focused our attention on neuronal inhibitory Gα(i/o)-coupled histamine H(3) and H(4) receptors. Our findings show that activation of neuronal H(3) and H(4) receptors inhibits the release of catecholamines elicited by BNP in cardiac synaptosomes and differentiated PC12 cells. This effect results from a decrease in intracellular Ca(2+) due to reduced intracellular cAMP/PKA activity, caused by H(3) and H(4) receptor-mediated PKG inhibition and consequent PDE3-induced increase in cAMP metabolism. Indeed, selective H(3) and H(4) receptor agonists each synergized with a PKG inhibitor and a PDE3 activator in attenuating BNP-induced norepinephrine release from cardiac sympathetic nerve endings. This indicates that PKG inhibition and PDE3 stimulation are pivotal for the H(3) and H(4) receptor-mediated attenuation of BNP-induced catecholamine release. Cardiac sympathetic overstimulation is characteristic of advanced heart failure, which was recently found not to be improved by the administration of recombinant BNP (nesiritide), despite the predicated beneficial effects of natriuretic peptides. Because excessive catecholamine release is likely to offset the desirable effects of natriuretic peptides, our findings suggest novel means to alleviate their adverse effects and improve their therapeutic potential.

Published

2012

5. Histamine 3 receptor activation reduces the expression of neuronal angiotensin II type 1 receptors in the heart.

Author

Hashikawa-Hobara N, Chan NY, and Levi R

Subjects

Angiotensin II metabolism, Animals, Guinea Pigs, Heart innervation, Male, Myocardial Ischemia metabolism, Myocardial Reperfusion Injury pathology, Nerve Endings metabolism, Nitric Oxide pharmacology, PC12 Cells, Protein Kinase C metabolism, Rats, Receptors, Histamine H3 drug effects, Sodium-Hydrogen Exchangers metabolism, Sympathetic Nervous System cytology, Sympathetic Nervous System drug effects, Sympathetic Nervous System metabolism, Synaptosomes metabolism, Tetradecanoylphorbol Acetate pharmacology, Heart drug effects, Histamine Agonists pharmacology, Myocardium metabolism, Neurons metabolism, Receptor, Angiotensin, Type 1 biosynthesis, Receptors, Histamine H3 physiology

Abstract

In severe myocardial ischemia, histamine 3 (H₃) receptor activation affords cardioprotection by preventing excessive norepinephrine release and arrhythmias; pivotal to this action is the inhibition of neuronal Na⁺/H⁺ exchanger (NHE). Conversely, angiotensin II, formed locally by mast cell-derived renin, stimulates NHE via angiotensin II type 1 (AT₁) receptors, facilitating norepinephrine release and arrhythmias. Thus, ischemic dysfunction may depend on a balance between the NHE-modulating effects of H₃ receptors and AT₁ receptors. The purpose of this investigation was therefore to elucidate the H₃/AT₁ receptor interaction in myocardial ischemia/reperfusion. We found that H₃ receptor blockade with clobenpropit increased norepinephrine overflow and arrhythmias in Langendorff-perfused guinea pig hearts subjected to ischemia/reperfusion. This coincided with increased neuronal AT₁ receptor expression. NHE inhibition with cariporide prevented both increases in norepinephrine release and AT₁ receptor expression. Moreover, norepinephrine release and AT₁ receptor expression were increased by the nitric oxide (NO) synthase inhibitor N(G)-methyl-L-arginine and the protein kinase C activator phorbol myristate acetate. H₃ receptor activation in differentiated sympathetic neuron-like PC12 cells permanently transfected with H₃ receptor cDNA caused a decrease in protein kinase C activity and AT₁ receptor protein abundance. Collectively, our findings suggest that neuronal H₃ receptor activation inhibits NHE by diminishing protein kinase C activity. Reduced NHE activity sequentially causes intracellular acidification, increased NO synthesis, and diminished AT₁ receptor expression. Thus, H₃ receptor-mediated NHE inhibition in ischemia/reperfusion not only opposes the angiotensin II-induced stimulation of NHE in cardiac sympathetic neurons, but also down-regulates AT₁ receptor expression. Cardioprotection ultimately results from the combined attenuation of angiotensin II and norepinephrine effects and alleviation of arrhythmias.

Published

2012

6. A study comparing the antisecretory effect of TAK-438, a novel potassium-competitive acid blocker, with lansoprazole in animals.

Author

Hori Y, Matsukawa J, Takeuchi T, Nishida H, Kajino M, and Inatomi N

Subjects

Animals, Anti-Ulcer Agents blood, Anti-Ulcer Agents pharmacokinetics, Cimetidine pharmacology, Dogs, Gastric Mucosa drug effects, Gastric Mucosa metabolism, H(+)-K(+)-Exchanging ATPase metabolism, Histamine pharmacology, Histamine Agonists pharmacology, Hydrogen-Ion Concentration, Lansoprazole, Male, Potassium metabolism, Pyrroles blood, Pyrroles pharmacokinetics, Rats, Rats, Sprague-Dawley, Sulfonamides blood, Sulfonamides pharmacokinetics, Time Factors, 2-Pyridinylmethylsulfinylbenzimidazoles pharmacology, Anti-Ulcer Agents pharmacology, Gastric Acid metabolism, Proton Pump Inhibitors pharmacology, Pyrroles pharmacology, Sulfonamides pharmacology

Abstract

Proton pump inhibitors (PPIs) are widely used for the treatment of acid-related diseases. However, several medical needs such as suppression of night-time acid secretion and rapid symptom relief remain unmet. In this study, we investigated the effects of 1-[5-(2-fluorophenyl)-1-(pyridin-3-ylsulfonyl)-1H-pyrrol-3-yl]-N-methylmethanamine monofumarate (TAK-438), a novel potassium-competitive acid blocker, on acid secretion in rats and dogs under various conditions, in comparison with the PPI lansoprazole [2-[[[3-methyl-4-(2,2,2-trifluoroethoxy)-2-pyridyl] methyl]sulfinyl]-1H-benzimidazole], to characterize the antisecretory action of TAK-438. TAK-438 showed a more potent and longer-lasting inhibitory effect than lansoprazole on the histamine-stimulated gastric acid secretion in rats and dogs. A pharmacokinetic study in rats showed that TAK-438 accumulated and was retained in the gastric tissue for more than 24 h, unlike that in the plasma. TAK-438 showed significant antisecretory activity with or without cimetidine pretreatment, in contrast to lansoprazole, which did not show antisecretory activity after cimetidine pretreatment in rats. TAK-438 increased the pH of the gastric perfusate to 5.7 in an unstimulated condition, and this effect was maintained in the presence of subsequent histamine stimulation. On the other hand, lansoprazole also increased the pH in an unstimulated condition, but this effect diminished after histamine stimulation. These results indicated that TAK-438 exerted a more potent and longer-lasting antisecretory effect than lansoprazole through high accumulation and slow clearance from the gastric tissue. In addition, TAK-438 was unaffected by the gastric secretory state, unlike PPIs. Therefore, TAK-438 can provide a novel mechanism of action to improve the present PPI-based treatment of acid-related diseases.

Published

2011

7. H3 receptors and pain modulation: peripheral, spinal, and brain interactions.

Author

Hough LB and Rice FL

Subjects

Animals, Brain drug effects, Histamine Agonists metabolism, Histamine Agonists pharmacology, Histamine Agonists therapeutic use, Humans, Pain drug therapy, Pain Measurement drug effects, Pain Measurement methods, Spinal Cord drug effects, Brain metabolism, Nociceptors metabolism, Pain metabolism, Receptors, Histamine H3 physiology, Spinal Cord metabolism

Abstract

Histamine H(3) receptors (H(3)Rs), distributed within the brain, the spinal cord, and on specific types of primary sensory neurons, can modulate pain transmission by several mechanisms. In the skin, H(3)Rs are found on certain Aβ fibers, and on keratinocytes and Merkel cells, as well as on deep dermal, peptidergic Aδ fibers terminating on deep dermal blood vessels. Activation of H(3)Rs on the latter in the skin, heart, lung, and dura mater reduces calcitonin gene-related peptide and substance P release, leading to anti-inflammatory (but not antinociceptive) actions. However, activation of H(3)Rs on the spinal terminals of these sensory fibers reduces nociceptive responding to low-intensity mechanical stimuli and inflammatory stimuli such as formalin. These findings suggest that H(3)R agonists might be useful analgesics, but these drugs have not been tested in clinically relevant pain models. Paradoxically, H(3) antagonists/inverse agonists have also been reported to attenuate several types of pain responses, including phase II responses to formalin. In the periaqueductal gray (an important pain regulatory center), the H(3) inverse agonist thioperamide releases neuronal histamine and mimics histamine's biphasic modulatory effects in thermal nociceptive tests. Newer H(3) inverse agonists with potent, selective, and brain-penetrating properties show efficacy in several neuropathic and arthritis pain models, but the sites and mechanisms for these actions remain poorly understood.

Published

2011

8. Effects of betahistine at histamine H3 receptors: mixed inverse agonism/agonism in vitro and partial inverse agonism in vivo.

Author

Gbahou F, Davenas E, Morisset S, and Arrang JM

Subjects

Administration, Oral, Animals, Arachidonic Acid metabolism, Betahistine administration & dosage, Brain cytology, Brain drug effects, Brain Chemistry drug effects, CHO Cells, Cricetinae, Cricetulus, Cyclic AMP biosynthesis, Histamine physiology, Histamine Agonists administration & dosage, Histamine H2 Antagonists metabolism, Histamine H3 Antagonists administration & dosage, Humans, Imidazoles metabolism, Injections, Intraperitoneal, Methylhistamines metabolism, Mice, Neurons drug effects, Pertussis Toxin pharmacology, Rats, Receptors, Histamine H3 genetics, Recombinant Proteins metabolism, Betahistine pharmacology, Histamine Agonists pharmacology, Histamine H3 Antagonists pharmacology, Receptors, Histamine H3 drug effects

Abstract

We previously suggested that therapeutic effects of betahistine in vestibular disorders result from its antagonist properties at histamine H(3) receptors (H(3)Rs). However, H(3)Rs exhibit constitutive activity, and most H(3)R antagonists act as inverse agonists. Here, we have investigated the effects of betahistine at recombinant H(3)R isoforms. On inhibition of cAMP formation and [(3)H]arachidonic acid release, betahistine behaved as a nanomolar inverse agonist and a micromolar agonist. Both effects were suppressed by pertussis toxin, were found at all isoforms tested, and were not detected in mock cells, confirming interactions at H(3)Rs. The inverse agonist potency of betahistine and its affinity on [(125)I]iodoproxyfan binding were similar in rat and human. We then investigated the effects of betahistine on histamine neuron activity by measuring tele-methylhistamine (t-MeHA) levels in the brains of mice. Its acute intraperitoneal administration increased t-MeHA levels with an ED(50) of 0.4 mg/kg, indicating inverse agonism. At higher doses, t-MeHA levels gradually returned to basal levels, a profile probably resulting from agonism. After acute oral administration, betahistine increased t-MeHA levels with an ED(50) of 2 mg/kg, a rightward shift probably caused by almost complete first-pass metabolism. In each case, the maximal effect of betahistine was lower than that of ciproxifan, indicating partial inverse agonism. After an oral 8-day treatment, the only effective dose of betahistine was 30 mg/kg, indicating that a tolerance had developed. These data strongly suggest that therapeutic effects of betahistine result from an enhancement of histamine neuron activity induced by inverse agonism at H(3) autoreceptors.

