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1. 4-(ω-(Alkyloxy)alkyl)-1H-imidazole Derivatives as Histamine H3 Receptor Antagonists/Agonists

Author

C. Robin Ganellin, Heinz H. Pertz, Michael Krause, Holger Stark, Schwartz Jc, A Huls, X Ligneau, Jean-Michel Batiment Arrang, W Schunack, and Galina Meier

Subjects
Stereochemistry, Histamine Antagonists, GTPgammaS, Ether, In Vitro Techniques, Ligands, Chemical synthesis, Histamine agonist, Cell Line, Histamine Agonists, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Ileum, In vivo, Drug Discovery, Animals, Humans, Receptors, Histamine H3, Receptor, Alkyl, Cerebral Cortex, chemistry.chemical_classification, Chemistry, Imidazoles, Muscle, Smooth, Myocardial Contraction, Rats, Guanosine 5'-O-(3-Thiotriphosphate), Molecular Medicine, Histamine H3 receptor, Muscle Contraction, Synaptosomes
Abstract

In an effort to develop new histamine H(3) receptor antagonists usable as pharmacological tools we present here novel unsymmetrical ether derivatives. Etherification of different omega-(1H-imidazol-4-yl)alkyl scaffolds led to compounds containing alkyl chains of increasing lengths either with or without unsaturated termini, cycloalkyl or arylalkyl moieties, or additional heteroatoms. When investigated in an in vitro assay on rat synaptosomes, the majority of compounds displayed potencies in the low nanomolar concentration range at the H(3) receptor, e.g., 4-(3-(3-cyclopentylpropyloxy)propyl)-1H-imidazole (27, K(i) = 7 nM). FUB 465, 4-(3-(ethoxy)propyl)-1H-imidazole (14), a useful tool for the characterization of constitutive activity of H(3) receptors in vivo in rodents, proved to be of high oral in vivo potency in mice (ED(50) = 0.26 mg/kg). Further, the influence of chosen compounds on specific [(35)S]GTPgammaS binding was assayed on HEK293 cell membranes expressing the human histamine H(3) receptor revealing partial agonism of the compounds in this particular model. These distinct responses are further hints for "protean agonism" in this class of compounds. Additionally, selected compounds were functionally investigated in vitro on isolated organs of the guinea-pig at H(3), H(1), and H(2) receptors.

Published
2004

2. Constitutive activity of the recombinant and native histamine H3 receptor

Author

J.-C. Schwartz, A. Rouleau, Holger Stark, Walter Schunack, Charon Robin Ganellin, J. Tardivel-Lacombe, J.M. Arrang, Florence Gbahou, X. Ligneau, and S. Morisset

Subjects
Thioperamide, General Medicine, Histamine H1 receptor, Biology, Pharmacology, chemistry.chemical_compound, Histamine receptor, chemistry, Histamine H2 receptor, Proxyfan, Ciproxifan, medicine, Inverse agonist, Histamine H3 receptor, medicine.drug
Abstract

Although constitutive activity was shown to occur with many recombinant and/or mutated G-protein-coupled receptors, the physiological relevance of the process has remained debated. We have further explored this important issue with the histamine H3 receptor (H3R), a presynaptic receptor regulating histamine neuron activity in the brain. Constitutive activity of the recombinant receptor was studied using [3H]arachidonic acid release, [35S]GTPγ[S] binding and inhibition of cAMP accumulation. Evidence for constructive activity was obtained in these three functional assays with two isoforms of the rat H3 receptor, as well as with the human H3 receptor, expressed at physiological densities. Several standard H3-receptor antagonists, such as thioperamide and ciproxifan, were in fact acting as potent inverse agonists. Proxyfan opposed both agonists and inverse agonists and was therefore identified as a neutral antagonist. Using these drugs, we show high constitutive activity of native receptors. [35S]GTPγ[S] binding demonstrated constitutive activity of H3 receptors expressed at a normal level in mouse or rat brain. Constitutive activity of presynaptic H3 autoreceptors modulates histamine release from cortical synaptosomes in vitro and controls histamine neuron activity in vivo. This implies that inverse agonists rather than neutral antagonists may find therapeutic applications.

Published
2003

3. Novel Histamine H3-Receptor Antagonists with Carbonyl-Substituted 4-(3-(Phenoxy)propyl)-1H-imidazole Structures like Ciproxifan and Related Compounds

Author

J.-C. Schwartz, Holger Stark, Charon Robin Ganellin, B Sadek, A Huls, Walter Schunack, X Ligneau, Michael Krause, and J.M. Arrang

Subjects
Ketone, Stereochemistry, Guinea Pigs, Drug Evaluation, Preclinical, Histamine Antagonists, In Vitro Techniques, Histamine Release, Chemical synthesis, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Histamine receptor, Ileum, In vivo, Ciproxifan, Drug Discovery, medicine, Animals, Receptors, Histamine H3, Imidazole, Receptors, Histamine H2, Heart Atria, Receptors, Histamine H1, Cerebral Cortex, chemistry.chemical_classification, Imidazoles, Antagonist, Muscle, Smooth, Haplorhini, Atrial Function, Rats, chemistry, Molecular Medicine, Histamine, Muscle Contraction, Synaptosomes, medicine.drug
Abstract

Novel histamine H(3)-receptor antagonists possessing a 4-(3-(phenoxy)propyl)-1H-imidazole structure generally substituted in the para-position of the phenyl ring have been synthesized according to Mitsunobu or S(N)Ar reactions. With in vitro and in vivo screening for H(3)-receptor antagonist potency, the carbonyl-substituted derivatives proved to be highly active compounds. A number of compounds showed in vitro affinities in the subnanomolar concentration range, and the 4-hexanoyl (10) and 4-acetyl-3-methyl (29) substituted derivatives showed in vivo antagonist potencies of about 0.1 mg/kg after po administration. Many proxifans were also tested for their affinities at other histamine receptor subtypes thereby demonstrating their pronounced H(3)-receptor subtype selectivity. Since the cyclopropyl ketone derivative 14 (ciproxifan) had high affinity in vitro as well as high potency in vivo, it was selected for further studies in monkeys. It showed good oral absorption and long-lasting, dose-dependent plasma levels making it a promising compound for drug development.

Published
2000

4. Synthesis of Potent Non-imidazole Histamine H3-Receptor Antagonists

Author

A Piripitsi, J.M. Arrang, X Ligneau, Walter Schunack, Fabien Leurquin, J.-C. Schwartz, Charon Robin Ganellin, and Monique Garbarg

Subjects
chemistry.chemical_compound, chemistry, Tertiary amine, Stereochemistry, Drug Discovery, Antagonist, Pharmaceutical Science, Imidazole, Amine gas treating, Histamine H3 receptor, Chemical synthesis, Pyrrolidine, Histamine
Abstract

Histamine has been converted into a non-imidazole H3-receptor histamine antagonist by addition of a 4-phenylbutyl group at the N alpha-position followed by removal of the imidazole ring. The resulting compound, N-ethyl-N-(4-phenylbutyl)amine, remarkably has a Ki = 1.3 microM as an H3 antagonist. Using this as a lead compound, a novel series of homologous O and S isosteric tertiary amines was synthesised and structure-activity studies furnished N-(5-phenoxypentyl)pyrrolidine (Ki = 0.18 +/- 0.10 microM, for [3H]histamine release from rat cerebral cortex synaptosomes) which, more importantly, was active in vivo. Substitution of NO2 into the para position of the phenoxy group gave N-(5-p-nitrophenoxypentyl)pyrrolidine, UCL 1972 (Ki = 39 +/- 11 nM), ED50 = 1.1 +/- 0.6 mg/kg per os in mice on brain tele-methylhistamine levels.

Published
1998

5. 4-Alkynylphenyl Imidazolylpropyl Ethers as Selective Histamine H3-Receptor Antagonists with High Oral Central Nervous System Activity

Author

Walter Schunack, Holger Stark, M. Garbarg, X. Ligneau, J.‐C. Schwartz, and M. Krause

Subjects
Guinea Pigs, Central nervous system, Histamine Antagonists, Administration, Oral, Ether, In Vitro Techniques, Histamine Release, Mice, chemistry.chemical_compound, Ileum, In vivo, Oral administration, Drug Discovery, medicine, Animals, Receptors, Histamine H3, Receptors, Histamine H2, Receptors, Histamine H1, Cerebral Cortex, Chemistry, Myocardium, Imidazoles, Antagonist, In vitro, Rats, HYDIA, medicine.anatomical_structure, Biochemistry, Molecular Medicine, Histamine H3 receptor, Ethers, Synaptosomes
Abstract

In search for potent and therapeutically useful H3-receptor antagonists, we prepared novel 4-alkynylphenyl ether derivatives of 3-(1H-imidazol-4-yl)propanol in a convenient synthetic route. All compounds were tested for in vitro and in vivo H3-receptor antagonist activity as well as for H3-receptor selectivity versus H1- and H2-receptors. The presented 4-alkynylphenyl ethers are highly potent and selective H3 antagonists showing oral activity and improved brain penetration. Particularly 4-ethynylphenyl 3-(1H-imidazol-4-yl)propyl ether (14a) displays striking in vitro and in vivo activity with a -log Ki value of 8.6 and an ED50 value of 0.12 mg/kg. At present 14a is the most potent H3-receptor antagonist in vivo and may therefore be a potential drug for the therapy of H3-receptor-dependent diseases of the central nervous system (CNS).

