Your search keyword '"Harper TW"' showing total 38 results

1. Orally bioavailable amine-linked macrocyclic inhibitors of factor XIa.

Author

Fang T, Corte JR, Gilligan PJ, Jeon Y, Osuna H, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Wexler RR, and Lam PYS

Subjects

Administration, Oral, Animals, Binding Sites, Drug Design, Factor XIa metabolism, Half-Life, Macrocyclic Compounds metabolism, Macrocyclic Compounds pharmacokinetics, Molecular Dynamics Simulation, Protein Structure, Tertiary, Pyridines chemistry, Rats, Serine Proteinase Inhibitors metabolism, Serine Proteinase Inhibitors pharmacokinetics, Structure-Activity Relationship, Amines chemistry, Factor XIa antagonists & inhibitors, Macrocyclic Compounds chemistry, Serine Proteinase Inhibitors chemical synthesis

Abstract

The discovery of orally bioavailable FXIa inhibitors has been a challenge. Herein, we describe our efforts to address this challenge by optimization of our imidazole-based macrocyclic series. Our optimization strategy focused on modifications to the P2 prime, macrocyclic amide linker, and the imidazole scaffold. Replacing the amide of the macrocyclic linker with amide isosteres led to the discovery of substituted amine linkers which not only maintained FXIa binding affinity but also improved oral exposure in rats. Combining the optimized macrocyclic amine linker with a pyridine scaffold afforded compounds 23 and 24 that were orally bioavailable, single-digit nanomolar FXIa inhibitors with excellent selectivity against relevant blood coagulation enzymes., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

2. Potent, Orally Bioavailable, and Efficacious Macrocyclic Inhibitors of Factor XIa. Discovery of Pyridine-Based Macrocycles Possessing Phenylazole Carboxamide P1 Groups.

Author

Corte JR, Pinto DJP, Fang T, Osuna H, Yang W, Wang Y, Lai A, Clark CG, Sun JH, Rampulla R, Mathur A, Kaspady M, Neithnadka PR, Li YC, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Harper TW, Huang C, Zheng JJ, Bozarth JM, Wu Y, Wong PC, Crain EJ, Seiffert DA, Luettgen JM, Lam PYS, Wexler RR, and Ewing WR

Subjects

Animals, Biological Availability, Blood Coagulation drug effects, Crystallography, X-Ray, Drug Design, Drug Discovery, Fibrinolytic Agents pharmacokinetics, Humans, Imidazoles chemical synthesis, Imidazoles pharmacology, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds pharmacology, Models, Molecular, Partial Thromboplastin Time, Rabbits, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors pharmacology, Structure-Activity Relationship, Thrombosis drug therapy, Factor XIa antagonists & inhibitors, Fibrinolytic Agents chemical synthesis, Fibrinolytic Agents pharmacology, Pyridines chemical synthesis, Pyridines pharmacology

Abstract

Factor XIa (FXIa) inhibitors are promising novel anticoagulants, which show excellent efficacy in preclinical thrombosis models with minimal effects on hemostasis. The discovery of potent and selective FXIa inhibitors which are also orally bioavailable has been a challenge. Here, we describe optimization of the imidazole-based macrocyclic series and our initial progress toward meeting this challenge. A two-pronged strategy, which focused on replacement of the imidazole scaffold and the design of new P1 groups, led to the discovery of potent, orally bioavailable pyridine-based macrocyclic FXIa inhibitors. Moreover, pyridine-based macrocycle 19 , possessing the phenylimidazole carboxamide P1, exhibited excellent selectivity against relevant blood coagulation enzymes and displayed antithrombotic efficacy in a rabbit thrombosis model.

Published

2020

3. Discovery of Potent Protease-Activated Receptor 4 Antagonists with in Vivo Antithrombotic Efficacy.

Author

Miller MM, Banville J, Friends TJ, Gagnon M, Hangeland JJ, Lavallée JF, Martel A, O'Grady H, Rémillard R, Ruediger E, Tremblay F, Posy SL, Allegretto NJ, Guarino VR, Harden DG, Harper TW, Hartl K, Josephs J, Malmstrom S, Watson C, Yang Y, Zhang G, Wong P, Yang J, Bouvier M, Seiffert DA, Wexler RR, Lawrence RM, Priestley ES, and Marinier A

Subjects

Animals, Benzofurans chemistry, Benzofurans pharmacokinetics, Biological Availability, Disease Models, Animal, Fibrinolytic Agents chemistry, Fibrinolytic Agents pharmacokinetics, HEK293 Cells, Hemorrhage metabolism, Humans, Macaca fascicularis, Models, Chemical, Molecular Structure, Platelet Aggregation drug effects, Receptors, Thrombin genetics, Receptors, Thrombin metabolism, Structure-Activity Relationship, Thrombosis metabolism, Benzofurans pharmacology, Fibrinolytic Agents pharmacology, Hemorrhage prevention & control, Receptors, Thrombin antagonists & inhibitors, Thrombosis prevention & control

Abstract

In an effort to identify novel antithrombotics, we have investigated protease-activated receptor 4 (PAR4) antagonism by developing and evaluating a tool compound, UDM-001651 , in a monkey thrombosis model. Beginning with a high-throughput screening hit, we identified an imidazothiadiazole-based PAR4 antagonist chemotype. Detailed structure-activity relationship studies enabled optimization to a potent, selective, and orally bioavailable PAR4 antagonist, UDM-001651 . UDM-001651 was evaluated in a monkey thrombosis model and shown to have robust antithrombotic efficacy and no prolongation of kidney bleeding time. This combination of excellent efficacy and safety margin strongly validates PAR4 antagonism as a promising antithrombotic mechanism.

Published

2019

4. Discovery of Clinical Candidate BMS-823778 as an Inhibitor of Human 11β-Hydroxysteroid Dehydrogenase Type 1 (11β-HSD-1).

Author

Li J, Kennedy LJ, Walker SJ, Wang H, Li JJ, Hong Z, O'Connor SP, Ye XY, Chen S, Wu S, Yoon DS, Nayeem A, Camac DM, Ramamurthy V, Morin PE, Sheriff S, Wang M, Harper TW, Golla R, Seethala R, Harrity T, Ponticiello RP, Morgan NN, Taylor JR, Zebo R, Maxwell B, Moulin F, Gordon DA, and Robl JA

Abstract

BMS-823778 ( 2 ), a 1,2,4-triazolopyridinyl-methanol derived analog, was identified as a potent and selective inhibitor of human 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD-1) enzyme (IC 50 = 2.3 nM) with >10,000-fold selectivity over 11β-HSD-2. Compound 2 exhibits robust acute pharmacodynamic effects in cynomolgus monkeys (ED 50 = 0.6 mg/kg) and in diet-induced obese (DIO) mice (ED 50 = 34 mg/kg). Compound 2 also showed excellent inhibition in an ex vivo adipose DIO mouse model (ED 50 = 5.2 mg/kg). Oral bioavailability ranges from 44% to 100% in preclinical species. Its favorable development properties, pharmacokinetics, high adipose-to-plasma concentration ratio, and preclinical pharmacology profile have prompted the evaluation of 2 for the treatment of type 2 diabetes and metabolic syndrome in phase 2 clinical trials., Competing Interests: The authors declare no competing financial interest.

