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13. Imide and lactam derivatives of N-benzylpyroglutamyl-L-phenylalanine as VCAM/VLA-4 antagonists.

Author

Tilley JW, Kaplan G, Rowan K, Schwinge V, and Wolitzky B

Subjects
Cell Adhesion drug effects, Enzyme-Linked Immunosorbent Assay, Humans, Imides chemistry, Inhibitory Concentration 50, Integrin alpha4beta1, Lactams chemistry, Molecular Structure, Tumor Cells, Cultured, Dipeptides chemistry, Dipeptides pharmacology, Imides pharmacology, Integrins antagonists & inhibitors, Lactams pharmacology, Phenylalanine analogs & derivatives, Pyrrolidonecarboxylic Acid analogs & derivatives, Receptors, Lymphocyte Homing antagonists & inhibitors
Abstract

A series of imides and lactams derived from 4-amino-N-benzylpyroglutamyl-L-phenylalanine was prepared and evaluated for activity as VCAM/VLA-4 antagonists. Imides were more potent than the corresponding lactams; several had subnanomolar IC50s in an ELISA based assay and were also highly effective at blocking VLA-4 expressing Ramos cell binding to VCAM coated plates.

Published
2001
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14. Cyclic thioether peptide mimetics as VCAM-VLA-4 antagonists.

Author

Fotouhi N, Joshi P, Tilley JW, Rowan K, Schwinge V, and Wolitzky B

Subjects
Integrin alpha4beta1, Molecular Mimicry, Integrins antagonists & inhibitors, Peptides, Cyclic chemistry, Peptides, Cyclic pharmacology, Receptors, Lymphocyte Homing antagonists & inhibitors, Sulfides chemistry, Vascular Cell Adhesion Molecule-1 drug effects
Abstract

Selective substitution of a sulfur atom by carbon in a highly potent 13-membered cyclic disulfide was accomplished by intramolecular displacement of a bromide. The potency of the resulting thioethers in the VCAM/VLA-4 assay was dependent on ring size and the position of the sulfur atom.

Published
2000
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15. The design and synthesis of potent cyclic peptide VCAM-VLA-4 antagonists incorporating an achiral Asp-Pro mimetic.

Author

Fotouhi N, Joshi P, Fry D, Cook C, Tilley JW, Kaplan G, Hanglow A, Rowan K, Schwinge V, and Wolitzky B

Subjects
Drug Design, Integrin alpha4beta1, Molecular Mimicry, Peptides, Cyclic chemistry, Aspartic Acid chemistry, Integrins antagonists & inhibitors, Peptides, Cyclic chemical synthesis, Peptides, Cyclic pharmacology, Proline chemistry, Receptors, Lymphocyte Homing antagonists & inhibitors, Vascular Cell Adhesion Molecule-1 drug effects
Abstract

The Asp-Pro sequence of the cyclic peptide Ac-HN-Tyr-Cys*-Asp-Pro-Cys*-OH (1) could be replaced with the achiral dipeptide mimetic 1-(2-aminoethyl)cyclpentylcarboxylic acid with retention of potent inhibition of the VCAM-VLA-4 interaction.

Published
2000
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16. N-benzylpyroglutamyl-L-phenylalanine derivatives as VCAM/VLA-4 antagonists.

Author

Chen L, Tilley JW, Guthrie RW, Mennona F, Huang TN, Kaplan G, Trilles R, Miklowski D, Huby N, Schwinge V, Wolitzky B, and Rowan K

Subjects
Cell Line, Enzyme-Linked Immunosorbent Assay, Humans, Integrin alpha4beta1, Phenylalanine chemistry, Phenylalanine pharmacology, Recombinant Proteins antagonists & inhibitors, Structure-Activity Relationship, Integrins antagonists & inhibitors, Phenylalanine analogs & derivatives, Receptors, Lymphocyte Homing antagonists & inhibitors, Vascular Cell Adhesion Molecule-1 drug effects
Abstract

A series of N-(N-benzylpyroglutamyl)-4-substituted-L-phenylalanine derivatives was prepared as VLA-4/VCAM antagonists. Analogues substituted by electron deficient benzoylamino groups bearing bulky ortho substituents had low-nM potency in an ELISA assay and low-microM activity in a cell based assay.

Published
2000
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17. N-acyl phenylalanine analogues as potent small molecule VLA-4 antagonists.

Author

Chen L, Tilley JW, Huang TN, Miklowski D, Trilles R, Guthrie RW, Luk K, Hanglow A, Rowan K, Schwinge V, and Wolitzky B

Subjects
Acylation, Integrin alpha4beta1, Structure-Activity Relationship, Integrins antagonists & inhibitors, Phenylalanine analogs & derivatives, Phenylalanine pharmacology, Receptors, Lymphocyte Homing antagonists & inhibitors
Abstract

We have identified a series of low molecular weight (Mr < 500) N-acylphenylalanines that are effective inhibitors of the VCAM-VLA-4 interaction. Investigation of the SAR of the N-acyl moiety led to the identification of N-benzylpyroglutamyl derivatives as being particularly potent.

