Search

Your search keyword '"Desmeules, Jules Alexandre"' showing total 122 results
Start Over Author "Desmeules, Jules Alexandre"
122 results on '"Desmeules, Jules Alexandre"'

4. Impact of SARS-CoV-2 Infection (COVID-19) on Cytochromes P450 Activity Assessed by the Geneva Cocktail

Author

Lenoir, Camille, Terrier, Jean, Gloor, Yvonne, Curtin, François, Rollason, Victoria, Desmeules, Jules Alexandre, Daali, Youssef, Reny, Jean-Luc, and Samer, Caroline Flora

Abstract

Coronavirus disease 2019 (COVID-19), caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection, is a severe acute respiratory syndrome with an underlying inflammatory state. We have previously demonstrated that acute inflammation modulates cytochromes P450 (CYPs) activity in an isoform-specific manner. We therefore hypothesized that COVID-19 might also impact CYP activity, and thus aimed to evaluate the impact of acute inflammation in the context of SARS-CoV-2 infection on the six main human CYPs activity. This prospective observational study was conducted in 28 patients hospitalized at the Geneva University Hospitals (Switzerland) with a diagnosis of moderate to severe COVID-19. They received the Geneva phenotyping cocktail orally during the first 72 hours of hospitalization and after 3 months. Capillary blood samples were collected 2 hours after cocktail administration to assess the metabolic ratios (MRs) of CYP1A2, 2B6, 2C9, 2C19, 2D6, and 3A. C-reactive protein (CRP), interleukin 6 (IL-6), and tumor necrosis factor-alpha (TNF-alpha) levels were also measured in blood. CYP1A2, CYP2C19, and CYP3A MRs decreased by 52.6% (P = 0.0001), 74.7% (P = 0.0006), and 22.8% (P = 0.045), respectively, in patients with COVID-19. CYP2B6 and CYP2C9 MRs increased by 101.1% (P = 0.009) and 55.8% (P = 0.0006), respectively. CYP2D6 MR variation did not reach statistical significance (P = 0.072). As expected, COVID-19 was a good acute inflammation model as mean serum levels of CRP, IL-6, and TNF-alpha were significantly (P < 0.001) higher during SARS-CoV-2 infection. CYP activity are modulated in an isoform-specific manner by SARS-CoV-2 infection. The pharmacokinetics of CYP substrates, whether used to treat the disease or as the usual treatment of patients, could be therefore clinically impacted., Clinical Pharmacology & Therapeutics, 110 (5), ISSN:0009-9236, ISSN:1532-6535

Published
2021

6. Influence of Inflammation on Cytochromes P450 Activity in Adults: A Systematic Review of the Literature

Author

Lenoir, Camille, Rollason, Victoria, Desmeules, Jules Alexandre, and Samer, Caroline Flora

Subjects
Disease-drug interaction, Inflammation, ddc:615, ddc:617, Cytokines, Pharmacokinetic, Cytochrome P450
Abstract

Background: Available in-vitro and animal studies indicate that inflammation impacts cytochromes P450 (CYP) activityviamultiple and complex transcriptional and post-transcriptional mechanisms, depending on the specific CYP isoforms and the nature of inflammation mediators. It is essential to review the current published data on the impact of inflammation on CYP activities in adults to support drug individualization based on comorbidities and diseases in clinical practice. Methods: This systematic review was conducted in PubMed through 7th January 2021 looking for articles that investigated the consequences of inflammation on CYP activities in adults. Information on the source of inflammation, victim drugs (and CYPs involved), effect of disease-drug interaction, number of subjects, and study design were extracted. Results: The search strategy identified 218 studies and case reports that met our inclusion criteria. These articles were divided into fourteen different sources of inflammation (such as infection, autoimmune diseases, cancer, therapies with immunomodulator…). The impact of inflammation on CYP activities appeared to be isoform-specific and dependent on the nature and severity of the underlying disease causing the inflammation. Some of these drug-disease interactions had a significant influence on drug pharmacokinetic parameters and on clinical management. For example, clozapine levels doubled with signs of toxicity during infections and the concentration ratio between clopidogrel's active metabolite and clopidogrel is 48-fold lower in critically ill patients. Infection and CYP3A were the most cited perpetrator of inflammation and the most studied CYP, respectively. Moreover, some data suggest that resolution of inflammation results in a return to baseline CYP activities. Conclusion: Convincing evidence shows that inflammation is a major factor to be taken into account in drug development and in clinical practice to avoid any efficacy or safety issues because inflammation modulates CYP activities and thus drug pharmacokinetics. The impact is different depending on the CYP isoform and the inflammatory disease considered. Moreover, resolution of inflammation appears to result in a normalization of CYP activity. However, some results are still equivocal and further investigations are thus needed.

Published
2021

7. Pourquoi proposer la thérapie cognitivo-comportementale dans les douleurs chroniques ?

Author

Souche, Alain, Piguet, Valérie, Desmeules, Jules Alexandre, and Cedraschi, Christine

Subjects
ddc:616, Cognitive Behavioral Therapy, Chronic Pain/therapy, Psychotherapy, Group, Quality of Life, Humans, General Medicine
Abstract

Cognitive and behavioral techniques (CBT) are used in the approach of chronic pain, based on the assumption that pain and disability are not (only) influenced by somatic issues but also by psychosocial factors. CBT aim to improving quality of life while targeting disability. Psychoeducation, activity-centered and cognitive techniques are central, drawing on the identification of an activity that is not only important and meaningful for the patient but also realistic. This should allow the patient to overcome the impossibility to function « as before » while figuring out how to cope « as for now ». The ways to explore possible alternative options during the group therapy is presented and discussed.

Published
2019
Full Text
View/download PDF

10. Impact of Acute Inflammation on Cytochromes P450 Activity Assessed by the Geneva Cocktail

Author

Lenoir, Camille, primary, Daali, Youssef, additional, Rollason, Victoria, additional, Curtin, François, additional, Gloor, Yvonne, additional, Bosilkovska, Marija, additional, Walder, Bernhard, additional, Gabay, Cem, additional, Nissen, Michael John, additional, Desmeules, Jules Alexandre, additional, Hannouche, Didier, additional, and Samer, Caroline Flora, additional

Published
2021
Full Text
View/download PDF

12. Gestion de la douleur aiguë chez les patients sous traitements de substitution aux opioïdes

Author

Manguzzi, Elena, Wainstein, Laura, Desmeules, Jules Alexandre, and Broers, Barbara

Subjects
ddc:617, fungi, General Medicine
Abstract

Treatment of acute nociceptive pain in patients with opioid substitution therapy (OST) is an actual topic. The clinical features of this population, as pain sensibility, and the pharmacological features of OST, require an individualized care which must be adjusted to the patient's pain and the OST used. This article offers a summary of the main possible pharmacological strategies by highlighting the features of pain in these patients and removing the barriers to an effective management. Generally, the OST is kept and a multimodal analgesia is added according to the intensity of the pain. Multimodal analgesia includes non pharmacological measures, non opioid drugs and/or opioid drugs which must be chosen according to the OST. Collaboration between different health professionals provides an effective management of pain in order to protect this vulnerable population from the negative health consequences of an insufficiently relieved pain.