Published

2018

5. Discovery of a Parenteral Small Molecule Coagulation Factor XIa Inhibitor Clinical Candidate (BMS-962212).

Author

Pinto DJP, Orwat MJ, Smith LM 2nd, Quan ML, Lam PYS, Rossi KA, Apedo A, Bozarth JM, Wu Y, Zheng JJ, Xin B, Toussaint N, Stetsko P, Gudmundsson O, Maxwell B, Crain EJ, Wong PC, Lou Z, Harper TW, Chacko SA, Myers JE Jr, Sheriff S, Zhang H, Hou X, Mathur A, Seiffert DA, Wexler RR, Luettgen JM, and Ewing WR

Subjects

Animals, Anticoagulants pharmacokinetics, Anticoagulants pharmacology, Blood Coagulation drug effects, Crystallography, X-Ray, Dogs, Drug Discovery, Factor XIa chemistry, Factor XIa metabolism, Humans, Isoquinolines pharmacokinetics, Isoquinolines pharmacology, Male, Molecular Docking Simulation, Rabbits, Rats, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacokinetics, Small Molecule Libraries pharmacology, Small Molecule Libraries therapeutic use, Thrombosis blood, para-Aminobenzoates pharmacokinetics, para-Aminobenzoates pharmacology, Anticoagulants chemistry, Anticoagulants therapeutic use, Factor XIa antagonists & inhibitors, Isoquinolines chemistry, Isoquinolines therapeutic use, Thrombosis drug therapy, para-Aminobenzoates chemistry, para-Aminobenzoates therapeutic use

Abstract

Factor XIa (FXIa) is a blood coagulation enzyme that is involved in the amplification of thrombin generation. Mounting evidence suggests that direct inhibition of FXIa can block pathologic thrombus formation while preserving normal hemostasis. Preclinical studies using a variety of approaches to reduce FXIa activity, including direct inhibitors of FXIa, have demonstrated good antithrombotic efficacy without increasing bleeding. On the basis of this potential, we targeted our efforts at identifying potent inhibitors of FXIa with a focus on discovering an acute antithrombotic agent for use in a hospital setting. Herein we describe the discovery of a potent FXIa clinical candidate, 55 (FXIa K i = 0.7 nM), with excellent preclinical efficacy in thrombosis models and aqueous solubility suitable for intravenous administration. BMS-962212 is a reversible, direct, and highly selective small molecule inhibitor of FXIa.

Published

2017

6. Macrocyclic inhibitors of Factor XIa: Discovery of alkyl-substituted macrocyclic amide linkers with improved potency.

Author

Corte JR, Yang W, Fang T, Wang Y, Osuna H, Lai A, Ewing WR, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Quan ML, Wexler RR, and Lam PYS

Subjects

Amides chemical synthesis, Amides chemistry, Crystallography, X-Ray, Dose-Response Relationship, Drug, Factor XIa metabolism, Humans, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds chemistry, Models, Molecular, Molecular Structure, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Structure-Activity Relationship, Amides pharmacology, Drug Discovery, Factor XIa antagonists & inhibitors, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

Optimization of macrocyclic inhibitors of FXIa is described which focused on modifications to both the macrocyclic linker and the P1 group. Increases in potency were discovered through interactions with a key hydrophobic region near the S1 prime pocket by substitution of the macrocyclic linker with small alkyl groups. Both the position of substitution and the absolute stereochemistry of the alkyl groups on the macrocyclic linker which led to improved potency varied depending on the ring size of the macrocycle. Replacement of the chlorophenyltetrazole cinnamide P1 in these optimized macrocycles reduced the polar surface area and improved the oral bioavailability for the series, albeit at the cost of a decrease in potency., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

7. Discovery of Clinical Candidate 2-((2S,6S)-2-Phenyl-6-hydroxyadamantan-2-yl)-1-(3'-hydroxyazetidin-1-yl)ethanone [BMS-816336], an Orally Active Novel Selective 11β-Hydroxysteroid Dehydrogenase Type 1 Inhibitor.

Author

Ye XY, Chen SY, Wu S, Yoon DS, Wang H, Hong Z, O'Connor SP, Li J, Li JJ, Kennedy LJ, Walker SJ, Nayeem A, Sheriff S, Camac DM, Ramamurthy V, Morin PE, Zebo R, Taylor JR, Morgan NN, Ponticiello RP, Harrity T, Apedo A, Golla R, Seethala R, Wang M, Harper TW, Sleczka BG, He B, Kirby M, Leahy DK, Li J, Hanson RL, Guo Z, Li YX, DiMarco JD, Scaringe R, Maxwell B, Moulin F, Barrish JC, Gordon DA, and Robl JA

Subjects

11-beta-Hydroxysteroid Dehydrogenase Type 1 chemistry, 11-beta-Hydroxysteroid Dehydrogenase Type 1 metabolism, Actins antagonists & inhibitors, Adamantane administration & dosage, Adamantane chemistry, Adamantane pharmacology, Administration, Oral, Animals, Azetidines administration & dosage, Azetidines chemistry, Biological Availability, Crystallography, X-Ray, Dogs, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors chemistry, Female, Half-Life, Humans, Hypothalamo-Hypophyseal System drug effects, Inhibitory Concentration 50, Macaca fascicularis, Male, Mice, Obese, Rats, Structure-Activity Relationship, 11-beta-Hydroxysteroid Dehydrogenase Type 1 antagonists & inhibitors, Adamantane analogs & derivatives, Azetidines pharmacology, Enzyme Inhibitors pharmacology

Abstract

BMS-816336 (6n-2), a hydroxy-substituted adamantyl acetamide, has been identified as a novel, potent inhibitor against human 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) enzyme (IC 50 3.0 nM) with >10000-fold selectivity over human 11β-hydroxysteroid dehydrogenase type 2 (11β-HSD2). 6n-2 exhibits a robust acute pharmacodynamic effect in cynomolgus monkeys (ED 50 0.12 mg/kg) and in DIO mice. It is orally bioavailable (%F ranges from 20 to 72% in preclinical species) and has a predicted pharmacokinetic profile of a high peak to trough ratio and short half-life in humans. This ADME profile met our selection criteria for once daily administration, targeting robust inhibition of 11β-HSD1 enzyme for the first 12 h period after dosing followed by an "inhibition holiday" so that the potential for hypothalamic-pituitary-adrenal (HPA) axis activation might be mitigated. 6n-2 was found to be well-tolerated in phase 1 clinical studies and represents a potential new treatment for type 2 diabetes, metabolic syndrome, and other human diseases modulated by glucocorticoid control.

Published

2017

8. Structure-Based Design of Macrocyclic Factor XIa Inhibitors: Discovery of the Macrocyclic Amide Linker.

Author

Corte JR, Fang T, Osuna H, Pinto DJ, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Decicco CP, Wexler RR, and Quan ML

Subjects

Drug Discovery, Hydrogen Bonding, Ligands, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacokinetics, Molecular Structure, Serine Proteinase Inhibitors pharmacokinetics, Amides chemistry, Factor XIa antagonists & inhibitors, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors pharmacology

Abstract

A novel series of macrocyclic FXIa inhibitors was designed based on our lead acyclic phenyl imidazole chemotype. Our initial macrocycles, which were double-digit nanomolar FXIa inhibitors, were further optimized with assistance from utilization of structure-based drug design and ligand bound X-ray crystal structures. This effort resulted in the discovery of a macrocyclic amide linker which was found to form a key hydrogen bond with the carbonyl of Leu41 in the FXIa active site, resulting in potent FXIa inhibitors. The macrocyclic FXIa series, exemplified by compound 16, had a FXIa K i = 0.16 nM with potent anticoagulant activity in an in vitro clotting assay (aPTT EC 1.5x = 0.27 μM) and excellent selectivity against the relevant blood coagulation enzymes.

Published

2017

9. Orally bioavailable pyridine and pyrimidine-based Factor XIa inhibitors: Discovery of the methyl N-phenyl carbamate P2 prime group.

Author

Corte JR, Fang T, Pinto DJ, Orwat MJ, Rendina AR, Luettgen JM, Rossi KA, Wei A, Ramamurthy V, Myers JE Jr, Sheriff S, Narayanan R, Harper TW, Zheng JJ, Li YX, Seiffert DA, Wexler RR, and Quan ML

Subjects

Administration, Oral, Animals, Anticoagulants administration & dosage, Anticoagulants pharmacokinetics, Blood Coagulation drug effects, Crystallography, X-Ray, Dogs, Factor XIa metabolism, Humans, Models, Molecular, Phenylcarbamates administration & dosage, Phenylcarbamates chemistry, Phenylcarbamates pharmacokinetics, Phenylcarbamates pharmacology, Pyridines administration & dosage, Pyridines pharmacokinetics, Pyrimidines administration & dosage, Pyrimidines pharmacokinetics, Anticoagulants chemistry, Anticoagulants pharmacology, Factor XIa antagonists & inhibitors, Pyridines chemistry, Pyridines pharmacology, Pyrimidines chemistry, Pyrimidines pharmacology