Published
2000
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18. The effect of aspartate hydroxylation on calcium binding to epidermal growth factor-like modules in coagulation factors IX and X.

Author

Sunnerhagen MS, Persson E, Dahlqvist I, Drakenberg T, Stenflo J, Mayhew M, Robin M, Handford P, Tilley JW, and Campbell ID

Subjects
Amino Acid Sequence, Aspartic Acid chemistry, Epidermal Growth Factor chemistry, Humans, Hydroxylation, In Vitro Techniques, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Protein Structure, Tertiary, Structure-Activity Relationship, Tyrosine chemistry, Calcium metabolism, Calcium-Binding Proteins chemistry, Factor IX metabolism, Factor X metabolism
Abstract

Hydroxylation of aspartic acid to erythro-beta-aspartic acid (Hya) occurs in epidermal growth factor (EGF)-like modules in numerous extracellular proteins with diverse functions. Several EGF-like modules with the consensus sequence for hydroxylation bind Ca2+, and it has therefore been suggested that the hydroxyl group is essential for Ca2+ binding. To determine directly the influence of beta-hydroxylation on calcium binding in the EGF-like modules from coagulation factors IX and X, we have now measured calcium binding to both the fully beta-hydroxylated and the non-beta-hydroxylated modules of the two proteins. At low ionic strength, the Hya-containing module of factor X has a slightly higher Ca2+ affinity, but at physiological salt concentrations this difference is no longer significant for either factor IX or X. Analysis of the 1H NMR chemical shift differences between the hydroxylated and nonhydroxylated factor X modules show that hydroxylation has no effect on the domain fold. Furthermore, measurements on factor IX show that hydroxylation has no effect on the Ca2+/Mg2+ specificity of the ion binding site. We conclude that the hydroxyl group is not a direct ligand for the calcium ion in these EGF-like modules, nor is it essential for high-affinity Ca2+ binding.

Published
1993

19. CCK satiety is differentially mediated by high- and low-affinity CCK receptors in mice and rats.

Author

Weatherford SC, Laughton WB, Salabarria J, Danho W, Tilley JW, Netterville LA, Schwartz GJ, and Moran TH

Subjects
Animals, Benzodiazepinones pharmacology, Cholecystokinin antagonists & inhibitors, Devazepide, Dose-Response Relationship, Drug, Eating drug effects, Glucose, Male, Mice, Mice, Inbred ICR, Rats, Rats, Sprague-Dawley, Sincalide analogs & derivatives, Sucrose, Receptors, Cholecystokinin physiology, Satiety Response, Sincalide pharmacology
Abstract

Cholecystokinin-JMV-180 (JMV-180) is an analogue of cholecystokinin C-terminal octapeptide (CCK-8), which has been shown to be an agonist at the proposed CCK pancreatic high-affinity site and a functional antagonist at the pancreatic low-affinity site in rats and to have agonist activity at both high- and low-affinity sites in the mouse. In this study we used JMV-180 to evaluate the potential participation of these two CCK-A sites in the satiety effect of CCK-8 in rats and mice. When tested at doses that ranged from 0.01 to 9.2 mumol/kg, JMV-180 did not reliably affect food intake of solid or liquid test diets in rats. When combined with CCK-8 (3.2 or 8.5 nmol/kg) JMV-180 dose dependently reversed the satiety effect of CCK-8. In contrast to these results in the rat, both JMV-180 (3.7-14.8 mumol/kg) and CCK-8 (1.7-6.8 nmol/kg) dose dependently reduced the intake of 20% sucrose in mice. Both CCK-8- and JMV-180-induced suppression of food intake were attenuated by the CCK-A antagonist MK-329 (24.8 nmol/kg). The results of these studies suggest that agonist activity at sites pharmacologically similar to the CCK pancreatic high-affinity site is not sufficient for expression of CCK satiety, whereas agonist activity at low-affinity-like sites is necessary to reduce food intake. Thus the anorexic activity of CCK appears to be mediated through an interaction with a receptor site pharmacologically similar to the pancreatic low-affinity CCK receptor site.

Published
1993
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20. Analogs of CCK incorporating conformationally constrained replacements for Asp32.

Author

Tilley JW, Danho W, Madison V, Fry D, Swistok J, Makofske R, Michalewsky J, Schwartz A, Weatherford S, and Triscari J

Subjects
Amino Acid Sequence, Animals, Appetite Depressants pharmacology, Aspartic Acid, Cattle, Cholecystokinin chemical synthesis, Cholecystokinin pharmacology, In Vitro Techniques, Male, Models, Molecular, Molecular Sequence Data, Protein Conformation, Rats, Rats, Sprague-Dawley, Receptors, Cholecystokinin metabolism, Structure-Activity Relationship, Appetite Depressants chemical synthesis, Cholecystokinin analogs & derivatives
Published
1992
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21. Analogs of Ac-CCK-7 incorporating dipeptide mimics in place of Met28-Gly29.