Published

2010

9. Structural requirements for inverse agonism and neutral antagonism of indole-, benzimidazole-, and thienopyrrole-derived histamine H4 receptor ligands.

Author

Schneider EH, Strasser A, Thurmond RL, and Seifert R

Subjects

Animals, Benzimidazoles chemistry, Binding, Competitive, Cell Line, Drug Antagonism, Drug Inverse Agonism, Histamine Agonists chemistry, Histamine Antagonists chemistry, Humans, Indoles chemistry, Ligands, Pyrroles chemistry, Radioligand Assay, Receptors, Histamine H4, Structure-Activity Relationship, Thiophenes chemistry, Benzimidazoles pharmacology, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Indoles pharmacology, Pyrroles pharmacology, Receptors, G-Protein-Coupled metabolism, Receptors, Histamine metabolism, Thiophenes pharmacology

Abstract

The human histamine H(4) receptor (hH(4)R), coexpressed with Galpha(i2) and Gbeta(1)gamma(2) in Sf9 insect cells, is highly constitutively active, and thioperamide [THIO; N-cyclohexyl-4-(imidazol-4-yl)-1-piperidinecarbothioamide] is one of the most efficacious hH(4)R inverse agonists. High constitutive hH(4)R activity may have pathophysiological implications in which case inverse agonists may behave differently than neutral antagonists. To learn more about the structural requirements for hH(4)R inverse agonism, we investigated 25 compounds (indole, benzimidazole, and thienopyrrole derivatives) structurally related to the standard antagonist JNJ-7777120 [1-[(5-chloro-1H-indol-2-yl)carbonyl]-4-methyl-piperazine]. We characterized the compounds in radioligand binding assays by using [(3)H]histamine ([(3)H]HA) and in steady-state GTPase assays in the presence (antagonist mode) and absence (inverse agonist mode) of the agonist HA, yielding the following results: 1) Twenty-two compounds were inverse agonists (efficacy: 15-62% of the THIO effect), and only three compounds (12%) showed neutral antagonism. Thus, inverse agonism is far more common than neutral antagonism. 2) The inverse agonistic efficacy of the R5-monosubstituted indole-derived compounds increased with the volume of R5. R5 may interact with Trp(6.48) of the rotamer toggle switch and stabilize the inactive receptor conformation. 3) A subset of compounds showed large differences between the K(i) value from [(3)H]HA competition binding and the EC(50) value from steady-state GTPase assays, whereas the K(b) values were closer to the K(i) values. Thus, the two-state model should be extended to a model comprising a constitutively active hH(4)R state, which can be discriminated by inverse agonists from a structurally distinct HA-stabilized active state.

Published

2010

10. No evidence for functional selectivity of proxyfan at the human histamine H3 receptor coupled to defined Gi/Go protein heterotrimers.

Author

Schnell D, Burleigh K, Trick J, and Seifert R

Subjects

Animals, Cell Line, GTP-Binding Protein alpha Subunit, Gi2 genetics, GTP-Binding Protein alpha Subunits, Gi-Go genetics, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Humans, Ligands, Protein Multimerization, Receptors, Histamine H3 genetics, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, GTP-Binding Protein alpha Subunits, Gi-Go metabolism, Imidazoles pharmacology, Receptors, Histamine H3 metabolism

Abstract

Numerous structurally diverse ligands were developed to target the human histamine H(3) receptor (hH(3)R), a presynaptic G(i)/G(o)-coupled auto- and heteroreceptor. Proxyfan was identified to be functionally selective, with different efficacies toward G(i)/G(o)-dependent hH(3)R signaling pathways. However, the underlying molecular mechanism of functional selectivity of proxyfan is still unclear. In the current study, we investigated the role of different Galpha(i/o) proteins in hH(3)R signaling, using a baculovirus/Sf9 cell expression system. We tested the hypothesis that ligand-specific coupling differences to defined G(i)/G(o)-heterotrimers are responsible for functional selectivity of proxyfan at hH(3)R. In Sf9 membranes, full-length hH(3)R (445 amino acids) was expressed in combination with an excess of different mammalian G proteins (Galpha(i1), Galpha(i2), Galpha(i3), or Galpha(o1) and beta(1)gamma(2) dimers, respectively). In addition, we constructed the fusion proteins hH(3)R-Galpha(i2) and hH(3)R-Galpha(o1) to ensure clearly defined receptor/G protein stoichiometries. Steady-state GTPase experiments were performed to directly measure the impact of each G protein on hH(3)R signal transduction. The hH(3)R coupled similarly to all G proteins. We also observed similar ligand-independent or constitutive activity. Proxyfan and various other imidazole-containing ligands, including full agonists, partial agonists, and inverse agonists, showed very similar pharmacological profiles not influenced by the type of G protein coexpressed. Selected ligands, examined in membranes expressing the fusion proteins hH(3)R-Galpha(i2) and hH(3)R-Galpha(o1) (plus beta(1)gamma(2) dimers), yielded very similar results. Collectively, our data indicate that hH(3)R couples similarly to different Galpha(i/o)-subunits and that ligand-specific active receptor conformations, resulting in G protein-coupling preferences, do not exist for proxyfan or other imidazole compounds investigated.

Published

2010

11. Autoregulation of McA-RH7777 hepatoma cell proliferation by histamine H3 receptors.

Author

Davenas E, Rouleau A, Morisset S, and Arrang JM

Subjects

Animals, Binding Sites, COS Cells, Cell Line, Tumor, Chlorocebus aethiops, Cytochrome P-450 Enzyme System metabolism, Histamine metabolism, Histamine Agonists pharmacology, Histamine H3 Antagonists pharmacology, Homeostasis drug effects, Immunohistochemistry, Liver Neoplasms, Experimental, Receptors, Histamine H3 biosynthesis, Reverse Transcriptase Polymerase Chain Reaction, Cell Proliferation drug effects, Histamine physiology, Histamine Release drug effects, Homeostasis physiology, Receptors, Histamine H3 physiology

Abstract

Previous studies have suggested that histamine (HA) acts as an autocrine growth factor. We have explored the modulation of cell proliferation by HA using McA-RH7777 hepatoma cells. High L-histidine decarboxylase (HDC) expression and HA synthesis were found in McA-RH7777 cells. Whereas extracellular HA reached submicromolar concentrations, intracellular levels were very low, indicating that HA was secreted by the cells. McA-RH7777 cells also express H3-receptor (H3R) transcripts and proteins. Reverse transcriptase-polymerase chain reaction analysis detected only transcripts for the long isoform. Immunocytochemistry performed with a selective H3R antibody showed that most cells were immunoreactive. H3R binding sites (Bmax approximately 30 fmol/mg protein) were identified when [125I] iodoproxyfan binding was displaced by the agonist imetit. High-affinity binding also occurred at cytochrome P450 enzymes. This binding was not inhibited by HA, H3R agonists, or by a nonimidazole H3R antagonist but was displaced by imidazole H3R antagonists or by ketoconazole, a imidazole-containing cytochrome inhibitor. HA inhibited proliferation of McA-RH7777 hepatoma cells. The absence of uptake system, its much higher potency at H3Rs, and its low intracellular levels suggested that HA interacted with H3Rs rather than cytochromes. In agreement, both imidazole H3R antagonists, a nonimidazole H3R antagonist, and the HDC inhibitor alpha-monofluoromethyl histidine increased cell proliferation (up to approximately 60%), revealing a H3R-mediated inhibition by endogenous HA. Moreover, exogenous HA inhibited the increase induced by alpha-FMH or H3R antagonists with a nanomolar potency. In conclusion, our findings show that HA regulates proliferation of McA-RH7777 hepatoma cells by interacting with autoinhibitory H3Rs.

Published

2008

12. In vitro pharmacology of clinically used central nervous system-active drugs as inverse H(1) receptor agonists.

Author

Bakker RA, Nicholas MW, Smith TT, Burstein ES, Hacksell U, Timmerman H, Leurs R, Brann MR, and Weiner DM

Subjects

Animals, COS Cells, Chlorocebus aethiops, Cloning, Molecular, Histamine Agonists pharmacology, Humans, Methylhistamines pharmacology, Mice, NIH 3T3 Cells, Pyrilamine pharmacology, Central Nervous System Agents pharmacology, Histamine H1 Antagonists pharmacology, Receptors, Histamine H1 drug effects

Abstract

The human histamine H(1) receptor (H(1)R) is a prototypical G protein-coupled receptor and an important, well characterized target for the development of antagonists to treat allergic conditions. Many neuropsychiatric drugs are also known to potently antagonize this receptor, underlying aspects of their side effect profiles. We have used the cell-based receptor selection and amplification technology assay to further define the clinical pharmacology of the human H(1)R by evaluating >130 therapeutic and reference drugs for functional receptor activity. Based on this screen, we have reported on the identification of 8R-lisuride as a potent stereospecific partial H(1)R agonist (Mol Pharmacol 65:538-549, 2004). In contrast, herein we report on a large number of varied clinical and chemical classes of drugs that are active in the central nervous system that display potent H(1)R inverse agonist activity. Absolute and rank order of functional potency of these clinically relevant brain-penetrating drugs may possibly be used to predict aspects of their clinical profiles, including propensity for sedation.

Published

2007

13. GSK189254, a novel H3 receptor antagonist that binds to histamine H3 receptors in Alzheimer's disease brain and improves cognitive performance in preclinical models.

