Your search keyword '"Percival MD"' showing total 74 results

51. Etoricoxib (MK-0663): preclinical profile and comparison with other agents that selectively inhibit cyclooxygenase-2.

Author

Riendeau D, Percival MD, Brideau C, Charleson S, Dubé D, Ethier D, Falgueyret JP, Friesen RW, Gordon R, Greig G, Guay J, Mancini J, Ouellet M, Wong E, Xu L, Boyce S, Visco D, Girard Y, Prasit P, Zamboni R, Rodger IW, Gresser M, Ford-Hutchinson AW, Young RN, and Chan CC

Subjects

Algorithms, Animals, Anti-Inflammatory Agents pharmacology, Arachidonic Acid metabolism, CHO Cells, Cricetinae, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors toxicity, Etoricoxib, Gastrointestinal Diseases chemically induced, Gastrointestinal Diseases pathology, Humans, Ionophores metabolism, Isoenzymes blood, Male, Membrane Proteins, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Prostaglandin-Endoperoxide Synthases blood, Pyridines toxicity, Rats, Rats, Sprague-Dawley, Recombinant Proteins blood, Recombinant Proteins metabolism, Substrate Specificity, Sulfones toxicity, Thromboxane B2 biosynthesis, Cyclooxygenase Inhibitors pharmacology, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism, Pyridines pharmacology, Sulfones pharmacology

Abstract

We report here the preclinical profile of etoricoxib (MK-0663) [5-chloro-2-(6-methylpyridin-3-yl)-3-(4-methylsulfonylphenyl) pyridine], a novel orally active agent that selectively inhibits cyclooxygenase-2 (COX-2), that has been developed for high selectivity in vitro using whole blood assays and sensitive COX-1 enzyme assays at low substrate concentration. Etoricoxib selectively inhibited COX-2 in human whole blood assays in vitro, with an IC(50) value of 1.1 +/- 0.1 microM for COX-2 (LPS-induced prostaglandin E2 synthesis), compared with an IC(50) value of 116 +/- 8 microM for COX-1 (serum thromboxane B2 generation after clotting of the blood). Using the ratio of IC(50) values (COX-1/COX-2), the selectivity ratio for the inhibition of COX-2 by etoricoxib in the human whole blood assay was 106, compared with values of 35, 30, 7.6, 7.3, 2.4, and 2.0 for rofecoxib, valdecoxib, celecoxib, nimesulide, etodolac, and meloxicam, respectively. Etoricoxib did not inhibit platelet or human recombinant COX-1 under most assay conditions (IC(50) > 100 microM). In a highly sensitive assay for COX-1 with U937 microsomes where the arachidonic acid concentration was lowered to 0.1 microM, IC(50) values of 12, 2, 0.25, and 0.05 microM were obtained for etoricoxib, rofecoxib, valdecoxib, and celecoxib, respectively. These differences in potency were in agreement with the dissociation constants (K(i)) for binding to COX-1 as estimated from an assay based on the ability of the compounds to delay the time-dependent inhibition by indomethacin. Etoricoxib was a potent inhibitor in models of carrageenan-induced paw edema (ID(50) = 0.64 mg/kg), carrageenan-induced paw hyperalgesia (ID(50) = 0.34 mg/kg), LPS-induced pyresis (ID(50) = 0.88 mg/kg), and adjuvant-induced arthritis (ID(50) = 0.6 mg/kg/day) in rats, without effects on gastrointestinal permeability up to a dose of 200 mg/kg/day for 10 days. In squirrel monkeys, etoricoxib reversed LPS-induced pyresis by 81% within 2 h of administration at a dose of 3 mg/kg and showed no effect in a fecal 51Cr excretion model of gastropathy at 100 mg/kg/day for 5 days, in contrast to lower doses of diclofenac or naproxen. In summary, etoricoxib represents a novel agent that selectively inhibits COX-2 with 106-fold selectivity in human whole blood assays in vitro and with the lowest potency of inhibition of COX-1 compared with other reported selective agents.

Published

2001

52. Novel, nonpeptidic cyanamides as potent and reversible inhibitors of human cathepsins K and L.

Author

Falgueyret JP, Oballa RM, Okamoto O, Wesolowski G, Aubin Y, Rydzewski RM, Prasit P, Riendeau D, Rodan SB, and Percival MD

Subjects

Animals, Bone Resorption pathology, Bone and Bones drug effects, Bone and Bones metabolism, Catalytic Domain, Cathepsin K, Cathepsin L, Cattle, Collagen metabolism, Cysteine chemistry, Cysteine Endopeptidases, Cysteine Proteinase Inhibitors chemistry, Cysteine Proteinase Inhibitors pharmacokinetics, Cysteine Proteinase Inhibitors pharmacology, Glutathione chemistry, Humans, In Vitro Techniques, Kinetics, Magnetic Resonance Spectroscopy, Nitriles chemistry, Nitriles pharmacokinetics, Nitriles pharmacology, Osteoclasts drug effects, Osteoclasts metabolism, Pyrrolidines chemistry, Pyrrolidines pharmacokinetics, Pyrrolidines pharmacology, Rabbits, Rats, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacokinetics, Sulfonamides pharmacology, Cathepsins antagonists & inhibitors, Cysteine Proteinase Inhibitors chemical synthesis, Endopeptidases, Nitriles chemical synthesis, Pyrrolidines chemical synthesis, Sulfonamides chemical synthesis

Abstract

Compounds containing a 1-cyanopyrrolidinyl ring were identified as potent and reversible inhibitors of cathepsins K and L. The original lead compound 1 inhibits cathepsins K and L with IC(50) values of 0. 37 and 0.45 M, respectively. Modification of compound 1 by replacement of the quinoline moiety led to the synthesis of N-(1-cyano-3-pyrrolidinyl)benzenesulfonamide (2). Compound 2 was found to be a potent inhibitor of cathepsins K and L with a K(i) value of 50 nM for cathepsin K. Replacement of the 1-cyanopyrrolidine of compound 2 by a 1-cyanoazetidine increased the potency of the inhibitor by 10-fold. This increase in potency is probably due to an enhanced chemical reactivity of the compound toward the thiolate of the active site of the enzyme. This is demonstrated when the assay is performed in the presence of glutathione at pH 7.0 which favors the formation of a GSH thiolate anion. Under these assay conditions, there is a loss of potency in the 1-cyanoazetidine series due to the formation of an inactive complex between the GSH thiolate and the 1-cyanoazetidine inhibitors. 1-Cyanopyrrolidinyl inhibitors exhibited time-dependent inhibition which allowed us to determine the association and dissociation rate constants with human cathepsin K. The kinetic data obtained showed that the increase of potency observed between different 1-cyanopyrrolidinyl inhibitors is due to an increase of k(on) values and that the association of the compound with the enzyme fits an apparent one-step mechanism. (13)C NMR experiments performed with the enzyme papain showed that compound 2 forms a covalent isothiourea ester adduct with the enzyme. As predicted by the kinetic analysis, the addition of the irreversible inhibitor E64 to the enzyme-cyanopyrrolidinyl complex totally abolished the signal of the isothiourea bond as observed by (13)C NMR, thereby demonstrating that the formation of the covalent bond with the active site cysteine residue is reversible. Finally, compound 2 inhibits bone resorption in an in vitro assay involving rabbit osteoclasts and bovine bone with an IC(50) value of 0.7 M. 1-Cyanopyrrolidine represents a new class of nonpeptidic compounds that inhibit cathepsin K and L activity and proteolysis of bone collagen.

