Your search keyword '"Marta L. Capone"' showing total 35 results

1. Risk management profile of etoricoxib: an example of personalized medicine

Author

Paola Patrignani, Stefania Tacconelli, and Marta L Capone

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Paola Patrignani, Stefania Tacconelli, Marta L CaponeDepartment of Medicine and Center of Excellence on Aging, “G. D’Annunzio” University School of Medicine, and “Gabriele D’Annunzio” University Foundation, CeSI, Chieti, ItalyAbstract: The development of nonsteroidal anti-inflammatory drugs (NSAIDs) selective for cyclooxygenase (COX)-2 (named coxibs) has been driven by the aim of reducing the incidence of serious gastrointestinal (GI) adverse events associated with the administration of traditional (t) NSAIDs – mainly dependent on the inhibition of COX-1 in GI tract and platelets. However, their use has unravelled the important protective role of COX-2 for the cardiovascular (CV) system, mainly through the generation of prostacyclin. In a recent nested-case control study, we found that patients taking NSAIDs (both coxibs and tNSAIDs) had a 35% increase risk of myocardial infarction. The increased incidence of thrombotic events associated with profound inhibition of COX-2-dependent prostacyclin by coxibs and tNSAIDs can be mitigated, even if not obliterated, by a complete suppression of platelet COX-1 activity. However, most tNSAIDs and coxibs are functional COX-2 selective for the platelet (ie, they cause a profound suppression of COX-2 associated with insufficient inhibition of platelet COX-1 to translate into inhibition of platelet function), which explains their shared CV toxicity. The development of genetic and biochemical markers will help to identify the responders to NSAIDs or who are uniquely susceptible at developing thrombotic or GI events by COX inhibition. We will describe possible strategies to reduce the side effects of etoricoxib by using biochemical markers of COX inhibition, such as whole blood COX-2 and the assessment of prostacyclin biosynthesis in vivo.Keywords: etoricoxib, nonsteroidal antiinflammatory drugs, COX-2, gastrointestinal toxicity, cardiovascular toxicity, prostacyclin

Published

2008

2. Reduced Variability to Aspirin Antiplatelet Effect by the Coadministration of Statins in High-Risk Patients for Cardiovascular Disease

Author

Alessandra Meneguzzi, L. Grossi, Luigia Di Francesco, Annalisa Bruno, Ettore Porreca, Patrizia Ballerini, Stefano Manarini, Cristiano Fava, Giacomo Levantesi, Paola Patrignani, Concetta Di Febbo, Marta L. Capone, Melania Dovizio, Virgilio Evangelista, Pietro Minuz, Stefania Tacconelli, and Ilaria D'Agostino

Subjects

Male, 0301 basic medicine, Thromboxane, Atorvastatin, thromboxane A2, 030204 cardiovascular system & hematology, Gastroenterology, Thromboxane A2, chemistry.chemical_compound, 0302 clinical medicine, Risk Factors, cardiovascular disease, Secondary Prevention, MRP4, cyclooxygenase-1, low-dose aspirin, platelets, statins, Medicine, Pharmacology (medical), Platelet, Aspirin, Acetylation, Middle Aged, Primary Prevention, Thromboxane B2, Cardiovascular Diseases, Platelet aggregation inhibitor, Drug Therapy, Combination, Female, lipids (amino acids, peptides, and proteins), Tablets, Enteric-Coated, medicine.drug, Blood Platelets, medicine.medical_specialty, Statin, medicine.drug_class, Biological Availability, In Vitro Techniques, 03 medical and health sciences, Internal medicine, Humans, Aged, Pharmacology, business.industry, 030104 developmental biology, chemistry, Cyclooxygenase 1, Hydroxymethylglutaryl-CoA Reductase Inhibitors, business, Platelet Aggregation Inhibitors

Abstract

We studied the influence of cardiovascular (CV) risk factors, previous CV events, and cotreatments with preventive medicines, on residual platelet thromboxane (TX)B2 production in 182 patients chronically treated with enteric coated (EC)-aspirin (100 mg/day). The response to aspirin was also verified by assessing arachidonic acid-induced platelet aggregation and urinary 11-dehydro-TXB2 levels. Residual serum TXB2 levels exceeded the upper limit value for an adequate aspirin response in 14% of individuals. This phenomenon was detected at 12 hours after dosing with aspirin. The coadministration of statins (mostly atorvastatin) was an independent predictor of residual serum TXB2 levels, and the percentage of patients with enhanced values was significantly lower in statin users vs. nonusers. We provide evidence in vitro that atorvastatin reduced residual TXB2 generation by increasing the extent of acetylation of platelet COX-1 by aspirin. In conclusion, the coadministration of statins may counter the mechanisms associated with reduced bioavailability of aspirin detected in some individuals with CV disease.

Published

2018

3. Differential association between human prostacyclin receptor polymorphisms and the development of venous thrombosis and intimal hyperplasia: a clinical biomarker study

Author

Scott Gleim, John Hwa, Kent Sierra, Min Ding, Ryan J. Horvath, Stefania Tacconelli, Valeria Moretta, Maria Domenica Guglielmi, Luigia Di Francesco, Jeremiah Stitham, Giovanna Baccante, Paola Patrignani, Karen Douville, Concetta Di Febbo, Marta L. Capone, and Ettore Porreca

Subjects

Adult, Male, medicine.medical_specialty, Intimal hyperplasia, Genetic Linkage, Prostacyclin, Receptors, Epoprostenol, Polymorphism, Single Nucleotide, Von Willebrand factor, Internal medicine, Genetics, medicine, Humans, Platelet, Genetic Testing, Platelet activation, General Pharmacology, Toxicology and Pharmaceutics, Molecular Biology, Prostacyclin receptor, Genetics (clinical), Aged, Venous Thrombosis, Hyperplasia, biology, business.industry, Middle Aged, Platelet Activation, medicine.disease, Thrombosis, Thromboxane B2, P-Selectin, Venous thrombosis, Endocrinology, biology.protein, Molecular Medicine, Female, Tunica Intima, business, Biomarkers, medicine.drug

Abstract

Objective and methods The role of prostacyclin in the development of venous thrombosis and vascular dysfunction in humans is unclear. In patients with deep vein thrombosis (DVT, n=34) and controls (matched for age, sex, indexes of systemic inflammation and metabolic status, n=20), we studied (i) differences on systemic markers of vascular disease and platelet activation and (ii) the influence of prostacyclin receptor gene (PTGIR) polymorphisms. Main results Enhanced levels of urinary 11 -dehydro-thromboxane (TX)B 2 and plasma [soluble(s)] P-selectin, mostly platelet derived, were detected in DVT patients, whereas plasma von Willebrand factor levels and intima-media thickness of the common carotid arteries were not significantly different. In all patients' cohorts, we identified five PTGIR polymorphisms (three nonsynonymous: P226T, R212C, V196L; two synonymous: V53V, S328S). In the four individuals carriers of R212C polymorphism (three in DVT, one in controls), intima-media thickness values were significantly (P= 0.0043) higher than those detected in individuals of all cohorts [1.68 ±0.38, 1.55 (1.4-2.2) vs. 1.05 ± 0.33, 1.08 (0.01 -1.68) mm, respectively, mean ± SD, median (range)]. Moreover, enhanced sP-selectin and 11-dehydro.TXB 2 , in DVT versus controls, were statistically significant only in carriers of both synonymous PTGIR polymorphisms V53V/S328S. Only the PTGIR mutant R212C was dysfunctional when examined in an in vitro overexpression system. Conclusion Our results suggest a propensity of enhanced platelet activation in DVT patients with PTGIR polymorphisms V53V/S328S. Moreover, we identified a dysfunctional PTGIR polymorphism (R212C) associated with intimal hyperplasia.

Published

2008

4. Cardiovascular effects of valdecoxib: transducing human pharmacology results into clinical read-outs

Author

Marta L. Capone, Paola Patrignani, Stefania Tacconelli, Luigia Di Francesco, and Maria Petrelli

Subjects

Clinical Trials as Topic, Sulfonamides, Aspirin, Clinical pharmacology, Dose-Response Relationship, Drug, business.industry, Analgesic, Prostacyclin, Isoxazoles, General Medicine, Pharmacology, Valdecoxib, law.invention, Diclofenac, Cardiovascular Diseases, Parecoxib, law, Animals, Humans, Medicine, Pharmacology (medical), Antipyretic, business, medicine.drug

Abstract

Valdecoxib is an NSAID that is selective for COX-2 (commonly named coxibs). It exhibits anti-inflammatory, analgesic and antipyretic properties in animal models and humans due to inhibition of prostanoid synthesis primarily by affecting COX-2. In this review, the clinical results of cardiovascular effects of valdecoxib and its prodrug parecoxib were analyzed and the information from animal models and clinical pharmacology was exploited, that is, pharmacodynamic and pharmacokinetic data, to give a mechanistic interpretation. Similarly to other coxibs and some traditional (t)NSAIDs less selective for COX-2, such as diclofenac, valdecoxib may increase the risk of thrombotic events through a prostacyclin-based mechanism. The rapid and elevated thrombotic risk detected in two coronary artery bypass graft surgery trials with parecoxib and valdecoxib is coherent with almost complete suppression of COX-2 by supratherapeutic doses (particularly parecoxib), which plausibly translates into a deep suppression of prostacyclin. Drug potency, that is, the degree of suppression of COX-2-dependent prostacyclin, is proposed to represent a strong determinant in the increased incidence of thrombotic events associated with the use of COX-2 inhibitors and some tNSAIDs.

