Your search keyword '"Towner RD"' showing total 24 results

1. Investigation of the terminal P4 domain in a series of D-phenylglycinamide-based factor Xa inhibitors.

Author

Franciskovich JB, Masters JJ, Weber WW, Klimkowski VJ, Chouinard M, Sipes PR, Johnson LM, Snyder DW, Chastain MK, Craft TJ, Towner RD, Gifford-Moore DS, Froelich LL, Smallwood JK, Foster RS, Smith GF, Liebeschuetz JW, Murray CW, and Young SC

Subjects

Anticoagulants chemical synthesis, Anticoagulants chemistry, Anticoagulants pharmacology, Antithrombin III chemistry, Crystallography, X-Ray, Factor Xa chemistry, Factor Xa metabolism, Glycine chemical synthesis, Glycine chemistry, Glycine pharmacology, Humans, Models, Molecular, Molecular Structure, Protein Binding, Structure-Activity Relationship, Antithrombin III chemical synthesis, Antithrombin III pharmacology, Glycine analogs & derivatives

Abstract

Several P4 domain derivatives of the general d-phenylglycinamide-based scaffold (2) were synthesized and evaluated for their ability to bind to the serine protease factor Xa. Some of the more potent compounds were evaluated for their anticoagulant effects in vitro. A select subset containing various P1 indole constructs was further evaluated for their pharmacokinetic properties after oral administration to rats.

Published

2007

2. Anthranilamide inhibitors of factor Xa.

Author

Mendel D, Marquart AL, Joseph S, Waid P, Yee YK, Tebbe AL, Ratz AM, Herron DK, Goodson T, Masters JJ, Franciskovich JB, Tinsley JM, Wiley MR, Weir LC, Kyle JA, Klimkowski VJ, Smith GF, Towner RD, Froelich LL, Buben J, and Craft TJ

Subjects

Anticoagulants chemistry, Antithrombin III chemistry, Binding Sites, Chemistry, Pharmaceutical methods, Dose-Response Relationship, Drug, Drug Design, Drug Evaluation, Preclinical, Fluorescent Dyes chemical synthesis, Humans, Kinetics, Models, Chemical, Molecular Conformation, Structure-Activity Relationship, ortho-Aminobenzoates chemical synthesis, Antithrombin III chemical synthesis, Factor Xa Inhibitors, Fluorescent Dyes pharmacology, ortho-Aminobenzoates pharmacology

Abstract

SAR about the B-ring of a series of N(2)-aroyl anthranilamide factor Xa (fXa) inhibitors is described. B-ring o-aminoalkylether and B-ring p-amine probes of the S1' and S4 sites, respectively, afforded picomolar fXa inhibitors that performed well in in vitro anticoagulation assays.

Published

2007

3. Non-amidine-containing 1,2-dibenzamidobenzene inhibitors of human factor Xa with potent anticoagulant and antithrombotic activity.

Author

Masters JJ, Franciskovich JB, Tinsley JM, Campbell C, Campbell JB, Craft TJ, Froelich LL, Gifford-Moore DS, Hay LA, Herron DK, Klimkowski VJ, Kurz KD, Metz JT, Ratz AM, Shuman RT, Smith GF, Smith T, Towner RD, Wiley MR, Wilson A, and Yee YK

Subjects

Animals, Anticoagulants chemistry, Anticoagulants therapeutic use, Benzamides chemistry, Benzamides therapeutic use, Benzene Derivatives chemistry, Benzene Derivatives therapeutic use, Disease Models, Animal, Factor Xa metabolism, Fibrinolytic Agents chemistry, Fibrinolytic Agents therapeutic use, Humans, Piperidines chemistry, Rabbits, Structure-Activity Relationship, Thrombosis prevention & control, Anticoagulants pharmacology, Benzamides pharmacology, Benzene Derivatives pharmacology, Factor Xa Inhibitors, Fibrinolytic Agents pharmacology

Published

2000

4. 1,2-Dibenzamidobenzene inhibitors of human factor Xa.