Published

2001

53. Potency and selectivity of inhibition of cathepsin K, L and S by their respective propeptides.

Author

Guay J, Falgueyret JP, Ducret A, Percival MD, and Mancini JA

Subjects

Amino Acid Sequence, Animals, Cathepsin K, Cathepsin L, Cathepsins chemistry, Cloning, Molecular, Cysteine Endopeptidases, Escherichia coli, Humans, Kinetics, Molecular Sequence Data, Papain antagonists & inhibitors, Rats, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins chemistry, Recombinant Proteins pharmacology, Sequence Alignment, Sequence Homology, Amino Acid, Cathepsins antagonists & inhibitors, Cysteine Proteinase Inhibitors pharmacology, Endopeptidases, Enzyme Precursors pharmacology

Abstract

The prodomains of several cysteine proteases of the papain family have been shown to be potent inhibitors of their parent enzymes. An increased interest in cysteine proteases inhibitors has been generated with potential therapeutic targets such as cathepsin K for osteoporosis and cathepsin S for immune modulation. The propeptides of cathepsin S, L and K were expressed as glutathione S-transferase-fusion proteins in Escherichia coli. The proteins were purified on glutathione affinity columns and the glutathione S-transferase was removed by thrombin cleavage. All three propeptides were tested for inhibitor potency and found to be selective within the cathepsin L subfamily (cathepsins K, L and S) compared with cathepsin B or papain. Inhibition of cathepsin K by either procathepsin K, L or S was time-dependent and occurred by an apparent one-step mechanism. The cathepsin K propeptide had a Ki of 3.6-6.3 nM for each of the three cathepsins K, L and S. The cathepsin L propeptide was at least a 240-fold selective inhibitor of cathepsin K (Ki = 0.27 nM) and cathepsin L (Ki = 0.12 nM) compared with cathepsin S (Ki = 65 nM). Interestingly, the cathepsin S propeptide was more selective for inhibition of cathepsin L (Ki = 0.46 nM) than cathepsin S (Ki = 7.6 nM) itself or cathepsin K (Ki = 7.0 nM). This is in sharp contrast to previously published data demonstrating that the cathepsin S propeptide is equipotent for inhibition of human cathepsin S and rat and paramecium cathepsin L [Maubach, G., Schilling, K., Rommerskirch, W., Wenz, I., Schultz, J. E., Weber, E. & Wiederanders, B. (1997), Eur J. Biochem. 250, 745-750]. These results demonstrate that limited selectivity of inhibition can be measured for the procathepsins K, L and S vs. the parent enzymes, but selective inhibition vs. cathepsin B and papain was obtained.

Published

2000

54. Inhibition of cathepsin K by nitric oxide donors: evidence for the formation of mixed disulfides and a sulfenic acid.

Author

Percival MD, Ouellet M, Campagnolo C, Claveau D, and Li C

Subjects

Animals, CHO Cells, Catalysis drug effects, Cathepsin K, Cathepsins metabolism, Cricetinae, Dose-Response Relationship, Drug, Enzyme Activation drug effects, Gas Chromatography-Mass Spectrometry, Glutathione analogs & derivatives, Glutathione pharmacology, Humans, Hydrogen-Ion Concentration, Molsidomine analogs & derivatives, Molsidomine pharmacology, Nitroso Compounds pharmacology, Penicillamine analogs & derivatives, Penicillamine pharmacology, S-Nitroso-N-Acetylpenicillamine, S-Nitrosoglutathione, Time Factors, Cathepsins antagonists & inhibitors, Disulfides metabolism, Nitric Oxide Donors pharmacology, Nitroprusside pharmacology, Protease Inhibitors pharmacology, Sulfenic Acids metabolism

Abstract

The cysteine protease cathepsin K is believed to play a key role in bone resorption as it has collagenolytic activity and is expressed predominantly and in high levels in bone resorbing osteoclast cells. The addition of nitric oxide (NO) and NO donors to osteoclasts in vitro results in a reduction of bone resorption, although the mechanism of this effect is not fully understood. The S-nitroso derivatives of glutathione (GSNO) and N-acetylpenicillamine (SNAP) and the non-thiol NO donors NOR-1 and NOR-3 all inhibited the activity of purified cathepsin K in a time- and concentration-dependent manner (IC(50) values after 15 min of preincubation at pH 7.5 of 28, 105, 0.4, and 10 microM, respectively). Cathepsin K activity in Chinese hamster ovary cells stably transfected with cathepsin K was also inhibited by the above NO donors with similar potencies. GSNO at 100 microM also completely inhibited the autocatalytic maturation at pH 4.0 of procathepsin K to cathepsin K. The inhibition of cathepsin K by GSNO was rapidly reversed by DTT, but inhibition by NOR-1 was not reversed by DTT, and analysis of the inhibited cathepsin K for S-nitrosylation using the Greiss reaction gave negative results in both cases. Analysis of the protein by electrospray liquid chromatography/mass spectrometry showed that the inhibition of cathepsin K by GSNO resulted in a mass increase of 306 +/- 2 Da, consistent with the formation of a glutathione adduct. Prior inhibition of cathepsin K by the active site thiol-modifying inhibitor E-64 blocked the modification by GSNO, indicating that the glutathione adduct is likely formed at the active site cysteine. Treatment of cathepsin K with NOR-1 resulted in a mass increase of between 30 and 50 Da, corresponding to the oxidation of a cysteine to sulfinic and sulfonic acids. Cotreatment of cathepsin K with NOR-1 plus the sulfenic acid reagent dimedone resulted in a mass increase of approximately 141 Da, which is consistent with the formation of a dimedone adduct. This result demonstrates that the NOR-1-dependent formation of cathepsin K sulfinic and sulfonic acids occurs via a sulfenic acid. These results show that inhibition of cathepsin K activity and its autocatalytic maturation represent two potential mechanisms by which NO can exert its inhibitory effect on bone resorption. This work also shows that oxidative thiol modifications besides S-nitrosylation should be considered when the effects of NO and NO donors on critical thiol-containing proteins are investigated.

Published

1999

55. Rofecoxib [Vioxx, MK-0966; 4-(4'-methylsulfonylphenyl)-3-phenyl-2-(5H)-furanone]: a potent and orally active cyclooxygenase-2 inhibitor. Pharmacological and biochemical profiles.

Author

Chan CC, Boyce S, Brideau C, Charleson S, Cromlish W, Ethier D, Evans J, Ford-Hutchinson AW, Forrest MJ, Gauthier JY, Gordon R, Gresser M, Guay J, Kargman S, Kennedy B, Leblanc Y, Leger S, Mancini J, O'Neill GP, Ouellet M, Patrick D, Percival MD, Perrier H, Prasit P, and Rodger I

Subjects

12-Hydroxy-5,8,10,14-eicosatetraenoic Acid metabolism, Animals, Arachidonate 15-Lipoxygenase metabolism, Arachidonic Acid metabolism, Arthritis, Experimental blood, Arthritis, Experimental metabolism, Blood Platelets drug effects, Blood Platelets enzymology, COS Cells, Cell Line, Cricetinae, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Digestive System drug effects, Dogs, Edema chemically induced, Edema prevention & control, Female, Humans, Hyperalgesia chemically induced, Hyperalgesia prevention & control, In Vitro Techniques, Leukotriene B4 biosynthesis, Male, Membrane Proteins, Microsomes drug effects, Microsomes enzymology, Rats, Rats, Inbred Lew, Saimiri, Sulfones, Cyclooxygenase Inhibitors pharmacology, Isoenzymes metabolism, Lactones pharmacology, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