Published
1998

6. Diphenylmethyl ethers: synthesis and histamine H3-receptor antagonist in vitro and in vivo activity

Author

K. Purand, Holger Stark, X. Ligneau, Annette Hüls, Walter Schunack, J.M. Arrang, and J.-C. Schwartz

Subjects
Stereochemistry, Organic Chemistry, Clinical Biochemistry, Antagonist, Pharmaceutical Science, Ether, Biochemistry, In vitro, Propanol, chemistry.chemical_compound, chemistry, In vivo, Drug Discovery, Molecular Medicine, High activity, Histamine H3 receptor, Molecular Biology, Histamine
Abstract

New potent histamine H3-receptor antagonists containing an ether group were synthesized from 3-(1H-imidazole-4-yl)propanol and various substituted diphenylmethyl chlorides. Some of the designed ethers showed high activity at histamine H3-receptors under in vitro as well as under in vivo conditions. Their activity at histamine H1- and H2-receptors was also investigated proving a pharmacological H 3 - H 1 - antagonistic profile.

Published
1996

7. [125I]Iodoproxyfan and Related Compounds: A Reversible Radioligand and Novel Classes of Antagonists with High Affinity and Selectivity for the Histamine H3 Receptor

Author

J.‐C. Schwartz, Holger Stark, K. Purand, Annette Hüls, Walter Schunack, X. Ligneau, and M. Garbarg

Subjects
Cerebral Cortex, Stereochemistry, Methylhistamines, Guinea Pigs, Histamine Antagonists, Imidazoles, Antagonist, Muscarinic acetylcholine receptor M3, Ether, In Vitro Techniques, Radioligand Assay, Rats, Iodine Radioisotopes, Structure-Activity Relationship, chemistry.chemical_compound, chemistry, Drug Discovery, Radioligand, Animals, Molecular Medicine, Structure–activity relationship, Histamine H3 receptor, H3 receptor antagonist
Abstract

The synthesis and biological evaluation of new histamine H3 receptor antagonists with an iodinated aryl partial structure are described as part of an extensive research program to find model compounds for the development of a new radioligand with high H3 receptor affinity and specific activity. All compounds were tested for their H3 receptor antagonist activity in a [3H]-histamine-release assay with synaptosomes from rat cerebral cortex. The new leads with potent H3 receptor antagonist activity belong to a series of derivatives of 3-(1H-imidazol-4-yl)propanol with carbamate (4-7), ester (8-16), and ether (17-22) as functional groups. Structure-activity relationships are discussed. The most active compound in the functional test (-log Ki = 8.3) and in binding studies with [3H]-(R)-alpha-methylhistamine on rat cerebral cortex (-log Ki = 9.0) in vitro was 3-(1H-imidazol-4-yl)propyl (4-iodophenyl)methyl ether (iodoproxyfan, 19) exhibiting no central H3 receptor antagonist activity in vivo. The potency of iodoproxyfan is more than 300 times lower at H1, H2, alpha1, alpha2, beta1, 5-HT2A, 5-HT3, and M3 receptors than at histamine H3 receptors. Because of the high potency and selectivity of 19, this compound has also been prepared in the [125I]-iodinated form by a nucleophilic halogen exchange reaction using the corresponding bromo derivative 22 as a precursor. The newly prepared [125I]iodoproxyfan (23) possesses advantageous pharmacological properties and fulfills all criteria of a useful radioligand.

Published
1996

8. Novel Carbamates as Potent Histamine H3 Receptor Antagonists with High in Vitro and Oral in Vivo Activity

Author

J.‐C. Schwartz, Holger Stark, Walter Schunack, M. Garbarg, X. Ligneau, Jean-Michel Arrang, Agnès Rouleau, and K. Purand

Subjects
Clobenpropit, Guinea Pigs, Histamine Antagonists, Phenylcarbamates, Administration, Oral, Mice, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Drug Discovery, medicine, Animals, Receptors, Histamine H2, Receptors, Histamine H1, Cerebral Cortex, Thioperamide, Molecular Structure, Chemistry, Imidazoles, Antagonist, Burimamide, In vitro, Rats, Biochemistry, Molecular Medicine, Carbamates, Histamine H3 receptor, Histamine, Synaptosomes, medicine.drug
Abstract

The known histamine H3 receptor antagonists burimamide, thioperamide, clobenpropit, and a related homohistamine thioamide derivative were taken as templates in search for new leads. Novel histamine H3 receptor antagonists structurally described as carbamate derivatives of 3-(1H-imidazol-4-yl)propanol were prepared in high yields by treatment of the alcohol with corresponding isocyanates or carbamoyl chlorides and investigated for their H3 receptor antagonist activity. Different chain lengths and various substituents possessing different electronic and steric parameters were introduced and structure-activity relationships established. In different functional tests, the new antagonists showed high H3 receptor antagonist potencies in vitro (-log Ki values of 6.4-8.4) at synaptosomes of rat cerebral cortex and low activities at histamine H1 and H2 receptor subtypes. They were also screened for their central in vivo activity in mice after peroral administration. The most promising compounds (2, 16, 19) showed ED(50) values of about 1-2 mg/kg and thus are potential drugs for the therapy of H3 receptor dependent diseases. Some of the novel carbamate derivatives are H3 receptor selective compounds with high in vitro and in vivo activity.

Published
1996

9. Design of Potent Non-Thiourea H3-Receptor Histamine Antagonists

Author

M. Garbarg, Schwartz Jc, Y. S. Khalaf, X. Ligneau, W. Tertiuk, J.‐M. Arrang, S. K. Hosseini, and Charon Robin Ganellin

Subjects
Cerebral Cortex, Thioperamide, Trifluoromethyl, Stereochemistry, Histamine Antagonists, Thiourea, Thio, In Vitro Techniques, Chemical synthesis, Rats, chemistry.chemical_compound, chemistry, Drug Design, Drug Discovery, medicine, Animals, Molecular Medicine, Imidazole, Histamine H3 receptor, Histamine, Synaptosomes, medicine.drug
Abstract

Starting from thioperamide, the first potent and selective H 3 -receptor histamine antagonist, analogues have been synthesized and tested in vitro on rat cerebral cortex to explore structure-activity relationships. The aim has been to design potent compounds which do not possess the thiourea group of thioperamide and which may have improved brain penetration. In a short series of open chain thiourea analogues, the optimum chain length for H 3 -antagonist potency was found to be (CH 2 ) 3 . Compounds derived from histamine and possessing an aromatic nitrogen-containing heterocycle on the side chain amino group in place of thiourea show H 3 -antagonist activity. Furthermore, when the heterocycle is 2-pyridyl, electron-withdrawing substituents (e.g. NO 2 , CF 3 , CO 2 Me) in the pyridine 5-position increased potency. The synthesis of 4-[4(5)-imidazolyl]piperidine and its conversion into the (trifluoromethyl)pyridyl analogue 5b of thioperamide is described ; however, 5b is not as potent as thioperamide. Replacing imidazole by pyridine or substituting imidazole on the remote N considerably reduced potency. Replacing the side-chain NH by S increased potency still further and the most potent compound is 2-{[2-[4(5)-imidazolyl]ethyl]thio}-5-nitropyridine (UCL 1199) which has K i = 4.8 nM

Published
1995

10. Preclinical evaluation of the abuse potential of Pitolisant, a histamine H₃ receptor inverse agonist/antagonist compared with Modafinil

Author

M, Uguen, D, Perrin, S, Belliard, X, Ligneau, P M, Beardsley, J M, Lecomte, and J C, Schwartz

Subjects
Male, Behavior, Animal, Dose-Response Relationship, Drug, Drug Inverse Agonism, Dopamine, Dopaminergic Neurons, Drug Evaluation, Preclinical, Histamine Antagonists, Modafinil, Drugs, Investigational, Wakefulness-Promoting Agents, Motor Activity, Macaca mulatta, Research Papers, Nucleus Accumbens, Rats, Behavior, Addictive, Histamine Agonists, Mice, Piperidines, Animals, Receptors, Histamine H3, Central Nervous System Stimulants, Benzhydryl Compounds, Drug Antagonism
Abstract

Pitolisant, a histamine H₃ receptor inverse agonist/antagonist is currently under Phase III clinical trials for treatment of excessive daytime sleepiness namely in narcoleptic patients. Its drug abuse potential was investigated using in vivo models in rodents and monkeys and compared with those of Modafinil, a psychostimulant currently used in the same indications.Effects of Pitolisant on dopamine release in the nucleus accumbens, on spontaneous and cocaine-induced locomotion, locomotor sensitization were monitored. It was also tested in three standard drug abuse tests i.e. conditioned place preference in rats, self-administration in monkeys and cocaine discrimination in mice as well as in a physical dependence model.Pitolisant did not elicit any significant changes in dopaminergic indices in rat nucleus accumbens whereas Modafinil increased dopamine release. In rodents, Pitolisant was without any effect on locomotion and reduced the cocaine-induced hyperlocomotion. In addition, no locomotor sensitization and no conditioned hyperlocomotion were evidenced with this compound in rats whereas significant effects were elicited by Modafinil. Finally, Pitolisant was devoid of any significant effects in the three standard drug abuse tests (including self-administration in monkeys) and in the physical dependence model.No potential drug abuse liability for Pitolisant was evidenced in various in vivo rodent and primate models, whereas the same does not seem so clear in the case of Modafinil.

