Your search keyword '"Blythin DJ"' showing total 11 results

1. Antiinflammatory activity of substituted 6-hydroxypyrimido[2,1-f]purine-2,4,8(1H,3H,9H)-triones. Atypical nonsteroidal antiinflammatory agents

Author

Verbiar Ll, Daniel M. Solomon, L. A. Bober, Blythin Dj, P. J. S. Chiu, Spitler J, James J. Kaminski, David J. Conn, Shing Chun Wong, and Martin S. Domalski

Subjects

Male, Drug, Purine, Gastrointestinal Diseases, Stereochemistry, media_common.quotation_subject, Anti-Inflammatory Agents, Biological Availability, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Drug Discovery, Animals, Structure–activity relationship, Cyclooxygenase Inhibitors, Ulcer, media_common, chemistry.chemical_classification, Arthritis, Rats, Inbred Strains, Biological activity, Tautomer, Rats, Pyrimidines, chemistry, Purines, Lactam, Molecular Medicine, Tricyclic

Abstract

A novel class of antiinflammatory drugs, which are substituted derivatives of the fused tricyclic system 6-hydroxypyrimido[2,1-f]purine-2,4,8(1H,3H,9H)-trione, is described. Synthetic procedures and structure determination with the assistance of X-ray crystallography are discussed. Semiempirical molecular orbital calculations are used to investigate the relative stability of the possible isomers and tautomers of the title compounds. A biological profile of the class, and of several of the more potent analogues, in several antiinflammatory models, including the adjuvant-induced arthritis and the collagen II models, is defined. Several members of the class are shown to possess extremely low ulcerogenic effects in spite of exhibiting cyclooxygenase inhibition. A preliminary bioavailability study of two of the lead structures is presented. The compounds 6-72 appear to constitute a class of drugs that shows interesting potential antiarthritic activity and also exhibits an activity profile different from that of the standard classical NSAI drugs, as determined by a comparison of the profile of this class of drug with that of several standard agents. Certain findings from toxicological studies have precluded the further development of compounds within this group, although related structural types are being investigated.

Published

1986

2. Discovery of oxazole-based PDE4 inhibitors with picomolar potency.

Author

Kuang R, Shue HJ, Xiao L, Blythin DJ, Shih NY, Chen X, Gu D, Schwerdt J, Lin L, Ting PC, Cao J, Aslanian R, Piwinski JJ, Prelusky D, Wu P, Zhang J, Zhang X, Celly CS, Billah M, and Wang P

Subjects

Animals, Anti-Inflammatory Agents pharmacology, Cyclic N-Oxides chemistry, Cyclic Nucleotide Phosphodiesterases, Type 4 metabolism, Drug Discovery, Humans, Models, Molecular, Oxazoles pharmacology, Phosphodiesterase 4 Inhibitors pharmacology, Quinolines chemistry, Quinolines pharmacology, Rats, Structure-Activity Relationship, Tumor Necrosis Factor-alpha antagonists & inhibitors, Anti-Inflammatory Agents chemical synthesis, Cyclic Nucleotide Phosphodiesterases, Type 4 chemistry, Oxazoles chemical synthesis, Phosphodiesterase 4 Inhibitors chemical synthesis, Quinolines chemical synthesis

Abstract

Optimization of oxazole-based PDE4 inhibitors has led to the discovery of a series of quinolyl oxazoles, with 4-benzylcarboxamide and 5-α-aminoethyl groups which exhibit picomolar potency against PDE4. Selectivity profiles and in vivo biological activity are also reported., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

3. Discovery of a highly potent series of oxazole-based phosphodiesterase 4 inhibitors.

Author

Kuang R, Shue HJ, Blythin DJ, Shih NY, Gu D, Chen X, Schwerdt J, Lin L, Ting PC, Zhu X, Aslanian R, Piwinski JJ, Xiao L, Prelusky D, Wu P, Zhang J, Zhang X, Celly CS, Minnicozzi M, Billah M, and Wang P

Subjects

Animals, Cyclic Nucleotide Phosphodiesterases, Type 4 drug effects, Models, Molecular, Oxazoles chemistry, Phosphodiesterase Inhibitors chemistry, Rats, Oxazoles pharmacology, Phosphodiesterase Inhibitors pharmacology

Abstract

Substituted quinolyl oxazoles were discovered as a novel and highly potent series of phosphodiesterase 4 (PDE4) inhibitors. Structure-activity relationship studies revealed that the oxazole core, with 4-carboxamide and 5-aminomethyl groups, is a novel PDE4 inhibitory pharmacophore. Selectivity profiles and in vivo biological activity are also reported.