Author

Medhurst AD, Atkins AR, Beresford IJ, Brackenborough K, Briggs MA, Calver AR, Cilia J, Cluderay JE, Crook B, Davis JB, Davis RK, Davis RP, Dawson LA, Foley AG, Gartlon J, Gonzalez MI, Heslop T, Hirst WD, Jennings C, Jones DN, Lacroix LP, Martyn A, Ociepka S, Ray A, Regan CM, Roberts JC, Schogger J, Southam E, Stean TO, Trail BK, Upton N, Wadsworth G, Wald JA, White T, Witherington J, Woolley ML, Worby A, and Wilson DM

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Alzheimer Disease metabolism, Alzheimer Disease pathology, Alzheimer Disease physiopathology, Animals, Benzazepines metabolism, Benzazepines pharmacokinetics, Binding, Competitive, Brain metabolism, Brain pathology, Cell Line, Dogs, Histamine Agonists metabolism, Histamine Agonists pharmacokinetics, Histamine Agonists pharmacology, Histamine Antagonists metabolism, Histamine Antagonists pharmacokinetics, Humans, Male, Maze Learning drug effects, Mice, Middle Aged, Neurotransmitter Agents metabolism, Niacinamide metabolism, Niacinamide pharmacokinetics, Niacinamide pharmacology, Nootropic Agents metabolism, Nootropic Agents pharmacokinetics, Rats, Rats, Sprague-Dawley, Rats, Wistar, Receptors, Histamine H3 analysis, Sus scrofa, Benzazepines pharmacology, Brain drug effects, Histamine Antagonists pharmacology, Niacinamide analogs & derivatives, Nootropic Agents pharmacology, Receptors, Histamine H3 metabolism

Abstract

6-[(3-Cyclobutyl-2,3,4,5-tetrahydro-1H-3-benzazepin-7-yl)oxy]-N-methyl-3-pyridinecarboxamide hydrochloride (GSK189254) is a novel histamine H(3) receptor antagonist with high affinity for human (pK(i) = 9.59 -9.90) and rat (pK(i) = 8.51-9.17) H(3) receptors. GSK189254 is >10,000-fold selective for human H(3) receptors versus other targets tested, and it exhibited potent functional antagonism (pA(2) = 9.06 versus agonist-induced changes in cAMP) and inverse agonism [pIC(50) = 8.20 versus basal guanosine 5'-O-(3-[(35)S]thio)triphosphate binding] at the human recombinant H(3) receptor. In vitro autoradiography demonstrated specific [(3)H]GSK189254 binding in rat and human brain areas, including cortex and hippocampus. In addition, dense H(3) binding was detected in medial temporal cortex samples from severe cases of Alzheimer's disease, suggesting for the first time that H(3) receptors are preserved in late-stage disease. After oral administration, GSK189254 inhibited cortical ex vivo R-(-)-alpha-methyl[imidazole-2,5(n)-(3)H]histamine dihydrochloride ([(3)H]R-alpha-methylhistamine) binding (ED(50) = 0.17 mg/kg) and increased c-Fos immunoreactivity in prefrontal and somatosensory cortex (3 mg/kg). Microdialysis studies demonstrated that GSK189254 (0.3-3 mg/kg p.o.) increased the release of acetylcholine, noradrenaline, and dopamine in the anterior cingulate cortex and acetylcholine in the dorsal hippocampus. Functional antagonism of central H(3) receptors was demonstrated by blockade of R-alpha-methylhistamine-induced dipsogenia in rats (ID(50) = 0.03 mg/kg p.o.). GSK189254 significantly improved performance of rats in diverse cognition paradigms, including passive avoidance (1 and 3 mg/kg p.o.), water maze (1 and 3 mg/kg p.o.), object recognition (0.3 and 1 mg/kg p.o.), and attentional set shift (1 mg/kg p.o.). These data suggest that GSK189254 may have therapeutic potential for the symptomatic treatment of dementia in Alzheimer's disease and other cognitive disorders.

Published

2007

14. Mutations of Cys-17 and Ala-271 in the human histamine H2 receptor determine the species selectivity of guanidine-type agonists and increase constitutive activity.

Author

Preuss H, Ghorai P, Kraus A, Dove S, Buschauer A, and Seifert R

Subjects

Adenylyl Cyclases metabolism, Alanine genetics, Animals, Baculoviridae genetics, Cell Line, Cell Membrane drug effects, Cell Membrane metabolism, Cysteine genetics, GTP Phosphohydrolases metabolism, GTP-Binding Protein alpha Subunits, Gs genetics, GTP-Binding Protein alpha Subunits, Gs metabolism, Guanosine Triphosphate pharmacology, Guinea Pigs, Histamine pharmacology, Histamine Agonists chemistry, Histamine H2 Antagonists pharmacology, Humans, Receptors, Histamine H2 metabolism, Recombinant Fusion Proteins metabolism, Species Specificity, Spodoptera, Transfection, Guanidine chemistry, Histamine Agonists pharmacology, Mutation, Missense, Receptors, Histamine H2 genetics

Abstract

In a steady-state GTPase activity assay, N-[3-(1H-imidazol-4-yl)propyl)]guanidines and N(G)-acylated derivatives are more potent and efficacious at fusion proteins of guinea pig (gpH(2)R-G(salphaS)) than human (hH(2)R-G(salphaS)) histamine H(2) receptor, coupled to the short splice variant of G(salpha), G(salphaS). Whereas Ala-271 (hH(2)R) and Asp-271 (gpH(2)R) in transmembrane domain 7 were identified to determine the potency differences of guanidine-type agonists, the molecular basis for the efficacy differences remains to be elucidated. A homology model of the gpH(2)R suggested that an H-bond between Tyr-17 and Asp-271 stabilizes an active receptor conformation of the gpH(2)R. In the present study, we generated a mutant hH(2)R-G(salphaS) with Cys-17--> Tyr-17/Ala-271--> Asp-271 exchanges (hH(2)R-->gpH(2)R) that exhibited an enhanced level of constitutive GTPase activity and adenylyl cyclase activity compared with wild-type hH(2)R-G(salphaS) and gpH(2)R-G(salphaS). Potencies and efficacies of guanidines and N(G)-acylguanidines were increased at this mutant receptor compared with hH(2)R-G(salphaS), but they were still lower than at gpH(2)R-G(salphaS), suggesting that aside from Tyr-17 and Asp-271 additional amino acids contribute to the distinct pharmacological profiles of both species isoforms. Another hH(2)R-G(salphaS) mutant with a Cys-17--> Tyr-17 exchange showed inefficient coupling to G(salphaS) as revealed by reduced agonist-stimulated GTPase and basal adenylyl cyclase activities. Collectively, our present pharmacological study confirms the existence of an H-bond between Tyr-17 and Asp-271 favoring the stabilization of an active receptor conformation. Distinct potencies and efficacies of agonists and inverse agonists further support the concept of ligand-specific conformations in wild-type and mutant H(2)R-G(salphaS) fusion proteins.

Published

2007

15. Constitutive activity and ligand selectivity of human, guinea pig, rat, and canine histamine H2 receptors.

Author

Preuss H, Ghorai P, Kraus A, Dove S, Buschauer A, and Seifert R

Subjects

Adenylyl Cyclases metabolism, Animals, Baculoviridae genetics, Cell Line, Cell Membrane drug effects, Cell Membrane metabolism, Dogs, GTP Phosphohydrolases metabolism, GTP-Binding Protein alpha Subunits, Gs genetics, GTP-Binding Protein alpha Subunits, Gs metabolism, Guinea Pigs, Histamine pharmacology, Humans, Ligands, Metiamide pharmacology, Rats, Receptors, Histamine H2 genetics, Recombinant Fusion Proteins metabolism, Recombinant Proteins metabolism, Species Specificity, Spodoptera, Transfection, Histamine Agonists pharmacology, Histamine H2 Antagonists pharmacology, Receptors, Histamine H2 metabolism

Abstract

Previous studies revealed pharmacological differences between human and guinea pig histamine H(2) receptors (H(2)Rs) with respect to the interaction with guanidine-type agonists. Because H(2)R species variants are structurally very similar, comparative studies are suited to relate different properties of H(2)R species isoforms to few molecular determinants. Therefore, we systematically compared H(2)Rs of human (h), guinea pig (gp), rat (r), and canine (c). Fusion proteins of hH(2)R, gpH(2)R, rH(2)R, and cH(2)R, respectively, and the short splice variant of G(salpha), G(salphaS), were expressed in Sf9 insect cells. In the membrane steady-state GTPase activity assay, cH(2)R-G(salphaS) but neither gpH(2)R-G(salphaS) nor rH(2)R-G(salphaS) showed the hallmarks of increased constitutive activity compared with hH(2)R-G(salphaS), i.e., increased efficacies of partial agonists, increased potencies of agonists with the extent of potency increase being correlated with the corresponding efficacies at hH(2)R-G(salphaS), increased inverse agonist efficacies, and decreased potencies of antagonists. Furthermore, in membranes expressing nonfused H(2)Rs without or together with mammalian G(salphaS) or H(2)R-G(salpha) fusion proteins, the highest basal and GTP-dependent increases in adenylyl cyclase activity were observed for cH(2)R. An example of ligand selectivity is given by metiamide, acting as an inverse agonist at hH(2)R-G(salphaS), gpH(2)R-G(salphaS), and rH(2)R-G(salphaS) in the GTPase assay in contrast to being a weak partial agonist with decreased potency at cH(2)R-G(salphaS). In conclusion, the cH(2)R exhibits increased constitutive activity compared with hH(2)R, gpH(2)R, and rH(2)R, and there is evidence for ligand-specific conformations in H(2)R species isoforms.

Published

2007

16. BF2.649 [1-{3-[3-(4-Chlorophenyl)propoxy]propyl}piperidine, hydrochloride], a nonimidazole inverse agonist/antagonist at the human histamine H3 receptor: Preclinical pharmacology.

Author

Ligneau X, Perrin D, Landais L, Camelin JC, Calmels TP, Berrebi-Bertrand I, Lecomte JM, Parmentier R, Anaclet C, Lin JS, Bertaina-Anglade V, la Rochelle CD, d'Aniello F, Rouleau A, Gbahou F, Arrang JM, Ganellin CR, Stark H, Schunack W, and Schwartz JC

Subjects

Acetylcholine metabolism, Animals, Cats, Dopamine metabolism, Electroencephalography drug effects, Guinea Pigs, Histamine Release drug effects, Humans, Imidazoles metabolism, Male, Methylhistamines pharmacology, Mice, Mice, Inbred C57BL, Piperidines pharmacokinetics, Prefrontal Cortex drug effects, Prefrontal Cortex metabolism, Receptors, Histamine H3 physiology, Scopolamine pharmacology, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Piperidines pharmacology, Receptors, Histamine H3 drug effects

Abstract

Histamine H3 receptor inverse agonists are known to enhance the activity of histaminergic neurons in brain and thereby promote vigilance and cognition. 1-{3-[3-(4-Chlorophenyl)propoxy]propyl}piperidine, hydrochloride (BF2.649) is a novel, potent, and selective nonimidazole inverse agonist at the recombinant human H3 receptor. On the stimulation of guanosine 5'-O-(3-[35S]thio)triphosphate binding to this receptor, BF2.649 behaved as a competitive antagonist with a Ki value of 0.16 nM and as an inverse agonist with an EC50 value of 1.5 nM and an intrinsic activity approximately 50% higher than that of ciproxifan. Its in vitro potency was approximately 6 times lower at the rodent receptor. In mice, the oral bioavailability coefficient, i.e., the ratio of plasma areas under the curve after oral and i.v. administrations, respectively, was 84%. BF2.649 dose dependently enhanced tele-methylhistamine levels in mouse brain, an index of histaminergic neuron activity, with an ED50 value of 1.6 mg/kg p.o., a response that persisted after repeated administrations for 17 days. In rats, the drug enhanced dopamine and acetylcholine levels in microdialysates of the prefrontal cortex. In cats, it markedly enhanced wakefulness at the expense of sleep states and also enhanced fast cortical rhythms of the electroencephalogram, known to be associated with improved vigilance. On the two-trial object recognition test in mice, a promnesiant effect was shown regarding either scopolamine-induced or natural forgetting. These preclinical data suggest that BF2.649 is a valuable drug candidate to be developed in wakefulness or memory deficits and other cognitive disorders.