Author

Herron DK, Goodson T Jr, Wiley MR, Weir LC, Kyle JA, Yee YK, Tebbe AL, Tinsley JM, Mendel D, Masters JJ, Franciskovich JB, Sawyer JS, Beight DW, Ratz AM, Milot G, Hall SE, Klimkowski VJ, Wikel JH, Eastwood BJ, Towner RD, Gifford-Moore DS, Craft TJ, and Smith GF

Subjects

Anticoagulants chemistry, Anticoagulants metabolism, Binding Sites, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Factor Xa chemistry, Factor Xa metabolism, Humans, Models, Molecular, Phenylenediamines chemistry, Phenylenediamines metabolism, Phenylenediamines pharmacology, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors metabolism, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides metabolism, Sulfonamides pharmacology, Thrombin metabolism, Anticoagulants chemical synthesis, Enzyme Inhibitors chemical synthesis, Factor Xa Inhibitors, Phenylenediamines chemical synthesis, Sulfonamides chemical synthesis, Thrombin antagonists & inhibitors

Abstract

High-throughput screening of a combinatorial library of diamidophenols yielded lead compounds with the ability to inhibit human factor Xa (fXa) at micromolar concentrations (e.g. compound 4, fXa apparent K(ass) = 0.64 x 10(6) L/mol). SAR studies in this novel structural series of fXa inhibitors showed that the phenolic hydroxyl group was not essential for activity. The best activity was found in substituted 1,2-dibenzamidobenzenes in which the phenyl group of one benzoyl group (A-ring) was substituted in the 4-position with relatively small lipophilic or polarizable groups such as methoxy, vinyl, or chloro and the phenyl group of the other benzoyl group (B-ring) was substituted in the 4-position with larger lipophilic groups such as tert-butyl or dimethylamino. The central phenyl ring (C-ring) tolerated a wide variety of substituents, but methoxy, methanesulfonamido, hydroxyl, and carboxyl substitution produced slightly higher levels of activity than other substituents when present in combination with favorable B-ring substitution. Methylation of the amide nitrogen atoms was found to greatly decrease activity. Compound 12 is the highest affinity fXa inhibitor in this group of compounds, having fXa apparent K(ass) = 25.5 x 10(6) L/mol, about 40x more active than the original lead. This lead series does not show potent inhibition of human thrombin. A model for the binding of these ligands to the fXa active site is proposed. The model is consistent with the observed SAR and can serve to guide future SAR studies.

Published

2000

5. N(2)-Aroylanthranilamide inhibitors of human factor Xa.

Author

Yee YK, Tebbe AL, Linebarger JH, Beight DW, Craft TJ, Gifford-Moore D, Goodson T Jr, Herron DK, Klimkowski VJ, Kyle JA, Sawyer JS, Smith GF, Tinsley JM, Towner RD, Weir L, and Wiley MR

Subjects

Anticoagulants chemistry, Anticoagulants metabolism, Benzamides chemistry, Benzamides metabolism, Binding Sites, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Factor Xa chemistry, Factor Xa metabolism, Humans, Models, Molecular, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides metabolism, Anticoagulants chemical synthesis, Benzamides chemical synthesis, Enzyme Inhibitors chemical synthesis, Factor Xa Inhibitors, Sulfonamides chemical synthesis

Abstract

Reversal of the A-ring amide link in 1,2-dibenzamidobenzene 1 (fXa K(ass) = 0.81 x 10(6) L/mol) led to a series of human factor Xa (hfXa) inhibitors based on N(2)-aroylanthranilamide 4. Expansion of the SAR around 4 showed that only small planar substituents could be accommodated in the A-ring for binding to the S1 site of hfXa. Bulky groups such as 4-isopropyl, 4-tert-butyl, and 4-dimethylamino were favored in the B-ring to interact with the S4 site of hfXa. The central (C) ring containing a 5-methanesulfonamido group yielded greater activity than carbamoyl groups. Combining the beneficial features from the B- and C-ring SAR, compound 55 represents the most potent hfXa inhibitor in the N(2)-aroylanthranilamide 4 series with hfXa K(ass) = 58 x 10(6) L/mol (K(i) = 11.5 nM).