Author

Tilley JW, Danho W, Shiuey SJ, Kulesha I, Swistok J, Makofske R, Michalewsky J, Triscari J, Nelson D, and Weatherford S

Subjects
Amino Acid Sequence, Animals, Cattle, Cholecystokinin pharmacology, Corpus Striatum drug effects, Corpus Striatum metabolism, Dipeptides chemistry, Feeding Behavior drug effects, Glycine chemistry, In Vitro Techniques, Magnetic Resonance Spectroscopy, Male, Methionine chemistry, Molecular Sequence Data, Pancreas drug effects, Pancreas metabolism, Protein Conformation, Rats, Rats, Sprague-Dawley, Receptors, Cholecystokinin drug effects, Receptors, Cholecystokinin metabolism, Cholecystokinin analogs & derivatives
Abstract

A series of analogs of Ac-CCK-7 [Ac-Tyr(SO3H)-Met28-Gly29-Trp-Met-Asp- Phe-NH2, (1)] were prepared in which the Met28-Gly29 dipeptide was replaced by omega-aminoalkanoic acids. Compounds were assessed in binding assays using homogenated rat pancreatic membranes and bovine striatum as the source of CCK-A and CCK-B receptors, respectively, and for anorectic activity after intraperitoneal administration to rats. The analog incorporating 4-aminobutanoic acid (5) was only 8 times less potent than 1 in the pancreatic binding assay, was more potent in the striatal binding assay, and was more potent than 1 in reducing food intake in rats. Using a bioactive cyclic analog of Ac-CCK-7 as a template, several rigid spacers were designed and tested as substitutes for the Met28-Gly29 dipeptide. The analogs incorporating 3-aminobenzoic acid (20) and (1S)-trans-2-aminocyclopentanecarboxylic acid (26) proved highly effective in the binding assays and as anorectic agents. We hypothesize that for stimulation of CCK-A receptors, the main function of the N-terminal tripeptide of Ac-CCK-7 is to orient the tyrosine sulfate with respect to Trp30 and that the bioactive arrangement of these elements lies among those which are readily available to both 20 and 26. NOESY and distance-constrained molecular dynamics experiments carried out on 20 and 26 identified conformations in which the relative orientation of the tyrosine hydroxide and the alpha-carbon atom of tryptophan were similar, providing the basis for further drug design efforts.

Published
1992
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22. Structure activity studies of tryptophan30 modified analogs of Ac-CCK-7.

Author

Danho W, Tilley JW, Shiuey SJ, Kulesha I, Swistok J, Makofske R, Michalewsky J, Wagner R, Triscari J, and Nelson D

Subjects
Amino Acid Sequence, Animals, Appetite Depressants chemistry, Blood Proteins chemistry, Cattle, Corpus Striatum chemistry, Molecular Sequence Data, Pancreas chemistry, Peptide Fragments analysis, Rats, Sincalide analysis, Structure-Activity Relationship, Peptide Fragments chemistry, Sincalide chemistry, Tryptophan chemistry
Abstract

Cholecystokinin represents a family of gut hormones which among other activities, have been proposed to participate in satiety signaling. Ac-CCK-7[Ac-Tyr(SO3H)-Met-Gly-Trp30-Met-Asp-Phe-NH2 (2)] possesses the full spectrum of activity and potency of the intact hormone; thus analogs of 2 may be useful as anorectic agents. A series of derivatives has been prepared in which the tryptophan indole moiety of 2 has been modified. The new compounds were assayed in CCK binding assays using homogenated rat pancreatic membranes and bovine striatum as a source of CCK-A and CCK-B receptors respectively and in vivo in rats for anorectic activity. Although previous studies have concluded that the indole ring of Trp30 is a critical pharmacophore for the interaction of CCK with both its A and B type receptors, we find 2-Nal30-Ac-CCK-7 (20) to be nearly equipotent to 2 in both CCK binding and as an anorectic agent sensitive to blockade by the Merck CCK-A receptor antagonist MK-329. The extreme structural sensitivity of this anorectic activity is illustrated by the 1-naphthylalanine30 (19) and (benzo[b]thien-2-yl)alanine30 (21) analogs which are 30 and 100 times less potent than 2 respectively. Other mono- and bicyclic Trp30 replacements, including substituted phenylalanines, 3-quinolinylalanine, and 2-(5,6,7,8-tetrahydro)naphthylalanine, gave inactive compounds.

Published
1992
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23. Structure activity of C-terminal modified analogs of Ac-CCK-7.