Published

2007

17. N1-(3-cyclohexylbutanoyl)-N2-[3-(1H-imidazol-4-yl)propyl]guanidine (UR-AK57), a potent partial agonist for the human histamine H1- and H2-receptors.

Author

Xie SX, Kraus A, Ghorai P, Ye QZ, Elz S, Buschauer A, and Seifert R

Subjects

Animals, Binding, Competitive, GTP Phosphohydrolases metabolism, Guanidines chemistry, Guinea Pigs, Histamine Agonists chemistry, Histamine H1 Antagonists pharmacology, Humans, Imidazoles chemistry, Insecta genetics, Molecular Structure, Pyrilamine pharmacology, Receptors, Histamine H1 genetics, Receptors, Histamine H2 genetics, Species Specificity, Structure-Activity Relationship, Transfection, Guanidines pharmacology, Histamine Agonists pharmacology, Imidazoles pharmacology, Receptors, Histamine H1 metabolism, Receptors, Histamine H2 metabolism

Abstract

Both the histamine H1-receptor (H1R) and H2-receptor (H2R) exhibit pronounced species selectivity in their pharmacological properties; i.e., bulky agonists possess higher potencies and efficacies at guinea pig (gp) than at the corresponding human (h) receptor isoforms. In this study, we examined the effects of NG-acylated imidazolylpropylguanidines substituted with a single phenyl or cyclohexyl substituent on H1R and H2R species isoforms expressed in Sf9 insect cells. N1-(3-Cyclohexylbutanoyl)-N2-[3-(1H-imidazol-4-yl)propyl]guanidine (UR-AK57) turned out to be the most potent hH2R agonist identified so far (EC50 of 23 nM in the GTPase assay at the hH2R-Gsalpha fusion protein expressed in Sf9 insect cells). UR-AK57 was almost a full-hH2R agonist and only slightly less potent and efficacious than at gpH2R-Gsalpha. Several NG-acylated imidazolylpropylguanidines showed similar potency at hH2R and gpH2R. Most unexpectedly, UR-AK57 exhibited moderately strong partial hH1R agonism with a potency similar to that of histamine, whereas at gpH1R, UR-AK57 was only a very weak partial agonist. Structure/activity relationship studies revealed that both the alkanoyl chain connecting the aromatic or alicyclic substituent with the guanidine moiety and the nature of the carbocycle (cyclohexyl versus phenyl ring) critically determine the pharmacological properties of this class of compounds. Collectively, our data show that gpH1R and gpH R do not necessarily exhibit preference for bulky agonists (2) compared with hH1R and hH2R, respectively, and that UR-AK57 is a promising starting point for the development of both potent and efficacious hH1R and hH2R agonists.

Published

2006

18. Assessment of the influence of histaminergic actions on cocaine-like effects of 3alpha-diphenylmethoxytropane analogs.

Author

Campbell VC, Kopajtic TA, Newman AH, and Katz JL

Subjects

Animals, Benztropine analogs & derivatives, Benztropine metabolism, Benztropine pharmacology, Binding, Competitive drug effects, Brain drug effects, Brain metabolism, Cocaine analogs & derivatives, Cocaine metabolism, Discrimination Learning drug effects, Dopamine Uptake Inhibitors metabolism, Dopamine Uptake Inhibitors pharmacology, Guanidines metabolism, Histamine Agonists metabolism, Histamine Agonists pharmacology, Histamine H1 Antagonists metabolism, Histamine H1 Antagonists pharmacology, In Vitro Techniques, Male, Methylhistamines metabolism, Motor Activity drug effects, Pyrilamine metabolism, Rats, Rats, Sprague-Dawley, Receptors, Histamine H3 drug effects, Cocaine pharmacology, Histamine physiology, Tropanes pharmacology

Abstract

Previous studies demonstrated that analogs of benztropine (BZT) possess high affinity for the dopamine (DA) transporter (DAT) but generally have behavioral effects different from those of cocaine, suggesting either unique actions at the DA transporter or that another action of these drugs interferes with cocaine-like effects. Because the parent compound has histamine-antagonistic effects, the affinity of its analogs for histamine H(1), H(2), and H(3) receptors were compared with DA transporter affinity to assess whether those differences predicted the amount of cocaine-like activity. All of the compounds displaced [(3)H]mepyramine from H(1), [(125)I]iodoaminopotentidine from H(2), and [(3)H]N-alpha-methylhistamine from H(3) histamine receptors with affinities ranging from 15.7 to 37,600, 218 to >4430, and 4040 to >150,000 nM, respectively. Affinities at histamine H(1) receptors were, respectively, approximately 25- or 300-fold greater than those at H(2) or H(3) histamine receptors. Relative affinities for H(1) and DAT binding did not reliably predict the degree of cocaine-like stimulation of locomotor activity. In addition, interactions of various histaminic agents with cocaine assessed whether an action at any of the histamine sites could interfere with cocaine-like effects. None of the histaminic agents fully substituted for cocaine in rats trained to discriminate 10 mg/kg cocaine from saline nor did any of the compounds antagonize or otherwise diminish the discriminative stimulus effects of cocaine. The results suggest that affinity for histamine receptors cannot account for the diminished cocaine-like effects of the BZT analogs and suggest alternatively that these compounds have actions different from those of cocaine but likely mediated by their interaction with the DAT.

Published

2005

19. Evaluation of histamine H1-, H2-, and H3-receptor ligands at the human histamine H4 receptor: identification of 4-methylhistamine as the first potent and selective H4 receptor agonist.

Author

Lim HD, van Rijn RM, Ling P, Bakker RA, Thurmond RL, and Leurs R

Subjects

Cell Line, Humans, Imidazoles metabolism, Indoles metabolism, Isothiuronium analogs & derivatives, Isothiuronium metabolism, Ligands, Piperazines metabolism, Radioligand Assay, Receptors, G-Protein-Coupled metabolism, Receptors, Histamine metabolism, Receptors, Histamine H4, Histamine Agonists pharmacology, Methylhistamines pharmacology, Receptors, G-Protein-Coupled agonists, Receptors, Histamine H1 metabolism, Receptors, Histamine H2 metabolism, Receptors, Histamine H3 metabolism

Abstract

The histamine H(4) receptor (H(4)R) is involved in the chemotaxis of leukocytes and mast cells to sites of inflammation and is suggested to be a potential drug target for asthma and allergy. So far, selective H(4)R agonists have not been identified. In the present study, we therefore evaluated the human H(4)R (hH(4)R) for its interaction with various known histaminergic ligands. Almost all of the tested H(1)R and H(2)R antagonists, including several important therapeutics, displaced less than 30% of specific [(3)H]histamine binding to the hH(4)R at concentrations up to 10 microM. Most of the tested H(2)R agonists and imidazole-based H(3)R ligands show micromolar-to-nanomolar range hH(4)R affinity, and these ligands exert different intrinsic hH(4)R activities, ranging from full agonists to inverse agonists. Interestingly, we identified 4-methylhistamine as a high-affinity H(4)R ligand (K(i) = 50 nM) that has a >100-fold selectivity for the hH(4)R over the other histamine receptor subtypes. Moreover, 4-methylhistamine potently activated the hH(4)R (pEC(50) = 7.4 +/- 0.1; alpha = 1), and this response was competitively antagonized by the selective H(4)R antagonist JNJ 7777120 [1-[(5-chloro-1H-indol-2-yl)-carbonyl]-4-methylpiperazine] (pA(2) = 7.8). The identification of 4-methylhistamine as a potent H(4)R agonist is of major importance for future studies to unravel the physiological roles of the H(4)R.

Published

2005

20. G protein-dependent pharmacology of histamine H3 receptor ligands: evidence for heterogeneous active state receptor conformations.

Author

Krueger KM, Witte DG, Ireland-Denny L, Miller TR, Baranowski JL, Buckner S, Milicic I, Esbenshade TA, and Hancock AA

Subjects

Animals, Cyclic AMP metabolism, Electric Stimulation, GTP-Binding Proteins chemistry, GTP-Binding Proteins genetics, Guanosine 5'-O-(3-Thiotriphosphate) metabolism, Guinea Pigs, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Histamine Release drug effects, Ileum drug effects, Ileum metabolism, Imidazoles pharmacology, Ligands, Male, Membranes metabolism, Neurotransmitter Agents metabolism, Protein Conformation, Radioligand Assay, Rats, Rats, Sprague-Dawley, Receptors, G-Protein-Coupled drug effects, Signal Transduction drug effects, Transfection, GTP-Binding Proteins physiology, Receptors, Histamine H3 drug effects

Abstract

Previously reported pharmacological studies using the imidazole-containing histamine H3 receptor ligands GT-2331 (Cipralisant) and proxyfan resulted in a range of classifications (antagonist, agonist, and protean) for these compounds. We examined the role that the signaling system, with particular emphasis on the type of G protein, had on the pharmacology observed for H3 ligands. Ligands were assessed using assays measuring neurotransmitter release, cAMP, and guanosine 5'-O-(3-[35S]thio)triphosphate ([35S]GTPgammaS) binding. Whereas clobenpropit and ciproxifan were consistently antagonists, GT-2331, proxyfan, and imetit exhibited differential activity. Although GT-2331 and proxyfan exhibited little agonist activity in neurotransmitter release assays, both demonstrated full agonism relative to (R)-alpha-methylhistamine in cAMP assays. In [35S]GTPgammaS binding assays, GT-2331 and proxyfan demonstrated partial agonism. Imetit showed full agonism in most assays, but it was slightly less efficacious in a neurotransmitter release assay and in [35S]GTPgammaS binding at the human H3 receptor. To further examine these ligands, we coexpressed G alpha16 or chimeric G alpha q/i5 in human embryonic kidney cells expressing the human H3 receptor and assayed intracellular calcium and cAMP levels. GT-2331, proxyfan, and imetit demonstrated full agonism in all assays of cAMP activity. However, in cells expressing G alpha16, they exhibited minimal agonism in calcium mobilization assays, whereas imetit showed partial agonism. When G alpha q/i5 was used, the activity of both GT-2331 and proxyfan increased, whereas imetit became a full agonist. These results demonstrate that GT-2331 and proxyfan's differential pharmacology at the H3 receptor depends on the type of G protein used and provide indirect evidence for differential ligand-bound active states that mediate signaling by the H3 receptor.

Published

2005

21. Pharmacological characterization of the novel histamine H3-receptor antagonist N-(3,5-dichlorophenyl)-N'-[[4-(1H-imidazol-4-ylmethyl)phenyl]-methyl]-urea (SCH 79687).