Published
2012

11. Unsymmetrically substituted guanidines as potent histamine H3-receptor antagonists

Author

J.-C. Schwartz, Holger Stark, X. Ligneau, M. Krause, Walter Schunack, and J.M. Arrang

Subjects
chemistry.chemical_classification, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Prodrug, Biochemistry, chemistry.chemical_compound, chemistry, Drug Discovery, Molecular Medicine, Histamine H3 receptor, Guanidine, Molecular Biology, Guanidine derivatives, Histamine, Alkyl
Abstract

Unsymmetrically trisubstituted and disubstituted guanidine derivatives of (1H-imidazol-4-yl)alkyl amines were synthesized and investigated for histamine H3-receptor activity. Electron-withdrawing substitution of the guanidino group resulted in antagonists with a potential prodrug character. The H3-receptor selective N1-cyclohexylmethyl-N2-[3-(1H-imidazol-4-yl)propyl]guanidine possesses a -log Ki of 9.1.

Published
1994

12. ChemInform Abstract: A Novel Series of (Phenoxyalkyl)imidazoles as Potent H3-Receptor Histamine Antagonists

Author

Garbarg M, W. Tertiuk, Charon Robin Ganellin, Athmani S, A. Fkyerat, Benny Bang-Andersen, Schwartz Jc, and X Ligneau

Subjects
chemistry.chemical_compound, Trifluoromethyl, chemistry, In vivo, Stereochemistry, Imidazole, Potency, General Medicine, Histamine H3 receptor, Antagonism, In vitro, Histamine
Abstract

[[(4-Nitrophenyl)X]alkyl]imidazole isosteres (where X = NH, S, CH2S, O) of previously described [[(5-nitropyrid-2-yl)X]ethyl]imidazoles (where X = NH, S) have been synthesized and evaluated for H3-receptor histamine antagonism in vitro (Ki for [3H]histamine release from rat cerebral cortex synaptosomes) and in vivo (ED50 per os in mice on brain tele-methylhistamine levels). Encouraging results led to the synthesis and testing of a novel series of substituted (phenoxyethyl)- and (phenoxypropyl)imidazoles. From the latter, 4-[3-(4-cyanophenoxy)propyl]-1H-imidazole (10a, UCL 1390; Ki = 12 nM, ED50 = 0.54 mg/kg) and 4-[3-[4-(trifluoromethyl)phenoxy]propyl]-1H-imidazole (10c, UCL 1409; Ki = 14 nM, ED50 = 0.60 mg/kg) have been selected as potential candidates for drug development. For 16 [(aryloxy)ethyl]imidazoles the relationship between in vitro and in vivo potency is described by the equation log ED50 = 0.47 log Ki + 0.20 (r = 0.78).

Published
2010

13. ChemInform Abstract: Design of Potent Non-Thiourea H3-Receptor Histamine Antagonists

Author

Y. S. Khalaf, J.‐M. Arrang, Charon Robin Ganellin, S. K. Hosseini, X. Ligneau, M. Garbarg, W. Tertiuk, and Schwartz Jc

Subjects
Thioperamide, Trifluoromethyl, Stereochemistry, Thio, General Medicine, chemistry.chemical_compound, chemistry, Thiourea, medicine, Imidazole, Piperidine, Histamine H3 receptor, Histamine, medicine.drug
Abstract

Starting from thioperamide, the first potent and selective H 3 -receptor histamine antagonist, analogues have been synthesized and tested in vitro on rat cerebral cortex to explore structure-activity relationships. The aim has been to design potent compounds which do not possess the thiourea group of thioperamide and which may have improved brain penetration. In a short series of open chain thiourea analogues, the optimum chain length for H 3 -antagonist potency was found to be (CH 2 ) 3 . Compounds derived from histamine and possessing an aromatic nitrogen-containing heterocycle on the side chain amino group in place of thiourea show H 3 -antagonist activity. Furthermore, when the heterocycle is 2-pyridyl, electron-withdrawing substituents (e.g. NO 2 , CF 3 , CO 2 Me) in the pyridine 5-position increased potency. The synthesis of 4-[4(5)-imidazolyl]piperidine and its conversion into the (trifluoromethyl)pyridyl analogue 5b of thioperamide is described ; however, 5b is not as potent as thioperamide. Replacing imidazole by pyridine or substituting imidazole on the remote N considerably reduced potency. Replacing the side-chain NH by S increased potency still further and the most potent compound is 2-{[2-[4(5)-imidazolyl]ethyl]thio}-5-nitropyridine (UCL 1199) which has K i = 4.8 nM

Published
2010

17. Azole derivatives as histamine H3 receptor antagonists, part I: thiazol-2-yl ethers

Author

X. Ligneau, Jean-Claude Camelin, Kathleen Isensee, J.-C. Schwartz, Y. von Coburg, Kerstin Sander, M. Walter, and Holger Stark

Subjects
Azoles, Molecular model, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Ether, Biochemistry, Chemical synthesis, Cell Line, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Moiety, Humans, Receptors, Histamine H3, Molecular Biology, chemistry.chemical_classification, Chemistry, Organic Chemistry, Thiazoles, Molecular Medicine, Azole, Histamine H3 receptor, Pharmacophore, Histamine, Ethers, Histamine H3 Antagonists
Abstract

Most human histamine H3 receptor (hH3R) antagonists follow a general structural blueprint, containing a basic moiety linked by a spacer to a substituted core element. In this investigation the acceptance of thiazol-2-yl ether moieties in the core region is proved with some ether derivatives showing hH3R binding affinities in the nanomolar concentration range. A diversity of structural motifs is used as substituents to enhance the in vitro hH3R binding affinity.

Published
2010

18. Azole derivatives as histamine H3 receptor antagonists, part 2: C-C and C-S coupled heterocycles

Author

Miriam Walter, Holger Stark, X. Ligneau, J.-C. Schwartz, Tim Kottke, Kathleen Isensee, and Jean-Claude Camelin

Subjects
Azoles, Stereochemistry, Clinical Biochemistry, Triazole, Pharmaceutical Science, Oxadiazole, Biochemistry, Cell Line, chemistry.chemical_compound, Structure-Activity Relationship, Heterocyclic Compounds, Drug Discovery, Humans, Receptors, Histamine H3, Thiazole, Molecular Biology, Oxazole, chemistry.chemical_classification, Organic Chemistry, Carbon, chemistry, Molecular Medicine, Azole, Bioisostere, Pharmacophore, Histamine H3 receptor, Sulfur, Histamine H3 Antagonists, Protein Binding
Abstract

With a small series of compounds we demonstrated the variability in the core region of the human histamine H(3) receptor (hH(3)R) antagonist structural blueprint by introducing polar azole groups (oxazole, oxadiazole, thiazole and triazole). Additional variations achieved by coupling different residues to the heterocyclic core structure led to further optimisation of in vitro receptor binding of the novel azole derivatives.

Published
2010

19. ChemInform Abstract: Development of FUB 181, a Selective Histamine H3-Receptor Antagonist of High Oral in vivo Potency with 4-(ω-(Arylalkyloxy)alkyl)-1H-imidazole Structure

Author

J.‐M. Arrang, J.‐C. Schwartz, K. Purand, Heinz H. Pertz, A. Huels, Holger Stark, X. Ligneau, and Walter Schunack

Subjects
chemistry.chemical_classification, chemistry.chemical_compound, chemistry, Stereochemistry, In vivo, Antagonist, Potency, Imidazole, General Medicine, Histamine H3 receptor, Alkyl
Published
2010

21. ChemInform Abstract: Substituted N-Phenylcarbamates as Histamine H3 Receptor Antagonists with Improved in vivo Potency

Author

W Schunack, J.‐C. Schwartz, S. Reidemeister, X. Ligneau, Holger Stark, and Charon Robin Ganellin

Subjects
chemistry.chemical_compound, Phenylcarbamates, chemistry, In vivo, Muscarinic acetylcholine receptor, Antagonist, Potency, Muscarinic acetylcholine receptor M3, General Medicine, Pharmacology, Histamine H3 receptor, Histamine
Abstract

Novel substituted N-phenylcarbamates as derivatives of 3-(1 H-imidazol-4-yl)propanol were prepared and tested for their antagonist potency in vitro and in vivo at histamine H3 receptors. Structural modifications with different alkyl and acetyl moieties were performed in an attempt to optimize pharmacodynamic and pharmacokinetic effects. Most compounds are active in a functional test for histamine H3 receptors on rat cerebral cortex synaptosomes as well as in a peripheral model on guinea pig ileum. But only carbamates without too bulky lipophilic residues showed pronounced to high antagonist potency on the enhancement of endogenous histamine in brain after p.o. administration to mice (ED50 values of 5.5 to 0.86 mg.kg-1). The tested compounds presented weak activities at histamine H1, H2, and muscarinic M3 receptors thus demonstrating their H3-receptor selectivity.

Published
2010

22. ChemInform Abstract: Importance of the Lipophilic Group in Carbamates Having Histamine H3-Receptor Antagonist Activity

Author

X. Ligneau, Astrid Sasse, Katarzyna Kieć-Kononowicz, Holger Stark, M. Wiecek, W Schunack, Sigurd Elz, Charon Robin Ganellin, and J.‐C. Schwartz

Subjects
Thioperamide, Carbamate, Stereochemistry, medicine.medical_treatment, Antagonist, General Medicine, Pharmacology, In vitro, chemistry.chemical_compound, chemistry, In vivo, medicine, Potency, Histamine H3 receptor, Histamine, medicine.drug
Abstract

In order to evaluate changes in the lipophilic part of designed carbamates concerning their potential histamine H3-receptor antagonist properties a new series of O-[3-(1H-imidazol-4-yl)propanol]carbamates was derived containing N-mono- or di-alkenyl, alkynyl, cycloalkyl, or double-branched alkyl substituents. The compounds were tested in vitro for their H3-receptor antagonist activity on synaptosomes of rat cerebral cortex and shared moderate to high antagonist activity in vitro. In this series 3-(1H-imidazol-4-yl)propyl N-(4-pentenyl)carbamate (4) was the most potent compound in vitro (Ki = 6.3 nM). H3-receptor antagonist activity in the central nervous system (CNS) was detected for most compounds in the in vivo H3-receptor assay based upon measurement of brain N tau-methylhistamine levels after p.o. administration to mice. The most effective carbamate in vivo, 3-(1H-imidazol-4-yl)propyl N-(allyl)carbamate (3), showed higher CNS potency (ED50 = 0.48 mg/kg p.o.) than the reference antagonist thioperamide. For some novel carbamates their histamine H1- and H2-receptor activities were determined on isolated organs of guinea-pig thereby demonstrating their high H3-receptor selectivity.

