Your search keyword '"Armin Buschauer"' showing total 24 results

1. Abolishing Dopamine D2long/D3 Receptor Affinity of Subtype-Selective Carbamoylguanidine-Type Histamine H2 Receptor Agonists

Author

Merlin Bresinsky, Lisa Forster, Steffen Pockes, Denise Mönnich, Andrea Strasser, Harald Hübner, Peter Gmeiner, Katharina Tropmann, Hans-Joachim Wittmann, and Armin Buschauer

Subjects

0303 health sciences, Chemistry, Central nervous system, Subtype selective, 01 natural sciences, Affinities, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, medicine.anatomical_structure, Histamine H2 receptor, Biochemistry, Docking (molecular), Dopamine receptor D3, Dopamine, Drug Discovery, medicine, Molecular Medicine, Receptor, 030304 developmental biology, medicine.drug

Abstract

3-(2-Amino-4-methylthiazol-5-yl)propyl-substituted carbamoylguanidines are potent, subtype-selective histamine H2 receptor (H2R) agonists, but their applicability as pharmacological tools to elucidate the largely unknown H2R functions in the central nervous system (CNS) is compromised by their concomitant high affinity toward dopamine D2-like receptors (especially to the D3R). To improve the selectivity, a series of novel carbamoylguanidine-type ligands containing various heterocycles, spacers, and side residues were rationally designed, synthesized, and tested in binding and/or functional assays at H1-4 and D2long/3 receptors. This study revealed a couple of selective candidates (among others 31 and 47), and the most promising ones were screened at several off-target receptors, showing good selectivities. Docking studies suggest that the amino acid residues (3.28, 3.32, E2.49, E2.51, 5.42, and 7.35) are responsible for the different affinities at the H2- and D2long/3-receptors. These results provide a solid base for the exploration of the H2R functions in the brain in further studies.

Published

2021

2. UR-DEBa242: A Py-5-Labeled Fluorescent Multipurpose Probe for Investigations on the Histamine H3 and H4 Receptors

Author

Ulla Seibel, Günther Bernhardt, David Wifling, Timo Littmann, Edith Bartole, Lukas Grätz, and Armin Buschauer

Subjects

0303 health sciences, Chemistry, 01 natural sciences, Fluorescence, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, Biochemistry, Drug Discovery, Molecular Medicine, Histamine H3 receptor, Receptor, Histamine, 030304 developmental biology

Abstract

Comprehensively characterized fluorescent probes for the histamine H3 receptor (H3R) and especially for the H4R orthologs [e.g., human (h) and mouse (m)] are highly needed as versatile complementar...

Published

2020

3. [3H]UR-DEBa176: A 2,4-Diaminopyrimidine-Type Radioligand Enabling Binding Studies at the Human, Mouse, and Rat Histamine H4 Receptors

Author

Günther Bernhardt, Takeaki Ozawa, Timo Littmann, Edith Bartole, Miho Tanaka, and Armin Buschauer

Subjects

0303 health sciences, Reporter gene, Chemistry, Ligand, Stereochemistry, 01 natural sciences, Radioligand Assay, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, Diaminopyrimidine, Drug Discovery, Radioligand, Molecular Medicine, Structure–activity relationship, Receptor, Histamine, 030304 developmental biology

Abstract

Differences in sequence homology between human (h), mouse (m), and rat (r) histamine H4 receptors (H4R) cause discrepancies regarding affinities, potencies, and/or efficacies of ligands and therefore compromise translational animal models and the applicability of radioligands. Aiming at a radioligand enabling robust and comparative binding studies at the h/m/rH4Rs, 2,4-diaminopyrimidines were synthesized and pharmacologically investigated. The most notable compounds identified were two (partial) agonists with comparable potencies at the h/m/rH4Rs: UR-DEBa148 (N-neopentyl-4-(1,4,6,7-tetrahydro-5H-imidazo[4,5-c]pyridin-5-yl)pyrimidin-2-amine bis(2,2,2-trifluoroacetate), 43), the most potent [pEC50 (reporter gene assay) = 9.9/9.6/10.3] compound in the series being slightly G-protein biased and UR-DEBa176 [(R)-4-[3-(dimethylamino)pyrrolidin-1-yl]-N-neopentylpyrimidin-2-amine bis(2,2,2-trifluoroacetate), 46, pEC50 (reporter gene assay) = 8.7/9.0/9.2], a potential "cold" form of a tritiated H4R ligand. After radiolabeling, binding studies with [3H]UR-DEBa176 ([3H]46) at the h/m/rH4Rs revealed comparable Kd values (41/17/22 nM), low nonspecific binding (11-17%, ∼Kd), and fast associations/dissociations (25-30 min) and disclosed [3H]UR-DEBa176 as useful molecular tool to determine h/m/rH4R binding affinities for H4R ligands.