Published
2018
Full Text
View/download PDF

13. Gender Differences in Cardiovascular Pharmacotherapy-the Example of Hypertension: A Mini Review

Author

Kalibala, Jacklean, Pechere, Antoinette, and Desmeules, Jules Alexandre

Subjects
ddc:616, Pharmacology, Cardiovascular drugs, ddc:617, Hypertension, Gender, Sex, Pharmacokinetics, ddc:610
Abstract

Cardiovascular disease (CVD) is the leading cause of mortality worldwide in both sexes. Despite considerable progress in better understanding the patterns of disease in women, they are still often undertreated and benefit less from evidence-based treatment. Hypertension is a key contributor to CVD and is also one of the most potent risk factors for heart failure in women. Even with the wide variety of available drugs, blood pressure control is globally suboptimal. Current guidelines do not suggest differential treatment of hypertension for women; however, a growing body of research suggests gender dimorphism in the pathophysiology of hypertension and pharmacological response to cardiovascular drugs. The clinical relevance of theses sex-divergent effects of drugs is still under investigation. Owing to the exponential relationship between blood pressure and cardiovascular mortality, even a modest decrease in blood pressure or therapeutic adhesion could be clinically elevant. In this review, we explore the known pharmacological and pharmacokinetic sex differences with special attention to the main classes of antihypertensive treatment. Current data shows frequently higher drug exposures in women and more frequent adverse drug reactions in all antihypertensive drug groups. As far as cardiovascular prevention is concerned, sex-specific data is often lacking in clinical trials, highlighting the necessity to further study CVD and their treatment in both men and women.

Published
2020

14. Pain interventions in adults with intellectual disability: A scoping review and pharmacological considerations

Author

Lonchampt, Sophie, Gerber, Fabienne, Aubry, Jean-Michel, Desmeules, Jules Alexandre, Kosel, Markus Mathaus, and Besson, Marie

Subjects
ddc:616.89, ddc:617
Abstract

Having to deal on a daily routine with prescriptions in adults with intellectual disability (ID), we systematically reviewed the literature on the specificities of pain interventions in that population, focusing on medication and trying to gather practical information on appropriate pain treatments. Given the scarcity of the literature on the topic, we also discussed the pharmacological considerations to be taken into account when prescribing analgesic drugs in that vulnerable population.

Published
2020

15. Opioïdes chez les patients âgés: Faux-amis ?

Author

El Biali, Myriam, Desmeules, Jules Alexandre, and Besson, Marie

Subjects
ddc:617, Gériatrie, Opioïdes, Antalgie
Abstract

La mise en place d'une antalgie par opioïdes chez les patients âgés représente souvent un défi. Si les opioïdes peuvent conduire à des effets indésirables dangereux, surtout chez une population gériatrique vulnérable, un contrôle insuffisant des douleurs entraîne, quant à lui, une diminution parfois dramatique de l' état fonctionnel et de la qualité de vie des patients. Cet article propose de discuter ces enjeux et de revoir les principes pour une prescription plus sûre des opioïdes en gériatrie.

Published
2020

18. Prediction of cytochromes P450 3A and 2C19 modulation by both inflammation and drug interactions using physiologically based pharmacokinetics.

Author

Lenoir, Camille, Niederer, Amine, Rollason, Victoria, Desmeules, Jules Alexandre, Daali, Youssef, and Samer, Caroline Flora

Subjects
CYTOCHROMES, OMEPRAZOLE, DRUG interactions, BLOOD plasma, PHARMACOKINETICS, CYTOCHROME P-450 CYP3A, CYTOCHROME oxidase
Abstract

Xenobiotics can interact with cytochromes P450 (CYPs), resulting in drug–drug interactions, but CYPs can also contribute to drug–disease interactions, especially in the case of inflammation, which downregulates CYP activities through pretranscriptional and posttranscriptional mechanisms. Interleukin‐6 (IL‐6), a key proinflammatory cytokine, is mainly responsible for this effect. The aim of our study was to develop a physiologically based pharmacokinetic (PBPK) model to foresee the impact of elevated IL‐6 levels in combination with drug interactions with esomeprazole on CYP3A and CYP2C19. Data from a cohort of elective hip surgery patients whose CYP3A and CYP2C19 activities were measured before and after surgery were used to validate the accurate prediction of the developed models. Successive steps were to fit models for IL‐6, esomeprazole, and omeprazole and its metabolite from the literature and to validate them. The models for midazolam and its metabolite were obtained from the literature. When appropriate, a correction factor was applied to convert drug concentrations from whole blood to plasma. Mean ratios between simulated and observed areas under the curve for omeprazole/5‐hydroxy omeprazole, esomeprazole, and IL‐6 were 1.53, 1.06, and 0.69, respectively, indicating an accurate prediction of the developed models. The impact of IL‐6 and esomeprazole on the exposure to CYP3A and CYP2C19 probe substrates and respective metabolites were correctly predicted. Indeed, the ratio between predicted and observed mean concentrations were <2 for all observations (ranging from 0.51 to 1.7). The impact of IL‐6 and esomeprazole on CYP3A and CYP2C19 activities after a hip surgery were correctly predicted with the developed PBPK models. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

19. Safety issues of pharmacological acute pain treatment in children

Author

Rodieux, Frédérique, Piguet, Valérie, Desmeules, Jules Alexandre, and Samer, Caroline Flora

Subjects
ddc:615, ddc:617
Abstract

Acute nociceptive pain management in children is a major public health concern. Effective and safe pain treatment is essential, but safety data cannot be simply extrapolated from adults to children due to pharmacokinetic and pharmacodynamic specificities. In addition, the frequent absence of child-specific data, the difficulty to assess drug tolerability, and the infants' inability to communicate properly and voluntarily report adverse drug reactions make children more vulnerable to safety issues. Awareness of the possible toxicity of analgesics is important but should not lead to suboptimal dosing and underuse of analgesia. A better assessment and individualization of treatment should allow effective prescribing of analgesics in more secure conditions. This article aims to review the safety of acetaminophen, nonsteroidal anti-inflammatory drugs, and opioids in children and the precautions that should be taken.