Published

2008

5. Celecoxib, ibuprofen, and the antiplatelet effect of aspirin in patients with osteoarthritis and ischemic heart disease

Author

Maria Zurro, Thomas S. Price, Raffaele De Caterina, Maria G. Sciulli, Stefania Tacconelli, Francesco Santarelli, Marilena Grana, Daniele Sacchetta, Marco Zimarino, Giulia Renda, Marta L. Capone, Elisabetta D'Amelio, Paola Patrignani, and Carlo Patrono

Subjects

Male, Platelet Aggregation, Platelet Function Tests, Thromboxane, Analgesic, Myocardial Ischemia, Ibuprofen, Pharmacology, Drug Administration Schedule, chemistry.chemical_compound, Double-Blind Method, Osteoarthritis, medicine, Humans, Pharmacology (medical), Antipyretic, Aged, Sulfonamides, Aspirin, Arachidonic Acid, biology, business.industry, Middle Aged, Adenosine Diphosphate, Thromboxane B2, Treatment Outcome, chemistry, Celecoxib, Anesthesia, biology.protein, Pyrazoles, Drug Therapy, Combination, Female, Cyclooxygenase, business, Platelet Aggregation Inhibitors, medicine.drug

Abstract

Background and Objective We performed a placebo-controlled, randomized study to address whether celecoxib or ibuprofen undermines the functional range of inhibition of platelet cyclooxygenase (COX)–1 activity by aspirin in patients with osteoarthritis and stable ischemic heart disease. Methods Twenty-four patients who were undergoing long-term treatment with aspirin (100 mg daily) for cardioprotection were coadministered celecoxib, 200 mg twice daily, ibuprofen, 600 mg 3 times daily, or placebo for 7 days. Results The coadministration of placebo or celecoxib did not undermine the aspirin-related inhibition of platelet COX-1 activity, as assessed by measurements of serum thromboxane B2 (TXB2) levels, as well as platelet function. In contrast, a significant (P < .001) increase in serum TXB2 level was detected on day 7 before drug administration (median, 19.13 ng/mL [range, 1–47.5 ng/mL]) and at 24 hours after the coadministration of aspirin and ibuprofen (median, 22.28 ng/mL [range, 4.9–44.4 ng/mL]) versus baseline (median, 1.65 ng/mL [range, 0.55–79.8 ng/mL]); this was associated with a significant increase in arachidonic acid-induced platelet aggregation (P < .01) and adenosine diphosphate-induced platelet aggregation (P < .05) and a decrease in the time to form an occlusive thrombus in the platelet function analyzer (P < .01). The urinary excretion of 11-dehydro-TXB2, an index of systemic thromboxane biosynthesis, was not significantly affected by the coadministration of treatment drugs. At steady state, a comparable and persistent inhibition of lipopolysaccharide-stimulated prostaglandin E2 generation, a marker of COX-2 activity ex vivo, was caused by ibuprofen (≥80%) or celecoxib (≥70%) but not placebo. Conclusions Unlike ibuprofen, celecoxib did not interfere with the inhibition of platelet COX-1 activity and function by aspirin despite a comparable suppression of COX-2 ex vivo in patients with osteoarthritis and stable ischemic heart disease. Clinical Pharmacology & Therapeutics (2006) 80, 264–274; doi: 10.1016/j.clpt.2006.05.004

Published

2006

6. Heterogeneity in the suppression of platelet cyclooxygenase-1 activity by aspirin in coronary heart disease

Author

Giulia Renda, Marta L. Capone, Paola Patrignani, Virgilio Evangelista, Emanuela Ricciotti, Stefano Manarini, Maria G. Sciulli, S. Tacconelli, and A. G. Rebuzzi

Subjects

Blood Platelets, Lipopolysaccharides, Male, medicine.medical_specialty, Neutrophils, Thromboxane, Coronary Disease, Gastroenterology, Thromboxane A2, Internal medicine, Humans, Medicine, Cyclooxygenase Inhibitors, Pharmacology (medical), Platelet, Myocardial infarction, Antipyretic, Calcimycin, Aged, Whole blood, Pharmacology, Aspirin, Arachidonic Acid, biology, business.industry, Unstable angina, Middle Aged, medicine.disease, Thromboxane B2, Cyclooxygenase 2, Anesthesia, Indans, Cyclooxygenase 1, biology.protein, Female, Cyclooxygenase, business, medicine.drug

Abstract

Background and Objectives Complete and persistent suppression of platelet thromboxane (TX) A2 biosynthesis by aspirin is mandatory to fulfill its cardioprotection. We explored the determinants of heterogeneity of TXB2 generation in clotting whole blood, a capacity index of platelet cyclooxygenase (COX) activity, in patients with coronary heart disease (CHD) versus healthy subjects treated with low-dose aspirin on a long-term basis. Methods We studied 30 patients with CHD (ie, chronic stable angina, unstable angina, and acute myocardial infarction) and 10 healthy subjects, who were treated with low-dose aspirin (100 mg daily) on a long-term basis, 12 hours after the administration of 160 mg aspirin to ensure saturation of platelet COX-1 activity. Serum TXB2 levels were assessed. The contribution of blood COX-2 to TXA2 biosynthesis was explored by evaluation of the effect of a selective COX-2 inhibitor (L-745,337) added to heparinized whole blood stimulated with Ca++ ionophore A23187 (20 μmol/L) for 1 hour or lipopolysaccharide (0.1 μg/mL) for 4 hours. Results In healthy subjects serum TXB2 levels ranged from 0.6 to 7.9 ng/mL (median, 2.1 ng/mL; mean ± SD, 3.2 ± 2.6 ng/mL). In CHD patients we detected enhanced variability in serum TXB2 generation (median, 3.1 ng/mL [range, 0.15–47 ng/mL]; mean, 8.5 ± 12.3 ng/mL), which in 8 patients (27%) exceeded the mean value + 2 SDs detected in healthy subjects (ie, 8.4 ng/mL), set as the limit value for an adequate inhibition of platelet COX-1 by aspirin. Elevated whole-blood TXB2 generation was not dependent on leukocyte count, COX-2 activity, or cigarette smoking but was plausibly a result of defective suppression of platelet COX-1 activity. Conclusions Heterogeneity in the suppression of platelet COX-1 activity by aspirin occurred in CHD patients. The measurement of the serum TXB2 level seems to be an appropriate biomarker to identify patients who have an inadequate inhibition of platelet COX-1 activity by aspirin. Clinical Pharmacology & Therapeutics (2006) 80, 115–125; doi: 10.1016/j.clpt.2006.04.011

Published

2006

7. Pharmacodynamic interaction of naproxen with low-dose aspirin in healthy subjects

Author

Gabriele Merciaro, Emanuela Ricciotti, Paola Patrignani, Patrizia Di Gregorio, Maria G. Sciulli, Giulia Renda, Marta L. Capone, Stefania Tacconelli, and Marilena Grana

Subjects

Adult, Naproxen, Platelet Aggregation, In Vitro Techniques, Pharmacology, Prostaglandin-Endoperoxide Synthase, Pharmacokinetics, medicine, Humans, Drug Interactions, Cardioprotection, Aspirin, business.industry, Arthritis, Anti-Inflammatory Agents, Non-Steroidal, Healthy subjects, Membrane Proteins, Thromboxane B2, Cardiovascular Diseases, Prostaglandin-Endoperoxide Synthases, Pharmacodynamics, Anesthesia, Cyclooxygenase 1, Drug Therapy, Combination, Cardiology and Cardiovascular Medicine, business, Low dose aspirin, medicine.drug

Abstract

ObjectivesWe investigated the occurrence of pharmacodynamic interaction between low-dose aspirin and naproxen.BackgroundThe uncertainty of cardioprotection by naproxen has encouraged its combination with aspirin in patients with arthritis and cardiovascular disease.MethodsThe incubation of washed platelets with naproxen for 5 min before the addition of aspirin reduced the irreversible inhibition of thromboxane (TX)B2production by aspirin. The pharmacodynamic interaction between the two drugs was then investigated in four healthy volunteers who received aspirin (100 mg daily) for 6 days and then the combination of aspirin and naproxen for further 6 days: aspirin 2 h before naproxen (500 mg, twice-daily dosing). After 14 days of washout, naproxen was given 2 h before aspirin for further 6 days.ResultsThe inhibition of serum TXB2production (index of platelet cyclooxygenase [COX]-1 activity) and platelet aggregation ex vivo and urinary 11-dehydro-TXB2levels (index of TXB2biosynthesis in vivo) by aspirin alone (99 ± 0.2%, 95 ± 0.6%, and 81 ± 4%, respectively) was not significantly altered by the co-administration of naproxen, given either 2 h after aspirin or in reverse order. In a second study, the concurrent administration of a single dose of aspirin and naproxen did not affect platelet TXB2production and aggregation at 1 h after dosing, when aspirin alone causes maximal inhibitory effect. Moreover, the rapid recovery of platelet COX-1 activity and function supports the occurrence of a pharmacodynamic interaction between naproxen and aspirin.ConclusionsNaproxen interfered with the inhibitory effect of aspirin on platelet COX-1 activity and function. This pharmacodynamic interaction might undermine the sustained inhibition of platelet COX-1 that is necessary for aspirin’s cardioprotective effects.

Published

2005

8. Clinical Pharmacology of Platelet, Monocyte, and Vascular Cyclooxygenase Inhibition by Naproxen and Low-Dose Aspirin in Healthy Subjects

Author

Carlo Patrono, Gabriele Merciaro, Marilena Grana, Paola Patrignani, Stefania Tacconelli, Maria G. Sciulli, Pietro Minuz, Marta L. Capone, Patrizia Di Gregorio, and Emanuela Ricciotti

Subjects

Adult, Blood Platelets, Male, Naproxen, Cardiotonic Agents, Thromboxane, Prostaglandin, Prostacyclin, 6-Ketoprostaglandin F1 alpha, Pharmacology, Dinoprostone, Monocytes, chemistry.chemical_compound, naproxene, prostaciclina, trombossano, piastrine, monociti, Physiology (medical), Humans, Medicine, Cyclooxygenase Inhibitors, Prostaglandins I, Platelet, Aspirin, Cross-Over Studies, Cyclooxygenase 2 Inhibitors, biology, business.industry, Endothelial Cells, Membrane Proteins, Middle Aged, Isoenzymes, Thromboxane B2, Eicosanoid, chemistry, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Cyclooxygenase 1, biology.protein, Female, Endothelium, Vascular, Cyclooxygenase, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Background—The current controversy on the potential cardioprotective effect of naproxen prompted us to evaluate the extent and duration of platelet, monocyte, and vascular cyclooxygenase (COX) inhibition by naproxen compared with low-dose aspirin.Methods and Results—We performed a crossover, open-label study of low-dose aspirin (100 mg/d) or naproxen (500 mg BID) administered to 9 healthy subjects for 6 days. The effects on thromboxane (TX) and prostacyclin biosynthesis were assessed up to 24 hours after oral dosing. Serum TXB2, plasma prostaglandin (PG) E2, and urinary 11-dehydro-TXB2and 2,3-dinor-6-keto-PGF1αwere measured by previously validated radioimmunoassays. The administration of naproxen or aspirin caused a similar suppression of whole-blood TXB2production, an index of platelet COX-1 activity ex vivo, by 94±3% and 99±0.3% (mean±SD), respectively, and of the urinary excretion of 11-dehydro-TXB2, an index of systemic biosynthesis of TXA2in vivo, by 85±8% and 78±7%, respectively, that persisted throughout the dosing interval. Naproxen, in contrast to aspirin, significantly reduced systemic prostacyclin biosynthesis by 77±19%, consistent with differential inhibition of monocyte COX-2 activity measured ex vivo.Conclusions—The regular administration of naproxen 500 mg BID can mimic the antiplatelet COX-1 effect of low-dose aspirin. Naproxen, unlike aspirin, decreased prostacyclin biosynthesis in vivo.