Published

2007

4. Cyclic urea derivatives as potent NK1 selective antagonists. Part II: Effects of fluoro and benzylic methyl substitutions.

Author

Shue HJ, Chen X, Schwerdt JH, Paliwal S, Blythin DJ, Lin L, Gu D, Wang C, Reichard GA, Wang H, Piwinski JJ, Duffy RA, Lachowicz JE, Coffin VL, Nomeir AA, Morgan CA, Varty GB, and Shih NY

Subjects

Animals, Anti-Anxiety Agents chemical synthesis, Benzyl Alcohols chemistry, Crystallography, X-Ray, Drug Evaluation, Preclinical, Fluorine chemistry, Gerbillinae, Models, Molecular, Molecular Structure, Motor Activity drug effects, Structure-Activity Relationship, Urea chemical synthesis, Anti-Anxiety Agents chemistry, Anti-Anxiety Agents pharmacology, Neurokinin-1 Receptor Antagonists, Urea analogs & derivatives, Urea pharmacology

Abstract

A series of novel five-membered urea derivatives as potent NK1 receptor antagonists is described. The effects of substitution of a 4-fluoro group at the phenyl ring and the introduction of an alpha-methyl group at the benzylic position to improve potency and duration of in vivo activity are discussed. Several compounds with high affinity and sustained in vivo activity were identified.

Published

2006

5. Cyclic urea derivatives as potent NK1 selective antagonists.

Author

Shue HJ, Chen X, Shih NY, Blythin DJ, Paliwal S, Lin L, Gu D, Schwerdt JH, Shah S, Reichard GA, Piwinski JJ, Duffy RA, Lachowicz JE, Coffin VL, Liu F, Nomeir AA, Morgan CA, and Varty GB

Subjects

Animals, Biological Availability, Dose-Response Relationship, Drug, Gerbillinae, Heterocyclic Compounds chemical synthesis, Heterocyclic Compounds pharmacokinetics, Heterocyclic Compounds pharmacology, Motor Activity drug effects, Protein Binding, Rats, Structure-Activity Relationship, Urea pharmacokinetics, Urea pharmacology, Neurokinin-1 Receptor Antagonists, Urea analogs & derivatives

Abstract

A series of novel five- and six-membered ring urea derivatives have been described as potent and selective NK1 receptor antagonists. Several compounds in this series exhibited good oral activity and brain penetration. Syntheses of these compounds are also described herein.

Published

2005

6. Synthesis and NK(1)/NK(2) binding activities of a series of diacyl-substituted 2-arylpiperazines.

Author

Blythin DJ, Chen X, Piwinski JJ, Shih NY, Shue HJ, Anthes JC, and McPhail AT

Subjects

Amino Acids chemistry, Animals, Cricetinae, Crystallography, X-Ray, Guinea Pigs, In Vitro Techniques, Male, Models, Molecular, Molecular Conformation, Piperazines chemistry, Piperidines pharmacology, Receptors, Neurokinin-1 chemistry, Receptors, Neurokinin-1 drug effects, Receptors, Neurokinin-2 chemistry, Receptors, Neurokinin-2 drug effects, Stereoisomerism, Structure-Activity Relationship, Trachea drug effects, Vas Deferens drug effects, Vas Deferens metabolism, Piperazines chemical synthesis, Receptors, Neurokinin-1 metabolism, Receptors, Neurokinin-2 metabolism

Abstract

The synthesis and binding affinity for hNK(1) and hNK(2) receptors of a series of diacyl substituted 2-aryl piperazines are described. SAR evaluation led to the racemic derivative 11g as an apparent dual inhibitor. Chiral chromatographic separation of 11g led to the observation that NK(1) activity was shown by one enantiomer (13a) and NK(2) activity was shown by the other enantiomer (13b). X-ray crystallographic analysis of the crystalline di-BOC derivative of the NK(2) active piperazine (15) showed that the 2R configuration was associated with NK(2) activity. Further derivatization indicated that dual NK(1)/NK(2) activity could be built into the 2R series.