Published
2019

22. Phase 1 Trials of rVSV Ebola Vaccine in Africa and Europe : Preliminary Report

Author

Agnandji, Selidji T, Csaki Huttner, Angela, Zinser, Madeleine E, Njuguna, Patricia, Dahlke, Christine, Fernandes, José F, Yerly, Sabine, Dayer, Julie-Anne, Kraehling, Verena, Kasonta, Rahel, Adegnika, Akim A, Altfeld, Marcus, Auderset, Floriane, Bache, Emmanuel B, Biedenkopf, Nadine, Borregaard, Saskia, Brosnahan, Jessica S, Burrow, Rebekah, Combescure, Christophe, Desmeules, Jules Alexandre, Eickmann, Markus, Fehling, Sarah K, Finckh, Axel, Goncalves Cabecinhas, Ana Rita, Grobusch, Martin P, Hooper, Jay, Jambrecina, Alen, Kabwende, Anita L, Kaya, Gurkan, Kimani, Domtila, Lell, Bertrand, Lemaître, Barbara, Lohse, Ansgar W, Massinga-Loembe, Marguerite, Matthey, Alain, Mordmüller, Benjamin, Nolting, Anne, Ogwang, Caroline, Ramharter, Michael, Schmidt-Chanasit, Jonas, Schmiedel, Stefan, Silvera, Peter, Stahl, Felix R, Staines, Henry M, Strecker, Thomas, Stubbe, Hans C, Tsofa, Benjamin, Zaki, Sherif, Fast, Patricia, Moorthy, Vasee, Kaiser, Laurent, Krishna, Sanjeev, Becker, Stephan, Kieny, Marie-Paule, Bejon, Philip, Kremsner, Peter G, Addo, Marylyn M, Siegrist, Claire-Anne, and VSV Ebola Consortium (VEBCON)

Subjects
ddc:616
Abstract

The replication-competent recombinant vesicular stomatitis virus (rVSV)–based vaccine expressing a Zaire ebolavirus (ZEBOV) glycoprotein was selected for rapid safety and immunogenicity testing before its use in West Africa.

Published
2016

23. Prescription d'antidépresseurs dans le traitement de la douleur : rôle de la pharmacogénétique

Author

Rodieux, Frédérique, Piguet, Valérie, Berney, Patricia Elisabeth, Desmeules, Jules Alexandre, and Besson, Marie

Subjects
ddc:615, ddc:617, Antidepressive Agents/pharmacokinetics/therapeutic use, Pharmacogenetics, Humans, Single Nucleotide, Pain/drug therapy/genetics, Polymorphism, Metabolic/genetics, Drug Prescriptions, Pain Management/methods, Inactivation
Abstract

Antidepressants, mainly tricyclic and non-selective reuptake inhibitors of serotonin antidepressants, are part of the treatment of chronic pain. The management is complicated by a large interindividual variability of efficacy and tolerance. Important part of this variability is associated with nucleotide polymorphisms of genes encoding enzymes involved in the pharmacokinetics and pharmacodynamics of these molecules. Identification of these genetic variants could to predict clinical consequences and allowed individualized adjustments in medication or dosage. This article presents the current knowledge on the influence of genetics on the efficacy and adverse effects of antidepressants used in chronic pain treatment.

Published
2015

24. Cannabinoïdes médicaux dans les douleurs chroniques : aspects pharmacologiques

Author

Ing Lorenzini, Kuntheavy, Broers, Barbara, Lalive d'Epinay, Patrice, Dayer, Pierre, Desmeules, Jules Alexandre, and Piguet, Valérie

Subjects
ddc:615, Cannabinoids/pharmacology/therapeutic use, Treatment Outcome, ddc:617, Humans, Drug Interactions, ddc:616.07, Chronic Pain/drug therapy, Medical Marijuana/pharmacology/therapeutic use, Switzerland, ddc:613
Abstract

In Switzerland, medical cannabinoids can be prescribed under compassionate use after special authorization in justified indications such as refractory pain. Evidence of efficacy in pain is limited and the clinical benefit seems to be modest. Their drug-drug interactions (DDI) profile is poorly documented. Cytochromes P450 (CYP) 2C9 and 3A4 are involved in the metabolism of tetrahydrocannabinol and cannabidiol, which implies possible DDI with CYP450 inhibitor and inducer, such as anticonvulsivants and HIV protease inhibitors, which may be prescribed in patients with neuropathic pain.

Published
2015

25. Quel programme informatique de détection des interactions médicamenteuses néfastes ?

Author

Ing Lorenzini, Kuntheavy, Reutemann, Barbara, Samer, Caroline Flora, Guignard, Bertrand, Bonnabry, Pascal, Dayer, Pierre, Perrier, Arnaud, and Desmeules, Jules Alexandre

Subjects
ddc:615, ddc:617, ddc:618.97, Drug Information Services, Humans, Drug Interactions, Software
Abstract

Adverse drug events (ADE) are a major public health issue, with drug-drug interactions (DDI) being one of well-recognized causes of ADE that could be preventable by the use of DDI screening software. We compared the ability of four programs to detect clinically important DDI. We tested 62 drug pairs with and 12 drug pairs without clinically important DDI. Lexi-Interact and Epocrates were the most sensitive (95%) compared to the Compendium and Theriaque (80 and 73%, respectively). The Compendium and Theriaque also showed the lowest negative predictive value. All programs showed high specificity and positive predictive value. The qualitative assessment showed the best performances for Compendium and Lexi-Interact. The last one seems to be the best screening program, but the Compendium is in French and is freely available.