The discoveries that cyclooxygenase (COX)-2 is an inducible form of COX involved in inflammation and that COX-1 is the major isoform responsible for the production of prostaglandins (PGs) in the gastrointestinal tract have provided a rationale for the development of specific COX-2 inhibitors as a new class of anti-inflammatory agents with improved gastrointestinal tolerability. In the present study, the preclinical pharmacological and biochemical profiles of rofecoxib [Vioxx, also known as MK-0966, 4-(4'-methylsulfonylphenyl)-3-phenyl-2-(5H)-furanone], an orally active COX-2 inhibitor, are described. Rofecoxib is a potent inhibitor of the COX-2-dependent production of PGE(2) in human osteosarcoma cells (IC(50) = 26 +/- 10 nM) and Chinese hamster ovary cells expressing human COX-2 (IC(50) = 18 +/- 7 nM) with a 1000-fold selectivity for the inhibition of COX-2 compared with the inhibition of COX-1 activity (IC(50) > 50 microM in U937 cells and IC(50) > 15 microM in Chinese hamster ovary cells expressing human COX-1). Rofecoxib is a time-dependent inhibitor of purified human recombinant COX-2 (IC(50) = 0.34 microM) but caused inhibition of purified human COX-1 in a non-time-dependent manner that could only be observed at a very low substrate concentration (IC(50) = 26 microM at 0.1 microM arachidonic acid concentration). In an in vitro human whole blood assay, rofecoxib selectively inhibited lipopolysaccharide-induced, COX-2-derived PGE(2) synthesis with an IC(50) value of 0.53 +/- 0.02 microM compared with an IC(50) value of 18.8 +/- 0.9 microM for the inhibition of COX-1-derived thromboxane B(2) synthesis after blood coagulation. Using the ratio of the COX-1 IC(50) values over the COX-2 IC(50) values in the human whole blood assay, selectivity ratios for the inhibition of COX-2 of 36, 6.6, 2, 3, and 0.4 were obtained for rofecoxib, celecoxib, meloxicam, diclofenac, and indomethacin, respectively. In several in vivo rodent models, rofecoxib is a potent inhibitor of carrageenan-induced paw edema (ID(50) = 1.5 mg/kg), carrageenan-induced paw hyperalgesia (ID(50) = 1.0 mg/kg), lipopolysaccharide-induced pyresis (ID(50) = 0.24 mg/kg), and adjuvant-induced arthritis (ID(50) = 0.74 mg/kg/day). Rofecoxib also has a protective effect on adjuvant-induced destruction of cartilage and bone structures in rats. In a (51)Cr excretion assay for detection of gastrointestinal integrity in either rats or squirrel monkeys, rofecoxib has no effect at doses up to 200 mg/kg/day for 5 days. Rofecoxib is a novel COX-2 inhibitor with a biochemical and pharmacological profile clearly distinct from that of current nonsteroidal anti-inflammatory drugs and represents a new therapeutic class of anti-inflammatory agents for the treatment of the symptoms of osteoarthritis and rheumatoid arthritis with improved gastrointestinal tolerability.

Published

1999

56. The discovery of rofecoxib, [MK 966, Vioxx, 4-(4'-methylsulfonylphenyl)-3-phenyl-2(5H)-furanone], an orally active cyclooxygenase-2-inhibitor.

Author

Prasit P, Wang Z, Brideau C, Chan CC, Charleson S, Cromlish W, Ethier D, Evans JF, Ford-Hutchinson AW, Gauthier JY, Gordon R, Guay J, Gresser M, Kargman S, Kennedy B, Leblanc Y, Léger S, Mancini J, O'Neill GP, Ouellet M, Percival MD, Perrier H, Riendeau D, Rodger I, and Zamboni R

Subjects

Administration, Oral, Animals, Biological Availability, CHO Cells, Cricetinae, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors chemistry, Humans, Indomethacin adverse effects, Indomethacin pharmacology, Inhibitory Concentration 50, Lactones administration & dosage, Lactones adverse effects, Membrane Proteins, Rats, Sulfones, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Isoenzymes chemistry, Lactones chemical synthesis, Lactones pharmacology, Prostaglandin-Endoperoxide Synthases chemistry

Abstract

The development of a COX-2 inhibitor rofecoxib (MK 966, Vioxx) is described. It is essentially equipotent to indomethacin both in vitro and in vivo but without the ulcerogenic side effect due to COX-1 inhibition.

Published

1999

57. Structure-based design of COX-2 selectivity into flurbiprofen.

Author

Bayly CI, Black WC, Léger S, Ouimet N, Ouellet M, and Percival MD

Subjects

Binding Sites, Crystallography, X-Ray, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors chemistry, Drug Design, Flurbiprofen analogs & derivatives, Flurbiprofen chemistry, Humans, Membrane Proteins, Molecular Structure, Cyclooxygenase Inhibitors metabolism, Flurbiprofen metabolism, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

Comparative computer modeling of the X-ray crystal structures of cyclooxygenase isoforms COX-1 and COX-2 has led to the design of COX-2 selectivity into the nonselective inhibitor flurbiprofen. The COX-2 modeling was based on a postulated binding mode for flurbiprofen and took advantage of a small alcove in the COX-2 active site created by different positions of the Leu384 sidechain between COX-1 and COX-2. The design hypothesis was tested by synthesis and biological assay of a series of flurbiprofen analogs, culminating in the discovery of several inhibitors having up to 78-fold selectivity for COX-2 over COX-1.

Published

1999

58. Analysis of prostaglandin G/H synthase-2 inhibition using peroxidase-induced luminol luminescence.

Author

Forghani F, Ouellet M, Keen S, Percival MD, and Tagari P

Subjects

Anti-Inflammatory Agents, Non-Steroidal pharmacology, Arachidonic Acid metabolism, Binding, Competitive, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Dose-Response Relationship, Drug, Humans, Ibuprofen pharmacology, Indicators and Reagents analysis, Indicators and Reagents metabolism, Inhibitory Concentration 50, Kinetics, Luminol analogs & derivatives, Luminol metabolism, Membrane Proteins, Recombinant Proteins metabolism, Sensitivity and Specificity, Thiophenes pharmacology, Time Factors, Cyclooxygenase Inhibitors pharmacology, Isoenzymes metabolism, Luminol analysis, Peroxidases metabolism, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

The inducible form of the heme-protein prostaglandin G/H synthase (PGHS-2 or COX-2) has been established as a pivotal enzyme in the cascade of events leading to inflammation, hyperalgesia, and pyresis and represents a major therapeutic target in inflammatory disease. Accordingly, we have exploited the heme-catalyzed hydroperoxidase activity of recombinant hCOX-2 to generate luminescence in the presence of luminol, or a cyclic naphthalene hydrazide, and the substrate arachidonic acid. Arachidonate-induced luminescence was shown to be an index of real-time catalytic activity and demonstrated the turnover inactivation of the enzyme. Luminol luminescence was proportional to hCOX-2 concentration and gave accurate Km determinations for arachidonate. Inhibition of hCOX-2 activity, measured by luminescence, by a variety of selective (for COX-2) and nonselective inhibitors showed rank orders of potency similar to those observed with other in vitro and whole cell methods using the recombinant protein. The sensitivity of the luminescence assay also allowed determination of inhibitor potency at substrate concentrations below Km, distinguishing competitive inhibitors such as ibuprofen from time-dependent inhibitors such as DuP-697. Finally the use of higher quantum-yielding luminol analogues allowed measurement of cyclooxygenase activity at extremely low substrate and protein concentrations, enabling a variety of novel assay formats.

