Your search keyword '"Koboldt CM"' showing total 21 results

1. Valdecoxib: assessment of cyclooxygenase-2 potency and selectivity.

Author

Gierse JK, Zhang Y, Hood WF, Walker MC, Trigg JS, Maziasz TJ, Koboldt CM, Muhammad JL, Zweifel BS, Masferrer JL, Isakson PC, and Seibert K

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arthritis, Experimental drug therapy, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Humans, Hyperalgesia drug therapy, Inflammation drug therapy, Male, Membrane Proteins, Rats, Rats, Inbred Lew, Rats, Sprague-Dawley, Cyclooxygenase Inhibitors pharmacology, Isoxazoles pharmacology, Prostaglandin-Endoperoxide Synthases drug effects, Sulfonamides pharmacology

Abstract

The discovery of a second isoform of cyclooxygenase (COX) led to the search for compounds that could selectively inhibit COX-2 in humans while sparing prostaglandin formation from COX-1. Celecoxib and rofecoxib were among the molecules developed from these efforts. We report here the pharmacological properties of a third selective COX-2 inhibitor, valdecoxib, which is the most potent and in vitro selective of the marketed COX-2 inhibitors that we have studied. Recombinant human COX-1 and COX-2 were used to screen for new highly potent and in vitro selective COX-2 inhibitors and compare kinetic mechanisms of binding and enzyme inhibition with other COX inhibitors. Valdecoxib potently inhibits recombinant COX-2, with an IC(50) of 0.005 microM; this compares with IC values of 0.05 microM for celecoxib, 0.5 microM for rofecoxib, and 5 microM for etoricoxib. Unique binding interactions of valdecoxib with COX-2 translate into a fast rate of inactivation of COX-2 (110,000 M/s compared with 7000 M/s for rofecoxib and 80 M/s for etoricoxib). The overall saturation binding affinity for COX-2 of valdecoxib is 2.6 nM (compared with 1.6 nM for celecoxib, 51 nM for rofecoxib, and 260 nM for etoricoxib), with a slow off-rate (t(1/2) approximately 98 min). Valdecoxib inhibits COX-1 in a competitive fashion only at very high concentrations (IC(50) = 150 microM). Collectively, these data provide a mechanistic basis for the potency and in vitro selectivity of valdecoxib for COX-2. Valdecoxib showed similar activity in the human whole-blood COX assay (COX-2 IC(50) = 0.24 microM; COX-1 IC(50) = 21.9 microM). We also determined whether this in vitro potency and selectivity translated to significant potency in vivo. In rats, valdecoxib demonstrated marked potency in acute and chronic models of inflammation (air pouch ED(50) = 0.06 mg/kg; paw edema ED(50) = 5.9 mg/kg; adjuvant arthritis ED(50) = 0.03 mg/kg). In these same animals, COX-1 was spared at doses greater than 200 mg/kg. These data provide a basis for the observed potent anti-inflammatory activity of valdecoxib in humans.

Published

2005

2. Cloning, expression, and selective inhibition of canine cyclooxygenase-1 and cyclooxygenase-2.

Author

Gierse JK, Staten NR, Casperson GF, Koboldt CM, Trigg JS, Reitz BA, Pierce JL, and Seibert K

Subjects

Amino Acid Sequence, Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cloning, Molecular, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Dose-Response Relationship, Drug, Gene Expression, Gene Library, Humans, Isoenzymes biosynthesis, Isoenzymes metabolism, Kidney enzymology, Membrane Proteins, Polymerase Chain Reaction, Prostaglandin-Endoperoxide Synthases biosynthesis, Prostaglandin-Endoperoxide Synthases metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Sequence Alignment, Substrate Specificity, Cyclooxygenase Inhibitors pharmacology, Dogs genetics, Isoenzymes antagonists & inhibitors, Isoenzymes genetics, Prostaglandin-Endoperoxide Synthases genetics

Abstract

Cyclooxygenase (COX) performs the critical initial reaction in the arachidonic metabolic cascade, leading to formation of proinflammatory prostaglandins, thromboxanes, and prostacyclins. The discovery of a second COX isoform (COX-2) associated with inflammation led to agents that selectively inhibit COX-2. Cyclooxygenase-2 inhibitors are also being developed for canine applications. To assess the compound potency on canine enzymes, canine COX-1 and COX-2 were cloned, expressed, and purified. Cyclooxygenase-1 was cloned from a canine kidney complementary DNA (cDNA) library, with 96 % sequence homology to human COX-1. Cyclooxygenase-2 was cloned from canine kidney and lipopolysaccharide-stimulated macrophage cDNA libraries, with a 93 % sequence homology to human COX-2. The arachidonic acid Michaelis constants for canine COX-1 and COX-2 were 4.8 and 6.6 micrometer, respectively, compared with 9.6 and 10.2 micrometer for ovine. Inhibition results indicated that, for all compounds tested, there was no significant difference between potencies determined for canine enzymes and those for human enzymes.