Published

2019

4. Abolishing Dopamine D

Author

Katharina, Tropmann, Merlin, Bresinsky, Lisa, Forster, Denise, Mönnich, Armin, Buschauer, Hans-Joachim, Wittmann, Harald, Hübner, Peter, Gmeiner, Steffen, Pockes, and Andrea, Strasser

Subjects

Binding Sites, Molecular Structure, Receptors, Dopamine D2, Guinea Pigs, Receptors, Dopamine D3, Guanidines, Rats, Histamine Agonists, Molecular Docking Simulation, Mice, Structure-Activity Relationship, Thiazoles, HEK293 Cells, Sf9 Cells, Animals, Humans, Receptors, Histamine H2

Abstract

3-(2-Amino-4-methylthiazol-5-yl)propyl-substituted carbamoylguanidines are potent, subtype-selective histamine H

Published

2021

5. UR-DEBa242: A Py-5-Labeled Fluorescent Multipurpose Probe for Investigations on the Histamine H

Author

Edith, Bartole, Lukas, Grätz, Timo, Littmann, David, Wifling, Ulla, Seibel, Armin, Buschauer, and Günther, Bernhardt

Subjects

HEK293 Cells, Sf9 Cells, Animals, Humans, Receptors, Histamine H3, Fluorescent Dyes, Receptors, Histamine H4

Abstract

Comprehensively characterized fluorescent probes for the histamine H

Published

2020

6. Conformational Restriction and Enantioseparation Increase Potency and Selectivity of Cyanoguanidine-Type Histamine H4 Receptor Agonists

Author

Uwe Nordemann, Roland Geyer, Andrea Strasser, Armin Buschauer, and Hans-Joachim Wittmann

Subjects

Models, Molecular, 0301 basic medicine, Agonist, Protein Conformation, medicine.drug_class, Stereochemistry, Molecular Conformation, Molecular Dynamics Simulation, Spodoptera, Guanidines, 01 natural sciences, Receptors, G-Protein-Coupled, Histamine Agonists, Mice, Radioligand Assay, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Sf9 Cells, medicine, Animals, Humans, Luciferase, Histamine H4 receptor, Guanidine, Receptors, Histamine H4, 010405 organic chemistry, Imidazoles, Stereoisomerism, 0104 chemical sciences, Chiral column chromatography, HEK293 Cells, 030104 developmental biology, Membrane, chemistry, Guanosine 5'-O-(3-Thiotriphosphate), Receptors, Histamine, Molecular Medicine, Selectivity, Linker

Abstract

2-Cyano-1-[4-(1H-imidazol-4-yl)butyl]-3-[2-(phenylsulfanyl)ethyl]guanidine (UR-PI376, 1) is a potent and selective agonist of the human histamine H4 receptor (hH4R). To gain information on the active conformation, we synthesized analogues of 1 with a cyclopentane-1,3-diyl linker. Affinities and functional activities were determined at recombinant hHxR (x: 1-4) subtypes on Sf9 cell membranes (radioligand binding, [(35)S]GTPγS, or GTPase assays) and in part in luciferase assays on human or mouse H4R (HEK-293 cells). The most potent H4R agonists among 14 racemates were separated by chiral HPLC, yielding eight enantiomerically pure compounds. Configurations were assigned based on X-ray structures of intermediates and a stereocontrolled synthetic pathway. (+)-2-Cyano-1-{[trans-(1S,3S)-3-(1H-imidazol-4-yl)cyclopentyl]methyl}-3-[2-(phenylsulfanyl)ethyl]guanidine ((1S,3S)-UR-RG98, 39a) was the most potent H4R agonist in this series (EC50 11 nM; H4R vs H3R,100-fold selectivity; H1R, H2R, negligible activities), whereas the optical antipode proved to be an H4R antagonist ([(35)S]GTPγS assay). MD simulations confirmed differential stabilization of the active and inactive H4R state by the enantiomers.

Published

2016

7. Nω-Carbamoylation of the Argininamide Moiety: An Avenue to Insurmountable NPY Y1 Receptor Antagonists and a Radiolabeled Selective High-Affinity Molecular Tool ([3H]UR-MK299) with Extended Residence Time

Author

Max Keller, Burkhard König, Stefanie Dukorn, Günther Bernhardt, Kilian K. Kuhn, Armin Buschauer, Lisa Schindler, Christoph Hutzler, Catherine Mollereau, and Stefan Weiss

Subjects

Receptors, Neuropeptide, Fura-2, Arginine, Stereochemistry, chemistry.chemical_element, CHO Cells, Calcium, Binding, Competitive, Cell Line, Structure-Activity Relationship, chemistry.chemical_compound, Cricetulus, Cricetinae, Drug Discovery, Animals, Humans, Moiety, Structure–activity relationship, Neuropeptide Y, Guanidine, Diphenylacetic Acids, Fluorescent Dyes, Antagonist, Amides, Receptors, Neuropeptide Y, Dissociation constant, chemistry, Isotope Labeling, Molecular Probes, Molecular Medicine, Radiopharmaceuticals, Half-Life

Abstract

Analogues of the argininamide-type NPY Y1 receptor (Y1R) antagonist BIBP3226, bearing carbamoyl moieties at the guanidine group, revealed subnanomolar Ki values and caused depression of the maximal response to NPY (calcium assay) by up to 90% in a concentration- and time-dependent manner, suggesting insurmountable antagonism. To gain insight into the mechanism of binding of the synthesized compounds, a tritiated antagonist, (R)-N(α)-diphenylacetyl-N(ω)-[2-([2,3-(3)H]propionylamino)ethyl]aminocarbonyl-(4-hydroxybenzyl)arginin-amide ([(3)H]UR-MK299, [(3)H]38), was prepared. [(3)H]38 revealed a dissociation constant in the picomolar range (Kd 0.044 nM, SK-N-MC cells) and very high Y1R selectivity. Apart from superior affinity, a considerably lower target off-rate (t1/2 95 min) was characteristic of [(3)H]38 compared to that of the higher homologue containing a tetramethylene instead of an ethylene spacer (t1/2 3 min, Kd 2.0 nM). Y1R binding of [(3)H]38 was fully reversible and fully displaceable by nonpeptide antagonists and the agonist pNPY. Therefore, the insurmountable antagonism observed in the functional assay has to be attributed to the extended target-residence time, a phenomenon of relevance in drug research beyond the NPY receptor field.