Published

1998

59. Zinc dependent activation of cAMP-specific phosphodiesterase (PDE4A).

Author

Percival MD, Yeh B, and Falgueyret JP

Subjects

3',5'-Cyclic-AMP Phosphodiesterases isolation & purification, Cations, Divalent pharmacology, Chromatography, Gel, Chromatography, Ion Exchange, Enzyme Activation, Humans, Kinetics, Magnesium pharmacology, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Zinc metabolism, 3',5'-Cyclic-AMP Phosphodiesterases metabolism, Zinc pharmacology

Abstract

Cyclic nucleotide phosphodiesterases (PDE), including PDE4A, contain two consensus sequences (HX3HX24-26E) which have been associated with Zn2+ binding and activation with other proteins. This study shows that Zn2+ activates purified recombinant human PDE4A with an EC50 of <1 microM. The EC50 for Mg2+, the generally accepted activating metal ion, is approximately 100 microM. Zn2+ concentrations higher than 5 microM are inhibitory. Mn2+, Co2+ and Ni2+ also activate PDE4A with EC50 values of approximately 2, 3 and 10 microM, respectively. PDE4A binds 65Zn2+ with a Kd of 0.4 microM and approximately 1:1 stoichiometry. Titrations of PDE4A inhibition with Mg2+ and Zn2+ as activating metal ions showed that the competitive inhibitors R-Rolipram, CDP-840, RS-14203 and KF18280 are shifted at least 10-fold to lower potency in the presence of Zn2+. The effect is likely at the site of inhibitor binding as the Km for cAMP in the presence of Mg2+ and Zn2+ is similar (1-3 microM). The Kd of [3H]-R-Rolipram for PDE4A was increased at least 30-fold from 3 nM (with Mg2+) by the presence of Zn2+. The high affinity of Zn2+ for PDE4A indicates that this metal may play a role in the regulation of PDE4A activity., (Copyright 1997 Academic Press.)

Published

1997

60. The interaction of arginine 106 of human prostaglandin G/H synthase-2 with inhibitors is not a universal component of inhibition mediated by nonsteroidal anti-inflammatory drugs.

Author

Greig GM, Francis DA, Falgueyret JP, Ouellet M, Percival MD, Roy P, Bayly C, Mancini JA, and O'Neill GP

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Arginine chemistry, CHO Cells drug effects, Chromatography, High Pressure Liquid, Cricetinae, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Dose-Response Relationship, Drug, Humans, Immunoblotting, Isoenzymes drug effects, Isoenzymes metabolism, Membrane Proteins, Mutagenesis, Site-Directed, Prostaglandin-Endoperoxide Synthases drug effects, Prostaglandin-Endoperoxide Synthases metabolism, Transfection, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes genetics, Prostaglandin-Endoperoxide Synthases genetics

Abstract

The three-dimensional cocrystal structures of ovine prostaglandin G/H synthase-1 (PGHS-1) with S-flurbiprofen and murine PGHS-2 with S-flurbiprofen and indomethacin reveal that the carboxylate acid groups of these nonsteroidal anti-inflammatory drugs (NSAIDs) form a salt bridge with the guanidinium group of Arg120 in PGHS-1 and Arg106 in PGHS-2. Mutagenesis studies confirmed that the Arg120 residue of PGHS-1 is critical for binding of substrate and inhibitors through ionic interactions of its guanidinium group with the carboxylate moieties of arachidonic acid and certain NSAIDs. We report here that the analogous R106E substitution in human PGHS-2 results in a catalytically active enzyme with a 30-fold higher Km value for arachidonic acid. Comparison of the inhibition of hPGHS-2(R106E) with wild-type hPGHS-2 by 11 structurally diverse selective and nonselective PGHS inhibitors revealed a 0-1000-fold decrease in inhibitory potency on the mutant enzyme. The loss of inhibitory potency of NSAIDs on hPGHS-2(R106E) could not be correlated with the presence or absence of a carboxylate functional group in the inhibitor, as was demonstrated previously for the PGHS-1(R120E) mutant, or with the selective or nonselective nature of the PGHS inhibitor. The decreases in the inhibitory potencies on hPGHS-2(R106E) by the carboxylate-containing NSAIDs flurbiprofen, indomethacin, meclofenamic acid, and diclofenac on hPGHS-2(R106E) were 965-, 48-, 5.5-, and 4.5-fold, respectively. The nonuniversal requirement for interaction of the carboxylate group of certain NSAIDs with the Arg106 residue in hPGHS-2 is supported by the observation that the methyl ester derivative of indomethacin was a more potent inhibitor than indomethacin on both hPGHS-2 and hPGHS-2(R106E). The greatest loss of potency for inhibition of hPGHS-2(R106E) was observed with the hPGHS-2-selective sulfonamide-containing inhibitors NS-398 and flosulide. The PGHS-2-selective inhibitor DuP697 and a desbromo-sulfonamide analogue of DuP697 displayed equivalent potency on hPGHS-2(R106E) and hPGHS-2. The change in inhibitory potency of NS-398 on hPGHS-2(R106E) was due to a difference in the kinetics of inhibition, with NS-398 displaying time-dependent inhibition of hPGHS-2 but time-independent inhibition of PGHS-2(R106E). The time-dependent inhibition of hPGHS-2 by DuP697 was not affected by the presence of the R106E mutation. We conclude that the Arg106 residue of hPGHS-2 is involved in binding arachidonic acid and certain NSAIDs, but interactions with Arg106 are not a universal requirement for inhibition by either carboxylate-containing NSAIDs or PGHS-2-selective inhibitors.

Published

1997

61. Biochemical and pharmacological profile of a tetrasubstituted furanone as a highly selective COX-2 inhibitor.

Author

Riendeau D, Percival MD, Boyce S, Brideau C, Charleson S, Cromlish W, Ethier D, Evans J, Falgueyret JP, Ford-Hutchinson AW, Gordon R, Greig G, Gresser M, Guay J, Kargman S, Léger S, Mancini JA, O'Neill G, Ouellet M, Rodger IW, Thérien M, Wang Z, Webb JK, Wong E, and Chan CC

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, CHO Cells cytology, CHO Cells drug effects, Cricetinae, Cyclooxygenase 1, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Cyclooxygenase Inhibitors administration & dosage, Cyclooxygenase Inhibitors therapeutic use, Digestive System drug effects, Dinoprostone biosynthesis, Dose-Response Relationship, Drug, Edema drug therapy, Fever drug therapy, Furans administration & dosage, Furans therapeutic use, Humans, Hyperalgesia drug therapy, Indomethacin toxicity, Isoenzymes blood, Isoenzymes drug effects, Lipopolysaccharides toxicity, Male, Membrane Proteins, Peroxidases metabolism, Prostaglandin-Endoperoxide Synthases blood, Prostaglandin-Endoperoxide Synthases drug effects, Rats, Rats, Sprague-Dawley, Recombinant Proteins metabolism, Saimiri, Structure-Activity Relationship, Thromboxane B2 biosynthesis, Transfection, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Furans pharmacology, Isoenzymes metabolism, Peroxidases antagonists & inhibitors, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