Published

2004

9. Clinical pharmacology of etoricoxib: a novel selectiveCOX2 inhibitor

Author

Stefania Tacconelli, Marta L. Capone, and Paola Patrignani

Subjects

medicine.medical_specialty, Pyridines, Perforation (oil well), Arthritis, Pharmacology, Cardiovascular System, law.invention, Arthritis, Rheumatoid, Etoricoxib, law, Internal medicine, Osteoarthritis, Humans, Medicine, Cyclooxygenase Inhibitors, Drug Interactions, Pharmacology (medical), Sulfones, Clinical Trials as Topic, Pain, Postoperative, Clinical pharmacology, Cyclooxygenase 2 Inhibitors, Dose-Response Relationship, Drug, Arthritis, Gouty, business.industry, Membrane Proteins, General Medicine, medicine.disease, Valdecoxib, Symptomatic relief, Isoenzymes, Clinical trial, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Rheumatoid arthritis, business, Low Back Pain, medicine.drug

Abstract

The development of COX2 inhibitors with improved biochemical selectivity (such as etoricoxib and valdecoxib) over that of commercially available coxibs has been driven by the potential advantage of safety using higher coxib doses for increased efficacy. Etoricoxib has been approved in the UK as a once-daily medicine for symptomatic relief in the treatment of osteoarthritis (OA), rheumatoid arthritis (RA) and acute gouty arthritis. It is currently approved with additional indications (i.e., for relief of acute pain associated with dental surgery, for primary dysmenorrhoea and for chronic musculo-skeletal pain, including chronic lower-back pain) in Mexico, Brazil and Peru. Etoricoxib has an in vitro COX1/COX2 IC(50) ratio of 344, the highest of any coxib. The administration of therapeutic doses of etoricoxib to healthy subjects does not affect COX1 activity in circulating platelets and gastric biopsies. The profound inhibition of monocyte COX2 activity at 24 h after dosing, as predicted by a pharmacological half-life of approximately 22 h, supports a once-daily dosing regimen of etoricoxib. In randomised, well-controlled clinical trials, etoricoxib has been shown to have a comparable clinical efficacy with traditional NSAIDs. Combined analysis of efficacy trials with etoricoxib versus non-selective NSAIDs has shown that the drug halves both investigator-reported upper gastrointestinal perforation, ulcers and bleeds (PUBs) and confirmed PUBs, and reduces the need for gastroprotective agents and gastrointestinal comedications by approximately 40%. The risk of lower extremity oedema and hypertension adverse experiences with etoricoxib was low and generally similar to comparator NSAIDs in a combined analysis of eight Phase III studies in OA, RA, chronic low-back pain and surveillance endoscopy. Large, randomised clinical trials have been planned to confirm the renal, gastrointestinal and cardiovascular safety of etoricoxib.

Published

2003

10. Effects of acetaminophen on constitutive and inducible prostanoid biosynthesis in human blood cells

Author

Francesca Seta, Maria G. Sciulli, Giuseppa Pistritto, Emanuela Ricciotti, Stefania Tacconelli, Marta L. Capone, and Paola Patrignani

Subjects

Pharmacology, biology, Chemistry, Thromboxane, Prostaglandin, Biological activity, Thromboxane B2, chemistry.chemical_compound, Biochemistry, Enzyme inhibitor, biology.protein, medicine, Platelet, Prostaglandin E2, Whole blood, medicine.drug

Abstract

1. Acetaminophen, an analgesic and antipyretic drug with weak antiinflammatory properties, has been suggested to act as a tissue-selective inhibitor of prostaglandin H synthases (PGHSs) (e.g. COX-1 and COX-2) through its reducing activity, that is influenced by the different cellular levels of peroxides. 2. We have studied the effects of acetaminophen on inducible and constitutive prostanoid biosynthesis in monocytes and platelets in vitro. To discriminate between the inhibitory effect of the drug on PGHS-isozymes vs PGE-synthases (PGESs), parallel measurements of PGE(2) and thromboxane (TX) B(2) were carried out. Since antioxidant enzymes and cofactors, present in plasma, may affect acetaminophen-dependent inhibition of prostanoids, comparative experiments in whole blood vs isolated monocytes were performed. 3. Acetaminophen inhibited LPS-induced whole blood PGE(2) and TXB(2) production, in a concentration-dependent fashion [IC(50) microM (95% confidence intervals): 44 (27-70) and 94 (79-112), respectively]. Therapeutic plasma concentrations (100 and 300 microM) of the drug more profoundly reduced PGE(2) than TXB(2) (71 +/- 3 vs 54 +/- 4 and 95 +/- 0.8 vs 78 +/- 2%, respectively, mean +/- s.e.mean, n = 6, P < 0.01). 4. Differently, in isolated monocytes stimulated with LPS, both PGE(2) and TXB(2) production was maximally reduced by only 60%. 5 At 100 and 300 microM, the drug caused a similar and incomplete inhibition of platelet PGE(2) and TXB(2) production during whole blood clotting (45 +/- 4 vs 54 +/- 4 and 75 +/- 2 vs 75 +/- 1%, respectively, mean +/- s.e.mean, n = 4). 6 In conclusion, therapeutic concentrations of acetaminophen caused an incomplete inhibition of platelet COX-1 and monocyte COX-2 but in the presence of plasma, the drug almost completely suppressed inducible PGE(2) biosynthesis through its inhibitory effects on both COX-2 and inducible PGES.

Published

2003

11. Increased Oxidative Stress and Platelet Activation in Patients With Hypertension and Renovascular Disease

Author

Laura Menapace, Alessandro Lechi, Pietro Minuz, Enrico Arosio, Marta L. Capone, Chiara Bencini, Cecilia Del Vecchio, Simone Palatresi, Stefania Tacconelli, Maurizio Degan, Paola Patrignani, Giancarlo Mansueto, Stefania Gaino, Alberto Morganti, Rosamaria Tommasoli, Carlo Patrono, Francesca Seta, and Clara Santonastaso

Subjects

Blood Glucose, Male, Homocysteine, Thromboxane, Dinoprost, Essential hypertension, Plasma renin activity, Antioxidants, Renin-Angiotensin System, Angiotensin, chemistry.chemical_compound, Reference Values, Renin, Stenosis, F2-Isoprostanes, Angiotensin II, Vitamins, Middle Aged, Cholesterol, Hypertension, Renovascular, Hypertension, Female, Cardiology and Cardiovascular Medicine, Adult, medicine.medical_specialty, Adolescent, Urinary system, Urology, Renal Artery Obstruction, Physiology (medical), Internal medicine, medicine, Humans, Platelet activation, Triglycerides, Aged, Creatinine, business.industry, Vascular disease, Angioplasty, Platelet Activation, medicine.disease, Thromboxane B2, Oxidative Stress, Cross-Sectional Studies, Endocrinology, chemistry, Lipid Peroxidation, business, Biomarkers

Abstract

Background— Hypertensive patients with renovascular disease (RVD) may be exposed to increased oxidative stress, possibly related to activation of the renin-angiotensin system. Methods and Results— We measured the urinary excretion of 8-iso-prostaglandin (PG) F 2α and 11-dehydro-thromboxane (TX) B 2 as indexes of in vivo lipid peroxidation and platelet activation, respectively, in 25 patients with RVD, 25 patients with essential hypertension, and 25 healthy subjects. Plasma renin activity in peripheral and renal veins, angiotensin II in renal veins, cholesterol, glucose, triglycerides, homocysteine, and antioxidant vitamins A, C, and E were also determined. Patients were also studied 6 months after a technically successful angioplasty of the stenotic renal arteries. Urinary 8-iso-PGF 2α was significantly higher in patients with RVD (median, 305 pg/mg creatinine; range, 124 to 1224 pg/mg creatinine) than in patients with essential hypertension (median, 176 pg/mg creatinine; range, 48 to 384 pg/mg creatinine) or in healthy subjects (median, 123 pg/mg creatinine; range, 58 to 385 pg/mg creatinine). Urinary 11-dehydro-TXB 2 was also significantly higher in RVD patients compared with healthy subjects. In RVD patients , urinary 8-iso-PGF 2α correlated with 11-dehydro-TXB 2 ( r s =0.48; P r s =0.67; P r s =0.65; P =0.005) ratios. A reduction in 8-iso-PGF 2α after angioplasty was observed in RVD patients with high baseline levels of lipid peroxidation. Changes in 8-iso-PGF 2α were related to baseline lipid peroxidation ( r s =−0.73; P r s =−0.70; P r s =−0.63; P Conclusions— Lipid peroxidation is markedly enhanced in hypertensive patients with RVD and is related to activation of the renin-angiotensin system. Moreover, persistent platelet activation triggered or amplified by bioactive isoprostanes may contribute to the progression of cardiovascular and renal damage in this setting.