Published
2010

23. Fluorinated non-imidazole histamine H3 receptor antagonists

Author

Jean-Claude Camelin, Holger Stark, Michael Amon, A. Galaparti, Kathleen Isensee, Marc Capet, X. Ligneau, and J.-C. Schwartz

Subjects
Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Pyrrolidine, Alicyclic compound, chemistry.chemical_compound, Mice, In vivo, Drug Discovery, Imidazole, Moiety, Animals, Receptors, Histamine H3, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Imidazoles, Fluorine, chemistry, Molecular Medicine, Piperidine, Histamine H3 receptor, Histamine, Histamine H3 Antagonists, Protein Binding
Abstract

Fluorine substituents have become a widespread and important component in drug design and development. Here, the synthesis of fluorine containing compounds and some corresponding precursor molecules are presented for potential isotope labelling as well as their data obtained with in vitro and in vivo screenings. The compounds vary in the basic centres (piperidine or pyrrolidine) and are fluoro substituted in different positions of the basic alicyclic moiety. Pharmacological evaluation resulted in ligands with high affinities at hH3 receptor in the nanomolar and subnanomolar concentration range and some with high antagonist in vivo potencies.

Published
2009

24. Search for histamine H3 receptor antagonists with combined inhibitory potency at Ntau-methyltransferase: ether derivatives

Author

J, Apelt, S, Grassmann, X, Ligneau, H H, Pertz, C R, Ganellin, J M, Arrang, J C, Schwartz, W, Schunack, and H, Stark

Subjects
Chemical Phenomena, Chemistry, Physical, Histamine Antagonists, Imidazoles, CHO Cells, Methyltransferases, Kidney, Binding, Competitive, Rats, Structure-Activity Relationship, Histamine H2 Antagonists, Cricetinae, Animals, Humans, Receptors, Histamine H3, Female, Indicators and Reagents, Ethers
Abstract

With the recent development of new hybrid compounds having histamine H3 receptor antagonist with combined histamine Ntau-methyltransferase (HMT) inhibitory potency an innovative approach was described in the research of novel lead compounds modulating histaminergic neurotransmission. Several compounds containing an ether moiety derived from the recently published 4-(3-piperidinopropoxy)phenylaminoquinoline derivatives (like FUB 836), were synthesized in this study and tested for their affinity at cloned human histamine H3 (hH3) receptors and on the inhibition of rat HMT. Besides different heterocycles, e.g. nitro- or amino-substituted pyridines, quinolines, benzothiazole or pyrroline, three classes of compounds were produced: heteroaromatic 3-piperidinopropyl ethers, keto- or imino-substituted 4-(3-piperidinopropyl)phenyl ethers and 4-(3-piperidinopropyl)phenyl ethers with substituted (alkyl)aminopyridines. Whereas the (3-piperidinopropoxy)heterocycles showed only moderate activities on both test models, the 4-(3-piperidinopropoxy)phenyl derivatives were identified as potent histamine H3 receptor ligands and/or HMT inhibitors. Ki values up to 0.42 nM were found for the affinity to the hH3 receptor. HMT inhibitory potency was identified with IC50 values about 0.3 microM for the most potent compounds in this series. Comparison of the pyridine-containing derivatives to recently published quinoline analogues showed a decrease in potencies for the pyridines. The dual activity, H3 receptor affinity and HMT inhibition, was moderate to good. For all compounds affinities at hH3 receptors were higher than their inhibitory HMT potencies. The described new histamine H3 receptor antagonists with an ether moiety represent a further promising step in our investigations for a dual activity.

Published
2005

25. Influence of bulky substituents on histamine h(3) receptor agonist/antagonist properties

Author

J.‐M. Arrang, A Rouleau, S Elz, Astrid Sasse, Holger Stark, W Schunack, X Ligneau, Charon Robin Ganellin, and Schwartz Jc

Subjects
Agonist, medicine.drug_class, Stereochemistry, Agonist-antagonist, Histamine Antagonists, Ether, CHO Cells, Partial agonist, Histamine Agonists, chemistry.chemical_compound, Mice, Radioligand Assay, Structure-Activity Relationship, In vivo, Cricetinae, Drug Discovery, medicine, Animals, Humans, Receptors, Histamine H3, Chemistry, Imidazoles, Electrophoresis, Capillary, Stereoisomerism, Rats, Molecular Medicine, Carbamates, Histamine H3 receptor, Enantiomer, Histamine
Abstract

Novel derivatives of 3-(1H-imidazol-4-yl)propanol were designed on the basis of lead compounds belonging to the carbamate or ether series possessing (partial) agonist properties on screening assays of the histamine H(3) receptor. One pair of enantiomers in the series of alpha-methyl-branched chiral carbamates was stereoselectively prepared in high optical yields. Enantiomeric purity was checked by Mosher amide derivatives of precursors and capillary electrophoresis of the final compounds with trimethyl-beta-cyclodextrin as chiral selector, and was determined to be/=95%. The novel compounds were investigated in various histamine H(3) receptor assays in vitro and in vivo. Some compounds displayed partial agonist activity on synaptosomes of rat brain cortex, whereas others exhibited antagonist properties only. Selected compounds were investigated in [(125)I]iodoproxyfan binding studies on the human histamine H(3) receptor and showed high affinity in the nanomolar concentration range. Under in vivo conditions after oral administration to mice, some of the compounds exhibited partial or full agonist activity in the brain at low dosages. The (S)-enantiomer of one pair of chiral carbamates (9) proved to be the eutomer; thus, the (S)-enantiomer was selected for further pharmacological studies. In a peripheral in vivo test model in rats, measuring the level of inhibition of capsaicin-induced plasma extravasation, (S)-9 again proved its high oral agonist potency with full intrinsic activity (ED(50) values of 0.07-0.1 mg/kg depending on tissue).

Published
2002

27. Development of a new class of nonimidazole histamine H(3) receptor ligands with combined inhibitory histamine N-methyltransferase activity

Author

Holger Stark, X Ligneau, W Schunack, Schwartz Jc, J.‐M. Arrang, Pertz Hh, Joachim Apelt, and Charon Robin Ganellin

Subjects
Histamine N-Methyltransferase, Guinea Pigs, Histamine Antagonists, CHO Cells, Neurotransmission, In Vitro Techniques, Ligands, Histamine receptor, chemistry.chemical_compound, Mice, Radioligand Assay, Structure-Activity Relationship, Piperidines, Ileum, Cricetinae, Drug Discovery, Animals, Humans, Receptors, Histamine H3, Enzyme Inhibitors, Receptor, Histamine N-methyltransferase, Chemistry, Histaminergic, Histamine N-methyltransferase activity, Brain, Muscle, Smooth, Rats, Biochemistry, Quinolines, Molecular Medicine, Histamine H3 receptor, Histamine
Abstract

In search of novel ways to enhance histaminergic neurotransmission in the central nervous system, a new class of nonimidazole histamine H(3) receptor ligands were developed that simultaneously possess strong inhibitory activity on the main histamine metabolizing enzyme, histamine N-methyltransferase (HMT). The novel compounds contain an aminoquinoline moiety, which is an important structural feature for HMT inhibitory activity, connected by different spacers to a piperidino group (for H(3) receptor antagonism). Variation of the spacer structure provides two different series of compounds. One series, having only an alkylene spacer between the basic centers, led to highly potent HMT inhibitors with moderate to high affinity at human histamine H(3) receptors. The second series possesses a p-phenoxypropyl spacer, which may be extended by another alkylene chain. This latter series also showed strong inhibitory activity on HMT, and in most cases, the H(3) receptor affinity even surpassed that of the first series. One of the most potent compounds with this dual mode of action is 4-(4-(3-piperidinopropoxy)phenylamino)quinoline (34) (hH(3), K(i) = 0.09 nM; HMT, IC(50) = 51 nM). This class of compounds showed high antagonist potency and good H(3) receptor selectivity in functional assays in guinea pig on H(1), H(2), and H(3) receptors. Because of low or missing in vivo activity of two selected compounds, the proof of concept of these valuable pharmacological tools for the supposed superior overall enhancing effect on histaminergic neurotransmission failed to appear hitherto.