Abstract

Pyridine-based Factor XIa (FXIa) inhibitor (S)-2 was optimized by modifying the P2 prime, P1, and scaffold regions. This work resulted in the discovery of the methyl N-phenyl carbamate P2 prime group which maintained FXIa activity, reduced the number of H-bond donors, and improved the physicochemical properties compared to the amino indazole P2 prime moiety. Compound (S)-17 was identified as a potent and selective FXIa inhibitor that was orally bioavailable. Replacement of the basic cyclohexyl methyl amine P1 in (S)-17 with the neutral p-chlorophenyltetrazole P1 resulted in the discovery of (S)-24 which showed a significant improvement in oral bioavailability compared to the previously reported imidazole (S)-23. Additional improvements in FXIa binding affinity, while maintaining oral bioavailability, was achieved by replacing the pyridine scaffold with either a regioisomeric pyridine or pyrimidine ring system., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

10. Novel phenylalanine derived diamides as Factor XIa inhibitors.

Author

Smith LM 2nd, Orwat MJ, Hu Z, Han W, Wang C, Rossi KA, Gilligan PJ, Pabbisetty KB, Osuna H, Corte JR, Rendina AR, Luettgen JM, Wong PC, Narayanan R, Harper TW, Bozarth JM, Crain EJ, Wei A, Ramamurthy V, Morin PE, Xin B, Zheng J, Seiffert DA, Quan ML, Lam PYS, Wexler RR, and Pinto DJP

Subjects

Anilides chemical synthesis, Animals, Crystallography, X-Ray, Dogs, Phenylalanine chemical synthesis, Rabbits, Structure-Activity Relationship, Anilides pharmacology, Factor XIa antagonists & inhibitors, Phenylalanine analogs & derivatives, Phenylalanine pharmacology

Abstract

The synthesis, structural activity relationships (SAR), and selectivity profile of a potent series of phenylalanine diamide FXIa inhibitors will be discussed. Exploration of P1 prime and P2 prime groups led to the discovery of compounds with high FXIa affinity, good potency in our clotting assay (aPPT), and high selectivity against a panel of relevant serine proteases as exemplified by compound 21. Compound 21 demonstrated good in vivo efficacy (EC50=2.8μM) in the rabbit electrically induced carotid arterial thrombosis model (ECAT)., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

11. Design, synthesis and evaluation of phenethylaminoheterocycles as K(v)1.5 inhibitors.

Author

Johnson JA, Xu N, Jeon Y, Finlay HJ, Kover A, Conder ML, Sun H, Li D, Levesque P, Hsueh MM, Harper TW, Wexler RR, and Lloyd J

Subjects

Animals, Carbamates chemical synthesis, Carbamates chemistry, Dose-Response Relationship, Drug, Heart Atria drug effects, Heart Rate drug effects, Humans, Indazoles chemical synthesis, Indazoles chemistry, Models, Molecular, Molecular Structure, Potassium Channel Blockers chemical synthesis, Potassium Channel Blockers chemistry, Rabbits, Rats, Structure-Activity Relationship, Carbamates pharmacology, Drug Design, Indazoles pharmacology, Kv1.5 Potassium Channel antagonists & inhibitors, Potassium Channel Blockers pharmacology

Abstract

Phenethylaminoheterocycles have been prepared and assayed for inhibition of the Kv1.5 potassium ion channel as a potential approach to the treatment of atrial fibrillation. A diverse set of heterocycles were identified as potent Kv1.5 inhibitors and were advanced to pharmacodynamic evaluation based on selectivity and pharmacokinetic profile. Heterocycle optimization and template modification lead to the identification of compound 24 which demonstrated increased atrial effective refractory period in the rabbit pharmacodynamic model with mild effects on blood pressure and heart rate., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

12. Discovery of 3-hydroxy-4-cyano-isoquinolines as novel, potent, and selective inhibitors of human 11β-hydroxydehydrogenase 1 (11β-HSD1).

Author

Wu SC, Yoon D, Chin J, van Kirk K, Seethala R, Golla R, He B, Harrity T, Kunselman LK, Morgan NN, Ponticiello RP, Taylor JR, Zebo R, Harper TW, Li W, Wang M, Zhang L, Sleczka BG, Nayeem A, Sheriff S, Camac DM, Morin PE, Everlof JG, Li YX, Ferraro CA, Kieltyka K, Shou W, Vath MB, Zvyaga TA, Gordon DA, and Robl JA

Subjects

Animals, Cell Line, Diabetes Mellitus, Type 2 drug therapy, Enzyme Inhibitors pharmacokinetics, Humans, Isoquinolines pharmacokinetics, Mice, Mice, Inbred BALB C, Structure-Activity Relationship, 11-beta-Hydroxysteroid Dehydrogenase Type 1 antagonists & inhibitors, 11-beta-Hydroxysteroid Dehydrogenase Type 1 metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Isoquinolines chemistry, Isoquinolines pharmacology

Abstract

Derived from the HTS hit 1, a series of hydroxyisoquinolines was discovered as potent and selective 11β-HSD1 inhibitors with good cross species activity. Optimization of substituents at the 1 and 4 positions of the isoquinoline group in addition to the core modifications, with a special focus on enhancing metabolic stability and aqueous solubility, resulted in the identification of several compounds as potent advanced leads., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

13. 1-Aminobenzotriazole, a known cytochrome P450 inhibitor, is a substrate and inhibitor of N-acetyltransferase.

Author

Sun Q, Harper TW, Dierks EA, Zhang L, Chang S, Rodrigues AD, and Marathe P

Subjects

Acetaminophen metabolism, Acetylation drug effects, Animals, Arylamine N-Acetyltransferase antagonists & inhibitors, Arylamine N-Acetyltransferase metabolism, Glucuronosyltransferase metabolism, Humans, Isoenzymes antagonists & inhibitors, Isoenzymes metabolism, Male, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Procainamide metabolism, Rats, Rats, Sprague-Dawley, Sulfotransferases metabolism, Umbelliferones metabolism, Cytochrome P-450 Enzyme Inhibitors, Cytochrome P-450 Enzyme System metabolism, Triazoles metabolism, Triazoles pharmacology

Abstract

1-Aminobenzotriazole (ABT) has been used widely as a nonselective in vitro and in vivo inhibitor of cytochrome P450 enzymes. To date, however, it has not been evaluated as an inhibitor of UDP-glucuronosyltransferase (UGT), sulfotransferase (SULT), and N-acetyltransferase (NAT). In the present study, ABT was shown not to inhibit UGT and SULT activity (acetaminophen and 7-hydroxycoumarin as substrates) in rat liver microsomes and rat liver 9000 g supernatant fraction (RLS9), respectively. However, it did inhibit the RLS9-catalyzed N-acetylation of procainamide (IC(50) ∼ 30 μM), and no preincubation time dependence was evident. In agreement, oral ABT (100 mg/kg, 2 h predose) decreased the clearance of intravenous procainamide (45%) in rats, accompanied by a decreased N-acetylprocainamide-to-procainamide ratio in urine (0.74 versus 0.21) and plasma (area under the curve ratio 0.59 versus 0.11). Additional studies with human forms of NAT (hNAT1 and hNAT2) revealed that ABT is a more potent inhibitor of hNAT2 compared with hNAT1 (IC(50) 158 μM versus > 1 mM). Consistent with the IC(50) estimate, formal inhibition studies revealed that inhibition of hNAT2 was competitive with an inhibition constant of 67 μM. In accordance with the competitive inhibition, ABT was shown to undergo N-acetylation in the presence of both human NAT forms, with hNAT1 exhibiting less activity under the same assay conditions (∼40% of hNAT2). In summary, the results described herein indicate that ABT is a substrate and inhibitor of NAT. Such an interaction should be considered when using ABT as a nonselective inhibitor of P450, especially when NAT-dependent metabolism is also involved.