Published

2000

6. Fused bicyclic Gly-Asp beta-turn mimics with potent affinity for GPIIb-IIIa. Exploration of the arginine isostere.

Author

Fisher MJ, Giese U, Harms CS, Kinnick MD, Lindstrom TD, McCowan JR, Mest HJ, Morin JM Jr, Mullaney JT, Paal M, Rapp A, Rühter G, Ruterbories KJ, Sall DJ, Scarborough RM, Schotten T, Stenzel W, Towner RD, Um SL, Utterback BG, Wyss VL, and Jakubowski JA

Subjects

Adenosine Diphosphate pharmacology, Animals, Arginine chemistry, Benzamidines chemistry, Biological Availability, Drug Evaluation, Enzyme-Linked Immunosorbent Assay, Fibrinogen metabolism, Humans, Inhibitory Concentration 50, Models, Molecular, Platelet Aggregation drug effects, Platelet Glycoprotein GPIIb-IIIa Complex metabolism, Prodrugs chemical synthesis, Prodrugs chemistry, Prodrugs pharmacokinetics, Protein Binding drug effects, Protein Structure, Secondary, Rats, Stereoisomerism, Acetates metabolism, Amidines metabolism, Platelet Glycoprotein GPIIb-IIIa Complex antagonists & inhibitors, Tetralones

Abstract

6-[4-Amidinobenzoyl]amino]-tetralone-2-acetic acid is a potent antagonist of GPIIb-IIIa. Substitution in the meta position of the benzamidine, or replacement with a heteroaryl amidine was tolerated in this series. Use of an acyl-linked 4-alkyl piperidine as an arginine isostere also provided active compounds. Compounds from this series provided substantial systemic exposure in the rat following oral administration.

Published

2000

7. Fused bicyclic Gly-Asp beta-turn mimics with specific affinity for GPIIb-IIIa.

Author

Fisher MJ, Arfstan AE, Giese U, Gunn BP, Harms CS, Khau V, Kinnick MD, Lindstrom TD, Martinelli MJ, Mest HJ, Mohr M, Morin JM Jr, Mullaney JT, Nunes A, Paal M, Rapp A, Rühter G, Ruterbories KJ, Sall DJ, Scarborough RM, Schotten T, Sommer B, Stenzel W, Towner RD, and Um SL

Subjects

Administration, Oral, Animals, Benzopyrans chemistry, Benzopyrans pharmacokinetics, Benzopyrans pharmacology, Binding, Competitive, Biological Availability, Enzyme-Linked Immunosorbent Assay, Guinea Pigs, Humans, Isoquinolines chemistry, Isoquinolines pharmacokinetics, Isoquinolines pharmacology, Molecular Mimicry, Platelet Aggregation drug effects, Platelet Glycoprotein GPIIb-IIIa Complex antagonists & inhibitors, Protein Structure, Secondary, Rats, Structure-Activity Relationship, Tetrahydronaphthalenes chemistry, Tetrahydronaphthalenes pharmacokinetics, Tetrahydronaphthalenes pharmacology, Benzopyrans chemical synthesis, Isoquinolines chemical synthesis, Oligopeptides chemistry, Platelet Glycoprotein GPIIb-IIIa Complex metabolism, Tetrahydronaphthalenes chemical synthesis

Abstract

Disubstituted isoquinolones 2 and 3 have affinity for GPIIb-IIIa and represent leads for further structural evaluation. Structure-activity studies centered on the bicyclic beta-turn mimic contained in these molecules indicated that this moiety could accommodate a variety of modifications. Specifically, monocyclic, 6, 5-bicyclic, and 6,7-bicyclic structures provide compounds with affinity for GPIIb-IIIa. Within the 6,6-series, isoquinoline, tetralin, tetralone, and benzopyran nuclei yield potent antagonists that are specific for GPIIb-IIIa. Attachment of the arginine isostere (benzamidine) to the supporting nucleus can be accomplished with an ether or amide linkage, although the latter enhances activity. Several compounds in this series provided measurable blood levels after oral dosing. Conversion of the acid moiety in these molecules to an ester generally provided compounds which gave greater systemic exposure after oral administration. Absolute bioavailabilities in the rat for the ethyl ester prodrug derivatives of the tetralin, tetralone, and benzopyran analogues of 3 were 28%, 23%, and 24%, respectively.