1. DFU (5,5-dimethyl-3-(3-fluorophenyl)-4-(4-methylsulphonyl)phenyl-2(5H)-furan one) was identified as a novel orally active and highly selective cyclo-oxygenase-2 (COX-2) inhibitor. 2. In CHO cells stably transfected with human COX isozymes, DFU inhibited the arachidonic acid-dependent production of prostaglandin E2 (PGE2) with at least a 1,000 fold selectivity for COX-2 (IC50 = 41 +/- 14 nM) over COX-1 (IC50 > 50 microM). Indomethacin was a potent inhibitor of both COX-1 (IC50 = 18 +/- 3 nM) and COX-2 (IC50 = 26 +/- 6 nM) under the same assay conditions. The large increase in selectivity of DFU over indomethacin was also observed in COX-1 mediated production of thromboxane B2 (TXB2) by Ca2+ ionophore-challenged human platelets (IC50 > 50 microM and 4.1 +/- 1.7 nM, respectively). 3. DFU caused a time-dependent inhibition of purified recombinant human COX-2 with a Ki, value of 140 +/- 68 microM for the initial reversible binding to enzyme and a kappa 2 value of 0.11 +/- 0.06 s-1 for the first order rate constant for formation of a tightly bound enzyme-inhibitor complex. Comparable values of 62 +/- 26 microM and 0.06 +/- 0.01 s-1, respectively, were obtained for indomethacin. The enzyme-inhibitor complex was found to have a 1:1 stoichiometry and to dissociate only very slowly (t1/2 = 1-3 h) with recovery of intact inhibitor and active enzyme. The time-dependent inhibition by DFU was decreased by co-incubation with arachidonic acid under non-turnover conditions, consistent with reversible competitive inhibition at the COX active site. 4. Inhibition of purified recombinant human COX-1 by DFU was very weak and observed only at low concentrations of substrate (IC50 = 63 +/- 5 microM at 0.1 microM arachidonic acid). In contrast to COX-2, inhibition was time-independent and rapidly reversible. These data are consistent with a reversible competitive inhibition of COX-1. 5. DFU inhibited lipopolysaccharide (LPS)-induced PGE2 production (COX-2) in a human whole blood assay with a potency (IC50 = 0.28 +/- 0.04 microM) similar to indomethacin (IC50 = 0.68 +/- 0.17 microM). In contrast, DFU was at least 500 times less potent (IC50 > 97 microM) than indomethacin at inhibiting coagulation-induced TXB2 production (COX-1) (IC50 = 0.19 +/- 0.02 microM). 6. In a sensitive assay with U937 cell microsomes at a low arachidonic acid concentration (0.1 microM), DFU inhibited COX-1 with an IC50 value of 13 +/- 2 microM as compared to 20 +/- 1 nM for indomethacin. CGP 28238, etodolac and SC-58125 were about 10 times more potent inhibitors of COX-1 than DFU. The order of potency of various inhibitors was diclofenac > indomethacin approximately naproxen > nimesulide approximately meloxicam approximately piroxicam > NS-398 approximately SC-57666 > SC-58125 > CGP 28238 approximately etodolac > L-745,337 > DFU. 7. DFU inhibited dose-dependently both the carrageenan-induced rat paw oedema (ED50 of 1.1 mg kg-1 vs 2.0 mg kg-1 for indomethacin) and hyperalgesia (ED50 of 0.95 mg kg-1 vs 1.5 mg kg-1 for indomethacin). The compound was also effective at reversing LPS-induced pyrexia in rats (ED50 = 0.76 mg kg-1 vs 1.1 mg kg-1 for indomethacin). 8. In a sensitive model in which 51Cr faecal excretion was used to assess the integrity of the gastrointestinal tract in rats, no significant effect was detected after oral administration of DFU (100 mg kg-1, b.i.d.) for 5 days, whereas chromium leakage was observed with lower doses of diclofenac (3 mg kg-1), meloxicam (3 mg kg-1) or etodolac (10-30 mg kg-1). A 5 day administration of DFU in squirrel monkeys (100 mg kg-1) did not affect chromium leakage in contrast to diclofenac (1 mg kg-1) or naproxen (5 mg kg-1). 9. The results indicate that COX-1 inhibitory effects can be detected for all selective COX-2 inhibitors tested by use of a sensitive assay at low substrate concentration. The novel inhibitor DFU shows the lowest inhibitory potency against COX-1, a consistent high selectivity of inhibition of COX-2 over COX-1 (>300 fold) with enzyme, whole cell and whole blood assays, with no detectable loss of integrity of the gastrointestinal tract at doses >200 fold higher than efficacious doses in models of inflammation, pyresis and hyperalgesia. These results provide further evidence that prostanoids derived from COX-1 activity are not important in acute inflammatory responses and that a high therapeutic index of anti-inflammatory effect to gastropathy can be achieved with a selective COX-2 inhibitor.

Published

1997

62. Investigation of human cyclooxygenase-2 glycosylation heterogeneity and protein expression in insect and mammalian cell expression systems.

Author

Percival MD, Bastien L, Griffin PR, Kargman S, Ouellet M, and O'Neill GP

Subjects

Animals, Baculoviridae genetics, Base Sequence, COS Cells, Carbohydrate Sequence, Cell Line, Consensus Sequence, Cyclooxygenase 2, Drosophila, Gene Expression, Glycosylation, Humans, Mass Spectrometry, Membrane Proteins, Molecular Sequence Data, Molecular Structure, Mutagenesis, Site-Directed, Oligodeoxyribonucleotides genetics, Oligosaccharides chemistry, Oligosaccharides genetics, Point Mutation, Recombinant Proteins chemistry, Recombinant Proteins genetics, Spodoptera, Vaccinia virus genetics, Isoenzymes chemistry, Isoenzymes genetics, Prostaglandin-Endoperoxide Synthases chemistry, Prostaglandin-Endoperoxide Synthases genetics

Abstract

Human cyclooxygenase-2 (hCox-2) is a key enzyme in the biosynthesis of prostaglandins and the target of nonsteroidal anti-inflammatory drugs. Recombinant hCox-2 overexpressed in a vaccinia virus (VV)-COS-7 system comprises two glycoforms. Removal of the N-glycosylation consensus sequence at Asn580 (N580Q and S582A mutants) resulted in the expression of protein comprising a single glycoform, consistent with the partial N-glycosylation at this site in the wild-type (WT) enzyme. The specific cyclooxygenase activities of the purified WT and N580Q mutant were equivalent (40 +/- 3 mumol O2/min/mg) and titrations with diclofenac showed no difference in inhibitor sensitivities of WT and both mutants. Results of the expression of WT and N580Q hCox-2 in a Drosophila S2 cell system were also consistent with the N-glycosylation at this site, but low levels of activity were obtained. High levels of N-glycosylation heterogeneity are observed in hCox-2 expressed using recombinant baculovirus (BV) in Sf9 cells. Expression of a double N-glycosylation site mutant in Sf9 cells, N580Q/N592Q, resulted in a decrease in glycosylation but no clear decrease in heterogeneity, indicating that the high degree of N-glycosylation heterogeneity observed with the BV-Sf9 system is not due to partial glycosylation of both Asn580 and Asn592. N-linked oligosaccharide profiling of purified VV and BV WT and S582A mutant hCox-2 showed the presence of high mannose structures, (Man)n (GlcNAc)2, n = 9, 8, 7, 6. The S582A mutant was the most homogeneous with (Man)9(GlcNAc)2 comprising greater than 50% of oligosaccharides present. Analysis of purified VV WT and S582A mutant hCox-2 by liquid chromatography-electrospray ionization-mass spectrometry showed an envelope of peaks separated by approximately 160 Da, corresponding to differences of a single monosaccharide. The difference between the highest mass peaks of the two envelopes, of approximately 1500 Da, is consistent with the wild-type enzyme containing an additional high mannose oligosaccharide.