Author

McLeod RL, Rizzo CA, West RE Jr, Aslanian R, McCormick K, Bryant M, Hsieh Y, Korfmacher W, Mingo GG, Varty L, Williams SM, Shih NY, Egan RW, and Hey JA

Subjects

Animals, Cats, Drug Interactions, Female, Guinea Pigs, Haplorhini, Histamine Agonists pharmacokinetics, Histamine Antagonists pharmacokinetics, Humans, Ileum drug effects, Ileum metabolism, Loratadine pharmacology, Male, Methylhistamines pharmacokinetics, Methylhistamines pharmacology, Nasal Decongestants pharmacology, Rats, Receptors, Histamine H3 drug effects, Saphenous Vein drug effects, Saphenous Vein metabolism, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Imidazoles pharmacology, Phenylurea Compounds pharmacology, Receptors, Histamine H3 metabolism

Abstract

We present the pharmacological and pharmacokinetic profiles of a novel histamine H3 receptor antagonist, N-(3,5-dichlorophenyl)-N'-[[4-(1H-imidazol-4-ylmethyl)phenyl]-methyl]-urea (SCH 79687). The H3-receptor binding Ki values for SCH 79687 were 1.9 and 13 nM in the rat and guinea pig (GP), respectively. The Ki values for SCH 79687 at histamine H1 and H2 receptors were greater than 1 microM. SCH 79687 showed a 41- and 82-fold binding selectivity for the H3 receptor over alpha 2A-adrenoceptors and imidazoline I2, and >500-fold H3 selectivity compared with over 60 additional receptors. The pA2 value for SCH 79687 in the GP ileum electrical field-stimulated (EFS) contraction was 9.6 +/- 0.3. Similar H3 antagonist activity was observed in the EFS cryopreserved and fresh tissue isolated human saphenous vein (HSV) assays (pKb = 9.4 +/- 0.3 and 10.1 +/- 0.4). SCH 79687 (30 nM) did not block clonidine-induced inhibition of EFS-induced contractions in HSV. SCH 79687 (ED50 = 0.3 mg/kg i.v.) attenuated (R)-alpha-methylhistamine inhibition of sympathetic hypertensive responses in the GP. At the time of activity evaluation, the GP plasma SCH 79687 concentration was 25 ng/ml at the dose of 0.3 mg/kg i.v. In feline nasal studies, combined administration of SCH 79687 (3 mg/kg i.v.) and the H1-antagonist loratadine (3 mg/kg i.v.), at individual doses that do not produce decongestion, inhibited the compound 48/80-induced congestion by 47%. The alpha-adrenergic agonist phenylpropanolamine (PPA; 1 mg/kg i.v.) also attenuated compound 48/80 nasal responses by 42%. Unlike the H3/H1 combination that did not affect blood pressure (BP), PPA (1 mg/kg i.v.) significantly increased BP compared with control animals by a maximum of 31 mm Hg. Orally, SCH 79687 (10 mg/kg) plus loratadine (10 mg/kg) also produced decongestion without effects on BP. In pharmacokinetic studies, oral dosing with SCH 79687 in the rat (10 mg/kg) and monkey (3 mg/kg) achieved plasma Cmax and area under the curve values greater than 1.5 and 12.1 microg. h/ml, respectively. SCH 79687 is an orally active H3 antagonist with a good pharmacokinetic profile that, in combination with an H1 antagonist, demonstrates decongestant efficacy comparable with oral sympathomimetic decongestants but without hypertensive liabilities.

Published

2003

22. Multiple differences in agonist and antagonist pharmacology between human and guinea pig histamine H1-receptor.

Author

Seifert R, Wenzel-Seifert K, Burckstummer T, Pertz HH, Schunack W, Dove S, Buschauer A, and Elz S

Subjects

Amino Acid Sequence, Animals, Binding Sites, Electrophoresis, GTP Phosphohydrolases metabolism, Guinea Pigs, Histamine, Humans, Molecular Sequence Data, Protein Conformation, Receptors, Histamine H1 chemistry, Receptors, Histamine H1 drug effects, Receptors, Histamine H2 drug effects, Receptors, Histamine H2 metabolism, Recombinant Proteins chemistry, Recombinant Proteins drug effects, Recombinant Proteins metabolism, Species Specificity, Tritium, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Pyrilamine pharmacology, Receptors, Histamine H1 metabolism

Abstract

Species isoforms of histamine H2-, H3-, and H4-receptors differ in their pharmacological properties. The study aim was to dissect differences between the human H1R (hH1R) and guinea pig H1R (ghH1R). We coexpressed hH1R and gpH1R with regulators of G-protein signaling in Sf9 insect cells and analyzed the GTPase activity of Gq-proteins. Small H1R agonists showed similar effects at hH1R and gpH1R, whereas bulkier 2-phenylhistamines and histaprodifens were up to approximately 10-fold more potent at gpH1R than at hH1R. Most 2-phenylhistamines and histaprodifens were more efficacious at gpH1R than at hH1R. Several first-generation H1R antagonists were approximately 2-fold, and arpromidine-type H1R antagonists up to approximately 10-fold more potent at gpH1R than at hH1R. [3H]Mepyramine competition binding studies confirmed the potency differences of the GTPase studies. Phe-153-->Leu-153 or Ile-433-->Val-433 exchange in hH1R (hH1R-->gpH1R) resulted in poor receptor expression, low [3H]mepyramine affinity, and functional inactivity. The Phe-153-->Leu-153/Ile-433-->Val-433 double mutant expressed excellently but only partially changed the pharmacological properties of hH1R. Small H1R agonists and 2-phenylhistamines interacted differentially with human and guinea pig H2R in terms of potency and efficacy, respectively. Our data show the following: 1) there are differences in agonist- and antagonist-pharmacology of hH1R and gpH1R encompassing diverse classes of bulky ligands. These differences may be explained by higher conformational flexibility of gpH1R relative to hH1R; 2) Phe-153 and Ile-433 are critical for proper folding and expression of hH1R; and 3) H2R species isoforms distinguish between H1R agonists.

Published

2003

23. A novel phenylaminotetralin radioligand reveals a subpopulation of histamine H(1) receptors.

Author

Booth RG, Moniri NH, Bakker RA, Choksi NY, Nix WB, Timmerman H, and Leurs R

Subjects

Animals, Binding, Competitive drug effects, CHO Cells, COS Cells, Cell Membrane drug effects, Cell Membrane metabolism, Cell Membrane ultrastructure, Chlorocebus aethiops, Cricetinae, DNA, Complementary biosynthesis, DNA, Complementary genetics, Guinea Pigs, Histamine pharmacology, Humans, Ileum drug effects, Ileum metabolism, Inositol Phosphates metabolism, Ligands, NF-kappa B drug effects, Pyrilamine, Receptors, Histamine H1 genetics, Thermodynamics, Transfection, Type C Phospholipases metabolism, Histamine Agonists pharmacology, Radiopharmaceuticals pharmacology, Receptors, Histamine H1 drug effects, Tetrahydronaphthalenes pharmacology

Abstract

Previously, (-)-trans-1-phenyl-3-N,N-dimethylamino-1,2,3,4-tetrahydronaphthalene ([-]-trans-H(2)-PAT) was shown to activate stereospecifically histamine H(1) receptors coupled to modulation of tyrosine hydroxylase activity in guinea pig and rat forebrain in vitro and in vivo. Furthermore, the novel radioligand [(3)H](-)-trans-H(2)-PAT was shown to label selectively H(1) receptors in guinea pig and rat brain with high affinity (K(D), ~0.1 and 0.5 nM, respectively) and a B(max) about 50 and 15%, respectively, of that observed for the H(1) antagonist radioligand [(3)H]mepyramine. In the current study, [(3)H](-)-trans-H(2)-PAT-labeled cloned guinea pig and human H(1) receptors in Chinese hamster ovary (CHO) cell membranes with high affinity (K(D), ~0.08 and 0.23 nM, respectively) and a B(max) about 15% of that observed for [(3)H]mepyramine. The binding of H(2)-PAT to H(1) receptors in both CHO-H(1) cell lines was stereoselective with the (-)-trans-isomer having affinity (K(i), ~1.5 nM) about 4-, 20-, and 50-times higher than the (-)-cis-, (+)-trans-, and (+)-cis-isomers, respectively; the affinity of (-)-trans-H(2)-PAT was unaffected by excess GTP. In functional assays, (-)-trans-H(2)-PAT was a full antagonist of histamine H(1)-mediated stimulation of phospholipase C (PLC) and [(3)H]inositol phosphates (IP) formation in CHO-H(1) cells, a full inverse agonist of constitutively active H(1) receptors in COS-7-H(1) cells, and a full competitive antagonist (pA(2) = 9.2) of histamine H(1)-mediated contraction of guinea pig ileum. It is concluded that (-)-trans-H(2)-PAT is an antagonist at H(1) receptors coupled to PLC/IP formation and smooth muscle contraction. Meanwhile, the observation that [(3)H](-)-trans-H(2)-PAT labels only a subpopulation of H(1) receptors and that (-)-trans-H(2)-PAT activates H(1) receptors coupled to modulation of tyrosine hydroxylase suggests that there may be post-translational H(1) receptor heterogeneity.

Published

2002

24. The role of transmembrane helix 5 in agonist binding to the human H3 receptor.

Author

Uveges AJ, Kowal D, Zhang Y, Spangler TB, Dunlop J, Semus S, and Jones PG

Subjects

Amino Acid Sequence, Cells, Cultured, Colforsin pharmacology, Cyclic AMP metabolism, Humans, Models, Molecular, Molecular Sequence Data, Mutagenesis, Mutation, Radioligand Assay, Receptors, Histamine H3 genetics, Sequence Homology, Amino Acid, Histamine Agonists pharmacology, Receptors, Histamine H3 metabolism

Abstract

We have used alanine scanning mutagenesis to identify residues in transmembrane domain 5 of the histamine H3 receptor that are important for agonist binding. All of the mutants generated were functionally expressed as demonstrated by their ability to bind [(125)I]iodoproxyfan with comparable affinity to the wild-type receptor and their ability to inhibit forskolin-stimulated cAMP formation when activated by histamine. Many mutations produced small changes in the potency of histamine, but the most pronounced reduction in potency and affinity of the agonists, histamine, R-alpha-methylhistamine, imetit, and impentamine, was seen with mutation of glutamate 206. Our modeling suggests that this residue plays a key role in ligand binding by interacting with the imidazole ring of histamine. Interestingly, L199A greatly reduced agonist potency in functional assays but had only minor effects on agonist affinity, implicating a role for this residue in the mechanism of receptor activation. We also studied the functional effects of the mutations by linking the receptor to calcium signaling using a chimeric G protein. A comparison of the two functional assays demonstrated contrasting effects on agonist activity. Histamine, imetit, and impentamine were full agonists in the cAMP assay, but imetit exhibited only partial agonist activity through the chimeric G protein. Furthermore, impentamine, another potent agonist in the cAMP assay, was only able to activate the E206A mutant in the calcium assay despite being inactive at the wild-type receptor. These observations suggest that the agonist receptor complexes formed by these three different H3 agonists are not conformationally equivalent.