Published

2002

3. A three-step kinetic mechanism for selective inhibition of cyclo-oxygenase-2 by diarylheterocyclic inhibitors.

Author

Walker MC, Kurumbail RG, Kiefer JR, Moreland KT, Koboldt CM, Isakson PC, Seibert K, and Gierse JK

Subjects

Animals, Binding, Competitive, Celecoxib, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Isoxazoles pharmacology, Kinetics, Meloxicam, Mice, Prostaglandin-Endoperoxide Synthases, Pyrazoles pharmacology, Sheep, Sulfonamides pharmacology, Thiazines pharmacology, Thiazoles pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes antagonists & inhibitors

Abstract

Cyclo-oxygenase (COX) enzymes are the targets for non-steroidal anti-inflammatory drugs (NSAIDs). These drugs demonstrate a variety of inhibitory mechanisms, which include simple competitive, as well as slow binding and irreversible inhibition. In general, most NSAIDs inhibit COX-1 and -2 by similar mechanisms. A unique class of diarylheterocyclic inhibitors has been developed that is highly selective for COX-2 by virtue of distinct inhibitory mechanisms for each isoenzyme. Several of these inhibitors, with varying selectivity, have been utilized to probe the mechanisms of COX inhibition. Results from analysis of both steady-state and time-dependent inhibition were compared. A generalized mechanism for inhibition, consisting of three sequential reversible steps, can account for the various types of kinetic behaviour observed with these inhibitors.

Published

2001

4. Cyclooxygenase assays.

Author

Gierse JK and Koboldt CM

Subjects

Animals, Cyclooxygenase 1 analysis, Cyclooxygenase 1 metabolism, Cyclooxygenase 2 analysis, Cyclooxygenase 2 metabolism, Dinoprostone analysis, Dinoprostone metabolism, Enzyme-Linked Immunosorbent Assay methods, Humans, Oxygen Consumption, Peroxidase analysis, Peroxidase metabolism, Prostaglandin-Endoperoxide Synthases metabolism, Tissue Extracts chemistry, Prostaglandin-Endoperoxide Synthases analysis

Published

2001

5. Characterization of the recombinant IKK1/IKK2 heterodimer. Mechanisms regulating kinase activity.

Author

Huynh QK, Boddupalli H, Rouw SA, Koboldt CM, Hall T, Sommers C, Hauser SD, Pierce JL, Combs RG, Reitz BA, Diaz-Collier JA, Weinberg RA, Hood BL, Kilpatrick BF, and Tripp CS

Subjects

Catalysis, Dimerization, Electrophoresis, Polyacrylamide Gel, Humans, I-kappa B Kinase, Kinetics, Molecular Weight, Recombinant Proteins chemistry, Protein Serine-Threonine Kinases chemistry

Abstract

Nuclear factor kappa B (NF-kappaB) is a ubiquitous, inducible transcription factor that regulates the initiation and progression of immune and inflammatory stress responses. NF-kappaB activation depends on phosphorylation and degradation of its inhibitor protein, IkappaB, initiated by an IkappaB kinase (IKK) complex. This IKK complex includes a catalytic heterodimer composed of IkappaB kinase 1 (IKK1) and IkappaB kinase 2 (IKK2) as well as a regulatory adaptor subunit, NF-kappaB essential modulator. To better understand the role of IKKs in NF-kappaB activation, we have cloned, expressed, purified, and characterized the physiological isoform, the rhIKK1/rhIKK2 heterodimer. We compared its kinetic properties with those of the homodimers rhIKK1 and rhIKK2 and a constitutively active rhIKK2 (S177E, S181E) mutant. We demonstrate activation of these recombinantly expressed IKKs by phosphorylation during expression in a baculoviral system. The K(m) values for ATP and IkappaBalpha peptide for the rhIKK1/rhIKK2 heterodimer are 0.63 and 0.60 micrometer, respectively, which are comparable to those of the IKK2 homodimer. However, the purified rhIKK1/rhIKK2 heterodimer exhibits the highest catalytic efficiency (k(cat)/K(m)) of 47.50 h(-1) micrometer(-1) using an IkappaBalpha peptide substrate compared with any of the other IKK isoforms, including rhIKK2 (17.44 h(-1) micrometer(-1)), its mutant rhIKK2 (S177E, S181E, 1.18 h(-1) micrometer(-1)), or rhIKK1 (0.02 h(-1) micrometer(-1)). Kinetic analysis also indicates that, although both products of the kinase reaction, ADP and a phosphorylated IkappaBalpha peptide, exhibited competitive inhibitory kinetics, only ADP with the low K(i) of 0.77 micrometer may play a physiological role in regulation of the enzyme activity.