Published

1997

63. Inhibitor-induced changes in the intrinsic fluorescence of human cyclooxygenase-2.

Author

Houtzager V, Ouellet M, Falgueyret JP, Passmore LA, Bayly C, and Percival MD

Subjects

Acetylation, Animals, Baculoviridae genetics, Cell Line, Cyclooxygenase 2, Cyclooxygenase 2 Inhibitors, Humans, Kinetics, Membrane Proteins, Recombinant Proteins chemistry, Recombinant Proteins genetics, Spectrometry, Fluorescence, Spodoptera, Tryptophan chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes chemistry, Prostaglandin-Endoperoxide Synthases chemistry

Abstract

The steady state tryptophan fluorescence of apo-human cyclooxygenase-2 (hCox-2) is quenched approximately 40%-50% by the slow binding inhibitors diclofenac, indomethacin, ketoprofen, NS-398, and DuP-697. The effects of these inhibitors on tryptophan fluorescence are both time and concentration dependent. Addition of each inhibitor results in a rapid fluorescence decrease, followed by a slower time dependent quenching. The slow, time dependent loss of fluorescence follows first-order kinetics, the rate constants for the process increasing with inhibitor concentration in a saturation-type manner. The rapid fluorescence loss also increases with increasing inhibitor concentration in the same manner. These results are consistent with the initial formation of a rapid equilibrium complex of enzyme and inhibitor (EI), followed by the slower formation of a tightly bound enzyme-inhibitor complex (EI*). The fluorescence of the EI complex is not significantly different from that of the EI* complex. The kinetic parameters of each inhibitor derived for this process (Ki and kon) are close to those obtained by determination of the rate constants for the onset of enzyme inhibition, thereby linking the fluorescence changes with inhibitor binding. The reversible inhibitors ibuprofen and docosahexaenoic acid do not quench the protein fluorescence but do decrease both the rate of the slow fluorescence loss and the magnitude of the initial rapid fluorescence decrease caused by the slow binding inhibitors, consistent with their competitive behavior. ASA-acetylated apo-hCox-2 shows the same fluorescence-quenching behavior in the presence of most of the above inhibitors. However, acetylation apparently blocks the binding of diclofenac, whereas the affinity of ibuprofen is increased. The effects of the collisional quenching agents iodide and acrylamide on both the native and inhibited enzyme are small (< 20% quenching at 0.3 M), showing that inhibitor binding does not result in an increased solvent accessibility of protein tryptophans. The cause of the inhibitor-induced quenching of the intrinsic apo-hCox-2 fluorescence is likely energy transfer to the bound inhibitor. Calculations based on the inhibitor-tryptophan distances in ovine Cox-1 indicate that the distances are within the required range for significant quenching to occur.

Published

1996

64. Effect of inhibitor time-dependency on selectivity towards cyclooxygenase isoforms.

Author

Ouellet M and Percival MD

Subjects

Cyclooxygenase Inhibitors metabolism, Dose-Response Relationship, Drug, Flurbiprofen metabolism, Flurbiprofen pharmacology, Humans, Indomethacin metabolism, Indomethacin pharmacology, Kinetics, Meclofenamic Acid metabolism, Meclofenamic Acid pharmacology, Nitrobenzenes administration & dosage, Nitrobenzenes metabolism, Nitrobenzenes pharmacology, Recombinant Proteins, Sulfonamides administration & dosage, Sulfonamides metabolism, Sulfonamides pharmacology, Cyclooxygenase Inhibitors pharmacology, Isoenzymes metabolism, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

Cyclooxygenase (Cox) is a key enzyme in the biosynthesis of prostaglandins and, as such, is the target of non-steroidal anti-inflammatory drugs (NSAIDs). Two isoforms exist, being expressed constitutively (Cox-1), or inducibly in response to inflammatory mediators (Cox-2). Currently available NSAIDs inhibit both isoforms somewhat equipotently but selective Cox-2 inhibition may eliminate unwanted side effects. We have characterized the kinetic mechanisms of the interactions of purified recombinant human cyclooxygenase-1 and -2 (hCox-1, hCox-2) with the selective Cox-2 inhibitor N-(2-cyclohexyloxy-4-nitrophenyl)methanesulphonamide (NS-398) and some classical non-selective NSAIDs. NS-398, flurbiprofen, meclofenamic acid and indomethacin are time-dependent, irreversible inhibitors of hCox-2. The inhibition is consistent with a two-step process, involving an initial rapid equilibrium binding of enzyme and inhibitor, characterized by Ki, followed by the slow formation of a tightly bound enzyme-inhibitor complex, characterized by a first-order rate constant kon. NS-398 is a time-independent inhibitor of hCox-1, consistent with the formation of a reversible enzyme-inhibitor complex. Flurbiprofen, meclofenamic acid and indomethacin are also time-dependent inhibitors of hCox-1 and hence show little selectivity for one isoform over the other. Flufenamic acid is time independent towards both isoforms and is also non-selective. The high degree of selectivity of NS-398 towards Cox-2 results therefore from the difference in the nature of the time-dependency of inhibition of the two isoforms.

Published

1995

65. Purification and characterization of recombinant human cyclooxygenase-2.

Author

Percival MD, Ouellet M, Vincent CJ, Yergey JA, Kennedy BP, and O'Neill GP

Subjects

Arachidonic Acid metabolism, Baculoviridae genetics, Detergents pharmacology, Fatty Acids, Unsaturated metabolism, Heme metabolism, Humans, Molecular Weight, Oxygen metabolism, Oxygenases metabolism, Peroxidases metabolism, Prostaglandin-Endoperoxide Synthases genetics, Prostaglandin-Endoperoxide Synthases isolation & purification, Protein Conformation, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Spectrophotometry, Substrate Specificity, Vaccinia virus genetics, Prostaglandin-Endoperoxide Synthases metabolism

Abstract

Recombinant human cyclooxygenase-2 (hCox-2, Prostaglandin G/H synthase-2) has been purified from baculovirus-Sf9 and vaccina virus-Cos-7 cell expression systems. The detergent-solubilized, purified enzyme is heterogeneous in terms of its glycosylation. The vaccinia virus hCox-2 is a mixture of two glycoforms, whereas baculovirus hCox-2 comprises at least four species. The specific cyclooxygenase activities of both enzymes are 43 mumol O2/min/mg with arachidonic acid which is within the range of values reported for ovine Cox-1. The Km values of arachidonic acid for hCox-2 and ovine Cox-1 are 0.9 and 2.7 microM, respectively. Six other C-18 and C-20 fatty acids containing at least one 1,4-cis,cis-pentadiene moiety were also identified as substrates for hCox-2. Linoleic and gamma-linolenic acid were determined by mass spectrometry as being hydroxylated primarily at the C-9 and C-13 positions, whereas linolenic acid was hydroxylated primarily at the C-12 and C-16 positions. hCox-2 binds heme such that maximal activity is observed at a stoichiometry of 1.0 heme per enzyme subunit. The apparent molecular mass of hCox-2, determined by gel filtration chromatography in the presence of 2.0% beta-octylglucoside, is consistent with a dimeric structure. The results of this study indicate that the physical and catalytic properties of recombinant hCox-2 are very similar to that of the extensively studied ovine Cox-1.