Published

2002

12. The Biochemical Selectivity of Novel COX-2 Inhibitors in Whole Blood Assays of COX-isozyme Activity

Author

Paola Patrignani, Stefania Tacconelli, Marta L. Capone, Emanuela Ricciotti, and Maria G. Sciulli

Subjects

Adult, Male, medicine.medical_specialty, Pyridines, Thromboxane, Prostaglandin, In Vitro Techniques, Pharmacology, Etoricoxib, Lactones, chemistry.chemical_compound, Humans, Medicine, Cyclooxygenase Inhibitors, Sulfones, Rofecoxib, Whole blood, Sulfonamides, Cyclooxygenase 2 Inhibitors, biology, business.industry, Membrane Proteins, Isoxazoles, General Medicine, Valdecoxib, Surgery, Isoenzymes, Italy, chemistry, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Enzyme inhibitor, Cyclooxygenase 1, Celecoxib, biology.protein, Female, business, medicine.drug

Abstract

We have evaluated the biochemical selectivity of novel cyclo-oxygenase (COX)-2 inhibitors, etoricoxib, valdecoxib, DFU and DFP, vs rofecoxib and celecoxib, using the human whole blood assays of COX-isozyme activity, in vitro. Compounds were incubated with human whole blood samples, allowed to clot for 1 h at 37 degrees C, or stimulated with lipopolysaccharide (10 microg/ml) for 24 h at 37 degrees C. Serum thromboxane (TX) B2 and plasma prostaglandin (PG) E2 levels were measured by specific radioimmunoassays as indices of platelet COX-1 and monocyte COX-2 activity, respectively. Valdecoxib, etoricoxib, DFU and DFP inhibited platelet COX-1 and monocyte COX-2 with the following COX-1/COX-2 IC50 ratios: 61.5, 344, 660 and 1918, respectively. The reference compounds, celecoxib and rofecoxib had corresponding values of 29.6 and 272. In conclusion, a second wave of COX-2 inhibitors with higher biochemical selectivity than the existing coxibs has been developed. Whether their administration will be associated with improved clinical efficacy and/or safety vis-à-vis celecoxib and rofecoxib remains to be established.

Published

2002

13. The human pharmacology of monocyte cyclooxygenase 2 inhibition by cortisol and synthetic glucocorticoids

Author

Carlo Patrono, M. R. Panara, Paola Patrignani, Emanuela Ricciotti, Giovanna Santini, Francesca Seta, Marta L. Capone, Stefania Tacconelli, and Maria G. Sciulli

Subjects

Lipopolysaccharides, medicine.medical_specialty, Hydrocortisone, Arthritis, Pharmacology, Methylprednisolone, Dexamethasone, Dinoprostone, Monocytes, Arthritis, Rheumatoid, In vivo, Internal medicine, medicine, Humans, Cyclooxygenase Inhibitors, Pharmacology (medical), Glucocorticoids, Whole blood, Cyclooxygenase 2 Inhibitors, biology, Monocyte, Membrane Proteins, Radioimmunoassay, medicine.disease, Isoenzymes, Endocrinology, medicine.anatomical_structure, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Cyclooxygenase 1, biology.protein, Cyclooxygenase, Ex vivo, medicine.drug

Abstract

Background We studied the concentration dependence of the inhibitory effects of cortisol, 6-methylprednisolone, and dexamethasone on cyclooxygenase-2 (COX-2) expression and activity in human monocytes in response to lipopolysaccharide (LPS) in vitro. Moreover, we characterized the time and dose dependence of the inhibitory effects of 6-methylprednisolone, administered to healthy subjects, on LPS-inducible prostaglandin E2 (PGE2) biosynthesis in whole blood ex vivo. Methods Heparinized whole-blood samples obtained from healthy subjects and patients with rheumatoid arthritis were incubated with LPS (10 μg/ml) for 24 hours at 37°C, and PGE2 was measured in plasma as an index of monocyte COX-2 activity. Comparative experiments were performed in LPS-stimulated isolated monocytes. The levels of COX-2-like immunoreactivity in monocyte lysates were measured by a specific Western blot technique. PGE2 was evaluated by radioimmunoassay. Results Nanomolar concentrations of cortisol, 6-methylprednisolone, and dexamethasone suppressed LPS-induced PGE2 biosynthesis both in whole blood and in isolated monocytes in vitro with relative potencies similar to those reported for their anti-inflammatory effects in vivo. The administration of single oral doses (4, 8, or 16 mg) of 6-methylprednisolone caused a dose- and time-dependent inhibition of whole-blood COX-2 activity. Whole-blood samples obtained from patients with rheumatoid arthritis treated with comparable maintenance doses of glucocorticoids produced significantly lower levels of LPS-inducible PGE2 than were found in untreated patients. Conclusions Therapeutic plasma levels of synthetic glucocorticoids down-regulate inducible prostanoid biosynthesis in circulating monocytes. This effect may represent a readily measurable surrogate marker of their clinical efficacy for dose-finding studies. Clinical Pharmacology & Therapeutics (2001) 70, 475–483; doi: 10.1016/S0009-9236(01)14130-5

Published

2001

14. NSAIDs and cardiovascular disease

Author

Stefania Tacconelli, Paola Patrignani, and Marta L. Capone

Subjects

medicine.medical_specialty, Aspirin, Cyclooxygenase 2 Inhibitors, business.industry, Anti-Inflammatory Agents, Non-Steroidal, Arthritis, Valdecoxib, medicine.disease, Surgery, Diclofenac, Cardiovascular Diseases, Internal medicine, Rheumatoid arthritis, medicine, Celecoxib, Humans, media_common.cataloged_instance, European union, Cardiology and Cardiovascular Medicine, business, Etoricoxib, Rofecoxib, Drug Labeling, media_common, medicine.drug

Abstract

Non-steroidal anti-inflammatory drugs (NSAIDs) are a chemically heterogeneous group of agents to treat symptoms of acute pain and chronic inflammatory and degenerative joint diseases, such as rheumatoid arthritis (RA) and osteoarthritis (OA).1 They act mostly through the inhibition of cyclooxygenase-2 (COX-2)-dependent prostanoids. They comprise traditional (t) NSAIDs and NSAIDs selective for COX-2, named cyclooxygenase-2 inhibitors, developed to reduce the gastrointestinal (GI) toxicity of tNSAIDs, which is dependent, at least in part, on the inhibition of COX-1. Placebo-controlled trials have established that cyclooxygenase-2 inhibitors (rofecoxib, valdecoxib and celecoxib) confer a small but absolute increase in the incidence of thrombotic vascular events.2 An overview of data derived from trials with cyclooxygenase-2 inhibitors suggests that myocardial infarction (MI) predominates over stroke.3 The cardiovascular (CV) hazard associated with the use of cyclooxygenase-2 inhibitors led to the voluntary withdrawal from the United States (US) and European Union (EU) markets of rofecoxib and valdecoxib, in 2004 and 2005 respectively. Recently, the Food and Drug Administration (FDA) has formally rejected manufacturer application for approval of another cyclooxygenase-2 inhibitor, etoricoxib, as a prescription pain reliever. The FDA decision was influenced by the results of safety analyses from the MEDAL (Multinational Etoricoxib vs Diclofenac Arthritis Long Term) Program, a pooling from three randomised, double-blind clinical trials: the MEDAL study and the EDGE and EDGE II studies.4 The authors reported that etoricoxib (60 or 90 mg daily, mean duration of therapy 18 months) and the tNSAID diclofenac (150 mg/d, ie, 50 mg three times daily or 75 mg twice daily) administered to OA or RA patients have comparable rates, constant over time, of thrombotic CV events. However, the increase in heart failure, hypertension, and oedema shown with etoricoxib and the fact that the cyclooxygenase-2 inhibitor did not reduce complicated peptic ulcer attenuated the safety benefit of …

Published

2007

15. Reduced thromboxane biosynthesis in carriers of toll-like receptor 4 polymorphisms in vivo

Author

Maria Domenica Guglielmi, Concetta Di Febbo, Marta L. Capone, Paola Patrignani, Valeria Moretta, Stefania Tacconelli, Maria G. Sciulli, Ivana Antonucci, Ettore Porreca, Liborio Stuppia, Emanuela Ricciotti, and Giovanna Baccante

Subjects

Male, Heterozygote, medicine.medical_specialty, Carotid Artery, Common, Thromboxane, Immunology, Prostacyclin, Biochemistry, Thromboxane A2, chemistry.chemical_compound, Risk Factors, In vivo, Internal medicine, medicine, Humans, Platelet, Ultrasonography, Polymorphism, Genetic, biology, Wild type, Cell Biology, Hematology, Middle Aged, Epoprostenol, Toll-Like Receptor 4, Phenotype, Endocrinology, Eicosanoid, chemistry, Cardiovascular Diseases, Case-Control Studies, biology.protein, Female, lipids (amino acids, peptides, and proteins), Cyclooxygenase, medicine.drug

Abstract

The recent demonstration that platelets express a functional toll-like receptor 4 (TLR4) prompted us to explore the influence of TLR4 polymorphisms (Asp299Gly alone or in combination with Thr399Ile) on thromboxane A(2) (TXA(2)) biosynthesis in vivo. In 17 subjects with TLR4 polymorphisms versus 17 wild type (untreated with aspirin, matched for age, sex, and cardiovascular risk factors), intima-media thickness in the common carotid arteries was significantly lower. Average urinary excretion of 11-dehydro-TXB(2), an index of systemic biosynthesis of TX, was significantly reduced by 65%. The urinary excretion of 2,3-dinor-6-keto-prostaglandin F(1alpha), an index of systemic biosynthesis of prostacyclin, was marginally depressed but the prostacyclin/TXA(2) biosynthesis ratio was significantly higher than in wild type. Selective inhibition of cyclooxygenase 2-dependent prostacyclin (by rofecoxib or etoricoxib) was associated with increased urinary excretion of 11-dehydro-TXB(2) in carriers of TLR4 polymorphisms, but not in wild-type, suggesting a restrainable effect of prostacyclin on platelet function in vivo in this setting. Reduced TXA(2) biosynthesis may contribute to the protective cardiovascular phenotype of TLR4 polymorphisms.