Published
2002

28. Importance of the lipophilic group in carbamates having histamine H3-receptor antagonist activity

Author

K, Kieć-Kononowicz, M, Wiecek, A, Sasse, X, Ligneau, S, Elz, C R, Ganellin, J C, Schwartz, H, Stark, and W, Schunack

Subjects
Brain Chemistry, Cerebral Cortex, Chemical Phenomena, Chemistry, Physical, Guinea Pigs, Histamine Antagonists, Muscle, Smooth, In Vitro Techniques, Rats, Mice, Ileum, Animals, Receptors, Histamine H3, Indicators and Reagents, Carbamates, Muscle Contraction, Synaptosomes
Abstract

In order to evaluate changes in the lipophilic part of designed carbamates concerning their potential histamine H3-receptor antagonist properties a new series of O-[3-(1H-imidazol-4-yl)propanol]carbamates was derived containing N-mono- or di-alkenyl, alkynyl, cycloalkyl, or double-branched alkyl substituents. The compounds were tested in vitro for their H3-receptor antagonist activity on synaptosomes of rat cerebral cortex and shared moderate to high antagonist activity in vitro. In this series 3-(1H-imidazol-4-yl)propyl N-(4-pentenyl)carbamate (4) was the most potent compound in vitro (Ki = 6.3 nM). H3-receptor antagonist activity in the central nervous system (CNS) was detected for most compounds in the in vivo H3-receptor assay based upon measurement of brain N tau-methylhistamine levels after p.o. administration to mice. The most effective carbamate in vivo, 3-(1H-imidazol-4-yl)propyl N-(allyl)carbamate (3), showed higher CNS potency (ED50 = 0.48 mg/kg p.o.) than the reference antagonist thioperamide. For some novel carbamates their histamine H1- and H2-receptor activities were determined on isolated organs of guinea-pig thereby demonstrating their high H3-receptor selectivity.

Published
2002

29. The histamine H3 receptor and its ligands

Author

H, Stark, J M, Arrang, X, Ligneau, M, Garbarg, C R, Ganellin, J C, Schwartz, and W, Schunack

Subjects
Histamine Agonists, Radioisotopes, Anti-Inflammatory Agents, Imidazoles, Animals, Brain, Humans, Hypnotics and Sedatives, Receptors, Histamine H3, Amines, Ligands, Antidepressive Agents
Published
2002

30. Substituted N-phenylcarbamates as histamine H3 receptor antagonists with improved in vivo potency

Author

S, Reidemeister, H, Stark, X, Ligneau, C R, Ganellin, J C, Schwartz, and W, Schunack

Subjects
Cerebral Cortex, Receptor, Muscarinic M3, Methylhistamines, Guinea Pigs, Histamine Antagonists, Muscarinic Antagonists, In Vitro Techniques, Histamine Release, Receptors, Muscarinic, Rats, Mice, Histamine H2 Antagonists, Ileum, Histamine H1 Antagonists, Animals, Receptors, Histamine H3, Carbamates, Muscle Contraction, Synaptosomes
Abstract

Novel substituted N-phenylcarbamates as derivatives of 3-(1 H-imidazol-4-yl)propanol were prepared and tested for their antagonist potency in vitro and in vivo at histamine H3 receptors. Structural modifications with different alkyl and acetyl moieties were performed in an attempt to optimize pharmacodynamic and pharmacokinetic effects. Most compounds are active in a functional test for histamine H3 receptors on rat cerebral cortex synaptosomes as well as in a peripheral model on guinea pig ileum. But only carbamates without too bulky lipophilic residues showed pronounced to high antagonist potency on the enhancement of endogenous histamine in brain after p.o. administration to mice (ED50 values of 5.5 to 0.86 mg.kg-1). The tested compounds presented weak activities at histamine H1, H2, and muscarinic M3 receptors thus demonstrating their H3-receptor selectivity.

Published
2000

31. Novel partial agonists for the histamine H(3) receptor with high in vitro and in vivo activity

Author

Reidemeister S, Astrid Sasse, Charon Robin Ganellin, W Schunack, S Elz, A Huls, Holger Stark, Schwartz Jc, and X Ligneau

Subjects
Agonist, Intrinsic activity, medicine.drug_class, Histamine Antagonists, Histamine H1 receptor, In Vitro Techniques, Imetit, Partial agonist, Histamine Agonists, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Histamine H2 receptor, Ileum, Drug Discovery, medicine, Animals, Cerebral Cortex, Methylhistamines, Imidazoles, Muscle, Smooth, Electric Stimulation, Rats, Biochemistry, chemistry, Molecular Medicine, Histamine H3 receptor, Histamine, Ethers, Muscle Contraction, Synaptosomes
Abstract

Novel branched N-alkylcarbamates and aliphatic ethers derived from 3-(1H-imidazol-4-yl)propanol were prepared. The compounds were investigated on two functional histamine H(3)-receptor assays. Some compounds displayed partial agonist activity on synaptosomes of rat brain cortex but behaved as pure competitive antagonists on the guinea pig ileum. Under in vivo conditions after po application to mice, some of the compounds showed partial or full agonist activity. Highest in vivo potency was found for the 3,3-dimethylbutyl ether 10 (ED(50) = 0.29 mg/kg, full intrinsic activity). These novel agonists are structurally diverse from classical aminergic histamine H(3)-receptor agonists (e.g., (R)-alpha-methylhistamine, imetit) as they lack a basic moiety in the side chain, which is supposed to be important for the activation of the receptor protein. The selectivity for the histamine H(3) receptor was proven by determination of H(1)- and H(2)-receptor activity on functional assays of the guinea pig.

Published
1999

32. Synthesis of potent non-imidazole histamine H3-receptor antagonists

Author

C R, Ganellin, F, Leurquin, A, Piripitsi, J M, Arrang, M, Garbarg, X, Ligneau, W, Schunack, and J C, Schwartz

Subjects
Pyrrolidines, Molecular Structure, Methylhistamines, Histamine Antagonists, Administration, Oral, Brain, Butylamines, Rats, Structure-Activity Relationship, Animals, Receptors, Histamine H3, Amines, Histamine, Synaptosomes
Abstract

Histamine has been converted into a non-imidazole H3-receptor histamine antagonist by addition of a 4-phenylbutyl group at the N alpha-position followed by removal of the imidazole ring. The resulting compound, N-ethyl-N-(4-phenylbutyl)amine, remarkably has a Ki = 1.3 microM as an H3 antagonist. Using this as a lead compound, a novel series of homologous O and S isosteric tertiary amines was synthesised and structure-activity studies furnished N-(5-phenoxypentyl)pyrrolidine (Ki = 0.18 +/- 0.10 microM, for [3H]histamine release from rat cerebral cortex synaptosomes) which, more importantly, was active in vivo. Substitution of NO2 into the para position of the phenoxy group gave N-(5-p-nitrophenoxypentyl)pyrrolidine, UCL 1972 (Ki = 39 +/- 11 nM), ED50 = 1.1 +/- 0.6 mg/kg per os in mice on brain tele-methylhistamine levels.

Published
1999

33. Neurochemical and behavioral effects of ciproxifan, a potent histamine H3-receptor antagonist

Author

X, Ligneau, J, Lin, G, Vanni-Mercier, M, Jouvet, J L, Muir, C R, Ganellin, H, Stark, S, Elz, W, Schunack, and J, Schwartz

Subjects
Male, Behavior, Animal, Methylhistamines, Guinea Pigs, Histamine Antagonists, Imidazoles, Electroencephalography, Neocortex, Rats, Iodine Radioisotopes, Mice, Radioligand Assay, Cats, Animals, Receptors, Histamine H3, Female, Rats, Wistar
Abstract

Ciproxifan, i.e., cyclopropyl-(4-(3-1H-imidazol-4-yl)propyloxy) phenyl) ketone, belongs to a novel chemical series of histamine H3-receptor antagonists. In vitro, it behaved as a competitive antagonist at the H3 autoreceptor controlling [3H]histamine release from synaptosomes and displayed similar Ki values (0.5-1.9 nM) at the H3 receptor controlling the electrically-induced contraction of guinea pig ileum or at the brain H3 receptor labeled with [125I]iodoproxyfan. Ciproxifan displayed at least 3-orders of magnitude lower potency at various aminergic receptors studied in functional or binding tests. In vivo, measurement of drug plasma levels, using a novel radioreceptor assay in mice receiving ciproxifan p.o. or i.v., led to an oral bioavailability ratio of 62%. Oral administration of ciproxifan to mice enhanced by approximately 100% histamine turnover rate and steady state level of tele-methylhistamine with an ED50 of 0.14 mg/kg. Ciproxifan reversed the H3-receptor agonist induced enhancement of water consumption in rats with and ID50 of 0.09 +/- 0.04 mg/kg, i.p. In cats, ciproxifan (0.15-2 mg/kg, p.o.) induced marked signs of neocortical electroencephalogram activation manifested by enhanced fast-rhythms density and an almost total waking state. In rats, ciproxifan enhanced attention as evaluated in the five-choice task performed using a short stimulus duration. Ciproxifan appears to be an orally bioavailable, extremely potent and selective H3-receptor antagonist whose vigilance- and attention-promoting effects are promising for therapeutic applications in aging disorders.