Published
2012

26. Fracture atypique du fémur sous bisphosphonates, un effet indésirable à ne pas manquer

Author

Ing Lorenzini, Kuntheavy, Meier, Raphaël, Suva, Domizio, Dayer, Pierre, Desmeules, Jules Alexandre, and Peter, Robin

Subjects
Femoral Fractures/chemically induced/radiography, Diphosphonates/administration & dosage/adverse effects, ddc:617, Humans, Bone Density Conservation Agents/administration & dosage/adverse effects, Osteoporosis/drug therapy
Abstract

Atypical femur fractures represent a new disease entity associated with the use of oral bisphosphonates. This review summarizes the current understanding of this phenomenon. These fractures are usually transverse, affecting the proximal third of the femoral shaft. They occur after minor or no trauma, include a thickening of the lateral femoral cortex, a delayed consolidation time and prodromal symptoms. In this context, the risk/benefit ratio of bisphosphonates remains favorable if the indication is adequate. In case of fracture, indication to treatment should be reevaluated. Pain or discomfort in the thigh in a patient receiving bisphosphonate should lead to radiological investigations in order to detect the possible occurrence of a stress fracture.

Published
2012

27. Pharmacokinetic-pharmacodynamic modelling of opioids in healthy human volunteers. a minireview

Author

Ing Lorenzini, Kuntheavy, Daali, Youssef, Dayer, Pierre, and Desmeules, Jules Alexandre

Subjects
Analgesics, Opioid, Time Factors, ddc:617, Analgesics, Opioid/pharmacokinetics/pharmacology, Pain/drug therapy, Drug Design, Animals, Humans, Pain, Models, Biological, Half-Life, Pain Measurement
Abstract

Pain is characterized by its multi-dimensional nature, explaining in part why the pharmacokinetic/pharmacodynamic (PK/PD) relationships are not straightforward for analgesics. The first part of this MiniReview gives an overview of PK, PD and PK/PD models, as well as of population approach used in analgesic studies. The second part updates the state-of-the-art in the PK/PD relationship of opioids, focusing on data obtained on experimental human pain models, a useful tool to characterize the PD of analgesics. For the so-called weak opioids such as codeine, experimental human studies showed that analgesia relies mainly upon biotransformation into morphine. However, the time-course of plasma concentrations of morphine did not always reflect the time-course of effects, the major site of action being the central nervous system. For tramadol, a correlation has been observed between the analgesic response and the PK of the (+)R-O-demethyl-tramadol metabolite. For 'stronger' opioids such as oxycodone, studies assessing the PK/PD of oxycodone suggested that active metabolite oxymorphone also strongly contributes to the analgesia and that analgesia may also be partially related through an action to peripherally located κ-opioid receptors. Different models have been proposed to describe the time-course of buprenorphine. An effect-compartment model was adopted to describe the PK/PD of morphine and its active metabolite, morphine-6-glucuronide (M6G). A longer blood-effect site equilibration half-life t(1/2) k(e0) was observed for M6G, suggesting a longer onset of action. The studies assessing the PK/PD of fentanyl and its derivatives showed a short t(1/2) k(e0) for analgesia, between 0.2 and 9 min., reflecting a short onset of effect. In conclusion, depending on the speed of transfer between the plasma and the effect site as well as the participation of active metabolites, the time-course of the analgesic effects can be close to the plasma concentrations (alfentanil and derivates) or observed with a prolonged delay (codeine, buprenorphine, morphine). These PK/PD data can be used to better characterize the differences between opioids, and partly explain the important observed variability among opioids in experimental conditions and should be systematically evaluated during drug development to better predict their selection in specific clinical conditions.

Published
2011

28. A randomized, controlled trial validates a peripheral supra-additive antihyperalgesic effect of a paracetamol-ketorolac combination

Author

Ing Lorenzini, Kuntheavy, Besson, Marie, Daali, Youssef, Salomon, Denis, Dayer, Pierre, and Desmeules, Jules Alexandre

Subjects
Adult, Male, Antipyretics, Pain, Gas Chromatography-Mass Spectrometry, Ketorolac/administration & dosage/pharmacokinetics, Young Adult, Double-Blind Method, Acetaminophen/administration & dosage/pharmacokinetics, Pain/drug therapy, Inflammation/drug therapy, Humans, Radiodermatitis/drug therapy/pathology, Acetaminophen, ddc:616, Inflammation, Hyperalgesia/drug therapy, Analgesics, Cross-Over Studies, ddc:617, digestive, oral, and skin physiology, Anti-Inflammatory Agents, Non-Steroidal, Middle Aged, Analgesics/administration & dosage, Drug Combinations, Antipyretics/administration & dosage/pharmacokinetics, Hyperalgesia, Anti-Inflammatory Agents, Non-Steroidal/therapeutic use, Radiodermatitis, Ketorolac
Abstract

The combination of paracetamol with non-steroidal anti-inflammatory drugs (NSAIDs) is widely used; however, the nature and mechanism of their interaction are still debated. A double-blind, pharmacokinetic/pharmacodynamic, randomized, cross-over, placebo-controlled study was carried out in human healthy volunteers. The aim was to explore the existence of a positive interaction between paracetamol 1 g and ketorolac 20 mg administered intravenously on experimental pain models in human beings. The effects of the paracetamol-ketotolac combination were compared with similar doses of respective single analgesic and to placebo on the sunburn model (UVB-induced inflammation), cold pain tolerance and the nociceptive flexion reflex. The kinetics of the plasma concentrations of paracetamol and ketorolac were measured using 2D-liquid chromatography-mass spectrometry. Thirteen volunteers were screened, and 11 completed the study. Ketorolac significantly decreased primary hyperalgesia to heat stimuli compared with paracetamol (p < 0.014). The combination performed better than paracetamol (p < 0.001) and placebo (p < 0.042), increasing heat pain threshold by 1.5°C. The combination radically reduced primary hyperalgesia to mechanical stimulation (39%) compared with placebo (p < 0.002) and single agents (paracetamol p < 0.024 and ketorolac p < 0.032). The combination also reduced, slightly although significantly, the intensity of pain (10%) for the cold pressor test (versus placebo: p < 0.012, paracetamol: p < 0.019 and ketorolac p < 0.004). None of the treatments significantly affected the central models of pain at this dosage level. No pharmacokinetic interactions were observed. These results suggest a supra-additive pharmacodynamic interaction between paracetamol and ketorolac in an inflammatory pain model. The mechanism of this interaction could mainly rely on a peripheral contribution of paracetamol to the effect of NSAIDs.