Published

1999

8. Benzylamine antioxidants: relationship between structure, peroxyl radical scavenging, lipid peroxidation inhibition, and cytoprotection.

Author

Yu MJ, McCowan JR, Phebus LA, Towner RD, Ho PP, Keith PT, Luttman CA, Saunders RD, Ruterbories KJ, and Lindstrom TD

Subjects

Animals, Antioxidants pharmacology, Benzylamines pharmacology, Blood Pressure drug effects, Brain metabolism, Hippocampus drug effects, Hydrogen Peroxide pharmacology, Iron pharmacology, Male, Membrane Lipids metabolism, Neurons drug effects, Peroxides, Rabbits, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Antioxidants chemical synthesis, Benzylamines chemical synthesis, Free Radical Scavengers, Lipid Peroxidation drug effects

Abstract

Three homologous series of 3,5-dialkoxy-4-hydroxybenzylamines were prepared and tested (1) as peroxyl radical scavengers in homogeneous aqueous solution, (2) as inhibitors of iron-dependent peroxidation of rabbit brain vesicular membrane lipids, and (3) as cytoprotective agents using primary cultures of rat hippocampal neurons exposed to hydrogen peroxide. The structural requirements for efficient radical trapping in homogeneous solution differed from those for effective lipid peroxidation inhibition: In homogeneous solution a kinetic preference existed for smaller, less sterically encumbered substituents flanking the reactive phenolic hydroxyl group. Lipid peroxidation inhibition, on the other hand, required longer more lipophilic substituents. Consequently, a lipophilic alkoxyl substituent at C3 and a small substituent at C5 appeared optimal for efficient radical scavenging activity in both lipid and homogeneous solution. Maximal cytoprotection of rat hippocampal neurons exposed to hydrogen peroxide was also associated with more lipophilic derivatives although substituent length and substituent bulk may represent independent parameters for relating structure and efficacy in this system.

Published

1993

9. Phenothiazines as lipid peroxidation inhibitors and cytoprotective agents.

Author

Yu MJ, McCowan JR, Thrasher KJ, Keith PT, Luttman CA, Ho PP, Towner RD, Bertsch B, Horng JS, and Um SL

Subjects

Animals, Antioxidants chemical synthesis, Antioxidants chemistry, Brain metabolism, Copper metabolism, Hippocampus cytology, Hippocampus drug effects, Hydrogen Peroxide pharmacology, Iron pharmacology, Lipoproteins, LDL metabolism, Macrophages metabolism, Membrane Lipids metabolism, Mice, Mice, Inbred BALB C, Neurons cytology, Neurons drug effects, Peritoneal Cavity cytology, Phenothiazines chemical synthesis, Phenothiazines chemistry, Rabbits, Rats, Structure-Activity Relationship, Antioxidants pharmacology, Cell Survival drug effects, Lipid Peroxidation drug effects, Phenothiazines pharmacology

Abstract

A series of phenothiazines was synthesized and evaluated as in vitro inhibitors of iron-dependent lipid peroxidation. The MIC (minimum tested concentration that gave greater than or equal to 50% inhibition) for 2-(10H-phenothiazin-2-yloxy)-N,N-dimethylethanolamine methanesulfonate (6) was 0.26 microM. Whereas methyl substitution at N-10 diminished activity nearly 100-fold, other structural modifications such as varying the amine group, the distance separating the amine substituent from the phenothiazine nucleus, and the linking group had little effect. Compound 6 was more effective than probucol, a known antioxidant, in blocking Cu2+ catalyzed oxidation of low-density lipoprotein (LDL) as measured by competitive scavenger receptor mediated degradation of 125I-labeled acetyl-LDL by mouse peritoneal macrophage cells in vitro. At a concentration of 5 microM, compound 6 also protected primary cultures of rat hippocampal neurons exposed to hydrogen peroxide (50 microM) when assessed 18 h later by fluorescein diacetate and propidium iodide uptake.