Published
1998

34. Development of FUB 181, a selective histamine H3-receptor antagonist of high oral in vivo potency with 4-(omega-(arylalkyloxy)alkyl)-1H-imidazole structure

Author

H, Stark, A, Hüls, X, Ligneau, K, Purand, H, Pertz, J M, Arrang, J C, Schwartz, and W, Schunack

Subjects
Cerebral Cortex, Receptor, Muscarinic M3, Dose-Response Relationship, Drug, Methylhistamines, Guinea Pigs, Histamine Antagonists, Imidazoles, Administration, Oral, Receptors, Muscarinic, Rats, Mice, Structure-Activity Relationship, Receptors, Adrenergic, alpha-1, Receptors, Serotonin, Alkanes, Animals, Receptors, Histamine H3, Receptor, Serotonin, 5-HT2A, Receptors, Adrenergic, beta-2, Receptors, Adrenergic, beta-1, Receptors, Serotonin, 5-HT3, Synaptosomes
Abstract

A series of 4-(omega-(arylalkyloxy)alkyl)-1H-imidazoles and related sulphur-containing compounds have been prepared and evaluated for their histamine H3-autoreceptor antagonist in vitro potency in an assay on synaptosomes of rat cerebral cortex. In addition, the in vivo potency has been determined from the changes in N tau-methylhistamine levels in brain after p.o. administration to mice. Compounds with different alkyl chains and various aryl moities have been synthesized and tested to explore structure-activity relationships. Within this series of novel antagonists, (1H-imid-azol-4-yl)methyl and 2-(1H-imidazol-4-yl)ethyl ether derivatives showed low to moderate H3-receptor antagonist potency, whereas the corresponding allyl and propyl derivatives were compounds with high antagonist in vitro potency. Corresponding thioether or sulphoxide derivatives also showed antagonists activity. Additionally, some ether derivatives possessed high in vivo potency as well. The most active ether derivatives under in vivo conditions were 4-(3-(3-(4-fluorophenyl)propyloxy)propyl)-1H-imidazole (11b) and the corresponding chloro compound 11c (FUB 181) with ED50 values of 0.76 and 0.80 mg/kg, respectively. On the other hand, all compounds tested showed weak activity at histamine H1 or H2 receptors. Furthermore, the most promising ether FUB 181 exhibited low activity at adrenergic alpha 1, beta 1/2, serotonergic 5-HT2A, 5-HT3, and muscarinic M3 receptors. Time-course investigations of FUB 181 in mice showed a rapid mode of action with the highest value 3 h after p.o. application. Thus, FUB 181 appears to block histamine H3 receptors potently and selectively.

Published
1998

35. Search for novel leads for histamine H3-receptor antagonists: oxygen-containing derivatives

Author

H, Stark, A, Hüls, X, Ligneau, J M, Arrang, J C, Schwartz, and W, Schunack

Subjects
Brain Chemistry, Cerebral Cortex, Oxygen, Mice, Histamine H2 Antagonists, Methylhistamines, Guinea Pigs, Histamine Antagonists, Histamine H1 Antagonists, Animals, Receptors, Histamine H3, In Vitro Techniques, Rats
Abstract

This study was performed in order to develop new leads for antagonists of the histamine H3-receptor subtype. omega-(1 H-Imidazol-4-yl)alkyl derivatives with ester, ketone or alcohol functionality in the side chain were synthesized and tested concerning their H3-receptor antagonist activity on synaptosomes of rat cerebral cortex. The novel compounds, which possess no nitrogen-containing polar group in the side chain of the imidazole moiety, presented moderate to high antagonist potency in vitro. In this series 3-(1 H-imidazol-4-yl)propyl-3-cyclopentylpropanoate (4) was the most potent compound in vitro with -log Ki = 8.5. Unfortunately, no central antagonist H3-receptor activity was detectable for ester derivatives in the in vitro H3-receptor assay based upon measurement of brain N tau-methylhistamine levels after p.o. administration to mice. Some of these novel antagonists are useful tools for investigations on ligand-receptor interaction because of their distinct receptor activities. On the other hand, the ketone derivative 1-(1 H-imidazol-4-yl)-7-phenyl-4-heptanone (9) in vitro presented an ED50-value of 3.5 +/- 1.5 mg/kg p.o. thus proving to be a new lead for further drug investigations. The most potent compounds in vitro and in vivo also showed high H3-receptor selectivity when tested at other histamine receptor subtypes.

Published
1997

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

Author

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

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

37. Search for novel leads for histamine H3-receptor antagonists: amine derivatives

Author

H, Stark, X, Ligneau, R, Lipp, J M, Arrang, J C, Schwartz, and W, Schunack

Subjects
Brain Chemistry, Cerebral Cortex, Methylhistamines, Guinea Pigs, Histamine Antagonists, Radioimmunoassay, In Vitro Techniques, Ligands, Rats, Mice, Histamine H2 Antagonists, Ileum, Animals, Receptors, Histamine H3, Heart Atria, Muscle Contraction
Abstract

In search for novel leads for histamine H3-receptor antagonists a number of amine derivatives of different (1 H-imidazol-4-yl)anilines and omega-(1 H-imidazol-4-yl)alkanamines were prepared. Pharmacological in vitro H3-receptor investigations of the prepared urea, amide, inverse amide, thioamide, and thiourea derivatives on synaptosomes of rat cerebral cortex proved that the aniline derivatives are inactive at H3-receptors, whereas derivatives of the omega-(1 H-imidazol-4-yl)-alkanamines showed moderate to good activity. Some compounds are active in the nanomolar concentration range. The most potent compounds in this series are the thioamide derivative 7 and the urea derivatives 11, 12 of 3-(1 H-imidazol-4-yl) propanamine. Therefore, the urea derivatives were tested in vitro on isolated organs of the guinea pig for their activity on the other two histamine receptor subtypes proving their high selectivity. In vivo studies of the effects of the urea derivatives 11 and 12 on brain Nt-methylhistamine levels, a test of central H3-receptor activity after peroral application to mice, showed no detectable activity. Thus, the urea type antagonists are useful potent and selective H3-receptor tools for in vitro studies and for investigations of ligand-receptor interactions.

Published
1997

38. A novel series of (phenoxyalkyl)imidazoles as potent H3-receptor histamine antagonists

Author

W. Tertiuk, A. Fkyerat, Benny Bang-Andersen, X Ligneau, Athmani S, Schwartz Jc, Garbarg M, and Charon Robin Ganellin

Subjects
Histamine Antagonists, Ether, In Vitro Techniques, Chemical synthesis, Medicinal chemistry, Histamine Release, chemistry.chemical_compound, Mice, In vivo, Drug Discovery, Imidazole, Animals, Receptors, Histamine H3, Cerebral Cortex, Trifluoromethyl, Molecular Structure, Methylhistamines, Antagonist, Imidazoles, Brain, Rats, chemistry, Potassium, Molecular Medicine, Histamine H3 receptor, Histamine, Synaptosomes
Abstract

[[(4-Nitrophenyl)X]alkyl]imidazole isosteres (where X = NH, S, CH2S, O) of previously described [[(5-nitropyrid-2-yl)X]ethyl]imidazoles (where X = NH, S) have been synthesized and evaluated for H3-receptor histamine antagonism in vitro (Ki for [3H]histamine release from rat cerebral cortex synaptosomes) and in vivo (ED50 per os in mice on brain tele-methylhistamine levels). Encouraging results led to the synthesis and testing of a novel series of substituted (phenoxyethyl)- and (phenoxypropyl)imidazoles. From the latter, 4-[3-(4-cyanophenoxy)propyl]-1H-imidazole (10a, UCL 1390; Ki = 12 nM, ED50 = 0.54 mg/kg) and 4-[3-[4-(trifluoromethyl)-phenoxy]propyl]-1H-imidazole (10c, UCL 1409; Ki = 14 nM, ED50 = 0.60 mg/kg) have been selected as potential candidates for drug development. For 16 [(aryloxy)ethyl]imidazoles the relationship between in vitro and in vivo potency is described by the equation log ED50 = 0.47 log Ki + 0.20 (r = 0.78).

Published
1996

39. Structure-activity studies with histamine H3-receptor ligands

Author

C R, Ganellin, A, Fkyerat, S K, Hosseini, Y S, Khalaf, A, Piripitsi, W, Tertiuk, J M, Arrang, M, Garbarg, X, Ligneau, and J C, Schwartz

Subjects
Histamine Agonists, Structure-Activity Relationship, Histamine Antagonists, Animals, Humans
Abstract

Starting from thioperamide, the first potent and selective H3-receptor histamine antagonist, analogues have been synthesised and tested in vitro on rat cerebral cortex to explore structure-activity relationships. The aim has been to design compounds which do not possess the thiourea group of thioperamide and which may have improved brain penetration. Some compounds derived from histamine and possessing an aromatic nitrogen-containing heterocycle on the side-chain amino group show strong H3-antagonist activity. These have served as leads to provide aryloxyethyl- and aryloxy-propylimidazoles which are potent H3 antagonists of histamine. Structure-activity studies of the very potent and selective agonist, imetit (S-[2-imidazol-4-yl)ethyl]isothiourea), have explored the the transition between agonist, partial agonist and antagonist. The isosteric isourea is also a potent agonist. N,N'-Dibutyl-[S-[3-(imidazol-4-yl)propyl]isothiourea is a very potent antagonist having Ki = 1.5 nM.