Published

2006

16. Low-dose naproxen interferes with the antiplatelet effects of aspirin in healthy subjects: recommendations to minimize the functional consequences

Author

Luigia Di Francesco, Thomas S. Price, Annalisa Bruno, Anita Jeyam, Paola Tontodonati, Stefania Tacconelli, Giulia Renda, Marta L. Capone, Gabriele Merciaro, Paola Patrignani, L. Grossi, Patrizia Di Gregorio, Paola Anzellotti, and Luis A. García Rodríguez

Subjects

Adult, Blood Platelets, Male, Naproxen, Immunology, Analgesic, Naproxen Sodium, Pharmacology, chemistry.chemical_compound, Young Adult, Rheumatology, Reference Values, medicine, Immunology and Allergy, Humans, Pharmacology (medical), Platelet, Drug Interactions, Antipyretic, Aspirin, Arachidonic Acid, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Platelet-Rich Plasma, Anti-Inflammatory Agents, Non-Steroidal, Crossover study, Thromboxane B2, chemistry, Female, Collagen, business, Platelet Aggregation Inhibitors, medicine.drug

Abstract

Objective To investigate whether low-dose naproxen sodium (220 mg twice a day) interferes with aspirin's antiplatelet effect in healthy subjects. Methods We performed a crossover, open-label study in 9 healthy volunteers. They received for 6 days 3 different treatments separated by 14 days of washout: 1) naproxen 2 hours before aspirin, 2) aspirin 2 hours before naproxen, and 3) aspirin alone. The primary end point was the assessment of serum thromboxane B2 (TXB2) 24 hours after the administration of naproxen 2 hours before aspirin on day 6 of treatment. In 5 volunteers, the rate of recovery of TXB2 generation (up to 72 hours after drug discontinuation) was assessed in serum and in platelet-rich plasma stimulated with arachidonic acid (AA) or collagen. Results Twenty-four hours after the last dosing on day 6 in volunteers receiving aspirin alone or aspirin before naproxen, serum TXB2 was almost completely inhibited (median [range] 99.1% [97.4–99.4%] and 99.1% [98.0–99.7%], respectively). Naproxen given before aspirin caused a slightly lower inhibition of serum TXB2 (median [range] 98.0% [90.6–99.4%]) than aspirin alone (P = 0.0007) or aspirin before naproxen (P = 0.0045). All treatments produced a maximal inhibition of AA-induced platelet aggregation. At 24 hours, compared with baseline, collagen-induced platelet aggregation was still inhibited by aspirin alone (P = 0.0003), but not by aspirin given 2 hours before or after naproxen. Compared with administration of aspirin alone, the sequential administration of naproxen and aspirin caused a significant parallel upward shift of the regression lines describing the recovery of platelet TXB2. Conclusion Sequential administration of 220 mg naproxen twice a day and low-dose aspirin interferes with the irreversible inhibition of platelet cyclooxygenase 1 afforded by aspirin. The interaction was smaller when giving naproxen 2 hours after aspirin. The clinical consequences of these 2 schedules of administration of aspirin with naproxen remain to be studied in randomized clinical trials.

Published

2011

17. Glucose and collagen regulate human platelet activity through aldose reductase induction of thromboxane

Author

Ettore Porreca, Wai Ho Tang, Paola Patrignani, John Hwa, Cristiano Fava, Virgilio Evangelista, Giacomo Levantesi, Jeffrey J. Rade, Jeremiah Stitham, Pietro Minuz, Concetta Di Febbo, Marta L. Capone, Stefania Tacconelli, Li Wen, Kathleen A. Martin, and Scott Gleim

Subjects

Adult, Blood Glucose, Male, collagen, medicine.medical_specialty, Platelet Aggregation, Thromboxane, In Vitro Techniques, Models, Biological, Mitogen-Activated Protein Kinase 14, Aldehyde Reductase, Internal medicine, Diabetes mellitus, Glucose, platelet, aldose reductase, thromboxane, Diabetes Mellitus, medicine, Humans, Platelet, Platelet activation, Enzyme Inhibitors, Protein Kinase C, Aged, Aged, 80 and over, Venous Thrombosis, Aldose reductase, Aspirin, Phospholipase C gamma, Chemistry, Thromboxanes, General Medicine, Middle Aged, Platelet Activation, medicine.disease, Oxidative Stress, Endocrinology, Eicosanoid, Case-Control Studies, Platelet aggregation inhibitor, Female, Reactive Oxygen Species, Platelet Aggregation Inhibitors, Signal Transduction, Research Article, medicine.drug

Abstract

Diabetes mellitus is associated with platelet hyperactivity, which leads to increased morbidity and mortality from cardiovascular disease. This is coupled with enhanced levels of thromboxane (TX), an eicosanoid that facilitates platelet aggregation. Although intensely studied, the mechanism underlying the relationship among hyperglycemia, TX generation, and platelet hyperactivity remains unclear. We sought to identify key signaling components that connect high levels of glucose to TX generation and to examine their clinical relevance. In human platelets, aldose reductase synergistically modulated platelet response to both hyperglycemia and collagen exposure through a pathway involving ROS/PLCγ2/PKC/p38α MAPK. In clinical patients with platelet activation (deep vein thrombosis; saphenous vein graft occlusion after coronary bypass surgery), and particularly those with diabetes, urinary levels of a major enzymatic metabolite of TX (11-dehydro-TXB2 [TX-M]) were substantially increased. Elevated TX-M persisted in diabetic patients taking low-dose aspirin (acetylsalicylic acid, ASA), suggesting that such patients may have underlying endothelial damage, collagen exposure, and thrombovascular disease. Thus, our study has identified multiple potential signaling targets for designing combination chemotherapies that could inhibit the synergistic activation of platelets by hyperglycemia and collagen exposure.

Published

2011

18. Measurement of 8-iso-prostaglandin F2alpha in biological fluids as a measure of lipid peroxidation

Author

Stefania, Tacconelli, Marta L, Capone, and Paola, Patrignani

Subjects

Solid Phase Extraction, Radioimmunoassay, Humans, Lipid Peroxidation, Dinoprost, Gas Chromatography-Mass Spectrometry, Mass Spectrometry, Chromatography, Liquid

Abstract

Several lines of evidence suggest that reactive oxygen species are implicated in human disease, including atherosclerosis, hypertension, and restenosis after angioplasty. The measurement of F(2)-isoprostanes (F(2)-iPs), formed nonenzymatically through free radical catalyzed attack on esterified arachidonate, provides a reliable tool for identifying populations with enhanced rates of lipid peroxidation. Among F(2)-isoPs, 8-iso-PGF(2alpha) (also referred to IPF(2alpha)-III) and IPF(2alpha)-VI are the most frequently measured in biological fluids. A variety of methods have been proposed to measure F(2)-isoprostanes in urine and plasma. Mass spectrometry has been developed for the measurement of both F(2)-isoprostanes but its use is limited as it is time-consuming and highly expensive. We have developed validated enzyme immunoassay (EIA) and radioimmunoassay (RIA) techniques using highly specific antisera for the measurement of 8-iso-PGF(2alpha). In contrast, the commercially available immunoassay kits are limited for their poor specificity. The measurement of specific isoprostanes, such as 8-iso-PGF(2alpha), in urine is a reliable, noninvasive index of lipid peroxidation that is of valuable help in dose-finding studies of natural and synthetic antioxidant agents.

Published

2010

19. Measurement of 8-Iso-Prostaglandin F2α in Biological Fluids as a Measure of Lipid Peroxidation

Author

Stefania Tacconelli, Marta L. Capone, and Paola Patrignani

Subjects

chemistry.chemical_classification, Reactive oxygen species, Chromatography, Antioxidant, medicine.diagnostic_test, medicine.medical_treatment, Radioimmunoassay, Urine, Isoprostanes, Lipid peroxidation, chemistry.chemical_compound, Enzyme, chemistry, Immunoassay, medicine

Abstract

Several lines of evidence suggest that reactive oxygen species are implicated in human disease, including atherosclerosis, hypertension, and restenosis after angioplasty. The measurement of F(2)-isoprostanes (F(2)-iPs), formed nonenzymatically through free radical catalyzed attack on esterified arachidonate, provides a reliable tool for identifying populations with enhanced rates of lipid peroxidation. Among F(2)-isoPs, 8-iso-PGF(2alpha) (also referred to IPF(2alpha)-III) and IPF(2alpha)-VI are the most frequently measured in biological fluids. A variety of methods have been proposed to measure F(2)-isoprostanes in urine and plasma. Mass spectrometry has been developed for the measurement of both F(2)-isoprostanes but its use is limited as it is time-consuming and highly expensive. We have developed validated enzyme immunoassay (EIA) and radioimmunoassay (RIA) techniques using highly specific antisera for the measurement of 8-iso-PGF(2alpha). In contrast, the commercially available immunoassay kits are limited for their poor specificity. The measurement of specific isoprostanes, such as 8-iso-PGF(2alpha), in urine is a reliable, noninvasive index of lipid peroxidation that is of valuable help in dose-finding studies of natural and synthetic antioxidant agents.

Published

2010

20. NSAIDs and cardiovascular disease: transducing human pharmacology results into clinical read-outs in the general population

Author

Stefania Tacconelli, Luis A. García Rodríguez, Paola Patrignani, and Marta L. Capone

Subjects

Population, Prostacyclin, Pharmacology, Mice, In vivo, medicine, Animals, Humans, Cyclooxygenase Inhibitors, Prostaglandins I, education, Adverse effect, Whole blood, education.field_of_study, biology, Cyclooxygenase 2 Inhibitors, business.industry, Anti-Inflammatory Agents, Non-Steroidal, General Medicine, Cardiovascular Diseases, Cyclooxygenase 2, biology.protein, Cyclooxygenase 1, Biomarker (medicine), Cyclooxygenase, business, Ex vivo, medicine.drug

Abstract

Traditional (t) non-steroidal anti-inflammatory drugs (NSAIDs) and selective cyclooxygenase (COX)-2 inhibitors (coxibs) are important and efficacious drugs for the management of musculoskeletal symptoms. These drugs have both beneficial and adverse effects due to the inhibition of prostanoids. Although the tNSAID and coxib inhibition of COX-2-dependent prostaglandin (PG)E(2) production is effective in ameliorating symptoms of inflammation and pain, a small but consistent increased risk of myocardial infarction has been detected in association with their use. Convincing evidence suggests that cardiovascular toxicity associated with the administration of these compounds occurs through a common mechanism involving inhibition of COX-2-dependent prostacyclin. The development of biomarkers that predict the impact of NSAIDs on COX-1 and COX-2 activities in vitro, ex vivo and in vivo has been essential to read-out the clinical consequences of the varying degrees of inhibition of the two COX-isozymes in humans. Whole blood assays for COX-1 and COX-2 might be candidates as surrogate end-points of toxicity and efficacy of NSAIDs. Using a biomarker strategy, we have shown that the degree of inhibition of COX-2 and the functional selectivity with which it is achieved are relevant to the level of cardiovascular hazard from NSAIDs and relate to drug potency (exposure). We propose that the assessment of COX-2 in whole blood ex vivo, either alone or in combination with urinary levels of 2,3-dinor-6-keto-PGF(1 alpha) a biomarker of prostacyclin biosynthesis in vivo, may represent a valid surrogate end-point to predict cardiovascular risk for functionally selective COX-2 inhibitors.