Published

2011

14. Pyrazole-based sulfonamide and sulfamides as potent inhibitors of mammalian 15-lipoxygenase.

Author

Ngu K, Weinstein DS, Liu W, Langevine C, Combs DW, Zhuang S, Chen X, Madsen CS, Harper TW, Ahmad S, and Robl JA

Subjects

Amides chemical synthesis, Amides pharmacology, Animals, Arachidonate 15-Lipoxygenase metabolism, CHO Cells, Cricetinae, Cricetulus, Humans, Hydroxyeicosatetraenoic Acids blood, Lipoxygenase Inhibitors chemical synthesis, Lipoxygenase Inhibitors pharmacology, Rabbits, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Sulfonamides pharmacology, Amides chemistry, Arachidonate 15-Lipoxygenase chemistry, Lipoxygenase Inhibitors chemistry, Pyrazoles chemistry

Abstract

A series of inhibitors of mammalian 15-lipoxygenase (15-LO) based on a 3,4,5-tri-substituted pyrazole scaffold is described. Replacement of a sulfonamide functionality in the lead series with a sulfamide group resulted in improved physicochemical properties generating analogs with enhanced inhibition in cell-based and whole blood assays., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

15. In silico prediction of biliary excretion of drugs in rats based on physicochemical properties.

Author

Luo G, Johnson S, Hsueh MM, Zheng J, Cai H, Xin B, Chong S, He K, and Harper TW

Subjects

Animals, Bile chemistry, Bile Ducts, Carboxylic Acids analysis, Carboxylic Acids chemistry, Carboxylic Acids pharmacokinetics, Catheters, Indwelling, Chemical Phenomena, Computational Biology, Drugs, Investigational analysis, Least-Squares Analysis, Male, Models, Biological, Rats, Rats, Sprague-Dawley, Solubility, Surface Properties, Bile metabolism, Drugs, Investigational chemistry, Drugs, Investigational pharmacokinetics, Expert Systems

Abstract

Evaluating biliary excretion, a major elimination pathway for many compounds, is important in drug discovery. The bile duct-cannulated (BDC) rat model is commonly used to determine the percentage of dose excreted as intact parent into bile. However, a study using BDC rats is time-consuming and cost-ineffective. The present report describes a computational model that has been established to predict biliary excretion of intact parent in rats as a percentage of dose. The model was based on biliary excretion data of 50 Bristol-Myers Squibb Co. compounds with diverse chemical structures. The compounds were given intravenously at <10 mg/kg to BDC rats, and bile was collected for at least 8 h after dosing. Recoveries of intact parents in bile were determined by liquid chromatography with tandem mass spectrometry. Biliary excretion was found to have a fairly good correlation with polar surface area (r = 0.76) and with free energy of aqueous solvation (DeltaG(solv aq)) (r = -0.67). In addition, biliary excretion was also highly corrected with the presence of a carboxylic acid moiety in the test compounds (r = 0.87). An equation to calculate biliary excretion in rats was then established based on physiochemical properties via a multiple linear regression. This model successfully predicted rat biliary excretion for 50 BMS compounds (r = 0.94) and for 25 previously reported compounds (r = 0.86) whose structures are markedly different from those of the 50 BMS compounds. Additional calculations were conducted to verify the reliability of this computation model.

Published

2010

16. Polymerase chain reaction analysis of aqueous and vitreous specimens in the diagnosis of posterior segment infectious uveitis.

Author

Harper TW, Miller D, Schiffman JC, and Davis JL

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Chorioretinitis diagnosis, Chorioretinitis parasitology, Chorioretinitis virology, DNA, Protozoan analysis, DNA, Viral analysis, Eye Infections parasitology, Eye Infections virology, False Positive Reactions, Female, Humans, Infant, Male, Middle Aged, Predictive Value of Tests, Retrospective Studies, Sensitivity and Specificity, Uveitis, Posterior parasitology, Uveitis, Posterior virology, Aqueous Humor parasitology, Aqueous Humor virology, Diagnostic Techniques, Ophthalmological, Eye Infections diagnosis, Polymerase Chain Reaction methods, Uveitis, Posterior diagnosis, Vitreous Body parasitology, Vitreous Body virology

Abstract

Purpose: To assess polymerase chain reaction (PCR) analysis of intraocular fluid as a test for infectious uveitis of the posterior segment in a representative patient population., Design: Retrospective, interventional case series., Methods: One hundred and thirty-three patients with possible infectious chorioretinitis underwent PCR testing of aqueous or vitreous in a university setting. Baseline characteristics predictive of test positivity were identified. Positive and negative predictive values were calculated., Results: Four hundred and thirty-three PCR tests of 105 aqueous and 38 vitreous specimens (mean, 3.3 tests per patient) identified 77 of the 95 patients with a final clinical diagnosis of infectious uveitis (81%). Herpes simplex virus, varicella zoster virus, and cytomegalovirus PCR analysis were performed in almost all cases, with fewer tests for toxoplasmosis or Epstein-Barr virus. Clinical features associated with positive PCR results were retinal vascular inflammation (P < .001), optic nerve involvement (P = .008), immunocompromised state (P = .039), and extensive retinitis (P = .002). Cases sampled within one week of presentation were more likely to have positive PCR results than those sampled later (P = .071). The predictive value of positive and negative tests was 98.7% and 67.9%, respectively, in this patient group. Alteration in treatment based on PCR and syphilis serologic results led to resolution in 25 of 26 patients after treatment was changed., Conclusions: PCR testing is a useful adjunct in the diagnosis of infectious causes of posterior uveitis. Cases with vascular or optic nerve inflammation, extensive retinitis, or immunocompromise are more likely to have positive PCR results and may benefit from PCR testing of aqueous humor.

Published

2009

17. Lack of toxicity during long-term follow-up of intraocular metallic fragments after pars plana vitrectomy.

Author

Harper TW, Flynn HW Jr, Berrocal A, Thompson JT, and Parel JM

Subjects

Electroretinography, Eye Foreign Bodies physiopathology, Female, Fluorescein Angiography, Follow-Up Studies, Humans, Iatrogenic Disease, Lens Implantation, Intraocular, Middle Aged, Phacoemulsification, Photography, Retina diagnostic imaging, Tomography, Optical Coherence, Ultrasonography, Visual Acuity, Vitrectomy instrumentation, Eye Foreign Bodies diagnosis, Retina pathology, Stainless Steel, Vitrectomy adverse effects, Vitreous Hemorrhage surgery

Abstract

A 45-year-old woman underwent pars plana vitrectomy for vitreous hemorrhage in the right eye 20 years prior to presentation. She also had prior phacoemulsification and intraocular lens implantation and subsequent laser capsulotomy in the right eye. Multiple preretinal metallic fragments were visible on the retinal surface and were presumed to be stainless steel fragments from the vitrectomy instrument. The fragments were documented by color photography, fluorescein angiography, optical coherence tomography, and echography. Visual acuity was 20/30, electrophysiologic testing was normal, and no signs of toxicity were present. No surgical intervention was planned.

Published

2008

18. Optimization of 1H-tetrazole-1-alkanenitriles as potent orally bioavailable growth hormone secretagogues.

Author

Hernández AS, Swartz SG, Slusarchyk D, Yan M, Seethala RK, Sleph P, Grover G, Dickinson K, Giupponi L, Harper TW, Humphreys WG, Longhi DA, Flynn N, Murphy BJ, Gordon DA, Biller SA, Robl JA, and Tino JA

Subjects

Administration, Oral, Animals, Biological Availability, Cytochrome P-450 Enzyme System metabolism, Dogs, Magnetic Resonance Spectroscopy, Molecular Structure, Nitriles chemical synthesis, Nitriles pharmacokinetics, Pituitary Gland, Rats, Structure-Activity Relationship, Tetrazoles chemical synthesis, Tetrazoles pharmacokinetics, Growth Hormone metabolism, Nitriles pharmacology, Tetrazoles pharmacology

Abstract

1H-tetrazole-1-alkanenitrile SR-9g exhibits a >10-fold in vivo potency enhancement over the lead nitrile 1 and has acceptable oral bioavailability in rats and dogs. An enantiospecific synthesis of 1H-tetrazole-1-alkanenitrile nitriles 9 has been developed.

Published

2008

19. Reaction phenotyping: current industry efforts to identify enzymes responsible for metabolizing drug candidates.

Author

Harper TW and Brassil PJ

Subjects

Animals, Cytochrome P-450 Enzyme System genetics, Drug Industry trends, Humans, Cytochrome P-450 Enzyme System metabolism, Drug Industry methods, Pharmaceutical Preparations metabolism, Phenotype

Abstract

Reaction phenotyping studies to identify specific enzymes involved in the metabolism of drug candidates are increasingly important in drug discovery efforts. Experimental approaches used for CYP reaction phenotyping include incubations with cDNA expressed CYP enzyme systems and incubations containing specific CYP enzyme inhibitors. Since both types of experiments present specific advantages as well as known drawbacks, these studies are generally viewed as complementary approaches. Although glucuronidation pathways are also known to present potential drug-drug interaction issues as well as challenges related to their polymorphic expression, reaction phenotyping approaches for glucuronidation are generally limited to cDNA expressed systems due to lack of availability of specific UGT inhibitors. This article presents a limited review of current approaches to reaction phenotyping studies used within the pharmaceutical industry.