Published
1995

40. [125I]iodoproxyfan, a new antagonist to label and visualize cerebral histamine H3 receptors

Author

X, Ligneau, M, Garbarg, M L, Vizuete, J, Diaz, K, Purand, H, Stark, W, Schunack, and J C, Schwartz

Subjects
Brain Chemistry, Male, Guanylyl Imidodiphosphate, Binding Sites, Methylhistamines, Histamine Antagonists, Imidazoles, Corpus Striatum, Rats, Iodine Radioisotopes, Kinetics, Animals, Autoradiography, Receptors, Histamine H3, Rats, Wistar
Abstract

Iodoproxyfan, i.e., 3-(1H-imidazol-4-yl)propyl-(4-iodophenyl)-methyl ether, is a novel potent and selective histamine H3 receptor antagonist. [125I]Iodoproxyfan binding to membranes of the rat striatum was reversible and saturable. Specific binding defined with 1 microM (R)-alpha-methylhistamine corresponded to 65% of the total at 30 pM. Scatchard analysis indicated a Kd of 65 pM and maximal binding capacity of 78 fmol/mg of protein. The specificity of [125I]Iodoproxyfan binding to H3 receptors was demonstrated by its pharmacological profile. A series of H3 receptor agonists inhibited [125I]iodoproxyfan binding with a similar maximal effect and with the expected order of potency and stereoselectivity ratio. H3 receptor antagonists inhibited the specific binding with the expected Ki values. In the presence of guanylnucleotides, 40% of sites exhibited a approximately 40-fold lower affinity for histamine, indicating that the H3 receptor belongs to the superfamily of G protein-coupled receptors and revealing the existence of two populations of sites. Well contrasted autoradiographic pictures of total [125I]iodoproxyfan binding to sections of the rat brain were obtained in a short time and over a low nonspecific binding. The heterogenous distribution of H3 receptors with high labeling of anterior cerebral cortex, ventral striatum and other limbic areas was confirmed. In addition, a clearly distinguishable laminated pattern of labeling was evidenced in the cerebral cortex and hippocampal formation. Hence, this new probe should be useful for sensitive assay and localization of the H3 receptor.

Published
1994

41. 5. Histamine receptor expression¶Impact of lipophilicity on the pharmacological properties of histamine H3-receptor antagonists of the cycloalkyl carbamate class

Author

Astrid Sasse, Walter Schunack, Katarzyna Kieć-Kononowicz, X Ligneau, Małgorzata Więcek, J.-C. Schwartz, and Holger Stark

Subjects
Pharmacology, Carbamate, Chemistry, medicine.medical_treatment, Immunology, Lipophilicity, Pharmacology toxicology, Thin layer, medicine, Structure–activity relationship, Histamine H3 receptor, Receptor
Published
2002

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

Author

M, Garbarg, J M, Arrang, A, Rouleau, X, Ligneau, M D, Tuong, J C, Schwartz, and C R, Ganellin

Subjects
Cerebral Cortex, Histamine N-Methyltransferase, Methylhistamines, Guinea Pigs, Imidazoles, Thiourea, Histamine Release, Rats, Histamine Agonists, Mice, Animals, Receptors, Histamine, Receptors, Histamine H3, Urea
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

43. Corrigendum to 'Fluorinated non-imidazole histamine H3 receptor antagonists' [Bioorg. Med. Chem. Lett. 19 (2009) 2172]

Author

X. Ligneau, J.-C. Schwartz, A. Garlapati, Holger Stark, Marc Capet, Michael Amon, Kathleen Isensee, and Jean-Claude Camelin

Subjects
chemistry.chemical_compound, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Imidazole, Histamine H3 receptor, Molecular Biology, Biochemistry
Abstract

Corrigendum Corrigendum to ‘‘Fluorinated non-imidazole histamine H3 receptor antagonists” [Bioorg. Med. Chem. Lett. 19 (2009) 2172] K. Isensee , M. Amon , A. Garlapati , X. Ligneau , J.-C. Camelin , M. Capet , J.-C. Schwartz , H. Stark a,* a Johann Wolfgang Goethe-Universitat, Institut fur Pharmazeutische Chemie, Biozentrum, ZAFES/LiFF/CMP, Max-von-Laue-Str. 9, 60438 Frankfurt, Germany Department of Medicinal Chemistry, University College of Pharmaceutical Sciences, Kakatiya University, Warangal 506 009, AP, India Bioprojet-Biotech, 4 rue du Chesnay Beauregard, BP 96205, 35762 Saint Gregoire Cedex, France

Published
2009

44. Administration of oxathridine, a first-in-class histamine-3 receptor partial agonist in healthy male volunteers: Central nervous system depression and pseudo-hallucinations.

Author

Dijkstra FM, Zuiker RGJA, Heuberger JAAC, Kanhai KMS, De Kam M, Duvauchelle T, Lecomte JM, Labeeuw O, Landais L, Ligneau X, Robert P, Capet M, Schwartz JC, and van Gerven JMA

Subjects
Humans, Male, Electroencephalography, Central Nervous System, Hallucinations, Double-Blind Method, Healthy Volunteers, Dose-Response Relationship, Drug, Histamine, Depression
Abstract

Aims: To characterise the safety, tolerability, pharmacokinetics (PK) and pharmacodynamics (PD) of single ascending doses of oxathridine, a first-in-class histamine-3 receptor partialagonist, in healthy male volunteers., Methods: A randomised, double-blind, placebo-controlled study including the NeuroCart, consisting of a battery of drug sensitive neurophysiological tests, was performed. Oxathridine was administered orally as an aqueous solution. After dosing, safety and NeuroCart tests (adaptive tracking [AT], body sway [BS], saccadic peak velocity [SPV], smooth pursuit [SP] eye movements, VAS according to Bond and Lader, VAS according to Bowdle [VAS B&L, Bowdle], pharmaco-electroencephalogram [pEEG], Sustained Attention to Response Task [SART]) were performed at set times., Results: Forty volunteers completed the study. Given doses were: 0.5, 2.5, 5, 0.25 and 1.5 mg. At 5 mg, unacceptable and unanticipated adverse events (AEs) of (orthostatic) hypotension and pseudo-hallucinations were reported. Statistically significant effects ([CI]; p-value) of 2.5 mg and 5 mg oxathridine were observed on AT ([-8.28, -1.60]; p = 0.0048), ([-8.10, -1.51]; p = 0.00530), BS ([0.6, 80.2]; p = 0.0455), ([5.9, 93.1]; p = 0.0205) and SPV ([-59.0, -15.9]; p = 0.0011), ([-43.9, -1.09]; p = 0.0399), respectively. Oxathridine 5 mg significantly increased all three VAS Bowdle subscale scores; VAS external ([0.183, 0.476]; p = <.0001), VAS internal ([0.127, 0.370]; p = 0.0001) and VAS feeling high ([0.263, 0.887]; p = 0.0006)., Conclusion: NeuroCart tests indicated central nervous system (CNS) depressant effects. Oxathridine also unexpectedly caused pseudohallucinations. Although this led to the decision to stop further development of oxathridine, these observations suggest that the H3R system could be an interesting new target for the development of novel antipsychotics., (© 2023 British Pharmacological Society.)

Published
2024
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45. Pitolisant, a wake-promoting agent devoid of psychostimulant properties: Preclinical comparison with amphetamine, modafinil, and solriamfetol.

Author

Krief S, Berrebi-Bertrand I, Nagmar I, Giret M, Belliard S, Perrin D, Uguen M, Robert P, Lecomte JM, Schwartz JC, Finance O, and Ligneau X

Subjects
3,4-Dihydroxyphenylacetic Acid metabolism, Adrenergic Uptake Inhibitors pharmacology, Animals, Corpus Striatum metabolism, Disorders of Excessive Somnolence etiology, Dopamine metabolism, Dopamine Plasma Membrane Transport Proteins drug effects, Dopamine Plasma Membrane Transport Proteins metabolism, Dopamine Uptake Inhibitors pharmacology, Drug Evaluation, Preclinical, Drug Inverse Agonism, Histamine Antagonists pharmacology, Mice, Narcolepsy drug therapy, Neostriatum drug effects, Neostriatum metabolism, Norepinephrine Plasma Membrane Transport Proteins drug effects, Norepinephrine Plasma Membrane Transport Proteins metabolism, Nucleus Accumbens drug effects, Nucleus Accumbens metabolism, Phenylalanine pharmacology, Receptors, Histamine H3, Sleep Apnea, Obstructive complications, Amphetamine pharmacology, Carbamates pharmacology, Corpus Striatum drug effects, Disorders of Excessive Somnolence drug therapy, Feeding Behavior drug effects, Locomotion drug effects, Modafinil pharmacology, Phenylalanine analogs & derivatives, Piperidines pharmacology, Wakefulness-Promoting Agents pharmacology
Abstract

Several therapeutic options are currently available to treat excessive daytime sleepiness (EDS) in patients suffering from narcolepsy or obstructive sleep apnea. However, there are no comparisons between the various wake-promoting agents in terms of mechanism of action, efficacy, or safety. The goal of this study was to compare amphetamine, modafinil, solriamfetol, and pitolisant at their known primary pharmacological targets, histamine H3 receptors (H3R), dopamine, norepinephrine, and serotonin transporters, and in various in vivo preclinical models in relation to neurochemistry, locomotion, behavioral sensitization, and food intake. Results confirmed that the primary pharmacological effect of amphetamine, modafinil, and solriamfetol was to increase central dopamine neurotransmission, in part by inhibiting its transporter. Furthermore, solriamfetol increased levels of extracellular dopamine in the nucleus accumbens, and decreased the 3,4-dihydroxyphenyl acetic acid (DOPAC)/DA ratio in the striatum, as reported for modafinil and amphetamine. All these compounds produced hyperlocomotion, behavioral sensitization, and hypophagia, which are common features of psychostimulants and of compounds with abuse potential. In contrast, pitolisant, a selective and potent H3R antagonist/inverse agonist that promotes wakefulness, had no effect on striatal dopamine, locomotion, or food intake. In addition, pitolisant, devoid of behavioral sensitization by itself, attenuated the hyperlocomotion induced by either modafinil or solriamfetol. Therefore, pitolisant presents biochemical, neurochemical, and behavioral profiles different from those of amphetamine and other psychostimulants such as modafinil or solriamfetol. In conclusion, pitolisant is a differentiated therapeutic option, when compared with psychostimulants, for the treatment of EDS, as this agent does not show any amphetamine-like properties within in vivo preclinical models., (© 2021 Bioprojet Biotech. Pharmacology Research & Perspectives published by British Pharmacological Society and American Society for Pharmacology and Experimental Therapeutics and John Wiley & Sons Ltd.)