Author

Tilley JW, Danho W, Shiuey SJ, Kulesha I, Sarabu R, Swistok J, Makofske R, Olson GL, Chiang E, and Rusiecki VK

Subjects
Amino Acid Sequence, Animals, Cattle, Molecular Sequence Data, Pancreas metabolism, Peptide Fragments metabolism, Phenylalanine chemistry, Rats, Sincalide metabolism, Structure-Activity Relationship, Amylases metabolism, Peptide Fragments chemistry, Receptors, Cholecystokinin chemistry, Sincalide chemistry
Abstract

Previous work indicates that both the C-terminal phenylalanine amide and the tryptophan moieties of cholecystokinin (CCK) are critical pharmacophores for interaction with either the A or B receptor subtypes. We have examined a series of analogs of Ac-CCK-7 [Ac-Tyr(SO3H)-Met-Gly-Trp-Met-Asp-Phe33-NH2] (2) in which the phenyl ring of the C-terminal Phe-NH2 has been modified. Compounds were assessed in binding assays using homogenated rat pancreatic membranes and bovine striatum as the source of CCK-A and CCK-B receptors respectively and for anorectic activity after intraperitoneal administration to rats. Substitution of a number of cycloalkyl or bicyclic aryl moieties for the phenyl ring of phenylalanine33 including cyclopentyl (20), cyclohexyl (21), cyclooctyl (23), 2-(5,6,7,8-tetrahydro)naphthyl (26), 2-naphthyl (27), and 1-naphthyl (29) led to analogs with 10-70 times the anorectic potency of 2. The anorectic activity of 21 was blocked by the specific CCK-A receptor antagonist MK-329. Other bulky aliphatic groups in place of the phenylalanine33 aromatic ring such as isopropyl, 2-adamantyl and cyclohexylmethyl gave derivatives similar to 2 in potency. While most of the new compounds were comparable to CCK in binding assays, 23, 26, 27 and 29 were exceptionally potent with IC50s 10(-11)-10(-14) M in the pancreas. Compounds 23 and 29 were further evaluated for their ability to stimulate amylase secretion and found to have potencies similar to that of CCK. The dissociation between potency in the binding and amylase secretion assays suggests that they may interact with a high affinity binding site which is not coupled to amylase secretion. We conclude that CCK receptors possess a generous hydrophobic pocket capable of accommodating large alkyl groups in place of the side chain of phenylalanine33 and that the pharmacological profile of CCK analogs can be tailored by appropriate exploitation of this finding.

Published
1992
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24. Carboxylic acids and tetrazoles as isosteric replacements for sulfate in cholecystokinin analogues.

Author

Tilley JW, Danho W, Lovey K, Wagner R, Swistok J, Makofske R, Michalewsky J, Triscari J, Nelson D, and Weatherford S

Subjects
Animals, Cattle, Cell Membrane metabolism, Chemical Phenomena, Chemistry, Corpus Striatum metabolism, Eating drug effects, Food Deprivation, Male, Molecular Structure, Pancreas metabolism, Rats, Rats, Inbred Strains, Receptors, Cholecystokinin metabolism, Sincalide chemistry, Sincalide metabolism, Sincalide pharmacology, Structure-Activity Relationship, Carboxylic Acids chemistry, Sincalide analogs & derivatives, Sulfates chemistry, Tetrazoles chemistry
Abstract

A series of analogues of the satiety-inducing peptide cholecystokinin (CCK-8) was prepared in which the sulfated tyrosine required for activation of peripheral receptors was replaced with a carboxy(alkyl)- or tetrazolyl(alkyl)-phenylalanine to investigate whether an organic acid could serve the role of the sulfate group at the receptor. The necessary intermediates were prepared by previously reported procedures or by alkylation of carboxy(alkyl)- or tetrazolyl(alkyl)phenylmethyl bromides with a glycine-derived anion followed by protecting-group manipulations, and these were incorporated into derivatives of acetyl-CCK-7 using solid-phase synthesis. Peptide analogues were evaluated in a CCK-binding assay for affinity for either peripheral (CCK-A) receptors using homogenated rat pancreatic membranes as the receptor source or for central (CCK-B) receptors using bovine striatum as the receptor source. They were further evaluated for effects on food intake in rats after intraperitoneal (ip) injection. A number of the compounds reported are active in the CCK-A receptor binding assay although less potent than acetyl-CCK-7 and decrease food intake with comparable potency to acetyl-CCK-7. In a meal feeding model designed to assess appetite suppressant activity, acetyl-CCK-7 has an ED50 of 7 nmol/kg ip, while the ED50s of Ac-Phe(4-CH2CO2H)-Met-Gly-Trp-Met-Asp-Phe-NH2 (28) and Ac-Phe[4-(tetrazol-5-yl)]-Met-Gly-Trp-Met-Asp-Phe-NH2 (34) were 9 and 11 nmol/kg ip, respectively. An analogue of 28 lacking the N-terminal acetamido group, 3-[4-(carboxymethyl)-phenyl]propanoyl-Met-Gly-Trp-Met-Asp-Phe-NH2 (50), was also active in the meal feeding assay with an ED50 of 3 nmol/kg ip. Its anorexic effect was blocked by simultaneous administration of the CCK-A receptor antagonist MK 329, indicating that the observed anorexic activity is mediated by CCK-A receptors. We conclude from this work that the requirement for a negative charge at the CCK-A receptor provided in the natural substrate by a sulfate group can be satisfied by organic acids.