Published

2008

20. Discovery of selective imidazole-based inhibitors of mammalian 15-lipoxygenase: highly potent against human enzyme within a cellular environment.

Author

Weinstein DS, Liu W, Ngu K, Langevine C, Combs DW, Zhuang S, Chen C, Madsen CS, Harper TW, and Robl JA

Subjects

Animals, CHO Cells, Cricetinae, Cricetulus, Humans, Imidazoles chemistry, Male, Rats, Rats, Sprague-Dawley, Imidazoles pharmacology, Lipoxygenase Inhibitors chemistry, Lipoxygenase Inhibitors pharmacology

Abstract

A series of 2,4,5-tri-substituted imidazoles has proven to be highly potent in inhibiting mammalian 15-lipoxygenase (15-LO) with excellent selectivity over human isozymes 5- and P-12-LO. Non-symmetrical sulfamides (e.g., 21a-n) were found to be suitable replacements for the earlier arylsulfonamide-containing members of this series (e.g., 2, 14a-p). Several members of these series also demonstrated potent inhibition of human 15-LO in a cell-based assay.

Published

2007

21. Arylpropanolamines: selective beta3 agonists arising from strategies to mitigate phase I metabolic transformations.

Author

Washburn WN, Harper TW, Wu G, Godfrey JD, McCann P, Girotra R, Shao C, Zhang H, Gavai A, Mikkilineni A, Dejneka T, Ahmed S, Caringal Y, Hangeland J, Zhang M, Cheng PT, Russell AD, Skwish S, Slusarchyk DA, Allen GT, Frohlich BH, Abboa-Offei BE, Cap M, Waldron TL, George RJ, Tesfamariam B, Dickinson KE, Seymour AA, and Sher PM

Subjects

Adrenergic beta-Agonists chemistry, Alkylation, Oxidation-Reduction, Propanolamines chemistry, Structure-Activity Relationship, Adrenergic beta-3 Receptor Agonists, Adrenergic beta-Agonists pharmacology, Propanolamines pharmacology

Abstract

Utilization of N-substituted-4-hydroxy-3-methylsulfonanilidoethanolamines 1 as selective beta(3) agonists is complicated by their propensity to undergo metabolic oxidative N-dealkylation, generating 0.01-2% of a very potent alpha(1) adrenergic agonist 2. A summary of the SAR for this hepatic microsomal conversion precedes presentation of strategies to maintain the advantages of chemotype 1 while mitigating the consequences of N-dealkylation. This effort led to the identification of 4-hydroxy-3-methylsulfonanilidopropanolamines 15 for which the SAR for the unique stereochemical requirements for binding to the beta adrenergic receptors culminated in the identification of the potent, selective beta(3) agonist 15f.

Published

2007

22. Multiple pathways are involved in the oral absorption of BMS-262084, a tryptase inhibitor, in rats: role of paracellular transport, binding to trypsin, and P-glycoprotein efflux.

Author

Kamath AV, Morrison RA, Harper TW, Lan SJ, Marino AM, and Chong S

Subjects

Administration, Oral, Animals, Azetidines administration & dosage, Azetidines pharmacology, Biological Availability, Caco-2 Cells, Dipeptides metabolism, Dose-Response Relationship, Drug, Humans, Hypoglycemic Agents, Injections, Intra-Arterial, Insulin, Intestinal Absorption, Piperazines administration & dosage, Piperazines pharmacology, Protein Binding, Rats, Rats, Sprague-Dawley, Serine Endopeptidases metabolism, Serine Proteinase Inhibitors administration & dosage, Serine Proteinase Inhibitors pharmacology, Tight Junctions drug effects, Tryptases, ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Azetidines pharmacokinetics, Piperazines pharmacokinetics, Serine Proteinase Inhibitors pharmacokinetics, Trypsin metabolism

Abstract

BMS-262084 is a potent and selective beta-lactam tryptase inhibitor with therapeutic potential for treating asthma. The oral bioavailability of BMS-262084 was low in rats (4% at a dose of 0.5 mg/kg) due to poor absorption. BMS-262084 was excreted mainly unchanged in the urine, suggesting minimal metabolism in rats. The objective of this study was to investigate the mechanisms of oral absorption of BMS-262084 in rats. Modulation of intestinal tight junctions, binding to trypsin, and involvement of the intestinal dipeptide transport system and P-glycoprotein (P-gp) in the absorption of BMS-262084 were examined. Coadministration of BMS-262084 with SQ-29852, a substrate of the intestinal dipeptide transport system, did not change the oral absorption of BMS-262084. An increase in the dose of BMS-262084 from 0.5 to 50 mg/kg resulted in a 3.7-fold increase in its oral absorption. Inulin absorption was enhanced upon coadministration with BMS-262084, suggesting the opening of tight junctions in the intestinal epithelium. Coadministration of aprotinin, a trypsin inhibitor, increased the oral absorption of BMS-262084 several fold. In vitro, using Caco-2 cells, BMS-262084 appeared to be a P-gp substrate, with an efflux ratio of 14. These results suggest that absorption of BMS-262084 is mediated by several concurrent mechanisms. At higher doses of BMS-262084, increased absorption may be primarily due to opening of tight junctions in the intestinal epithelium and consequent absorption via the paracellular pathway, while at lower doses, binding to trypsin may contribute to limiting its absorption. P-gp efflux may also play a role in influencing the absorption of BMS-262084. The intestinal dipeptide transporter system does not appear to be involved in the absorption of BMS-262084.

Published

2005

23. Dansyl glutathione as a trapping agent for the quantitative estimation and identification of reactive metabolites.

Author

Gan J, Harper TW, Hsueh MM, Qu Q, and Humphreys WG

Subjects

Biotransformation, Chromatography, High Pressure Liquid, Cyclohexane Monoterpenes, Dinitrochlorobenzene pharmacology, Fluorescence, Glutathione Disulfide metabolism, Humans, Liver enzymology, Mass Spectrometry, Monoterpenes pharmacology, Oxidation-Reduction, Spectrometry, Fluorescence, Sulfhydryl Compounds chemistry, Sulfhydryl Compounds metabolism, Dansyl Compounds chemistry, Glutathione metabolism, Glutathione Transferase metabolism, Liver metabolism

Abstract

A sensitive and quantitative method was developed for the estimation of reactive metabolite formation in vitro. The method utilizes reduced glutathione (GSH) labeled with a fluorescence tag as a trapping agent and fluorescent detection for quantitation. The derivatization of GSH was accomplished by reaction of oxidized glutathione (GSSG) with dansyl chloride to form dansylated GSSG. Subsequent reduction of the disulfide bond yielded dansylated GSH (dGSH). Test compounds were incubated with human liver microsomes in the presence of dGSH and NADPH, and the resulting mixtures were analyzed by HPLC coupled with a fluorescence detector and a mass spectrometer for the quantitation and mass determination of the resulting dGSH adducts. The comparative chemical reactivity of dGSH vs GSH was investigated by monitoring the reaction of each with 1-chloro-2,4-dinitrobenzene or R-(+)-pulegone after bioactivation. dGSH was found to be equivalent to GSH in chemical reactivity toward both thiol reactive molecules. dGSH did not serve as a cofactor for glutathione S-transferase (GST)-mediated conjugation of 3,4-dichloronitrobenzene in incubations with either human liver S9 fractions or a recombinant GST, GSTM1-1. Reference compounds were tested in this assay, including seven compounds that have been reported to form GSH adducts along with seven drugs that are among the most prescribed in the current U.S. market and have not been reported to form GSH adducts. dGSH adducts were detected and quantitated in incubations with all seven positive reference compounds; however, there were no dGSH adducts observed with any of the widely prescribed drugs. In comparison with existing methods, this method is sensitive, quantitative, cost effective, and easy to implement.