Published

2015

8. Loratadine and Analogues: Discovery and Preliminary Structure–Activity Relationship of Inhibitors of the Amino Acid Transporter B0AT2

Author

Armin Buschauer, Serena Cuboni, Klaus T. Wanner, Christian Devigny, Barbara Hauger, Georg Höfner, Sebastian Pomplun, Matthias Eder, Florian Holsboer, B. Hoogeland, Andrea Strasser, and Felix Hausch

Subjects

Histamine H1 Antagonists, Non-Sedating, Patch-Clamp Techniques, Chemistry, Pharmaceutical, Green Fluorescent Proteins, Nerve Tissue Proteins, Histamine H1 receptor, Loratadine, Pharmacology, Binding, Competitive, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, medicine, Humans, Structure–activity relationship, Receptors, Histamine H1, Amino acid transporter, Receptor, IC50, Chemistry, Cell Membrane, Antagonist, Brain, Transporter, Electrophysiology, Kinetics, Amino Acid Transport Systems, Neutral, HEK293 Cells, Biochemistry, Molecular Medicine, medicine.drug

Abstract

B(0)AT2, encoded by the SLC6A15 gene, is a transporter for neutral amino acids that has recently been implicated in mood and metabolic disorders. It is predominantly expressed in the brain, but little is otherwise known about its function. To identify inhibitors for this transporter, we screened a library of 3133 different bioactive compounds. Loratadine, a clinically used histamine H1 receptor antagonist, was identified as a selective inhibitor of B(0)AT2 with an IC50 of 4 μM while being less active or inactive against several other members of the SLC6 family. Reversible inhibition of B(0)AT2 was confirmed by electrophysiology. A series of loratadine analogues were synthesized to gain insight into the structure-activity relationships. Our studies provide the first chemical tool for B(0)AT2.

Published

2014

9. High Affinity Agonists of the Neuropeptide Y (NPY) Y4 Receptor Derived from the C-Terminal Pentapeptide of Human Pancreatic Polypeptide (hPP): Synthesis, Stereochemical Discrimination, and Radiolabeling

Author

Max Keller, Oliver Reiser, Stefanie Dukorn, Thomas Ertl, Kilian K. Kuhn, Armin Buschauer, and Günther Bernhardt

Subjects

0301 basic medicine, Agonist, Arginine, medicine.drug_class, Stereochemistry, Stereoisomerism, CHO Cells, Pancreatic Polypeptide, Pentapeptide repeat, 03 medical and health sciences, Cricetulus, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Amino Acid Sequence, Protein Precursors, Receptor, Peptide sequence, Chemistry, Neuropeptide Y receptor, Receptors, Neuropeptide Y, 030104 developmental biology, HEK293 Cells, Biochemistry, Molecular Medicine, Linker

Abstract

The diastereomeric mixture of d/l-2,7-diaminooctanedioyl-bis(YRLRY-NH2) (BVD-74D, 2) was described in the literature as a high affinity Y4 receptor agonist. Here we report on the synthesis and pharmacological characterization of the pure diastereomers (2R,7R)- and (2S,7S)-2 and a series of homo- and heterodimeric analogues in which octanedioic acid was used as an achiral linker. To investigate the role of the Arg residues, one or two arginines were replaced by Ala. Moreover, N(ω)-(6-aminohexylaminocarbonyl)Arg was introduced as an arginine replacement (17). (2R,7R)-2 was superior to (2S,7S)-2 in binding and functional cellular assays and equipotent with 17. [(3)H]Propionylation of one amino group in the linker of (2R,7R)-2 or at the primary amino group in 17 resulted in high affinity Y4R radioligands ([(3)H]-(2R,7R)-10, [(3)H]18) with subnanomolar Kd values.

Published

2016

10. The Bivalent Ligand Approach Leads to Highly Potent and Selective Acylguanidine-Type Histamine H2 Receptor Agonists

Author

Nicole Kagermeier, Miroslaw Lopuch, Stefan Dove, Tobias Birnkammer, Irena Brunskole, Armin Buschauer, Günther Bernhardt, Anja Spickenreither, Roland Seifert, and Sigurd Elz

Subjects

chemistry.chemical_compound, Histamine H2 receptor, Chemistry, Ligand, Stereochemistry, Drug Discovery, Molecular Medicine, Imidazole, Structure–activity relationship, Protomer, Binding site, Receptor, Histamine