Published

2002

25. Histamine regulation of interleukin-18-initiating cytokine cascade is associated with down-regulation of intercellular adhesion molecule-1 expression in human peripheral blood mononuclear cells.

Author

Takahashi HK, Yoshida A, Iwagaki H, Yoshino T, Itoh H, Morichika T, Yokoyama M, Akagi T, Tanaka N, Mori S, and Nishibori M

Subjects

Cell Aggregation drug effects, Dose-Response Relationship, Drug, Flow Cytometry, Histamine Agonists pharmacology, Humans, Indicators and Reagents, Monocytes drug effects, Receptors, Histamine H2 drug effects, Cytokines biosynthesis, Down-Regulation drug effects, Histamine physiology, Intercellular Adhesion Molecule-1 biosynthesis, Interleukin-18 physiology, Monocytes metabolism

Abstract

In the previous study, we demonstrated that interleukin (IL)-18 up-regulated intercellular adhesion molecule-1 (ICAM-1) expression on monocytes in human peripheral blood mononuclear cells (PBMC) and that heterotypic interaction between monocytes/T or NK cells through ICAM-1/LFA-1 intensified the production of IL-12, interferon-gamma (IFN-gamma), and tumor necrosis factor-alpha (TNF-alpha) in PBMC. In the present study, we demonstrate that histamine inhibited the ICAM-1 expression in monocytes induced by IL-18 using flow cytometry and that the responses of IL-12, IFN-gamma, and TNF-alpha induced by IL-18 were concentration dependently inhibited by coexisting histamine, whereas IL-18-inhibited IL-10 production was reversed by the same concentrations of histamine. The modulatory effects of histamine on ICAM-1 expression and cytokine production were all concentration dependently antagonized by famotidine but not by d-chlorpheniramine and thioperamide, and were mimicked by selective H(2)-receptor agonists but not by H(1)- and H(3)-receptor agonists, indicating the involvement of H(2)-receptors in histamine action. The inhibition of IL-18-induced IFN-gamma by histamine was ascribed to the strong inhibition of IL-12 production by histamine. Histamine thus operates the negative feedback mechanism against IL-18-activated cytokine cascade through the strong inhibitory effect on ICAM-1 expression and IL-12 production in monocytes, contributing to the formation of diverse pattern of cytokine activation from Th1 to Th2, depending on the monocyte/macrophage activation and cytokine environment.

Published

2002

26. Similar apparent constitutive activity of human histamine H(2)-receptor fused to long and short splice variants of G(salpha).

Author

Wenzel-Seifert K, Kelley MT, Buschauer A, and Seifert R

Subjects

Alternative Splicing, Animals, Cell Membrane metabolism, Cells, Cultured, Cimetidine pharmacology, GTP Phosphohydrolases drug effects, GTP Phosphohydrolases metabolism, GTP-Binding Protein alpha Subunits, Gs genetics, Guanidine analogs & derivatives, Guanidine pharmacology, Guanosine 5'-O-(3-Thiotriphosphate) metabolism, Histamine Agonists pharmacology, Histamine H2 Antagonists pharmacology, Humans, Insecta, Radioligand Assay, Receptors, Histamine H2 genetics, Recombinant Fusion Proteins metabolism, Sulfur Radioisotopes, Transfection, Tritium, Cimetidine analogs & derivatives, GTP-Binding Protein alpha Subunits, Gs metabolism, Receptors, Histamine H2 metabolism

Abstract

Fusion proteins allow for the analysis of receptor/G protein coupling under defined conditions. The beta(2)-adrenoceptor (beta(2)AR) fused to the long splice variant of G(salpha) (G(salphaL)) exhibits a higher apparent constitutive activity than the beta(2)-adrenoceptor fused to the short splice variant of G(salpha) (G(salphaS)). Experimentally, this results in higher efficacy and potency of partial agonists and in higher efficacy of inverse agonists at the beta(2)AR fused to G(salphaL) relative to the beta(2)AR fused to G(salphaS), indicating that the agonist-free beta(2)AR and the beta(2)AR occupied by partial agonists promote GDP dissociation from G(salphaL) more efficiently than from G(salphaS). In fact, the GDP affinity of G(salphaS) fused to the beta(2)AR is higher than the GDP affinity of G(salphaL) fused to the beta(2)AR. We asked the question whether the histamine H(2)-receptor (H(2)R) exhibits similar coupling to G(salpha) splice variants as the beta(2)AR. To address this question, we studied H(2)R-G(salpha) fusion proteins expressed in Sf9 cells. In contrast to beta(2)AR-G(salpha) fusion proteins, the potencies and efficacies of partial agonists and the efficacies of inverse agonists were similar at the H(2)R fused to G(salphaL) and G(salphaS) as assessed by guanosine-5'-O-(3-thio)triphosphate binding and/or steady-state GTPase activity. However, the time course analysis of guanosine-5'-O-(3-thio)triphosphate binding indicated that G(salphaS) fused to the H(2)R possesses a higher GDP-affinity than G(salphaL) fused to the H(2)R. Our data show that the H(2)R fused to G(salphaL) and G(salphaS) possesses similar constitutive activity and is insensitive to differences in GDP affinity of G(salpha) splice variants. Thus, GDP affinity of G proteins does not generally determine constitutive activity of receptors.

Published

2001

27. Cloning and characterization of a novel human histamine receptor.

Author

Morse KL, Behan J, Laz TM, West RE Jr, Greenfeder SA, Anthes JC, Umland S, Wan Y, Hipkin RW, Gonsiorek W, Shin N, Gustafson EL, Qiao X, Wang S, Hedrick JA, Greene J, Bayne M, and Monsma FJ Jr

Subjects

Amino Acid Sequence, Cells, Cultured, Cloning, Molecular, Histamine Agonists pharmacology, Humans, Imidazoles pharmacology, Molecular Sequence Data, RNA, Messenger genetics, RNA, Messenger metabolism, Radioligand Assay, Receptors, Histamine drug effects, Receptors, Histamine H3 drug effects, Sequence Homology, Amino Acid, Thiourea pharmacology, Tissue Distribution, Transfection, Histamine metabolism, Receptors, Histamine genetics, Receptors, Histamine H3 genetics, Thiourea analogs & derivatives

Abstract

Histamine exerts its numerous physiological functions through interaction with G protein-coupled receptors. Three such receptors have been defined at both the pharmacological and molecular level, while pharmacological evidence hints at the existence of further subtypes. We report here the cloning and characterization of a fourth histamine receptor subtype. Initially discovered in an expressed-sequence tag database, the full coding sequence (SP9144) was subsequently identified in chromosome 18 genomic sequence. This virtual coding sequence exhibited highest homology to the H(3) histamine receptor and was used to generate a full-length clone by polymerase chain reaction (PCR). The distribution of mRNA encoding SP9144 was restricted to cells of the immune system as determined by quantitative PCR. HEK-293 cells transiently transfected with SP9144 and a chimeric G protein alpha-subunit (Galpha(q/i1,2)) exhibited increases in intracellular [Ca(2+)] in response to histamine but not other biogenic amines. SP9144-transfected cells exhibited saturable, specific, high-affinity binding of [(3)H]histamine, which was potently inhibited by H(3) receptor-selective compounds. The rank order and potency of these compounds at SP9144 differed from the rank order at the H(3) receptor. Although SP9144 apparently coupled to Galpha(i), HEK-293 cells stably transfected with SP9144 did not exhibit histamine-mediated inhibition of forskolin-stimulated cAMP levels. However, both [(35)S]GTPgammaS binding and phosphorylation of mitogen-activated protein kinase were stimulated by histamine via SP9144 activation. In both of these assays, SP9144 exhibited evidence of constitutive activation. Taken together, these data demonstrate that SP9144 is a unique, fourth histamine receptor subtype.

Published

2001

28. Signaling mechanisms coupled to presynaptic A(1)- and H(3)-receptors in the inhibition of cholinergic contractile responses of the guinea pig ileum.

Author

Lee JJ and Parsons ME

Subjects

Acetylcholine metabolism, Adenosine pharmacology, Animals, Calcium Channel Blockers pharmacology, Cyclic AMP metabolism, Cyclic AMP physiology, Cyclic GMP metabolism, Cyclic GMP physiology, Electric Stimulation, Female, Guinea Pigs, Histamine Agonists pharmacology, Ileum drug effects, Ileum innervation, Ileum physiology, Male, Methylhistidines pharmacology, Muscle Contraction drug effects, Muscle, Smooth drug effects, Muscle, Smooth innervation, Neurons drug effects, Neurons metabolism, Signal Transduction drug effects, Synaptic Transmission physiology, Acetylcholine antagonists & inhibitors, Muscle Contraction physiology, Muscle, Smooth physiology, Receptors, Histamine H3 physiology, Receptors, Purinergic P1 physiology, Signal Transduction physiology

Abstract

The mechanisms coupled to adenosine A(1)- and histamine H(3)-receptors have been examined in the presynaptic inhibition of acetylcholine (ACh) release from the guinea pig ileum. Electrically evoked twitch contractions were used as a measure of neuronal ACh release. A(1)- and H(3)-receptors were activated by adenosine and R-(alpha)-methylhistamine (RAMH), respectively. The neuroinhibitory effect of adenosine and RAMH was augmented in the presence of the N-type Ca(2+) channel blocker, omega-conotoxin GVIA but unaffected by the L-type Ca(2+) channel blocker, nifedipine. The irreversible adenylyl cyclase inhibitor, MDL-12330A, potentiated the action of both adenosine and RAMH. Conversely, neither agonist was affected by the cAMP phosphodiesterase III and IV inhibitors, SKF-95654 and Ro-20-1724, respectively, or the cAMP antagonist, (R(p))-adenosine 3',5'-cyclic monophosphorothioate triethylamine. The neuromodulatory effect of adenosine, only, was potentiated by the cGMP phosphodiesterase V inhibitors, SKF-96231 and 1,3-dimethyl-6-(2-propoxy-5-methanesulfonylamidophenyl)- pyrazolo[3, 4-d]pyrimidin-4-(5H)-one but was unmodified by the cGMP analog, 8-bromo-cGMP or the guanylyl cyclase inhibitors, N-methylhydroxylamine and 1H-[1,2,4]oxadiazolo[4, 3-a]quinoxaline-1-one (ODQ). N-Methylhydroxylamine reduced, and ODQ potentiated, the inhibitory action of H(3)-receptor activation, but 8-bromo-cGMP was without effect. The study suggests that presynaptic A(1)- and H(3)-receptors inhibit cholinergic neurotransmission in the guinea pig ileum by limiting the availability of intraneuronal Ca(2+) via inhibition of N-type Ca(2+) channels. The balance of evidence does not support the involvement of the adenylyl cyclase/cAMP or guanylyl cyclase/cGMP systems.