Published

2000

6. Selective cyclooxygenase-2 inhibitors: heteroaryl modified 1,2-diarylimidazoles are potent, orally active antiinflammatory agents.

Author

Khanna IK, Yu Y, Huff RM, Weier RM, Xu X, Koszyk FJ, Collins PW, Cogburn JN, Isakson PC, Koboldt CM, Masferrer JL, Perkins WE, Seibert K, Veenhuizen AW, Yuan J, Yang DC, and Zhang YY

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Anti-Inflammatory Agents, Non-Steroidal toxicity, Arthritis, Experimental drug therapy, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors chemistry, Cyclooxygenase Inhibitors pharmacology, Cyclooxygenase Inhibitors toxicity, Dogs, Edema drug therapy, Gastrointestinal Hemorrhage chemically induced, Humans, Hyperalgesia drug therapy, Imidazoles chemistry, Imidazoles pharmacology, Imidazoles toxicity, Intestines drug effects, Intestines pathology, Membrane Proteins, Mice, Nitriles chemical synthesis, Pyridines chemistry, Rats, Stomach drug effects, Stomach pathology, Structure-Activity Relationship, Sulfonamides chemical synthesis, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Cyclooxygenase Inhibitors chemical synthesis, Imidazoles chemical synthesis, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

A series of heteroaryl modified 1,2-diarylimidazoles has been synthesized and found to be potent and highly selective (1000-9000-fold) inhibitors of the human COX-2. 3-Pyridyl derived COX-2 selective inhibitor (25) exhibited excellent activity in acute (carrageenan induced paw edema, ED(50) = 5.4 mg/kg) and chronic (adjuvant induced arthritis, ED(50) = 0.25 mg/kg) models of inflammation. The relatively long half-life of 25 in rat and dog prompted investigation of the pyridyl and other heteroaromatic systems containing potential metabolic functionalities. A number of substituted pyridyl and thiazole containing compounds (e.g., 44, 46, 54, 76, and 78) demonstrated excellent oral activity in every efficacy model evaluated. Several orally active diarylimidazoles exhibited desirable pharmacokinetics profiles and showed no GI toxicity in the rat up to 100 mg/kg in both acute and chronic models. The paper describes facile and practical syntheses of the targeted diarylimidazoles. The structure-activity relationships and antiinflammatory properties of a series of diarylimidazoles are discussed.

Published

2000

7. N-[[(5-methyl-3-phenylisoxazol-4-yl)-phenyl]sulfonyl]propanamide, sodium salt, parecoxib sodium: A potent and selective inhibitor of COX-2 for parenteral administration.

Author

Talley JJ, Bertenshaw SR, Brown DL, Carter JS, Graneto MJ, Kellogg MS, Koboldt CM, Yuan J, Zhang YY, and Seibert K

Subjects

Acylation, Animals, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors administration & dosage, Dogs, Injections, Isoxazoles administration & dosage, Macaca fascicularis, Male, Rats, Cyclooxygenase Inhibitors pharmacology, Isoenzymes antagonists & inhibitors, Isoenzymes pharmacology, Isoxazoles pharmacology, Prostaglandin-Endoperoxide Synthases pharmacology

Published

2000

8. 4-[5-Methyl-3-phenylisoxazol-4-yl]- benzenesulfonamide, valdecoxib: a potent and selective inhibitor of COX-2.

Author

Talley JJ, Brown DL, Carter JS, Graneto MJ, Koboldt CM, Masferrer JL, Perkins WE, Rogers RS, Shaffer AF, Zhang YY, Zweifel BS, and Seibert K

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arthritis, Experimental drug therapy, Cyclooxygenase 2, Edema drug therapy, Enzyme Inhibitors pharmacology, Humans, Isoenzymes blood, Isoxazoles pharmacology, Membrane Proteins, Prostaglandin-Endoperoxide Synthases blood, Rats, Recombinant Proteins antagonists & inhibitors, Sulfonamides pharmacology, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Enzyme Inhibitors chemical synthesis, Isoenzymes pharmacology, Isoxazoles chemical synthesis, Prostaglandin-Endoperoxide Synthases pharmacology, Sulfonamides chemical synthesis

Published

2000

9. 4,5-Diaryloxazole inhibitors of cyclooxygenase-2 (COX-2).

Author

Talley JJ, Bertenshaw SR, Brown DL, Carter JS, Graneto MJ, Koboldt CM, Masferrer JL, Norman BH, Rogier DJ Jr, Zwwifel BS, and Seibert K

Subjects

Animals, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Humans, Membrane Proteins, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes drug effects, Oxazoles pharmacology, Prostaglandin-Endoperoxide Synthases drug effects

Abstract

A series of methysulfonyl or sulfonamido substituted 4,5-diaryloxazole were prepared and evaluated for their ability to inhibit the inducible form of cyclooxygenase (COX-2) in vitro and in vivo. Several unique substitution patterns were identified that led to potent and selective inhibitors of COX-2. In general, 2-trifluoromethly-4,5-diaryloxazoles substituted with a methylsulfonyl or sulfonamido group were particularly potent inhibitors. One of the more potent compounds with a selectivity for COX-2 of about 800 fold was 4b (SC-299). SC-299, a highly fluorescent molecule, may be useful for spectroscopic studies on preferential inhibitor binding to COX-2.