Published

2005

24. BMS-201620: a selective beta 3 agonist.

Author

Washburn WN, Sun CQ, Bisacchi G, Wu G, Cheng PT, Sher PM, Ryono D, Gavai AV, Poss K, Girotra RN, McCann PJ, Mikkilineni AB, Dejneka TC, Wang TC, Merchant Z, Morella M, Arbeeny CM, Harper TW, Slusarchyk DA, Skwish S, Russell AD, Allen GT, Tesfamariam B, Frohlich BH, Abboa-Offei BE, Cap M, Waldron TL, George RJ, Young D, Dickinson KE, and Seymour AA

Subjects

Adrenergic beta-Agonists chemical synthesis, Animals, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Glycine chemical synthesis, Glycine chemistry, Haplorhini, Humans, Methylation, Receptors, Adrenergic, beta-3 metabolism, Stereoisomerism, Structure-Activity Relationship, Adrenergic beta-3 Receptor Agonists, Adrenergic beta-Agonists pharmacology, Glycine analogs & derivatives, Glycine pharmacology

Abstract

A series of N-(4-hydroxy-3-methylsulfonanilidoethanol)arylglycinamides were prepared and evaluated for their human beta3 adrenergic receptor agonist activity. SAR studies led to the identification of BMS-201620 (39), a potent beta3 full agonist (Ki = 93 nM, 93% activation). Based on its favorable safety profile, BMS-201620 was chosen for clinical evaluation.

Published

2004

25. Shift in pH of biological fluids during storage and processing: effect on bioanalysis.

Author

Fura A, Harper TW, Zhang H, Fung L, and Shyu WC

Subjects

Animals, Buffers, Chromatography, High Pressure Liquid, Digestive System chemistry, Hydrogen-Ion Concentration, Indicators and Reagents, Lung chemistry, Mass Spectrometry, Methanol chemistry, Rats, Reference Standards, Solvents, Time Factors, Bile chemistry, Body Fluids chemistry, Specimen Handling, Urine chemistry

Abstract

The pH of ex vivo plasma, bile and urine was monitored at different times and temperatures of storage, and following different sample processing methods such as ultrafiltration, centrifugation, precipitation and evaporation. The results showed that the pH of ex vivo plasma, bile and urine increased upon storage, and following sample processing and could lead to significant degradation of pH-labile compounds. Several compounds were used to illustrate the impact of pH shifts on drug stability and interpretation of results obtained from in vivo studies. For example, after 1 h of incubation (37 degrees C) in rat plasma (pH 8.3), about 60%, of I was lost. However, in phosphate buffer, losses were about 12% at pH 7.4 and 40% at pH 8.0. Plasma pH also increased during ultrafiltration, centrifugation and extraction. After methanol precipitation of plasma proteins, and evaporation of the supernatant and redissolution of the residue, the resulting solution had a pH of 9.5. Under these conditions, II was degraded by 60% but was stable when phosphate buffer was used to maintain the pH at 7.4. The shift in plasma pH can yield misleading results from in vivo studies if the pH is not controlled. For example, the major circulating metabolite of II was also formed in plasma ex-vivo. This ex vivo degradation was prevented when blood samples were collected into tubes containing 0.1 volume of phosphate buffer (0.3 M, pH 5). The pH of ex vivo plasma can best be stabilized at physiological conditions using 10% CO2 atmosphere in a CO2 incubator. Changes in pH of ex vivo urine and bile samples can have similar adverse effect on pH-labile samples. Thus, processing of plasma samples under a 10% CO2 atmosphere is a method of choice for stability or protein binding studies in plasma, whereas citrate or phosphate buffers are suitable for stabilizing pH in bile and urine and for plasma samples requiring extensive preparations or long term storage.

Published

2003

26. Discovery of N-[2-[2-[[3-methoxy-4-(5-oxazolyl)phenyl]amino]-5-oxazolyl]phenyl]-N-methyl-4- morpholineacetamide as a novel and potent inhibitor of inosine monophosphate dehydrogenase with excellent in vivo activity.

Author

Dhar TG, Shen Z, Guo J, Liu C, Watterson SH, Gu HH, Pitts WJ, Fleener CA, Rouleau KA, Sherbina NZ, McIntyre KW, Shuster DJ, Witmer MR, Tredup JA, Chen BC, Zhao R, Bednarz MS, Cheney DL, MacMaster JF, Miller LM, Berry KK, Harper TW, Barrish JC, Hollenbaugh DL, and Iwanowicz EJ

Subjects

Animals, Antibody Formation drug effects, Arthritis, Experimental drug therapy, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme-Linked Immunosorbent Assay, Male, Mice, Mice, Inbred BALB C, Morpholines chemistry, Morpholines pharmacology, Mycophenolic Acid pharmacology, Oxazoles chemistry, Oxazoles pharmacology, Rats, Rats, Inbred Lew, Structure-Activity Relationship, Enzyme Inhibitors chemical synthesis, IMP Dehydrogenase antagonists & inhibitors, Morpholines chemical synthesis, Mycophenolic Acid analogs & derivatives, Oxazoles chemical synthesis

Abstract

Inosine monophosphate dehydrogenase (IMPDH) is a key enzyme that is involved in the de novo synthesis of purine nucleotides. Novel 2-aminooxazoles were synthesized and tested for inhibition of IMPDH catalytic activity. Multiple analogues based on this chemotype were found to inhibit IMPDH with low nanomolar potency. One of the analogues (compound 23) showed excellent in vivo activity in the inhibition of antibody production in mice and in the adjuvant induced arthritis model in rats.

Published

2002

27. Beta 3 agonists. Part 1: evolution from inception to BMS-194449.

Author

Washburn WN, Sher PM, Poss KM, Girotra RN, McCann PJ, Gavai AV, Mikkilineni AB, Mathur A, Cheng P, Dejneka TC, Sun CQ, Wang TC, Harper TW, Russell AD, Slusarchyk DA, Skwish S, Allen GT, Hillyer DE, Frohlich BH, Abboa-Offei BE, Cap M, Waldron TL, George RJ, Tesfamariam B, Ciosek CP Jr, Ryono D, Young DA, Dickinson KE, Seymour AA, Arbeeny CM, and Gregg RE

Subjects

Administration, Oral, Animals, Biological Availability, Chlorocebus aethiops, Drug Evaluation, Preclinical, Ethanolamines, Humans, Rats, Structure-Activity Relationship, Adrenergic beta-3 Receptor Agonists, Adrenergic beta-Agonists chemistry, Adrenergic beta-Agonists pharmacology, Anilides chemistry, Anilides pharmacology, Ethanolamine chemistry, Ethanolamine pharmacology

Abstract

Screening of the BMS collection identified 4-hydroxy-3-methylsulfonanilidoethanolamines as full beta 3 agonists. Substitution of the ethanolamine nitrogen with a benzyl group bearing a para hydrogen bond acceptor promoted beta(3) selectivity. SAR elucidation established that highly selective beta(3) agonists were generated upon substitution of C(alpha) with either benzyl to form (R)-1,2-diarylethylamines or with aryl to generate 1,1-diarylmethylamines. This latter subset yielded a clinical candidate, BMS-194449 (35).(1)

Published

2001

28. BMS-196085: a potent and selective full agonist of the human beta(3) adrenergic receptor.

Author

Gavai AV, Sher PM, Mikkilineni AB, Poss KM, McCann PJ, Girotra RN, Fisher LG, Wu G, Bednarz MS, Mathur A, Wang TC, Sun CQ, Slusarchyk DA, Skwish S, Allen GT, Hillyer DE, Frohlich BH, Abboa-Offei BE, Cap M, Waldron TL, George RJ, Tesfamariam B, Harper TW, Ciosek CP Jr, Young DA, Dickinson KE, Seymour AA, Arbeeny CM, and Washburn WN

Subjects

Administration, Oral, Adrenergic beta-1 Receptor Agonists, Animals, Blood Glucose metabolism, Chlorocebus aethiops, Drug Evaluation, Preclinical, Fatty Acids blood, Humans, Mice, Mice, Obese, Receptors, Adrenergic, beta-1 metabolism, Receptors, Adrenergic, beta-3 metabolism, Structure-Activity Relationship, Adrenergic Agonists chemistry, Adrenergic Agonists pharmacology, Adrenergic beta-3 Receptor Agonists, Anilides chemistry, Anilides pharmacology

Abstract

A series of 4-hydroxy-3-methylsulfonanilido-1,2-diarylethylamines were prepared and evaluated for their human beta(3) adrenergic receptor agonist activity. SAR studies led to the identification of BMS-196085 (25), a potent beta(3) full agonist (K(i)=21 nM, 95% activation) with partial agonist (45%) activity at the beta(1) receptor. Based on its desirable in vitro and in vivo properties, BMS-196085 was chosen for clinical evaluation.