Abstract

Bivalent histamine H(2) receptor (H(2)R) agonists were synthesized by connecting pharmacophoric 3-(2-amino-4-methylthiazol-5-yl)-, 3-(2-aminothiazol-5-yl)-, 3-(imidazol-4-yl)-, or 3-(1,2,4-triazol-5-yl)propylguanidine moieties by N(G)-acylation with alkanedioic acids of various chain lengths. The compounds were investigated for H(2)R agonism in GTPase and [(35)S]GTPγS binding assays at guinea pig (gp) and human (h) H(2)R-Gsα(S) fusion proteins including various H(2)R mutants, at the isolated gp right atrium, and in GTPase assays for activity on recombinant H(1), H(3), and H(4) receptors. The bivalent ligands are H(2)R partial or full agonists, up to 2 orders of magnitude more potent than monovalent acylguanidines and, with octanedioyl or decanedioyl spacers, up to 4000 times more potent than histamine at the gpH(2)R. In contrast to their imidazole analogues, the aminothiazoles are highly selective for H(2)R vs other HR subtypes. Compounds with (theoretically) sufficient spacer length (20 CH(2) groups) to simultaneously occupy two orthosteric binding sites in H(2)R dimers are nearly inactive, whereas the highest potency resides in compounds with considerably shorter spacers. Thus, there is no evidence for interaction with H(2)R dimers. The high agonistic potency may result from interaction with an accessory binding site at the same receptor protomer.

Published

2012

11. Acylguanidines as Bioisosteres of Guanidines: NG-Acylated Imidazolylpropylguanidines, a New Class of Histamine H2 Receptor Agonists

Author

Patrick Igel, David Schnell, Max Keller, Armin Buschauer, Manfred Zabel, Günther Bernhardt, Stefan Dove, Carsten Götte, Sigurd Elz, Erich H. Schneider, Roland Seifert, Anja Kraus, and Prasanta Ghorai

Subjects

Models, Molecular, Agonist, Time Factors, Stereochemistry, medicine.drug_class, Acylation, Guinea Pigs, Drug Evaluation, Preclinical, Crystallography, X-Ray, Guanidines, Chemical synthesis, Partial agonist, Cell Line, Histamine Agonists, Structure-Activity Relationship, chemistry.chemical_compound, Histamine H2 receptor, Drug Discovery, medicine, Animals, Humans, Moiety, Receptors, Histamine H2, Receptor, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Imidazoles, Molecular Medicine, Bioisostere, Histamine

Abstract

N1-Aryl(heteroaryl)alkyl-N2-[3-(1H-imidazol-4-yl)propyl]guanidines are potent histamine H2-receptor (H2R) agonists, but their applicability is compromised by the lack of oral bioavailability and CNS penetration. To improve pharmacokinetics, we introduced carbonyl instead of methylene adjacent to the guanidine moiety, decreasing the basicity of the novel H2R agonists by 4-5 orders of magnitude. Some acylguanidines with one phenyl ring were even more potent than their diaryl analogues. As demonstrated by HPLC-MS, the acylguanidines (bioisosteres of the alkylguanidines) were absorbed from the gut of mice and detected in brain. In GTPase assays using recombinant receptors, acylguanidines were more potent at the guinea pig than at the human H2R. At the hH1R and hH3R, the compounds were weak to moderate antagonists or partial agonists. Moreover, potent partial hH4R agonists were identified. Receptor subtype selectivity depends on the imidazolylpropylguanidine moiety (privileged structure), opening an avenue to distinct pharmacological tools including potent H4R agonists.

Published

2008

12. Mimicking of Arginine by Functionalized N(ω)-Carbamoylated Arginine As a New Broadly Applicable Approach to Labeled Bioactive Peptides: High Affinity Angiotensin, Neuropeptide Y, Neuropeptide FF, and Neurotensin Receptor Ligands As Examples

Author

Chiara Cabrele, Harald Hübner, Sabrina Biselli, Peter Gmeiner, Catherine Mollereau, Max Keller, David Wifling, Jürgen Einsiedel, Jaroslava Svobodová, Günther Bernhardt, Armin Buschauer, Kilian K. Kuhn, Patrick Vanderheyden, Experimental Pharmacology, Molecular and Biochemical Pharmacology, and Department of Bio-engineering Sciences

Subjects

0301 basic medicine, Receptors, Neuropeptide, Peptide, Arginine, Ligands, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Peptide synthesis, Humans, Receptors, Neurotensin, Neuropeptide Y, Neuropeptide FF, Neurotensin receptor, Cells, Cultured, Neurotensin, chemistry.chemical_classification, Receptors, Angiotensin, Dose-Response Relationship, Drug, Molecular Structure, Research Support, Non-U.S. Gov't, Angiotensin II, Neuropeptide Y receptor, Peptide Fragments, Amino acid, 030104 developmental biology, chemistry, Biochemistry, Molecular Medicine, Oligopeptides

Abstract

Derivatization of biologically active peptides by conjugation with fluorophores or radionuclide-bearing moieties is an effective and commonly used approach to prepare molecular tools and diagnostic agents. Whereas lysine, cysteine, and N-terminal amino acids have been mostly used for peptide conjugation, we describe a new, widely applicable approach to peptide conjugation based on the nonclassical bioisosteric replacement of the guanidine group in arginine by a functionalized carbamoylguanidine moiety. Four arginine-containing peptide receptor ligands (angiotensin II, neurotensin(8-13), an analogue of the C-terminal pentapeptide of neuropeptide Y, and a neuropeptide FF analogue) were subject of this proof-of-concept study. The N(ω)-carbamoylated arginines, bearing spacers with a terminal amino group, were incorporated into the peptides by standard Fmoc solid phase peptide synthesis. The synthesized chemically stable peptide derivatives showed high receptor affinities with Ki values in the low nanomolar range, even when bulky fluorophores had been attached. Two new tritiated tracers for angiotensin and neurotensin receptors are described.