Published

1999

10. Kinetic basis for selective inhibition of cyclo-oxygenases.

Author

Gierse JK, Koboldt CM, Walker MC, Seibert K, and Isakson PC

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Binding, Competitive, Celecoxib, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors pharmacology, Dinoprostone metabolism, Humans, Ibuprofen pharmacology, Indomethacin pharmacology, Inhibitory Concentration 50, Isoenzymes metabolism, Kinetics, Male, Membrane Proteins, Mice, Naproxen pharmacology, Oxygen metabolism, Pyrazoles, Sheep, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Tetramethylphenylenediamine metabolism, Thermodynamics, Anti-Inflammatory Agents, Non-Steroidal metabolism, Cyclooxygenase Inhibitors metabolism, Prostaglandin-Endoperoxide Synthases metabolism, Sulfonamides metabolism

Abstract

Non-steroidal anti-inflammatory drugs (NSAIDs) inhibit the formation of prostaglandins by cyclo-oxygenases (COX). The discovery of a second COX isoform (COX-2) associated with inflammation led to agents that selectively inhibit COX-2, e.g. celecoxib. We evaluated the kinetics of inhibition of celecoxib and several NSAIDs. Celecoxib displays classic competitive kinetics on COX-1 (Ki=10-16 microM). An initial competitive interaction with COX-2 can also be discerned with celecoxib (Ki=11-15 microM), followed by a time-dependent interaction leading to potent inhibition, characterized as inactivation (Kinact=0.03-0.5 s-1). Half-maximal inhibition (IC50) using end-point assays reflects the competitive component on COX-1 (IC50=4-19 microM) and the inactivation component on COX-2 (IC50=0.003-0.006 microM). NSAIDs exhibit four distinct modes of COX inhibition based on kinetic behaviour: (1) competitive, e.g. ibuprofen; (2) weak binding, time-dependent, e.g. naproxen, oxicams; (3) tight binding, time-dependent, e.g. indomethacin; (4) covalent, e.g. aspirin. In addition, most NSAIDs display different kinetic behaviour for each isoform. Weakly binding inhibitors show variable behaviour in enzyme assays, with apparent inhibitory activity being markedly influenced by experimental conditions; determination of kinetic constants with this class is unreliable and IC50 values are strongly dependent on assay conditions. Although IC50 determinations are useful for structure/activity analyses, the complex and distinct mechanisms of enzyme inhibition of each COX isoform by the NSAIDs renders comparison of inhibitory activity on COX-1 and COX-2 using IC50 ratios of questionable validity.

Published

1999

11. Synthesis and activity of sulfonamide-substituted 4,5-diaryl thiazoles as selective cyclooxygenase-2 inhibitors.

Author

Carter JS, Kramer S, Talley JJ, Penning T, Collins P, Graneto MJ, Seibert K, Koboldt CM, Masferrer J, and Zweifel B

Subjects

Animals, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors chemical synthesis, Humans, Membrane Proteins, Models, Chemical, Rats, Isoenzymes drug effects, Prostaglandin-Endoperoxide Synthases drug effects, Sulfonamides chemistry, Thiazoles chemical synthesis

Abstract

A series of sulfonamide-substituted 4,5-diarylthiazoles was prepared via three synthetic routes as selective COX-2 inhibitors. Recently in the synthesis of selective COX-2 inhibitors we have discovered that the sulfonamide moiety is a suitable replacement for the methylsulfonyl moiety yielding compounds with activity both in vitro and in vivo.

Published

1999

12. Design and synthesis of sulfonyl-substituted 4,5-diarylthiazoles as selective cyclooxygenase-2 inhibitors.

Author

Carter JS, Rogier DJ, Graneto MJ, Seibert K, Koboldt CM, Zhang Y, and Talley JJ

Subjects

Animals, Cyclooxygenase 2, Inhibitory Concentration 50, Rats, Isoenzymes drug effects, Prostaglandin-Endoperoxide Synthases drug effects, Sulfones chemistry, Thiazoles chemical synthesis

Abstract

A series of novel sulfone substituted 4,5-diarylthiazoles have been synthesized and evaluated for their inhibition of the two isoforms of human cyclooxygenase (COX-1 and COX-2). This series displays exceptionally selective COX-2 inhibition.