Published

1992

10. Anti-inflammatory effects of LY221068 and LY269415.

Author

Panetta JA, Benslay DN, Shadle JK, Towner RD, and Ho PP

Subjects

Animals, Arthritis, Experimental drug therapy, Calcimycin pharmacology, Guinea Pigs, Humans, In Vitro Techniques, Lipid Peroxidation drug effects, Lipoxygenase Inhibitors pharmacology, Prostaglandin-Endoperoxide Synthases metabolism, Rabbits, Rats, Thiazoles therapeutic use, Thiazolidines, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Thiazoles pharmacology

Abstract

LY221068, 5-[[3,5-bis(1,1-dimethylethyl)-4-hydroxy phenyl]methylene]-3-(dimethylamino)-4-thiazolidinone, and the monomethylamino analog, LY269415, are anti-oxidants and potent inhibitors of iron dependent lipid peroxidation and 5-lipoxygenase enzyme. Since oxygen radical species, lipid peroxides and products of the arachidonic acid cascade have been implicated as important mediators in a variety of inflammatory diseases including arthritis, LY221068 and LY269415 were studied in the Freund's Complete Adjuvant Induced Arthritis (FCA) model in rats. The compounds were administered orally and inhibition of bone damage and paw swelling of both the injected and uninjected paws was assessed. At 50 mg/kg p.o., LY221068 inhibited soft tissue swelling in the uninjected paw by 72% while LY269415 at 25 mg/kg p.o. exhibited 74% inhibition. Bone damage was also significantly inhibited by both compounds. In a dose response study, the minimum effective dose for LY221068 was 10 mg/kg p.o. and for LY269415 was 5 mg/kg p.o. In the established FCA model in rats, LY221068 at 50 mg/kg p.o. inhibited the uninjected paw swelling by 71% while LY269415 at 25 mg/kg p.o. inhibited 70%. These results suggest that LY221068 and LY269415 may be useful in the treatment of arthritis.

Published

1991

11. Xanthine oxidase inhibition does not limit canine infarct size.

Author

Werns SW, Grum CM, Ventura A, Hahn RA, Ho PP, Towner RD, Fantone JC, Schork MA, and Lucchesi BR

Subjects

Animals, Dogs, Free Radicals, Male, Time Factors, Xanthine Oxidase physiology, Myocardial Infarction drug therapy, Myocardial Reperfusion Injury prevention & control, Oxypurinol therapeutic use, Thiazoles therapeutic use, Xanthine Oxidase antagonists & inhibitors

Abstract

Background: Evidence supporting the role of xanthine oxidase in myocardial reperfusion injury is based on studies with pharmacological interventions used to inhibit enzyme function. Controversy exists, however, regarding the true role of xanthine oxidase in reperfusion injury. This study was performed to determine whether xanthine oxidase inhibition limits myocardial injury due to coronary artery occlusion and reperfusion., Methods and Results: Anesthetized dogs underwent coronary artery occlusion (90 minutes) and reperfusion (6 hours). Oxypurinol (28 mg/kg) or amflutizole (30 mg/kg), chemically unrelated inhibitors of xanthine oxidase, or vehicle was infused intravenously 15 minutes before and 3 hours after reperfusion. Regional myocardial blood flow was determined with radiolabeled microspheres. Infarct size was determined with the tetrazolium method. Myocardial infarct size (percent of risk region) was less in oxypurinol-treated dogs, 32 +/- 16%, compared with that of the control group, 46 +/- 15%. Infarct size for the amflutizole-treated dogs, 40 +/- 21%, was not significantly different from that of the control group. There were no differences in rate-pressure product or collateral blood flow to account for differences in infarct size. Uric acid concentration in the coronary venous plasma increased after reperfusion in the dogs treated with vehicle but not in the drug-treated dogs. Xanthine oxidase inhibition was demonstrated in each of the drug treatment groups, but only oxypurinol limited the extent of myocardial injury., Conclusions: Previously reported cardioprotective effects of allopurinol, noted to occur only when the drug was administered chronically, may be related to a property of oxypurinol, a major metabolite of allopurinol. The beneficial effect of oxypurinol is unrelated to inhibition of superoxide formation during xanthine oxidase-catalyzed oxidation of xanthine and hypoxanthine.