Published
1991
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25. Propenyl carboxamide derivatives as antagonists of platelet activating factor.

Author

Guthrie RW, Kaplan GL, Mennona FA, Tilley JW, Kierstead RW, O'Donnell M, Crowley H, Yaremko B, and Welton AF

Subjects
Administration, Oral, Animals, Binding, Competitive, Blood Platelets metabolism, Bridged Bicyclo Compounds chemistry, Bridged Bicyclo Compounds metabolism, Bronchoconstrictor Agents antagonists & inhibitors, Chemical Phenomena, Chemistry, Physical, Dogs, Guinea Pigs, In Vitro Techniques, Platelet Activating Factor metabolism, Pyridines chemistry, Pyridines metabolism, Receptors, Cell Surface drug effects, Structure-Activity Relationship, Bridged Bicyclo Compounds chemical synthesis, Platelet Activating Factor antagonists & inhibitors, Platelet Membrane Glycoproteins, Pyridines chemical synthesis, Receptors, Cell Surface metabolism, Receptors, G-Protein-Coupled
Abstract

A series of N-[4-(3-pyridinyl)butyl] 3-substituted propenyl carboxamide derivatives bearing an unsaturated bicyclic moiety in the 3-position was prepared and evaluated for PAF (platelet activating factor) antagonist activity. These compounds represent conformationally constrained direct analogues of the corresponding potent 5-aryl-pentadienecarboxamides (5). Most of the new compounds were active in a PAF-binding assay employing whole, washed dog platelets as the receptor source and inhibited PAF-induced bronchoconstriction in guinea pigs after intravenous administration. However, oral activity in the PAF-induced bronchoconstriction model was highly sensitive to the nature and substitution of the bicyclic ring system. The most interesting compounds included [R-(E)]-(1-butyl-6-methoxy-2-naphthyl)-N-[1-methyl-4-(3- pyridinyl)butyl]-2-propenamide (4b), [R-(E)]-(3-butyl-6-methoxy-2- benzo[b]thiophene-yl)-N-[1-methyl-4-(3-pyridinyl)butyl]-2-propenamide (4k), and [R-(E)]-(3-butyl-6-methoxy-1-methyl-2-indoly)-N-[1-ethyl-4- (3-pyridinyl)butyl]-2-propenamide (4l) which inhibited PAF-induced broncho-constriction in guinea pigs with IC50s of 3.0-5.4 mg/kg, when the animals were challenged 2 h after drug treatment. They were also highly effective 6 h after a 50 mg/kg oral dose. This study supports the notion that the key remote aromatic ring present in the 5-arylpentadienecarboxamides (5) is preferentially coplanar with the diene system for good PAF antagonist activity.

Published
1990
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26. The metabolism of 14C-cibenzoline in dogs and rats.

Author

Loh AC, Williams TH, Tilley JW, Sasso GJ, Szuna AJ, Carbone JJ, Toome V, and Leinweber FJ

Subjects
Administration, Oral, Animals, Anti-Arrhythmia Agents metabolism, Bile analysis, Biotransformation, Carbon Radioisotopes, Chromatography, High Pressure Liquid, Dogs, Feces analysis, Imidazoles administration & dosage, Imidazoles analysis, Imidazoles urine, Male, Mass Spectrometry methods, Rats, Rats, Inbred Strains, Imidazoles metabolism
Abstract

The disposition of the new antiarrhythmic agent cibenzoline (CBZ) (racemic 4,5-dihydro-2-(2,2-diphenylcyclopropyl)-1H-imidazole) in three male dogs was investigated after oral administration of 13.8 mg/kg of 14C-CBZ base. Within 6 days, 60.5 +/- 6.0% of the dose was excreted in urine and 19.2 +/- 4.6% in feces. In 0-24-hr urine, unchanged drug was excreted (41.6% of the dose) as well as the unconjugated 4,5-dehydro metabolite (DHCBZ, 3.7%), conjugated p-hydroxybenzophenone (0.8%, only in one dog), and a phenolic metabolite, p-hydroxycibenzoline (HCBZ) in a rearranged form (RHCBZ) at 5.2% of the dose (free plus conjugated). Studies with synthetic HCBZ indicated that unrearranged HCBZ was excreted and that rearrangement occurred during purification. CBZ from dog urine displayed slight optical activity, based on ORD/CD data, corresponding to an optical purity of 15% of the S-(-)-CBZ, indicating a limited extent of stereoselective metabolism of CBZ in dogs. After an oral 50-mg/kg dose of 14C-CBZ succinate, male rats excreted in 3 days 27.0 +/- 2.8% in urine and 41.5 +/- 2.6% of the dose in feces, and in a repeated experiment 32.1 +/- 1.9% in urine and 54.5 +/- 0.7% in feces. CBZ (7.6%) and DHCBZ (0.2%) were determined in 0-24-hr urine, and CBZ (4.2%) and RHCBZ (4.2% of the dose) were determined in 0-24-hr feces. RHCBZ (3.1%), m-methoxy p-hydroxycibenzoline (8.3%), and p-hydroxybenzophenone (5.3% of the dose) were identified as glucuronide/sulfate conjugates in bile from rats. Evidence that p-hydroxybenzophenone arose from an unstable unidentified metabolite is discussed.