Published

1999

13. Pharmacological analysis of cyclooxygenase-1 in inflammation.

Author

Smith CJ, Zhang Y, Koboldt CM, Muhammad J, Zweifel BS, Shaffer A, Talley JJ, Masferrer JL, Seibert K, and Isakson PC

Subjects

Animals, Blood Platelets drug effects, Blood Platelets metabolism, Carrageenan, Celecoxib, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Dinoprostone metabolism, Edema, Hyperalgesia, Indomethacin pharmacology, Male, Membrane Proteins, Models, Biological, Rats, Rats, Sprague-Dawley, Recombinant Proteins metabolism, Sulfonamides pharmacology, Thromboxane B2 blood, Arthritis, Experimental enzymology, Cyclooxygenase Inhibitors pharmacology, Inflammation enzymology, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism, Pyrazoles pharmacology

Abstract

The enzymes cyclooxygenase-1 and cyclooxygenase-2 (COX-1 and COX-2) catalyze the conversion of arachidonic acid to prostaglandin (PG) H2, the precursor of PGs and thromboxane. These lipid mediators play important roles in inflammation and pain and in normal physiological functions. While there are abundant data indicating that the inducible isoform, COX-2, is important in inflammation and pain, the constitutively expressed isoform, COX-1, has also been suggested to play a role in inflammatory processes. To address the latter question pharmacologically, we used a highly selective COX-1 inhibitor, SC-560 (COX-1 IC50 = 0.009 microM; COX-2 IC50 = 6.3 microM). SC-560 inhibited COX-1-derived platelet thromboxane B2, gastric PGE2, and dermal PGE2 production, indicating that it was orally active, but did not inhibit COX-2-derived PGs in the lipopolysaccharide-induced rat air pouch. Therapeutic or prophylactic administration of SC-560 in the rat carrageenan footpad model did not affect acute inflammation or hyperalgesia at doses that markedly inhibited in vivo COX-1 activity. By contrast, celecoxib, a selective COX-2 inhibitor, was anti-inflammatory and analgesic in this model. Paradoxically, both SC-560 and celecoxib reduced paw PGs to equivalent levels. Increased levels of PGs were found in the cerebrospinal fluid after carrageenan injection and were markedly reduced by celecoxib, but were not affected by SC-560. These results suggest that, in addition to the role of peripherally produced PGs, there is a critical, centrally mediated neurological component to inflammatory pain that is mediated at least in part by COX-2.

Published

1998

14. 1,2-Diarylimidazoles as potent, cyclooxygenase-2 selective, and orally active antiinflammatory agents.

Author

Khanna IK, Weier RM, Yu Y, Xu XD, Koszyk FJ, Collins PW, Koboldt CM, Veenhuizen AW, Perkins WE, Casler JJ, Masferrer JL, Zhang YY, Gregory SA, Seibert K, and Isakson PC

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal adverse effects, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Arthritis, Experimental drug therapy, Carrageenan, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors pharmacology, Cyclooxygenase Inhibitors therapeutic use, Edema chemically induced, Edema drug therapy, Gastrointestinal Diseases chemically induced, Humans, Imidazoles chemistry, Imidazoles pharmacology, Imidazoles therapeutic use, Membrane Proteins, Mice, Molecular Structure, Rats, Structure-Activity Relationship, Sulfonamides pharmacology, Sulfonamides therapeutic use, Sulfones pharmacology, Sulfones therapeutic use, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Cyclooxygenase Inhibitors chemical synthesis, Imidazoles chemical synthesis, Isoenzymes, Prostaglandin-Endoperoxide Synthases, Sulfonamides chemical synthesis, Sulfones chemical synthesis

Abstract

Series of 1,2-diarylimidazoles has been synthesized and found to contain highly potent and selective inhibitors of the human COX-2 enzyme. The paper describes a short synthesis of the target 1,2-diarylimidazoles starting with aryl nitriles. Different portions of the diarylimidazole (I) were modified to establish SAR. Systematic variations of the substituents in the aryl ring B have yielded very potent (IC50 = 10-100 nm) and selective (1000-12500) inhibitors of the COX-2 enzyme. The study on the influence of substituents in the imidazole ring established that a CF3 group at position 4 gives the optimum oral activity. A number of the diarylimidazoles showed excellent inhibition in the adjuvant induced arthritis model (e.g., ED50 = 0.02 mpk for 22 and 34). The diarylimidazoles are also potent inhibitors of carrageenan-induced edema (ED50 = 9-30 mpk) and hyperalgesia (ED50 = 11-40 mpk). Several orally active diarylimidazoles show no GI toxicity in the rat and mouse up to 200 mpk.

Published

1997

15. 1,2-Diarylpyrroles as potent and selective inhibitors of cyclooxygenase-2.