Published
2011

29. Effet placebo analgésique : apport des neurosciences

Author

Berna, Chantal Simone, Cojan, Yann, Vuilleumier, Patrik, and Desmeules, Jules Alexandre

Subjects
ddc:617, Endorphins/pharmacology, Osteoarthritis, Knee/complications, Neurosciences, Analgesia/psychology, Placebo Effect, ddc:616.8, Treatment Outcome, Naloxone/therapeutic use, Chronic Disease, Pain/drug therapy/etiology, Humans, Narcotic Antagonists/therapeutic use, Female, Prefrontal Cortex/drug effects, Placebos/therapeutic use, Dopamine/pharmacology, Aged
Abstract

Over the past twenty years, neuroscience has changed our understanding of placebo analgesia. Often perceived by researchers as a response bias adding noise to the assessment of efficacy, in the patients' view, it is associated with charlatanism. The origin of the word, qualifying a patient's response to "please" the doctor, did not help its rightful appreciation. However, today the placebo analgesia is considered as a psychobiological phenomenon. Thanks to pharmacological manipulations and the development of functional brain imaging, the neural circuitry involved in this effect as well as the role of endorphins and dopamine have been identified. This article describes our current knowledge about this fascinating phenomenon: a psychological modulation can lead to a biological effect.

Published
2011

30. Le placebo, un allié mésestimé

Author

Cedraschi, Christine, Allaz, Anne-Françoise, Piguet, Valérie, and Desmeules, Jules Alexandre

Subjects
ddc:618.97
Abstract

Le point de vue des patients – en particulier leurs représentations de ce qui leur arrive et leurs attentes par rapport au traitement – ainsi que l'importance d'indicateurs de réussite du traitement centrés sur le patient sont largement reconnus. L'influence des attentes sur les résultats du traitement fait l'objet de beaucoup d'attention. Les attentes constituent l'un des principaux mécanismes de l'effet placebo qu'elles modulent et auquel elles peuvent servir d'intermédiaire. La chirurgie soulève ici des questions intéressantes dans la mesure où le processus chirurgical, qui nécessite une hospitalisation, s'accompagne d'éléments tels qu'un cérémonial lié à la préparation de l'acte chirurgical, le recours à des techniques sophistiquées, mais aussi une reconnaissance de l'atteinte corporelle du fait de la nécessité d'une opération.

Published
2011

32. The effects of CYP2D6 and CYP3A activities on the pharmacokinetics of immediate release oxycodone

Author

Samer, Caroline Flora, Daali, Youssef, Wagner, M., Hopfgartner, Gerard, Eap, Chin Bin, Rebsamen, M. C., Rossier, Michel, Hochstrasser, Denis, Dayer, P., and Desmeules, Jules Alexandre

Subjects
Adult, Male, Genotype, Ketoconazole/pharmacology, Receptors, Opioid, mu, Polymorphism, Genetic, digestive system, Young Adult, Double-Blind Method, Cytochrome P-450 CYP2D6 Inhibitors, Cytochrome P-450 CYP3A, Humans, Drug Interactions, ddc:610, ddc:576, Enzyme Inhibitors, ddc:616, Enzyme Inhibitors/pharmacology, ddc:615, Drug Interactions/genetics, Cross-Over Studies, ddc:617, Cytochrome P-450 CYP3A/antagonists & inhibitors/*metabolism, Cytochrome P-450 CYP2D6/antagonists & inhibitors/*genetics/*metabolism, Metabolic Detoxication, Phase I/genetics, Oxycodone/administration & dosage/blood/chemistry/*pharmacokinetics, Receptors, Opioid, mu/metabolism, Quinidine, Research Papers, Analgesics, Opioid, Ketoconazole, Phenotype, Analgesics, Opioid/administration & dosage/blood/chemistry/*pharmacokinetics, Quinidine/pharmacology, Cytochrome P-450 CYP2D6, Cytochrome P-450 CYP3A Inhibitors, Metabolic Detoxication, Phase I, Oxycodone
Abstract

BACKGROUND AND PURPOSE: There is high interindividual variability in the activity of drug-metabolizing enzymes catalysing the oxidation of oxycodone [cytochrome P450 (CYP) 2D6 and 3A], due to genetic polymorphisms and/or drug-drug interactions. The effects of CYP2D6 and/or CYP3A activity modulation on the pharmacokinetics of oxycodone remains poorly explored. EXPERIMENTAL APPROACH: A randomized crossover double-blind placebo-controlled study was performed with 10 healthy volunteers genotyped for CYP2D6 [six extensive (EM), two deficient (PM/IM) and two ultrarapid metabolizers (UM)]. The volunteers randomly received on five different occasions: oxycodone 0.2 mg x kg(-1) and placebo; oxycodone and quinidine (CYP2D6 inhibitor); oxycodone and ketoconazole (CYP3A inhibitor); oxycodone and quinidine+ketoconazole; placebo. Blood samples for plasma concentrations of oxycodone and metabolites (oxymorphone, noroxycodone and noroxymorphone) were collected for 24 h after dosing. Phenotyping for CYP2D6 (with dextromethorphan) and CYP3A (with midazolam) were assessed at each session. KEY RESULTS: CYP2D6 activity was correlated with oxymorphone and noroxymorphone AUCs and C(max) (-0.71 < Spearman correlation coefficient rhos < -0.92). Oxymorphone C(max) was 62% and 75% lower in PM than EM and UM. Noroxymorphone C(max) reduction was even more pronounced (90%). In UM, oxymorphone and noroxymorphone concentrations increased whereas noroxycodone exposure was halved. Blocking CYP2D6 (with quinidine) reduced oxymorphone and noroxymorphone C(max) by 40% and 80%, and increased noroxycodone AUC(infinity) by 70%. Blocking CYP3A4 (with ketoconazole) tripled oxymorphone AUC(infinity) and reduced noroxycodone and noroxymorphone AUCs by 80%. Shunting to CYP2D6 pathway was observed after CYP3A4 inhibition. CONCLUSIONS AND IMPLICATIONS: Drug-drug interactions via CYP2D6 and CYP3A affected oxycodone pharmacokinetics and its magnitude depended on CYP2D6 genotype.