Published
1986

27. Biphenylcarboxamide derivatives as antagonists of platelet-activating factor.

Author

Tilley JW, Clader JW, Zawoiski S, Wirkus M, LeMahieu RA, O'Donnell M, Crowley H, and Welton AF

Subjects
Animals, Biphenyl Compounds pharmacology, Biphenyl Compounds therapeutic use, Bronchial Spasm drug therapy, Carboxylic Acids pharmacology, Carboxylic Acids therapeutic use, Chemical Phenomena, Chemistry, Dogs, Guinea Pigs, Male, Structure-Activity Relationship, Biphenyl Compounds chemical synthesis, Carboxylic Acids chemical synthesis, Platelet Activating Factor antagonists & inhibitors
Abstract

A series of N-[4-(3-pyridinyl)butyl]-1,1'-biphenyl-4-carboxamides was prepared, and the compounds were evaluated for platelet-activating factor (PAF) antagonist activity in a binding assay employing washed, whole dog platelets and in vivo for their ability to inhibit PAF-induced bronchoconstriction in the guinea pig. The inclusion of a methyl group in the R configuration on the side-chain carbon adjacent to the carboxamide nitrogen atom of these derivatives resulted in a marked enhancement of potency in the binding assay for compounds unsubstituted in the biphenyl 2-position and, more importantly, in improved oral bioavailability. Previous work with related pyrido[2,1-b]-quinazoline-8-carboxamides suggests that the presence of such an alkyl group improves bioavailability by rendering the resulting compounds resistant to degradation by liver amidases. The most interesting compounds to emerge from this work are (R)-2-bromo-3',4'-dimethoxy-N-[1-methyl-4-(3-pyridinyl)butyl]-1,1'-bi phe nyl- 4-carboxamide (33) and (R)-2-butyl-3',4'-dimethoxy-N-[1-methyl-4-(3-pyridinyl)butyl]- 1,1'-biphenyl-4-carboxamide (40) each of which inhibits PAF-induced bronchoconstriction in the guinea pig by greater than 55%. 6 h after an oral dose of 50 mg/kg.

Published
1989
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28. Adamantylthiourea derivatives as antiviral agents.

Author

Tilley JW, Levitan P, and Kramer MJ

Subjects
Adamantane chemical synthesis, Adamantane pharmacology, Amantadine therapeutic use, Animals, Antiviral Agents therapeutic use, Lethal Dose 50, Mice, Orthomyxoviridae Infections drug therapy, Thiourea chemical synthesis, Thiourea pharmacology, Adamantane analogs & derivatives, Antiviral Agents chemical synthesis, Thiourea analogs & derivatives
Abstract

A series of nine 3-substituted 1-adamantylthioureas was prepared and tested for antiviral activity against influenza A2/Asian/J305 virus in vivo and in vitro. Protective dose 50 values were calculated for three of the compounds. One of these compounds, 7, has antiviral activity which compares favorably with that of amantadine.

Published
1979
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29. Antagonists of slow-reacting substance of anaphylaxis. 1. Pyrido[2,1-b]quinazolinecarboxylic acid derivatives.

Author

Tilley JW, Levitan P, Welton AF, and Crowley HJ

Subjects
Animals, Biological Assay, Guinea Pigs, Ileum drug effects, Indicators and Reagents, Leukotriene E4, Muscle Contraction drug effects, Quinazolines pharmacology, Rats, SRS-A analogs & derivatives, SRS-A pharmacology, Structure-Activity Relationship, Quinazolines chemical synthesis, SRS-A antagonists & inhibitors
Abstract

Members of a series of basic amide and ester derivatives of 2-substituted pyrido[2,1-b]quinazoline-8-carboxylic acids were prepared and evaluated for their ability to prevent slow-reacting substance of anaphylaxis (SRS-A) induced contractions of guinea pig ilea. The results indicate that the presence of a branched-chain alkyl group in the 2-position and a sterically demanding substituted aminoethyl carboxylate or carboxamide in the 8-position give optimal in vitro activity. The phenylpiperazine 25 was further found to block SRS-A-related symptomatology after intravenous administration in two animal models.

Published
1983
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30. Pyrido[2,1-b]quinazolinecarboxamide derivatives as platelet activating factor antagonists.