Author

Khanna IK, Weier RM, Yu Y, Collins PW, Miyashiro JM, Koboldt CM, Veenhuizen AW, Currie JL, Seibert K, and Isakson PC

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Carrageenan, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors therapeutic use, Edema chemically induced, Edema drug therapy, Humans, Membrane Proteins, Molecular Structure, Pyrroles chemistry, Pyrroles therapeutic use, Rats, Recombinant Proteins, Structure-Activity Relationship, Sulfonamides therapeutic use, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Cyclooxygenase Inhibitors chemical synthesis, Cyclooxygenase Inhibitors pharmacology, Isoenzymes, Prostaglandin-Endoperoxide Synthases, Pyrroles chemical synthesis, Pyrroles pharmacology, Sulfonamides chemical synthesis, Sulfonamides pharmacology

Abstract

Series of 1,2-diarylpyrroles has been synthesized and found to contain very potent and selective inhibitors of the human cyclooxygenase-2 (COX-2) enzyme. The paper describes short and practical syntheses of the target molecules utilizing the Paal-Knorr reaction. Electrophilic substitution on 1 proceeds in a regioselective fashion, and the method was used to generate a number of tetrasubstituted pyrroles. Detailed SAR on the series has been studied by modifications of the aryl rings and the substituents in the pyrrole ring. Diarylpyrrole 1 is a very potent (COX-2, IC50 = 60 nm) and selective (COX-1/COX-2 = > 1700) inhibitor whereas the isomeric 2 is completely inactive against COX-2. Modifications of the substituents on the fluorophenyl ring in 1 yields very potent inhibitors of COX-2 (IC50 = 40-80 nm) with excellent selectivity (1200 to > 2500) vs COX-1. Analog 20 containing a sulfonamide group is an excellent inhibitor of COX-2 with an IC50 of 14 nm. Tetrasubstituted pyrroles containing groups such as COCF3, SO2CF3, or CH2OAr at position 3 in the pyrrole ring give excellent inhibitors (COX-2, IC50 = 30-120 nm). In vivo testing in the carrageenan-induced paw edema model in the rat establishes that the 1,2-diarylpyrroles are orally active antiinflammatory agents. Compound 3 is the most potent inhibitor of edema with an ED50 of 4.7 mpk.

Published

1997

16. Synthesis and biological evaluation of the 1,5-diarylpyrazole class of cyclooxygenase-2 inhibitors: identification of 4-[5-(4-methylphenyl)-3-(trifluoromethyl)-1H-pyrazol-1-yl]benze nesulfonamide (SC-58635, celecoxib).

Author

Penning TD, Talley JJ, Bertenshaw SR, Carter JS, Collins PW, Docter S, Graneto MJ, Lee LF, Malecha JW, Miyashiro JM, Rogers RS, Rogier DJ, Yu SS, AndersonGD, Burton EG, Cogburn JN, Gregory SA, Koboldt CM, Perkins WE, Seibert K, Veenhuizen AW, Zhang YY, and Isakson PC

Subjects

Animals, Arthritis, Experimental drug therapy, Arthritis, Rheumatoid drug therapy, Carrageenan pharmacology, Celecoxib, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors chemistry, Cyclooxygenase Inhibitors pharmacokinetics, Hyperalgesia drug therapy, Magnetic Resonance Spectroscopy, Male, Membrane Proteins, Molecular Structure, Osteoarthritis drug therapy, Pyrazoles, Rats, Rats, Inbred Lew, Rats, Sprague-Dawley, Structure-Activity Relationship, Cyclooxygenase Inhibitors chemical synthesis, Cyclooxygenase Inhibitors pharmacology, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism, Sulfonamides chemical synthesis, Sulfonamides pharmacology

Abstract

A series of sulfonamide-containing 1,5-diarylpyrazole derivatives were prepared and evaluated for their ability to block cyclooxygenase-2 (COX-2) in vitro and in vivo. Extensive structure-activity relationship (SAR) work was carried out within this series, and a number of potent and selective inhibitors of COX-2 were identified. Since an early structural lead (1f, SC-236) exhibited an unacceptably long plasma half-life, a number of pyrazole analogs containing potential metabolic sites were evaluated further in vivo in an effort to identify compounds with acceptable pharmacokinetic profiles. This work led to the identification of 1i (4-[5-(4-methylphenyl)-3-(trifluoromethyl)- H-pyrazol-1-yl]benzenesulfonamide, SC-58635, celecoxib), which is currently in phase III clinical trials for the treatment of rheumatoid arthritis and osteoarthritis.

Published

1997

17. A single amino acid difference between cyclooxygenase-1 (COX-1) and -2 (COX-2) reverses the selectivity of COX-2 specific inhibitors.