Published
2010

33. Impact of genetic polymorphisms and drug-drug interactions on clopidogrel and prasugrel response variability

Author

Ancrenaz, Virginie, Daali, Youssef, Fontana, Pierre, Besson, M., Samer, Caroline Flora, Dayer, P., and Desmeules, Jules Alexandre

Subjects
ddc:616, Polymorphism, Genetic, ddc:617, Biological Availability, Cytochrome P-450 Enzyme System/genetics/metabolism, Platelet Aggregation Inhibitors/pharmacokinetics/*pharmacology, Piperazines/pharmacokinetics/*pharmacology, Thiophenes/pharmacokinetics/*pharmacology, Purinergic P2Y Receptor Antagonists/pharmacology, Animals, Humans, Drug Interactions, cardiovascular diseases, ddc:610, Ticlopidine/*analogs & derivatives/pharmacokinetics/pharmacology, circulatory and respiratory physiology
Abstract

Thienopyridine antiaggregating platelet agents (clopidogrel and prasugrel) act as irreversible P2Y12 receptor inhibitors. They are used with aspirin to prevent thrombotic complications after an acute coronary syndrome or percutaneous coronary intervention. A large interindividual variability in response to clopidogrel and to a lesser extent to prasugrel is observed and may be related to their metabolism. Clopidogrel and prasugrel are indeed prodrugs converted into their respective active metabolites by several cytochromes P450 (CYPs). Besides clopidogrel inactivation (85%) by esterases to the carboxylic acid, clopidogrel is metabolized by CYPs to 2-oxo-clopidogrel (15%) and further metabolized to an unstable but potent platelet-aggregating inhibitor. Prasugrel is more potent than clopidogrel with a better bioavailability and lower pharmacodynamic variability. Prasugrel is completely converted by esterases to an intermediate oxo-metabolite (R-95913) further bioactivated by CYPs. Numerous clinical studies have shown the influence of CYP2C19 polymorphism on clopidogrel antiplatelet activity. Moreover, unwanted drug-drug pharmacokinetic interactions influencing CYP2C19 activity and clopidogrel bioactivation such as with proton pump inhibitors remain a matter of intense controversy. Several studies have also demonstrated that CYP3A4/5 and CYP1A2 are important in clopidogrel bioactivation and should also be considered as potential targets for unwanted drug-drug interactions. Prasugrel bioactivation is mainly related to CYP3A4 and 2B6 activity and therefore the question of the effect of drug-drug interaction on its activity is open. The purpose of this review is to critically examine the current literature evaluating the influence of genetic and environmental factors such as unwanted drug-drug interaction affecting clopidogrel and prasugrel antiplatelet activity.

Published
2010

34. Modulation cognitive et émotionnelle de la douleur: mécanismes de certaines approches cliniques révélés par les neurosciences

Author

Berna, Chantal Simone and Desmeules, Jules Alexandre

Subjects
genetic structures, ddc:617, Affect/physiology, Humans, Perception/physiology, Pain/physiopathology, sense organs, Brain/physiology, Cognition/physiology
Abstract

Cognitive and affective strategies are frequently used in clinical practice to modulate pain perception. They seem to rely on a descending neural system, which is able to inhibit the afferent nociceptive signal. Herein, we will review experiments on healthy volunteers, which explored the central mechanisms involved in the change in pain perception due to the modulation of attention, expectations or mood. A growing understanding of the cognitive and emotional modulation of pain perception has validated empirical practices in the acute pain context. This body of work, associated to the investigation of the dysfunction of this modualtion in chronic pain patients, could lead to developing new therapies, which would complement current treatments.

Published
2009

35. Two-dimensional liquid chromatography-ion trap mass spectrometry for the simultaneous determination of ketorolac enantiomers and paracetamol in human plasma: application to a pharmacokinetic study

Author

Ing Lorenzini, Kuntheavy, Desmeules, Jules Alexandre, Besson, Marie, Veuthey, Jean-Luc, Dayer, Pierre, and Daali, Youssef

Subjects
ddc:616, ddc:615, Two-dimensional liquid chromatography, Spectrometry, Mass, Electrospray Ionization, ddc:617, Stereoisomerism, Analgesics, Non-Narcotic, Chiral separation, Paracetamol, Humans, Pharmacokinetics, Ketorolac, Acetaminophen, Chromatography, Liquid
Abstract

A bioanalytical method was developed for the simultaneous determination of paracetamol and ketorolac enantiomers in human plasma using two-dimensional liquid chromatography-mass spectrometry. Separation was first achieved in a reversed-phase C18 column by using a gradient solvent system consisting of 0.1% aqueous formic acid and acetonitrile (ACN). The effluent between 8.9 and 9.9 min, corresponding to phenacetin and racemic ketorolac peaks, was transferred to a polysaccharide-based chiral column (ChiralPak AD-RH) by using a six-port switching valve. Ketorolac enantiomers were subsequently separated on the chiral column using an isocratic mobile phase composed of ACN/0.1% formic acid 50:50 (v/v). The total run-time was less than 18 min. This innovative strategy prolongs the lifetime of chiral columns by avoiding damages due to the sample matrix. The detection was carried out with an ion trap mass spectrometer equipped with an electrospray ionisation source. The tested ranges were 0.05-20 microg/ml for paracetamol and 0.005-2 microg/ml for each ketorolac enantiomer. This method was fully validated and showed good performances in terms of trueness (80-110%) and precision (6.7-13.2%). The mean extraction recoveries were 60%, 72% and 76% for paracetamol, R-ketorolac and S-ketorolac, respectively. Finally, this procedure was successfully applied to a pharmacokinetic study.

Published
2008

36. La prescription « off-label »

Author

Blondon, Katherine, Desmeules, Jules Alexandre, Vogt-Ferrier, Nicole Barbara, Besson, Marie, Kondo-Oestreicher, Mitsuko, and Dayer, Pierre

Subjects
Health Knowledge, Attitudes, Practice, Informed Consent, ddc:617, Humans, Safety, Drug Prescriptions, Physician's Practice Patterns/ethics/legislation & jurisprudence, Switzerland, Drug Labeling
Abstract

Prescribing a medication for a condition not described in the label approved by national regulatory bodies (in Switzerland, Swissmedic) is called "off-label" prescribing. Unlicensed drug use is common in all fields of medicine and may be encountered in therapeutic guidelines. The term does not imply improper nor illegal use, and may provide the only available treatment for "orphan" conditions, or for certain populations (children, pregnant women, very old patients). Off-label drug use should be based on sound scientific evidence of efficacy and safety. In Switzerland, patients need to be informed that health insurance coverage is not guaranteed with off-label use. The prescribing physician bears the responsibility of off-label use with the possibility of unanticipated risks, and should therefore be prepared for possible malpractice suits.