Published

1994

66. High-level expression of active human cyclooxygenase-2 in insect cells.

Author

Cromlish WA, Payette P, Culp SA, Ouellet M, Percival MD, and Kennedy BP

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Baculoviridae genetics, Base Sequence, Cell Line, Cloning, Molecular, Cyclooxygenase Inhibitors pharmacology, DNA, Complementary genetics, Glycoside Hydrolases pharmacology, Glycosylation, Humans, Hydroxyeicosatetraenoic Acids biosynthesis, Microsomes enzymology, Molecular Sequence Data, Prostaglandin-Endoperoxide Synthases metabolism, Recombinant Proteins, Transfection, Gene Expression, Prostaglandin-Endoperoxide Synthases genetics, Spodoptera metabolism

Abstract

Active human cyclooxygenase-2 (Cox-2) was expressed at high levels in insect cells using a recombinant baculovirus. The specific activity of Cox-2 in the microsomes of infected cells was 0.51 mumol O2/min/mg and was comparable to that obtained for partially purified Cox-2 from ovine placenta (0.55 mumol O2/min/mg). The Cox-2 enzyme expressed in insect cells was glycosylated to varying extents and most of the cyclooxygenase activity was in the high-speed microsomal pellet. The insect-cell-expressed enzyme also showed characteristic 15-hydroxyeicosa-tetraenoic acid production after aspirin treatment and had typical inhibition profiles with a number of known nonsteroidal antiinflammatory drugs.

Published

1994

67. Characterization of the non-heme iron center of human 5-lipoxygenase by electron paramagnetic resonance, fluorescence, and ultraviolet-visible spectroscopy: redox cycling between ferrous and ferric states.

Author

Chasteen ND, Grady JK, Skorey KI, Neden KJ, Riendeau D, and Percival MD

Subjects

Binding Sites, Electron Spin Resonance Spectroscopy, Ferric Compounds chemistry, Ferrous Compounds chemistry, Humans, Nonheme Iron Proteins, Oxidation-Reduction, Spectrometry, Fluorescence, Spectrophotometry, Ultraviolet, Arachidonate 5-Lipoxygenase chemistry, Metalloproteins chemistry

Abstract

Purified human 5-lipoxygenase, a non-heme iron containing enzyme, has been characterized by electron paramagnetic resonance, (EPR), ultraviolet (UV)-visible and fluorescence spectroscopy. As isolated, the enzyme is largely in the ferrous state and shows a weak X-band EPR signal extending from 0 to 700 G at 15 K, tentatively ascribed to integer spin Fe(II). Titration of the protein with 13-HPOD (13-hydroperoxyoctadecadienoic acid) generates a strong multicomponent EPR signal in the g' approximately 6 region, a yellow color associated with an increased absorption between 310 and 450 nm (epsilon 330nm = 2400 M-1 cm-1), and a 17% decrease in the intrinsic protein fluorescence. The multiple component nature of the g' approximately 6 signal indicates that the metal center in its oxidized state exists in more than one but related forms. The g' approximately 6 EPR signal and the yellow color reach a maximum when approximately 1 mol of 13-HPOD is added/mol of iron; the resultant EPR spectrum accounts quantitatively for all of the iron in the protein with a signal at g' = 4.3 representing less than 3% of the total iron in the majority of samples. Addition of a hydroxyurea reducing agent abolished the g' approximately 6 signal and yellow color of the protein and also reversed the decrease in fluorescence caused by the oxidant 13-HPOD. The results indicate that the g' approximately 6 EPR signal, the yellow color, and the decreased fluorescence are associated with the formation of the Fe(III) form of the enzyme.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

68. Investigation of the mechanism of non-turnover-dependent inactivation of purified human 5-lipoxygenase. Inactivation by H2O2 and inhibition by metal ions.

Author

Percival MD, Denis D, Riendeau D, and Gresser MJ

Subjects

Arachidonate 5-Lipoxygenase isolation & purification, Arachidonate 5-Lipoxygenase metabolism, Catalase metabolism, Cations, Divalent, Chromatography, High Pressure Liquid, Dithiothreitol pharmacology, Enzyme Activation, Humans, Kinetics, Leukotrienes biosynthesis, Metalloproteins isolation & purification, Metalloproteins metabolism, Nonheme Iron Proteins, Oxidation-Reduction, Recombinant Proteins antagonists & inhibitors, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Hydrogen Peroxide pharmacology, Lipoxygenase Inhibitors, Metals metabolism

Abstract

Human 5-lipoxygenase is a non-heme iron protein which is reported to be highly unstable in the presence of oxygen. The results of this investigation demonstrate that H2O2 generated during air oxidation of thiols is the main factor in non-turnover-dependent inactivation of purified recombinant human 5-lipoxygenase for the following reasons: catalase protects against oxygen-dependent inactivation of the enzyme in the presence of dithiothreitol; the active, stable enzyme can be prepared under aerobic conditions with the exclusion of dithiothreitol and contaminating metal ions; 10 microM H2O2 causes the rapid inactivation of the enzyme. The native (ferrous) enzyme is approximately seven times more sensitive to inactivation by H2O2 than the ferric enzyme, suggesting that the mechanism of inactivation involves a Fenton-type reaction of the ferrous enzyme with H2O2, resulting in the formation of an activated oxygen species. Purification of 5-lipoxygenase under aerobic conditions (no dithiothreitol) results in an increase in both the specific activity of the purified protein [up to 70 mumol 5(S)-hydroperoxy-6-trans-8, 11, 14-cis-icosatetraenoic acid (5-HPETE)/mg protein] and in the ratio of specific activity to enzyme iron content compared to enzyme purified under anaerobic conditions in the presence of dithiothreitol. The reaction of the highly active 5-lipoxygenase enzyme shows a dependence on physiological intracellular calcium concentrations, half-maximal product formation being obtained at 0.9 microM free Ca2+. The maximal enzyme activity is also dependent on EDTA and dithiothreitol and low amounts of carrier protein, as well as the known activators PtdCho and ATP. Ca2+ can be substituted by Mn2+, Ba2+ and Sr2+, although lower levels of stimulation are obtained. 5-Lipoxygenase is strongly inhibited by low concentrations (< or = 10 microM) of Zn2+ and Cu2+. The inhibition by Cu2+ is apparently irreversible, whereas that by Zn2+ is slowly reversed (t1/2 = 2 min) in the presence of excess EDTA. These observations on the mechanism of non-turnover-dependent inactivation of 5-lipoxygenase, and the optimisation of assay conditions, have facilitated the purification of large quantities of relatively stable enzyme that will be useful for further kinetic and physical studies.

Published

1992

69. The characterization of 5 histidine-serine mutants of human 5-lipoxygenase.

Author

Percival MD and Ouellet M

Subjects

Animals, Arachidonate 5-Lipoxygenase genetics, Baculoviridae genetics, Cell Line, Enzyme Stability, Humans, Insecta, Kinetics, Spectrophotometry, Ultraviolet, Transfection, Arachidonate 5-Lipoxygenase metabolism, Histidine, Mutagenesis, Site-Directed, Serine

Abstract

The physical and catalytic properties of 5 histidine-serine mutants of human 5-lipoxygenase (5-LO) have been characterized. The mutants HS363, HS391 and HS400 have activities, pH optima and stabilities similar to those of the wild type enzyme. The iron content of each of these mutants is 0.30-0.53 mol Fe/mol 5-LO which is within the range observed for the wild type enzyme. HS368 contains iron (0.15 and 0.43 mol Fe/mol 5-LO in 2 preparations) but has no detectable oxygenase, leukotriene A4 synthase or anaerobic arachidonate-dependent hydroperoxidase activities. HS368 does have significant reducing agent-dependent hydroperoxidase activity suggesting that His-368 may not be an iron ligand but rather may be involved in interactions with arachidonic acid or the formation of the arachidonyl radical intermediate. HS373 contains no iron and has no detectable activities.