Published

2016

13. Replacement of Thr32 and Gln34 in the C-terminal neuropeptide Y fragment 25-36 by cis-cyclobutane and cis-cyclopentane β-amino acids shifts selectivity toward the Y(4) receptor

Author

Chiara Cabrele, Oliver Reiser, Günther Bernhardt, Rosa M. Ortuño, Raquel Gutiérrez-Abad, Łukasz Berlicki, Melanie Kaske, Armin Buschauer, and Ona Illa

Subjects

Models, Molecular, Stereochemistry, Cyclobutane, Substrate Specificity, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Tumor Cells, Cultured, Pancreatic polypeptide, Humans, Neuropeptide Y, Amino Acids, Receptor, G protein-coupled receptor, chemistry.chemical_classification, Binding Sites, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Neuropeptide Y receptor, Amino acid, Receptors, Neuropeptide Y, Helix, Molecular Medicine, Selectivity, Cyclobutanes

Abstract

Neuropeptide Y (NPY) and pancreatic polypeptide (PP) control central and peripheral processes by activating the G protein coupled receptors YxR (x = 1, 2, 4, 5). We present analogs of the C-terminal fragments 25-36 and 32-36 of NPY and PP containing (1R,2S)-cyclobutane (βCbu) or (1R,2S)-cyclopentane (βCpe) β-amino acids, which display exclusively Y4R affinity. In particular, [βCpe(34)]-NPY-(25-36) is a Y4R selective partial agonist (EC50 41 ± 6 nM, Emax 71%) that binds Y4R with a Ki of 10 ± 2 nM and a selectivity100-fold relative to Y1R and Y2R and50-fold relative to Y5R. Comparably, [Y(32), βCpe(34)]-NPY(PP)-(32-36) selectively binds and activates Y4R (EC50 94 ± 21 nM, Emax 73%). The NMR structure of [βCpe(34)]-NPY-(25-36) in dodecylphosphatidylcholine micelles shows a short helix at residues 27-32, while the C-terminal segment R(33)βCpe(34)R(35)Y(36) is extended. The biological properties of the βCbu- or βCpe-containing NPY and PP C-terminal fragments encourage the future application of these β-amino acids in the synthesis of selective Y4R ligands.

Published

2013

14. The bivalent ligand approach leads to highly potent and selective acylguanidine-type histamine H₂ receptor agonists

Author

Tobias, Birnkammer, Anja, Spickenreither, Irena, Brunskole, Miroslaw, Lopuch, Nicole, Kagermeier, Günther, Bernhardt, Stefan, Dove, Roland, Seifert, Sigurd, Elz, and Armin, Buschauer

Subjects

Recombinant Fusion Proteins, Cell Membrane, Guinea Pigs, Heart, In Vitro Techniques, Ligands, Guanidines, Histamine Agonists, Structure-Activity Relationship, Mutation, GTP-Binding Protein alpha Subunits, Gs, Animals, Humans, Receptors, Histamine H2, Protein Multimerization, Promoter Regions, Genetic

Abstract

Bivalent histamine H(2) receptor (H(2)R) agonists were synthesized by connecting pharmacophoric 3-(2-amino-4-methylthiazol-5-yl)-, 3-(2-aminothiazol-5-yl)-, 3-(imidazol-4-yl)-, or 3-(1,2,4-triazol-5-yl)propylguanidine moieties by N(G)-acylation with alkanedioic acids of various chain lengths. The compounds were investigated for H(2)R agonism in GTPase and [(35)S]GTPγS binding assays at guinea pig (gp) and human (h) H(2)R-Gsα(S) fusion proteins including various H(2)R mutants, at the isolated gp right atrium, and in GTPase assays for activity on recombinant H(1), H(3), and H(4) receptors. The bivalent ligands are H(2)R partial or full agonists, up to 2 orders of magnitude more potent than monovalent acylguanidines and, with octanedioyl or decanedioyl spacers, up to 4000 times more potent than histamine at the gpH(2)R. In contrast to their imidazole analogues, the aminothiazoles are highly selective for H(2)R vs other HR subtypes. Compounds with (theoretically) sufficient spacer length (20 CH(2) groups) to simultaneously occupy two orthosteric binding sites in H(2)R dimers are nearly inactive, whereas the highest potency resides in compounds with considerably shorter spacers. Thus, there is no evidence for interaction with H(2)R dimers. The high agonistic potency may result from interaction with an accessory binding site at the same receptor protomer.