Published

2009

21. Effects of AF3442 [N-(9-ethyl-9H-carbazol-3-yl)-2-(trifluoromethyl)benzamide], a novel inhibitor of human microsomal prostaglandin E synthase-1, on prostanoid biosynthesis in human monocytes in vitro

Author

Claudio Milanese, Stefania Tacconelli, Maria Alessandra Alisi, Luigia Di Francesco, Andrea Di Francesco, Annalisa Bruno, Emanuela Ricciotti, Melania Dovizio, Giorgina Mangano, Isabella Coletta, Lorenzo Polenzani, Paola Anzellotti, Marta L. Capone, and Paola Patrignani

Subjects

Lipopolysaccharides, Carbazoles, Prostaglandin, Pharmacology, Prostaglandin E synthase, Biochemistry, Dinoprostone, Monocytes, chemistry.chemical_compound, Cell Line, Tumor, Microsomes, medicine, Humans, Prostaglandin E2, Enzyme Inhibitors, Benzamide, Prostaglandin-E Synthases, biology, Dose-Response Relationship, Drug, Chemistry, Prostanoid, Epoprostenol, Intramolecular Oxidoreductases, Benzamides, biology.protein, Prostaglandins, Prostaglandin H2, lipids (amino acids, peptides, and proteins), Cyclooxygenase, medicine.drug

Abstract

Inhibitors of microsomal prostaglandin (PG) E synthase-1 (mPGES-1) are being developed for the relief of pain. Redirection of the PGH(2) substrate to other PG synthases, found both in vitro and in vivo, in mPGES-1 knockout mice, may influence their efficacy and safety. We characterized the contribution of mPGES-1 to PGH(2) metabolism in lipopolysaccharide (LPS)-stimulated isolated human monocytes and whole blood by studying the synthesis of prostanoids [PGE(2), thromboxane (TX)B(2), PGF(2alpha) and 6-keto-PGF(1alpha)] and expression of cyclooxygenase (COX)-isozymes and down-stream synthases in the presence of pharmacological inhibition by the novel mPGES-1 inhibitor AF3442 [N-(9-ethyl-9H-carbazol-3-yl)-2-(trifluoromethyl)benzamide]. AF3442 caused a concentration-dependent inhibition of PGE(2) in human recombinant mPGES-1 with an IC(50) of 0.06microM. In LPS-stimulated monocytes, AF3442 caused a concentration-dependent reduction of PGE(2) biosynthesis with an IC(50) of 0.41microM. At 1microM, AF3442 caused maximal selective inhibitory effect of PGE(2) biosynthesis by 61+/-3.3% (mean+/-SEM, P

Published

2009

22. Risk management profile of etoricoxib: an example of personalized medicine

Author

Stefania Tacconelli, Marta L. Capone, and Paola Patrignani

Subjects

cardiovascular toxicity, etoricoxib, nonsteroidal antiinflammatory drugs, Prostacyclin, RM1-950, Review, Pharmacology, medicine, Pharmacology (medical), Platelet, Myocardial infarction, General Pharmacology, Toxicology and Pharmaceutics, gastrointestinal toxicity, Adverse effect, Whole blood, Chemical Health and Safety, biology, business.industry, prostacyclin, General Medicine, COX-2, medicine.disease, Toxicity, biology.protein, Cyclooxygenase, Therapeutics. Pharmacology, business, Safety Research, Etoricoxib, medicine.drug

Abstract

Paola Patrignani, Stefania Tacconelli, Marta L CaponeDepartment of Medicine and Center of Excellence on Aging, “G. D’Annunzio” University School of Medicine, and “Gabriele D’Annunzio” University Foundation, CeSI, Chieti, ItalyAbstract: The development of nonsteroidal anti-inflammatory drugs (NSAIDs) selective for cyclooxygenase (COX)-2 (named coxibs) has been driven by the aim of reducing the incidence of serious gastrointestinal (GI) adverse events associated with the administration of traditional (t) NSAIDs – mainly dependent on the inhibition of COX-1 in GI tract and platelets. However, their use has unravelled the important protective role of COX-2 for the cardiovascular (CV) system, mainly through the generation of prostacyclin. In a recent nested-case control study, we found that patients taking NSAIDs (both coxibs and tNSAIDs) had a 35% increase risk of myocardial infarction. The increased incidence of thrombotic events associated with profound inhibition of COX-2-dependent prostacyclin by coxibs and tNSAIDs can be mitigated, even if not obliterated, by a complete suppression of platelet COX-1 activity. However, most tNSAIDs and coxibs are functional COX-2 selective for the platelet (ie, they cause a profound suppression of COX-2 associated with insufficient inhibition of platelet COX-1 to translate into inhibition of platelet function), which explains their shared CV toxicity. The development of genetic and biochemical markers will help to identify the responders to NSAIDs or who are uniquely susceptible at developing thrombotic or GI events by COX inhibition. We will describe possible strategies to reduce the side effects of etoricoxib by using biochemical markers of COX inhibition, such as whole blood COX-2 and the assessment of prostacyclin biosynthesis in vivo.Keywords: etoricoxib, nonsteroidal antiinflammatory drugs, COX-2, gastrointestinal toxicity, cardiovascular toxicity, prostacyclin

Published

2009

23. Human pharmacology of naproxen sodium

Author

Stefania Tacconelli, Luigia Di Francesco, Patrizia Di Gregorio, Marta L. Capone, Gabriele Merciaro, Maria G. Sciulli, Paola Patrignani, and Paola Anzellotti

Subjects

Adult, Blood Platelets, Lipopolysaccharides, Naproxen, Platelet Aggregation, Thromboxane, Prostacyclin, Naproxen Sodium, 6-Ketoprostaglandin F1 alpha, Pharmacology, Dinoprostone, Monocytes, medicine, Humans, Platelet, Cyclooxygenase Inhibitors, Aspirin, Arachidonic Acid, biology, Dose-Response Relationship, Drug, Chemistry, Epoprostenol, Thromboxane B2, Cyclooxygenase 2, biology.protein, Cyclooxygenase 1, Molecular Medicine, Cyclooxygenase, Ex vivo, medicine.drug

Abstract

We compared the variability in degree and recovery from steady-state inhibition of cyclooxygenase (COX)-1 and COX-2 ex vivo and in vivo and platelet aggregation by naproxen sodium at 220 versus 440 mg b.i.d. and low-dose aspirin in healthy subjects. Six healthy subjects received consecutively naproxen sodium (220 and 440 mg b.i.d.) and aspirin (100 mg daily) for 6 days, separated by washout periods of 2 weeks. COX-1 and COX-2 inhibition was determined using ex vivo and in vivo indices of enzymatic activity: 1) the measurement of serum thromboxane (TX)B(2) levels and whole-blood lipopolysaccharide-stimulated prostaglandin (PG)E(2) levels, markers of COX-1 in platelets and COX-2 in monocytes, respectively; 2) the measurement of urinary 11-dehydro-TXB(2) and 2,3-dinor-6-keto-PGF(1alpha) levels, markers of systemic TXA(2) biosynthesis (mostly COX-1-derived) and prostacyclin biosynthesis (mostly COX-2-derived), respectively. Arachidonic acid (AA)-induced platelet aggregation was also studied. The maximal inhibition of platelet COX-1 (95.9 +/- 5.1 and 99.2 +/- 0.4%) and AA-induced platelet aggregation (92 +/- 3.5 and 93.7 +/- 1.5%) obtained at 2 h after dosing with naproxen sodium at 220 and 440 mg b.i.d., respectively, was indistinguishable from aspirin, but at 12 and 24 h after dosing, we detected marked variability, which was higher with naproxen sodium at 220 mg than at 440 mg b.i.d. Assessment of the ratio of inhibition of urinary 11-dehydro-TXB(2) versus 2,3-dinor-6-keto-PGF(1alpha) showed that the treatments caused a more profound inhibition of TXA(2) than prostacyclin biosynthesis in vivo throughout dosing interval. In conclusion, neither of the two naproxen doses mimed the persistent and complete inhibition of platelet COX-1 activity obtained by aspirin, but marked heterogeneity was mitigated by the higher dose of the drug.

Published

2007

24. Clinical pharmacology of etoricoxib

Author

Paola Patrignani, Marta L. Capone, and Stefania Tacconelli

Subjects

medicine.medical_specialty, Heart disease, Pyridines, Osteoarthritis, Toxicology, law.invention, Etoricoxib, Diclofenac, law, Internal medicine, medicine, Humans, Sulfones, Adverse effect, Pharmacology, Clinical Trials as Topic, Clinical pharmacology, Cyclooxygenase 2 Inhibitors, business.industry, General Medicine, medicine.disease, Surgery, Discontinuation, Rheumatoid arthritis, business, medicine.drug

Abstract

Etoricoxib is a highly selective COX-2 inhibitor (coxib) approved in Europe for the treatment of osteoarthritis (OA), rheumatoid arthritis and acute gouty arthritis. Etoricoxib is an effective analgesic drug that has shown some improved efficacy versus traditional NSAIDs and it is the only coxib approved for the treatment of acute gouty arthritis. Moreover, recent studies evidence its efficacy in patients with ankylosing spondylitis. In the Etoricoxib Diclofenac Gastrointestinal Evaluation study performed in patients with OA, etoricoxib significantly reduced the rate of discontinuation by 50% due to gastrointestinal adverse events versus diclofenac. Comparable rates of thrombotic cardiovascular events were detected. Rates of discontinuation due to hypertension-related adverse effects were higher on etoricoxib than diclofenac. Similarly to other selective COX-2 inhibitors, etoricoxib is contraindicated in patients with ischaemic heart disease or stroke and it should be used with caution in patients with risk factors for heart disease. The European Medicines Agency has contraindicated the use of etoricoxib in patients with uncontrolled hypertension. Selective COX-2 inhibitors remain an appropriate choice in patients at low cardiovascular risk, but with increased risk of gastrointestinal complications.