Published
2008

37. Les toxidermies médicamenteuses

Author

Thielen Klee, Anne-Marie, Toutous Trellu, Laurence Marie, and Desmeules, Jules Alexandre

Subjects
Skin Diseases/chemically induced, ddc:617, Drug-Related Side Effects and Adverse Reactions, Drug Eruptions/diagnosis/etiology, Product Surveillance, Postmarketing, Adverse Drug Reaction Reporting Systems, Humans, Drug Monitoring
Abstract

Drug-eruptions are common adverse events that may be potentially severe. This review focuses on the principal clinical presentations of drug-eruptions, the identification procedure of the causal drug and the best ways of notifying serious or unexpected adverse events (pharmaco-vigilance) in order to identify the high-risk therapeutic classes.

Published
2008

38. Prise en charge médicamenteuse de la douleur neuropathique : quelle place pour les traitements topiques?

Author

Besson, Marie, Desmeules, Jules Alexandre, and Piguet, Valérie

Subjects
ddc:617, Nervous System Diseases/complications, Administration, Topical, Anesthetics, Local/administration & dosage, Pain/drug therapy/etiology, Humans, Analgesia, Lidocaine/administration & dosage, Analgesics/administration & dosage
Abstract

Neuropathic pain is challenging to treat, partly because of the systemic side effects of the commonly used medications. Therefore topical analgesics are potentially very usefull. Lidocain, capsaicin, amitriptyline and ketamine have been used topically on a pathophysiological basis and because of their favourable safety profile. Application of lidocain 5%, capsaicin 0.025-0.075% and doxepin 3.3% is effective, although moderately in peripheric neuropathic pain with allodynia and should be considered as a therapeutic option. However, this option should be evaluated on an individual basis. The efficacy of topical amitriptyline and ketamine is not demonstrated.

Published
2008

39. Pharmacogenetics of analgesics: toward the individualization of prescription

Author

Rollason, Victoria, Samer, Caroline Flora, Piguet, Valérie, Dayer, Pierre, and Desmeules, Jules Alexandre

Subjects
ddc:615, Carrier Proteins/genetics, Metabolic Detoxication, Drug/genetics, ddc:617, Cytochrome P-450 Enzyme System/genetics, Genetic Variation, Humans, Drug Prescriptions/standards, Pharmacogenetics, Analgesics/pharmacokinetics/pharmacology/therapeutic use
Abstract

The use of analgesics is based on the empiric administration of a given drug with clinical monitoring for efficacy and toxicity. However, individual responses to drugs are influenced by a combination of pharmacokinetic and pharmacodynamic factors that can sometimes be regulated by genetic factors. Whereas polymorphic drug-metabolizing enzymes and drug transporters may affect the pharmacokinetics of drugs, polymorphic drug targets and disease-related pathways may influence the pharmacodynamic action of drugs. After a usual dose, variations in drug toxicity and inefficacy can be observed depending on the polymorphism, the analgesic considered and the presence or absence of active metabolites. For opioids, the most studied being morphine, mutations in the ABCB1 gene, coding for P-glycoprotein (P-gp), and in the micro-opioid receptor reduce morphine potency. Cytochrome P450 (CYP) 2D6 mutations influence the analgesic effect of codeine and tramadol, and polymorphism of CYP2C9 is potentially linked to an increase in nonsteroidal anti-inflammatory drug-induced adverse events. Furthermore, drug interactions can mimic genetic deficiency and contribute to the variability in response to analgesics. This review summarizes the available data on the pharmacokinetic and pharmacodynamic consequences of known polymorphisms of drug-metabolizing enzymes, drug transporters, drug targets and other nonopioid biological systems on central and peripheral analgesics.

Published
2008

40. Automédication chez les sans-papiers latino-américains : entre le nécessaire et l'inapproprié

Author

Besson, Marie, Desmeules, Jules Alexandre, Wolff, Hans, and Gaspoz, Jean-Michel

Subjects
Transients and Migrants, ddc:617, Self Medication/statistics & numerical data, Emigrants and Immigrants, Humans, Hispanic Americans, Switzerland, ddc:613, Latin America/ethnology
Abstract

Self-medication is well known risk in Latin America. This situation can partly be explain by the difficult access to doctors and poorly regulated drug sales. Illegal Latino-American immigrants import their practice of self-medication and their drugs with them. The economic advantage of this practice makes it popular and confronts medical practitioners to question the benefice/risk of such behavior. Taking the particular situation of illegal Latino-American immigrants, this review discusses the necessity of abording systematically the question of self-medication during a medical consultation.

Published
2007

42. Entre sel et gènes ou pharmacogénomique des antihypertenseurs

Author

Ernandez, Thomas, Pechere, Antoinette, Dayer, Pierre, and Desmeules, Jules Alexandre

Subjects
ddc:616, Polymorphism, Genetic, Sodium/metabolism, ddc:617, Antihypertensive Agents/pharmacology/therapeutic use, Humans, Genomics, Blood Pressure/drug effects, Hypertension/drug therapy/genetics/metabolism
Abstract

Pharmacogenomics studies the links between polymorphisms (genetic variants) and the variability of the response to some treatments in a given individual. Pharmacogenomics thus allows to explore polymorphisms that could potentially explain heterogeneous efficacy of diuretics, ACE inhibitors or angiotensin receptor blockers, beta-blockers and calcium channel blockers among populations of varied ethnical origin. There have been many studies on the relation between the efficacy of these treatments and the specific polymorphisms involved in the regulation of blood pressure. So far, no unique mutation is by itself predictive of the therapeutic response to these drugs; more elaborated polygenetic models are required so that pharmacogenomics can one day offer an individualized prescription for a complicated disease such as high blood pressure.

Published
2006

44. Le traitement de l'hypertension artérielle : un défi pour le praticien

Author

Seboe, Paul, Pechere, Antoinette, Desmeules, Jules Alexandre, and Dayer, Pierre

Subjects
ddc:616, Antihypertensive Agents/therapeutic use, ddc:617, Hypertension/drug therapy, Humans, ddc:613
Abstract

Hypertension is associated with a greater risk of developing a stroke or a coronary heart disease, but remains, for the meanwhile, undertreated in a vast majority of patients. Non pharmacological interventions can reduce blood pressure and should be recommended to every patient suffering from hypertension. Nevertheless, a drug therapy must often be introduced. The threshold at which a treatment should be started depends mostly on the cardiovascular risk of each patient and the benefit of antihypertensive drug therapy depends primarily on the reduction of the blood pressure itself.