Published

2012

15. Synthesis and structure-activity relationships of cyanoguanidine-type and structurally related histamine H4 receptor agonists

Author

Roland Seifert, Patrick Igel, Roland Geyer, Andrea Strasser, Armin Buschauer, and Stefan Dove

Subjects

Agonist, Models, Molecular, Stereochemistry, medicine.drug_class, Protein Conformation, Guanidines, Receptors, G-Protein-Coupled, Substrate Specificity, Histamine Agonists, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Histamine H2 receptor, Drug Discovery, medicine, Inverse agonist, Structure–activity relationship, Animals, Humans, Histamine H4 receptor, Guanidine, Receptor, Receptors, Histamine H4, Chemistry, Hydrolysis, Isotope Labeling, Molecular Medicine, Receptors, Histamine, Guanosine Triphosphate, Histamine

Abstract

Recently, we identified high-affinity human histamine H3 (hH3R) and H4 receptor (hH4R) ligands among a series of NG-acylated imidazolylpropylguanidines, which were originally designed as histamine H2 receptor (H2R) agonists. Aiming at selectivity for hH4R, the acylguanidine group was replaced with related moieties. Within a series of cyanoguanidines, 2-cyano-1-[4-(1H-imidazol-4-yl)butyl]-3-[(2-phenylthio)ethyl]guanidine (UR-PI376, 67) was identified as the most potent hH4R agonist (pEC50 = 7.47, alpha = 0.93) showing negligible hH1R and hH2R activities and significant selectivity over the hH3R (pKB = 6.00, alpha = -0.28), as determined in steady-state GTPase assays using membrane preparations of hH(x)R-expressing Sf9 cells. In contrast to previously described selective H4R agonists, this compound and other 3-substituted derivatives are devoid of agonistic activity at the other HR subtypes. Modeling of the binding mode of 67 suggests that the cyanoguanidine moiety forms charge-assisted hydrogen bonds not only with the conserved Asp-94 but also with the hH4R-specific Arg-341 residue. 2-Carbamoyl-1-[2-(1H-imidazol-4-yl)ethyl]-3-(3-phenylpropyl)guanidine (UR-PI97, 88) was unexpectedly identified as a highly potent and selective hH3R inverse agonist (pKB = 8.42, >300-fold selectivity over the other HR subtypes).

Published

2009

16. N(G)-acylated imidazolylpropylguanidines as potent histamine H4 receptor agonists: selectivity by variation of the N(G)-substituent

Author

David Schnell, Patrick Igel, Sigurd Elz, Roland Seifert, Armin Buschauer, and Erich H. Schneider

Subjects

Agonist, Insecta, Intrinsic activity, Stereochemistry, medicine.drug_class, Recombinant Fusion Proteins, Substituent, Alpha (ethology), Chemical synthesis, Guanidines, Cell Line, Receptors, G-Protein-Coupled, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, medicine, Structure–activity relationship, Animals, Humans, Histamine H4 receptor, Receptors, Histamine H4, Imidazoles, chemistry, Molecular Medicine, Receptors, Histamine, Selectivity

Abstract

3-(1H-Imidazol-4-yl)propylguanidine (SKF 91486, 4) was identified as a potent partial agonist at the human histamine H(3) receptor (hH(3)R) and human histamine H(4) receptor (hH(4)R). With the aim to increase selectivity for the hH(4)R, the guanidine group in 4 was acylated. N(1)-Acetyl-N(2)-[3-(1H-imidazol-4-yl)propyl]guanidine (UR-PI288, 13) was a potent full agonist at the hH(4)R (pEC(50) = 8.31; alpha = 1.00), possessing more than 1000- and 100-fold selectivity relative to the hH(1)R and hH(2)R, respectively, and possessing only low intrinsic activity (alpha = 0.27) at the hH(3)R.

Published

2009

17. Potent and selective inhibitors of breast cancer resistance protein (ABCG2) derived from the p-glycoprotein (ABCB1) modulator tariquidar

Author

Burkhard König, Christine Müller, Matthias Kühnle, Gert Fricker, Michael Egger, Günther Bernhardt, Anne Mahringer, and Armin Buschauer

Subjects

ATP Binding Cassette Transporter, Subfamily B, Abcg2, Tariquidar, Antineoplastic Agents, Breast Neoplasms, Pharmacology, Inhibitory Concentration 50, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Chemosensitizing agent, ATP Binding Cassette Transporter, Subfamily G, Member 2, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Cytotoxicity, P-glycoprotein, biology, Chemistry, Multidrug resistance-associated protein 2, Drug Resistance, Multiple, Multidrug Resistance-Associated Protein 2, Neoplasm Proteins, Biochemistry, Enzyme inhibitor, biology.protein, Quinolines, Molecular Medicine, ATP-Binding Cassette Transporters, Female, Efflux, medicine.drug

Abstract

The efflux pumps ABCB1 (p-gp, MDR1) and ABCG2 (BCRP) are expressed to a high extent by endothelial cells at the blood-brain barrier (BBB) and other barrier tissues and are involved in drug resistance of tumor (stem) cells. Whereas numerous ABCB1 inhibitors are known, only a few ABCG2 modulators with submicromolar activity have been published. Starting from tariquidar (4) analogues as ABCB1 modulators, minimal structural modifications resulted in a drastic shift in favor of ABCG2 inhibition. Highest potency was found when the 3,4-dimethoxy-2-(quinoline-3-carbonylamino)benzoyl moiety in 4 was replaced with a 4-methoxycarbonylbenzoyl moiety bearing a hetarylcarboxamido group in 3-position, e.g., quinoline-3-carboxamido (5, IC(50): 119 nM) or quinoline-2-carboxamido (6, IC(50): 60 nM, flow cytometric mitoxantrone efflux assay, topotecan-resistant MCF-7 breast cancer cells); the selectivity for ABCG2 over ABCB1 was about 100-500 fold and the compounds were inactive at ABCC2 (MRP2). Chemosensitivity assays against MCF-7/Topo cells revealed that the nontoxic inhibitor 6 completely reverted ABCG2-mediated topotecan resistance at concentrations >100 nM, whereas 5 showed ABCG2 independent cytotoxicity. ABCG2 inhibitors might be useful for cancer treatment with respect to reversal of multidrug resistance, overcoming the BBB and targeting of tumor stem cells.