Published

2002

7. Antagonism of GABA(B) receptors by morpholino-2-acetic acid derivatives Sch 54679 and Sch 51324 in rat brain.

Author

Ong J, Marino V, Parker DA, Kerr DI, and Blythin DJ

Subjects

Animals, Baclofen pharmacology, Dose-Response Relationship, Drug, Electric Stimulation, Electrophysiology, GABA Agonists pharmacology, GABA-B Receptor Agonists, In Vitro Techniques, Male, Morpholines chemistry, Neocortex drug effects, Neocortex physiology, Neurotransmitter Uptake Inhibitors pharmacology, Nipecotic Acids pharmacology, Oximes pharmacology, Rats, Rats, Sprague-Dawley, Tritium, gamma-Aminobutyric Acid drug effects, gamma-Aminobutyric Acid metabolism, GABA Antagonists pharmacology, GABA-B Receptor Antagonists, Morpholines pharmacology

Abstract

In rat neocortical slices maintained in Mg2+-free Krebs medium, baclofen depressed the rate of spontaneous discharges in a concentration-dependent manner (EC50 = 4.5 microM). This depression was reversibly antagonised by 5-(S,R)-hydroxymethyl-5-methylmorpholinyl-2-(R,S)-acetic acid (Sch 54679) and 2-(R,S)-5-[spirocyclopentyl]-morpholinyl-acetic acid (Sch 51324) (respective pA2 values of 5.8+/-0.15 and 5.4+/-0.2). In electrically-stimulated slices preloaded with [3H]gamma-aminobutyric acid (GABA), Sch 54679 (EC50 = 3 microM) was 2.3 times more potent than Sch 51324 (EC50 = 7 microM) in increasing [3H]GABA release through antagonism of GABA(B) autoreceptors. These structurally novel analogues may be pharmacologically useful for elucidating GABA(B) receptor functions.

Published

1999

8. The morpholino-acetic acid analogue Sch 50911 is a selective GABA(B) receptor antagonist in rat neocortical slices.

Author

Ong J, Marino V, Parker DA, Kerr DI, and Blythin DJ

Subjects

Animals, Baclofen pharmacology, Dose-Response Relationship, Drug, In Vitro Techniques, Male, Rats, Rats, Sprague-Dawley, GABA Antagonists pharmacology, GABA-B Receptor Antagonists, Morpholines pharmacology, Neocortex drug effects

Abstract

The pharmacological properties of (+)-(S)-5,5-dimethylmorpholinyl-2-acetic acid (Sch 50911) were evaluated on GABA(B) receptors in rat neocortical slices. The GABA(B) receptor agonist, baclofen, produced a concentration-dependent depression of the frequency of spontaneous discharges in slices maintained in Mg2+-free Krebs medium with an EC50 of 6 microM, reversibly antagonised by Sch 50911 (5, 10 and 25 microM) with an apparent pA2 of 6.0 +/- 0.1. The (-) enantiomer Sch 50910 (500 microM) and the racemic des-methyl analogue Sch 48588 (500 microM) were inactive. In slices preloaded with [3H]GABA, Sch 50911 antagonised GABA(B) autoreceptors, increasing the electrically-stimulated 3H overflow in a concentration-dependent manner, with an IC50 of 3 microM. The maximal effect (148 +/- 10.5%) was found at 10 microM, but at 50 microM the response was reduced to 67 +/- 19%. In contrast, evoked release was unaffected by Sch 50910 (100 microM) whilst Sch 48588 at 100 microM increased the overflow by 51.3 +/- 11.6%. In summary, Sch 50911 is a relatively potent antagonist of considerable potential in studies of GABA(B) receptor function.

Published

1998

9. Synthesis of a series of sulfinic acid analogs of GABA and evaluation of their GABAB receptor affinities.

Author

Carruthers NI, Spitler JM, Wong SC, Blythin DJ, Chen X, Shue HJ, She HS, Lee JF, Rizzo C, Ting PC, and West RE Jr

Subjects

Structure-Activity Relationship, Sulfinic Acids metabolism, gamma-Aminobutyric Acid metabolism, Receptors, GABA-B metabolism, Sulfinic Acids chemical synthesis, gamma-Aminobutyric Acid chemical synthesis

Abstract

A series of gamma-aminobutyric acid (GABA) 1 analogs was prepared in which the carboxylic acid group of GABA was replaced with a sulfinic acid group and their affinity for the GABAB receptor investigated.