Published

2001

29. Design and synthesis of 4-substituted benzamides as potent, selective, and orally bioavailable I(Ks) blockers.

Author

Lloyd J, Schmidt JB, Rovnyak G, Ahmad S, Atwal KS, Bisaha SN, Doweyko LM, Stein PD, Traeger SC, Mathur A, Conder ML, DiMarco J, Harper TW, Jenkins-West T, Levesque PC, Normandin DE, Russell AD, Serafino RP, Smith MA, and Lodge NJ

Subjects

Administration, Oral, Animals, Benzamides chemistry, Benzamides pharmacology, Biological Availability, Chromatography, High Pressure Liquid, Crystallography, X-Ray, Drug Design, In Vitro Techniques, KCNQ Potassium Channels, KCNQ1 Potassium Channel, Oocytes metabolism, Oocytes physiology, Oxadiazoles chemistry, Oxadiazoles pharmacology, Patch-Clamp Techniques, Potassium Channels metabolism, Rats, Stereoisomerism, Structure-Activity Relationship, Xenopus, Benzamides chemical synthesis, Oxadiazoles chemical synthesis, Potassium Channel Blockers chemical synthesis, Potassium Channel Blockers chemistry, Potassium Channel Blockers pharmacology, Potassium Channels, Voltage-Gated

Abstract

Multiple delayed rectifier potassium currents, including I(Ks), are responsible for the repolarization and termination of the cardiac action potential, and blockers of these currents may be useful as antiarrhythmic agents. Modification of compound 5 produced 19(S) that is the most potent I(Ks) blocker reported to date with >5000-fold selectivity over other cardiac ion channels. Further modification produced 24A with 23% oral bioavailability.

Published

2001

30. Cardioselective anti-ischemic ATP-sensitive potassium channel openers.

Author

Atwal KS, Grover GJ, Ahmed SZ, Ferrara FN, Harper TW, Kim KS, Sleph PG, Dzwonczyk S, Russell AD, and Moreland S

Subjects

Animals, Aorta drug effects, Aorta physiology, Benzopyrans pharmacokinetics, Benzopyrans pharmacology, Benzopyrans therapeutic use, Biological Availability, Cocaine chemical synthesis, Cocaine metabolism, Cocaine pharmacology, Cromakalim, Guanidines pharmacokinetics, Guanidines therapeutic use, Molecular Structure, Potassium Channels drug effects, Pyrroles pharmacology, Rats, Structure-Activity Relationship, Vasodilation drug effects, Adenosine Triphosphate pharmacology, Benzopyrans chemistry, Cocaine analogs & derivatives, Guanidines chemistry, Ion Channel Gating drug effects, Myocardial Ischemia drug therapy, Potassium Channels physiology

Published

1993

31. Isolation and identification of lysophosphatidylcholines as endogenous modulators of thromboxane receptors.

Author

Phillipson DW, Tymiak AA, Tuttle JG, Hartl KS, Harper TW, Bolgar MS, Allen GT, and Ogletree ML

Subjects

Animals, Aorta, Thoracic drug effects, Aorta, Thoracic metabolism, Carbon Radioisotopes, Chromatography, High Pressure Liquid, Esters blood, Esters pharmacology, Fatty Acids blood, Fatty Acids pharmacology, Fatty Acids physiology, Humans, In Vitro Techniques, Lysophosphatidylcholines pharmacology, Magnetic Resonance Spectroscopy methods, Male, Muscle, Smooth, Vascular drug effects, Muscle, Smooth, Vascular metabolism, Protons, Radioligand Assay, Rats, Rats, Sprague-Dawley, Spectrometry, Mass, Fast Atom Bombardment, Lysophosphatidylcholines blood, Receptors, Thromboxane antagonists & inhibitors, Receptors, Thromboxane physiology

Abstract

Inhibition of thromboxane receptor radioligand binding to human platelet membranes has been employed as the basis for a radioreceptor assay designed to measure thromboxane receptor binding activity in samples of biological fluids. This method was used during phase 1 clinical evaluation of the thromboxane receptor antagonist SQ 30,741. Frequently, baseline plasma samples as well as plasma samples from placebo-treated subjects showed significant inhibition of radioligand binding in the radioreceptor assay, suggesting the presence of endogenous thromboxane receptor ligands. This receptor binding activity was stable and could be monitored in blood from normal volunteers using a modification of the radioreceptor assay. In order to identify the substance responsible for the observed activity, the activity present in pooled bovine blood was isolated and evaluated by a combination of FAB/MS, 1H-NMR, 13C-NMR and co-injection with reference standards on HPLC. Several endogenous thromboxane receptor ligands were identified as L-alpha-lysophosphatidylcholine (LPC) species. One major species, palmitoyl-LPC, contracted isolated rat aortic spirals, and these contractions could be delayed or prevented, but not reversed by the thromboxane receptor antagonist SQ 29,548. Palmitoyl-LPC slightly potentiated aortic contractions induced by the thromboxane receptor agonist, U-46,619, and diminished in a concentration-dependent manner the antagonism by SQ 29,548 of contractile responses to U-46,619. These findings are consistent with a potential for LPC species to bind and activate thromboxane receptors.

Published

1993

32. Metabolism of leukotrienes B4 and C4 in the isolated perfused rat lung.

Author

Harper TW, Westcott JY, Voelkel N, and Murphy RC

Subjects

Animals, Chromatography, High Pressure Liquid, In Vitro Techniques, Kinetics, Male, Perfusion, Pulmonary Artery, Rats, Rats, Inbred Strains, Tritium, Leukotriene B4 metabolism, Lung metabolism, SRS-A metabolism

Abstract

Isolated rat lungs perfused with physiological buffer containing leukotriene C4 were found to rapidly metabolize leukotriene C4 to leukotriene C4 sulfoxide, leukotriene D4, and leukotriene E4. Addition of leukotriene C4 to the recirculating perfusion buffer was observed to cause a persistent increase in the pulmonary arterial pressure. Leukotriene C4 instilled into the airway of the perfused lung was also rapidly metabolized to these same products with retention of the products within the lung. In contrast, leukotriene B4 injected into the perfusion fluid was recovered unchanged in the lung effluent. Leukotriene B4 instilled into the airway of the perfused lung was observed to rapidly traverse the alveolar membranes and was recovered intact in the lung effluent. No evidence for formation of the 20-hydroxy or the 20-carboxy metabolites of leukotriene B4 by the isolated perfused rat lung was observed.

Published

1984

33. Rapid extraction of leukotrienes from biologic fluids and quantitation by high-performance liquid chromatography.

Author

Metz SA, Hall ME, Harper TW, and Murphy RC

Subjects

Chromatography, High Pressure Liquid, Humans, Body Fluids analysis, Leukotriene B4 isolation & purification

Published

1983

34. Identification and functional characterization of leukotriene B4 20-hydroxylase of human polymorphonuclear leukocytes.

Author

Soberman RJ, Harper TW, Murphy RC, and Austen KF

Subjects

Cytochrome P-450 Enzyme System blood, Cytochrome P450 Family 4, Cytosol enzymology, Humans, Kinetics, Leukotriene B4, Mixed Function Oxygenases blood, Neutrophils enzymology

Abstract

A single reaction product was formed during the incubation of 1.5 microM (5S,12R)-dihydroxy-6,14-cis-8,10-trans-[3H]icosatetraenoic acid (leukotriene B4, LTB4) for 30 min at 37 degrees C in 10 mM potassium phosphate buffer (pH 7.5) with 100 microM NADPH and the 150,000 X g supernatant of sonicated human polymorphonuclear leukocytes (PMN). The reaction product exhibited the same mobility on reversed-phase HPLC (RP-HPLC) and TLC as standard 20-hydroxy-LTB4 (20-OH-LTB4). When the omega-oxidation product of [3H]LTB4 was eluted from a Sep-Pak, resolved by RP-HPLC, and analyzed by GC/MS, its structure was determined to be solely 20-OH-LTB4. The Km of the 20-hydroxylase for [3H]LTB4 at its optimal pH of 7.5 was 0.22 +/- 0.08 microM (mean +/- SD, n = 4) and the Vmax was 48 +/- 11 pmol/min X mg of protein (mean +/- SD, n = 4). When the concentration of [3H]LTB4 was fixed at 1.5 microM, the Km for NADPH was 1.01 +/- 0.59 microM (mean +/- SD, n = 3). The location in the 150,000 X g supernatant of the LTB4 20-hydroxylase distinguishes it from the cytochrome P-450 system of liver, lung, and kidney microsomes and from the NADPH oxidase-cytochrome b-245 system of the human PMN. The LTB4 20-hydroxylase is either a unique cytochrome P-450 or other monooxygenase.