Author

Tilley JW, Burghardt B, Burghardt C, Mowles TF, Leinweber FJ, Klevans L, Young R, Hirkaler G, Fahrenholtz K, and Zawoiski S

Subjects
Animals, Blood Pressure drug effects, Dogs, Guinea Pigs, Male, Platelet Aggregation drug effects, Quinazolines chemical synthesis, Quinazolines pharmacology, Rats, Rats, Inbred Strains, Saimiri, Structure-Activity Relationship, Platelet Activating Factor antagonists & inhibitors
Abstract

A series of N-[(heteroaryl)alkyl]pyrido[2,1-b]quinazolines were evaluated for their ability to inhibit the binding of radiolabeled platelet activating factor (PAF) to its receptor on dog platelets. The most potent compounds in this series were found to be pyrido[2,1-b]quinazoline-8-carboxamides possessing a four- or six-carbon chain between the carboxamide nitrogen atom and a 3-pyridinyl or 5-pyrimidinyl moiety. Since earlier metabolism studies with pyridoquinazolinecarboxamides suggest that the carboxamide moiety is labile to hydrolysis in vivo, attempts were made to find isosteric replacements for this group. The substitutions examined led to a loss of activity; however, insertion of a methyl group on the carbon atom alpha to the carboxamide nitrogen led to an enantioselective enhancement of potency. (R)-2-(1-Methylethyl)-N-[1-methyl-4-(3-pyridinyl)butyl]-11-oxo-11H- pyrido[2,1-b]quinazoline-8-carboxamide (34) was more potent than the corresponding S enantiomer in the PAF binding assay and was also shown to be more resistant to degradation by amidases present in whole liver homogenates obtained from guinea pig, dog, and squirrel monkey. The corresponding rac-2-(1-methylethyl)-N-[1-methyl-4-(3-pyridinyl)butyl]-11-oxo-11H- pyrido[2,1-b]quinazoline-8-carboxamide (33) was found to inhibit transient PAF-induced thrombocytopenia and decreases in blood pressure in guinea pigs after intravenous or oral administration and to have a duration of action of greater than 5 h after an oral dose of 200 mg/kg. Compound 33 thus represents the prototype of a new class of orally active PAF antagonists.

Published
1988
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31. Antihypertensive (2-aminoethyl)thiourea derivatives. 1.

Author

Tilley JW, Levitan P, Kierstead RW, and Cohen M

Subjects
Animals, Avoidance Learning drug effects, Blood Pressure drug effects, Chemical Phenomena, Chemistry, Clonidine pharmacology, Dogs, Male, Phenylthiourea chemical synthesis, Phenylthiourea pharmacology, Rats, Saimiri, Species Specificity, Antihypertensive Agents chemical synthesis, Phenylthiourea analogs & derivatives
Abstract

Structure-activity studies were carried out on a series of antihypertensive 1-(2-aminoethyl)-3-(substituted phenyl)thioureas. From this class of compounds, the 2,6-dichlorophenyl analogue 2 was found to have potent oral antihypertensive activity in two hypertensive rat models and the renal hypertensive dog. In addition to its effect on blood pressure, 2 displayed sedative effects which had a marked species specificity.

Published
1980
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32. N-(heterocyclic alkyl)pyrido[2,1-b]quinazoline-8-carboxamides as orally active antiallergy agents.

Author

Tilley JW, Levitan P, Lind J, Welton AF, Crowley HJ, Tobias LD, and O'Donnell M

Subjects
Administration, Oral, Animals, Blood Platelets enzymology, Bronchi drug effects, Guinea Pigs, Humans, In Vitro Techniques, Indicators and Reagents, Leukotriene E4, Magnetic Resonance Spectroscopy, Mass Spectrometry, Pyridines administration & dosage, Pyridines pharmacology, Quinazolines administration & dosage, Quinazolines pharmacology, SRS-A analogs & derivatives, SRS-A pharmacology, Spectrophotometry, Infrared, Structure-Activity Relationship, Thromboxane-A Synthase blood, Bronchi physiology, Histamine H1 Antagonists chemical synthesis, Muscle Contraction drug effects, Pyridines chemical synthesis, Quinazolines chemical synthesis, SRS-A antagonists & inhibitors
Abstract

A series of N-(heterocyclic alkyl)pyrido[2,1-b]quinazoline-8-carboxamides were evaluated for their ability to antagonize slow-reacting substance of anaphylaxis (SRS-A) induced contractions of guinea pig ilea and to inhibit thromboxane synthase in vitro. The results indicated that those pyrido[2,1-b]quinazoline-8-carboxamides bearing a branched-chain alkyl moiety in the 2-position and a four to six atom linear chain between a 3- or 4-substituted pyridine or a 1-substituted imidazole ring and the carboxamide nitrogen atom showed the best combination of potencies in the two assays. Several of these compounds were found to be orally active inhibitors of LTE4-induced bronchoconstriction in the guinea pig and LTE4-induced skin wheal formation in the rat. One of the most potent analogues, 2-(1-methyl-ethyl)-N-(1H-imidazol-1-ylbutyl)-11-oxo-11H-pyrido [2,1-b]quinazoline-8-carboxamide (36), was selected for extensive pharmacological investigation. It was found that this compound was not a specific inhibitor of LTE4-induced symptomatology, but exhibited more general activity by inhibiting bronchospasm in guinea pigs induced by LTC4, LTD4, PAF, and histamine and skin wheal formation in rats and guinea pigs induced by LTC4, LTD4, and PAF. In addition, 36 was orally active in the passive cutaneous anaphylaxis assay, suggesting that it also exhibits mediator release inhibitory activity. On the basis of the overall pharmacological profile of 36 and its closely related analogues, it was concluded that these compounds may be useful for the treatment of asthma.