Published

1998

10. The pharmacology of SCH 50911: a novel, orally-active GABA-beta receptor antagonist.

Author

Bolser DC, Blythin DJ, Chapman RW, Egan RW, Hey JA, Rizzo C, Kuo SC, and Kreutner W

Subjects

Administration, Oral, Animals, Antitussive Agents antagonists & inhibitors, Antitussive Agents pharmacology, Baclofen antagonists & inhibitors, Baclofen pharmacology, CHO Cells, Cats, Cholinergic Agents pharmacology, Cricetinae, GABA Antagonists administration & dosage, GABA Antagonists metabolism, Guinea Pigs, Humans, Ileum drug effects, Ileum physiology, In Vitro Techniques, Male, Morpholines administration & dosage, Morpholines metabolism, Muscle Contraction drug effects, Protein Binding, Rats, Rats, Sprague-Dawley, Receptors, GABA-B metabolism, Trachea drug effects, Trachea physiology, GABA Antagonists pharmacology, GABA-B Receptor Antagonists, Morpholines pharmacology

Abstract

Experiments were conducted to characterize the pharmacology of SCH 50911 ((+)-5,5-dimethyl-2-morpholineacetic acid hydrochloride), a structurally novel GABA-B receptor antagonist. Although more potent GABA-B antagonists have been reported, in this study SCH 50911 was compared with CGP 35348, a moderately potent and selective GABA-B antagonist with acceptable in vivo activity. SCH 50911 was more potent to inhibit the binding of GABA to the GABA-B receptor in rat brain (IC50 = 1.1 microM) than CGP 35348 (IC50 = 62 microM). SCH 50911 had no binding affinity for GABA-A, histamine H1, histamine H3, dopamine D1, dopamine D2, serotonin 5-HT2, or muscarinic m1, m2, or m4 receptors. However, SCH 50911 (IC50 = 2.2 microM) was active in a nonspecific muscarinic receptor binding assay, but was devoid of muscarinic agonist or antagonist activity in the isolated guinea pig ileum. SCH 50911 blocked inhibitory responses to baclofen of the guinea pig trachea in a competitive manner (pA2 = 5.8 +/- 0.004). CGP 35348 was 19-fold less potent in this assay (pA2 = 4.6 +/- 0.15). In vivo, SCH 50911 (ED50 = 2.9 mg kg-1, s.c.) and CGP 35348 (ED50 = 5.8 mg kg-1, s.c.) blocked the antitussive effects of baclofen in the guinea pig. In the cat, both SCH 50911 (10 mg kg-1, i.v.) and CGP 35348 (10 mg kg-1, i.v.) shifted the antitussive dose response relationship for baclofen to the right.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1995

11. Antiinflammatory activity of substituted 6-hydroxypyrimido[2,1-f]purine-2,4,8(1H,3H,9H)-triones. Atypical nonsteroidal antiinflammatory agents.

Author

Blythin DJ, Kaminski JJ, Domalski MS, Spitler J, Solomon DM, Conn DJ, Wong SC, Verbiar LL, Bober LA, and Chiu PJ

Subjects

Animals, Anti-Inflammatory Agents metabolism, Anti-Inflammatory Agents pharmacology, Arthritis drug therapy, Biological Availability, Cyclooxygenase Inhibitors, Gastrointestinal Diseases chemically induced, Male, Purines pharmacology, Pyrimidines pharmacology, Rats, Rats, Inbred Strains, Structure-Activity Relationship, Ulcer chemically induced, Anti-Inflammatory Agents chemical synthesis, Purines chemical synthesis, Pyrimidines chemical synthesis

Abstract

A novel class of antiinflammatory drugs, which are substituted derivatives of the fused tricyclic system 6-hydroxypyrimido[2,1-f]purine-2,4,8(1H,3H,9H)-trione, is described. Synthetic procedures and structure determination with the assistance of X-ray crystallography are discussed. Semiempirical molecular orbital calculations are used to investigate the relative stability of the possible isomers and tautomers of the title compounds. A biological profile of the class, and of several of the more potent analogues, in several antiinflammatory models, including the adjuvant-induced arthritis and the collagen II models, is defined. Several members of the class are shown to possess extremely low ulcerogenic effects in spite of exhibiting cyclooxygenase inhibition. A preliminary bioavailability study of two of the lead structures is presented. The compounds 6-72 appear to constitute a class of drugs that shows interesting potential antiarthritic activity and also exhibits an activity profile different from that of the standard classical NSAI drugs, as determined by a comparison of the profile of this class of drug with that of several standard agents. Certain findings from toxicological studies have precluded the further development of compounds within this group, although related structural types are being investigated.

Published

1986