Published

2000

29. Anti-inflammatory and antinociceptive properties of BP 2-94, a histamine H(3)-receptor agonist prodrug.

Author

Rouleau A, Stark H, Schunack W, and Schwartz JC

Subjects

Animals, Cystitis drug therapy, Edema drug therapy, Imines pharmacokinetics, Male, Methylhistamines pharmacology, Mice, Phenols pharmacokinetics, Analgesics pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Histamine Agonists pharmacology, Imines pharmacology, Phenols pharmacology, Prodrugs pharmacology, Receptors, Histamine H3 drug effects

Abstract

BP 2-94 is an azomethine prodrug of (R)-alpha-methylhistamine [(R)-alpha-MeHA], a potent and selective histamine H(3)-receptor agonist. When administered orally to mice BP 2-94 was distributed to various peripheral tissues where it released the active drug. BP 2-94 displayed anti-inflammatory and antinociceptive properties in mice. It dose-dependently inhibited carrageenan-induced paw edema with an ED(50) value of 0.17 +/- 0.05 micromol/kg (p.o.) and a maximal effect of 47%. It also reduced Freund's complete adjuvant-induced paw edema in preventive as well as in curative fashion. Repeated oral administrations of BP 2-94 reduced the pre-established Freund's complete adjuvant-induced edema with an ED(50) value of 5 +/- 2 micromol/kg (p.o.) and a maximal effect of 47%. The antiedema effects of BP 2-94 and indomethacin were additive. BP 2-94 was also efficient in reducing cyclophosphamide-induced cystitis in mice: it decreased leukocyte infiltration by 62% and plasma protein extravasation by 73% in urinary bladder. In addition, BP 2-94 displayed antinociceptive activity in the capsaicin-induced licking test via H(3)-receptor stimulation. Its antinociceptive effect was dose dependent, occurring with an ED(50) value of 0.4 +/- 0.1 micromol/kg (p.o.) and a maximal reduction of licking duration by 69%. No tolerance to the antinociceptive effect was observed after repeated administration of BP 2-94 for 3 days. These observations with BP 2-94 suggest that H(3)-receptor agonists might represent a novel class of anti-inflammatory and antinociceptive agents.

Published

2000

30. Histamine suppresses A-type potassium current in myenteric neurons from guinea pig small intestine.

Author

Starodub AM and Wood JD

Subjects

Animals, Cimetidine pharmacology, Cyclic AMP metabolism, Dimaprit pharmacology, Drug Interactions, Excitatory Postsynaptic Potentials drug effects, Excitatory Postsynaptic Potentials physiology, Guinea Pigs, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Intestine, Small drug effects, Male, Membrane Potentials drug effects, Membrane Potentials physiology, Myenteric Plexus cytology, Myenteric Plexus physiology, Neurons metabolism, Neurons physiology, Patch-Clamp Techniques, Potassium Channels physiology, Receptors, Histamine H2 physiology, Histamine pharmacology, Intestine, Small innervation, Myenteric Plexus drug effects, Neurons drug effects, Potassium Channel Blockers

Abstract

Perforated patch-clamp methods for recording ionic currents in the whole-cell configuration were used to test the hypothesis that the ionic mechanisms for the excitatory actions of histamine on enteric neurons include suppression of A-type K(+) current (I(A)). Histamine and the selective histamine H(2) receptor agonist, dimaprit, reduced the amplitude of I(A) without affecting the slope factor for I(A) steady-state inactivation curves. Suppression of I(A) was restricted to after hyperpolarization-type myenteric neurons that were immunoreactive for calbindin. The selective histamine H(2) receptor antagonist cimetidine suppressed the action of histamine and dimaprit. Elevation of intraneuronal cAMP by forskolin, a membrane-permeant analog of cAMP, and treatment with a phosphodiesterase inhibitor suppressed I(A.) The results are consistent with the hypothesis that suppression of I(A) is part of the ionic mechanism responsible for elevation of excitability during both slow synaptic excitation and slow synaptic excitation-like responses evoked by paracrine mediators, such as histamine, in after hyperpolarization-type myenteric neurons.

Published

2000

31. Differential effect of histamine 3 receptor-active agents on brain, but not peritoneal, mast cell activation.

Author

Rozniecki JJ, Letourneau R, Sugiultzoglu M, Spanos C, Gorbach J, and Theoharides TC

Subjects

Animals, Brain metabolism, Cell Survival drug effects, Histamine Release drug effects, Male, Mast Cells physiology, Mast Cells ultrastructure, Neurons metabolism, Rats, Rats, Sprague-Dawley, Serotonin metabolism, Brain cytology, Brain drug effects, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Mast Cells drug effects, Methylhistamines pharmacology, Peritoneal Cavity cytology, Piperidines pharmacology, Receptors, Histamine H3 physiology

Abstract

The activation of presynaptic histamine 3 (H(3)) receptors inhibits the release of histamine and other neurotransmitters from central nervous system neurons. Rat brain mast cells (MCs) release histamine and 5-hydroxytryptamine (5-HT) in response to neuropeptides and neurotransmitters secreted from adjacent neurons. Dura MCs also degranulate in response to antidromic trigeminal nerve stimulation and with acute psychological stress. Such findings have implicated brain MCs in certain neuroinflammatory disorders, such as migraines. We investigated the ultrastructural appearance of control and stimulated thalamic/hypothalamic (brain) MCs before and after treatment with the H(3) receptor agonist N(alpha)-methylhistamine (N(alpha)-mH) and the H(3) receptor antagonist thioperamide (Th). Ultrastructural investigation of brain MCs stimulated with compound 48/80 revealed extensive intragranular changes that paralleled 5-HT secretion but without degranulation by exocytosis typical of connective tissue MCs. N(alpha)-mH significantly reduced these morphological changes, as well as 5-HT release from brain MCs and neurons stimulated with KCl; conversely, Th augmented both histamine and 5-HT release from brain neurons and MCs. Neither N(alpha)-mH nor Th had any effect on peritoneal MCs. Simultaneous addition of both drugs largely antagonized each other's effects on brain MC activation and 5-HT secretion. Ultrastructural observations and lack of lactic dehydrogenase release in the perfusate excluded any cytotoxic effect. The ability of H(3) agonists to inhibit brain MC activation, as well as secretion of 5-HT from both brain MCs and neurons, may be useful in the management of migraines.

Published

1999

32. The role of histamine H1, H2 and H3 receptors on enteric ascending synaptic transmission in the guinea pig ileum.

Author

Izzo AA, Costa M, Mascolo N, and Capasso F

Subjects

Animals, Cimetidine pharmacology, Dimaprit pharmacology, Electric Stimulation, Guinea Pigs, Histamine pharmacology, Histamine Agonists pharmacology, Histamine Antagonists pharmacology, Male, Motor Neurons drug effects, Motor Neurons metabolism, Muscle Contraction, Pyrilamine pharmacology, Receptors, Histamine drug effects, Synaptic Transmission drug effects, Ileum innervation, Muscle, Smooth innervation, Receptors, Histamine metabolism

Abstract

The role of histamine H1-, H2- and H3-receptors was studied on neural transmission in ascending excitatory pathways of the guinea pig ileum. A two-compartment (oral and anal compartments) bath was used: ascending neural pathways were activated by electrical stimulation in the anal compartment and the resulting contraction of the circular muscle in the oral compartment was recorded. Drugs were applied in the anal compartment and each agonist was evaluated in the presence of the antagonists of the other two receptors. In the presence of cimetidine (10 microM) and thioperamide (1 microM), histamine (0.03-3 microM) depressed the nerve-mediated contractions (5-70% inhibition, P <.05-.01). The inhibitory effect of histamine was antagonized by mepyramine. At the higher concentrations (10 and 30 microM), histamine elicited contractions of the circular muscle in the oral compartment, and these were abolished by mepyramine (1 microM) and tetrodotoxin (0.6 microM). The H2 agonists dimaprit (30 and 100 microM) and amphamine (0.1-300 microM) produced small contractions of the circular muscle in the oral compartment. These contractile responses were abolished by tetrodotoxin (0.6 microM) and cimetidine (10 microM). The H3 agonist R-alpha-methylhistamine (0.001-1 microM) inhibited (2-58%, P <.05) the nerve-mediated contractions. This inhibitory effect was antagonized by the H3 antagonist thioperamide. These results indicate that 1) histamine, acting at H1 receptors, at lower concentrations depresses synaptic transmission, although at higher concentrations activates the enteric excitatory ascending pathway; 2) activation of H2 receptors by H2 agonists stimulates the enteric excitatory ascending pathways and 3) activation of H3 receptors inhibits synaptic transmission.

Published

1998

33. Sch 50971, an orally active histamine H3 receptor agonist, inhibits central neurogenic vascular inflammation and produces sedation in the guinea pig.

Author

McLeod RL, Aslanian R, del Prado M, Duffy R, Egan RW, Kreutner W, McQuade R, and Hey JA

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal, Capillary Permeability drug effects, Electroencephalography drug effects, Guinea Pigs, Male, Motor Activity drug effects, Pentobarbital pharmacology, Reflex drug effects, Sleep drug effects, Histamine Agonists pharmacology, Hypnotics and Sedatives pharmacology, Imidazoles pharmacology, Migraine Disorders drug therapy, Pyrrolidines pharmacology, Receptors, Histamine H3 drug effects

Abstract

We studied the actions of Sch 50971, a novel histamine H3 receptor agonist, in an experimental neurogenic model of migraine and characterized its sedative and respiratory actions. Sch 50971 (i.v. and p.o) inhibited plasma protein extravasation in the dura mater of guinea pigs after electrical stimulation of the trigeminal ganglia. The minimum effective doses of Sch 50971 were 3.0 mg/kg i.v. and 10 mg/kg p.o., which produced a 40% and 42% decrease in plasma protein extravasation, respectively. The effects of Sch 50971 (3.0 mg/kg i.v. ) were blocked by the histamine H3 antagonist thioperamide (3.0 mg/kg i.v.). The 5-HT1D agonist, sumatriptan (0.3 mg/kg i.v.), and the histamine H3 agonist, (R)-alpha-methylhistamine (0.3 mg/kg), also inhibited plasma extravasation by 40 and 46%. In sedation studies, Sch 50971 (1-100 mg/kg p.o.) potentiated pentobarbital-induced sleep. The ED40 min for Sch 50971, the benzodiazepines triazolam and diazepam, the histamine H1 antagonist diphenhydramine and the H3 receptor agonist (R)-alpha-methylhistamine were 7.0, 0.5, 2.3, 14.1 and 23.4 mg/kg p. o., respectively. The sedative effects of oral Sch 50971 was blocked by thioperamide (10 microgram i.c.v.). The sedative activity of Sch 50971 was also examined using EEG activity, locomotor activity and sleep. In conscious guinea pigs, Sch 50971 (10 mg/kg p.o.) depressed locomotor activity, increased total sleep time and produced EEG patterns consistent with physiological sleep. Sch 50971 decreased beta wave activity but had no effects on delta wave activity, theta activity or alpha wave activity. In contrast, triazolam (1.0 mg/kg p. o.) depressed delta and theta wave activity and produced large increases in alpha and beta wave activity. In conclusion, Sch 50971 is an orally active, potent and selective agonist of histamine H3 receptors that may act to ameliorate the sequelae of migraine headaches, where activation of histamine H3 receptors may be beneficial. Sch 50971 also decreases motor activity and promotes EEG activity consistent with physiological sleep.