Published
1987
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33. Pentadienyl carboxamide derivatives as antagonists of platelet-activating factor.

Author

Guthrie RW, Kaplan GL, Mennona FA, Tilley JW, Kierstead RW, Mullin JG, LeMahieu RA, Zawoiski S, O'Donnell M, and Crowley H

Subjects
Amides pharmacology, Animals, Bronchi drug effects, Capillary Permeability drug effects, Chemical Phenomena, Chemistry, Dogs, Guinea Pigs, Male, Pyridines pharmacology, Rats, Rats, Inbred Strains, Amides chemical synthesis, Platelet Activating Factor antagonists & inhibitors, Pyridines chemical synthesis
Abstract

A series of N-[4-(3-pyridinyl)butyl]-5,5-disubstituted-pentadienamides was prepared and evaluated for PAF-antagonist activity. Compounds were assayed in vitro in a PAF-binding assay employing washed, whole dog platelets as the receptor source and in vivo after intravenous or oral administration for their ability to prevent PAF-induced bronchoconstriction in guinea pigs. Criteria required for good oral activity in the latter model include an (E,-E)-5-phenyl-2,4-pentadienamide, a second phenyl or a four- or five-carbon alkyl moiety in the 5-position of the diene, and an (R)-[1-alkyl-4-(3-pyridinyl)butyl] substituent on the carboxamide nitrogen atom. The alkyl substituent on this side chain can be methyl, ethyl, or cyclopropyl. Two members of this series, [R-(E)]-5,5-bis(4-methoxy-phenyl)-N- [1-methyl-4-(3-pyridinyl)butyl]- 2,4-pentadienamide (31) and [R-(E,E)]-5-(4-methoxyphenyl)-N-[1-methyl-4- (3-pyridinyl)butyl]-2,4-decadienamide (58), were selected for further pharmacological evaluation. Both were found to be substantially longer acting after oral administration than the corresponding S enantiomers in the guinea pig bronchoconstriction assay. A second in vivo model used to evaluate PAF antagonists determines the ability of test compounds to decrease the area of skin wheals induced by an intradermal injection of PAF. In this model, using both rats and guinea pigs, compounds 31 and 58 were found to be as active as the reference PAF antagonist 3-[4-(2-chlorophenyl)-9-methyl-6H- 1-(4-morpholinyl)-1-propanone (45).

Published
1989
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34. Pyrido[2,1-b]quinazolinecarboxylic acids as orally active antiallergy agents.

Author

Tilley JW, LeMahieu RA, Carson M, Kierstead RW, Baruth HW, and Yaremko B

Subjects
Administration, Oral, Animals, Male, Passive Cutaneous Anaphylaxis drug effects, Quinazolines administration & dosage, Quinazolines pharmacology, Rats, Structure-Activity Relationship, Hypersensitivity drug therapy, Quinazolines chemical synthesis
Abstract

A series of 8-substituted pyrido[2,1-]quinazoline-2-carboxylic acids was prepared by the nickel carbonyl mediated carboxylation of the corresponding bromides. The activities of these compounds in the rat PCA test are comparable to those of the corresponding 2-substituted pyrido[2,1-b]quinazoline-8-carboxylic acids.

Published
1980
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35. Aminoadamantane derivatives.

Author

Tilley JW and Kramer MJ

Subjects
Amantadine pharmacology, Amantadine toxicity, Animals, Antiviral Agents pharmacology, Humans, Memantine pharmacology, Nervous System Diseases drug therapy, Rimantadine pharmacology, Amantadine analogs & derivatives
Published
1981
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36. Antihypertensive (2-aminoethyl)thiourea derivatives. 2.

Author

Tilley JW, Ramuz H, Hefti F, and Gerold M

Subjects
Animals, Heart Rate drug effects, Male, Rats, Thiourea pharmacology, Antihypertensive Agents chemical synthesis, Thiourea analogs & derivatives
Abstract

Starting with 2,6-dichlorophenyl isothiocyanate, 1-(2-aminoethyl)-2-cyano-3-(2,6-dichlorophenyl)guanidine (2) was prepared in three steps. In contrast to the corresponding thiourea 1, this compound was essentially inactive as an antihypertensive agent.

Published
1980
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