Published

2006

25. Pharmacodynamic of cyclooxygenase inhibitors in humans

Author

Stefania Tacconelli, Luigia Di Francesco, Marta L. Capone, Andrea Sacchetti, Paola Patrignani, and Maria G. Sciulli

Subjects

Blood Platelets, Physiology, Pharmacology, Biochemistry, Gene Expression Regulation, Enzymologic, Diclofenac, medicine, Animals, Humans, Cyclooxygenase Inhibitors, Rofecoxib, biology, business.industry, Anti-Inflammatory Agents, Non-Steroidal, Cell Biology, Valdecoxib, Meloxicam, Therapeutic Equivalency, Cyclooxygenase 2, Gastric Mucosa, biology.protein, Cyclooxygenase 1, Lumiracoxib, Cyclooxygenase, Endothelium, Vascular, business, Etoricoxib, Biomarkers, medicine.drug, Nimesulide

Abstract

We provide comprehensive knowledge on the differential regulation of expression and catalysis of cyclooxygenase (COX)-1 and COX-2 in health and disease which represents an essential requirement to read out the clinical consequences of selective and nonselective inhibition of COX-isozymes in humans. Furthermore, we describe the pharmacodynamic and pharmacokinetic characteristics of major traditional nonsteroidal anti-inflammatory drugs (tNSAIDs) and coxibs (selective COX-2 inhibitors) which play a prime role in their efficacy and toxicity. Important information derived from our pharmacological studies has clarified that nonselective COX inhibitors should be considered the tNSAIDs with a balanced inhibitory effect on both COX-isozymes (exemplified by ibuprofen and naproxen). In contrast, the tNSAIDs meloxicam, nimesulide and diclofenac (which are from 18- to 29-fold more potent towards COX-2 in vitro) and coxibs (i.e. celecoxib, valdecoxib, rofecoxib, etoricoxib and lumiracoxib, which are from 30- to 433-fold more potent towards COX-2 in vitro) should be comprised into the cluster of COX-2 inhibitors. However, the dose and frequency of administration together with individual responses will drive the degree of COX-2 inhibition and selectivity achieved in vivo. The results of clinical pharmacology of COX inhibitors support the concept that the inhibition of platelet COX-1 may translate into an increased incidence of serious upper gastrointestinal bleeding but this effect on platelet COX-1 may mitigate the cardiovascular hazard associated with the profound inhibition of COX-2-dependent prostacyclin (PGI2).

Published

2006

26. De novo synthesis of cyclooxygenase-1 counteracts the suppression of platelet thromboxane biosynthesis by aspirin

Author

Luigia Di Francesco, Andrea Sacchetti, Marta L. Capone, Stefano Manarini, Antonio Scilimati, Emanuela Ricciotti, Paola Patrignani, Virgilio Evangelista, Angelo Di Santo, Maria G. Sciulli, Sandra D’Angelo, and Stefania Tacconelli

Subjects

Adult, Blood Platelets, medicine.medical_specialty, Physiology, Thromboxane, chemistry.chemical_compound, Thromboxane A2, Phosphatidylinositol 3-Kinases, Thrombin, Internal medicine, medicine, Humans, Platelet, Phosphatidylinositol, RNA, Messenger, Aspirin, biology, Dose-Response Relationship, Drug, Chemistry, Middle Aged, Endocrinology, Eicosanoid, Protein Biosynthesis, biology.protein, Cyclooxygenase 1, Cyclooxygenase, Cardiology and Cardiovascular Medicine, Platelet Aggregation Inhibitors, medicine.drug

Abstract

Aspirin affords cardioprotection through the acetylation of serine 529 in human cyclooxygenase-1 (COX-1) of anucleated platelets, inducing a permanent defect in thromboxane A 2 (TXA 2 )–dependent platelet function. However, heterogeneity of COX-1 suppression by aspirin has been detected in cardiovascular disease and may contribute to failure to prevent clinical events. The recent recognized capacity of platelets to make proteins de novo paves the way to identify new mechanisms involved in the variable response to aspirin. We found that in washed human platelets, the complete suppression of TXA 2 biosynthesis by aspirin, in vitro, recovered in response to thrombin and fibrinogen in a time-dependent fashion (at 0.5 and 24 hours, TXB 2 averaged 0.1±0.03 and 3±0.8 ng/mL; in the presence of arachidonic acid [10 μmol/L], it was 2±0.7 and 25±7 ng/mL, respectively), and it was blocked by translational inhibitors, by rapamycin, and by inhibitors of phosphatidylinositol 3-kinase. The results that COX-1 mRNA was readily detected in resting platelets and that [ 35 S]-methionine was incorporated into COX-1 protein after stimulation strongly support the occurrence of de novo COX-1 synthesis in platelets. This process may interfere with the complete and persistent suppression of TXA 2 biosynthesis by aspirin necessary for cardioprotection.

Published

2006

27. The future of traditional nonsteroidal antiinflammatory drugs and cyclooxygenase-2 inhibitors in the treatment of inflammation and pain

Author

Maria G, Sciulli, Marta L, Capone, Stefania, Tacconelli, and Paola, Patrignani

Subjects

Inflammation, Cyclooxygenase 2 Inhibitors, Cyclooxygenase 2, Anti-Inflammatory Agents, Non-Steroidal, Cyclooxygenase 1, Prostaglandins, Animals, Humans, Pain

Abstract

Prostanoids act leading roles in a myriad of physiologic and pathologic processes because these autacoids participate in the amplification of biological responses induced by innumerable stimuli. The formation of prostanoids is operated by two synthases named cyclooxygenase(COX)-1 and COX-2. Traditional nonsteroidal antiinflammatory drugs (tNSAIDs) and COX-2 inhibitors (coxibs) give rise to antipyretic, analgesic, and antiinflammatory actions, through their reversible clogging of the COX channel of COX-2 - apart from aspirin which modifies irreversibly the catalytic activity of COX-2. tNSAIDs and COX-2 inhibitors resulted clinically equivalent for the relief of acute pain and symptoms of arthropathies but they failed to modify disease progression. Clinical evidence of the possible contribution of COX-1 in inflammation and pain in some occasion - as suggested by experimental and pharmacology studies - is orphan because none efficacy trial with COX inhibitors was designed to establish it. COX-2 inhibitors were developed with the aim to reduce the incidence of serious gastrointestinal (GI) adverse effects associated with the administration of tNSAIDs ensued as a consequence of the inhibition of cytoprotective COX-1-derived prostanoids. However, the reduced incidence of serious GI adverse effects compared to tNSAIDs demonstrated for 2 COX-2 inhibitors (e.g. rofecoxib and lumiracoxib) has been countered by an increased incidence of myocardial infarction and stroke detected in 5 placebo controlled trials involving the COX-2 inhibitors celecoxib, rofecoxib and valdecoxib. The future of COX-2 inhibitors will be an example of personalised medicine as their use will be restricted to patients who do not respond to tNSAIDs or with increased risk of GI complications.

Published

2005

28. Platelet activation in patients with colorectal cancer

Author

Paola Patrignani, Stefania Tacconelli, P. Filabozzi, Marta L. Capone, Emanuela Ricciotti, R. Padovano, Maria G. Sciulli, V. Carnevale, and Marilena Grana

Subjects

Male, medicine.medical_specialty, Colorectal cancer, Urinary system, Clinical Biochemistry, Gastroenterology, Excretion, chemistry.chemical_compound, Internal medicine, medicine, Humans, Platelet, Cyclooxygenase Inhibitors, Platelet activation, Aged, Aspirin, Creatinine, business.industry, Membrane Proteins, Cell Biology, Middle Aged, medicine.disease, Platelet Activation, Thromboxane B2, Endocrinology, chemistry, Prostaglandin-Endoperoxide Synthases, Cyclooxygenase 1, Female, business, Colorectal Neoplasms, Ex vivo, Biomarkers, Platelet Aggregation Inhibitors, medicine.drug

Abstract

Aspirin may reduce the risk of colorectal neoplasia at doses similar to those recommended for the prevention of cardiovascular disease. Thus, we aimed to address whether enhanced platelet activation, as assessed by the measurement of the urinary excretion of 11-dehydro-TXB 2 (a major enzymatic metabolite of TXB 2 ), occurs in patients with colorectal cancer. In 10 patients with colorectal cancer, the urinary excretion of 11-dehydro-TXB 2 was significantly higher than in 10 controls, matched for sex, age and cardiovascular risk factors [1001(205–5571) versus 409(113–984)pg/mg creatinine, respectively, median (range), P 0.05 ]. The administration of aspirin 50mg daily for 5 consecutive days to colorectal cancer patients caused a cumulative inhibition of platelet cyclooxygenase (COX)-1 activity either ex vivo, as assessed by the measurement of serum TXB 2 levels, or in vivo, as assessed by urinary 11-dehydro-TXB 2 excretion. In conclusion, enhanced platelet activation occurs in colorectal cancer patients. Permanent inactivation of platelet COX-1 by low-dose aspirin might restore anti-tumor reactivity.

Published

2005

29. New insights into COX-2 biology and inhibition

Author

Maria G. Sciulli, Marta L. Capone, Paola Patrignani, and Stefania Tacconelli

Subjects

Angiogenesis, Prostaglandin, Inflammation, Pharmacology, Models, Biological, chemistry.chemical_compound, medicine, Animals, Humans, Cyclooxygenase Inhibitors, Brain Diseases, Cyclooxygenase 2 Inhibitors, business.industry, General Neuroscience, Neurodegeneration, Anti-Inflammatory Agents, Non-Steroidal, Prostanoid, Cancer, Membrane Proteins, Anandamide, medicine.disease, Cytoprotection, chemistry, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Neurology (clinical), medicine.symptom, business, Signal Transduction

Abstract

It is now established that prostanoids play important roles in many cellular responses and pathophysiologic processes including modulation of the inflammatory reaction, erosion of cartilage and juxtaarticular bone, gastrointestinal cytoprotection and ulceration, angiogenesis and cancer, hemostasis and thrombosis, renal hemodynamics, and progression of kidney disease. The initial step in the formation of prostanoids, i.e., the conversion of free arachidonic acid (AA) to prostaglandin (PG)G(2) and then to PGH(2), is controlled by two PGH synthases (COX-1 and COX-2). Selective inhibitors of COX-2 (coxibs) have established efficacy in the treatment of pain and inflammation comparable to that of nonselective nonsteroidal anti-inflammatory drugs (NSAIDs) but exhibit enhanced gastrointestinal safety. Several lines of evidence suggest a critical role of COX-2 expression in cancer and selective COX-2 inhibitors may represent novel chemopreventive tools. Moreover, it has been suggested that COX-2 inhibitors may contribute to maintain high levels of chemotherapeutics in tumor tissues by preventing the overexpression of the multidrug resistance protein MDR1/P-gp. The place of COX-2 inhibitors in neurological diseases continues to attract basic and clinical investigation. The possible involvement of COX-2 in neurodegeneration, substained by the results of epidemiological studies with nonselective NSAIDs, has not been confirmed by the results of initial clinical trials with coxibs in Alzheimer's disease. Recently, the involvement of COX-2 in endogenous cannabinoid system has been suggested. Interestingly, COX-2-mediated oxygenation of arachidonylethanolamide (anandamide, AEA) and 2-arachidonylglycerol (2-AG) provides diverse sets of novel lipids that are structurally related to prostaglandins.