Published

2009

18. Guanidine-acylguanidine bioisosteric approach in the design of radioligands: synthesis of a tritium-labeled N(G)-propionylargininamide ([3H]-UR-MK114) as a highly potent and selective neuropeptide Y Y1 receptor antagonist

Author

Max Keller, Günther Bernhardt, Christoph Hutzler, Armin Buschauer, Nathalie Pop, and Annette G. Beck-Sickinger

Subjects

Stereochemistry, Chemistry, Pharmaceutical, CHO Cells, Arginine, Tritium, Chemical synthesis, chemistry.chemical_compound, Cricetulus, Cell Line, Tumor, Cricetinae, Drug Discovery, Radioligand, Animals, Humans, Guanidine, Chromatography, High Pressure Liquid, BIBP-3226, Binding Sites, Chemistry, Antagonist, Ligand (biochemistry), Neuropeptide Y receptor, Receptors, Neuropeptide Y, Kinetics, Drug Design, Molecular Medicine, Bioisostere

Abstract

Synthesis and characterization of (R)-N(alpha)-(2,2-diphenylacetyl)-N-(4-hydroxybenzyl)-N(omega)-([2,3-(3)H]-propanoyl)argininamide ([(3)H]-UR-MK114), an easily accessible tritium-labeled NPY Y(1) receptor (Y(1)R) antagonist (K(B): 0.8 nM, calcium assay, HEL cells) derived from the (R)-argininamide BIBP 3226, is reported. The radioligand binds with high affinity (K(D), saturation: 1.2 nM, kinetic experiments: 1.1 nM, SK-N-MC cells) and selectivity for Y(1)R over Y(2), Y(4), and Y(5) receptors. The title compound is a useful pharmacological tool for the determination of Y(1)R ligand affinities, quantification of Y(1)R binding sites, and autoradiography.

Published

2008

19. Iodoaminopotentidine and related compounds: a new class of ligands with high affinity and selectivity for the histamine H2 receptor

Author

Martial Ruat, Walter Schunack, Juergen Hirschfeld, Armin Buschauer, Sigurd Elz, Elisabeth Traiffort, Jean Schwartz, Freie Universität Berlin, Unité de Neurobiologie et Pharmacologie Moléculaire [Centre Paul Broca] (U109 INSERM ), Groupe hospitalier Broca-Institut National de la Santé et de la Recherche Médicale (INSERM), and PERIGNON, Alain

Subjects

Male, MESH: Muscle Contraction, [SDV.NEU.NB]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, MESH: Sulfonamides, [SDV.NEU.PC] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Psychology and behavior, Carboxamide, Guanidines, Iodine Radioisotopes, chemistry.chemical_compound, MESH: Structure-Activity Relationship, Histamine H2 receptor, Heart Rate, Drug Discovery, MESH: Animals, MESH: Heart Rate, Guanidine, Receptor, chemistry.chemical_classification, Sulfonamides, Aniline Compounds, [SDV.NEU.PC]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Psychology and behavior, [SDV.NEU.SC]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Cognitive Sciences, MESH: Iodine Radioisotopes, Atrial Function, MESH: Atrial Function, MESH: Guanidines, Molecular Medicine, MESH: Vasoconstriction, Aliphatic compound, Histamine, Muscle Contraction, Azides, Stereochemistry, medicine.drug_class, Guinea Pigs, MESH: Receptors, Histamine H2, MESH: Guinea Pigs, MESH: Aniline Compounds, Structure-Activity Relationship, medicine, Structure–activity relationship, Animals, Receptors, Histamine H2, Heart Atria, [SDV.NEU.NB] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Neurobiology, MESH: Azides, MESH: Male, Sulfonamide, chemistry, Vasoconstriction, MESH: Heart Atria, [SDV.NEU.SC] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC]/Cognitive Sciences