Author

Gierse JK, McDonald JJ, Hauser SD, Rangwala SH, Koboldt CM, and Seibert K

Subjects

Amino Acid Sequence, Animals, Binding Sites, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Humans, Isoleucine, Membrane Proteins, Mutagenesis, Site-Directed, Sheep, Structure-Activity Relationship, Valine, Anti-Inflammatory Agents, Non-Steroidal chemistry, Cyclooxygenase Inhibitors chemistry, Isoenzymes chemistry, Prostaglandin-Endoperoxide Synthases chemistry

Abstract

Nonsteroidal anti-inflammatory drugs (NSAIDs) currently available for clinical use inhibit both COX-1 and COX-2. This suggests that clinically useful NSAIDs inhibit pro-inflammatory prostaglandins (PGs) derived from the activity of COX-2, as well as PGs in tissues like the stomach and kidney (via COX-1). A new class of compounds has recently been developed (SC-58125) that have a high degree of selectivity for the inducible form of cyxlooxygenase (COX-2) over the constitutive form (COX-1). This unique class of compounds exhibit a time-dependent irreversible inhibition of COX-2, while reversibly inhibiting COX-1. The molecular basis of this selectivity was probed by site-directed mutagenesis of the active site of COX-2. The sequence differences in the active site were determined by amino acid replacement of the COX-2 sequences based on the known crystal structure of COX-1, which revealed a single amino acid difference in the active site (valine 509 to isoleucine) and a series of differences at the mouth of the active site. Mutants with the single amino acid substitution in the active site and a combination of three changes in the mouth of the active site were made in human COX-2, expressed in insect cells and purified. The single amino acid change of valine 509 to isoleucine confers selectivity of COX-2 inhibitors in the class of SC-58125 and others of the same class (SC-236, NS-398), while commonly used NSAIDs such as indomethacin showed no change in selectivity. Substitutions of COX-1 sequences in COX-2 at the mouth of the active site of COX-2 did not change the selectivity of SC-58125. This indicates that the single amino acid substitution of isoleucine at position 509 for a valine is sufficient to confer COX-2 selectivity in this example of a diaryl-heterocycle COX inhibitor.

Published

1996

18. Novel terphenyls as selective cyclooxygenase-2 inhibitors and orally active anti-inflammatory agents.

Author

Li JJ, Norton MB, Reinhard EJ, Anderson GD, Gregory SA, Isakson PC, Koboldt CM, Masferrer JL, Perkins WE, Seibert K, Zhang Y, Zweifel BS, and Reitz DB

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Arthritis, Experimental drug therapy, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors administration & dosage, Cyclooxygenase Inhibitors chemistry, Cyclooxygenase Inhibitors therapeutic use, Magnetic Resonance Spectroscopy, Mass Spectrometry, Rats, Terphenyl Compounds administration & dosage, Terphenyl Compounds chemistry, Terphenyl Compounds therapeutic use, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes drug effects, Prostaglandin-Endoperoxide Synthases drug effects, Terphenyl Compounds pharmacology

Abstract

A novel series of terphenyl methyl sulfones and sulfonamides have been shown to be highly potent and selective cyclooxygenase-2 (COX-2) inhibitors. The sulfonamide analogs 17 and 21 were found to be much more potent COX-2 inhibitors and orally active anti-inflammatory agents than the corresponding methyl sulfone analogs 16 and 20, respectively, albeit with some decrease in COX-2 selectivity. Structure-activity relationship studies have determined that incorporation of two fluorine atoms in the central phenyl group, as in 20 and 21, is extremely advantageous for both in vitro COX-2 potency and selectivity as well as in vivo activity. Several noticeable examples in the 1,2-diaryl-4,5-difluorobenzenesulfonamide series are 21a-c,k,l,n (COX-2, IC50 = 0.002-0.004 microM), in which all have in vitro COX-1/COX-2 selectivity > 1000. In addition, sulfonamides 21a,b,d,g,j,m,n,q were shown to have greatly enhanced oral activity with more than 90% inhibition of prostaglandin E2 production in the air pouch model of inflammation. Furthermore, sulfonamide 21b was found to be very active in the rat adjuvant-induced arthritis model (ED50 = 0.05 mg/kg) and carrageenan-induced hyperalgesia assay (ED50 = 38.7 mg/kg) with no indication of gastrointestinal toxicity in rats at doses as high as 200 mg/kg.

Published

1996

19. Diarylspiro[2.4]heptenes as orally active, highly selective cyclooxygenase-2 inhibitors: synthesis and structure-activity relationships.