Published

2004

30. Clinical pharmacology of novel selective COX-2 inhibitors

Author

Marta L. Capone, Stefania Tacconelli, and Paola Patrignani

Subjects

Pharmacology, law.invention, Parecoxib, law, Drug Discovery, medicine, Humans, Cyclooxygenase Inhibitors, Rofecoxib, Randomized Controlled Trials as Topic, Clinical pharmacology, biology, Cyclooxygenase 2 Inhibitors, business.industry, Membrane Proteins, Valdecoxib, Isoenzymes, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, Celecoxib, biology.protein, Cyclooxygenase 1, Prostaglandins, Lumiracoxib, Cyclooxygenase, business, Etoricoxib, medicine.drug

Abstract

Novel coxibs (i.e. etoricoxib, valdecoxib, parecoxib and lumiracoxib) with enhanced biochemical cyclooxygenase (COX)-2 selectivity over that of rofecoxib and celecoxib have been recently developed. They have the potential advantage to spare COX-1 activity, thus reducing gastrointestinal toxicity, even when administered at high doses to improve efficacy. They are characterized by different pharmacodynamic and pharmacokinetics features. The higher biochemical selectivity of valdecoxib than celecoxib, evidenced in vitro, may be clinically relevant leading to an improved gastrointestinal safety. Interestingly, parecoxib, a pro-drug of valdecoxib, is the only injectable coxib. Etoricoxib shows only a slightly improved COX-2 selectivity than rofecoxib, a highly selective COX-2 inhibitor that has been reported to halve the incidence of serious gastrointestinal toxicity compared to nonselective nonsteroidal antiinflammatory drugs (NSAIDs). Lumiracoxib, the most selective COX-2 inhibitor in vitro, is the only acidic coxib. The hypothesis that this chemical property may lead to an increased and persistent drug accumulation in inflammatory sites and consequently to an improved clinical efficacy, however, remains to be verified. Several randomized clinical studies suggest that the novel coxibs have comparable efficacy to nonselective NSAIDs in the treatment of osteoarthritis, rheumatoid arthritis and acute pain, but they share similar renal side-effects. The apparent dose-dependence of renal toxicity may limit the use of higher doses of the novel coxibs for improved efficacy. Large-size randomized clinical trials are ongoing to define the gastrointestinal and cardiovascular safety of the novel coxibs.

Published

2004

31. Determinants of platelet activation in human essential hypertension

Author

Stefania Tacconelli, Alessandro Lechi, Paola Patrignani, Carlo Patrono, Clara Santonastaso, Stefania Gaino, Marta L. Capone, Pietro Minuz, Rosamaria Tommasoli, Giovanni Faccini, Maurizio Degan, Enrico Arosio, Anna Fornasiero, Francesca Seta, and Giorgio Talamini

Subjects

Adult, Male, medicine.medical_specialty, essential, hypertension, Adolescent, Homocysteine, thromboxanes, medicine.medical_treatment, Urinary system, Dinoprost, Fibrinogen, Essential hypertension, chemistry.chemical_compound, Hypertensive retinopathy, Internal medicine, Internal Medicine, medicine, Humans, oxidative stress, Platelet activation, Aged, F2-Isoprostanes, business.industry, Vitamin E, essential, platelets, thromboxanes, oxidative stress, urine, Middle Aged, Platelet Activation, medicine.disease, urine, Thromboxane B2, Blood pressure, Endocrinology, chemistry, platelets, Female, business, medicine.drug

Abstract

Experimental data suggest that oxidative stress might be enhanced in hypertension and contribute to platelet activation. We hypothesized that both oxidative stress and platelet activation could be related to the clinical characteristics of hypertensive patients. The urinary excretion of 11-dehydrothromboxane (TX) B 2 , reflecting in vivo platelet activation, was measured in 75 patients with mild to severe essential hypertension and 75 pair-matched, healthy controls. The urinary excretion of 8-iso-prostaglandin (PG) F 2α was determined as an index of in vivo lipid peroxidation. Urinary 11-dehydro-TXB 2 was significantly higher in essential hypertensives compared with controls. Although no statistically significant difference in urinary 8-iso-PGF 2α was observed between patients and controls, plasma vitamin C was lower and plasma homocysteine higher in hypertensive patients than in controls. Both urinary 11-dehydro-TXB 2 and 8-iso-PGF 2α were higher in patients with advanced hypertensive retinopathy compared with patients without retinopathy. Multivariate linear regression analysis identified urinary 8-iso-PGF 2α , plasma fibrinogen, homocysteine, and vitamin E as the only variables independently correlated with urinary 11-dehydro-TXB 2 . Logistic regression analysis showed that high urinary 8-iso-PGF 2α , plasma fibrinogen, and homocysteine, as well as low plasma vitamin E, advanced retinopathy, elevated diastolic blood pressure, and the absence of antihypertensive treatment, were predictors of high urinary 11-dehydro-TXB 2 . We demonstrated increased oxidative stress and persistent platelet activation in essential hypertensives with advanced vascular lesions. These findings might help identify hypertensive patients who are at increased risk of cardiovascular events and who might benefit from long-term antiplatelet therapy.

Published

2004

32. Effects of acetaminophen on constitutive and inducible prostanoid biosynthesis in human blood cells

Author

Maria G, Sciulli, Francesca, Seta, Stefania, Tacconelli, Marta L, Capone, Emanuela, Ricciotti, Giuseppa, Pistritto, and Paola, Patrignani

Subjects

Adult, Male, Blood Cells, Dose-Response Relationship, Drug, Papers, Prostaglandins, Humans, lipids (amino acids, peptides, and proteins), Female, Acetaminophen

Abstract

1. Acetaminophen, an analgesic and antipyretic drug with weak antiinflammatory properties, has been suggested to act as a tissue-selective inhibitor of prostaglandin H synthases (PGHSs) (e.g. COX-1 and COX-2) through its reducing activity, that is influenced by the different cellular levels of peroxides. 2. We have studied the effects of acetaminophen on inducible and constitutive prostanoid biosynthesis in monocytes and platelets in vitro. To discriminate between the inhibitory effect of the drug on PGHS-isozymes vs PGE-synthases (PGESs), parallel measurements of PGE(2) and thromboxane (TX) B(2) were carried out. Since antioxidant enzymes and cofactors, present in plasma, may affect acetaminophen-dependent inhibition of prostanoids, comparative experiments in whole blood vs isolated monocytes were performed. 3. Acetaminophen inhibited LPS-induced whole blood PGE(2) and TXB(2) production, in a concentration-dependent fashion [IC(50) microM (95% confidence intervals): 44 (27-70) and 94 (79-112), respectively]. Therapeutic plasma concentrations (100 and 300 microM) of the drug more profoundly reduced PGE(2) than TXB(2) (71 +/- 3 vs 54 +/- 4 and 95 +/- 0.8 vs 78 +/- 2%, respectively, mean +/- s.e.mean, n = 6, P0.01). 4. Differently, in isolated monocytes stimulated with LPS, both PGE(2) and TXB(2) production was maximally reduced by only 60%. 5 At 100 and 300 microM, the drug caused a similar and incomplete inhibition of platelet PGE(2) and TXB(2) production during whole blood clotting (45 +/- 4 vs 54 +/- 4 and 75 +/- 2 vs 75 +/- 1%, respectively, mean +/- s.e.mean, n = 4). 6 In conclusion, therapeutic concentrations of acetaminophen caused an incomplete inhibition of platelet COX-1 and monocyte COX-2 but in the presence of plasma, the drug almost completely suppressed inducible PGE(2) biosynthesis through its inhibitory effects on both COX-2 and inducible PGES.

Published

2003

33. Response to 'Pharmacodynamic Interaction Between Aspirin and Ibuprofen: A Plausible Mechanism of Aspirin Resistance'

Author

Marco Zimarino, Marilena Grana, Maria G. Sciulli, E. D'amelio, Carlo Patrono, Maria Zurro, Francesco Santarelli, Paola Patrignani, Giulia Renda, Marta L. Capone, R. De Caterina, Stefania Tacconelli, and Daniele Sacchetta

Subjects

Pharmacology, Aspirin, Mechanism (biology), business.industry, Pharmacodynamics, medicine, Pharmacology (medical), Ibuprofen, business, ASPIRIN RESISTANCE, medicine.drug

Published

2008

34. W12-P-064 Incomplete suppression of platelet COX-1 activity associated with aspirin-resistant thromboxane biosynthesis in acute coronary syndromes

Author

P. Patrignani, A.G. Rebuzzi, Emanuela Ricciotti, Giulia Renda, Maria G. Sciulli, Marta L. Capone, and S. Tacconelli

Subjects

Aspirin, Thromboxane, business.industry, General Medicine, Pharmacology, chemistry.chemical_compound, Biosynthesis, chemistry, Internal Medicine, Medicine, Platelet, Cardiology and Cardiovascular Medicine, business, medicine.drug

Published

2005

35. Enhaced cortisol secretion does not control aspirin-insensitivess thromboxane biosynthesis in patients with acute coronary syndromes

Author

Francesca Seta, Paola Patrignani, Stefania Tacconelli, Giulia Renda, Marta L. Capone, Antonio Giuseppe Rebuzzi, and Maria G. Sciulli

Subjects

Cortisol secretion, medicine.medical_specialty, Aspirin, Thromboxane, business.industry, chemistry.chemical_compound, Endocrinology, Biosynthesis, chemistry, Internal medicine, medicine, In patient, Cardiology and Cardiovascular Medicine, business, medicine.drug

Published

2002