Published

1991

12. Characterization of LY233569 on 5-lipoxygenase and reperfusion injury of ischemic myocardium.

Author

Hahn RA, MacDonald BR, Simpson PJ, Wang L, Towner RD, Ho PP, Goodwin M, Breau AP, Suarez T, and Mihelich ED

Subjects

Animals, Coronary Vessels physiology, Dogs, Guinea Pigs, Humans, Leukotrienes physiology, Male, Myocardial Infarction prevention & control, Myocardial Reperfusion Injury drug therapy, Neutrophils enzymology, Random Allocation, Cinnamates pharmacology, Lipoxygenase Inhibitors, Myocardial Reperfusion Injury enzymology, Sulfhydryl Compounds pharmacology, Sulfides

Abstract

LY233569 produced concentration-dependent inhibition of isolated guinea pig 5-lipoxygenase (5-LPO) and 5-LPO activity of human polymorphonuclear leukocytes in vitro; IC50 values were 0.4 and 0.1 microM, respectively. LY233569 also inhibited (IC50 approximately 1.8 microM) zymosan-stimulated production of leukotriene B4 in canine whole blood but had little or no concomitant effect on the production of thromboxane B2. Concentrations of LY233569 as high as 10 microM did not inhibit production or scavenge superoxide from activated human neutrophils. In normal anesthetized dogs, infusion of LY233569 (0.11 mg/kg/min, i.v.) for 6 hr produced persistent inhibition (approximately 80%) of leukotriene B4 production in blood challenged ex vivo with zymosan; the plasma concentration (approximately 4 microM) of LY233569 was consistent with in vitro data illustrating selective and maximal inhibition of 5-LPO. In subsequent experiments, myocardial infarct size was measured after 1 hr of occlusion of the circumflex coronary artery and 5 hr of reperfusion. Continuous infusion of LY233569 (0.11 mg/kg/min, i.v.) had little or no effect on base-line systolic arterial pressure, cardiac rate and the pressure rate product when compared with time-related changes observed in control dogs. LY233569 infusion also did not alter the degree of ST-segment deviation or the intensity and duration of cardiac arrhythmias associated with coronary artery occlusion and reperfusion. Resultant myocardial infarct sizes were 45 +/- 5% of the left ventricle placed at risk in control dogs and 43 +/- 4% in dogs given LY233569. Myeloperoxidase activity of infarcted myocardium did not differ between groups.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1991

13. Cardiovascular effect and stimulus-dependent inhibition of superoxide generation from human neutrophils by tibenelast, 5,6-diethoxybenzo(b)thiophene-2-carboxylic acid, sodium salt (LY186655).

Author

Ho PP, Wang LY, Towner RD, Hayes SJ, Pollock D, Bowling N, Wyss V, and Panetta JA

Subjects

Animals, Arachidonic Acid, Arachidonic Acids metabolism, Blood Pressure drug effects, Cats, Dogs, Guinea Pigs, Heart Rate drug effects, Humans, In Vitro Techniques, Myocardial Contraction drug effects, Neutrophils metabolism, Phosphodiesterase Inhibitors pharmacology, Stimulation, Chemical, Bronchodilator Agents pharmacology, Neutrophils drug effects, Superoxides metabolism, Thiophenes pharmacology

Abstract

Tibenelast (LY186655), 5,6,-diethoxybenzo(b)thiophene-2-carboxylic acid, sodium salt, is an orally active anti-anaphylactic compound in guinea pigs, and has been shown to prevent bronchospasm in moderately severe asthmatic patients. Pharmacological studies with tibenelast demonstrated that it is a selective phosphodiesterase (PDE) inhibitor in that it is moderately active against the lung and stomach enzyme while being a very weak inhibitor of the heart enzyme. The compound was without cardiovascular effects at anti-anaphylactic doses. In contrast to theophylline, tibenelast did not have a direct inotropic effect in the cat papillary muscle system. The concentration that inhibited 50% of the enzymatic activity (IC50) for tibenelast was 20- to 30-fold lower for neutrophil PDE than for PDE of other tissues. It was 100 times more potent than aminophylline in inhibiting superoxide generation from platelet-activating factor (PAF)-primed polymorphonuclear leukocytes (PMNL) challenged with chemotactic factor, N-formyl-methionyl-leucyl-phenylalanine. However, tibenelast was less effective in the tumor necrosis factor-primed system, and did not inhibit superoxide generation during phagocytosis or when other soluble stimuli, such as phorbo-12-myristate-13-acetate or the calcium ionophore A23187, were used. Furthermore, tibenelast did not inhibit enzymes involved in arachidonic acid metabolism. These results suggest that tibenelast probably inhibits superoxide release from PMNL via a selective inhibition on PDE.