Published

1992

70. Binding energy and catalysis: deoxyfluoro sugars as probes of hydrogen bonding in phosphoglucomutase.

Author

Percival MD and Withers SG

Subjects

Animals, Catalysis, Deoxyglucose chemical synthesis, Deoxyglucose chemistry, Fluorodeoxyglucose F18, Glucosephosphates pharmacology, Hydrogen Bonding, Kinetics, Phosphoglucomutase antagonists & inhibitors, Protein Binding, Rabbits, Spectrophotometry, Ultraviolet, Substrate Specificity, Thermodynamics, Deoxyglucose analogs & derivatives, Glucose-6-Phosphate analogs & derivatives, Phosphoglucomutase chemistry

Abstract

Estimates of the contributions of hydrogen-bonding interactions with each of the sugar hydroxyls to the binding of the substrate alpha-D-glucopyranosyl phosphate both in the ground state and at the transition state for the initial phosphoryl transfer have been obtained by kinetic studies. Michaelis parameters (kcat and Km) for a complete series of deoxy- and deoxyfluoro-alpha-D-glucopyranosyl phosphates provide insight into specific interactions with each hydroxyl at the transition state. Inhibition constants (Ki) for a series of deoxygenated and fluorinated analogues of the competitive inhibitor 6-deoxy-6-fluoro-alpha-D-glucopyranosyl phosphate provide insight into ground-state interactions. Interactions at each hydroxyl are found to strengthen only slightly upon progressing from the ground state to the transition state in contrast to that seen with glycogen phosphorylase [Street et al. (1989) Biochemistry 28, 1581] where transition-state interactions became much stronger. This is in accord with the mechanisms for these two enzymes where no distortion of the sugar ring occurs for phosphoglucomutase, whereas considerable distortion is expected for glycogen phosphorylase.

Published

1992

71. 19F NMR investigations of the catalytic mechanism of phosphoglucomutase using fluorinated substrates and inhibitors.

Author

Percival MD and Withers SG

Subjects

Animals, Cadmium pharmacology, Catalysis, Deoxyglucose analogs & derivatives, Deoxyglucose pharmacology, Fluorine, Glucosephosphates pharmacology, Magnetic Resonance Spectroscopy, Phosphoglucomutase antagonists & inhibitors, Protein Binding, Rabbits, Substrate Specificity, Glucose-6-Phosphate analogs & derivatives, Glucosephosphates chemistry, Phosphoglucomutase chemistry

Abstract

The complexes of phosphoglucomutase with a number of fluorinated substrate analogues have been investigated by 19F NMR and the effects of the binding of Li+ and Cd2+ to these complexes determined. Very large downfield chemical shift changes (-14 to -19 ppm) accompanied binding of the inhibitors 6-deoxy-6-fluoro-alpha-D-glucopyranosyl phosphate and alpha-glucosyl fluoride 6-phosphate to the phosphoenzyme. Smaller shift changes were observed for ligands substituted with fluorine at other positions. Addition of Li+ to enzyme/fluorinated ligand complexes caused a 10(2)- to 10(3)-fold decrease in ligand dissociation constants as witnessed by the change from intermediate to slow-exchange conditions in the NMR spectra. Measurement of the 19F NMR spectra of complexes of the Li(+)-enzyme with each of the fluoroglucose 1-phosphates and 6-phosphates has provided some insight into the environment of each of these fluorines (thus also parent hydroxyls) in each of the complexes. Results obtained argue strongly against a single sugar binding mode for the glucose 1- and 6-phosphates. Two enzyme-bound species were detected in the 19F NMR spectra of the complexes formed by reaction of the Cd(2+)-phosphoenzyme complex with the 2- and 3-fluoroglucose phosphates. These are tentatively assigned as the fluoroglucose 1,6-bisphosphate species bound in two different modes to the dephosphoenzyme. Only one bound species was observed in the case of the 4-fluoroglucose phosphates.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1992

72. Human 5-lipoxygenase contains an essential iron.

Author

Percival MD

Subjects

Arachidonate 5-Lipoxygenase metabolism, Chromatography, Affinity, Humans, Lipoxygenase Inhibitors, Protein Conformation, Arachidonate 5-Lipoxygenase chemistry, Iron chemistry

Abstract

The iron content of human 5-lipoxygenase has been determined by a colorimetric assay using the chromogenic ligand FerroZine. The highly active enzyme was obtained from a baculovirus expression system and purified using an ATP-agarose chromatography column (Denis, D., Falgueyret, J.-P., Riendeau, D., and Abramovitz, M. (1991) J. Biol. Chem. 266, 5072-5079). A linear correlation was observed between the enzyme's specific activity and iron content in six different preparations. Enzyme with the highest specific activity (24 mumol of 5-hydroperoxyeicosatetraenoic acid/mg of protein) contained 1.1 mol of iron/mol of enzyme, whereas inactive enzyme contained no detectable iron. The iron is tightly bound to the enzyme and could only be released after inactivation of the enzyme by exposure to oxygen.

Published

1991

73. TUMORS--Oncology Registry System.

Author

Percival MD

Subjects

Humans, Microcomputers, Software, Databases, Factual, Neoplasms, Registries

Abstract

The TUMORS Oncology Registry database and functionality has been designed in cooperation with Certified Tumor Registrars and Oncologists, exceeding current American College of Surgeons requirements. The Networked Data Management System provides secure in-house registry functions with additional benefits of Central Databases for Case Consolidation, Shared Followup and Biostatistical Functions. The system used readily available Microcomputer Technologies and is developed from a Sound Background of experience in Networked, Consortium Oriented Oncology Registries. Using the latest in microcomputer LAN Compatible Database Management Systems, the system embodies the Most Recent Generation of Oncology Registry Software and is currently enjoying its first year of implementation. The demonstration includes examples of Data Entry, Query, Report and Statistical Functions operating on an IBM AT Compatible PC connected to a Laser Printer.

Published

1991

74. Inhibition of phosphoglucomutase by vanadate.

Author

Percival MD, Doherty K, and Gresser MJ

Subjects

Glucose-6-Phosphate, Glucosephosphates metabolism, Leuconostoc drug effects, Leuconostoc enzymology, Phosphoglucomutase antagonists & inhibitors, Vanadates pharmacology

Abstract

Phosphoglucomutase is inhibited by a complex formed from alpha-D-glucose 1-phosphate (Glc-1-P) and inorganic vanadate (Vi). Both the inhibition at steady state and the rate of approach to steady state are dependent on the concentrations of both Glc-1-P and Vi. Inhibition is competitive versus alpha-D-glucose 1,6-bisphosphate (Glc-P2) and is ascribed to binding of the 6-vanadate ester of Glc-1-P (V-6-Glc-1-P) to the dephospho form of phosphoglucomutase (E). The inhibition constant for V-6-Glc-1-P at pH 7.4 was determined from steady-state kinetic measurements to be 2 x 10(-12) M. The first-order rate constant for approach to steady state increases hyperbolically with inhibitor concentration. The results are consistent with rapid equilibrium binding of V-6-Glc-1-P to E, with dissociation constant 1 x 10(-9) M, followed by rate-limiting conversion of the E.V-6-Glc-1-P complex to another species, E*.V-6-Glc-1-P, with first-order rate constant 4 x 10(-2)s-1. The rate constant determined for the reverse reaction, conversion of E*.V-6-Glc-1-P to E.V-6-Glc-1-P, is 2.5 x 10(-4)s-1. Formation of E*.V-6-Glc-1-P can also occur via binding of glucose 6-vanadate to the phospho form of phosphoglucomutase (E-P) followed by phosphoryl transfer and rearrangement of the enzyme-product complex.

Published

1990