Published

1998

34. Bioavailability, antinociceptive and antiinflammatory properties of BP 2-94, a histamine H3 receptor agonist prodrug.

Author

Rouleau A, Garbarg M, Ligneau X, Mantion C, Lavie P, Advenier C, Lecomte JM, Krause M, Stark H, Schunack W, and Schwartz JC

Subjects

Adult, Animals, Dose-Response Relationship, Drug, Humans, Inflammation drug therapy, Male, Mice, Rats, Rats, Wistar, Biological Availability, Histamine Agonists pharmacology, Imines pharmacology, Nociceptors drug effects, Phenols pharmacology, Prodrugs pharmacology

Abstract

(R)alpha-Methylhistamine [(R)alpha-MeHA], a potent and selective histamine H3 receptor agonist in vitro and in vivo in rodents, was found to display comparatively low plasma level in healthy human volunteers, attributable to an extensive methylation of the drug's imidazole ring by histamine-N-methyltransferase. To limit this inactivation process, BP 2-94, ie., (R)-(-)-2-[[N-[1-(1H-imidazol-4-yl)-2-propyl]imino]phenylmethyl] phenol, was selected as a prodrug. A sensitive radioimmunoassay was developed to study the generation of (R)alpha-MeHA slowly released from BP 2-94 in vitro and in vivo by chemical hydrolysis. In mice after oral administration of BP 2-94 high levels of both prodrug and (R)alpha-MeHA were detected in plasma and various tissues except in the brain. In humans receiving 0.1 mmol BP 2-94 orally, plasma levels of (R)alpha-MeHA-like immunoreactivity decayed with a t(1/2) more than 24 hr, the area under the curve being two orders of magnitude higher than after oral administration of (R)alpha-MeHA. BP 2-94 displayed antiinflammatory and antinociceptive properties in rodents, related to the H3 receptor stimulation. It dose-dependently inhibited capsaicin-induced plasma protein extravasation in many rat tissues with ED50s of 0.6 to 14 micromol/kg p.o., and maximal reductions by 35 to 87%. BP 2-94 also reduced zymosan-induced paw swelling in mice with an ED50 of 1 micromol/kg p.o. and showed marked activity in the phenylbenzoquinone-induced writhing (ED50 = 0.03 micromol/kg, p.o.) or formalin tests in mice, but not in the hot plate jump test. From its pharmacokinetics and pharmacological profile BP 2-94 appears to be a promising novel therapeutic agent in disorders such as asthma, migraine or a variety of inflammatory diseases and pain associated with these disorders.

Published

1997

35. H3-receptor activation inhibits cholinergic stimulation of acid secretion in isolated rabbit fundic glands.

Author

Bado A, Laigneau JP, Moizo L, Cherifi Y, and Lewin MJ

Subjects

Animals, Carbachol pharmacology, Gastric Fundus metabolism, Gastric Mucosa metabolism, Histamine Antagonists pharmacology, In Vitro Techniques, Methylhistamines pharmacology, Muscarinic Antagonists pharmacology, N-Methylscopolamine, Piperidines pharmacology, Rabbits, Ranitidine pharmacology, Receptors, Muscarinic drug effects, Receptors, Muscarinic metabolism, Scopolamine Derivatives metabolism, Cholinergic Antagonists, Gastric Acid metabolism, Gastric Fundus drug effects, Gastric Mucosa drug effects, Histamine Agonists pharmacology, Receptors, Histamine H3 drug effects

Abstract

We previously reported evidence for H3-receptor inhibition of cholinergic stimulation of acid secretion by isolated rabbit gastric glands. Because this inhibition was unsensitive to H2 antagonists, we postulated that the parietal cell should bear a H3-receptor. In the present study, we investigated the effects of M1-M3 muscarinic receptors antagonists on carbachol- and thioperamide-induced acid secretion (14CAP uptake) by isolated rabbit gastric glands. Furthermore, we examined whether H3-receptor ligands could affect [3H]-N-methylscopolamine binding to the isolated rabbit parietal cells. Both carbachol and thioperamide concentration-dependently stimulated 14CAP uptake in the glands with maximal responses being achieved for 100 microM and 0.1 microM, respectively. These stimulations were concentration-dependently inhibited by the H3-receptor agonists R(alpha)-methylhistamine and imetit. Maximal inhibitions did not exceed 60% for 1 microM. The muscarinic receptor antagonists, hexa-sila-difenidol p-fluoro analog (M3), pirenzepine (M1) and gallamine (M2) inhibited carbachol-induced 14CAP uptake with IC50 of 50 nM, 10 microM and >> 100 microM, respectively. Thioperamide-induced 14CAP uptake was also inhibited by hexa-sila-difenidol p-fluoro analog and pirenzepine with IC50 of 90 nM and 12 microM, respectively; whereas gallamine had no effect. [3H]-N-methylscopolamine binding to isolated parietal cells was inhibited by atropine and pFHHSiD with IC50 of 15 nM and 132 nM, respectively. Neither R(alpha)-MeHA nor thioperamide did affect this binding although a H3-receptor inhibitory effect was observed on carbachol-induced 14CAP uptake by the cells. These data support that H3-receptor activation inhibits M3-mediated cholinergic stimulation of acid secretion through mechanisms operating downstream to the receptors sites.

Published

1995

36. Histamine H3-receptor signaling in the heart: possible involvement of Gi/Go proteins and N-type Ca++ channels.

Author

Endou M, Poli E, and Levi R

Subjects

Animals, Atrial Function, Cardiotonic Agents pharmacology, Drug Synergism, Electric Stimulation, Guinea Pigs, Heart innervation, Heart Atria drug effects, Histamine, Histamine Agonists pharmacology, In Vitro Techniques, Male, Methylhistamines pharmacology, Myocardial Contraction drug effects, Norepinephrine metabolism, Norepinephrine pharmacology, Signal Transduction drug effects, Sympathetic Nervous System drug effects, Sympathetic Nervous System physiology, omega-Conotoxin GVIA, Adrenergic Fibers physiology, Calcium Channels physiology, GTP-Binding Proteins physiology, Heart drug effects, Heart physiology, Peptides pharmacology, Pertussis Toxin, Receptors, Histamine H3 drug effects, Signal Transduction physiology, Virulence Factors, Bordetella pharmacology

Abstract

Discovered as inhibitory autoreceptors in central histaminergic pathways, histamine H3-receptors may also modulate peripheral cholinergic and central adrenergic function. Recently, H3-receptors were reported to inhibit adrenergic inotropic responses in guinea pig atria, possibly at prejunctional sites. We have assessed whether the H3-mediated modulation of cardiac adrenergic activities results from a reduction in norepinephrine release. We have found that (R) alpha-methylhistamine, the selective histamine H3-receptor agonist, attenuates the inotropic and chronotropic response of isolated guinea pig atria to transmural stimulation of adrenergic nerve endings. This attenuation was associated with a marked reduction in endogenous norepinephrine release. In contrast (R) alpha-methylhistamine did not modify the chronotropic effect of exogenous norepinephrine. The attenuation of adrenergic responses by (R) alpha-methylhistamine was 1) prevented by thioperamide, the selective H3-receptor antagonist; 2) attenuated by pertussis-toxin pretreatment and 3) potentiated by the N-type Ca(++)-channel blocker omega-conotoxin, which also potentiated the sympathetic modulatory effects of adrenergic-alpha 2 and adenosine-A1 receptor agonists. Our findings indicate that prejunctional histamine H3-receptors modulate the depolarization-dependent norepinephrine release from sympathetic nerve endings in the guinea pig myocardium. These receptors are probably coupled to a pertussis-toxin-sensitive Gi/Go protein and probably effect a reduction in Ca++ current. We have previously reported that sympathetic stimulation elicits a frequency-dependent release of cardiac histamine, whereas others had found that adrenergic activity regulates histamine's rapid turnover pool. Accordingly, presynaptic H3-receptors are likely to serve a modulatory role in cardiac adrenergic function.

Published

1994

37. S-[2-(4-imidazolyl)ethyl]isothiourea, a highly specific and potent histamine H3 receptor agonist.

Author

Garbarg M, Arrang JM, Rouleau A, Ligneau X, Tuong MD, Schwartz JC, and Ganellin CR

Subjects

Animals, Cerebral Cortex enzymology, Cerebral Cortex metabolism, Guinea Pigs, Histamine N-Methyltransferase metabolism, Histamine Release drug effects, Methylhistamines metabolism, Mice, Rats, Receptors, Histamine H3, Thiourea analogs & derivatives, Urea pharmacology, Cerebral Cortex drug effects, Histamine Agonists pharmacology, Imidazoles pharmacology, Receptors, Histamine drug effects, Urea analogs & derivatives

Abstract

The effects of a new agonist of histamine (HA) H3 receptors, Imetit (S-[2-(4-(imidazolyl)ethyl]isothiourea) were investigated in vitro and in vivo and compared to those of (R)-alpha-methylhistamine [(R)-alpha-MeHA], a prototypic drug. Imetit inhibited the binding of [3H](R-alpha-MeHA to rat brain membranes with a Ki value of 0.1 +/- 0.01 nM. The release of endogenously synthesized [3H]HA induced by K(+)-depolarization from rat brain slices and synaptosomes was inhibited by Imetit with EC50 values of 1.0 +/- 0.3 and 2.8 +/- 0.7 nM, respectively. Imetit behaved as a full agonist and was about 4 times more potent than (R)-alpha-MeHA and 60 times more potent than HA. Thioperamide, a selective H3 receptor antagonist, elicited a parallel rightward shift of the concentration-response curve for Imetit with an apparent Ki value of 5.6 +/- 1.4 nM. Imetit potencies relative to HA were less than 0.1% and only 0.6% at HA H1 and H2 receptor reference systems, respectively. Imetit was found not to be a substrate or an inhibitor of HMT. After p.o. administration to mice or rats, Imetit decreased (by approximately 50%) the tele-MeHA level in the cerebral cortex with ED50 values of 1.0 +/- 0.3 and 1.6 +/- 0.3 mg/kg, respectively. This effect was still maximal after 6 hr. The in vivo potency and duration of action of Imetit were in the same range as those of (R)-alpha-MeHA. It is therefore concluded that Imetit represents a new potent and selective HA H3 receptor agonist.

Published

1992