Published
2021
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46. Nonclinical cardiovascular safety of pitolisant: comparing International Conference on Harmonization S7B and Comprehensive in vitro Pro-arrhythmia Assay initiative studies.

Author

Ligneau X, Shah RR, Berrebi-Bertrand I, Mirams GR, Robert P, Landais L, Maison-Blanche P, Faivre JF, Lecomte JM, and Schwartz JC

Subjects
Animals, Arrhythmias, Cardiac physiopathology, Computer Simulation, Disease Models, Animal, Dogs, Electrocardiography, Female, Humans, Ion Channels drug effects, Ion Channels metabolism, Male, Myocytes, Cardiac metabolism, Purkinje Fibers drug effects, Purkinje Fibers metabolism, Rabbits, Research Design, Arrhythmias, Cardiac chemically induced, Myocytes, Cardiac drug effects, Piperidines adverse effects
Abstract

Background and Purpose: We evaluated the concordance of results from two sets of nonclinical cardiovascular safety studies on pitolisant., Experimental Approach: Nonclinical studies envisaged both in the International Conference on Harmonization (ICH) S7B guideline and Comprehensive in vitro Pro-arrhythmia Assay (CiPA) initiative were undertaken. The CiPA initiative included in vitro ion channels, stem cell-derived human ventricular myocytes, and in silico modelling to simulate human ventricular electrophysiology. ICH S7B-recommended assays included in vitro hERG (K V 11.1) channels, in vivo dog studies with follow-up investigations in rabbit Purkinje fibres and the in vivo Carlsson rabbit pro-arrhythmia model., Key Results: Both sets of nonclinical data consistently excluded pitolisant from having clinically relevant QT-liability or pro-arrhythmic potential. CiPA studies revealed pitolisant to have modest calcium channel blocking and late I Na reducing activities at high concentrations, which resulted in pitolisant reducing dofetilide-induced early after-depolarizations (EADs) in the ICH S7B studies. Studies in stem cell-derived human cardiomyocytes with dofetilide or E-4031 given alone and in combination with pitolisant confirmed these properties. In silico modelling confirmed that the ion channel effects measured are consistent with results from both the stem cell-derived cardiomyocytes and rabbit Purkinje fibres and categorized pitolisant as a drug with low torsadogenic potential. Results from the two sets of nonclinical studies correlated well with those from two clinical QT studies., Conclusions and Implications: Our findings support the CiPA initiative but suggest that sponsors should consider investigating drug effects on EADs and the use of pro-arrhythmia models when the results from CiPA studies are ambiguous., (© 2017 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published
2017
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47. Synthesis and evaluation of a 2-benzothiazolylphenylmethyl ether class of histamine H4 receptor antagonists.

Author

Labeeuw O, Levoin N, Billot X, Danvy D, Calmels T, Krief S, Ligneau X, Berrebi-Bertrand I, Robert P, Lecomte JM, Schwartz JC, and Capet M

Subjects
Benzothiazoles chemistry, Benzothiazoles pharmacology, Cell Line, Drug Evaluation, Preclinical, Humans, Receptors, Histamine, Receptors, Histamine H4, Benzothiazoles chemical synthesis, Histamine Antagonists chemical synthesis, Histamine Antagonists pharmacology, Receptors, G-Protein-Coupled antagonists & inhibitors
Abstract

Synthesis and biological evaluation of a new class of histamine H 4 receptor ligands, distinct from the previously reported chemotypes, are described. A virtual screening of our corporate compound collection identified a hit with an undesired dual H3R/H4R activity. Chemical exploration led to the discovery of a more potent and selective 2-benzothiazolylphenylmethyl ether lead compound., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published
2016
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48. Preclinical evaluation of the abuse potential of Pitolisant, a histamine H₃ receptor inverse agonist/antagonist compared with Modafinil.

Author

Uguen M, Perrin D, Belliard S, Ligneau X, Beardsley PM, Lecomte JM, and Schwartz JC

Subjects
Animals, Behavior, Addictive prevention & control, Behavior, Animal drug effects, Benzhydryl Compounds adverse effects, Central Nervous System Stimulants adverse effects, Dopamine chemistry, Dopamine metabolism, Dopaminergic Neurons drug effects, Dopaminergic Neurons metabolism, Dose-Response Relationship, Drug, Drug Antagonism, Drug Evaluation, Preclinical, Drug Inverse Agonism, Drugs, Investigational administration & dosage, Drugs, Investigational therapeutic use, Histamine Agonists administration & dosage, Histamine Agonists therapeutic use, Histamine Antagonists administration & dosage, Histamine Antagonists therapeutic use, Macaca mulatta, Male, Mice, Modafinil, Motor Activity drug effects, Nucleus Accumbens drug effects, Nucleus Accumbens metabolism, Piperidines administration & dosage, Piperidines therapeutic use, Rats, Receptors, Histamine H3 chemistry, Wakefulness-Promoting Agents administration & dosage, Wakefulness-Promoting Agents therapeutic use, Behavior, Addictive chemically induced, Drugs, Investigational adverse effects, Histamine Agonists adverse effects, Histamine Antagonists adverse effects, Piperidines adverse effects, Receptors, Histamine H3 metabolism, Wakefulness-Promoting Agents adverse effects
Abstract

Background and Purpose: Pitolisant, a histamine H₃ receptor inverse agonist/antagonist is currently under Phase III clinical trials for treatment of excessive daytime sleepiness namely in narcoleptic patients. Its drug abuse potential was investigated using in vivo models in rodents and monkeys and compared with those of Modafinil, a psychostimulant currently used in the same indications., Experimental Approach: Effects of Pitolisant on dopamine release in the nucleus accumbens, on spontaneous and cocaine-induced locomotion, locomotor sensitization were monitored. It was also tested in three standard drug abuse tests i.e. conditioned place preference in rats, self-administration in monkeys and cocaine discrimination in mice as well as in a physical dependence model., Key Results: Pitolisant did not elicit any significant changes in dopaminergic indices in rat nucleus accumbens whereas Modafinil increased dopamine release. In rodents, Pitolisant was without any effect on locomotion and reduced the cocaine-induced hyperlocomotion. In addition, no locomotor sensitization and no conditioned hyperlocomotion were evidenced with this compound in rats whereas significant effects were elicited by Modafinil. Finally, Pitolisant was devoid of any significant effects in the three standard drug abuse tests (including self-administration in monkeys) and in the physical dependence model., Conclusions and Implications: No potential drug abuse liability for Pitolisant was evidenced in various in vivo rodent and primate models, whereas the same does not seem so clear in the case of Modafinil., (© 2013 The Authors. British Journal of Pharmacology © 2013 The British Pharmacological Society.)

Published
2013
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49. Novel and highly potent histamine H3 receptor ligands. Part 3: an alcohol function to improve the pharmacokinetic profile.

Author

Labeeuw O, Levoin N, Poupardin-Olivier O, Calmels T, Ligneau X, Berrebi-Bertrand I, Robert P, Lecomte JM, Schwartz JC, and Capet M

Subjects
Animals, Binding Sites, Cyclohexanols chemical synthesis, Cyclohexanols pharmacokinetics, Drug Inverse Agonism, Half-Life, Histamine H3 Antagonists chemical synthesis, Histamine H3 Antagonists pharmacokinetics, Humans, Male, Mice, Molecular Docking Simulation, Protein Binding, Protein Structure, Tertiary, Receptors, Histamine H3 genetics, Receptors, Histamine H3 metabolism, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Cyclohexanols chemistry, Ethanol chemistry, Histamine H3 Antagonists chemistry, Ligands, Receptors, Histamine H3 chemistry
Abstract

Synthesis and biological evaluation of potent histamine H3 receptor antagonists incorporating a hydroxyl function are described. Compounds in this series exhibited nanomolar binding affinities for human receptor, illustrating a new possible component for the H3 pharmacophore. As demonstrated with compound BP1.4160 (cyclohexanol 19), the introduction of an alcohol function counter-intuitively allowed to reach high in vivo efficiency and favorable pharmacokinetic profile with reduced half-life., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published
2013
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50. Novel and highly potent histamine H3 receptor ligands. Part 2: exploring the cyclohexylamine-based series.

Author

Labeeuw O, Levoin N, Poupardin-Olivier O, Calmels T, Ligneau X, Berrebi-Bertrand I, Robert P, Lecomte JM, Schwartz JC, and Capet M

Subjects
Animals, Cyclohexylamines chemical synthesis, Cyclohexylamines chemistry, Dose-Response Relationship, Drug, Histamine Agonists chemical synthesis, Histamine Agonists chemistry, Humans, Ligands, Mice, Models, Molecular, Molecular Structure, Receptors, Histamine H3 metabolism, Stereoisomerism, Structure-Activity Relationship, Trans-Activators metabolism, Transcriptional Regulator ERG, Cyclohexylamines pharmacology, Histamine Agonists pharmacology, Trans-Activators antagonists & inhibitors
Abstract

Synthesis and biological evaluation of novel and potent cyclohexylamine-based histamine H3 receptor inverse agonists are described. Compounds in this newly identified series exhibited subnanomolar binding affinities for human receptor and no significant interaction with hERG channel. One derivative (10t) demonstrated enhanced in vivo efficiency and preferential brain distribution, both properties suitable for potential clinical evaluation., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published
2011
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