Published

1985

35. Characterization and separation of the arachidonic acid 5-lipoxygenase and linoleic acid omega-6 lipoxygenase (arachidonic acid 15-lipoxygenase) of human polymorphonuclear leukocytes.

Author

Soberman RJ, Harper TW, Betteridge D, Lewis RA, and Austen KF

Subjects

12-Hydroxy-5,8,10,14-eicosatetraenoic Acid, Arachidonate Lipoxygenases, Calcium metabolism, Chromatography, Ion Exchange, Humans, Hydrogen-Ion Concentration, Hydroxyeicosatetraenoic Acids metabolism, Isoenzymes metabolism, Kinetics, Structure-Activity Relationship, Substrate Specificity, Lipoxygenase blood, Neutrophils enzymology

Abstract

The cytosolic fraction of human polymorphonuclear leukocytes precipitated with 60% ammonium sulfate produced 5-lipoxygenase products from [14C]arachidonic acid and omega-6 lipoxygenase products from both [14C]linoleic acid and, to a lesser extent, [14C]- and [3H]arachidonic acid. The arachidonyl 5-lipoxygenase products 5-hydroperoxy-6,8,11,14-eicosatetraenoic acid (5-HPETE) and 5-hydroxy-6,8,11,14-eicosatetraenoic acid (5-HETE) derived from [14C]arachidonic acid, and the omega-6 lipoxygenase products 13-hydroperoxy-9,11-octadecadienoic acid (13-OOH linoleic acid) and 13-hydroxy-9,11-octadecadienoic acid (13-OH linoleic acid) derived from [14C]linoleic acid and 15-hydroxyperoxy-5,8,11,13-eicosatetraenoic acid (15-HPETE), and 15-hydroxy-5,8,11,13-eicosatetraenoic acid (15-HETE) derived from [14C]- and [3H]arachidonic acid were identified by TLC-autoradiography and by reverse-phase high-performance liquid chromatography (RP-HPLC). Products were quantitated by counting samples that had been scraped from replicate TLC plates and by determination of the integrated optical density during RP-HPLC. The arachidonyl 5-lipoxygenase had a pH optimum of 7.5 and was 50% maximally active at a Ca2+ concentration of 0.05 mM; the Km for production of 5-HPETE/5-HETE from arachidonic acid was 12.2 +/- 4.5 microM (mean +/- S.D., n = 3), and the Vmax was 2.8 +/- 0.9 nmol/min X mg protein (mean +/- S.D., n = 3). The omega-6 linoleic lipoxygenase had a pH optimum of 6.5 and was 50% maximally active at a Ca2+ concentration of 0.1 mM in the presence of 5 mM EGTA. When the arachidonyl 5-lipoxygenase and the omega-6 lipoxygenase were separated by DEAE-Sephadex ion exchange chromatography, the omega-6 lipoxygenase exhibited a Km of 77.2 microM and a Vmax of 9.5 nmol/min X mg protein (mean, n = 2) for conversion of linoleic acid to 13-OOH/13-OH linoleic acid and a Km of 63.1 microM and a Vmax of 5.3 nmol/min X mg protein (mean, n = 2) for formation of 15-HPETE/15-HETE from arachidonic acid.

Published

1985

36. Metabolism of leukotriene B4 in isolated rat hepatocytes. Identification of a novel 18-carboxy-19,20-dinor leukotriene B4 metabolite.

Author

Harper TW, Garrity MJ, and Murphy RC

Subjects

Chemical Phenomena, Chemistry, Chromatography, High Pressure Liquid, Gas Chromatography-Mass Spectrometry, Spectrophotometry, Ultraviolet, Leukotriene B4 metabolism, Liver metabolism

Abstract

Isolated rat heptocytes were found to metabolize leukotriene B4 (LTB4) to a number of products which could be separated by reverse phase high performance liquid chromatography (HPLC). After incubation of LTB4 with hepatocytes for 15 min, the known omega-oxidized metabolites, 20-hydroxy- and 20-carboxy-LTB4, were identified by HPLC retention time and gas chromatography-mass spectrometry. An early fraction corresponding to 15% of the initial LTB4 was structurally characterized as a novel metabolite, 18-carboxy-19,20-dinor-LTB4, by ultraviolet spectroscopy and gas chromatography-mass spectrometry of the derivatized and derivatized, reduced metabolite. The short HPLC retention time of this metabolite was consistent with its reduced lipophilicity. An additional minor metabolite was tentatively identified as 3-hydroxy-LTB4. These two novel metabolites provide evidence for beta-oxidation as an important route of hepatic biotransformation of LTB4 and 20-hydroxy-LTB4.

Published

1986

37. Gas-chromatographic resolution of enantiomeric secondary alcohols. Stereoselective reductive metabolism of ketones in rabbit-liver cytosol.

Author

Gal J, DeVito D, and Harper TW

Subjects

Alcohols isolation & purification, Animals, Chromatography, Gas, Cyanates, Cytosol metabolism, Ketones isolation & purification, Male, Oxidation-Reduction, Rabbits, Stereoisomerism, Structure-Activity Relationship, Alcohols metabolism, Isocyanates, Ketones metabolism, Liver metabolism

Abstract

Chiral secondary alcohols were treated with (S)-(-)-1-phenylethyl isocyanate. For each racemic alcohol, the resulting diastereomeric urethane derivatives were resolved on flexible fused-silica capillary GLC columns with retention times of 15 min or less. Derivatization of individual enantiomers showed that the urethane derivatives of (R)-(-)-2-octanol, (R)-(+)-1-phenylethyl alcohol, and (S)-(+)-2,2,2-trifluoro-1-phenylethanol are eluted before the corresponding diastereomers. The procedure is simple and rapid, and is suitable for the determination of the enantiomeric composition of chiral alcohols extracted from biological media. A series of aliphatic alcohols, aryl alkyl carbinols, and arylalkyl alkyl carbinols were resolved with the procedure, and the degree of resolution varied from good to excellent. Eight achiral ketones were incubated, individually, with rabbit-liver 90,000 g supernatant fractions, and the enantiomeric composition of the alcohol metabolites was determined with the GLC procedure. The reductions proceeded with high stereoselectivity to give alcohol products of 90% or greater enantiomeric purity. The reduction of 2-octanone and acetophenone gave predominant alcohols of (S)-configuration, in agreement with the Baumann-Prelog rule. The configuration of the predominant alcohols arising in the reduction of the remainder of the ketones could not be firmly established, but the evidence suggests that they are also of the (S)-configuration. Fluorine or methyl substitution in the ortho position of acetophenone produced an increase in the stereoselectivity, and the alcohol produced from ortho-methylacetophenone was enantiomerically greater than 99% pure.

Published

1981

38. Rapid extraction of leukotrienes from biologic fluids and quantitation by high-performance liquid chromatography.

Author

Metz SA, Hall ME, Harper TW, and Murphy RC

Subjects

Cell Line, Chromatography, High Pressure Liquid methods, Humans, Isomerism, Mast-Cell Sarcoma metabolism, Leukotriene B4 isolation & purification, SRS-A isolation & purification

Abstract

Previous methods for the recovery and quantitation of leukotrienes have involved tedious extraction procedures, and high-performance liquid chromatographic (HPLC) techniques with significant limitations. We have designed a method to extract leukotrienes from biologic fluids using commercially available silica mini-columns requiring minimal preparation. Sample clarification is followed by a sensitive and reproducible HPLC technique which separates and quantifies the leukotrienes LTC4, LTD4, LTB4 (and at least three of their isomers). The entire procedure requires less than one hour per sample.

Published

1982