Published

1990

14. Reversal of platelet aggregation by aortic microsomes.

Author

Ho PP, Herrmann RG, Towner RD, and Walters CP

Subjects

Adenosine Diphosphate pharmacology, Animals, Arachidonic Acids pharmacology, Cattle, Humans, Thrombin pharmacology, Aorta physiology, Microsomes physiology, Platelet Aggregation drug effects

Published

1977

15. The anti-inflammatory effects of LY178002 and LY256548.

Author

Panetta JA, Benslay DN, Phillips ML, Towner RD, Bertsch B, Wang L, and Ho PP

Subjects

Animals, Arachidonic Acid, Arachidonic Acids metabolism, Arachidonic Acids pharmacology, Arthritis, Arthritis, Experimental metabolism, Cyclooxygenase Inhibitors, Freund's Adjuvant, Guinea Pigs, In Vitro Techniques, Neutrophils enzymology, Thiazolidines, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arthritis, Experimental drug therapy, Thiazoles pharmacology

Abstract

LY178002 (5-[3,5-bis(1,1-dimethylethyl)-4-hydroxyphenyl]methylene-4-thiazolidinon e) and its N-methyl analog, LY256548, inhibit the enzymatic activity of phospholipase A2, 5-lipoxygenase and fatty acid cycloxygenase. They also inhibit leukotriene B4 production from human polymorphonuclear leukocytes stimulated with the calcium ionophore A23187. Since products of the arachidonic acid cascade have been implicated as important mediators in a variety of inflammatory diseases including arthritis, LY178002 and LY256548 were studied in the Freund's Complete Adjuvant-Induced Arthritis (FCA) model in rats. The compounds were administered orally and inhibition of bone damage and paw swelling was assessed of both the injected and uninjected paws. At 50 mg/kg LY178002 inhibited soft tissue swelling in the uninjected paw by 81% while LY256548 exhibited 57% inhibition. Bone damage was also significantly inhibited by both compounds. A dose response was conducted. The minimum effective dose for LY178002 was 10 mg/kg p.o. In the established FCA model LY178002 at 50 mg/kg p.o. inhibited the uninjected paw swelling by 75% while LY256548 did not show this level of activity. These results suggest that LY178002 and LY256548 may be useful in the treatment of arthritis.

Published

1989

16. Purification of prostaglandin A isomerase from rabbit serum.

Author

Ho PP, Towner RD, and Sullivan HR

Subjects

Aluminum, Ammonium Sulfate, Animals, Buffers, Chromatography, Gas, Chromatography, Gel, Ethylmaleimide pharmacology, Hot Temperature, Hydrogen-Ion Concentration, Isomerases antagonists & inhibitors, Isomerases isolation & purification, Kinetics, Mass Spectrometry, Prostaglandins analysis, Rabbits, Time Factors, Isomerases blood

Published

1974

17. Purification and characterization of fatty acid cyclooxygenase from human platelets.

Author

Ho PP, Towner RD, and Esterman MA

Subjects

Chromatography, Agarose, Chromatography, Gel, Electrophoresis, Disc, Humans, Isoelectric Focusing, Molecular Weight, Prostaglandin-Endoperoxide Synthases blood, Prostaglandins H metabolism, Ultrafiltration, Blood Platelets enzymology, Prostaglandin-Endoperoxide Synthases isolation & purification