Published
2005

45. Polymorphisme génétique et interactions médicamenteuses: leur importance dans le traitement de la douleur

Author

Samer, Caroline Flora, Piguet, Valérie, Dayer, Pierre, and Desmeules, Jules Alexandre

Subjects
Drug Interactions/genetics, Cytochrome P-450 Enzyme System/metabolism, Phenotype, Polymorphism, Genetic, ddc:617, Anti-Inflammatory Agents, Non-Steroidal/metabolism, Cytochrome P-450 CYP2D6/metabolism, Pain/drug therapy, Animals, Cytochrome P-450 CYP3A, Humans, Analgesics/metabolism/pharmacology/therapeutic use
Abstract

To evaluate the impact of certain genetic polymorphisms on variable responses to analgesics

Published
2005

46. Sélection d'un médicament dans une classe thérapeutique donnée : l'exemple des «inhibiteurs de l'HMG-CoA réductase»

Author

Girardin, François, Desmeules, Jules Alexandre, and Dayer, Pierre

Subjects
ddc:616, Hydroxymethylglutaryl-CoA Reductase Inhibitors/adverse effects/therapeutic use, Humans
Abstract

The HMG-CoA reductase inhibitors have similar therapeutic targets and indications. However, their potential pharmacokinetic drug-drug interaction profile may play a significant role in their safety profile in polymedicated and polymorbid patients and can serve as a selection criterion. If their utility is clearly demonstrated in selected conditions, their safety profile remains of concern. Beside dose-related hepatic and muscular injury, other rare and important adverse drug reactions have been reported after prolonged administration such as polyneuropathy, fibrotic interstitial pulmonary disease and lupus-like syndrome. Teratogenicity has also been associated with statin therapy.

Published
2005

47. P-glycoprotein: a clue to vitamin K antagonist stabilization

Author

Gschwind, Liliane, primary, Rollason, Victoria, additional, Boehlen, Françoise, additional, Rebsamen, Michela, additional, Combescure, Christophe, additional, Matthey, Alain, additional, Bonnabry, Pascal, additional, Dayer, Pierre, additional, and Desmeules, Jules Alexandre, additional

Published
2015
Full Text
View/download PDF

48. Influence du cycle mentruel sur le seuil de la douleur expérimentale

Author

Besson, M., Piguet, Valérie, Desmeules, Jules Alexandre, Kondo Ostreicher, Mitsuko, Grandjean, R., Herrmann, François, and Dayer, P.

Subjects
ddc:617, ddc:618.97, ddc:613
Abstract

Objectif: évaluer l'impact du cycle menstruel sur le seuil de la douleur en réponse a un stimulus électrique chez 23 volontaires sains de sexe féminin avec et sans contraception orale. Méthode: nous avons suivi et comparé l'évolution longitudinale (3x/semaine durant un cycle menstruel complet) du réflexe nociceptif RIII, et du seuil subjectif de la douleur chez 23 volontaires, 13 avec et 10 sans contraception orale. Résultats: les volontaires sans contraception orale tendent a avoir des seuils nociceptif moyens plus bas que les volontaires sous contraception orale lors des phases menstruelle, folliculaire et lutéale. Lors de l'ovulation, cette différence s'accentue encore et devient significative (32.53 [41.03-24.04] vs 25,99 [33.97-18.02] mAmp, p = 0.04). Les données de l'évaluation subjective évoluent dans le même sens, sans être toutefois statistiquement significatives et sans nadir pendant l'ovulation. Conclusions: A l'instar des travaux expérimentaux parus sur la question, notre étude conforte l'idée d'un impact du cycle menstruel sur le seuil de la douleur. Bien qu'incomplète cette étude soulève le voile d'une influence des variations hormonales d'une part sur la transmission du message nociceptif au niveau central et d'autre part sur son intégration subjective qui pourrait être dissociée.

Published
2004

49. Clinical pharmacology and rationale of analgesic combinations

Author

Desmeules, Jules Alexandre, Rollason, Victoria, Piguet, Valérie, and Dayer, Pierre

Subjects
Analgesics, Drug Combinations, ddc:617, fungi, Pharmacology, Clinical, food and beverages, Analgesics/pharmacology, Humans, Pain, Pain/prevention & control
Abstract

Oral fixed drug combination analgesics have potential advantages over monotherapy, but these can only be attained through careful design.The main reasons for developing combination analgesics are to gain efficacy and to reduce toxicity. Analgesic combinations interact pharmacokinetically, or pharmacodynamically, or both, in positive or negative terms. The t(max) value for both enantiomers of tramadol occur two hours following administration, and that for the active, (+)-M1 metabolite occurs after three hours. Thus, pairing tramadol with acetaminophen, a rapid-onset analgesic, represents a pharmacokinetically rational combination. Analgesic combinations should satisfy two important pharmacodynamic criteria: the components of the combination should display additive or synergistic analgesia; and this interaction should allow lower doses of each substance to be used in combination, resulting in an improved safety profile. Clinical studies of the pharmacodynamic between oral tramadol and acetaminophen in third molar extraction and cold pressor models have provided evidence that this combination provides better efficacy than either individual component of the combination.In summary, combination analgesics can play a valuable role in pain management. However, dubious combinations (directed against the same targets or with unwanted interactions) and 'old fashioned' fixed-dose multiple analgesic agent combinations should be avoided. Fixed-dose combination analgesics are of value only when they have been developed according to rational pharmacokinetic and pharmacodynamic criteria, and when claims for their benefits have been supported by evidence-based data and well-designed clinical studies.

Published
2003

50. Effet analgesique des opiaces en usage cutane: quelle est leur efficacite?

Author

Rollason, Victoria, Desmeules, Jules Alexandre, and Vogt-Ferrier, Nicole Barbara

Subjects
ddc:615, ddc:617, Analgesics, Opioid/administration & dosage/therapeutic use, Pain/drug therapy, Administration, Topical, Animals, Humans
Abstract

Recent research has revealed the presence of opioid receptors in inflamed peripheral tissues. This gives rise to the possibility of treating the pain caused by wounds with the advantage of reducing the secondary effects related to the use of opioids and at the same time rendering their use more efficacious. The theory of a peripheral analgesic action of opioids has been tested in a variety of situations, in particular in brachial plexus blocks and intra-articular injections. In addition, the analgesic effect of opioids has been tested by cutaneous application for various conditions but on only a limited number of patients. On the basis of these case reports, we cannot conclude that the peripheral use of opioids is efficacious and the topical use of opioids cannot be recommended unless done within the framework of a controlled clinical trial.

Published
2001

Catalog

Books, media, physical & digital resources
See catalog results