Abstract

International audience; The synthesis and biological evaluation of a new class of histamine H2 antagonists with N-cyano-N'-[omega-[3-(1-piperidinylmethyl)phenoxy] alkyl]guanidine partial structure are described as part of an extensive research program to find model compounds for the development of new radioligands with high H2 affinity and specific activity. High receptor affinity is achieved by an additional (substituted) aromatic ring, which is connected with the third guanidine N by a carbon chain spacer and an amine, carboxamide, ester, or sulfonamide link ("polar group"). In functional studies for H2 antagonistic activity and other pharmacological actions [e.g. H1 antihistaminic, antimuscarinic, antiadrenergic (alpha 1, beta 1), 5-HT2 blocking activity] in the isolated guinea pig atrium and ileum and rat aorta and tail artery, the compounds proved to be highly potent and selective histamine H2 receptor antagonists. The H2 antagonistic activity is mainly depending on the length of both the N'-alkyl chain (chain A) and the N"-spacer (chain B). Compounds with a C3 chain A and a C2 chain B are most potent in the preferred group of substances, i.e., the carboxamide series. A wide variety of substituents at the aromatic ring is tolerated, among them iodine, amino, and azido groups. These compounds are up to 32 times more potent than cimetidine in the isolated guinea pig right atrium. The replacement of the carboxamide by an ester group (44c) is well tolerated, while replacement of the cyanoguanidine by an urea group results in nearly 100-fold decrease in activity (46c,e). The iodinated benzamides are among the most potent H2 antagonists known so far. The [125I]-labeled form of 31f ([125I]iodoaminopotentidine, [125I]-N-[2-(4-amino-3-iodobenzamido) ethyl]-N'-cyano-N"-[3-[3-(1-piperidinylmethyl) phenoxy]propyl]guanidine) and its photolabile analogue 31h ([125I]iodoazidopotentidine, [125I]-N-[2-(4-azido-3- iodobenzamido)ethyl]-N'-cyano-N"-[3-[3-(1-piperidinyl-methyl)pheno xy] propyl]guanidine) proved to be useful probes for reversible and irreversible labeling of the histamine H2 receptor. Radioligand binding studies in guinea pig cerebral membranes revealed considerably higher H2 receptor affinity for 31f (pKi = 9.15), 31h (pKi = 8.58), and some analogues than functional experiments (guinea pig atrium), presumably reflecting an easier access to the H2 receptors in membranes.

Published

1992

20. Synthesis and Structure−Activity Relationships of Cyanoguanidine-Type and Structurally Related Histamine H4Receptor Agonists§.

Author

Patrick Igel, Roland Geyer, Andrea Strasser, Stefan Dove, Roland Seifert, and Armin Buschauer

Published

2009

21. Potent and Selective Inhibitors of Breast Cancer Resistance Protein (ABCG2) Derived from the p-Glycoprotein (ABCB1) Modulator Tariquidar.

Author

Matthias Kühnle, Michael Egger, Christine Müller, Anne Mahringer, Günther Bernhardt, Gert Fricker, Burkhard König, and Armin Buschauer

Published

2009

22. Guanidine−Acylguanidine Bioisosteric Approach in the Design of Radioligands: Synthesis of a Tritium-Labeled NG-Propionylargininamide ([3H]-UR-MK114) as a Highly Potent and Selective Neuropeptide Y Y1Receptor Antagonist.

Author

Max Keller, Nathalie Pop, Christoph Hutzler, Annette G. Beck-Sickinger, Günther Bernhardt, and Armin Buschauer

Published

2008

23. Acylguanidines as Bioisosteres of Guanidines: NG-Acylated Imidazolylpropylguanidines, a New Class of Histamine H2Receptor Agonists.

Author

Prasanta Ghorai, Anja Kraus, Max Keller, Carsten Götte, Patrick Igel, Erich Schneider, David Schnell, Günther Bernhardt, Stefan Dove, Manfred Zabel, Sigurd Elz, Roland Seifert, and Armin Buschauer

Published

2008

24. Synthesis and in vitro pharmacology of arpromidine and related phenyl(pyridylalkyl)guanidines, a potential new class of positive inotropic drugs

Author

Armin Buschauer

Subjects

Cardiotonic Agents, Chemical Phenomena, Stereochemistry, Guinea Pigs, Substituent, Thio, In Vitro Techniques, Guanidines, Structure-Activity Relationship, chemistry.chemical_compound, Impromidine, Histamine H2 receptor, Drug Discovery, medicine, Animals, Moiety, Potency, Receptors, Histamine H2, Guanidine, Chemistry, Imidazoles, Heart, Histamine H1 Antagonists, Molecular Medicine, Pheniramine, medicine.drug

Abstract

Replacement of the cimetidine moiety in impromidine (1,N1-[3-(1H-imidazol-4-yl)propyl]-N2-[2-[[(5-methyl-1H-imidazol-4- yl)methyl]thio]ethyl]guanidine) by more lipophilic H2-nonspecific pheniramine-like structures resulted in potent H2 agonists with up to 160 times the activity of histamine in the isolated, spontaneously beating guinea pig right atrium. Additionally, the compounds proved to be moderate H1 antagonists. Highest H2-agonistic potency was found in compounds characterized by a three-membered carbon chain connecting the aromatic rings and the guanidine group. The activity in the atrium was increased 2-4-fold by halogen substituents in the meta or para position of the phenyl ring. Highest H1-antagonistic potency resides in the group of para-halogenated compounds, p-F representing the optimal substituent in both receptor models. The corresponding guanidine 52 (arpromidine, N1-[3-(4-fluorophenyl)-3-pyridin-2-ylpropyl]-N2-[3-(1H-imidazol-4- yl)propyl]guanidine) combines about 100 times the activity of histamine at the H2 receptor with H1-antagonistic potency in the range of pheniramine. Further increase in the activity on the atrium was achieved by disubstitution with halogen on the phenyl ring, such as 3,4-F2, 3,5-F2, and 3,4-Cl2 (63-65). The 2-pyridyl group in arpromidine was replaced by 3-pyridyl without significant change in H2 agonistic activity, whereas the 4-pyridyl and phenyl analogues were less active. The rank order of potency in the atrium was in good agreement with the positive inotropic effects found in isolated, perfused guinea pig hearts, where 63-65 were the most potent compounds as well.

Published

1989