Abstract

The fatty acid cyclooxygenase (EC 1.14.99.1) that produces the prostaglandin, thromboxane, and prostacyclin precursor (PGH2), was solubilized from human platelet microsomes in 20 sucrose and 1.0% Triton X-100. The enzyme was purified 300-fold by electrofocusing, Sephadex G-200 gel filtration, and hydrophobic chromatography on ethyl agarose. The cyclooxygenase catalyzed the conversion of arachidonic acid to prostaglandin endoperioxide, PGH2, that was trapped at -25 degrees C and separated on TLC at -20 degrees C. PGH2 was hydrolyzed to HHT in acidic pH, or was chemically converted to PGE2 in slightly alkaline pH in the absence of cofactors. The enzyme showed a broad pH optimum in the range of 7-9. Hemin containing substances such as methemoglobin were absolutely required as cofactors, while tryptophan, epinephrine, phenol, and hydroquinone stimulated the PGH2 formation. Metal ions, such as ZN2+ and Cd2+ inhibited the enzyme reaction at 0.1 to 1 mM. The molecular weight of the purified enzyme was estimated at 79,432 by sodium dodecyl sulfate disc gel electrophoresis at pH 8.0. The properties of the human platelet enzyme was generally similar to the sheep vesicular enzyme in the method of solubilization, pH optimum, and molecular weight.

Published

1980

18. Affinity chromatography of 15-hydroxyprostaglandin dehydrogenase from dog lung.

Author

Ho PP and Towner RD

Subjects

Animals, Chromatography, Affinity, Dogs, Alcohol Oxidoreductases isolation & purification, Hydroxyprostaglandin Dehydrogenases isolation & purification, Lung enzymology

Published

1976

19. A rapid method for determining ATP by the firefly luciferin-luciferase system.

Author

Neufeld HA, Towner RD, and Pace J

Subjects

Adenosine Triphosphate pharmacology, Animals, Light, Adenosine Triphosphate analysis, Biological Assay methods, Firefly Luciferin analysis, Insecta analysis, Luciferases analysis

Published

1975

20. Dog liver 3-hydroxy-3-methylglutaryl coenzyme A reductase.

Author

Ho PP, Esterman MA, Towner RD, and Turner RK

Subjects

Animals, Dogs, Eating, Female, Hydroxymethylglutaryl CoA Reductases isolation & purification, Kinetics, Male, Methods, Solubility, Alcohol Oxidoreductases metabolism, Hydroxymethylglutaryl CoA Reductases metabolism, Microsomes, Liver enzymology

Abstract

A rapid and sensitive assay method for 3-hydroxy-3-methylglutaryl coenzyme A reductase (HMG-coA reductase, EC 1.1.1.34) is described. HMG-coA reductase is demonstrated in dog liver microsomes, and the converted reaction product has been identified as mevalonolactone. The enzyme activity undergoes cyclic variation and increases by more than tenfold 5 h after feeding. The properties of dog liver enzyme are generally similar to the rat liver enzyme in the method of solubilization, cold inactivation, pH optimum, and Km values.

Published

1977

21. CHEMILUMINESCENCE OF LUMINOL IN THE PRESENCE OF HEMATIN COMPOUNDS.

Author

NEUFELD HA, CONKLIN CJ, and TOWNER RD

Subjects

Heme, Hemin, Hydrogen Peroxide, Indicators and Reagents, Luminescence, Luminol, Microchemistry, Research

Published

1965

22. Some characteristics of riboflavin chemiluminescence.

Author

Towner RD, Neufeld HA, and Shevlin PB

Subjects

Alcaligenes, Buffers, Darkness, Fluorescence, Hydrogen Peroxide, Hydrogen-Ion Concentration, Luminescent Measurements, Osmium, Photometry instrumentation, Spectrophotometry, Ultraviolet Rays, Riboflavin

Published

1970

23. Biochemical and microbiological studies on 6-substituted penicillins.

Author

Ho PP, Towner RD, Indelicato JM, Spitzer WA, and Koppel GA

Subjects

Escherichia coli drug effects, Hydrolysis, Microbial Sensitivity Tests, Penicillin G pharmacology, Penicillin V pharmacology, Protease Inhibitors, Structure-Activity Relationship, Penicillins

Published

1972

24. Letter: Biochemical and microbiological studies on 7-methoxycephalosporins.

Author

Ho PP, Towner RD, Indelicato JM, Wilham WJ, Spitzer WA, and Koppel GA

Subjects

Cell Wall enzymology, Hydrogen-Ion Concentration, Hydrolysis, Methyl Ethers pharmacology, Peptide Elongation Factors, Peptides, Structure-Activity Relationship, Acyltransferases antagonists & inhibitors, Cephalosporins pharmacology

Published

1973