Author

Huang HC, Li JJ, Garland DJ, Chamberlain TS, Reinhard EJ, Manning RE, Seibert K, Koboldt CM, Gregory SA, Anderson GD, Veenhuizen AW, Zhang Y, Perkins WE, Burton EG, Cogburn JN, Isakson PC, and Reitz DB

Subjects

Analgesics chemical synthesis, Analgesics pharmacology, Animals, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arthritis, Experimental drug therapy, Carrageenan pharmacology, Cyclooxygenase Inhibitors pharmacokinetics, Cyclooxygenase Inhibitors pharmacology, Edema drug therapy, Humans, Intestines drug effects, Magnetic Resonance Spectroscopy, Male, Mice, Rats, Rats, Inbred Lew, Rats, Sprague-Dawley, Spiro Compounds chemistry, Spiro Compounds pharmacokinetics, Spiro Compounds pharmacology, Stomach drug effects, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacokinetics, Sulfonamides pharmacology, Sulfones chemistry, Sulfones pharmacokinetics, Sulfones pharmacology, Anti-Inflammatory Agents, Non-Steroidal chemistry, Cyclooxygenase Inhibitors chemical synthesis, Spiro Compounds chemical synthesis, Sulfonamides chemical synthesis, Sulfones chemical synthesis

Abstract

A novel series of 5,6-diarylspiro[2.4]hept-5-enes was shown to provide highly potent and selective cyclooxygenase-2 (COX-2) inhibitors. A study of structure-activity relationships in this series suggests that 3,4-disubstituted phenyl analogs are generally more selective than 4-substituted phenyl analogs and that replacement of the methyl sulfone group on the 6-phenyl ring with a sulfonamide moiety results in compounds with superior in vivo pharmacological properties, although with lower COX-2 selectivity. Several compounds have been shown to possess promising pharmacological properties in adjuvant-induced arthritis and edema analgesia models. The absence of gastrointestinal (GI) toxicity at 200 mpk of several selected compounds in rats and mice corresponds well with the weak potency for inhibition of COX-1 observed in the enzyme assay. Methyl sulfone 55 and sulfonamide 24 were shown to have superior in vivo pharmacological profiles, low GI toxicity, and good oral bioavailability and duration of action.

Published

1996

20. 1,2-Diarylcyclopentenes as selective cyclooxygenase-2 inhibitors and orally active anti-inflammatory agents.

Author

Li JJ, Anderson GD, Burton EG, Cogburn JN, Collins JT, Garland DJ, Gregory SA, Huang HC, Isakson PC, and Koboldt CM

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal chemical synthesis, Arthritis, Experimental drug therapy, Cyclooxygenase Inhibitors chemical synthesis, Cyclopentanes chemical synthesis, Dose-Response Relationship, Drug, Edema chemically induced, Edema drug therapy, Indomethacin pharmacology, Magnetic Resonance Spectroscopy, Male, Mice, Molecular Structure, Rats, Rats, Inbred Lew, Rats, Sprague-Dawley, Sulfonamides chemical synthesis, Sulfones chemical synthesis, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Cyclopentanes pharmacology, Sulfonamides pharmacology, Sulfones pharmacology

Abstract

A series of 1,2-diarylcyclopentene methyl sulfones and sulfonamides have been shown to be remarkably potent and selective cyclooxygenase-2 (COX-2) inhibitors. The methyl sulfone analogs 7 showed excellent COX-2 activity, with IC50s ranging from 0.003 (7f,n) to 0.87 (7o) microM. In addition, most analogs of 7 showed no activity (IC50 > 100 microM) against the COX-1 enzyme. Replacement of the methyl sulfone moiety with a sulfonamide group gave a slightly more potent (typically 2-5-fold) but less selective COX-2 inhibitor, mainly due to an increase (20- > 100-fold) in COX-1 activity. However, in vitro COX-1/COX-2 selectivity for the sulfonamides 8 could be increased in many cases by simply incorporating a substituent at the 3-position of the phenyl group. Furthermore, in vitro selectivity increased with the size and number of substituents, as demonstrated in the selectivity trend of 8k (8000) > 8j (1900) > 8i (500) > 8h (100). More importantly, the sulfonamide COX-2 inhibitors showed greatly enhanced oral activity in the rat model of established adjuvant-induced arthritis, with inhibition values of 79.0% (8a), 81.5% (8c), and 83.0% (8g) at 1 mg/kg. On the basis of its overall biological profile, sulfonamide 8c was evaluated as a potential clinical candidate, displaying an ED50 of 22 mpk in the rat carrageenan-induced paw edema model and an ED50 of 0.16 mpk in the rat established adjuvant-induced arthritis model with no indication of gastrointestinal toxicity in rats and mice at 200 mpk. In addition, a preparative-scale synthetic route to sulfonamide 8c has been developed.

Published

1995

21. Selective cyclooxygenase inhibitors: novel 1,2-diarylcyclopentenes are potent and orally active COX-2 inhibitors.

Author

Reitz DB, Li JJ, Norton MB, Reinhard EJ, Collins JT, Anderson GD, Gregory SA, Koboldt CM, Perkins WE, and Seibert K

Subjects

Administration, Oral, Animals, Arthritis, Experimental drug therapy, Cyclooxygenase Inhibitors administration & dosage, Cyclooxygenase Inhibitors chemical synthesis, Cyclopentanes administration & dosage, Cyclopentanes chemical synthesis, Mice, Rats, Cyclooxygenase Inhibitors pharmacology, Cyclopentanes pharmacology

Published

1994